Abstract

Human infection with species of the Leishmania genus causes a wide range of disease manifestationsranging from asymptomatic infection to clinical leishmaniasis, which can be severe and even fatal. In Brazil,Leishmania braziliensis is the most frequent species causing cutaneous leishmaniasis and its more severeform mucosal leishmaniasis, whereas Leishmania chagasi is responsible for visceral leishmaniasis. Theoutcome of either L. braziliensis and L. chagasi infections can include self-resolution, or they can evolve intoclinically apparent and severe disease. Mucosal leishmaniasis patients have a biased immune response toparasite antigens manifested by high TNF-oc and IFN-y but low IL-10 production, and decreasedresponsiveness to suppression by IL-10 and TGF-p. In contrast, VL patients present with high levels of IL-10and TNF-a and low levels of INF-y The major goals of this project are to identify genes involved insusceptibility/resistance to distinct clinical forms of leishmaniasis.
The specific aims of this project are: (1) Tostrengthen linkage findings of VL population. New multiplex will be used for fine mapping studies to localizethe genes, supplemented by family based association analysis that incorporates information from simplexfamilies. (2) To expand candidate genes and their role in determining risk of ML among families ascertainedthrough cutaneous or mucosal leishmaniasis cases (3.) To examine autosomal SNP markers genotyped forthis project in addition to markers on the Y chromosome and mitochondrial DNA in families with mucosal,cutaneous and visceral leishmaniasis to assess the extent of genetic admixture in these populations. We willincorporate this admixture information into the analytical strategy. Since the general Brazilian population is amixture of three major racial groups (European, African and Amerindian), formal admixture analysis shouldprovide a better test for genes controlling risk to different clinical outcomes of Leishmania infection. Wehope at the end of the study to have a better understanding of innate human immune factors involved indetermining the severity of disease due to the Leishmania species. Such knowledge may reveal arms of theimmune system that are important for cure.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Allergy and Infectious Diseases (NIAID)
Type
Specialized Center (P50)
Project #
2P50AI030639-16
Application #
7284025
Study Section
Special Emphasis Panel (ZAI1-GSM-M (J1))
Project Start
2007-07-01
Project End
2012-06-30
Budget Start
2008-07-01
Budget End
2009-06-30
Support Year
16
Fiscal Year
2008
Total Cost
$188,710
Indirect Cost

  Institution

Name
Federal University of Bahia
Department
Type
DUNS #
900845397
City
Salvador
State
Country
Brazil
Zip Code
40110-160

  Publications

Sousa, Rosana; Andrade, Viviane M; Bair, Thomas et al. (2018) Early Suppression of Macrophage Gene Expression by Leishmania braziliensis. Front Microbiol 9:2464
Silva, Silvana C; Guimarães, Luiz Henrique; Silva, Juliana A et al. (2018) Molecular epidemiology and in vitro evidence suggest that Leishmania braziliensis strain helps determine antimony response among American tegumenary leishmaniasis patients. Acta Trop 178:34-39
Teixeira, D G; Monteiro, G R G; Martins, D R A et al. (2017) Comparative analyses of whole genome sequences of Leishmania infantum isolates from humans and dogs in northeastern Brazil. Int J Parasitol 47:655-665
Lima, Josivan Gomes; Nobrega, Lucia Helena C; Lima, Natalia Nobrega et al. (2017) Normal bone density and trabecular bone score, but high serum sclerostin in congenital generalized lipodystrophy. Bone 101:21-25
Lima, Ádila L M; de Lima, Iraci D; Coutinho, José F V et al. (2017) Changing epidemiology of visceral leishmaniasis in northeastern Brazil: a 25-year follow-up of an urban outbreak. Trans R Soc Trop Med Hyg 111:440-447
Kelly, Patrick H; Bahr, Sarah M; Serafim, Tiago D et al. (2017) The Gut Microbiome of the Vector Lutzomyia longipalpis Is Essential for Survival of Leishmania infantum. MBio 8:
Gimblet, Ciara; Meisel, Jacquelyn S; Loesche, Michael A et al. (2017) Cutaneous Leishmaniasis Induces a Transmissible Dysbiotic Skin Microbiota that Promotes Skin Inflammation. Cell Host Microbe 22:13-24.e4
Almeida, Lucas; Silva, Juliana A; Andrade, Viviane M et al. (2017) Analysis of expression of FLI1 and MMP1 in American cutaneous leishmaniasis caused by Leishmania braziliensis infection. Infect Genet Evol 49:212-220
Weirather, Jason L; Duggal, Priya; Nascimento, Eliana L et al. (2017) Comprehensive candidate gene analysis for symptomatic or asymptomatic outcomes of Leishmania infantum infection in Brazil. Ann Hum Genet 81:41-48
Novais, Fernanda O; Carvalho, Augusto M; Clark, Megan L et al. (2017) CD8+ T cell cytotoxicity mediates pathology in the skin by inflammasome activation and IL-1? production. PLoS Pathog 13:e1006196

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