Lentiviral Transgenic MicroRNA-Based shRNA Suppressed Mouse Cytochromosome P450 3A (CYP3A) Expression in a Dose-Dependent and Inheritable Manner

Cytochomosome P450 enzymes (CYP) are heme-containing monooxygenases responsible for oxidative metabolism of many exogenous and endogenous compounds including drugs. The species difference of CYP limits the extent to which data obtained from animals can be translated to humans in pharmacodynamics or...

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Autores principales: Wang, Yong, Hu, Hai-Hong, Pang, Hao, Zhou, Xiao-Yang, Yu, Lu-Shan, Wang, Lu-Lu, Liu, Cang'e, Guo, Ke-Nan, Zhao, Cong, Liu, Qin, Zeng, Ben-Hua, Tang, Huan, Shang, Hai-Tao, Zeng, Su, Wei, Hong
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2012
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3265487/
https://www.ncbi.nlm.nih.gov/pubmed/22291988
http://dx.doi.org/10.1371/journal.pone.0030560
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author Wang, Yong
Hu, Hai-Hong
Pang, Hao
Zhou, Xiao-Yang
Yu, Lu-Shan
Wang, Lu-Lu
Liu, Cang'e
Guo, Ke-Nan
Zhao, Cong
Liu, Qin
Zeng, Ben-Hua
Tang, Huan
Shang, Hai-Tao
Zeng, Su
Wei, Hong
author_facet Wang, Yong
Hu, Hai-Hong
Pang, Hao
Zhou, Xiao-Yang
Yu, Lu-Shan
Wang, Lu-Lu
Liu, Cang'e
Guo, Ke-Nan
Zhao, Cong
Liu, Qin
Zeng, Ben-Hua
Tang, Huan
Shang, Hai-Tao
Zeng, Su
Wei, Hong
author_sort Wang, Yong
collection PubMed
description Cytochomosome P450 enzymes (CYP) are heme-containing monooxygenases responsible for oxidative metabolism of many exogenous and endogenous compounds including drugs. The species difference of CYP limits the extent to which data obtained from animals can be translated to humans in pharmacodynamics or pharmacokinetics studies. Transgenic expression of human CYP in animals lacking or with largely reduced endogenous CYP counterparts is recognized as an ideal strategy to correct CYP species difference. CYP3A is the most abundant CYP subfamily both in human and mammals. In this study, we designed a microRNA-based shRNA (miR-shRNA) simultaneously targeting four members of mouse CYP3A subfamily (CYP3A11, CYP3A16, CYP3A41 and CYP3A44), and transgenic mice expressing the designed miR-shRNA were generated by lentiviral transgenesis. Results showed that the CYP3A expression level in transgenic mice was markedly reduced compared to that in wild type or unrelated miR-shRNA transgenic mice, and was inversely correlated to the miR-shRNA expression level. The CYP3A expression levels in transgenic offspring of different generations were also remarkably lower compared to those of controls, and moreover the inhibition rate of CYP3A expression remained comparable over generations. The ratio of the targeted CYP3A transcriptional levels was comparable between knockdown and control mice of the same gender as detected by RT-PCR DGGE analysis. These data suggested that transgenic miR-shRNA suppressed CYP3A expression in a dose-dependent and inheritable manner, and transcriptional levels of the targeted CYP3As were suppressed to a similar extent. The observed knockdown efficacy was further confirmed by enzymatic activity analysis, and data showed that CYP3A activities in transgenic mice were markedly reduced compared to those in wild-type or unrelated miR-shRNA transgenic controls (1.11±0.71 vs 5.85±1.74, 5.9±2.4; P<0.01). This work laid down a foundation to further knock down the remaining murine CYP3As or CYPs of other subfamilies, and a basis to generate CYP knockdown animals of other species.
