Your search keyword '"Huiqing Shen"' showing total 10 results

1. Gut Dysbiosis Drives Inflammatory Bowel Disease Through the CCL4L2‐VSIR Axis in Glycogen Storage Disease

Author

Jiaoli Lan, Yuxin Zhang, Cuiyuan Jin, Huan Chen, Zexiong Su, Jiaxing Wu, Ni Ma, Xiaoyan Zhang, Yiyun Lu, Yongxin Chen, Xiaolu Zeng, Huiqiong Zhang, Guilang Zheng, Yueyu Sun, Chun Wang, Yan Hu, Yifei Wang, Yumei Liu, Zhaoyang Zeng, Liyun Shi, Jun He, Aihua Cao, Yichao Wang, Xu Pan, Gulei Jin, Ying Wang, Xun Jiang, Huiqing Shen, Qing Tang, Xiaoli Xie, Yuan Xiao, Xuemei Zhong, Xuchao Zhang, Liang Zeng, Liping Ye, Jing Xie, Lanlan Geng, Zhiling Li, Xiaohui Wu, Ren Mao, Shaojun Zhang, Siyuan Huang, Suling Liu, Hanshi Zeng, Wanfu Xu, Sitang Gong, Yuxiong Guo, and Min Yang

Subjects

CCL4L2‐VSIR, glycogen storage disease, gut microbiota, inflammatory bowel disease, macrophage, Science

Abstract

Abstract Patients with glycogen storage disease type Ib (GSD‐Ib) frequently have inflammatory bowel disease (IBD). however, the underlying etiology remains unclear. Herein, this study finds that digestive symptoms are commonly observed in patients with GSD‐Ib, presenting as single or multiple scattered deep round ulcers, inflammatory pseudo‐polyps, obstructions, and strictures, which differ substantially from those in typical IBD. Distinct microbiota profiling and single‐cell clustering of colonic mucosae in patients with GSD are conducted. Heterogeneous oral pathogenic enteric outgrowth induced by GSD is a potent inducer of gut microbiota immaturity and colonic macrophage accumulation. Specifically, a unique population of macrophages with high CCL4L2 expression is identified in response to pathogenic bacteria in the intestine. Hyper‐activation of the CCL4L2‐VSIR axis leads to increased expression of AGR2 and ZG16 in epithelial cells, which mediates the unique progression of IBD in GSD‐Ib. Collectively, the microbiota‐driven pathomechanism of IBD is demonstrated in GSD‐Ib and revealed the active role of the CCL4L2‐VSIR axis in the interaction between the microbiota and colonic mucosal immunity. Thus, targeting gut dysbiosis and/or the CCL4L2‐VISR axis may represent a potential therapy for GSD‐associated IBD.

Published

2024

2. Ambient sulfur dioxide and hospital expenditures and length of hospital stay for respiratory diseases: A multicity study in China

Author

Dawei Cao, Dashan Zheng, Zhengmin (Min) Qian, Huiqing Shen, Yi Liu, Qiyong Liu, Jimin Sun, Shiyu Zhang, Guangyuan Jiao, Xiaoran Yang, Michael G. Vaughn, Chongjian Wang, Xinri Zhang, and Hualiang Lin

Subjects

Respiratory disease, Sulfur dioxide, Hospital cost, Hospital admission, Length of hospital stay, Environmental pollution, TD172-193.5, Environmental sciences, GE1-350

