Advances in the management of erythropoietic protoporphyria - role of afamelanotide.

IF 2.6 Q2 GENETICS & HEREDITY Application of Clinical Genetics Pub Date : 2016-12-12 eCollection Date: 2016-01-01 DOI:10.2147/TACG.S122030
Ashley M Lane, Jerome T McKay, Herbert L Bonkovsky
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引用次数: 19

Abstract

Erythropoietic protoporphyria (EPP) and the phenotypically similar disease X-linked protoporphyria (XLPP) are inherited cutaneous porphyrias characterized clinically by acute non-blistering photosensitivity, intolerance to sunlight, and significantly reduced quality of life. They are due to marked overproduction of protoporphyrin (PP) chiefly by erythroblasts and reticulocytes. In EPP, the underlying genetic defect is in the ferrochelatase gene, which encodes the final enzyme in the heme synthetic pathway. In XLPP, the genetic defect is a gain-of-function mutation, usually a four-base deletion, in the gene that encodes the enzyme 5-aminolevulinic acid synthase-2, the first and rate-controlling enzyme of heme synthesis in developing red blood cells. The excess PP causes acute and painful photosensitivity, being activated by light in the long ultraviolet to blue spectrum (380-420 nm, the Soret band). Although several treatments have been proposed, presently no very effective treatment exists for EPP or XLPP. Afamelanotide (Scenesse®) is a first-in-class synthetic analog of α-melanocyte stimulating hormone. Afamelanotide mimics the naturally occurring hormone to increase skin pigmentation by increasing melanin production in melanocytes, resulting in increased sunlight tolerance in those with EPP/XLPP. Afamelanotide is currently approved for use in the European Union and Switzerland, and it is under review in the United States by the Food and Drug Administration for use in patients with EPP/XLPP. This paper provides a review of the clinical characteristics and current therapies for EPP/XLPP. We discuss the pharmacology, clinical efficacy, safety, and tolerability of afamelanotide and summarize the results of several key Phase II and III clinical trials. These data indicate that afamelanotide is a promising therapy for those with these debilitating diseases.

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红细胞原卟啉症的治疗进展——阿麦兰肽的作用。
红细胞生成性原生卟啉症(EPP)和表型相似的疾病x连锁原生卟啉症(XLPP)是遗传性皮肤卟啉症,临床特征为急性非起泡性光敏性,对阳光不耐受,生活质量显著降低。它们主要是由于红细胞和网织红细胞大量产生原卟啉(PP)。在EPP中,潜在的遗传缺陷是铁螯合酶基因,该基因编码血红素合成途径中的最后一种酶。在XLPP中,遗传缺陷是一种功能获得突变,通常是4个碱基的缺失,在编码5-氨基乙酰丙酸合成酶-2的基因中,5-氨基乙酰丙酸合成酶-2是发育中的红细胞中血红素合成的第一个和速率控制酶。过量的PP会引起急性和痛苦的光敏,被长紫外到蓝色光谱(380-420 nm, Soret波段)的光激活。虽然提出了几种治疗方法,但目前尚无非常有效的治疗方法。Afamelanotide (Scenesse®)是一流的α-促黑素细胞激素的合成类似物。Afamelanotide模拟自然产生的激素,通过增加黑色素细胞中黑色素的产生来增加皮肤色素沉着,从而增加EPP/XLPP患者的阳光耐受性。Afamelanotide目前已被欧盟和瑞士批准用于EPP/XLPP患者,美国食品和药物管理局正在对其进行审查。现就EPP/XLPP的临床特点及治疗现状作一综述。我们讨论了afamelanotide的药理学、临床疗效、安全性和耐受性,并总结了几个关键的II期和III期临床试验的结果。这些数据表明,对于那些患有这些衰弱性疾病的人来说,afamelanotide是一种很有希望的治疗方法。
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来源期刊
Application of Clinical Genetics
Application of Clinical Genetics Biochemistry, Genetics and Molecular Biology-Genetics
CiteScore
5.40
自引率
0.00%
发文量
20
审稿时长
16 weeks
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