Your search keyword '"Wenqian Shi"' showing total 12 results

1. Decoding frontotemporal and cell-type-specific vulnerabilities to neuropsychiatric disorders and psychoactive drugs

Author

Jiatong Ji, Honglu Chao, Huimei Chen, Jun Liao, Wenqian Shi, Yangfan Ye, Tian Wang, Yongping You, Ning Liu, Jing Ji, and Enrico Petretto

Subjects

frontal lobe, temporal lobe, psychiatric disorder, single-cell RNA sequencing, psychoactive drugs, Biology (General), QH301-705.5

Abstract

Frontotemporal lobe abnormalities are linked to neuropsychiatric disorders and cognition, but the role of cellular heterogeneity between temporal lobe (TL) and frontal lobe (FL) in the vulnerability to genetic risk factors remains to be elucidated. We integrated single-nucleus transcriptome analysis in ‘fresh’ human FL and TL with genetic susceptibility, gene dysregulation in neuropsychiatric disease and psychoactive drug response data. We show how intrinsic differences between TL and FL contribute to the vulnerability of specific cell types to both genetic risk factors and psychoactive drugs. Neuronal populations, specifically PVALB neurons, were most highly vulnerable to genetic risk factors for psychiatric disease. These psychiatric disease-associated genes were mostly upregulated in the TL, and dysregulated in the brain of patients with obsessive-compulsive disorder, bipolar disorder and schizophrenia. Among these genes, GRIN2A and SLC12A5, implicated in schizophrenia and bipolar disorder, were significantly upregulated in TL PVALB neurons and in psychiatric disease patients’ brain. PVALB neurons from the TL were twofold more vulnerable to psychoactive drugs than to genetic risk factors, showing the influence and specificity of frontotemporal lobe differences on cell vulnerabilities. These studies provide a cell type resolved map of the impact of brain regional differences on cell type vulnerabilities in neuropsychiatric disorders.

Published

2024

2. Atox1 protects hippocampal neurons after traumatic brain injury via DJ-1 mediated anti-oxidative stress and mitophagy

Author

Pengzhan Zhao, Wenqian Shi, Yangfan Ye, Ke Xu, Jingming Hu, Honglu Chao, ZeQiang Tao, Lei Xu, Wei Gu, Liuchao Zhang, Tian Wang, Xinyue Wang, and Jing Ji

Subjects

Traumatic brain injury, Hippocampal neuron, Atox1, DJ-1, Oxidative stress, Medicine (General), R5-920, Biology (General), QH301-705.5

Abstract

Regulation of the oxidative stress response is crucial for the management and prognosis of traumatic brain injury (TBI). The copper chaperone Antioxidant 1 (Atox1) plays a crucial role in regulating intracellular copper ion balance and impacting the antioxidant capacity of mitochondria, as well as the oxidative stress state of cells. However, it remains unknown whether Atox1 is involved in modulating oxidative stress following TBI. Here, we investigated the regulatory role of Atox1 in oxidative stress on neurons both in vivo and in vitro, and elucidated the underlying mechanism through culturing hippocampal HT-22 cells with Atox1 mutation. The expression of Atox1 was significantly diminished following TBI, while mice with overexpressed Atox1 exhibited a more preserved hippocampal structure and reduced levels of oxidative stress post-TBI. Furthermore, the mice displayed notable impairments in learning and memory functions after TBI, which were ameliorated by the overexpression of Atox1. In the stretch injury model of HT-22 cells, overexpression of Atox1 mitigated oxidative stress by preserving the normal morphology and network connectivity of mitochondria, as well as facilitating the elimination of damaged mitochondria. Mechanistically, co-immunoprecipitation and mass spectrometry revealed the binding of Atox1 to DJ-1. Knockdown of DJ-1 in HT-22 cells significantly impaired the antioxidant capacity of Atox1. Mutations in the copper-binding motif or sequestration of free copper led to a substantial decrease in the interaction between Atox1 and DJ-1, with overexpression of DJ-1 failing to restore the antioxidant capacity of Atox1 mutants. The findings suggest that DJ-1 mediates the ability of Atox1 to withstand oxidative stress. And targeting Atox1 could be a potential therapeutic approach for addressing post-traumatic neurological dysfunction.

