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首页> 外文期刊>Biomaterials >Targeting inhibition of Foxp3 by a CD28 2 '-Fluro oligonucleotide aptamer conjugated to P60-peptide enhances active cancer immunotherapy
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Targeting inhibition of Foxp3 by a CD28 2 '-Fluro oligonucleotide aptamer conjugated to P60-peptide enhances active cancer immunotherapy

机译:通过CD28 2'-Fluro寡核苷酸适体鉴定FoxP3的抑制作用与P60肽缀合的Aptamer增强了活性癌症免疫疗法

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摘要

The specific inhibition of Treg function has long been a major technical challenge in cancer immunotherapy. So far no single cell-surface marker has been identified that could be used to distinguish Treg cells from other lymphocytes. The only available specific marker mostly expressed in Treg is Foxp3, which is an intracellular transcription factor. A targeting molecule able to penetrate the membrane and inhibit Foxp3 within the cell is needed. P60-peptide is able to do that, but due to lack of target specificity, the doses are extremely high. In this study we have shown as a proof of concept that P60 Foxp3 inhibitor peptide can be conjugated with a CD28 targeting aptamer to deliver the peptide to CD28-expressing cells. The AptCD28-P60 construct is a clinically feasible reagent that improves the efficacy of the unconjugated P60 peptide very significantly. This approach was used to inhibit Treg function in a vaccination context, and it has shown a significant improvement in the induced immune response, entailing a lower tumor load in an antigen-specific cancer vaccine protocol. (c) 2016 Elsevier Ltd. All rights reserved.
机译:Treg函数的具体抑制长期以来一直是癌症免疫疗法的主要技术挑战。到目前为止,未鉴定单个细胞表面标记物,其可用于将Treg细胞与其他淋巴细胞区分开。唯一在Treg中表达的特定特异性标记是Foxp3,其是细胞内转录因子。需要一种能够穿透膜并抑制细胞内的FoxP3的靶向分子。 P60-肽能够做到这一点,但由于缺乏靶特异性,剂量非常高。在本研究中,我们已经显示为概念证据,即P60 FoxP3抑制剂肽可以与靶向适体的CD28缀合,以将肽递送至CD28的表达细胞。 APTCD28-P60构建体是一种临床可行的试剂,可显着提高未缀合的P60肽的功效。该方法用于抑制疫苗接种背景下的Treg函数,并且它显示出诱导的免疫应答的显着改善,在抗原特异性癌症疫苗方案中抑制肿瘤载荷。 (c)2016 Elsevier Ltd.保留所有权利。

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