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A fragment of the HMGN2 protein homes to the nuclei of tumor cells and tumor endothelial cells in vivo

机译:HMGN2蛋白的片段在体内归巢于肿瘤细胞和肿瘤内皮细胞的细胞核

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摘要

We used a screening procedure to identify protein domains from phage-displayed cDNA libraries that bind both to bone marrow endothelial progenitor cells and tumor vasculature. Screening phage for binding of progenitor cell-enriched bone marrow cells in vitro, and for homing to HL-60 human leukemia cell xenograft tumors in vivo, yielded a cDNA fragment that encodes an N-terminal fragment of human high mobility group protein 2 (HMGN2, formerly HMG-17). Upon i.v. injection, phage displaying this HMGN2 fragment homed to HL-60 and MDA-MB-435 tumors. Testing of subfragments localized the full binding activity to a 31-aa peptide (F3) in the HMGN2 sequence. Fluorescein-labeled F3 peptide bound to and was internalized by HL-60 cells and human MDA-MB-435 breast cancer cells, appearing initially in the cytoplasm and then in the nuclei of these cells. Fluorescent F3 accumulated in HL-60 and MDA-MB-435 tumors after an i.v. injection, appearing in the nuclei of tumor endothelial cells and tumor cells. Thus, F3 can carry a payload (phage, fluorescein) to a tumor and into the cell nuclei in the tumor. This peptide may be suitable for targeting cytotoxic drugs and gene therapy vectors into tumors.
机译:我们使用了一种筛选程序,从噬菌体展示的cDNA文库中鉴定出与骨髓内皮祖细胞和肿瘤脉管系统结合的蛋白质结构域。在体外筛选富集祖细胞的骨髓的噬菌体,并在体内归巢到HL-60人白血病细胞异种移植肿瘤,获得了一个cDNA片段,该片段编码人高迁移率族蛋白2(HMGN2)的N端片段。 ,以前是HMG-17)。在i.v.注射后,噬菌体展示了该HMGN2片段,该片段位于HL-60和MDA-MB-435肿瘤中。亚片段的测试将全部结合活性定位于HMGN2序列中的31-aa肽(F3)。荧光素标记的F3肽与HL-60细胞和人MDA-MB-435乳腺癌细胞结合并被其内在化,最初出现在细胞质中,然后出现在这些细胞的细胞核中。静脉内注射后,荧光F3累积在HL-60和MDA-MB-435肿瘤中。注射后,出现在肿瘤内皮细胞和肿瘤细胞的细胞核中。因此,F3可以将有效载荷(噬菌体,荧光素)携带至肿瘤并进入肿瘤的细胞核。该肽可能适合于将细胞毒性药物和基因治疗载体靶向肿瘤。

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