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生长抑素-多巴胺嵌合体:一种治疗神经内分泌肿瘤的新方法。

Somatostatin-dopamine chimeras: a novel approach to treatment of neuroendocrine tumors.

机构信息

IPSEN, Milford, Massachusetts 01757, U SA.

出版信息

Horm Metab Res. 2011 Nov;43(12):854-7. doi: 10.1055/s-0031-1287769. Epub 2011 Oct 11.

DOI:10.1055/s-0031-1287769
PMID:21989554
Abstract

A combination of basic research observations concerning the interaction of somatostatin (SST) and dopamine (DA) receptors, and clinical reports of enhanced efficacy of combined SST and DA analogue treatment in suppressing GH hypersecretion, lead to the concept of creating chimeric molecules combining structural features of both compound classes. The resulting SST/DA chimeras retain the ability to interact with receptors of both families and display greatly enhanced potency and efficacy, as compared with that of individual SST or DA receptor agonists. In vitro studies with pituitary adenoma cells from acromegalic patients have demonstrated that the chimeric molecules have exceptional activity with regard to suppression of GH and prolactin secretion. Similarly, potent suppression of ACTH secretion from Cushing's-causing corticotroph tumors, and suppression of nonfunctioning pituitary adenoma proliferation has been observed. The chimeric SST/DA compounds are also quite potent and efficacious in suppressing both GH and IGF1 in vivo when tested in nonhuman primates, with no effect on either insulin secretion or glycemic control. Initial clinical studies examining acute, subcutaneous administration of the chimeric SST/DA compound, BIM-23A760, revealed both prolonged circulating half-life and extended duration of biological effect. With chronic administration, however, BIM-23A760 was found to produce a metabolite with dopaminergic activity that gradually accumulates and interferes with the activity of the parent compound. Consequently, efforts are currently underway to produce a second-generation chimera for treatment of neuroendocrine disease.

摘要

基础研究观察到生长抑素 (SST) 和多巴胺 (DA) 受体相互作用,以及联合 SST 和 DA 类似物治疗增强抑制 GH 分泌过多的疗效的临床报告,这导致了创建结合这两类化合物结构特征的嵌合分子的概念。所得的 SST/DA 嵌合体保留了与两种受体家族相互作用的能力,并表现出比单独的 SST 或 DA 受体激动剂更高的效力和功效。体外研究表明,在肢端肥大症患者的垂体腺瘤细胞中,嵌合分子在抑制 GH 和催乳素分泌方面具有非凡的活性。同样,也观察到对库欣病引起的促肾上腺皮质激素肿瘤的 ACTH 分泌的强烈抑制,以及对无功能垂体腺瘤增殖的抑制。在非人类灵长类动物中进行的体内研究表明,嵌合 SST/DA 化合物在抑制 GH 和 IGF1 方面也非常有效,对胰岛素分泌或血糖控制没有影响。初步的临床研究检查了急性皮下给予嵌合 SST/DA 化合物 BIM-23A760 的效果,发现其循环半衰期延长,生物学效应持续时间延长。然而,在慢性给药时,发现 BIM-23A760 会产生具有多巴胺能活性的代谢物,该代谢物逐渐积累并干扰母体化合物的活性。因此,目前正在努力生产第二代嵌合体以治疗神经内分泌疾病。

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