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2
Humanized monoclonal antibody against parathyroid hormone-related protein suppresses osteolytic bone metastasis of human breast cancer cells derived from MDA-MB-231.抗甲状旁腺激素相关蛋白的人源化单克隆抗体可抑制源自MDA-MB-231的人乳腺癌细胞的溶骨性骨转移。
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C-reactive protein binds to integrin α2 and Fcγ receptor I, leading to breast cell adhesion and breast cancer progression.C-反应蛋白与整合素 α2 和 Fcγ 受体 I 结合,导致乳腺细胞黏附并促进乳腺癌进展。
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Breast cancer cells expressing cancer-associated sialyl-Tn antigen have less capacity to develop osteolytic lesions in a mouse model of skeletal colonization.表达癌相关唾液酸化-Tn 抗原的乳腺癌细胞在骨骼定植的小鼠模型中形成溶骨性病变的能力较低。
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Anti-CD26 monoclonal antibody-mediated G1-S arrest of human renal clear cell carcinoma Caki-2 is associated with retinoblastoma substrate dephosphorylation, cyclin-dependent kinase 2 reduction, p27(kip1) enhancement, and disruption of binding to the extracellular matrix.抗CD26单克隆抗体介导的人肾透明细胞癌Caki-2细胞G1期到S期的阻滞与视网膜母细胞瘤底物去磷酸化、细胞周期蛋白依赖性激酶2减少、p27(kip1)增强以及与细胞外基质结合的破坏有关。
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Antiangiogenic therapy of established tumors in human skin/severe combined immunodeficiency mouse chimeras by anti-endoglin (CD105) monoclonal antibodies, and synergy between anti-endoglin antibody and cyclophosphamide.通过抗内皮糖蛋白(CD105)单克隆抗体对人皮肤/严重联合免疫缺陷小鼠嵌合体中已形成肿瘤进行抗血管生成治疗,以及抗内皮糖蛋白抗体与环磷酰胺之间的协同作用。
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Integrin α2β1 inhibits MST1 kinase phosphorylation and activates Yes-associated protein oncogenic signaling in hepatocellular carcinoma.整合素α2β1抑制MST1激酶磷酸化并激活肝细胞癌中Yes相关蛋白致癌信号通路。
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本文引用的文献

1
Extracellular matrix signatures of human primary metastatic colon cancers and their metastases to liver.人类原发性转移性结肠癌及其肝转移灶的细胞外基质特征
BMC Cancer. 2014 Jul 18;14:518. doi: 10.1186/1471-2407-14-518.
2
Small Macrocycles As Highly Active Integrin α2β1 Antagonists.作为高活性整合素α2β1拮抗剂的小分子大环化合物
ACS Med Chem Lett. 2014 Jan 10;5(2):193-8. doi: 10.1021/ml4004556. eCollection 2014 Feb 13.
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Extracellular matrix signatures of human mammary carcinoma identify novel metastasis promoters.人类乳腺癌的细胞外基质特征鉴定出新的转移促进因子。
Elife. 2014 Mar 11;3:e01308. doi: 10.7554/eLife.01308.
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Collective invasion in breast cancer requires a conserved basal epithelial program.乳腺癌的群体侵袭需要一个保守的基底上皮程序。
Cell. 2013 Dec 19;155(7):1639-51. doi: 10.1016/j.cell.2013.11.029. Epub 2013 Dec 12.
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Human bone marrow mesenchymal stem cells induce collagen production and tongue cancer invasion.人骨髓间充质干细胞诱导胶原产生和舌癌侵袭。
PLoS One. 2013 Oct 21;8(10):e77692. doi: 10.1371/journal.pone.0077692. eCollection 2013.
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Antibody therapeutics in cancer.癌症的抗体治疗。
Science. 2013 Sep 13;341(6151):1192-8. doi: 10.1126/science.1241145.
7
Lung cancer cells that survive ionizing radiation show increased integrin α2β1- and EGFR-dependent invasiveness.存活于电离辐射下的肺癌细胞表现出增强的整合素α2β1 和 EGFR 依赖性侵袭性。
PLoS One. 2013 Aug 8;8(8):e70905. doi: 10.1371/journal.pone.0070905. eCollection 2013.
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Extracellular matrix determinants and the regulation of cancer cell invasion stratagems.细胞外基质决定因子与癌细胞侵袭策略的调控。
J Microsc. 2013 Sep;251(3):250-60. doi: 10.1111/jmi.12064.
9
MT1-MMP-dependent control of skeletal stem cell commitment via a β1-integrin/YAP/TAZ signaling axis.MT1-MMP 依赖性调控β1 整合素/YAP/TAZ 信号轴控制骨骼干细胞的定向分化。
Dev Cell. 2013 May 28;25(4):402-16. doi: 10.1016/j.devcel.2013.04.011. Epub 2013 May 16.
10
Combining phenotypic and proteomic approaches to identify membrane targets in a 'triple negative' breast cancer cell type.采用表型和蛋白质组学方法鉴定“三阴性”乳腺癌细胞类型中的膜靶标。
Mol Cancer. 2013 Feb 13;12:11. doi: 10.1186/1476-4598-12-11.

