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Background:
Systematic Review

Overdiagnosis Due to Screening Mammography for Breast Cancer among Women Aged 40 Years and Over: A Systematic Review and Meta-Analysis

by
Arwa F. Flemban
Pathology Department, Faculty of Medicine, Umm Al-Qura University, Makkah 21955, Saudi Arabia
J. Pers. Med. 2023, 13(3), 523; https://doi.org/10.3390/jpm13030523
Submission received: 29 December 2022 / Revised: 3 February 2023 / Accepted: 11 March 2023 / Published: 14 March 2023
(This article belongs to the Section Methodology, Drug and Device Discovery)
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Abstract

:
The current systematic review and meta-analysis was conducted to estimate the incidence of overdiagnosis due to screening mammography for breast cancer among women aged 40 years and older. A PRISMA systematic search appraisal and meta-analysis were conducted. A systematic literature search of English publications in PubMed, Web of Science, EMBASE, Scopus, and Google Scholar was conducted without regard to the region or time period. Generic, methodological, and statistical data were extracted from the eligible studies. A meta-analysis was completed by utilizing comprehensive meta-analysis software. The effect size estimates were calculated using the fail-safe N test. The funnel plot and the Begg and Mazumdar rank correlation tests were employed to find any potential bias among the included articles. The strength of the association between two variables was assessed using Kendall’s tau. Heterogeneity was measured using the I-squared (I2) test. The literature search in the five databases yielded a total of 4214 studies. Of those, 30 articles were included in the final analysis, with sample sizes ranging from 451 to 1,429,890 women. The vast majority of the articles were retrospective cohort designs (24 articles). The age of the recruited women ranged between 40 and 89 years old. The incidence of overdiagnosis due to screening mammography for breast cancer among women aged 40 years and older was 12.6%. There was high heterogeneity among the study articles (I2 = 99.993), and the pooled event rate was 0.126 (95% CI: 15 0.101–0.156). Despite the random-effects meta-analysis showing a high degree of heterogeneity among the articles, the screening tests have to allow for a certain degree of overdiagnosis (12.6%) due to screening mammography for breast cancer among women aged 40 years and older. Furthermore, efforts should be directed toward controlling and minimizing the harmful consequences associated with breast cancer screening.

