Next Article in Journal
Energy Efficiency in Historic Architecture: The “Ex Institute of Zoology and Comparative Anatomy” in Palermo
Next Article in Special Issue
Modified Periosteal Inhibition (MPI) Technique for Immediate Implants: A Multi-Center Retrospective Case Series Study
Previous Article in Journal
Enhancing Molten Sulfur Filtration during Sulfuric Acid Manufacturing for Phosphate Fertilizer Production in Morocco with Cellulose-Based Filter Aids
Previous Article in Special Issue
In Vitro Evaluation of Antibacterial and Antibiofilm Activity of Different Chlorhexidine-Containing Mouthwash Formulations against Streptococcus mutans
 
 
Search for Articles:
Title / Keyword
Author / Affiliation / Email
Journal
Article Type
 
 
Advanced Search
 
Section
Special Issue
Volume
Issue
Number
Page
 
Journals
Applied Sciences
Volume 13
Issue 15
10.3390/app13158880
applsci-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:
Review

Photobiomodulation as a Therapeutic Strategy in Burning Mouth Syndrome: A Scoping Review

by
Francesco Spadari
1,2,
Federica Pulicari
1,2,*,
Martina Ghizzoni
3,
Massimo Porrini
1,2,
Moreno Bosotti
1,2 and
Matteo Pellegrini
1,2,*
1
Department of Biomedical Surgical and Dental Sciences, University of Milan, 20122 Milan, Italy
2
Maxillo-Facial and Odontostomatology Unit, Foundation IRCCS Ca’ Granda Ospedale Maggiore Policlinico, 20122 Milan, Italy
3
Section of Dentistry, Department of Clinical, Surgical, Diagnostic and Pediatric Sciences, University of Pavia, 27100 Pavia, Italy
*
Authors to whom correspondence should be addressed.
Appl. Sci. 2023, 13(15), 8880; https://doi.org/10.3390/app13158880
Submission received: 9 May 2023 / Revised: 6 July 2023 / Accepted: 31 July 2023 / Published: 1 August 2023
(This article belongs to the Special Issue Current Advances in Dentistry)
Browse Figure
Versions Notes

Abstract

:
Burning mouth syndrome (BMS) is considered an atypical oral clinical-symptomatological condition because its etiopathogenesis is not yet fully clarified. It is mainly characterized by the symptom of burning, which occurs chronically and with various intensities. It is essential for making a diagnosis of BMS, clinical negativities, and instrumental investigations. It mainly affects the female sex, in the pre-post-climactic phases. A peripheral neuropathic matrix of the pain symptoms has been repeatedly demonstrated. However, this subjectivity is associated with personalities with anxiety-depressive traits, affective-behavioral difficulties, and disorders of the psycho-algogenic sphere. Numerous treatments are reported in the literature, which have rarely met lasting healing parameters. In this clinical landscape, photobiomodulation therapy (PBMT) can be considered a possible therapeutic alternative. Our study aims to present a scoping review of how photobiomodulation is used in BMS therapy and to analyze the outcome of the therapy. A literature review focused on the photobiomodulation treatment for burning mouth syndrome was conducted in the main scientific databases: PubMed, SCOPUS, and Web of Science. The results of our research highlight encouraging results regarding photobiomodulation, as in all studies, there is a reduction in symptoms.

1. Introduction

Burning mouth syndrome (BMS) is categorized as an idiopathic oral condition due to its yet-to-be-fully-understood etiology and pathogenesis, along with its atypical symptomatology and clinical characteristics [1,2,3]. In 1994, the International Association for the Study of Pain (IASP) identified three distinct groups of chronic oral and facial pain with neurogenic, vascular, and idiopathic origins.
Subsequently, the Headache Classification Committee of the International Headache Society (IHS) in 2013 and 2018, along with the International Classification of Orofacial Pain (ICOP) in 2020, defined BMS as “Intraoral burning or dysaesthesia sensation, recurring daily for more than 2 h per day over more than 3 months, without clinically evident causative lesions”. A diagnosis of BMS is confirmed when individuals report oral burning symptoms without any observable clinical signs, and diagnostic investigations reveal a normal condition [2,3,4].
When oral symptomatology has a definable local and systemic cause, and locally there are clinical signs or instrumental tests that testify to a disease, it is correct to speak of secondary BMS [5,6].
Factors that can cause intraoral burning include iron, zinc, vitamin B12 or folic acid deficiencies, pharmacological causes, hyposalivation, Sjögren’s syndrome, erosive and ulcerative lesions of the mucosa, oral infections, inappropriate prostheses, and para-functional habits [5,6]. When we have an oral burning pain condition, without clinical signs and with an unknown origin, we will speak instead of primary BMS or idiopathic BMS [6,7,8].
The various etiological and pathophysiological aspects would lead to considering primary BMS as a complex multifactorial clinical condition, although it has also been associated with psychological and endocrinological disorders [9,10,11,12].
In the late 1980s, neurophysiological, neuropathological, and imaging studies led to the hypothesis that BMS could be a neuropathic pain condition [13,14,15,16]. Therefore, we can consider at least three lines of research that have characterized the studies on the etiology and pathogenesis of idiopathic BMS: a peripheral and central neurological basis, and an endocrinological and psychological matrix [8]. The pathophysiology of BMS is still unknown [8].
Three distinct subclasses of primary burning mouth syndrome (BMS) can be identified. The first subgroup (50–65%) is characterized by peripheral neuropathy affecting the small diameter fibers of the intra-oral mucosa. The second subgroup (20–25%) comprises patients with subclinical trigeminal lingual nerve system pathology, which clinically resembles the other two subgroups. The third subgroup (20–40%) aligns with the concept of central pain, potentially linked to the reduced function of dopaminergic neurons in the basal ganglia [8]. The development of neuropathic pain in primary BMS is thought to be closely related to small fiber damage. Recent studies in primary BMS have emphasized the role of small myelinated Aδ fibers and unmyelinated C fibers [15,17,18]. Additionally, approximately 50% of patients with primary BMS experience significant pain relief after lidocaine anesthesia of the lingual nerve, suggesting a peripheral origin of the pain [18]. The taste and pain neurological circuits appear to be intricately interconnected. Damage to the chorda tympani results in the inhibition of its function, leading to reduced control over the activity of other nerves. Consequently, deafferentation of the Aδ gustatory fibers of the chorda tympani nerve may result in lingual burning pain symptoms [19,20]. Alternatively, the diminished signaling of Aδ channels with preserved C-fiber function could also contribute to the burning pain experienced in primary BMS [8,21].
Patients with BMS often report dysgeusia or phantom taste sensations. [8,21,22,23,24,25]. In the pathogenesis of primary BMS, the possible involvements of the central nervous system related to the sensorium of the mouth and face regions have been considered [26,27]. Alterations in the basal ganglia would cause signs of dopaminergic system dysfunction, like Parkinson’s disease, and bilateral oral pain distribution. The dopaminergic system has a pain-inhibitory role [25,26,27,28,29,30]. The blink reflex habituation, reflecting depletion of endogenous dopamine in the putamen, as is usually seen in Parkinson’s disease, suggests the hypothesis that ineffective endogenous inhibitory pain control by the brain dopamine-opioid system predisposes the individual patient to chronic neuropathic pain [27,28]. Furthermore, patients with primary BMS report similar benefits from sleep duration as those with Parkinson’s disease, due to increased brain dopamine tone during nighttime sleep. Also, patients diagnosed with major depression reported BMS, and this pathology has been associated with decreased brain dopamine. Genetic studies provide other insights into low brain dopamine tone in the etiology of BMS. The C957T dopamine D2 receptor polymorphism affects D2 receptor function in the striatum and influences the synaptic concentration of endogenous dopamine; homozygotes for the T allele have the lowest dopaminergic tone in the striatum and appear to be more common in patients with facial neuropathic pain, including primary BMS T alleles that are also found in patients with facial neuropathic pain, including primary BMS [29,30,31,32]. Sex hormones have neuroprotective effects and modulate the function of various neurotransmitters and peripheral receptors [33,34]. In 2009, it was highlighted that in subjects after menopause, there was a deficiency or dysfunction of adrenal steroids with decreased neuroprotective effects on neural tissues [13]. It has been seen that a deficiency of ovarian hormones would lead to an atrophy of the lining epithelia, including the lingual and oral ones. Interestingly, this epithelial atrophy was observed in parallel with the reduction of unmyelinated C fibers [35,36,37]. The high prevalence of anxiety disorders and depression seen in BMS is associated with a history of chronic post-traumatic stress and chronic major anxiety leading to impaired adrenal steroid production. Among the various dysfunctional pain disorders, BMS is characterized by underlying hypercortisolism [38,39,40], which reaches 70% in primary BMS [41]. Initially, it was thought that dry mouth was only a subjective impression of BMS patients and not due to reduced actual salivary flow. However, it was possible to confirm that, compared to healthy subjects, the salivary flow was slightly reduced when unstimulated and did not change when stimulated with lemon [42]. It has been hypothesized that neuroprotective steroid deficiency leads to reduced function of the minor salivary glands and contributes to the induction of xerostomia. It has been confirmed that alterations of the emotional-instinctive and psycho-anxiety dimensions are conditions commonly encountered in BMS patients. However, no significant differences were found between the emotional and psychological characteristics of BMS patients and chronic pain patients [31,43,44,45,46]. Interestingly, most of the psychiatric and personality disorders associated with BMS have low brain dopamine tones in common. [47,48,49,50,51]. The purpose of our scoping review is to investigate whether photobiomodulation can be useful in the treatment of the disease and which protocols have been studied up to now.

