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SMS 201-995的临床评估。肠道神经内分泌肿瘤的长期治疗、口服给药的疗效以及在非肿瘤性不适当促甲状腺激素分泌过多症中的可能应用。

Clinical evaluation of SMS 201-995. Long-term treatment in gut neuroendocrine tumours, efficacy of oral administration, and possible use in non-tumoural inappropriate TSH hypersecretion.

作者信息

Williams G, Anderson J V, Williams S J, Bloom S R

机构信息

Department of Medicine, Royal Postgraduate Medical School, Hammersmith Hospital, London, UK.

出版信息

Acta Endocrinol Suppl (Copenh). 1987;286:26-36.

PMID:2892335
Abstract

Long-acting somatostatin analogues such as SMS 201-995 (Sandoz) are being evaluated in a wide range of clinical indications, including gut neuroendocrine tumours and acrogemaly. Long-term continuous SMS 201-995 treatment has achieved useful symptomatic improvement in diarrhoea in 4 patients with metastatic VIPomas who had relapsed following previous treatment. Clinical improvement has outlasted suppression of VIP secretion (suggesting an additional direct antisecretory action of SMS 201-995) and has occurred despite expansion of hepatic metastases. In 6 patients with tumours secreting gastrin and/or glucagon, secretion of these peptides was acutely inhibited by SMS 201-995. However, endocrine and clinical responses to chronic treatment have been less consistent. SMS 201-995 is active orally at doses of 4-8 mg and when given thrice-daily to 6 patients with active acromegaly, suppressed mean 24-h growth hormone levels by 51-88%. Despite significantly reduced plasma insulin concentrations, glucose tolerance did not deteriorate. SMS 201-995 was also effective in suppressing thyroid-stimulating hormone (TSH) and thyroid hormone secretion in a patient with mild thyrotoxicosis due to non-tumoural inappropriate TSH hypersecretion. In all cases SMS 201-995 treatment has been well tolerated and has few side-effects.

摘要

长效生长抑素类似物,如SMS 201-995(山德士公司生产),正在多种临床适应症中进行评估,包括肠道神经内分泌肿瘤和肢端肥大症。长期持续使用SMS 201-995治疗,使4例先前治疗后复发的转移性血管活性肠肽瘤患者的腹泻症状得到了有效改善。临床症状的改善持续时间超过了血管活性肠肽分泌的抑制时间(提示SMS 201-995具有额外的直接抗分泌作用),并且尽管肝转移灶有所增大,但症状仍有改善。在6例分泌胃泌素和/或胰高血糖素的肿瘤患者中,SMS 201-995可急性抑制这些肽的分泌。然而,长期治疗的内分泌和临床反应不太一致。SMS 201-995口服剂量为4-8毫克时具有活性,当每日三次给予6例活动性肢端肥大症患者时,可使24小时平均生长激素水平降低51%-88%。尽管血浆胰岛素浓度显著降低,但葡萄糖耐量并未恶化。SMS 201-995对一名因非肿瘤性不适当促甲状腺激素分泌过多导致轻度甲状腺毒症的患者,在抑制促甲状腺激素(TSH)和甲状腺激素分泌方面也有效。在所有病例中,SMS 201-995治疗耐受性良好,副作用很少。

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