一种用于快速生成治疗性抗人癌单克隆抗体的3D基质平台。

A 3D matrix platform for the rapid generation of therapeutic anti-human carcinoma monoclonal antibodies.

作者信息

Dudley David T, Li Xiao-Yan, Hu Casey Y, Kleer Celina G, Willis Amanda L, Weiss Stephen J

机构信息

Division of Molecular Medicine and Genetics, Department of Internal Medicine, Life Sciences Institute, and.

Department of Pathology, University of Michigan, Ann Arbor, MI 48109.

出版信息

Proc Natl Acad Sci U S A. 2014 Oct 14;111(41):14882-7. doi: 10.1073/pnas.1410996111. Epub 2014 Sep 29.

DOI:10.1073/pnas.1410996111
PMID:25267635
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC4205646/
Abstract

Efforts to develop unbiased screens for identifying novel function-blocking monoclonal antibodies (mAbs) in human carcinomatous states have been hampered by the limited ability to design in vitro models that recapitulate tumor cell behavior in vivo. Given that only invasive carcinoma cells gain permanent access to type I collagen-rich interstitial tissues, an experimental platform was established in which human breast cancer cells were embedded in 3D aldimine cross-linked collagen matrices and used as an immunogen to generate mAb libraries. In turn, cancer-cell-reactive antibodies were screened for their ability to block carcinoma cell proliferation within collagen hydrogels that mimic the in vivo environment. As a proof of principle, a single function-blocking mAb out of 15 identified was selected for further analysis and found to be capable of halting carcinoma cell proliferation, inducing apoptosis, and exerting global changes in gene expression in vitro. The ability of this mAb to block carcinoma cell proliferation and metastatic activity was confirmed in vivo, and the target antigen was identified by mass spectroscopy as the α2 subunit of the α2β1 integrin, one of the major type I collagen-binding receptors in mammalian cells. Validating the ability of the in vitro model to predict patterns of antigen expression in the disease setting, immunohistochemical analyses of tissues from patients with breast cancer verified markedly increased expression of the α2 subunit in vivo. These results not only highlight the utility of this discovery platform for rapidly selecting and characterizing function-blocking, anticancer mAbs in an unbiased fashion, but also identify α2β1 as a potential target in human carcinomatous states.

摘要

在人类癌状态下开发无偏倚筛选方法以鉴定新型功能阻断单克隆抗体(mAb)的努力,因设计能够在体内重现肿瘤细胞行为的体外模型的能力有限而受到阻碍。鉴于只有侵袭性癌细胞才能永久进入富含I型胶原蛋白的间质组织,因此建立了一个实验平台,将人乳腺癌细胞嵌入3D醛亚胺交联胶原蛋白基质中,并用作免疫原以生成mAb文库。反过来,筛选与癌细胞反应的抗体,以检测其在模拟体内环境的胶原蛋白水凝胶中阻断癌细胞增殖的能力。作为原理验证,从鉴定出的15种抗体中选择了一种单一的功能阻断mAb进行进一步分析,发现其能够在体外阻止癌细胞增殖、诱导细胞凋亡并引起基因表达的整体变化。该mAb阻断癌细胞增殖和转移活性的能力在体内得到证实,并且通过质谱鉴定靶抗原为α2β1整合素的α2亚基,α2β1整合素是哺乳动物细胞中主要的I型胶原蛋白结合受体之一。对乳腺癌患者组织进行免疫组织化学分析,验证了体外模型预测疾病环境中抗原表达模式的能力,结果显示体内α2亚基的表达明显增加。这些结果不仅突出了该发现平台在以无偏倚方式快速选择和表征功能阻断性抗癌mAb方面的实用性,还将α2β1确定为人类癌状态下的潜在靶点。