Lipid-Raft-Targeted Molecular Self-Assembly Inactivates YAP to Treat Ovarian Cancer

The Yes-associated protein (YAP) is a major oncoprotein responsible for cell proliferation control. YAP's oncogenic activity is regulated by both the Hippo kinase cascade and uniquely by a mechanical-force-induced actin remodeling process. Inspired by reports that ovarian cancer cells specifica...

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Veröffentlicht in:Nano letters 2021-01, Vol.21 (1), p.747-755
Hauptverfasser: Li, Guanying, Hu, Xunwu, Nie, Pingping, Mang, Dingze, Jiao, Shi, Zhang, Shijin, Roy, Sona Rani, Yukawa, Sachie, Asahina, Shunsuke, Sugasawa, Hiroaki, Cortes, William, Zhou, Zhaocai, Zhang, Ye
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Sprache:eng
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Zusammenfassung:The Yes-associated protein (YAP) is a major oncoprotein responsible for cell proliferation control. YAP's oncogenic activity is regulated by both the Hippo kinase cascade and uniquely by a mechanical-force-induced actin remodeling process. Inspired by reports that ovarian cancer cells specifically accumulate the phosphatase protein ALPP on lipid rafts that physically link to actin cytoskeleton, we developed a molecular self-assembly (MSA) technology that selectively halts cancer cell proliferation by inactivating YAP. We designed a ruthenium-complex-peptide precursor molecule that, upon cleavage of phosphate groups, undergoes self-assembly to form nanostructures specifically on lipid rafts of ovarian cancer cells. The MSAs exert potent, cancer-cell-specific antiproliferative effects in multiple cancer cell lines and in mouse xenograft tumor models. Our work illustrates how basic biochemical insights can be exploited as the basis for a nanobiointerface fabrication technology which links nanoscale protein activities at specific subcellular locations to molecular biological activities to suppress cancer cell proliferation.
ISSN:1530-6984
1530-6992
DOI:10.1021/acs.nanolett.0c04435