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1. Oridonin attenuates atherosclerosis by inhibiting foam macrophage formation and inflammation through FABP4/PPARγ signalling.

Author

Zhang, Ming, Hou, Lianjie, Tang, Wanying, Lei, Weixing, Lin, Huiling, Wang, Yu, Long, Haijiao, Lin, Shuyun, Chen, Zhi, Wang, Guangliang, and Zhao, Guojun

Subjects
ATP-binding cassette transporters, NUCLEAR receptors (Biochemistry), PEROXISOME proliferator-activated receptors, ATHEROSCLEROSIS, FOAM, MACROPHAGES, CARDIOVASCULAR diseases, CARDIOVASCULAR disease related mortality
Abstract

Both lipid accumulation and inflammatory response in lesion macrophages fuel the progression of atherosclerosis, leading to high mortality of cardiovascular disease. A therapeutic strategy concurrently targeting these two risk factors is promising, but still scarce. Oridonin, the bioactive medicinal compound, is known to protect against inflammatory response and lipid dysfunction. However, its effect on atherosclerosis and the underlying molecular mechanism remain elusive. Here, we showed that oridonin attenuated atherosclerosis in hyperlipidemic ApoE knockout mice. Meanwhile, we confirmed the protective effect of oridonin on the oxidized low‐density lipoprotein (oxLDL)‐induced foam macrophage formation, resulting from increased cholesterol efflux, as well as reduced inflammatory response. Mechanistically, the network pharmacology prediction and further experiments revealed that oridonin dramatically facilitated the expression of peroxisome proliferator‐activated receptor gamma (PPARγ), thereby regulating liver X receptor‐alpha (LXRα)‐induced ATP‐binding cassette transporter A1 (ABCA1) expression and nuclear factor NF‐kappa‐B (NF‐κB) translocation. Antagonist of PPARγ reversed the cholesterol accumulation and inflammatory response mediated by oridonin. Besides, RNA sequencing analysis revealed that fatty acid binding protein 4 (FABP4) was altered responding to lipid modulation effect of oridonin. Overexpression of FABP4 inhibited PPARγ activation and blunted the benefit effect of oridonin on foam macrophages. Taken together, oridonin might have potential to protect against atherosclerosis by modulating the formation and inflammatory response in foam macrophages through FABP4/PPARγ signalling. [ABSTRACT FROM AUTHOR]

Published
2023
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2. Macrophage Gpx4 deficiency aggravates foam cell formation by regulating the expression of scavenger receptors, ABCA1, and ABCG1.

Author

Zhou, Jingquan, Wu, Suhua, Chen, Xiaoqin, Hou, Lianjie, Zhong, Qiong, Luo, Weixia, Dai, Chunni, and Dai, Xiaoyan

Subjects
FOAM cells, MACROPHAGES, GLUTATHIONE peroxidase, OXIDATIVE stress, ENDOTHELIN receptors, LOW density lipoproteins, LOW density lipoprotein receptors
Abstract

Macrophage‐derived foam cell formation is critical for the initiation and development of atherosclerosis, which contributes to atherosclerotic cardiovascular disease (ASCVD). Glutathione peroxidase 4 (GPX4), a crucial ferroptosis regulator, protects cells from excessive oxidative stress by neutralizing lipid peroxidation. However, the role of macrophage GPX4 in foam cell formation remains unknown. We reported that oxidized low‐density lipoprotein (oxLDL) upregulated GPX4 expression in macrophages. Using the Cre‐loxP system, we generated myeloid cell‐specific Gpx4 knockout (Gpx4myel‐KO) mice. Bone marrow‐derived macrophages (BMDMs) were isolated from WT and Gpx4myel‐KO mice and incubated with modified low‐density lipoprotein (LDL). We found that Gpx4 deficiency promoted foam cell formation and increased the internalization of modified LDL. Mechanistic studies unveiled that Gpx4 knockout upregulated scavenger receptor type A and LOX‐1 expression and downregulated ABCA1 and ABCG1 expression. Collectively, our study lends a novel insight into the role of GPX4 in suppressing macrophage‐derived foam cell formation and suggests GPX4 as a promising therapeutic target to interfere with atherosclerosis‐related diseases. [ABSTRACT FROM AUTHOR]

Published
2023
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4. Exploring the Unique Characteristics of High-Pore-Volume Waterflooding and Enhanced Oil Recovery Mechanisms in Offshore Sandstone Reservoirs Using Nuclear Magnetic Resonance Technology.

