Hereditary Angioedema: Novel Molecules for Treatment of Acute Attacks and Long-Term Prophylaxis

B. Covella, M. Giliberti, Adriano Montinaro, Luigi Rossi, Vincenzo Montinaro
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Abstract

Hereditary angioedema (HAE) is a rare disease caused by a genetic alteration of the SERPING1 gene and characterized by recurrent attacks of angioedema that involve the skin, and the mucosae of the gastrointestinal tract and upper airways, which significantly affect the quality of life of patients. Nowadays there are effective drugs for both 1. treating acute attacks and 2. preventing attacks with a long-term prophylaxis. However, there are some unmet needs for HAE treatment, and therefore several novel molecules are under active testing for this clinical condition. Novel drugs will simplify the mode of administration (oral versus parenteral for both on demand treatment or long-term prophylaxis), prolong the interval between administrations (up to 3–6 months of efficacy with a single administration), target more specifically the central enzymes involved in the generation of bradykinin, the ultimate mediator of angioedema (prekallikrein, activated plasma kallikrein or activated factor XII), and potentially determine a definitive cure for the disease by genetic manipulation of the altered gene (SERPING1) or other downstream genes (KLKB1). In this review we provide a panoramic view of all new medications that are under active experimentation and will probably transform and enrich all of the therapeutic armamentarium for treating this disease.
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遗传性血管性水肿:治疗急性发作和长期预防的新分子
遗传性血管性水肿(HAE)是一种罕见疾病,由 SERPING1 基因的遗传改变引起,其特点是血管性水肿反复发作,累及皮肤、胃肠道粘膜和上呼吸道,严重影响患者的生活质量。目前,已有一些有效的药物可用于:1. 治疗急性发作;2. 长期预防发作。然而,HAE 的治疗仍有一些需求尚未得到满足,因此,目前正在对几种新型分子药物进行积极的临床试验。新型药物将简化给药方式(口服或非肠外给药,用于按需治疗或长期预防),延长给药间隔时间(单次给药疗效可达 3-6 个月),更有针对性地靶向参与产生缓激肽的中枢酶、血管性水肿的最终介质缓激肽(前激肽原、活化血浆激肽或活化因子 XII)的中心酶,并通过对改变的基因(SERPING1)或其他下游基因(KLKB1)进行遗传操作,有可能最终治愈该疾病。在这篇综述中,我们将对正在积极实验的所有新药进行全景式介绍,这些新药很可能会改变和丰富治疗这种疾病的所有治疗手段。
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