Telomerase reverse transcriptase promotes cancer cell proliferation by augmenting tRNA expression
Ekta Khattar, … , Yuin Han Loh, Vinay Tergaonkar
Ekta Khattar, … , Yuin Han Loh, Vinay Tergaonkar
Published September 19, 2016
Citation Information: J Clin Invest. 2016;126(10):4045-4060. https://doi.org/10.1172/JCI86042.
View: Text | PDF
Research Article Oncology

Telomerase reverse transcriptase promotes cancer cell proliferation by augmenting tRNA expression

Abstract

Transcriptional reactivation of telomerase reverse transcriptase (TERT) reconstitutes telomerase activity in the majority of human cancers. Here, we found that ectopic TERT expression increases cell proliferation, while acute reductions in TERT levels lead to a dramatic loss of proliferation without any change in telomere length, suggesting that the effects of TERT could be telomere independent. We observed that TERT determines the growth rate of cancer cells by directly regulating global protein synthesis independently of its catalytic activity. Genome-wide TERT binding across 5 cancer cell lines and 2 embryonic stem cell lines revealed that endogenous TERT, driven by mutant promoters or oncogenes, directly associates with the RNA polymerase III (pol III) subunit RPC32 and enhances its recruitment to chromatin, resulting in increased RNA pol III occupancy and tRNA expression in cancers. TERT-deficient mice displayed marked delays in polyomavirus middle T oncogene–induced (PyMT-induced) mammary tumorigenesis, increased survival, and reductions in tRNA levels. Ectopic expression of either RPC32 or TERT restored tRNA levels and proliferation defects in TERT-depleted cells. Finally, we determined that levels of TERT and tRNA correlated in breast and liver cancer samples. Together, these data suggest the existence of a unifying mechanism by which TERT enhances translation in cells to regulate cancer cell proliferation.

Authors

Ekta Khattar, Pavanish Kumar, Chia Yi Liu, Semih Can Akıncılar, Anandhkumar Raju, Manikandan Lakshmanan, Julien Jean Pierre Maury, Yu Qiang, Shang Li, Ern Yu Tan, Kam M. Hui, Ming Shi, Yuin Han Loh, Vinay Tergaonkar

×

Figure 9

Correlation analysis between TERT and pretranscripts of tRNAs in cancers.

Options: View larger image (or click on image) Download as PowerPoint
Correlation analysis between TERT and pretranscripts of tRNAs in cancers...
(A and B) Correlation analysis between TERT and pre–tRNA-Leu and pre–tRNA-Tyr expression in breast cancer (BC) types (n = 5 of each type) which include TNBC, luminal breast cancer, and HER2+ breast cancer. ΔCt values were plotted for the analysis, and R2 values were calculated in Microsoft Excel. (C and D) Correlation analysis between TERT and pre–tRNA-Leu and pre–tRNA-Tyr expression in RNA extracted from patients’ HCC cells (n = 9). ΔCt values were plotted for the analysis, and R2 values were calculated in Microsoft Excel. (E) Model shows that normal cells do not express TERT and thus have normal proliferation. Upon telomerase reactivation in cancer cells, TERT is expressed. TERT associates with the RPC32 subunit of RNA pol III and augments tRNA expression. This increase is responsible for the increased proliferation of cancer cells.