| Literature DB >> 33427367 |
Ning Tang1,2, Hanhui Li1,2, Lihong Zhang1,3, Xueyun Zhang1,3, Yanni Chen1,2, Hao Shou1,2, Shuaishuai Feng1,2, Xinhua Chen4, Yan Luo1,3, Ruikang Tang5, Ben Wang1,2.
Abstract
Cancer chemotherapy typically relies on drug endocytosis and inhibits tumor cell proliferation via intracellular pathways; however, severe side effects may arise. In this study, we performed a first attempt to develop macromolecular-induced extracellular chemotherapy involving biomineralization by absorbing calcium from the blood through a new type of drug, polysialic acid conjugated with folate (folate-polySia), which selectively induces biogenic mineral formation on tumor cells and results in the pathological calcification of tumors. The macromolecule-initiated extracellular calcification causes cancer cell death mainly by intervening with the glycolysis process in cancer cells. Systemic administration of folate-polySia inhibited cervical and breast tumor growth and dramatically improved survival rates in mice. This study provides an extracellular therapeutic approach for malignant tumor diseases via calcification that is ready for clinical trials and offers new insights into macromolecular anticancer drug discovery.Entities:
Keywords: antitumor therapy; biomineralization; calcification; macromolecular drug; polysialic acid
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Year: 2021 PMID: 33427367 DOI: 10.1002/anie.202016122
Source DB: PubMed Journal: Angew Chem Int Ed Engl ISSN: 1433-7851 Impact factor: 15.336