Preclinical validation of a live attenuated dermotropic Leishmania vaccine against vector transmitted fatal visceral leishmaniasis

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作者
Subir Karmakar
Nevien Ismail
Fabiano Oliveira
James Oristian
Wen Wei Zhang
Swarnendu Kaviraj
Kamaleshwar P. Singh
Abhishek Mondal
Sushmita Das
Krishna Pandey
Parna Bhattacharya
Greta Volpedo
Sreenivas Gannavaram
Monika Satoskar
Sanika Satoskar
Rajiv M. Sastry
Timur Oljuskin
Telly Sepahpour
Claudio Meneses
Shinjiro Hamano
Pradeep Das
Greg Matlashewski
Sanjay Singh
Shaden Kamhawi
Ranadhir Dey
Jesus G. Valenzuela
Abhay Satoskar
Hira L. Nakhasi
机构
[1] FDA,Division of Emerging and Transfusion Transmitted Diseases, CBER
[2] NIH,Vector Molecular Biology Section, Laboratory of Malaria and Vector Research, National Institute of Allergy and Infectious Diseases
[3] McGill University,Department of Microbiology and Immunology
[4] Hinjawadi Phase II,Gennova Biopharmaceuticals
[5] Rajendra Memorial Research Institute of Medical Sciences,Department of Pathology and Microbiology
[6] Ohio State University,Department of Parasitology, Institute of Tropical Medicine (NEKKEN)
[7] Nagasaki University,The Joint Usage/Research Center on Tropical Disease, Institute of Tropical Medicine (NEKKEN)
[8] Nagasaki University,undefined
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摘要
Visceral Leishmaniasis (VL), a potentially fatal disease is caused by Leishmania donovani parasites with no vaccine available. Here we produced a dermotropic live attenuated centrin gene deleted Leishmania major (LmCen−/−) vaccine under Good Laboratory Practices and demonstrated that a single intradermal injection confers robust and durable protection against lethal VL transmitted naturally via bites of L. donovani-infected sand flies and prevents mortality. Surprisingly, immunogenicity characteristics of LmCen−/− parasites revealed activation of common immune pathways like L. major wild type parasites. Spleen cells from LmCen−/− immunized and L. donovani challenged hamsters produced significantly higher Th1-associated cytokines including IFN-γ, TNF-α, and reduced expression of the anti-inflammatory cytokines like IL-10, IL-21, compared to non-immunized challenged animals. PBMCs, isolated from healthy people from non-endemic region, upon LmCen−/− infection also induced more IFN-γ compared to IL-10, consistent with our immunogenicity data in LmCen−/− immunized hamsters. This study demonstrates that the LmCen−/− parasites are safe and efficacious against VL and is a strong candidate vaccine to be tested in a human clinical trial.
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