下颌骨重建后骨皮皮瓣相关骨髓炎:一项新出现的复杂骨感染的队列研究。

IF 1.8 Q3 INFECTIOUS DISEASES
Journal of Bone and Joint Infection Pub Date : 2022-06-10 eCollection Date: 2022-01-01 DOI:10.5194/jbji-7-127-2022
Clément Javaux, Clémentine Daveau, Clotilde Bettinger, Mathieu Daurade, Céline Dupieux-Chabert, Fabien Craighero, Carine Fuchsmann, Philippe Céruse, Arnaud Gleizal, Nicolas Sigaux, Tristan Ferry, Florent Valour, The Lyon Bji Study Group
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引用次数: 0

摘要

骨皮瓣(OCF)下颌骨重建术存在手术部位感染的高风险。本研究旨在描述ocf相关性骨髓炎的诊断、治疗和预后。在我院治疗的所有下颌骨重建后ocf相关骨髓炎患者均纳入回顾性队列研究(2012-2019)。微生物学根据金标准手术样本进行描述,考虑到所有有毒病原体,以及至少两个样本上存在的潜在污染物。采用logistic回归和Kaplan-Meier曲线分析评估治疗失败的决定因素。纳入的48例患者(中位年龄60.5 (IQR, 52.4-66.6)岁)受益于OCF下颌骨重建,主要用于癌症(n = 27 / 48;56.3% %)或放射性骨坏死(n = 12 / 48;25.0 %)。ocf相关性骨髓炎多为早期(术后≤3个月;N = 43 / 48;89.6 %),表现为局部炎症(n = 28 / 47;59.6 %),不愈合(伤口裂开)或窦道(n = 28 / 47;59.6 %)和/或骨骼或器械暴露(n = 21 / 47;44.7 %)。主要病原为肠杆菌科(n = 25 / 41;61.0 %),链球菌(n = 22 / 41;53.7 %),金黄色葡萄球菌(n = 10 / 41;24.4 %),肠球菌(n = 9 / 41;22.0 %),非发酵革兰氏阴性杆菌(n = 8 / 41;19.5 %),厌氧菌(n = 8 / 41;19.5 %)。39例患者(81.3 %)受益于手术,包括25 / 39例(64.1 %)的清除术和种植体保留(DAIR),与93 (IQR, 64-128)天的抗菌治疗相关。随访18 (IQR, 11-31)个月,治疗失败24 / 48(50.0 %)。治疗结果的决定因素为DAIR (OR, 3.333;95 % CI, 1.020-10.898)和早期传染病专科转诊(≤2周OR, 0.236;95 % ci, 0.062-0.933)。下颌骨重建术后ocf相关性骨髓炎是难以治疗的感染。我们的研究结果提倡多学科管理,包括由复杂的微生物文献驱动的早期传染病专家转诊来管理抗菌治疗。
本文章由计算机程序翻译,如有差异,请以英文原文为准。

Osteocutaneous-flap-related osteomyelitis following mandibular reconstruction: a cohort study of an emerging and complex bone infection.

Osteocutaneous-flap-related osteomyelitis following mandibular reconstruction: a cohort study of an emerging and complex bone infection.

Osteocutaneous flap (OCF) mandible reconstruction is at high risk for surgical site infection. This study aimed to describe diagnosis, management, and outcome of OCF-related osteomyelitis. All patients managed at our institution for an OCF-related osteomyelitis following mandible reconstruction were included in a retrospective cohort study (2012-2019). Microbiology was described according to gold-standard surgical samples, considering all virulent pathogens, and potential contaminants if present on at least two samples. Determinants of treatment failure were assessed by logistic regression and Kaplan-Meier curve analysis. The 48 included patients (median age 60.5 (IQR, 52.4-66.6) years) benefited from OCF mandible reconstruction mostly for carcinoma ( n = 27 / 48 ; 56.3 %) or osteoradionecrosis ( n = 12 / 48 ; 25.0 %). OCF-related osteomyelitis was mostly early ( 3 months post-surgery; n = 43 / 48 ; 89.6 %), presenting with local inflammation ( n = 28 / 47 ; 59.6 %), nonunion (wound dehiscence) or sinus tract ( n = 28 / 47 ; 59.6 %), and/or bone or device exposure ( n = 21 / 47 ; 44.7 %). Main implicated pathogens were Enterobacteriaceae ( n = 25 / 41 ; 61.0 %), streptococci ( n = 22 / 41 ; 53.7 %), Staphylococcus aureus ( n = 10 / 41 ; 24.4 %), enterococci ( n = 9 / 41 ; 22.0 %), non-fermenting Gram-negative bacilli ( n = 8 / 41 ; 19.5 %), and anaerobes ( n = 8 / 41 ; 19.5 %). Thirty-nine patients (81.3 %) benefited from surgery, consisting of debridement with implant retention (DAIR) in 25 / 39 (64.1 %) cases, associated with 93 (IQR, 64-128) days of antimicrobial therapy. After a follow-up of 18 (IQR, 11-31) months, 24 / 48 (50.0 %) treatment failures were observed. Determinants of treatment outcomes were DAIR (OR, 3.333; 95 % CI, 1.020-10.898) and an early infectious disease specialist referral (OR, 0.236 if 2  weeks; 95 % CI, 0.062-0.933). OCF-related osteomyelitis following mandibular reconstruction represents difficult-to-treat infections. Our results advocate for a multidisciplinary management, including an early infectious-disease-specialist referral to manage the antimicrobial therapy driven by complex microbiological documentation.

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