A novel function of AAA-ATPase p97/VCP in the regulation of cell motility.

Oncotarget

School of Biological Sciences, College of Science, Nanyang Technological University, Singapore 637551, Singapore.

Published: January 2020

AI Article Synopsis

  • Scientists found that a protein called p97/VCP can affect how cells move and how a part of the cell called actin behaves.
  • When they removed p97/VCP from cells, actin became more stable, and the cells couldn't move as well as before.
  • This study showed that p97/VCP helps control another protein called RhoA, which is important for cell movement, and that losing p97/VCP might contribute to cancer.

Article Abstract

High level of the multifunctional AAA-ATPase p97/VCP is often correlated to the development of cancer; however, the underlying mechanism is not understood completely. Here, we report a novel function of p97/VCP in actin regulation and cell motility. We found that loss of p97/VCP promotes stabilization of F-actin, which cannot be reversed by actin-destabilizing agent, Cytochalasin D. Live-cell imaging demonstrated reduced actin dynamics in p97/VCP-knockdown cells, leading to compromised cell motility. We further examined the underlying mechanism and found elevated RhoA protein levels along with increased phosphorylation of its downstream effectors, ROCK, LIMK, and MLC upon the knockdown of p97/VCP. Since p97/VCP is indispensable in the ubiquitination-dependent protein degradation pathway, we investigated if the loss of p97/VCP hinders the protein degradation of RhoA. Knockdown of p97/VCP resulted in a higher amount of ubiquitinated RhoA, suggesting p97/VCP involvement in the proteasome-dependent protein degradation pathway. Finally, we found that p97/VCP interacts with FBXL19, a molecular chaperone known to guide ubiquitinated RhoA for proteasomal degradation. Reduction of p97/VCP may result in the accumulation of RhoA which, in turn, enhances cytoplasmic F-actin formation. In summary, our study uncovered a novel function of p97/VCP in actin regulation and cell motility via the Rho-ROCK dependent pathway which provides fundamental insights into how p97/VCP is involved in cancer development.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC6967774PMC
http://dx.doi.org/10.18632/oncotarget.27419DOI Listing

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