ORIGINAL ARTICLE

Melanoma revives an embryonic migration program to promote plasticity and invasion

  1. Caleb M. Bailey1,
  2. Jason A. Morrison1,
  3. Paul M. Kulesa1,2

Article first published online: 2 AUG 2012

DOI: 10.1111/j.1755-148X.2012.01025.x

Issue

Pigment Cell & Melanoma Research

Pigment Cell & Melanoma Research

Volume 25, Issue 5, pages 573–583, September 2012

Additional Information

How to Cite

Bailey, C. M., Morrison, J. A. and Kulesa, P. M. (2012), Melanoma revives an embryonic migration program to promote plasticity and invasion. Pigment Cell & Melanoma Research, 25: 573–583. doi: 10.1111/j.1755-148X.2012.01025.x

Author Information

  1. 1

     Stowers Institute for Medical Research, Kansas City, MO, USA

  2. 2

     Department of Cell Biology and Anatomy, University of Kansas School of Medicine, Kansas City, KS, USA

*P. M. Kulesa, e-mail: pmk@stowers.org

Publication History

  1. Issue published online: 28 AUG 2012
  2. Article first published online: 2 AUG 2012
  3. Accepted manuscript online: 9 JUN 2012 09:04AM EST
  4. PUBLCATION DATA Received 24 February 2012, revised and accepted for publication 23 May 2012, published online 9 June 2012

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Keywords:

  • neural crest;
  • melanoma;
  • metastasis;
  • cell migration;
  • in vivo model

Summary

Cancer cells must regulate plasticity and invasion to survive and metastasize. However, the identification of targetable mechanisms to inhibit metastasis has been slow. Signaling programs that drive stem and progenitor cells during normal development offer an inroad to discover mechanisms common to metastasis. Using a chick embryo transplant model, we have compared molecular signaling programs of melanoma and their embryonic progenitors, the neural crest. We report that malignant melanoma cells hijack portions of the embryonic neural crest invasion program. Genes associated with neural crest induction, delamination, and migration are dynamically regulated by melanoma cells exposed to an embryonic neural crest microenvironment. Specifically, we demonstrate that metastatic melanoma cells exploit neural crest-related receptor tyrosine kinases to increase plasticity and facilitate invasion while primary melanocytes may actively suppress these responses under the same microenvironmental conditions. We conclude that aberrant regulation of neural crest developmental genes promotes plasticity and invasiveness in malignant melanoma.

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