1. Introduction

Breast cancer is the most common invasive cancer in women globally [1]. Breast cancer was the most frequently diagnosed malignancy in 2020. The World Health Organization (WHO) stated that 2.3 million new cases were diagnosed and it resulted in 685,000 fatalities worldwide in 2020 [2]. The WHO also reported that, as of the end of 2020, there were 7.8 million women alive who had been diagnosed with breast cancer in the past 5 years, making it the world’s most prevalent cancer [3]. Breast cancer incidence is closely correlated with an increase in age [4]. Only 5% of all breast cancers occur in women under 40 [5]. Early identification and treatment of breast cancer are effective in high-income nations, and there is a limited benefit of screening in low-income countries due to expenses [6].
Mammography and the early detection of breast cancer save the lives of two out of three women, highlighting the benefit of mammography screening. A vast amount of published work highlights the benefit of early diagnosis of breast cancer via mammography screening. In the late 20th century, screening mammography was implemented in high-income nations, based on the finding that it decreased the mortality rate from breast cancer, without proper consideration or knowledge of potential risks [7]. Additionally, mammography screening programs started before the development of hormonal therapy and other targeted therapies for breast cancer. Thus, early mammography randomized control trial results showed poor adherence to the principles of screening set by the World Health Organization [8]. This sparked a debate in research about the benefits and drawbacks of mammography-based breast cancer screening [9,10].
Several risks are associated with breast cancer screening with mammography, including overdiagnosis and false-positive results. With the increase in breast cancer awareness and the success of breast cancer early detection campaigns, the number of women enrolling for mammography has increased significantly. False-positive cases are usually detected with confirmation and are not subjected to further treatment, however, this results in additional costs for confirmatory tests and required procedures. On the other hand, the risk of overdiagnosis is difficult to determine [11].
Over more than 15 years, there has been increasing awareness of the overdiagnosis of breast cancer. Cancer overdiagnosis is the detection of tumors that would not become symptomatic, nor would they have progressed to life-threatening disease during the life of the patient being screened [12]. Overdiagnosis refers to a screen-detected malignancy that would not have progressed to clinical or symptomatic presentation during the individual’s lifetime and would not have been diagnosed nor caused the individual any harm in the absence of screening. This somewhat contested harm of cancer screening, one that is inherently difficult to quantify, adds to the complexity of the outcomes associated with mammography screening [13]. Overdiagnosis is currently a growing ethical dilemma due to the burdens it places on patients and healthcare systems, including physical, labor, and financial strains [14]. Almost all cancer patients are provided with therapy since it is currently impossible to determine whether patients would benefit or suffer harm from early detection and treatment. So, overtreatment of overdiagnosed cases can increase mortality rates with no beneficial outcomes [15]. Overdiagnosed cases are subjected to overtreatment, unnecessary surgery, radiotherapy, and other adjuvant therapy. This overtreatment does not benefit patients and may cause undue harm in the form of physical and psychological effects that lower quality of life and shorten life expectancy [15]. There is another layer of complexity added to the topic of overdiagnosis: the difficulty of producing a precise estimate of its magnitude in newly diagnosed cases. Therefore, it is crucial for science and public health to determine the prevalence and frequency of overdiagnosis.
Overdiagnosis is an unexpected but inevitable danger when trying to detect pre-symptomatic cancer in age groups at considerable risk of death from other causes. However, early detection of breast cancer may result in a decrease in mortality [16]. There has been no universally accepted method to measure the value of the overdiagnosis of breast cancer [17]. The first hurdle in estimating the value of overdiagnosis involves the nature and subtype of breast cancer. Breast cancer is a heterogeneous disease and involves both in-situ and invasive subtypes. On initial thought, in-situ cancers’ progression to invasive cancers takes longer and, thus, results in a longer lead time [18]. This has led to the notion that there could be a higher risk of overdiagnosis for in-situ tumors compared to invasive ones; however, this notion was proven false, as the nature of tumors includes high genetic and inherited diversity [18]. This is why there has been a high level of variation in reported overdiagnosis in previous studies, ranging from 0 to 54% [19,20]. The studies that utilized lead time adjustment found that overdiagnosis was as low as 5%, while the observational studies reported overdiagnosis rates as high as 54% [19]. Another level of complexity is added because some forms of invasive carcinoma are non-progressive and can regress in the patient’s lifetime. This has led several studies to include the growth rate of tumors in determining overdiagnosis, which has resulted in an underestimation of the value of overdiagnosis [21].
The statistics and evidence from published work have reported variations in both the decreases in mortality and overdiagnosis using mammography [17]. Additionally, the magnitude of collective harm resulting from overdiagnosis does not essentially outweigh the benefit of breast cancer screening. Thus, many studies have recommended the planning of modifications to screening programs to reach a proper balance of benefits with minimal levels of harm [17]. These plans should be based on correctly assessing the level of overdiagnosis that causes unwanted harm while simultaneously measuring the benefit of screening in terms of mortality reduction. Further, the complete disclosure of these data to participants in the screening program should occur to make sure that they are aware of all of the potential benefits as well as harms associated with screening.
Furthermore, based on this evidence, more effort should be put into studying approaches to reducing the overtreatment of breast cancer-detected cases [22]. Thus, this systematic review and meta-analysis aim to fill this evidence gap. Women who want to be screened must accept an additional risk of diagnosis and treatment, including the risk of overdiagnosis and overtreatment, if they want to lower their risk of dying from breast cancer [23]. However, establishing the incidence and frequency of overdiagnosis is critically important to determine whether the net benefit justifies the resources required for screening and to provide the best information possible to help healthy women weigh the potential benefits versus the potential harms of participating in breast cancer screening. Therefore, the current systematic review and meta-analysis were conducted to estimate the incidence of overdiagnosis due to screening mammography for breast cancer among women aged 40 years and over.

2. Materials and Methods

2.1. PRISMA Guidelines and Protocol Registration

The Preferred Reporting Items for Systematic Reviews and Meta-Analyses (PRISMA) criteria were followed in the creation of this systematic review and meta-analysis (Table S1). The International Prospective Register of Systematic Reviews received the study protocol for registration (PROSPERO, registration No. CRD42022383242).

