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成人隐匿性自身免疫性糖尿病:葡萄糖、胰岛素及次级肽对善得定治疗的反应

Adult onset nesidioblastosis: response of glucose, insulin, and secondary peptides to therapy with Sandostatin.

作者信息

Mozell E J, Woltering E A, O'Dorisio T M, Phillipson B E, Fletcher J, Fletcher W S, Howe B, Hill D, Rhea D

机构信息

Department of Surgery, Oregon Health Sciences University, Portland.

出版信息

Am J Gastroenterol. 1990 Feb;85(2):181-8.

PMID:2405644
Abstract

Adult onset nesidioblastosis (AON) is an extremely rare entity associated with hypersecretion of insulin. Previous reports have demonstrated that the somatostatin analog, Sandostatin (SMS), will control the clinical symptoms induced by infantile nesidioblastosis. We hypothesized that insulin, C-peptide, and secondary peptide secretion from AON is provocable. We also hypothesized that SMS would suppress both basal and provoked primary and secondary peptide secretion in AON. To test this hypothesis, in a patient with AON, 13 gut peptide levels were determined at set intervals during provocative testing with a test meal, a calcium infusion, a secretin bolus, and a glucagon bolus. These tests were repeated under the influence of SMS. Insulin, C-peptide, and pancreatic polypeptide (PP) levels were elevated in the basal state. SMS suppressed all three peptides (mean 68%) (p less than 0.05). Basal fasting glucose rose by 65%, and glucose ratios were raised throughout all four tests. Insulin:glucose ratios decreased during SMS therapy. Insulin and PP secretion was increased by all four provocative tests (mean 458% and 665% above baseline, respectively). C-peptide was provoked by three tests (mean 204%). Peptides with normal basal values were also provocable. GRP and glucagon were provoked by secretin stimulation (182%, 186%, respectively). Calcium infusion stimulated CIP release by 372%. SMS suppressed the peak provoked peptide levels in all positive provocation tests (p less than 0.05). Peak provoked insulin values were decreased by 59%, C-peptide by 75%, and PP by 92%. Peak provoked glucagon, CRP, neurotensin, and GIP levels were decreased by 20%, 65%, 51%, and 73%, respectively. The patient has been maintained on SMS (25 micrograms bid) for 1 yr and has shown decreased insulin levels, normal glucose levels, and, at 1 yr, leads an asymptomatic normal life. SMS is able to suppress primary and secondary peptide secretion in both the fasting and provoked state. The long-term efficacy of SMS may be predicted by its ability to suppress primary peptide release during peak provocation.

摘要

成人隐匿性自身免疫性糖尿病(AON)是一种极其罕见的与胰岛素分泌过多相关的疾病。既往报道显示,生长抑素类似物善龙(SMS)可控制婴儿隐匿性自身免疫性糖尿病引发的临床症状。我们推测AON患者的胰岛素、C肽及次级肽分泌是可激发的。我们还推测SMS会抑制AON患者基础状态及激发状态下的初级和次级肽分泌。为验证这一假设,我们对一名AON患者在进行试餐、钙剂输注、注射促胰液素及注射胰高血糖素激发试验期间,按设定时间间隔测定了13种肠肽水平。这些试验在SMS的影响下重复进行。基础状态下胰岛素、C肽及胰多肽(PP)水平升高。SMS抑制了这三种肽(平均抑制68%)(p<0.05)。基础空腹血糖升高了65%,且在所有四项试验中血糖比值均升高。SMS治疗期间胰岛素:血糖比值降低。所有四项激发试验均使胰岛素和PP分泌增加(分别比基线水平平均升高458%和665%)。三项试验激发了C肽分泌(平均升高204%)。基础值正常的肽也可被激发。促胰液素刺激激发了胃泌素释放肽(GRP)和胰高血糖素分泌(分别升高182%、186%)。钙剂输注使酪酪肽(CIP)释放增加372%。在所有阳性激发试验中,SMS均抑制了激发后的肽峰值水平(p<0.05)。激发后的胰岛素峰值降低了59%,C肽降低了75%,PP降低了92%。激发后的胰高血糖素、降钙素基因相关肽(CRP)、神经降压素及葡萄糖依赖性促胰岛素多肽(GIP)峰值水平分别降低了20%、65%、51%和73%。该患者已接受SMS(25微克,每日两次)治疗1年,胰岛素水平降低,血糖水平正常,且在1年时无症状,生活正常。SMS能够抑制空腹及激发状态下的初级和次级肽分泌。SMS的长期疗效可通过其在激发峰值时抑制初级肽释放的能力来预测。

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