Next Article in Journal
Bactericidal Effect of Different Photochemical-Based Therapy Options on Implant Surfaces—An In Vitro Study
Previous Article in Journal
The Relationship between Selective Digestive Decontamination and Nosocomial Infections in Patients Receiving Continuous Renal Replacement Therapy in ICUs: A Multicenter Study
 
 
Search for Articles:
Title / Keyword
Author / Affiliation / Email
Journal
Article Type
 
 
Advanced Search
 
Section
Special Issue
Volume
Issue
Number
Page
 
Journals
JCM
Volume 13
Issue 14
10.3390/jcm13144213
jcm-logo
Submit to this Journal Review for this Journal Propose a Special Issue
Article Menu

Article Menu

share Share announcement Help format_quote Cite question_answer Discuss in SciProfiles thumb_up
...
Endorse textsms
...
Comment
first_page
settings
Order Article Reprints
Font Type:
Arial Georgia Verdana
Font Size:
Aa Aa Aa
Line Spacing:
Column Width:
Background:
Systematic Review

Management of Malignant Bowel Obstruction in Patients with Gynaecological Cancer: A Systematic Review

by
Richárd Tóth
1,
Zsófia Tóth
1,
Lotti Lőczi
1,2,
Marianna Török
1,2,
Nándor Ács
1,
Szabolcs Várbíró
1,2,3,
Márton Keszthelyi
1,*,† and
Balázs Lintner
1,†
1
Department of Obstetrics and Gynaecology, Semmelweis University, 1082 Budapest, Hungary
2
Workgroup of Research Management, Doctoral School, Semmelweis University, 1085 Budapest, Hungary
3
Department of Obstetrics and Gynaecology, University of Szeged, 6725 Szeged, Hungary
*
Author to whom correspondence should be addressed.
These authors contributed equally to this work.
J. Clin. Med. 2024, 13(14), 4213; https://doi.org/10.3390/jcm13144213
Submission received: 16 June 2024 / Revised: 6 July 2024 / Accepted: 17 July 2024 / Published: 19 July 2024
(This article belongs to the Special Issue Laparoscopy and Surgery in Gynecologic Oncology)
Browse Figures
Versions Notes

Abstract

:
Objectives: This systematic review aimed to evaluate current surgical and non-surgical management strategies for malignant bowel obstruction (MBO) in patients with gynaecological cancer. Methods: Comprehensive literature searches were conducted across MEDLINE, Embase, CENTRAL, and Scopus, without restrictions on language or publication date. Following the removal of duplicates, 4866 articles were screened, with 34 meeting the inclusion criteria. Results: Surgical intervention remains the definitive treatment for MBO, offering longer symptom-free periods and improved survival, particularly when conservative methods fail. However, the selection of surgical candidates is crucial due to the high risk of morbidity and the potential for significant complications. Non-surgical treatments, such as the use of Gastrografin, Octreotide, and Dexamethasone, along with invasive procedures like nasogastric tubing, percutaneous gastrostomy, and stent placement, offer varying degrees of symptom relief and are often considered when surgery is not feasible. Conclusions: In this article we provide a potential therapeutic algorithm for the management of patients with MBO. This review underscores the urgent need for high-quality research to develop clear, evidence-based guidelines for MBO management in patients with gynaecologic cancer. Establishing standardised protocols will improve patient outcomes by aiding clinicians in making informed, individualised treatment decisions.

1. Introduction

Gynaecological malignancies were responsible for 680,000 deaths globally in 2022, with incidence rates continuing to rise. According to WHO calculations, mortality from these types of cancers is predicted to reach 1.1 million cases per year by 2040 [1]. Although various preventive measures and advancements in targeted therapies [2] have extended survival rates, clinicians are frequently confronted with complex decisions regarding palliative care. While administering antitumor therapy or performing surgeries are guided by well-established protocols, palliative care decisions often rely on individualised clinical judgement due to the lack of robust evidence [3].
A particular area of focus is on the management of malignant bowel obstructions (MBOs). Malignant bowel obstruction is a clinical syndrome that is caused by malignant disease, antitumoral treatment, or its complications, and once it occurs it tends to recur. For this reason, some authors entitle it an occlusive state rather than a single event [4].
Studies indicate that MBO occurs in 25–60% of patients with gynaecological cancers [5,6]. The consequences of occlusion evoke severe symptoms, significantly damage the quality of life of the patients, and can be life-threatening.

1.1. Pathomechanism of Malignant Bowel Obstruction

Bowel obstructions can be categorised into mechanical and functional types, each requiring different management strategies. Mechanical obstructions, which include intraluminal causes like faecal impaction or intraluminal tumour growth and extraluminal causes like tumours or adhesions, physically block the intestines. Functional obstructions, such as paralytic ileus or pseudo-obstruction, involve impaired intestinal motility without a physical blockage. Additionally, obstructions can be partial or complete and may occur in the small or large bowel, with each presenting distinct symptoms and clinical challenges. Accurate differentiation of these types is crucial for effective treatment and improving patient outcomes.
Bowel occlusions typically develop gradually, though symptoms can appear suddenly, and the causes are often multifactorial [7].
Mechanically, bowel occlusion can result from infiltration of the bowel or mesentery by a tumour or from a bulky tumour exerting external pressure on the bowel [8]. In colorectal cancer, the primary cause of occlusion is intraluminal tumour growth [9]. Conversely, intraluminal occlusion is less common in gynaecologic tumours.
Functional bowel obstruction, such as adynamic ileus, represents another mechanism of transit disorder contributing to bowel occlusion [10]. These disorders can arise from infiltration of the muscular layer, nerves of the bowel, or the celiac plexus, leading to decreased motility. These can be exacerbated by the side effects of chemotherapy or pain medications. Although it is rare in gynaecologic cancer patients, paraneoplastic syndrome can also contribute to functional obstructions. Furthermore, intra-abdominal adhesions, which may form after surgery, chemotherapy, or radiotherapy, play a significant role in the development of bowel occlusions [11]. A summary of MBO pathogenesis is presented in Figure 1.

1.2. Diagnosis of Malignant Bowel Obstruction

The diagnosis of MBO is established by clinical symptoms and a history of malignant disease. Nausea and vomiting, abdominal pain and distension, and constipation are the leading signs. In 10–20% of patients bowel obstruction is the first presentation of malignant disease, which is associated with worse prognosis [12,13].
Besides clinical symptoms and physical examination, X-ray or CT are the cornerstones of the diagnosis. Intraluminal fluid levels, preocclusive distension, and postocclusive normal bowel diameter are diagnostic for this disease [14].

1.3. Management of Malignant Bowel Obstructions (MBOs)

In the management of MBOs, a variety of treatment options are available. In the diagnostic process, diatrizoate meglumine plays an important role, but at the same time this can be therapeutic and potentially speed recovery as well [15]. Possessing high osmotic activity and a mild laxative effect, diatrizoate meglumine draws fluid to the bowel lumen, reducing wall oedema and stimulating peristalsis [16]. In cases of non-responders to diatrizoate meglumine, the next therapeutic step is the application of conservative methods, usually a combination of opioids, corticosteroids, and anti-secretory drugs [17].
As the main pathogenic event is the accumulation of bowel content, therapeutic efforts are made towards its reduction. Somatostatin analogues (octreotide, lanreotide) and anticholinergics such as hyoscine butylbromide decrease bowel motility and bowel and pancreatic secretion [18].
Pain in the majority of the cases is severe and colicky; its alleviation is hardly possible with the exclusive use of non-steroids. Thus, opioids remain commonly used due to their double effect: analgesia and decreased bowel motility.
Corticosteroids having anti-inflammatory and anti-secretory attributes, and can effectively reduce the amount of intraluminal content and wall oedema by promoting water and salt absorption [19].
Placement of a nasogastric tube is a beneficial temporary intervention, as it effectively decompresses the stomach, relieving symptoms such as abdominal distension, pain, and nausea caused by fluid accumulation. This decompression reduces the risk of aspiration, which can have a high mortality rate if vomiting occurs. Additionally, nasogastric tubes can provide a route for medication and nutrition in patients unable to tolerate oral intake, ensuring continued support during treatment [20].
Percutaneous endoscopic gastrostomy (PEG), a procedure where a feeding tube is placed directly into the stomach through the abdominal wall, is often used for patients with gastrointestinal obstructions. PEG is indicated for long-term enteral nutrition in conditions like distal gastric obstruction, which prevents adequate oral intake. It is also used for gastric decompression, helping to relieve symptoms and prevent complications associated with obstructions in the gastrointestinal tract [21]. Stent placement in the obstructed bowel is a minimally invasive procedure typically performed endoscopically to relieve blockage and restore function, providing immediate symptom relief and improving quality of life. Though effective, it can have complications such as stent migration, perforation, and re-obstruction, necessitating careful patient selection and expert execution. Overall, stent placement plays a vital role in the palliative management of MBO, offering a balance of efficacy and safety for patients with advanced malignancies [22].
Surgical interventions in these cases might be challenging for the surgeon and demanding for the patient. An eye must be kept on the intention of the treatment, as the goal is not cytoreduction and resolution of all of the occlusions. Types of operations vary from bowel resection to bypass or stoma formation, according to the localisation and possible multiplicity of the obstruction sites.
Among patients with gynaecological cancer, management of MBO presents a significant clinical challenge due to the lack of clear guidelines and standardised protocols. This ambiguity complicates decision-making processes for clinicians aiming to improve quality of life for affected patients. Surgical interventions, while associated with higher morbidity and mortality rates, often provide the most definitive solution by offering prolonged symptom-free periods and potentially more effective relief from obstruction [5]. Conversely, conservative treatments tend to have lower morbidity but do not significantly extend survival [23,24]. This necessitates a careful, individualised approach to patient care. Recently, the Multinational Association for Supportive Care in Cancer (MASCC) highlighted the need for a multidisciplinary approach to manage malignant bowel obstruction (MBO) in patients with cancer and to support their families [17]. Our review, based on a robust literature search, builds on these recommendations by systematically evaluating current surgical and non-surgical strategies for MBO in patients with gynaecological cancer. By synthesising the latest data, we aim to enhance clinical decision-making and improve patient outcomes, addressing critical gaps in the existing literature and underscoring the importance of prospective, innovative studies to assist clinicians navigating this complex and uncertain field.

2. Materials and Methods

The study’s protocol was registered on PROSPERO under reference number CRD42024543407. We declare that no Preferred Reporting Items for Systematic Reviews and Meta-Analyses (PRISMA) registration was performed for this study; however, our systematic review adheres to the guidelines outlined in the PRISMA 2020 Statement. Furthermore, we adhered to the recommendations provided in Version 6.3 of the Cochrane Handbook for Systematic Reviews of Interventions.

2.1. Eligibility Criteria

Our analysis encompassed research involving patients diagnosed with gynaecologic cancer experiencing malignant bowel obstruction, identified through clinical symptoms or radiological examination.

2.2. Information Sources

We conducted a systematic literature search in four medical databases––MEDLINE (via PubMed), Embase, CENTRAL, and Scopus––from inception to 10 May 2024.

2.3. Search Strategy

We applied the following search key for all fields in the given search engines: (gynaecological cancer OR gynaecologic oncology OR gynaecological tumour) AND (malignant bowel obstruction OR MBO OR intestinal obstruction OR malignant gastrointestinal obstruction). No language or other restrictions were imposed.

2.4. Selection Process

Following a systematic search of the databases and subsequent duplicate removal, selection was conducted according to PICO criteria. EndNote X9 reference manager software (Clarivate Analytics, Philadelphia, PA, USA) facilitated this process. Two independent authors (R.G.T. and Zs.T.) individually screened publications for title, abstract, and full text. To ensure the reliability of the selection process, Cohen’s kappa was calculated after both title and abstract selection, and again after full-text selection. This statistical measure quantified the inter-rater agreement beyond chance, adhering to Cochrane’s rigorous standards for conducting systematic reviews and meta-analyses.

2.5. Selection Protocol

Clinical Questions

The primary question guiding our review was: what is the most effective treatment for MBO in gynaecological malignancies?

