Factors associated with the development of leprosy in Brazilian contacts: a systematic review

Alecrin, Edilamar Silva de; Oliveira, Ana Laura Grossi de; Guimarães, Nathália Sernizon; Lyon, Sandra; Martins, Maria Auxiliadora Parreiras; Rocha, Manoel Otávio da Costa

doi:10.1590/S1678-9946202264055

ABSTRACT

People who interact with leprosy patients in their environment, neighborhood, family, or social relationships are at risk to develop the disease. This systematic review investigated the risk and protective factors associated with the development of leprosy in Brazilian contacts. The studies were found in Cochrane Library, PubMed (MEDLINE), Embase, Virtual Health Library, grey literature and hand search until July 2021. The study selection, data extraction and quality assessment were independently performed by two investigators. The quality assessment was performed using the Newcastle-Ottawa Scale (NOS). This review was registered in PROSPERO (CRD42020160680). Seventeen articles fulfilled the inclusion criteria (n=544). The immunological and molecular factors, such as Anti-phenolic Glycolipid Antibodies (Anti-PGL-1) seropositivity, negative Mitsuda test, absence of Bacillus Calmette-Guérin (BCG) scar, positive Polymerase Chain Reaction (PCR) in blood; age and race; conviviality, education, contact time and type of contact, as well as elements related to the index case (bacilloscopic index; genetic conditions, family relationships), and some combined factors were shown to be relevant risk factors associated with the development of the disease in Brazilian leprosy contacts. The protective factors reported were the presence of one or more BCG scars, positive Mitsuda test, and education level. All selected studies were considered of high quality according to NOS. The knowledge of disease-related risk and protective factors provides the scientific basis for decision-making in the management of the disease in leprosy contacts.

Leprosy; Risk factors; Protective factors; Public health surveillance; Systematic review

INTRODUCTION

Leprosy is an infectious disease caused by Mycobacterium leprae, also known as Hansen’s bacillus, which affects the skin and peripheral nerves. The main route for leprosy transmission is through the upper airways. This disease is important for public health, mainly due to its high potential to cause physical disabilities¹1. Walker SL, Lockwood DN. Leprosy. Clin Dermatol. 2007;25:165-72.. The late diagnosis of leprosy is a global concern since 7,198 new cases of leprosy have already been diagnosed with grade-2 disabilities (G2Ds). Most of them were contacts of leprosy patients²2. World Health Organization. Global leprosy (Hansen disease) update, 2020: impact of COVID-19 on global leprosy control: weekly epidemiological record. [cited 2022 Aug 11]. Available from: https://www.who.int/publications/i/item/who-wer9636-421-444
https://www.who.int/publications/i/item/... .

In 2020, 127,396 new cases of leprosy were reported worldwide, comprising 19,195 in the Americas. Brazil is the second country with the highest number of new cases and presents a high burden of the disease. In 2020, 17,979 new cases were reported in Brazil, 8.3% with grade 2 disability. In children, 878 new cases were reported, 4% with grade 2 disability²2. World Health Organization. Global leprosy (Hansen disease) update, 2020: impact of COVID-19 on global leprosy control: weekly epidemiological record. [cited 2022 Aug 11]. Available from: https://www.who.int/publications/i/item/who-wer9636-421-444
https://www.who.int/publications/i/item/... .

Leprosy contacts can be defined as people who interact with an individual diagnosed in their environment, neighborhood, family, or social relationships. A household contact carries an increased risk of developing the disease when compared to the general population³3. Bührer-Sékula S, Smits HL, Gussenhoven GC, van Leeuwen J, Amador S, Fujiwara T, et al. Simple and fast lateral flow test for classification of leprosy patients and identification of contacts with high risk of developing leprosy. J Clin Microbiol. 2003;41:1991-5.,⁴4. Douglas JT, Cellona RV, Fajardo TT Jr, Abalos RM, Balagon MV, Klatser PR. Prospective study of serological conversion as a risk factor for development of leprosy among household contacts. Clin Vaccine Immunol. 2004;11:897-900.. Multiple factors that can lead to illness in contacts have been described in the literature encompassing aspects related to the index case (IC)⁵5. Carvalho AP, Fabri AC, Oliveira RC, Lana FC. Factors associated with anti-phenolic glycolipid-I seropositivity among the household contacts of leprosy cases. BMC Infect Dis. 2015;15:219., immunological factors⁴4. Douglas JT, Cellona RV, Fajardo TT Jr, Abalos RM, Balagon MV, Klatser PR. Prospective study of serological conversion as a risk factor for development of leprosy among household contacts. Clin Vaccine Immunol. 2004;11:897-900.,⁶6. Hacker MA, Duppre NC, Nery JA, Sales AM, Sarno EN. Characteristics of leprosy diagnosed through the surveillance of contacts: a comparison with index cases in Rio de Janeiro, 1987-2010. Mem Inst Oswaldo Cruz. 2012;107 Suppl 1:49-54.

7. Sarno EN, Duppre NC, Sales AM, Hacker MA, Nery JA, Matos HJ. Leprosy exposure, infection and disease: a 25-year surveillance study of leprosy patient contacts. Mem Inst Oswaldo Cruz. 2012;107:1054-9.

8. Araujo S, Rezende MM, Sousa DC, Rosa MR, Santos DC, Goulart LR, et al. Risk-benefit assessment of Bacillus Calmette-Guérin vaccination, anti-phenolic glycolipid I serology, and Mitsuda test response: 10-year follow-up of household contacts of leprosy patients. Rev Soc Bras Med Trop. 2015;48:739-45.

9. Setia MS, Steinmaus C, Ho CS, Rutherford GW. The role of BCG in prevention of leprosy: a meta-analysis. Lancet Infect Dis. 2006;6:162-70.

10. Goulart IM, Souza DO, Marques CR, Pimenta VL, Gonçalves MA, Goulart LR. Risk and protective factors for leprosy development determined by epidemiological surveillance of household contacts. Clin Vaccine Immunol. 2008;15:101-5.-¹¹11. Merle CS, Cunha SS, Rodrigues LC. BCG vaccination and leprosy protection: review of current evidence and status of BCG in leprosy control. Expert Rev Vaccines. 2010;9:209-22., nutritional aspects¹²12. Wagenaar I, van Muiden L, Alam K, Bowers R, Hossain MA, Kispotta K, et al. Diet-related risk factors for leprosy: a case-control study. PLoS Negl Trop Dis. 2015;9:e0003766.,¹³13. Kerr-Pontes LR, Montenegro AC, Barreto ML, Werneck GL, Feldmeier H. Inequality and leprosy in Northeast Brazil: an ecological study. Int J Epidemiol. 2004;33:262-9., family relationships, and social factors⁸8. Araujo S, Rezende MM, Sousa DC, Rosa MR, Santos DC, Goulart LR, et al. Risk-benefit assessment of Bacillus Calmette-Guérin vaccination, anti-phenolic glycolipid I serology, and Mitsuda test response: 10-year follow-up of household contacts of leprosy patients. Rev Soc Bras Med Trop. 2015;48:739-45.,¹³13. Kerr-Pontes LR, Montenegro AC, Barreto ML, Werneck GL, Feldmeier H. Inequality and leprosy in Northeast Brazil: an ecological study. Int J Epidemiol. 2004;33:262-9.

14. Imbiriba EN, Silva Neto NA, Souza WV, Pedrosa V, Cunha MG, Garnelo L. Desigualdade social, crescimento urbano e hanseníase em Manaus: abordagem espacial. Rev Saude Publica. 2009;43:656-65.

15. Sales AM, Ponce de Leon A, Düppre NC, Hacker MA, Nery JA, Sarno EN, et al. Leprosy among patient contacts: a multilevel study of risk factors. PLoS Negl Trop Dis. 2011;5:e1013.

16. Freitas LR, Duarte EC, Garcia LP. Leprosy in Brazil and its association with characteristics of municipalities: ecological study, 2009-2011. Trop Med Int Health. 2014;19:1216-25.-¹⁷17. Deps PD, Guedes BV, Filho JB, Andreatta MK, Marcari RS, Rodrigues LC. Characteristics of known leprosy contact in a high endemic area in Brazil. Lepr Rev. 2006;77:34-40., among others. Therefore, the purpose of this systematic review was to investigate factors associated with the development of the disease in Brazilian leprosy contacts.

MATERIALS AND METHODS

Study registration

This systematic review complies with the Cochrane Handbook for Systematic Reviews of Interventions¹⁸18. Cochrane Training. Cochrane handbook for systematic reviews of interventions, version 6.2, 2021. [cited 2022 Aug 11] Available from: https://training.cochrane.org/handbook/archive/v6.2
https://training.cochrane.org/handbook/a... and PRISMA (Preferred Reporting Items for Systematic Reviews and Meta-Analysis) guidelines¹⁹19. Moher D, Shamseer L, Clarke M, Ghersi D, Liberati A, Petticrew M, et al. Preferred reporting items for systematic review and meta-analysis protocols (PRISMA-P) 2015 statement. Syst Rev. 2015;4:1.. The study protocol was registered in the International Prospective Register of Systematic Reviews (PROSPERO) under the reference code CRD42020160680. The preliminary version of the study protocol was revised to adapt the inclusion criteria and focus on primary studies developed within the Brazilian population.

Search strategy and eligibility criteria

The research question was defined by using the PECO formulation guidance, as follows: Population (P): leprosy contacts; exposure (E): risk factors for leprosy contacts becoming ill; comparator (C): leprosy contacts who did not develop the illness after exposure; outcome (O): illness. The outcomes of interest included the factors associated with the development of the disease in Brazilian leprosy contacts.

The following databases were considered to search for articles: MEDLINE (by PubMed), Embase (by OVID), Cochrane Library, LILACS, WHOLIS, HANSENIASE, IBECS, Health Department of the Sao Paulo State, BDENF – Nursing, CUMED, and BINACIS (by Virtual Health Library). The grey literature was screened on MedNar, OpenGrey and ProQuest. A hand search was also performed in the lists of the selected articles. The complete search strategies and their descriptors were presented in Supplementary Table S1.

No language restrictions were applied to the search, although the full-text review was limited to articles published in English, Spanish, and Portuguese. The period of publication was limited to the period from January 2004 to July 2021, considering the previous systematic review²⁰20. Moet FJ, Meima A, Oskam L, Richardus JH. Risk factors for the development of clinical leprosy among contacts, and their relevance for targeted interventions. Lepr Rev. 2004;75:310-26.. Studies were eligible for inclusion if: they presented the description of household contacts, peridomiciliary and social leprosy contacts; risk and/or protective factors for healthy Brazilian contacts; observational studies. The choice to include observational studies allowed for the synthetization of data from analytical studies comparing groups of leprosy contacts who developed or did not develop the disease and investigating risk/protective factors with data collected in real-world scenarios. Both genders and different age groups were included. The studies were excluded if they were classified as reviews, case reports, interviews, letters to the editor, or experimental studies.

