Regulation of Btk function by a major autophosphorylation site within the SH3 domain

被引：262

作者：

Park, H

Wahl, MI

Afar, DEH

Turck, CW

Rawlings, DJ

Tam, C

Scharenberg, AM

Kinet, JP

Witte, ON

机构：

[1] UNIV CALIF LOS ANGELES, CEDARS SINAI MED GENET TRAINING PROGRAM, LOS ANGELES, CA 90048 USA

[2] UNIV CALIF SAN FRANCISCO, HOWARD HUGHES MED INST, DEPT MED, CARDIOVASC RES INST, SAN FRANCISCO, CA 94143 USA

[3] BETH ISRAEL HOSP, LAB ALLERGY & IMMUNOL, BOSTON, MA 02215 USA

[4] HARVARD UNIV, SCH MED, BOSTON, MA 02215 USA

[5] HOWARD HUGHES MED INST, LOS ANGELES, CA 90095 USA

[6] UNIV CALIF LOS ANGELES, INST MOLEC BIOL, LOS ANGELES, CA 90095 USA

来源：

IMMUNITY | 1996年 / 4卷 / 05期

关键词：

D O I：

10.1016/S1074-7613(00)80417-3

中图分类号：

R392 [医学免疫学]; Q939.91 [免疫学];

学科分类号：

100102 ;

摘要：

Bruton's tyrosine kinase (Btk) plays a crucial role in B cell development. Overexpression of Btk with a Src family kinase increases tyrosine phosphorylation and catalytic activity of Btk. This occurs by transphosphorylation at Y551 in the Btk catalytic domain and the enhancement of Btk autophosphorylation at a second site. A gain-of-function mutant called Btk* containing E41 to K change within the pleckstrin homology domain induces fibroblast transformation. Btk* enhances the transphosphorylation of Y551 by endogenous Src family tyrosine kinases and autophosphorylation at the second site. We mapped the major Btk autophosphorylation site to Y223 within the SH3 domain. Mutation of Y223 to F blocks Btk autophosphorylation and dramatically potentiates the transforming activity of Btk* in fibroblasts. The location of Y223 in a potential ligand-binding pocket suggests that autophosphorylation regulates SH3-mediated signaling by Btk.

引用

页码：515 / 525

页数：11

共 57 条

[1] BRUTON TYROSINE KINASE IS TYROSINE-PHOSPHORYLATED AND ACTIVATED IN PRE-B LYMPHOCYTES AND RECEPTOR-LIGATED B-CELLS
AOKI, Y
ISSELBACHER, KJ
PILLAI, S
[J]. PROCEEDINGS OF THE NATIONAL ACADEMY OF SCIENCES OF THE UNITED STATES OF AMERICA, 1994, 91 (22) : 10606 - 10609
[2] INVOLVEMENT OF P59FYN(T) IN INTERLEUKIN-5 RECEPTOR SIGNALING
APPLEBY, MW
KERNER, JD
CHIEN, S
MALISZEWSKI, CR
BONDADAA, S
PERLMUTTER, RM
[J]. JOURNAL OF EXPERIMENTAL MEDICINE, 1995, 182 (03) : 811 - 820
[3] Boyle WJ., 1991, METHOD ENZYMOL, V201, P110
[4] CAMBIER JC, 1994, ANNU REV IMMUNOL, V12, P457, DOI 10.1146/annurev.immunol.12.1.457
[5] THE WHEN AND HOW OF SRC REGULATION
COOPER, JA
HOWELL, B
[J]. CELL, 1993, 73 (06) : 1051 - 1054
[6] THE PROTEIN PRODUCT OF THE C-CBL PROTOONCOGENE IS PHOSPHORYLATED AFTER B-CELL RECEPTOR STIMULATION AND BINDS THE SH3 DOMAIN OF BRUTONS TYROSINE KINASE
CORY, GOC
LOVERING, RC
HINSHELWOOD, S
MACCARTHYMORROGH, L
LEVINSKY, RJ
KINNON, C
[J]. JOURNAL OF EXPERIMENTAL MEDICINE, 1995, 182 (02) : 611 - 615
[7] RESTRICTION OF THE INVITRO AND INVIVO TYROSINE PROTEIN-KINASE ACTIVITIES OF PP60C-SRC RELATIVE TO PP60V-SRC
COUSSENS, PM
COOPER, JA
HUNTER, T
SHALLOWAY, D
[J]. MOLECULAR AND CELLULAR BIOLOGY, 1985, 5 (10) : 2753 - 2763
[8] MUTATION ANALYSIS OF THE BRUTONS TYROSINE KINASE GENE IN X-LINKED AGAMMAGLOBULINEMIA - IDENTIFICATION OF A MUTATION WHICH AFFECTS THE SAME CODON AS IS ALTERED IN IMMUNODEFICIENT XID MICE
DEWEERS, M
MENSINK, RGJ
KRAAKMAN, MEM
SCHUURMAN, RKB
HENDRIKS, RW
[J]. HUMAN MOLECULAR GENETICS, 1994, 3 (01) : 161 - 166
[9] MUTATIONAL ANALYSIS OF THE SRC SH3 DOMAIN - THE SAME RESIDUES OF THE LIGAND-BINDING SURFACE ARE IMPORTANT FOR INTRAMOLECULAR AND INTERMOLECULAR INTERACTIONS
ERPEL, T
SUPERTIFURGA, G
COURTNEIDGE, SA
[J]. EMBO JOURNAL, 1995, 14 (05) : 963 - 975
[10] 2 BINDING ORIENTATIONS FOR PEPTIDES TO THE SRC SH3 DOMAIN - DEVELOPMENT OF A GENERAL-MODEL FOR SH3-LIGAND INTERACTIONS
FENG, SB
CHEN, JK
YU, HT
SIMON, JA
SCHREIBER, SL
[J]. SCIENCE, 1994, 266 (5188) : 1241 - 1247

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