口服 NPC43 可对抗链脲佐菌素诱导的 1 型糖尿病小鼠的高血糖,并激活胰岛素受体。
Oral administration of NPC43 counters hyperglycemia and activates insulin receptor in streptozotocin-induced type 1 diabetic mice.
机构信息
Division of Life Sciences, Alltech, Inc, Nicholasville, Kentucky, USA
Department of OB/GYN, University of Louisville School of Medicine, Louisville, Kentucky, USA.
出版信息
BMJ Open Diabetes Res Care. 2020 Sep;8(1). doi: 10.1136/bmjdrc-2020-001695.
INTRODUCTION
Adenosine, 5'-Se-methyl-5'-seleno-,2',3'-diacetate (NPC43) is a recently identified small, non-peptidyl molecule which restores normal insulin signaling in a mouse model of type 2 diabetes (Lan ). The present study investigated the ability of NPC43 as an oral and injectable insulin-replacing agent to activate insulin receptor (INSR) and counter hyperglycemia in streptozotocin (STZ)-induced type 1 diabetic (T1D) mice.
RESEARCH DESIGN AND METHODS
In this study, STZ was intraperitoneally injected into wild-type mice to induce hyperglycemia and hypoinsulinemia, the main features of T1D. These STZ-induced T1D mice were given NPC43 orally or intraperitoneally and blood glucose levels were measured using a glucometer. Protein levels of phosphorylated and total Insrβ, protein kinase B (Akt) and AS160 (critical for glucose uptake) in the skeletal muscle and liver of STZ-induced T1D mice following oral NPC43 treatment were determined by western blot analysis. In addition, hepatic expression of activated Insr in STZ-induced T1D mice after intraperitoneal NPC43 treatment was measured by ELISA. Student's t-test was used for statistical analysis.
RESULTS
Oral administration of NPC43 at a dose of 5.4 or 10.8 mg/kg body weight (mpk) effectively lowered blood glucose levels in STZ-induced T1D mice at ≥1 hour post-treatment and the glucose-lowering activity of oral NPC43 persisted for 5 hours. Blood glucose levels were also reduced in STZ-induced T1D mice following intraperitoneal NPC43 (5.4 mpk) treatment. Protein levels of phosphorylated Insrβ, Akt and AS160 were significantly increased in the skeletal muscle and liver of STZ-induced T1D mice after oral NPC43 (5.4 mpk) treatment. In addition, activation of hepatic Insr was observed in STZ-induced T1D mice following intraperitoneal NPC43 (5.4 mpk) treatment.
CONCLUSIONS
We conclude that NPC43 is a de facto fast-acting oral and injectable insulin mimetic which activates Insr and mitigates hyperglycemia in a mouse model of T1D.
简介
腺苷 5'-亚甲基-5'-硒代-2',3'-二乙酸酯(NPC43)是一种最近发现的小分子非肽类分子,可恢复 2 型糖尿病小鼠模型中的正常胰岛素信号(Lan)。本研究探讨了 NPC43 作为口服和注射用胰岛素替代物的能力,以激活胰岛素受体(INSR)并对抗链脲佐菌素(STZ)诱导的 1 型糖尿病(T1D)小鼠的高血糖。
研究设计和方法
在这项研究中,将 STZ 腹腔注射到野生型小鼠中,以诱导高血糖和低胰岛素血症,这是 T1D 的主要特征。这些 STZ 诱导的 T1D 小鼠给予 NPC43 口服或腹腔内注射,并使用血糖仪测量血糖水平。通过 Western blot 分析测定 STZ 诱导的 T1D 小鼠口服 NPC43 治疗后骨骼肌和肝脏中磷酸化和总 Insrβ、蛋白激酶 B(Akt)和 AS160(葡萄糖摄取的关键)的蛋白水平。此外,通过 ELISA 测定 STZ 诱导的 T1D 小鼠腹腔内 NPC43 治疗后肝内激活的 Insr 的表达。使用 Student's t 检验进行统计分析。
结果
口服剂量为 5.4 或 10.8mg/kg 体重(mpk)的 NPC43 可有效降低 STZ 诱导的 T1D 小鼠的血糖水平,在治疗后≥1 小时起效,口服 NPC43 的降血糖作用持续 5 小时。腹腔内 NPC43(5.4mpk)治疗也降低了 STZ 诱导的 T1D 小鼠的血糖水平。口服 NPC43(5.4mpk)治疗后,STZ 诱导的 T1D 小鼠骨骼肌和肝脏中磷酸化 Insrβ、Akt 和 AS160 的蛋白水平显著升高。此外,腹腔内 NPC43(5.4mpk)治疗后观察到 STZ 诱导的 T1D 小鼠肝内 Insr 的激活。
结论
我们得出结论,NPC43 是一种事实上的速效口服和注射用胰岛素模拟物,可激活 Insr 并缓解 1 型糖尿病小鼠模型中的高血糖。
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