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Birmingham vasculitis activity and chest manifestation at diagnosis can predict hospitalised infection in ANCA-associated vasculitis

机译:伯明翰血管炎活动和胸部表现在诊断中可以预测ANCA相关血管炎的住院感染

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We investigated the development rate and time, risk factors, predictors, and aetiologies of hospitalised infection in Korean patients with anti-neutrophil cytoplasmic antibody (ANCA)-associated vasculitis (AAV). We retrospectively reviewed the medical records of 154 patients with AAV. Hospitalised infection was considered only when patients were admitted for serious infection related to AAV or AAV treatment. The gap-time was defined as the period from diagnosis to the first hospitalised infection or to the last visit for uninfected patients. We calculated Birmingham vasculitis activity score (BVAS) or BVAS for granulomatosis with polyangiitis (GPA) and five factor score (FFS (2009)) and reviewed medications administered. We set the optimal cut-offs of BVAS and that of FFS (2009) at diagnosis at 20.5 and 1.5. Forty-four patients (28.6%) were admitted for serious infection. One-, 5- and 10-year hospitalised infection free survival rates were 85.1, 77.9 and 72.7%, respectively. In multivariable logistic regression analysis of significant variables in comparison analysis, only chest manifestation at diagnosis (OR 2.692) was remarkably associated with hospitalised infection. In multivariable Cox hazard model analysis of significant variables in Kaplan-Meier analysis, BVAS at diagnosis 20.5 (HR 2.375) and chest manifestation at diagnosis (HR 2.422) were independent predictors of hospitalised infection during the gap-time. Bacterial pneumonia was the most common infectious aetiology (N = 29), followed by fungal infection including aspergillosis (N = 6). BVAS and chest manifestation at diagnosis can predict hospitalised infection during the gap-time.
机译:我们调查了韩国抗中性粒细胞细胞质抗体(ANCA) - 分配血管炎(AAV)的韩国患者住院感染的开发率和时间,危险因素,预测因子和疾病。我们回顾性地审查了154名AAV患者的病历。只有当患者因与AAV或AAV治疗相关的严重感染时,才考虑住院感染。间隙时间被定义为从诊断到第一次住院感染的时间或最后一次访问未感染的患者。我们计算伯明翰血管炎活动评分(BVAS)或BVA,用于肉芽肿(GPA)和五因素评分(FFS(2009))和审查给药的药物。我们在20.5和1.5的诊断中设置了BVA的最佳截止和FFS(2009)。患有44名患者(28.6%)被认真感染。一年,5年和10年住院感染的免疫存活率分别为85.1,77.9和72.7%。在比较分析中显着变量的多变量逻辑回归分析中,只有诊断(或2.692)的胸部表现出显着与住院感染有关。在Kaplan-Meier分析中的显着变量的多变量的多变量Cox危险模型中,BVA在诊断时诊断(HR 2.422)和胸部表现(HR 2.422)是间隙时间内住院感染的独立预测因子。细菌性肺炎是最常见的传染病学(n = 29),其次是小曲霉(n = 6)的真菌感染。在诊断时,BVA和胸部表现可以预测间隙时间内的住院感染。

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