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Cleavage of Histone 3 by Cathepsin D in the Involuting Mammary Gland

The post-lactational regression of mammary gland is a complex multi-step process designed to conserve the biological function of the gland for next pregnancy. This developmental stage is a biological intrigue with great relevance to breast cancer research, and thus has been the subject of intensive...

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Autores principales: Khalkhali-Ellis, Zhila, Goossens, William, Margaryan, Naira V., Hendrix, Mary J. C.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2014
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4108390/
https://www.ncbi.nlm.nih.gov/pubmed/25054204
http://dx.doi.org/10.1371/journal.pone.0103230
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author Khalkhali-Ellis, Zhila
Goossens, William
Margaryan, Naira V.
Hendrix, Mary J. C.
author_facet Khalkhali-Ellis, Zhila
Goossens, William
Margaryan, Naira V.
Hendrix, Mary J. C.
author_sort Khalkhali-Ellis, Zhila
collection PubMed
description The post-lactational regression of mammary gland is a complex multi-step process designed to conserve the biological function of the gland for next pregnancy. This developmental stage is a biological intrigue with great relevance to breast cancer research, and thus has been the subject of intensive scrutiny. Multipronged studies (microarray, proteomics profiling, animal knock-out models) have provided a repertoire of genes critical to involution. However, the caveat of these approaches remains in their failure to reveal post-translational modification(s), an emerging and critical aspect of gene regulation in developmental processes and mammary gland remodeling. The massive surge in the lysosomal enzymes concurrent with the onset of involution has been known for decades, and considered essential for “clearance” purposes. However, functional significance of these enzymes in diverse biological processes distinct from their proteolytic activity is just emerging. Studies from our laboratory had indicated specific post-translational modifications of the aspartyl endopeptidase Cathepsin D (CatD) at distinct stages mammary gland development. This study addresses the biological significance of these modifications in the involution process, and reveals that post-translational modifications drive CatD into the nucleus to cleave Histone 3. The cleavage of Histone 3 has been associated with cellular differentiation and could be critical instigator of involution process. From functional perspective, deregulated expression and increased secretion of CatD are associated with aggressive and metastatic phenotype of breast cancer. Thus unraveling CatD’s physiological functions in mammary gland development will bridge the present gap in understanding its pro-tumorigenic/metastatic functions, and assist in the generation of tailored therapeutic approaches.
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spelling pubmed-41083902014-07-24 Cleavage of Histone 3 by Cathepsin D in the Involuting Mammary Gland Khalkhali-Ellis, Zhila Goossens, William Margaryan, Naira V. Hendrix, Mary J. C. PLoS One Research Article The post-lactational regression of mammary gland is a complex multi-step process designed to conserve the biological function of the gland for next pregnancy. This developmental stage is a biological intrigue with great relevance to breast cancer research, and thus has been the subject of intensive scrutiny. Multipronged studies (microarray, proteomics profiling, animal knock-out models) have provided a repertoire of genes critical to involution. However, the caveat of these approaches remains in their failure to reveal post-translational modification(s), an emerging and critical aspect of gene regulation in developmental processes and mammary gland remodeling. The massive surge in the lysosomal enzymes concurrent with the onset of involution has been known for decades, and considered essential for “clearance” purposes. However, functional significance of these enzymes in diverse biological processes distinct from their proteolytic activity is just emerging. Studies from our laboratory had indicated specific post-translational modifications of the aspartyl endopeptidase Cathepsin D (CatD) at distinct stages mammary gland development. This study addresses the biological significance of these modifications in the involution process, and reveals that post-translational modifications drive CatD into the nucleus to cleave Histone 3. The cleavage of Histone 3 has been associated with cellular differentiation and could be critical instigator of involution process. From functional perspective, deregulated expression and increased secretion of CatD are associated with aggressive and metastatic phenotype of breast cancer. Thus unraveling CatD’s physiological functions in mammary gland development will bridge the present gap in understanding its pro-tumorigenic/metastatic functions, and assist in the generation of tailored therapeutic approaches. Public Library of Science 2014-07-23 /pmc/articles/PMC4108390/ /pubmed/25054204 http://dx.doi.org/10.1371/journal.pone.0103230 Text en © 2014 Khalkhali-Ellis 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
Khalkhali-Ellis, Zhila
Goossens, William
Margaryan, Naira V.
Hendrix, Mary J. C.
Cleavage of Histone 3 by Cathepsin D in the Involuting Mammary Gland
title Cleavage of Histone 3 by Cathepsin D in the Involuting Mammary Gland
title_full Cleavage of Histone 3 by Cathepsin D in the Involuting Mammary Gland
title_fullStr Cleavage of Histone 3 by Cathepsin D in the Involuting Mammary Gland
title_full_unstemmed Cleavage of Histone 3 by Cathepsin D in the Involuting Mammary Gland
title_short Cleavage of Histone 3 by Cathepsin D in the Involuting Mammary Gland
title_sort cleavage of histone 3 by cathepsin d in the involuting mammary gland
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4108390/
https://www.ncbi.nlm.nih.gov/pubmed/25054204
http://dx.doi.org/10.1371/journal.pone.0103230
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