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血浆微生物无细胞游离 DNA 下一代测序在发热性中性粒细胞减少症的诊断和管理中的应用。

Plasma Microbial Cell-free DNA Next-generation Sequencing in the Diagnosis and Management of Febrile Neutropenia.

机构信息

School of Medicine, Division of Infectious Diseases, University of Colorado Denver, Aurora, Colorado, USA.

Division of Infectious Diseases, Carolinas Medical Center, Atrium Health, Charlotte, North Carolina, USA.

出版信息

Clin Infect Dis. 2022 May 3;74(9):1659-1668. doi: 10.1093/cid/ciab324.

Abstract

BACKGROUND

Standard testing fails to identify a pathogen in most patients with febrile neutropenia (FN). We evaluated the ability of the Karius microbial cell-free DNA sequencing test (KT) to identify infectious etiologies of FN and its impact on antimicrobial management.

METHODS

This prospective study (ClinicalTrials.gov; NCT02912117) enrolled and analyzed 55 patients with FN. Up to 5 blood samples were collected per subject within 24 hours of fever onset (T1) and every 2 to 3 days. KT results were compared with blood culture (BC) and standard microbiological testing (SMT) results.

RESULTS

Positive agreement was defined as KT identification of ≥1 isolate also detected by BC. At T1, positive and negative agreement were 90% (9/10) and 31% (14/45), respectively; 61% of KT detections were polymicrobial. Clinical adjudication by 3 independent infectious diseases specialists categorized Karius results as: unlikely to cause FN (N = 0); definite (N = 12): KT identified ≥1 organism also found by SMT within 7 days; probable (N = 19): KT result was compatible with a clinical diagnosis; possible (N = 10): KT result was consistent with infection but not considered a common cause of FN. Definite, probable, and possible cases were deemed true positives. Following adjudication, KT sensitivity and specificity were 85% (41/48) and 100% (14/14), respectively. Calculated time to diagnosis was generally shorter with KT (87%). Adjudicators determined real-time KT results could have allowed early optimization of antimicrobials in 47% of patients, by addition of antibacterials (20%) (mostly against anaerobes [12.7%]), antivirals (14.5%), and/or antifungals (3.6%); and antimicrobial narrowing in 27.3% of cases.

CLINICAL TRIALS REGISTRATION

NCT02912117.

CONCLUSION

KT shows promise in the diagnosis and treatment optimization of FN.

摘要

背景

标准检测未能确定大多数发热性中性粒细胞减少症(FN)患者的病原体。我们评估了卡里乌斯微生物无细胞 DNA 测序检测(KT)识别 FN 的传染性病因及其对抗菌药物管理的影响的能力。

方法

这项前瞻性研究(ClinicalTrials.gov;NCT02912117)纳入并分析了 55 例 FN 患者。每位患者在发热发作后 24 小时内(T1)最多采集 5 份血样,每 2-3 天采集一次。KT 结果与血培养(BC)和标准微生物学检测(SMT)结果进行比较。

结果

阳性一致定义为 KT 鉴定的≥1 种分离株也被 BC 检测到。在 T1 时,阳性和阴性一致率分别为 90%(9/10)和 31%(14/45);61%的 KT 检测为混合感染。由 3 名独立的传染病专家进行临床判断,将卡里乌斯的结果分为:不太可能引起 FN(N=0);确定(N=12):KT 鉴定的≥1 种微生物在 7 天内也通过 SMT 检测到;可能(N=19):KT 结果与临床诊断相符;可能(N=10):KT 结果与感染相符,但不被认为是 FN 的常见原因。确定、可能和可能的病例被认为是真正的阳性。经判断后,KT 的灵敏度和特异性分别为 85%(41/48)和 100%(14/14)。一般来说,KT 的诊断时间更短(87%)。判断者确定实时 KT 结果可使 47%的患者通过添加抗菌药物(20%)(主要针对厌氧菌[12.7%])、抗病毒药物(14.5%)和/或抗真菌药物(3.6%)来优化抗菌药物;并使 27.3%的病例减少抗菌药物的使用。

临床试验注册

NCT02912117。

结论

KT 在 FN 的诊断和治疗优化方面显示出前景。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/a23d/9070798/62d3efbe4b85/ciab324f0001.jpg

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