[Clinical Characteristics and Prognosis of Myelodysplastic Syndromes Patients with RUNX1 Gene Mutation].

Yi Chen, Yue-Ru Ji, Jing-Yi Zhang, Wei-Wei Qin, Cang-Chun Liu, Li Liu, Xue-Qian Yan
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Abstract

Objective: To investigate the clinical characteristics and survival analysis of myelodysplastic syndromes (MDS) with RUNX1 gene mutation.

Methods: Clinical data of 177 newly diagnosed MDS patients admitted to the Department of Hematology, the Second Affiliated Hospital of Air Force Military Medical University from October 1, 2015 to October 31, 2022 were retrospectively analyzed. Gene mutation detection was performed by second-generation sequencing technology, and clinical characteristics and prognosis of patients with RUNX1 gene mutation were analyzed.

Results: A total of 30 cases (16.95%) of RUNX1 gene mutations were detected, including 15 missense mutations (50.0%), 9 frameshift deletion mutations (30.0%), 4 splice site mutations (13.3%), 1 insertion mutation (3.3%), and 1 nonsense mutation (3.3%). Patients with RUNX1 mutations had a median age of 68.5 years at diagnosis (range: 62.25-78.50 years old). There were no significantly differences between RUNX1 mutations and wild type patients in age distribution, gender, peripheral blood white blood cell count, hemoglobin level, bone marrow and peripheral blood blasts ratio, IPSS-R cytogenetics, IPSS-R stage, etc. (P >0.05). However, there were statistically significant differences in platelet count and whether complicated karyotype. Compared with patients without RUNX1 gene mutation, patients with RUNX1 gene mutation had lower platelet count (P =0.018), and were less likely to have complicatedkaryotype at initial diagnosis (P =0.01). Cox proportional hazards model analysis showed that when other covariates remained unchanged, the higher the platelet count, the better the survival of patients (HR=0.995, 95%CI : 0.990-0.999, P =0.036); In the IPSS-M prognostic stratification, keeping other covariates unchanged, the risk of progression or death of myelodysplastic syndrome was significantly lower in the medium to high-risk and low-risk groups compared with the high-risk group (HR=0.149, 95%CI : 0.031-0.721, P =0.018; HR=0.026, 95%CI : 0.003-0.234, P =0.001). Survival analysis showed that MDS patients with RUNX1 gene mutation had worse overall survival time (P < 0.001). Patients with RUNX1 mutation had worse OS than non-mutation patients in the early WHO group. RUNX1 mutation and IPSS-M risk stratification mean OS and mean LFS were worse in low-risk patients than in non-mutated patients.

Conclusion: RUNX1 gene mutation is an adverse prognostic factor in MDS patients, especially in the IPSS-M prognosis stratification group of low-risk, medium-low risk, medium-high risk and WHO classification of early patients.

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[RUNX1基因突变的骨髓增生异常综合征患者的临床特征和预后】。]
目的研究骨髓增生异常综合征(MDS)RUNX1基因突变的临床特征和生存分析:回顾性分析空军军医大学第二附属医院血液科2015年10月1日至2022年10月31日收治的177例新诊断MDS患者的临床资料。采用二代测序技术检测基因突变,分析RUNX1基因突变患者的临床特征和预后:结果:共检测出30例(16.95%)RUNX1基因突变,包括15例错义突变(50.0%)、9例框移缺失突变(30.0%)、4例剪接位点突变(13.3%)、1例插入突变(3.3%)和1例无义突变(3.3%)。RUNX1突变患者确诊时的中位年龄为68.5岁(范围:62.25-78.50岁)。RUNX1突变型与野生型患者在年龄分布、性别、外周血白细胞计数、血红蛋白水平、骨髓与外周血胚泡比例、IPSS-R细胞遗传学、IPSS-R分期等方面无明显差异(P>0.05)。但在血小板计数和是否复杂核型方面,差异有统计学意义。与无RUNX1基因突变的患者相比,RUNX1基因突变患者的血小板计数较低(P =0.018),且初诊时复杂核型的可能性较小(P =0.01)。Cox比例危险模型分析显示,当其他协变量不变时,血小板计数越高,患者的生存率越高(HR=0.995,95%CI:0.990-0.999,P=0.036);在IPSS-M预后分层中,保持其他协变量不变,与高危组相比,中高危组和低危组骨髓增生异常综合征进展或死亡风险显著降低(HR=0.149,95%CI : 0.031-0.721,P =0.018;HR=0.026,95%CI : 0.003-0.234,P =0.001)。生存期分析显示,RUNX1基因突变的MDS患者总生存期较短(P < 0.001)。在WHO早期组中,RUNX1基因突变患者的OS比非突变患者更差。RUNX1基因突变和IPSS-M风险分层的低危患者的平均OS和平均LFS均比非突变患者差:结论:RUNX1基因突变是MDS患者的不良预后因素,尤其是在IPSS-M预后分层的低危、中低危、中高危组和WHO分类的早期患者中。
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来源期刊
中国实验血液学杂志
中国实验血液学杂志 Medicine-Medicine (all)
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