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Fc-Small Molecule Antibody Mimetics

机译:Fc小分子抗体模拟物

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摘要

Antibody therapeutics are a promising drug class due to their high specificity and favorable pharmacokinetics. While there are many methods for the development of antibodies specific to disease associated antigens, selecting antibodies against functional epitopes with high specificity and affinity can be difficult for certain epitopes. We describe a generalizable method for synthesizing antibody mimetics by site specifically conjugating small molecules (with high affinity and specificity to disease associated antigens) to an Pc fragment to develop drugs with the benefits of an antibody. As a proof of concept, an E269pAcPhe Pc antibody Pc fragment was produced and subsequently site-specifically labeled with a linker-modified folic acid compound to generate an Fc-folic acid antibody-mimetic. This was chosen as the model system because the high-affinity folate receptor FR-alpha is highly expressed in a number of cancer types including breast and ovarian cancer. The specificity of the Fc-folic acid conjugate was assessed via flowcytometry with the folate-receptor positive breast cancer cell line MDA-MB-231 by measuring Fc-folic acid binding in both the absence and presence of an excess of folic acid. Fc-small molecule conjugates could be developed into a unique class of antibody-like therapeutics.
机译:抗体疗法由于其高特异性和良好的药代动力学而成为一种很有前途的药物。尽管有许多方法可以开发出与疾病相关的抗原特异的抗体,但是对于某些表位而言,选择具有高特异性和亲和力的功能性表位的抗体可能很困难。我们描述了通过位点特异性结合小分子(对疾病相关抗原具有高亲和力和特异性)与Pc片段以开发具有抗体益处的药物来合成抗体模拟物的通用方法。作为概念证明,产生了E269pAcPhe Pc抗体Pc片段,随后用接头修饰的叶酸化合物进行了位点特异性标记,以生成模拟Fc-叶酸的抗体。之所以选择该模型作为模型系统,是因为高亲和力的叶酸受体FR-α在包括乳腺癌和卵巢癌在内的许多癌症类型中都高度表达。通过叶酸-受体阳性乳腺癌细胞系MDA-MB-231的流式细胞术,通过在不存在和存在过量叶酸的情况下测量Fc-叶酸的结合,来评估Fc-叶酸结合物的特异性。 Fc-小分子偶联物可以发展成一类独特的抗体样治疗剂。

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