Skip to main content
  • Research article
  • Open access
  • Published:

Small contribution of gold mines to the ongoing tuberculosis epidemic in South Africa: a modeling-based study

A Correction to this article was published on 28 December 2018

This article has been updated

Abstract

Background

Gold mines represent a potential hotspot for Mycobacterium tuberculosis (Mtb) transmission and may be exacerbating the tuberculosis (TB) epidemic in South Africa. However, the presence of multiple factors complicates estimation of the mining contribution to the TB burden in South Africa.

Methods

We developed two models of TB in South Africa, a static risk model and an individual-based model that accounts for longer-term trends. Both models account for four populations — mine workers, peri-mining residents, labor-sending residents, and other residents of South Africa — including the size and prevalence of latent TB infection, active TB, and HIV of each population and mixing between populations. We calibrated to mine- and country-level data and used the static model to estimate force of infection (FOI) and new infections attributable to local residents in each community compared to other residents. Using the individual-based model, we simulated a counterfactual scenario to estimate the fraction of overall TB incidence in South Africa attributable to recent transmission in mines.

Results

We estimated that the majority of FOI in each community is attributable to local residents: 93.9% (95% confidence interval 92.4–95.1%), 91.5% (91.4–91.5%), and 94.7% (94.7–94.7%) in gold mining, peri-mining, and labor-sending communities, respectively. Assuming a higher rate of Mtb transmission in mines, 4.1% (2.6–5.8%), 5.0% (4.5–5.5%), and 9.0% (8.8–9.1%) of new infections in South Africa are attributable to gold mine workers, peri-mining residents, and labor-sending residents, respectively. Therefore, mine workers with TB disease, who constitute ~ 2.5% of the prevalent TB cases in South Africa, contribute 1.62 (1.04–2.30) times as many new infections as TB cases in South Africa on average. By modeling TB on a longer time scale, we estimate 63.0% (58.5–67.7%) of incident TB disease in gold mining communities to be attributable to recent transmission, of which 92.5% (92.1–92.9%) is attributable to local transmission.

Conclusions

Gold mine workers are estimated to contribute a disproportionately large number of Mtb infections in South Africa on a per-capita basis. However, mine workers contribute only a small fraction of overall Mtb infections in South Africa. Our results suggest that curtailing transmission in mines may have limited impact at the country level, despite potentially significant impact at the mining level.

Peer Review reports

Background

Gold mines in South Africa have historically been implicated in initiating the tuberculosis (TB) epidemic in South Africa. As Packard notes, “The immense size of the mine labor force, over 200,000 on the Rand alone by 1910, together with the appalling health conditions that existed on the mines, ensured that they would play a central role in the early development of TB in southern Africa” [1].

To what extent gold mines continue to contribute to TB in South Africa, however, is subject to debate. Several factors complicate this question. Within the mines, crowding, insufficient ventilation, and warm, humid air may increase the rate of Mycobacterium tuberculosis (Mtb) transmission. Biological and social factors may then affect the extent to which Mtb spreads among mine workers and from mine workers to other groups. For example, mine workers and residents of other areas with whom they interact may already have latent tuberculosis infection (LTBI), which confers partial immunity to reinfection despite posing a longer-term risk for reactivation in the future [2]. Both mine workers and residents of other communities may also carry high burdens of HIV infection, increasing their rate of reactivation [3,4,5]. Finally, mixing patterns between mine workers and other residents may determine to what extent mine workers contribute to the larger epidemic [2, 6]. For example, estimating the risk of TB infection in peri-mining residents due to mine workers requires one to account for the probability that susceptible peri-mining residents come into contact with infectious mine workers, which depends on the size of each group, the prevalence of LTBI and active TB in each group, and the amount of time the groups spend together. On a longer time scale, labor-related migration and repatriation of mine workers are also likely to affect how widely mine workers may spread infections [2, 6].

Mathematical models have served as useful tools for understanding the TB epidemic in South Africa. For example, at the country level, models have been used to predict the impact of implementing different interventions [7,8,9,10]. Models have also proved useful for understanding more local disease dynamics, e.g., at the level of a city [11] or in specific environments such as a prison [12] or a household [13]. More recently, models have also been applied to the gold mines in South Africa to understand the results of the Thibela TB study, which tested a sustained campaign of preventive therapy among mine workers [14, 15]. However, models have not yet addressed how mine workers mix with other groups and whether these interactions contribute to overall TB burden.

To estimate the contribution of gold mines to the ongoing TB epidemic in South Africa, we developed two computational models and applied them to gold mine workers and mining-related groups in South Africa. First, we developed a simplified static risk model that accounts for data on gold mine workers and peri-mining, labor-sending, and other residents of South Africa and estimates the force of infection (FOI) and fraction of transmission events (new infections) in each community that are attributable to local residents compared to residents from other areas. Secondly, we developed a dynamic, individual-based model of TB that accounts for longer-term trends in demographics and risk factors and also features a more detailed disease natural history to estimate the fraction of incidence attributable to transmission from gold mine workers. Together, these tools provide quantitative estimates that address to what extent gold mines are continuing to contribute to the TB epidemic in South Africa.

Methods

Epidemiological data sources

We consider four residency groups in South Africa: gold mine workers, peri-mining residents, labor-sending residents, and other residents of South Africa. Our primary data source for mine workers was data collected during the Thibela TB study [16]. Peri-mining communities were identified based on proximity to Thibela TB study sites, comprising the Lejweleputswa (Free State province), West Rand (Gauteng province), and Dr Kenneth Kaunda (North West province) districts. Labor-sending communities were identified as the OR Tambo and Alfred Nzo (Eastern Cape province) and Ugu and Sisonke (KwaZulu-Natal province) districts. Other residents of South Africa were assumed to comprise all remaining districts. Residents of areas outside of South Africa were not considered.

Input parameters

In the models we accounted for three general categories of parameters: population size, disease natural history, and population mixing. Population sizes were taken from the South Africa Census 2011 [17]. For the mine worker population, we considered both gold mine workers and mine workers of other commodities, representing an upper limit on the at-risk population [18, 19]. The epidemiological characteristics of each population were derived from the literature. Measurements of TB incidence and prevalence at the country level were taken from World Health Organization estimates [20] and at the mine level from the Thibela TB study [21], while HIV prevalence and antiretroviral therapy (ART) coverage were taken from Joint United Nations Programme on HIV/AIDS (UNAIDS)-based measurements [22]. Disease natural history parameters were similar to those found in other TB models and included the rate at which infected individuals progress to active disease as a result of primary disease or reactivation, the effect of HIV on reactivation, and the frequency of different forms of active disease (smear-positive, smear-negative, and extra-pulmonary) and relative infectiousness of each form (Additional file 1: Table S1). Parameters specific to mining included a multiplier for increased Mtb transmission in the mines, the prevalence of silicosis among mine workers, and the effect of silicosis on reactivation (Additional file 1: Table S2). South Africa-specific estimates of healthcare access and treatment effectiveness via directly observed therapy short-course (DOTS) were also included (Additional file 1: Table S3). Population mixing parameters were taken from national tourism surveys [23] as well as data collected during the Thibela TB study (Additional file 1: Table S4).

