ΔNp63 knockdown mice: A mouse model for AEC syndrome

ΔNp63 knockdown mice: A mouse model for AEC syndrome

Dominant mutations in TP63 cause ankyloblepharon ectodermal dysplasia and clefting (AEC), an ectodermal dysplasia characterized by skin fragility. Since ΔNp63α is the predominantly expressed TP63 isoform in postnatal skin, we hypothesized that mutant ΔNp63α proteins are primarily responsible for ski...

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Main Authors: Maranke I. Koster, Barbara Marinari, Aimee S. Payne, Piranit N. Kantaputra, Antonio Costanzo, Dennis R. Roop
Format: Journal
Published: 2018
Subjects:
Biochemistry, Genetics and Molecular Biology
Medicine
Online Access:https://www.scopus.com/inward/record.uri?partnerID=HzOxMe3b&scp=69249091010&origin=inward
http://cmuir.cmu.ac.th/jspui/handle/6653943832/48855
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Institution: Chiang Mai University
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spelling th-cmuir.6653943832-488552018-08-16T02:14:17Z ΔNp63 knockdown mice: A mouse model for AEC syndrome Maranke I. Koster Barbara Marinari Aimee S. Payne Piranit N. Kantaputra Antonio Costanzo Dennis R. Roop Biochemistry, Genetics and Molecular Biology Medicine Dominant mutations in TP63 cause ankyloblepharon ectodermal dysplasia and clefting (AEC), an ectodermal dysplasia characterized by skin fragility. Since ΔNp63α is the predominantly expressed TP63 isoform in postnatal skin, we hypothesized that mutant ΔNp63α proteins are primarily responsible for skin fragility in AEC patients. We found that mutant ΔNp63α proteins expressed in AEC patients function as dominant-negative molecules, suggesting that the human AEC skin phenotype could be mimicked in mouse skin by downregulating ΔNp63α. Indeed, downregulating ΔNp63 expression in mouse epidermis caused severe skin erosions, which resembled lesions that develop in AEC patients. In both cases, lesions were characterized by suprabasal epidermal proliferation, delayed terminal differentiation, and basement membrane abnormalities. By failing to provide structural stability to the epidermis, these defects likely contribute to the observed skin fragility. The development of a mouse model for AEC will allow us to further unravel the genetic pathways that are normally regulated by ΔNp63 and that may be perturbed in AEC patients. Ultimately, these studies will not only contribute to our understanding of the molecular mechanisms that cause skin fragility in AEC patients, but may also result in the identification of targets for novel therapeutic approaches aimed at treating skin erosions. © 2009 Wiley-Liss, Inc. 2018-08-16T02:05:53Z 2018-08-16T02:05:53Z 2009-09-01 Journal 15524833 15524825 2-s2.0-69249091010 10.1002/ajmg.a.32794 https://www.scopus.com/inward/record.uri?partnerID=HzOxMe3b&scp=69249091010&origin=inward http://cmuir.cmu.ac.th/jspui/handle/6653943832/48855
institution Chiang Mai University
building Chiang Mai University Library
country Thailand
collection CMU Intellectual Repository
topic Biochemistry, Genetics and Molecular Biology
Medicine
spellingShingle Biochemistry, Genetics and Molecular Biology
Medicine
Maranke I. Koster
Barbara Marinari
Aimee S. Payne
Piranit N. Kantaputra
Antonio Costanzo
Dennis R. Roop
ΔNp63 knockdown mice: A mouse model for AEC syndrome
description Dominant mutations in TP63 cause ankyloblepharon ectodermal dysplasia and clefting (AEC), an ectodermal dysplasia characterized by skin fragility. Since ΔNp63α is the predominantly expressed TP63 isoform in postnatal skin, we hypothesized that mutant ΔNp63α proteins are primarily responsible for skin fragility in AEC patients. We found that mutant ΔNp63α proteins expressed in AEC patients function as dominant-negative molecules, suggesting that the human AEC skin phenotype could be mimicked in mouse skin by downregulating ΔNp63α. Indeed, downregulating ΔNp63 expression in mouse epidermis caused severe skin erosions, which resembled lesions that develop in AEC patients. In both cases, lesions were characterized by suprabasal epidermal proliferation, delayed terminal differentiation, and basement membrane abnormalities. By failing to provide structural stability to the epidermis, these defects likely contribute to the observed skin fragility. The development of a mouse model for AEC will allow us to further unravel the genetic pathways that are normally regulated by ΔNp63 and that may be perturbed in AEC patients. Ultimately, these studies will not only contribute to our understanding of the molecular mechanisms that cause skin fragility in AEC patients, but may also result in the identification of targets for novel therapeutic approaches aimed at treating skin erosions. © 2009 Wiley-Liss, Inc.
format Journal
author Maranke I. Koster
Barbara Marinari
Aimee S. Payne
Piranit N. Kantaputra
Antonio Costanzo
Dennis R. Roop
author_facet Maranke I. Koster
Barbara Marinari
Aimee S. Payne
Piranit N. Kantaputra
Antonio Costanzo
Dennis R. Roop
author_sort Maranke I. Koster
title ΔNp63 knockdown mice: A mouse model for AEC syndrome
title_short ΔNp63 knockdown mice: A mouse model for AEC syndrome
title_full ΔNp63 knockdown mice: A mouse model for AEC syndrome
title_fullStr ΔNp63 knockdown mice: A mouse model for AEC syndrome
title_full_unstemmed ΔNp63 knockdown mice: A mouse model for AEC syndrome
title_sort δnp63 knockdown mice: a mouse model for aec syndrome
publishDate 2018
url https://www.scopus.com/inward/record.uri?partnerID=HzOxMe3b&scp=69249091010&origin=inward
http://cmuir.cmu.ac.th/jspui/handle/6653943832/48855
_version_ 1681423305214525440

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