Gaucher disease is a rare inborn error of glycosphingolipid metabolism due to deficiency of lysosomal acid β-glucocerebrosidase; the condition has totemic significance for the development of orphan drugs. A designer therapy, which harnesses the mannose receptor to complement the functional defect in macrophages, ameliorates the principal clinical manifestations in hematopoietic bone marrow and viscera. While several aspects of Gaucher disease (particularly those affecting the skeleton and brain) are refractory to treatment, enzyme (replacement) therapy has become a pharmaceutical blockbuster. Human β-glucocerebrosidase was originally obtained from placenta and the Genzyme Corporation (Allston, MA) subsequently developed a recombinant product. After purification, the enzyme is modified to reveal terminal mannose residues which facilitate selective uptake of the protein, imiglucerase (Cerezyme®), in macrophage-rich tissues. The unprecedented success of Cerezyme has attracted fierce competition: two biosimilar agents, velaglucerase-alfa, VPRIV® (Shire Human Genetic Therapies, Dublin, Ireland) and taliglucerase-alfa (Protalix, Carmiel, Israel), are now approved or in late-phase clinical development as potential ‘niche busters’. Oral treatments have advantages over biological agents for disorders requiring lifelong therapy and additional stratagems which utilize small, orally active molecules have been introduced; these include two chemically distinct compounds which inhibit uridine diphosphate glucose: N-acylsphingosine glucosyltransferase, the first step in the biosynthesis of glucosylceramide – a key molecular target in Gaucher disease and other glycosphingolipidoses. Academic and commercial enterprises in biotechnology have combined strategically to expand the therapeutic repertoire in Gaucher disease. The innovative potential of orphan drug legislation has been realized – with prodigious rewards for companies embracing its humanitarian precepts. In the era before enzyme therapy, bone marrow transplantation was shown to correct systemic disease in Gaucher patients by supplying a source of competent donor macrophages. As a radical advance on cell- or protein-replacement techniques, contemporary methods for transferring genes to autologous hematopoietic stem cells, and to the brain, merit further exploration. At present, the inflated pharmaceutical niche of Gaucher disease appears to be resilient, but if the remaining unmet needs of patients are to be convincingly addressed and commercial development sustained, courageous scientific investment and clinical experimentation will be needed.
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机译:高雪氏病是由于溶酶体酸β-葡萄糖脑苷脂酶缺乏引起的糖鞘脂代谢的罕见先天性错误。该病对于孤儿药的开发具有图腾意义。利用甘露糖受体来补充巨噬细胞功能缺陷的设计疗法可改善造血骨髓和内脏的主要临床表现。尽管高雪氏病的几个方面(尤其是影响骨骼和大脑的疾病)难以治疗,但酶(替代)疗法已成为药物领域的重磅炸弹。人β-葡萄糖脑苷脂酶最初是从胎盘获得的,Genzyme公司(马萨诸塞州Allston)随后开发了重组产品。纯化后,对该酶进行修饰以显示末端甘露糖残基,从而有助于在富含巨噬细胞的组织中选择性摄取蛋白质伊米苷酶(Cerezyme ®)。 Cerezyme的空前成功吸引了激烈的竞争:两种生物仿制药,分别是velaglucerase-alfa,VPRIV ®(Shire Human Genetic Therapies,爱尔兰都柏林)和taliglucerase-alfa(Protalix,Carmiel,以色列)现在已被批准或处于后期临床开发中,有望成为潜在的“小众破坏者”。对于需要终身治疗的疾病,口服治疗优于生物制剂,并且已经引入了利用小的口服活性分子的其他策略。其中包括抑制尿苷二磷酸葡萄糖的两种化学性质不同的化合物:N-酰基鞘氨醇葡萄糖基转移酶,这是生物合成葡糖神经酰胺的第一步-戈谢病和其他糖鞘脂的关键分子靶标。生物技术领域的学术和商业企业已经战略性地合并在一起,以扩大高雪氏病的治疗范围。孤儿药立法的创新潜力已得到实现–对于接受其人道主义戒律的公司而言,这是巨大的回报。在酶治疗之前的时代,通过提供合格的供体巨噬细胞来源,证明了骨髓移植可以纠正高雪患者的全身疾病。作为细胞或蛋白质置换技术的根本性进步,当代将基因转移至自体造血干细胞以及转移至大脑的方法值得进一步探索。目前,膨胀的戈谢病(Gaucher)病药物小生境似乎具有复原力,但是如果要令人信服地解决患者的剩余未满足需求并维持商业发展,则需要勇敢的科学投资和临床实验。
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