Published

2024

3. Meningioma achieves malignancy and erastin-induced ferroptosis resistance through FOXM1-AURKA-NRF2 axis

Author

Yangfan Ye, Lei Xu, Liuchao Zhang, Pengzhan Zhao, Wanzhi Cai, Guoqiang Fu, Tian Wang, Zeqiang Tao, Wenqian Shi, Wei Gu, Jingming Hu, Guangyao Yuan, Yutian Wei, Ke Xu, Zhongyuan Bao, Honglu Chao, Ning Liu, Lin Zhao, Yiming Tu, and Jing Ji

Subjects

Meningioma, Ferroptosis, Protein kinase, AURKA, NRF2, Medicine (General), R5-920, Biology (General), QH301-705.5

Abstract

The oncogene Aurora kinase A (AURKA) has been implicated in various tumor, yet its role in meningioma remains unexplored. Recent studies have suggested a potential link between AURKA and ferroptosis, although the underlying mechanisms are unclear. This study presented evidence of AURKA upregulation in high grade meningioma and its ability to enhance malignant characteristics. We identified AURKA as a suppressor of erastin-induced ferroptosis in meningioma. Mechanistically, AURKA directly interacted with and phosphorylated kelch-like ECH-associated protein 1 (KEAP1), thereby activating nuclear factor erythroid 2 related factor 2 (NFE2L2/NRF2) and target genes transcription. Additionally, forkhead box protein M1 (FOXM1) facilitated the transcription of AURKA. Suppression of AURKA, in conjunction with erastin, yields significant enhancements in the prognosis of a murine model of meningioma. Our study elucidates an unidentified mechanism by which AURKA governs ferroptosis, and strongly suggests that the combination of AURKA inhibition and ferroptosis-inducing agents could potentially provide therapeutic benefits for meningioma treatment.

Published

2024

4. Lineage Replacement and Genetic Changes of Four HR-HPV Types during the Period of Vaccine Coverage: A Six-Year Retrospective Study in Eastern China

Author

Wenjie Qu, Chen Hua, Yaping Wang, Yan Wang, Lu Zhang, Zhiheng Wang, Wenqian Shi, Fang Chen, Zhiyong Wu, Qian Wang, Lu Lu, Shibo Jiang, Long Sui, and Yanyun Li

Subjects

human papillomavirus, vaccine, lineage replacement, vaccine escape, Medicine

Abstract

Objective: This study aimed to provide clinical evidence for lineage replacement and genetic changes of High-Risk Human Papillomavirus (HR-HPV) during the period of vaccine coverage and characterize those changes in eastern China. Methods: This study consisted of two stages. A total of 90,583 patients visiting the Obstetrics and Gynecology Hospital of Fudan University from March 2018 to March 2022 were included in the HPV typing analysis. Another 1076 patients who tested positive for HPV31, 33, 52, or 58 from November 2020 to August 2023 were further included for HPV sequencing. Vaccination records, especially vaccine types and the third dose administration time, medical history, and cervical cytology samples were collected. Viral DNA sequencing was then conducted, followed by phylogenetic analysis and sequence alignment. Results: The overall proportion of HPV31 and 58 infections increased by 1.23% and 0.51%, respectively, while infection by HPV33 and 52 decreased by 0.42% and 1.43%, respectively, within the four-year vaccination coverage period. The proportion of HPV31 C lineage infections showed a 22.17% increase in the vaccinated group, while that of the HPV58 A2 sublineage showed a 12.96% increase. T267A and T274N in the F-G loop of HPV31 L1 protein, L150F in the D-E loop, and T375N in the H-I loop of HPV58 L1 protein were identified as high-frequency escape-related mutations. Conclusions: Differences in epidemic lineage changes and dominant mutation accumulation may result in a proportional difference in trends of HPV infection. New epidemic lineages and high-frequency escape-related mutations should be noted during the vaccine coverage period, and regional epidemic variants should be considered during the development of next-generation vaccines.

