Endothelial Phosphatase VE-PTP Participates in Vasculogenic Mimicry by Preventing Autophagic Degradation of VE-Cadherin

Daniel Delgado-Bellido; Concepción Bueno-Galera; Laura López-Jiménez; Angel Garcia-Diaz; F Javier Oliver

doi:10.3389/fonc.2020.00018

Endothelial Phosphatase VE-PTP Participates in Vasculogenic Mimicry by Preventing Autophagic Degradation of VE-Cadherin

Front Oncol. 2020 Jan 24:10:18. doi: 10.3389/fonc.2020.00018. eCollection 2020.

Authors

Daniel Delgado-Bellido¹, Concepción Bueno-Galera¹, Laura López-Jiménez¹, Angel Garcia-Diaz¹, F Javier Oliver¹

Affiliation

¹ Instituto de Parasitología y Biomedicina López Neyra, CSIC, CIBERONC, Granada, Spain.

Abstract

Aberrant extra-vascular expression of VE-cadherin has been observed in metastasis associated with Vasculogenic Mimicry (VM); we have recently shown that in VM prone cells VE-cadherin is mainly in the form of phospho-VE-cadherin in Y658 allowing increased plasticity that potentiates VM development in malignant cells. In the current study, we present results to show that human malignant melanoma cells VM+, express the VE-cadherin phosphatase VE-PTP. VE-PTP forms a complex with VE-Cadherin and p120-catenin and the presence of this complex act as a safeguard to prevent VE-Cadherin protein degradation by autophagy. Indeed, VE-PTP silencing results in complete degradation of VE-cadherin with the features of autophagy. In summary, this study shows that VE-PTP is involved in VM formation and disruption of VE-PTP/VE-Cadherin/p120 complex results in enhanced autophagy in aggressive VM⁺ cells. Thus, we identify VE-PTP as a key player in VM development by regulating VE-cadherin protein degradation through autophagy.

Keywords: VE-PTP; VE-cadherin; autophagy; melanoma; vascular endothelial receptor protein tyrosine phosphatase; vasculogenic mimicry (VM).