Senescence Induced by UVB in Keratinocytes Impairs Amino Acids Balance

Skin is one of the most exposed organs to external stress. Namely, UV rays are the most harmful stress that could induce important damage leading to skin aging and cancers. At the cellular level, senescence is observed in several skin cell types and contributes to skin aging. However, the origin of...

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Veröffentlicht in:JOURNAL OF INVESTIGATIVE DERMATOLOGY 2023-04, Vol.143 (4)
Hauptverfasser: Bauwens, Emilie, Paree, Tom, Meurant, Sebastien, Bouriez, Ines, Hannart, Clotilde, Wera, Anne-Catherine, Khelfi, Alexis, Fattaccioli, Antoine, Burteau, Sophie, Demazy, Catherine, Fransolet, Maude, De Schutter, Clementine, Martin, Nathalie, Thery, Julien, Decanter, Gauthier, Penel, Nicolas, Bury, Marina, Pluquet, Olivier, Garmyn, Marjan, Debacq-Chainiaux, Florence
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container_title JOURNAL OF INVESTIGATIVE DERMATOLOGY
container_volume 143
creator Bauwens, Emilie
Paree, Tom
Meurant, Sebastien
Bouriez, Ines
Hannart, Clotilde
Wera, Anne-Catherine
Khelfi, Alexis
Fattaccioli, Antoine
Burteau, Sophie
Demazy, Catherine
Fransolet, Maude
De Schutter, Clementine
Martin, Nathalie
Thery, Julien
Decanter, Gauthier
Penel, Nicolas
Bury, Marina
Pluquet, Olivier
Garmyn, Marjan
Debacq-Chainiaux, Florence
description Skin is one of the most exposed organs to external stress. Namely, UV rays are the most harmful stress that could induce important damage leading to skin aging and cancers. At the cellular level, senescence is observed in several skin cell types and contributes to skin aging. However, the origin of skin senescent cells is still unclear but is probably related to exposure to stresses. In this work, we developed an in vitro model of UVB-induced premature senescence in normal human epidermal keratinocytes. UVB-induced senescent keratinocytes display a common senescent phenotype resulting in an irreversible cell cycle arrest, an increase in the proportion of senescence-associated β-galactosidase‒positive cells, unrepaired DNA damage, and a long-term DNA damage response activation. Moreover, UVB-induced senescent keratinocytes secrete senescence-associated secretory phenotype factors that influence cutaneous squamous cell carcinoma cell migration. Finally, a global transcriptomic study highlighted that senescent keratinocytes present a decrease in the expression of several amino acid transporters, which is associated with reduced intracellular levels of glycine, alanine, and leucine. Interestingly, the chemical inhibition of the glycine transporter SLC6A9/Glyt1 triggers senescence features.
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Namely, UV rays are the most harmful stress that could induce important damage leading to skin aging and cancers. At the cellular level, senescence is observed in several skin cell types and contributes to skin aging. However, the origin of skin senescent cells is still unclear but is probably related to exposure to stresses. In this work, we developed an in vitro model of UVB-induced premature senescence in normal human epidermal keratinocytes. UVB-induced senescent keratinocytes display a common senescent phenotype resulting in an irreversible cell cycle arrest, an increase in the proportion of senescence-associated β-galactosidase‒positive cells, unrepaired DNA damage, and a long-term DNA damage response activation. Moreover, UVB-induced senescent keratinocytes secrete senescence-associated secretory phenotype factors that influence cutaneous squamous cell carcinoma cell migration. 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title Senescence Induced by UVB in Keratinocytes Impairs Amino Acids Balance
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