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用于放射免疫治疗的人源化A33免疫缀合物的制备及临床前评估。

Preparation and preclinical evaluation of humanised A33 immunoconjugates for radioimmunotherapy.

作者信息

King D J, Antoniw P, Owens R J, Adair J R, Haines A M, Farnsworth A P, Finney H, Lawson A D, Lyons A, Baker T S

机构信息

Celltech Therapeutics Ltd., Slough, UK.

出版信息

Br J Cancer. 1995 Dec;72(6):1364-72. doi: 10.1038/bjc.1995.516.

DOI:10.1038/bjc.1995.516
PMID:8519646
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC2034099/
Abstract

A humanised IgG1/k version of A33 (hA33) has been constructed and expressed with yields up to 700 mg l-1 in mouse myeloma NS0 cells in suspension culture. The equilibrium dissociation constant of hA33 (KD = 1.3 nM) was shown to be equivalent to that of the murine antibody in a cell-binding assay. hA33 labelled with yttrium-90 using the macrocyclic chelator 12N4 (DOTA) was shown to localise very effectively to human colon tumour xenografts in nude mice, with tumour levels increasing as blood concentration fell up to 144 h. A Fab' variant of hA33 with a single hinge thiol group to facilitate chemical cross-linking has also been constructed and expressed with yields of 500 mg l-1. Trimaleimide cross-linkers have been used to produce a trivalent Fab fragment (hA33 TFM) that binds antigen on tumour cells with greater avidity than hA33 IgG. Cross-linkers incorporating 12N4 or 9N3 macrocycles have been used to produce hA33 TFM labelled stably and site specifically with yttrium-90 or indium-111 respectively. These molecules have been used to demonstrate that hA33 TFM is cleared more rapidly than hA33 IgG from the circulation of animals but does not lead to accumulation of these metallic radionuclides in the kidney. 90Y-labelled hA33 TFM therefore appears to be the optimal form of the antibody for radioimmunotherapy of colorectal carcinoma.

摘要

已构建出A33的人源化IgG1/k版本(hA33),并在悬浮培养的小鼠骨髓瘤NS0细胞中表达,产量高达700 mg l-1。在细胞结合试验中,hA33的平衡解离常数(KD = 1.3 nM)显示与鼠源抗体相当。使用大环螯合剂12N4(DOTA)用钇-90标记的hA33在裸鼠体内对人结肠肿瘤异种移植瘤的定位非常有效,在长达144小时内,随着血液浓度下降,肿瘤部位的含量增加。还构建并表达了具有单个铰链巯基以促进化学交联的hA33 Fab'变体,产量为500 mg l-1。三马来酰亚胺交联剂已用于产生三价Fab片段(hA33 TFM),其与肿瘤细胞上抗原的结合亲和力高于hA33 IgG。已使用包含12N4或9N3大环的交联剂分别产生稳定且位点特异性地用钇-90或铟-111标记的hA33 TFM。这些分子已用于证明hA33 TFM在动物循环中的清除速度比hA33 IgG快,但不会导致这些金属放射性核素在肾脏中积累。因此,90Y标记的hA33 TFM似乎是用于结直肠癌放射免疫治疗的最佳抗体形式。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/d9cd/2034099/539bd5030638/brjcancer00046-0033-a.jpg
https://cdn.ncbi.nlm.nih.gov/pmc/blobs/d9cd/2034099/539bd5030638/brjcancer00046-0033-a.jpg
https://cdn.ncbi.nlm.nih.gov/pmc/blobs/d9cd/2034099/539bd5030638/brjcancer00046-0033-a.jpg

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