D-dimer levels in assessing severity and clinical outcome in patients with community-acquired pneumonia. A secondary analysis of a randomised clinical trial

SnijdersD.; SchoorlM.; BartelsP.C.; VanDerWerfT.S.; BoersmaW.G.

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D-dimer levels in assessing severity and clinical outcome in patients with community-acquired pneumonia. A secondary analysis of a randomised clinical trial

机译：D-二聚体水平在评估社区获得性肺炎患者的严重程度和临床结局方面。一项随机临床试验的二级分析

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Background: D-dimer levels are in several studies elevated in patients with CAP. In this study we assess the use of D-dimer levels and its association with severity assessment and clinical outcome in patients hospitalised with community-acquired pneumonia. Methods: In a subset of randomised trial patients with community-acquired pneumonia serial D-dimer levels was analysed. CURB-65 scores were calculated at admission. Results: A total of 147 patients were included. D-dimer levels at admission were higher in patients with severe CAP (2166 ± 1258 versus1630 ± 1197 μg/l, p = 0.03), with clinical failure at day 30 (2228 ± 1512 versus 1594 ± 1078 μg/l, p = 0.02) and with early failure (2499 ± 1817 μg/l versus 1669 ± 1121 μg/l, p = 0.01). Non-survivors had higher D-dimer levels (3025 ± 2105 versus 1680 ± 1128 μg/l, p = 0.05). None of the 16 patients with D-dimer levels < 500 μg/l died. In multivariate analysis D-dimer levels were not associated with clinical outcome. D-dimer levels have poor accuracy for predicting clinical outcome at day 30 (AUC 0.62, 95% CI 0.51-0.73) or 30 day mortality (AUC 0.71 (95% CI 0.51-0.91)). Addition of D-dimer levels to CURB-65 did not increase accuracy. No differences were observed in serial D-dimer levels between patients with clinical success or failure at day 30. Conclusion: D-dimer levels are elevated in patients with CAP. Significantly higher D-dimer levels are found in patients with clinical failure and with severe CAP. D-dimer levels as single biomarker or as addition to the CURB-65 have no added value for predicting clinical outcome or mortality. D-dimer levels < 500 μg/l may identify candidates at low risk for complications.

机译：背景：在几项研究中，CAP患者的D-二聚体水平升高。在这项研究中，我们评估了社区获得性肺炎住院患者中D-二聚体水平的使用及其与严重程度评估和临床结局的关系。方法：在一项随机试验的亚组中，分析社区获得性肺炎系列D-二聚体水平。入院时计算CURB-65分数。结果：共纳入147例患者。患有严重CAP的患者入院时D-二聚体水平较高（2166±1258对1630±1197μg/ l，p = 0.03），第30天临床失败（2228±1512对1594±1078μg/ l，p = 0.02 ）并具有早期故障（2499±1817μg/ l与1669±1121μg/ l，p = 0.01）。非幸存者具有更高的D-二聚体水平（3025±2105与1680±1128μg/ l，p = 0.05）。 D-二聚体水平<500μg/ l的16名患者均未死亡。在多变量分析中，D-二聚体水平与临床结果无关。 D-二聚体水平在第30天（AUC 0.62，95％CI 0.51-0.73）或30天死亡率（AUC 0.71（95％CI 0.51-0.91））预测临床结果的准确性较差。在CURB-65中添加D-二聚体水平不会提高准确性。在第30天，临床成功或失败的患者之间的连续D-二聚体水平未见差异。结论：CAP患者的D-二聚体水平升高。临床衰竭和严重CAP的患者发现D-二聚体水平显着升高。 D-二聚体水平作为单一生物标志物或作为CURB-65的补充物，对预测临床结果或死亡率没有附加价值。 D-二聚体水平<500μg/ l可能会确定低并发症发生率的候选人。

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《European journal of internal medicine》 |2012年第5期|共6页
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SnijdersD.; SchoorlM.; BartelsP.C.; VanDerWerfT.S.; BoersmaW.G.;
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正文语种 eng
中图分类内科学;
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Biomarker; Community-acquired pneumonia; CURB-65; D-dimer; Severity scores;

机译：生物标志物;社区获得性肺炎;CURB-65;D-二聚体;严重程度评分;

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D-dimer levels in assessing severity and clinical outcome in patients with community-acquired pneumonia. A secondary analysis of a randomised clinical trial

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