SOD1 而非 SOD3 缺乏加速 C57BL/6-Ins2(Akita) 糖尿病小鼠的糖尿病肾脏损伤。
SOD1, but not SOD3, deficiency accelerates diabetic renal injury in C57BL/6-Ins2(Akita) diabetic mice.
机构信息
Division of Endocrinology, Metabolism and Geriatric Medicine, Akita University Graduate School of Medicine, 1-1-1 Hondo, Akita 010-8543, Japan.
出版信息
Metabolism. 2012 Dec;61(12):1714-24. doi: 10.1016/j.metabol.2012.05.005. Epub 2012 May 25.
Superoxide dismutase (SOD) is a major defender against excessive superoxide generated under hyperglycemia. We have recently reported that renal SOD1 (cytosolic CuZn-SOD) and SOD3 (extracellular CuZn-SOD) isoenzymes are remarkably down-regulated in KK/Ta-Ins2(Akita) diabetic mice, which exhibit progressive diabetic nephropathy (DN), but not in DN-resistant C57BL/6- Ins2(Akita) (C57BL/6-Akita) diabetic mice. To determine the role of SOD1 and SOD3 in DN, we generated C57BL/6-Akita diabetic mice with deficiency of SOD1 and/or SOD3 and investigated their renal phenotype at the age of 20 weeks. Increased glomerular superoxide levels were observed in SOD1(-/-)SOD3(+/+) and SOD1(-/-)SOD3(-/-) C57BL/6-Akita mice but not in SOD1(+/+)SOD3(-/-) C57BL/6-Akita mice. The SOD1(-/-)SOD3(+/+) and SOD1(-/-)SOD3(-/-) C57BL/6-Akita mice exhibited higher glomerular filtration rate, increased urinary albumin levels, and advanced mesangial expansion as compared with SOD1(+/+)SOD3(+/+) C57BL/6-Akita mice, yet the severity of DN did not differ between the SOD1(-/-)SOD3(+/+) and SOD1(-/-)SOD3(-/-) C57BL/6-Akita groups. Increased renal mRNA expression of transforming growth factor-β1 (TGF-β1) and connective tissue growth factor (CTGF), reduced glomerular nitric oxide (NO), and increased renal prostaglandin E2 (PGE2) production were noted in the SOD1(-/-)SOD3(+/+) and SOD1(-/-)SOD3(-/-) C57BL/6-Akita mice. This finding indicates that such renal changes in fibrogenic cytokines, NO, and PGE2, possibly caused by superoxide excess, would contribute to the development of overt albuminuria by promoting mesangial expansion, endothelial dysfunction, and glomerular hyperfiltration. The present results demonstrate that deficiency of SOD1, but not SOD3, increases renal superoxide in the setting of diabetes and causes overt renal injury in nephropathy-resistant diabetic mice, and that SOD3 deficiency does not provide additive effects on the severity of DN in SOD1-deficient C57BL/6-Akita mice.
超氧化物歧化酶(SOD)是一种主要的防御机制,可以抵抗高血糖状态下产生的过多超氧自由基。我们最近报道,在 KK/Ta-Ins2(Akita)糖尿病小鼠中,肾脏 SOD1(细胞质 CuZn-SOD)和 SOD3(细胞外 CuZn-SOD)同工酶的表达显著下调,这些小鼠表现出进行性糖尿病肾病(DN),而在 DN 抗性 C57BL/6-Ins2(Akita)(C57BL/6-Akita)糖尿病小鼠中则没有。为了确定 SOD1 和 SOD3 在 DN 中的作用,我们生成了 SOD1 和/或 SOD3 缺失的 C57BL/6-Akita 糖尿病小鼠,并在 20 周龄时研究了它们的肾脏表型。在 SOD1(-/-)SOD3(+/+)和 SOD1(-/-)SOD3(-/-)C57BL/6-Akita 小鼠中观察到肾小球中超氧自由基水平升高,但在 SOD1(+/+)SOD3(-/-)C57BL/6-Akita 小鼠中则没有。与 SOD1(+/+)SOD3(+/+)C57BL/6-Akita 小鼠相比,SOD1(-/-)SOD3(+/+)和 SOD1(-/-)SOD3(-/-)C57BL/6-Akita 小鼠的肾小球滤过率更高,尿白蛋白水平升高,系膜扩张更严重,但 SOD1(-/-)SOD3(+/+)和 SOD1(-/-)SOD3(-/-)C57BL/6-Akita 两组之间的 DN 严重程度没有差异。在 SOD1(-/-)SOD3(+/+)和 SOD1(-/-)SOD3(-/-)C57BL/6-Akita 小鼠中,肾脏 TGF-β1(TGF-β1)和结缔组织生长因子(CTGF)的 mRNA 表达增加,肾小球一氧化氮(NO)减少,前列腺素 E2(PGE2)生成增加。这一发现表明,这种纤维化细胞因子、NO 和 PGE2 的肾脏变化可能是由于超氧自由基过多引起的,通过促进系膜扩张、内皮功能障碍和肾小球高滤过,导致明显的白蛋白尿。本研究结果表明,糖尿病状态下 SOD1 缺乏而非 SOD3 缺乏会增加肾脏中的超氧自由基,并导致 DN 抗性糖尿病小鼠出现明显的肾脏损伤,而 SOD3 缺乏在 SOD1 缺陷的 C57BL/6-Akita 小鼠中对 DN 的严重程度没有相加作用。
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