4.7 Article

Development and Evaluation of a PSMA-Targeted Nanosystem Co-Packaging Docetaxel and Androgen Receptor siRNA for Castration-Resistant Prostate Cancer Treatment

PHARMACEUTICS (2022)

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Journal

PHARMACEUTICS
Volume 14, Issue 5, Pages -

Publisher

MDPI
DOI: 10.3390/pharmaceutics14050964

Keywords

prostate cancer; androgen receptor; siRNA delivery; docetaxel; PSMA targeting

Categories

Pharmacology & Pharmacy

Funding

  1. CAMS Innovation Fund for Medical Sciences (CIFMS) [2021-I2M-1-026]
  2. National Natural Science Foundation of China (China) [82073778]
  3. Fundamental Research Funds for the Central Universities (China) [3332021044]
  4. Bethune Urinary Cancer Special Research Fund (China) [mnzl202014]
  5. CSCO Navigation Cancer Research Fund (China) [Y-2019AZQN-0398]

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In this study, a nanosystem was designed for the treatment of prostate cancer, carrying both docetaxel and androgen receptor siRNA. The results demonstrated that the nanosystem exhibited prolonged blood circulation, selective targeting, and enhanced antitumor effects, holding great potential for efficient treatment of castration-resistant prostate cancer by combining chemotherapy and siRNA silencing of androgen-related signaling pathways.
Primary prostate cancer (PC) progresses to castration-resistant PC (CRPC) during androgen deprivation therapy (ADR) in early stages of prostate cancer. Thus, rather than blocking the androgen-related pathway further, docetaxel (DTX)-based therapy has become the most effective and standard first-line chemotherapy for CRPC. Although the therapy is successful in prolonging the survival of patients with CRPC, chemotherapy resistance develops due to the abnormal activation of the androgen receptor (AR) signaling pathway. Thus, to optimize DTX efficacy, continued maximum suppression of androgen levels and AR signaling is required. Here, we designed a prostate-specific membrane antigen (PSMA)-targeted nanosystem to carry both DTX and AR siRNA (Di-PP/AR-siRNA/DTX) for CRPC treatment. Specifically, DTX was encapsulated into the hydrophobic inner layer, and the AR siRNA was then condensed with the cationic PEI block in the hydrophilic outer layer of the PEI-PLGA polymeric micelles. The micelles were further coated with PSMA-targeted anionic polyethylene glycol-polyaspartic acid (Di-PEG-PLD). In vitro and in vivo results demonstrated that the resulting Di-PP/AR-siRNA/DTX exhibited prolonged blood circulation, selective targeting, and enhanced antitumor effects. Consequently, Di-PP/AR-siRNA/DTX holds great potential for efficient CRPC treatment by combining chemotherapy and siRNA silencing of androgen-related signaling pathways.

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