Selection of studies and data extraction

The electronic search results from defined databases were uploaded to the Rayyan Qatar Computing Research Institute²¹21. Ouzzani M, Hammady H, Fedorowicz Z, Elmagarmid A. Rayyan: a web and mobile app for systematic reviews. Syst Rev. 2016;5:210.. The study selection and data extraction were independently performed by two investigators. A third reviewer resolved any existing disagreements. We used a standardized Microsoft Excel sheet for the data extraction including the author(s), publication year, title, journal, study design, setting, number of study participants, comparative groups (leprosy contacts and healthy participants), gender, age, events among contacts, prevalence or incidence of leprosy among contacts, contact classifications (household, neighbors, and social contacts), and risk and protective factors involved in the development of leprosy among contacts. The funding sources of the studies were also described, when available. The data of risk and protective factors were summarized considering the: immunological factors, genetic aspects, social determinants, factors related to the relationship with the contacts and with the index cases, combined factors, factors related to the index case, and factors in people who were less than 15 years old. The factors were expressed as odds ratios (ORs), adjusted odds ratios (aORs), hazard ratios (HRs), relative risk (RR), adjusted relative risk (aRR), confidence intervals (CI), and/or p-values.

Risk of bias and quality assessment

The relevant study data were screened and assessed for quality using the adapted Newcastle-Ottawa Scale (NOS). This scale is used for the quality assessment of case-control and cohort studies²²22. Wells GA, Shea B, O’Connell D, Peterson J, Welch V, Losos MT, et al The Newcastle-Ottawa Scale (NOS) for assessing the quality of non randomised studies in meta-analyses. [cited 2022 Aug 11]. Available from http://www.ohri.ca/programs/clinical_epidemiology/oxford.htm
http://www.ohri.ca/programs/clinical_epi... . The NOS stars awarded for each quality item enabled a quick visual evaluation, with the highest-quality studies awarded nine or more stars. Studies scored above six stars are considered of high quality.

RESULTS

The factors associated with the development of the disease in Brazilian leprosy contacts included sociodemographic, genetic, and immunological variables. The main risk factors reported were Anti-phenolic Glycolipid Antibodies (Anti-PGL-1) seropositivity, negative Mitsuda test, absence of Bacillus Calmette-Guérin (BCG) scars, positive Polymerase Chain Reaction (PCR) in blood; age and race; conviviality, contact time, and type of contact; bacilloscopic index and education of leprosy index cases, as well as consanguinity/family relationships. The presence of BCG vaccine scar, anti-PGL-1 seronegativity, and positive Mitsuda test were described as protective factors. The heterogeneity of the reported variables hindered the comparison among studies and the performance of a meta-analysis. A summary of the selection process of articles is detailed in the PRISMA flow diagram (Figure 1). We identified 544 records from electronic databases and selected 17 studies for this systematic review. We provided a list of all potentially relevant studies that were read in full but were excluded during the selection process ( Supplementary Table S2).

Figure 1
PRISMA 2020 flow diagram summarizing the systematic search and review process.

Study characteristics

The summary of the studies is shown in Table 1 and Table 2. Of the 17 reports, 72,876 leprosy contacts were enrolled. Regarding the study design, 15 cohort⁷7. Sarno EN, Duppre NC, Sales AM, Hacker MA, Nery JA, Matos HJ. Leprosy exposure, infection and disease: a 25-year surveillance study of leprosy patient contacts. Mem Inst Oswaldo Cruz. 2012;107:1054-9.,⁸8. Araujo S, Rezende MM, Sousa DC, Rosa MR, Santos DC, Goulart LR, et al. Risk-benefit assessment of Bacillus Calmette-Guérin vaccination, anti-phenolic glycolipid I serology, and Mitsuda test response: 10-year follow-up of household contacts of leprosy patients. Rev Soc Bras Med Trop. 2015;48:739-45.,¹⁰10. Goulart IM, Souza DO, Marques CR, Pimenta VL, Gonçalves MA, Goulart LR. Risk and protective factors for leprosy development determined by epidemiological surveillance of household contacts. Clin Vaccine Immunol. 2008;15:101-5.,¹⁵15. Sales AM, Ponce de Leon A, Düppre NC, Hacker MA, Nery JA, Sarno EN, et al. Leprosy among patient contacts: a multilevel study of risk factors. PLoS Negl Trop Dis. 2011;5:e1013.,²³23. TiemiNagao-Dias A, Macedo AC, Rodrigues RO, Pedroza FH, Albuquerque AA, Moreira FA, et al. Serum anti-PGL-1 IgG, IgM, and IgA in a 3-year follow-up study of 4–15-year-old leprosy contacts. Pediatr Infect Dis J. 2019;38:e193-8.

24. Gomes RR, Antunes DE, Santos DF, Sabino EF, Oliveira DB, Goulart IM. BCG vaccine and leprosy household contacts: protective effect and probability to becoming sick during follow-up. Vaccine. 2019;37:6510-7.

25. Manta FS, Barbieri RR, Moreira SJ, Santos PT, Nery JA, Duppre NC, et al. Quantitative PCR for leprosy diagnosis and monitoring in household contacts: a follow-up study, 2011–2018. Sci Rep. 2019;9:16675.

26. Teixeira CS, Pescarini JM, Alves FJ, Nery JS, Sanchez MN, Teles C, et al. Incidence of and factors associated with leprosy among household contacts of patients with leprosy in Brazil. JAMA Dermatol. 2020;156:640-8.

27. Durães SM, Guedes LS, Cunha MD, Cavaliere FA, Oliveira ML. Estudo de 20 focos familiares de hanseníase no município de Duque de Caxias, Rio de Janeiro. An Bras Dermatol. 2005;80 Supl 3:S295-300.

28. Durães SM, Guedes LS, Cunha MD, Magnanini MM, Oliveira ML. Epidemiologic study of 107 cases of families with leprosy in Duque de Caxias, Rio de Janeiro, Brazil. An Bras Dermatol. 2010;85:339-45.

29. Düppre NC, Camacho LA, Sales AM, Illarramendi X, Nery JA, Sampaio EP, et al. Impact of PGL-I seropositivity on the protective effect of BCG vaccination among leprosy contacts: a cohort study. PLoS Negl Trop Dis. 2012;6:e1711.

30. Liu PT, Wheelwright M, Teles R, Komisopoulou E, Edfeldt K, Ferguson B, et al. MicroRNA-21 targets the vitamin D–dependent antimicrobial pathway in leprosy. Nat Med. 2012;18:267-73.

31. Santos DS, Duppre NC, Sales AM, Nery JA, Sarno EN, Hacker MA. Kinship and leprosy in the contacts of leprosy patients: cohort at the Souza Araújo Outpatient Clinic, Rio de Janeiro, RJ, 1987–2010. J Trop Med. 2013;2013:596316.

32. Barreto JG, Bisanzio D, Frade MA, Moraes TM, Gobbo AR, Guimarães LS, et al. Spatial epidemiology and serologic cohorts increase the early detection of leprosy. BMC Infect Dis. 2015;15:527.-³³33. Araujo S, Freitas LO, Goulart LR, Goulart IM. Molecular evidence for the aerial route of infection of Mycobacterium leprae and the role of asymptomatic carriers in the persistence of leprosy. Clin Infect Dis. 2016;63:1412-20. and two case-control studies³⁴34. Rodrigues TS, Gomes LC, Cortela DC, Silva EA, Silva CA, Ferreira SM. Factors associated with leprosy in children contacts of notified adults in an endemic region of Midwest Brazil. J Pediatr (Rio J). 2020;96:593-9.,³⁵35. Santos DF, Mendonça MR, Antunes DE, Sabino EF, Pereira RC, Goulart LR, et al. Molecular, immunological and neurophysiological evaluations for early diagnosis of neural impairment in seropositive leprosy household contacts. PLoS Negl Trop Dis. 2018;12:e0006494. were included in this review. All selected studies were considered of high quality according to NOS with scores of 7 and 8 (Table 1). The details on the assessment of the quality of studies using the NOS are presented in Supplementary Table S3. Most studies (13; 76.5%) were funded, comprising eleven studies funded by the Brazilian government or its partnership with Brazilian research agencies¹⁰10. Goulart IM, Souza DO, Marques CR, Pimenta VL, Gonçalves MA, Goulart LR. Risk and protective factors for leprosy development determined by epidemiological surveillance of household contacts. Clin Vaccine Immunol. 2008;15:101-5.,¹⁵15. Sales AM, Ponce de Leon A, Düppre NC, Hacker MA, Nery JA, Sarno EN, et al. Leprosy among patient contacts: a multilevel study of risk factors. PLoS Negl Trop Dis. 2011;5:e1013.,²⁴24. Gomes RR, Antunes DE, Santos DF, Sabino EF, Oliveira DB, Goulart IM. BCG vaccine and leprosy household contacts: protective effect and probability to becoming sick during follow-up. Vaccine. 2019;37:6510-7.

25. Manta FS, Barbieri RR, Moreira SJ, Santos PT, Nery JA, Duppre NC, et al. Quantitative PCR for leprosy diagnosis and monitoring in household contacts: a follow-up study, 2011–2018. Sci Rep. 2019;9:16675.-²⁶26. Teixeira CS, Pescarini JM, Alves FJ, Nery JS, Sanchez MN, Teles C, et al. Incidence of and factors associated with leprosy among household contacts of patients with leprosy in Brazil. JAMA Dermatol. 2020;156:640-8.,²⁹29. Düppre NC, Camacho LA, Sales AM, Illarramendi X, Nery JA, Sampaio EP, et al. Impact of PGL-I seropositivity on the protective effect of BCG vaccination among leprosy contacts: a cohort study. PLoS Negl Trop Dis. 2012;6:e1711.,³¹31. Santos DS, Duppre NC, Sales AM, Nery JA, Sarno EN, Hacker MA. Kinship and leprosy in the contacts of leprosy patients: cohort at the Souza Araújo Outpatient Clinic, Rio de Janeiro, RJ, 1987–2010. J Trop Med. 2013;2013:596316.

32. Barreto JG, Bisanzio D, Frade MA, Moraes TM, Gobbo AR, Guimarães LS, et al. Spatial epidemiology and serologic cohorts increase the early detection of leprosy. BMC Infect Dis. 2015;15:527.

33. Araujo S, Freitas LO, Goulart LR, Goulart IM. Molecular evidence for the aerial route of infection of Mycobacterium leprae and the role of asymptomatic carriers in the persistence of leprosy. Clin Infect Dis. 2016;63:1412-20.-³⁴34. Rodrigues TS, Gomes LC, Cortela DC, Silva EA, Silva CA, Ferreira SM. Factors associated with leprosy in children contacts of notified adults in an endemic region of Midwest Brazil. J Pediatr (Rio J). 2020;96:593-9.,³⁶36. Reis EM, Araujo S, Lobato J, Neves AF, Costa AV, Gonçalves MA, et al. Mycobacterium leprae DNA in peripheral blood may indicate a bacilli migration route and high-risk for leprosy onset. Clin Microbiol Infect. 2014;20:447-52., and three were funded by an international non-governmental organization (Netherlands Leprosy Relief)²⁷27. Durães SM, Guedes LS, Cunha MD, Cavaliere FA, Oliveira ML. Estudo de 20 focos familiares de hanseníase no município de Duque de Caxias, Rio de Janeiro. An Bras Dermatol. 2005;80 Supl 3:S295-300.

28. Durães SM, Guedes LS, Cunha MD, Magnanini MM, Oliveira ML. Epidemiologic study of 107 cases of families with leprosy in Duque de Caxias, Rio de Janeiro, Brazil. An Bras Dermatol. 2010;85:339-45.-²⁹29. Düppre NC, Camacho LA, Sales AM, Illarramendi X, Nery JA, Sampaio EP, et al. Impact of PGL-I seropositivity on the protective effect of BCG vaccination among leprosy contacts: a cohort study. PLoS Negl Trop Dis. 2012;6:e1711..

