4.7 Article

CYRI-A limits invasive migration through macropinosome formation and integrin uptake regulation

Journal

JOURNAL OF CELL BIOLOGY
Volume 220, Issue 9, Pages -

Publisher

ROCKEFELLER UNIV PRESS
DOI: 10.1083/jcb.202012114

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Funding

  1. Cancer Research UK [A17196, A31287, A24452, A19257]

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The study reveals that CYRI-A is a key regulator of macropinosome formation and integrin internalization, being transiently recruited to nascent macropinosomes and dependent on PI3K and RAC1 activity for its function.
The Scar/WAVE complex drives actin nucleation during cell migration. Interestingly, the same complex is important in forming membrane ruffles during macropinocytosis, a process mediating nutrient uptake and membrane receptor trafficking. Mammalian CYRI-B is a recently described negative regulator of the Scar/WAVE complex by RAC1 sequestration, but its other para Logue, CYRI-A, has not been characterized. Here, we implicate CYRI-A as a key regulator of macropinosome formation and integrin internalization. We find that CYRI-A is transiently recruited to nascent macropinosomes, dependent on PI3K and RAC1 activity. CYRI-A recruitment precedes RAB5A recruitment but follows sharply after RAC1 and actin signaling, consistent with it being a local inhibitor of actin polymerization. Depletion of both CYRI-A and -B results in enhanced surface expression of the alpha 5 beta 1 integrin via reduced internalization. CYRI depletion enhanced migration, invasion, and anchorage-independent growth in 3D. Thus, CYRI-A is a dynamic regulator of macropinocytosis, functioning together with CYRI-B to regulate integrin trafficking.

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