2.2. Literature Search Strategy

Without regard to the region or time period, the author conducted a thorough and methodical search of English publications published in PubMed, Web of Science, EMBASE, Scopus, and Google Scholar. A mixture of search techniques was used to broaden the scope of the search: the first was a MESH (medical subject header) search using the terms “Overdiagnosis”, “Mammography”, and “Breast Cancer”; the second was a free-text search using the following phrases (Women, Female, Breast Neoplasms, Incidence, Trend, Breast Neoplasms/epidemiology, Mass Screening, Mammography, Screening, and Overdiagnosis). Synonyms were combined using the boolean operator (OR), and cases and tests were combined using the boolean operator (AND) (Table S2).

2.3. Eligibility Criteria (Inclusion/Exclusion)

Articles examined the incidence of overdiagnosis due to screening mammography for breast cancer among women aged 40 years and over were included in this systematic review and meta-analysis. However, review articles, case report articles, articles written in languages other than English, articles deficient in relevant information, and articles without the full text were excluded.

2.4. Study Screening

The EndNote V.X8 software was deployed for the management of the article screening process. The duplicates were deleted, and then, the author methodically chose the included articles by screening the titles, abstracts, and full texts of the publications.

2.5. Data Extraction

The necessary information was gathered into a standardized table with the following headings: first author name and year of publication, study setting, study design, study participants, sample size, type of mammography, screening period, screening interval, number of positive screenings, and calculation of the overdiagnosis rates (%). Additionally, to improve accuracy and critical appraisal, data extraction was conducted by three independent researchers, and disputes between researchers were resolved through consensus.

2.6. Quality Assessment

The effectiveness of the included studies was evaluated using the Quality Assessment Tool for Quantitative Studies (QATFQS), which was developed by the Effective Public Health Practice Project (EPHPP) [24]. Each object was subjected to eight tool questions, which were individually graded with a “1” signifying excellent quality, a “2” signifying good quality, and a “3” signifying bad quality. The next step was to determine the overall ranking for each study using the following criteria: “1” indicates good quality (no poor ratings), “2” indicates moderate quality (one weak rating), and “3” indicates mediocre quality (two or more weak ratings) [25].

2.7. Meta-Analysis

The meta-analysis was completed using Comprehensive Meta-Analysis Software (CMA, version 3, BioStat, Tampa, FL, USA) (CMA, version 3, BioStat, Tampa, FL, USA). The effect size estimates of the included studies were calculated using the fail-safe N test.
The funnel plot was used to identify potential publication bias, and the Begg and Mazumdar rank correlation test was employed to find any potential bias among the included publications. The strength of the association between two variables was assessed using Kendall’s tau.
The heterogeneity between the included articles was measured using the I-squared (I2) statistic, and values of 25%, 50%, and 75% were classified as low, moderate, and high estimates, respectively [26]. When the p-value is more than 0.05, statistical heterogeneity is believed to be non-significant. The high degree of variability served as the impetus for the adoption of a random-effects model [27].

3. Results

3.1. Search Findings

The search in the five databases yielded a total of 4214 articles: 1631 in PubMed, 467 in Web of Science, 113 in EMBASE, 538 in Scopus, and 1456 in Google Scholar. After eliminating the duplicate entries, 1941 articles were left. Then, after filtering the titles and abstracts, 960 and 288 articles, respectively, were eliminated. The remaining 123 articles’ full texts were evaluated. Of these, 93 items were ultimately disqualified for not fitting the inclusion requirements. In the end, 30 articles were chosen for qualitative synthesis and meta-analysis after the screening procedure (Figure 1).

3.2. Characteristics of the Included Articles

The first study on the incidence of overdiagnosis due to screening mammography for breast cancer among women aged 40 years and over was published in 2004; two articles were published in 2006, one article in 2009, one article in 2010, two articles in 2011, three articles in 2012, three articles in 2013, one article in 2014, two articles in 2015, five articles in 2016, three articles in 2017, two articles in 2019, one article in 2020, one article in 2021, and two articles in 2022. Most studies were conducted in Norway (four) and the United Kingdom (four), followed by the United States (three), France (three), Denmark (three), Australia (three), the Netherlands (two), Belgium (one), Italy (one), Taiwan (one), Canada (one), Sweden (one), and Finland (one). The vast majority of the articles employed a retrospective cohort design (24 articles). The age of the recruited women in the included articles ranged between 40 and 89 years old. The sample size of the included articles ranged between 451 and 1,429,890 women, with an average of 237,019 women.
All the included articles reported that the type of mammography was biennial two-view mammography. The screening interval in the included articles ranged between 2 and 40 years, with an average of 15.1 years. The calculation of overdiagnosis (%) in the included articles ranged between 0.7% and 52% years, with an average of 16.6% (Table 1).