2.6. Title and Abstract Selection

Both randomised and non-randomised studies were included, provided they involved adult women with MBO who underwent any kind of treatment. Studies or publications without original research data, such as reviews, letters, commentaries, and protocols, were excluded.

2.7. Full-Text Selection

Studies were included if they used the same measurement units for outcomes. Studies not matching the PICO framework or with inappropriate values were excluded.

2.8. Data Collection Process

Two authors (R.G.T. and Zs.T.) independently extracted data into an Excel spreadsheet (Office 365, Microsoft 16.86, Redmond, WA, USA).

Data Items

We collected the following data from the eligible articles: first author, year of publication, study type, study design, demographic data, details of treatments received, and data on outcomes for statistical analysis. The relief of the bowel obstruction symptoms can be measured through various methods, including improvements in symptoms such as abdominal pain, nausea, vomiting, and constipation. A third reviewer (L.L.) resolved discrepancies.

2.9. Assessment of Bias and Assessment of Grade

The aim of this review was to extract, analyse, and compare outcome reports, counting their frequency, to determine the outcomes most commonly used in the evaluation of malignant bowel obstruction. This review did not intend to draw conclusions about treatment effectiveness, nor about the research design of the included studies.
To ensure the reliability of the included studies, we followed the NHS Executive guidelines from the Reviews on Commissioning Cancer Services. These guidelines categorise evidence quality by study design, from randomised controlled trials (Grade I) to cross-sectional studies (Grade IV). We assessed each study’s design, methodological quality (including sample size and follow-up duration), and potential biases (such as selection, performance, and drop-out biases). Outcome measures’ appropriateness and consistency were also reviewed. Two authors (R.G.T. and Zs.T.) independently reviewed each study, with discrepancies resolved by a third reviewer (L.L.), ensuring the inclusion of only high-quality studies [25].

2.10. Calculation of Cohen’s Kappa

In accordance with Cochrane’s rigorous standards for conducting systematic reviews and meta-analyses, Cohen’s kappa was calculated to protocolize the selection process and guarantee its systematic and comprehensive nature. The first calculation was made after title and abstract selection, and the second after full-text selection. Cohen’s kappa (κ) is calculated using the following formula:
κ = p 0 p e 1 p e
where P0 is the observed agreement, which is the proportion of agreement between the two raters, and Pe is the expected agreement, which is the proportion of agreement that would be expected by chance alone. The observed agreement is calculated by summing the counts of items where the raters agree (the diagonal elements) and dividing by the total number of items.

3. Results

3.1. Included Studies

Our systematic search resulted 5731 records. After eliminating 865 duplicates, 4866 articles underwent screening, resulting in the exclusion of 4788 during title and abstract evaluation. Additionally, 32 articles were excluded during full-text assessment. Subsequently, four articles were excluded due to data unsuitability, leaving 34 articles selected for systematic review. Inter-reviewer agreement was assessed using Cohen’s kappa (k = 0.84 for the first step and k = 0.87 for the second step of selection), with any discrepancies resolved by a third reviewer (L.L.). The characteristics of the studies identified for the systematic review, as well as the patient characteristics of the studies included, are detailed in Table 1.
In total, 2068 patients were included from 34 studies. The studies identified were mainly observational studies, but there were no restrictions in the type of studies included. The inclusion criteria included all studies reporting management of malignant bowel obstruction associated with gynaecological malignancy, with no year of publication limitations and no limitations in the type of treatment and type of management or follow-up.

3.2. Medical Management

The medical management of malignant bowel obstruction (MBO) remains a significant challenge in clinical practice, particularly due to the limited number of studies available on various treatment options. Among these, the use of diatrizoate meglumine (Gastrografin), somatostatin analogues (octreotide), and dexamethasone has shown promising results in alleviating symptoms and aiding in surgical decision-making. This section reviews the current evidence on these medical treatments, highlighting their efficacy and role in the comprehensive management of MBO.

3.2.1. Diatrizoate Meglumine

A limited number of comparable studies are available on the use of Gastrografin in patients with malignant bowel obstruction. Heng’s retrospective analysis confirmed the efficacy of diatrizoate meglumine, with 84% of occlusions resolving after administration and 75% of these cases improving within the first 24 h. Notably, no significant complications were reported. The true value of diatrizoate meglumine lies in its ability to help determine the optimal timing for surgery. This is crucial, because conservative treatment success rates are low in cases of complete bowel obstruction, necessitating timely surgical intervention. Diatrizoate meglumine’s role is highly important in both symptom relief and the timing and decision-making of surgical interventions for patients with MBO [52].

3.2.2. Somatostatin Analogues

Octreotide emerged as the predominant medication investigated for managing MBO, with eight studies exploring its efficacy. The majority of patients in these studies were diagnosed with ovarian cancer, and no restrictions were observed based on the type of bowel involvement. Symptom resolution varied across studies, occurring within a timeframe spanning from 24 h to 4 days, with doses ranging from 100 μg/day to 0.9 mg/day. Two studies examined the use of octreotide in single doses [23,32]. Additionally, two randomised controlled trials (RCTs) included in the analysis revealed octreotide’s significant efficacy in symptom relief within 24 h compared to butylscopolamine [37,58].
In a comprehensive evaluation of the long-acting form of octreotide (LAR) in patients with recurrent ovarian cancer, Matulonis et al. administered 30 mg depot injections on Day 1 alongside subcutaneous octreotide for 2 weeks, providing sustained relief from bowel dysfunction. This approach demonstrated both safety and utility, with three out of fifteen patients experiencing a major reduction in malignant bowel obstruction (MBO) symptoms and two showing a minor response, while no significant toxicities related to octreotide or LAR were reported. Remarkably, some patients remained on LAR depot for over 9 months, suggesting its potential for long-term symptom management [40]. Similarly, Watari et al. investigated octreotide’s efficacy in controlling vomiting in patients with advanced gynaecologic cancer and inoperable gastrointestinal obstruction. Octreotide, administered via continuous infusion for two weeks, exhibited a high rate of vomiting control, with an overall response rate of 81.8%. Particularly noteworthy was its effectiveness in patients without nasogastric tubes, with an overall response rate of 93.1%. Furthermore, the absence of major adverse events associated with octreotide underscores its safety profile and potential to enhance quality of life by obviating the need for nasogastric tube placement in this patient population [42].
Walter et al. prospectively evaluated “triple therapy” consisting of dexamethasone, metoclopramide, and octreotide in managing non-surgical MBO. Despite the small sample size of 17 patients, the therapy exhibited promising results, with complete resolution of nausea and improvement in other symptoms such as pain and constipation. Although adverse effects such as bradycardia were noted in two patients, there were no incidences of bowel perforation [57].
A study conducted by Daniele et al. suggests that a tailored medical protocol, particularly involving anti-secretory drugs like octreotide, remains the standard of care for frail patients or those with contraindications to surgery [48].
While complications such as bowel perforation and necrosis were noted in a minority of cases, overall octreotide presents as a valuable adjunct in the management of MBO.

3.2.3. Dexamethasone

The use of dexamethasone in managing MBO in patients with gynaecological cancer has demonstrated promising outcomes. Our analysis compromising three studies involving 163 patients exclusively diagnosed with ovarian cancer highlights its efficacy. The dosage ranged from 4 mg/day to 8 mg twice a day. The use of dexamethasone is limited specifically to cases of small bowel obstruction, whether administered intravenously or subcutaneously. Dexamethasone typically achieves resolution of bowel obstruction within 5 to 7 days. While adverse events such as unpleasant perianal sensations are noted in some cases, overall success rates are encouraging, ranging around 89%. These findings underscore dexamethasone’s role as a valuable therapeutic option in managing MBO in patients with gynaecological cancer, offering relief and potentially improving their quality of life [34,36,55]. A summary of the abovementioned data is presented in Table 2.

3.3. Invasive Interventions

3.3.1. Percutaneous Gastrostomy

Percutaneous gastrostomy is a procedure used to insert a tube through the abdominal wall into the stomach. This tube provides a direct means of feeding or gastric decompression for patients who are unable to take adequate nutrition orally or who need relief from symptoms such as vomiting and nausea due to impaired gastric motility. Percutaneous gastroscopy can be performed surgically, endoscopically, or with radiologic intervention. In the case of MBO, the less invasive method is preferable, as the other procedures are highly symptomatic.
Patients treated with this option are usually not eligible for operations because of their general condition or their abdominal status, e.g., there are occlusions on more sites of the small bowel. However, this method is technically feasible, with a low rate of intervention failure.
Studies consistently report high technical success rates, often close to 100% [27,29,30,38,39]. The reduction in symptoms, particularly nausea and vomiting, is substantial, with many studies reporting symptom relief in nearly all patients [31]. Gastrostomy has positive effects on the quality of life of the patients [49]. Survival times post-procedure vary significantly, with median or mean survival ranging from as short as 17 days to as long as 74 days [31,38]. Despite its effectiveness in symptom relief, PEG procedures are associated with complications, including leakage, peritonitis, site infections, and, in some cases, more severe issues like sepsis and autodigestion of the abdominal wall [27,30]. Overall, PEG demonstrates substantial efficacy in palliation for MBO, though the risk of complications necessitates careful patient management and selection [31,44,50,56]. Side effects and success rates are described in Table 3.
Total parenteral nutrition is a consequence of this intervention, although the majority of patients will be able to take sips of beverages for comfort after the insertion of gastric tubing.

3.3.2. Stent Placement

Gynaecological malignancies, especially ovarian cancer, can cause obstruction of the large bowel. It would be evident to use intraluminal colonic stents to restore the lumen of the bowel. Milek et al. investigated a new stent developed by themselves, which proved the efficacy and feasibility of the application of large bowel stents. In total, 85% of all patients felt decompression of the obstructed gastrointestinal tract after the first stent implantation [51]. In one case two stents were implanted due to insufficient coverage of the stricture. Another study led by Jutzi et al. showed that they had a technical success rate of 75% on their sample of 32 patients, whilst the clinical success rate was 47%, and 37.5% of the subjects had a complication requiring intervention [45].
Taking all these studies into account, the results are contradictory. Although the intervention is feasible and offers a good option for treatment, there was a meaningful need for intervention because of the complications caused by the stents. There is also a limitation by the nature of the disease, as it spreads on the peritoneal surface and can cause obstructions at different levels, while stenting is rather ideal for localised pathologies.

