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巴西单中心 167 例阵发性睡眠性血红蛋白尿患者的基线特征、疾病负担和长期随访分析。

Analysis of baseline characteristics, disease burden and long-term follow-up of 167 patients with Paroxysmal Nocturnal Hemoglobinuria at a single center in Brazil.

机构信息

Hospital de Clínicas, Federal University of Paraná, UFPR, Brazil.

Hospital de Clínicas, Federal University of Paraná, UFPR, Brazil.

出版信息

Blood Cells Mol Dis. 2021 Dec;92:102605. doi: 10.1016/j.bcmd.2021.102605. Epub 2021 Sep 15.

DOI:10.1016/j.bcmd.2021.102605
PMID:34537447
Abstract

UNLABELLED

Paroxysmal nocturnal hemoglobinuria (PNH) can occur as a hemolytic form or small PNH clone found in a patient with bone marrow failure.

METHODS

Describe Brazilian retrospective PNH cohort and identify the impact of disease burden on long-term follow-up.

RESULTS

167 patients, mean age at diagnosis 28.4 (7.1-71.2 years), four years mean interval between onset of cytopenia/aplasia diagnosis and PNH clone detection. Patients were divided into 15 Classic PNH, 55 Hemolytic PNH with bone marrow hypoplasia (PNH/AA), and 97 Subclinical PNH (sc-PNH). Hypocellular bone marrow was found in 89.2%; 55 had hemoglobinuria and 22 thrombosis during monitoring. WBC PNH clone correlated with RBC PNH clone, LDH and cytopenia. Subclinical patients had lower median lower RBC clone (2.0% vs 24.0% vs 57.8%) and WBC clone (11.7% vs 58.8% vs 81.2%) than PNH/AA and Classic PNH, respectively. PNH granulocyte clone was 89.1% in thrombotic patients. Ten-year overall survival 80.4% and mortality in transplanted patients 9.6%. Sepsis was mortality cause in subclinical PNH (16/18, 88.8%), and thrombosis in hemolytic PNH (11/13, 84.6%).

CONCLUSION

Large PNH clones and LDH burden were associated with increased hemolysis and thrombosis risks, while young patients were associated with small PNH clones and subclinical form of the disease. Knowledge of the patient profile, the low risk associated with HSCT, and the use of long-term IST may be instrumental in the clinical management of PNH in restricted-resources countries.

摘要

未注明

阵发性夜间血红蛋白尿(PNH)可表现为溶血性形式或骨髓衰竭患者中发现的小 PNH 克隆。

方法

描述巴西回顾性 PNH 队列,并确定疾病负担对长期随访的影响。

结果

167 例患者,诊断时的平均年龄为 28.4(7.1-71.2 岁),发病至骨髓衰竭/再生障碍性贫血诊断和 PNH 克隆检测之间的平均间隔为 4 年。患者分为 15 例经典 PNH、55 例溶血性 PNH 伴骨髓增生不良(PNH/AA)和 97 例亚临床 PNH(sc-PNH)。89.2%的患者骨髓细胞减少;55 例有血红蛋白尿,22 例在监测期间发生血栓形成。白细胞 PNH 克隆与红细胞 PNH 克隆、LDH 和细胞减少相关。亚临床患者的中位 RBC PNH 克隆(2.0%比 24.0%比 57.8%)和 WBC PNH 克隆(11.7%比 58.8%比 81.2%)均低于 PNH/AA 和经典 PNH。血栓形成患者的 PNH 粒细胞克隆为 89.1%。10 年总生存率为 80.4%,移植患者死亡率为 9.6%。亚临床 PNH 的死亡原因是感染(16/18,88.8%),溶血性 PNH 是血栓形成(11/13,84.6%)。

结论

大 PNH 克隆和 LDH 负担与溶血和血栓形成风险增加相关,而年轻患者与小 PNH 克隆和疾病的亚临床形式相关。了解患者特征、HSCT 相关的低风险以及长期 IST 的使用可能对资源有限国家的 PNH 临床管理具有重要意义。

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