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CD20 表达可预测实体器官移植后儿童移植后淋巴增殖性疾病(PTLD)的生存情况。

CD20 expression predicts survival in paediatric post-transplant lymphoproliferative disease (PTLD) following solid organ transplantation.

机构信息

Departments of Pediatrics, Columbia University, New York-Presbyterian Morgan Stanley Children's Hospital New York, NY, USA.

出版信息

Br J Haematol. 2011 Mar;152(6):733-42. doi: 10.1111/j.1365-2141.2010.08448.x. Epub 2011 Jan 30.

Abstract

The prognostic role of CD20 expression and Epstein-Barr virus (EBV) positivity in post-transplant lymphoproliferative disease (PTLD) after solid organ transplantation (SOT) in paediatric patients is poorly understood. We retrospectively examined the relationship of CD20 and EBV with the time interval from SOT to PTLD diagnosis, and PTLD-related event-free (EFS) and overall survival (OS) in 45 consecutive PTLD patients (≤25 years) following SOT. These 45 paediatric SOT patients (28 heart, 11 liver, six kidney) were diagnosed with PTLD 45 months (mean; SD 43; range 4-153; median 24·5) after SOT, with PTLD diagnosis at 118 months (mean) (SD 77; range 14-287) of age. Of 40 evaluable tumours (11 monomorphic, 19 polymorphic, five early lesions, five rare subtypes), 32 (80%) had detectable EBV and 28 (70%) were classified as CD20(+) . Patients whose PTLD expressed CD20 or EBV had shorter intervals between SOT and PTLD onset (28 vs. 64 or 77 months for CD20 and EBV respectively) (P < 0·02), even after adjusting for age at SOT. Patients with CD20(+) tumours had higher 5-year PTLD-related EFS (83·7% vs. 28·6%, P < 0·001) and OS (95·8% vs. 56·3%, P = 0·01). EBV expression was unrelated to PTLD-related EFS or OS. CD20 expression is associated with timing of development of PTLD and predicts survival in PTLD diagnosed following paediatric SOT.

摘要

在儿童实体器官移植(SOT)后,CD20 表达和 EBV 阳性在移植后淋巴增殖性疾病(PTLD)中的预后作用知之甚少。我们回顾性研究了 CD20 和 EBV 与从 SOT 到 PTLD 诊断的时间间隔以及 45 例连续 PTLD 患者(≤25 岁)的 PTLD 相关无事件(EFS)和总生存(OS)之间的关系。这些 45 例儿科 SOT 患者(28 例心脏,11 例肝脏,6 例肾脏)在 SOT 后 45 个月(平均;SD 43;范围 4-153;中位数 24.5)被诊断为 PTLD,PTLD 诊断在 118 个月(平均)(SD 77;范围 14-287)时的年龄。在 40 例可评估肿瘤中(11 例单形性,19 例多形性,5 例早期病变,5 例罕见亚型),32 例(80%)可检测到 EBV,28 例(70%)被分类为 CD20(+)。PTLD 表达 CD20 或 EBV 的患者,SOT 与 PTLD 发病之间的间隔时间更短(分别为 28 个月与 CD20 和 EBV 分别为 64 或 77 个月)(P < 0.02),即使在调整了 SOT 时的年龄后也是如此。CD20(+)肿瘤患者的 5 年 PTLD 相关 EFS(83.7%比 28.6%,P < 0.001)和 OS(95.8%比 56.3%,P = 0.01)更高。EBV 表达与 PTLD 相关 EFS 或 OS 无关。CD20 表达与 PTLD 的发病时间有关,并预测儿科 SOT 后诊断的 PTLD 的生存。

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