小鼠单侧输尿管阻塞造成的肾损伤缺乏性别差异

IF 2.3 4区医学 Q2 PERIPHERAL VASCULAR DISEASE

Kidney & blood pressure research Pub Date : 2024-01-01 Epub Date: 2024-01-05 DOI:10.1159/000535809

Samaneh Goorani, Abdul Hye Khan, Abhishek Mishra, Ashraf El-Meanawy, John D Imig

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引用次数: 0

摘要

简介肾脏纤维化是慢性肾脏病（CKD）发生和发展的关键事件，被认为是所有类型 CKD 的最终共同途径。女性的 CKD 患病率较高，但男性的终末期肾病（ESRD）患病率更高。此外，低出生体重和低肾小球数量与 CKD 的风险增加有关。本研究考察了单侧输尿管梗阻（UUO）诱导的雌雄野生型（ROP +/+）和突变型（ROP Os/+）小鼠肾脏纤维化的发展和严重程度：方法：对雌雄 ROP +/+ 和 ROP Os/+ 小鼠进行 UUO，并在 10 天实验期结束时收集肾组织。肾脏组织学分析和 mRNA 表达确定了肾脏纤维化、肾小管损伤、胶原沉积、细胞外基质蛋白和免疫细胞浸润：结果：雌雄 UUO 小鼠均表现出明显的肾损伤、肾纤维化和肾细胞外基质生成。ROP +/+和ROP Os/+小鼠的肾脏纤维化和α-平滑肌肌动蛋白的增加程度相似。ROP +/+和ROP Os/+ UUO小鼠的肾小管铸型形成和肾脏巨噬细胞浸润也没有性别差异。有趣的是，与UUO ROP Os/+小鼠相比，UUO ROP +/+小鼠的肾脏纤维化和α-平滑肌肌动蛋白是后者的1.5-3倍。与 ROP Os/+ 小鼠相比，ROP +/+ 小鼠在 UUO 后的肾脏炎症表型也要高出 30-45%。同样，与 UUO ROP Os/+ 小鼠相比，UUO ROP +/+ 小鼠细胞外基质和肾脏纤维化基因的表达量更高。与这些研究结果相反，患有 UUO 的 ROP Os/+ 小鼠表现出肾小球肥大，肾小球簇面积比患有 UUO 的 ROP +/+ 小鼠大 50%。在任何一种基因型的 ROP 小鼠中，肾小球肥大都与性别无关。这些发现提供了证据，证明肾小球数量少会导致 UUO 诱导 ROP Os/+ 小鼠肾小球肥大，但不会加重肾脏纤维化、炎症和肾小管损伤：综上所述，我们证明肾小球数量少会导致肾小球肥大，但不会导致肾脏纤维化和肾小管损伤。我们还证明，在任何一种 ROP 小鼠基因型中，UUO 引起的变化都不受性别的影响。

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Kidney Injury by Unilateral Ureteral Obstruction in Mice Lacks Sex Differences.

Introduction: Renal fibrosis is a critical event in the development and progression of chronic kidney disease (CKD), and it is considered the final common pathway for all types of CKD. The prevalence of CKD is higher in females; however, males have a greater prevalence of end-stage renal disease. In addition, low birth weight and low nephron number are associated with increased risk for CKD. This study examined the development and severity of unilateral ureter obstruction (UUO)-induced renal fibrosis in male and female wild-type (ROP +/+) and mutant (ROP Os/+) mice, a mouse model of low nephron number.

Methods: Male and female ROP +/+ and ROP Os/+ mice were subjected to UUO, and kidney tissue was collected at the end of the 10-day experimental period. Kidney histological analysis and mRNA expression determined renal fibrosis, tubular injury, collagen deposition, extracellular matrix proteins, and immune cell infiltration.

Results: Male and female UUO mice demonstrated marked renal injury, kidney fibrosis, and renal extracellular matrix production. Renal fibrosis and α-smooth muscle actin were increased to a similar degree in ROP +/+ and ROP Os/+ mice with UUO of either sex. There were also no sex differences in renal tubular cast formation or renal infiltration of macrophage in ROP +/+ and ROP Os/+ UUO mice. Interestingly, renal fibrosis and α-smooth muscle actin were 1.5-3-fold greater in UUO-ROP +/+ compared to UUO-ROP Os/+ mice. Renal inflammation phenotypes following UUO were also 30-45% greater in ROP +/+ compared to ROP Os/+ mice. Likewise, expression of extracellular matrix and renal fibrotic genes was greater in UUO-ROP +/+ mice compared to UUO-ROP Os/+ mice. In contrast to these findings, ROP Os/+ mice with UUO demonstrated glomerular hypertrophy with 50% greater glomerular tuft area compared to ROP +/+ with UUO. Glomerular hypertrophy was not sex-dependent in any of the genotypes of ROP mice. These findings provide evidence that low nephron number contributes to UUO-induced glomerular hypertrophy in ROP Os/+ mice but does not enhance renal fibrosis, inflammation, and renal tubular injury.

Conclusion: Taken together, we demonstrate that low nephron number contributes to enhanced glomerular hypertrophy but not kidney fibrosis and tubular injury. We also demonstrate that none of the changes caused by UUO was affected by sex in any of the ROP mice genotypes.

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来源期刊

Kidney & blood pressure research 医学-泌尿学与肾脏学

CiteScore

4.80

自引率

3.60%

发文量

审稿时长

6-12 weeks

期刊介绍： This journal comprises both clinical and basic studies at the interface of nephrology, hypertension and cardiovascular research. The topics to be covered include the structural organization and biochemistry of the normal and diseased kidney, the molecular biology of transporters, the physiology and pathophysiology of glomerular filtration and tubular transport, endothelial and vascular smooth muscle cell function and blood pressure control, as well as water, electrolyte and mineral metabolism. Also discussed are the (patho)physiology and (patho) biochemistry of renal hormones, the molecular biology, genetics and clinical course of renal disease and hypertension, the renal elimination, action and clinical use of drugs, as well as dialysis and transplantation. Featuring peer-reviewed original papers, editorials translating basic science into patient-oriented research and disease, in depth reviews, and regular special topic sections, ''Kidney & Blood Pressure Research'' is an important source of information for researchers in nephrology and cardiovascular medicine.