Literature DB >> 31740794

Delivery of nitric oxide with a nanocarrier promotes tumour vessel normalization and potentiates anti-cancer therapies.

Yun-Chieh Sung1,2, Pei-Ru Jin1, Li-An Chu3, Fu-Fei Hsu4, Mei-Ren Wang5, Chih-Chun Chang1, Show-Jen Chiou6, Jiantai Timothy Qiu7,8,9, Dong-Yu Gao1, Chu-Chi Lin9, Yu-Sing Chen9, Yi-Chiung Hsu10, Jane Wang2, Fu-Nien Wang11, Pei-Lun Yu11, Ann-Shyn Chiang3,12,13,14, Anthony Yan-Tang Wu15,16,17, John Jun-Sheng Ko1,15, Charles Pin-Kuang Lai15,16,18, Tsai-Te Lu19,20, Yunching Chen21.   

Abstract

Abnormal tumour vasculature has a significant impact on tumour progression and response to therapy. Nitric oxide (NO) regulates angiogenesis and maintains vascular homeostasis and, thus, can be delivered to normalize tumour vasculature. However, a NO-delivery system with a prolonged half-life and a sustained release mechanism is currently lacking. Here we report the development of NanoNO, a nanoscale carrier that enables sustained NO release to efficiently deliver NO into hepatocellular carcinoma. Low-dose NanoNO normalizes tumour vessels and improves the delivery and effectiveness of chemotherapeutics and tumour necrosis factor-related, apoptosis-inducing, ligand-based therapy in both primary tumours and metastases. Furthermore, low-dose NanoNO reprogrammes the immunosuppressive tumour microenvironment toward an immunostimulatory phenotype, thereby improving the efficacy of cancer vaccine immunotherapy. Our findings demonstrate the ability of nanoscale NO delivery to efficiently reprogramme tumour vasculature and immune microenvironments to overcome resistance to cancer therapy, resulting in a therapeutic benefit.

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Year:  2019        PMID: 31740794     DOI: 10.1038/s41565-019-0570-3

Source DB:  PubMed          Journal:  Nat Nanotechnol        ISSN: 1748-3387            Impact factor:   39.213


  35 in total

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