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Conformation-sensing antibodies stabilize the oxidized form of PTP1B and inhibit its phosphatase activity

机译:构象敏感抗体可稳定PTP1B的氧化形式并抑制其磷酸酶活性

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摘要

Protein tyrosine phosphatase 1B (PTP1B) plays important roles in downregulation of insulin and leptin signaling and is an established therapeutic target for diabetes and obesity. PTP1B is regulated by reactive oxygen species (ROS) produced in response to various stimuli, including insulin. The reversibly oxidized form of the enzyme (PTP1B-OX) is inactive and undergoes profound conformational changes at the active site. We generated conformation-sensor antibodies, in the form of single-chain variable fragments (scFvs), that stabilize PTP1B-OX and thereby inhibit its phosphatase function. Expression of conformation-sensor scFvs as intracellular antibodies (intrabodies) enhanced insulin-induced tyrosyl phosphorylation of the β subunit of the insulin receptor and its substrate IRS-1 and increased insulin-induced phosphorylation of PKB/AKT. Our data suggest that stabilization of the oxidized, inactive form of PTP1B with appropriate therapeutic molecules may offer a paradigm for phosphatase drug development.
机译:蛋白酪氨酸磷酸酶1B(PTP1B)在胰岛素和瘦素信号的下调中起重要作用,并且是糖尿病和肥胖症的既定治疗靶标。 PTP1B由响应各种刺激(包括胰岛素)产生的活性氧(ROS)调节。酶(PTP1B-OX)的可逆氧化形式是无活性的,并且在活性位点发生深刻的构象变化。我们生成了单链可变片段(scFvs)形式的构象传感器抗体,可稳定PTP1B-OX,从而抑制其磷酸酶功能。构象传感器scFvs作为细胞内抗体(体内抗体)的表达增强了胰岛素诱导的胰岛素受体β亚基及其底物IRS-1的酪氨酰磷酸化,并增加了胰岛素诱导的PKB / AKT的磷酸化。我们的数据表明,用适当的治疗性分子稳定PTP1B的氧化,失活形式可能为磷酸酶药物开发提供了范例。

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