Lower limb amputations among individuals living with diabetes mellitus in low- and middle-income countries: A systematic review protocol

Eyitayo Omolara Owolabi; Davies Adeloye; Anthony Idowu Ajayi; Michael McCaul; Justine Davies; Kathryn M Chu

doi:10.1371/journal.pone.0266907

. 2022 Apr 14;17(4):e0266907. doi: 10.1371/journal.pone.0266907

Lower limb amputations among individuals living with diabetes mellitus in low- and middle-income countries: A systematic review protocol

Eyitayo Omolara Owolabi ¹, Davies Adeloye ², Anthony Idowu Ajayi ^3,^*, Michael McCaul ⁴, Justine Davies ⁵, Kathryn M Chu ¹

Editor: Daoud Al-Badriyeh⁶

PMCID: PMC9009695 PMID: 35421192

Abstract

Background

The burden of diabetes mellitus (DM) and its associated complications continue to burgeon, particularly in low- and middle-income countries (LMICs). Lower limb amputation (LLA) is one of the most life-altering complications of DM, associated with significant morbidity, mortality and socio-economic impacts. High-income countries have reported a decreasing incidence of DM-associated LLA, but the situation in many LMICs is unknown. We aim to conduct a systematic review to determine the incidence and prevalence of DM-associated LLA in LMICs to better inform appropriate interventions and health system response.

Methods and analysis

A systematic search of the literature will be conducted on five databases: MEDLINE, Embase, Cumulative Index of Nursing and Allied Health Literature (CINAHL), Scopus and African Journal Online (AJOL). Only observational, quantitative studies reporting the incidence and/or prevalence of DM-related LLA will be considered. A validated study design-specific critical appraisal tool will be used to assess the risk of bias in individual studies. We will determine the incidence of LLA by examining the number of new cases of LLA among individuals with confirmed DM diagnosis during the specified period, while the prevalence will be based on the total number of all new and existing LLAs in a population. LLA will be considered as the resection of the lower limb from just above the knee to any point down to the toe. If heterogeneity is low to moderate, a random-effects meta-analysis will be conducted on extracted crude prevalence/incidence rates, with the median and interquartile range also reported. The systematic review will be performed in accordance with the JBI guideline for prevalence and incidence review. Study reporting will follow the Preferred Reporting Items for Systematic Review and Meta-Analyses (PRISMA) guideline.

Prospero registration number

CRD42021238656.

Introduction

The burden of Diabetes Mellitus (DM) continues to grow, especially in low- and middle-income countries (LMICs) [1]. Since 1980, the number of persons living with DM globally has nearly quadrupled [1], with almost 80% of them residing in LMICs [2]. The rising DM prevalence is largely attributable to demographic transition, population ageing, obesity and unhealthy lifestyle behaviours [1].

DM leads to several systemic complications, with lower limb amputation (LLA) being one of the most life altering [3]. Specifically, DM contributes to the development of microvascular and macrovascular complications such as peripheral arterial disease (PAD) and peripheral neuropathy (PN) which predispose to non-healing, infected or gangrenous foot ulcers, which ultimately lead to LLA [4, 5]. The risk of PAD, PN and LLA significantly increases with longer duration and poorly controlled DM [4]. LLA risk among individuals with poorly controlled DM is 26% higher with every percentage increase in glycated haemoglobin (HbA1c), a measure of glycaemic status [6].

LLA poses a substantial health, psychological [7] and socio-economic burden, both at individual and country level [8–10], and greatly affects quality of life [11]. It is also associated with disability and premature mortality [12]. In 2016, there were an estimated 1.5 million years lived with disability (YLD) resulting from amputations, a 32% increase from 1990 [13]. Not only does LLA have deleterious impacts in its own right, it is also associated with increased risk for other DM complications such as cardiovascular diseases [14].

