Interleukin 17A Participates in Renal Inflammation Associated to Experimental and Human Hypertension

白细胞介素 17A 参与与实验和人类高血压相关的肾脏炎症

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作者:Macarena Orejudo, Raul R Rodrigues-Diez, Raquel Rodrigues-Diez, Ana Garcia-Redondo, Laura Santos-Sánchez, Javier Rández-Garbayo, Pablo Cannata-Ortiz, Adrian M Ramos, Alberto Ortiz, Rafael Selgas, Sergio Mezzano, Carolina Lavoz, Marta Ruiz-Ortega

Abstract

Hypertension is now considered as an inflammatory disease, and the kidney is a key end-organ target. Experimental and clinical studies suggest that interleukin 17A (IL-17A) is a promising therapeutic target in immune and chronic inflammatory diseases, including hypertension and kidney disease. Elevated circulating IL-17A levels have been observed in hypertensive patients. Our aim was to investigate whether chronically elevated circulating IL-17A levels could contribute to kidney damage, using a murine model of systemic IL-17A administration. Blood pressure increased after 14 days of IL-17A infusion in mice when compared with that in control mice, and this was associated to kidney infiltration by inflammatory cells, including CD3+ and CD4+ lymphocytes and neutrophils. Moreover, proinflammatory factors and inflammatory-related intracellular mechanisms were upregulated in kidneys from IL-17A-infused mice. In line with these findings, in the model of angiotensin II infusion in mice, IL-17A blockade, using an anti-IL17A neutralizing antibody, reduced kidney inflammatory cell infiltrates and chemokine overexpression. In kidney biopsies from patients with hypertensive nephrosclerosis, IL-17A positive cells, mainly Th17 and γδ T lymphocytes, were found. Overall, the results support a pathogenic role of IL-17A in hypertensive kidney disease-associated inflammation. Therapeutic approaches targeting this cytokine should be explored to prevent hypertension-induced kidney injury.

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