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Table 1
Study characteristics of the included articles.

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Table 2
Risk factors associated with illness in leprosy contacts.

Most studies recruited contacts in outpatient settings (70.6%), followed by home visits (23.5%) and population-based studies with medical record reviews (5.9%). Most studies were conducted in the Southeastern region (64.7%), followed by the Northeastern (11.7%), Northern (5.8%), and Central-western (5.8%) regions, as well as national-level studies (12%). The age of the participants ranged from 0 to 90 years old. Twelve studies addressed only household contacts and five addressed household, social, and neighborhood contacts.

Risk factors associated with the illness in leprosy contacts

Immunological factors

Positive Anti-PGL-1/positive ELISA

Seven studies investigated the association between the illness among contacts and the presence of positive PGL-1/positive ELISA⁸8. Araujo S, Rezende MM, Sousa DC, Rosa MR, Santos DC, Goulart LR, et al. Risk-benefit assessment of Bacillus Calmette-Guérin vaccination, anti-phenolic glycolipid I serology, and Mitsuda test response: 10-year follow-up of household contacts of leprosy patients. Rev Soc Bras Med Trop. 2015;48:739-45.,¹⁰10. Goulart IM, Souza DO, Marques CR, Pimenta VL, Gonçalves MA, Goulart LR. Risk and protective factors for leprosy development determined by epidemiological surveillance of household contacts. Clin Vaccine Immunol. 2008;15:101-5.,²³23. TiemiNagao-Dias A, Macedo AC, Rodrigues RO, Pedroza FH, Albuquerque AA, Moreira FA, et al. Serum anti-PGL-1 IgG, IgM, and IgA in a 3-year follow-up study of 4–15-year-old leprosy contacts. Pediatr Infect Dis J. 2019;38:e193-8.,²⁹29. Düppre NC, Camacho LA, Sales AM, Illarramendi X, Nery JA, Sampaio EP, et al. Impact of PGL-I seropositivity on the protective effect of BCG vaccination among leprosy contacts: a cohort study. PLoS Negl Trop Dis. 2012;6:e1711.,³²32. Barreto JG, Bisanzio D, Frade MA, Moraes TM, Gobbo AR, Guimarães LS, et al. Spatial epidemiology and serologic cohorts increase the early detection of leprosy. BMC Infect Dis. 2015;15:527.,³³33. Araujo S, Freitas LO, Goulart LR, Goulart IM. Molecular evidence for the aerial route of infection of Mycobacterium leprae and the role of asymptomatic carriers in the persistence of leprosy. Clin Infect Dis. 2016;63:1412-20.,³⁵35. Santos DF, Mendonça MR, Antunes DE, Sabino EF, Pereira RC, Goulart LR, et al. Molecular, immunological and neurophysiological evaluations for early diagnosis of neural impairment in seropositive leprosy household contacts. PLoS Negl Trop Dis. 2018;12:e0006494.. One study reported a risk of developing leprosy 5.58 times higher when ML Flow was positive in contacts¹⁰10. Goulart IM, Souza DO, Marques CR, Pimenta VL, Gonçalves MA, Goulart LR. Risk and protective factors for leprosy development determined by epidemiological surveillance of household contacts. Clin Vaccine Immunol. 2008;15:101-5.. This result was in line with another study showing that positive Anti-PGL-1 in contacts had a 3.2-fold greater chance of becoming ill compared to those with negative Anti-PGL-1 (OR=3.2; 95% CI: 1.6-6.1)²⁹29. Düppre NC, Camacho LA, Sales AM, Illarramendi X, Nery JA, Sampaio EP, et al. Impact of PGL-I seropositivity on the protective effect of BCG vaccination among leprosy contacts: a cohort study. PLoS Negl Trop Dis. 2012;6:e1711..

Other findings related to the risk of illness between positive and seronegative Anti-PGL-1 in contacts included estimates of RR=2.7 (95% CI: 1.29-5.87)³²32. Barreto JG, Bisanzio D, Frade MA, Moraes TM, Gobbo AR, Guimarães LS, et al. Spatial epidemiology and serologic cohorts increase the early detection of leprosy. BMC Infect Dis. 2015;15:527.; RR=5.688 (95% CI: 3.2412-9.9824)⁸8. Araujo S, Rezende MM, Sousa DC, Rosa MR, Santos DC, Goulart LR, et al. Risk-benefit assessment of Bacillus Calmette-Guérin vaccination, anti-phenolic glycolipid I serology, and Mitsuda test response: 10-year follow-up of household contacts of leprosy patients. Rev Soc Bras Med Trop. 2015;48:739-45.; and RR=5.97 (95% CI: 1.45-24.5)³³33. Araujo S, Freitas LO, Goulart LR, Goulart IM. Molecular evidence for the aerial route of infection of Mycobacterium leprae and the role of asymptomatic carriers in the persistence of leprosy. Clin Infect Dis. 2016;63:1412-20..

Furthermore, seropositive contacts had a 4.04 times greater chance of neural impairment compared to seronegative contacts (OR=4.04; 95% CI: 1.24-13.21)³⁵35. Santos DF, Mendonça MR, Antunes DE, Sabino EF, Pereira RC, Goulart LR, et al. Molecular, immunological and neurophysiological evaluations for early diagnosis of neural impairment in seropositive leprosy household contacts. PLoS Negl Trop Dis. 2018;12:e0006494.. Positive Anti-PGL-1 in contacts between 4 and 15 years old was reported to be associated with the development of disease, presenting RR=8.5 (95% CI: 4.0-18.0)²³23. TiemiNagao-Dias A, Macedo AC, Rodrigues RO, Pedroza FH, Albuquerque AA, Moreira FA, et al. Serum anti-PGL-1 IgG, IgM, and IgA in a 3-year follow-up study of 4–15-year-old leprosy contacts. Pediatr Infect Dis J. 2019;38:e193-8..

Mitsuda test

Two studies identified an association between the illness and a negative Mitsuda test⁷7. Sarno EN, Duppre NC, Sales AM, Hacker MA, Nery JA, Matos HJ. Leprosy exposure, infection and disease: a 25-year surveillance study of leprosy patient contacts. Mem Inst Oswaldo Cruz. 2012;107:1054-9.,¹⁰10. Goulart IM, Souza DO, Marques CR, Pimenta VL, Gonçalves MA, Goulart LR. Risk and protective factors for leprosy development determined by epidemiological surveillance of household contacts. Clin Vaccine Immunol. 2008;15:101-5.. An estimated 6.25-fold increased risk of developing the disease was described for contacts with Mitsuda results ≤7 mm¹⁰10. Goulart IM, Souza DO, Marques CR, Pimenta VL, Gonçalves MA, Goulart LR. Risk and protective factors for leprosy development determined by epidemiological surveillance of household contacts. Clin Vaccine Immunol. 2008;15:101-5. (OR =0.16; 95% CI: 0.05-0.46) and a 3-fold increased risk in a cohort followed for 25 years (OR=3.093; 95% CI: 1.735-5.514)⁷7. Sarno EN, Duppre NC, Sales AM, Hacker MA, Nery JA, Matos HJ. Leprosy exposure, infection and disease: a 25-year surveillance study of leprosy patient contacts. Mem Inst Oswaldo Cruz. 2012;107:1054-9..

BCG vaccine scars

Three studies identified an association between illness and the absence of BCG scars⁷7. Sarno EN, Duppre NC, Sales AM, Hacker MA, Nery JA, Matos HJ. Leprosy exposure, infection and disease: a 25-year surveillance study of leprosy patient contacts. Mem Inst Oswaldo Cruz. 2012;107:1054-9.,¹⁰10. Goulart IM, Souza DO, Marques CR, Pimenta VL, Gonçalves MA, Goulart LR. Risk and protective factors for leprosy development determined by epidemiological surveillance of household contacts. Clin Vaccine Immunol. 2008;15:101-5.,²⁹29. Düppre NC, Camacho LA, Sales AM, Illarramendi X, Nery JA, Sampaio EP, et al. Impact of PGL-I seropositivity on the protective effect of BCG vaccination among leprosy contacts: a cohort study. PLoS Negl Trop Dis. 2012;6:e1711.. They pointed out a 3.7 times higher risk for contacts without a scar¹⁰10. Goulart IM, Souza DO, Marques CR, Pimenta VL, Gonçalves MA, Goulart LR. Risk and protective factors for leprosy development determined by epidemiological surveillance of household contacts. Clin Vaccine Immunol. 2008;15:101-5., and a 1.8 times higher risk among unvaccinated contacts⁷7. Sarno EN, Duppre NC, Sales AM, Hacker MA, Nery JA, Matos HJ. Leprosy exposure, infection and disease: a 25-year surveillance study of leprosy patient contacts. Mem Inst Oswaldo Cruz. 2012;107:1054-9..

Four studies identified that the presence of a BCG vaccine scar was considered a protective factor for developing leprosy⁸8. Araujo S, Rezende MM, Sousa DC, Rosa MR, Santos DC, Goulart LR, et al. Risk-benefit assessment of Bacillus Calmette-Guérin vaccination, anti-phenolic glycolipid I serology, and Mitsuda test response: 10-year follow-up of household contacts of leprosy patients. Rev Soc Bras Med Trop. 2015;48:739-45.,¹⁰10. Goulart IM, Souza DO, Marques CR, Pimenta VL, Gonçalves MA, Goulart LR. Risk and protective factors for leprosy development determined by epidemiological surveillance of household contacts. Clin Vaccine Immunol. 2008;15:101-5.,²⁴24. Gomes RR, Antunes DE, Santos DF, Sabino EF, Oliveira DB, Goulart IM. BCG vaccine and leprosy household contacts: protective effect and probability to becoming sick during follow-up. Vaccine. 2019;37:6510-7.,³¹31. Santos DS, Duppre NC, Sales AM, Nery JA, Sarno EN, Hacker MA. Kinship and leprosy in the contacts of leprosy patients: cohort at the Souza Araújo Outpatient Clinic, Rio de Janeiro, RJ, 1987–2010. J Trop Med. 2013;2013:596316.. The presence of at least one BCG vaccine scar showed a 2.44 times greater protection against neural impairment in leprosy contacts³⁵35. Santos DF, Mendonça MR, Antunes DE, Sabino EF, Pereira RC, Goulart LR, et al. Molecular, immunological and neurophysiological evaluations for early diagnosis of neural impairment in seropositive leprosy household contacts. PLoS Negl Trop Dis. 2018;12:e0006494..

