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Dilated Thin-Walled Blood and Lymphatic Vessels in Human Endometrium: A Potential Role for VEGF-D in Progestin-Induced Break-Through Bleeding

Progestins provide safe, effective and cheap options for contraception as well as the treatment of a variety of gynaecological disorders. Episodes of irregular endometrial bleeding or breakthrough bleeding (BTB) are a major unwanted side effect of progestin treatment, such that BTB is the leading ca...

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Autores principales: Donoghue, Jacqueline F., McGavigan, C. Jay, Lederman, Fiona L., Cann, Leonie M., Fu, Lulu, Dimitriadis, Eva, Girling, Jane E., Rogers, Peter A. W.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2012
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3284580/
https://www.ncbi.nlm.nih.gov/pubmed/22383980
http://dx.doi.org/10.1371/journal.pone.0030916
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author Donoghue, Jacqueline F.
McGavigan, C. Jay
Lederman, Fiona L.
Cann, Leonie M.
Fu, Lulu
Dimitriadis, Eva
Girling, Jane E.
Rogers, Peter A. W.
author_facet Donoghue, Jacqueline F.
McGavigan, C. Jay
Lederman, Fiona L.
Cann, Leonie M.
Fu, Lulu
Dimitriadis, Eva
Girling, Jane E.
Rogers, Peter A. W.
author_sort Donoghue, Jacqueline F.
collection PubMed
description Progestins provide safe, effective and cheap options for contraception as well as the treatment of a variety of gynaecological disorders. Episodes of irregular endometrial bleeding or breakthrough bleeding (BTB) are a major unwanted side effect of progestin treatment, such that BTB is the leading cause for discontinued use of an otherwise effective and popular medication. The cellular mechanisms leading to BTB are poorly understood. In this study, we make the novel finding that the large, dilated, thin walled vessels characteristic of human progestin-treated endometrium include both blood and lymphatic vessels. Increased blood and lymphatic vessel diameter are features of VEGF-D action in other tissues and we show by immunolocalisation and Western blotting that stromal cell decidualisation results in a significant increase in VEGF-D protein production, particularly of the proteolytically processed 21 kD form. Using a NOD/scid mouse model with xenografted human endometrium we were able to show that progestin treatment causes decidualisation, VEGF-D production and endometrial vessel dilation. Our results lead to a novel hypothesis to explain BTB, with stromal cell decidualisation rather than progestin treatment per se being the proposed causative event, and VEGF-D being the proposed effector agent.
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spelling pubmed-32845802012-03-01 Dilated Thin-Walled Blood and Lymphatic Vessels in Human Endometrium: A Potential Role for VEGF-D in Progestin-Induced Break-Through Bleeding Donoghue, Jacqueline F. McGavigan, C. Jay Lederman, Fiona L. Cann, Leonie M. Fu, Lulu Dimitriadis, Eva Girling, Jane E. Rogers, Peter A. W. PLoS One Research Article Progestins provide safe, effective and cheap options for contraception as well as the treatment of a variety of gynaecological disorders. Episodes of irregular endometrial bleeding or breakthrough bleeding (BTB) are a major unwanted side effect of progestin treatment, such that BTB is the leading cause for discontinued use of an otherwise effective and popular medication. The cellular mechanisms leading to BTB are poorly understood. In this study, we make the novel finding that the large, dilated, thin walled vessels characteristic of human progestin-treated endometrium include both blood and lymphatic vessels. Increased blood and lymphatic vessel diameter are features of VEGF-D action in other tissues and we show by immunolocalisation and Western blotting that stromal cell decidualisation results in a significant increase in VEGF-D protein production, particularly of the proteolytically processed 21 kD form. Using a NOD/scid mouse model with xenografted human endometrium we were able to show that progestin treatment causes decidualisation, VEGF-D production and endometrial vessel dilation. Our results lead to a novel hypothesis to explain BTB, with stromal cell decidualisation rather than progestin treatment per se being the proposed causative event, and VEGF-D being the proposed effector agent. Public Library of Science 2012-02-17 /pmc/articles/PMC3284580/ /pubmed/22383980 http://dx.doi.org/10.1371/journal.pone.0030916 Text en Donoghue et al. http://creativecommons.org/licenses/by/4.0/ This is an open-access article distributed under the terms of the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are properly credited.
spellingShingle Research Article
Donoghue, Jacqueline F.
McGavigan, C. Jay
Lederman, Fiona L.
Cann, Leonie M.
Fu, Lulu
Dimitriadis, Eva
Girling, Jane E.
Rogers, Peter A. W.
Dilated Thin-Walled Blood and Lymphatic Vessels in Human Endometrium: A Potential Role for VEGF-D in Progestin-Induced Break-Through Bleeding
title Dilated Thin-Walled Blood and Lymphatic Vessels in Human Endometrium: A Potential Role for VEGF-D in Progestin-Induced Break-Through Bleeding
title_full Dilated Thin-Walled Blood and Lymphatic Vessels in Human Endometrium: A Potential Role for VEGF-D in Progestin-Induced Break-Through Bleeding
title_fullStr Dilated Thin-Walled Blood and Lymphatic Vessels in Human Endometrium: A Potential Role for VEGF-D in Progestin-Induced Break-Through Bleeding
title_full_unstemmed Dilated Thin-Walled Blood and Lymphatic Vessels in Human Endometrium: A Potential Role for VEGF-D in Progestin-Induced Break-Through Bleeding
title_short Dilated Thin-Walled Blood and Lymphatic Vessels in Human Endometrium: A Potential Role for VEGF-D in Progestin-Induced Break-Through Bleeding
title_sort dilated thin-walled blood and lymphatic vessels in human endometrium: a potential role for vegf-d in progestin-induced break-through bleeding
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3284580/
https://www.ncbi.nlm.nih.gov/pubmed/22383980
http://dx.doi.org/10.1371/journal.pone.0030916
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