Clinical Genetics Branch and.
Cancer Genomics Research Laboratory, Division of Cancer Epidemiology and Genetics, National Cancer Institute, Bethesda, MD.
Blood. 2022 Aug 25;140(8):909-921. doi: 10.1182/blood.2022016508.
Patients with severe aplastic anemia (SAA) can have an unrecognized inherited bone marrow failure syndrome (IBMFS) because of phenotypic heterogeneity. We curated germline genetic variants in 104 IBMFS-associated genes from exome sequencing performed on 732 patients who underwent hematopoietic cell transplant (HCT) between 1989 and 2015 for acquired SAA. Patients with pathogenic or likely pathogenic (P/LP) variants fitting known disease zygosity patterns were deemed unrecognized IBMFS. Carriers were defined as patients with a single P/LP variant in an autosomal recessive gene or females with an X-linked recessive P/LP variant. Cox proportional hazard models were used for survival analysis with follow-up until 2017. We identified 113 P/LP single-nucleotide variants or small insertions/deletions and 10 copy number variants across 42 genes in 121 patients. Ninety-one patients had 105 in silico predicted deleterious variants of uncertain significance (dVUS). Forty-eight patients (6.6%) had an unrecognized IBMFS (33% adults), and 73 (10%) were carriers. No survival difference between dVUS and acquired SAA was noted. Compared with acquired SAA (no P/LP variants), patients with unrecognized IBMFS, but not carriers, had worse survival after HCT (IBMFS hazard ratio [HR], 2.13; 95% confidence interval[CI], 1.40-3.24; P = .0004; carriers HR, 0.96; 95% CI, 0.62-1.50; P = .86). Results were similar in analyses restricted to patients receiving reduced-intensity conditioning (n = 448; HR IBMFS = 2.39; P = .01). The excess mortality risk in unrecognized IBMFS attributed to death from organ failure (HR = 4.88; P < .0001). Genetic testing should be part of the diagnostic evaluation for all patients with SAA to tailor therapeutic regimens. Carriers of a pathogenic variant in an IBMFS gene can follow HCT regimens for acquired SAA.
患有严重再生障碍性贫血(SAA)的患者可能患有未被识别的遗传性骨髓衰竭综合征(IBMFS),这是由于表型异质性所致。我们对 1989 年至 2015 年间因获得性 SAA 接受造血细胞移植(HCT)的 732 例患者的外显子组测序中的 104 个 IBMFS 相关基因进行了种系遗传变异分析。患有与已知疾病纯合子模式相符的致病性或可能致病性(P/LP)变异的患者被认为是未被识别的 IBMFS。携带者定义为在常染色体隐性基因中具有单一 P/LP 变异的患者或女性中具有 X 连锁隐性 P/LP 变异的患者。采用 Cox 比例风险模型进行生存分析,随访至 2017 年。我们在 121 例患者的 42 个基因中发现了 113 个 P/LP 单核苷酸变异或小插入/缺失和 10 个拷贝数变异,91 例患者有 105 个经计算机预测为意义未明的有害变异(dVUS)。48 例患者(6.6%)患有未被识别的 IBMFS(33%为成年人),73 例为携带者。未发现 dVUS 与获得性 SAA 之间的生存差异。与获得性 SAA(无 P/LP 变异)相比,HCT 后未被识别的 IBMFS 患者(而非携带者)的生存状况更差(IBMFS 危险比[HR],2.13;95%置信区间[CI],1.40-3.24;P =.0004;携带者 HR,0.96;95% CI,0.62-1.50;P =.86)。在对接受强度降低的调理治疗的患者(n = 448;HR IBMFS = 2.39;P =.01)进行的分析中,结果相似。未被识别的 IBMFS 中器官衰竭导致的死亡导致的死亡风险增加(HR = 4.88;P <.0001)。所有 SAA 患者的诊断评估都应包括基因检测,以调整治疗方案。IBMFS 基因致病性变异的携带者可以遵循获得性 SAA 的 HCT 方案。
