Your search keyword '"He Chengqiang"' showing total 16 results

1. RTCB deficiency triggers colitis in mice by influencing the NF-κB and Wnt/β-catenin signaling pathways

Author

Liu Peiyan, Zhang Ruitao, Song Xiaotong, Tian Xiaohua, Guan Yichao, Li Licheng, He Mei, He Chengqiang, and Ding Naizheng

Subjects

RTCB, colitis, NF-κB, Wnt/β-catenin, LGR5, Biochemistry, QD415-436, Genetics, QH426-470

Abstract

RNA terminal phosphorylase B (RTCB) has been shown to play a significant role in multiple physiological processes. However, the specific role of RTCB in the mouse colon remains unclear. In this study, we employ a conditional knockout mouse model to investigate the effects of RTCB depletion on the colon and the potential molecular mechanisms. We assess the efficiency and phenotype of Rtcb knockout using PCR, western blot analysis, histological staining, and immunohistochemistry. Compared with the control mice, the Rtcb-knockout mice exhibit compromised colonic barrier integrity and prominent inflammatory cell infiltration. In the colonic tissues of Rtcb-knockout mice, the protein levels of TNF-α, IL-8, and p-p65 are increased, whereas the levels of IKKβ and IκBα are decreased. Moreover, the level of GSK3β is increased, whereas the levels of Wnt3a, β-catenin, and LGR5 are decreased. Collectively, our findings unveil a close association between RTCB and colonic tissue homeostasis and demonstrate that RTCB deficiency can lead to dysregulation of both the NF-κB and Wnt/β-catenin signaling pathways in colonic cells.

Published

2024

2. Enhanced fluoride removal using Mg-Zr binary metal oxide nanoparticles confined in a strong-base anion exchanger

Author

He, Chengqiang, Sun, Yue, Gu, Yingpeng, and Ji, Hongyu

Published

2024

3. Efficient degradation of diazinon and adsorption of released phosphate through activating peroxymonosulfate by Zr-doped ZIF-8 encapsulated CoFe2O4 composite

Author

Ji, Hongyu, Sun, Yue, Zheng, Weisheng, and He, Chengqiang

Published

2023

4. RTCB deficiency triggers colitis in mice by influencing the NF-κB and Wnt/β-catenin signaling pathways

Author

Liu, Peiyan, primary, Zhang, Ruitao, additional, Song, Xiaotong, additional, Tian, Xiaohua, additional, Guan, Yichao, additional, Li, Licheng, additional, He, Mei, additional, He, Chengqiang, additional, and Ding, Naizheng, additional

Published

2023

5. Development of a recombinase polymerase amplification combined with a lateral flow dipstick assay for rapid detection of the Mycoplasma bovis

Author

Zhao, Guimin, Hou, Peili, Huan, Yanjun, He, Chengqiang, Wang, Hongmei, and He, Hongbin

Published

2018

6. DDIT3 antagonizes innate immune response to promote bovine alphaherpesvirus 1 replication via the DDIT3-SQSTM1-STING pathway

Author

Wang, Song, primary, Ma, Xiaomei, additional, Guo, Jin, additional, Li, Fangxu, additional, Chen, Tianhua, additional, Ma, Wenqing, additional, He, Chengqiang, additional, Wang, Hongmei, additional, and He, Hongbin, additional

Published

2022

7. Development of a recombinase polymerase amplification combined with lateral-flow dipstick assay for detection of bovine ephemeral fever virus

Author

Hou, Peili, primary, Zhao, Guimin, additional, Wang, Hongmei, additional, He, Chengqiang, additional, Huan, Yanjun, additional, and He, Hongbin, additional

Published

2018

8. Biopanning of polypeptides binding to bovine ephemeral fever virus G1 protein from phage display peptide library

Author

Hou, Peili, primary, Zhao, Guimin, additional, He, Chengqiang, additional, Wang, Hongmei, additional, and He, Hongbin, additional

Published

2018

9. Rapid visual detection of Mycobacterium avium subsp. paratuberculosis by recombinase polymerase amplification combined with a lateral flow dipstick

Author

Zhao, Guimin, primary, Wang, Hongmei, additional, Hou, Peili, additional, He, Chengqiang, additional, and He, Hongbin, additional

