Abstract

Ongoing studies in this project concern the basic cell biology, biochemistry and molecular biology of Leishmania, a group of protozoan pathogens of humans. All Leishmania parasites undergo a cyclic developmental cycle: 1) in mammals, they transform into and multiply as obligate intracellular [amastigote] forms within the phago-lysosomal system of host macrophages and 2) in their hematophagous sandfly-vector hosts, they differentiate into, and multiply as, extracellular [promastigote] forms within the insect's alimentary tract. Various species of this organism cause over 12 million cases of human disease worldwide. In infected humans, these parasites destroy macrophages within the skin or internal organs (spleen, liver and bone marrow) causing either disfiguring ulcerative cutaneous lesions (e.g., caused by L. mexicana) or degenerative and fatal visceral disease (e.g., caused by L. donovani). Previous studies from our laboratory have established that Leishmania parasites are apically polarized secretory cells and that they constitutively secrete over 40 different soluble protein, glycoprotein and carbohydrate constituents into their growth media in vitro. Such soluble, extracellularly secreted products can readily diffuse away from these parasites and permeate their environments. In nature, these organisms reside and multiply within various aqueous micro environments in their several hosts. Since these organisms actively secrete a variety of different enzymes that could alter such host micro- environments, an understanding of the nature of these parasite enzymes seems essential. To that end, several parasite secretory enzymes are investigated toward defining their functional roles in the survival, maintenance, growth and transmission of these organisms. Further, genes encoding these proteins are being identified and characterized toward defining their expression and regulation during parasite growth, development and differentiation. Experiments involving both the in situ deletion and over-expression of such genes should demonstrate whether their encoded proteins are, in fact, essential to this parasite's survival.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Allergy and Infectious Diseases (NIAID)
Type
Intramural Research (Z01)
Project #
1Z01AI000745-02
Application #
6160743
Study Section
Special Emphasis Panel (LPD)
Project Start
Project End
Budget Start
Budget End
Support Year
2
Fiscal Year
1997
Total Cost
Indirect Cost

  Institution

Name
National Institute of Allergy and Infectious Diseases
Department
Type
DUNS #
City
State
Country
United States
Zip Code

  Publications

Steinfelder, Svenja; Andersen, John F; Cannons, Jennifer L et al. (2009) The major component in schistosome eggs responsible for conditioning dendritic cells for Th2 polarization is a T2 ribonuclease (omega-1). J Exp Med 206:1681-90
Rogers, Matthew E; Hajmova, Martina; Joshi, Manju B et al. (2008) Leishmania chitinase facilitates colonization of sand fly vectors and enhances transmission to mice. Cell Microbiol 10:1363-72
Silverman, J Maxwell; Chan, Simon K; Robinson, Dale P et al. (2008) Proteomic analysis of the secretome of Leishmania donovani. Genome Biol 9:R35
Gerald, Noel J; Coppens, Isabelle; Dwyer, Dennis M (2008) Molecular characterization and expression of a novel kinesin which localizes with the kinetoplast in the human pathogen, Leishmania donovani. Cell Motil Cytoskeleton 65:269-80
McGugan Jr, Glen C; Joshi, Manju B; Dwyer, Dennis M (2007) Identification and biochemical characterization of unique secretory nucleases of the human enteric pathogen, Entamoeba histolytica. J Biol Chem 282:31789-802
Lustig, Yaniv; Vagima, Yaron; Goldshmidt, Hanoch et al. (2007) Down-regulation of the trypanosomatid signal recognition particle affects the biogenesis of polytopic membrane proteins but not of signal peptide-containing proteins. Eukaryot Cell 6:1865-75
Joshi, Manju B; Dwyer, Dennis M (2007) Molecular and functional analyses of a novel class I secretory nuclease from the human pathogen, Leishmania donovani. J Biol Chem 282:10079-95
Yamage, Mat; Joshi, Manju B; Dwyer, Dennis M (2007) Episomally driven antisense mRNA abrogates the hyperinducible expression and function of a unique cell surface class I nuclease in the primitive trypanosomatid parasite, Crithidia luciliae. J Mol Biol 373:296-307
Gerald, Noel J; Coppens, Isabelle; Dwyer, Dennis M (2007) Molecular dissection and expression of the LdK39 kinesin in the human pathogen, Leishmania donovani. Mol Microbiol 63:962-79
Marotta, Diane E; Gerald, Noel; Dwyer, Dennis M (2006) Rab5b localization to early endosomes in the protozoan human pathogen Leishmania donovani. Mol Cell Biochem 292:107-17

Showing the most recent 10 out of 23 publications