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Role of EP2 and EP4 receptor-selective agonists of prostaglandin E2 in acute and chronic kidney failure

机译:前列腺素E2的EP2和EP4受体选择性激动剂在急慢性肾衰竭中的作用

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We tested the efficacy of three selective agonists of prostaglandin E2 (PGE2) receptor, EP2 (CP-536,745-01), EP2/4 (CP-043,305-02), and EP4 (CP-044,519-02), in two models of acute and chronic kidney failure. In the nephrotoxic mercury chloride (HgCl2) rat model of acute kidney failure systemically administered EP4 agonist reduced the serum creatinine values and increased the survival rate. Although the EP2 or the EP2/4 agonist did not change the serum creatinine values, the EP2 receptor agonist increased the survival rate. Histological evaluation of kidneys from EP4-treated rats indicated less proximal tubular necrosis and less apoptotic cells. In a rat model of chronic renal failure, the three receptor agonists decreased the serum creatinine and increased the glomerular filtration rate at 9 weeks following therapy. Kidneys treated with the EP4 agonist had less glomerular sclerosis, better preservation of proximal and distal tubules and blood vessels, increased convoluted epithelium proliferation and less apoptotic cells. Nephrectomy had no influence on the expression of the EP4 receptor, whereas EP2 receptor expression was reduced by 50% and then corrected following treatment with EP2 and EP2/4 receptor agonists. These findings suggest that PGE2 has an important role in acute kidney failure via the EP4 receptor, whereas in chronic kidney failure both EP2 and EP4 receptors are equally important in preserving the progression of chronic kidney failure. Thus, agonism of EP2 and EP4 receptors may provide a basis for treating acute and chronic kidney failure.
机译:我们在以下两种模型中测试了前列腺素E2(PGE2)受体,EP2(CP-536,745-01),EP2 / 4(CP-043,305-02)和EP4(CP-044,519-02)三种选择性激动剂的疗效急慢性肾功能衰竭。在肾毒性氯化汞(HgCl2)大鼠模型中,系统性给予EP4激动剂可导致急性肾功能衰竭,降低血清肌酐值并提高生存率。尽管EP2或EP2 / 4激动剂不会改变血清肌酐值,但EP2受体激动剂可提高存活率。 EP4处理的大鼠肾脏的组织学评估表明,近端肾小管坏死较少,凋亡细胞较少。在慢性肾衰竭的大鼠模型中,这三种受体激动剂在治疗后9周降低了血清肌酐并提高了肾小球滤过率。用EP4激动剂治疗的肾脏肾小球硬化少,近端和远端小管和血管的保存更好,回旋上皮细胞增殖增加,凋亡细胞减少。肾切除术对EP4受体的表达没有影响,而EP2受体的表达降低了50%,然后在用EP2和EP2 / 4受体激动剂治疗后得以纠正。这些发现表明,PGE 2通过EP 4受体在急性肾衰竭中具有重要作用,而在慢性肾衰竭中,EP 2和EP 4受体在保持慢性肾衰竭的进展中同样重要。因此,EP2和EP4受体的激动作用可为治疗急性和慢性肾功能衰竭提供基础。

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