Published

2018

10. Rapid detection of infectious bovine Rhinotracheitis virus using recombinase polymerase amplification assays

Author

Hou, Peili, primary, Wang, Hongmei, additional, Zhao, Guimin, additional, He, Chengqiang, additional, and He, Hongbin, additional

Published

2017

11. Biopanning of polypeptides binding to bovine ephemeral fever virus G1 protein from phage display peptide library.

Author

Hou, Peili, Zhao, Guimin, He, Chengqiang, Wang, Hongmei, and He, Hongbin

Subjects

POLYPEPTIDES, GLYCOPROTEINS, LIGANDS (Biochemistry), NUCLEOCAPSIDS, EPITOPES

Abstract

Background: The bovine ephemeral fever virus (BEFV) glycoprotein neutralization site 1 (also referred as G1 protein) , is a critical protein responsible for virus infectivity and eliciting immune-protection, however, binding peptides of BEFV G1 protein are still unclear. Thus, the aim of the present study was to screen specific polypeptides, which bind BEFV G1 protein with high-affinity and inhibit BEFV replication. Methods: The purified BEFV G1 was coated and then reacted with the M13-based Ph.D.-7 phage random display library. The peptides for target binding were automated sequenced after four rounds of enrichment biopanning. The amino acid sequences of polypeptide displayed on positive clones were deduced and the affinity of positive polypeptides with BEFV G1 was assayed by ELISA. Then the roles of specific G1-binding peptides in the context of BEFV infection were analyzed. Results: The results showed that 27 specific peptide ligands displaying 11 different amino acid sequences were obtained and the T18 and T25 clone had a higher affinity to G1 protein than the other clones. Then their antiviral roles of two phage clones (T25 and T18) showed that both phage polypeptide T25 and T18 exerted inhibition on BEFV replication compared to control group. Moreover, synthetic peptide based on T18 (HSIRYDF) and T25 (YSLRSDY) alone or combined use on BEFV replication showed that the synthetic peptides could effectively inhibit the formation of cytopathic plaque and significantly inhibit BEFV RNA replication in a dose-dependent manner. Conclusion: Two antiviral peptide ligands binding to bovine ephemeral fever virus G1 protein from phage display peptide library were identified, which may provide a potential research tool for diagnostic reagents and novel antiviral agents. [ABSTRACT FROM AUTHOR]

Published

2018

12. Identification of Short Hairpin RNA Targeting Foot-And-Mouth Disease Virus with Transgenic Bovine Fetal Epithelium Cells

Author

Wang, Hongmei, primary, Wu, Jianming, additional, Liu, Xiao, additional, He, Hongbin, additional, Ding, Fangrong, additional, Yang, Hongjun, additional, Cheng, Lei, additional, Liu, Wenhao, additional, Zhong, Jifeng, additional, Dai, Yunping, additional, Li, Guangpeng, additional, He, Chengqiang, additional, Yu, Li, additional, and Li, Jianbin, additional

Published

2012

13. Germ cell nuclear factor directly represses the transcription of peroxisome proliferator-activated receptor delta gene

Author

He, Chengqiang, primary, Ding, Naizheng, additional, and Kang, Jie, additional

Published

2008

14. Genome comparison of a novel foot-and-mouth disease virus with other FMDV strains

Author

Feng, Qian, primary, Yu, Huan, additional, Liu, Yingying, additional, He, Chengqiang, additional, Hu, Jingsong, additional, Sang, Huachun, additional, Ding, Neizheng, additional, Ding, Mingxiao, additional, Fung, Yin-Wan Wendy, additional, Lau, Lok-Ting, additional, Yu, Albert Cheung-Hoi, additional, and Chen, Jianguo, additional

Published

2004

15. Biopanning of polypeptides binding to bovine ephemeral fever virus G 1 protein from phage display peptide library.

Author

Hou P, Zhao G, He C, Wang H, and He H

Subjects

Amino Acid Sequence, Animals, Antibodies, Viral, Bacteriophages, Cattle, Cell Line, Enzyme-Linked Immunosorbent Assay, Ephemeral Fever metabolism, Ephemeral Fever virology, Ephemeral Fever Virus, Bovine genetics, Glycoproteins genetics, Peptide Library, Peptides genetics, Protein Binding, Ephemeral Fever Virus, Bovine physiology, Glycoproteins metabolism, Peptides metabolism

