HIV infection and multidrug resistant tuberculosis: a systematic review and meta-analysis

We researched on PubMed, Google Scholar, and Science Direct databases to select eligible peer-reviewed articles for our systematic review and meta-analysis. Relevant observational studies (cross-sectional, case-control, and cohort) were screened to assess the association between HIV infection and MDR-TB, published from January 1, 2010, to July 30, 2020 (date of the last search). The screening language was restricted to English. The particular keywords used for searching articles were “Multidrug-resistant tuberculosis” or “MDR-TB” or “Drug-resistant TB” or “Risk factors of MDR-TB” or “Predictors of MDR-TB” and “HIV” or “Human Immunodeficiency Virus”. A summary of search terms is provided in Appendix A. Search results were compiled using a citation management software Zotero. In addition to databases used, we explored references of selected studies to incorporate all potential pertinent articles to construct our summary estimates. The study adheres to the Preferred Reporting Items for Systematic Review and meta-analysis (PRISMA) guidelines [17]. The protocol was registered in the PROSPERO database-CRD42019132752.

The primary outcome of the meta-analysis was an unadjusted odds ratio exhibiting the crude association between HIV infection and MDR-TB. The articles that reported or provided adequate data to calculate the frequency of MDR-TB and non-MDR-TB, subdivided by HIV status (positive or negative), were included in our systematic review. We included studies where MDR-TB is the outcome of interest. We contacted the author for the insufficient information given in any study. If the author didn’t reply, we excluded the article. To be eligible for inclusion, any drug susceptibility testing method (culture on solid and/or liquid media, molecular techniques, clinical records, Table 1) were accepted for the diagnosis of multidrug-resistant tuberculosis (Mycobacterium tuberculosis strain resistant at least to rifampicin and isoniazid). The comparison group (non-MDR-TB) consisted of drug-susceptible tuberculosis patients and/or resistant to any single drug. HIV status was ascertained by HIV test reports, clinical/hospital records, databases/registers, or directly from patients. Studies reported on non-tuberculous mycobacterium, case reports, case studies, systematic review, meta-analysis, a duplicate publication of the same study, and studies with only abstract were excluded. We also didn’t include grey literature (theses and dissertations). Studies with less than three HIV/MDR-TB participants were excluded because these studies cause the analysis to be heterogeneous. Titles and abstracts of the studies obtained from database searches were screened independently by two reviewers ZZS and FH. Full text of potential articles was further reviewed for eligibility regardless of the study base (hospital or population). Articles might have been eliminated for more than one rationale. Any disagreements were discussed with senior authors (JB or AH) until a consensus was reached or by the arbitration of AH alone.

A pre-specified and standardized form was used for data abstraction. For the estimation of the crude odds ratios, key data on the number of MDR-TB HIV positive, number of MDR-TB HIV negative, number of non-MDR-TB HIV positive, and number of non-MDR-TB HIV negative patients were extracted from each study. Additionally, data on the name of the first author, country, year of publication, years of recruitment, study design (cross-sectional, case-control or cohort), source of data (hospital/medical records, lab reports, database/register, or direct from the patients), methods carried out to determine drug resistance pattern, number of enrolled TB patients, the mean or median age of the MDR-TB cases, proportion of male patients among MDR-TB cases (%), type of MDR-TB (primary, secondary or both), form of tuberculosis (pulmonary, both pulmonary and extra-pulmonary or not defined), and proportion of the patients with extra-pulmonary tuberculosis among MDR-TB cases (%) were entered in the spreadsheet. We further stratified the articles based on global regions (defined by World Health Organization) income level (World Bank classification by income, GNI per capita) and burden for MDR-TB (list used by WHO 2016–2020) of the countries [1, 72]. Data abstraction from individual studies was executed by two trios of investigators (AI, JB & ZZS and HRK, DHH & FH), from March 2019 to June 2020. The presence of any inconsistency in data extraction was verified by a seventh investigator (AH).

Two trios of investigators (AI, JB & ZZS and HRK, DHH & FH) scored each study to ascertain methodological quality independently. The corresponding author (AH) subsequently examined all the assessments. Furthermore, contentions aroused in the course of quality scoring were resolved through discussions between investigators. It was evaluated using the Newcastle-Ottawa Scale (NOS). It consists of three domains: selection, comparability, and exposure or outcome of interest. Few points on the NOS related to appropriate methods for evaluating exposure variables and outcomes were designed for the relevance to our research question (Supplementary file 1). Two outcome groups were considered comparable if the HIV status was adjusted for the previous history of diagnosis with tuberculosis and/or any other sociodemographic variable (e.g., age, sex, etc.). These studies also reflect high or medium NOS scores (Supplementary file 2). Articles were given scores to reflect methodological stringency, lucidity, and transparency in reporting. Nevertheless, we did not exclude any articles based on quality scoring. It may exclude studies coming from resource-limited settings. Therefore, we did not provide insight into this particular cluster of studies. Moreover, the PRISMA statement consists of a checklist of 27 items and is given in Supplementary file 3.

We performed data analysis using meta and metafor packages in the R statistical software (version 3.5.1). We calculated crude odds ratio with a 95% confidence interval (CI) for individual study from the abstracted frequencies (numerators and denominators). After that, we estimated the pooled odds ratio (overall) using the random-effects model, allowing the true effect size to vary from study to study. The summary estimate (OR) for the association between HIV infection and MDR-TB were reported with 95% CI. The calculated odds ratio of each study and the combined effect estimate with 95% CI were graphically represented by forest plots. Publication bias was assessed by observing the symmetry of funnel plots visually. Further confirmation was conducted using Egger’s test (weighted regression with multiplicative dispersion model), while the p-value < 0.10 was suggestive of statistical significance. Heterogeneity across the selected studies was assessed by I² statistic (> 75% signifies substantial, 50–75% moderate and 25–50% low heterogeneity). The I² statistic represents the percentage of total variation across studies due to heterogeneity rather than chance. We also conducted a sensitivity analysis that removed the study contributing to the highest weight to evaluate the robustness of the findings.

Analysis of the subgroups was carried out to determine the pooled odds ratio for each group and to look for potential explanations of the heterogeneity. Pre-determined subgroups were WHO global regions (Africa, Europe, South-east Asia, America, Pacific, and Eastern Mediterranean), the income level of the country (high, upper-middle, lower-middle and low), the burden for MDR-TB on the country (high and low), design of the study (cross-sectional, case-control and cohort), type of MDR-TB (primary, secondary and both), mean or median age 40 years and older, and diagnostic method used for MDR-TB (culture and culture and/or molecular technique). Funnel plot asymmetry and egger’s tests were done to assess the presence of publication bias in each subgroup.

We conducted sensitivity analyses that excluded each of the following types of studies: studies with fewer than 1000 participants; studies from countries in Africa; and studies published in 2015 or earlier. Forest plots are reported in Supplementary file 5. When considering studies of more than 1000 participants, the OR of MDR-TB among HIV infected individuals tends to be 1.41 (OR=1.41, CI=1.13–1.76). The OR is 1.38 (CI=1.01–1.88) considering studies published after 2015. The OR is also 1.46 when studies outside African studies (OR=1.46, CI=1.14–1.87) are considered. The findings are, therefore, similar to the meta-analysis with 54 studies.