Published

2024

5. Analysis of publications on HPV genotype co-infection: a bibliometric study on existing research

Author

Tianyi Bi, Yingxin Gong, Jiayin Mo, Yan Wang, Wenjie Qu, Yaping Wang, Wenqian Shi, Feifei Zhang, Long Sui, and Yanyun Li

Subjects

bibliometric analysis, human papillomavirus, co-infection, web of science, VOSviewer, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282

Abstract

PurposeTo identify the bibliometric information of Human papillomavirus (HPV) genotype co-infection in certain literature database over the past two decades.MethodsWeb of Science was used as the main database to identify all eligible articles focusing on HPV genotype co-infection at the date of October 16, 2022. From this journal database, we identified 463 articles on HPV genotype co-infection, conducted statistical analysis according to the author, journal, publication year and month, country or region, keyword and impact factor.ResultsThe articles included in our analysis were published between 1994 and 2022. The index of citations per year ranged from 170.4 to 13.1. These articles were from 78 countries or regions, with most publications from the United States (n = 73), followed by China (n = 65) and Italy (n = 50). The journal that contributed the most publications on HPV heterotypic gene co-infection was PLOS ONE with a total of 29 articles, followed by JOURNAL OF MEDICAL VIROLOGY (n = 28), INFECTIOUS AGENTS AND CANCER (n = 14) and JOURNAL OF CLINICAL VIROLOGY (n = 12). Among existing research in the field of HPV co-infection, we found that epidemiological distribution and infection mechanism has been the two major topics for scholars, and studies on detection methods for HPV multiple genotypes were also included.ConclusionOver decades, epidemiological studies and mechanism investigationhas been the central topics when it comes to HPV genotypes co-infection. Studies on HPV co-infection remained relatively insufficient, mainly stays in qualitative level while detailed infection data and high quality literature publications were still lack of valuable discussion.

Published

2023

6. Multiplex CRISPR/Cas9-mediated knockout of soybean LNK2 advances flowering time

Author

Zhaobo Li, Qun Cheng, Zhuoran Gan, Zhihong Hou, Yuhang Zhang, Yongli Li, Haiyang Li, Haiyang Nan, Cen Yang, Linnan Chen, Sijia Lu, Wenqian Shi, Liyu Chen, Yanping Wang, Chao Fang, Liping Kong, Tong Su, Shichen Li, Kun Kou, Lingshuang Wang, Fanjiang Kong, Baohui Liu, and Lidong Dong

Subjects

Soybean, LNK2, CRISPR/Cas9, Genome editing, Flowering time, Agriculture, Agriculture (General), S1-972

Abstract

Flowering time is an important agronomic trait for soybean yield and adaptation. However, the genetic basis of soybean adaptation to diverse latitudes is still not clear. Four NIGHT LIGHT-INDUCIBLE AND CLOCK-REGULATED 2 (LNK2) homeologs of Arabidopsis thaliana LNK2 were identified in soybean. Three single-guide RNAs were designed for editing the four LNK2 genes. A transgene-free homozygous quadruple mutant of the LNK2 genes was developed using the CRISPR (clustered regularly interspaced short palindromic repeats)/Cas9 (CRISPR-associated protein 9). Under long-day (LD) conditions, the quadruple mutant flowered significantly earlier than the wild-type (WT). Quantitative real-time PCR (qRT-PCR) revealed that transcript levels of LNK2 were significantly lower in the quadruple mutant than in the WT under LD conditions. LNK2 promoted the expression of the legume-specific E1 gene and repressed the expression of FT2a. Genetic markers were developed to identify LNK2 mutants for soybean breeding. These results indicate that CRISPR/Cas9-mediated targeted mutagenesis of four LNK2 genes shortens flowering time in soybean. Our findings identify novel components in flowering-time control in soybean and may be beneficial for further soybean breeding in high-latitude environments.

