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单链可变片段对结肠癌中前基质金属蛋白酶-7的抗癌作用。

Anticancer effect of a single-chain variable fragment against pro-matrix metalloproteinase-7 in colon cancer.

作者信息

Min Shinhye, Jang Bohee, Yun Ji-Hye, Yang Hyeonju, Sung Jee Young, Lim Ga-Eun, Kim Yong-Nyun, Lee Weontae, Oh Eok-Soo

机构信息

Department of Life Sciences, Ewha Womans University, Seoul 03760, South Korea.

Center for Genome Engineering, Institute for Basic Science, 55, Expo-ro, Yuseong-gu, Daejeon 34126, South Korea; Epinogen, Ltd., 604 KBIZ DMC Tower, Seoul 03929, South Korea.

出版信息

Matrix Biol. 2025 Feb;135:125-134. doi: 10.1016/j.matbio.2024.12.009. Epub 2024 Dec 27.

DOI:10.1016/j.matbio.2024.12.009
PMID:39805673
Abstract

Disrupting the interaction between matrix metalloproteinase-7 (MMP-7) and syndecan-2 (SDC-2) can yield anticancer effects in colon cancer cells. Here, a single-chain variable fragment (scFv) targeting the pro-domain of MMP-7 was generated as a potential candidate anticancer agent. Among the generated scFvs, those designated 1B7 and 1C3 showed the strongest abilities to inhibit the ability of MMP-7 pro-domain to directly interact with SDC-2 in vitro and decrease the cancer activities of human HT29 colon adenocarcinoma cells. Consistently, 1B7 and 1C3 inhibited the cell-surface localization of pro-MMP-7, reduced the gelatinolytic activity of MMP-7, and suppressed the cancer activities of metastatic HCT116 human colon carcinoma cells. Notably, 1B7 inhibited the primary tumor growth and lung metastasis of CT26 mouse colon cancer cells in a mouse model. Compared to 1B7, the 1B7-Fc fusion antibody showed better anti-tumorigenic activity against HCT116 cells in culture and a syngeneic mouse model. Together, these data suggest that 1B7-Fc exerts anticancer effects by interfering with the interaction of MMP-7 and SDC-2 and could be a promising therapeutic antibody for colon cancer.

摘要

破坏基质金属蛋白酶-7(MMP-7)与多功能蛋白聚糖-2(SDC-2)之间的相互作用可在结肠癌细胞中产生抗癌作用。在此,生成了一种靶向MMP-7前结构域的单链可变片段(scFv)作为潜在的候选抗癌剂。在生成的scFv中,命名为1B7和1C3的scFv在体外表现出最强的抑制MMP-7前结构域与SDC-2直接相互作用的能力,并降低了人HT29结肠腺癌细胞的癌活性。同样,1B7和1C3抑制了前MMP-7在细胞表面的定位,降低了MMP-7的明胶分解活性,并抑制了转移性HCT116人结肠癌细胞的癌活性。值得注意的是,在小鼠模型中,1B7抑制了CT26小鼠结肠癌细胞的原发性肿瘤生长和肺转移。与1B7相比,1B7-Fc融合抗体在培养物和同基因小鼠模型中对HCT116细胞表现出更好的抗肿瘤活性。总之,这些数据表明1B7-Fc通过干扰MMP-7与SDC-2的相互作用发挥抗癌作用,可能是一种有前景的结肠癌治疗抗体。

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