复发霍奇金淋巴瘤大剂量化疗后的特发性肺炎综合征
Idiopathic pneumonia syndrome after high-dose chemotherapy for relapsed Hodgkin's disease.
作者信息
Rubio C, Hill M E, Milan S, O'Brien M E, Cunningham D
机构信息
The Cancer Research Campaign Section of Medicine, The Royal Marsden Hospital, Sutton, Surrey, UK.
出版信息
Br J Cancer. 1997;75(7):1044-8. doi: 10.1038/bjc.1997.178.
The risk of idiopathic pneumonia syndrome (IPS) in patients with Hodgkin's disease (HD) undergoing high-dose chemotherapy (HDC) is significant, and once developed IPS is potentially fatal. The aim of this study was to quantify this risk accurately and determine prognostic factors for its development and course. Using a computerized database, all patients with HD treated with BCNU (carmustine) containing HDC and haematopoietic support at The Royal Marsden between November 1985 and March 1994 were identified. Patient characteristics, previous treatments, disease status at HDC, dose of BCNU, incidence and severity of IPS and survival were all determined and analysed. During the study period, 94 patients received HDC, of whom 26 (28%) had a first episode of IPS within a year of HDC and 23 within 6 months. The median time to presentation after HDC was 93 days (range 12-336 days). The only factors that significantly increased the risk of developing IPS on multivariate analysis were dose of BCNU (P for trend = 0.03) and female sex (P = 0.04). Of these 26 patients, 14 had complete resolution of all symptoms, three had persisting pulmonary symptoms at 6 months and the remaining nine died of IPS at a median of 74 days (19-418 days). All the patients who died from IPS had the first symptoms within 6 months of HDC and all received doses of BCNU > 475 mg m(-2) (P for trend = 0.001). For women receiving > 475 mg m(-2) the risk of death was significantly higher than for men (P = 0.035) but not for those receiving < 475 mg m(-2). Previous lung disease, persisting residual disease before HDC, previous bleomycin or previous mantle radiotherapy did not increase either the incidence of IPS or risk of a fatal outcome. We conclude that the main avoidable risk factor for fatal IPS after HDC is dose of BCNU, and this is especially true for women. If < 475 mg m(-2) is given, even patients with previous mantle radiotherapy and/or previous bleomycin have a very low risk of developing fatal lung toxicity if lung function tests are normal.
接受大剂量化疗(HDC)的霍奇金淋巴瘤(HD)患者发生特发性肺炎综合征(IPS)的风险很高,一旦发生IPS则可能致命。本研究的目的是准确量化这一风险,并确定其发生和病程的预后因素。利用计算机数据库,确定了1985年11月至1994年3月期间在皇家马斯登医院接受含卡莫司汀(BCNU)的HDC及造血支持治疗的所有HD患者。确定并分析了患者特征、既往治疗、HDC时的疾病状态、BCNU剂量、IPS的发生率和严重程度以及生存率。在研究期间,94例患者接受了HDC,其中26例(28%)在HDC后1年内首次发生IPS,23例在6个月内发生。HDC后出现症状的中位时间为93天(范围12 - 336天)。多因素分析中,显著增加发生IPS风险的唯一因素是BCNU剂量(趋势P值 = 0.03)和女性性别(P = 0.04)。在这26例患者中,14例所有症状完全缓解,3例在6个月时仍有肺部症状,其余9例死于IPS,中位死亡时间为74天(19 - 418天)。所有死于IPS的患者在HDC后6个月内出现首发症状,且均接受了剂量> 475 mg/m²的BCNU(趋势P值 = 0.001)。接受> 475 mg/m²的女性患者死亡风险显著高于男性(P = 0.035),但接受< 475 mg/m²的患者则不然。既往肺部疾病、HDC前持续存在的残留疾病、既往使用博来霉素或既往进行斗篷野放疗均未增加IPS的发生率或致命结局的风险。我们得出结论,HDC后致命性IPS的主要可避免风险因素是BCNU剂量,对女性尤其如此。如果给予< 475 mg/m²,即使是既往接受过斗篷野放疗和/或既往使用过博来霉素的患者,若肺功能测试正常,发生致命性肺毒性的风险也非常低。
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