Published

2021

7. A Lightweight Convolutional Neural Network for Real-Time Facial Expression Detection

Author

Ning Zhou, Renyu Liang, and Wenqian Shi

Subjects

Emotion classification, lightweight CNN, real-time, expression detection, Electrical engineering. Electronics. Nuclear engineering, TK1-9971

Abstract

In this paper our group proposes and designs a lightweight convolutional neural network (CNN) for detecting facial emotions in real-time and in bulk to achieve a better classification effect. We verify whether our model is effective by creating a real-time vision system. This system employs multi-task cascaded convolutional networks (MTCNN) to complete face detection and transmit the obtained face coordinates to the facial emotions classification model we designed firstly. Then it accomplishes the task of emotion classification. Multi-task cascaded convolutional networks have a cascade detection feature, one of which can be used alone, thereby reducing the occupation of memory resources. Our expression classification model employs Global Average Pooling to replace the fully connected layer in the traditional deep convolution neural network model. Each channel of the feature map is associated with the corresponding category, eliminating the black box characteristics of the fully connected layer to a certain extent. At the same time, our model marries the residual modules and depth-wise separable convolutions, reducing large quantities of parameters and making the model more portable. Finally, our model is tested on the FER-2013 dataset. It only takes 3.1% of the 16GB memory, that is, only 0.496GB memory is needed to complete the task of classifying facial expressions. Not only can our model be stored in an 872.9 kilobytes file, but also its accuracy has reached 67% on the FER-2013 dataset. And it has good detection and recognition effects on those figures which are out of the dataset.

Published

2021

8. Antagonistic Peptides That Specifically Bind to the First and Second Extracellular Loops of CCR5 and Anti-IL-23p19 Antibody Reduce Airway Inflammation by Suppressing the IL-23/Th17 Signaling Pathway

Author

Yingli Zhang, Rongrong Liang, Aicen Xie, Wenqian Shi, Huarong Huang, and Yingqiang Zhong

Subjects

Pathology, RB1-214

Abstract

Asthma is a heterogeneous chronic inflammatory disorder of the airways with a complex etiology, which involves a variety of cells and cellular components. Therefore, the aim of the study was to investigate the effects and mechanisms of antagonistic peptides that specifically bind to the first and second extracellular loops of CCR5 (GH and HY peptides, respectively) and anti-interleukin-23 subunit p19 (anti-IL-23p19) in the airway and thereby mediate inflammation and the IL-23/T helper 17 (Th17) cell pathway in asthmatic mice. An experimental asthma model using BALB/c mice was induced by ovalbumin (OVA) and treated with peptides that are antagonistic to CCR5 or with anti-IL-23p19. The extents of the asthmatic inflammation and mucus production were assessed. In addition, bronchoalveolar lavage fluid (BALF) was collected, the cells were counted, and the IL-4 level was detected by ELISA. The IL-23/Th17 pathway-related protein and mRNA levels in the lung tissues were measured, and the positive production rates of Th17 cells in the thymus, spleen, and peripheral blood were detected. The groups treated with one of the two peptides and/or anti-IL-23p19 showed significant reductions in allergic inflammation and mucus secretion; decreased expression levels of IL-23p19, IL-23R, IL-17A and lactoferrin (LTF); and reduced proportions of Th17 cells in the thymus, spleen, and peripheral blood. Specifically, among the four treatment groups, the anti-IL-23p19 with HY peptide group exhibited the lowest positive production rate of Th17 cells. Our data also showed a significant and positive correlation between CCR5 and IL-23p19 protein expression. These findings suggest that the administration of peptides antagonistic to CCR5 and/or anti-IL-23p19 can reduce airway inflammation in asthmatic mice, most likely through inhibition of the IL-23/Th17 signaling pathway, and the HY peptide can alleviate inflammation not only through the IL-23/Th17 pathway but also through other mechanisms that result in the regulation of inflammation.

Published

2020

9. A Lightweight Convolutional Neural Network for Real-Time Facial Expression Detection

Author

Wenqian Shi, Ning Zhou, and Renyu Liang

Subjects

General Computer Science, Computer science, Emotion classification, Feature extraction, real-time, 02 engineering and technology, Convolutional neural network, Facial recognition system, 030218 nuclear medicine & medical imaging, lightweight CNN, 03 medical and health sciences, 0302 clinical medicine, 0202 electrical engineering, electronic engineering, information engineering, General Materials Science, Face detection, Facial expression, Artificial neural network, business.industry, 020208 electrical & electronic engineering, General Engineering, Pattern recognition, expression detection, Kernel (image processing), Feature (computer vision), Artificial intelligence, lcsh:Electrical engineering. Electronics. Nuclear engineering, business, lcsh:TK1-9971