Abstract

Background: Ambient sulfur dioxide (SO2) has been associated with morbidity and mortality of respiratory diseases, however, its effect on length of hospital stays (LOS) and cost for these diagnoses remain unclear. Methods: We collected hospital admission information for respiratory diseases from all 11 cities in the Shanxi Province of China during 2017–2019. We assessed individual-level exposure by using an inverse distance weighting approach based on geocoded residential addresses. A generalized additive model was built to delineate city-specific effects of SO2 on hospitalization, hospital expenditure, and length of hospital stay for respiratory diseases. The overall effects were obtained by random-effects meta-analysis. We further estimated the respiratory burden attributable to SO2 by comparing different reference concentrations. Results: We observed significant effects of SO2 exposure on respiratory diseases. At the provincial level, each 10 μg/m3 increase in SO2 on lag03 was associated with a 0.63% (95% CI: 0.14–0.11) increase in hospital admission, an increase of 4.56 days (95% CI: 1.16–7.95) of hospital stay, and 3647.97 renminbi (RMB, Chinese money) (95% CI: 1091.05–6204.90) in hospital cost. We estimated about 6.13 (95% CI: 1.33–11.10) thousand hospital admissions, 65.77 million RMB (95% CI: 19.67–111.87) in hospital expenditure, and 82.13 (95% CI: 20.87–143.40) thousand days of hospital stay could have potentially been avoided had the daily SO2 concentrations been reduced to WHO’s reference concentration (40 µg/m3). Variable values in correspondence with this reference concentration could reduce the hospital cost and LOS of each case by 52.67 RMB (95% CI: 15.75–89.59) and 0.07 days (95% CI: 0.02–0.117). Conclusion: This study provides evidence that short-term ambient SO2 exposure is an important risk factor of respiratory diseases, indicating that continually tightening policies to reduce SO2 levels could effectively reduce respiratory disease burden in Shanxi Province.

Published

2022

3. Transcriptome Analysis of Ivosidenib-Mediated Inhibitory Functions on Non-Small Cell Lung Cancer

Author

Juan Wu, Ru Chen, Huiqing Shen, Ting Yan, Yu Qian, Yaping Zhang, Zhuoya Huang, Pengzhou Kong, Min Pang, and Xinri Zhang

Subjects

ivosidenib, RNA-seq, bioinformatic analysis, ceRNA, non-small cell lung cancer, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282

Abstract

Ivosidenib is an isocitrate dehydrogenase mutant inhibitor that the US Food and Drug Administration recently approved for the treatment of leukemia. Studies suggested that ivosidenib may inhibit the progression of non-small cell lung cancer (NSCLC). In the present study, we explored RNAs and their potential regulatory mechanisms by which ivosidenib treats NSCLC cells. We used MTT assays, Transwell assays, and flow cytometry to measure the anti-tumor effects of ivosidenib in NSCLC cells. We performed whole transcriptome sequencing to determine differentially expressed mRNAs (DE-mRNAs) and non-coding RNAs (ncRNA). We used GO and KEGG pathway enrichment analyses to identify the functions and potential mechanisms. According to miRNA target interactions, we constructed a competing endogenous network. Ivosidenib inhibited the proliferation, invasion, and migration of NSCLC cells and inhibited tumor growth in vivo. We identified 212 DE-mRNAs, four DE-miRNAs, and 206 DE-lncRNAs in ivosidenib-treated NSCLC cells compared to untreated NSCLC cells. DE-mRNAs were significantly enriched in the cancer-associated pathways, including the TGF-β signaling pathway, the PI3K-Akt signaling pathway, the Jak-STAT signaling pathway, the MAPK signaling pathway, the Rap1 signaling pathway, and cell adhesion molecules. Based on the competing endogenous RNA hypothesis, we constructed lncRNA-miRNA-mRNA networks to elucidate the regulatory relationships between mRNA and ncRNA. We found that qRT-PCR results showed corresponding expression trends of differential genes with sequencing data. Our results provide insights into the molecular basis of ivosidenib suppression of NSCLC.

Published

2021

4. Systematic Transcriptome Analysis Reveals the Inhibitory Function of Cinnamaldehyde in Non-Small Cell Lung Cancer

Author

Ru Chen, Juan Wu, Chang Lu, Ting Yan, Yu Qian, Huiqing Shen, Yujing Zhao, Jianzhen Wang, Pengzhou Kong, and Xinri Zhang

Subjects

cinnamaldehyde, long non-coding RNAs, micro RNAs, non-small cell lung cancer, messenger RNAs, Therapeutics. Pharmacology, RM1-950