Author

Liu, Junrong, Li, Hangyu, Xu, Jianchun, Liu, Shuyang, Liu, Rongjiang, Hou, Lianjie, and Tan, Qizhi

Subjects
ENHANCED oil recovery, NUCLEAR magnetic resonance, OIL field flooding, POROSITY, SANDSTONE
Abstract

Simple Summary: The characteristics of high-pore-volume (high-PV) waterflooding and the mechanisms of enhanced oil recovery (EOR) are unclear. an experiment was conducted using nuclear magnetic resonance (NMR) technology-assisted waterflooding to monitor oil migration and pore structure changes during the displacement process. We quantified the ultimate oil displacement efficiency waterflooding and microscopic oil recovery at the pore scale. Additionally, the variations in petrophysical properties seen during this process were analyzed. The experiment revealed that the high-PV displacement process had a high EOR effect, even in the ultrahigh water cut stage. During this period, oil production came mainly from the mesopores. Furthermore, flooding changed the rock structure, increasing the pore volume. However, these changes were inconsistent at both the pore scale and spatial scale. At the pore scale, the volume of macropores decreased, while that of the micropores and mesopores increased. At the spatial scale, the porosity and the average pore size at the front end increased, while those at the back end decreased due to particle migration during flooding. Our findings suggested that pore structure variations at the front ends of experimental cores were representative of those in reservoirs, indicating that high-PV waterflooding could increase the permeabilities of reservoirs. A single paragraph of about 200 words maximum. For research articles, abstracts should give a pertinent overview of the work. We strongly encourage authors to use the following style of structured abstracts, but without headings: (1) Background: Place the question addressed in a broad context and highlight the purpose of the study; (2) Methods: briefly describe the main methods or treatments applied; (3) Results: summarize the article's main findings; (4) Conclusions: indicate the main conclusions or interpretations. The abstract should be an objective representation of the article and it must not contain results that are not presented and substantiated in the main text and should not exaggerate the main conclusions. [ABSTRACT FROM AUTHOR]

Published
2023
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6. Numerical Simulation of the Enrichment of Chemotactic Bacteria in Oil-Water Two-Phase Transfer Fields of Heterogeneous Porous Media.

Author

Wang, Xiaopu, Hou, Lianjie, He, Tianhao, Diao, Zhenhan, Yao, Chuanjin, Long, Tao, and Fan, Ling

Subjects
NONAQUEOUS phase liquids, POROUS materials, OIL-water interfaces, OIL spills, TWO-phase flow, PETROLEUM
Abstract

Oil pollution in soil-groundwater systems is difficult to remove, and a large amount of residual oil is trapped in the low permeable layer of the heterogeneous aquifer. Aromatic hydrocarbons in oil have high toxicity and low solubility in water, which are harmful to the ecological environment. Chemotactic degrading bacteria can perceive the concentration gradient of non-aqueous phase liquid (NAPL) pollutants in the groundwater environment, and enrich and proliferate around the pollutants, thus achieving a more efficient and thorough remediation effect. However, the existing theoretical models are relatively simple. The physical fields of oil–water two-phase flow and oil-phase solute convection and diffusion in water are not coupled, which further restricts the accuracy of studies on bacterial chemotaxis to NAPL. In this study, geometric models based on the actual microfluidic experimental study were constructed. Based on the phase field model, diffusion convection equation and chemotaxis velocity equation, the effects of heterogeneity of porous media, wall wettability and groundwater flow rate on the residual oil and the concentration distribution of chemotaxis bacteria were studied. Under all of the simulation conditions, the residual oil in the high permeable area was significantly lower than that in the low permeable area, and the wall hydrophilicity enhanced the water flooding effect. Chemotactic bacteria could react to the concentration gradient of pollutants dissolved into water in the oil phase, and enrich near the oil–water interface with high concentration of NAPL, and the density of chemotactic bacteria at the oil–water interface can be up to 1.8–2 times higher than that in the water phase at flow rates from 1.13 to 6.78 m/d. [ABSTRACT FROM AUTHOR]

Published
2022
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7. Dihydromyricetin resists inflammation‐induced muscle atrophy via ryanodine receptor‐CaMKK‐AMPK signal pathway.

