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Oral Insulin-Mimetic Compounds That Act Independently of Insulin

机译:独立于胰岛素发挥作用的口服胰岛素模拟化合物

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摘要

The hallmarks of insulin action are the stimulation and suppression of anabolic and catabolic responses, respectively. These responses are orchestrated by the insulin pathway and are initiated by the binding of insulin to the insulin receptor, which leads to activation of the receptor's intrinsic tyrosine kinase. Severe defects in the insulin pathway, such as in types A and B and advanced type 1 and 2 diabetes lead to severe insulin resistance, resulting in a partial or complete absence of response to exogenous insulin and other known classes of antidiabetes therapies. We have characterized a novel class of arylalkylamine vanadium salts that exert potent insulin-mimetic effects downstream of the insulin receptor in adipocytes. These compounds trigger insulin signaling, which is characterized by rapid activation of insulin receptor substrate-1, Akt, and glycogen synthase kinase-3 independent of insulin receptor phosphorylation. Administration of these compounds to animal models of diabetes lowered glycemia and normalized the plasma lipid profile. Arylalkylamine vanadium compounds also showed antidiabetic effects in severely diabetic rats with undetectable circulating insulin. These results demonstrate the feasibility of insulin-like regulation in the complete absence of insulin and downstream of the insulin receptor. This represents a novel therapeutic approach for diabetic patients with severe insulin resistance.
机译:胰岛素作用的标志分别是对同化和分解代谢反应的刺激和抑制。这些反应是由胰岛素途径精心策划的,并且是由胰岛素与胰岛素受体的结合而引发的,从而导致受体内在的酪氨酸激酶的激活。胰岛素途径中的严重缺陷,例如在A型和B型以及晚期1型和2型糖尿病中,会导致严重的胰岛素抵抗,导致部分或完全不对外源胰岛素和其他已知类型的抗糖尿病疗法产生反应。我们已经表征了一类新的芳基烷基胺钒盐,其在脂肪细胞中的胰岛素受体下游发挥强效的胰岛素模拟作用。这些化合物触发胰岛素信号转导,其特征是胰岛素受体底物1,Akt和糖原合酶激酶3的快速活化独立于胰岛素受体的磷酸化。将这些化合物施用于糖尿病动物模型可降低血糖并使血浆脂质分布正常化。芳基烷基胺钒化合物在严重糖尿病大鼠中还具有抗糖尿病作用,其中循环胰岛素无法检测到。这些结果证明了在完全不存在胰岛素和胰岛素受体下游的情况下进行胰岛素样调节的可行性。这代表了具有严重胰岛素抵抗的糖尿病患者的新治疗方法。

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