Reichenspurner H, Girgis R E, Robbins R C, Yun K L, Nitschke M, Berry G J, Morris R E, Theodore J, Reitz B A
Department of Cardiothoracic Surgery, Stanford University School of Medicine, California 94305-5247, USA.
Ann Thorac Surg. 1996 Nov;62(5):1467-72; discussion 1472-3. doi: 10.1016/0003-4975(96)00776-X.
Obliterative bronchiolitis (OB) is the main chronic complication after heart-lung (HLTx) and lung transplantation (LTx), limiting the long-term success of both transplant procedures.
Since 1981, 135 HLTxs and 61 isolated LTxs were performed in 184 patients at Stanford University.
The overall prevalence of OB in patients surviving longer than 3 months postoperatively was 64% after HLTx and 68% after LTx. The actuarial freedom from OB was 72%, 51%, 44%, and 29% at 1, 2, 3, and 5 years, respectively, after HLTx and LTx. An analysis of potential risk factors revealed that the frequency and severity of acute rejection episodes (p < 0.001) and the appearance of lymphocytic bronchiolitis on biopsy (p < 0.05) were significantly associated with the development of OB. With regard to diagnosis of OB, pulmonary function tests show early reductions of the forced expiratory flow between 25% and 75% of the forced vital capacity with subsequent decreases in the forced expiratory volume in 1 second. The sensitivity of transbronchial biopsies has increased to 71% since 1993. Current treatment consists of augmented immunosuppression. Concurrent acute rejection episodes or active OB on biopsy have been treated aggressively with high-dose steroid pulses. Analysis of data from 73 patients with OB after HLTx and LTx revealed actuarial 1-, 3-, 5-, and 10-year survival of 89%, 71%, 44%, and 17% versus 86%, 77%, 63% and 56% in patients without OB (p < 0.05 by log-rank analysis). The main complication and cause of death in patients with OB was superimposed respiratory tract infection, which was treated aggressively.
Early diagnosis of OB using pulmonary function tests or transbronchial biopsy is possible and important, because immediate treatment initiation has led to acceptable survival rates, with nearly 50% of affected patients still alive 5 years after transplantation. Current experimental research on OB suggests that immune injury is the main pathogenetic event of airway obliteration in animal models; rapamycin and leflunomide are new immunosuppressive agents that may have the potential to prevent and treat airway obliteration.
闭塞性细支气管炎(OB)是心肺移植(HLTx)和肺移植(LTx)后的主要慢性并发症,限制了这两种移植手术的长期成功率。
自1981年以来,斯坦福大学对184例患者进行了135例心肺移植和61例单纯肺移植。
术后存活超过3个月的患者中,心肺移植后OB的总体患病率为64%,肺移植后为68%。心肺移植和肺移植后1、2、3和5年无OB的精算生存率分别为72%、51%、44%和29%。对潜在危险因素的分析显示,急性排斥反应发作的频率和严重程度(p<0.001)以及活检时淋巴细胞性细支气管炎的出现(p<0.05)与OB的发生显著相关。关于OB的诊断,肺功能测试显示用力呼气流量在用力肺活量的25%至75%之间早期降低,随后1秒用力呼气量下降。自1993年以来,经支气管活检的敏感性已提高到71%。目前的治疗包括加强免疫抑制。对活检时并发的急性排斥反应发作或活动性OB已采用大剂量类固醇冲击进行积极治疗。对73例心肺移植和肺移植后发生OB的患者的数据分析显示,有OB患者的精算1年、3年、5年和10年生存率分别为89%、71%、44%和17%,而无OB患者为86%、77%、63%和56%(对数秩分析p<0.05)。OB患者的主要并发症和死亡原因是叠加的呼吸道感染,对此进行了积极治疗。
使用肺功能测试或经支气管活检对OB进行早期诊断是可能且重要的,因为立即开始治疗已带来了可接受的生存率,近50%的受影响患者在移植后5年仍存活。目前关于OB的实验研究表明,免疫损伤是动物模型中气道闭塞的主要致病事件;雷帕霉素和来氟米特是可能具有预防和治疗气道闭塞潜力的新型免疫抑制剂。
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