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生长抑素类似物在肢端肥大症和胃肠胰神经内分泌肿瘤中的应用:过去、现在与未来

Somatostatin analogues in acromegaly and gastroenteropancreatic neuroendocrine tumours: past, present and future.

作者信息

Öberg Kjell, Lamberts Steven W J

机构信息

University HospitalUppsala, Sweden

Erasmus Medical CenterRotterdam, The Netherlands.

出版信息

Endocr Relat Cancer. 2016 Dec;23(12):R551-R566. doi: 10.1530/ERC-16-0151. Epub 2016 Oct 3.

DOI:10.1530/ERC-16-0151
PMID:27697899
Abstract

Acromegaly is a hormonal disorder that arises when the pituitary gland secretes excess growth hormone (GH), which in turn stimulates a concomitant increase in serum insulin-like growth factor 1 (IGF-1) levels. Gastroenteropancreatic neuroendocrine tumours (GEP-NET) constitute a heterogeneous group of tumours that can secrete serotonin and a variety of peptide hormones that may cause characteristic symptoms known as carcinoid syndrome or other symptoms and hormonal hypersecretion syndromes depending on the tumour's site of origin. Current medical therapy for the treatment of acromegaly and GEP-NET involves the administration of somatostatin analogues that effectively suppress excess hormone secretion. After its discovery in 1979, octreotide became the first synthetic biologically stable somatostatin analogue with a short-acting formulation of octreotide introduced into clinical practice in the late 1980s. Lanreotide, another somatostatin analogue, became available in the mid-1990s initially as a prolonged-release formulation administered every 10 or 14 days. Long-acting release formulations of both octreotide (Sandostatin LAR and Novartis) and lanreotide (Somatuline Autogel, Ipsen), based on microparticle and nanoparticle drug-delivery technologies, respectively, were later developed, which allowed for once-monthly administration and improved convenience. First-generation somatostatin analogues remain one of the cornerstones of medical therapy in the management of pituitary and GEP-NET hormone hypersecretion, with octreotide having the longest established efficacy and safety profile of the somatostatin analogue class. More recently, pasireotide (Signifor), a next-generation multireceptor-targeted somatostatin analogue, has emerged as an alternative therapeutic option for the treatment of acromegaly. This review summarizes the development and clinical success of somatostatin analogues.

摘要

肢端肥大症是一种激素紊乱疾病,当垂体分泌过量生长激素(GH)时就会引发,这进而会刺激血清胰岛素样生长因子1(IGF-1)水平随之升高。胃肠胰神经内分泌肿瘤(GEP-NET)是一组异质性肿瘤,可分泌血清素和多种肽类激素,这些激素可能会导致类癌综合征等特征性症状,或根据肿瘤起源部位导致其他症状和激素分泌过多综合征。目前用于治疗肢端肥大症和GEP-NET的药物疗法包括使用生长抑素类似物,其可有效抑制激素分泌过多。1979年被发现后,奥曲肽成为首个合成的生物稳定生长抑素类似物,其短效制剂于20世纪80年代末引入临床实践。另一种生长抑素类似物兰瑞肽于20世纪90年代中期上市,最初是每10或14天给药一次的长效释放制剂。基于微粒和纳米颗粒药物递送技术,后来分别开发了奥曲肽(善龙,诺华)和兰瑞肽(索马杜林自动凝胶,益普生)的长效释放制剂,这使得给药频率变为每月一次,并提高了便利性。第一代生长抑素类似物仍然是治疗垂体和GEP-NET激素分泌过多的药物疗法的基石之一,奥曲肽在生长抑素类似物类别中具有最长的既定疗效和安全性记录。最近,新一代多受体靶向生长抑素类似物帕西瑞肽(Signifor)已成为治疗肢端肥大症的替代治疗选择。本综述总结了生长抑素类似物的研发情况及其临床成效。

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