| 抗大肠癌噬菌体人单链抗体的初步鉴定及序列分析 |
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| 引用本文: | 朱建高,胡锦跃,李官成,李跃辉,周国华,孙去病,李小玲.抗大肠癌噬菌体人单链抗体的初步鉴定及序列分析[J].中南大学学报(医学版),2002,27(2):95-98. |
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| 作者姓名: | 朱建高 胡锦跃 李官成 李跃辉 周国华 孙去病 李小玲 |
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| 作者单位: | 中南大学湘雅医学院肿瘤研究所,长沙,410078 |
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| 基金项目: | 国家自然科学基金资助项目 (3 990 0 14 1) |
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| 摘 要: | 目的 :对抗大肠癌细胞的单克隆噬菌体单链抗体进行初步鉴定和测序分析。方法 :采用细胞ELISA ,免疫组化 ,DNA序列测定和计算机分析方法 ,对 5个单克隆噬菌体抗体 (CH2 73,CH2 0 5 ,CH2 0 9,CHA12 ,CH72 3)进行初步鉴定和序列分析。结果 :5个抗体均对人大肠癌细胞、人胚肾上皮细胞和其它某些人肿瘤细胞反应 ,也与人正常肝细胞有弱阳性反应 ,但不与鼠源性的癌细胞和正常细胞反应。细胞免疫组化进一步证实了ELISA结果的正确性。大肠癌免疫组化对大肠癌组织有特异性的结合反应 ,而不与正常大肠组织反应。测序结果为CH2 73ScFv全长 732bp ;V ,D ,J分别属于VH3 30 D1 2 6 JH3 linker V1 13 JL2 ,GenBank序号为AY0 2 8777和AY0 2 8996 ;CH2 0 5全长 36 6bp ,V ,D ,J分别VH1 4 6 D6 13 JH3,GenBank序号为AF35 936 5 ;CH2 0 9,CHA12和CH72 3的ScFv基因完全相同 ,全长 72 3bp ,其VH DH JH与CH2 73ScFv基因中的VH DH JH 完全一致 ,V ,D ,J分别属于VH3 30 D1 2 6 JH3 linker L2 Jκ2 ,GenBank序号为AF36 3774。结论 :噬菌体抗体具有结合人大肠癌组织和细胞的活性 ,为进一步开发临床应用人源抗肿瘤抗体和小分子抗体片段奠定基础
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| 关 键 词: | 结肠肿瘤 癌 免疫组化 噬菌体抗体 单链抗体 免疫球蛋白可变区基因 序列分析 |
| 文章编号: | 1000-5625(2002)02-0095-04 |
| 修稿时间: | 2001年10月10 |
Primary characterization and sequence analysis of anti-colorectal cancer phage fusion antibodies |
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| ZHU Jian gao,Hu Jin yue,LI Guan cheng,et al..Primary characterization and sequence analysis of anti-colorectal cancer phage fusion antibodies[J].Journal of Central South University (Medical Sciences)Journal of Central South University (Medical Sciences),2002,27(2):95-98. |
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| Authors: | ZHU Jian gao Hu Jin yue LI Guan cheng |
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| Affiliation: | (Cancer Research Institute, Xiangya School of Medicine,Central South University, Changsha, 410078,China) |
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| Abstract: | Objective To identify 5 phage fusion antibodies against colorectal cancer from in vitro immunized phage library and analyze their sequences. Methods Cell ELISA, immunohistochemistry, DNA sequencing and computer analysis were employed. Results Five clones of phage antibodies were tested by cell ELISA, and all of them reacted to human colorectal cancer cell lines, human embryo kidney endothelial cell line and some tumor cell lines, but not to mouse original cell lines. They also reacted weakly to human hepatic cell lines. The binding specificity of the phage antibodies for colorectal cancer cells was confirmed by immunohistochemistry with cultured cells and colorectal carcinoma and colon tissue sections. They reacted to colorectal carcinoma cell lines, human embryo kidney endothelial cell lines and nasopharyngeal carcinoma cell lines. CH273 reacted specifically to colorectal cancer cells in human colorectal carcinoma sections but not to any of the cells in human colon sections. The 5 clones were further analyzed after their DNA sequencing. The sequences of CH723, CH209 and CHA12 were identical. The lengths of CH273, CH205 and CH723 were 732bp, 366bp and 723bp, respectively. The VDJ regions of CH273, CH205 and CH723 belonged to V H3 30 D1 26 J H3 linker V1 13 J L2,V H1 46 D6 13 J H3 and V H3 30 D1 26 J H3 linker L2 Jκ2,respectively. Conclusion Phage antibodies’ binding to colorectal tissues and cells are confirmed, on which human anti tumor ScFv and V H fragments may be further developed and applied to clinical therapy. |
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| Keywords: | colonic neoplasms carcinoma immunohistochemistry phage antibody single chain antibody variable region of immunoglobulin gene sequence analysis |
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