Author

Hou, Lianjie, Jiang, Fangyi, Huang, Bo, Zheng, Weijie, Jiang, Yufei, Cai, Gengyuan, Liu, Dewu, Hu, Ching Yuan, and Wang, Chong

Subjects
MUSCULAR atrophy, CELLULAR signal transduction, SKELETAL muscle, RYANODINE receptors, RYANODINE, INSULIN sensitivity, DISABILITIES
Abstract

Skeletal muscle plays a pivotal role in the maintenance of physical and metabolic health. Skeletal muscle atrophy usually results in physical disability, inferior quality of life and higher health care costs. The higher incidence of muscle atrophy in obese and ageing groups is due to increased levels of inflammatory factors during obesity and ageing. Dihydromyricetin, as a bioactive polyphenol, has been used for anti‐inflammatory, anti‐tumour and improving insulin sensitivity. However, there are no published reports demonstrated the dihydromyricetin effect on inflammation‐induced skeletal muscle atrophy. In this study, we first confirmed the role of dihydromyricetin in inflammation‐induced skeletal muscle atrophy in vivo and in vitro. Then, we demonstrated that dihydromyricetin resisted inflammation‐induced skeletal muscle atrophy by activating Ca2+‐CaMKK‐AMPK through signal pathway blockers, Ca2+ probes and immunofluorescence. Finally, we clarified that dihydromyricetin activated Ca2+‐CaMKK‐AMPK signalling pathway through interaction with the ryanodine receptor, its target protein, by drug affinity responsive target stability (DARTS). Our results not only demonstrated that dihydromyricetin resisted inflammation‐induced muscle atrophy via the ryanodine receptor‐CaMKK‐AMPK signal pathway but also discovered that the target protein of dihydromyricetin is the ryanodine receptor. Our results provided experimental data for the development of dihydromyricetin as a functional food and new therapeutic strategies for treating or preventing skeletal muscle atrophy. [ABSTRACT FROM AUTHOR]

Published
2021
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10. MiR-92b-3p inhibits proliferation and migration of C2C12 cells.

Author

Ye, Zijian, Shi, Jia, Ning, Zuocheng, Hou, Lianjie, Hu, Ching Yuan, and Wang, Chong

Subjects
CELL migration, MUSCLE growth, CELL proliferation, SKELETAL muscle, CELL differentiation
Abstract

Skeletal muscle, a critical component of the mammalian body, is essential for normal body movement. miRNAs are well documented in gene post-transcription regulation in many biological processes, including muscle development and maintenance. miR-92b-3p, which is often associated with tumorigenesis, has never been explored in myoblast development. Here, we used murine-derived C2C12 myoblasts to explore the potential functions of miR-92b-3p in skeletal muscle development. Our results demonstrated that miR-92b-3p mimics inhibited C2C12 cell proliferation and migration, whereas miR-92b-3p inhibitor promoted C2C12 cell proliferation and migration. C2C12 cell differentiation was not affected by miR-92b-3p mimics, according to immunofluorescence and qPCR results. Serum- and glucocorticoid-induced kinase 3 (SGK3) was predicted and validated as a target of miR-92b-3p. Overexpression of SGK3 promoted C2C12 cell proliferation. SGK3 and miR-92b-3p formed a regulatory pathway to modulate C2C12 cell proliferation. In conclusion, miR-92b-3p inhibited C2C12 cell proliferation by targeting SGK3 and impeded C2C12 cell migration. [ABSTRACT FROM AUTHOR]

Published
2020
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11. MiR-339 attenuates LPS-induced intestinal epithelial cells inflammatory responses and apoptosis by targeting TLR4.

