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首页> 外文期刊>BMC Nephrology >Urine concentration ability is reduced to the same degree in adult dominant polycystic kidney disease compared with other chronic kidney diseases in the same CKD-stage and lower THAN in healthy control subjects - a CASE control study
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Urine concentration ability is reduced to the same degree in adult dominant polycystic kidney disease compared with other chronic kidney diseases in the same CKD-stage and lower THAN in healthy control subjects - a CASE control study

机译:与同一CKD-阶段的其他慢性肾疾病相比,尿液浓度能力降低到成人占多环肾病中的相同程度,低于健康对照组织 - 一种案例对照研究

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Concentration of the urine is primarily regulated via vasopressin dependent aquaporin-2 water channels in the apical membrane of kidney principal cells. It is unclear whether urine concentration ability in ADPKD differs from other patients with similar degree of impaired renal function (non-ADPKD patients). The purpose of this case control study was to measure urine concentration ability in ADPKD patients compared to non-ADPKD patients and healthy controls. A seventeen hour long water deprivation test was carried out in 17 ADPKD patients (CKD I-IV), 16 non-ADPKD patients (CKD I-IV), and 18 healthy controls. Urine was collected in 4 consecutive periods during water deprivation (12?h, 1?h, 2?h and 2?h, respectively) and analyzed for osmolality (u-Osm), output (UO), fractional excretion of sodium (FENa), aquaporin2 (u-AQP2) and ENaC (u-ENaC). Blood samples were drawn trice (after 13-, 15-, and 17?h after water deprivation) for analyses of osmolality (p-Osm), vasopressin (p-AVP), and aldosterone (p-Aldo). U-Osm was significantly lower and FENa significantly higher in both ADPKD patients and non-ADPKD patients compared to healthy controls during the last three periods of water deprivation. During the same periods, UO was higher and secretion rates of u-AQP2 and u-ENaC were lower and at the same level in the two groups of patients compared to controls. P-AVP and p-Osm did not differ significantly between the three groups. P-Aldo was higher in both groups of patients than in controls. Urine concentration ability was reduced to the same extent in patients with ADPKD and other chronic kidney diseases with the same level of renal function compared to healthy controls. The lower urine excretion of AQP2 and ENaC suggests that the underlying mechanism may be a reduced tubular response to vasopressin and aldosterone. Current Controlled Trial NCT04363554 , date of registration: 20.08.2017.
机译:尿液浓度主要通过肾主细胞的顶端膜中的血压加压素依赖性水素-2水通道调节。目前尚不清楚ADPKD中尿液浓度能力是否与肾功能受损相似程度(非ADPKD患者)的其他患者不同。与非ADPKD患者和健康对照相比,这种情况控制研究的目的是测量ADPKD患者的尿液浓度能力。在17例ADPKD患者(CKD I-IV),16名非ADPKD患者(CKD I-IV)和18例健康对照中进行了17个小时的缺水试验。在水剥夺期间在4个连续时间内收集尿液(分别为12?H,1?H,2·H和2·H,分析渗透压(U-OSM),输出(UO),钠分数排泄(Fena ),Aquaporin2(U-AQP2)和ENAC(U-ENAC)。血液样品被拉出滴眼液(在水剥夺后13-,15-和17·H后)用于分析渗透压溶液(P-OSM),加压加压素(P-AVP)和醛固酮(P-ALDO)。 u-OSM显着较低,患者和非ADPKD患者的福尼显着较高,与过去三期的水剥夺期间的健康对照。在同一时期,UO更高,与对照相比,两组患者中的U-AQP2和U-ENAC的分泌率较高,在同一水平下。 P-AVP和P-OSM在三组之间没有显着差异。两组患者的P-Aldo比对照组更高。与健康对照相比,尿液浓度能力降低到患者患者和其他慢性肾功能较为肾功能水平相同的慢性肾功能的程度。 AQP2和ENAc的尿液排泄较低表明潜在机制可能是对血压加压素和醛固酮的减少的管状反应。目前对照试验NCT04363554,日期(注册):20.08.2017。

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