The burden of diabetes-related complications is especially high across LMICs [1], where access to quality DM care is limited [15]. With regard to LLA among persons living with diabetes, perhaps, one of the challenges in the response so far has been a poor understanding and awareness of the disease epidemiology in LMICs, which limits targeted response. While individual studies on LLA prevalence and incidence do exist in LMICs [16–19], no study has synthesised data from this region. Existing reviews had a global inclusion criteria [20, 21] but only one of them included few LMICs in their final analysis but did not follow a systematic approach [21]. Reasons for low or no representation of LMICs in previous studies is not known and estimates from these studies may not accurately reflect the situation in LMICs. In this study, we will define LMICs according to the World Bank income categories [22], taking care to apply our data synthesis and analyses to the WHO regions. This, to the best of our knowledge, will be the first systematic review of LLA among persons with diabetes in LMICs using this approach. This study therefore offers up-to-date data on the incidence and prevalence of diabetes-related LLA that can inform a much-needed response, priorities setting and further research.

Aim and objectives

We aim to conduct a systematic review to determine the incidence and prevalence of DM-related LLA in LMICs.

Secondary objectives of the systematic review include:

to determine the incidence of re-amputations and contralateral amputations and, where possible;
to investigate time trends in the incidence and prevalence of LLA among DM individuals in LMICs.

Methods

This systematic review on the incidence and prevalence of LLA in LMICs will follow the Joanna Briggs Institute (JBI) methodology for systematic reviews of prevalence and incidence [23]. The study protocol is in accordance with the PRISMA protocol checklist for systematic reviews [24, 25].

Eligibility criteria

Inclusion criteria

Types of studies. Prospective and retrospective observational studies, specifically, descriptive and analytic cross- sectional studies reporting the incidence and/or prevalence of lower limb amputations among individuals with confirmed DM diagnosis for a specified period will be included. Also included will be randomised controlled trials (RCTs) with baseline data providing prevalence estimates. Studies involving both DM and non-DM individuals will also be included as long as estimates of LLA among the DM population are provided. There is no age or gender restriction for the participants. For duplicate or overlapping studies, the study with the most detailed data will be included, with additional data, if necessary, extracted from others.

Context. This review will be limited to studies conducted in LMICs. Countries currently listed by the World Bank as low-income, lower-middle-income and upper-middle-income based on income levels, will be considered LMICs [22].

Language. Only studies written in English or with an available English version, or with the possibility of translating the full article via Google Translate, will be included.

Study period. Our focus will be on the past three decades; we will therefore include studies conducted from 1990 until 28^th February 2022.

Exclusion criteria

Qualitative studies on LLA among persons with diabetes;
Studies that reported traumatic LLA or cancer-related LLA;
Case reports, case series, case-control, reviews, viewpoints, letters or opinion-based articles, and
RCTs without a representative population denominator.

Information sources and search strategy

Electronic searches

A comprehensive systematic search of the literature will be conducted on five databases: MEDLINE, Embase, Scopus, CINAHL, and African Journals Online (AJOL) using a combination of MeSH terms and keywords such as “diabetes”, “amputation”, “lower limb amputation”, “lower extremity amputation”, “amputee” and “incidence” (see S1 Appendix). Terms representing similar concepts will be separated using the Boolean operator “OR” while terms representing different concepts will be separated using the Boolean operator “AND”. Hand searching for relevant articles from the reference list of reviews and included studies will be conducted. Where the full text of relevant studies cannot be retrieved, efforts will be made to request the full text from study corresponding authors.

Searching of other sources

Unpublished studies/grey literature will be hand searched through Google Scholar and grey literature databases such as WHO Library, OpenSIGLE and Open Grey using the study keywords.

Study records

Data management and study selection process

Articles retrieved from databases will be imported in Endnote to remove duplicates. Articles will then be exported into Covidence Systematic Review software (Veritas Health Innovation, Melbourne, Australia) for data management.

After duplicates have been removed from search results, initial screening of titles and abstracts will be conducted independently by two authors following the selection criteria; discrepancies will be resolved by discussion or with a third reviewer. Full text-review of the included studies will also be conducted independently by two authors. All disagreements will be resolved by discussion between two authors and if required, with a third reviewer. The reasons for the exclusion of full text articles will be given. A detailed description and summary of the search results and the selection process will be presented using a PRISMA flow diagram. Details of all the included studies will be reported in a table of included studies.