3.3.3. Surgical Interventions

Surgery is the treatment option to choose when conservative methods do not seem to be effective in 3–7 days [35]. Surgical interventions can be demanding for the patient, and sometimes a longer period is needed for recovery, mainly for those patients whose baseline condition is already impaired. Thus, the widespread application of surgical interventions is limited, although they offer a longer symptom-free period and might prolong survival of the patients, even under palliative circumstances. Even though one must not lose the main objective of the procedure: pain relief and comfort enhancement.
Surgical interventions can improve quality of life, as there is a higher chance for patients to tolerate solid intake or fluids, and there is less need for total parenteral nutrition, like in the case of gastrostomies [23]. Chi et al. found that return of symptoms and death are less likely to occur in patients who went through a surgical intervention than those who received an endoscopic solution for their symptoms [41]. Despite all the negative effects, the reason to support surgical interventions in palliative cases is the fact that all the studies which we found in the literature proved a longer survival in this group of patients.
It is still controversial who are the patients who can benefit from surgeries and what are the indicators of worse outcomes. Many studies examined this aspect and found correlations between survival and prognostic factors such as low albumin or elevated blood urea nitrogen or alkaline phosphatase or clinical factors like age, radiotherapy, ascites, carcinomatosis, multiple obstructions, or a palpable mass [26]. On the other hand, there are studies which do not support this [23].
In some very selected cases disseminated tumour spread results in a very complex surgery. Foutopoulou et al. found it feasible to perform these operations even if they resulted in short-bowel syndrome and consecutive total parenteral nutrition; however, they advised to treat these patients conservatively, as these operations can cause severe morbidity and a reduction in quality of life [43]. A later study conducted in the same centres by Armbrust et al. suggested that even these kinds of surgeries can extend therapeutic opportunities in highly selected patients [59].
It is essential to determine who are the ones who can benefit from surgeries and whose operation is feasible to avoid surgical failure and inappropriate interventions. Lodoli et al. suggest some features that could predict failure. According to them, surgery on a proximal occlusion has a higher chance of ineffectiveness due to shortening of the already anatomically short jejunal mesentery. Interestingly, they found that bowel dilatation without a real obstruction can result in surgical failure as well. Their explanation was decreased motility of the bowels because of widespread peritoneal infiltration that prevented surgeons from creating ostomies [54].
Previous studies suggest that age, disease extent, and nutritional status are important factors as well, from which they have created a risk stratification tool [28]. According to these and their own data, Perri et al. suggest a scoring system in which they take albumin level, presence of ascites more than 2 L, age, and non-ovarian tumour origin into account [46]. Another group of investigators found factors like ECOG status, platinum sensitivity, ascites  < 500 mL, type of stoma, and number of anastomoses to be the factors influencing results, emphasizing the importance of pre-operative frailty assessment [59]. Although, according to Daniele et al., cachexia, low performance status, and poor nutritional status emerged as significant predictors of worse survival, irrespective of the chosen treatment modality [48].
During the treatment of MBO it is crucial to have a reliable triage system to shorten the length of hospitalization and to avoid unnecessary surgical interventions in order to provide the highest quality of life possible. As MBO occurs subacutely, it is possible to start its treatment in an outpatient setting. Lee at al. developed an MBO programme which proved to achieve all its goals, as the rate of surgical interventions, frequency of recurrent episodes of MBO, and length of hospital stay were lower in the intervention group, and the possible chance of continuation of oncologic care was higher [53].
The studies included in the review were graded to monitor their quality according to the criteria set out by the NHS Executive in their Reviews on Commissioning Cancer Services. This grading ensured that only the strongest evidence was considered (Table 4).
The basic characteristics of the studies included are summarized and detailed in Table 1, providing an overview of the patient demographics and study designs.
All the methods discussed in the manuscript have been summarised in Table 5 according to their advantages and disadvantages, providing a clear comparison for readers.

4. Discussion

Despite all the efforts and all the management options, malignant bowel obstruction remains a potentially lethal condition, with poor survival expectations [60,61]. Inadequately chosen therapeutic interventions may result in long-term hospitalisation or severe side effects [62,63]. However, under palliative circumstances the main aims are symptom and pain management and enhancement of quality of life, which should be reflected in the patient–physician communication as well [62,63]. Nevertheless, healthcare providers should seek for long-lasting therapeutic options, often using an invasive method, in order to provide the best quality of life achievable. Decisions about invasive measures must be made with the active involvement of the patient and the family of the patient. This is highlighted by the fact that personal factors, spiritual beliefs, and psychological and psycho-social factors play an important role in this process [64].
The active involvement of patients and their families is crucial, considering the frequency and severity of complications of potential surgical interventions. In order to decrease complications, numerous attempts have been made to determinate the factors influencing surgical outcomes; however, their results have often been inconclusive. Factors that appear to be reliable in evaluating potential risks include blood albumin levels, the presence of ascites, the complexity of the surgery (e.g., stoma placement, residual bowel length, number of bowel resections), general performance status, and frailty [28,46,65]. Furthermore, some authors suggest that patients’ life expectancy must be taken into consideration as well [19].
However, surgical solutions should be prioritised, as surgical interventions provide lower recurrence rate of obstructive episodes, longer symptom-free survival, and longer overall survival [35,41,48,66,67] than less demanding procedures. This statement is supported by a review of 868 patients carried out by Furnes et al. [68]. According to them, surgery was successful in relieving obstructive symptoms and provided the possibility of diet reintroduction and earlier discharge. Nevertheless, some authors suggest that longer survival rates may be attributed to the possible reintroduction of chemotherapy [69]. However, chemotherapy alone has not proved to be effective in the restoration of bowel function in heavily pretreated patients [70].
When a decision on surgery is made, interventions must be accomplished [71] in a moderate manner, keeping in mind the intention of the procedure. The chosen type of surgery depends on the location and the possible multiplicity of the obstruction, but always must be tailored to each single situation. Under these circumstances cytoreduction is no longer the goal of the operation, and symptom management procedures (e.g., bowel resections, bypasses, ostomies) should be carried out instead.
In case of inoperability, the treatments of choice are less invasive measures: stent placement or percutaneous gastrostomy. Stents are recommended mainly in cases of large bowel or duodenal obstructions, when they are present solitarily [45]. The application of stents promises a high success rate for implantation, with a relatively low chance for further surgical intervention and prolonged survival [72,73].
If there are multiple sites of obstruction, gastrostomy seems to be the better solution for management. Gastrostomies are advised even in very vulnerable patients, as this procedure proved to be feasible in numerous studies and provided good symptom control, equally if they were performed radiologically or endoscopically [27,29,30,31,33,38,39,44,49,50,56]. Both gastrostomies and jejunostomies result in short bowel syndrome, leading to the necessity of total parenteral nutrition; thus, the involvement of nutritional specialists is inevitable in the management of these patients [74].
Until a decision on surgical intervention is made, administration of several drugs is needed in order to relieve the patient’s symptoms.
Some authors suggest that therapy should start with conservative management of MBO, as spontaneous or treatment-evoked resolution can happen in a great proportion of patients. However, conservative treatment might have a bridge function as well until the surgical intervention, as it offers the possibility of optimising the patient for intervention.
Initial, symptomatic care should have three major directions, as follows: pain management, control of vomiting, and control of basic homeostatic parameters.
Supportive care must cover the restoration of basic homeostatic parameters. During pathophysiological changes, increased secretion of intestinal fluids, extravasation as a response to inflammatory reactions, and consequential emesis, significant electrolyte imbalance develops [75].
In the majority of the cases pain management cannot be carried out without the use of opioids. In this setting bowel movement inhibition plays an adjuvant role, as it reduces cramping. Following resolution of a malignant bowel obstruction (MBO) episode, it is essential to minimise the long-term use of opioids to avoid potential side effects and dependency. Pain management should be guided by the WHO analgesic ladder, which recommends a stepwise approach to pain relief. This involves starting with non-steroidal anti-inflammatory drugs (NSAIDs) and adjuvants, such as antidepressants or anticonvulsants, to address pain and enhance analgesic effects. If these medications prove insufficient, clinicians should then consider the use of minor opioids. Only if these measures fail to provide adequate pain relief should major opioids be introduced [76].
In a great part of cases bowel function can be restored using diatrizoate meglumine, which is used in the diagnostics of MBO routinely. Our search showed 84% effectivity in the restoration of the bowel function. A meta-analysis from Branco et al. [77] confirms this, as it concludes from 14 studies that, if the contrast material does not appear in the large bowel in 24 h, surgery is inevitable in 99% of cases. Parallelly, Galardi et al. found that patients who underwent a small bowel diatrizoate meglumine follow-through test were operated on earlier than those who did not [78].
In our systematic review we found that, in the management of vomiting, somatostatin analogues showed promising results in the management of MBO, reducing the main pathogenic event, which is the accumulation of bowel content. Somatostatin analogues decrease bowel motility and bowel and pancreatic secretion [18]. Therapeutic efficacy regarding symptom control proved to be at least 82%, and in most of the studies 100% symptom control was achieved in less than 4 days of application, without major complications. The preferred drug was mainly octreotide in a 0.3 mg/day dosage.
In the management of MBOs, corticosteroids were widely investigated according to their anti-inflammatory and anti-secretory attributes, reducing the amount of intraluminal contents and wall oedema by promoting water and salt absorption [19]. Among these substances the use of dexamethasone was the most common, showing a significant response in MBO, as complete response rate was achieved in at least half of the patients.
The most promising conservative treatment for MBO might be the combination of dexamethasone, lanreotide, and metoclopramide [79]; in this manner combined anti-inflammatory, secretion-reducing, and motility-restoring action can be achieved.
There is substantial evidence in the literature demonstrating that established palliative care programs significantly improve quality of life for patients. The integration of palliative care into general oncologic treatment should be implemented as early as possible to maximise benefits [80,81]. Oncologic patients having intra-abdominal disseminated cancer are at high risk of developing bowel obstruction. For this group of patients, it is important to provide dietary interventions and offer laxatives preventing constipation, which can exacerbate obstruction [47]. Assessing the chance of MBO, as early detection is shown to improve outcomes of necessary interventions and well-established local management protocols, can decrease hospital stay and improve quality of life for patients [53].
Besides clinical symptoms and physical examination, radiologic methods play a crucial role in setting the diagnosis of MBO. CT scan can have a higher value in further therapy management than conventional X-ray, considering its capability to determine the location and possible multiplicity of the obstruction. Contrast enhancement is widely used to determine obstructions, whether those are complete or not. Besides, in a remarkable part of cases the use of Gastrografin can resolve symptoms; nevertheless, its predictive value is the most important [52].
Parallel with diagnostics, clinicians must actively engage with the patients’ symptoms and start supportive care on pain management and electrolyte restoration.
Another direction of supportive care is to relieve nausea and vomiting, which can be rapidly decreased with the placement of a nasogastric tube (NGT). The use of nasogastric tubes belongs to basic care in cases of small bowel occlusion. The use of nasogastric tubing is fundamental in the care of patients with small bowel occlusion, primarily for symptom relief, but also helps to reduce distension of the stomach and small bowel. However, limited data support its routine use. In 2014 Paradis et al. [82] conducted a systematic search on data related to this topic, from 1966 to 2014. They found only one paper with relevant data, but this was not strong enough to make it into evidence [83]. According to this retrospective study conducted by Fonseca et al. [37], a significant association was found between NGT placement and the development of pneumonia and respiratory failure. Patients with NGTs had longer resolution times and extended hospital stays. Although NGTs can quickly relieve symptoms, their prolonged use can disturb patients and affect their quality of life. Nasogastric tubes are quite uncomfortable, and long-term use can provoke epistaxis, necrosis on the nasal wings, laryngeal disorders, regurgitation, and aspiration pneumonia, thus increasing the length of hospital stay and decreasing the most important value in the palliative setting, quality of life. These results highlight the need for selective NGT use, considering risks and benefits individually. However, the use of NGTs remains the standard of care in the acute phase.
The most promising conservative treatment of MBO seems to be the combination of dexamethasone, octreotide, and metoclopramide.
Synthesising all the data found, we tried to provide a treatment algorithm which can be a useful guide in the palliative care of patients with gynaecologic cancer suffering from malignant bowel obstruction (Figure 2). For a summary of the therapeutic algorithm see Figure 3.
Current society guidelines suggest that treatment algorithms must be managed individually, as evidence is lacking on treatment modalities, thus encouraging further investigations on this topic [17,64]. Review of the literature reveals that decision-making in the management of MBO is complex and not straightforward. Treatment plans must be personalised and involve a multidisciplinary team, considering all aspects of the patient’s condition. It is crucial to acknowledge that patients’ perspectives on their treatment may differ significantly from those of healthcare providers, necessitating a holistic approach in care [84].
To facilitate easier decision making, the development of risk-stratifying algorithms is necessary to identify patients who would benefit from surgery [85]; on the other hand, robust prospective trials are needed in this field to collect data on specific treatment modalities to be capable of creating universal guidance for the management of this patient population.

5. Conclusions

The optimal management of malignant bowel obstruction remains controversial. This review aimed to summarise the current literature to provide guidance on the management of this condition.

5.1. Implications for Practice

Given the limited availability of strong evidence, it is challenging to establish a single therapeutic approach for patients with malignant bowel obstruction. Our recommendation represents one perspective and highlights the need for individualised treatment strategies. Due to the absence of definitive guidelines, healthcare providers must tailor treatment plans to each patient’s specific circumstances, acknowledging that the objectives of treatment may differ between patients. The development of holistic, patient-centred management pathways is crucial.