Author

Xie, Meiying, Zhang, Lina, Li, Luoye, Fan, Minhuan, and Hou, Lianjie

Abstract

Background: Intestinal epithelial cells are important for defending against pathogen infection. LPS is an endotoxin that is highly antigenic and cytotoxic produced by bacteria. LPS disrupts the intestine epithelium integrity and induced the intestinal epithelial cell inflammation and apoptosis. Our previous study has predicted the function of exosome miRNAs through bioinformatics analysis, and we found that miR-339 had a potential function in cell inflammation response. To our knowledge, no published paper has demonstrated the miR-339 function in protecting the intestine epithelium against bacterial infection. Objective: The objective of this study is to evaluate the miR-339 function in regulating intestinal epithelial cells to defend against bacterial infection through biological experiments and bioinformatics analyses. Methods: Through the miR-339 transfection experiment and TLR4 interfering experiment, we evaluated the function of miR-339 and TLR4 in the process of inflammatory responses and apoptosis. Through Bioinformatics analyses and dual-luciferase reporter experiment, we identified the target gene of miR-339. Results: miR-339 attenuates LPS-induced intestinal epithelial cells inflammatory responses through the TLR4/NF-κB signaling pathway and inhibited LPS-induced apoptosis through the P53 signaling pathway. TLR4 is the target gene of miR-339. TLR4 reduced LPS-induced proinflammatory responses and apoptosis. Conclusions: In conclusion, miR-339 protected the intestine epithelial cells from LPS-induced cell inflammation and apoptosis through targeting TLR4. This study expanded our understanding of how miRNAs and genes work collaboratively in regulating intestinal epithelial cells to defend against bacterial infection. [ABSTRACT FROM AUTHOR]

Published
2020
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12. Whole genome sequence analysis reveals genetic structure and X-chromosome haplotype structure in indigenous Chinese pigs.

Author

Tong, Xiong, Hou, Lianjie, He, Weiming, Mei, Chugang, Huang, Bo, Zhang, Chi, Hu, Chingyuan, and Wang, Chong

Subjects
GENOMES, SEQUENCE analysis, HAPLOTYPES, PHYLOGENY, X chromosome
Abstract

Chinese indigenous pigs exhibit considerable phenotypic diversity, but their population structure and the genetic basis of agriculturally important traits need further exploration. Here, we sequenced the whole genomes of 24 individual pigs representing 22 breeds distributed throughout China. For comparison with European and commercial breeds (one pig per breed), we included seven published pig genomes with our new genomes for analyses. Our results showed that breeds grouped together based on morphological classifications are not necessarily more genetically similar to each other than to breeds from other groups. We found that genetic material from European pigs likely introgressed into five Chinese breeds. We have identified two new subpopulations of domestic pigs that encompass morphology-based criteria in China. The Southern Chinese subpopulation comprises the classical South Chinese Type and part of the Central China Type. In contrast, the Northern Chinese subpopulation comprises the North China Type, the Lower Yangtze River Basin Type, the Southwest Type, the Plateau Type, and the remainder of the Central China Type. Eight haplotypes and two recombination sites were identified within a conserved 40.09 Mb linkage-disequilibrium (LD) block on the X chromosome. Potential candidate genes (LEPR, FANCC, COL1A1, and PCCA) influencing body size were identified. Our findings provide insights into the phylogeny of Chinese indigenous pig breeds and benefit gene mining efforts to improve major economic traits. [ABSTRACT FROM AUTHOR]

Published
2020
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13. PRDM16 Represses the Pig White Lipogenesis through Promoting Lipolysis Activity.

Author

Gu, Ting, Xu, Guli, Jiang, Chengfeng, Hou, Lianjie, Wu, Zhenfang, and Wang, Chong

Subjects
FAT cells, LIPID metabolism, MITOCHONDRIAL physiology, ANIMAL experimentation, CELL differentiation, GENE expression, STAINS & staining (Microscopy), SWINE, TRANSFERASES, TRIGLYCERIDES, WESTERN immunoblotting, DNA-binding proteins, OXIDATIVE stress, PHYSIOLOGY
Abstract

