Digestive vacuole biogenesis in the malaria parasite
Project Number7F32AI066826-03
Former Number5F32AI066826-03
Contact PI/Project LeaderLEE, MARCUS C
Awardee OrganizationCOLUMBIA UNIVERSITY HEALTH SCIENCES
Description
Abstract Text
DESCRIPTION (provided by applicant): This application aims to understand the biogenesis of the digestive vacuole (DV) of the malaria parasite, Plasmodium falciparum. This acidic, lysosomal-like organelle is responsible for the degradation of large quantities of hemoglobin ingested from the host erythrocyte. The DV is also the site of action of the largest and historically the most clinically useful family of antimalarial drugs, the 4-aminoquinolines. Despite the importance of this organelle to parasite development and antimalarial chemotherapy, little is currently known about how both biosynthetic parasite proteins and components of the host cell cytosol are delivered to the DV during the intraerythrocytic lifecycle. I propose to determine which trafficking steps are essential for the transport of parasite and host cell proteins to the DV by genetic and chemical disruption of defined stages of intracellular transport. These studies will enable us to address the hypothesis that one pathway of parasite protein trafficking to the DV relies upon the Sec and Vps components of protein secretion and sorting. Our second major hypothesis is that uptake of hemoglobin and some host erythrocyte cytosol components proceeds via dynamin-dependent endocytosis.
Public Health Relevance Statement
Data not available.
NIH Spending Category
No NIH Spending Category available.
Project Terms
4-aminoquinolineAblationAddressAmino AcidsAntimalarialsApplied GeneticsBiogenesisBiological AssayCatabolismCell membraneCellsChemicalsChloroquineChloroquine resistanceCytosolDefectDevelopmentDisruptionDrug Metabolic DetoxicationDynaminEndocytosisEndopeptidasesErythrocytesEventFamilyFellowshipFluorescence MicroscopyGenesGeneticGenomeHemeHemoglobinHumanIndividualInfectionIngestionIntracellular TransportMalariaMediatingMembraneMembrane ProteinsMethodsNamesOrganellesOrthologous GeneOxidative StressParasitesPathway interactionsPeptide HydrolasesPhysiologic pulsePlasmodiumPlasmodium falciparumPoint MutationProtein SecretionProteinsPulse takingQuinineRoleRouteSiteSorting - Cell MovementStagingSuperoxide DismutaseTestingVacuolar Protein SortingVacuoleYeastschemical geneticschemotherapyhistidine-rich proteinsinsightintracellular protein transportloss of functionplasmepsinprotein transportresearch studytraffickinguptakeyeast protein
National Institute of Allergy and Infectious Diseases
CFDA Code
855
DUNS Number
621889815
UEI
QHF5ZZ114M72
Project Start Date
20-July-2005
Project End Date
19-July-2008
Budget Start Date
20-July-2007
Budget End Date
19-July-2008
Project Funding Information for 2007
Total Funding
$58,036
Direct Costs
$58,036
Indirect Costs
Year
Funding IC
FY Total Cost by IC
2007
National Institute of Allergy and Infectious Diseases
$58,036
Year
Funding IC
FY Total Cost by IC
Sub Projects
No Sub Projects information available for 7F32AI066826-03
Publications
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The Project Outcomes shown here are displayed verbatim as submitted by the Principal Investigator (PI) for this award. Any opinions, findings, and conclusions or recommendations expressed are those of the PI and do not necessarily reflect the views of the National Institutes of Health. NIH has not endorsed the content below.
No Outcomes available for 7F32AI066826-03
Clinical Studies
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