Hematology Division, Tokyo Metropolitan Cancer and Infectious Diseases Center, Komagome Hospital, Tokyo, Japan.
Department of Hematology, Kanazawa University, Kanazawa, Japan.
Front Immunol. 2024 Jan 15;14:1329403. doi: 10.3389/fimmu.2023.1329403. eCollection 2023.
Paroxysmal nocturnal hemoglobinuria (PNH) is a rare hematological disease characterized by intravascular hemolysis, thrombosis, and bone marrow (BM) failure. Although PNH is caused by excessive proliferation of hematopoietic stem cell (HSC) clones with loss of function mutations in phosphatidylinositol N-acetylglucosaminyltransferase subunit A () genes, what drives PNH clones to expand remains elusive.
We present a case of a 26-year-old female who presented with hemolytic anemia, thrombocytopenia, and leukopenia. Flow cytometry analysis of peripheral blood showed that 71.9% and 15.3% of the granulocytes and erythrocytes were glycosylphosphatidylinositol-anchored protein deficient (GPI[-]) cells. The patient was diagnosed with PNH with non-severe aplastic anemia. Deep-targeted sequencing covering 390 different genes of sorted GPI(-) granulocytes revealed three different mutations (p.I69fs, variant allele frequency (VAF) 24.2%; p.T192P, VAF 5.8%; p.V300fs, VAF 5.1%) and no other mutations. She received six cycles of eculizumab and oral cyclosporine. Although the patient's serum lactate dehydrogenase level decreased, she remained dependent on red blood cell transfusion. Six months after diagnosis, she received a syngeneic bone marrow transplant (BMT) from a genetically identical healthy twin, following an immune ablative conditioning regimen consisting of cyclophosphamide 200 mg/kg and rabbit anti-thymocyte globulin 10 mg/kg. After four years, the patient's blood count remained normal without any signs of hemolysis. However, the peripheral blood still contained 0.2% GPI (-) granulocytes, and the three mutations that had been detected before BMT persisted at similar proportions to those before transplantation (p.I69fs, VAF 36.1%; p.T192P, VAF 3.7%; p.V300fs, VAF 8.6%) in the small PNH clones that persisted after transplantation.
The PNH clones that had increased excessively before BMT decreased, but persisted at low percentages for more than four years after the immunoablative conditioning regimen followed by syngeneic BMT. These findings indicate that as opposed to conventional theory, immune pressure on HSCs, which caused BM failure before BMT, was sufficient for -mutated HSCs to clonally expand to develop PNH.
阵发性睡眠性血红蛋白尿症(PNH)是一种罕见的血液系统疾病,其特征为血管内溶血、血栓形成和骨髓(BM)衰竭。尽管 PNH 是由造血干细胞(HSC)克隆过度增殖引起的,这些克隆存在磷脂酰肌醇 N-乙酰葡糖胺转移酶亚单位 A()基因功能丧失突变,但导致 PNH 克隆扩增的原因仍不清楚。
我们报告了一例 26 岁女性,因溶血性贫血、血小板减少和白细胞减少就诊。外周血流式细胞术分析显示,71.9%和 15.3%的粒细胞和红细胞缺乏糖基磷脂酰肌醇锚定蛋白(GPI[-])。患者被诊断为非重型再生障碍性贫血伴 PNH。对分选的 GPI(-)粒细胞进行深度靶向测序,共发现三种不同的 突变(p.I69fs,杂合变异等位基因频率(VAF)24.2%;p.T192P,VAF 5.8%;p.V300fs,VAF 5.1%),未发现其他突变。患者接受了 6 个周期的依库珠单抗和口服环孢素治疗。尽管患者的血清乳酸脱氢酶水平下降,但仍依赖红细胞输血。诊断后 6 个月,患者接受了来自遗传上完全相同的健康双胞胎的同基因骨髓移植(BMT),移植前给予环磷酰胺 200mg/kg 和兔抗胸腺细胞球蛋白 10mg/kg 的免疫清除预处理方案。四年后,患者的血细胞计数仍保持正常,无溶血迹象。然而,外周血中仍有 0.2%的 GPI(-)粒细胞,且在移植前已检测到的三种 突变在移植后持续存在,比例与移植前相似(p.I69fs,VAF 36.1%;p.T192P,VAF 3.7%;p.V300fs,VAF 8.6%),在移植后持续存在的小 PNH 克隆中。
BMT 前过度增加的 PNH 克隆减少,但在免疫清除预处理方案联合同基因 BMT 后,仍以低比例持续存在超过 4 年。这些发现表明,与传统理论相反,导致 BMT 前 BM 衰竭的 HSC 免疫压力足以使 -突变的 HSC 克隆性扩增,从而发展为 PNH。
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