2. Materials and Methods

2.1. Focused Questions

Can photobiomodulation be useful in the treatment of burning mouth syndrome? What are the protocols used in photobiomodulation therapy?

2.2. Eligibility Criteria

This review followed specific inclusion and exclusion criteria. The inclusion criteria were as follows: (I) the study model should be interventional studies, observational studies, cohort studies, or case series/case reports studies; (II) participants must be diagnosed with burning mouth syndrome; (III) the intervention under investigation should be photobiomodulation; and (IV) the outcome of interest should be clinical results for neuropathic pain treatment. Only studies that met all these inclusion criteria were considered in the review.
On the other hand, certain studies were excluded based on the following exclusion criteria: (I) articles published in non-English languages that were available only in abstract form; (II) duplicate studies that were identical or substantially overlapped with other included studies; (III) studies not relevant to the purpose of the full-text articles, or not suitable for addressing the focused questions, such as those analyzing different supplementary treatments or whose content did not match the abstract; (IV) ex vivo or experimental animal studies, which did not involve human participants; (V) studies lacking approval from an ethics committee; and (VI) narrative reviews, systematic reviews, or systematic and meta-analysis reviews, which were not in the scope of this particular review.

2.3. Search Strategy

In accordance with the JBI methodology for scoping reviews, the research process involved three main steps: (i) an initial limited search conducted on databases like PubMed (MEDLINE), Scopus, and Web of Science; (ii) selection of key terms from the retrieved articles to create an effective search strategy; and (iii) an additional search of the reference lists of all included articles to identify further relevant research.
Furthermore, the review followed the PCC model, which revolves around three essential elements: population (individuals undergoing PBMT procedures), concept (PBMT as a treatment for neuropathic pain), and context (without restricting the review to any specific cultural aspect or setting). The review focused on analyzing the abstracts of studies that examined the effects of photobiomodulation procedures and their clinical outcomes.
Throughout the literature review process, the preferred reporting items for scoping reviews (PRISMA-ScR) consensus guidelines were adhered to (see Table S1, Supplementary Materials).

2.4. Research

The Medical Subject Heading (MeSH) terms used for the search included burning mouth syndrome, stomatopyrosis, photobiomodulation, photobiomodulation therapy, and low-level laser therapy. An electronic search was conducted on PubMed (MEDLINE), Scopus, and Web of Science databases, focusing on articles published between 2010 and 2023. The data extraction phase took place from February 2023 to April 2023, with the last search performed on 15 April 2023.
Four reviewers (F.P., M.Po., M.G., and M.Pe.) carried out the search, and any disagreements or discrepancies were resolved through consensus, with input from two additional reviewers (F.S. and M.B.). Titles and abstracts of the initially retrieved articles were thoroughly analyzed, and studies that were not relevant were excluded. Full texts of all relevant articles were reviewed and scrutinized, with findings documented, and similar studies meeting the inclusion criteria were identified. The present protocol has been registered on the Open Science Framework platform with the registration https://osf.io/a9hqu (accessed on 8 May 2023). The detailed strategies employed for each electronic database search are presented in Table S2 (Supplementary Materials).

2.5. Quality Assessment of Included Studies

A methodological quality risk of bias assessment was used in this review, JBI critical appraisal for randomized controlled trials.

3. Results

The primary search identified 186 articles based on MeSH terms. Following this, 160 articles were removed (5 abstracts of articles published in non-English languages, 98 duplicates, and 57 because they were not pertinent), and 26 articles were screened based on title and abstracts. The remaining 15 full-text articles were assessed for eligibility. Additionally, 4 full-text articles were further excluded because they were irrelevant articles. The 11 relevant articles were finally included and analyzed in this review. The flow chart of the review process is described in Figure 1.

Risk of Bias

The JBI critical appraisal tool was applied to assess the risk of bias in the studies included in this review (Table 1), using the judging criteria for risk of bias shown in Table S3 (Supplementary Materials).

