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Race Does Not Predict Melanocyte Heterogeneous Responses to Dermal Fibroblast-Derived Mediators

INTRODUCTION: Abnormal pigmentation following cutaneous injury causes significant patient distress and represents a barrier to recovery. Wound depth and patient characteristics influence scar pigmentation. However, we know little about the pathophysiology leading to hyperpigmentation in healed shall...

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Autores principales: Sirimahachaiyakul, Pornthep, Sood, Ravi F., Muffley, Lara A., Seaton, Max, Lin, Cheng-Ta, Qiao, Liang, Armaly, Jeffrey S., Hocking, Anne M., Gibran, Nicole S.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2015
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4587942/
https://www.ncbi.nlm.nih.gov/pubmed/26418010
http://dx.doi.org/10.1371/journal.pone.0139135
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author Sirimahachaiyakul, Pornthep
Sood, Ravi F.
Muffley, Lara A.
Seaton, Max
Lin, Cheng-Ta
Qiao, Liang
Armaly, Jeffrey S.
Hocking, Anne M.
Gibran, Nicole S.
author_facet Sirimahachaiyakul, Pornthep
Sood, Ravi F.
Muffley, Lara A.
Seaton, Max
Lin, Cheng-Ta
Qiao, Liang
Armaly, Jeffrey S.
Hocking, Anne M.
Gibran, Nicole S.
author_sort Sirimahachaiyakul, Pornthep
collection PubMed
description INTRODUCTION: Abnormal pigmentation following cutaneous injury causes significant patient distress and represents a barrier to recovery. Wound depth and patient characteristics influence scar pigmentation. However, we know little about the pathophysiology leading to hyperpigmentation in healed shallow wounds and hypopigmentation in deep dermal wound scars. We sought to determine whether dermal fibroblast signaling influences melanocyte responses. METHODS AND MATERIALS: Epidermal melanocytes from three Caucasians and three African-Americans were genotyped for single nucleotide polymorphisms (SNPs) across the entire genome. Melanocyte genetic profiles were determined using principal component analysis. We assessed melanocyte phenotype and gene expression in response to dermal fibroblast-conditioned medium and determined potential mesenchymal mediators by proteome profiling the fibroblast-conditioned medium. RESULTS: Six melanocyte samples demonstrated significant variability in phenotype and gene expression at baseline and in response to fibroblast-conditioned medium. Genetic profiling for SNPs in receptors for 13 identified soluble fibroblast-secreted mediators demonstrated considerable heterogeneity, potentially explaining the variable melanocyte responses to fibroblast-conditioned medium. DISCUSSION: Our data suggest that melanocytes respond to dermal fibroblast-derived mediators independent of keratinocytes and raise the possibility that mesenchymal-epidermal interactions influence skin pigmentation during cutaneous scarring.
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spelling pubmed-45879422015-10-02 Race Does Not Predict Melanocyte Heterogeneous Responses to Dermal Fibroblast-Derived Mediators Sirimahachaiyakul, Pornthep Sood, Ravi F. Muffley, Lara A. Seaton, Max Lin, Cheng-Ta Qiao, Liang Armaly, Jeffrey S. Hocking, Anne M. Gibran, Nicole S. PLoS One Research Article INTRODUCTION: Abnormal pigmentation following cutaneous injury causes significant patient distress and represents a barrier to recovery. Wound depth and patient characteristics influence scar pigmentation. However, we know little about the pathophysiology leading to hyperpigmentation in healed shallow wounds and hypopigmentation in deep dermal wound scars. We sought to determine whether dermal fibroblast signaling influences melanocyte responses. METHODS AND MATERIALS: Epidermal melanocytes from three Caucasians and three African-Americans were genotyped for single nucleotide polymorphisms (SNPs) across the entire genome. Melanocyte genetic profiles were determined using principal component analysis. We assessed melanocyte phenotype and gene expression in response to dermal fibroblast-conditioned medium and determined potential mesenchymal mediators by proteome profiling the fibroblast-conditioned medium. RESULTS: Six melanocyte samples demonstrated significant variability in phenotype and gene expression at baseline and in response to fibroblast-conditioned medium. Genetic profiling for SNPs in receptors for 13 identified soluble fibroblast-secreted mediators demonstrated considerable heterogeneity, potentially explaining the variable melanocyte responses to fibroblast-conditioned medium. DISCUSSION: Our data suggest that melanocytes respond to dermal fibroblast-derived mediators independent of keratinocytes and raise the possibility that mesenchymal-epidermal interactions influence skin pigmentation during cutaneous scarring. Public Library of Science 2015-09-29 /pmc/articles/PMC4587942/ /pubmed/26418010 http://dx.doi.org/10.1371/journal.pone.0139135 Text en © 2015 Sirimahachaiyakul 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
Sirimahachaiyakul, Pornthep
Sood, Ravi F.
Muffley, Lara A.
Seaton, Max
Lin, Cheng-Ta
Qiao, Liang
Armaly, Jeffrey S.
Hocking, Anne M.
Gibran, Nicole S.
Race Does Not Predict Melanocyte Heterogeneous Responses to Dermal Fibroblast-Derived Mediators
title Race Does Not Predict Melanocyte Heterogeneous Responses to Dermal Fibroblast-Derived Mediators
title_full Race Does Not Predict Melanocyte Heterogeneous Responses to Dermal Fibroblast-Derived Mediators
title_fullStr Race Does Not Predict Melanocyte Heterogeneous Responses to Dermal Fibroblast-Derived Mediators
title_full_unstemmed Race Does Not Predict Melanocyte Heterogeneous Responses to Dermal Fibroblast-Derived Mediators
title_short Race Does Not Predict Melanocyte Heterogeneous Responses to Dermal Fibroblast-Derived Mediators
title_sort race does not predict melanocyte heterogeneous responses to dermal fibroblast-derived mediators
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4587942/
https://www.ncbi.nlm.nih.gov/pubmed/26418010
http://dx.doi.org/10.1371/journal.pone.0139135
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