Development of a Cancer Cells Self‑activating and MiR‑125a‑5p Expressing Poly‑pharmacological Nanodrug for Cancer Treatment

Overview

Journal Int J Mol Med

Specialty Genetics

Date 2022 Jun 15

PMID 35703361

Authors

Yung-Chieh Chang

Min-Chieh Shieh

Yen-Hsuan Chang

Wei-Lun Huang

Wu-Chou Su

Fong-Yu Cheng

Chun Hei Antonio Cheung

Affiliations

Soon will be listed here.

Abstract

Cancer cells can acquire resistance to targeted therapeutic agents when the designated targets or their downstream signaling molecules develop protein conformational or activity changes. There is an increasing interest in developing poly‑pharmacologic anticancer agents to target multiple oncoproteins or signaling pathways in cancer cells. The microRNA 125a‑5p (miR‑125a‑5p) is a tumor suppressor, and its expression has frequently been downregulated in tumors. By contrast, the anti‑apoptotic molecule BIRC5/SURVIVIN is highly expressed in tumors but not in the differentiated normal tissues. In the present study, the development of a gene promoter‑driven, miR‑125a‑5p expressing, poly‑L‑lysine‑conjugated magnetite iron poly‑pharmacologic nanodrug (pL‑MNP‑pSur‑125a) was reported. The cancer cells self‑activating property and the anticancer effects of this nanodrug were examined in both the multidrug efflux protein ABCB1/MDR1‑expressing/‑non‑expressing cancer cells and . It was demonstrated that pL‑MNP‑pSur‑125a decreased the expression of ERBB2/HER2, HDAC5, BIRC5, and SP1, which are hot therapeutic targets for cancer . Notably, pL‑MNP‑pSur‑125a also downregulated the expression of TDO2 in the human KB cervical carcinoma cells. PL‑MNP‑pSur‑125a decreased the viability of various ‑expressing cancer cells, regardless of the tissue origin or the expression of ABCB1, but not of the human ‑non‑expressing HMEC‑1 endothelial cells. , pL‑MNP‑pSur‑125a exhibited potent antitumor growth effects, but without inducing liver toxicity, in various zebrafish human‑ABCB1‑expressing and ABCB1‑non‑expressing tumor xenograft models. In conclusion, pL‑MNP‑pSur‑125a is an easy‑to‑prepare and a promising poly‑pharmacological anticancer nanodrug that has the potential to manage numerous malignancies, particularly for patients with BIRC5/ABCB1‑related drug resistance after prolonged chemotherapeutic treatments.

Citing Articles

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PMID: 39272948 PMC: 11394585. DOI: 10.3390/cancers16173090.

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