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疑似感染患者中C反应蛋白反应与抗生素处方之间的相互作用。

Interplay between C-reactive protein responses and antibiotic prescribing in people with suspected infection.

作者信息

Gu Qingze, Yuan Kevin, Wei Jia, Yoon Chang Ho, Danielsen Anders Skyrud, Luk Augustine, Eyre David W, Walker A Sarah

机构信息

Nuffield Department of Medicine, University of Oxford, Oxford, UK.

Nuffield Department of Population Health, Big Data Institute, University of Oxford, Oxford, UK.

出版信息

BMC Infect Dis. 2025 Aug 5;25(1):987. doi: 10.1186/s12879-025-11381-9.

Abstract

BACKGROUND

Serial measurements of C-reactive protein (CRP) are often taken in hospitals to assess recovery from infection, but their utility remains debated. Previous studies, including our development of CRP centile reference charts for suspected bloodstream infections (BSI), suggest variability in CRP responses across infection types. Here we investigated the association between serial CRP percentile changes, antibiotic prescribing patterns, and patient outcomes in a large cohort with suspected infection, acknowledging that CRP is one of multiple factors in clinical decision-making.

METHODS

We analysed 51,544 suspected infection episodes (defined by blood culture collection) from 36,578 patients in Oxfordshire, UK (2016-2021). Episodes were categorised by blood culture results: Gram-positive, Gram-negative, polymicrobial, contaminants, or culture-negative (having previously shown that 51% culture-negatives have CRP responses indistinguishable from culture-positives). The spectrum of antibiotic prescriptions and their changes over time were tracked. Multinomial logistic regression, adjusted for clinical covariates, assessed the association between CRP percentile changes and subsequent prescribing decisions. Linear mixed models evaluated CRP trajectories post-prescribing, and logistic regression associations between early CRP changes (days 1-4) and 5-30-day mortality.

RESULTS

Broad-spectrum antibiotics were predominantly used within the first three days after blood culture collection, followed by a notable shift to narrow-spectrum antibiotics for Gram-positive infections, but with slower de-escalation for Gram-negative and polymicrobial infections. CRP percentile changes were modestly associated with subsequent antibiotic adjustments; in particular, suboptimal recovery, indicated by an increase in CRP centiles, was associated with a higher rate of antibiotic escalation (16.5% vs. 10.7% in expected recovery) and, conversely, faster than expected recovery in CRP was associated with de-escalation (23.6% vs. 17.2%). However, 61.8% of decisions were unchanged despite CRP trends. The relationship between various prescribing decisions and subsequent CRP percentile changes was complex and challenging to estimate, likely due to testing bias. CRP percentile changes during the 4 days post blood culture collection were strongly associated with 5-30-day mortality, highlighting their potential utility as a prognostic indicator.

CONCLUSIONS

While CRP monitoring can inform antibiotic stewardship, its association with prescribing decisions is probably only modest, underscoring the need to integrate a range of clinical factors to optimise infection management.

摘要

背景

医院经常对C反应蛋白(CRP)进行系列测量,以评估感染后的恢复情况,但其效用仍存在争议。先前的研究,包括我们为疑似血流感染(BSI)制定CRP百分位数参考图表的研究,表明不同感染类型的CRP反应存在差异。在此,我们调查了一大群疑似感染患者的系列CRP百分位数变化、抗生素处方模式与患者预后之间的关联,同时认识到CRP只是临床决策中的多个因素之一。

方法

我们分析了英国牛津郡36578名患者的51544次疑似感染发作(通过血培养采集定义,时间为2016 - 2021年)。发作根据血培养结果分类:革兰氏阳性、革兰氏阴性、混合菌感染、污染物或培养阴性(此前已表明51%的培养阴性患者的CRP反应与培养阳性患者难以区分)。追踪抗生素处方的范围及其随时间的变化。在对临床协变量进行调整后,采用多项逻辑回归评估CRP百分位数变化与后续处方决策之间的关联。线性混合模型评估处方后CRP的变化轨迹,以及早期CRP变化(第1 - 4天)与5 - 30天死亡率之间的逻辑回归关联。

结果

广谱抗生素主要在血培养采集后的头三天内使用,随后对于革兰氏阳性感染明显转向窄谱抗生素,但革兰氏阴性和混合菌感染的降阶梯速度较慢。CRP百分位数变化与随后的抗生素调整有适度关联;特别是,CRP百分位数升高表明恢复欠佳,与抗生素升级率较高相关(预期恢复组为10.7%,恢复欠佳组为16.5%),相反,CRP恢复快于预期与降阶梯相关(预期恢复组为17.2%,恢复快于预期组为23.6%)。然而,尽管有CRP趋势,61.8%的决策未改变。各种处方决策与随后的CRP百分位数变化之间的关系复杂且难以估计,可能是由于检测偏倚。血培养采集后4天内的CRP百分位数变化与5 - 30天死亡率密切相关,突出了其作为预后指标的潜在效用。

结论

虽然CRP监测可为抗生素管理提供信息,但其与处方决策的关联可能仅为适度,这强调了整合一系列临床因素以优化感染管理的必要性。

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