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

Wen 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:10.3390/ijms25042123

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

Wen 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

Medicine

Roswell Park Cancer Institute
SUNY Buffalo
Purdue University

Research output: Contribution to journal › Article › peer-review

28 Scopus citations

Abstract

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.

Original language	English
Article number	2123
Journal	International Journal of Molecular Sciences
Volume	25
Issue number	4
DOIs	https://doi.org/10.3390/ijms25042123
State	Published - Feb 2024

Keywords

PSMA
cancer stem cells
folate receptor
miRNA ligand conjugates
miRNA therapeutics
microRNA
microRNA-34a
prostate cancer

Access to Document

10.3390/ijms25042123

Cite this

Li, W., Wang, Y., Liu, X., Wu, S., Wang, M., Turowski, S. G., Spernyak, J. A., Tracz, A., Abdelaal, A. M., Sudarshan, K., Puzanov, I., Chatta, G., Kasinski, A. L., & Tang, D. G. (2024). Developing Folate-Conjugated miR-34a Therapeutic for Prostate Cancer: Challenges and Promises. International Journal of Molecular Sciences, 25(4), Article 2123. https://doi.org/10.3390/ijms25042123

@article{525fe3bb46c4447bb5a4f86aaca3447b,

title = "Developing Folate-Conjugated miR-34a Therapeutic for Prostate Cancer: Challenges and Promises",

abstract = "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{\textquoteright}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 = "PSMA, cancer stem cells, folate receptor, miRNA ligand conjugates, miRNA therapeutics, microRNA, microRNA-34a, prostate cancer",

author = "Wen Li and Yunfei Wang and Xiaozhuo Liu and Shan Wu and Moyi Wang and Turowski, \{Steven G.\} and Spernyak, \{Joseph A.\} and Amanda Tracz and Abdelaal, \{Ahmed M.\} and Kasireddy Sudarshan and Igor Puzanov and Gurkamal Chatta and Kasinski, \{Andrea L.\} and Tang, \{Dean G.\}",

note = "Publisher Copyright: {\textcopyright} 2024 by the authors.",

year = "2024",

month = feb,

doi = "10.3390/ijms25042123",

language = "English",

volume = "25",

journal = "International Journal of Molecular Sciences",

issn = "1661-6596",

publisher = "Multidisciplinary Digital Publishing Institute (MDPI)",

number = "4",

}

TY - JOUR

T1 - Developing Folate-Conjugated miR-34a Therapeutic for Prostate Cancer

T2 - Challenges and Promises

AU - Li, Wen

AU - Wang, Yunfei

AU - Liu, Xiaozhuo

AU - Wu, Shan

AU - Wang, Moyi

AU - Turowski, Steven G.

AU - Spernyak, Joseph A.

AU - Tracz, Amanda

AU - Abdelaal, Ahmed M.

AU - Sudarshan, Kasireddy

AU - Puzanov, Igor

AU - Chatta, Gurkamal

AU - Kasinski, Andrea L.

AU - Tang, Dean G.

PY - 2024/2

Y1 - 2024/2

N2 - 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.

AB - 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.

KW - PSMA

KW - cancer stem cells

KW - folate receptor

KW - miRNA ligand conjugates

KW - miRNA therapeutics

KW - microRNA

KW - microRNA-34a

KW - prostate cancer

UR - https://www.scopus.com/pages/publications/85186264213

U2 - 10.3390/ijms25042123

DO - 10.3390/ijms25042123

M3 - Article

C2 - 38396800

AN - SCOPUS:85186264213

SN - 1661-6596

VL - 25

JO - International Journal of Molecular Sciences

JF - International Journal of Molecular Sciences

IS - 4

M1 - 2123

ER -

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

Abstract

Keywords

Access to Document

Other files and links

Fingerprint

Cite this