Genetic factors

Consanguinity

Four studies have identified the association between illness and consanguinity¹⁵15. Sales AM, Ponce de Leon A, Düppre NC, Hacker MA, Nery JA, Sarno EN, et al. Leprosy among patient contacts: a multilevel study of risk factors. PLoS Negl Trop Dis. 2011;5:e1013.,²⁷27. Durães SM, Guedes LS, Cunha MD, Cavaliere FA, Oliveira ML. Estudo de 20 focos familiares de hanseníase no município de Duque de Caxias, Rio de Janeiro. An Bras Dermatol. 2005;80 Supl 3:S295-300.,²⁸28. Durães SM, Guedes LS, Cunha MD, Magnanini MM, Oliveira ML. Epidemiologic study of 107 cases of families with leprosy in Duque de Caxias, Rio de Janeiro, Brazil. An Bras Dermatol. 2010;85:339-45.,³¹31. Santos DS, Duppre NC, Sales AM, Nery JA, Sarno EN, Hacker MA. Kinship and leprosy in the contacts of leprosy patients: cohort at the Souza Araújo Outpatient Clinic, Rio de Janeiro, RJ, 1987–2010. J Trop Med. 2013;2013:596316.. The probability of getting sick among consanguineous family members was higher than among non-consanguineous individuals, with estimates reported as OR=2.8 (95% CI: 1.77-7.74)³⁵35. Santos DF, Mendonça MR, Antunes DE, Sabino EF, Pereira RC, Goulart LR, et al. Molecular, immunological and neurophysiological evaluations for early diagnosis of neural impairment in seropositive leprosy household contacts. PLoS Negl Trop Dis. 2018;12:e0006494. and OR=1.89 (95% CI: 1.42-2.51)¹⁵15. Sales AM, Ponce de Leon A, Düppre NC, Hacker MA, Nery JA, Sarno EN, et al. Leprosy among patient contacts: a multilevel study of risk factors. PLoS Negl Trop Dis. 2011;5:e1013.. When the kinship is of the first degree, the chance of developing leprosy was OR=2.42 (95% CI: 1.75; 3.35)²⁸28. Durães SM, Guedes LS, Cunha MD, Magnanini MM, Oliveira ML. Epidemiologic study of 107 cases of families with leprosy in Duque de Caxias, Rio de Janeiro, Brazil. An Bras Dermatol. 2010;85:339-45.. Regarding incident cases, the reported risk factors were: being father or mother (aRR=10.93; 95% CI: 3.48-34.27); son (aRR=5.34; 95% CI: 1.74-16.38); brother (aRR=7.03; 95% CI: 2.41-20.46), uncle, nephew, cousin, grandfather and grandson (RR=3.71; 95% CI: 1.24-11.06); wife, fiancé and partner (aRR=7.53; 95% CI: 2.51-22.57). There was also an association between kinship and illness for co-prevalent cases³¹31. Santos DS, Duppre NC, Sales AM, Nery JA, Sarno EN, Hacker MA. Kinship and leprosy in the contacts of leprosy patients: cohort at the Souza Araújo Outpatient Clinic, Rio de Janeiro, RJ, 1987–2010. J Trop Med. 2013;2013:596316..

Mycobacterium leprae positive PCR

Two studies identified an association between the illness and a positive PCR³³33. Araujo S, Freitas LO, Goulart LR, Goulart IM. Molecular evidence for the aerial route of infection of Mycobacterium leprae and the role of asymptomatic carriers in the persistence of leprosy. Clin Infect Dis. 2016;63:1412-20.,³⁶36. Reis EM, Araujo S, Lobato J, Neves AF, Costa AV, Gonçalves MA, et al. Mycobacterium leprae DNA in peripheral blood may indicate a bacilli migration route and high-risk for leprosy onset. Clin Microbiol Infect. 2014;20:447-52.. The ML0024 qPCR positivity at the time of diagnosis of the index case showed an OR=14.78 for developing leprosy (95% CI: 3.6-60.8; p<0.0001). Another study suggested the combination of this marker with other prognostic markers for contact management³⁶36. Reis EM, Araujo S, Lobato J, Neves AF, Costa AV, Gonçalves MA, et al. Mycobacterium leprae DNA in peripheral blood may indicate a bacilli migration route and high-risk for leprosy onset. Clin Microbiol Infect. 2014;20:447-52.. The qPCR was positive in blood samples of 104 contacts. The probability of disease outcome was estimated, as well as the relative risk, by comparing the results of the household contacts who had the disease with the results of those without clinical manifestations during the follow-up (LR+ and RR=5.54; 95% CI: 1.30-23.62)³³33. Araujo S, Freitas LO, Goulart LR, Goulart IM. Molecular evidence for the aerial route of infection of Mycobacterium leprae and the role of asymptomatic carriers in the persistence of leprosy. Clin Infect Dis. 2016;63:1412-20.. Another study identified that positivity for qPCR in peripheral blood presented a 2.08 times higher concerning the neural impairment in leprosy contacts (OR=2.08; 95% CI: 1.08-4.02)³⁵35. Santos DF, Mendonça MR, Antunes DE, Sabino EF, Pereira RC, Goulart LR, et al. Molecular, immunological and neurophysiological evaluations for early diagnosis of neural impairment in seropositive leprosy household contacts. PLoS Negl Trop Dis. 2018;12:e0006494..

Sociodemographic determinants

Age

Three studies identified the age of the contact as a risk factor associated with illness²⁵25. Manta FS, Barbieri RR, Moreira SJ, Santos PT, Nery JA, Duppre NC, et al. Quantitative PCR for leprosy diagnosis and monitoring in household contacts: a follow-up study, 2011–2018. Sci Rep. 2019;9:16675.,²⁶26. Teixeira CS, Pescarini JM, Alves FJ, Nery JS, Sanchez MN, Teles C, et al. Incidence of and factors associated with leprosy among household contacts of patients with leprosy in Brazil. JAMA Dermatol. 2020;156:640-8.,³⁴34. Rodrigues TS, Gomes LC, Cortela DC, Silva EA, Silva CA, Ferreira SM. Factors associated with leprosy in children contacts of notified adults in an endemic region of Midwest Brazil. J Pediatr (Rio J). 2020;96:593-9.. Overall, there was a variation for extreme ages, such as children younger than 15 years old (aOR=3.41; 95% CI: 1.24-9.39), contacts older than 50 years old (aOR=3.11; 95% CI: 2.03-4.76)²⁶26. Teixeira CS, Pescarini JM, Alves FJ, Nery JS, Sanchez MN, Teles C, et al. Incidence of and factors associated with leprosy among household contacts of patients with leprosy in Brazil. JAMA Dermatol. 2020;156:640-8., and also people older than 60 years old (HR=32.4; 95% CI: 3.6-290.3)²⁵25. Manta FS, Barbieri RR, Moreira SJ, Santos PT, Nery JA, Duppre NC, et al. Quantitative PCR for leprosy diagnosis and monitoring in household contacts: a follow-up study, 2011–2018. Sci Rep. 2019;9:16675..

Ethnicity

Being of African descent and having black or brown skin color were reported to have a RR=1.66 among incident cases (95% CI: 1.14-2.42) and aOR=1.32 for prevalent cases (95% CI:1.02-1.70)³¹31. Santos DS, Duppre NC, Sales AM, Nery JA, Sarno EN, Hacker MA. Kinship and leprosy in the contacts of leprosy patients: cohort at the Souza Araújo Outpatient Clinic, Rio de Janeiro, RJ, 1987–2010. J Trop Med. 2013;2013:596316..

Education

One study identified the association between the schooling of the contact and leprosy disease. In the analysis of prevalent cases, an aOR=1.33 (95% CI: 0.81-2.18) was identified in contacts who had between 4 and 10 years of schooling, and aOR=2.18 (95% CI: 1.42-3.35) for contacts with less than 4 years of schooling³¹31. Santos DS, Duppre NC, Sales AM, Nery JA, Sarno EN, Hacker MA. Kinship and leprosy in the contacts of leprosy patients: cohort at the Souza Araújo Outpatient Clinic, Rio de Janeiro, RJ, 1987–2010. J Trop Med. 2013;2013:596316..

Factors related to cohabitation

Four studies identified an association between illness and type of contact¹⁵15. Sales AM, Ponce de Leon A, Düppre NC, Hacker MA, Nery JA, Sarno EN, et al. Leprosy among patient contacts: a multilevel study of risk factors. PLoS Negl Trop Dis. 2011;5:e1013.,²⁶26. Teixeira CS, Pescarini JM, Alves FJ, Nery JS, Sanchez MN, Teles C, et al. Incidence of and factors associated with leprosy among household contacts of patients with leprosy in Brazil. JAMA Dermatol. 2020;156:640-8.,²⁸28. Durães SM, Guedes LS, Cunha MD, Magnanini MM, Oliveira ML. Epidemiologic study of 107 cases of families with leprosy in Duque de Caxias, Rio de Janeiro, Brazil. An Bras Dermatol. 2010;85:339-45.,³¹31. Santos DS, Duppre NC, Sales AM, Nery JA, Sarno EN, Hacker MA. Kinship and leprosy in the contacts of leprosy patients: cohort at the Souza Araújo Outpatient Clinic, Rio de Janeiro, RJ, 1987–2010. J Trop Med. 2013;2013:596316.. The risk of becoming ill among household contacts was confirmed with aOR=2.44 (95% CI: 1.69; 3.4) when compared to non-household contacts²⁸28. Durães SM, Guedes LS, Cunha MD, Magnanini MM, Oliveira ML. Epidemiologic study of 107 cases of families with leprosy in Duque de Caxias, Rio de Janeiro, Brazil. An Bras Dermatol. 2010;85:339-45.; OR=1.96 (95% CI: 1.29-2.98) for incident cases¹⁵15. Sales AM, Ponce de Leon A, Düppre NC, Hacker MA, Nery JA, Sarno EN, et al. Leprosy among patient contacts: a multilevel study of risk factors. PLoS Negl Trop Dis. 2011;5:e1013., and OR=1.33 (95% CI: 1.02-1.73) for co-prevalent cases, which was in line with another study³¹31. Santos DS, Duppre NC, Sales AM, Nery JA, Sarno EN, Hacker MA. Kinship and leprosy in the contacts of leprosy patients: cohort at the Souza Araújo Outpatient Clinic, Rio de Janeiro, RJ, 1987–2010. J Trop Med. 2013;2013:596316. presenting aOR=1.33 (95% CI: 1.00-1.77) for co-prevalent cases. An OR=1.48 (95% CI: 1.17-1.88) was reported for household contacts of the multibacillary patients²⁶26. Teixeira CS, Pescarini JM, Alves FJ, Nery JS, Sanchez MN, Teles C, et al. Incidence of and factors associated with leprosy among household contacts of patients with leprosy in Brazil. JAMA Dermatol. 2020;156:640-8..

One study identified an association between illness and the time living together and/or cohabiting, showing that the longer the time of exposure to the bacillus, the greater the chance of becoming ill³¹31. Santos DS, Duppre NC, Sales AM, Nery JA, Sarno EN, Hacker MA. Kinship and leprosy in the contacts of leprosy patients: cohort at the Souza Araújo Outpatient Clinic, Rio de Janeiro, RJ, 1987–2010. J Trop Med. 2013;2013:596316.. Living together for over 5 years with the index case showed an aOR=1.48 (95% CI: 1.02-2.15) for becoming ill when analyzing the prevalent cases³¹31. Santos DS, Duppre NC, Sales AM, Nery JA, Sarno EN, Hacker MA. Kinship and leprosy in the contacts of leprosy patients: cohort at the Souza Araújo Outpatient Clinic, Rio de Janeiro, RJ, 1987–2010. J Trop Med. 2013;2013:596316..

