Molecular Immunology Unit, Hospital Universitario Puerta de Hierro Majadahonda, 28222 Madrid, Spain.
J Biol Chem. 2011 Feb 18;286(7):5197-203. doi: 10.1074/jbc.M110.161927. Epub 2010 Dec 14.
Tumor-associated cell surface antigens and tumor-associated vascular markers have been used as a target for cancer intervention strategies. However, both types of targets have limitations due to accessibility, low and/or heterogeneous expression, and presence of tumor-associated serum antigen. It has been previously reported that a mitochondrial/cell surface protein, p32/gC1qR, is the receptor for a tumor-homing peptide, LyP-1, which specifically recognizes an epitope in tumor cells, tumor lymphatics, and tumor-associated macrophages/myeloid cells. Using antibody phage technology, we have generated an anti-p32 human monoclonal antibody (2.15). The 2.15 antibody, expressed in single-chain fragment variable and in trimerbody format, was then characterized in vivo using mice grafted subcutaneously with MDA-MB-231 human breast cancers cells, revealing a highly selective tumor uptake. The intratumoral distribution of the antibody was consistent with the expression pattern of p32 in the surface of some clusters of cells. These results demonstrate the potential of p32 for antibody-based tumor targeting strategies and the utility of the 2.15 antibody as targeting moiety for the selective delivery of imaging and therapeutic agents to tumors.
肿瘤相关细胞表面抗原和肿瘤相关血管标记物已被用作癌症干预策略的靶点。然而,由于可及性、低表达和/或异质性以及肿瘤相关血清抗原的存在,这两种类型的靶点都存在局限性。先前有报道称,线粒体/细胞表面蛋白 p32/gC1qR 是肿瘤归巢肽 LyP-1 的受体,该肽特异性识别肿瘤细胞、肿瘤淋巴管和肿瘤相关巨噬细胞/髓样细胞中的表位。我们使用抗体噬菌体技术生成了抗 p32 的人源单克隆抗体(2.15)。2.15 抗体以单链片段可变形式和三聚体形式表达,然后在皮下接种 MDA-MB-231 人乳腺癌细胞的小鼠中进行体内表征,显示出高度选择性的肿瘤摄取。抗体在肿瘤内的分布与细胞表面某些簇中 p32 的表达模式一致。这些结果表明 p32 具有用于基于抗体的肿瘤靶向策略的潜力,并且 2.15 抗体可用作靶向部分,将成像和治疗剂选择性递送至肿瘤。
