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The role of the ShcD and RET interaction in neuroblastoma survival and migration.

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posted on 2018-04-24, 13:23 authored by Z. A. Mabruk, S. B. M. Ahmed, A. C. Thomas, Sally A. Prigent
Preliminary screening data showed that the ShcD adaptor protein associates with the proto-oncogene RET receptor tyrosine kinase. In the present study, we aimed to investigate the molecular interaction between ShcD and RET in human neuroblastoma cells and study the functional impact of this interaction. We were able to show that ShcD immunoprecipitated with RET from SK-N-AS neuroblastoma cell lysates upon GDNF treatment. This result was validated by ShcD-RET co-localization, which was visualized using a fluorescence microscope. ShcD-RET coexpression promoted ShcD and RET endosomal localization, resulting in unexpected inhibition of the downstream ERK and AKT pathways. Interestingly, ShcD-RET association reduced the viability and migration of SK-N-AS cells. Although ShcD was previously shown to trigger melanoma cell migration and tumorigenesis, our data showed an opposite role for ShcD in neuroblastoma SK-N-AS cells via its association with RET in GDNF-treated cells. In conclusion, ShcD acts as a switch molecule that promotes contrasting biological responses depending on the stimulus ad cell type.

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Citation

Biochemistry and Biophysics Reports, 2018, 13, pp. 99-108

Author affiliation

/Organisation/COLLEGE OF LIFE SCIENCES/Biological Sciences/Molecular & Cell Biology

Version

  • VoR (Version of Record)

Published in

Biochemistry and Biophysics Reports

Publisher

Elsevier

eissn

2405-5808

Acceptance date

2018-01-11

Copyright date

2018

Available date

2018-04-24

Publisher version

https://www.sciencedirect.com/science/article/pii/S2405580817301759?via=ihub#!

Language

en

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