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Pulse mTOR inhibitor treatment effectively controls cyst growth but leads to severe parenchymal and glomerular hypertrophy in rat polycystic kidney disease

机译:脉冲mTOR抑制剂治疗可有效控制囊肿的生长,但会导致大鼠多囊肾疾病中严重的实质和肾小球肥大

摘要

The efficacy of mammalian target of rapamycin (mTOR) inhibitors is currently tested in patients affected by autosomal dominant polycystic kidney disease. Treatment with mTOR inhibitors has been associated with numerous side effects. However, the renal-specific effect of mTOR inhibitor treatment cessation in polycystic kidney disease is currently unknown. Therefore, we compared pulse and continuous everolimus treatment in Han:SPRD rats. Four-week-old male heterozygous polycystic and wild-type rats were administered everolimus or vehicle by gavage feeding for 5 wk, followed by 7 wk without treatment, or continuously for 12 wk. Cessation of everolimus did not result in the appearance of renal cysts up to 7 wk postwithdrawal despite the reemergence of S6 kinase activity coupled with an overall increase in cell proliferation. Pulse everolimus treatment resulted in striking noncystic renal parenchymal enlargement and glomerular hypertrophy that was not associated with compromised kidney function. Both treatment regimens ameliorated kidney function, preserved the glomerular-tubular connection, and reduced proteinuria. Pulse treatment at an early age delays cyst development but leads to striking glomerular and parenchymal hypertrophy. Our data might have an impact when long-term treatment using mTOR inhibitors in patients with autosomal dominant polycystic kidney disease is being considered.
机译:目前正在受常染色体显性遗传多囊肾疾病影响的患者中测试哺乳动物雷帕霉素靶标(mTOR)的疗效。用mTOR抑制剂治疗与许多副作用有关。然而,目前尚不清楚在多囊性肾脏疾病中停止mTOR抑制剂治疗的肾脏特异性作用。因此,我们比较了Han:SPRD大鼠的脉冲和连续依维莫司治疗。给四周大的雄性杂合多囊性和野生型大鼠通过饲喂法饲喂依维莫司或媒介物5周,然后不治疗地连续7周,或连续12周。依维莫司的戒断在戒断后直至7周内都不会导致肾囊肿的出现,尽管S6激酶活性重新出现,同时细胞增殖总体增加。脉冲依维莫司治疗导致非囊性肾实质实质增大和肾小球肥大,与肾脏功能受损无关。两种治疗方案均可改善肾功能,保留肾小球-肾小管连接,并减少蛋白尿。早期进行脉冲治疗可延缓囊肿的发展,但会导致肾小球和实质性肥大。当考虑在常染色体显性多囊肾病患者中使用mTOR抑制剂进行长期治疗时,我们的数据可能会产生影响。

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