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Humanization and directed evolution of the selenium-containing scFv phage abzyme

According to the binding site structure and the catalytic mechanism of the native glutathione peroxidase (GPX), three glutathione derivatives, GSH-S-DNP butyl ester (hapten Be), GSH-S-DNP hexyl ester (hapten He) and GSH-S-DNP hexamethylene ester (hapten Hme) were synthesized. By a four-round panning...

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Autores principales: Xu, Yan, Li, Pengju, Nie, Jiaojiao, Zhao, Qi, Guan, Shanshan, Kuai, Ziyu, Qiao, Yongbo, Jiang, Xiaoyu, Li, Ying, Li, Wei, Shi, Yuhua, Kong, Wei, Shan, Yaming
Formato: Online Artículo Texto
Lenguaje:English
Publicado: The Royal Society of Chemistry 2018
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9080455/
https://www.ncbi.nlm.nih.gov/pubmed/35539266
http://dx.doi.org/10.1039/c8ra02798f
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author Xu, Yan
Li, Pengju
Nie, Jiaojiao
Zhao, Qi
Guan, Shanshan
Kuai, Ziyu
Qiao, Yongbo
Jiang, Xiaoyu
Li, Ying
Li, Wei
Shi, Yuhua
Kong, Wei
Shan, Yaming
author_facet Xu, Yan
Li, Pengju
Nie, Jiaojiao
Zhao, Qi
Guan, Shanshan
Kuai, Ziyu
Qiao, Yongbo
Jiang, Xiaoyu
Li, Ying
Li, Wei
Shi, Yuhua
Kong, Wei
Shan, Yaming
author_sort Xu, Yan
collection PubMed
description According to the binding site structure and the catalytic mechanism of the native glutathione peroxidase (GPX), three glutathione derivatives, GSH-S-DNP butyl ester (hapten Be), GSH-S-DNP hexyl ester (hapten He) and GSH-S-DNP hexamethylene ester (hapten Hme) were synthesized. By a four-round panning with a human synthetic scFv phage library against three haptens, the enrichment of the scFv phage particles with specific binding activity could be determined. Three phage particles were selected binding to each glutathione derivative, respectively. After a two-step chemical mutation to convert the serine residues of the scFv phage particles into selenocysteine residues, GPX activity could be observed and determined upto 3000 U μmol(−1) in the selenium-containing scFv phage abzyme which was isolated by affinity capture against the hapten Be. Also the scFv phage abzymes elicited by different antigens displayed different catalytic activities. After a directed evolution by DNA shuffling to improve the affinity to the hapten Be, a secondary library with GPX activity was created in which the catalytic activity of the selenium-containing scFv phage abzyme could be increased 17%. This study might be helpful for new haptens or antigens design to optimize the abzymes with high binding activities and might also provide a novel scheme for GPX mimic candidates for drug development.
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spelling pubmed-90804552022-05-09 Humanization and directed evolution of the selenium-containing scFv phage abzyme Xu, Yan Li, Pengju Nie, Jiaojiao Zhao, Qi Guan, Shanshan Kuai, Ziyu Qiao, Yongbo Jiang, Xiaoyu Li, Ying Li, Wei Shi, Yuhua Kong, Wei Shan, Yaming RSC Adv Chemistry According to the binding site structure and the catalytic mechanism of the native glutathione peroxidase (GPX), three glutathione derivatives, GSH-S-DNP butyl ester (hapten Be), GSH-S-DNP hexyl ester (hapten He) and GSH-S-DNP hexamethylene ester (hapten Hme) were synthesized. By a four-round panning with a human synthetic scFv phage library against three haptens, the enrichment of the scFv phage particles with specific binding activity could be determined. Three phage particles were selected binding to each glutathione derivative, respectively. After a two-step chemical mutation to convert the serine residues of the scFv phage particles into selenocysteine residues, GPX activity could be observed and determined upto 3000 U μmol(−1) in the selenium-containing scFv phage abzyme which was isolated by affinity capture against the hapten Be. Also the scFv phage abzymes elicited by different antigens displayed different catalytic activities. After a directed evolution by DNA shuffling to improve the affinity to the hapten Be, a secondary library with GPX activity was created in which the catalytic activity of the selenium-containing scFv phage abzyme could be increased 17%. This study might be helpful for new haptens or antigens design to optimize the abzymes with high binding activities and might also provide a novel scheme for GPX mimic candidates for drug development. The Royal Society of Chemistry 2018-05-10 /pmc/articles/PMC9080455/ /pubmed/35539266 http://dx.doi.org/10.1039/c8ra02798f Text en This journal is © The Royal Society of Chemistry https://creativecommons.org/licenses/by/3.0/
spellingShingle Chemistry
Xu, Yan
Li, Pengju
Nie, Jiaojiao
Zhao, Qi
Guan, Shanshan
Kuai, Ziyu
Qiao, Yongbo
Jiang, Xiaoyu
Li, Ying
Li, Wei
Shi, Yuhua
Kong, Wei
Shan, Yaming
Humanization and directed evolution of the selenium-containing scFv phage abzyme
title Humanization and directed evolution of the selenium-containing scFv phage abzyme
title_full Humanization and directed evolution of the selenium-containing scFv phage abzyme
title_fullStr Humanization and directed evolution of the selenium-containing scFv phage abzyme
title_full_unstemmed Humanization and directed evolution of the selenium-containing scFv phage abzyme
title_short Humanization and directed evolution of the selenium-containing scFv phage abzyme
title_sort humanization and directed evolution of the selenium-containing scfv phage abzyme
topic Chemistry
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9080455/
https://www.ncbi.nlm.nih.gov/pubmed/35539266
http://dx.doi.org/10.1039/c8ra02798f
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