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Data from Silencing PinX1 Compromises Telomere Length Maintenance As Well As Tumorigenicity in Telomerase-Positive Human Cancer Cells

Authors :
Jun Jian Huang
Hsiang-fu Kung
Yang Chao Chen
Ying Peng
Cui Fen Huang
Pei Tang Huang
Xiao Xiong Wang
Pingxun Yang
Shi Peng Sun
Jian Lin
Zhi Long Wang
Rui Jin
Feng Feng
Hang Hang Ma
Yun Xiu Bai
Bin Zhang
Publication Year :
2023
Publisher :
American Association for Cancer Research (AACR), 2023.

Abstract

The nucleolar protein PinX1 has been proposed to be a putative tumor suppressor due to its binding to and inhibition of the catalytic activity of telomerase, an enzyme that is highly expressed in most human cancers in which it counteracts telomere shortening–induced senescence to confer cancer cell immortalization. However, the role of PinX1 in telomere regulation, as well as in cancer, is still poorly understood. In this study, we showed that the PinX1 protein is constitutively expressed in various human cells regardless of their telomerase activity and malignant status. Most interestingly, we found that silencing PinX1 expression by a potent short hairpin RNA construct led to a robust telomere length shortening and growth inhibition in telomerase-positive but not in telomerase-negative human cancer cells. We further showed that silencing PinX1 significantly reduced the endogenous association of telomerase with the Pot1-containing telomeric protein complex, and therefore, could account for the phenotypic telomere shortening in the affected telomerase-positive cancer cells. Our results thus reveal a novel positive role for PinX1 in telomerase/telomere regulations and suggest that the constitutive expression of PinX1 attributes to telomere maintenance by telomerase and tumorigenicity in cancer cells. [Cancer Res 2009;69(1):75–83]

Details

Database :
OpenAIRE
Accession number :
edsair.doi.dedup.....23ee7278eaca17342828ab896a9bddf0