The positive regulatory domain containing 16 (PRDM16) gene is a dominant transcriptional regulator that favors the "browning" of white adipocytes in rodents. Since the "browning" of white fat is important in pig in terms of producing heat fighting against cold environment, avoiding obesity, and improving meat quality, understanding the critical role that PRDM16 gene played in pig adipose "browning" and energy metabolism is of great significance. However, the constitution of pig fat differs a lot from rodents and human as they do not have brown adipose tissue (BAT) even in the newborn piglets. In this study, we isolated porcine primary preadipocytes and investigated the function of PRDM16 during preadipocytes differentiation. Our results showed that overexpression of the PR domain of PRDM16 repressed the differentiation of porcine preadipocytes, indicated by oil red O staining and the deposition of the triglyceride. Overexpression of the PR domain significantly increased the level of lipolysis and mitochondrial oxidative capacity detected by Western blotting during differentiation. Furthermore, we purified the protein coded by the PR domain and demonstrated that this protein has the H3K9me1 methyltransferase activity. In conclusion, the PR domain of the porcine PRDM16 gene repressed the mature of the porcine preadipocytes by promoting its oxidative activity. [ABSTRACT FROM AUTHOR]

Published
2019
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14. Browning of Pig White Preadipocytes by Co-Overexpressing Pig PGC-1α and Mice UCP1.

Author

Hou, Lianjie, Xie, Meiying, Cao, Lingbo, Shi, Jia, Xu, Guli, Hu, Chingyuan, and Wang, Chong

Subjects
BROWN adipose tissue, FAT cells, OXIDATIVE phosphorylation, IMMUNOPRECIPITATION, ALTERNATIVE treatment for obesity, BODY temperature regulation, PHYSIOLOGY
Abstract

Background/Aims: Brown adipose tissue (BAT) is critical for mammals’ survival in the cold environment. BAT-dependent non-shivering thermogenesis is attributed to uncoupling protein 1 (UCP1)’s disengagement of oxidative phosphorylation from ATP synthesis and dissipates energy as heat. Thus individuals with a substantial amount of BAT are better equipped during cold stress and less likely to become obese. Recently, our laboratory has shown pig adipocytes have no UCP1 protein. The inability of newborn piglets to generate heat contributed to its high death rate. Repairing the genetic defect of UCP1 in pig adipocytes has implications in defending against cold for piglets and developing an alternative treatment for human obesity. Methods: Q-PCR, western blotting (WB) and oxygen consumption measurement were used to enable functional UCP1 protein in preadipocytes. Immunoprecipitation (IP), chromatin immunoprecipitation (CHIP), and dual-luciferase reporter assay system were used to clarify the thermogenesis mechanism of functional UCP1. Results: Only co-overexpressing mice UCP1 and pig PGC-1α increased not only the mitochondrial number but also the uncoupled respiration rate in the transfected pig adipocytes. The functional mice UCP1 increased the pig PGC-1α activity through the AMPK-SIRT1 pathway. The active form PGC-1α interacted with transcription factors Lhx8, Zic1, ERRα, and PPARα to regulate the expression of mitochondrial energy metabolism and adipocytes browning-related genes. Conclusion: Our data suggest a model in which pig PGC-1α and mice UCP1 work collaboratively to restore uncoupling respiration in pig preadipocytes. These results have great implications for piglet survival and developing an alternative treatment for human obesity in the future. [ABSTRACT FROM AUTHOR]

Published
2018
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17. In vitro antiviral activity of germacrone against porcine parvovirus.

Author

Chen, Ye, Dong, Yunxia, Jiao, Yiren, Hou, Lianjie, Shi, Yuzhen, Gu, Ting, Zhou, Pei, Shi, Zhongyuan, Xu, Lulu, and Wang, Chong

Subjects
PARVOVIRUS diseases, ANTIVIRAL agents, MESSENGER RNA, VIRUS diseases in swine, PROTEIN synthesis, VIRAL replication, IN vitro studies, THERAPEUTICS
Abstract

Porcine parvovirus (PPV) infections can lead to significant losses to the swine industry by causing reproductive failure in pigs. Germacrone has been reported to efficiently suppress the replication of influenza virus. In this report, the antiviral activity of germacrone on PPV in swine testis (ST) cells was investigated. Here, we show for the first time that germacrone protects cells from PPV infection and suppresses the synthesis of viral mRNA and protein. Furthermore, we show that germacrone inhibits PPV replication at an early stage in a dose-dependent manner. These findings suggest that germacrone is a potential candidate for anti-PPV therapy. [ABSTRACT FROM AUTHOR]

Published
2015
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18. PFN2a Suppresses C2C12 Myogenic Development by Inhibiting Proliferation and Promoting Apoptosis via the p53 Pathway.