5.2. Implications for Future Research

The objective of this study was to synthesise the latest data on malignant bowel obstructions in gynaecological cancers. Our systematic review underscores the lack of high-quality evidence, with most studies being retrospective, and the few prospective studies involving small patient cohorts. Data heterogeneity, originating from differences in patient populations, data collection methods, local management practices, and treatment intentions, further complicates comparability.
Future investigations should prioritise prospective data collection through multicentre international collaborations to generate robust evidence and address outstanding questions in the management of malignant bowel obstruction.

Author Contributions

Conceptualization, R.T., M.K. and B.L.; methodology, M.K. and B.L.; validation, R.T., M.K. and M.T.; formal analysis, R.T., M.K. and B.L.; investigation, R.T., Z.T., L.L., M.T., N.Á., S.V., M.K. and B.L.; data curation, R.T., M.K., M.T. and B.L.; writing—original draft preparation, R.T., Z.T., L.L., M.T., N.Á., S.V., M.K., and B.L.; writing—review and editing, R.T., Z.T., L.L., M.T., N.Á., S.V., M.K. and B.L.; visualization, R.T. and M.K.; supervision, M.K., M.T. and B.L.; project administration, M.K.; funding acquisition, M.T. and S.V. All authors have read and agreed to the published version of the manuscript.

Funding

This research was funded by the Semmelweis Science and Innovation Fund (STIA-OTKA-2021 for S.V.) and the Hungarian Hypertension Society (for S.V. and M.T.).

Institutional Review Board Statement

Not applicable.

Informed Consent Statement

Not applicable.

Data Availability Statement

The published article contains all generated and analyzed data from this series.

Conflicts of Interest

The authors declare no conflicts of interest.

