Discovery of novel vaccine candidates and drug targets against visceral leishmaniasis using proteomics and transcriptomics.

Shraddha Kumari, Awanish Kumar, Mukesh Samant, Neeloo Singh, Anuradha Dube

Division of Parasitology, Central Drug Research Institute, Post Box No. 173, Lucknow-226 001, India. .

Journal Article: Current drug targets (impact factor: 3.93). 12/2008; 9(11):938-47.

Abstract

Among the three clinical forms (cutaneous, mucosal and visceral) of leishmaniasis visceral (VL) one is the most devastating type caused by the invasion of the reticuloendothelial system of human by Leishmania donovani, L. infantum and L. chagasi. India and Sudan account for about half the world's burden of VL. Current control strategy is based on chemotherapy, which is difficult to administer, expensive and becoming ineffective due to the emergence of drug resistance. An understanding of resistance mechanism(s) operating in clinical isolates might provide additional leads for the development of new drugs. Further, due to the lack of fully effective treatment the search for novel immune targets is also needed. So far, no vaccine exists for VL despite indications of naturally developing immunity. Therefore, an urgent need for new and effective leishmanicidal agents and for this identification of novel drug and vaccine targets is imperative. The availability of the complete genome sequence of Leishmania has revolutionised many areas of leishmanial research and facilitated functional genomic studies as well as provided a wide range of novel targets for drug designing. Most notably, proteomics and transcriptomics have become important tools in gaining increased understanding of the biology of Leishmania to be explored on a global scale, thus accelerating the pace of discovery of vaccine/drug targets. In addition, these approaches provide the information regarding genes and proteins that are expressed and under which conditions. This review provides a comprehensive view about those proteins/genes identified using proteomics and transcriptomic tools for the development of vaccine/drug against VL.

Source: PubMed

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Keywords

complete genome sequence
 
Current control strategy
 
drug resistance
 
effective leishmanicidal agents
 
effective treatment
 
facilitated functional genomic studies
 
L. infantum
 
leishmanial research
 
leishmaniasis visceral
 
new drugs
 
novel drug
 
novel immune targets
 
novel targets
 
proteins/genes
 
resistance mechanism(s)
 
three clinical forms
 
transcriptomic tools
 
vaccine targets
 
vaccine/drug
 
vaccine/drug targets