4. Discussion

The response to treatment in patients with primary BMS is influenced by various pathological factors, including neuropathic components, central vulnerability, and psychiatric comorbidity. These problems are often intricate and interconnected, and addressing them requires a comprehensive approach rather than relying on a single therapy [50]. Like other neuropathic pain conditions, BMS poses challenges in treatment. On average, only 40% of patients experience benefits from their current neuropathic pain medications [51].
Another issue related to BMS treatment is the lack of consistent and continuous medication usage. While psychotropic medications show effectiveness in BMS treatment, approximately 15% of patients discontinue their medication. Implementing motivational interviewing can enhance appropriate adherence to medication [52,53]. Often, a combination of medications is recommended, along with treatments utilized for other neuropathic pain conditions [52,53]. Tricyclic antidepressants such as amitriptyline and clomipramine have been tried for BMS, with only 19% of patients reporting very poor outcomes and side effects such as dry mouth [54,55]. Antidepressants belonging to the group of selective serotonin reuptake inhibitors (SSRIs) such as chlordiazepoxide, diazepam, amisulpride, paroxetine, or sertraline hydrochloride have also been recommended with good results, but with the most side effects such as dizziness, insomnia, nausea, and somnolence [54,55].
Trazodone was not effective in improving BMS symptoms [56]. Anticonvulsants such as gabapentin and pregabalin are routinely recommended in the pharmacotherapy of BMS, but therapeutic success has not been achieved [55,56]. Systemic and local treatment with clonazepam should be considered in the treatment of BMS.
Clonazepam is a benzodiazepine and a γ-aminobutyric acid (GABA) receptor agonist. This receptor is widely present in the central nervous system and peripheral tissues, and this drug acting on this receptor may have positive results in the treatment of this syndrome [55,56,57,58]. Pure small-fiber peripheral neuropathy may be better controlled with local clonazepam and central mechanisms may benefit more from systemic clonazepam [55,56,57,58]. Clonazepam, like other benzodiazepines, can cause side effects, mainly drowsiness, impairment of memory and cognitive functions, and dependence on long-term use. Although systemic absorption is low, no side effects have been reported with topical application [55,56,57,58].
α-lipoic acid (ALA) has been used to treat diabetic neuropathy because it is thought to act as a com- and coenzyme, produce energy (ATP), improve glucose metabolism and stimulate nerve growth factor (NGF) production. In addition, ALA stimulates the elevation of cellular glutathione levels and may prevent peripheral neuropathy [59,60,61,62,63].
There have been indications for the use of capsaicin in the pharmacological management of burning pain. Capsaicin induces desensitization and depletion of substance P leading to analgesia. A double-blind cross-over study revealed that a 0.025% capsaicin mouth rinse significantly reduced pain with no side effects [63,64,65,66]. Additionally, various topical treatments, such as saliva substitutes, may be helpful when a peripheral mechanism is suspected [66].
To talk about photobiomodulation, it is necessary to start from the assumption that light is a type of electromagnetic radiation and is considered an indispensable source of energy. A photochemical reaction is normally induced by the interaction of light, particularly ultraviolet, visible, and near-infrared light, with external matter. There are numerous examples of interactions between light and biological systems: photosynthesis; the reactions of the photoreceptors of the retina; the synthesis of vitamin D [67].
Since 2015, we have been talking about photobiomodulation (PBM) to describe the scientific basis of the use of non-ionizing electromagnetic energy to trigger photochemical changes within cellular structures and tissues [68].
PBM has analgesic and anti-inflammatory therapeutic effects, can stimulate biological tissues, and has documented antimicrobial effects [68].
Therefore, the correct use of the PBM can relieve painful symptoms, significantly reduce an inflammatory process, and accelerate and improve the healing of damaged tissues [69].
The mechanism of action of PBM is not yet fully understood. The most popular theory is that light is absorbed by mitochondrial cytochrome C oxidase (CcOx), causing an increase in adenosine triphosphate (Adenosine TriPhosphate ATP) [69,70].
PBM, on the other hand, can induce a brief rise in reactive oxygen species (ROS) before decreasing oxidative stress. Nitric oxide (NO) competes with oxygen and binds to CcOx in cells with varying degrees of hypoxia, limiting oxygen use and thus mitochondrial cell respiration. PBM may restore this inhibition by dissociating NO from its binding location on CcOx, allowing mitochondria to enhance ATP synthesis and cellular energy [69,70].
Another possible mechanism of PBM could be an increase in the concentrations of Ca2+ ions, important for cellular metabolism and homeostasis, and cellular signal transmissions. Furthermore, the cellular temperature changes after a PBM must be considered [67,68,69,70,71,72,73].
PBM is not considered a heat treatment; however, selective absorption by CcOx can lead to intracellular thermal micro-changes that can positively influence the behavior of cells and tissues [73,74].
The analgesic properties of PBM have been repeatedly recognized. It has been seen to reduce chronic low back pain, chronic neck pain, and other types of chronic pain such as BMS [49,74,75,76,77,78,79].
Furthermore, at the oral level, it has proved to be useful in preventing and treating oral mucositis in cancer patients, in reducing pain and swelling after third molar extraction, in suffering from the temporomandibular joints, in orthodontic pain, and in reducing inflammation of the oral lichen [49,80,81,82,83,84,85,86,87,88].
Primary BMS is to be considered a chronic oral pain pathology where PBM could perform a part of the new local therapeutic strategies. Indeed, in recent years, with the diagnostic and cognitive advances of the disease, PBM has emerged as a potential non-invasive treatment with no apparent side effects.
Many therapeutic experiences have provided encouraging results in the reduction of oral burning symptoms. However, further therapeutic experiences will be needed to confirm and better protocol PBM treatments and correctly relate them to the clinical and symptomatic data of patients with BMS [57,58,59,60].
In the analysis of the results in the literature, there are some studies where an improvement in pain symptoms in patients with BMS has been found. Sleep values were compared and measured with the VAS and the improvement rates ranged from 4 to 15% [58,59,62].
The study conducted by Scardina et al. highlights the improvement in microcirculatory patterns after photobiomodulation was applied in patients with BMS, analyzed by videocapillaroscope. The improvement of the pattern has been noticed lasting for a long time after the therapy [56].
As regards the parameters used by the authors of the articles analyzed, the wavelengths used are variable, from a minimum of 685 nm [55] to a maximum of 1064 nm [38] with a preference; however, for the wavelength of 810–830 nm [52,53,54,56,57,59,62]. All the studies confirm the improvement of the symptoms. For the evaluation of the symptoms, the OHIP-14 questionnaires and the VAS scale were mainly used [52,53,54,55,56,57,58,59,60,61,62]. In fact, all the studies report an improvement in VAS scale values and OHIP values, especially after almost three applications of photobiomodulation. The follow-up shows a prolonged analgesic effect, which was found by Hanna et al., even nine months after discontinuation of treatment. In all studies, the absence of side effects of photobiomodulation is highlighted, even in follow-ups. The therapy is well accepted by the patients and easy to perform for the operator. Finally, it should be noted that the results of the improvement in the quality of life are recorded on average after seven weeks of application of the therapy, with an average of one session per week.
Table 2 shows the results of the literature review that satisfies the proposed research questions are summarized.

5. Conclusions

Various treatment options for BMS exist, but their efficacy based on evidence-based research remains unsatisfactory due to the diversity of studies and treatments employed. Among the treatments investigated, clonazepam and ALA have shown promising results in multiple studies, but further research with larger sample sizes is required to establish them as a first-line treatment for BMS patients. Notably, some studies have demonstrated similar outcomes between treatment and placebo evaluations, emphasizing the importance of exploring the psychological and/or psychiatric characteristics of patients. A multidisciplinary approach may be necessary for addressing BMS treatment. Photobiomodulation represents a potential therapeutic strategy for managing burning mouth symptoms. However, further investigation is warranted to fully understand its effectiveness in BMS treatment. Numerous studies on patients confirm that laser treatment can alleviate symptoms, with long-lasting effects. The advantages of this therapy are the easy execution by the clinician, the lack of adverse effects, and the good compliance by the patient. Despite this, it should be emphasized that it would be advisable to conduct future studies on larger patient samples; to standardize the operating protocols both in terms of therapeutic sessions, wavelengths to be used, and tests necessary to formulate a diagnosis precise; and correct classification of the symptomatology.

Supplementary Materials

The following supporting information can be downloaded at: https://www.mdpi.com/article/10.3390/app13158880/s1, Table S1: PRISMA-ScR Checklist; Table S2: Search strategies for electronic databases; Table S3: JBI critical appraisal checklist for randomized controlled trials, a tool used for risk of bias assessment.

Author Contributions

Conceptualization, F.S.; methodology, F.S.; software, M.P. (Matteo Pellegrini); validation, M.P. (Matteo Pellegrini), F.P. and M.P. (Massimo Porrini); formal analysis, M.P. (Massimo Porrini); investigation, F.P.; resources, M.G.; data curation, M.B.; writing—original draft preparation, F.S.; writing—review and editing, F.P.; visualization, M.B.; supervision, F.S.; project administration, M.P. (Matteo Pellegrini). All authors have read and agreed to the published version of the manuscript.