References

  1. Ferlay, J.; Laversanne, M.; Ervik, M.; Lam, F.; Colombet, M.; Mery, L.; Piñeros, M.; Znaor, A.; Soerjomataram, I.; Bray, F. Global Cancer Observatory: Cancer Tomorrow (Version 1.1); International Agency for Research on Cancer: Lyon, France, 2024; Volume 2024.
  2. Baradács, I.; Teutsch, B.; Váradi, A.; Bilá, A.; Vincze, Á.; Hegyi, P.; Fazekas, T.; Komoróczy, B.; Nyirády, P.; Ács, N.; et al. PARP inhibitor era in ovarian cancer treatment: A systematic review and meta-analysis of randomized controlled trials. J. Ovarian Res. 2024, 17, 53. [Google Scholar] [CrossRef] [PubMed]
  3. Temkin-Greener, H.; Ladswig, S.; Caprio, T.; Norton, S.; Quill, T.; Olsan, T.; Cai, X.; Mukamel, D.B. Developing palliative care practice guidelines and standards for nursing home-based palliative care teams: A Delphi study. J. Am. Med. Dir. Assoc. 2015, 16, e81–e87. [Google Scholar] [CrossRef] [PubMed]
  4. Martinez Castro, P.; Vargas, L.; Mancheño, A.; Martín Utrilla, S.; Pascual, F.; Romero, I.; Zorrero, C.; Bosch, J.M.; Poveda, A.; Minig, L. Malignant Bowel Obstruction in Relapsed Ovarian Cancer With Peritoneal Carcinomatosis: An Occlusive State. Int. J. Gynecol. Cancer 2017, 27, 1367–1372. [Google Scholar] [CrossRef] [PubMed]
  5. Kolomainen, D.F.; Barton, D.P. Surgical management of bowel obstruction in gynaecological malignancies. Curr. Opin. Support. Palliat. Care 2011, 5, 55–59. [Google Scholar] [CrossRef] [PubMed]
  6. Dvoretsky, P.M.; Richards, K.A.; Angel, C.; Rabinowitz, L.; Beecham, J.B.; Bonfiglio, T.A. Survival time, causes of death, and tumor/treatment-related morbidity in 100 women with ovarian cancer. Hum. Pathol. 1988, 19, 1273–1279. [Google Scholar] [CrossRef]
  7. Markogiannakis, H.; Messaris, E.; Dardamanis, D.; Pararas, N.; Tzertzemelis, D.; Giannopoulos, P.; Larentzakis, A.; Lagoudianakis, E.; Manouras, A.; Bramis, I. Acute mechanical bowel obstruction: Clinical presentation, etiology, management and outcome. World J. Gastroenterol. 2007, 13, 432–437. [Google Scholar] [CrossRef] [PubMed]
  8. Tuca, A.; Guell, E.; Martinez-Losada, E.; Codorniu, N. Malignant bowel obstruction in advanced cancer patients: Epidemiology, management, and factors influencing spontaneous resolution. Cancer Manag. Res. 2012, 4, 159–169. [Google Scholar] [CrossRef]
  9. Fernandes, D.; Domingues, S.; Gonçalves, B.M.; Bastos, P.; Ferreira, A.; Rodrigues, A.; Gonçalves, R.; Lopes, L.; Rolanda, C. Acute Treatment of Malignant Colorectal Occlusion: Real Life Practice. GE Port. J. Gastroenterol. 2016, 23, 66–75. [Google Scholar] [CrossRef] [PubMed]
  10. Batke, M.; Cappell, M.S. Adynamic ileus and acute colonic pseudo-obstruction. Med. Clin. N. Am. 2008, 92, 649–670, ix. [Google Scholar] [CrossRef]
  11. Brüggmann, D.; Tchartchian, G.; Wallwiener, M.; Münstedt, K.; Tinneberg, H.R.; Hackethal, A. Intra-abdominal adhesions: Definition, origin, significance in surgical practice, and treatment options. Dtsch. Arztebl. Int. 2010, 107, 769–775. [Google Scholar] [CrossRef]
  12. Estes, J.M.; Leath, C.A., 3rd; Straughn, J.M., Jr.; Rocconi, R.P.; Kirby, T.O.; Huh, W.K.; Barnes, M.N., 3rd. Bowel resection at the time of primary debulking for epithelial ovarian carcinoma: Outcomes in patients treated with platinum and taxane-based chemotherapy. J. Am. Coll. Surg. 2006, 203, 527–532. [Google Scholar] [CrossRef] [PubMed]
  13. Gillette-Cloven, N.; Burger, R.A.; Monk, B.J.; McMeekin, D.S.; Vasilev, S.; DiSaia, P.J.; Kohler, M.F. Bowel resection at the time of primary cytoreduction for epithelial ovarian cancer. J. Am. Coll. Surg. 2001, 193, 626–632. [Google Scholar] [CrossRef]
  14. Pothiawala, S.; Gogna, A. Early diagnosis of bowel obstruction and strangulation by computed tomography in emergency department. World J. Emerg. Med. 2012, 3, 227–231. [Google Scholar] [CrossRef]
  15. Syrmis, W.; Richard, R.; Jenkins-Marsh, S.; Chia, S.C.; Good, P. Oral water soluble contrast for malignant bowel obstruction. Cochrane Database Syst. Rev. 2018, 3, Cd012014. [Google Scholar] [CrossRef] [PubMed]
  16. Choi, H.K.; Chu, K.W.; Law, W.L. Therapeutic value of gastrografin in adhesive small bowel obstruction after unsuccessful conservative treatment: A prospective randomized trial. Ann. Surg. 2002, 236, 1–6. [Google Scholar] [CrossRef] [PubMed]
  17. Madariaga, A.; Lau, J.; Ghoshal, A.; Dzierżanowski, T.; Larkin, P.; Sobocki, J.; Dickman, A.; Furness, K.; Fazelzad, R.; Crawford, G.B.; et al. MASCC multidisciplinary evidence-based recommendations for the management of malignant bowel obstruction in advanced cancer. Support. Care Cancer 2022, 30, 4711–4728. [Google Scholar] [CrossRef] [PubMed]
  18. Ripamonti, C.; Mercadante, S.; Groff, L.; Zecca, E.; De Conno, F.; Casuccio, A. Role of octreotide, scopolamine butylbromide, and hydration in symptom control of patients with inoperable bowel obstruction and nasogastric tubes: A prospective randomized trial. J. Pain Symptom Manag. 2000, 19, 23–34. [Google Scholar] [CrossRef]
  19. Hsu, K.; Prommer, E.; Murphy, M.C.; Lankarani-Fard, A. Pharmacologic Management of Malignant Bowel Obstruction: When Surgery Is Not an Option. J. Hosp. Med. 2019, 14, 367–373. [Google Scholar] [CrossRef] [PubMed]
  20. Sigmond, D.F.; An, J. Nasogastric Tube. In StatPearls [Internet]; Updated 31 October 2022; StatPearls Publishing: Treasure Island, FL, USA, 2024. Available online: https://www.ncbi.nlm.nih.gov/books/NBK556063/ (accessed on 16 July 2024).
  21. Vudayagiri, L.; Hoilat, G.J.; Gemma, R. Percutaneous Endoscopic Gastrostomy Tube. In StatPearls [Internet]; Updated 7 August 2023; StatPearls Publishing: Treasure Island, FL, USA, 2024. Available online: https://www.ncbi.nlm.nih.gov/books/NBK535371/ (accessed on 16 July 2024).
  22. Moutzoukis, M.; Argyriou, K.; Kapsoritakis, A.; Christodoulou, D. Endoscopic luminal stenting: Current applications and future perspectives. World J. Gastrointest. Endosc. 2023, 15, 195–215. [Google Scholar] [CrossRef] [PubMed]
  23. Mangili, G.; Aletti, G.; Frigerio, L.; Franchi, M.; Panacci, N.; Viganò, R.; De Marzi, P.; Zanetto, F.; Ferrari, A. Palliative care for intestinal obstruction in recurrent ovarian cancer: A multivariate analysis. Int. J. Gynecol. Cancer 2005, 15, 830–835. [Google Scholar] [CrossRef]
  24. Bryan, D.N.; Radbod, R.; Berek, J.S. An analysis of surgical versus chemotherapeutic intervention for the management of intestinal obstruction in advanced ovarian cancer. Int. J. Gynecol. Cancer 2006, 16, 125–134. [Google Scholar] [CrossRef]
  25. Mann, T.; Executive, N. Clinical Guidelines: Using Clinical Guidelines to Improve Patient Care within the NHS; NHS Executive: Leeds, UK, 1996. [Google Scholar]
  26. Castaldo, T.W.; Petrilli, E.S.; Ballon, S.C.; Lagasse, L.D. Intestinal operations in patients with ovarian carcinoma. Am. J. Obstet. Gynecol. 1981, 139, 80–84. [Google Scholar] [CrossRef]
  27. Malone, J.M., Jr.; Koonce, T.; Larson, D.M.; Freedman, R.S.; Carrasco, C.H.; Saul, P.B. Palliation of small bowel obstruction by percutaneous gastrostomy in patients with progressive ovarian carcinoma. Obstet. Gynecol. 1986, 68, 431–433. [Google Scholar] [CrossRef]
  28. Larson, J.E.; Podczaski, E.S.; Manetta, A.; Whitney, C.W.; Mortel, R. Bowel obstruction in patients with ovarian carcinoma: Analysis of prognostic factors. Gynecol. Oncol. 1989, 35, 61–65. [Google Scholar] [CrossRef]
  29. Lee, M.J.; Saini, S.; Brink, J.A.; Morrison, M.C.; Hahn, P.F.; Mueller, P.R. Malignant small bowel obstruction and ascites: Not a contraindication to percutaneous gastrostomy. Clin. Radiol. 1991, 44, 332–334. [Google Scholar] [CrossRef]
  30. Cunningham, M.J.; Bromberg, C.; Kredentser, D.C.; Collins, M.B.; Malfetano, J.H. Percutaneous gastrostomy for decompression in patients with advanced gynecologic malignancies. Gynecol. Oncol. 1995, 59, 273–276. [Google Scholar] [CrossRef]
  31. Cannizzaro, R.; Bortoluzzi, F.; Valentini, M.; Scarabelli, C.; Campagnutta, E.; Sozzi, M.; Fornasarig, M.; Poletti, M. Percutaneous endoscopic gastrostomy as a decompressive technique in bowel obstruction due to abdominal carcinomatosis. Endoscopy 1995, 27, 317–320. [Google Scholar] [CrossRef]
  32. Mangili, G.; Franchi, M.; Mariani, A.; Zanaboni, F.; Rabaiotti, E.; Frigerio, L.; Bolis, P.F.; Ferrari, A. Octreotide in the management of bowel obstruction in terminal ovarian cancer. Gynecol. Oncol. 1996, 61, 345–348. [Google Scholar] [CrossRef]
  33. Campagnutta, E.; Cannizzaro, R.; Gallo, A.; Zarrelli, A.; Valentini, M.; De Cicco, M.; Scarabelli, C. Palliative treatment of upper intestinal obstruction by gynecological malignancy: The usefulness of percutaneous endoscopic gastrostomy. Gynecol. Oncol. 1996, 62, 103–105. [Google Scholar] [CrossRef] [PubMed]
  34. Hardy, J.; Ling, J.; Mansi, J.; Isaacs, R.; Bliss, J.; A’Hern, R.; Blake, P.; Gore, M.; Shepherd, J.; Hanks, G. Pitfalls in placebo-controlled trials in palliative care: Dexamethasone for the palliation of malignant bowel obstruction. Palliat. Med. 1998, 12, 437–442. [Google Scholar] [CrossRef] [PubMed]
  35. Gadducci, A.; Iacconi, P.; Fanucchi, A.; Cosio, S.; Miccoli, P.; Genazzani, A.R. Survival after intestinal obstruction in patients with fatal ovarian cancer: Analysis of prognostic variables. Int. J. Gynecol. Cancer 1998, 8, 177–182. [Google Scholar] [CrossRef]
  36. Philip, J.; Lickiss, N.; Grant, P.T.; Hacker, N.F. Corticosteroids in the management of bowel obstruction on a gynecological oncology unit. Gynecol. Oncol. 1999, 74, 68–73. [Google Scholar] [CrossRef]
  37. Mercadante, S.; Ripamonti, C.; Casuccio, A.; Zecca, E.; Groff, L. Comparison of octreotide and hyoscine butylbromide in controlling gastrointestinal symptoms due to malignant inoperable bowel obstruction. Support. Care Cancer 2000, 8, 188–191. [Google Scholar] [CrossRef] [PubMed]
  38. Brooksbank, M.A.; Game, P.A.; Ashby, M.A. Palliative venting gastrostomy in malignant intestinal obstruction. Palliat. Med. 2002, 16, 520–526. [Google Scholar] [CrossRef] [PubMed]
  39. Pothuri, B.; Montemarano, M.; Gerardi, M.; Shike, M.; Ben-Porat, L.; Sabbatini, P.; Barakat, R.R. Percutaneous endoscopic gastrostomy tube placement in patients with malignant bowel obstruction due to ovarian carcinoma. Gynecol. Oncol. 2005, 96, 330–334. [Google Scholar] [CrossRef] [PubMed]
  40. Matulonis, U.A.; Seiden, M.V.; Roche, M.; Krasner, C.; Fuller, A.F.; Atkinson, T.; Kornblith, A.; Penson, R. Long-acting octreotide for the treatment and symptomatic relief of bowel obstruction in advanced ovarian cancer. J. Pain Symptom Manag. 2005, 30, 563–569. [Google Scholar] [CrossRef] [PubMed]
  41. Chi, D.S.; Phaëton, R.; Miner, T.J.; Kardos, S.V.; Diaz, J.P.; Leitao, M.M., Jr.; Gardner, G.; Huh, J.; Tew, W.P.; Konner, J.A.; et al. A prospective outcomes analysis of palliative procedures performed for malignant intestinal obstruction due to recurrent ovarian cancer. Oncologist 2009, 14, 835–839. [Google Scholar] [CrossRef] [PubMed]
  42. Watari, H.; Hosaka, M.; Wakui, Y.; Nomura, E.; Hareyama, H.; Tanuma, F.; Hattori, R.; Azuma, M.; Kato, H.; Takeda, N.; et al. A prospective study on the efficacy of octreotide in the management of malignant bowel obstruction in gynecologic cancer. Int. J. Gynecol. Cancer 2012, 22, 692–696. [Google Scholar] [CrossRef] [PubMed]
  43. Fotopoulou, C.; Braicu, E.I.; Kwee, S.L.; Kuhberg, M.; Richter, R.; Pietzner, K.; Feldheiser, A.; Bahra, M.; Schmidt, S.C.; Sehouli, J. Salvage surgery due to bowel obstruction in advanced or relapsed ovarian cancer resulting in short bowel syndrome and long-life total parenteral nutrition: Surgical and clinical outcome. Int. J. Gynecol. Cancer 2013, 23, 1495–1500. [Google Scholar] [CrossRef] [PubMed]
  44. Rath, K.S.; Loseth, D.; Muscarella, P.; Phillips, G.S.; Fowler, J.M.; O’Malley, D.M.; Cohn, D.E.; Copeland, L.J.; Eisenhauer, E.L.; Salani, R. Outcomes following percutaneous upper gastrointestinal decompressive tube placement for malignant bowel obstruction in ovarian cancer. Gynecol. Oncol. 2013, 129, 103–106. [Google Scholar] [CrossRef]
  45. Jutzi, L.; Russell, D.; Ho, S.; Kwon, J.S. The role of palliative colorectal stents in gynaecologic malignancy. Gynecol. Oncol. 2014, 134, 566–569. [Google Scholar] [CrossRef] [PubMed]
  46. Perri, T.; Korach, J.; Ben-Baruch, G.; Jakobson-Setton, A.; Ben-David Hogen, L.; Kalfon, S.; Beiner, M.; Helpman, L.; Rosin, D. Bowel obstruction in recurrent gynecologic malignancies: Defining who will benefit from surgical intervention. Eur. J. Surg. Oncol. 2014, 40, 899–904. [Google Scholar] [CrossRef] [PubMed]
  47. Isbister, W.H.; Elder, P.; Symons, L. Non-operative management of malignant intestinal obstruction. J. R. Coll. Surg. Edinb. 1990, 35, 369–372. [Google Scholar] [PubMed]
  48. Daniele, A.; Ferrero, A.; Fuso, L.; Mineccia, M.; Porcellana, V.; Vassallo, D.; Biglia, N.; Menato, G. Palliative care in patients with ovarian cancer and bowel obstruction. Support. Care Cancer 2015, 23, 3157–3163. [Google Scholar] [CrossRef] [PubMed]
  49. Zucchi, E.; Fornasarig, M.; Martella, L.; Maiero, S.; Lucia, E.; Borsatti, E.; Balestreri, L.; Giorda, G.; Annunziata, M.A.; Cannizzaro, R. Decompressive percutaneous endoscopic gastrostomy in advanced cancer patients with small-bowel obstruction is feasible and effective: A large prospective study. Support. Care Cancer 2016, 24, 2877–2882. [Google Scholar] [CrossRef] [PubMed]
  50. Dittrich, A.; Schubert, B.; Kramer, M.; Lenz, F.; Kast, K.; Schuler, U.; Schuler, M.K. Benefits and risks of a percutaneous endoscopic gastrostomy (PEG) for decompression in patients with malignant gastrointestinal obstruction. Support. Care Cancer 2017, 25, 2849–2856. [Google Scholar] [CrossRef] [PubMed]
  51. Miłek, T.; Pasek, K.; Ciostek, P.; Alkalaya, H.; Timorek, A.; Sawicki, W.; Cendrowski, K. Using our own developed stent in the palliative treatment of obstruction in the left half of the colon due to ovarian cancer. Ginekol. Pol. 2017, 88, 1–4. [Google Scholar] [CrossRef] [PubMed]
  52. Heng, S.; Hardy, J.; Good, P. A retrospective audit on usage of Diatrizoate Meglumine (Gastrografin(®)) for intestinal obstruction or constipation in patients with advanced neoplasms. Palliat. Med. 2018, 32, 294–298. [Google Scholar] [CrossRef] [PubMed]
  53. Lee, Y.C.; Jivraj, N.; Wang, L.; Chawla, T.; Lau, J.; Croke, J.; Allard, J.P.; Stuart-McEwan, T.; Nathwani, K.; Bowering, V.; et al. Optimizing the Care of Malignant Bowel Obstruction in Patients with Advanced Gynecologic Cancer. J. Oncol. Pract. 2019, 15, e1066–e1075. [Google Scholar] [CrossRef]
  54. Lodoli, C.; Covino, M.; Attalla El Halabieh, M.; Santullo, F.; Di Giorgio, A.; Abatini, C.; Rotolo, S.; Rodolfino, E.; Giovinazzo, F.; Fagotti, A.; et al. Prognostic Factors for Surgical Failure in Malignant Bowel Obstruction and Peritoneal Carcinomatosis. Front. Surg. 2021, 8, 769658. [Google Scholar] [CrossRef]
  55. Jones, A.P.M.; McGauran, M.F.G.; Jagasia, N.; Hiscock, R.J.; Hyde, S.; Grant, P. Efficacy of dexamethasone in the management of malignant small bowel obstruction in advanced epithelial ovarian cancer. Support. Care Cancer 2022, 30, 2821–2827. [Google Scholar] [CrossRef] [PubMed]
  56. Cole, J.M.; Khan, S.Z.; Marks, J.M.; Armstrong, A.J.; Zanotti, K.M.; Juza, R.M. Enhanced gastric decompression for palliation of malignant bowel obstruction. Surg. Endosc. 2023, 37, 4000–4004. [Google Scholar] [CrossRef]
  57. Walter, M.; Hansen, E.; Hamid, S.; Carozza, D.; Mann, G.; Roche, C.; George, A.; Attwood, K.; Case, A. Palliative Management of Inoperable Malignant Bowel Obstruction: Prospective, Open Label, Phase 2 Study at an NCI Comprehensive Cancer Center. J. Pain Symptom Manag. 2024, 67, 20–26. [Google Scholar] [CrossRef] [PubMed]
  58. Peng, X.; Wang, P.; Li, S.; Zhang, G.; Hu, S. Randomized clinical trial comparing octreotide and scopolamine butylbromide in symptom control of patients with inoperable bowel obstruction due to advanced ovarian cancer. World J. Surg. Oncol. 2015, 13, 50. [Google Scholar] [CrossRef] [PubMed]
