WNT5A-induced activation of the protein kinase C substrate MARCKS is required for melanoma cell invasion

Purusottam Mohapatra, Vikas Yadav, Maren Toftdahl, Tommy Andersson

Research output: Contribution to journalArticlepeer-review

Abstract

WNT5A is a well-known mediator of melanoma cell invasion and metastasis via its ability to activate protein kinase C (PKC), which is monitored by phosphorylation of the endogenous PKC substrate myristoylated alanine-rich c-kinase substrate (MARCKS). However, a possible direct contribution of MARCKS in WNT5A-mediated melanoma cell invasion has not been investigated. Analyses of melanoma patient databases suggested that similar to WNT5A expression, MARCKS expression appears to be associated with increased metastasis. A relationship between the two is suggested by the findings that recombinant WNT5A (rWNT5A) induces both increased expression and phosphorylation of MARCKS, whereas WNT5A silencing does the opposite. Moreover, WNT5A-induced invasion of melanoma cells was blocked by siRNA targeting MARCKS, indicating a crucial role of MARCKS expression and/or its phosphorylation. Next, we employed a peptide inhibitor of MARCKS phosphorylation that did not affect MARCKS expression and found that it abolished WNT5A-induced melanoma cell invasion. Similarly, rWNT5A induced the accumulation of phosphorylated MARCKS in membrane protrusions at the leading edge of melanoma cells. Our results demonstrate that WNT5A-induced phosphorylation of MARCKS is not only an indicator of PKC activity but also a crucial regulator of the metastatic behavior of melanoma and therefore an attractive future antimetastatic target in melanoma patients.

Original languageEnglish
Article number346
JournalCancers
Volume12
Issue number2
DOIs
Publication statusPublished - 2020 Feb 4

Subject classification (UKÄ)

  • Cell and Molecular Biology

Free keywords

  • Invasion
  • MANS peptide
  • MARCKS
  • Melanoma
  • Phosphorylation
  • WNT5A

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