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首页> 外文期刊>Bioconjugate Chemistry >preparation and Evaluation of Glycosylated Arginine-Glycine-Aspartate (RGD) Derivatives for Integrin Targeting
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preparation and Evaluation of Glycosylated Arginine-Glycine-Aspartate (RGD) Derivatives for Integrin Targeting

机译:整合素靶向的糖基化精氨酸-甘氨酸-天冬氨酸(RGD)衍生物的制备和评价

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摘要

Arginine-glycine-aspartate (RGD) derivatives were prepared by a combination of solid-phase and solution-phase synthesis for selective targeting of alpha_vbeta3 integrin expressed in tumors.In order to evaluate the value of a triazole moiety as a proposed amide isostere,the side chain glycosylated cyclic RGD (cRGD) peptides were synthesized with either a natural amide linkage or a triazole.Affinity of the cRGD constructs for the alpha_vbeta3 integrin was determined in a solid-phase competitive binding assay,showing strong similarity in binding affinity for each of the compounds under evaluation.Furthermore,the in vivo tumor targeting potential of glycosylated cRGD peptides,linked via amide or triazole,was investigated by determining the biodistribution of ~(125)I-labeled derivatives in mice with tumors expressing alpha_vbeta3.All of the cyclic RGD derivatives showed preferential uptake in the subcutaneous tumors,with the highest tumor-to-blood ratio measured for the triazole-linked glycosylated derivative.The results of the present study are a clear indication of the value of the triazole moiety as a suitable amide isostere in the development of glycosylated peptides as pharmaceuticals.
机译:通过固相和溶液相合成相结合的方法制备精氨酸-甘氨酸-天冬氨酸(RGD)衍生物,以选择性靶向肿瘤中表达的α_vbeta3整联蛋白。为了评估三唑部分作为拟议的酰胺等排物的价值,侧链糖基化环状RGD(cRGD)肽是通过天然酰胺键或三唑合成的.cRGD构建体对α_vbeta3整联蛋白的亲和力在固相竞争结合测定中确定,显示出对每种此外,通过测定〜(125)I标记的衍生物在具有表达α_vbeta3的肿瘤的小鼠中的生物分布,研究了通过酰胺或三唑连接的糖基化cRGD肽在体内的靶向肿瘤的潜力。 RGD衍生物在皮下肿瘤中表现出优先摄取,三唑连接的糖具有最高的肿瘤血比糖基化衍生物。本研究的结果清楚地表明了三唑部分作为糖基化肽作为药物开发中的合适酰胺等排物的价值。

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