  59. Armbrust, R.; Chekerov, R.; Sander, S.; Biebl, M.; Chopra, S.; Krell, J.; Rinne, N.; Nixon, K.; Fotopoulou, C.; Sehouli, J. Surgery due to mechanical bowel obstruction in relapsed ovarian cancer: Clinical and surgical results of a bicentric analysis of 87 patients. Arch. Gynecol. Obstet. 2022, 305, 963–968. [Google Scholar] [CrossRef] [PubMed]
  60. DeBernardo, R. Surgical management of malignant bowel obstruction: Strategies toward palliation of patients with advanced cancer. Curr. Oncol. Rep. 2009, 11, 287–292. [Google Scholar] [CrossRef] [PubMed]
  61. Feuer, D.J.; Broadley, K.E.; Shepherd, J.H.; Barton, D.P. Systematic review of surgery in malignant bowel obstruction in advanced gynecological and gastrointestinal cancer. The Systematic Review Steering Committee. Gynecol. Oncol. 1999, 75, 313–322. [Google Scholar] [CrossRef]
  62. Clarke-Pearson, D.L.; Chin, N.O.; DeLong, E.R.; Rice, R.; Creasman, W.T. Surgical management of intestinal obstruction in ovarian cancer. I. Clinical features, postoperative complications, and survival. Gynecol. Oncol. 1987, 26, 11–18. [Google Scholar] [CrossRef]
  63. Pothuri, B.; Vaidya, A.; Aghajanian, C.; Venkatraman, E.; Barakat, R.R.; Chi, D.S. Palliative surgery for bowel obstruction in recurrent ovarian cancer:an updated series. Gynecol. Oncol. 2003, 89, 306–313. [Google Scholar] [CrossRef]
  64. Colombo, N.; Sessa, C.; du Bois, A.; Ledermann, J.; McCluggage, W.G.; McNeish, I.; Morice, P.; Pignata, S.; Ray-Coquard, I.; Vergote, I.; et al. ESMO-ESGO consensus conference recommendations on ovarian cancer: Pathology and molecular biology, early and advanced stages, borderline tumours and recurrent disease†. Ann. Oncol. 2019, 30, 672–705. [Google Scholar] [CrossRef]
  65. Krebs, H.B.; Goplerud, D.R. Surgical management of bowel obstruction in advanced ovarian carcinoma. Obstet. Gynecol. 1983, 61, 327–330. [Google Scholar] [PubMed]
  66. Mooney, S.J.; Winner, M.; Hershman, D.L.; Wright, J.D.; Feingold, D.L.; Allendorf, J.D.; Neugut, A.I. Bowel obstruction in elderly ovarian cancer patients: A population-based study. Gynecol. Oncol. 2013, 129, 107–112. [Google Scholar] [CrossRef] [PubMed]
  67. Suidan, R.S.; He, W.; Sun, C.C.; Zhao, H.; Ramondetta, L.M.; Badgwell, B.D.; Bodurka, D.C.; Lu, K.H.; Giordano, S.H.; Meyer, L.A. Treatment Patterns, Outcomes, and Costs for Bowel Obstruction in Ovarian Cancer. Int. J. Gynecol. Cancer 2017, 27, 1350–1359. [Google Scholar] [CrossRef] [PubMed]
  68. Furnes, B.; Svensen, R.; Helland, H.; Ovrebo, K. Challenges and outcome of surgery for bowel obstruction in women with gynaecologic cancer. Int. J. Surg. 2016, 27, 158–164. [Google Scholar] [CrossRef] [PubMed]
  69. Helyer, L.K.; Law, C.H.; Butler, M.; Last, L.D.; Smith, A.J.; Wright, F.C. Surgery as a bridge to palliative chemotherapy in patients with malignant bowel obstruction from colorectal cancer. Ann. Surg. Oncol. 2007, 14, 1264–1271. [Google Scholar] [CrossRef] [PubMed]
  70. Abu-Rustum, N.R.; Barakat, R.R.; Venkatraman, E.; Spriggs, D. Chemotherapy and total parenteral nutrition for advanced ovarian cancer with bowel obstruction. Gynecol. Oncol. 1997, 64, 493–495. [Google Scholar] [CrossRef]
  71. Patterson, M.; Greenley, S.; Ma, Y.; Bullock, A.; Curry, J.; Smithson, J.; Lind, M.; Johnson, M.J. Inoperable malignant bowel obstruction: Palliative interventions outcomes—Mixed-methods systematic review. BMJ Support. Palliat. Care 2024, 13, e515–e527. [Google Scholar] [CrossRef] [PubMed]
  72. Caceres, A.; Zhou, Q.; Iasonos, A.; Gerdes, H.; Chi, D.S.; Barakat, R.R. Colorectal stents for palliation of large-bowel obstructions in recurrent gynecologic cancer: An updated series. Gynecol. Oncol. 2008, 108, 482–485. [Google Scholar] [CrossRef]
  73. Pothuri, B.; Guirguis, A.; Gerdes, H.; Barakat, R.R.; Chi, D.S. The use of colorectal stents for palliation of large-bowel obstruction due to recurrent gynecologic cancer. Gynecol. Oncol. 2004, 95, 513–517. [Google Scholar] [CrossRef]
  74. Patel, P.S.; Fragkos, K.; Keane, N.; Wilkinson, D.; Johnson, A.; Chan, D.; Roberts, B.; Neild, P.; Yalcin, M.; Allan, P.; et al. Nutritional care pathways in cancer patients with malignant bowel obstruction: A retrospective multi-centre study. Clin. Nutr. ESPEN 2024, 59, 118–125. [Google Scholar] [CrossRef]
  75. Rami Reddy, S.R.; Cappell, M.S. A Systematic Review of the Clinical Presentation, Diagnosis, and Treatment of Small Bowel Obstruction. Curr. Gastroenterol. Rep. 2017, 19, 28. [Google Scholar] [CrossRef]
  76. Jadad, A.R.; Browman, G.P. The WHO analgesic ladder for cancer pain management. Stepping up the quality of its evaluation. JAMA 1995, 274, 1870–1873. [Google Scholar] [CrossRef] [PubMed]
  77. Branco, B.C.; Barmparas, G.; Schnüriger, B.; Inaba, K.; Chan, L.S.; Demetriades, D. Systematic review and meta-analysis of the diagnostic and therapeutic role of water-soluble contrast agent in adhesive small bowel obstruction. Br. J. Surg. 2010, 97, 470–478. [Google Scholar] [CrossRef] [PubMed]
  78. Galardi, N.; Collins, J.; Friend, K. Use of early gastrografin small bowel follow-through in small bowel obstruction management. Am. Surg. 2013, 79, 794–796. [Google Scholar] [CrossRef] [PubMed]
  79. Mercadante, S.; Ferrera, P.; Villari, P.; Marrazzo, A. Aggressive pharmacological treatment for reversing malignant bowel obstruction. J. Pain Symptom Manag. 2004, 28, 412–416. [Google Scholar] [CrossRef] [PubMed]
  80. Ferrell, B.R.; Temel, J.S.; Temin, S.; Smith, T.J. Integration of Palliative Care Into Standard Oncology Care: ASCO Clinical Practice Guideline Update Summary. J. Oncol. Pract. 2017, 13, 119–121. [Google Scholar] [CrossRef]
  81. Smith, T.J.; Temin, S.; Alesi, E.R.; Abernethy, A.P.; Balboni, T.A.; Basch, E.M.; Ferrell, B.R.; Loscalzo, M.; Meier, D.E.; Paice, J.A.; et al. American Society of Clinical Oncology provisional clinical opinion: The integration of palliative care into standard oncology care. J. Clin. Oncol. 2012, 30, 880–887. [Google Scholar] [CrossRef]
  82. Paradis, M. Towards evidence-based emergency medicine: Best BETs from the Manchester Royal Infirmary. BET 1: Is routine nasogastric decompression indicated in small bowel occlusion? Emerg. Med. J. 2014, 31, 248–249. [Google Scholar] [CrossRef]
  83. Fonseca, A.L.; Schuster, K.M.; Maung, A.A.; Kaplan, L.J.; Davis, K.A. Routine nasogastric decompression in small bowel obstruction: Is it really necessary? Am. Surg. 2013, 79, 422–428. [Google Scholar] [CrossRef]
  84. Frey, M.K.; Ellis, A.E.; Koontz, L.M.; Shyne, S.; Klingenberg, B.; Fields, J.C.; Chern, J.Y.; Blank, S.V. Ovarian cancer survivors’ acceptance of treatment side effects evolves as goals of care change over the cancer continuum. Gynecol. Oncol. 2017, 146, 386–391. [Google Scholar] [CrossRef]
  85. Paul Olson, T.J.; Pinkerton, C.; Brasel, K.J.; Schwarze, M.L. Palliative surgery for malignant bowel obstruction from carcinomatosis: A systematic review. JAMA Surg. 2014, 149, 383–392. [Google Scholar] [CrossRef] [PubMed]
Jcm 13 04213 g001
Figure 1. Pathogenesis of and points of intervention in MBO.
Figure 1. Pathogenesis of and points of intervention in MBO.
Jcm 13 04213 g001
Jcm 13 04213 g002
Figure 2. PRISMA flow diagram of the screening and selection process.
Figure 2. PRISMA flow diagram of the screening and selection process.
Jcm 13 04213 g002
Jcm 13 04213 g003
Figure 3. Therapeutic algorithm of MBO.
Figure 3. Therapeutic algorithm of MBO.
Jcm 13 04213 g003
Table 1. Basic characteristics of the studies.
Table 1. Basic characteristics of the studies.
Author, Year, GradePopulation, Study Design, Duration of Study, SurvivalInterventionOutcome MeasuresNotes/Side Effects
Castaldo et al. [26]; 1981419 patients with ovarian cc. (between 1968 and 1977); retrospective study; group 1—mean survival was 16 months; group 2—mean survival was 18 monthsgroup 1—intestinal surgery during their initial laparotomy; group 2—intestinal surgery during re-exploration, no symptoms; group 3—intestinal surgery during re-exploration, symptomaticgroup 1—pts discharged within 18 days due to infrequent complications; group 2—infrequent complications but major when occurred; group 3—major complicationspostoperative death; wound infection
wound dehiscence; recurrent SBO; sepsis; enterocutaneous fistula; pulmonary embolus; GI bleeding
Malone et al. [27]; 198610 patients with ovarian cc; retrospective study; between November 1984 and August 1985; mean survival was 35 dayspercutaneous gastrostomy symptom reduction—10/10 (100%); technical success rate—10/10(100%)1 leakage around tube, autodigestion of abdominal wall 1, pain 36 h 1, pyrexial 24 h 10/10 (100%)
Larson et al. [28]; 198933 patients with intestinal obstruction due to ovarian cc. (between 1980 and 1987); retrospective study; median survival time: 92 days without surgery and 102 days with surgerysurgical interventionsurvival time significantly related to the prognostic indexN/A
Lee et al. [29]; 199112 patients with gynaecological cancer: 10 ovarian, 1 endocervical, 1 endometrial; retrospective study; duration of study—N/A; OS—N/Ainterventional radiologysymptom reduction—12/12 (100%); technical success rate—12/12(100%)1 peritonitis, 3 leakage
Cunningham et al. [30]; 199520 patients with gynaecological cancer: 10 ovarian, 6 endometrial, 3 cervical, 1 peritoneal; retrospective study; between July 1989 and June 1993; mean OS was 70 daysinterventional radiologysymptom reduction—18/20; technical success rate—20/20 (100%)1 sepsis, 2 leakage
Cannizzaro et al. [31], 199522 patients—14 ovarian, 5 endometrial, 3 colon cc.; prospective study; duration of study was 1 year; mean OS was 74 days (13–272)endoscopysymptom reduction—21/21 (100%); technical success rate—21/22 (95.5%)1 spontaneous dislodgement, 1 persistent bloating, 1 mild site infection
Mangili et al. [32]; 199613 patients with gastrointestinal obstruction due to advanced ovarian cancer from January 1992 to May 1994; clinical trial; mean survival from discharge was 15 days (8/13 pts were discharged from the hospital); mean survival from the diagnosis of MBO was 27.1 days8 pts—nasogastric drainage and 6 received parenteral nutrition/ hydration; octreotide—a starting dose of 0.3 up to 0.6 mg (mean 0.44 mg) a day by subcutaneous bolus or continuous infusioncomplete relief of symptoms was achieved within 3.07 days (range 1 ± 6 days); vomiting stopped within 2 ± 3 days of starting treatment in most patients; in 8 pts with nasogastric tube, drainage decreased from 2000 to under 100 mL/day after the start of octreotide treatmentno side effects
Campagnutta et al. [33]; 199634 patients with gynaecological cancer: ovarian cc: 29 patients, endometrial cc: 2, uterine sarcoma in 2, and cervical carcinoma in 1; prospective study, not feasible for surgery34 endoscopy PEG27/32 (84.4%) symptomatic relief4 patients: nausea, vomiting
Hardy et al. [34], 1998patients with MBO due to ovarian cc.; trial 1: 25 pts; trial 2: 14 pts; combined: 39 pts; double-blind, placebo-controlled cross-over study; trial 1: 36-month period; trial 2: 24-month period; median overall survival (diagnosis to death) was
19 months		placebo (normal saline) or dexamethasone 4 mg intravenously (iv), every 6 h for five daysresolution of the bowel obstruction at day 5; response rate: trial 1: 15/22; trial 2: 6/13; combined: 21/35 (60%)unpleasant perianal sensation
Gadducci et al. [35]; 199867 patients with epithelial ovarian cancer (between 1989 and 1997), 50.7% developed intestinal obstruction during the study; retrospective study; between 1989 and 1997; median survival was 23 months22 patients: surgical interventions: - gastrostomy; jejunostomy; ileostomy; partial gastric resection; ileal resection; right or left colon resection; Hartman procedure; Sigmoid colostomy; transverse colostomy; ureter resection; ileo-ileal by-pass; 12 patients conservative therapyfrom the 22 pts, 10 underwent further chemotherapy: died after a median interval of 275 days; the other 12 pts did not receive chemotherapy: died after a median interval of 45 days; 2 pts underwent further surgery for obstruction: died within 30 dayscardiovascular complications, bowel perforation, DIC, hematemesis, AML, cachexia
Philip et al. [36]; 199933 patients with MBO due to gynaecological cc. (mostly ovarian cc.); prospective cohort study; between 30 January 1994 and 30 January 1995; mean survival of the responding pts was 39 daysdexamethasone: 8 mg/day iv/sc 8 mg/day divided doses9 pts (69%) had a response—decreased pain, nausea, and vomiting and improved oral intake (31 days)patient 11: reduced dose because of mild proximal myopathy affecting the lower limbs
Mercadante et al. [37]; 200018 patient with inoperable bowel obstruction due to ovarian, vulva, rectum, pancreas, breast, stomach, liver, small bowel cc.; randomised controlled trial (RCT); OS—N/A; duration of study—N/Aoctreotide (OCT) 0.3 mg daily vs. hyoscine butylbromide (HB) 60 mg dailysymptom relief within 24 h—OCT > HBincreased fluid intake correlated with less nausea
Brooksbank et al. [38]; 200251 patients—16 ovarian; retrospective study; between 1989 and 1997; median OS was 17 days46 endoscopy, 4 laparotomy, 1 interventional radiologysymptom reduction—47/51 (92%), technical success rate—endoscopy 46/ 48 (96%), total 51/51 (100%)1 hematoma, 6 leakage
Pothuri et al. [39]; 200594 patients with ovarian cancer; retrospective study; between 1995 and 2002; median OS was 8 weeks (95% CI, 6–10)92 endoscopy, 2 interventional radiologysymptom reduction—86/94 (91%), technical success rate—94/94 (100%)1 peritonitis, 8 leakage, 3 site infection, 3 blockage, 2 catheter malfunction, 2 bleeding
Matulonis et al. [40]; 200515 patients with MBO due to recurrent ovarian cancer; clinical pilot study; between 2002 and 2004; mean survival was 226 days,
median survival was 89 days		100 μg OCT subcutaneously, followed by 30 mg LAR intramuscularlycomplete symptom relief within 3.07 days, vomiting stopped within 2–3 daysno significant toxicities
Mangili et al. [23]; 200547 patients with intestinal obstruction due to recurrent epithelial ovarian cancer; retrospective study; duration of study—N/A; mean survival from the diagnosis of MBO was 79 days27 patients—surgery (21 intestinal procedures, 2 gastrostomy tubes, 4 pts inoperable), 20 patients received octreotide (mean dosage of 0.48 mg/day), from which 1 patient required nasogastric tubeoctreotide—controlled vomiting in all cases (except 1: NGT), complete symptom relief within 3 days; Surgery—16 of 21 pts (76%) tolerated low-residue diet 18% surgical correction not possible (mesentery infiltration); 22% complications: wound infection, dehiscence, fistula; oct-1 patient—fistula
Chi et al. [41]; 200926 patient with MBO due to ovarian cc.; prospective study; between July 2002 to July 2003; survival time: operative procedure: 191 days, endoscopic procedure: 78 daysPEG, colonic stent, intestinal bypass, ileostomy, colostomy76% symptom relief3.8% death, 11.5 % major complications
Watari et al. [42]; 201222 patients with MBO due to cc.; Endometrial or cervical cc.: 6 pts, ovarian cc.: 12 pts, peritoneal cc.: 3 pts, endometrial-ovarian cc.: 1 pt; prospective study; between 2006 and 2009; OS—N/A300 μg/d OCT subcutaneously or intravenously as a continuous injection for 7 days + for another 7 days15 patients (68.2%) had a response of CC, and 3 patients (13.6%) had a response of PC, with an overall response rate (CC/PC) of 81.8%no side effects
Fotopoulou et al. [43]; 201337 patients with epithelial ovarian cc.; retrospective cohort study; between May 2003 and January 2012; median OS was 5.6 months; surgical intervention, stent placement, conservative therapyno significant differences in survival any major complications 19 (51%): sepsis 1, pulmonary embolism 2, peritonitis 4, pleural effusion 3, relaparotomy 12, anastomotic insufficiency 5, abscess, secondary wound healing, postoperative bleeding 2, intestinal perforation 1, rupture of abdominal wall closure 1; peritonitis 100% short small bowel syndrome