Data extraction

The standardised JBI data extraction tool for prevalence and incidence review will be adapted [23]. The data extraction tool will be pilot tested using three randomly selected (included) full-text articles after which the tool will be refined and adjusted as necessary. Double (independent) extraction of data will be conducted, and the extracted information will be compared. Where a discrepancy exists between the two extractions, both authors will re-assess identified studies and correct any errors. When necessary, study authors will be contacted to request missing information for clarifications.

Data items and description

General study information

General study information to be extracted include the first and last authors’ names, study title, year of publication, the main affiliation of the primary and senior authors and the data source.

Study characteristics

Study characteristics to be extracted include study population (described by age and sex), study setting/country, study design and period, funding source, year of data collection, sample size, and study denominator (population-level or health facility).

Outcome data

We will extract data on LLA type and location, number of DM individuals in the setting at the specified time, the incidence of LLA reported among DM individuals, the prevalence of LLA reported among DM individuals, the type of LLA (major, minor or both), with a description of it (first, re-amputation or contralateral amputation), the confidence interval and the absolute number of cases.

Case definitions

DM will be defined as specified by the study authors; we will capture the criteria used by authors in order to appraise heterogeneity.

LLA will be defined as the resection of a segment of the lower limb through the tibia and fibula, knee or ankle joint, or femur down to the toe. Major amputations are resections proximal to the tarsometatarsal joint while minor amputations are resections occurring distal or through the tarsometatarsal joint [26].

Study outcomes and prioritisation

The primary outcome of this review is the incidence and prevalence of DM-related LLA in LMICs. Incidence will be defined as the number of new cases of LLA divided by the total DM population in the study during the specified period. Incidence measures will include incidence rate and cumulative incidence. Reporting of incidence at person level will be one amputation per person (the first or the highest) and both levels of amputation, major and minor will be considered. Prevalence will be defined as the total number of DM-related LLAs in the population for a given period.

Assessment of methodological quality of studies

Eligible studies reporting prevalence data that meet the inclusion criteria will be critically appraised for methodological quality using the validated JBI critical appraisal tool for prevalence studies [23]. Studies reporting incidence data will be appraised using a validated tool appropriate for the study design. For instance, cohort studies will be critically appraised using the validated Newcastle-Ottawa quality appraisal tool for non-randomised studies [27]. Critical appraisals will be done at the study level by two independent reviewers. Discrepancies will be resolved by discussion, or with a third reviewer. Studies rated as high (score of >8 of 10) to moderate quality (score of 6–8) will be included in the analysis while low-quality studies (score of 0–5) will be excluded.

Data analysis and presentation of results

The median and interquartile range of all crude incidence rates will be reported. A Freeman–Tukey double-arcsine transformation will be applied to normalise data, given an expected wide variation in extracted crude estimates from studies. Transformed data will be used to calculate summary proportion and 95% CI using a random effects model. A meta-analysis of the estimates of prevalence and incidence will be conducted if studies are sufficiently homogenous. We will assess heterogeneity using the X² and I² tests. I² cut-off values of 0%, 25%, 50% and 75% will represent no, low, moderate and high level of heterogeneity respectively [28]. We will conduct the meta-analysis following the DerSimonian and Laird method [29]. Due to potential of high level of heterogeneity, the DerSimonian-Laird random-effects model is preferred. The DerSimonian and Laird method is widely adopted in the literature and performs robustly in various scenarios including skew-normal and extreme distributions for the effects [30].

Where meta-analysis is not possible, a narrative synthesis of results will be done, using tables and figures as appropriate for data visualisation. Also, in case of heterogeneity, we will carry out sub-group analysis and meta-regression analyses to show the potential sources of heterogeneity. Sub-group analysis will show the distribution across age group, sex and study regions. There should be at least ten studies for each variable in the model for meta-regression analysis to be performed [31]. A sensitivity analysis will be performed to assess the robustness of the study estimates, enabling us to assess the effect of omitting onestudy at a time on the pooled estimate [31]. Lastly, a funnel plot asymmetry test and Egger’s test will be used to assess publication bias, if there are more than ten included studies [31].

Assessment of certainty of evidence

We will use the grading of recommendations, assessment, development and evaluation (GRADE) instrument and Gradepro Software to assess the quality of the synthesised findings. Included studies will be assessed by study design, heterogeneity, consistency, directness, precision and publication bias. The evidence will be described as high, moderate, low or very low quality.

