Endothelial cells overexpressing CXCR1/2 are renoprotective in rats with acute kidney injury.

IF 3.7 2区 医学 Q1 PHYSIOLOGY
Dongqi Xing, Fadi G Hage, Wenguang Feng, Yuanyuan Guo, Suzanne Oparil, Paul W Sanders
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引用次数: 0

Abstract

Inflammation that develops with the release of chemokines and cytokines during acute kidney injury (AKI) has been shown to participate in functional renal recovery. Although a major research focus has been on the role of macrophages, the family of C-X-C motif chemokines that promote neutrophil adherence and activation also increases with kidney ischemia-reperfusion (I/R) injury. This study tested the hypothesis that intravenous delivery of endothelial cells (ECs) that overexpress (C-X-C motif) chemokine receptors 1 and 2 (CXCR1 and CXCR2, respectively) improves outcomes in kidney I/R injury. Overexpression of CXCR1/2 enhanced homing of endothelial cells to I/R-injured kidneys and limited interstitial fibrosis, capillary rarefaction, and tissue injury biomarkers (serum creatinine concentration and urinary kidney injury molecule-1) following AKI and also reduced expression of P-selectin and the rodent (C-X-C motif) chemokine cytokine-induced neutrophil chemoattractant (CINC)-2β as well as the number of myeloperoxidase-positive cells in the postischemic kidney. The serum chemokine/cytokine profile, including CINC-1, showed similar reductions. These findings were not observed in rats given endothelial cells transduced with an empty adenoviral vector (null-ECs) or a vehicle alone. These data indicate that extrarenal endothelial cells that overexpress CXCR1 and CXCR2, but not null-ECs or vehicle alone, reduce I/R kidney injury and preserve kidney function in a rat model of AKI.NEW & NOTEWORTHY Inflammation facilitates kidney ischemia-reperfusion (I/R) injury. Endothelial cells (ECs) that were modified to overexpress (C-X-C motif) chemokine receptor (CXCR)1/2 (CXCR1/2-ECs) were injected immediately following kidney I/R injury. The interaction of CXCR1/2-ECs, but not ECs transduced with an empty adenoviral vector, with injured kidney tissue preserved kidney function and reduced production of inflammatory markers, capillary rarefaction, and interstitial fibrosis. The study highlights a functional role for the C-X-C chemokine pathway in kidney damage following I/R injury.

过表达 CXCR1/2 的内皮细胞对急性肾损伤大鼠具有肾保护作用。
急性肾损伤(AKI)期间随着趋化因子和细胞因子的释放而产生的炎症已被证明参与了肾功能的恢复。虽然研究的重点是巨噬细胞的作用,但促进中性粒细胞粘附和活化的 C-X-C motif 趋化因子家族也会随着肾脏缺血再灌注(I/R)损伤而增加。本研究测试了一种假设,即静脉注射过量表达(C-X-C 矩阵)趋化因子受体 1 和 2(分别为 CXCR1 和 CXCR2)的内皮细胞(EC)可改善肾脏 I/R 损伤的预后。CXCR1/2的过表达增强了内皮细胞向I/R损伤肾脏的归巢,并限制了肾间质纤维化、毛细血管稀疏、和组织损伤生物标志物(血清肌酐浓度和尿肾损伤分子-1),还能降低缺血后肾脏中 P-选择素和啮齿类(C-X-C 矩阵)趋化因子细胞因子诱导的中性粒细胞趋化因子(CINC)-2β 的表达以及髓过氧化物酶阳性细胞的数量。包括 CINC-1 在内的血清趋化因子/细胞因子谱也出现了类似的减少。用空腺病毒载体(null-ECs)或单独的载体转导内皮细胞的大鼠没有观察到这些结果。这些数据表明,过表达 CXCR1 和 CXCR2 的肾外内皮细胞,而不是空-ECs 或单独的载体,可以减轻 I/R 肾损伤,并保护大鼠 AKI 模型中的肾功能。在肾脏I/R损伤后立即注射经修饰过量表达(C-X-C motif)趋化因子受体(CXCR)1/2的内皮细胞(ECs)(CXCR1/2-ECs)。CXCR1/2-ECs(而非用空腺病毒载体转导的 ECs)与损伤肾组织的相互作用可保护肾功能,并减少炎症标志物的产生、毛细血管稀疏和间质纤维化。该研究强调了C-X-C趋化因子通路在I/R损伤后肾脏损伤中的功能性作用。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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来源期刊
CiteScore
8.40
自引率
7.10%
发文量
154
审稿时长
2-4 weeks
期刊介绍: The American Journal of Physiology - Renal Physiology publishes original manuscripts on timely topics in both basic science and clinical research. Published articles address a broad range of subjects relating to the kidney and urinary tract, and may involve human or animal models, individual cell types, and isolated membrane systems. Also covered are the pathophysiological basis of renal disease processes, regulation of body fluids, and clinical research that provides mechanistic insights. Studies of renal function may be conducted using a wide range of approaches, such as biochemistry, immunology, genetics, mathematical modeling, molecular biology, as well as physiological and clinical methodologies.
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