Abstract

Background: The bovine ephemeral fever virus (BEFV) glycoprotein neutralization site 1 (also referred as G 1 protein), is a critical protein responsible for virus infectivity and eliciting immune-protection, however, binding peptides of BEFV G 1 protein are still unclear. Thus, the aim of the present study was to screen specific polypeptides, which bind BEFV G 1 protein with high-affinity and inhibit BEFV replication., Methods: The purified BEFV G 1 was coated and then reacted with the M13-based Ph.D.-7 phage random display library. The peptides for target binding were automated sequenced after four rounds of enrichment biopanning. The amino acid sequences of polypeptide displayed on positive clones were deduced and the affinity of positive polypeptides with BEFV G 1 was assayed by ELISA. Then the roles of specific G 1 -binding peptides in the context of BEFV infection were analyzed., Results: The results showed that 27 specific peptide ligands displaying 11 different amino acid sequences were obtained, and the T18 and T25 clone had a higher affinity to G 1 protein than the other clones. Then their antiviral roles of two phage clones (T25 and T18) showed that both phage polypeptide T25 and T18 exerted inhibition on BEFV replication compared to control group. Moreover, synthetic peptide based on T18 (HSIRYDF) and T25 (YSLRSDY) alone or combined use on BEFV replication showed that the synthetic peptides could effectively inhibit the formation of cytopathic plaque and significantly inhibit BEFV RNA replication in a dose-dependent manner., Conclusion: Two antiviral peptide ligands binding to bovine ephemeral fever virus G 1 protein from phage display peptide library were identified, which may provide a potential research tool for diagnostic reagents and novel antiviral agents.

Published

2018

16. Short hairpin RNA-mediated silencing of bovine rotavirus NSP4 gene prevents diarrhoea in suckling mice.

Author

Chen F, Wang H, He H, Song L, Wu J, Gao Y, Liu X, He C, Yang H, Chen L, Wang L, Li G, Li Y, Kaplan DE, and Zhong J

Subjects

Animals, Animals, Suckling, Diarrhea virology, Glycoproteins biosynthesis, Mice, Mice, Inbred BALB C, RNA, Small Interfering genetics, Rotavirus genetics, Toxins, Biological biosynthesis, Viral Nonstructural Proteins biosynthesis, Virulence Factors biosynthesis, Diarrhea prevention & control, Gene Silencing, Glycoproteins antagonists & inhibitors, RNA, Small Interfering metabolism, Rotavirus pathogenicity, Toxins, Biological antagonists & inhibitors, Viral Nonstructural Proteins antagonists & inhibitors, Virulence Factors antagonists & inhibitors

Abstract

While RNA interference (RNAi) has been widely used to study rotavirus gene function in vitro, the potential therapeutic role for RNAi in vivo has not been explored. To this end, we constructed two recombinant lentiviral vectors containing short hairpin RNA (shRNA) against non-structural protein-4 (NSP4) of bovine rotavirus (BRV), RNAi-351 and RNAi-492. RNAi-351 and RNAi-492 strongly suppressed the transient expression of a FLAG-tagged NSP4 fusion protein in 293T cells. In BRV-susceptible MA104 cells, RNAi-492 more potently silenced NSP4 mRNA than RNAi-351 and combination of the two shRNAs almost completely silenced viral NSP4 gene expression. While 100% of suckling mice exposed to BRV and control shRNA developed severe diarrhoea, no suckling mice exposed to BRV in the presence of RNAi-492 or a combination of RNAi-492/RNAi-351 developed severe diarrhoea, and only 20 and 3.3% developed mild diarrhoea, respectively. In addition, RNAi-492 and RNAi-351 markedly abrogated rotaviral replication in MA104 cells and significantly inhibited BRV replication in mouse pups. These results indicated that shRNAs silencing NSP4 gene had substantial antiviral properties and inhibited replication of BRV in a sequence-specific manner that may have clinical application.

Published

2011