Description of static risk model (spreadsheet model)

To account for the current state of the TB epidemic in mining and mining-related communities in South Africa and short-term, sub-annum processes that relate to TB transmission between these communities, we developed a static risk model. The model represents a Taylor series-type approximation of dynamic processes such as the generation of new infections given the number of susceptibles and prevalent cases in each population and the effect of risk factors such as increased Mtb transmission in the mines and HIV in the overall population. These quantities are not updated iteratively in the model; therefore, the model represents a short-term, 1-year projection of these quantities.

The static risk model (spreadsheet model) was encoded in Excel and comprises formulas to calculate the FOI (per-susceptible rate of infection) and number of infections occurring in each group (Fig. 1a). A “who acquires infection from whom” (WAIFW) matrix [24] was derived where each element βij represents the rate of Mtb transmission from infectives in group j to susceptibles in group i for every community k where contact was assumed possible (spreadsheet matrix 1). Each element of the WAIFW matrix was based on a base rate of transmission β0 which we defined as the number of new infections generated by each infective case per year averaged over smear-positive, smear-negative, and extra-pulmonary forms of disease. β0 was multiplied by a community-specific transmission multiplier ck, which accounts for multiple environmental factors and was calibrated in the individual-based model, and the fractions of each year pik and pjk that individuals from groups i and j, respectively, spend in community k (Fig. 1b). pik and pjk were converted to a frequency of contact between individuals from groups i and j in community k by dividing by the total number of individuals Nk present in community k at any given time, i.e., assuming frequency-dependent transmission [25]. βij was then calculated by summing this product over the set A of all communities k where groups i and j spend time.

$$ {\beta}_{ij}={\beta}_0{\sum}_{k\in A}\frac{c_k{p}_{ik}{p}_{jk}}{N_k} $$
Fig. 1
figure 1

Disease state transitions and groups represented in the static risk and individual-based models. a Disease transitions in the static risk model were limited to new infections and reactivation from existing latent infections, while the individual-based model also represented longer-term processes such as new infections contributing to prevalence (not shown). b Population mixing patterns as fraction of time per annum spent in a different community (for short-term mixing) or probability of residency change per annum (for longer-term migration). Both static risk and individual-based models represent short-term mixing, but only the individual-based model represents longer-term migration. S+/− silicosis presence/absence, M mining resident, LS labor-sending resident

Additional quantities were derived using the WAIFW matrix:

  • λij: The FOI among susceptibles in group i attributable to infectives from group j, calculated by multiplying βij by the number of infectives in group j (spreadsheet matrix 2). The sum over all j for a given i provides the overall probability of infection per year for susceptibles in group i.

  • Lij: The rate of infection in group i per-capita attributable to group j, calculated by multiplying λij by the fraction of group i who are susceptible where susceptible is defined as uninfected or latently infected but susceptible to reinfection (spreadsheet matrix 3).

  • PAF(λij): The population attributable fraction (PAF) of FOI in group i attributable to group j, calculated by dividing each by the sum of λij over all j for a given i (spreadsheet matrix 4).

  • PAF(Lj): The PAF of all new infections in South Africa attributable to group j, calculated by dividing the number of infections attributable to group j (i.e., the sum of Lij over all i for a given j) by the total number of infections (i.e., the sum of Lij over all i and all j) (spreadsheet matrix 5).

  • pcPAF(Lj): The PAF of all new infections in South Africa attributable to group j relative to the size of j (i.e., per-capita j) calculated by dividing PAF(Lj) by the fraction of the South African population that group j represents (spreadsheet matrix 6). This represents the contribution of a particular group relative to its population size including both susceptible and infected individuals.

In the static risk model we also calculated a near-term estimate of TB incidence Ii in each group i (Fig. 1a). In this case near-term refers to 1 year in the future, as prevalence after the first year was not updated to include new cases or losses due to treatment or death. Near-term incidence accounted for TB cases from primary disease resulting from new infections in a given year and TB cases from reactivation of a stable pool of latent infections. Specifically near-term incidence was calculated as the sum of incidence from five sources: (1) primary disease from new infections (k1Li), (2) reactivation from non-silicotic, non-HIV-positive latent infections (k2(1 – Si)(1 – Hi)Pi), (3) reactivation from non-silicotic, HIV-positive latent infections (k2m0,H(1 – Si)HiPi), (4) reactivation from silicotic, non-HIV-positive latent infections (k2ms,0Si(1 – Hi)Pi), and (5) reactivation from silicotic, HIV-positive latent infections (k2ms,HSiHiPi). Here k1 and k2 represent base rates of primary disease in newly infected and reactivation in latently infected individuals, respectively, and Li was derived from Lij above. Si, Hi, and Pi represent the stable prevalence of silicosis, HIV, and LTBI in group i, and ms,0, m0,H, and ms,H represent multipliers on k2 for silicotic, HIV-positive, and simultaneously silicotic and HIV-positive individuals, respectively. HIV-positive latent infections were further subdivided into those receiving or not receiving ART, each assigned a separate multiplier on k2. Because the static risk model did not account for longer-term migration, e.g., for mine workers repatriating to labor-sending areas, the prevalence of silicotics in non-mining areas was assumed to be zero. The resulting values of Ii were compared to published values for mine workers from the Thibela TB study and for all South Africa from WHO estimates (spreadsheet matrix 7).

Monte Carlo simulations were performed where the mine-specific transmission rate and immunity from reinfection were sampled from normal distributions, while all other parameters were held at baseline values. For the mine-specific transmission rate, 95% of the density was assumed to lie within −20% and +20% of the baseline value. This range was selected based on the Gammaitoni-Nucci equation [26], which specifies that the probability of an individual acquiring an infection in a confined space increases exponentially as the inverse of ventilation rate. Therefore, a −20% or +20% difference in transmission rate could result from a +25% or −17% change in ventilation rate, respectively; these were similar to values from the individual-based model calibration (cf. Additional file 1: Figure S2B, S2C). For immunity from reinfection, 95% of the density was assumed to lie within −40% and +40% of the baseline value. One thousand randomly drawn pairs of values for these two parameters were used, and 95% confidence intervals (CIs) were taken from the 0.025 and 0.975 quantiles of the resulting output values. Both the static risk model and the individual-based model as well as input parameter files are available on GitHub (https://github.com/SCTX/mining_contribution).