Abstract

Cinnamaldehyde (CA) is the main component extracted from the traditional Chinese medicine cinnamon. Recent studies revealed that CA has antiviral and anti-tumor effects. However, the effect and mechanism of CA on non-small cell lung cancer (NSCLC) through whole transcriptome sequencing integrated analysis have not been systematically investigated. In this study, whole transcriptome sequencing was used to identify differentially expressed messenger RNAs (mRNAs), micro RNAs (miRNAs), and long non-coding RNAs (lncRNAs) that were influenced by CA and screen regulatory pathways. The results showed that CA significantly inhibited proliferation, invasion, and migration, whereas it induced the apoptosis of NSCLC cells. CA inhibited tumor growth in vivo. Gene ontology and Kyoto Encyclopedia of Genes and Genomes analysis revealed that these differentially expressed mRNAs were potentially implicated in the CA-suppressing malignant phenotypes of NSCLC. According to the competing endogenous RNA (ceRNA) hypothesis, a ceRNA network was constructed, including 13 mRNAs, 6 miRNAs, and 11 lncRNAs. Kyoto Encyclopedia of Genes and Genomes analysis of the 13 mRNAs in the ceRNA network showed that suppressors of cytokine signaling 1 (SOCS1), BTG anti-proliferation factor 2 (BTG2), and Bruton tyrosine kinase (BTK) were significantly enriched in the JAK/STAT signaling pathway, RNA degradation, and nuclear factor-κB (NF-κB) signaling pathway related to cancer. These findings indicated that SOCS1, BTG2, and BTK play an essential role in CA against NSCLC. Meanwhile, based on the ceRNA network, three lncRNAs (long intergenic non-protein coding RNA 1504 [LINC01504], LINC01783, and THUMPD3 antisense RNA 1 [THUMPD3-AS1]) and three miRNAs (has-miR-155-5p, has-miR-7-5p, and has-miR-425-5p) associated with SOCS1, BTG2, and BTK may be important in CA against NSCLC. Taken together, the present study demonstrated the activity of CA against lung cancer and its potential use as a therapeutic agent.

Published

2021

5. Different negative biases of anxiety in discrimination and reasoning

Author

Huiqing Shen, Ruizhi Huang, Yayan Song, Zihan Zhou, Feng Guo, Shiyu Yan, Huilin Qiu, and Ke Jiang

Abstract

Background As an important feature of anxiety disorders, anxiety refers to the emotional response to the anticipation of future threat, and excessive anxiety is more likely to trigger multi-kinds of disease symptoms. The aim of this study was to detect different performance of high-anxiety and low-anxiety individuals to deal with the discrimination and reasoning tasks and the mutual influence between the two tasks. Methods A modified “reasoning-discrimination” paradigm with the discrimination (d’) of discrimination task and the projectability of the reasoning task as response variables was used. Sixty-nine participants assessed through STAI, GAD-7 and interviews, divided into two groups. Results The results revealed that all individuals showed emotional bias in discrimination tasks, but as to complex tasks, the d’ of the high-anxiety group was lower than that of the low-anxiety group, especially in neutral and positive conditions; in reasoning tasks, the difference between the two groups of emotional effects was not significant. Conclusions The findings suggest that high anxiety could impair the discrimination ability, especially the discrimination ability of the positive information, and lead to a greater negative bias. And the effects of anxiety in different cognitive domains are probably not universal, but specific.

Published

2023

6. Associations of Ambient NO

Author

Dashan, Zheng, Dawei, Cao, Shiyu, Zhang, Huiqing, Shen, Yi, Liu, Qiyong, Liu, Jimin, Sun, Guangyuan, Jiao, Jianzhen, Wang, Xiaoran, Yang, Xinri, Zhang, and Hualiang, Lin

Abstract

Numerous epidemiological studies have documented the association between ambient nitrogen dioxide (NOThis study collected the respiratory hospitalization, hospital expenditure, and LOS for respiratory diseases from 2017-2019 in Shanxi, China, and comprehensively evaluated the association between ambient NOThis study provides evidence on the association between ambient NO

Published

2022

7. Transcriptome Analysis of Ivosidenib-Mediated Inhibitory Functions on Non-Small Cell Lung Cancer

Author

Pengzhou Kong, Huiqing Shen, Yaping Zhang, Ru Chen, Xin-ri Zhang, Juan Wu, Yu Qian, Min Pang, Zhuoya Huang, and Ting Yan

Subjects

Cancer Research, medicine.diagnostic_test, Competing endogenous RNA, Cell adhesion molecule, ivosidenib, RNA-Seq, ceRNA, Biology, lcsh:Neoplasms. Tumors. Oncology. Including cancer and carcinogens, Non-coding RNA, lcsh:RC254-282, bioinformatic analysis, Flow cytometry, Transcriptome, Oncology, medicine, Cancer research, Rap1, RNA-seq, Signal transduction, non-small cell lung cancer, Original Research

