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Does Secretory Clearance Follow Glomerular Filtration Rate in Chronic Kidney Diseases? Reconsidering the Intact Nephron Hypothesis

机译:在慢性肾脏疾病中分泌清除是否遵循肾小球滤过率?重新考虑完整的Nephron假设

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摘要

Drug‐dose modification in chronic kidney disease (CKD) utilizes glomerular filtration rate (GFR) with the implicit assumption that multiple renal excretory processes decline in parallel as CKD progresses. We compiled published pharmacokinetic data to evaluate if GFR predicts renal clearance changes as a function of CKD severity. For each drug, we calculated ratio of renal clearance to filtration clearance (Rnf). Of 21 drugs with Rnf >0.74 in subjects with GFR >90 mL/min (implying filtration and secretion), 13 displayed significant change in Rnf vs. GFR (slope of linear regression statistically different from zero), which indicates failure of GFR to predict changes in secretory clearance. The dependence was positive (n = 3; group A) or negative (n = 10; group B). Eight drugs showed no correlation (group C). Investigated drugs were small molecules, mostly hydrophilic, and ionizable, with some characterized as renal transporter substrates. In conclusion, dosing adjustments in CKD require refinement; in addition to GFR, biomarkers of tubular function are needed for secreted drugs.
机译:慢性肾脏病(CKD)中的药物剂量调整利用肾小球滤过率(GFR),隐含的假设是随着CKD的发展,多个肾脏排泄过程平行下降。我们汇总了已发表的药代动力学数据,以评估GFR是否预测肾清除率随CKD严重程度而变。对于每种药物,我们计算了肾脏清除率与过滤清除率(Rnf)的比率。在GFR> 90 mL / min的受试者中21种Rnf> 0.74的药物(暗示过滤和分泌)中,有13种Rnf与GFR的变化显着(线性回归的斜率在统计学上不同于零),这表明GFR无法预测分泌清除率的变化。依赖性为正(n = 3; A组)或负(n = 10; B组)。八种药物没有相关性(C组)。研究的药物为小分子,大部分为亲水性且可离子化,其中一些特征为肾脏转运底物。总之,CKD的剂量调整需要完善。除了GFR,分泌药物还需要肾小管功能的生物标志物。

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