Factors related to the index case

Regarding the index case, the relevant factors for the development of the disease in the group of contacts were education¹⁵15. Sales AM, Ponce de Leon A, Düppre NC, Hacker MA, Nery JA, Sarno EN, et al. Leprosy among patient contacts: a multilevel study of risk factors. PLoS Negl Trop Dis. 2011;5:e1013. and bacilloscopic index¹⁵15. Sales AM, Ponce de Leon A, Düppre NC, Hacker MA, Nery JA, Sarno EN, et al. Leprosy among patient contacts: a multilevel study of risk factors. PLoS Negl Trop Dis. 2011;5:e1013.,³¹31. Santos DS, Duppre NC, Sales AM, Nery JA, Sarno EN, Hacker MA. Kinship and leprosy in the contacts of leprosy patients: cohort at the Souza Araújo Outpatient Clinic, Rio de Janeiro, RJ, 1987–2010. J Trop Med. 2013;2013:596316.. For prevalent cases, the chance of becoming ill among contacts of multibacillary patients with bacillary index (BI) from one to three presented an OR=1.79 (95% CI: 1.19–2.17) when compared to the index case with BI zero. For BI higher than 3, the result was OR=4.07 (95% CI: 2.73-6.09) when compared to patients with BI zero¹⁵15. Sales AM, Ponce de Leon A, Düppre NC, Hacker MA, Nery JA, Sarno EN, et al. Leprosy among patient contacts: a multilevel study of risk factors. PLoS Negl Trop Dis. 2011;5:e1013..

For incident cases, the chance of developing illness for contacts of a leprosy patient with BI higher than 3 was RR=5.27 (95% CI: 2.96-9.38) and for contacts of patients with BI between 0.1 to 3 was aRR=3.68 (95% CI: 1.99-6.82)³¹31. Santos DS, Duppre NC, Sales AM, Nery JA, Sarno EN, Hacker MA. Kinship and leprosy in the contacts of leprosy patients: cohort at the Souza Araújo Outpatient Clinic, Rio de Janeiro, RJ, 1987–2010. J Trop Med. 2013;2013:596316.. The index case for education up to 4 years showed an OR=2.72 (95% CI: 1.54-4.79) and education from 4 to 10 years presented an OR=2.40 (95% CI: 1.30-4.42), being a risk factor among co-prevalent cases¹⁵15. Sales AM, Ponce de Leon A, Düppre NC, Hacker MA, Nery JA, Sarno EN, et al. Leprosy among patient contacts: a multilevel study of risk factors. PLoS Negl Trop Dis. 2011;5:e1013..

Combined risks

Two studies identified an association between BCG, ML Flow, Mitsuda test, and the development of leprosy among the contacts⁸8. Araujo S, Rezende MM, Sousa DC, Rosa MR, Santos DC, Goulart LR, et al. Risk-benefit assessment of Bacillus Calmette-Guérin vaccination, anti-phenolic glycolipid I serology, and Mitsuda test response: 10-year follow-up of household contacts of leprosy patients. Rev Soc Bras Med Trop. 2015;48:739-45.,¹⁰10. Goulart IM, Souza DO, Marques CR, Pimenta VL, Gonçalves MA, Goulart LR. Risk and protective factors for leprosy development determined by epidemiological surveillance of household contacts. Clin Vaccine Immunol. 2008;15:101-5.. The relationship between the amount of BCG scars, Mitsuda test, and ML Flow serological test was identified. The presence of one or two BCG vaccine scars among the leprosy contacts showed a higher cellular immune response in the Mitsuda test.

Factors in children under 15 years old

The following factors were associated with leprosy after adjustments: age (OR=3.41; 95% CI: 1.24-9.39), residence area (OR=2.60; 95% CI: 1.11-6.09), garbage disposal (OR=7.31; 95% CI: 1.91-27.98), family history of the disease (OR=8.76; 95% CI: 3.41-22.50), and length of residence (OR=3.36; 95% CI: 1.45-7.78)²⁶26. Teixeira CS, Pescarini JM, Alves FJ, Nery JS, Sanchez MN, Teles C, et al. Incidence of and factors associated with leprosy among household contacts of patients with leprosy in Brazil. JAMA Dermatol. 2020;156:640-8..

Becoming ill among individuals aged from 8 to 14 years old presented an OR=3.4 (95% CI: 1.24-9.39) when compared to individuals aged from 1 to 7 years old. Those living in rural areas who developed the disease presented an OR=2.6 (95% CI: 1.11-6.09) compared to people living in urban areas. Developing leprosy had an OR=7.3 (95% CI: 1.91-27.98) when garbage was burned or buried compared to those with access to garbage collection. Children with a family history of leprosy presented an OR=8.76 (95% CI: 3,41-22.50) to develop the disease compared to those with no family history. The probability of leprosy occurrence was 3.3 times higher when living in a residence for more than 5 years with the index case than living for less time in the same residence²⁶26. Teixeira CS, Pescarini JM, Alves FJ, Nery JS, Sanchez MN, Teles C, et al. Incidence of and factors associated with leprosy among household contacts of patients with leprosy in Brazil. JAMA Dermatol. 2020;156:640-8..

Protective factors against illness in leprosy contacts

The protective factors against illness were the presence of one or more BCG vaccine scars⁸8. Araujo S, Rezende MM, Sousa DC, Rosa MR, Santos DC, Goulart LR, et al. Risk-benefit assessment of Bacillus Calmette-Guérin vaccination, anti-phenolic glycolipid I serology, and Mitsuda test response: 10-year follow-up of household contacts of leprosy patients. Rev Soc Bras Med Trop. 2015;48:739-45.,¹⁰10. Goulart IM, Souza DO, Marques CR, Pimenta VL, Gonçalves MA, Goulart LR. Risk and protective factors for leprosy development determined by epidemiological surveillance of household contacts. Clin Vaccine Immunol. 2008;15:101-5.,²⁴24. Gomes RR, Antunes DE, Santos DF, Sabino EF, Oliveira DB, Goulart IM. BCG vaccine and leprosy household contacts: protective effect and probability to becoming sick during follow-up. Vaccine. 2019;37:6510-7.,³¹31. Santos DS, Duppre NC, Sales AM, Nery JA, Sarno EN, Hacker MA. Kinship and leprosy in the contacts of leprosy patients: cohort at the Souza Araújo Outpatient Clinic, Rio de Janeiro, RJ, 1987–2010. J Trop Med. 2013;2013:596316.,³⁵35. Santos DF, Mendonça MR, Antunes DE, Sabino EF, Pereira RC, Goulart LR, et al. Molecular, immunological and neurophysiological evaluations for early diagnosis of neural impairment in seropositive leprosy household contacts. PLoS Negl Trop Dis. 2018;12:e0006494., positive Mitsuda test⁸8. Araujo S, Rezende MM, Sousa DC, Rosa MR, Santos DC, Goulart LR, et al. Risk-benefit assessment of Bacillus Calmette-Guérin vaccination, anti-phenolic glycolipid I serology, and Mitsuda test response: 10-year follow-up of household contacts of leprosy patients. Rev Soc Bras Med Trop. 2015;48:739-45. and the level of education of leprosy contacts²⁶26. Teixeira CS, Pescarini JM, Alves FJ, Nery JS, Sanchez MN, Teles C, et al. Incidence of and factors associated with leprosy among household contacts of patients with leprosy in Brazil. JAMA Dermatol. 2020;156:640-8.. The protection factors are described in Table 3.

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Table 3
Protective factors against illness in leprosy contacts.

DISCUSSION

This systematic review described the factors associated with the development of disease in leprosy contacts of the Brazilian population. In this review, all selected studies were classified as of high quality which indicates the consistency of their results. Most studies were funded by organizations with no potential economic interests, which may contribute to a more independent interpretation of the data. The identification of risk and protective factors in the Brazilian population can substantiate the establishment of strategies for early case detection, monitoring of leprosy contacts, and controlling the disease, helping health managers to improve the effectiveness of actions in public health. The heterogeneity of the variables described revealed the complexity of assessing a neglected disease and may compromise the identification of important factors to be considered for decision-making in healthcare. A broad overview of risk and protective factors was provided to enrich the discussion on the disease development process in leprosy contacts.

Immunological factors

The selected studies confirmed the importance of Anti-PGL-1 serology for the identification of contacts at higher risk of illness. It is known that Anti-PGL-1 serology has a strong association with smear microscopy since the gradual increase in BI is accompanied by a semiquantitative increase in antibody levels measured by the test³⁷37. Santos GG, Marcucci G, Guimarães Júnior J, Margarido LC, Lopes LH. Pesquisa de Mycobacterium leprae em biópsias de mucosa oral por meio da reação em cadeia da polimerase. An Bras Dermatol. 2007;82:245-9.,³⁸38. Santos AR, Degrave WM, Suffys PN. Use of polymerase chain reaction (PCR) in leprosy research. Indian J Lepr. 1999;71:101-10.. The findings corroborate other studies, which identified that this test helps to detect contacts that tend to develop leprosy regardless of the clinical form of the index case³3. Bührer-Sékula S, Smits HL, Gussenhoven GC, van Leeuwen J, Amador S, Fujiwara T, et al. Simple and fast lateral flow test for classification of leprosy patients and identification of contacts with high risk of developing leprosy. J Clin Microbiol. 2003;41:1991-5.,³⁹39. Bührer-Sékula S. PGL-I leprosy serology. Rev Soc Bras Med Trop. 2008;41 Suppl 2:3-5.,⁴⁰40. Moura RS, Calado KL, Oliveira ML, Bührer-Sékula S. Leprosy serology using PGL-I: a systematic review. Rev Soc Bras Med Trop. 2008;41 Suppl 2:11-8. and that illness among seropositive individuals can vary from 2 to 13%⁴4. Douglas JT, Cellona RV, Fajardo TT Jr, Abalos RM, Balagon MV, Klatser PR. Prospective study of serological conversion as a risk factor for development of leprosy among household contacts. Clin Vaccine Immunol. 2004;11:897-900.,⁸8. Araujo S, Rezende MM, Sousa DC, Rosa MR, Santos DC, Goulart LR, et al. Risk-benefit assessment of Bacillus Calmette-Guérin vaccination, anti-phenolic glycolipid I serology, and Mitsuda test response: 10-year follow-up of household contacts of leprosy patients. Rev Soc Bras Med Trop. 2015;48:739-45.,¹⁰10. Goulart IM, Souza DO, Marques CR, Pimenta VL, Gonçalves MA, Goulart LR. Risk and protective factors for leprosy development determined by epidemiological surveillance of household contacts. Clin Vaccine Immunol. 2008;15:101-5.,²⁹29. Düppre NC, Camacho LA, Sales AM, Illarramendi X, Nery JA, Sampaio EP, et al. Impact of PGL-I seropositivity on the protective effect of BCG vaccination among leprosy contacts: a cohort study. PLoS Negl Trop Dis. 2012;6:e1711.,⁴¹41. Brasil MT, Oliveira LR, Rímoli NS, Cavallari S, Gonçalves OS, Lessa ZL, et al. Sorologia anti PGL-1 e risco de ocorrência de hanseníase em área de alta endemicidade do Estado de São Paulo: quatro anos de seguimento. Rev Bras Epidemiol. 2003;6:262-71.. A systematic review and meta-analysis of cohort studies classified contacts according to positivity for Anti-PGL-1 in the first assessment with at least a one-year follow-up showed that contacts who were Anti-PGL-1 positive at the start of the study were three times more likely to develop leprosy⁴²42. Penna ML, Penna GO, Iglesias PC, Natal S, Rodrigues LC. Anti-PGL-1 Positivity as a risk marker for the development of leprosy among contacts of leprosy cases: systematic review and meta-analysis. PLoS Negl Trop Dis. 2016;10:e0004703.. These data reinforce the importance of testing to monitor leprosy contacts⁷7. Sarno EN, Duppre NC, Sales AM, Hacker MA, Nery JA, Matos HJ. Leprosy exposure, infection and disease: a 25-year surveillance study of leprosy patient contacts. Mem Inst Oswaldo Cruz. 2012;107:1054-9..

