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Functionalized turmeric nanovesicles for precision delivery of doxorubicin in colorectal carcinoma treatment

Affiliation
College of Pharmacy ,Jiamusi University ,Jiamusi ,China
Meng, Chen;
Affiliation
Key Laboratory of Functional and Clinical Translational Medicine ,Fujian Province University ,Xiamen Medical College ,Xiamen ,China
Yi, Xue;
Affiliation
Key Laboratory of Functional and Clinical Translational Medicine ,Fujian Province University ,Xiamen Medical College ,Xiamen ,China
Duan, Meitao;
Affiliation
Guangzhou HC Pharmaceutical Co., Ltd ,Guangzhou ,China
Mahal, Ahmed;
Affiliation
Key Laboratory of Functional and Clinical Translational Medicine ,Fujian Province University ,Xiamen Medical College ,Xiamen ,China
Zhang, Zhiqiang;
Affiliation
Key Laboratory of Functional and Clinical Translational Medicine ,Fujian Province University ,Xiamen Medical College ,Xiamen ,China
Ren, Jungang;
Affiliation
Key Laboratory of Functional and Clinical Translational Medicine ,Fujian Province University ,Xiamen Medical College ,Xiamen ,China
Chen, Ming;
Affiliation
College of Pharmacy ,Jiamusi University ,Jiamusi ,China
Yang, Lin;
Affiliation
College of Pharmacy ,Jiamusi University ,Jiamusi ,China
Xu, Moxun;
Affiliation
Department of Pharmaceutical Chemistry ,College of Pharmacy ,King Saud University ,Riyadh ,Saudi Arabia
Obaidullah, Ahmad J.;
Affiliation
Key Laboratory of Functional and Clinical Translational Medicine ,Fujian Province University ,Xiamen Medical College ,Xiamen ,China
Song, Linwei;
Affiliation
College of Pharmacy ,Jiamusi University ,Jiamusi ,China
Li, Shuxian;
Affiliation
Key Laboratory of Functional and Clinical Translational Medicine ,Fujian Province University ,Xiamen Medical College ,Xiamen ,China
Wang, Chen

Nanoscale vesicles have emerged as promising biocompatible vehicles for precision drug delivery, owing to their inherent therapeutic properties and versatile structural configurations. This study introduces an innovative biomanufacturing strategy utilizing curcumin-extracted nanovesicles (TNVs) conjugated with a cancer-selective peptide and encapsulated with doxorubicin to optimize therapeutic outcomes in colorectal malignancies. TNVs were purified through refined ultracentrifugation protocols, demonstrating uniform saucer-shaped morphology with an average size of 162.42 ± 3.67 nm and stable bilayer architecture dominated by triglyceride (30%) and ceramide (11.8%) constituents. Peptide-mediated surface functionalization substantially improved intracellular internalization efficiency in HCT-116 colon carcinoma models. The engineered TNV-P-D formulation exhibited potent tumoricidal activity (IC 50 = 54.8 μg/ mL), outperforming both unbound doxorubicin (IC 50 = 795.2 ng/mL) and nonfunctionalized TNV-DOX counterparts (IC 50 = 129.7 μg/mL). Cell cycle profiling revealed G1-phase blockade (91.3% G1-phase occupancy), corroborating the platform’s proliferation-inhibiting capacity. In murine CT26. WT xenograft models, TNV-P-D administration achieved significant tumor regression (65% volume reduction, p< 0.001) while preserving hepatobiliary function and demonstrating negligible multiorgan toxicity. These results position peptide-augmented phytovesicles as a multifunctional therapeutic system capable of dual-action tumor targeting and systemic toxicity mitigation in colorectal oncology.

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License Holder: Copyright © 2025 Meng, Yi, Duan, Mahal, Zhang, Ren, Chen, Yang, Xu, Obaidullah, Song, Li and Wang.

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