4.7 Article

Leep1 interacts with PIP3 and the Scar/WAVE complex to regulate cell migration and macropinocytosis

Journal

JOURNAL OF CELL BIOLOGY
Volume 220, Issue 7, Pages -

Publisher

ROCKEFELLER UNIV PRESS
DOI: 10.1083/jcb.202010096

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Funding

  1. Ministry of Science and Technology of the People's Republic of China [2016YFA0500202]
  2. Strategic Priority Research Program of the Chinese Academy of Sciences [XDB37020304]
  3. National Natural Science Foundation of China [31770894, 31872828]

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This study identifies a novel polarity regulator, Leep1, in the model system Dictyostelium, which selectively localizes at the leading edge of cells by binding to PIP3 to negatively regulate the Scar/WAVE complex, thereby modulating the dynamics of protrusive structures at the leading edge.
Polarity is essential for diverse functions in many cell types. Establishing polarity requires targeting a network of specific signaling and cytoskeleton molecules to different subregions of the cell, yet the full complement of polarity regulators and how their activities are integrated over space and time to form morphologically and functionally distinct domains remain to be uncovered. Here, by using the model system Dictyostelium and exploiting the characteristic chemoattractant-stimulated translocation of polarly distributed molecules, we developed a proteomic screening approach, through which we identified a leucine-rich repeat domain-containing protein we named Leep1 as a novel polarity regulator. We combined imaging, biochemical, and phenotypic analyses to demonstrate that Leep1 localizes selectively at the leading edge of cells by binding to PIP3, where it modulates pseudopod and macropinocytic cup dynamics by negatively regulating the Scar/WAVE complex. The spatiotemporal coordination of PIP3 signaling, Leep1, and the Scar/WAVE complex provides a cellular mechanism for organizing protrusive structures at the leading edge.

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