Description of individual-based model

While the static risk model accounts for the current state of the TB epidemic and processes occurring on a sub-annum time scale, particularly population mixing, it does not update the prevalence of different disease states iteratively and does not represent longer-term changes in demographics and risk factors such as HIV. To provide a longer-term representation of the TB epidemic, we developed a dynamic, individual-based model; this model was coded in C++ and based on the TB model available in the EMOD software package [27]. We briefly describe the model here; parameter values and additional details are provided in Additional file 1: Tables S1–S4. Individuals were assigned one of the following disease states: susceptible, latently infected, active pre-symptomatic, active symptomatic, and recovered. Individuals transitioned between these states randomly according to exponentially distributed delays. Birth and non-disease death processes were represented whereby individuals were added to and removed from the simulation at rates consistent for South Africa. A residency status in one of the four groups in the model (mining, peri-mining, labor-sending, and other South Africa) was assigned at birth. Residency status was retained for the lifetime of the individual except for individuals born with labor-sending group status who transitioned to mining status during adulthood and then back to labor-sending status upon retirement. Short-term mixing between groups representing regular visits from mine workers to peri-mining or labor-sending communities was specified by an interaction matrix as in the static risk model. The numbers of discrete agents in the model were scaled in the output to reflect the sizes of the real populations: individuals in mining, peri-mining, and labor-sending groups by approximately 50:1 and in other South Africa by approximately 400:1. These scale factors corresponded to 2011 population sizes of approximately 0.5 million (M), 2.1 M, and 3.4 M in mining, peri-mining, and labor-sending areas, respectively, and 47 M in the remainder of South Africa [17].

Two risk factors were represented in the individual-based model, HIV infection and silicosis. HIV infection was distributed to individuals according to age-specific rates of infection; these were generated from the EMOD HIV model calibrated to South Africa [28] and assumed to be the same across residency groups [29,30,31]. The EMOD HIV model assigned a CD4 count to each individual which declined linearly with time in the absence of treatment [29,30,31]. ART was distributed to HIV-positive individuals according to eligibility guidelines in South Africa and matched population coverage estimates [22]. ART had the effect of increasing CD4 levels in the model [29,30,31]. Silicosis was acquired by mining group individuals at a rate consistent with radiographic observations in mine workers, at approximately 1% per year of employment [32,33,34] (Additional file 1: Table S2).

Susceptible individuals in the model were infected at a rate that differed by residency group and depended on the total infectiousness of other groups and the frequency of group interactions. The infectiousness of each group depended on the prevalence of different forms of active TB, where pre-symptomatic, smear-negative, and extra-pulmonary forms of disease were assumed to contribute less infectiousness than smear-positive disease. Data on the frequency of group interactions were specified by a WAIFW matrix as in the static risk model [35].

Infected individuals transitioned to active disease with one of two rates representing primary and reactivation disease. Active disease in the model included a pre-symptomatic period of set duration followed by symptomatic disease of smear-positive, smear-negative, or extra-pulmonary forms. Individuals persisted in symptomatic disease until progressing to self-cure, treatment, or death. HIV and silicosis had the effect of increasing the rate of reactivation, represented as multipliers on the base rate of reactivation [36]. For HIV-positive individuals, the magnitude of the increase varied as the inverse of CD4 level.

Individuals with active symptomatic disease were assumed to seek care at high or low rates corresponding to high- or low-quality access to care, respectively, broadly representing different levels of care in South Africa. Upon accessing care, symptomatic individuals were assumed to receive a sputum smear or GeneXpert test, depending on whether care was sought before or during DOTS availability. The probability of a positive test result corresponded to observed test sensitivities. If a positive test result was obtained, an individual was assumed to undergo treatment, with a rate of disease clearance that depended on whether treatment was given before or during DOTS availability. Following treatment, individuals transitioned to a recovered state that was identical to the susceptible state but assumed to have a reduced probability of reinfection due to immunity.

Individual-based model calibration and application

Several historical population-wide events were simulated in the individual-based model. During each simulation the model was seeded and run for a specified burn-in period. With a burn-in period of 100 simulated years, incidence and mortality were observed to be stable in the different groups in the model, consistent with endemic TB. HIV, DOTS, and ART were introduced at simulated years 1985, 2002, and 2007, respectively, representing country-wide trends.

The model was calibrated to TB incidence in mining areas measured during the Thibela TB study [21] and TB incidence and mortality at the country level for multiple years [37]. Parameters for the transmission rate in mining areas and immunity to reinfection following previous TB exposure were varied during calibration. The transmission rate in mining areas was parameterized as a multiple of the base transmission rate and represented the aggregate environmental factors, e.g., reduced ventilation rates, that may increase Mtb transmission in mines. A likelihood score for each parameter combination was computed using a likelihood function based on a normal distribution where the differences between published high and low estimates of incidence and mortality were taken to represent 95% CIs and the three epidemiological indicators were equally weighted. The joint posterior distribution of the two parameters conditional on the data were estimated via incremental mixture importance sampling (IMIS) [38]. The joint distribution was found to be unimodal and strongly peaked; therefore, parameters for subsequent simulations were set at the maximum a posteriori estimate (joint posterior distribution, Additional file 1: Figure S2A; marginal distributions, Figure S2B, S2C in Additional file 1). For consistency, the values for these parameters were also used in the spreadsheet model. The posterior estimate of the reduction in susceptibility to reinfection was similar to previous estimates of bacille Calmette-Guerin (BCG) protection against active disease, 0.58 (95% CI 0.35–1.01) [39]. Technical details regarding the calibration procedure are available in Additional file 1.

To measure the incidence attributable to mine workers using the individual-based model, we simulated two counterfactual scenarios: first, having no Mtb transmission in the mines and, second, having no Mtb transmission in any area. These scenarios were identical to the baseline scenario until simulated year 2012 when Mtb transmission was stopped in the model. Other processes such as disease progression continued unchanged. The numbers of new cases of active disease between simulated years 2014 and 2019 were counted for each counterfactual scenario and compared to the baseline scenario. This calculation was repeated for each residency group in the model.

Results

Most force of infection in communities is attributable to local residents

We used a static risk model to calculate the FOI and number of transmission events (new infections) in different mining-related communities in South Africa and predict the near-term (following-year) incidence in these communities (Fig. 1a). The model accounted for a number of factors including a higher rate of Mtb transmission due to environmental factors and the amount of time that residents reported spending in their own versus other communities, where mixing was assumed to be proportional to the time spent in each community (Fig. 1b).