Discussion

The burden of DM has been projected to grow exponentially in LMICs in the near future, while the quality of care remains poor [15]. The incidence of LLA among diabetics is considered one of the markers of diabetes care quality, while the prevalence helps us to understand the extent and depth of the disease burden. Also, the worldwide prevalence of LLA is varies. To the best of our knowledge, this proposed study will be the first to provide an estimate of the incidence and prevalence of LLA among persons living with DM in LMICs. An understanding of the LLA burden will inform targeted response. Also, its distribution across various socio-demographic groups, as defined by age or gender, for instance, may help in identifying populations at risk and designing appropriate interventions targeting those groups. Likewise, variance across countries may inform future research studies which might look at the DM care in settings with a lower incidence of LLA and identify lessons that may be translated to other resource-limited settings. This review will follow a systematic approach using a predefined protocol and following standard recommendations for data extraction [32]. Potential limitations that may be encountered include heterogeneity in the individual studies related to the quality of the study designs, definitions used, or methods of assessing outcomes. We will, however, provide a detailed narrative report highlighting these discrepancies and provide suggestions for improving future studies.

Supporting information

S1 Appendix. Search strategy.

(DOCX)

Click here for additional data file.^{(19.2KB, docx)}

S1 Checklist

(DOCX)

Click here for additional data file.^{(32.9KB, docx)}

Funding Statement

The author(s) received no specific funding for this work.

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PLoS One. doi: 10.1371/journal.pone.0266907.r001

Decision Letter 0

Daoud Al-Badriyeh

27 Jan 2022

PONE-D-21-29205Lower limb amputations among individuals living with diabetes mellitus in low- and middle-income countries: a systematic review protocolPLOS ONE

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Please provide detailed responses to the reviewer's comments and suggestions, including clarifying the rationale behind this study in LMICs when similar studies in other settings exist already. Why/how would LLAs differ in LMICs, and what are the anticipated implications of this, needs elaboration. This is an important aspect of a study protocol.

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Comments to the Author

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Reviewer #1: Partly

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Reviewer #1: Partly

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Reviewer #1: Yes

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Reviewer #1: The study aimed to assess the incidence and prevalence of LLA as a complication of DM in LMICs. The study objectives are methodology clear, yet the significance, novelty, and implications were not highlighted clearly. There are several ideas that were repeated in different sections which negatively affected the flow and readability of the text. While the study appears to be sound, there are several grammatical errors. I advise the authors to work with a writing coach or copy editor.

Introduction: The flow of the introduction is a bit confusing and not easy to follow. There are several ideas that were repeated in this section.

Line 55-57: The sentence is long with 3 different ideas; I suggest splitting it into sentences.

Line 74: This idea was already stated earlier in the previous paragraphs.

Line 82: The sentence is long with 3 different ideas; I suggest splitting it into sentences.

Line 83: This sentence is about the decrease of LLA in HICs which was already mentioned before in the same paragraph (lines 75-77). Also, why Africa is mentioned as part of the sentence?

The last paragraph of the introduction does not clearly emphasize rationale of this study or the current research gaps.

Methods and analysis: There are several ideas that were repeated in this section.

I suggest using the Preferred Reporting Items for Systematic Reviews and Meta-analyses Protocols (PRISMA-P) guidelines for this protocol.

Line 124: Why would you limit the search to studies conducted from 1999? There is no clear epidemiological reason to limit the search to a specific time period.

In the inclusion criteria: Is there is any minimum sample size for each study or measure to be included?

In the exclusion criteria, will you exclude RCTs (which may report a prevalence measure at the baseline), case reports, or case series?

In the exclusion criteria, will you consider duplicate or overlapping studies (i.e., if two published studies are using the same population sample but there are conducting different analyses)?

Line 141: Why only from the first ten pages?

The data management section implies the same information as the screening process. Thus, I suggest merging them into one paragraph to avoid repetition.

Line 161: I suggest specifying what are study population measures that will be extracted, like "study population and its characteristics (sex, age, etc)".

