A Human Integrin-α3 Mutation Confers Major Renal Developmental Defects

The development of the mammalian kidney is a highly complex process dependent upon the interplay of various cell types, secreted morphogens, and the extra-cellular matrix (ECM). Although integrins are the most important receptors for ECM proteins and are ubiquitously expressed during kidney developm...

Descripción completa

Detalles Bibliográficos
Autores principales: Shukrun, Rachel, Vivante, Asaf, Pleniceanu, Oren, Vax, Einav, Anikster, Yair, Dekel, Benjamin, Lotan, Danny
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2014
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3951280/
https://www.ncbi.nlm.nih.gov/pubmed/24621570
http://dx.doi.org/10.1371/journal.pone.0090879
_version_ 1782307104074235904
author Shukrun, Rachel
Vivante, Asaf
Pleniceanu, Oren
Vax, Einav
Anikster, Yair
Dekel, Benjamin
Lotan, Danny
author_facet Shukrun, Rachel
Vivante, Asaf
Pleniceanu, Oren
Vax, Einav
Anikster, Yair
Dekel, Benjamin
Lotan, Danny
author_sort Shukrun, Rachel
collection PubMed
description The development of the mammalian kidney is a highly complex process dependent upon the interplay of various cell types, secreted morphogens, and the extra-cellular matrix (ECM). Although integrins are the most important receptors for ECM proteins and are ubiquitously expressed during kidney development, mice lacking expression of integrin α3 (Itga3) do not demonstrate a reduced number of nephrons, but mostly a disorganized GBM (glomerular basement membrane) leading to proteinuria. Thus, ITGA3 is considered mostly a passive GBM stabilizer and not an active player in nephrogenesis. Recently, mutations in the human ITGA3 were shown to cause congenital nephrotic syndrome, epidermolysis bullosa and interstitial lung disease, otherwise termed NEP syndrome (Nephrotic syndrome, Epidermolysis bullosa and Pulmonary disease). Herein, we performed histological and molecular analysis on the kidneys of a single patient from the initial cohort harboring an ITGA3 mutation, to illuminate the role of ITGA3 in human renal development. We show the patient to harbor a unique phenotype at birth, including severe unilateral renal hypodysplasia. Interrogation of global gene expression in the hypodysplastic kidney versus three controls (fetal, child and adult kidneys) revealed perturbed expression in several renal developmental pathways implicated in hypodysplasia, including the Wnt, BMP (bone morphogenetic protein) and TGF (transforming growth factor) pathways. Moreover, the affected kidney showed upregulation of early embryonic genes (e.g. OCT4 and PAX8) concomitant with downregulated kidney differentiation markers, implying a defect in proper renal differentiation. In conclusion, we show for the first time that ITGA3 is not merely a passive anchor for renal ECM proteins, as predicted by mouse models. Instead, our results may suggest it plays a central role in the interplay of cells, morphogens and ECM, required for proper nephrogenesis, thus adding ITGA3 to the list of CAKUT (congenital anomalies of the kidney and urinary tract)-causing genes.
format Online
Article
Text
id pubmed-3951280
institution National Center for Biotechnology Information
language English
publishDate 2014
publisher Public Library of Science
record_format MEDLINE/PubMed