As a check on the static risk model, we compared FOI output from the model to data on the annual risk of TB infection (ARTI) in children. Under baseline parameters, we estimated FOI to be 21.2% (95% CI 16.4–26.1%) in mine workers, 4.3% (95% CI 4.3–4.3%, indicating a difference of < 0.05%) in peri-mining residents, 5.8% (95% CI 5.8–5.8%) in labor-sending residents, and 3.5% (95% CI 3.5–3.5%) in other South African residents (Table 1, Additional file 1: Table S5). CIs were derived by sampling parameter values for mine-specific transmission and immunity following previous infection. The FOI estimate for other South African residents in the model was found to be consistent with available ARTI measurements: 2.5–4.2% (across Western Cape, 2005, [40]), 3.8–4.5% (in Cape Town, 2005, [41]), 3.9–4.8% (in Cape Town, 2009, [42]), and 2.1–5.2% (in Johannesburg, 2013, [43]).

Table 1 Force of infection (per-susceptible rate of infection) attributable to each population

Using the static risk model, we then calculated the fraction of FOI in each community attributable to each residency group. We estimated that the majority of each community’s FOI was attributable to local residents: 93.9% (95% CI 92.4–95.1%), 91.5% (95% CI 91.4–91.5%), 94.7% (95% CI 94.6–94.7%), and 98.8% (95% CI 98.8–98.8%) in mining, peri-mining, labor-sending, and other SA communities, respectively (Table 1, Additional file 1: Table S5). Despite the amount of time mine workers were assumed to spend in other areas (up to 20% per annum), the FOI in peri-mining, labor-sending, and other SA communities attributable to mine workers was estimated to be 5.8% (95% CI 5.8–5.8%), 3.6% (95% CI 3.5–3.6%), and 0.1% (95% CI 0.1–0.1%), respectively.

Gold mine workers contribute more TB infections per capita than other residents

Using the preceding FOI and data on susceptible individuals, i.e., either uninfected or latently infected but susceptible to reinfection, we estimated the number of new infections expected to occur in each community and compared these results to published TB incidence for different communities. For mine workers and the overall population, we estimated TB incidence to be 2963 (95% CI 2208–3858) and 989 (95% CI 980–1000) per 100,000 individuals, respectively. These were similar to published values for these communities, 2957 (in control cluster mines during the Thibela TB study, between 2006 and 2010 [21]) and 977 (717–1276) (in South Africa, 2008 [20, 44]) per 100,000 (Additional file 1: Table S6).

Using the static risk model, we also estimated the fraction of infections occurring each year attributable to each residency group. Out of the overall number of new infections occurring in South Africa per annum, we estimated that 4.0% (95% CI 2.6–5.8%), 5.0% (95% CI 4.5–5.5%), and 9.0% (95% CI 8.8–9.1%) were attributable to mining, peri-mining, and labor-sending residents, respectively (Table 2, Additional file 1: Table S7). When scaled to the fraction of the overall population in South Africa that each group represents, mine workers, peri-mining residents, and labor-sending residents contributed 4.32 (95% CI 2.77–6.15), 1.21 (95% CI 1.09–1.34), and 1.39 (95% CI 1.36–1.41) times as many infections as South Africans as a whole (Table 2, Additional file 1: Table S7). Similarly, when scaled to the fraction of the overall number of prevalent cases in South Africa found in each group, mine workers, peri-mining residents, and labor-sending residents contributed 1.62 (95% CI 1.04–2.30), 1.14 (95% CI 1.02–1.25), and 1.07 (95% CI 1.05–1.09) times as many infections as South Africans as a whole (Table 2, Additional file 1: Table S7). Therefore, while mine workers contribute a larger number of infections on a per-capita or per-prevalent case basis than other South Africans, the majority of these infections occur among mine workers themselves.

Table 2 New infections in all South Africa attributable to each population

Local recent transmission is the source of the majority of incident TB cases in gold mines

To measure the impact of Mtb transmission in the mines on incidence, we used a dynamic, individual-based model of TB in South Africa. In this model we accounted for longer-term demographic changes and additional pathways leading to active disease including reactivation from transmission occurring over a longer time window. We calibrated the model to several epidemiological indicators including incidence and mortality over multiple years [21, 37]. Model estimates of TB incidence and mortality overlapped published ranges, both at the country level (Fig. 2a, b; Additional file 1: Figure S3A, S3B) and at the mining level (Fig. 2c, d; Additional file 1: Figure S3C, S3D). In particular, model incidence reproduced measurements from the Thibela TB study, showing a threefold higher incidence in the mines compared to South Africa overall (Fig. 2a, c). Model incidence in the mines preceding the Thibela TB study was exceeded 4000 per 100,000 (Fig. 2c), consistent with previous studies on mine workers [45]. Model mortality due to TB among mine workers was approximately 1% per annum (Fig. 2d), which was consistent with a range that includes the 0.9% all-cause mortality rate and 4.3% all-cause mortality-plus-medically boarded rate observed as a secondary outcome of the Thibela TB study [21]. As an additional test of the model, including South Africa-specific parameters derived from calibration, we used the model to simulate the Thibela TB study intervention of widely available preventive therapy. Following a cessation of the intervention, we observed a rebound in model incidence similar to the rebound observed during the Thibela TB study (Additional file 1: Figure S4A).

Fig. 2
figure 2

Simulated time series of the TB epidemic in different communities in South Africa. Means and 95% CIs were derived from 200 stochastic realizations of the model where input parameters were set at the mode of the posterior distribution of two calibration parameters. a TB incidence in peri-mining, labor-sending, and other South Africa residents. b TB mortality in peri-mining, labor-sending, and other South Africa residents. In a and b, the population-weighted mean of the four populations in the model is also shown. c TB incidence in mine workers. d TB mortality in mine workers. e Methodology for computing the fraction of incidence attributable to recent Mtb transmission in the mines. The upper curve is identical to the curve in c, while the lower curve represents the mean and 95% CI of stochastic realizations that were identical to c until simulated year 2012, after which Mtb transmission from mine workers was stopped but all other aspects of the model remained unchanged. Attribution was calculated from the difference in incidence between simulated years 2014 and 2019

To estimate the fraction of incident cases attributable to gold mines, we simulated a counterfactual scenario of stoppage of Mtb transmission in mining areas and measured the subsequent change in incidence over several years (Fig. 2e). By doing so, we estimated that recent Mtb transmission in the mines contributed 58.2% (95% CI 57.8–58.9%), 4.8% (95% CI 4.3–5.2%), and 4.9% (4.4–5.2%) of the TB incidence in mining, peri-mining, and labor-sending residents, respectively (Table 3). Among other residents of South Africa, the counterfactual scenario had a smaller effect that resulted in a time course that overlapped the baseline scenario at all time points, i.e., within the stochastic noise of the simulation (Table 3). In South Africa as a whole, the fraction of TB incidence due to recent Mtb transmission in the mines was estimated to be 2.4% (95% CI 1.4–3.3%) (Table 3). To test the robustness of this measurement, we performed a series of one-way sensitivity analyses based on varying the infectiousness in each community separately (mining, peri-mining, labor-sending, and other South Africa). In all cases, the resulting fraction of TB incidence due to recent Mtb transmission in the mines was found to vary maximally between 1 and 4% (Additional file 1: Figure S5).