Abstract

In this paper our group proposes and designs a lightweight convolutional neural network (CNN) for detecting facial emotions in real-time and in bulk to achieve a better classification effect. We verify whether our model is effective by creating a real-time vision system. This system employs multi-task cascaded convolutional networks (MTCNN) to complete face detection and transmit the obtained face coordinates to the facial emotions classification model we designed firstly. Then it accomplishes the task of emotion classification. Multi-task cascaded convolutional networks have a cascade detection feature, one of which can be used alone, thereby reducing the occupation of memory resources. Our expression classification model employs Global Average Pooling to replace the fully connected layer in the traditional deep convolution neural network model. Each channel of the feature map is associated with the corresponding category, eliminating the black box characteristics of the fully connected layer to a certain extent. At the same time, our model marries the residual modules and depth-wise separable convolutions, reducing large quantities of parameters and making the model more portable. Finally, our model is tested on the FER-2013 dataset. It only takes 3.1% of the 16GB memory, that is, only 0.496GB memory is needed to complete the task of classifying facial expressions. Not only can our model be stored in an 872.9 kilobytes file, but also its accuracy has reached 67% on the FER-2013 dataset. And it has good detection and recognition effects on those figures which are out of the dataset.

Published

2021

10. TextRank Keyword Extraction Algorithm Using Word Vector Clustering Based on Rough Data-Deduction

Author

Ning Zhou, Wenqian Shi, Renyu Liang, and Na Zhong

Subjects

Article Subject, General Computer Science, Knowledge Bases, General Mathematics, General Neuroscience, Computer applications to medicine. Medical informatics, R858-859.7, Neurosciences. Biological psychiatry. Neuropsychiatry, General Medicine, Cluster Analysis, Algorithms, Problem Solving, Research Article, RC321-571

Abstract

When TextRank algorithm based on graph model constructs graph associative edges, the co-occurrence window rules only consider the relationships between local terms. Using the information in the document itself is limited. In order to solve the above problems, an improved TextRank keyword extraction algorithm based on rough data reasoning combined with word vector clustering, RDD-WRank, was proposed. Firstly, the algorithm uses rough data reasoning to mine the association between candidate keywords, expands the search scope, and makes the results more comprehensive. Then, based on Wikipedia online open knowledge base, word embedding technology is used to integrate Word2Vec into the improved algorithm, and the word vector of TextRank lexical graph nodes is clustered to adjust the voting importance of nodes in the cluster. Compared with the traditional TextRank algorithm and the Word2Vec algorithm combined with TextRank, the experimental results show that the improved algorithm has significantly improved the extraction accuracy, which proves that the idea of using rough data reasoning can effectively improve the performance of the algorithm to extract keywords.

Published

2022

11. Natural variation of the Dt2 promoter controls plant height and node number in semi-determinant soybean

Author

Chunmei Liao, Hui Yang, Tong Su, Chao Fang, Hao Du, Yanping Wang, Baohui Liu, Lixin Ma, Tai Li, Lingping Kong, Milan He, Shichen Li, Xiaohui Zhao, Bize Yang, Linnan Chen, Wenqian Shi, Cen Yang, Lingshuang Wang, Yongli Li, Fanjiang Kong, Sijia Lu, and Kun Kou

Subjects

Genetics, Candidate gene, education.field_of_study, Population, food and beverages, Single-nucleotide polymorphism, Plant Science, Quantitative trait locus, Biology, Article, Polymorphism (computer science), Allele, education, Indel, Agronomy and Crop Science, Molecular Biology, Gene, Biotechnology