Line 164: "time trend reported where available". This is not clear. What is the time trend you are going to extract is it the time since diagnosis of DM, time since LLA, years of data collection?

For the quality assessment tool, since it was adapted, a validation method should be considered before applying it (e.g., face validity, content validity, etc.).

Study outcomes paragraph: A clear definition of the outcomes should be mentioned. Also, it seems that it is written in separate lines, not as one paragraph.

Data analysis and result presentation: No clear or detailed plan for data synthesis and analysis is presented.

Line 178: I suggest removing this sentence as it is already mentioned under "data items and description".

Lines 181-183: The two sentences should be moved to the "study outcomes paragraph" as they represent a definition of the study's primary outcome (i.e., incidence).

Lines 182-183: How you are going to combine two incidence measures in the data synthesis and analysis while they have different denominators (i.e., either DM population at a country level or DM population presenting at healthcare facility). More clarification should be provided.

Lines 185-187: I think it would be good to add any potential reasons for not conducing a meta-analysis. A justification for using DerSimonian-Laird random-effects model should be stated. Also, will you consider any method for data transformation?

Discussion: This section does not reflect the significance and novelty of the current study, as well as the implications of the future findings.

Minor issues

Line 66: HbA1c was abbreviated without prior definition.

Line 59: Better to write it as "access to healthcare services"

Lines 130-133: Be consistent in the letter case of keywords.

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PLoS One. 2022 Apr 14;17(4):e0266907. doi: 10.1371/journal.pone.0266907.r002

Author response to Decision Letter 0

21 Mar 2022

Editor’s Comment: Please provide detailed responses to the reviewer's comments and suggestions, including clarifying the rationale behind this study in LMICs when similar studies in other settings exist already. Why/how would LLAs differ in LMICs, and what are the anticipated implications of this, needs elaboration. This is an important aspect of a study protocol.

Response: The burden of diabetes-related complications is especially high across LMICs where access to quality DM care is limited. With regard to LLA among persons living with diabetes, perhaps, one of the challenges in the response so far has been a poor understanding and awareness of the disease epidemiology in LMICs, which limits targeted response. While individual studies on LLA prevalence and incidence do exist in LMICs [16-19], no study has synthesised data from this region. Existing reviews had a global inclusion criteria [20, 21] but only one of them included few LMICs in their final analysis and that specific one did not follow a systematic approach [21]. Reasons for low or no representation of LMICs in previous studies is not known and estimates from these studies may not accurately reflect the situation in LMICs. In this study, we will define LMICs according to the World Bank income categories [22], taking care to apply our data synthesis and analyses to the sub-regions. This, to the best of our knowledge, will be the first systematic review of LLA among persons with diabetes in LMICs using this approach. This study therefore offers up-to-date data on the incidence and prevalence of diabetes-related LLA that can inform a much-needed response, priorities setting and further research.

Reviewer 1

Comment 1: Introduction: The flow of the introduction is a bit confusing and not easy to follow. There are several ideas that were repeated in this section.

Line 55-57: The sentence is long with 3 different ideas; I suggest splitting it into sentences.

Response: Thank you for the correction. We have now done a professional language editing to ensure clarity and flow of the write-up. We have separated these sentences and now reads:

“The burden of Diabetes Mellitus (DM) continues to grow, especially in low- and middle-income countries (LMICs) [1]. Since 1980, the number of persons living with DM globally has nearly quadrupled [1], with almost 80% of them residing in LMICs [2]. The rising DM prevalence is largely attributable to demographic transition, population ageing, obesity and unhealthy lifestyle behaviours”

Comment 2: Line 74: This idea was already stated earlier in the previous paragraphs.

Response: We have deleted the repeated statement on line 74.

Comment 3: Line 82: The sentence is long with 3 different ideas; I suggest splitting it into sentences.