Funding

This research received no external funding.

Institutional Review Board Statement

Not applicable.

Informed Consent Statement

Not applicable.

Data Availability Statement

Upon request to the corresponding author, the data are available for use. The protocol of the review was registered with the Open Science Framework (OSF) with https://osf.io/a9hqu (accessed on 8 May 2023) and registered from osf.io/svkgn.

Conflicts of Interest

The authors declare no conflict of interest.

References

  1. Merskey, H.; Bogduk, N. Classification of Chronic Pain: Descriptions of Chronic Pain Syndromes and Definitions of Pain Terms, 2nd ed.; IASP Task Force on Taxonomy; IASP: Washington, DC, USA, 1994. [Google Scholar]
  2. Headache Classification Committee of the International Headache Society (IHS). The International Classification of Headache disorders, 3rd edition (beta version). Cephalalgia 2013, 33, 629–808. [Google Scholar] [CrossRef] [PubMed] [Green Version]
  3. Headache Classification Committee of the International Headache Society (IHS). The International Classification of Headache Disorders, 3rd edition. Cephalalgia 2018, 38, 1–211. [Google Scholar] [CrossRef] [PubMed]
  4. Orofacial Pain Classification Committee of the International Headache Society (IHS). International Classification of Orofacial Pain, 1st edition (ICOP). Cephalagia 2020, 40, 129–221. [Google Scholar] [CrossRef] [Green Version]
  5. Nasri-Heir, C. Burning mouth syndrome. Alpha Omega 2012, 105, 76–81. [Google Scholar]
  6. Scala, A.; Checchi, L.; Montevecchi, M.; Marini, I.; Giamberardino, M. Burning mouth syndrome: Overview and patient management. Crit. Rev. Oral Biol. Med. 2003, 14, 275–291. [Google Scholar] [CrossRef] [Green Version]
  7. Jääskeläinen, S.K.; Woda, A. Burning mouth syndrome. Cephalalgia 2017, 37, 627–647. [Google Scholar] [CrossRef] [Green Version]
  8. Jääskeläinen, S.K. Pathophysiology of primary burning mouth syndrome. Clin. Neurophysiol. 2012, 123, 71–77. [Google Scholar] [CrossRef]
  9. Van der Ploeg, H.M.; van der Wal, N.; Eijkman, M.A.; van der Waal, I. Psychological aspects of patients with burning mouth syndrome. Oral Surg. Oral Med. Oral Pathol. 1987, 63, 664–668. [Google Scholar] [CrossRef]
  10. Davies, S.; Underhill, H.C.; Abdel-Karim, A.; Christmas, D.M.; Bolea-Alamanac, B.M.; Potokar, J.; Herrod, J.; Prime, S.S. Individual oral symptoms in burning mouth syndrome may be associated differentially with depression and anxiety. Acta Odontol. Scand. 2016, 74, 155–160. [Google Scholar] [CrossRef] [PubMed]
  11. Umezaki, Y.; Miura, A.; Watanabe, M.; Takenoshita, M.; Uezato, A.; Torihara, A.; Nishikawa, T.; Toyofuku, A. Oral cenesthopathy. Biopsychosoc. Med. 2016, 10, 20. [Google Scholar] [CrossRef] [Green Version]
  12. Imamura, Y.; Shinozaki, T.; Okada-Ogawa, A.; Noma, N.; Shinoda, M.; Iwata, K.; Wada, A.; Abe, O.; Wang, K.; Svensson, P. An updated review on pathophysiology and management of burning mouth syndrome with endocrinological, psychological and neuropathic perspectives. J. Oral Rehabil. 2019, 46, 574–587. [Google Scholar] [CrossRef] [PubMed] [Green Version]
  13. Woda, A.; Dao, T.; Gremeau-Richard, C. Steroid dysregulation and stomatodynia (burning mouth syndrome). J. Orofac. Pain. 2009, 23, 202–210. [Google Scholar]
  14. Grushka, M.; Sessle, B.J.; Howley, T.P. Psychophysical assessment of tactile, pain and thermal sensory functions in burning mouth syndrome. Pain 1987, 28, 169–184. [Google Scholar] [CrossRef] [PubMed]
  15. Lauria, G.; Majorana, A.; Borgna, M.; Lombardi, R.; Penza, P.; Padovani, A.; Sapelli, P. Trigeminal small-fibre sensory neuropathy causes burning mouth syndrome. Pain 2005, 115, 332–337. [Google Scholar] [CrossRef] [PubMed]
  16. Hagelberg, N.; Forssell, H.; Rinne, J.O.; Scheinin, H.; Taiminen, T.; Aalto, S.; Luutonen, S.; Någren, K.; Jääskeläinen, S. Striatal dopamine D1 and D2 receptors in burning mouth syndrome. Pain 2003, 101, 149–154. [Google Scholar] [CrossRef]
  17. Lauritano, D.; Spadari, F.; Formaglio, F.; Zambellini Artini, M.; Salvato, A. Aspetti eziopatogenetici, clinico-diagnostici e terapeutici della sindrome bocca bruciante. Minerva Stomatol. 1998, 47, 239–251. [Google Scholar]
  18. Grémeau-Richard, C.; Dubray, C.; Aublet-Cuvelier, B.; Ughetto, S.; Woda, A. Effect of lingual nerve block on burning mouth syndrome (stomatodynia). A randomized crossover trial. Pain 2010, 149, 27–32. [Google Scholar]
  19. Bartoshuk, L.M.; Snyder, D.J.; Grushka, M.; Berger, A.M.; Duffy, V.B.; Kveton, J.F. Taste damage: Previously unsuspected consequences. Chem. Senses 2005, 30, i218–i219. [Google Scholar] [CrossRef]
  20. Kolkka-Palomaa, M.; Jääskeläinen, S.K.; Laine, M.A.; Teerijoki-Oksa, T.; Sandell, M.; Forssell, H. Pathophysiology of primary burning mouth syndrome with special focus on taste dysfunction: A review. Oral Dis. 2015, 21, 937–948. [Google Scholar] [CrossRef]
  21. Imura, H.; Shimada, M.; Yamazaki, Y.; Sugimoto, K. Characteristic changes of saliva and taste in burning mouth syndrome patients. J. Oral Pathol. Med. 2016, 45, 231–236. [Google Scholar] [CrossRef]
  22. Eliav, E.; Kamran, B.; Schaham, R.; Czerninski, R.; Gracely, R.H.; Benoliel, R. Evidence of chorda tympani dysfunction in patients with burning mouth syndrome. J. Am. Dent. Assoc. 2007, 138, 628–633. [Google Scholar] [CrossRef] [PubMed]
  23. Nasri-Heir, C.; Gomes, J.; Heir, G.M.; Ananthan, S.; Benoliel, R.; Teich, S.; Eliav, E. The role of sensory input of the chorda tympani nerve and the number of fungiform papillae in burning mouth syndrome. Oral Surg. Oral Med. Oral Pathol. Oral Radiol. Endod. 2011, 112, 65–72. [Google Scholar] [CrossRef] [PubMed]
  24. Formaker, B.K.; Frank, M.E. Taste function in patients with oral burning. Chem. Senses 2000, 25, 575–581. [Google Scholar] [CrossRef] [Green Version]
  25. Craig, A.D. How do you feel? Interoception: The sense of the physiological condition of the body. Nat. Rev. Neurosci. 2002, 3, 655–666. [Google Scholar] [CrossRef] [PubMed]