Abstract

Ivosidenib is an isocitrate dehydrogenase mutant inhibitor that the US Food and Drug Administration recently approved for the treatment of leukemia. Studies suggested that ivosidenib may inhibit the progression of non-small cell lung cancer (NSCLC). In the present study, we explored RNAs and their potential regulatory mechanisms by which ivosidenib treats NSCLC cells. We used MTT assays, Transwell assays, and flow cytometry to measure the anti-tumor effects of ivosidenib in NSCLC cells. We performed whole transcriptome sequencing to determine differentially expressed mRNAs (DE-mRNAs) and non-coding RNAs (ncRNA). We used GO and KEGG pathway enrichment analyses to identify the functions and potential mechanisms. According to miRNA target interactions, we constructed a competing endogenous network. Ivosidenib inhibited the proliferation, invasion, and migration of NSCLC cells and inhibited tumor growth in vivo. We identified 212 DE-mRNAs, four DE-miRNAs, and 206 DE-lncRNAs in ivosidenib-treated NSCLC cells compared to untreated NSCLC cells. DE-mRNAs were significantly enriched in the cancer-associated pathways, including the TGF-β signaling pathway, the PI3K-Akt signaling pathway, the Jak-STAT signaling pathway, the MAPK signaling pathway, the Rap1 signaling pathway, and cell adhesion molecules. Based on the competing endogenous RNA hypothesis, we constructed lncRNA-miRNA-mRNA networks to elucidate the regulatory relationships between mRNA and ncRNA. We found that qRT-PCR results showed corresponding expression trends of differential genes with sequencing data. Our results provide insights into the molecular basis of ivosidenib suppression of NSCLC.

Published

2021

8. Extracting Stops from Spatio-Temporal Trajectories within Dynamic Contextual Features

Author

Huiqing Shen, Tao Wu, Longgang Xiang, and Jianxin Qin

Subjects

stops identification, Point of interest, Computer science, SVM, lcsh:TJ807-830, Geography, Planning and Development, lcsh:Renewable energy sources, 0211 other engineering and technologies, Context (language use), 02 engineering and technology, Management, Monitoring, Policy and Law, computer.software_genre, 0502 economics and business, environmental context, lcsh:Environmental sciences, 021101 geological & geomatics engineering, lcsh:GE1-350, 050210 logistics & transportation, Renewable Energy, Sustainability and the Environment, business.industry, lcsh:Environmental effects of industries and plants, 05 social sciences, data mining, Support vector machine, Identification (information), lcsh:TD194-195, trajectory data, Trajectory, Global Positioning System, Data mining, business, Classifier (UML), computer

Abstract

Identifying stops from GPS trajectories is one of the main concerns in the study of moving objects and has a major effect on a wide variety of location-based services and applications. Although the spatial and non-spatial characteristics of trajectories have been widely investigated for the identification of stops, few studies have concentrated on the impacts of the contextual features, which are also connected to the road network and nearby Points of Interest (POIs). In order to obtain more precise stop information from moving objects, this paper proposes and implements a novel approach that represents a spatio-temproal dynamics relationship between stopping behaviors and geospatial elements to detect stops. The relationship between the candidate stops based on the standard time&ndash, distance threshold approach and the surrounding environmental elements are integrated in a complex way (the mobility context cube) to extract stop features and precisely derive stops using the classifier classification. The methodology presented is designed to reduce the error rate of detection of stops in the work of trajectory data mining. It turns out that 26 features can contribute to recognizing stop behaviors from trajectory data. Additionally, experiments on a real-world trajectory dataset further demonstrate the effectiveness of the proposed approach in improving the accuracy of identifying stops from trajectories.

