ملخص
We recently identified intersectin, a protein containing two EH and five SH3 domains, as a component of the endocytic machinery. The N-terminal SH3 domain (SH3A), unlike other SH3 domains from intersectin or various endocytic proteins, specifically inhibits intermediate events leading to the formation of clathrin-coated pits. We have now identified a brain-enriched, 170 kDa protein (p170) that interacts specifically with SH3A. Screening of combinatorial peptides reveals the optimal ligand for SH3A as Pp(V/I)PPR, and the 170 kDa mammalian son-of-sevenless (mSos1) protein, a guanine-nucleotide exchange factor for Ras, contains two copies of the matching sequence, PPVPPR. Immunodepletion studies confirm that p170 is mSos1. Intersectin and mSos1 are co-enriched in nerve terminals and are co-immunoprecipitated from brain extracts. SH3A competes with the SH3 domains of Grb2 in binding to mSos1, and the intersectin-mSos1 complex can be separated from Grb2 by sucrose gradient centrifugation. Overexpression of the SH3 domains of intersectin blocks epidermal growth factor-mediated Ras activation. These results suggest that intersectin functions in cell signaling in addition to its role in endocytosis and may link these cellular processes.
| اللغة الأصلية | الإنجليزيّة |
|---|---|
| الصفحات (من إلى) | 1263-1271 |
| عدد الصفحات | 9 |
| دورية | EMBO Journal |
| مستوى الصوت | 19 |
| رقم الإصدار | 6 |
| المعرِّفات الرقمية للأشياء | |
| حالة النشر | نُشِر - 15 مارس 2000 |
| منشور خارجيًا | نعم |
بصمة
أدرس بدقة موضوعات البحث “The endocytic protein intersectin is a major binding partner for the Ras exchange factor mSos1 in rat brain'. فهما يشكلان معًا بصمة فريدة.قم بذكر هذا
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