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首页> 美国卫生研究院文献>British Journal of Cancer >Comparison of the pharmacokinetics biodistribution and dosimetry of monoclonal antibodies OC125 OV-TL 3 and 139H2 as IgG and F(ab)2 fragments in experimental ovarian cancer.
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Comparison of the pharmacokinetics biodistribution and dosimetry of monoclonal antibodies OC125 OV-TL 3 and 139H2 as IgG and F(ab)2 fragments in experimental ovarian cancer.

机译:单克隆抗体OC125OV-TL 3和139H2作为IgG和F(ab)2片段在实验性卵巢癌中的药代动力学生物分布和剂量测定的比较。

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Monoclonal antibody (MAb) 139H2 was previously shown to localise specifically into ovarian cancer xenografts in nude mice. MAb 139H2 was compared with MAbs OC125 and OV-TL 3, all reactive with ovarian carcinomas, for the binding characteristics as IgG and F(ab')2 fragments with the use of the OVCAR-3 cell line grown in vitro and as s.c. xenografts. Immunoperoxidase staining of OVCAR-3 tissue sections with MAbs OC125 and 139H2 was heterogeneous, whereas MAb OV-TL 3 showed homogeneity. No differences in binding were observed between IgG and F(ab')2. The avidity expressed as apparent affinity constants of MAbs OC125, OV-TL 3 and 139H2 for OVAR-3 cells were 1 x 10(9) M-1, 1 x 10(9) M-1, and 1 x 10(8) M-1, while the number of antigenic determinants were 5 x 10(6), 1 x 10(6) and 7 x 10(6), respectively. In OVCAR-3 bearing nude mice the blood half-lives of the MAbs as IgG and F(ab')2 were approximately 50 h and 6 h, respectively. Maximum tumour uptake for the whole MAbs OC125, OV-TL 3, 139H2 and a control MAb 2C7 was 8.5%, 17.7%, 11.1% and 2.5% of the injected dose g-1, reached at 72 h after injection. For the respective F(ab')2 fragments, the maximum values were 5.2%, 10.0%, 5.5% and 1.9% of the injected dose g-1, reached between 6 h and 15 h. Tumour to non-tumour ratios were more favourable for the F(ab')2 fragments as compared to those for MAbs as IgG. Biodistribution in mice bearing a control tumour confirmed the specificity of tumour localisation of MAbs OC125, OV-TL 3 and 139H2. After injection of a tracer dose of 10 microCi of radiolabelled MAbs OC125, OV-TL 3 and 139H2 as IgG, tumours received 38 cGy, and 9 cGy. In our OVCAR-3 model, a ranking in efficiency in tumour localisation would indicate MAb OV-TL 3 as most favourable MAb, but cross-reactivity with subpopulations of human white blood cells might hamper its clinical use. Dosimetric data indicate a 4-fold higher radiation absorbed dose to tumours for IgG compared with F(ab')2 fragments.
机译:先前显示单克隆抗体(MAb)139H2在裸鼠体内特异地定位于卵巢癌异种移植物中。使用体外培养的OVCAR-3细胞系,将MAb 139H2与均与卵巢癌具有反应性的MAb OC125和OV-TL 3进行结合,比较其结合特性为IgG和F(ab')2片段。异种移植。单克隆抗体OC125和139H2对OVCAR-3组织切片的免疫过氧化物酶染色是异质的,而单克隆抗体OV-TL 3显示出同质性。在IgG和F(ab')2之间未观察到结合的差异。单克隆抗体OC125,OV-TL 3和139H2对OVAR-3细胞的表观亲和常数表示的亲和力分别为1 x 10(9)M-1、1 x 10(9)M-1和1 x 10(8) M-1,而抗原决定簇的数量分别为5 x 10(6),1 x 10(6)和7 x 10(6)。在携带OVCAR-3的裸鼠中,单克隆抗体IgG和F(ab')2的血液半衰期分别约为50 h和6 h。整个MAb OC125,OV-TL 3、139H2和对照MAb 2C7的最大肿瘤摄取为注射后72小时达到注射剂量g-1的8.5%,17.7%,11.1%和2.5%。对于各自的F(ab')2片段,最大值分别为注射剂量g-1的5.2%,10.0%,5.5%和1.9%,达到6小时至15小时之间。与单克隆抗体IgG相比,F(ab')2片段的肿瘤与非肿瘤比率更有利。在带有对照肿瘤的小鼠中的生物分布证实了单克隆抗体OC125,OV-TL 3和139H2在肿瘤中的定位特异性。在注射示踪剂量的10 microCi放射性标记的单克隆抗体OC125,OV-TL 3和139H2作为IgG后,肿瘤分别获得38 cGy和9 cGy。在我们的OVCAR-3模型中,肿瘤定位效率排名将表明MAb OV-TL 3是最有利的MAb,但与人白细胞亚群的交叉反应性可能会阻碍其临床应用。剂量学数据表明,与F(ab')2片段相比,IgG对肿瘤的辐射吸收剂量高4倍。

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