The Mitsuda test helps with the diagnosis of leprosy⁴³43. Lastória JC, Abreu MA. Leprosy: review of the epidemiological, clinical, and etiopathogenic aspects - Part 1. An Bras Dermatol. 2014;89:205-18., especially when combined with other tests, and can also be useful for monitoring household and social contacts of leprosy patients⁴⁴44. Beiguelman B. A reação de Mitsuda depois de oitenta anos. Hansenol Int. 1999;24:144-61.

45. Arruda MS, Arruda OS, Astolfi CS, Opromolla DV. Estudo das reações de Fernandez e Mitsuda em pacientes hansenianos e seus contatos. Hansenol Int. 1985;10:23-31.-⁴⁶46. Convit J, Avila JL, Goihman M, Pinardi ME. A test for the determination of competency in clearing bacilli in leprosy patients. Bull World Health Organ. 1972;46:821-6.. The results found regarding the Mitsuda test have also been elucidated by other authors. The Mitsuda positive reactions were observed between 59% and 88.2%⁴⁵45. Arruda MS, Arruda OS, Astolfi CS, Opromolla DV. Estudo das reações de Fernandez e Mitsuda em pacientes hansenianos e seus contatos. Hansenol Int. 1985;10:23-31.,⁴⁷47. Cardona-Castro NM, Restrepo-Jaramillo S, de la Ossa MG, Brennan PJ. Infection by Mycobacterium leprae of household contacts of lepromatous leprosy patients from a post-elimination leprosy region of Colombia. Mem Inst Oswaldo Cruz. 2005;100:703-7.,⁴⁸48. Contin LA, Alves CJ, Fogagnolo L, Nassif PW, Barreto JA, Lauris JR, et al. Use of the ML-Flow test as a tool in classifying and treating leprosy. An Bras Dermatol. 2011;86:91-5. of healthy contacts, and the proportion of positive reactions may increase with age⁴⁴44. Beiguelman B. A reação de Mitsuda depois de oitenta anos. Hansenol Int. 1999;24:144-61.. In a study with leprosy patients, the participation of the allele HLA-DQ1 in the absence of response to the Mitsuda test⁴⁹49. Souza FC, Marcos EV, Ura S, Opromolla PA, Nogueira ME. Estudo comparativo entre reação de Mitsuda e antígenos leucocitários humanos em pacientes hansenianos. Rev Soc Bras Med Trop. 2007;40:188-91. has been reported. Then, new studies that investigate cellular immunity in leprosy contacts would contribute substantially to getting new biomarkers³⁹39. Bührer-Sékula S. PGL-I leprosy serology. Rev Soc Bras Med Trop. 2008;41 Suppl 2:3-5..

Regarding the BCG vaccine scars, the increased immune response against leprosy after vaccination has already been demonstrated, and the administration of an additional dose of BCG has been reported to be even more protective⁹9. Setia MS, Steinmaus C, Ho CS, Rutherford GW. The role of BCG in prevention of leprosy: a meta-analysis. Lancet Infect Dis. 2006;6:162-70.,¹¹11. Merle CS, Cunha SS, Rodrigues LC. BCG vaccination and leprosy protection: review of current evidence and status of BCG in leprosy control. Expert Rev Vaccines. 2010;9:209-22.. A meta-analysis⁹9. Setia MS, Steinmaus C, Ho CS, Rutherford GW. The role of BCG in prevention of leprosy: a meta-analysis. Lancet Infect Dis. 2006;6:162-70. identified a protective effect of BCG of 26% among experimental studies and 61% among observational studies. The protection was greater against multibacillary forms of leprosy compared to paucibacillary forms. Another meta-analysis also confirmed that there is sufficient and convincing evidence for the protective effect of BCG vaccination against leprosy in patients⁵⁰50. Zodpey SP, Ambadekar NN, Thakur A. Effectiveness of Bacillus Calmette Guerin (BCG) vaccination in the prevention of leprosy: a population-based case–control study in Yavatmal District, India. Public Health. 2005;119:209-16..

The protective effect of BCG vaccination has been demonstrated with a range of 20-90%, and there is consistent evidence for its role in reducing the incidence of leprosy¹¹11. Merle CS, Cunha SS, Rodrigues LC. BCG vaccination and leprosy protection: review of current evidence and status of BCG in leprosy control. Expert Rev Vaccines. 2010;9:209-22.,⁵⁰50. Zodpey SP, Ambadekar NN, Thakur A. Effectiveness of Bacillus Calmette Guerin (BCG) vaccination in the prevention of leprosy: a population-based case–control study in Yavatmal District, India. Public Health. 2005;119:209-16.,⁵¹51. Moet FJ, Oskam L, Faber R, Pahan D, Richardus JH. A study on transmission and a trial of chemoprophylaxis in contacts of leprosy patients: design, methodology and recruitment findings of COLEP. Lepr Rev. 2004;75:376-88.. These findings support the introduction of BCG vaccination as a protective factor against the development of leprosy among contacts, and the absence of vaccine scar as a risk factor to become ill.

In summary, there is an association between Anti-PGL-1, IgM serology, Mitsuda test, and BCG scars with the risk of illness, especially when these factors are combined. Some follow-up studies on the illness of leprosy contacts positively correlated BCG scars, Mitsuda test, and ML Flow result⁷7. Sarno EN, Duppre NC, Sales AM, Hacker MA, Nery JA, Matos HJ. Leprosy exposure, infection and disease: a 25-year surveillance study of leprosy patient contacts. Mem Inst Oswaldo Cruz. 2012;107:1054-9.,⁸8. Araujo S, Rezende MM, Sousa DC, Rosa MR, Santos DC, Goulart LR, et al. Risk-benefit assessment of Bacillus Calmette-Guérin vaccination, anti-phenolic glycolipid I serology, and Mitsuda test response: 10-year follow-up of household contacts of leprosy patients. Rev Soc Bras Med Trop. 2015;48:739-45.,³⁹39. Bührer-Sékula S. PGL-I leprosy serology. Rev Soc Bras Med Trop. 2008;41 Suppl 2:3-5.. These results indicate the importance of performing these tests for the surveillance of leprosy contacts.

Genetic conditions

Consanguinity has been reported to be a risk factor for developing illness in leprosy contacts. Genetic-based studies have identified polymorphisms that may be associated with susceptibility to leprosy in index cases and contacts⁵²52. Moraes MO, Cardoso CC, Vanderborght PR, Pacheco AG. Genetics of host response in leprosy. Lepr Rev. 2006;77:189-202.

53. Manry J, Nédélec Y, Fava VM, Cobat A, Orlova M, Van Thuc N, et al. Deciphering the genetic control of gene expression following Mycobacterium leprae antigen stimulation. PLoS Genet. 2017;13:e1006952.-⁵⁴54. Oliveira AL, Chaves AT, Menezes CA, Guimarães NS, Bueno LL, Fujiwara RT, et al. Vitamin D receptor expression and hepcidin levels in the protection or severity of leprosy: a systematic review. Microbes Infect. 2017;19:311-22.. Genetic and/or environmental factors may exert a crucial influence on the transmission of M. leprae infection and/or the pathogenesis of leprosy⁵⁴54. Oliveira AL, Chaves AT, Menezes CA, Guimarães NS, Bueno LL, Fujiwara RT, et al. Vitamin D receptor expression and hepcidin levels in the protection or severity of leprosy: a systematic review. Microbes Infect. 2017;19:311-22.. There is a close genetic relationship in leprosy among family members, especially between children, parents, and siblings.

The blood PCR should be considered as a risk factor, but associated with other factors³⁶36. Reis EM, Araujo S, Lobato J, Neves AF, Costa AV, Gonçalves MA, et al. Mycobacterium leprae DNA in peripheral blood may indicate a bacilli migration route and high-risk for leprosy onset. Clin Microbiol Infect. 2014;20:447-52., reinforcing the importance of considering not only genetic factors but also other ones for a better understanding of the disease process. Blood PCR presented in leprosy contacts high sensitivity and allowed the detection of bacterial cells from the amplification of DNA fragments³⁷37. Santos GG, Marcucci G, Guimarães Júnior J, Margarido LC, Lopes LH. Pesquisa de Mycobacterium leprae em biópsias de mucosa oral por meio da reação em cadeia da polimerase. An Bras Dermatol. 2007;82:245-9.. For detection of the M. leprae bacillus, blood samples, cellular scrapings, skin biopsy, nerve, and nasal secretion can be used. However, in this review, positive PCR in the blood has been reported to be a risk factor for becoming ill and for nerve involvement in leprosy contacts.

Sociodemographic factors

Precarious living conditions have been reported to contribute to the persistence of leprosy transmission¹⁴14. Imbiriba EN, Silva Neto NA, Souza WV, Pedrosa V, Cunha MG, Garnelo L. Desigualdade social, crescimento urbano e hanseníase em Manaus: abordagem espacial. Rev Saude Publica. 2009;43:656-65.. Social inequality increases the susceptibility to various diseases, including leprosy¹³13. Kerr-Pontes LR, Montenegro AC, Barreto ML, Werneck GL, Feldmeier H. Inequality and leprosy in Northeast Brazil: an ecological study. Int J Epidemiol. 2004;33:262-9.. Another study reported an association between the development of leprosy and social conditions, even though these associations would not necessarily imply a causal connection¹⁶16. Freitas LR, Duarte EC, Garcia LP. Leprosy in Brazil and its association with characteristics of municipalities: ecological study, 2009-2011. Trop Med Int Health. 2014;19:1216-25. corroborating the findings of this review. Education level has been reported as a risk³¹31. Santos DS, Duppre NC, Sales AM, Nery JA, Sarno EN, Hacker MA. Kinship and leprosy in the contacts of leprosy patients: cohort at the Souza Araújo Outpatient Clinic, Rio de Janeiro, RJ, 1987–2010. J Trop Med. 2013;2013:596316. and protective²⁶26. Teixeira CS, Pescarini JM, Alves FJ, Nery JS, Sanchez MN, Teles C, et al. Incidence of and factors associated with leprosy among household contacts of patients with leprosy in Brazil. JAMA Dermatol. 2020;156:640-8. factor. Several studies pointed to a higher chance of getting sick with leprosy in the lower economic class population¹⁴14. Imbiriba EN, Silva Neto NA, Souza WV, Pedrosa V, Cunha MG, Garnelo L. Desigualdade social, crescimento urbano e hanseníase em Manaus: abordagem espacial. Rev Saude Publica. 2009;43:656-65.,¹⁶16. Freitas LR, Duarte EC, Garcia LP. Leprosy in Brazil and its association with characteristics of municipalities: ecological study, 2009-2011. Trop Med Int Health. 2014;19:1216-25.,⁵⁵55. Goltzman D, Hendy GN, White JH. Vitamin D and its receptor during late development. Biochim Biophys Acta. 2015;1849:171-80..

An integrative review⁵⁶56. Leano HA, Araújo KM, Bueno IC, Niitsuma EN, Lana FC. Socioeconomic factors related to leprosy: an integrative literature review. Rev Bras Enferm. 2019;72:1405-15. discussed that leprosy is highly influenced by the social context in which the patient is embedded. It has been emphasized that it is important to consider the socioeconomic factors to identify unfavorable indicators supporting the development of practices to reduce inequalities in the process of care for leprosy patients. These practices should go beyond health care, bringing an intersectoral articulation, with systemic and social care for leprosy patients.

