作者
Tiantian Zhang, Joseph HyungJoon Na, Samantha Li, Zhengming Chen, George Zhang, Sharon Pang, Anthony F Daniyan, Yi Li, Lei Shi, Yi‐Chieh Nancy Du
发表日期
2020/12
期刊
MedComm
卷号
1
期号
3
页码范围
328-337
简介
Bcl‐xL, an antiapoptotic protein, is frequently overexpressed in cancer to promote survival of tumor cells. However, we have previously shown that Bcl‐xL promotes migration, invasion, and metastasis independent of its antiapoptotic function in mitochondria. The pro‐metastatic function of Bcl‐xL may require its translocation into the nucleus. Besides overexpression, patient‐associated mutations of Bcl‐xL have been identified in large‐scale cancer genomics projects. Understanding the functions of these mutations will guide the development of precision medicine. Here, we selected four patient‐associated Bcl‐xL mutations, R132W, N136K, R165W, and A201T, to investigate their impacts on antiapoptosis, migration, and nuclear translocation. We found that all four mutation proteins could be detected in both the nucleus and cytosol. Although all four mutations disrupted the antiapoptosis function, one of these mutants …
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