CrkL directs ASAP1 to peripheral focal adhesions |
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| Authors: | Oda Atsushi Wada Ikuo Miura Koichi Okawa Katsuya Kadoya Toshihiko Kato Takashi Nishihara Hiroshi Maeda Masae Tanaka Shinya Nagashima Kazuo Nishitani Chiaki Matsuno Kazuhiko Ishino Masaho Machesky Laura M Fujita Hiroyoshi Randazzo Paul |
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| Affiliation: | Laboratory of Environmental Biology, Department of Preventive Medicine, Hokkaido University School of Medicine, Sapporo 060-8638, Japan. aoda@med.hokudai.ac.jp |
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| Abstract: | Searching for proteins in platelets that can interact with the N-terminal SH3 domain of CrkL (using a combination of a pull-down assay followed by mass spectrometry), we have found that human platelets express an ADP-ribosylation factor (Arf)-specific GTPase-activating protein (GAP), ASAP1, as a CrkL-binding protein. In spreading platelets, most endogenous ASAP1 is localized at peripheral focal adhesions. To determine the physiologic significance of the CrkL-ASAP1 association, we overexpressed CrkL, ASAP1, or both in combination in COS7 cells. Unlike endogenous ASAP1 in platelets, overexpressed ASAP1 showed diffuse cytoplasmic distribution. However, when co-expressed with wild-type CrkL, both endogenous and expressed ASAP1 accumulated at CrkL-induced focal adhesions. An SH2-mutated CrkL, which cannot localize at focal adhesions, failed to recruit ASAP1 into focal adhesions. Thus, CrkL appears to be a lynchpin between ASAP1 and peripheral focal adhesions. |
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