Table 3 Incidence attributable to recent transmission in mining areas

As a second counterfactual scenario, we simulated stoppage of transmission in all areas of South Africa and calculated the fraction of incident cases attributable to recent transmission from any source. Among mining residents, 63.0% (95% CI 58.5–67.7%) of the incident cases were predicted to result from recent transmission, 92.5% (95% CI 92.1–92.9%) of which were attributable to recent transmission in mining areas (Table 3). In contrast, among all South African residents, 37.4% (95% CI 35.2–40.0%) of the incident cases were predicted to result from recent transmission, 3.7% (95% CI 3.0–4.4%) of which were attributable to recent transmission in mining areas (Table 3). These figures were consistent with local Mtb transmission in mines being the source for the majority of incident TB cases in the mines but only a small fraction of the incident TB cases in the remainder of the country.

Discussion

Using two different modeling approaches, we found that gold mine workers are likely to be contributing to the TB burden in South Africa but primarily at the level of their own communities and not the larger population of South Africa, owing to the generalized nature of the TB epidemic in South Africa. Using a static risk model, we captured several parameters that determine the extent of Mtb transmission from mine workers: the size of different populations with whom mine workers interact, the prevalence of latent infection and active disease in each population, and the amount of time that residents from different populations spend with each other. Our model suggests that gold mine workers who number less than 0.5 M (< 1% of the population in South Africa) contribute approximately 4% of new infections in South Africa per annum. By comparison, residents in peri-mining and labor-sending areas who number approximately 2.1 M and 3.4 M (4% and 7% of the population) contribute approximately 5% and 9% of new infections in South Africa per annum, respectively. Therefore, mine workers contribute a disproportionately large number of new infections, as one might expect given their higher rates of disease and the setting in which they work. However, given their mixing patterns and other factors which we included in the model, we found that the effect is mostly at the level of their own communities. These factors include the amount of time that residents spend in other communities, which we estimated to be less than 25% per year, and the limited number of susceptibles available in other communities. For example, in high-burden areas such as peri-mining and labor-sending areas, more than 50% of the population may already be latently infected, reflecting a high FOI in these areas [42, 46].

We obtained similar results with an individual-based model which we used to simulate a counterfactual scenario of curtailed Mtb transmission in the mines for a period of more than 2 years. Using this approach, we estimated that 4% of the incidence in all of South Africa could be traced to recent transmission in the mines, similar to the attributable fraction of new infections. However, among mine workers themselves, greater than 50% of the incident cases could be traced to recent transmission in the mines, suggesting that ongoing transmission among mine workers continues to have a significant effect. This was consistent with results from Godfrey-Faussett and colleagues, who genotyped Mtb strains from mine workers and found that at least 50% of TB cases were due to transmission within the mines [47], as well as other studies showing a high degree of strain clustering in different parts of South Africa [46, 48, 49]. However, a more recent study of the Thibela TB study site by Mathema and colleagues has suggested that the fraction of incident TB cases in the mines due to recent infection may be lower than previously measured [50]. Additional work is needed to explain the differences in these results and connect results such as ours, based on simulation and counterfactuals, to results based on genetic clustering and molecular epidemiology.

Nonetheless, our results suggest that curtailing transmission in the mines may have a measurable impact on the number of new cases of TB disease in the mines on a relatively short time frame, within 5 years or less. This is similar to the time frame posited by Vynnycky and colleagues, who used modeling to simulate a set of mine-targeted interventions such as reduced treatment delay and scaled-up ART and found it was possible to obtain a significant impact [15]. Given our results and those of Vynnycky et al., health officials may wish to consider measuring the extent of recent transmission, such as through Mtb strain genotyping, on an ongoing basis. A decrease in the proportion of cases that cluster genotypically is expected to accompany effective programs and would provide additional evidence of the effectiveness of TB control programs.

Our study complements past efforts to measure the association between TB burden and mining such as the study by Stuckler and colleagues [51]. In that study, each 10% increase in mining production was associated with a 0.9% increase in TB incidence [51]. Our approach did not include mining production as a covariate, precluding a direct comparison of the results. In addition, we focused on the ongoing contribution of mine conditions, which differed from the focus of Stuckler et al. on historical mining production. Despite these differences, both our study and that of Stuckler et al. point to the need to consider mining in a larger context, whether that be population mixing or other comorbidities. For example, Stuckler et al. found that most of the effect of mining on TB was mediated by HIV prevalence; controlling for HIV greatly reduced the association with mining [51]. In our models, HIV plays a similarly large role and increases the activation rate of latent disease in all groups including mine workers. The large effect of HIV relative to mining production can also be seen directly by comparing the time courses for mining production, HIV prevalence, and TB incidence in South Africa. While mining production has decreased over the last two decades [52], TB incidence has more closely mirrored HIV prevalence, only beginning to decline after 2010 [53]. As ART usage continues to increase and HIV prevalence stabilizes, it will be interesting to observe whether decreases in mining production have a more discernible effect on TB incidence. Additional questions include whether decreasing mining production or Mtb transmission in the mines would have a different effect depending on HIV prevalence 5, 10, or 15 years in the future and more generally whether the impact of hotspot-targeted approaches depends on prior HIV control and whether hotspot targeting should be coordinated with HIV control programs. We plan to explore these questions in future applications of the model.

Our study also contributes to the growing literature on using quantitative approaches to investigate potential TB hotspots. Recently, Dowdy and colleagues used a model to study high TB burden areas in Rio de Janeiro, Brazil [54]. In that study, areas that comprised 6% of the city population were found to contribute 35% of the new infections in the city, resulting in a 5.8:1 attributable infection:population size ratio. This compares to the 4.3:1 attributable infection:population size ratio that we found for mine workers (Table 2). As the quality of TB monitoring and evaluation improves globally, it may be useful to define a set of functional criteria for TB hotspots, e.g., what attributable infection:population size ratios qualify an area to be a hotspot and how many susceptibles need to reside in the larger population for a hotspot to pose a risk. To encourage discussions in this area, we have made many of these outputs, along with modifiable assumptions, accessible in our spreadsheet model.

