Abstract

The peroxisome is a ubiquitous organelle of eukaryotic cells. Peroxisome participate in a wide variety of metabolic processes and defects in peroxisome biogenesis are the cause of numerous human diseases. These lethal inherited disorders are caused by defects in the biogenesis of peroxisome membranes or peroximal matrix protein import but all patients display mislocalization of matrix enzymes and loss of virtually all peroxisomal metabolic functions. This proposal is designed to improve our understanding of these diseases by testing our current working model of peroxisomal matrix protein import. In this model, predominantly cytoplasmic, partially peroxisomal import receptors recognize newly synthesized matrix enzymes. Docking factors on the peroxisome surface recruit these receptors and, if the receptors contain newly synthesized matrix enzymes, they are transferred to a translocation apparatus. At this point, the enzymes are dissociated from their receptors and translocated into the peroxisome lumen. This model also predicts that a recycling event releases the import receptors to the cytoplasms for additional rounds of protein import.
Specific Aim 1 examines the structure and function of the import receptors.
Specific aim 2 explores the mechanisms of import that occur following recognition but prior to translocation.
Specific aim 3 investigates several peroxin- peroxin interactions that are critical for matrix protein import.
The fourth aim supports studies of peroxisomal enzyme translocation in vitro. The significance of these studies is that they will improve our understanding of eukaryotic cell biology and the molecular basis of human disease by testing our current hypothesis of peroxisomal matrix protein import.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Diabetes and Digestive and Kidney Diseases (NIDDK)
Type
Research Project (R01)
Project #
2R01DK045787-10A1
Application #
6479861
Study Section
Special Emphasis Panel (ZRG1-CDF-4 (02))
Program Officer
Haft, Carol R
Project Start
1993-08-01
Project End
2007-03-31
Budget Start
2002-04-16
Budget End
2003-03-31
Support Year
10
Fiscal Year
2002
Total Cost
$402,619
Indirect Cost

  Institution

Name
Johns Hopkins University
Department
Biochemistry
Type
Schools of Medicine
DUNS #
045911138
City
Baltimore
State
MD
Country
United States
Zip Code
21218

  Publications

Yang, Jr-Ming; Gould, Stephen J (2013) The cis-acting signals that target proteins to exosomes and microvesicles. Biochem Soc Trans 41:277-82
Gan, Xin; Gould, Stephen J (2012) HIV Pol inhibits HIV budding and mediates the severe budding defect of Gag-Pol. PLoS One 7:e29421
Shen, Beiyi; Wu, Ning; Yang, Jr-Ming et al. (2011) Protein targeting to exosomes/microvesicles by plasma membrane anchors. J Biol Chem 286:14383-95
Shen, Beiyi; Fang, Yi; Wu, Ning et al. (2011) Biogenesis of the posterior pole is mediated by the exosome/microvesicle protein-sorting pathway. J Biol Chem 286:44162-76
Gan, Xin; Gould, Stephen J (2011) Identification of an inhibitory budding signal that blocks the release of HIV particles and exosome/microvesicle proteins. Mol Biol Cell 22:817-30
Fang, Yi; Wu, Ning; Gan, Xin et al. (2007) Higher-order oligomerization targets plasma membrane proteins and HIV gag to exosomes. PLoS Biol 5:e158
Booth, Amy M; Fang, Yi; Fallon, Jonathan K et al. (2006) Exosomes and HIV Gag bud from endosome-like domains of the T cell plasma membrane. J Cell Biol 172:923-35
Erdmann, Ralf; Gould, Stephen J (2002) Visualization and purification of yeast peroxisomes. Methods Enzymol 351:365-81
Harper, Courtney C; South, Sarah T; McCaffery, J Michael et al. (2002) Peroxisomal membrane protein import does not require Pex17p. J Biol Chem 277:16498-504
Jones, J M; Morrell, J C; Gould, S J (2001) Multiple distinct targeting signals in integral peroxisomal membrane proteins. J Cell Biol 153:1141-50

Showing the most recent 10 out of 44 publications