Development of skin-humanized mouse models of pachyonychia congenita

Marta García; Fernando Larcher; Robyn P. Hickerson; Eulalia Baselga; Sancy A. Leachman; Roger L. Kaspar; Marcela Del Rio

doi:10.1038/jid.2010.353

Development of skin-humanized mouse models of pachyonychia congenita

Marta García, Fernando Larcher, Robyn P. Hickerson, Eulalia Baselga, Sancy A. Leachman, Roger L. Kaspar, Marcela Del Rio

Research output: Contribution to journal › Article › peer-review

33 Scopus citations

Abstract

Molecular characterization and assessment of therapeutic outcomes for inherited cutaneous disorders requires faithful preclinical models. In this study we report the establishment of two different skin-humanized pachyonychia congenita (PC) model systems, based on permanent engraftment of bioengineered skin equivalents generated from patient skin cells onto immunodeficient mice. Using keratinocytes and fibroblasts isolated from unaffected skin biopsies of two PC patients carrying the p.Asn171Lys mutation of the keratin 6a gene (KRT6A), we were able to regenerate PC-derived human skin that appeared phenotypically normal, but developed sustained PC features after the use of an acute hyperproliferative stimulus (i.e., tape stripping). In contrast, the use of keratinocytes from an affected area (i.e., plantar callus) from a different patient carrying the KRT6A mutation p.Asn171Asp led to a full recapitulation of the phenotype that included marked acanthosis and epidermal blistering after minor trauma. The ability to generate large numbers of PC skin-engrafted mice will enable the testing of novel pharmacological or gene-based therapies for this as yet untreatable disease.

Original language	English (US)
Pages (from-to)	1053-1060
Number of pages	8
Journal	Journal of Investigative Dermatology
Volume	131
Issue number	5
DOIs	https://doi.org/10.1038/jid.2010.353
State	Published - May 2011
Externally published	Yes

ASJC Scopus subject areas

Biochemistry
Molecular Biology
Dermatology
Cell Biology

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10.1038/jid.2010.353

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@article{254c1336a8324944a35fcce609127ac6,

title = "Development of skin-humanized mouse models of pachyonychia congenita",

abstract = "Molecular characterization and assessment of therapeutic outcomes for inherited cutaneous disorders requires faithful preclinical models. In this study we report the establishment of two different skin-humanized pachyonychia congenita (PC) model systems, based on permanent engraftment of bioengineered skin equivalents generated from patient skin cells onto immunodeficient mice. Using keratinocytes and fibroblasts isolated from unaffected skin biopsies of two PC patients carrying the p.Asn171Lys mutation of the keratin 6a gene (KRT6A), we were able to regenerate PC-derived human skin that appeared phenotypically normal, but developed sustained PC features after the use of an acute hyperproliferative stimulus (i.e., tape stripping). In contrast, the use of keratinocytes from an affected area (i.e., plantar callus) from a different patient carrying the KRT6A mutation p.Asn171Asp led to a full recapitulation of the phenotype that included marked acanthosis and epidermal blistering after minor trauma. The ability to generate large numbers of PC skin-engrafted mice will enable the testing of novel pharmacological or gene-based therapies for this as yet untreatable disease.",

author = "Marta Garc{\'i}a and Fernando Larcher and Hickerson, {Robyn P.} and Eulalia Baselga and Leachman, {Sancy A.} and Kaspar, {Roger L.} and {Del Rio}, Marcela",

note = "Funding Information: We are grateful for the participation of the PC patients, without whom this study would not have been possible. We also thank Pachyonychia Congenita Project and the International Pachyonychia Congenita Consortium (IPCC) for their support and guidance and to Irwin McLean, University of Dundee, for help with the manuscript. We also thank Almudena Holguin, Blanca Duarte, and Maria Luisa Retamosa for skin grafting and Jesus Martinez for animal care. This work was supported in part by grants (R43AR055881) from the National Institutes of Health (to RLK), SAF2007-61019 and SAF2010-16976 from the Spanish Ministry of Science and Innovation (to MDR), PI081054 from ISCIII, and P-BIO-0306-2006 from Comunidad de Madrid (to FL). The CIBER for Rare Diseases is an initiative of the Spanish ISCIII. We would very much like to dedicate this paper to the memory of Dr Estela E Medrano.",

