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荚膜多糖特异性IgM和IgG抗体以及F(ab')2和Fab片段作为真菌感染放射免疫治疗递送载体的比较评估。

Comparative evaluation of capsular polysaccharide-specific IgM and IgG antibodies and F(ab')2 and Fab fragments as delivery vehicles for radioimmunotherapy of fungal infection.

作者信息

Dadachova Ekaterina, Bryan Ruth A, Huang Xianchun, Ortiz Geraldina, Moadel Tiffany, Casadevall Arturo

机构信息

Department of Nuclear Medicine, Albert Einstein College of Medicine, Bronx, New York 10461, USA.

出版信息

Clin Cancer Res. 2007 Sep 15;13(18 Pt 2):5629s-5635s. doi: 10.1158/1078-0432.CCR-07-0870.

Abstract

PURPOSE

The applicability of radioimmunotherapy with organism-specific monoclonal antibodies to treatment of infectious disease in experimental models has been recently shown for fungal, bacterial, and viral infections. To identify the best delivery vehicle for radioimmunotherapy of human pathogenic fungus Cryptococcus neoformans (CN), we have done comparative evaluation of capsular polysaccharide-specific antibodies with IgG1 and IgM isotypes and F(ab')2 and Fab fragments.

EXPERIMENTAL DESIGN

18B7 IgG1 and 13F1 IgM and their isotype-matching controls were radiolabeled with 188Re, and their binding to 24067 and H99 CN strains was evaluated by doing Scatchard and kinetics analyses. The doses delivered during in vitro radioimmunotherapy were estimated using a cellular dosimetry algorithm. The biodistribution of 188Re-labeled 18B7 and 13F1 and of 111In-labeled 18B7 and its F(ab')2 and Fab fragments was done in A/JCr mice systemically infected with 24067 CN strain.

RESULTS

18B7 IgG1 showed superior to 13F1 IgM binding to 24067 CN (Ka=1.7x10(9) mol/L(-1) and 5.4x10(7) mol/L(-1), respectively). Substantial killing of 24067 and H99 CN cells was achieved with 1 microCi 188Re-18B7 (55 cGy dose), whereas no killing was observed for 1 microCi 188Re-13F1 (2 cGy dose). In vivo 188Re-18B7 localized specifically in the lungs of CN-infected mice, whereas uptake of 188Re-13F1 was nonspecific. 111In-F(ab')2 fragments showed higher uptake in the lungs and lower in the liver at the 48-h time point in comparison with intact 111In-18B7.

CONCLUSIONS

Comparative evaluation of IgG and IgM and of F(ab')2 and Fab fragments as potential delivery vehicles for radioimmunotherapy of cryptococcal infection strongly suggests that affinity for the target antigen is an important prerequisite for successful targeting of infection in vivo and that in vitro affinity measurements may predict the in vivo efficacy of candidate monoclonal antibodies.

摘要

目的

近期已证明,在实验模型中,使用机体特异性单克隆抗体进行放射免疫疗法可用于治疗真菌、细菌和病毒感染性疾病。为确定用于人类致病真菌新型隐球菌(CN)放射免疫疗法的最佳递送载体,我们对具有IgG1和IgM同种型以及F(ab')2和Fab片段的荚膜多糖特异性抗体进行了比较评估。

实验设计

用188Re对18B7 IgG1和13F1 IgM及其同种型匹配对照进行放射性标记,并通过Scatchard分析和动力学分析评估它们与24067和H99 CN菌株的结合情况。使用细胞剂量测定算法估算体外放射免疫疗法期间递送的剂量。在全身感染24067 CN菌株的A/JCr小鼠中进行188Re标记的18B7和13F1以及111In标记的18B7及其F(ab')2和Fab片段的生物分布研究。

结果

18B7 IgG1与24067 CN的结合优于13F1 IgM(Ka分别为1.7×10(9) mol/L(-1)和5.4×10(7) mol/L(-1))。1微居里188Re-18B7(55 cGy剂量)可对24067和H99 CN细胞实现显著杀伤,而1微居里188Re-13F1(2 cGy剂量)未观察到杀伤作用。体内188Re-18B7特异性定位于CN感染小鼠的肺部,而188Re-13F1的摄取是非特异性摄取。与完整的111In-18B7相比,111In-F(ab')2片段在48小时时间点时在肺部的摄取较高,在肝脏中的摄取较低。

结论

对IgG和IgM以及F(ab')2和Fab片段作为隐球菌感染放射免疫疗法潜在递送载体的比较评估强烈表明,对靶抗原的亲和力是体内成功靶向感染的重要前提条件,并且体外亲和力测量可能预测候选单克隆抗体的体内疗效。

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