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spelling pubmed-32654872012-01-30 Lentiviral Transgenic MicroRNA-Based shRNA Suppressed Mouse Cytochromosome P450 3A (CYP3A) Expression in a Dose-Dependent and Inheritable Manner Wang, Yong Hu, Hai-Hong Pang, Hao Zhou, Xiao-Yang Yu, Lu-Shan Wang, Lu-Lu Liu, Cang'e Guo, Ke-Nan Zhao, Cong Liu, Qin Zeng, Ben-Hua Tang, Huan Shang, Hai-Tao Zeng, Su Wei, Hong PLoS One Research Article Cytochomosome P450 enzymes (CYP) are heme-containing monooxygenases responsible for oxidative metabolism of many exogenous and endogenous compounds including drugs. The species difference of CYP limits the extent to which data obtained from animals can be translated to humans in pharmacodynamics or pharmacokinetics studies. Transgenic expression of human CYP in animals lacking or with largely reduced endogenous CYP counterparts is recognized as an ideal strategy to correct CYP species difference. CYP3A is the most abundant CYP subfamily both in human and mammals. In this study, we designed a microRNA-based shRNA (miR-shRNA) simultaneously targeting four members of mouse CYP3A subfamily (CYP3A11, CYP3A16, CYP3A41 and CYP3A44), and transgenic mice expressing the designed miR-shRNA were generated by lentiviral transgenesis. Results showed that the CYP3A expression level in transgenic mice was markedly reduced compared to that in wild type or unrelated miR-shRNA transgenic mice, and was inversely correlated to the miR-shRNA expression level. The CYP3A expression levels in transgenic offspring of different generations were also remarkably lower compared to those of controls, and moreover the inhibition rate of CYP3A expression remained comparable over generations. The ratio of the targeted CYP3A transcriptional levels was comparable between knockdown and control mice of the same gender as detected by RT-PCR DGGE analysis. These data suggested that transgenic miR-shRNA suppressed CYP3A expression in a dose-dependent and inheritable manner, and transcriptional levels of the targeted CYP3As were suppressed to a similar extent. The observed knockdown efficacy was further confirmed by enzymatic activity analysis, and data showed that CYP3A activities in transgenic mice were markedly reduced compared to those in wild-type or unrelated miR-shRNA transgenic controls (1.11±0.71 vs 5.85±1.74, 5.9±2.4; P<0.01). This work laid down a foundation to further knock down the remaining murine CYP3As or CYPs of other subfamilies, and a basis to generate CYP knockdown animals of other species. Public Library of Science 2012-01-24 /pmc/articles/PMC3265487/ /pubmed/22291988 http://dx.doi.org/10.1371/journal.pone.0030560 Text en Wang et al. http://creativecommons.org/licenses/by/4.0/ This is an open-access article distributed under the terms of the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are properly credited.
spellingShingle Research Article
Wang, Yong
Hu, Hai-Hong
Pang, Hao
Zhou, Xiao-Yang
Yu, Lu-Shan
Wang, Lu-Lu
Liu, Cang'e
Guo, Ke-Nan
Zhao, Cong
Liu, Qin
Zeng, Ben-Hua
Tang, Huan
Shang, Hai-Tao
Zeng, Su
Wei, Hong
Lentiviral Transgenic MicroRNA-Based shRNA Suppressed Mouse Cytochromosome P450 3A (CYP3A) Expression in a Dose-Dependent and Inheritable Manner
title Lentiviral Transgenic MicroRNA-Based shRNA Suppressed Mouse Cytochromosome P450 3A (CYP3A) Expression in a Dose-Dependent and Inheritable Manner
title_full Lentiviral Transgenic MicroRNA-Based shRNA Suppressed Mouse Cytochromosome P450 3A (CYP3A) Expression in a Dose-Dependent and Inheritable Manner
title_fullStr Lentiviral Transgenic MicroRNA-Based shRNA Suppressed Mouse Cytochromosome P450 3A (CYP3A) Expression in a Dose-Dependent and Inheritable Manner
title_full_unstemmed Lentiviral Transgenic MicroRNA-Based shRNA Suppressed Mouse Cytochromosome P450 3A (CYP3A) Expression in a Dose-Dependent and Inheritable Manner
title_short Lentiviral Transgenic MicroRNA-Based shRNA Suppressed Mouse Cytochromosome P450 3A (CYP3A) Expression in a Dose-Dependent and Inheritable Manner
title_sort lentiviral transgenic microrna-based shrna suppressed mouse cytochromosome p450 3a (cyp3a) expression in a dose-dependent and inheritable manner
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3265487/
https://www.ncbi.nlm.nih.gov/pubmed/22291988
http://dx.doi.org/10.1371/journal.pone.0030560
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