year = "2011",

month = may,

doi = "10.1038/jid.2010.353",

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volume = "131",

pages = "1053--1060",

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T1 - Development of skin-humanized mouse models of pachyonychia congenita

AU - García, Marta

AU - Larcher, Fernando

AU - Hickerson, Robyn P.

AU - Baselga, Eulalia

AU - Leachman, Sancy A.

AU - Kaspar, Roger L.

AU - Del Rio, Marcela

N1 - Funding Information: We are grateful for the participation of the PC patients, without whom this study would not have been possible. We also thank Pachyonychia Congenita Project and the International Pachyonychia Congenita Consortium (IPCC) for their support and guidance and to Irwin McLean, University of Dundee, for help with the manuscript. We also thank Almudena Holguin, Blanca Duarte, and Maria Luisa Retamosa for skin grafting and Jesus Martinez for animal care. This work was supported in part by grants (R43AR055881) from the National Institutes of Health (to RLK), SAF2007-61019 and SAF2010-16976 from the Spanish Ministry of Science and Innovation (to MDR), PI081054 from ISCIII, and P-BIO-0306-2006 from Comunidad de Madrid (to FL). The CIBER for Rare Diseases is an initiative of the Spanish ISCIII. We would very much like to dedicate this paper to the memory of Dr Estela E Medrano.

PY - 2011/5

Y1 - 2011/5

N2 - Molecular characterization and assessment of therapeutic outcomes for inherited cutaneous disorders requires faithful preclinical models. In this study we report the establishment of two different skin-humanized pachyonychia congenita (PC) model systems, based on permanent engraftment of bioengineered skin equivalents generated from patient skin cells onto immunodeficient mice. Using keratinocytes and fibroblasts isolated from unaffected skin biopsies of two PC patients carrying the p.Asn171Lys mutation of the keratin 6a gene (KRT6A), we were able to regenerate PC-derived human skin that appeared phenotypically normal, but developed sustained PC features after the use of an acute hyperproliferative stimulus (i.e., tape stripping). In contrast, the use of keratinocytes from an affected area (i.e., plantar callus) from a different patient carrying the KRT6A mutation p.Asn171Asp led to a full recapitulation of the phenotype that included marked acanthosis and epidermal blistering after minor trauma. The ability to generate large numbers of PC skin-engrafted mice will enable the testing of novel pharmacological or gene-based therapies for this as yet untreatable disease.

AB - Molecular characterization and assessment of therapeutic outcomes for inherited cutaneous disorders requires faithful preclinical models. In this study we report the establishment of two different skin-humanized pachyonychia congenita (PC) model systems, based on permanent engraftment of bioengineered skin equivalents generated from patient skin cells onto immunodeficient mice. Using keratinocytes and fibroblasts isolated from unaffected skin biopsies of two PC patients carrying the p.Asn171Lys mutation of the keratin 6a gene (KRT6A), we were able to regenerate PC-derived human skin that appeared phenotypically normal, but developed sustained PC features after the use of an acute hyperproliferative stimulus (i.e., tape stripping). In contrast, the use of keratinocytes from an affected area (i.e., plantar callus) from a different patient carrying the KRT6A mutation p.Asn171Asp led to a full recapitulation of the phenotype that included marked acanthosis and epidermal blistering after minor trauma. The ability to generate large numbers of PC skin-engrafted mice will enable the testing of novel pharmacological or gene-based therapies for this as yet untreatable disease.

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Development of skin-humanized mouse models of pachyonychia congenita

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