Response: We have revised this section of the manuscript, which is the study justification section and it now reads:

“ The burden of diabetes-related complications is especially high across LMICs [1], where access to quality DM care is limited [15]. With regard to LLA among persons living with diabetes, perhaps, one of the challenges in the response so far has been a poor understanding and awareness of the disease epidemiology in LMICs, which limits targeted response. While individual studies on LLA prevalence and incidence do exist in LMICs [16-19], no study has synthesised data from this region. Existing reviews had a global inclusion criteria [20, 21] but only one of them included few LMICs in their final analysis but did not follow a systematic approach [21]. Reasons for low or no representation of LMICs in previous studies is not known and estimates from these studies may not accurately reflect the situation in LMICs. In this study, we will define LMICs according to the World Bank income categories [22], taking care to apply our data synthesis and analyses to the sub-regions. This, to the best of our knowledge, will be the first systematic review of LLA among persons with diabetes in LMICs using this approach. This study therefore offers up-to-date data on the incidence and prevalence of diabetes-related LLA that can inform a much-needed response, priorities setting and further research.”

Comment 4: Line 83: This sentence is about the decrease of LLA in HICs which was already mentioned before in the same paragraph (lines 75-77). Also, why Africa is mentioned as part of the sentence?

Response: We have revised this section as shown in response to comment 3.

Comment 5: The last paragraph of the introduction does not clearly emphasize the rationale of this study or the current research gaps.

Response: The last paragraph, that is, the justification for the study now reads:

“The burden of diabetes-related complications is especially high across LMICs [1], where access to quality DM care is limited [15]. With regard to LLA among persons living with diabetes, perhaps, one of the challenges in the response so far has been a poor understanding and awareness of the disease epidemiology in LMICs, which limits targeted response. While individual studies on LLA prevalence and incidence do exist in LMICs [16-19], no study has synthesised data from this region. Existing reviews had a global inclusion criteria [20, 21] but only one of them included few LMICs in their final analysis but did not follow a systematic approach [21]. Reasons for low or no representation of LMICs in previous studies is not known and estimates from these studies may not accurately reflect the situation in LMICs. In this study, we will define LMICs according to the World Bank income categories [22], taking care to apply our data synthesis and analyses to the sub-regions. This, to the best of our knowledge, will be the first systematic review of LLA among persons with diabetes in LMICs using this approach. This study therefore offers up-to-date data on the incidence and prevalence of diabetes-related LLA that can inform a much-needed response, priorities setting and further research.”

Methods and analysis:

Comment 6: There are several ideas that were repeated in this section.

I suggest using the Preferred Reporting Items for Systematic Reviews and Meta-analyses Protocols (PRISMA-P) guidelines for this protocol.

Response: The section has been re-ordered using the PRISMA-P guideline.

Comment 7: Line 124: Why would you limit the search to studies conducted from 1999? There is no clear epidemiological reason to limit the search to a specific time period.

Response: Given that we are also interested in exploring trends in epidemiology, with our focus on the past three decades, we will limit our analyses to studies conducted from 1990-2022.

Comment 8: In the inclusion criteria: Is there any minimum sample size for each study or measure to be included?

Response: As our study will involve multiple hierarchical datasets from each study (ie., prevalence across age- and sex- specific groups in each study), we are considering population denominators across each data point, and not necessarily sample size from the study, which is set at a minimum of 50.

Comment 9: In the exclusion criteria, will you exclude RCTs (which may report a prevalence measure at the baseline), case reports, or case series?

Response: Case reports and case series will be excluded. RCTs without a representative population denominator will be excluded.

Comment 10: In the exclusion criteria, will you consider duplicate or overlapping studies (i.e., if two published studies are using the same population sample but there are conducting different analyses)?

Response: For duplicate or overlapping studies, the study with the most detailed data will be included, and additional data, if necessary, extracted from others. We have now added a statement on this.

Comment 11: Line 141: Why only from the first ten pages?

Response: We have now removed this restriction.

Comment 12: The data management section implies the same information as the screening process. Thus, I suggest merging them into one paragraph to avoid repetition.

Response: We have now merged these sections:

“Articles retrieved from databases will be imported in Endnote to remove duplicates. Articles will then be exported into Covidence Systematic Review software (Veritas Health Innovation, Melbourne, Australia) for data management”.

Comment 13: Line 161: I suggest specifying what are study population measures that will be extracted, like "study population and its characteristics (sex, age, etc)".

Response: Study characteristics to be extracted include study population (described by age and sex), study setting/country, study design and period, funding source, year of data collection, sample size, and study denominator (population-level or health facility). We have now stated this.

