Department of Bone Marrow Transplantation, Hebei Yanda Lu Daopei Hospital, Langfang, China.
Department of Hematology and Immunology, Hebei Yanda Lu Daopei Hospital, Langfang, China.
Front Immunol. 2023 Jan 4;13:1066748. doi: 10.3389/fimmu.2022.1066748. eCollection 2022.
We aimed to evaluate prognostic factors of a second allogeneic stem cell transplantation (allo-HSCT2) among hematological malignancy patients who have relapsed after the first allo-HSCT(allo-HSCT1).
We retrospectively analyzed 199 hematological malignancy patients who received allo-HSCT2 as a salvage treatment post allo-HSCT1 relapse between November 2012 and October 2021.
The median age at allo-HSCT2 was 23 (range: 3-60) years. The median time to relapse after HSCT1 was 9 (range: 1-72) months. Prior to allo-HSCT2, patients had the following hematopoietic cell transplantation-comorbidity indexes (HCT-CI): 127 with a score of 0, 52 with a score of 1, and 20 with a score of 2 or greater. Fifty percent of patients received chimeric antigen receptor (CAR) T-cell therapy following HSCT1 relapse. Disease status was minimal residual disease (MRD)-negative complete remission (CR) among 119 patients, MRD-positive CR among 37 patients and non-remission (NR) for 43 patients prior to allo-HSCT2. Allo-HSCT2 was performed from a new donor in 194 patients (97.4%) and 134 patients (67.3%) received a graft with a new mismatched haplotype. The median follow-up time was 24 months (range: 6-98 months), and the 2-year OS and LFS were 43.8% ± 4.0% and 42.1% ± 4.1%, respectively. The 2-year cumulative incidence of relapse (CIR) and non-relapse mortality (NRM) was 30.0%±4.8% and 38.5%±3.8%, respectively. Cox regression multivariate analysis showed that disease statusof MRD-negative CR, HCT-CI score of 0 prior to allo-HSCT2, and new mismatched haplotype donor were predictive factors of improved OS and LFS compared to patients without these characteristics. Based on these three favorable factors, we developed a predictive scoring system for patients who received allo-HSCT2. Patients with a prognostic score of 3 who had the three factors showed a superior 2-year OS of 63.3% ± 6.7% and LFS of 63.3% ± 6.7% and a lower CIR of 5.5% ± 3.1% than patients with a prognostic score of 0. Allo-HSCT2 is feasible and patients with good prognostic features prior to allo-HSCT2 -disease status of CR/MRD- and HCT-CI score of 0 as well as a second donor with a new mismatched haplotype could have the maximal benefit from the second allo-HSCT.
Allo-HSCT2 is feasible and patients with good prognostic features prior to allo-HSCT2 -disease status of CR/MRD- and HCT-CI score of 0 as well as a second donor with a new mismatched haplotype could have the maximal benefit from the second allo-HSCT.
我们旨在评估血液恶性肿瘤患者在首次异基因造血干细胞移植(allo-HSCT1)后复发后接受第二次allo-HSCT(allo-HSCT2)的预后因素。
我们回顾性分析了 2012 年 11 月至 2021 年 10 月期间因 allo-HSCT1 后复发而接受 allo-HSCT2 作为挽救治疗的 199 例血液恶性肿瘤患者。
第二次 allo-HSCT 时的中位年龄为 23 岁(范围:3-60 岁)。HSCT1 后复发至 allo-HSCT2 的中位时间为 9 个月(范围:1-72 个月)。在第二次 allo-HSCT 之前,患者的造血细胞移植合并症指数(HCT-CI)为:127 分为 0 分,52 分为 1 分,20 分为 2 分或更高。50%的患者在 HSCT1 后复发后接受嵌合抗原受体(CAR)T 细胞治疗。第二次 allo-HSCT 前,119 例患者为微小残留病(MRD)阴性完全缓解(CR),37 例患者为 MRD 阳性 CR,43 例患者为未缓解(NR)。194 例患者(97.4%)从新供体进行第二次 allo-HSCT,134 例患者(67.3%)接受了新错配单倍型供体的移植物。中位随访时间为 24 个月(范围:6-98 个月),2 年 OS 和 LFS 分别为 43.8%±4.0%和 42.1%±4.1%。2 年累积复发率(CIR)和非复发死亡率(NRM)分别为 30.0%±4.8%和 38.5%±3.8%。Cox 回归多因素分析表明,第二次 allo-HSCT 前疾病状态为 MRD 阴性 CR、HCT-CI 评分为 0 分和新错配单倍型供体是 OS 和 LFS 改善的预测因素,与无这些特征的患者相比。基于这三个有利因素,我们为接受 allo-HSCT2 的患者开发了一个预测评分系统。具有 3 分预测评分且具有所有三个因素的患者 2 年 OS 为 63.3%±6.7%,LFS 为 63.3%±6.7%,CIR 为 5.5%±3.1%,优于预测评分 0 分的患者。第二次 allo-HSCT 前具有良好预后特征的患者(疾病状态为 CR/MRD 和 HCT-CI 评分为 0 以及第二个供体为新错配单倍型)可从第二次 allo-HSCT 中获得最大益处。
allo-HSCT2 是可行的,第二次 allo-HSCT 前具有良好预后特征的患者(疾病状态为 CR/MRD 和 HCT-CI 评分为 0 以及第二个供体为新错配单倍型)可从第二次 allo-HSCT 中获得最大益处。
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