Regarding proximity with the index case, it was observed that household contacts have a greater chance of becoming ill²⁹29. Düppre NC, Camacho LA, Sales AM, Illarramendi X, Nery JA, Sampaio EP, et al. Impact of PGL-I seropositivity on the protective effect of BCG vaccination among leprosy contacts: a cohort study. PLoS Negl Trop Dis. 2012;6:e1711.,⁵⁷57. Khadge S, Banu S, Bobosha K, Schip JJ, Goulart IM, Thapa P, et al. Longitudinal immune profiles in type 1 leprosy reactions in Bangladesh, Brazil, Ethiopia and Nepal. BMC Infect Dis. 2015;15:477., but it is necessary to consider that social contacts also need to be monitored to control the disease. Being a spouse or boy/girlfriend would increase the chances of becoming ill³¹31. Santos DS, Duppre NC, Sales AM, Nery JA, Sarno EN, Hacker MA. Kinship and leprosy in the contacts of leprosy patients: cohort at the Souza Araújo Outpatient Clinic, Rio de Janeiro, RJ, 1987–2010. J Trop Med. 2013;2013:596316.. This fact can be explained by the type of interaction with the index case in which the contacts have intimate and prolonged interaction with the patient. Most factors related to index cases are associated with the transmissibility of the disease. These refer to the number of bacilli to which the contacts would be exposed, increasing the risk of transmission. The low education of the index case has also been reported as a risk factor probably due to poor living conditions⁵⁶56. Leano HA, Araújo KM, Bueno IC, Niitsuma EN, Lana FC. Socioeconomic factors related to leprosy: an integrative literature review. Rev Bras Enferm. 2019;72:1405-15..

In children, the factors associated with the disease showed the greater vulnerability of children aged 8 to 14 years old, associated with living conditions and time of residence, as well as family history of the disease. Illness in children showed that the disease is continuous, that there are undetected patients, and that there is the persistence of leprosy transmission in the community⁵⁸58. Pires CA, Malcher CM, Abreu Júnior JM, Albuquerque TG, Corrêa IR, Daxbacher EL. Leprosy in children under 15 years: the importance of early diagnosis. Rev Paul Pediatr. 2012;30:292-5..

This study described the scientific evidence related to the development of leprosy in Brazilian contacts by synthetizing their various immunological, genetic and sociodemographic factors. The disease-related factors in leprosy contacts have been studied and provide the scientific basis for decision-making in disease management. However, establishing a causal relationship is still a challenge, in addition to the dynamics of convivial relationships and sociodemographic conditions.

CONCLUSION

The Anti-PGL-1 seropositivity, negative Mitsuda test, absence of BCG scar, positive PCR in blood; age and race; conviviality, education, contact time and type of contact, as well as elements related to the index case (bacilloscopic index; genetic conditions, family relationships), and some combined factors (e.g., Mitsuda, Anti-PGL-1, BCG scar) were shown to be relevant risk factors associated with the development of disease in Brazilian leprosy contacts. The protective factors reported were the presence of one or more BCG scars, positive Mitsuda test, and education level. The knowledge of disease-related risk and protective factors provides the scientific basis for decision-making in the management of leprosy in contacts and may substantiate the development of strategies for disease monitoring.

ACKNOWLEDGMENTS

This study received administrative support from the Graduate Program in Health Sciences: Infectious Diseases and Tropical Medicine. MOCR is a research fellow of the Conselho Nacional de Desenvolvimento Cientifico e Tecnologico (CNPq) and holds a productivity scholarship.

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³⁷
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³⁸
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³⁹
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⁴⁰
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⁴¹
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⁴²
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⁴³
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⁴⁴
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⁴⁵
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⁴⁶
Convit J, Avila JL, Goihman M, Pinardi ME. A test for the determination of competency in clearing bacilli in leprosy patients. Bull World Health Organ. 1972;46:821-6.
⁴⁷
Cardona-Castro NM, Restrepo-Jaramillo S, de la Ossa MG, Brennan PJ. Infection by Mycobacterium leprae of household contacts of lepromatous leprosy patients from a post-elimination leprosy region of Colombia. Mem Inst Oswaldo Cruz. 2005;100:703-7.
⁴⁸
Contin LA, Alves CJ, Fogagnolo L, Nassif PW, Barreto JA, Lauris JR, et al. Use of the ML-Flow test as a tool in classifying and treating leprosy. An Bras Dermatol. 2011;86:91-5.
⁴⁹
Souza FC, Marcos EV, Ura S, Opromolla PA, Nogueira ME. Estudo comparativo entre reação de Mitsuda e antígenos leucocitários humanos em pacientes hansenianos. Rev Soc Bras Med Trop. 2007;40:188-91.
⁵⁰
Zodpey SP, Ambadekar NN, Thakur A. Effectiveness of Bacillus Calmette Guerin (BCG) vaccination in the prevention of leprosy: a population-based case–control study in Yavatmal District, India. Public Health. 2005;119:209-16.
⁵¹
Moet FJ, Oskam L, Faber R, Pahan D, Richardus JH. A study on transmission and a trial of chemoprophylaxis in contacts of leprosy patients: design, methodology and recruitment findings of COLEP. Lepr Rev. 2004;75:376-88.
⁵²
Moraes MO, Cardoso CC, Vanderborght PR, Pacheco AG. Genetics of host response in leprosy. Lepr Rev. 2006;77:189-202.
⁵³
Manry J, Nédélec Y, Fava VM, Cobat A, Orlova M, Van Thuc N, et al. Deciphering the genetic control of gene expression following Mycobacterium leprae antigen stimulation. PLoS Genet. 2017;13:e1006952.
⁵⁴
Oliveira AL, Chaves AT, Menezes CA, Guimarães NS, Bueno LL, Fujiwara RT, et al. Vitamin D receptor expression and hepcidin levels in the protection or severity of leprosy: a systematic review. Microbes Infect. 2017;19:311-22.
⁵⁵
Goltzman D, Hendy GN, White JH. Vitamin D and its receptor during late development. Biochim Biophys Acta. 2015;1849:171-80.
⁵⁶
Leano HA, Araújo KM, Bueno IC, Niitsuma EN, Lana FC. Socioeconomic factors related to leprosy: an integrative literature review. Rev Bras Enferm. 2019;72:1405-15.
⁵⁷
Khadge S, Banu S, Bobosha K, Schip JJ, Goulart IM, Thapa P, et al. Longitudinal immune profiles in type 1 leprosy reactions in Bangladesh, Brazil, Ethiopia and Nepal. BMC Infect Dis. 2015;15:477.
⁵⁸
Pires CA, Malcher CM, Abreu Júnior JM, Albuquerque TG, Corrêa IR, Daxbacher EL. Leprosy in children under 15 years: the importance of early diagnosis. Rev Paul Pediatr. 2012;30:292-5.

Supplementary Material available from:

https://doi.org/10.48331/scielodata.34HR6I

FUNDING: This study was funded in part by the Coordenacao de Aperfeicoamento de Pessoal de Nivel Superior (CAPES). Financial Code 001.

Publication Dates

Publication in this collection
30 Sept 2022
Date of issue
2022

History

Received
6 Mar 2022
Accepted
13 July 2022

This is an Open Access article distributed under the terms of the Creative Commons Attribution Non-Commercial License, which permits unrestricted non-commercial use, distribution, and reproduction in any medium, provided the original work is properly cited.

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Cardona-Castro NM, Restrepo-Jaramillo S, de la Ossa MG, Brennan PJ. Infection by Mycobacterium leprae of household contacts of lepromatous leprosy patients from a post-elimination leprosy region of Colombia. Mem Inst Oswaldo Cruz. 2005;100:703-7.

[48] ⁴⁸
Contin LA, Alves CJ, Fogagnolo L, Nassif PW, Barreto JA, Lauris JR, et al. Use of the ML-Flow test as a tool in classifying and treating leprosy. An Bras Dermatol. 2011;86:91-5.

[49] ⁴⁹
Souza FC, Marcos EV, Ura S, Opromolla PA, Nogueira ME. Estudo comparativo entre reação de Mitsuda e antígenos leucocitários humanos em pacientes hansenianos. Rev Soc Bras Med Trop. 2007;40:188-91.

[50] ⁵⁰
Zodpey SP, Ambadekar NN, Thakur A. Effectiveness of Bacillus Calmette Guerin (BCG) vaccination in the prevention of leprosy: a population-based case–control study in Yavatmal District, India. Public Health. 2005;119:209-16.

[51] ⁵¹
Moet FJ, Oskam L, Faber R, Pahan D, Richardus JH. A study on transmission and a trial of chemoprophylaxis in contacts of leprosy patients: design, methodology and recruitment findings of COLEP. Lepr Rev. 2004;75:376-88.

[52] ⁵²
Moraes MO, Cardoso CC, Vanderborght PR, Pacheco AG. Genetics of host response in leprosy. Lepr Rev. 2006;77:189-202.

[53] ⁵³
Manry J, Nédélec Y, Fava VM, Cobat A, Orlova M, Van Thuc N, et al. Deciphering the genetic control of gene expression following Mycobacterium leprae antigen stimulation. PLoS Genet. 2017;13:e1006952.

[54] ⁵⁴
Oliveira AL, Chaves AT, Menezes CA, Guimarães NS, Bueno LL, Fujiwara RT, et al. Vitamin D receptor expression and hepcidin levels in the protection or severity of leprosy: a systematic review. Microbes Infect. 2017;19:311-22.

[55] ⁵⁵
Goltzman D, Hendy GN, White JH. Vitamin D and its receptor during late development. Biochim Biophys Acta. 2015;1849:171-80.

[56] ⁵⁶
Leano HA, Araújo KM, Bueno IC, Niitsuma EN, Lana FC. Socioeconomic factors related to leprosy: an integrative literature review. Rev Bras Enferm. 2019;72:1405-15.

[57] ⁵⁷
Khadge S, Banu S, Bobosha K, Schip JJ, Goulart IM, Thapa P, et al. Longitudinal immune profiles in type 1 leprosy reactions in Bangladesh, Brazil, Ethiopia and Nepal. BMC Infect Dis. 2015;15:477.

[58] ⁵⁸
Pires CA, Malcher CM, Abreu Júnior JM, Albuquerque TG, Corrêa IR, Daxbacher EL. Leprosy in children under 15 years: the importance of early diagnosis. Rev Paul Pediatr. 2012;30:292-5.

