RIP3 脙脙脙脙 and RIP3 脙脙脙脙, two novel splice variants of receptor-interacting protein 3 (RIP3), downregulate RIP3-induced apoptosis

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• 作者：Yang ; Yonghui ; Hu ; Weiping ; Feng ; Shanshan ; Ma ; Jun ; Wu ; Mian
• 刊名：Biochemical and Biophysical Research Communications
• 出版年：2005
• 期刊代码：159_0006291x
• 类别：bio
• 出版时间：June 24, 2005
• 卷：332
• 期：1
• 页码：181-187
• 文件大小：1.06 M

摘要

Receptor-interacting protein 3 (RIP3) is an apoptosis inducing member of the RIP family. Here we report two novel splice variants of human RIP3, designated RIP3 β and RIP3 γ respectively. Unlike full-length RIP3, both variants possess a truncated N-terminal kinase domain and a distinct and shorter C terminus, and therefore abrogate nucleocytoplasmic shuttling and apoptosis-inducing activity. Transient expression of either variant was found to downregulate RIP3-mediated apoptosis. Importantly, real-time PCR analysis reveals that the ratio of RIP3 γ to RIP3 is significantly increased in colon and lung cancers relative to their matched normal tissues, indicating that RIP3 γ might be a major splice form associated with tumorigenesis.