Author

Li, Huaqin, Hou, Lianjie, Zhang, Yu, Jiang, Fangyi, Zhu, Yifan, Li, Qing X., Hu, Ching Yuan, and Wang, Chong

Subjects
MYOBLASTS, APOPTOSIS, HISTONE deacetylase, P53 protein, SKELETAL muscle, TUMOR growth
Abstract

Skeletal muscle plays a crucial role in physical activity and in regulating body energy and protein balance. Myoblast proliferation, differentiation, and apoptosis are indispensable processes for myoblast myogenesis. Profilin 2a (PFN2a) is a ubiquitous actin monomer-binding protein and promotes lung cancer growth and metastasis through suppressing the nuclear localization of histone deacetylase 1 (HDAC1). However, how PFN2a regulates myoblast myogenic development is still not clear. We constructed a C2C12 mouse myoblast cell line overexpressing PFN2a. The CRISPR/Cas9 system was used to study the function of PFN2a in C2C12 myogenic development. We find that PFN2a suppresses proliferation and promotes apoptosis and consequentially downregulates C2C12 myogenic development. The suppression of PFN2a also decreases the amount of HDAC1 in the nucleus and increases the protein level of p53 during C2C12 myogenic development. Therefore, we propose that PFN2a suppresses C2C12 myogenic development via the p53 pathway. Si-p53 (siRNA-p53) reverses the PFN2a inhibitory effect on C2C12 proliferation and the PFN2a promotion effect on C2C12 apoptosis, and then attenuates the suppression of PFN2a on myogenic differentiation. Our results expand understanding of PFN2a regulatory mechanisms in myogenic development and suggest potential therapeutic targets for muscle atrophy-related diseases. [ABSTRACT FROM AUTHOR]

Published
2019
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19. MiR-501-3p Forms a Feedback Loop with FOS, MDFI, and MyoD to Regulate C2C12 Myogenesis.

Author

Hou, Lianjie, Zhu, Linhui, Li, Huaqin, Jiang, Fangyi, Cao, Lingbo, Hu, Ching Yuan, and Wang, Chong

Subjects
MYOBLASTS, MYOGENESIS, SKELETAL muscle, MUSCLE growth, MUSCLE mass, MEDICAL care costs
Abstract

Skeletal muscle plays an essential role in maintaining body energy homeostasis and body flexibility. Loss of muscle mass leads to slower wound healing and recovery from illness, physical disability, poor quality of life, and higher health care costs. So, it is critical for us to understand the mechanism of skeletal muscle myogenic differentiation for maintaining optimal health throughout life. miR-501-3p is a novel muscle-specific miRNA, and its regulation mechanism on myoblast myogenic differentiation is still not clear. We demonstrated that FOS was a direct target gene of miR-501-3p, and MyoD regulated miR-501-3p host gene Clcn5 through bioinformatics prediction. Our previous laboratory experiment found that MDFI overexpression promoted C2C12 myogenic differentiation and MyoD expression. The database also showed there is an FOS binding site in the MDFI promoter region. Therefore, we hypothesize that miR-501-3p formed a feedback loop with FOS, MDFI, and MyoD to regulate myoblast differentiation. To validate our hypothesis, we demonstrated miR-501-3p function in the proliferation and differentiation period of C2C12 cells by transfecting cells with miR-501-3p mimic and inhibitor. Then, we confirmed there is a direct regulatory relationship between miR-501-3p and FOS, MyoD and miR-501-3p, FOS and MDFI through QPCR, dual-luciferase reporter system, and ChIP experiments. Our results not only expand our understanding of the muscle myogenic development mechanism in which miRNA and genes participate in controlling skeletal muscle development, but also provide treatment strategies for skeletal muscle or metabolic-related diseases in the future. [ABSTRACT FROM AUTHOR]

Published
2019
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