Article numbers	Article	Study design	Leprosy contacts (n)	Index-cases (n)	Comparative group	Prevalence/Incidence for leprosy contacts detected	Classification	NOS score*	Funding sources
1	Durães et al.²⁷	cohort	254	20	--	55/254 (21.7%)	Household, peridomicile, and social contacts	7	NLR
2	Goulart et al.¹⁰	cohort	1,396	367 families	--	28 (2%)	Household contacts	8	FAPEMIG, CNPq, CAPES, FINEP, and the Brazilian Ministry of Health
3	Durães et al.²⁸	cohort	1,098	107	--	211 (20.3%)	Household and, peridomicile contacts	7	NLR
4	Sales et al.¹⁵	cohort	6,158	1,201		452 (7.3%)	Household and non-household contacts	8	CNPq, FAPERJ, and FIOCRUZ
5	Düppre et al.²⁹	cohort	2,135	668	--	46 (2.2%) coprevalent/ (60) 2.8% incidence. Incidence density of 5.08 per 1,000 people/year	Household contacts	8	FIOCRUZ, the Brazilian Ministry of Health, NLR and CNPq
6	Sarno et al.⁷	cohort	--	--	--	Incidence rate of 0.01694 cases per person-year in the first 5 years of follow-up	Household contacts	8	None
7	Santos et al.³¹	cohort	7,174	1,360	--	incidence of 2.01 per 1,000 people/year.	Household, family, and social contacts.	8	None
8	Reis et al.³⁶	cohort	826	200	--	26/826 (3.1%)	Household contacts	8	FAPEMIG, CNPq, CAPES and the National Fund for Health (Brazilian Ministry of Health).
9	Araújo et al.⁸	cohort	2,992	--	--	75 (2.5%)	Household contacts	8	None
10	Barreto et al.³²	cohort	750 time 1/ 254 time 2	--	--	43/254 (16.9%)	Household and social contacts	8	CNPq, CAPES, CAPES PROAMAZONIA, FAPESPA, SESPA, UFPA, FAEPA-HCFMRP-USP, NIH, MALTALEP, NIAID, PROPESP/UFPA and FADESP
11	Araújo et al.³³	cohort	104	--	--	7 (6.7%)	Household contacts	8	FAPEMIG, CNPQ, CAPES, and the National Fund for Health (Brazilian Ministry of Health).
12	Santos et al.³¹	case control	210	--	175 seropositive household contacts and 35 seronegative household contacts	4%(7/175) positive bacilloscopy/ 32.2% (19/59) neural thickening in the clinical evaluation	Intradomicile and extradomicile contacts.	8	CNPq and FAPEMIG

13	TiemiNagao-Dias et al.²³	cohort	68	--	--	8 (11.8%)	Household and peridomicile contacts	8	None
14	Gomes et al.²⁴	cohort	5,061	--	--	92/5,036 (1.8%)	Household contacts	8	CNPq and FAPEMIG

15	Manta et al.²⁵	cohort	2,437	--	--	69 (2.8%)	Household contacts	8	LRI, FAPERJ, CNPq, CAPES and the National Fund for Health (Brazilian Ministry of Health)
16	Teixeira et al.²⁶	cohort	42,725	17,876	--	829 (1.9%)	Household contacts	7	CNPQ, Wellcome Trust, CAPES
17	Rodrigues et al.³⁴	case-control	204	--	40 children <15 years (ex-intradomiciles and 164 <15 years	The overall incidence rate was 16.94 per 1,000 people/year of follow-up between 1987 and 1991.	Household and peridomicile contacts	7	Applied Research in Health Surveillance (Brazilian Ministry of Health)

Risk factors	Article	Results	Risk/chance estimates	CI (95%)	P-value	N Total
Positive ELISA/ ML flow	Goulart et al.¹⁰	ML flow (PGL-1)	OR=5.58	2.56–12.15	-	1,396
	Düppre et al.²⁹	PGLI (+)	OR=3.2	1.6–6.1	-	2,135
	Barreto et al.³²	Elisa + anti-PGL-I IgM	OR=2.7	1.29–5.87	<0.01	254
	Araújo et al.⁸	Elisa anti-PGL-I positive	RR=5.688	3.2412–9.9824	-	2,992
	Araújo et al.³³	Anti-PGL-I positive	LR+=3.69/ RR=5.97	[1.67–8.16]/ [1.45–24.5]	-	104
	Santos et al.³¹	Elisa positive anti-PGL-I IgM^a	OR=4.04	1.24–13.21	p=0.020	210
	TiemiNagao-Dias et al.²³	PGL-1 positive in contacts from 4 to 15 years	RR=8.5	4.0–18.0	<0.05	69
Negative Mitsuda Test	Goulart et al.¹⁰	The estimated risk of disease occurrence is 6.25 times higher. for contacts with a Mitsuda result ≤7 mm	OR=0.16	0.05–0.46	-	1,396
Negative Mitsuda Test	Sarno et al.⁷	Mitsuda reaction negative	OR=3.093	1.735–5.514	<0.001	-
Positive PCR in blood	Reis et al.³⁶	ML0024 qPCR positivity	OR=14.78	3.6–60.8	<0.0001	826
	Araújo et al.³³	Positive qPCR in blood samples	RR/LR+=5.54	1.30–23.62	-	104
	Santos et al.³¹	qPCR in peripheral blood positive	OR=2.08	1.08–4.02	p=0.028	210
BCG scar	Goulart et al.¹⁰	The absence of BCG scar risk is 3.7 times higher for contacts without scar	OR=0.27	0.13–0.59	-	1,396
	Sarno et al.⁷	Absence of BCG scar	OR=0.380	0.215–0.672	<0.001	-
	Düppre et al.²⁹	Higher risk among unvaccinated	OR=1.8	8.3–4.6	0.03	2,135
	Düppre et al.²⁹	BCG scar in contact PGL1+	aRR=4.1	1.8–8.2	-	2,135
Age	Manta et al.²⁵	Greater than 60	HR=32.4	3.6–290.3	0.0001	2,437
	Teixeira et al.²⁶	Older than 50 years	aOR=3.11	2.03–4.76	-	4,509
	Rodrigues et al.³⁴	Under 15 years old	aOR=3.41	1.24–9.39	0.018	204
Breed (skin color)	Santos et al.³¹	Black and brown skin color (prevalent)	aOR=1.32	1.02–1.70	0.034	7,012
Breed (skin color)	Santos et al.³¹	Black and brown skin color (incidents)	aRR=1.66	1.14–2.42	0.008	6,644
Education	Santos et al.³¹	Education up to 4 years	aOR=2.18	1.42–3.35	<0.001	4,443
Education	Santos et al.³¹	4 to 10 years of schooling	aOR=1.33	0.81–2.18	-	4,443
Contact time	Santos et al.³¹	Time of living >5 years with the index case	aOR=1.48	1.02–2.15	0.041	4,443
Contact type	Durães et al.²⁸	Household contact	aOR=2.44	1.69–3.4	<0.0001	1,040
	Sales et al.¹⁵	Household contact (co-prevalents)	OR=1.33	1.02–1.73	-	6,158
	Sales et al.¹⁵	Household contact	OR=1.96	1.29–2.98	-	6,158
	Santos et al.³¹	Household contact	aOR=1.33	1.00–1.77	0.048	7,012
	Teixeira et al.²⁶	Household contact	OR=1.48	1.17–1.88	-	42,725
Consanguinity/Relationship	Durães et al.²⁷	Consanguineous	OR=2.8	1.77–7.74	-	197
	Durães et al.²⁸	First degree kinship	OR=2.42	1.75–3.35	<0.0001	1,040
	Sales et al.¹⁵	Consanguineous	OR=1.89	1.42–2.51	-	6,158
	Santos et al.³¹	Spouse, fiance and boyfriend/girlfriend (prevalent)	aOR=1.25	0.74–2.11	-	7,012
	Santos et al.³¹	Parents (prevalent)	aOR=1.69	0.97–2.96	-	7,012
	Santos et al.³¹	Brother (prevalent)	aOR=2.75	1.65-4.57	<0.001	7,012
	Santos et al.³¹	Son (prevalent)	aOR=2.00	1.18–3.39	0.01	7,012
Consanguinity/Relationship	Santos et al.³¹	Other consanguine relatives (prevalent)	aOR=1.70	0.98–2.94	-	7,012
	Santos et al.³¹	Spouse, fiancé and partner (incidents)	RR=7.53	2.51–22.57	<0.001	6,831
	Santos et al.³¹	Uncle, nephew, cousin, grandfather, and grandson	aRR=3.71	1.24–11.06	0.0019	6,831
	Santos et al.³¹	Parents (incidents)	aRR=10.93	3.48–34.27	<0.001	6,831
	Santos et al.³¹	Brother (incidents)	aRR=7.03	2.41–20.46	<0.001	6,831
	Santos et al.³¹	Son (incidents)	aRR=5.34	1.74–16.38	0.003	6,831
Index case education	Sales et al.¹⁵	Up to 4 years of schooling	OR=2.72	1.54–4.79	-	6,158
Index case education	Sales et al.¹⁵	4 to 10 years of schooling	OR=2.40	1.30–4.42	-	6,158
Bacilloscopic index of the index case	Sales et al.¹⁵	Bacillary index from one to three compared to IC with BI 0 (co-prevalents)	OR=1.79	1.19–2.17	-	6,158
	Sales et al.¹⁵	Bacillary index greater than 3 compared to IC with BI 0	OR=4.07	2.73–6.09	-	6,158
	Sales et al.¹⁵	Bacillary index from one to three compared to IC with BI 0	OR=4.30	2.12–8.71	-	6,158
	Sales et al.¹⁵	Bacillary index greater than 3 compared to IC with BI 0 (co-prevalents)	OR=7.31	3.63–14.75	-	6,158
	Santos et al.³¹	BI 0.1 to 3.0 (incidents)	aRR=3.68	1.99–6.82	<0.001	7,012
	Santos et al.³¹	BI >3 (incidents)	aRR=5.27	2.96–9.38	<0.001	7,012
	Santos et al.³¹	BI 0.1 to 3.0 (prevalent)	aRR=3.68	1.99–6.82	<0.001	6,831
	Santos et al.³¹	BI >3 (prevalent)	aRR=5.27	2,96–9.38	<0.001	6,831
Factors in children under 15 years old	Rodrigues et al.³⁴	Age: 8 to 14 years compared to individuals aged 1 to 7 years	aOR=3.41	1.24–9.39	p=0.018	204
	Rodrigues et al.³⁴	Area of residence for children under 15(rural)	aOR=2.60	1.11–6.09	0.027	204
	Rodrigues et al.³⁴	Waste disposal (without garbage collection)	aOR=7.31	191–27.98	0.004	204
	Rodrigues et al.³⁴	Family history of the disease	aOR=8.76	3.41–22.50	0	204
	Rodrigues et al.³⁴	Contact time greater than 5 years	aOR=3.36	1.45–7.78	0.005	204
	Teixeira et al.²⁶	Male	aOR=1.70	1.20–2.42	-	20,629
Combined risks	Goulart et al.¹⁰	Ml flow; Mitsuda Test; BCG Scar	OR=24.47	9.7–61.5	-	1,396
	Goulart et al.¹⁰	BCG (-) and Mitsuda(+)	OR=19.16	8.1–45.5	-	1,396
	Barreto et al.³²	Absence of BCG scar, Mitsuda <7mm, and + anti-PGL-I	RR=8.109	5.1167–12.8511	-	2,992

Protective Factors	Article	Results	Statistical results	CI (95%)	p-value	N Total
BCG scars	Goulart et al.¹⁰	One or more BCG scars	72.9% – 0.27	0.13–0.59	-	1,396
	Santos et al.³¹	Presence of BCG scar	OR=0.30	0.22–0.41	-	7,174
	Santos et al.³¹	Presence of BCG scar	0.22-0.41	0.44–0.90	-	7,174
	Araújo et al.⁸	Two or more BCG scars	RR=0.0459	0.006–0.338	-	2,992
	Gomes et al.²⁴	Two scars compared to no BCG scars	RR=0.41	0.2016–0.8319	p= 0.007	5,661
	Santos et al.³¹	One BCG scar	OR =0.41	0.18–0.98	p= 0.044	210
Positive Mitsuda Test	Araújo et al.⁸	Mitsuda reactions >7 mm compared to 0-3 mm reactions	RR= 0.1446	0.0566–0.3696	-	2,992
Education/ schooling	Teixeira et al.²⁶	No schooling or preschool	aOR=0.59	0.38–0.92	-	819