spelling pubmed-39512802014-03-13 A Human Integrin-α3 Mutation Confers Major Renal Developmental Defects Shukrun, Rachel Vivante, Asaf Pleniceanu, Oren Vax, Einav Anikster, Yair Dekel, Benjamin Lotan, Danny PLoS One Research Article The development of the mammalian kidney is a highly complex process dependent upon the interplay of various cell types, secreted morphogens, and the extra-cellular matrix (ECM). Although integrins are the most important receptors for ECM proteins and are ubiquitously expressed during kidney development, mice lacking expression of integrin α3 (Itga3) do not demonstrate a reduced number of nephrons, but mostly a disorganized GBM (glomerular basement membrane) leading to proteinuria. Thus, ITGA3 is considered mostly a passive GBM stabilizer and not an active player in nephrogenesis. Recently, mutations in the human ITGA3 were shown to cause congenital nephrotic syndrome, epidermolysis bullosa and interstitial lung disease, otherwise termed NEP syndrome (Nephrotic syndrome, Epidermolysis bullosa and Pulmonary disease). Herein, we performed histological and molecular analysis on the kidneys of a single patient from the initial cohort harboring an ITGA3 mutation, to illuminate the role of ITGA3 in human renal development. We show the patient to harbor a unique phenotype at birth, including severe unilateral renal hypodysplasia. Interrogation of global gene expression in the hypodysplastic kidney versus three controls (fetal, child and adult kidneys) revealed perturbed expression in several renal developmental pathways implicated in hypodysplasia, including the Wnt, BMP (bone morphogenetic protein) and TGF (transforming growth factor) pathways. Moreover, the affected kidney showed upregulation of early embryonic genes (e.g. OCT4 and PAX8) concomitant with downregulated kidney differentiation markers, implying a defect in proper renal differentiation. In conclusion, we show for the first time that ITGA3 is not merely a passive anchor for renal ECM proteins, as predicted by mouse models. Instead, our results may suggest it plays a central role in the interplay of cells, morphogens and ECM, required for proper nephrogenesis, thus adding ITGA3 to the list of CAKUT (congenital anomalies of the kidney and urinary tract)-causing genes. Public Library of Science 2014-03-12 /pmc/articles/PMC3951280/ /pubmed/24621570 http://dx.doi.org/10.1371/journal.pone.0090879 Text en © 2014 Shukrun 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
Shukrun, Rachel
Vivante, Asaf
Pleniceanu, Oren
Vax, Einav
Anikster, Yair
Dekel, Benjamin
Lotan, Danny
A Human Integrin-α3 Mutation Confers Major Renal Developmental Defects
title A Human Integrin-α3 Mutation Confers Major Renal Developmental Defects
title_full A Human Integrin-α3 Mutation Confers Major Renal Developmental Defects
title_fullStr A Human Integrin-α3 Mutation Confers Major Renal Developmental Defects
title_full_unstemmed A Human Integrin-α3 Mutation Confers Major Renal Developmental Defects
title_short A Human Integrin-α3 Mutation Confers Major Renal Developmental Defects
title_sort human integrin-α3 mutation confers major renal developmental defects
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3951280/
https://www.ncbi.nlm.nih.gov/pubmed/24621570
http://dx.doi.org/10.1371/journal.pone.0090879
work_keys_str_mv AT shukrunrachel ahumanintegrina3mutationconfersmajorrenaldevelopmentaldefects
AT vivanteasaf ahumanintegrina3mutationconfersmajorrenaldevelopmentaldefects
AT pleniceanuoren ahumanintegrina3mutationconfersmajorrenaldevelopmentaldefects
AT vaxeinav ahumanintegrina3mutationconfersmajorrenaldevelopmentaldefects
AT aniksteryair ahumanintegrina3mutationconfersmajorrenaldevelopmentaldefects
AT dekelbenjamin ahumanintegrina3mutationconfersmajorrenaldevelopmentaldefects
AT lotandanny ahumanintegrina3mutationconfersmajorrenaldevelopmentaldefects
AT shukrunrachel humanintegrina3mutationconfersmajorrenaldevelopmentaldefects
AT vivanteasaf humanintegrina3mutationconfersmajorrenaldevelopmentaldefects
AT pleniceanuoren humanintegrina3mutationconfersmajorrenaldevelopmentaldefects
AT vaxeinav humanintegrina3mutationconfersmajorrenaldevelopmentaldefects
AT aniksteryair humanintegrina3mutationconfersmajorrenaldevelopmentaldefects
AT dekelbenjamin humanintegrina3mutationconfersmajorrenaldevelopmentaldefects
AT lotandanny humanintegrina3mutationconfersmajorrenaldevelopmentaldefects

Ejemplares similares