3.3. Unified Findings

The effect analysis of the 30 included articles in the current meta-analysis showed that the points of the estimate of the incidence of overdiagnosis due to screening mammography for breast cancer among women aged 40 years and over were 0.177 and 0.126 according to the fixed and random models, respectively. The Q-value, calculated using the homogeneity test, showed that the incidence of overdiagnosis due to screening mammography for breast cancer among women aged 40 years and over has a heterogenous structure (Q = 2137.239; p < 0.001) and (Q = 413,510.290; p-value < 0.001). As a result, the author completed the current meta-analysis using the random-effects model in order to lessen the misunderstandings that the discrepancy of the articles caused. The tau value was 0.480, which represents the true overall heterogeneity between the included articles.
A high level of heterogeneity was obtained, as indicated by the I-squared (I2) value of 99.993, thus indicating that the random-effects model for meta-analysis should be applied (Table 2).

3.4. The Incidence of Overdiagnosis Due to Screening Mammography for Breast Cancer among Women Aged 40 Years and Over

Despite the random-effects meta-analysis showing a high degree of heterogeneity among articles, I2 = 99.993, the pooled event rate (and 95% CI) was 0.126 (95%CI: 0.101–0.156) (Figure 2). Results indicated that the incidence of overdiagnosis due to screening mammography for breast cancer among women aged 40 years and over was 12.6%.

3.5. Fail-Safe N Method

By estimating how many studies with effect sizes of zero might be included in the meta-analysis before the result lost statistical significance, the fail-safe N method was used to evaluate the robustness of a significant finding. The Z-value for the observed studies was 1200.30110, indicating that publication bias could have affected the effect value that our meta-analysis produced (Table 3).

3.6. Rank Correlation

The Begg and Mazumdar test showed a weak negative association between the incidence of overdiagnosis due to screening mammography for breast cancer among women aged 40 years and over. The tau value, with and without continuity correction, was −0.10345. Furthermore, there was a weak negative association between the incidence of overdiagnosis due to screening mammography for breast cancer among women aged 40 years and over, where the tau value, with and without continuity correction, was −0.10115. Egger’s test for a regression intercept provided a p-value of 0.20746 for the incidence of overdiagnosis due to screening mammography for breast cancer among women aged 40 years and over, indicating the presence of publication bias (Table 4).

3.7. Publication Bias

The asymmetric funnel plots of the incidence of overdiagnosis due to screening mammography for breast cancer among women aged 40 years and over suggested publication bias (Figure 3).

