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13 November 2018 A high level of TGF-B1 promotes endometriosis development via cell migration, adhesiveness, colonization, and invasiveness
Upendra Kumar Soni, Sangappa Basanna Chadchan, Vijay Kumar, Vaibhave Ubba, Mohammad Tariq Ali Khan, Budai Shanmukha Vivek Vinod, Rituraj Konwar, Himangsu Kousik Bora, Srikanta Kumar Rath, Sharad Sharma, Rajesh Kumar Jha
Author Affiliations +
Abstract

Endometriosis is a prevalent gynecological disorder that eventually gives rise to painful invasive lesions. Increased levels of transforming growth factor-beta 1 (TGF-B1) have been reported in endometriosis. However, details of the effects of high TGF-B1 on downstream signaling in ectopic endometrial tissue remain obscure. We induced endometriotic lesions in mice by surgical auto-transplantation of endometrial tissues to the peritoneal regions. We then treated endometriotic (ectopic and eutopic endometrial tissues) and nonendometriotic (only eutopic endometrial tissues) animal groups with either active TGF-B1 or PBS. Our results demonstrate that externally supplemented TGF-B1 increases the growth of ectopically implanted endometrial tissues in mice, possibly via SMAD2/3 activation and PTEN suppression. Adhesion molecules integrins (beta3 and beta8) and FAK were upregulated in the ectopic endometrial tissue when TGF-B1 was administered. Phosphorylated E-cadherin, N-cadherin, and vimentin were enhanced in the ectopic endometrial tissue in the presence of TGF-B1 in the mouse model, and correlated with epithelial-mesenchymal transition (EMT) in ovarian endometriotic cells of human origin. Furthermore, in response to TGF-B1, the expression of RHOGTPases (RAC1, RHOC, and RHOG) was increased in the human endometriotic cells (ovarian cyst derived cells from endometriosis patient) and tissues from the mouse model of endometriosis (ectopic endometrial tissue). TGF-B1 enhanced the migratory, invasive, and colonizing potential of human endometriotic cells. Therefore, we conclude that TGF-B1 potentiates the adhesion of ectopic endometrial cells/tissues in the peritoneal region by enhancing the integrin and FAK signaling axis, and also migration via cadherin-mediated EMT and RHOGTPase signaling cascades.

Summary Sentence

TGF-B1 regulates the pathophysiology of endometriosis by specifically enhancing the migration, attachment, proliferation, colonization, and invasiveness of floating endometriotic cells or tissues, via the integrin-FAK, cadherin, and RHOGTPase signaling cascades.

© The Author(s) 2018. Published by Oxford University Press on behalf of Society for the Study of Reproduction. All rights reserved. For permissions, please e-mail: journals.permissions@oup.com
Upendra Kumar Soni, Sangappa Basanna Chadchan, Vijay Kumar, Vaibhave Ubba, Mohammad Tariq Ali Khan, Budai Shanmukha Vivek Vinod, Rituraj Konwar, Himangsu Kousik Bora, Srikanta Kumar Rath, Sharad Sharma, and Rajesh Kumar Jha "A high level of TGF-B1 promotes endometriosis development via cell migration, adhesiveness, colonization, and invasiveness," Biology of Reproduction 100(4), 917-938, (13 November 2018). https://doi.org/10.1093/biolre/ioy242
Received: 29 August 2017; Accepted: 12 November 2018; Published: 13 November 2018
KEYWORDS
3D-spheroids
cadherins
cell migration
colonization
EMT
focal adhesion kinase (FAK)
integrins
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