A humanized anti-VEGF rabbit monoclonal antibody inhibits angiogenesis and blocks tumor growth in xenograft models.
Rabbit antibodies have been widely used in research and diagnostics due to their high antigen specificity and affinity. Though these properties are also highly desirable for therapeutic applications, rabbit antibodies have remained untapped for human disease therapy. To evaluate the therapeutic pote...
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doaj-a08caa0a35da47ffa0d39785909958992020-11-25T02:03:30ZengPublic Library of Science (PLoS)PLoS ONE1932-62032010-01-0152e907210.1371/journal.pone.0009072A humanized anti-VEGF rabbit monoclonal antibody inhibits angiogenesis and blocks tumor growth in xenograft models.Yanlan YuPierre LeeYaohuang KeYongke ZhangQiu YuJonathan LeeMingzhen LiJialiang SongJungang ChenJihong DaiFernando Jose Rebelo Do CoutoZhiqiang AnWeimin ZhuGuo-Liang YuRabbit antibodies have been widely used in research and diagnostics due to their high antigen specificity and affinity. Though these properties are also highly desirable for therapeutic applications, rabbit antibodies have remained untapped for human disease therapy. To evaluate the therapeutic potential of rabbit monoclonal antibodies (RabMAbs), we generated a panel of neutralizing RabMAbs against human vascular endothelial growth factor-A (VEGF). These neutralizing RabMAbs are specific to VEGF and do not cross-react to other members of the VEGF protein family. Guided by sequence and lineage analysis of a panel of neutralizing RabMAbs, we humanized the lead candidate by substituting non-critical residues with human residues within both the frameworks and the CDR regions. We showed that the humanized RabMAb retained its parental biological properties and showed potent inhibition of the growth of H460 lung carcinoma and A673 rhabdomyosarcoma xenografts in mice. These studies provide proof of principle for the feasibility of developing humanized RabMAbs as therapeutics.http://europepmc.org/articles/PMC2816707?pdf=render |
collection |
DOAJ |
language |
English |
format |
Article |
sources |
DOAJ |
author |
Yanlan Yu Pierre Lee Yaohuang Ke Yongke Zhang Qiu Yu Jonathan Lee Mingzhen Li Jialiang Song Jungang Chen Jihong Dai Fernando Jose Rebelo Do Couto Zhiqiang An Weimin Zhu Guo-Liang Yu |
spellingShingle |
Yanlan Yu Pierre Lee Yaohuang Ke Yongke Zhang Qiu Yu Jonathan Lee Mingzhen Li Jialiang Song Jungang Chen Jihong Dai Fernando Jose Rebelo Do Couto Zhiqiang An Weimin Zhu Guo-Liang Yu A humanized anti-VEGF rabbit monoclonal antibody inhibits angiogenesis and blocks tumor growth in xenograft models. PLoS ONE |
author_facet |
Yanlan Yu Pierre Lee Yaohuang Ke Yongke Zhang Qiu Yu Jonathan Lee Mingzhen Li Jialiang Song Jungang Chen Jihong Dai Fernando Jose Rebelo Do Couto Zhiqiang An Weimin Zhu Guo-Liang Yu |
author_sort |
Yanlan Yu |
title |
A humanized anti-VEGF rabbit monoclonal antibody inhibits angiogenesis and blocks tumor growth in xenograft models. |
title_short |
A humanized anti-VEGF rabbit monoclonal antibody inhibits angiogenesis and blocks tumor growth in xenograft models. |
title_full |
A humanized anti-VEGF rabbit monoclonal antibody inhibits angiogenesis and blocks tumor growth in xenograft models. |
title_fullStr |
A humanized anti-VEGF rabbit monoclonal antibody inhibits angiogenesis and blocks tumor growth in xenograft models. |
title_full_unstemmed |
A humanized anti-VEGF rabbit monoclonal antibody inhibits angiogenesis and blocks tumor growth in xenograft models. |
title_sort |
humanized anti-vegf rabbit monoclonal antibody inhibits angiogenesis and blocks tumor growth in xenograft models. |
publisher |
Public Library of Science (PLoS) |
series |
PLoS ONE |
issn |
1932-6203 |
publishDate |
2010-01-01 |
description |
Rabbit antibodies have been widely used in research and diagnostics due to their high antigen specificity and affinity. Though these properties are also highly desirable for therapeutic applications, rabbit antibodies have remained untapped for human disease therapy. To evaluate the therapeutic potential of rabbit monoclonal antibodies (RabMAbs), we generated a panel of neutralizing RabMAbs against human vascular endothelial growth factor-A (VEGF). These neutralizing RabMAbs are specific to VEGF and do not cross-react to other members of the VEGF protein family. Guided by sequence and lineage analysis of a panel of neutralizing RabMAbs, we humanized the lead candidate by substituting non-critical residues with human residues within both the frameworks and the CDR regions. We showed that the humanized RabMAb retained its parental biological properties and showed potent inhibition of the growth of H460 lung carcinoma and A673 rhabdomyosarcoma xenografts in mice. These studies provide proof of principle for the feasibility of developing humanized RabMAbs as therapeutics. |
url |
http://europepmc.org/articles/PMC2816707?pdf=render |
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