4. Discussion

Mammography screening has benefits and drawbacks. Screening mammography lowers a woman’s chance of dying from breast cancer through the early detection of tumors while they are treatable and manageable. Yet, the benefit of mammography screening must be considered against the danger of unwarranted diagnosis and overtreatment that leads to physical, psychological, and financial harm, including the psychological and behavioral effects of labeling; the consequences of subsequent testing (including invasive tests), treatment, and follow-up; and the financial effects on the individual who is overdiagnosed and on society [58]. Additionally, according to the WHO regulations, screening invitations must be accompanied by accurate information about the advantages, risks, and uncertainties of screening mammography [59,60,61]. All relevant information regarding breast cancer mortality reduction due to treatment following early diagnosis and accurate statistics of the rates of overdiagnosis by mammography should be presented to women to help them make well-informed decisions [62].
The estimation of the level of overdiagnosis of breast cancer by screening mammography has been a hot topic in an era of emphasis on enhancing cost-effectiveness and achieving reductions in harm. Ong et al. (2015) showed that, in the United States (US), there were high costs resulting from false-positive mammograms and breast cancer overdiagnosis among women ages 40–59, as based on expenditure data from a major US healthcare insurance plan provider for 702,154 women in the years 2011–2013. The average expenditures for each false-positive mammogram, invasive breast cancer, and ductal carcinoma in situ in the 12 months following diagnosis were $852, $51,837, and $12,369, respectively. This translates to a national cost of $4 billion each year. They concluded that the costs associated with false-positive mammograms and breast cancer overdiagnosis appear to be much higher than previously documented. Screening has the potential to save lives. However, the economic impact of false-positive mammography results and breast cancer overdiagnosis must be considered in the debate about the appropriate populations for screening [63].
Biesheuvel and colleagues reported one of the earliest systematic reviews of breast cancer overdiagnosis and noted that source (primary) studies were prone to biases that may over- or under-estimate the magnitude of breast cancer overdiagnosis. They reported an extremely wide range of overdiagnosis estimates (from 0 to 62%) [64]. Therefore, the current systematic review and meta-analysis were conducted to estimate the incidence of overdiagnosis due to screening mammography for breast cancer among women aged 40 years and over. In the current systematic review and meta-analysis, a search of the five databases yielded a total of 4214 articles. Of these, 30 articles were included in the final analysis, with sample sizes ranging from 451 to 1,429,890 women and including an average of 237,019 women. The articles on the incidence of overdiagnosis due to screening mammography for breast cancer among women aged 40 years and over were published between 2004 and 2022. The age of the recruited women in the included articles ranged between 40 and 89 years old. Furthermore, most of the articles (24 articles) were retrospective cohort studies. Moreover, all the included articles reported that the type of mammography was biennial two-view mammography. Additionally, the screening interval in the included articles ranged between 2 and 40 years, with an average of 15.1 years.
The main results of the current systematic review and meta-analysis indicate that the incidence of overdiagnosis due to screening mammography for breast cancer among women aged 40 years and over was 12.6%. Evidence from observational studies and randomized controlled trials demonstrates that mammography screening lowers the chance of dying from breast cancer. These studies also provide substantial proof that overdiagnosis is a severe problem resulting from community breast screening [65,66,67]. According to the random-effects meta-analysis, there were high degrees of heterogeneity among the included articles [63]. The International Agency for Research on Cancer (IARC) Working Group noted that there was sufficient evidence of overdiagnosis [68]. The Euroscreen Group’s summary emphasized that the estimate of overdiagnosis was 6.5% (ranging from 1% to 10%), based on a systematic review of European studies, and they also incorporated a lead time adjustment [69,70]. This study’s conclusion was based on a systematic evaluation of studies conducted in Europe, and one of the main outcomes of this study was the lead time adjustment [71].
When a malignancy is overdiagnosed, it is one that would not have progressed to clinical or symptomatic manifestation during the patient’s lifetime, would not have been diagnosed, and would not have harmed the patient [72]. Overdiagnosis is difficult to quantify, and outcomes of mammography screening are complicated by this hotly debated harm of cancer screening. A variety of factors add to the complexity of quantifying overdiagnosis. These factors include the mean measurement of the definition of overdiagnosis (which could be presented as the rate or proportion being measured) and the denominator (which is measured either by the number of screened women in long-term follow-up or as a proportion of the cases diagnosed during the screening phase). These considerations contributed to the variability in the reported estimates of breast cancer overdiagnosis attributed to mammography screening. Another factor that adds to the complexity of determining mammography overdiagnosis is factoring in the heterogeneous nature of breast (ductal carcinoma in situ (DCIS)) or invasive cancer (or both). Additionally, the timing of measuring overdiagnosis and the length of follow-up following screening are important factors to add into consideration. Moreover, differences in study populations, including demographics and differences in underlying breast cancer risk, are further considerations. The effect of basic screening methodology is an important factor in measuring overdiagnosis. Other variations in screening practices, including the screening technology used, screening policy and frequency, population coverage, and uptake, are factors that should be considered in the estimation of the risk of overdiagnosis. Furthermore, statistical techniques, adjustments, and assumptions relating to lead time and disease progression (the latter of which is not limited to modeling studies); and the framing of the extent of overdiagnosis (relative or absolute estimates) should be clearly considered in overdiagnosis analysis studies [43,70,73].
Although overdiagnosis estimates are associated with a high degree of uncertainty, estimates of magnitude for the two outcomes of screening—the reduction in breast cancer mortality and overdiagnosis—differ across studies. Though the balance between the advantages and disadvantages of breast cancer screening, including overdiagnosis, is more delicate than first thought, the evidence offered in the overdiagnosis section does not disprove the value of breast cancer screening. Future efforts should be focused on ensuring that any changes in the implementation of breast cancer screening optimize the balance between benefits and harms, including assessing how planned and actual changes modify the risk of overdiagnosis. Further, women should be provided with well-calculated statistics and balanced information about the outcomes that may affect them when participating in screening. Additionally, researchers should focus on reducing the risk of ever-treating detected cases in screening programs.
One limitation of this systematic review and meta-analysis was the high heterogeneity among studies articles. This meta-analysis is the first study that shows the incidence of overdiagnosis due to screening mammography for breast cancer among women aged 40 years and over. The present meta-analysis study could be a data baseline for the incidence of overdiagnosis due to screening mammography for breast cancer among women and can guide other researchers to design new studies.

