Department of Hematology, Copenhagen University Hospital, Copenhagen, Denmark; Biotech Research and Innovation Center, Faculty of Health and Medical Sciences, University of Copenhagen, Copenhagen, Denmark; The Danish Stem Cell Center (Danstem), University of Copenhagen, Copenhagen, Denmark.
Department of Hematology, Oslo University Hospital, Oslo, Norway.
Transplant Cell Ther. 2021 Dec;27(12):991.e1-991.e9. doi: 10.1016/j.jtct.2021.08.028. Epub 2021 Sep 6.
Chronic myelomonocytic leukemia (CMML) is an aggressive disease in which survival after allogeneic hematopoietic stem cell transplantation (HCT) remains relatively poor. An assessment of prognostic factors is an important part of treatment decision making and has the potential to be greatly improved by the inclusion of molecular genetics. However, there is a significant knowledge gap in the interpretation of mutational patterns. This study aimed to describe outcomes of allogeneic HCT in patients with CMML in relation to clinical and molecular genetic risk factors. This retrospective study included 64 patients with CMML who underwent allogeneic HCT between 2008 and 2018, with a median follow-up of 5.4 years. Next-generation sequencing using targeted myeloid panels was carried out on saved material from 51 patients from the time of transplantation. Kaplan-Meier and Cox regression were used for analysis of overall survival (OS), and cumulative incidence with competing risks and Fine and Gray models were used for analysis of relapse and nonrelapse mortality (NRM). Mutations were detected in 48 patients (94%), indicating high levels of minimal residual disease (MRD) positivity at transplantation, even among those in complete remission (CR) (n = 14), 86% of whom had detectable mutations. The most frequently mutated genes were ASXL1 (37%), TET2 (37%), RUNX1 (33%), SRSF2 (26%), and NRAS (20%). Risk stratification using the CMML-specific Prognostic Scoring System molecular score (CPSS-Mol) resulted in 45% of patients moving to a higher risk-group compared with risk stratification using the CPSS. High leucocyte count (≥13 × 10/L), transfusion requirement, and previous intensive chemotherapy were associated with higher incidence of relapse. Being in CR was not linked to better outcomes. Neither ASXL1 nor RUNX1 mutation was associated with a difference in OS, relapse, or NRM, despite being high risk in the nontransplantation setting. TET2 mutations were associated with a significantly higher 3-year OS (73% versus 40%; P = .039). Achieving MRD-negative CR was rare in this CMML cohort, which may explain why we did not observe better outcomes for those in CR. This merits further investigation. Our analyses suggest that the negative impact of ASXL1 and RUNX1 mutations can be overcome by allogeneic HCT; however, risk stratification is complex in CMML and requires larger cohorts and multivariate models, presenting an ongoing challenge in this rare disease.
慢性粒单核细胞白血病(CMML)是一种侵袭性疾病,异基因造血干细胞移植(HCT)后的生存仍然相对较差。评估预后因素是治疗决策的重要组成部分,通过纳入分子遗传学,有可能得到极大改善。然而,在突变模式的解释方面存在着显著的知识差距。本研究旨在描述与临床和分子遗传学危险因素相关的 CMML 患者接受异基因 HCT 的结果。这项回顾性研究纳入了 64 例 2008 年至 2018 年间接受异基因 HCT 的 CMML 患者,中位随访时间为 5.4 年。对 51 例移植时保存的材料进行了靶向髓系的下一代测序。采用 Kaplan-Meier 和 Cox 回归分析总生存期(OS),采用竞争风险累积发生率和 Fine 和 Gray 模型分析复发和非复发死亡率(NRM)。在 48 例患者(94%)中检测到突变,表明移植时微小残留疾病(MRD)阳性率较高,即使在完全缓解(CR)患者中(n=14),86%的患者也可检测到突变。最常突变的基因是 ASXL1(37%)、TET2(37%)、RUNX1(33%)、SRSF2(26%)和 NRAS(20%)。使用 CMML 特异性预后评分系统分子评分(CPSS-Mol)进行风险分层,与使用 CPSS 进行风险分层相比,45%的患者转移到更高的风险组。白细胞计数较高(≥13×10/L)、输血需求和先前强化化疗与更高的复发率相关。处于 CR 状态与更好的结果无关。尽管在非移植环境中是高危因素,但 ASXL1 或 RUNX1 突变与 OS、复发或 NRM 无差异。TET2 突变与显著较高的 3 年 OS 相关(73%对 40%;P=0.039)。在这个 CMML 队列中,MRD 阴性的 CR 很少见,这可能解释了为什么我们没有观察到 CR 患者的更好结果。这值得进一步研究。我们的分析表明,ASXL1 和 RUNX1 突变的负面影响可以通过异基因 HCT 克服;然而,CMML 的风险分层很复杂,需要更大的队列和多变量模型,这在这种罕见疾病中仍然是一个挑战。
