首页> 美国卫生研究院文献>Journal of the Endocrine Society >Selective Somatostatin 5 (SST5) and Somatostatin 2 (SST2) Nonpeptide Agonists Potently Suppress Glucose- and Tolbutamide-Stimulated Dynamic Insulin Secretion From Isolated Human Islets
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Selective Somatostatin 5 (SST5) and Somatostatin 2 (SST2) Nonpeptide Agonists Potently Suppress Glucose- and Tolbutamide-Stimulated Dynamic Insulin Secretion From Isolated Human Islets

机译:选择性生长抑制菌素5(SST5)和生长抑制菌素2(SST2)非肽激动剂有效地抑制葡萄糖和甲醛酰胺刺激的动态胰岛素分泌来自分离的人类胰岛

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摘要

Congenital hyperinsulinism (HI) is the most common cause of persistent hypoglycemia in newborns and infants and arises from dysregulated insulin secretion. Rapid recognition and treatment are vital to prevent seizures, permanent developmental delays, coma, or even death. Very few medical options exist to treat congenital HI patients: the KATP channel activator diazoxide, the injectable somatostatin receptor peptide agonists octreotide and lanreotide, or chronic glucose infusions. However, side effects and/or limited efficacy render these therapies inadequate for many patients.
机译:先天性高胰岛素素(HI)是新生儿和婴儿持续低血糖症最常见的原因,并且由具有疑难解的胰岛素分泌出来。快速识别和治疗对于防止癫痫发作,永久性发展延误,昏迷或甚至死亡至关重要。很少有医疗选择治疗先天性患者:KATP通道激活剂二氮酰肟,可注射的生长抑素受体受体肽激动剂octreotide和甘油酯,或慢性葡萄糖输注。然而,副作用和/或有限的功效使这些治疗不足以适用于许多患者。

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