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Functional determinants of ras interference 1 mutants required for their inhbitory activity on endocytosis
Authors:Adriana Galvis
Institution:Department of Biological Sciences, Florida International University 11220 SW 8th Street, Miami, FL 33199, USA
Abstract:In this study, we initiated experiments to address the structure-function relationship of Rin1. A total of ten substitute mutations were created, and their effects on Rin1 function were examined. Of the ten mutants, four of them (P541A, E574A, Y577F, T580A) were defective in Rab5 binding, while two other Rin1 mutants (D537A, Y561F) partially interacted with Rab5. Mutations in several other residues (Y506F, Y523F, T572A, Y578F) resulted in partial loss of Rab5 function. Biochemical studies showed that six of them (D537A, P541A, Y561F, E574A, Y577F, T580A) were unable to activate Rab5 in an in vitro assay.In addition, Rin1: D537A and Rin1: Y561F mutants showed dominant inhibition of Rab5 function. Consistent with the biochemical studies, we observed that these two Rin1 mutants have lost their ability to stimulate the endocytosis of EGF, form enlarged Rab5-positive endosomes, or support in vitro endosome fusion. Based on these data, our results showed that mutations in the Vps9 domain of Rin1 lead to a loss-of-function phenotype, indicating a specific structure-function relationship between Rab5 and Rin1.
Keywords:EGF-receptor  Epidermal growth factor-receptor  Vps9  vacuolar protein sorting 9  Rin1  Ras interference 1  Gapex-5  RasGAP exchange factor Rab5  ALS2  amyotrophic lateral sclerosis 2  RAP-6  Rab5 Activator Protein-6  EEA1/NT  Early Endosomal Antigen 1/N-terminus  VARP  Vps9 ankyrin repeat protein  STAM  signal transduction adaptor molecule  HRP  horseradish peroxidase  RME6  Receptor mediated endocyosis 6
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