Afar D E, Park H, Howell B W, Rawlings D J, Cooper J, Witte O N
Department of Microbiology, Howard Hughes Medical Institute, University of California--Los Angeles, 90095-1662, USA.
Mol Cell Biol. 1996 Jul;16(7):3465-71. doi: 10.1128/MCB.16.7.3465.
Loss of function of Bruton's tyrosine kinase (Btk) results in X-linked immunodeficiencies characterized by a broad spectrum of signaling defects, including those dependent on Src family kinase-linked cell surface receptors. A gain-of-function mutant, Btk*, induces the growth of fibroblasts in soft agar and relieves the interleukin-5 dependence of a pre-B-cell line. To genetically define Btk signaling pathways, we used a strategy to either activate or inactivate Src family kinases in fibroblasts that express Btk*. The transformation potential of Btk* was dramatically increased by coexpression with a partly activated c-Src mutant (E-378 --> G). This synergy was further potentiated by deletion of the Btk Src homology 3 domain. Downregulation of Src family kinases by the C-terminal Src kinase (Csk) suppressed Btk* activation and biological potency. In contrast, kinase-inactive Csk (K-222 --> R), which functioned as a dominant negative molecule, synergized with Btk* in biological transformation. Activation of Btk* correlated with increased phosphotyrosine on transphosphorylation and autophosphorylation sites. These findings suggest that the Src and Btk kinase families form specific signaling units in tissues in which both are expressed.
布鲁顿酪氨酸激酶(Btk)功能丧失会导致X连锁免疫缺陷,其特征为广泛的信号缺陷,包括那些依赖于Src家族激酶连接的细胞表面受体的缺陷。一种功能获得性突变体Btk可诱导成纤维细胞在软琼脂中生长,并减轻前B细胞系对白介素-5的依赖性。为了从基因上定义Btk信号通路,我们采用了一种策略,即在表达Btk的成纤维细胞中激活或失活Src家族激酶。与部分激活的c-Src突变体(E-378→G)共表达可显著提高Btk的转化潜能。通过缺失Btk的Src同源3结构域,这种协同作用进一步增强。C末端Src激酶(Csk)下调Src家族激酶可抑制Btk的激活及其生物学活性。相反,作为显性负性分子发挥作用的激酶失活型Csk(K-222→R)在生物学转化中与Btk协同作用。Btk的激活与转磷酸化和自磷酸化位点上磷酸酪氨酸的增加相关。这些发现表明,Src和Btk激酶家族在两者均表达的组织中形成特定的信号单元。
