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新型合成环化整合素αvβ3结合肽ALOS4:在小鼠黑色素瘤模型中的抗肿瘤活性

Novel synthetic cyclic integrin αvβ3 binding peptide ALOS4: Antitumor activity in mouse melanoma models.

作者信息

Yacobovich Shiri, Tuchinsky Lena, Kirby Michael, Kardash Tetiana, Agranyoni Oryan, Nesher Elimelech, Redko Boris, Gellerman Gary, Tobi Dror, Gurova Katerina, Koman Igor, Ashur Fabian Osnat, Pinhasov Albert

机构信息

Department of Molecular Biology, Ariel University, Ariel, Israel.

Department of Cell Stress Biology, Roswell Park Cancer Institute, Buffalo, New York, USA.

出版信息

Oncotarget. 2016 Sep 27;7(39):63549-63560. doi: 10.18632/oncotarget.11363.

Abstract

ALOS4, a unique synthetic cyclic peptide without resemblance to known integrin ligand sequences, was discovered through repeated biopanning with pIII phage expressing a disulfide-constrained nonapeptide library. Binding assays using a FITC-labeled analogue demonstrated selective binding to immobilized αvβ3 and a lack of significant binding to other common proteins, such as bovine serum albumin and collagen. In B16F10 cell cultures, ALOS4 treatment at 72 h inhibited cell migration (30%) and adhesion (up to 67%). Immunofluorescent imaging an ALOS4-FITC analogue with B16F10 cells demonstrated rapid cell surface binding, and uptake and localization in the cytoplasm. Daily injections of ALOS4 (0.1, 0.3 or 0.5 mg/kg i.p.) to mice inoculated with B16F10 mouse melanoma cells in two different cancer models, metastatic and subcutaneous tumor, resulted in reduction of lung tumor count (metastatic) and tumor mass (subcutaneous) and increased survival of animals monitored to 45 and 60 days, respectively. Examination of cellular activity indicated that ALOS4 produces inhibition of cell migration and adhesion in a concentration-dependent manner. Collectively, these results suggest that ALOS4 is a structurally-unique selective αvβ3 integrin ligand with potential anti-metastatic activity.

摘要

ALOS4是一种独特的合成环肽,与已知的整合素配体序列没有相似性,它是通过用表达二硫键约束九肽文库的pIII噬菌体反复进行生物淘选而发现的。使用异硫氰酸荧光素(FITC)标记类似物的结合试验表明,它能选择性地结合固定化的αvβ3,而与其他常见蛋白质(如牛血清白蛋白和胶原蛋白)没有明显结合。在B16F10细胞培养中,72小时的ALOS4处理可抑制细胞迁移(30%)和黏附(高达67%)。用ALOS4-FITC类似物对B16F10细胞进行免疫荧光成像显示,其能快速结合细胞表面,并摄取和定位在细胞质中。在两种不同的癌症模型(转移性和皮下肿瘤)中,每天给接种B16F10小鼠黑色素瘤细胞的小鼠腹腔注射ALOS4(0.1、0.3或0.5毫克/千克),分别导致肺肿瘤数量(转移性)减少和肿瘤质量(皮下)减少,并使监测至45天和60天的动物存活率提高。细胞活性检测表明,ALOS4以浓度依赖的方式抑制细胞迁移和黏附。总体而言,这些结果表明ALOS4是一种结构独特的选择性αvβ3整合素配体,具有潜在的抗转移活性。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/b458/5325384/b92397e41296/oncotarget-07-63549-g001.jpg

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