While we accounted for several factors in our study, including HIV, silicosis, and population mixing, a number of assumptions would benefit from additional study. For example, our results assume that the prevalence of latent infection and active disease in the peri-mining and labor-sending areas was at least as high as those found in the general population of South Africa. While this is supported by historical data [1, 2] and available case notification data [55], our estimates could be improved with accurate measurements in these areas, such as may become available from future prevalence surveys in South Africa. The number of populations that are included in the models could also be expanded to include foreign workers. Although the proportion of workers from countries outside of South Africa has decreased in recent decades, a more comprehensive accounting should include other countries in southern Africa including Lesotho, Swaziland, and Mozambique [56]. Finally, how we represent mixing could also be refined to account for different scales. While we informed mixing in our models using tourism and labor migration data, these provide only a proxy of mixing and exclude more local influences, such as interactions within mining areas and hostels and on public transport [57, 58]. Investigating Mtb transmission at more granular levels may lead to more actionable findings for mitigating risk.

Despite these caveats, we believe our models account for the main factors likely to govern the contribution of gold mines to the TB epidemic: the size of the mine worker population, the TB burden in mine workers and other groups, and the amount of time mine workers spend in different areas. Together these factors suggest Mtb transmission in gold mines continues to feed infections in mines and mining-related communities but to a much smaller extent in the country as a whole. In evaluating the impact of interventions designed to curtail transmission in the mines, the effect on both scales should be considered.

Conclusions

Using two models that integrate diverse types of data, we estimate that gold mine workers contribute a disproportionately large number of Mtb infections in South Africa on a per-capita basis. However, due to their relatively small population and the generalized nature of the TB epidemic in South Africa, gold mine workers contribute only a small fraction of the total number of Mtb infections in South Africa. Our results suggest efforts at curtailing transmission in the mines may have limited impact at the country level despite a potentially significant impact on a relatively short time frame in the mines themselves.

Change history

  • 28 December 2018

    The original article [1] did not contain comprehensive information regarding two authors’ affiliations that may be considered a potential competing interest.

Abbreviations

ART:

Antiretroviral therapy

95% CI:

95% confidence interval

DOTS:

Directly observed therapy short-course

FOI:

Force of infection

LTBI:

Latent tuberculosis infection

M:

Million

Mtb :

Mycobacterium tuberculosis

PAF:

Population attributable fraction

TB:

Tuberculosis

WAIFW:

Who acquires infection from whom

References

  1. Packard RM. White plague, black labor: tuberculosis and the political economy of health and disease in South Africa. Berkeley: University of California Press; 1989.

    Google Scholar 

  2. Rees D, Murray J, Nelson G, Sonnenberg P. Oscillating migration and the epidemics of silicosis, tuberculosis, and HIV infection in South African gold miners. Am J Ind Med. 2010;53:398–404.

    Article  Google Scholar 

  3. Evian C, Fox M, MacLeod W, Slotow SJ, Rosen S. Prevalence of HIV in workforces in southern Africa, 2000-2001. S Afr Med J. 2004;94:125–30.

    PubMed  Google Scholar 

  4. Corno L, de Walque D. Mines, Migration and HIV/AIDS in Southern Africa. J Afr Econ. 2012;21:465–98.

  5. Stuckler D, Steele S, Lurie M, Basu S. Introduction: “dying for gold”: the effects of mineral mining on HIV, tuberculosis, silicosis, and occupational diseases in southern Africa. Int J Health Serv. 2013;43:639–49.

    Article  Google Scholar 

  6. Basu S, Stuckler D, Gonsalves G, Lurie M. The production of consumption: addressing the impact of mineral mining on tuberculosis in southern Africa. Glob Health. 2009;5:11.

    Article  Google Scholar 

  7. Knight GM, Dodd PJ, Grant AD, Fielding KL, Churchyard GJ, White RG. Tuberculosis prevention in South Africa. PLoS One. 2015;10:e0122514.

    Article  Google Scholar 

  8. Houben RMGJ, Dowdy DW, Vassall A, Cohen T, Nicol MP, Granich RM, et al. How can mathematical models advance tuberculosis control in high HIV prevalence settings? Int J Tuberc Lung Dis. 2014;18:509–14.

    Article  Google Scholar 

  9. Dowdy DW, Houben R, Cohen T, Pai M, Cobelens F, Vassall A, et al. Impact and cost-effectiveness of current and future tuberculosis diagnostics: the contribution of modelling. Int J Tuberc Lung Dis. 2014;18:1012–8.

    Article  Google Scholar 

  10. Houben RMGJ, Menzies NA, Sumner T, Huynh GH, Arinaminpathy N, Goldhaber-Fiebert JD, et al. Feasibility of achieving the 2025 WHO global tuberculosis targets in South Africa, China, and India: a combined analysis of 11 mathematical models. Lancet Glob Health. 2016;4:e806–15.

    Article  Google Scholar 

  11. Blaser N, Zahnd C, Hermans S, Salazar-Vizcaya L, Estill J, Morrow C, et al. Tuberculosis in Cape Town: an age-structured transmission model. Epidemics. 2016;14:54–61.

    Article  Google Scholar 

  12. Johnstone-Robertson S, Lawn SD, Welte A, Bekker L-G, Wood R. Tuberculosis in a South African prison: a transmission modelling analysis. S Afr Med J. 2011;101:809–13.

    PubMed  PubMed Central  Google Scholar 

  13. Wood R, Johnstone-Robertson S, Uys P, Hargrove J, Middelkoop K, Lawn SD, et al. Tuberculosis transmission to young children in a South African community: modeling household and community infection risks. Clin Infect Dis. 2010;51:401–8.

    Article  Google Scholar 

  14. Sumner T, Houben RMGJ, Rangaka MX, Maartens G, Boulle A, Wilkinson RJ, et al. Post-treatment effect of isoniazid preventive therapy on tuberculosis incidence in HIV-infected individuals on antiretroviral therapy. AIDS. 2016;30:1279–86.

    Article  CAS  Google Scholar 

  15. Vynnycky E, Sumner T, Fielding KL, Lewis JJ, Cox AP, Hayes RJ, et al. Tuberculosis control in South African gold mines: mathematical modeling of a trial of community-wide isoniazid preventive therapy. Am J Epidemiol. 2015;181:619–32.

    Article  Google Scholar 

  16. Fielding KL, Grant AD, Hayes RJ, Chaisson RE, Corbett EL, Churchyard GJ. Thibela TB: design and methods of a cluster randomised trial of the effect of community-wide isoniazid preventive therapy on tuberculosis amongst gold miners in South Africa. Contemp Clin Trials. 2011;32:382–92.

