Literature DB >> 23790635

Selective matrix (hyaluronan) interaction with CD44 and RhoGTPase signaling promotes keratinocyte functions and overcomes age-related epidermal dysfunction.

Lilly Y W Bourguignon1, Gabriel Wong, Weiliang Xia, Mao-Qiang Man, Walter M Holleran, Peter M Elias.   

Abstract

BACKGROUND: Mouse epidermal chronologic aging is closely associated with aberrant matrix (hyaluronan, HA)-size distribution/production and impaired keratinocyte proliferation/differentiation, leading to a marked thinning of the epidermis with functional consequence that causes a slower recovery of permeability barrier function.
OBJECTIVE: The goal of this study is to demonstrate mechanism-based, corrective therapeutic strategies using topical applications of small HA (HAS) and/or large HA (HAL) [or a sequential small HA (HAS) and large HA(HAL) (HAsHAL) treatment] as well as RhoGTPase signaling perturbation agents to regulate HA/CD44-mediated signaling, thereby restoring normal epidermal function, and permeability barrier homeostasis in aged mouse skin.
METHODS: A number of biochemical, cell biological/molecular, pharmacological and physiological approaches were used to investigate matrix HA-CD44-mediated RhoGTPase signaling in regulating epidermal functions and skin aging.
RESULTS: In this study we demonstrated that topical application of small HA (HAS) promotes keratinocyte proliferation and increases skin thickness, while it fails to upregulate keratinocyte differentiation or permeability barrier repair in aged mouse skin. In contrast, large HA (HAL) induces only minimal changes in keratinocyte proliferation and skin thickness, but restores keratinocyte differentiation and improves permeability barrier function in aged epidermis. Since neither HAS nor HAL corrects these epidermal defects in aged CD44 knock-out mice, CD44 likely mediates HA-associated epidermal functions in aged mouse skin. Finally, blockade of Rho-kinase activity with Y27632 or protein kinase-Nγ activity with Ro31-8220 significantly decreased the HA (HAS or HAL)-mediated changes in epidermal function in aged mouse skin.
CONCLUSION: The results of our study show first that HA application of different sizes regulates epidermal proliferation, differentiation and barrier function in aged mouse skin. Second, manipulation of matrix (HA) interaction with CD44 and RhoGTPase signaling could provide further novel therapeutic approaches that could be targeted for the treatment of various aging-related skin disorders.
Copyright © 2013 Japanese Society for Investigative Dermatology. Published by Elsevier Ireland Ltd. All rights reserved.

Entities:  

Keywords:  CD44; Keratinocyte functions; Matrix hyaluronan; RhoGTPase signaling; Skin aging

Mesh:

Substances:

Year:  2013        PMID: 23790635      PMCID: PMC3775883          DOI: 10.1016/j.jdermsci.2013.05.003

Source DB:  PubMed          Journal:  J Dermatol Sci        ISSN: 0923-1811            Impact factor:   4.563


  52 in total

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2.  CD44 interaction with tiam1 promotes Rac1 signaling and hyaluronic acid-mediated breast tumor cell migration.

Authors:  L Y Bourguignon; H Zhu; L Shao; Y W Chen
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4.  A role for protein kinase cepsilon in the inhibitory effect of epidermal growth factor on calcium-stimulated chloride secretion in human colonic epithelial cells.

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5.  Keratinocyte differentiation in hyperproliferative epidermis: topical application of PPARalpha activators restores tissue homeostasis.

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Review 6.  Hyaluronan: a multifunctional, megaDalton, stealth molecule.

Authors:  J Y Lee; A P Spicer
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7.  CD44v10 interaction with Rho-kinase (ROK) activates inositol 1,4,5-triphosphate (IP3) receptor-mediated Ca2+ signaling during hyaluronan (HA)-induced endothelial cell migration.

Authors:  Patrick A Singleton; Lilly Y W Bourguignon
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8.  The adhesion receptor CD44 promotes atherosclerosis by mediating inflammatory cell recruitment and vascular cell activation.

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10.  Fyn tyrosine kinase is a downstream mediator of Rho/PRK2 function in keratinocyte cell-cell adhesion.

Authors:  Enzo Calautti; Maddalena Grossi; Cristina Mammucari; Yumi Aoyama; Maria Pirro; Yoshitaka Ono; Jie Li; G Paolo Dotto
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1.  Regulation of Hyaluronan (HA) Metabolism Mediated by HYBID (Hyaluronan-binding Protein Involved in HA Depolymerization, KIAA1199) and HA Synthases in Growth Factor-stimulated Fibroblasts.

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Journal:  J Biol Chem       Date:  2015-10-30       Impact factor: 5.157

2.  A topical heparinoid-containing product improves epidermal permeability barrier homeostasis in mice.

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Review 3.  Matrix hyaluronan-activated CD44 signaling promotes keratinocyte activities and improves abnormal epidermal functions.

Authors:  Lilly Y W Bourguignon
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5.  Decreased Calcium-Sensing Receptor Expression Controls Calcium Signaling and Cell-To-Cell Adhesion Defects in Aged Skin.

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6.  Topical hesperidin enhances epidermal function in an aged murine model.

Authors:  George Man; Theodora M Mauro; Yongjiao Zhai; Peggy L Kim; Carolyn Cheung; Melanie Hupe; Debbie Crumrine; Peter M Elias; Mao-Qiang Man
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Review 7.  Selective Hyaluronan-CD44 Signaling Promotes miRNA-21 Expression and Interacts with Vitamin D Function during Cutaneous Squamous Cell Carcinomas Progression Following UV Irradiation.

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Review 8.  The vitamin D receptor: a tumor suppressor in skin.

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9.  Selective Activation of Cancer Stem Cells by Size-Specific Hyaluronan in Head and Neck Cancer.

Authors:  Marisa Shiina; Lilly Y W Bourguignon
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10.  Uncovering the dual role of RHAMM as an HA receptor and a regulator of CD44 expression in RHAMM-expressing mesenchymal progenitor cells.

Authors:  Mandana Veiseh; Sean J Leith; Cornelia Tolg; Sallie S Elhayek; S Bahram Bahrami; Lisa Collis; Sara Hamilton; James B McCarthy; Mina J Bissell; Eva Turley
Journal:  Front Cell Dev Biol       Date:  2015-10-15
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