从肾小管罕见疾病到急性肾损伤:进展与展望

IF 4.3 3区 材料科学 Q1 ENGINEERING, ELECTRICAL & ELECTRONIC
Jiaying Li, Fangxing Hou, Ning Lv, Ruohuan Zhao, Lei Zhang, Cai Yue, Min Nie, Limeng Chen
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引用次数: 0

摘要

背景:急性肾损伤(AKI)是一种以肾功能急剧恶化和死亡率升高为特征的严重疾病,传统的生物标志物缺乏敏感性和特异性。罕见的肾小管间质疾病包括一系列疾病,主要包括单基因疾病、免疫相关疾病和药物诱发的肾小管间质疾病。其临床表现各不相同,从电解质和酸碱失衡到肾功能不全,多达 20% 的病例伴有 AKI。有证据表明,罕见的肾小管间质性疾病可能为新型生物标记物和潜在的 AKI 治疗策略提供新的概念见解和视角。摘要:常染色体显性肾小管间质性疾病(ADTKD)和范可尼综合征(FS)是罕见的肾小管间质性疾病。在 ADTKD 中,UMOD 和 REN 通过影响氧化应激和肾小管肾小球反馈(TGF)而与 AKI 密切相关,这为 AKI 提供了潜在的新生物标志物。罕见肾小管间质疾病和 AKI 有着共同的病因和治疗反应。从机制上看,罕见的肾小管间质性疾病和 AKI 都涉及肾小管转运体损伤,最初表现为肾小管间质性疾病中的肾小管功能障碍,后来由于近端肾小管细胞凋亡、热凋亡或坏死等程序性细胞死亡(PCD)而发展为 AKI。此外,线粒体功能障碍已被确定为肾小管间质疾病和由药物、PSS 或单克隆疾病诱发的 AKI 的共同机制。最终,AKI 和 FS 患者及动物模型对原发疾病的治疗均反应良好。关键信息:在这篇综述中,我们概述了 ADTKD 和 FS,以确定它们与 AKI 的关联。线粒体功能障碍导致了罕见的肾小管间质疾病和 AKI,这可能是一个潜在的治疗靶点。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
From Rare Disorders of Kidney Tubules to Acute Renal Injury: Progress and Prospective
Background: Acute kidney injury (AKI) is a severe condition marked by rapid renal function deterioration and elevated mortality, with traditional biomarkers lacking sensitivity and specificity. Rare tubulointerstitial diseases encompass a spectrum of disorders, primarily including monogenic diseases, immune-related conditions, and drug-induced tubulointerstitial diseases. The clinical manifestations vary from the electrolyte and acid-base imbalance to kidney function insufficiency, which is associated with AKI in up to 20% of cases. Evidence indicated that rare tubulointerstitial diseases might provide new conceptual insights and perspectives for novel biomarkers and potential therapeutic strategies for AKI. Summary: Autosomal dominant tubulointerstitial kidney disease (ADTKD) and Fanconi syndrome (FS) are rare tubulointerstitial diseases. In ADTKD, UMOD and REN are closely related to AKI by affecting oxidative stress and tubuloglomerular feedback (TGF), which provide potential new biomarkers for AKI. Both rare tubulointerstitial diseases and AKI shared etiologies and treatment responses. From the mechanism standpoint, rare tubulointerstitial diseases and AKI involve tubular transporter injury, initially manifesting as tubular dysfunction in tubulointerstitial disorder and progressing to AKI because of the programmed cell death (PCD) with apoptosis, pyroptosis, or necroptosis of proximal tubule cells. Additionally, mitochondrial dysfunction has been identified as a common mechanism in both tubulointerstitial diseases and AKI induced by drugs, pSS, or monoclonal diseases. In the end, both AKI and FS patients and animal models responded well to the therapy of the primary diseases. Key messages: In this review, we describe an overview of ADTKD and FS to identify their associations with AKI. Mitochondrial dysfunction contributes to rare tubulointerstitial diseases and AKI, which might provide a potential therapeutic target.
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来源期刊
CiteScore
7.20
自引率
4.30%
发文量
567
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