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GapIII, a new brain‐enriched member of the GTPase‐activating protein family
Author(s) -
Baba H.,
Fuss B.,
Urano J.,
Poullet P.,
Watson J. B.,
Tamanoi F.,
Macklin W. B.
Publication year - 1995
Publication title -
journal of neuroscience research
Language(s) - English
Resource type - Journals
SCImago Journal Rank - 1.72
H-Index - 160
eISSN - 1097-4547
pISSN - 0360-4012
DOI - 10.1002/jnr.490410615
Subject(s) - neurofibromin 1 , biology , gtpase activating protein , gtpase , mutant , c2 domain , microbiology and biotechnology , protein family , amino acid , heat shock protein , g protein , biochemistry , gene , signal transduction , membrane
Ras GTPase‐activating proteins (GAPs) are negative regulators of ras, which controls proliferation and differentiation in many cells. Ras GAPs have been found in a variety of species from yeast to mammals. We describe here a newly identified mammalian GAP, GapIII, which was obtained by differential screening of a rat oligodendrocyte cDNA library. GapIII putatively encodes a 834 amino acid protein with a predicted molecular weight of 96 kDa, which contains a consensus GAP‐related domain (GRD). The protein encoded by this cDNA has high homology with Gap1 m , which was recently identified as a putative mammalian homolog of Drosophila Gapl. These proteins contain three structural domains, an N‐terminal calcium‐dependent phospholipid binding domain, GRD, and a C‐terminal PH/Btk domain. Because of the sequence homology and the structural similarities of this protein with Gapl m , we hypothesize that GapIII and Gap1 m may be members of a mammalian GAP gene family, separate from p120GAP, neurofibromin (NF1), and IQGAP. To confirm the GapIII protein activity, constructs containing different GapIII‐GRD domains were transformed into iral mutant yeast to determine their relative ability to replace IRA1 functionally. Constructs that contained essentially the full‐length protein (all three domains), the GRD alone, or the GRD plus PH/Btk domain suppressed heat shock sensitivity of iral, whereas constructs that contained the GRD with part of the PH/Btk domain had only a weak ability to suppress heat shock sensitivity. These results suggest that the GapIII GRD itself is sufficient to down‐regulate ras proteins in yeast. Expression of GapIII mRNA (4.2 kb) was examined by Northern analysis and in situ hybridization. This mRNA was expressed at highest levels in the brain, where its expression increased with development. Lower levels of the mRNA were expressed in the spleen and lung. Among neural cells, GapIII mRNA was expressed in neurons and oligodendrocytes, but not in astrocytes. Interestingly, the expression pattern in brain is reminiscent of type 1 NF1 expression reported by Gutmann et al. (Cell Growth Differ in press, 1995). We propose that in addition to p120GAP and neurofibromin, the GapIII/Gapl m family may be important for modulating ras activity in neurons and oligodendrocytes during normal brain development and in particular in the adult brain. © 1995 Wiley‐Liss, Inc.