Division of Molecular Biology and Biochemistry, School of Biological Sciences, University of Missouri-Kansas City, Kansas City, MO, USA.
Cell Adh Migr. 2012 Jul-Aug;6(4):356-64. doi: 10.4161/cam.21242. Epub 2012 Jul 1.
There is general agreement that many cancers are associated with aberrant phosphotyrosine signaling, which can be caused by the inappropriate activities of tyrosine kinases or tyrosine phosphatases. Furthermore, incorrect activation of signaling pathways has been often linked to changes in adhesion events mediated by cell surface receptors. Among these receptors, receptor protein tyrosine phosphatases (RPTPs) both antagonize tyrosine kinases as well as engage extracellular ligands. A recent wealth of data on this intriguing family indicates that its members can fulfill either tumor suppressing or oncogenic roles. The interpretation of these results at a molecular level has been greatly facilitated by the recent availability of structural information on the extra- and intracellular regions of RPTPs. These structures provide a molecular framework to understand how alterations in extracellular interactions can inactivate RPTPs in cancers or why the overexpression of certain RPTPs may also participate in tumor progression.
人们普遍认为,许多癌症都与异常的磷酸酪氨酸信号有关,这种信号可能是由酪氨酸激酶或酪氨酸磷酸酶的不当活性引起的。此外,信号通路的不正确激活通常与细胞表面受体介导的黏附事件的变化有关。在这些受体中,受体蛋白酪氨酸磷酸酶(RPTPs)既拮抗酪氨酸激酶,又与细胞外配体结合。最近大量关于这个有趣家族的研究数据表明,其成员可以发挥抑癌或致癌作用。RPTP 细胞外和细胞内区域的结构信息的最新可用性极大地促进了对这些结果在分子水平上的解释。这些结构为理解细胞外相互作用的改变如何使 RPTP 在癌症中失活,或者为什么某些 RPTP 的过表达也可能参与肿瘤进展提供了分子框架。
