摘要目的:探讨异基因造血干细胞移植（allo-HSCT）后发生T大颗粒淋巴细胞增多（T-LGL）患者的临床特征、相关因素以及对预后的影响。方法:回顾性分析2013年6月至2020年2月接受allo-HSCT的359例患者连续性资料，男216例，女143例，中位年龄为38（7~65）岁。分析T-LGL的临床特征、累积发生率，比较发生与未发生T-LGL患者的总生存（OS）率、无病生存（DFS）率、累积复发率（CIR）及非复发死亡率（NRM）的差异，并研究影响移植后发生T-LGL的相关因素。结果:共入组359例患者，T-LGL组17例，非LGL组342例，中位随访38（3~92）个月，移植后1、2、3年T-LGL累积发生率分别为3.64%（95% CI 1.09%~6.19%）、4.50%（95% CI 1.36%~7.64%）和4.84%（95% CI 1.10%~8.76%）；移植受者CMV再激活（ P=0.013）、EBV血症（ P=0.034）以及急性移植物抗宿主病（ P=0.027）均与T-LGL发生有关，且多因素分析显示，良性血液病[ P=0.027， OR=3.36（95% CI 1.15~9.89）]、单倍型移植[ P=0.030， OR=4.67（95% CI 1.16~18.75）]、无关供者移植[ P=0.041， OR=5.49（95% CI 1.10~28.16）]为移植后发生T-LGL的独立预测因素。两组患者移植后3年OS、DFS率、CIR以及NRM差异均有统计学意义[OS：100.0%对78.6%（95% CI 74.1%~83.1%）， P=0.04；DFS：100.0%对70.0%（95% CI 64.9%~75.1%）， P=0.01；CIR：0对16.1%（95% CI 11.8%~22.4%）， P<0.01；NRM：0对12.6%（95% CI 12.5%~12.6%）， P=0.02]。亚组分析结果显示，恶性疾病患者移植后发生T-LGL者预后良好，NRM、DFS率以及CIR差异均有统计学意义（ P值均<0.05），而良性疾病患者移植后发生T-LGL对预后无明显影响。 结论:恶性疾病患者移植后T-LGL可能是一个较为持久的良性临床过程，与免疫重建和T细胞调节机制相关的因素可作为移植后T-LGL发生的主要预测因素。

abstractsObjective:To explore the clinical characteristics, related factors, and prognostic effect of patients with T cell large granular lymphocytosis following allo-HSCT.Methods:Consecutive patients with T-LGL following allo-HSCT who visited our center from June 2013 to February 2020 were studied retrospectively. We compared patients undergoing allo-HSCT during this period. The clinical characteristics, related factors, cumulative incidence of patients with T-LGL and rates of overall survival (OS) , disease free survival (DFS) , relapse, and non-relapse mortality (NRM) were analyzed.Results:Total 359 patients were enrolled, including 17 with T-LGL and 342 without T-LGL following allo-HSCT. The median follow-up duration was 38 (3-92) month. The cumulative incidence at 1-, 2- and 3-years of T-LGL was 3.64% (95% CI 1.09%-6.19%) , 4.50% (95% CI 1.36%-7.64%) , and 4.84% (95% CI 1.10%-8.76%) , respectively. CMV reactivation ( P=0.013) , EB viremia ( P=0.034) , and aGVHD ( P=0.027) were associated with the development of T-LGL following allo-HSCT. Multivariate analysis showed that benign hematologic diseases[ P=0.027, OR=3.36 (95% CI 1.15-9.89) ] and haploidentical hematopoietic stem cell transplantation[ P=0.030, OR=4.67 (95% CI 1.16-18.75) ], unrelated donor transplantation[ P=0.041, OR=5.49 (95% CI 1.10-28.16) ] were independent predictive factors of T-LGL following allo-HSCT. There was a significant difference in the 3-year OS (100.0% vs. 78.6%, P=0.04) , DFS (100.0% vs. 70.0%, P=0.01) , and NRM (0 vs. 12.6%, P=0.02) between the 2 cohorts. Subgroup analysis showed that malignant diseases recipients who developed T-LGL had better outcomes after allo-HSCT, and there was a significant difference in the NRM ( P=0.042) , DFS ( P=0.013) , and cumulative relapse rate ( P=0.028) between the 2 cohorts. In contrast, the appearance of T-LGL after allo-HSCT in patients with benign diseases had no significant effect on the prognosis. Conclusions:T-LGL was a durable and clinically benign phenomenon occurring in allo-HSCT recipients with malignant diseases. Factors associated with immune reconstitution and T-cell regulatory mechanisms might be major predictors of T-LGL following allo-HSCT.