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靶向递送源自人甲种胎儿蛋白的抗癌生长抑制肽:国际多中心协作研究综述。

Targeted delivery of anti-cancer growth inhibitory peptides derived from human alpha-fetoprotein: review of an International Multi-Center Collaborative Study.

机构信息

Wadsworth Center, New York State Department of Health, Empire State Plaza, Albany, New York 12201, USA.

出版信息

J Drug Target. 2010 Sep;18(8):575-88. doi: 10.3109/10611861003587243.

DOI:10.3109/10611861003587243
PMID:20151941
Abstract

The alpha-fetoprotein derived growth inhibitory peptide (GIP) is a 34-amino acid peptide composed of three biologically active subfragments. GIP-34 and its three constituent segments have been synthesized, purified, and studied for biological activity. The GIP-34 and GIP-8 have been characterized as anticancer therapeutic peptides. An multicenter study was initiated to elucidate the means by which these peptide drugs could be targeted to tumor cells. The study first established which cancer types were specifically targeted by the GIP peptides in both in vitro and in vivo investigations. It was next demonstrated that radiolabeled peptide ((125)I GIP-34) is specifically localized to rodent breast tumors at 24 h post-injection. The radionuclide studies also provided evidence for a proposed cell surface receptor; this was confirmed in a further study using fluorescent-labeled GIP-nanobeads which localized at the plasma membrane of MCF-7 breast cancer cells. Finally, it was readily demonstrated that GIP conjugated to either fluorescein or doxorubicin (DOX) underwent tumor cell uptake; subsequently, DOX-GIP conjugates induced cytotoxic cell destruction indicating the utility of GIP segments as cancer therapeutic agents. Following a discussion of the preceding results, a candidate cell surface receptor family was proposed which correlated with previous published reports for a putative AFP/GIP receptor.

摘要

甲胎蛋白衍生的生长抑制肽(GIP)是一种由三个生物活性亚片段组成的 34 个氨基酸肽。已经合成、纯化并研究了 GIP-34 及其三个组成片段的生物活性。GIP-34 和 GIP-8 已被鉴定为抗癌治疗肽。一项多中心研究旨在阐明这些肽类药物如何靶向肿瘤细胞。该研究首先确定了 GIP 肽在体外和体内研究中靶向哪些特定的癌症类型。接下来证明,放射性标记的肽((125)I GIP-34)在注射后 24 小时内特异性定位于啮齿动物乳腺癌。放射性核素研究还为拟议的细胞表面受体提供了证据;在使用荧光标记的 GIP-纳米珠的进一步研究中证实了这一点,这些纳米珠定位于 MCF-7 乳腺癌细胞的质膜上。最后,很容易证明与荧光素或阿霉素(DOX)缀合的 GIP 被肿瘤细胞摄取;随后,DOX-GIP 缀合物诱导细胞毒性细胞破坏,表明 GIP 片段作为癌症治疗剂的效用。在讨论了前面的结果之后,提出了一个候选细胞表面受体家族,该家族与之前发表的关于假定的 AFP/GIP 受体的报告相关。

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