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首页> 外文期刊>American Journal of Physiology >MCP-1/CCL2: a new diagnostic marker and therapeutic target for progressive renal injury in diabetic nephropathy
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MCP-1/CCL2: a new diagnostic marker and therapeutic target for progressive renal injury in diabetic nephropathy

机译:MCP-1 / CCL2:糖尿病肾病进行性肾损伤的新诊断标志物和治疗靶标

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摘要

Despite current therapies, many diabetic patients will suffer from declining renal function in association with progressive kidney inflammation. Recently, animal model studies have demonstrated that kidney macrophage accumulation is a critical factor in the development of diabetic nephropathy. However, specific anti-inflammatory strategies are not yet being considered for the treatment of patients with diabetic renal injury. This review highlights the chemokine monocyte chemoattractant protein-1 (MCP-1)/CC-chemokine ligand 2 as a major promoter of inflammation, renal injury, and fibrosis in diabetic nephropathy. Researchers have found that diabetes induces kidney MCP-1 production and that urine MCP-1 levels can be used to assess renal inflammation in this disease. In addition, genetic deletion and molecular blocking studies in rodents have identified MCP-1 as an important therapeutic target for treating diabetic nephropathy. Evidence also suggests that a polymorphism in the human MCP-1 gene is associated with progressive kidney failure in type 2 diabetes, which may identify patients at higher risk who need additional therapy. These findings provide a strong rationale for developing specific therapies against MCP-1 and inflammation in diabetic nephropathy.
机译:尽管有当前的疗法,但是许多糖尿病患者将伴随进行性肾脏炎症而患有肾功能下降。最近,动物模型研究表明,肾脏巨噬细胞积累是糖尿病肾病发展的关键因素。但是,尚未考虑将特定的抗炎策略用于糖尿病肾损伤患者的治疗。这篇评论强调了趋化因子单核细胞趋化蛋白-1(MCP-1)/ CC趋化因子配体2是糖尿病肾病中炎症,肾脏损伤和纤维化的主要促进剂。研究人员发现,糖尿病会诱发肾脏MCP-1的产生,尿中MCP-1的水平可用于评估该疾病的肾脏炎症。此外,在啮齿动物中进行的基因删除和分子阻断研究已将MCP-1确定为治疗糖尿病性肾病的重要治疗靶标。证据还表明,人MCP-1基因的多态性与2型糖尿病的进行性肾衰竭有关,这可能确定了需要其他治疗的较高风险患者。这些发现为开发针对MCP-1和糖尿病性肾病中炎症的特异性疗法提供了有力的依据。

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