5. Conclusions

Despite the random-effects meta-analysis showing a high degree of heterogeneity among articles, the screening tests have to allow for a certain degree of overdiagnosis (12.6%) resulting from screening mammography for breast cancer among women aged 40 years and older. The magnitude of breast cancer overdiagnosis attributed to mammography screening is complicated by the heterogeneity of many of the elements, political and scientific, that define and interpret the evidence of this screening harm. There is sufficient evidence to acknowledge overdiagnosis as a serious harm caused by breast cancer screening. Based on the available evidence, it is reasonable to conclude that mammography screening reduces the risk of breast cancer death; however, the harms, including overdiagnosis, should be balanced. The snapshot of evidence presented on the incidence of overdiagnosis in this systematic review and meta-analysis, however, does not mean that population breast screening is worthless, given that screening reduces breast cancer deaths. Hence, efforts should be directed toward controlling and minimizing the harmful consequences associated with breast cancer screening. The changes in the implementation of mammography screening plans should ensure a balance between benefits and harms. Full disclosure to the participating women, of all of the outcomes that may affect them when they participate in screening, is necessary as well. This should be sublimated by changes in the regulation of management and treatment of diagnosed cases during screening to minimize overtreatment, thereby reducing the harm of overdiagnosis.

Supplementary Materials

The following supporting information can be downloaded at: https://www.mdpi.com/article/10.3390/jpm13030523/s1, Table S1: PRISMA recommendations checklist [74]; Table S2: PubMed search strategy.

Funding

This research received no external funding.

Institutional Review Board Statement

The protocol of the study was registered in The International Prospective Register of Systematic Reviews (PROSPERO, registration No. CRD42022383242).

Informed Consent Statement

Not applicable.

Data Availability Statement

Not applicable.

Acknowledgments

The author would like to extend her gratitude to Umm Al-Qura University for supplying the analysis program. The author is grateful to Samer Abuzerr and Saeed M. Kabrah for their help in the article assessment and screening process, data extraction, data analysis, and reviewing the manuscript.

Conflicts of Interest

The author declared that there is no conflict of interest in this work.