  26. Le Pichon, C.E.; Chesler, A.T. The functional and anatomical dissection of somatosensory subpopulations using mouse genetics. Front. Neuroanat. 2014, 8, 21. [Google Scholar] [CrossRef] [Green Version]
  27. Khalid, S.; Tubbs, R.S. Neuroanatomy and neuropsychology of pain. Cureus 2017, 9, e1754. [Google Scholar] [CrossRef] [PubMed] [Green Version]
  28. Chen, Z.S.; Wang, J. Pain, from perception to action: A computational perspective. iScience 2022, 26, 105707. [Google Scholar] [CrossRef]
  29. Kim, M.J.; Kho, H.S. Understanding of Burning Mouth Syndrome Based on Psychological Aspects. Chin. J. Dent. Res. 2018, 21, 9–19. [Google Scholar]
  30. Kenchadze, R.; Iverieli, M.; Okribelashvili, N.; Geladze, N.; Khachapuridze, N. The psychological aspects of burning mouth syndrome. Georgian Med. News. 2011, 194, 24–28. [Google Scholar]
  31. Taiminen, T.; Kuusalo, L.; Lehtinen, L.; Forssell, H.; Hagelberg, N.; Tenovuo, O.; Luutonen, S.; Pertovaara, A.; Jääskeläinen, S. Psychiatric (axis 1) and personality (axis 11) disorders in patients with burning mouth syndrome or atypical facial pain. Scand. J. Pain 2011, 2, 155–160. [Google Scholar] [CrossRef]
  32. Jääskeläinen, S.K.; Lindholm, P.; Valmunen, T.; Pesonen, U.; Taiminen, T.; Virtanen, A.; Lamusuo, S.; Forssell, H.; Hagelberg, N.; Hietala, J.; et al. Variation in the dopamine D2 receptor gene plays a key role in human pain and its modulation by transcranial magnetic stimulation. Pain 2014, 155, 2180–2187. [Google Scholar] [CrossRef] [PubMed]
  33. Coronel, M.F.; Labombarda, F.; González, S.L. Neuroactive steroids, nociception, and neuropathic pain: A flashback to go forward. Steroids 2016, 110, 77–87. [Google Scholar] [CrossRef] [PubMed] [Green Version]
  34. Rupprecht, R.; Holsboer, F. Neuroactive steroids: Mechanisms of action and neuropsychopharmacological perspectives. Neurosci. Trend. 1999, 22, 410–416. [Google Scholar] [CrossRef]
  35. Sardella, A.; Gualerzi, A.; Lodi, G.; Sforza, C.; Carrassi, A.; Donetti, E. Morphological evaluation of tongue mucosa in burning mouth syndrome. Arch. Oral Biol. 2012, 57, 94–101. [Google Scholar] [CrossRef]
  36. Walf, A.A.; Frye, C.A. A review and update of mechanisms of estrogen in the hippocampus and amygdala for anxiety and depression behavior. Neuropsychopharmacology 2006, 31, 1097–1111. [Google Scholar] [CrossRef] [PubMed]
  37. Lokuge, S.; Frey, B.; Foster, J.; Soares, C.; Steiner, M. Depression in women: Windows of vulnerability and new insights into the link between estrogen and serotonin. J. Clin. Psychiatry 2011, 72, e1563–e1569. [Google Scholar] [CrossRef] [PubMed] [Green Version]
  38. Gunn, B.G.; Cunningham, L.; Mitchell, S.G.; Swinny, J.D.; Lambert, J.J.; Belelli, D. GABAA receptor-acting neurosteroids: A role in the development and regulation of the stress response. Front. Neuroendocr. 2015, 36, 28–48. [Google Scholar] [CrossRef]
  39. Lamey, P.-J.; Freeman, R.; Eddie, S.-A.; Pankhurst, C.; Rees, T. Vulnerability and presenting symptoms in burning mouth syndrome. Oral Surg. Oral Med. Oral Pathol. Oral Radiol. Endod. 2005, 99, 48–54. [Google Scholar] [CrossRef] [PubMed]
  40. Koike, K.D.; Shinozaki, T.D.; Hara, K.D.; Noma, N.D.; Okada-Ogawa, A.D.; Asano, M.D.; Shinoda, M.D.; Eliav, E.D.; Gracely, R.H.; Iwata, K.D.; et al. Immune and endocrine function in patients with burning mouth syndrome. Clin. J. Pain 2014, 30, 168–173. [Google Scholar] [CrossRef]
  41. Buchanan, J.; Zakrzewska, J. Burning mouth syndrome. BMJ Clin. Evid. 2010, 7, 1301. [Google Scholar]
  42. Spadari, F.; Venesia, P.; Azzi, L.; Veronesi, G.; Costantino, D.; Croveri, F.; Farronato, D.; Tagliabue, A.; Tettamanti, L. Low basal salivary flow and burning mouth syndrome: New evidence in this enigmatic pathology. J. Oral Pathol. Med 2015, 44, 229–233. [Google Scholar] [CrossRef] [PubMed]
  43. Agha-Hosseini, F.; Mirzaii-Dizgah, I.; Mansourian, A.; Khayamzadeh, M. Relationship of stimulated saliva 17β-estradiol and oral dryness feeling in menopause. Maturitas 2009, 62, 197–199. [Google Scholar] [CrossRef] [PubMed]
  44. Agha-Hosseini, F.; Mirzaii-Dizgah, I.; Mirjalili, N. Relationship of stimulated whole saliva cortisol level with the severity of a feeling of dry mouth in menopausal women. Gerodontology 2012, 29, 43–47. [Google Scholar] [CrossRef] [PubMed]
  45. Tokura, T.; Kimura, H.; Ito, M.; Nagashima, W.; Sato, N.; Kimura, Y.; Arao, M.; Aleksic, B.; Yoshida, K.; Kurita, K.; et al. Temperament and character profiles of patients with burning mouth syndrome. J. Psychosom. Res. 2015, 78, 495–498. [Google Scholar] [CrossRef]
  46. Galli, F.; Lodi, G.; Sardella, A.; Vegni, E. Role of psychological factors in burning mouth syndrome: A systematic review and meta-analysis. Cephalalgia 2017, 37, 265–277. [Google Scholar] [CrossRef]
  47. Al Quran, F.A. Psychological profile in burning mouth syndrome. Oral Surg. Oral Med. Oral Pathol. Oral Radiol. Endod. 2004, 97, 339–344. [Google Scholar] [CrossRef]
  48. Lamb, A.B.; Lamey, P.J.; Reeve, P.E. Burning mouth syndrome: Psychological aspects. Br. Dent. J. 1988, 165, 256–260. [Google Scholar] [CrossRef]
  49. Pozza, D.H.; Fregapani, P.W.; Weber, J.B.; de Oliveira, M.G.; de Oliveira, M.A.M.; Neto, N.R.; de Macedo Sobrinho, J.B. Analgesic action of laser therapy (LLLT) in an animal model. Med. Oral Patol. Oral Cir. Bucal 2008, 13, E648–E652. [Google Scholar]
  50. Jääskeläinen, S.K.; Rinne, J.O.; Forssell, H.; Tenovuo, O.; Kaasinen, V.; Sonninen, P.; Bergman, J. Role of the dopaminergic system in chronic pain—A fluorodopa-PET study. Pain 2001, 90, 257–260. [Google Scholar] [CrossRef]
  51. Wood, P.B. Role of central dopamine in pain and analgesia. Expert Rev. Neurother. 2008, 8, 781–797. [Google Scholar] [CrossRef]
  52. Bardellini, E.; Amadori, F.; Conti, G.; Majorana, A. Efficacy of the photobiomodulation therapy in the treatment of the burning mouth syndrome. Med. Oral Patol. Oral Cir. Bucal 2019, 24, e787–e791. [Google Scholar] [CrossRef] [PubMed]