Rath et al. [44]; 201353 patients with ovarian cc.; retrospective study;
between 1/2002 and 12/2010; median OS was 46 days (2–736)		33 surgical, 13 interventional radiology, 6 endoscopysymptom reduction—49/53 (93%), technical success rate—53/53 (100%)9 blockage, 4 leakage, 5 site infection
Jutzi et al. [45]; 201432 patient with LBO and gynaecological malignancies (ovarian cc. 75%, uterine cc. 18,8%); retrospective cohort study; between January 2006 and February 2013; median survival time for all patients was 4.1 monthscolorectal stent placementclinical success 47%complication rate = 42%, 12 stent -related complications in 10 pts:—obstruction, stent migration, bowel perforation, rectal bleeding, rectovaginal fistula, diarrhoea
Perri et al. [46]; 201462 patients with gastrointestinal obstruction due to gynaecological (47) malignancies (ovarian (69.1%), primary-peritoneal (8.8%), cervical (11.8%), or uterine (10.3%)); retrospective study; between October. 2004 and January 2013; median postoperative survival was 106 dayscolostomy (26.5%), ileostomy (39.7%), colonic stent (1.5%), gastrostomy (7.3%), gastroenterostomy (5.9%), bypass/resection and anastomosis (19.1%)18 pts died prior to discharge within 3–81 days; bypass/resection and anastomosis: improved survival5 sepsis, 6 leak from anastomosis, 2 necrotizing fasciitis
Peng et al. [47]; 201597 patients with MBO due to advanced ovarian cancer; randomised controlled trial (RCT); between January 2010 and December 2013; OS—N/Aoctreotide (OCT) 0.3 mg/day vs. scopolamine butylbromide (SB) 60 mg/daysymptom relief within 24 h—OCT > SB N/A
Daniele et al. [48]; 201540 patients with MBO due to ovarian cancer; retrospective study; between October 2008 and January 2014; medical treatment group: median survival from MBO was 5,7 months; surgical treatment group: median survival from MBO was 13.6 months; 18 pts—medical treatment: morphine sulfate 60 mg, haloperidol 1.5 mg, OCT 0.3 mg, dexamethason 8 mg /d; 22 pts—surgerysymptom relief within 4 daysno side effects
Zucchi et al. [49]; 2016158 patients—96 ovarian, 13 colon, 8 endometrial, 41 other cc.; prospective study; between 2002 and 2012; Median OS was 57 days (4–472)endoscopysymptom reduction—110/142 (77%) complete, 12/142 (8%) controlled vomiting, technical success rate—142/158 (90%)3 dislodged, 20 site infection, 12 obstruction, 2 leakage, 3 bleeding, 1 catheter failure
Dittrich et al. [50]; 201776 patients—ovarian 24 (32%), colorectal 13 (17%), pancreatic 12 (16%), small intestine 5 (7%), gallbladder/biliary tract 5 (7%), gastric 4 (5%), breast 3 (4%), CUP 3 (4%), other 6 (8%); Retrospective studyendoscopy—PEGsignificant decrease of vomiting (p < 0.001)112 complications in 56 patients: stomal leakage (18/75 patients), mild wound pain (17/75), and tube occlusion (13/75) occurred most frequently
Miłek et al. [51]; 201713 patients with left half colon obstruction due to an inoperable metastatic ovarian cc.; prospective study; 2012–2014colorectal stent placementsuccessful decompression in 11 pts (85%)1 patient with stent migration (7.7% in 24 h), 1 outgrowth of the neoplasm beyond the upper edge of the stent and subsequent stricture of the intestine’s lumen (4 months)
Heng et al. [52]; 201871 patients (47 women): 24 (33.8%) with ovarian or primary peritoneal neoplasms, 14 (19.7%) bowel, 8 (11.2%) upper gastrointestinal, 5 (7%) pancreatic, 6 (8.5%) intra-abdominal neoplasms, 2 (2.8%) other neoplasms with intra-abdominal/peritoneal metastases, 12 (16.9%) other neoplasms without intra-abdominal/peritoneal metastases;
intestinal obstruction in 42 (59.2%) patients; retrospective study; between January 2013 and October 2015 (approximately 34 months), OS—N/A		50 mL Gastrografin—repeated small doses over several daysresolved occlusion in 84% after administration, 75% of these cases improving within the first 24 h10 patients (14%)—diarrhoea
Lee et al. [53]; 2019169 patients with MBO due to advanced gynaecological malignancies; retrospective cohort study; baseline program between 2014 and 2016, MBO program between 2016 and 2018; median OS: 141 days MBO program: 141 vs. baseline: 99surgery, chemotherapy, total parenteral nutrition, and supportive careshorter hospital length of stay in the MBO program group compared to the baseline groupN/A
Lodoli et al. [54]; 202176 patients with MBO due to gynaecological (67), GI (19), and other (12) malignancies; retrospective observational cross-sectional study; study time was 5 years (between 2014 and 2018); OS—N/Acolostomy 7.2%, ileostomy 62.3%, jejunostomy 30.4%, intestinal bypass, bowel resection, adhesiolysisSurgery achieved 77.5% 68% p.o. diet,
61.2% NPT, 49% hospice, 51% home		21.4% complication, 9.2% major
Jones et al. [55]; 202291 patients with epithelial ovarian cancer, partial or complete bowel obstruction; retrospective cohort study; between January 2005 and December 2016; median survival from the diagnosis of MBO was 3.8 monthsdexamethasone: median daily dose: 6–8 mg, twice daily; median total dose was between 26 and 40 mg89% (137 admissions); 44.8%—adequate symptom resolutionN/A
Armbrust et al. [49]; 202287 patients with ovarian cc.; retrospective cohort study; between 2012 and 2017; mean OS was 7.8 months5% colectomy or total colectomy, 46% small bowel resection, 12% primary anastomosisECOG status, platinum sensitivity, ascites  <  500 mL, the type of stoma and the number of anastomosis influenced the results42% TPN,
26% grade 3 complication, 13% secondary wound healing, 21% anastomotic leakages, transfusions (17%) or thromboembolic events, 30 d mortality—10% 30 d morbidity—74%
Cole et al. [56]; 202314 patients—8 gynaecologic, 3 colorectal, 1 bladder, 1 small bowel, 1 peritoneal serous; retrospective study; between November 2019 and July 2021; mean OS was 270 daysendoscopysymptom reduction—100%, technical success rate—100%N/A
Walter et al. [57]; 202417 patients (8 women) with MBO due to UG, GI, GYN, lung cancer; prospective study; between 21 October 2019 and 1 December 2021; overall median survival was 88.8 days; 6 months survival was 20%“triple therapy”: dexamethasone 4 mg BID, metoclopramide 10 mg Q6 and octreotide 300 mcg TID10 patients (66.7%)—deobstruction; resolution of the bowel obstruction or deobstruction was defined as, introduction of oral intake beyond sips of liquids with cessation of vomiting and or ability to remove
nasogastric tube (NGT) or tolerance of clamped venting gastrostomy tube
(GT), resumption of bowel movements		bradycardia in 2 pts, no incidence of bowel perforation
Abbreviations: NR: not reported, OS: overall survival, OC: ovarian cancer, EC: endometrial cancer, CC: cervical cancer, PC: peritoneal cancer, CRC: colorectal cancer, UC: uterine cancer, BC: bladder cancer, SB: small bowel, Gyn: gynaecologic malignancy, Pan.: pancreatic cancer.
Table 2. General characteristics of the articles regarding medical treatment.
Table 2. General characteristics of the articles regarding medical treatment.
AuthorStudy TypeMethodsOS (MD/MN)Symptom ReliefNotes/Side Effects
Hardy et al. [34] (1998)Double-blind, placebo-controlled, cross-overPlacebo or
DEX 4 × 4 mg/day iv, for five days
n = 39		570 days (MD)CR: 60%unpleasant perianal sensation
Philip et al. [36] (1999)Prospective cohortDEX: 8 mg/day iv/sc
n = 33		39 days (MN)OR: 69% mild proximal myopathy affecting the lower limbs
Mercadante et al. [37] (2000)Randomised controlled trialOCT 0.3 m/day vs.
HB 60 mg/day
n = 18		N/ACR in 24 h: OCT > HBincreased fluid intake correlated with less nausea
Mangili et al. [23] (2005)RetrospectiveOCT
n = 20		79 days (MN)CR: 95% in 3 daysone patient fistula
Matulonis et al. [40] (2005)Prospective interventional cohort study0.1 mg OCT sc,
+30 mg LAR im
n = 15		226 days (MN)CR in 3.07 daysno significant toxicities
Watari et al. [42] (2012)Prospective interventional cohortOCT: 0.3 mg/ days sc/iv for 7 + 7 days
n = 22		N/ACR: 68.2%
PR: 13.6%		no side effects
Daniele et al. [48] (2015)Retrospective observationalMS 60 mg/day,
HAL 1.5 mg/day,
OCT 0.3 mg/day,
DEX 8 mg/day;
n = 18		171 days (MD)CR 100% in 4 daysno side effects
Peng et al. [58] (2015)Randomised controlled trialOCT 0.3 mg/day
vs.
SB 60 mg/day
n = 97		N/ACR in 24 h: OCT > SBN/A
Heng et al. [52] (2018)Retrospective50 mL Gastrografin—repeated small doses over several days
n = 71 		N/ACR: 84%75% in 24 h10 patients (14%)—diarrhoea
Jones et al. [55] (2022)Retrospective cohortDEX: 2 × 6–8 mg/day;
n = 91		114 days (MD)CR: 44.8%N/A
Walter et al. [57] (2024)Prospective interventional cohort“triple therapy”:
DEX: 2 × 4 mg/day, MCP: 4 × 10 mg/day, OCT: 2 × 0.3 mg/day
n = 17		88.8 days (MD)CR: 66.7%bradycardia in two patients
Abbreviations: OCT: octreotide, SB: scopolamine butylbromide, HB: hyoscine butylbromide, LAR: lanreotide, MD: median, MN: mean, sc: subcutanenous, im: intramuscular, DEX: dexamethasone, MCP: metoclopramide, iv: intravenously, MS: morphine sulfate, HAL: haloperidol, CR: complete response, PR: partial response, OR: overall response.
Table 3. Studies evaluating gastrostomy outcomes in gynaecologic malignancies.
Table 3. Studies evaluating gastrostomy outcomes in gynaecologic malignancies.
AuthorStudy TypeMethod of
Gastrostomy Formation		Number of Cases and Cancer TypeOSSymptom ReliefDietNotes/Side
Effects		Technical Success
Malone et al. [27] (1986)RetrospectiveTranssectional radiologyn = 10
OC:10		Mean:
35 days (26–56)		10/10 (100%)NROA: 100%
Fever: 10 Leakage: 1 Abdominal wall autodigestion: 1
Pain for 36 h: 1 		10/10 (100%)
Lee et al. [29] (1991)RetrospectiveInterventional radiologyn = 12
OC: 10 CC: 1 EC: 1		NR12/12 (100%)NROA: 33%
Peritonitis: 1 Leakage: 3		12/12 (100%)
Cannizzaro et al. [31] (1995)ProspectiveEndoscopyn = 22
OC:14 EC: 5 CRC: 3		Mean 74 days (13–272)21/21 (100%)21/21 (100%)OA: 14%
Dislodgement: 1
Persistent bloating: 1 Mild site infection: 1		21/22 (95.5%)
Cunningham et al. [30] (1995)RetrospectiveInterventional radiology n= 20
OC: 10 EC: 6 CC: 3 PC: 1		Mean 70 days (3–173)18/20 (90%)12/20 (100%)OA: 15%
Sepsis: 1 Leakage: 2		20/20 (100%)
Campagnutta et al. [33] (1996)ProspectiveEndoscopy n = 34
OC: 29 EC: 2 UC: 2 CC: 1		Tube in place for median 74 days (5–210)27/32 (84%)27/32 (84%)OA: 6%
Mild site infections: 2		32/34 (94%)
Brooksbank et al. [38] (2002)RetrospectiveEndoscopy/ Laparotomy n = 51
CRC: 27 OC: 16 Other: 8		Median 17 days (1–190)47/51 (92%)NROA: 14%
Hematoma: 1 Leakage: 6		51/51 (100%)
Pothuri et al. [39] (2005)RetrospectiveInterventional radiologyn = 94
OC: 94		Median 8 weeks (95% CI, 6–10)86/94 (91%)89/92 (2 unknown) (97%)OA: 20%
Peritonitis: 1 Leakage: 8 Site infections: 3 Blockage: 3 Catheter malfunction: 2 Bleeding: 2		94/94 (100%)
Rath et al. [44] (2013)RetrospectiveEndoscopyn = 53
OC: 53		Median 46 days (2–736)49/53 (93%)48/53 (91%)OA: 34%
Blockage: 9 Leakage: 4 Site infections: 5		53/53 (100%)
Zucchi et al. [49] (2016)ProspectiveEndoscopy n = 158
OC: 96 CRC: 13 EC: 8 Other: 41		Median 57 days (4–472)110/142 (77%) complete 12/142 (8%) vomiting controlled110/142 (77%)OA: 26%
Dislodged: 3 Site infection: 20
Obstruction: 12
Leakage: 2 Bleeding: 3 Catheter failure: 1		142/158 (90%)
Dittrich et al. [50] (2017)RetrospectiveEndoscopyn = 76
OC: 26 CRC: 13 Pan.: 12 Other: 25 		Median 28 days (2–440)96% (73/75) vomiting 81% (62/75) nausea59/75 (79%)OA: 53%
Peritonitis: 3 Severe bleeding: 2
Repeated attempts: 7
Fever: 6
Leakage: 18 Wound infection: 9		68/76 (90%) primary 75/76 (99%) secondary
Cole et al. [56] 2022RetrospectiveEndoscopyn = 14
Gyn: 8 CRC: 3 BC: 1 SB: 1 PC: 1		Mean 270 days100%NRNR100%
Abbreviations: NR: not reported, OS: overall survival, OC: ovarian cancer, EC: endometrial cancer, CC: cervical cancer, PC: peritoneal cancer, CRC: colorectal cancer, UC: uterine cancer, BC: bladder cancer, SB: small bowel, Gyn: gynaecologic malignancy, Pan.: pancreatic cancer.
Table 4. Grading of used literature.
Table 4. Grading of used literature.
Author, YearMethodsGrade
Castaldo et al. [26]; 1981retrospective observationalIIIA
Malone et al. [27]; 1986retrospective observationalIIIA
Larson et al. [28]; 1989retrospective observationalIIIA
Lee et al. [29]; 1991retrospective observationalIIIA
Cunningham et al. [30]; 1995retrospective observationalIIIA
Cannizzaro et al. [31], 1995prospective single arm interventional studyIIA
Mangili et al. [32]; 1996retrospective observationalIIB
Campagnutta et al. [33]; 1996 prospective single arm interventional studyIIB
Hardy et al. [34]; 1998 prospective placebo-controlled cross-over studyIIIA
Gadducci et al. [35]; 1998retrospective observationalIIIA
Philip et al. [36]; 1999prospective cohortIIA
Mercadante et al. [37]; 2000randomised controlled trialIC
Brooksbank et al. [38]; 2002retrospective observationalIIIA
Mangili et al. [23]; 2005retrospective observationalIIIA
Matulonis et al. [40]; 2005prospective single-arm interventional studyIIC
Pothuri et al. [39]; 2005retrospective observationalIIIA
Chi et al. [41]; 2009prospective studyIIA
Watari et al. [42]; 2012prospective single-arm interventional studyIIA
Rath et al. [44]; 2013retrospective observationalIIIA
Fotopoulou et al. [43]; 2013retrospective observationalIIIA
Jutzi et al. [45]; 2014retrospective observationalIIIA
Perri et al. [46]; 2014retrospective observationalIIIA
Peng et al. [58]; 2015randomised controlled trialIB
Daniele et al. [48]; 2015retrospective observationalIIIA
Zucchi et al. [49]; 2016prospective single-arm interventional studyIIA
Dittrich et al. [50]; 2017retrospective observationalIIIB
Miłek et al. [51]; 2017prospective single-arm interventional studyIIB
Heng et al. [52]; 2018retrospective observationalIIIA
Lodoli et al. [54]; 2021retrospective observationalIIIA
Jones et al. [55]; 2022retrospective observationalIIIA
Armbrust et al. [59]; 2022retrospective observationalIIIA
Cole et al. [56]; 2023retrospective observationalIIIA
Walter et al. [57]; 2024prospective single-arm interventional studyIIA
Grading was performed according to the criteria set out by the NHS Executive in their Reviews on Commissioning Cancer Services.
Table 5. Treatment Strategies for Malignant Bowel Obstruction: Benefits and Drawbacks.
Table 5. Treatment Strategies for Malignant Bowel Obstruction: Benefits and Drawbacks.
Treatment MethodAdvantagesDisadvantages
Somatostatin analogues
Effective in symptom relief within 24 h to 4 days
Can be used long-term with minimal toxicity
Reduces bowel and pancreatic secretion
Requires continuous infusion or regular administration
May not be effective in all patients
Dexamethasone
Effective in symptom relief within 5 to 7 days
High success rates (around 89%)
Useful in cases of small bowel obstruction
Limited use in small bowel obstruction cases
Adverse events such as unpleasant perianal sensations in some patients
Diatrizoate meglumine
Effective in restoring bowel function (84% success rate)
If contrast material does not appear in the large bowel within 24 h, surgery is inevitable in 99% of cases
Percutaneous gastrostomy
Feasible in very vulnerable patients
Good symptom control
Leads to short bowel syndrome, requiring total parenteral nutrition
Not suitable for patients with multiple obstructions
Stent placement
High success rate for implantation
Relatively low chance of requiring further surgical intervention
Prolonged survival in certain cases
Recommended mainly for large bowel or duodenal obstructions
Less effective if multiple obstructions are present
Surgical interventions
Provides definitive relief from obstruction
Prolonged symptom-free periods
High morbidity and mortality rates
Not suitable for all patients, especially those with poor overall health
Disclaimer/Publisher’s Note: The statements, opinions and data contained in all publications are solely those of the individual author(s) and contributor(s) and not of MDPI and/or the editor(s). MDPI and/or the editor(s) disclaim responsibility for any injury to people or property resulting from any ideas, methods, instructions or products referred to in the content.

