PO.MCB10.01 · 分子与细胞生物学
Auro-Liposome miR-195 delivery system impedes ovarian cancer progression and enhances cisplatin-sensitivity
作者与单位
摘要 Abstract
Background: Ovarian cancer (OvCa) accounts for the highest mortality rate among all gynecological malignancy. This is mainly due to late-stage detection, early metastasis and drug-resistance. While most patients initially respond to chemotherapy, Cancer Stem-like Cells (CSCs) facilitate chemoresistance and tumor relapse. WNT7A, a key activator of beta-catenin signaling, is overexpressed in OvCa and promotes CSC characteristics, epithelial-mesenchymal transition (EMT), chemoresistance, whereas the tumor-suppressive miR-195 is downregulated. In this study, we investigated whether restoring miR-195 expression could inhibit cancer progression and improve drug-sensitivity by targeting WNT7A mediated beta-catenin signaling.
Methods: CSCs were enriched using anchorage-independent spheroid culture conditions. miR-195 expression levels were assessed by qRT-PCR. Functional assays were performed to determine the effect of miR-195 on CSC markers, EMT, drug-sensitivity. A luciferase reporter assay was utilized to validate the direct miR-195 binding within the WNT7A 3'UTR. beta-catenin activation and nuclear localization were analyzed by immunoblot, immunofluorescence. To mimic tumor microenvironment, multicellular aggregate model was generated using OvCa cell line (A2780-CP20), cancer-associated fibroblast (CAF19) and human microvascular endothelial cells (HMEC1) and for assessing AuLPs's potential as a miR-195 delivery system.
Results: Spheroid-derived CSCs displayed enhanced expression of stem cell markers NANOG, OCT4, cMYC, KLF4, accompanied by a significant reduction in miR-195 levels. Restoration of miR-195 expression inhibited spheroid growth, caused downregulation of stemness markers and enhanced cisplatin-sensitivity. miR-195 directly targeted WNT7A, leading to decreased nuclear localization of active beta-catenin and inhibition of WNT/beta-catenin signaling, EMT pathway. Furthermore, in vivo homing assay revealed that stable miR-195 re-expression significantly reduced A2780-CP20 adhesion to the mice omentum, highlighting its anti-metastatic role. Noticeably, our novel AuLPs system conferred superior intracellular delivery of miR-195 compared to commercial agents and more striking inhibition of oncogenic WNT7A/beta-catenin pathway and profound anti-tumor effect against multicellular aggregate.
Conclusions: miR-195 suppress OvCa progression by targeting cancer stemness, EMT and enhance cisplatin-sensitivity via directly modulating WNT7A/beta-catenin pathway and formulations of novel AuLPs delivery system offers a promising miRNA-based therapeutic strategy.
Acknowledgments: PHF and DOD'S Ovarian Cancer Academy grant (HT94252310772) to SKD.
利益披露 Disclosure
A. Dey Bhowmik, None..
P. Shaw, None..
P. Panja, None..
G. Rao, None..
R. Bhattacharya, None..
P. Mukherjee, None..
S. K. Dwivedi, None.