Taipei Medical University

A B C D E F G H I J K L M N O P Q R S T U V W X Y Z
Jin-Yuan Shih, Yuan-Chii G. Lee, Shuenn-Chen Yang, Tse-Ming Hong, CShih JY, Lee YCG, Yang SC, Hong TM, Huang CYF and Yang PC
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------>journal_name=Clinical and Experimental Metastasis
------>paper_name=Collapsin Response Mediator Protein-1: A Novel Invasion-Suppressor Gene
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------>fullAbstract=Numerous genetic changes are associated with metastasis of cancer cells. Previously, we used microarray to identify that collapsin response mediator protein-1 (CRMP-1) was involved in cancer invasion and metastasis. We further characterized that CRMP-1 was a novel invasion-suppression gene. Members of the CRMP gene family are intracellular phosphoproteins involved in the mediation of semaphorin induced F-actin depolymerization and growth cone collapse. The precise mechanism by which CRMP-I inhibits invasion is not yet clear. However, CRMP-1 transfected cells had fewer filopodia and less Matrigel-invasion abilities. A low expression of CRMP-I mRNA in lung cancer tissue was significantly associated with advanced disease, lymph node metastasis, early post-operative relapse, and shorter survival. In this article, we reviewed the functions of CRMPs and semaphorins and analyzed the structure and motifs of CRMP-1 by bioinformatics. As such, we hoped to shed further light on the mechanism by which CRMP-1 suppresses the invasion of cancer cells.
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------>authors=Jin-Yuan Shih, Yuan-Chii G. Lee, Shuenn-Chen Yang, Tse-Ming Hong, CShih JY, Lee YCG, Yang SC, Hong TM, Huang CYF and Yang PC
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------>updateTitle=Collapsin response mediator protein-1: a novel invasion-suppressor gene.
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A B C D E F G H I J K L M N O P Q R S T U V W X Y Z