    Article  Google Scholar 

  17. Stats SA. Census 2011. Statistics South Africa, Pretoria. 2011.

    Google Scholar 

  18. Statistics SA. Quarterly Labour Force Survey, Quarter 4, 2013 [Internet]. 2014. http://www.statssa.gov.za/publications/P0211/P02114thQuarter2013.pdf.

    Google Scholar 

  19. Chamber of Mines SA. Facts and Figures 2016 [Internet]. 2017. http://www.chamberofmines.org.za/industry-news/publications/facts-and-figures/send/17-facts-and-figures/442-facts-and-figures-2016.

    Google Scholar 

  20. World Health Organization. Global tuberculosis report 2016. Geneva: World Health Organization; 2016. http://apps.who.int/iris/bitstream/10665/250441/1/9789241565394-eng.pdf

    Google Scholar 

  21. Churchyard GJ, Fielding KL, Lewis JJ, Coetzee L, Corbett EL, Godfrey-Faussett P, et al. A trial of mass isoniazid preventive therapy for tuberculosis control. N Engl J Med. 2014;370:301–10.

    Article  CAS  Google Scholar 

  22. Johnson LF, Dorrington RE, Moolla H. Progress towards the 2020 targets for HIV diagnosis and antiretroviral treatment in South Africa. South Afr J HIV Med. 2017;18:8.

    Google Scholar 

  23. Statistics SA. Domestic Tourism Survey 2012 [Internet]. 2013. http://www.statssa.gov.za/publications/P03521/P035212012.pdf.

    Google Scholar 

  24. Anderson RM, May RM, Anderson B. Infectious diseases of humans: dynamics and control. Oxford: Oxford University Press; 1992.

    Google Scholar 

  25. Begon M, Bennett M, Bowers RG, French NP, Hazel SM, Turner J. A clarification of transmission terms in host-microparasite models: numbers, densities and areas. Epidemiol Infect. 2002;129:147–53.

    Article  CAS  Google Scholar 

  26. Gammaitoni L, Nucci MC. Using a mathematical model to evaluate the efficacy of TB control measures. Emerg Infect Dis. 1997;3:335–42.

    Article  CAS  Google Scholar 

  27. Huynh GH, Klein DJ, Chin DP, Wagner BG, Eckhoff PA, Liu R, et al. Tuberculosis control strategies to reach the 2035 global targets in China: the role of changing demographics and reactivation disease. BMC Med. 2015;13:88.

    Article  Google Scholar 

  28. Shisana O, Rehle T, Simbayi LC, Zuma K, Jooste S, Zungu N, et al. South African national HIV prevalence, incidence and behaviour survey, 2012. Cape Town: HSRC Press; 2014. http://repository.hsrc.ac.za/handle/20.500.11910/2490

    Google Scholar 

  29. Bershteyn A, Klein DJ, Wenger E, Eckhoff PA. Description of the EMOD-HIV Model v0.7 [Internet]. arXiv [q-bio.QM]. 2012. http://arxiv.org/abs/1206.3720.

    Google Scholar 

  30. Klein DJ, Eckhoff PA, Bershteyn A. Targeting HIV services to male migrant workers in southern Africa would not reverse generalized HIV epidemics in their home communities: a mathematical modeling analysis. Int Health. 2015;7:107–13.

    Article  Google Scholar 

  31. Eaton JW, Bacaër N, Bershteyn A, Cambiano V, Cori A, Dorrington RE, et al. Assessment of epidemic projections using recent HIV survey data in South Africa: a validation analysis of ten mathematical models of HIV epidemiology in the antiretroviral therapy era. Lancet Glob Health. 2015;3:e598–608.

    Article  Google Scholar 

  32. Nelson G, Girdler-Brown B, Ndlovu N, Murray J. Three decades of silicosis: disease trends at autopsy in South African gold miners. Environ Health Perspect. 2010;118:421–6.

    Article  Google Scholar 

  33. Churchyard GJ, Ehrlich R, TWN JM, Pemba L, Dekker K, Vermeijs M, et al. Silicosis prevalence and exposure-response relations in South African goldminers. Occup Environ Med. 2004;61:811–6.

    Article  CAS  Google Scholar 

  34. Murray J, Kielkowski D, Reid P. Occupational disease trends in black South African gold miners. An autopsy-based study. Am J Respir Crit Care Med. 1996;153:706–10.

    Article  CAS  Google Scholar 

  35. Hens N, Shkedy Z, Aerts M, Faes C, Van Damme P, Beutels P. Who acquires infection from whom? The traditional approach. Modeling infectious disease parameters based on serological and social contact data. New York: Springer; 2012. p. 219–32.

    Google Scholar 

  36. Corbett EL, Watt CJ, Walker N, Maher D, Williams BG, Raviglione MC, et al. The growing burden of tuberculosis: global trends and interactions with the HIV epidemic. Arch Intern Med. 2003;163:1009–21.

    Article  Google Scholar 

  37. Zumla A, George A, Sharma V, Herbert RHN, Oxley A, Oliver M. The WHO 2014 global tuberculosis report—further to go. Lancet Glob Health. 2015;3:e10–2.

    Article  Google Scholar 

  38. Raftery AE, Bao L. Estimating and projecting trends in HIV/AIDS generalized epidemics using incremental mixture importance sampling. Biometrics. 2010;66:1162–73.

    Article  Google Scholar 

  39. Mangtani P, Abubakar I, Ariti C, Beynon R, Pimpin L, Fine PEM, et al. Protection by BCG vaccine against tuberculosis: a systematic review of randomized controlled trials. Clin Infect Dis. 2014;58:470–80.

    Article  Google Scholar 

  40. Shanaube K, Sismanidis C, Ayles H, Beyers N, Schaap A, Lawrence K-A, et al. Annual risk of tuberculous infection using different methods in communities with a high prevalence of TB and HIV in Zambia and South Africa. PLoS One. 2009;4:e7749.

    Article  Google Scholar 

  41. Kritzinger FE, den Boon S, Verver S, Enarson DA, Lombard CJ, Borgdorff MW, et al. No decrease in annual risk of tuberculosis infection in endemic area in Cape Town, South Africa. Tropical Med Int Health. 2009;14:136–42.

    Article  Google Scholar 

  42. Wood R, Liang H, Wu H, Middelkoop K, Oni T, Rangaka MX, et al. Changing prevalence of tuberculosis infection with increasing age in high-burden townships in South Africa. Int J Tuberc Lung Dis. 2010;14:406–12.

    CAS  PubMed  PubMed Central  Google Scholar 

  43. Ncayiyana JR, Bassett J, West N, Westreich D, Musenge E, Emch M, et al. Prevalence of latent tuberculosis infection and predictive factors in an urban informal settlement in Johannesburg, South Africa: a cross-sectional study. BMC Infect Dis. 2016;16:661.

