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组合化学鉴定出针对α4β1整合素的高亲和力拟肽用于体内肿瘤成像。

Combinatorial chemistry identifies high-affinity peptidomimetics against alpha4beta1 integrin for in vivo tumor imaging.

作者信息

Peng Li, Liu Ruiwu, Marik Jan, Wang Xiaobing, Takada Yoshikazu, Lam Kit S

机构信息

Division of Hematology & Oncology, Department of Internal Medicine, UC Davis Cancer Center, University of California, Davis, 4501 X Street, Sacramento, California 95817, USA.

出版信息

Nat Chem Biol. 2006 Jul;2(7):381-9. doi: 10.1038/nchembio798. Epub 2006 Jun 11.

Abstract

Small peptide-based agents have attracted wide interest as cancer-targeting agents for diagnostic imaging and targeted therapy. There is a need to develop new high-affinity and high-specificity peptidomimetic or small-molecule ligands against cancer cell surface receptors. Here we report on the identification of a high-affinity peptidomimetic ligand (LLP2A; IC50 = 2 pM) against alpha4beta1 integrin using both diverse and highly focused one-bead-one-compound combinatorial peptidomimetic libraries in conjunction with high-stringency screening. We further demonstrate that LLP2A can be used to image alpha4beta1-expressing lymphomas with high sensitivity and specificity when conjugated to a near infrared fluorescent dye in a mouse xenograft model. Thus, LLP2A provides an important tool for noninvasive monitoring of alpha4beta1 expression and activity during tumor progression, and it shows great potential as an imaging and therapeutic agent for alpha4beta1-positive tumors.

摘要

基于小肽的药物作为用于诊断成像和靶向治疗的癌症靶向药物已引起广泛关注。需要开发针对癌细胞表面受体的新型高亲和力和高特异性拟肽或小分子配体。在此,我们报告了使用多样化且高度聚焦的单珠单化合物组合拟肽文库结合高严格筛选,鉴定出一种针对α4β1整合素的高亲和力拟肽配体(LLP2A;IC50 = 2 pM)。我们进一步证明,在小鼠异种移植模型中,当与近红外荧光染料偶联时,LLP2A可用于以高灵敏度和特异性对表达α4β1的淋巴瘤进行成像。因此,LLP2A为在肿瘤进展过程中无创监测α4β1的表达和活性提供了重要工具,并且它作为α4β1阳性肿瘤的成像和治疗药物显示出巨大潜力。

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