Graduate Group in Biophysics, Department of Pharmaceutical Chemistry, Helen Diller Family Comprehensive Cancer Center, University of California, San Francisco, San Francisco, California 94158, USA.
Cancer Res. 2010 Feb 15;70(4):1505-12. doi: 10.1158/0008-5472.CAN-09-1640. Epub 2010 Feb 9.
The cell surface protease membrane-type serine protease-1 (MT-SP1), also known as matriptase, is often upregulated in epithelial cancers. We hypothesized that dysregulation of MT-SP1 with regard to its cognate inhibitor hepatocyte growth factor activator inhibitor-1 (HAI-1), a situation that increases proteolytic activity, might be exploited for imaging purposes to differentiate malignant from normal tissue. In this study, we show that MT-SP1 is active on cancer cells and that its activity may be targeted in vivo for tumor detection. A proteolytic activity assay with several MT-SP1-positive human cancer cell lines showed that MT-SP1 antibodies that inhibit recombinant enzyme activity in vitro also bind and inhibit the full-length enzyme expressed on cells. In contrast, in the same assay, MT-SP1-negative cancer cell lines were inactive. Fluorescence microscopy confirmed the cell surface localization of labeled antibodies bound to MT-SP1-positive cells. To evaluate in vivo targeting capability, 0.7 to 2 nmoles of fluorescently labeled antibodies were administered to mice bearing tumors that were positive or negative for MT-SP1. Antibodies localized to MT-SP1-positive tumors (n = 3), permitting visualization of MT-SP1 activity, whereas MT-SP1-negative tumors (n = 2) were not visualized. Our findings define MT-SP1 activity as a useful biomarker to visualize epithelial cancers using a noninvasive antibody-based method.
细胞表面蛋白酶膜型丝氨酸蛋白酶-1(MT-SP1),也称为组织蛋白酶 G2,在多种上皮性肿瘤中过表达。我们假设 MT-SP1 与其同源抑制剂肝配蛋白激活素抑制剂-1(HAI-1)的失调,即增加蛋白水解活性的情况,可被用于成像目的以区分恶性和正常组织。在这项研究中,我们证明 MT-SP1 在癌细胞上具有活性,并且其活性可以在体内被靶向用于肿瘤检测。用几种 MT-SP1 阳性的人癌细胞系进行的蛋白水解活性测定表明,体外抑制重组酶活性的 MT-SP1 抗体也结合并抑制在细胞上表达的全长酶。相比之下,在相同的测定中,MT-SP1 阴性的癌细胞系没有活性。荧光显微镜证实了标记的抗体与 MT-SP1 阳性细胞结合的细胞表面定位。为了评估体内靶向能力,将 0.7 至 2 毫摩尔的荧光标记抗体施用于 MT-SP1 阳性或阴性的荷瘤小鼠。抗体定位于 MT-SP1 阳性肿瘤(n = 3),允许可视化 MT-SP1 活性,而 MT-SP1 阴性肿瘤(n = 2)则无法可视化。我们的发现将 MT-SP1 活性定义为使用非侵入性抗体方法可视化上皮性癌症的有用生物标志物。