Transient receptor potential cation channel subfamily C member 6 is involved in regulating cell cycle of endometrial carcinoma cells
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Supported by Science and Technology Key Research Project of Henan Science and Technology Department (162102310022), Key Scientific Research Project of Henan Universities and Colleges (13A320639), and Medical Science and Technology Key Research Project of Henan Province (201203120).

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    Abstract:

    Objective To study the expression of transient receptor potential cation channel subfamily C member 6 (TRPC6) in endometrial carcinoma tissues and their role in regulating cell cycle of endometrial carcinoma cells. Methods Quantitative real-time PCR and Western blotting were used to examine the expression of TRPC6 in 30 normal endometrial specimens, 30 atypical hyperplasia specimens and 32 endometrial carcinoma specimens. SKF96365 (an inhibitor of TRPC6 channel) and RNA interference (RNAi) targeting TRPC6 by small interference RNA (siRNA) were used to block TRPC6 so as to explore the role of TRPC6 in regulating the cell cycle of endometrial carcinoma cells HEC-1A. Results The expression levels of TRPC6 mRNA and protein in endometrial carcinoma were significantly higher than those in the atypical hyperplasia endometria and normal endometrial tissues (P<0.01). SKF96365 retarded cell cycle at G2/M phase in a dose-dependent manner and reduced HEC-1A cells of G0/G1 phase. Transfection with target-TRPC6 siRNA retarded cell cycle of HEC-1A cells at G2/M phase, and reduced HEC-1A cells of G0/G1 phase compared with negative control siRNA. Meanwhile, transfection with target-TRPC6 siRNA increased phosphorylated cell division cycle 2 (pCDC2) protein expression in HEC-1A cells. Conclusion The expression of TRPC6 is elevated in endometrial carcinoma tissues. TRPC6 may influence cell cycle through regulating pCDC2.

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History
  • Received:July 12,2019
  • Revised:October 20,2019
  • Adopted:January 03,2020
  • Online: January 17,2020
  • Published:
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