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Highly Conserved Testicular Localization of Claudin-11 in Normal and Impaired Spermatogenesis

In this study we tested expression of tight junction proteins in human, mouse and rat and analyzed the localization of claudin-11 in testis of patients with normal and impaired spermatogenesis. Recent concepts generated in mice suggest that the stage-specifically expressed claudin-3 acts as a basal...

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Autores principales: Stammler, Angelika, Lüftner, Benjamin Udo, Kliesch, Sabine, Weidner, Wolfgang, Bergmann, Martin, Middendorff, Ralf, Konrad, Lutz
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2016
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4972306/
https://www.ncbi.nlm.nih.gov/pubmed/27486954
http://dx.doi.org/10.1371/journal.pone.0160349
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author Stammler, Angelika
Lüftner, Benjamin Udo
Kliesch, Sabine
Weidner, Wolfgang
Bergmann, Martin
Middendorff, Ralf
Konrad, Lutz
author_facet Stammler, Angelika
Lüftner, Benjamin Udo
Kliesch, Sabine
Weidner, Wolfgang
Bergmann, Martin
Middendorff, Ralf
Konrad, Lutz
author_sort Stammler, Angelika
collection PubMed
description In this study we tested expression of tight junction proteins in human, mouse and rat and analyzed the localization of claudin-11 in testis of patients with normal and impaired spermatogenesis. Recent concepts generated in mice suggest that the stage-specifically expressed claudin-3 acts as a basal barrier, sealing the seminiferous epithelium during migration of spermatocytes. Corresponding mechanisms have never been demonstrated in humans. Testicular biopsies (n = 103) from five distinct groups were analyzed: normal spermatogenesis (NSP, n = 28), hypospermatogenesis (Hyp, n = 24), maturation arrest at the level of primary spermatocytes (MA, n = 24), Sertoli cell only syndrome (SCO, n = 19), and spermatogonial arrest (SGA, n = 8). Protein expression of claudin-3, -11 and occludin was analyzed. Human, mice and rat testis robustly express claudin-11 protein. Occludin was detected in mouse and rat and claudin-3 was found only in mice. Thus, we selected claudin-11 for further analysis of localization. In NSP, claudin-11 is located at Sertoli-Sertoli junctions and in Sertoli cell contacts towards spermatogonia. Typically, claudin-11 patches do not reach the basal membrane, unless flanked by the Sertoli cell body or patches between two Sertoli cell bodies. The amount of basal claudin-11 patches was found to be increased in impaired spermatogenesis. Only claudin-11 is expressed in all three species examined. The claudin-11 pattern is robust in man with impaired spermatogenesis, but the proportion of localization is altered in SCO and MA. We conclude that claudin-11 might represent the essential component of the BTB in human.
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spelling pubmed-49723062016-08-18 Highly Conserved Testicular Localization of Claudin-11 in Normal and Impaired Spermatogenesis Stammler, Angelika Lüftner, Benjamin Udo Kliesch, Sabine Weidner, Wolfgang Bergmann, Martin Middendorff, Ralf Konrad, Lutz PLoS One Research Article In this study we tested expression of tight junction proteins in human, mouse and rat and analyzed the localization of claudin-11 in testis of patients with normal and impaired spermatogenesis. Recent concepts generated in mice suggest that the stage-specifically expressed claudin-3 acts as a basal barrier, sealing the seminiferous epithelium during migration of spermatocytes. Corresponding mechanisms have never been demonstrated in humans. Testicular biopsies (n = 103) from five distinct groups were analyzed: normal spermatogenesis (NSP, n = 28), hypospermatogenesis (Hyp, n = 24), maturation arrest at the level of primary spermatocytes (MA, n = 24), Sertoli cell only syndrome (SCO, n = 19), and spermatogonial arrest (SGA, n = 8). Protein expression of claudin-3, -11 and occludin was analyzed. Human, mice and rat testis robustly express claudin-11 protein. Occludin was detected in mouse and rat and claudin-3 was found only in mice. Thus, we selected claudin-11 for further analysis of localization. In NSP, claudin-11 is located at Sertoli-Sertoli junctions and in Sertoli cell contacts towards spermatogonia. Typically, claudin-11 patches do not reach the basal membrane, unless flanked by the Sertoli cell body or patches between two Sertoli cell bodies. The amount of basal claudin-11 patches was found to be increased in impaired spermatogenesis. Only claudin-11 is expressed in all three species examined. The claudin-11 pattern is robust in man with impaired spermatogenesis, but the proportion of localization is altered in SCO and MA. We conclude that claudin-11 might represent the essential component of the BTB in human. Public Library of Science 2016-08-03 /pmc/articles/PMC4972306/ /pubmed/27486954 http://dx.doi.org/10.1371/journal.pone.0160349 Text en © 2016 Stammler 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 (http://creativecommons.org/licenses/by/4.0/) , which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are credited.
spellingShingle Research Article
Stammler, Angelika
Lüftner, Benjamin Udo
Kliesch, Sabine
Weidner, Wolfgang
Bergmann, Martin
Middendorff, Ralf
Konrad, Lutz
Highly Conserved Testicular Localization of Claudin-11 in Normal and Impaired Spermatogenesis
title Highly Conserved Testicular Localization of Claudin-11 in Normal and Impaired Spermatogenesis
title_full Highly Conserved Testicular Localization of Claudin-11 in Normal and Impaired Spermatogenesis
title_fullStr Highly Conserved Testicular Localization of Claudin-11 in Normal and Impaired Spermatogenesis
title_full_unstemmed Highly Conserved Testicular Localization of Claudin-11 in Normal and Impaired Spermatogenesis
title_short Highly Conserved Testicular Localization of Claudin-11 in Normal and Impaired Spermatogenesis
title_sort highly conserved testicular localization of claudin-11 in normal and impaired spermatogenesis
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4972306/
https://www.ncbi.nlm.nih.gov/pubmed/27486954
http://dx.doi.org/10.1371/journal.pone.0160349
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