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keratinocyte-specific ablation of mcpip1 impairs skin integrity and promotes local and systemic inflammation
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نویسنده
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konieczny piotr ,lichawska-cieslar agata ,kwiecinska patrycja ,cichy joanna ,pietrzycka roza ,szukala weronika ,declercq wim ,devos michael ,paziewska agnieszka ,rumienczyk izabela ,kulecka maria ,mikula michal ,fu mingui ,borowczyk julia ,santamaria-babí luis f ,jura jolanta
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منبع
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journal of molecular medicine - 2019 - دوره : 97 - شماره : 12 - صفحه:1669 -1684
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چکیده
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Mcpip1 (regnase-1, encoded by the zc3h12a gene) regulates the mrna stability of several inflammatory cytokines. due to the critical role of this rna endonuclease in the suppression of inflammation, mcpip1 deficiency in mice leads to the development of postnatal multiorgan inflammation and premature death. here, we generated mice with conditional deletion of mcpip1 in the epidermis (mcpip1eko). mcpip1 loss in keratinocytes resulted in the upregulated expression of transcripts encoding factors related to inflammation and keratinocyte differentiation, such as il-36α/γ cytokines, s100a8/a9 antibacterial peptides, and sprr2d/2h proteins. upon aging, the mcpip1eko mice showed impaired skin integrity that led to the progressive development of spontaneous skin pathology and systemic inflammation. furthermore, we found that the lack of epidermal mcpip1 expression impaired the balance of keratinocyte proliferation and differentiation. overall, we provide evidence that keratinocyte-specific mcpip1 activity is crucial for the maintenance of skin integrity as well as for the prevention of excessive local and systemic inflammation.
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کلیدواژه
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mcpip1 ,regnase-1 ,zc3h12a ,skin inflammation
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آدرس
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jagiellonian university, faculty of biochemistry, department of general biochemistry, poland, jagiellonian university, faculty of biochemistry, department of general biochemistry, poland, jagiellonian university, faculty of biochemistry, department of immunology, poland, jagiellonian university, faculty of biochemistry, department of immunology, poland, jagiellonian university, faculty of biochemistry, department of general biochemistry, poland, jagiellonian university, faculty of biochemistry, department of general biochemistry, poland, vib center for inflammation research center, molecular signaling and cell death unit, belgium. ghent university, department of biomedical molecular biology, belgium, vib center for inflammation research center, molecular signaling and cell death unit, belgium. ghent university, department of biomedical molecular biology, belgium, medical center for postgraduate education, hepatology and clinical oncology, department of gastroenterology, poland, medical center for postgraduate education, hepatology and clinical oncology, department of gastroenterology, poland, medical center for postgraduate education, hepatology and clinical oncology, department of gastroenterology, poland, maria sklodowska-curie memorial cancer center and institute of oncology, department of genetics, poland, university of missouri-kansas city, department of biomedical science and shock/trauma research center, school of medicine, usa, jagiellonian university, faculty of biochemistry, department of cell biology, poland. university of geneva, faculty of medicine, current address: department of pathology and immunology, switzerland, university de barcelona, faculty of biology, department of cellular biology, spain, jagiellonian university, faculty of biochemistry, department of general biochemistry, poland
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Authors
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