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Effect of 2'-phosphophloretin on renal function in chronic renal failure rats.

机译:2'-磷酸叶绿素对慢性肾衰竭大鼠肾功能的影响。

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摘要

Hyperhosphatemia and secondary hyperparathyroidism are common and severe complications of chronic renal failure. Therapies to reduce serum phosphate have been shown to reduce serum parathyroid hormone (PTH) and slow the progression of renal failure. The effect of the inhibitor of intestinal phosphate absorption, 2'-phosphophloretin (2'-PP), on serum and urine chemistry, renal histology, and cardiac structure in the uremic rat model of renal failure, 5/6 nephrectomy (5/6 NX), was examined. The effect of 2'-PP on serum phosphate, serum PTH, serum total Ca(2+), and ionized Ca(2+), Ca(2+) x P(i) product, urine protein, urine osmolality, and creatinine clearance in 5/6 NX rats was examined. Uremic rats in chronic renal failure were gavaged daily with 25 microM 2'-PP. Over the course of a 5-wk experiment, serum chemistry in untreated uremic rats, 2'-PP-treated uremic rats, and age-matched control rats with normal renal function was determined twice a week. Urine creatinine, urine osmolality, urine phosphate,and urine protein were determined once a week from 24-h collections. 2'-PP reduced serum phosphate 40 +/- 3% compared with a 17% increase in untreated uremic control rats. 2'-PP did not alter total serum Ca(2+). During 5-wk experiments, serum PTH increased 65 +/- 25% in untreated uremic rats and decreased 70 +/- 7% in uremic rats treated with 25 microM 2'-PP. Creatinine clearance decreased 20% in untreated uremic rats compared with a 100% increase in 2'-PP-treated uremic rats. Urine protein decreased and urine osmolality increased in uremic rats treated with 2'-PP. The mechanism of the effect of 2'-PP on serum phosphate was inhibition of intestinal phosphate absorption. 2-PP inhibited intestinal phosphate absorption 50% without altering dietary protein absorption or intestinal Ca(2+) absorption. Over the course of the 5-wk treatment with 2'-PP, uremic animals treated with 2'-PP had a 2-4% weight gain/wk, similar to the weight gain seen in age-matched control rats with normal renal function.
机译:高胆固醇血症和继发性甲状旁腺功能亢进是慢性肾功能衰竭的常见和严重并发症。减少血清磷酸盐的疗法已显示可减少血清甲状旁腺激素(PTH)并减慢肾衰竭的进展。肠磷酸盐吸收抑制剂2'-磷酸叶绿素(2'-PP)对5/6肾衰竭尿毒症大鼠模型中血清和尿液化学成分,肾脏组织学和心脏结构的影响NX)。 2'-PP对血清磷酸盐,血清PTH,血清总Ca(2+)和离子化Ca(2 +),Ca(2+)x P(i)产物,尿蛋白,尿渗透压和肌酐的影响检查了5/6只NX大鼠的清除率。每天用25 microM 2'-PP灌胃慢性肾衰竭的尿毒症大鼠。在5周实验过程中,每周两次测定未治疗的尿毒症大鼠,2'-PP治疗的尿毒症大鼠和年龄匹配的肾功能正常的对照大鼠的血清化学。每周24小时收集一次尿液中的肌酐,尿渗透压,尿磷酸盐,尿蛋白。 2'-PP使血清磷酸盐减少40 +/- 3%,而未治疗的尿毒症对照大鼠增加17%。 2'-PP不会改变总血清Ca(2+)。在5周实验中,未经治疗的尿毒症大鼠血清PTH升高65 +/- 25%,而接受25 microM 2'-PP治疗的尿毒症大鼠血清PTH降低70 +/- 7%。在未治疗的尿毒症大鼠中,肌酐清除率降低了20%,而在2'-PP治疗的尿毒症大鼠中,肌酐清除率降低了100%。用2'-PP处理的尿毒症大鼠尿蛋白减少,尿渗透压升高。 2'-PP对血清磷酸盐的作用机理是抑制肠道磷酸盐的吸收。 2-PP抑制肠磷酸盐吸收50%,而不改变饮食蛋白质吸收或肠Ca(2+)吸收。在用2'-PP进行5周治疗的过程中,用2'-PP治疗的尿毒症动物的体重增加/周为2-4%,类似于在具有正常肾脏功能的年龄匹配的对照大鼠中看到的体重增加。

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