Abstract

Soybean (Glycine max (L.) Merrill) is an important legume crop worldwide. Plant height (PH) is a quantitative trait that is closely related to node number (NN) and internode length (IL) on the main stem, which together affect soybean yield. To identify candidate genes controlling these three traits in soybean, we examined a recombinant inbred line (RIL) population derived from a cross between two soybean varieties with semi-determinate stems (Dt1Dt1Dt2Dt2), JKK378 and HXW. A quantitative trait locus (QTL) named qPH18 was identified that simultaneously controls PH, NN, and IL; this region harbors the semi-determinant gene Dt2. Sequencing of the Dt2 promoter from JKK378 identified three polymorphisms relative to HXW, including two single nucleotide polymorphism (SNPs) and an 18-bp insertion/deletion polymorphism (Indel). Dt2 expression was lower in the qPH18(JKK378) group than in the qPH18(HXW) group, whereas the expression level of the downstream gene Dt1 showed the opposite tendency. A transient transfection assay confirmed that Dt2 promoter activity is lower in JKK378 compared to HXW. We propose that the polymorphisms in the dominant Dt2 promoter underlie the differences in Dt2 expression and its downstream gene Dt1 in the two parents, thereby affecting PH, NN, IL, and grain weight per plant without altering stem growth habit. Compared to the PH18(HXW) allele, the qPH18(JKK378) allele suppresses Dt2 expression, which releases the inhibition of Dt1 expression, thus enhancing NN and grain yield. Our findings shed light on the mechanism underlying NN and PH in soybean and provide a molecular marker to facilitate breeding. SUPPLEMENTARY INFORMATION: The online version contains supplementary material available at 10.1007/s11032-021-01235-y.

Published

2021

12. Antagonistic Peptides That Specifically Bind to the First and Second Extracellular Loops of CCR5 and Anti-IL-23p19 Antibody Reduce Airway Inflammation by Suppressing the IL-23/Th17 Signaling Pathway

Author

Yingqiang Zhong, Wenqian Shi, Aicen Xie, Rongrong Liang, Yingli Zhang, and Huarong Huang

Subjects

Article Subject, Receptors, CCR5, Immunology, Inflammation, Spleen, Allergic inflammation, Mice, Protein Domains, medicine, Interleukin 23, Extracellular, Pathology, RB1-214, Animals, Databases, Protein, Mice, Inbred BALB C, biology, Chemistry, Cell Biology, Mucus, Asthma, Ovalbumin, Disease Models, Animal, medicine.anatomical_structure, biology.protein, Interleukin-23 Subunit p19, Th17 Cells, Female, medicine.symptom, Antibody, Peptides, Research Article, Protein Binding, Signal Transduction

Abstract

Asthma is a heterogeneous chronic inflammatory disorder of the airways with a complex etiology, which involves a variety of cells and cellular components. Therefore, the aim of the study was to investigate the effects and mechanisms of antagonistic peptides that specifically bind to the first and second extracellular loops of CCR5 (GH and HY peptides, respectively) and anti-interleukin-23 subunit p19 (anti-IL-23p19) in the airway and thereby mediate inflammation and the IL-23/T helper 17 (Th17) cell pathway in asthmatic mice. An experimental asthma model using BALB/c mice was induced by ovalbumin (OVA) and treated with peptides that are antagonistic to CCR5 or with anti-IL-23p19. The extents of the asthmatic inflammation and mucus production were assessed. In addition, bronchoalveolar lavage fluid (BALF) was collected, the cells were counted, and the IL-4 level was detected by ELISA. The IL-23/Th17 pathway-related protein and mRNA levels in the lung tissues were measured, and the positive production rates of Th17 cells in the thymus, spleen, and peripheral blood were detected. The groups treated with one of the two peptides and/or anti-IL-23p19 showed significant reductions in allergic inflammation and mucus secretion; decreased expression levels of IL-23p19, IL-23R, IL-17A and lactoferrin (LTF); and reduced proportions of Th17 cells in the thymus, spleen, and peripheral blood. Specifically, among the four treatment groups, the anti-IL-23p19 with HY peptide group exhibited the lowest positive production rate of Th17 cells. Our data also showed a significant and positive correlation between CCR5 and IL-23p19 protein expression. These findings suggest that the administration of peptides antagonistic to CCR5 and/or anti-IL-23p19 can reduce airway inflammation in asthmatic mice, most likely through inhibition of the IL-23/Th17 signaling pathway, and the HY peptide can alleviate inflammation not only through the IL-23/Th17 pathway but also through other mechanisms that result in the regulation of inflammation.

Published

2020