iScience (Dec 2023)

Expression of nonmuscle myosin IIC is regulated by non-canonical binding activity of miRNAs

  • Kumarjeet Banerjee,
  • Shekhar Saha,
  • Shaoli Das,
  • Suman Ghosal,
  • Indranil Ghosh,
  • Abhimanyu Basu,
  • Siddhartha S. Jana

Journal volume & issue
Vol. 26, no. 12
p. 108384

Abstract

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Summary: The expression of mechanoresponsive nonmuscle myosin II (NMII)C is found to be inducible during tumor progression, but its mechanism is yet to be explored. Here, we report a group of microRNAs (mmu-miR-200a-5p, mmu-miR-532-3p, mmu-miR-680, and mmu-miR-1901) can significantly repress the expression of nonmuscle myosin IIC (NMIIC). Interestingly, these microRNAs have both canonical and non-canonical binding sites at 3/UTR and coding sequence (CDS) of NMIIC’s heavy chain (HC) mRNA. Each of the miRNA downregulates NMHC-IIC to a different degree as assessed by dual-luciferase and immunoblot analyses. When we abolish the complementary base pairing at canonical binding site, mmu-miR-532-3p can still bind at non-canonical binding site and form Argonaute2 (AGO2)-miRNA complex to downregulate the expression of NMIIC. Modulating the expression of NMIIC by miR-532-3p in mouse mammary tumor cells, 4T1, increases its tumorigenic potential both in vitro and in vivo. Together, these studies provide the functional role of miRNA’s non-canonical binding mediated NMIIC regulation in tumor cells.

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