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GAPs: Terminator versus effector functions and the role(s) of ArfGAP1 in vesicle biogenesis

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Last modified
  • 02/20/2025
Type of Material
Authors
    Richard A Kahn, Emory University
Language
  • English
Date
  • 2011-03
Publisher
  • Landes Bioscience
Publication Version
Copyright Statement
  • © 2011 Landes Bioscience
License
Final Published Version (URL)
Title of Journal or Parent Work
ISSN
  • 2159-2780
Volume
  • 1
Issue
  • 2
Start Page
  • 49
End Page
  • 51
Abstract
  • Whether your passion is to understand and reverse disease processes or “simply” a better understanding of how cells work, anyone wishing to understand cell regulation today must have a detailed and accurate understanding of regulatory GTPase mechanisms and their application to specific pathways. This is becoming increasingly difficult as the details of signaling by members of different families of GTPases and their regulators expand. But this is all the more reason to continually ask, which aspects of GTPase signaling are distinct to a GTPase or its subfamily and which are conserved throughout the superfamily? We each have slightly different views of the key aspects of GTPase signaling that are derived from the main GTPases studied in our own labs; e.g., translocation onto a membrane is an essential and integral aspect of Arf activation but not of other GTPases. However, one aspect of GTPase signaling that I had come to believe to be widespread and of general importance is not universally accepted. In fact, through my conversations at the recent FASEB summer research conference on “Arf Family GTPases” and reading of the literature in a graduate tutorial class, I realized that it is not known or accepted by the majority of researchers. The question is the role of GTPase activating proteins (GAPs) in signaling. Are they “pure” terminators of signaling or do they serve effector functions?
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Keywords
Research Categories
  • Chemistry, Biochemistry

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