  53. De Pedro, M.; López-Pintor, R.M.; Casañas, E.; Hernández, G. Effects of photobiomodulation with low-level laser therapy in burning mouth syndrome: A randomized clinical trial. Oral Dis. 2020, 26, 1764–1776. [Google Scholar] [CrossRef] [PubMed]
  54. Hanna, R.; Bensadoun, R.J.; Beken, S.V.; Burton, P.; Carroll, J.; Benedicenti, S. Outpatient Oral Neuropathic Pain Management with Photobiomodulation Therapy: A Prospective Analgesic Pharmacotherapy-Paralleled Feasibility Trial. Antioxidants 2022, 11, 533. [Google Scholar] [CrossRef]
  55. Lončar-Brzak, B.; Škrinjar, I.; Brailo, V.; Vidović-Juras, D.; Šumilin, L.; Andabak-Rogulj, A. Burning Mouth Syndrome (BMS)-Treatment with Verbal and Written Information, B Vitamins, Probiotics, and Low-Level Laser Therapy: A Randomized Clinical Trial. Dent. J. 2022, 10, 44. [Google Scholar] [CrossRef] [PubMed]
  56. Scardina, G.A.; Casella, S.; Bilello, G.; Messina, P. Photobiomodulation Therapy in the Management of Burning Mouth Syndrome: Morphological Variations in the Capillary Bed. Dent. J. 2020, 8, 99. [Google Scholar] [CrossRef] [PubMed]
  57. Sikora, M.; Včev, A.; Siber, S.; Vučićević Boras, V.; Rotim, Ž.; Matijević, M. The Efficacy of Low-Level Laser Therapy in Burning Mouth Syndrome—A Pilot Study. Acta Clin. Croat. 2018, 57, 312–315. [Google Scholar] [CrossRef] [PubMed]
  58. Spanemberg, J.C.; López López, J.; de Figueiredo, M.A.; Cherubini, K.; Salum, F.G. Efficacy of low-level laser therapy for the treatment of burning mouth syndrome: A randomized, controlled trial. J. Biomed. Opt. 2015, 20, 098001. [Google Scholar] [CrossRef]
  59. Sugaya, N.N.; Silva, É.F.; Kato, I.T.; Prates, R.; Gallo, C.B.; Pellegrini, V.D. Low Intensity laser therapy in patients with burning mouth syndrome: A randomized, placebo-controlled study. Braz. Oral Res. 2016, 30, e108. [Google Scholar] [CrossRef] [Green Version]
  60. Sun, C.; Xu, P.; Zhang, Q.-Q.; Jiang, W.-W. Nd:YAG photobiomodulation treatment in burning mouth syndrome: A pilot study. Laser Dent. Sci. 2021, 5, 53–60. [Google Scholar] [CrossRef]
  61. Arduino, P.G.; Cafaro, A.; Garrone, M.; Gambino, A.; Cabras, M.; Romagnoli, E.; Broccoletti, R. A randomized pilot study to assess the safety and the value of low-level laser therapy versus clonazepam in patients with burning mouth syndrome. Lasers Med. Sci. 2016, 31, 811–816. [Google Scholar] [CrossRef]
  62. Valenzuela, S.; Lopez-Jornet, P. Effects of low-level laser therapy on burning mouth syndrome. J. Oral Rehabil. 2017, 44, 125–132. [Google Scholar] [CrossRef] [PubMed]
  63. Bushnell, M.C.; Ceko, M.; Low, L.A. Cognitive and emotional pain control and its interruption in chronic pain. Nat. Rev. Neurosci. 2013, 14, 502–511. [Google Scholar] [CrossRef] [PubMed] [Green Version]
  64. Finnerup, N.B.; Attal, N.; Haroutounian, S.; McNicol, E.; Baron, R.; Dworkin, R.H.; Gilron, I.; Haanpää, M.; Hansson, P.; Jensen, T.S.; et al. Pharmacotherapy for neuropathic pain in adults: A systematic review and meta-analysis. Lancet. Neurol. 2015, 14, 162–173. [Google Scholar] [CrossRef] [Green Version]
  65. Yamazaki, Y.; Hata, H.; Kitamori, S.; Onodera, M.; Kitagawa, Y. An open-label, noncomparative, dose escalation pilot study of the effect of paroxetine in treatment of burning mouth syndrome. Oral Surg. Oral Med. Oral Pathol. Oral Radiol. Endod. 2009, 107, e6–e11. [Google Scholar] [CrossRef]
  66. Maina, G.; Vitalucci, A.; Gandolfo, S.; Bogetto, F. Comparative efficacy of SSRIs and amisulpride in burning mouth syndrome: A single-blind study. J. Clin. Psychiatry 2002, 63, 38–43. [Google Scholar] [CrossRef]
  67. Birkinshaw, H.; Friedrich, C.M.; Cole, P.; Eccleston, C.; Serfaty, M.; Stewart, G.; White, S.; Moore, R.A.; Phillippo, D.; Pincus, T. Antidepressants for pain management in adults with chronic pain: A network meta-analysis. Cochrane Database Syst. Rev. 2023, 5, CD014682. [Google Scholar]
  68. Heckmann, S.M.; Heckmann, J.G.; Ungethüm, A.; Hujoel, P.; Hummel, T. Gabapentin has little or no effect in the treatment of burning mouth syndrome—Results of an open-label pilot study. Eur. J. Neurol. 2006, 13, e6–e7. [Google Scholar] [CrossRef] [PubMed]
  69. Cui, Y.; Xu, H.; Chen, F.; Liu, J.; Jiang, L.; Zhou, Y.; Chen, Q. Efficacy evaluation of clonazepam for symptom remission in burning mouth syndrome: A meta-analysis. Oral Dis. 2016, 22, 503–511. [Google Scholar] [CrossRef]
  70. Gremeau-Richard, C.; Woda, A.; Navez, M.L.; Attal, N.; Bouhassira, D.; Gagnieu, M.C.; Laluque, J.F.; Picard, P.; Pionchon, P.; Tubert, S. Topical clonazepam in stomatodynia: A randomized placebocontrolled study. Pain 2004, 108, 51–57. [Google Scholar] [CrossRef]
  71. Rodrìguez de Rivera Campillo, E.; López-López, J.; Chimenos-Küstner, E. Response to topical clonazepam in patients with burning mouth syndrome: A clinical study. Bull. Group. Int. Rech. Sci. Stomatol. Odontol. 2010, 49, 19–29. [Google Scholar] [PubMed]
  72. Marino, R.; Torretta, S.; Capaccio, P.; Pignataro, L.; Spadari, F. Different therapeutic strategies for burning mouth syndrome: Preliminary data. J. Oral Pathol. Med. Off. Publ. Int. Assoc. Oral Pathol. Am. Acad. Oral Pathol. 2010, 39, 611–616. [Google Scholar] [CrossRef]
  73. Tirosh, O.; Sen, C.K.; Roy, S.; Kobayashi, M.S.; Packer, L. Neuroprotective effects of alpha-lipoic acid and its positively charged amide analogue. Free Radic. Biol. Med. 1999, 26, 1418–1426. [Google Scholar] [CrossRef] [PubMed]
  74. Christy, J.; Noorani, S.; Sy, F.; Al-Eryani, K.; Enciso, R. Efficacy of alpha-lipoic acid in patients with burning mouth syndrome compared to that of placebo or other interventions: A systematic review with meta-analyses. J. Dent. Anesth. Pain Med. 2022, 22, 323–338. [Google Scholar] [CrossRef]
