药物对血清甲状旁腺激素、磷和钙水平的影响与 CKD 患者死亡率的关系：一项荟萃分析。

Association of Drug Effects on Serum Parathyroid Hormone, Phosphorus, and Calcium Levels With Mortality in CKD: A Meta-analysis.

机构信息

Department of Medicine, University of Otago, Christchurch, New Zealand.

Sydney School of Public Health, University of Sydney, NSW, Australia.

出版信息

Am J Kidney Dis. 2015 Dec;66(6):962-71. doi: 10.1053/j.ajkd.2015.03.036. Epub 2015 May 21.

DOI:10.1053/j.ajkd.2015.03.036

PMID:26003472

Abstract

BACKGROUND: Serum parathyroid hormone (PTH), phosphorus, and calcium levels are surrogate outcomes that are central to the evaluation of drug treatments in chronic kidney disease (CKD). This systematic review evaluates the evidence for the correlation between drug effects on biochemical (PTH, phosphorus, and calcium) and all-cause and cardiovascular mortality end points in adults with CKD. STUDY DESIGN: Systematic review and meta-analysis. SETTING & POPULATION: Adults with CKD. SELECTION CRITERIA FOR STUDIES: Randomized trials reporting drug effects on biochemical and mortality end points. INTERVENTION: Drug interventions with effects on serum PTH, phosphorus, and calcium levels, including vitamin D compounds, phosphate binders, cinacalcet, bisphosphonates, and calcitonin. OUTCOMES: Correlation between drug effects on biochemical and all-cause and cardiovascular mortality. RESULTS: 28 studies (6,999 participants) reported both biochemical and mortality outcomes and were eligible for analysis. Associations between drug effects on surrogate biochemical end points and corresponding effects on mortality were weak and imprecise. All correlation coefficients were less than 0.70, and 95% credible intervals were generally wide and overlapped with zero, consistent with the possibility of no association. The exception was an inverse correlation between drug effects on serum PTH levels and all-cause mortality, which was nominally significant (-0.64; 95% credible interval, -0.85 to -0.15), but the strength of this association was very imprecise. Risk of bias within available trials was generally high, further reducing confidence in the summary correlations. Findings were robust to adjustment for age, baseline serum PTH level, allocation concealment, CKD stage, and drug class. LIMITATIONS: Low power in analyses and combining evidence from many different drug comparisons with incomplete data across studies. CONCLUSIONS: Drug effects on serum PTH, phosphorus, and calcium levels are weakly and imprecisely correlated with all-cause and cardiovascular death in the setting of CKD. Risks of mortality (patient-level outcome) cannot be inferred from treatment-induced changes in biochemical outcomes in people with CKD. Similarly, existing data do not exclude a mortality benefit with treatment. Trials need to address patient-centered outcomes to evaluate drug effectiveness in this setting.

摘要

背景：血清甲状旁腺激素（PTH）、磷和钙水平是评估慢性肾脏病（CKD）药物治疗的关键替代指标。本系统评价评估了药物对 CKD 成人的生化指标（PTH、磷和钙）以及全因和心血管死亡率终点的影响与药物效果之间的相关性。

研究设计：系统评价和荟萃分析。

研究场所和人群：CKD 成人。

纳入研究的标准：报告药物对生化和死亡率终点影响的随机试验。

干预措施：包括维生素 D 化合物、磷结合剂、西那卡塞、双膦酸盐和降钙素在内的药物干预，以影响血清 PTH、磷和钙水平。

结局：药物对生化指标和全因及心血管死亡率的影响之间的相关性。

结果：28 项研究（6999 名参与者）报告了生化和死亡率结果，符合分析条件。药物对替代生化终点的影响与对死亡率的相应影响之间的相关性较弱且不精确。所有相关系数均小于 0.70，95%可信区间通常较宽，与零重叠，表明可能不存在关联。唯一的例外是药物对血清 PTH 水平的影响与全因死亡率之间呈负相关，这在名义上具有显著性（-0.64；95%可信区间，-0.85 至-0.15），但这种关联的强度非常不精确。可用试验中的偏倚风险普遍较高，进一步降低了对汇总相关性的置信度。在调整年龄、基线血清 PTH 水平、分配隐匿、CKD 分期和药物类别后，结果仍然稳健。

局限性：分析的效能较低，并且对来自许多不同药物比较的证据进行了合并，而这些比较在研究之间的数据并不完整。

结论：在 CKD 环境下，药物对血清 PTH、磷和钙水平的影响与全因和心血管死亡的相关性较弱且不精确。不能从 CKD 患者的生化结果治疗诱导变化推断出死亡率（患者水平结局）的风险。同样，现有数据也不排除治疗有生存获益的可能。试验需要解决以患者为中心的结局，以评估该环境下的药物疗效。