Comment 14: Line 164: "time trend reported where available". This is not clear. What is the time trend you are going to extract is it the time since diagnosis of DM, time since LLA, years of data collection?

Response: We intended to measure differences in LLA incidence over years (1990-2022), where possible. Year(s) of data collection data will be helpful to ascertain that, and we have changed to “year(s) of data collection” for clarity.

Comment 15: For the quality assessment tool, since it was adapted, a validation method should be considered before applying it (e.g., face validity, content validity, etc.).

Response: We will now be using the validated Joanna Briggs Institute (JBI) critical appraisal tool for prevalence studies. Studies reporting incidence data will be appraised using validated tools appropriate for the study design. For instance, cohort studies will be critically appraised using the validated Newcastle-Ottawa quality appraisal tool for non-randomised studies [28].

Comment 16: Study outcomes paragraph: A clear definition of the outcomes should be mentioned. Also, it seems that it is written in separate lines, not as one paragraph.

Response: We have now merged the sentences as a paragraph and the definition of outcome is now provided:

“The primary outcome of this review is the incidence and prevalence of DM-related LLA in LMICs. Incidence will be defined as the number of new cases of LLA divided by the total DM population in the study during the specified period. Incidence measures will include incidence rate and cumulative incidence. Reporting of incidence at person level will be one amputation per person (the first or the highest) and both levels of amputation, major and minor will be considered. Prevalence will be defined as the total number of DM-related LLAs in the population for a given period. “

Comment 17: Data analysis and result presentation: No clear or detailed plan for data synthesis and analysis is presented.

Response: We have now improved on our data analysis plan:

“Median and interquartile range of all crude incidence rates will be reported. A Freeman–Tukey double-arcsine transformation will be applied to normalize data given an expected wide variation in extracted crude estimates from studies. Transformed data will be used to calculate summary proportion and 95% CI using a random effects model. A meta-analysis of the estimates of prevalence and incidence will be conducted if studies are sufficiently homogenous. We will assess heterogeneity using the X2 and I2 tests. I2 cut-off values of 0%, 25%, 50% and 75% will represent no, low, moderate and high level of heterogeneity [28]. We will conduct the meta-analysis following DerSimonian and Laird method [29]. Due to potential heterogeneity, DerSimonian-Laird random-effects model is preferred. DerSimonian and Laird method is a widely documented in the literature and is robust in various scenarios including skew-normal and extreme distributions for the effects [30]. However, where meta-analysis is not possible, a narrative synthesis of results will be done, using tables and figures as appropriate for data visualization. Also, in case of heterogeneity, we will carry out sub-group analysis and meta-regression analyses to show the potential sources of heterogeneity. Sub-group analysis will show the distribution across age group, sex and study regions. There should be at least 10 studies for each variable in the model for meta-regression analysis to be performed [31]. A sensitivity analysis will be performed to assess the robustness of the study estimates by assessing the effect of omitting a study at a time on the pooled estimate [31]. Lastly, a funnel plot asymmetry test and Egger’s test will be used to assess publication bias, if there are more than 10 included studies [31].”

Comment 18: Line 178: I suggest removing this sentence as it is already mentioned under "data items and description".

Response: The sentence has been removed.

Comment 19: Lines 181-183: The two sentences should be moved to the "study outcomes paragraph" as they represent a definition of the study's primary outcome (i.e., incidence).

Response: We have now moved the sentences to the study outcome paragraph as shown under comment 16.

Comment 20: Lines 182-183: How you are going to combine two incidence measures in the data synthesis and analysis while they have different denominators (i.e., either DM population at a country level or DM population presenting at healthcare facility). More clarification should be provided.

Response: Analysis will be conducted separately for population and hospital-based studies.

Comment 21: Lines 185-187: I think it would be good to add any potential reasons for not conducting a meta-analysis. A justification for using DerSimonian-Laird random-effects model should be stated. Also, will you consider any method for data transformation?

