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胰腺癌中含多个SH3结构域蛋白相互作用组的鉴定:一种酵母双杂交方法。

Identification of multi-SH3 domain-containing protein interactome in pancreatic cancer: a yeast two-hybrid approach.

作者信息

Thalappilly Subhash, Suliman Muhtadi, Gayet Odile, Soubeyran Philippe, Hermant Aurélie, Lecine Patrick, Iovanna Juan L, Dusetti Nelson J

机构信息

INSERM U624, Stress Cellulaire, Marseille, France.

出版信息

Proteomics. 2008 Aug;8(15):3071-81. doi: 10.1002/pmic.200701157.

DOI:10.1002/pmic.200701157
PMID:18654987
Abstract

Pancreatic ductal adenocarcinoma (PDAC) is a fatal disease that shows minimal response to chemotherapy. Genetic changes involved in the progression of PDAC concern genes that encode proteins related to signal transduction networks. This fact reveals the importance in identifying the role and the relations between multiple signaling cascades in PDAC. One of the major factors that modulate signaling events is multidomain scaffold proteins that function by binding several proteins simultaneously, inducing their proximity and influencing the outcome of signaling. A particular group among them, containing multiple Src homology 3 (SH3) domains that can bind proteins containing proline-rich motifs, was associated to different aspects of cancer cell homeostasis. In this work, using a microarray-based analysis, we have shown that 13 multiple SH3 domain containing scaffold proteins are expressed in PDAC cells. Using a yeast two-hybrid approach, we have identified proteins that interact with these adaptor proteins. Among them we have found several molecules that modulate cell proliferation and survival (CIZ1, BIRC6, RBBP6), signaling (LTBP4, Notch2, TOM1L1, STK24) and membrane dynamics (PLSCR1, DDEF2, VCP). Our results indicate that interactions mediated by multi-SH3 domain-containing proteins could lead to the formation of dynamic protein complexes that function in pancreatic cancer cell signaling. The identification of such protein complexes is of paramount importance in deciphering pancreatic cancer biology and designing novel therapeutic approaches.

摘要

胰腺导管腺癌(PDAC)是一种致命疾病,对化疗反应甚微。PDAC进展过程中涉及的基因变化与编码信号转导网络相关蛋白的基因有关。这一事实揭示了确定PDAC中多个信号级联之间的作用和关系的重要性。调节信号事件的主要因素之一是多结构域支架蛋白,其通过同时结合几种蛋白质发挥作用,诱导它们靠近并影响信号转导结果。其中一个特殊的蛋白组含有多个能结合富含脯氨酸基序蛋白质的Src同源3(SH3)结构域,与癌细胞内环境稳定的不同方面相关。在这项研究中,我们通过基于微阵列的分析表明,13种含多个SH3结构域的支架蛋白在PDAC细胞中表达。利用酵母双杂交方法,我们鉴定了与这些衔接蛋白相互作用的蛋白质。其中我们发现了几种调节细胞增殖和存活(CIZ1、BIRC6、RBBP6)、信号转导(LTBP4、Notch2、TOM1L1、STK24)和膜动力学(PLSCR1、DDEF2、VCP)的分子。我们的结果表明,由含多个SH3结构域的蛋白质介导的相互作用可能导致形成在胰腺癌细胞信号转导中起作用的动态蛋白质复合物。鉴定此类蛋白质复合物对于解读胰腺癌生物学特性和设计新的治疗方法至关重要。

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