靶向 KLF2 作为糖尿病肾病肾小球内皮细胞损伤的新型疗法

IF 10.3 1区 医学 Q1 UROLOGY & NEPHROLOGY Journal of The American Society of Nephrology Pub Date : 2024-10-09 DOI:10.1681/ASN.0000000000000498
Lulin Min, Yixin Chen, Ruijie Liu, Zhengzhe Li, Leyi Gu, Sandeep Mallipattu, Bhaskar Das, Kyung Lee, John Cijiang He, Fang Zhong
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引用次数: 0

摘要

背景:糖尿病肾病是一种微血管疾病,肾小球内皮细胞损伤是糖尿病肾病发展过程中的一个关键病理事件。通过对肾小球转录组的无偏见筛选,我们先前发现 KLF2 是糖尿病肾脏中的一个高度调控基因。KLF2 对内皮细胞有保护作用,能抑制炎症、血栓活化和血管生成,所有这些对心血管疾病都有保护作用。我们以前曾证实,内皮细胞特异性消减 Klf2 会加剧糖尿病诱导的小鼠肾小球内皮细胞损伤和 DKD。因此,在本研究中,我们试图评估 KLF2 激活在小鼠 DKD 模型中的治疗潜力:我们首先研究了链脲佐菌素诱导的糖尿病小鼠内皮细胞特异性诱导性过表达 KLF2(KLF2ov)的效果。我们开发了小分子 KLF2 激活剂,并测试了 KLF2 活性的增加是否能阻碍 2 型糖尿病 db/db 和 BTBR ob/ob 小鼠的 DKD 进展:结果:与对照组糖尿病小鼠相比,糖尿病 KLF2ov 小鼠的白蛋白尿、肾小球内皮细胞损伤和糖尿病肾小球病变均有所减轻。新型 KLF2 激活剂化合物 6(C-6)能有效诱导下游 Nos3 的表达,抑制肾小球内皮细胞中 NF-kB 的激活。服用 C-6 可改善 db/db 和 BTBR ob/ob 小鼠的白蛋白尿和肾小球病变,这与肾小球内皮细胞和荚膜细胞损伤的改善有关:这些结果验证了 KLF2 是一种潜在的药物靶点,而 C-6 等 KLF2 激活剂是治疗 DKD 的一种新型疗法。
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Targeting KLF2 as a Novel Therapy for Glomerular Endothelial Cell Injury in Diabetic Kidney Disease.

Background: DKD is a microvascular disease, and glomerular endothelial cell injury is a key pathological event in DKD development. Through unbiased screening of glomerular transcriptomes, we previously identified KLF2 as a highly regulated gene in diabetic kidneys. KLF2 exhibits protective effects in endothelial cells by inhibiting inflammation, thrombotic activation, and angiogenesis, all of which are protective for cardiovascular disease. We previously demonstrated that endothelial cell-specific ablation of Klf2 exacerbated diabetes-induced glomerular endothelial cell injury and DKD in mice. Therefore in this study, we sought to assess the therapeutic potential of KLF2 activation in murine models of DKD.

Methods: We first examined the effects of endothelial cell-specific inducible overexpression of KLF2 (KLF2ov) in streptozotocin-induced diabetic mice. We developed small molecule KLF2 activators and tested whether increased KLF2 activity could impede DKD progression in type 2 diabetic db/db and BTBR ob/ob mice.

Results: Diabetic KLF2ov mice had attenuated albuminuria, glomerular endothelial cell injury, and diabetic glomerulopathy compared to control diabetic mice. Novel KLF2 activator, compound 6 (C-6) effectively induced downstream Nos3 expression and suppressed NF-kB activation in glomerular endothelial cells. The administration of C-6 improved albuminuria and glomerulopathy in db/db and BTBR ob/ob mice, which was associated with improved glomerular endothelial cell and podocyte injury.

Conclusions: These results validate KLF2 as a potential drug target and KLF2 activators such as C-6 as a novel therapy for DKD.

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来源期刊
Journal of The American Society of Nephrology
Journal of The American Society of Nephrology 医学-泌尿学与肾脏学
CiteScore
22.40
自引率
2.90%
发文量
492
审稿时长
3-8 weeks
期刊介绍: The Journal of the American Society of Nephrology (JASN) stands as the preeminent kidney journal globally, offering an exceptional synthesis of cutting-edge basic research, clinical epidemiology, meta-analysis, and relevant editorial content. Representing a comprehensive resource, JASN encompasses clinical research, editorials distilling key findings, perspectives, and timely reviews. Editorials are skillfully crafted to elucidate the essential insights of the parent article, while JASN actively encourages the submission of Letters to the Editor discussing recently published articles. The reviews featured in JASN are consistently erudite and comprehensive, providing thorough coverage of respective fields. Since its inception in July 1990, JASN has been a monthly publication. JASN publishes original research reports and editorial content across a spectrum of basic and clinical science relevant to the broad discipline of nephrology. Topics covered include renal cell biology, developmental biology of the kidney, genetics of kidney disease, cell and transport physiology, hemodynamics and vascular regulation, mechanisms of blood pressure regulation, renal immunology, kidney pathology, pathophysiology of kidney diseases, nephrolithiasis, clinical nephrology (including dialysis and transplantation), and hypertension. Furthermore, articles addressing healthcare policy and care delivery issues relevant to nephrology are warmly welcomed.
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