Share and Cite

MDPI and ACS Style

Tóth, R.; Tóth, Z.; Lőczi, L.; Török, M.; Ács, N.; Várbíró, S.; Keszthelyi, M.; Lintner, B. Management of Malignant Bowel Obstruction in Patients with Gynaecological Cancer: A Systematic Review. J. Clin. Med. 2024, 13, 4213. https://doi.org/10.3390/jcm13144213

AMA Style

Tóth R, Tóth Z, Lőczi L, Török M, Ács N, Várbíró S, Keszthelyi M, Lintner B. Management of Malignant Bowel Obstruction in Patients with Gynaecological Cancer: A Systematic Review. Journal of Clinical Medicine. 2024; 13(14):4213. https://doi.org/10.3390/jcm13144213

Chicago/Turabian Style

Tóth, Richárd, Zsófia Tóth, Lotti Lőczi, Marianna Török, Nándor Ács, Szabolcs Várbíró, Márton Keszthelyi, and Balázs Lintner. 2024. "Management of Malignant Bowel Obstruction in Patients with Gynaecological Cancer: A Systematic Review" Journal of Clinical Medicine 13, no. 14: 4213. https://doi.org/10.3390/jcm13144213

Note that from the first issue of 2016, this journal uses article numbers instead of page numbers. See further details here.

Article Metrics

Back to TopTop