Current Opinions on the Clinical Utility of Ravulizumab for the Treatment of Paroxysmal Nocturnal Hemoglobinuria.

IF 4.6 Q2 MATERIALS SCIENCE, BIOMATERIALS ACS Applied Bio Materials Pub Date : 2021-12-14 DOI:10.2147/TCRM.S273360
Carmelo Gurnari, Ishani Nautiyal, Simona Pagliuca
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引用次数: 1

Abstract

Paroxysmal nocturnal hemoglobinuria (PNH) is a rare disorder of hematopoietic stem cells genetically defined by the acquisition of somatic mutations in the X-linked phosphatidylinositol glycan anchor biosynthesis, class A (PIGA) gene. PIGA is essential for the synthesis of glycosyl phosphatidylinositol (GPI) anchor proteins and its mutations result in a deficiency of such molecules on the membrane of blood cells derived from the mutant clone. In particular, the lack of the GPI-linked complement regulatory proteins CD55 and CD59 is responsible for the increased sensitivity of PNH erythrocytes to complement-mediated destruction. Indeed, the classical clinical picture of PNH includes signs and symptoms of intravascular hemolysis along with variable degrees of cytopenia and a strong tendency to thrombosis, hallmarks of the disease. Before the introduction of anti-complement inhibitors, PNH was characterized by a high mortality primarily due to thrombotic events. The approval of the terminal anti-complement inhibitor eculizumab in 2007 introduced a paradigm shift in the treatment of the disease with improvement of the chronic hemolytic process and dramatic reduction of the thrombotic rate. However, eculizumab has a relatively short half-life when considering a life-long treatment, with obvious consequences as to the quality of life of treated patients necessitating relatively frequent drug administrations. Moreover, up to 30% of PNH patients undergoing eculizumab therapy show a suboptimal response, continuing to require red cell transfusions because of extravascular hemolysis or breakthrough hemolytic episodes. In 2019, the FDA approved the second-generation C5 inhibitor ravulizumab, a long-lasting agent with a better control of disease manifestations. Herein, we discuss the use of ravulizumab in PNH, its differences with first-generation C5 inhibitors, the research evidence supporting the safety and efficacy of this drug and its impact on costs for health systems and quality of life of PNH patients.

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Ravulizumab治疗阵发性夜间血红蛋白尿的临床应用现状。
发作性夜间血红蛋白尿症(PNH)是一种罕见的造血干细胞疾病,其遗传特征是获得X连锁磷脂酰肌醇聚糖锚生物合成a类(PIGA)基因的体细胞突变。PIGA对糖基磷脂酰肌醇(GPI)锚定蛋白的合成至关重要,其突变导致衍生自突变克隆的血细胞膜上缺乏此类分子。特别地,缺乏GPI连接的补体调节蛋白CD55和CD59是PNH红细胞对补体介导的破坏的敏感性增加的原因。事实上,PNH的经典临床表现包括血管内溶血的体征和症状,以及不同程度的细胞减少和强烈的血栓形成倾向,这是该疾病的特征。在引入抗补体抑制剂之前,PNH的特点是主要由于血栓性事件导致的高死亡率。2007年,终末抗补体抑制剂eculizumab的批准为该疾病的治疗带来了范式转变,改善了慢性溶血过程,并显著降低了血栓形成率。然而,在考虑终身治疗时,埃库珠单抗的半衰期相对较短,对接受治疗的患者的生活质量有明显影响,因此需要相对频繁地给药。此外,在接受埃库珠单抗治疗的PNH患者中,高达30%的患者表现出次优反应,由于血管外溶血或突破性溶血发作,仍需要输注红细胞。2019年,美国食品药品监督管理局批准了第二代C5抑制剂ravulizumab,这是一种对疾病表现有更好控制的长效药物。在此,我们讨论了拉武利珠单抗在PNH中的应用,它与第一代C5抑制剂的差异,支持该药物安全性和有效性的研究证据,以及它对PNH患者的卫生系统成本和生活质量的影响。
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来源期刊
ACS Applied Bio Materials
ACS Applied Bio Materials Chemistry-Chemistry (all)
CiteScore
9.40
自引率
2.10%
发文量
464
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