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Anti-CD3 mAbs for treatment of type 1 diabetes.

机译:用于治疗1型糖尿病的抗CD3单抗。

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The use of anti-CD3 monoclonal antibodies (mAbs) has moved from the bench to the bedside. The experience with the anti-human CD3 mAb OKT3 for treatment of transplant rejection identified limitations that were largely overcome with the creation of humanized non-FcR binding antibodies: Teplizumab, Otelixizumab and Visilizumab. Preclinical studies showed the ability of the drugs to reverse hyperglycaemia in diabetic non-obese diabetic (NOD) mice providing rationale for clinical trials with the agents. The former two drugs have been tested in subjects with new onset type 1 diabetes. They have both shown, in randomized clinical trials, an ability to reduce the loss of insulin production over the first 2 years of the disease. In addition, the need for exogenous insulin to maintain glucose control has been reduced. However, these agents alone do not restore normal glucose control, and future approaches will likely require combinations of agents with complementary immune or metabolic activity.
机译:抗CD3单克隆抗体(mAb)的使用已从工作台转移到床边。抗人CD3 mAb OKT3在治疗移植排斥中的经验确定了局限性,这些局限性在创建人源化非FcR结合抗体(特普珠单抗,奥替昔单抗和维西珠单抗)时得以克服。临床前研究表明,该药物具有逆转糖尿病非肥胖糖尿病(NOD)小鼠高血糖的能力,为使用该药物进行临床试验提供了依据。前两种药物已在患有新发1型糖尿病的受试者中进行了测试。他们都在随机临床试验中显示了在疾病的前两年内减少胰岛素产生损失的能力。另外,减少了维持葡萄糖控制所需的外源胰岛素。然而,仅这些试剂不能恢复正常的葡萄糖控制,未来的方法可能需要结合具有互补免疫或代谢活性的试剂。

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