International Journal of Molecular Sciences (Feb 2024)

Developing Folate-Conjugated miR-34a Therapeutic for Prostate Cancer: Challenges and Promises

  • Wen (Jess) Li,
  • Yunfei Wang,
  • Xiaozhuo Liu,
  • Shan Wu,
  • Moyi Wang,
  • Steven G. Turowski,
  • Joseph A. Spernyak,
  • Amanda Tracz,
  • Ahmed M. Abdelaal,
  • Kasireddy Sudarshan,
  • Igor Puzanov,
  • Gurkamal Chatta,
  • Andrea L. Kasinski,
  • Dean G. Tang

DOI
https://doi.org/10.3390/ijms25042123
Journal volume & issue
Vol. 25, no. 4
p. 2123

Abstract

Read online

Prostate cancer (PCa) remains a common cancer with high mortality in men due to its heterogeneity and the emergence of drug resistance. A critical factor contributing to its lethality is the presence of prostate cancer stem cells (PCSCs), which can self-renew, long-term propagate tumors, and mediate treatment resistance. MicroRNA-34a (miR-34a) has shown promise as an anti-PCSC therapeutic by targeting critical molecules involved in cancer stem cell (CSC) survival and functions. Despite extensive efforts, the development of miR-34a therapeutics still faces challenges, including non-specific delivery and delivery-associated toxicity. One emerging delivery approach is ligand-mediated conjugation, aiming to achieve specific delivery of miR-34a to cancer cells, thereby enhancing efficacy while minimizing toxicity. Folate-conjugated miR-34a (folate–miR-34a) has demonstrated promising anti-tumor efficacy in breast and lung cancers by targeting folate receptor α (FOLR1). Here, we first show that miR-34a, a TP53 transcriptional target, is reduced in PCa that harbors TP53 loss or mutations and that miR-34a mimic, when transfected into PCa cells, downregulated multiple miR-34a targets and inhibited cell growth. When exploring the therapeutic potential of folate–miR-34a, we found that folate–miR-34a exhibited impressive inhibitory effects on breast, ovarian, and cervical cancer cells but showed minimal effects on and targeted delivery to PCa cells due to a lack of appreciable expression of FOLR1 in PCa cells. Folate–miR-34a also did not display any apparent effect on PCa cells expressing prostate-specific membrane antigen (PMSA) despite the reported folate’s binding capability to PSMA. These results highlight challenges in the specific delivery of folate–miR-34a to PCa due to a lack of target (receptor) expression. Our study offers novel insights into the challenges and promises within the field and casts light on the development of ligand-conjugated miR-34a therapeutics for PCa.

Keywords