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首页> 外文期刊>BMC Nephrology >Obesity is not associated with progression to end stage renal disease in patients with biopsy-proven glomerular diseases
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Obesity is not associated with progression to end stage renal disease in patients with biopsy-proven glomerular diseases

机译:肥胖与活组织检查成熟的肾小球疾病患者的进展无关

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摘要

Body mass index (BMI) is associated with renal disease progression in unspecified CKD. The relationship between BMI and primary glomerular disease (GN) may be more complex. We aimed to evaluate the association between BMI and renal disease progression in patients with primary glomerular disease (GN). This was a single-centre retrospective cohort study performed in adult patients with biopsy-proven primary GN (excluding minimal change disease) from January 2000 to December 2015, with follow-up data until June 2017. BMI at time of biopsy was categorised as ≤25?kg/m2?25 to ≤30?kg/m2?30?kg/m2. We used univariate and multivariate survival analyses to evaluate factors associated with progression to a composite endpoint of stage 5 CKD or renal replacement therapy (Major Adverse Renal Event - MARE) censoring for competing risk of death using Fine and Gray subdistribution hazards model. We included 560 patients with biopsy-proven primary GN and available BMI data: 66.1% were male with median age 54.8 (IQR 41.1-66.2) years and BMI 28.2 (IQR 24.9-32.1) kg/m2. Those with BMI 25-30?kg/m2?30?kg/m2 (n?=?207) were older (p?=?0.007) with higher systolic and diastolic blood pressures (p?=?0.02 and 0.004 respectively) than those with BMI ?25?kg/m2 (n?=?132). There was a greater proportion of focal segmental glomerulosclerosis in those with higher BMI (3.9% in BMI ?25?kg/m2, 7.9% in BMI 25-30?kg/m2?30?kg/m2 of biopsies (p?=?0.01)), but similar proportions of other GN diagnoses across BMI groups. Baseline eGFR (p?=?0.40) and uPCR (p?=?0.17) were similar across BMI groups. There was no interaction between BMI and time to MARE (log-rank p?=?0.98) or death (log-rank p?=?0.42). Censoring for competing risk of death, factors associated with progression to MARE were: younger age, lower baseline eGFR and higher uPCR, but not BMI (SHR 0.99, 95%CI 0.97-1.01, p?=?0.31) nor blood pressure or GN diagnosis. BMI was not associated with progression to MARE in this patient cohort with primary GN. Efforts should be directed to managing other known risk factors for CKD progression.
机译:体重指数(BMI)与未指明的CKD中的肾病进展相关。 BMI和初级肾小球疾病(GN)之间的关系可能更复杂。我们旨在评估初级肾小球疾病患者(GN)患者BMI与肾病进展的关联。这是一个单中心回顾性队列研究,在2000年1月至2015年1月到2015年1月到2015年12月的成人验证的原发性GN(不包括最小变化疾病)进行了一项研究,直到2017年6月到2017年6月。活检时的BMI被分类为≤ 25?kg / m2?25至≤30?kg / m2?30?kg / m2。我们使用单变量和多变量的存活分析来评估与阶段5 CKD或肾置换疗法(主要不利肾事件 - MARE)的综合终点相关的因素进行审查,用于使用细小和灰色分布危害模型进行竞争死亡风险。我们包括560名活组织检查验证的主要GN患者,可用的BMI数据:66.1%是男性,中位数54.8岁(IQR 41.1-66.2)年和BMI 28.2(IQR 24.9-32.1)KG / M2。 BMI 25-30的那些kg / m2?30?kg / m2(n?=Δ207)较旧(p?= 0.007),具有较高的收缩量和舒张血压(p≤x0.02和0.004)比那些有BMI的人<25?kg / m2(n?=?132)。在具有较高BMI的局灶性节段性肾小球粥样硬化比例较高(BMI中的3.9%,BMI25Ω·kg / m 2,BMI 25-30 kg / m 2,7.9%?kg / m2?30?kg / m2的活组织检查(p?= ?0.01)),但在BMI组上的其他GN诊断的类似比例。基线EGFR(p?= 0.40)和UPCR(p?= 0.17)横跨BMI组相似。 BMI与母马的时间之间没有相互作用(日志排名P?=?0.98)或死亡(日志排名P?= 0.42)。竞争死亡风险的审查,与母马的进展相关的因素是:较年轻,较低的基线EGFR和更高的UPCR,但不是BMI(SHR 0.99,95%CI 0.97-1.01,P?= 0.31)也不是血压或GN诊断。 BMI与本患者队列的母马与初级GN的进展无关。应该努力管理CKD进展的其他已知风险因素。

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