Published

2021

9. SOX7 and GATA-4 are competitive activators of Fgf-3 transcription

Author

Akira Murakami, Sanami Ishida, Clive Dickson, and Huiqing Shen

Subjects

DNA, Complementary, Time Factors, Transcription, Genetic, Response element, Fibroblast Growth Factor 3, Molecular Sequence Data, E-box, Tretinoin, Embryoid body, Biology, Biochemistry, Binding, Competitive, Mice, SOX2, Transcription (biology), Genes, Reporter, Cell Line, Tumor, Cyclic AMP, SOXF Transcription Factors, Animals, Luciferases, Promoter Regions, Genetic, Molecular Biology, Transcription factor, In Situ Hybridization, General transcription factor, Base Sequence, Models, Genetic, Activator (genetics), Reverse Transcriptase Polymerase Chain Reaction, Endoderm, High Mobility Group Proteins, Cell Differentiation, Cell Biology, Blotting, Northern, Molecular biology, GATA4 Transcription Factor, DNA-Binding Proteins, Fibroblast Growth Factors, embryonic structures, RNA Interference, Protein Binding, Transcription Factors

Abstract

Fgf-3 is expressed in a dynamic and complex spatiotemporal pattern during mouse development. Previous studies identified GATA-4 as a transcription factor that binds the key regulatory element PS4A of the Fgf-3 promoter and stimulates transcription. Here we show that members of the SOX family of transcription factors also bind PS4A and differentially modulate transcription. At least five SOX genes, Sox2, Sox6, Sox7, Sox13, and Sox17, were expressed in F9 cells, and of these, Sox7 and Sox17 were dramatically induced in parallel with Fgf-3 following differentiation into parietal endoderm-like cells with retinoic acid and dibutyryl cAMP. Complexes could be detected on PS4A with SOX2, SOX7, and SOX17 by using nuclear extracts from differentiated F9 cells. However, only Sox7 expression markedly activated the Fgf-3 promoter in these cells. By contrast, SOX2 was a poor activator of Fgf-3 transcription, and when Sox2 was coexpressed with Gata4, it negatively modulated the strong activation mediated by GATA-4. More detailed analyses showed that SOX7 competes with GATA-4 for PS4A occupancy and to activate the Fgf-3 promoter. In situ hybridization analysis showed that Sox7 is co-expressed with Fgf-3 and Gata4 in the parietal endoderm of E7.5 mouse embryos. In culture, GATA-4-deficient embryonal stem cells were shown to express Fgf-3 upon differentiation into embryoid bodies, although at lower levels than were found in wild type embryonal stem cells. This Fgf-3 expression was virtually abolished when Sox7 expression was suppressed by RNA interference. These results show that SOX7 is a potent activator of Fgf-3 transcription.

Published

2004

10. SOX7 and GATA-4 Are Competitive Activators of Fgf-3 Transcription.

Author

Murakami, Akira, Huiqing Shen, Ishida, Sanami, and Dickson, Clive

Subjects

*FIBROBLAST growth factors, *TRANSCRIPTION factors, *PROMOTERS (Genetics), *GENETIC transcription, *PROTEIN binding, *BIOCHEMISTRY

Abstract

Fgf-3 is expressed in a dynamic and complex spatio- temporal pattern during mouse development. Previous studies identified GATA-4 as a transcription factor that binds the key regulatory element PS4A of the Fgf-3 promoter and stimulates transcription. Here we show that members of the SOX family of transcription factors also bind PS4A and differentially modulate transcription. At least five SOX genes, Sox2, Sox6, Sox7, Sox13, and Sox17, were expressed in F9 cells, and of these, Sox7 and Soxl7 were dramatically induced in parallel with Fgf-3 following differentiation into parietal endoderm-like cells with retinoic acid and dibutyryl cAMP. Complexes could be detected on PS4A with SOX2, SOX7, and SOX17 by using nuclear extracts from differentiated F9 cells. How- ever, only Sox7 expression markedly activated the Fgf-3 promoter in these cells. By contrast, SOX2 was a poor activator of Fgf-3 transcription, and when Sox2 was co-expressed with Gata4, it negatively modulated the strong activation mediated by GATA-4. More detailed analyses showed that SOX7 competes with GATA-4 for PS4A occupancy and to activate the Fgf-3 promoter. In situ hybridization analysis showed that Sox7 is co-expressed with Fgf-3 and Gata4 in the parietal endoderm of E7.5 mouse embryos. In culture, GATA-4-deficient embryonal stem cells were shown to express Fgf-3 upon differentiation into embryoid bodies, although at lower levels than were found in wild type embryonal stem cells. This Fgf-3 expression was virtually abolished when Sox7 expression was suppressed by RNA interference. These results show that SOX7 is a potent activator of Fgf-3 transcription. [ABSTRACT FROM AUTHOR]

Published

2004