Impact of single versus multiple spliceosome mutations on myelodysplastic syndrome.

Pakasticali Nagehan, Mirza Sabbir, Jinming Song, Hussaini Mohammad
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Abstract

Myelodysplastic syndromes (MDS) are myeloid neoplasms that are driven by genetic mutations. Generally, it is thought that a higher number of mutations is associated with worse prognosis. However, the impact of genetic mutations when they occur in the same functional class has not been well studied. Here we investigated the impact of multiple spliceosome mutations on prognosis in MDS patients, hypothesizing that multiple mutations in the same class are biologically redundant and would not affect prognosis. Departmental Next Generation Sequencing (NGS) database (>6000 cases) was queried and the data was analyzed to identify cases with spliceosome mutations (SF3B1, SRSF2, U2AF1, ZRSR2, U2AF1). Overall, 71 patients met criteria for the study. Cases with single spliceosome mutations (i.e., no other co-mutations whatsoever) were as follows: SF3B1 (38), SRSF2 (5), U2AF2 (11), and ZRSR2 (1). Cases with concurrent spliceosome mutations were as follows: SF3B1 + SRSF2 (5), SF3B1 + U2AF1 (1), SF3B1 + ZRSR2 (3), SRSF2 + U2AF1 (2), SRSF2 + ZRSR2 (1), U2AF1 + ZRSR2 (4). Four of 55 (7.3%) of patients in the single mutation group vs. 4 of 16 (25%) of patients in the concurrent mutation group progressed to acute myeloid leukemia (AML). Mean OS in the single mutation group was 103.5 months vs. 71.6 months in the multiple concurrent mutation group (χ2= 2.404; p= 0.12). Our results challenge the current dogma that increased mutation in MDS portend worse survival. We demonstrate that multiple mutations bear no impact on clinical prognosis when the additional mutations occur in same spliceosome class.

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单剪接体与多剪接体突变对骨髓增生异常综合征的影响。
骨髓增生异常综合征(MDS)是由基因突变引起的骨髓肿瘤。一般认为,突变数量越高,预后越差。然而,当基因突变发生在同一功能类别中时,其影响尚未得到很好的研究。在这里,我们研究了多个剪接体突变对MDS患者预后的影响,假设同一类中的多个突变在生物学上是多余的,不会影响预后。对部门下一代测序(NGS)数据库(>6000例)进行查询,并对数据进行分析,以确定剪接体突变的病例(SF3B1、SRSF2、U2AF1、ZRSR2和U2AF1)。总体而言,71名患者符合研究标准。单剪接体突变(即没有任何其他共突变)的病例如下:SF3B1(38)、SRSF2(5)、U2AF2(11)和ZRSR2(1)。同时发生剪接体突变的病例如下:SF3B1+SRSF2(5),SF3B1+U2AF1(1),SF3 B1+ZRSR2(3),SRSF2+U2AF1,SRSF2+ZRSR2,U2AF1+ZRSR2。单突变组55名患者中有4名(7.3%)进展为急性粒细胞白血病,而同时突变组16名患者中只有4名(25%)进展为AML。单突变组的平均OS为103.5个月,而多同时突变组为71.6个月(χ2=2.404;p=0.12)。我们的结果挑战了MDS突变增加预示生存率下降的现行教条。我们证明,当额外的突变发生在同一类剪接体中时,多个突变对临床预后没有影响。
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来源期刊
CiteScore
2.00
自引率
6.70%
发文量
25
审稿时长
11 weeks
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