  75. Femiano, F.; Scully, C. Burning mouth syndrome (BMS): Double blind controlled study of alpha-lipoic acid (thioctic acid) therapy. J. Oral Pathol. Med. 2002, 31, 267–269. [Google Scholar] [CrossRef] [PubMed]
  76. Reyad, A.A.; Mishriky, R.; Girgis, E. Pharmacological and non-pharmacological management of burning mouth syndrome: A systematic review. Dent. Med. Probl. 2020, 57, 295–304. [Google Scholar] [CrossRef]
  77. Silvestre, F.J.; Silvestre-Rangil, J.; Tamarit-Santafé, C.; Bautista, D. Application of a capsaicin rinse in the treatment of burning mouth syndrome. Med. Oral Patol. Oral Cir. Bucal 2012, 17, e1–e4. [Google Scholar] [CrossRef] [Green Version]
  78. Vyklický, L.; Nováková-Toušová, K.; Benedikt, J.; Samad ATouška, F.; Vlachova, V. Calcium-dependent desensitization of vanilloid receptor TRPV1: A mechanism possibly involved in analgesia induced by topical application of capsaicin. Physiol. Res. 2008, 57 (Suppl. S3), S59–S68. [Google Scholar] [CrossRef]
  79. De Souza, F.T.; Amaral, T.M.; dos Santos, T.P.; Abdo, E.N.; Aguiar, M.C.F.; Teixeira, A.L.; Kummer, A.M.; Abreu, M.H.N.G.; Silva, T.A. Burning mouth syndrome: A therapeutic approach involving mechanical salivary stimulation. Headache 2012, 52, 1026–1034. [Google Scholar] [CrossRef] [PubMed]
  80. Cronshaw, M.; Parker, S.; Arany, P. Feeling the heat: Evolutionary and microbial basis for the analgesic mechanisms of photobiomodulation therapy. Photobiomodul. Photomed. Laser Surg. 2019, 37, 517–526. [Google Scholar] [CrossRef]
  81. Kato, I.T.; Pellegrini, V.D.; Prates, R.A.; Ribeiro, M.S.; Wetter, N.U.; Sugaya, N.N. Low-level laser therapy in burning mouth syndrome patients: A pilot study. Photomed. Laser Surg. 2010, 28, 835–839. [Google Scholar] [CrossRef]
  82. Chow, R.T.; Johnson, M.I.; Lopes-Martins, R.A.; Bjordal, J.M. Efficacy of low-level laser therapy in the management of neck pain: A systematic review and meta-analysis of randomized placebo or active-treatment controlled trials. Lancet 2009, 374, 1897–1908. [Google Scholar] [CrossRef] [PubMed]
  83. Zadik, Y.; Arany, P.R.; Fregnani, E.R.; Bossi, P.; Antunes, H.S.; Bensadoun, R.J.; Gueiros, L.A.; Majorana, A.; Nair, R.G.; Ranna, V.; et al. Systematic review of photobiomodulation for the management of oral mucositis in cancer patients and clinical practice guidelines. Support. Care Cancer 2019, 27, 3969–3983. [Google Scholar] [CrossRef] [PubMed] [Green Version]
  84. Aras, M.H.; Güngörmüş, M. The effect of low-level laser therapy on trismus and facial swelling following surgical extraction of a lower third molar. Photomed. Laser Surg. 2009, 27, 21–24. [Google Scholar] [CrossRef] [PubMed]
  85. Salmos-Brito, J.A.; de Menezes, R.F.; Teixeira, C.E.; Gonzaga, R.K.; Rodrigues, B.H.; Braz, R. Evaluation of low-level laser therapy in patients with acute and chronic temporomandibular disorders. Lasers Med. Sci. 2013, 28, 57–64. [Google Scholar] [CrossRef]
  86. Doshi-Mehta, G.; Bhad-Patil, W.A. Efficacy of low-intensity laser therapy in reducing treatment time and orthodontic pain: A clinical investigation. Am. J. Orthod. Dentofac. Orthop. 2012, 141, 289–297. [Google Scholar] [CrossRef]
  87. Akram, Z.; Abduljabbar, T.; Vohra, F.; Javed, F. Efficacy of low-level laser therapy compared to steroid therapy in the treatment of oral lichen planus: A systematic review. J. Oral Pathol. Med. 2018, 47, 11–17. [Google Scholar] [CrossRef]
  88. Romeo, U.; Del Vecchio, A.; Capocci, M.; Maggiore, C.; Ripari, M. The low level laser therapy in the management of neurological burning mouth syndrome. A pilot study. Ann. Stomatol. 2010, 1, 14–18. [Google Scholar]
Applsci 13 08880 g001
Figure 1. Flow chart of the review process.
Figure 1. Flow chart of the review process.
Applsci 13 08880 g001
Table 1. The risk of bias in randomized controlled trials is represented by symbols (green for low risk of bias, yellow for high risk of bias, and blue for uncertain or unavailable data and medium risk of bias).
Table 1. The risk of bias in randomized controlled trials is represented by symbols (green for low risk of bias, yellow for high risk of bias, and blue for uncertain or unavailable data and medium risk of bias).
Author and Year of PublicationQ1Q2Q3Q4Q5Q6Q7Q8Q9Q10Q11Q12Q13Overall
Appraisal
Bardellini et al., 2019 [52]Applsci 13 08880 i001Applsci 13 08880 i001Applsci 13 08880 i001Applsci 13 08880 i001Applsci 13 08880 i001Applsci 13 08880 i001Applsci 13 08880 i001Applsci 13 08880 i001Applsci 13 08880 i001Applsci 13 08880 i001Applsci 13 08880 i001Applsci 13 08880 i001Applsci 13 08880 i001Applsci 13 08880 i001
De Pedro et al., 2020 [53]Applsci 13 08880 i001Applsci 13 08880 i001Applsci 13 08880 i001Applsci 13 08880 i003Applsci 13 08880 i003Applsci 13 08880 i001Applsci 13 08880 i001Applsci 13 08880 i001Applsci 13 08880 i001Applsci 13 08880 i001Applsci 13 08880 i001Applsci 13 08880 i001Applsci 13 08880 i001Applsci 13 08880 i001
Hanna et al., 2022 [54]Applsci 13 08880 i001Applsci 13 08880 i001Applsci 13 08880 i001Applsci 13 08880 i001Applsci 13 08880 i001Applsci 13 08880 i003Applsci 13 08880 i001Applsci 13 08880 i001Applsci 13 08880 i001Applsci 13 08880 i001Applsci 13 08880 i001Applsci 13 08880 i001Applsci 13 08880 i001Applsci 13 08880 i001
Lončar-Brzak et al., 2022 [55]Applsci 13 08880 i001Applsci 13 08880 i001Applsci 13 08880 i001Applsci 13 08880 i002Applsci 13 08880 i002Applsci 13 08880 i002Applsci 13 08880 i001Applsci 13 08880 i001Applsci 13 08880 i001Applsci 13 08880 i001Applsci 13 08880 i001Applsci 13 08880 i001Applsci 13 08880 i001Applsci 13 08880 i001
Scardina et al., 2020 [56]Applsci 13 08880 i001Applsci 13 08880 i001Applsci 13 08880 i001Applsci 13 08880 i002Applsci 13 08880 i002Applsci 13 08880 i002Applsci 13 08880 i001Applsci 13 08880 i001Applsci 13 08880 i001Applsci 13 08880 i001Applsci 13 08880 i001Applsci 13 08880 i001Applsci 13 08880 i001Applsci 13 08880 i001