Response: A justification has been provided:

A meta-analysis of the estimates of prevalence and incidence will be conducted if studies are sufficiently homogenous. We will assess heterogeneity using the X2 and I2 tests. I2 cut-off values of 0%, 25%, 50% and 75% will represent no, low, moderate and high level of heterogeneity [28]. We will conduct the meta-analysis following DerSimonian and Laird method [29]. Due to potential high heterogeneity, DerSimonian-Laird random-effects model is preferred. DerSimonian and Laird method is widely documented in the literature and is robust in various scenarios including skew-normal and extreme distributions for the effects [30]”

Comment 22: Discussion: This section does not reflect the significance and novelty of the current study, as well as the implications of the future findings.

Response: We have revised this section as appropriate. The section now read:

“The burden of DM has been projected to grow exponentially in LMICs in the near future, while the quality of care remains poor [15]. The incidence of LLA among diabetics is considered one of the markers of diabetes care quality, while the prevalence helps us to understand the extent and depth of the disease burden. Also, the worldwide prevalence of LLA is varies. To the best of our knowledge, this proposed study will be the first to provide an estimate of the incidence and prevalence of LLA among persons living with DM in LMICs. An understanding of the LLA burden will inform targeted response. Also, its distribution across various socio-demographic groups, as defined by age or gender, for instance, may help in identifying populations at risk and designing appropriate interventions targeting those groups. Likewise, variance across countries may inform future research studies which might look at the DM care in settings with a lower incidence of LLA and identify lessons that may be translated to other resource-limited settings. This review will follow a systematic approach using a predefined protocol and following standard recommendations for data extraction [32]. Potential limitations that may be encountered include heterogeneity in the individual studies related to the quality of the study designs, definitions used, or methods of assessing outcomes. We will, however, provide a detailed narrative report highlighting these discrepancies and provide suggestions for improving future studies.”

Comment 23: Line 66: HbA1c was abbreviated without prior definition.

Response: We have now defined HbA1c

Comment 24: Line 59: Better to write it as "access to healthcare services"

Response: We have revised this section.

Comment 25: Lines 130-133: Be consistent in the letter case of keywords.

Response: Thank you for your observation. We have adjusted these.

“A comprehensive systematic search of the literature will be conducted on five databases: MEDLINE, Embase, Scopus, CINAHL, and African Journals Online (AJOL) using a combination of MeSH terms and keywords such as “diabetes”, “amputation”, “lower limb amputation”, “lower extremity amputation”, “amputee”, “incidence “ and “population study”

PLoS One. doi: 10.1371/journal.pone.0266907.r003

Decision Letter 1

Daoud Al-Badriyeh

30 Mar 2022

Lower limb amputations among individuals living with diabetes mellitus in low- and middle-income countries: a systematic review protocol

PONE-D-21-29205R1

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PLoS One. doi: 10.1371/journal.pone.0266907.r004

Acceptance letter

Daoud Al-Badriyeh

5 Apr 2022

PONE-D-21-29205R1

Lower limb amputations among individuals living with diabetes mellitus in low- and middle-income countries: a systematic review protocol

Dear Dr. Ajayi:

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on behalf of

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Supplementary Materials

S1 Appendix. Search strategy.

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Lower limb amputations among individuals living with diabetes mellitus in low- and middle-income countries: A systematic review protocol

Eyitayo Omolara Owolabi

Davies Adeloye

Anthony Idowu Ajayi

Michael McCaul

Justine Davies

Kathryn M Chu

Roles

Abstract

Background

Methods and analysis

Prospero registration number

Introduction

Aim and objectives

Methods

Eligibility criteria

Inclusion criteria

Exclusion criteria

Information sources and search strategy

Electronic searches

Searching of other sources

Study records

Data management and study selection process

Data extraction

Data items and description

General study information

Study characteristics

Outcome data

Case definitions

Study outcomes and prioritisation

Assessment of methodological quality of studies

Data analysis and presentation of results

Assessment of certainty of evidence

Discussion

Supporting information

Funding Statement

References

Decision Letter 0

Daoud Al-Badriyeh

Roles

Author response to Decision Letter 0

Decision Letter 1

Daoud Al-Badriyeh

Roles

Acceptance letter

Daoud Al-Badriyeh

Roles

Associated Data

Supplementary Materials

ACTIONS

PERMALINK

RESOURCES

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