Tyrosine kinase-stimulated guanine nucleotide exchange activity of vav in T cell activation

Erich Gulbins; K. Mark Coggeshall; Gottfried Baier; Shulamit Katzav; Paul Burn; Amnon Altman

Tyrosine kinase-stimulated guanine nucleotide exchange activity of vav in T cell activation

Erich Gulbins^*, K. Mark Coggeshall, Gottfried Baier, Shulamit Katzav, Paul Burn, Amnon Altman

^*Corresponding author for this work

Research output: Contribution to journal › Article › peer-review

276 Scopus citations

Abstract

The hematopoietically expressed product of the vav proto-oncogene, Vav, shares homology with guanine nucleotide releasing factors (GRFs) [also called guanosine diphosphate-dissociatkKi stimulators (GDSs)] that activate Ras-related small guanosine triphosphate (GTP)-binding proteins. Human T cell lysates or Vav immunoprecipitates possessed GRF activity that increased after T cell antigen receptor (TCR)-CD3 triggering; an in vitro-translated Vav fragment that contained the putative GRF domain was also active. Vav-associated GRF stimulation after TCR-CD3 ligation paralleled its tyrosine phosphorylation; both were blocked by a protein tyrosine kinase (PTK) inhibitor. Vav also was a substrate for the p56^lck PTK. Thus, Vav is a PTK-regulated GRF that may be important in TCR-CD3-initiated signal transduction through the activation of Ras.

Original language	English
Pages (from-to)	822-825
Number of pages	4
Journal	Science
Volume	260
Issue number	5109
State	Published - 1993
Externally published	Yes

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title = "Tyrosine kinase-stimulated guanine nucleotide exchange activity of vav in T cell activation",

abstract = "The hematopoietically expressed product of the vav proto-oncogene, Vav, shares homology with guanine nucleotide releasing factors (GRFs) [also called guanosine diphosphate-dissociatkKi stimulators (GDSs)] that activate Ras-related small guanosine triphosphate (GTP)-binding proteins. Human T cell lysates or Vav immunoprecipitates possessed GRF activity that increased after T cell antigen receptor (TCR)-CD3 triggering; an in vitro-translated Vav fragment that contained the putative GRF domain was also active. Vav-associated GRF stimulation after TCR-CD3 ligation paralleled its tyrosine phosphorylation; both were blocked by a protein tyrosine kinase (PTK) inhibitor. Vav also was a substrate for the p56lck PTK. Thus, Vav is a PTK-regulated GRF that may be important in TCR-CD3-initiated signal transduction through the activation of Ras.",

author = "Erich Gulbins and Coggeshall, {K. Mark} and Gottfried Baier and Shulamit Katzav and Paul Burn and Amnon Altman",

year = "1993",

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T1 - Tyrosine kinase-stimulated guanine nucleotide exchange activity of vav in T cell activation

AU - Gulbins, Erich

AU - Coggeshall, K. Mark

AU - Baier, Gottfried

AU - Katzav, Shulamit

AU - Burn, Paul

AU - Altman, Amnon

PY - 1993

Y1 - 1993

N2 - The hematopoietically expressed product of the vav proto-oncogene, Vav, shares homology with guanine nucleotide releasing factors (GRFs) [also called guanosine diphosphate-dissociatkKi stimulators (GDSs)] that activate Ras-related small guanosine triphosphate (GTP)-binding proteins. Human T cell lysates or Vav immunoprecipitates possessed GRF activity that increased after T cell antigen receptor (TCR)-CD3 triggering; an in vitro-translated Vav fragment that contained the putative GRF domain was also active. Vav-associated GRF stimulation after TCR-CD3 ligation paralleled its tyrosine phosphorylation; both were blocked by a protein tyrosine kinase (PTK) inhibitor. Vav also was a substrate for the p56lck PTK. Thus, Vav is a PTK-regulated GRF that may be important in TCR-CD3-initiated signal transduction through the activation of Ras.

AB - The hematopoietically expressed product of the vav proto-oncogene, Vav, shares homology with guanine nucleotide releasing factors (GRFs) [also called guanosine diphosphate-dissociatkKi stimulators (GDSs)] that activate Ras-related small guanosine triphosphate (GTP)-binding proteins. Human T cell lysates or Vav immunoprecipitates possessed GRF activity that increased after T cell antigen receptor (TCR)-CD3 triggering; an in vitro-translated Vav fragment that contained the putative GRF domain was also active. Vav-associated GRF stimulation after TCR-CD3 ligation paralleled its tyrosine phosphorylation; both were blocked by a protein tyrosine kinase (PTK) inhibitor. Vav also was a substrate for the p56lck PTK. Thus, Vav is a PTK-regulated GRF that may be important in TCR-CD3-initiated signal transduction through the activation of Ras.

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Tyrosine kinase-stimulated guanine nucleotide exchange activity of vav in T cell activation

Abstract

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