Sikora et al., 2018 [57]Applsci 13 08880 i001Applsci 13 08880 i001Applsci 13 08880 i001Applsci 13 08880 i002Applsci 13 08880 i002Applsci 13 08880 i002Applsci 13 08880 i001Applsci 13 08880 i001Applsci 13 08880 i001Applsci 13 08880 i001Applsci 13 08880 i001Applsci 13 08880 i001Applsci 13 08880 i001Applsci 13 08880 i001
Spanemberg et al., 2015 [58]Applsci 13 08880 i001Applsci 13 08880 i001Applsci 13 08880 i001Applsci 13 08880 i001Applsci 13 08880 i003Applsci 13 08880 i001Applsci 13 08880 i001Applsci 13 08880 i001Applsci 13 08880 i001Applsci 13 08880 i001Applsci 13 08880 i001Applsci 13 08880 i001Applsci 13 08880 i001Applsci 13 08880 i001
Sugaya et al., 2016 [59]Applsci 13 08880 i001Applsci 13 08880 i001Applsci 13 08880 i001Applsci 13 08880 i002Applsci 13 08880 i002Applsci 13 08880 i002Applsci 13 08880 i001Applsci 13 08880 i001Applsci 13 08880 i001Applsci 13 08880 i001Applsci 13 08880 i001Applsci 13 08880 i001Applsci 13 08880 i001Applsci 13 08880 i001
Sun et al., 2021 [60]Applsci 13 08880 i001Applsci 13 08880 i001Applsci 13 08880 i001Applsci 13 08880 i002Applsci 13 08880 i002Applsci 13 08880 i002Applsci 13 08880 i001Applsci 13 08880 i001Applsci 13 08880 i001Applsci 13 08880 i001Applsci 13 08880 i001Applsci 13 08880 i001Applsci 13 08880 i001Applsci 13 08880 i001
Arduino et al., 2016 [61]Applsci 13 08880 i001Applsci 13 08880 i001Applsci 13 08880 i001Applsci 13 08880 i002Applsci 13 08880 i002Applsci 13 08880 i002Applsci 13 08880 i001Applsci 13 08880 i001Applsci 13 08880 i001Applsci 13 08880 i001Applsci 13 08880 i001Applsci 13 08880 i001Applsci 13 08880 i001Applsci 13 08880 i001
Valenzuela et al., 2017 [62]Applsci 13 08880 i001Applsci 13 08880 i001Applsci 13 08880 i001Applsci 13 08880 i001Applsci 13 08880 i002Applsci 13 08880 i002Applsci 13 08880 i001Applsci 13 08880 i001Applsci 13 08880 i001Applsci 13 08880 i001Applsci 13 08880 i001Applsci 13 08880 i001Applsci 13 08880 i001Applsci 13 08880 i001
Table 2. Results of the literature review.
Table 2. Results of the literature review.
Author and Year of
Publication		Type of
Laser		PowerWavelengthApplication MethodNumber of Application SpotsTime of
Application		Number of
Sessions		Questionnaires for Symptoms EvaluationOutcome
Bardellini et al., 2019
[52]		Diode Laser3.2 W660–970 nmScanning methodVariable per patient, depending on the most painful points3′ 51″ each spot10 applications once a weekVAS, OHIP-14Symptoms improvement
De Pedro et al., 2020
[53]		Diode Laser0.6 W810 nmScanning method, pulsed wave56 points (3 in the vestibular mucosa of the 4 quadrants, 4
in each lip mucosa, 6 in each of the two buccal mucosa, 6 in the
hard palate, 4 on each lateral edge of tongue, 6 in the dorsum of
the tongue and 4 sublingual points, with a distance in between
of 2 mm.)		10 s each spot10 applications once a weekVAS, SF-36, OHIP-14, Epworth, SCL-90, McGillSymptoms improvement
Hanna et al., 2022
[54]		Diode Laser200 mW810 nmScanning method, continuous wave9 spots30 s each spot10 applications twice a weekEQ-5D-5LSymptoms improvement
Lončar-Brzak et al., 2022
[55]		GaAlAs30 mW685 nmScanning method3 spots381 seach spot10 applications once a dayOHIP-14, VASSymptoms improvement
Scardina et al., 2020
[56]		Diode Laser4 W800 nmScanning method, continuous wave4 spots300 seach spot8 applications twice a weekVASSymptoms improvement, changes in microcircular pattern
Sikora et al., 2018
[57]		GaAlAs100 mW830 nmScanning method, pulsed waveVariable per patient, depending on the most painful points5 min each session10 applications once a weekVAS, OHIP-14, OHIP-CRO-14Symptoms improvement
Spanemberg et al., 2015
[58]		Diode Laser100 mW and 35 mW830 nm and 685 nmScanning method, continuous waveapex of the tongue (3 points), side of the tongue (4 points), dorsum of the tongue (10 points), buccal mucosa (8 points), labial
mucosa (5 points), hard palate (8 points), soft palate (3 points),
and gums or alveolar ridge mucosa (3 points per sextant)		50–58 seach spot, 50 sfor 830 nm wave and 58 sfor 685 nm wave10 applications once a weekOHIP-14Symptoms improvement
Sugaya et al., 2016
[59]		GaAlAs120 mW790 nmScanning method, continuous waveVariable per patient, depending on the most painful points50 seach spot4 applications twice a weekVASSymptoms improvement
Sun et al., 2021
[60]		Nd: YAG100 mW1064 nmScanning method, pulsed modeVariable per patient, depending on the most painful points30 sper cm24 applications once a weekVASSymptoms improvement
Arduino et al., 2016
[61]		GaAlAs300 mW980 nmScanning method, continuous waveVariable per patient, depending on the most painful points10 seach spot5 applications once a weekVAS, McGill, OHIP-49, Hospital Anxiety and Depression ScaleSymptoms improvement
Valenzuela et al., 2017
[62]		GaAlAs1 W815 nmScanning method, continuous waveVariable per patient, depending on the most painful points6 seach spot4 applications once a weekVAS, OHIP-14Symptoms improvement
Abbreviations: EQ-5D-5L, European Quality of Life-5 Dimensions-5 Levels; McGill, McGill Pain Scale; OHIP-CRO-14, Oral Health Impact Profile-Croatian-14; OHIP-14, Oral Health Impact Profile-14; OHIP-49, Oral Health Impact Profile-49; SF-36, Short Form Health Survey-36; SCL-90, Symptom Checklist-90.
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

Spadari, F.; Pulicari, F.; Ghizzoni, M.; Porrini, M.; Bosotti, M.; Pellegrini, M. Photobiomodulation as a Therapeutic Strategy in Burning Mouth Syndrome: A Scoping Review. Appl. Sci. 2023, 13, 8880. https://doi.org/10.3390/app13158880

AMA Style

Spadari F, Pulicari F, Ghizzoni M, Porrini M, Bosotti M, Pellegrini M. Photobiomodulation as a Therapeutic Strategy in Burning Mouth Syndrome: A Scoping Review. Applied Sciences. 2023; 13(15):8880. https://doi.org/10.3390/app13158880

Chicago/Turabian Style

Spadari, Francesco, Federica Pulicari, Martina Ghizzoni, Massimo Porrini, Moreno Bosotti, and Matteo Pellegrini. 2023. "Photobiomodulation as a Therapeutic Strategy in Burning Mouth Syndrome: A Scoping Review" Applied Sciences 13, no. 15: 8880. https://doi.org/10.3390/app13158880

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