Awardee OrganizationBETH ISRAEL DEACONESS MEDICAL CENTER
Description
Abstract Text
Lymphatic filariasis remains a major global health problem. Little is
known about parasite pathogenicity and modulation of host immune responses
in human filarial infections. In particular, interactions between
bloodborne microfilariae and host blood cells, including platelets,
leukocytes, and endothelial cells, are largely unexplored. In mammalian
cells, arachidonic acid is metabolized to eicosanoids, biologically active
lipid derivatives that mediate a wide range of inflammatory and immune
responses. Brugia malayi, a filarial parasite of humans, avidly
incorporates arachidonic acid and cal also metabolize arachidonic acid to
eicosanoids in vitro. Such parasite-derived eicosanoids could present
newly recognized mediators of the in vivo interactions between
microfilariae and host cells.
The major training goal of this Physician Scientist Award is to provide the
physician-applicant with training in concepts and methods of the basic
sciences relevant to the study of metazoan parasites, in order to provide
him with a solid foundation for developing an independent research career.
The major research goals of this proposal are to elucidate the biosynthesis
of eicosanoids in B. malayi microfilariae and their roles in mediating
interactions between these parasites and host blood cells.
Phase I of the Award will emphasize training in research methods as well as
coursework and seminars in biochemistry, cell biology, and immunology.
Studies of microfilarial eicosanoid production will be continued using
sensitive techniques of HPLC, TLC, and RIA to detect parasite products of
arachidonic acid metabolism. This phase will also provide intensive
training in analytical biochemistry techniques, including gas
chromatography - mass spectroscopy, to structurally characterize unknown
and novel parasite-derived eicosanoids. In Phase II, these techniques will
be applied and expanded to study the effects of microfilarial eicosanoids
on human blood cells, including leukocytes, platelets, and endothelial
cells. The effects of diethylcarbamazine, the major antifilarial drug, and
other pharmacologic inhibitors of mammalian eicosanoid biosynthesis on the
biosynthesis and actions of microfilarial eicosanoids will also be
assessed.
These investigations will help to define the role of parasite-derived
eicosanoids in the pathogenesis and immunology of human filariasis. While
these studies are focused on filarial parasites, other metazoan parasites
are likely to possess similar capabilities to form bioactive lipids.
Rigorous studies of parasite-derived eicosanoids may provide new insights
in the molecular means by which metazoan parasites elude natural or
vaccine-induced immunity. Such understanding may influence the development
of useful drugs and synthetic vaccines to control important metazoan
parasites. The educational and training components of this Award will
provide the applicant with the scientific expertise that will enable his to
successfully pursue basic studies of host-parasite interactions as an
independent investigator.
National Institute of Allergy and Infectious Diseases
CFDA Code
DUNS Number
071723621
UEI
C1CPANL3EWK4
Project Start Date
01-August-1990
Project End Date
31-July-1995
Budget Start Date
01-August-1993
Budget End Date
31-July-1994
Project Funding Information for 1993
Total Funding
$87,804
Direct Costs
$81,300
Indirect Costs
$6,504
Year
Funding IC
FY Total Cost by IC
1993
National Institute of Allergy and Infectious Diseases
$87,804
Year
Funding IC
FY Total Cost by IC
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