Extracellular serine empowers epidermal proliferation and psoriasis-like symptoms

丝氨酸羟甲基转移酶 丝氨酸 银屑病 角质形成细胞 甘氨酸 细胞生长 细胞外 嘌呤代谢 炎症 生物 生物化学 氨基酸 免疫学 体外
作者
Angela Cappello,Mara Mancini,Stefania Madonna,Serena Rinaldo,Alessio Paone,Claudia Scarponi,Antonio Belardo,L. Zolla,Alessandro Zuccotti,Emanuele Panatta,Sabatino Pallotta,Margherita Annicchiarico‐Petruzzelli,Cristina Albanesi,Francesca Cutruzzolá,Lu Wang,Jia Wang,Gerry Melino,Eleonora Candi
出处
期刊:Science Advances [American Association for the Advancement of Science (AAAS)]
卷期号:8 (50) 被引量:13
标识
DOI:10.1126/sciadv.abm7902
摘要

The contribution of nutrient availability to control epidermal cell proliferation, inflammation, and hyperproliferative diseases remains unknown. Here, we studied extracellular serine and serine/glycine metabolism using human keratinocytes, human skin biopsies, and a mouse model of psoriasis-like disease. We focused on a metabolic enzyme, serine hydroxymethyltransferase (SHMT), that converts serine into glycine and tetrahydrofolate-bound one‑carbon units to support cell growth. We found that keratinocytes are both serine and glycine auxotrophs. Metabolomic profiling and hypoxanthine supplementation indicated that SHMT silencing/inhibition reduced cell growth through purine depletion, leading to nucleotide loss. In addition, topical application of an SHMT inhibitor suppressed both keratinocyte proliferation and inflammation in the imiquimod model and resulted in a decrease in psoriasis-associated gene expression. In conclusion, our study highlights SHMT2 activity and serine/glycine availability as an important metabolic hub controlling both keratinocyte proliferation and inflammatory cell expansion in psoriasis and holds promise for additional approaches to treat skin diseases.
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