DIFFERENTIAL BINDING OF PP60(C-SRC) AND PP60(V-SRC) TO CYTOSKELETON IS MEDIATED BY SH2 AND CATALYTIC DOMAINS

The transforming protein of Rous sarcoma virus, pp60(v-src), and its n ormal cellular homolog, pp60(c-src), differ not only in oncogenic pote ntial but also in their subcellular localization and cytoskeletal bind ing ability. pp60(v-src) has been shown to stably associate with a det ergent-insoluble cytoskeletal matrix, whereas pp60(c-src) does not. We have generated a series of precise deletion and truncations of the Sr c homology domains within pp60(v-src) and pp60(c-src), based on the cr ystal and solution structures of these regions, to determine not only the region responsible for cytoskeletal association but also the mecha nism accounting for the differential binding observed. Here we show th at the SH2 domain, but not the SH3 domain, mediates cytoskeletal assoc iation of pp60(v-src) through a phosphotyrosine-dependent interaction. The ability to interact with the cytoskeletal matrix is regulated by the catalytic (SH1) domain. Truncation of the pp60(v-src) catalytic do main results in lower binding while removal of the catalytic domain of pp60(c-src) results in the acquisition of cytoskeletal binding simila r to that of the analogous v-src construct. These results indicate tha t the SH2 and catalytic domains function coordinately to regulate the cytoskeletal association of pp60(v-src) and pp60(c-src).