    Article  Google Scholar 

  44. World Health Organization. South Africa statistics summary (2002 - present). Global Health Observatory country views [Internet]. http://apps.who.int/gho/data/node.country.country-ZAF?lang=en. Accessed 11 Sep 2017.

  45. Corbett EL, Charalambous S, Fielding K, Clayton T, Hayes RJ, De Cock KM, et al. Stable incidence rates of tuberculosis (TB) among human immunodeficiency virus (HIV)-negative South African gold miners during a decade of epidemic HIV-associated TB. J Infect Dis. 2003;188:1156–63.

    Article  Google Scholar 

  46. Middelkoop K, Bekker L-G, Myer L, Dawson R, Wood R. Rates of tuberculosis transmission to children and adolescents in a community with a high prevalence of HIV infection among adults. Clin Infect Dis. 2008;47:349–55.

    Article  Google Scholar 

  47. Godfrey-Faussett P, Sonnenberg P, Shearer SC, Bruce MC, Mee C, Morris L, et al. Tuberculosis control and molecular epidemiology in a South African gold-mining community. Lancet. 2000;356:1066–71.

    Article  CAS  Google Scholar 

  48. Richardson M, van Lill SWP, van der Spuy GD, Munch Z, Booysen CN, Beyers N, et al. Historic and recent events contribute to the disease dynamics of Beijing-like Mycobacterium tuberculosis isolates in a high incidence region. Int J Tuberc Lung Dis. 2002;6:1001–11.

    CAS  PubMed  Google Scholar 

  49. Verver S, Warren RM, Munch Z, Vynnycky E, van Helden PD, Richardson M, et al. Transmission of tuberculosis in a high incidence urban community in South Africa. Int J Epidemiol. 2004;33:351–7.

    Article  Google Scholar 

  50. Mathema B, Lewis JJ, Connors J, Chihota VN, Shashkina E, van der Meulen M, et al. Molecular epidemiology of Mycobacterium tuberculosis among South African gold miners. Ann Am Thorac Soc. 2015;12:12–20.

    Article  Google Scholar 

  51. Stuckler D, Basu S, McKee M, Lurie M. Mining and risk of tuberculosis in sub-Saharan Africa. Am J Public Health. 2011;101:524–30.

    Article  Google Scholar 

  52. Statistics SA. Mineral accounts for South Africa, 1980–2001. Pretoria: South Africa; 2002.

    Google Scholar 

  53. World Health Organization. Global Tuberculosis Report 2013. Geneva: World Health Organization; 2013.

    Google Scholar 

  54. Dowdy DW, Golub JE, Chaisson RE, Saraceni V. Heterogeneity in tuberculosis transmission and the role of geographic hotspots in propagating epidemics. Proc Natl Acad Sci U S A. 2012;109:9557–62.

    Article  CAS  Google Scholar 

  55. Day C, Barron P, Massyn N, Padarath A, English R. District Health Barometer 2010/11. Durban: Health Systems Trust Google Scholar; 2011.

    Google Scholar 

  56. McGlashan ND, Harington JS, Chelkowska E. Changes in the geographical and temporal patterns of cancer incidence among black gold miners working in South Africa, 1964–1996. Br J Cancer. 2003;88:1361–9.

    Article  CAS  Google Scholar 

  57. Andrews JR, Morrow C, Wood R. Modeling the role of public transportation in sustaining tuberculosis transmission in South Africa. Am J Epidemiol. 2013;177:556–61.

    Article  Google Scholar 

  58. Middelkoop K, Mathema B, Myer L, Shashkina E, Whitelaw A, Kaplan G, et al. Transmission of tuberculosis in a South African community with a high prevalence of HIV infection. J Infect Dis. 2015;211:53–61.

    Article  CAS  Google Scholar 

Download references

Acknowledgements

The authors thank Randall Packard and Anna Bershteyn for productive discussions and Bill and Melinda Gates for their support of the Institute for Disease Modeling. RGW is funded by the UK Medical Research Council (MRC) and the UK Department for International Development (DFID) under the MRC/DFID Concordat agreement that is also part of the EDCTP2 programme supported by the European Union (MR/P002404/1), the Bill & Melinda Gates Foundation (TB Modelling and Analysis Consortium: OPP1084276/OPP1135288, SA Modelling for Policy: OPP1110334, CORTIS: OPP1137034, Vaccines: OPP1160830) and UNITAID (4214-LSHTM-Sept15; PO 8477-0-600).

Funding

This project was funded by a South Africa TB Think Tank grant from the Bill & Melinda Gates Foundation (OPP1110334).

Availability of data and materials

The static risk model (Excel file) and the individual-based model (source code, executable file, configuration files) are available from the authors’ GitHub repository (https://github.com/SCTX/mining_contribution) or upon request.

Author information

Authors and Affiliations

Authors

Contributions

STC and BGW analyzed the data, created the models, and drafted the manuscript. VNC, KLF, and ADG provided primary data from the Thibela TB study. RGW, GJC, RMH, and PAE conceptualized the study and provided guidance throughout the study. All authors contributed to revisions of the manuscript. All authors read and approved the final manuscript.

Corresponding author

Correspondence to Stewart T. Chang.

Ethics declarations

Ethics approval and consent to participate

Not applicable

Consent for publication

Not applicable

Competing interests

The authors declare that they have no competing interests.

Publisher’s Note

Springer Nature remains neutral with regard to jurisdictional claims in published maps and institutional affiliations.

Additional file

Additional file 1:

Supplemental materials, figures, and tables. (DOCX 2293 kb)

Rights and permissions

Open Access This article is distributed under the terms of the Creative Commons Attribution 4.0 International License (http://creativecommons.org/licenses/by/4.0/), which permits unrestricted use, distribution, and reproduction in any medium, provided you give appropriate credit to the original author(s) and the source, provide a link to the Creative Commons license, and indicate if changes were made. The Creative Commons Public Domain Dedication waiver (http://creativecommons.org/publicdomain/zero/1.0/) applies to the data made available in this article, unless otherwise stated.

Reprints and permissions

About this article

Check for updates. Verify currency and authenticity via CrossMark

Cite this article

Chang, S.T., Chihota, V.N., Fielding, K.L. et al. Small contribution of gold mines to the ongoing tuberculosis epidemic in South Africa: a modeling-based study. BMC Med 16, 52 (2018). https://doi.org/10.1186/s12916-018-1037-3

Download citation

  • Received:

  • Accepted:

  • Published:

  • DOI: https://doi.org/10.1186/s12916-018-1037-3

Keywords