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Jpm 13 00523 g001 550
Figure 1. Process for choosing articles.
Figure 1. Process for choosing articles.
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Jpm 13 00523 g002 550
Figure 2. Forest plot from the fixed- and random-effects analyses: the incidence of overdiagnosis due to screening mammography for breast cancer among women aged 40 years and over [21,22,23,24,25,26,27,28,29,30,31,32,33,34,35,36,37,38,39,40,41,42,43,44,45,46,47,48,49,50].
Figure 2. Forest plot from the fixed- and random-effects analyses: the incidence of overdiagnosis due to screening mammography for breast cancer among women aged 40 years and over [21,22,23,24,25,26,27,28,29,30,31,32,33,34,35,36,37,38,39,40,41,42,43,44,45,46,47,48,49,50].
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Figure 3. Publication bias of the incidence of overdiagnosis due to screening mammography for breast cancer among women aged 40 years and over.
Figure 3. Publication bias of the incidence of overdiagnosis due to screening mammography for breast cancer among women aged 40 years and over.
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Table
Table 1. The data extracted from the included articles.
Table 1. The data extracted from the included articles.
First Author Name and Year of Publication Study Setting Study DesignStudy ParticipantsSample SizeType of MammographyScreening PeriodScreening Interval (Years)Positive ScreeningCalculation of Overdiagnosis (%)
Paci et al., 2004 [28]ItalyRetrospective cohortWomen aged 50–69 years2780Biennial two-view mammography1990–199992626 invasive cancers and 154 other cancers5.0
Zackrisson et al., 2006 [29]SwedenRandomized screening trialWomen aged 45–69 years1,711,690Biennial two-view mammography1976–1986105050 breast cancer cases10.0
Olsen et al., 2006 [30]DenmarkRetrospective cohortWomen aged 50–69 years40,000Biennial two-view mammography1943–197734329 invasive cancers and 50 other cancers 7.8
Jorgensen et al., 2009 [31]DenmarkRetrospective cohortWomen aged 50–69 years115,270Biennial two-view mammography1991–2003135189 breast cancer cases35.0
Morrell et al., 2010 [32]AustraliaRetrospective cohortWomen aged 50–69 years100,000Biennial two-view mammography1999–20012830 breast cancer cases42.0
De Gelder et al., 2011 [33]NetherlandsRetrospective cohortWomen aged 49–74 years586,550Biennial two-view mammography2004–200624546 invasive cancers21.0
Seigneurin et al., 2011 [34]FranceRetrospective cohortWomen aged 50–69 years245,000Biennial two-view mammography1991–2006153675 invasive cancers and 68,600 carcinomas in-situ3.3
Puliti et al., 2012 [35]ItalyRetrospective cohortWomen aged 50–69 years52,282Biennial two-view mammography1991–199321583 breast cancer caces10.0
Gunsoy et al., 2012 [36]United KingdomRandomized controlled trialWomen aged 40–49 years53,890Biennial two-view mammography1991–201019151 invasive carcinomas and 43 in-situ carcinomas0.7
Kalager et al., 2012 [37]NorwayRetrospective cohortWomen aged 50–69 years7793Biennial two-view mammography1985–2005197793 invasive breasts cancers20.0
Pivot et al., 2013 [38]FranceCross-sectionalWomen aged 40–75 years451Biennial two-view mammography18–30 January 201312NM38.0
Coldman and Phillips 2013 [39]United KingdomRetrospective cohortWomen aged
40–89 years		1,387,197Biennial two-view mammography1970–20093974,189 invasive breasts cancers and 8286 ductal carcinomas in-situ17.3
Falk et al., 2013 [40]NorwayRetrospective cohortWomen aged 50–69 years702,131Biennial two-view mammography1995–20091494,085
invasive breast cancer tumors and
43,532 ductal carcinoma in-situ		10.0
Heinavaara et al., 2014 [41]FinlandRetrospective cohortWomen aged 50–59 years45–69Biennial two-view mammography1935–193942583 invasive breast carcinomas and 117 other breast carcinomas6.0
Beckmann et al., 2015 [42]AustraliaCase-controlWomen aged 45–85 years25,373Biennial two-view mammography2006–201044088 invasive breast cancer tumors and
495 ductal carcinoma in-situ		14.0
Beckmann et al., 2015 [43]AustraliaRetrospective cohortWomen aged 40–84 years100,000Biennial two-view mammography1989–2009208611 invasive breast cancers12.0
Yen et al., 2016 [44]TaiwanRetrospective cohortWomen aged 40–69 years1,429,890Biennial two-view mammography1999–2009104423 breast cancer cases13.0
Michalopoulos and Duffy 2016 [45]NorwayRetrospective cohortWomen aged 50–69 years500,000Biennial two-view mammography1996–20091310,014 screen-detected cancers16.0
