BaseSpace
Correlation Engine 2.0
Import Your Data
Literature

FAQ

More FAQs

Back to top
Clear Search sequence regions
(e.g. Apoptosis, HIV infection, Embryo, Biofuel, Phenobarbital, rs6983267, PBX1)
Bookmark Forward

Functional cross-talk between ras and rho pathways: a Ras-specific GTPase-activating protein (p120RasGAP) competitively inhibits the RhoGAP activity of deleted in liver cancer (DLC) tumor suppressor by masking the catalytic arginine finger.

Mamta Jaiswal, Radovan Dvorsky, Ehsan Amin, Sarah L Risse, Eyad K Fansa, Si-Cai Zhang, Mohamed S Taha, Aziz R Gauhar, Saeideh Nakhaei-Rad, Claus Kordes, Katja T Koessmeier, Ion C Cirstea, Monilola A Olayioye, Dieter Häussinger, Mohammad R Ahmadian

The Journal of biological chemistry 2014 Mar 07


filter terms:
  • cancer genes (1)
  • GTP (1)
  • gtpase (5)
  • humans (1)
  • isoforms (1)
  • liver cancer (5)
  • p120 (6)
  • p120rasgap (2)
  • protein human (1)
  • ras (3)
  • ras proteins (2)
  • ras- gap (1)
  • rho GTPase (2)
  • RhoGAP (11)
  • RhoGAP proteins (1)
  • SH3 (1)
  • sh3 domain (3)
  • tumor suppressor (2)
  • tumor suppressor proteins (2)
    • Sizes of these terms reflect their relevance to your search.

    The three deleted in liver cancer genes (DLC1-3) encode Rho-specific GTPase-activating proteins (RhoGAPs). Their expression is frequently silenced in a variety of cancers. The RhoGAP activity, which is required for full DLC-dependent tumor suppressor activity, can be inhibited by the Src homology 3 (SH3) domain of a Ras-specific GAP (p120RasGAP). Here, we comprehensively investigated the molecular mechanism underlying cross-talk between two distinct regulators of small GTP-binding proteins using structural and biochemical methods. We demonstrate that only the SH3 domain of p120 selectively inhibits the RhoGAP activity of all three DLC isoforms as compared with a large set of other representative SH3 or RhoGAP proteins. Structural and mutational analyses provide new insights into a putative interaction mode of the p120 SH3 domain with the DLC1 RhoGAP domain that is atypical and does not follow the classical PXXP-directed interaction. Hence, p120 associates with the DLC1 RhoGAP domain by targeting the catalytic arginine finger and thus by competitively and very potently inhibiting RhoGAP activity. The novel findings of this study shed light on the molecular mechanisms underlying the DLC inhibitory effects of p120 and suggest a functional cross-talk between Ras and Rho proteins at the level of regulatory proteins.

    Citation

    Mamta Jaiswal, Radovan Dvorsky, Ehsan Amin, Sarah L Risse, Eyad K Fansa, Si-Cai Zhang, Mohamed S Taha, Aziz R Gauhar, Saeideh Nakhaei-Rad, Claus Kordes, Katja T Koessmeier, Ion C Cirstea, Monilola A Olayioye, Dieter Häussinger, Mohammad R Ahmadian. Functional cross-talk between ras and rho pathways: a Ras-specific GTPase-activating protein (p120RasGAP) competitively inhibits the RhoGAP activity of deleted in liver cancer (DLC) tumor suppressor by masking the catalytic arginine finger. The Journal of biological chemistry. 2014 Mar 07;289(10):6839-6849

    Expand section icon Mesh Tags

    Expand section icon Substances


    PMID: 24443565

    View Full Text
    • Copyright © 2024 Illumina Inc. All rights reserved.