Baines et al., 2016 [46]CanadaRandomized screening trialWomen aged 40–59 years89,835Biennial two-view mammography1988–200517484 screen-detected cancers25.0
Falk and Hofvind 2016 [47]United KingdomRetrospective cohortWomen aged 50–79 years100,000Biennial two-view mammography2008–20102273 invasive breast cancers1.9
Seigneurin et al., 2016 [48]FranceRetrospective cohortWomen aged 50–74 years100,000Biennial two-view mammography2007–20103218 invasive breast cancers and 84 in-situ cancers17.0
Jorgensen et al., 2017 [49]DenmarkRetrospective cohortWomen aged 40–84 years94,932Biennial two-view mammography1980–201030271 invasive breast cancer tumors and 179 ductal carcinomas in situ24.4
van Luijt et al., 2017 [50]NorwayRetrospective cohortWomen aged 50–70 years100,000Biennial two-view mammography1970–200939324 breast cancer cases3.0
Autier et al., 2017 [51]NetherlandsRetrospective cohortWomen aged 50–75 years100,000Biennial two-view mammography1989–201223585 invasive breast cancers and 47 in-situ cancers52.0
Harding et al., 2019 [52]United StatesRetrospective cohortWomen aged ≥ 40 years645,057Biennial two-view mammography1996–200913104,000 breast cancer cases31.0
Fann et al., 2019 [53]SwedenRetrospective cohortWomen aged 50–70 years1346Biennial two-view mammography1996–1998 2006–201015NM11.8
Chootipongchaivat et al., 2020 [54]United StatesRetrospective cohortWomen aged ages 30–79 years100,000Biennial two-view mammography1975–201540NM6.5
Blyuss et al., 2021 [55]United KingdomCase-controlWomen aged 47–89 years163,146Biennial two-view mammography2010–20112NM9.5
Ryser et al., 2022 [56]United StatesRetrospective cohortWomen aged 50–74 years35,986Biennial two-view mammography2000–201818718 breast cancer cases15.4
Ding et al., 2022 [57]BelgiumRetrospective cohortWomen aged 50–69 years100,000Biennial two-view mammography2001–20111018 invasive breast cancers20.1
NM, not mentioned.
Table
Table 2. Effect analysis of included articles.
Table 2. Effect analysis of included articles.
ModelEffect Size and 95% IntervalPrediction IntervalBetween-StudyOther Heterogeneity Statistics
Number StudiesPoint EstimateLower LimitUpper LimitLower LimitUpper LimitTauTauSqQ-Valuedf (Q)p-ValueI-Squared
Fixed300.1770.1770.1770.0330.3790.6930.480413,510.290290.00099.993
Random300.1260.1010.156
Table
Table 3. Classic and Orwin’s fail-safe N outcomes.
Table 3. Classic and Orwin’s fail-safe N outcomes.
Classic Fail-Safe N MethodOrwin’s Fail-Safe N Method
Z-value for observed studies1200.30110The event rate observed in studies0.17712
p-value for observed studies0.00000The criterion for a “trivial” event rate0.50000
Alpha0.05000Mean event rate in missing studies0.50000
Tails2.00000Number of missing studies that would bring the p-value to > alpha (N-value)The criterion must fain between other values
Z for alphas1.95996
Number of observed studies30.00000
Number of missing studies that would bring the p-value to >alpha (N-value)1342.00000
Table
Table 4. Kendall’s tau with/without continuity correction and Egger’s regression intercept.
Table 4. Kendall’s tau with/without continuity correction and Egger’s regression intercept.
Kendall’s S Statistic (P-Q)−45.00000
Kendall’s tau with continuity correction
Tau−0.10345
Z-value for tau0.80285
p-value (1-tailed)0.21103
p-value (2-tailed)0.42206
Kendall’s tau without continuity correction
Tau−0.10115
Z-value for tau0.78501
p-value (1-tailed)0.21623
p-value (2-tailed)0.43245
Egger’s regression intercept
Intercept−27.36434
Standard error33.06605
95% low limit (2-tailed)−95.09708
95% upper limit (2-tailed)40.436839
t-value0.82757
df28.00000
p-value (1-tailed)0.20746
p-value (2-tailed)0.41491
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Flemban, A.F. Overdiagnosis Due to Screening Mammography for Breast Cancer among Women Aged 40 Years and Over: A Systematic Review and Meta-Analysis. J. Pers. Med. 2023, 13, 523. https://doi.org/10.3390/jpm13030523

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Flemban AF. Overdiagnosis Due to Screening Mammography for Breast Cancer among Women Aged 40 Years and Over: A Systematic Review and Meta-Analysis. Journal of Personalized Medicine. 2023; 13(3):523. https://doi.org/10.3390/jpm13030523

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Flemban, Arwa F. 2023. "Overdiagnosis Due to Screening Mammography for Breast Cancer among Women Aged 40 Years and Over: A Systematic Review and Meta-Analysis" Journal of Personalized Medicine 13, no. 3: 523. https://doi.org/10.3390/jpm13030523

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