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149 results on '"Jiang Hesheng"'

1. JUNB mediates oxaliplatin resistance via the MAPK signaling pathway in gastric cancer by chromatin accessibility and transcriptomic analysis

Author

Li Suyao, Wei Yichou, Sun Xun, Liu Mengling, Zhu Mengxuan, Yuan Yitao, Zhang Jiayu, Dong Yu, Hu Keshu, Ma Sining, Zhang Xiuping, Xu Bei, Jiang Hesheng, Gan Lu, and Liu Tianshu

Subjects
gastric cancer, JUNB, ATAC-seq, oxaliplatin resistance, MAPK signaling pathway, chromatin accessibility, Biochemistry, QD415-436, Genetics, QH426-470
Abstract

Currently, platinum-containing regimens are the most commonly used regimens for advanced gastric cancer patients, and chemotherapy resistance is one of the main reasons for treatment failure. Thus, it is important to reveal the mechanism of oxaliplatin resistance and to seek effective intervention strategies to improve chemotherapy sensitivity, thereby improving the survival and prognosis of gastric cancer patients. To understand the molecular mechanisms of oxaliplatin resistance, we generate an oxaliplatin-resistant gastric cancer cell line and conduct assay for transposase-accessible chromatin sequencing (ATAC-seq) and RNA sequencing (RNA-seq) for both parental and oxaliplatin-resistant AGS cells. A total of 3232 genomic regions are identified to have higher accessibility in oxaliplatin-resistant cells, and DNA-binding motif analysis identifies JUNB as the core transcription factor in the regulatory network. JUNB is overexpressed in oxaliplatin-resistant gastric cancer cells, and its upregulation is associated with poor prognosis in gastric cancer patients, which is validated by our tissue microarray data. Moreover, chromatin immunoprecipitation sequencing (ChIP-seq) analysis reveals that JUNB binds to the transcriptional start site of key genes involved in the MAPK signaling pathway. Knockdown of JUNB inhibits the MAPK signaling pathway and restores sensitivity to oxaliplatin. Combined treatment with the ERK inhibitor piperlongumine or MEK inhibitor trametinib effectively overcomes oxaliplatin resistance. This study provides evidence that JUNB mediates oxaliplatin resistance in gastric cancer by activating the MAPK pathway. The combination of MAPK inhibitors with oxaliplatin overcomes resistance to oxaliplatin, providing a promising treatment opportunity for oxaliplatin-resistant gastric cancer patients.

Published
2023
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2. Negative correlation between acetyl-CoA acyltransferase 2 and cetuximab resistance in colorectal cancer

Author

Yuan Yitao, Sun Xun, Liu Mengling, Li Suyao, Dong Yu, Hu Keshu, Zhang Jiayu, Xu Bei, Ma Sining, Jiang Hesheng, Hou Pengcong, Lin Yufu, Gan Lu, and Liu Tianshu

Subjects
colorectal cancer, cetuximab resistance, ACAA2, Kras mutation, Biochemistry, QD415-436, Genetics, QH426-470
Abstract

The emergence of anti-EGFR therapy has revolutionized the treatment of colorectal cancer (CRC). However, not all patients respond consistently well. Therefore, it is imperative to conduct further research to identify the molecular mechanisms underlying the development of cetuximab resistance in CRC. In this study, we find that the expressions of many metabolism-related genes are downregulated in cetuximab-resistant CRC cells compared to their sensitive counterparts. Specifically, acetyl-CoA acyltransferase 2 (ACAA2), a key enzyme in fatty acid metabolism, is downregulated during the development of cetuximab resistance. Silencing of ACAA2 promotes proliferation and increases cetuximab tolerance in CRC cells, while overexpression of ACAA2 exerts the opposite effect. RTK-Kras signaling might contribute to the downregulation of ACAA2 expression in CRC, and ACAA2 predicts CRC prognosis in patients with Kras mutations. Collectively, our data suggest that modulating ACAA2 expression contributes to secondary cetuximab resistance in Kras wild-type CRC patients. ACAA2 expression is related to Kras mutation and demonstrates a prognostic role in CRC patients with Kras mutation. Thus, ACAA2 is a potential target in CRC with Kras mutation.

Published
2023
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4. Development of pan-specific antibody against trimethyllysine for protein research

Author

Xiao Hao, Jiang Hesheng, Li Lin Hong, Wong Ronald PC, Liang Ziqian, and Li Gang

Subjects
Cytology, QH573-671
Abstract

Abstract Background Trimethylation of the Nε-lysine residues in a protein is one of the most important events of posttranslational modifications. Simple methods for rapid detection and isolation of the Nε-trimethylated protein species are needed. This report introduces a novel method to prepare the affinity purified antibody specific for the Nε-trimethylated lysine (tMeK). The applications of the purified antibody are also reported in this paper. Methods We generated the methylated keyhole limpet heomocyanin (KLH) under controlled chemical methylation reaction using CH3I and used it as an immunogen to raise anti-methylated lysine antibodies. The tMeK specific antibody was selectively isolated using a two-step affinity chromatography in which the mMeK/dMeK specific antibodies were removed and the tMeK specific antibody was captured. Finally, the eluted anti-tMeK antibody was characterized. Results The ELISA results indicated that the antibody reacted only to tMeK but not to mono- and dimethyllysine. Western-blot results showed that the Nε-trimethylated proteins were detected in both animal tissue and cultured cells and that the antibody signal could be competitively inhibited with free tMeK. Conclusion The specific tMeK antibody we developed is useful for one-step isolation of proteins with Nε-trimethyllysine residues and also for the detection, identification and localization of proteins with trimethyllysine residues in the cells.

Published
2008
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9. PROX1-mediated epigenetic silencing of SIRT3 contributes to proliferation and glucose metabolism in colorectal cancer

Author

Gan, Lu, primary, Li, Qingguo, additional, Nie, Wei, additional, Zhang, Yi, additional, Jiang, Hesheng, additional, Tan, Cong, additional, Zhang, Long, additional, Zhang, Jieyun, additional, Li, Qian, additional, Hou, Pengcong, additional, Yuan, Yitao, additional, Sun, Xun, additional, Liu, Dongmei, additional, Sheng, Weiqi, additional, Liu, Tianshu, additional, Xu, Midie, additional, and Guo, Weijian, additional

Published
2023
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28. China at the Crossroads: The Economics of Tobacco and Health

Author

Hu, Teh-wei, primary, Mao, Zhengzhong, additional, Ong, Michael, additional, Tong, Elisa, additional, Tao, Ming, additional, Jiang, Hesheng, additional, Hammond, Katharine, additional, Smith, Kirk R, additional, de Beyer, Joy, additional, and Yurekli, Ayda, additional

Published
2008
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35. Dosage Compensation and Gene Expression of the X Chromosome in Sheep

Author

Duan, Jingyue (Ellie), primary, Flock, Kaleigh, additional, Jue, Nathanial, additional, Zhang, Mingyuan, additional, Jones, Amanda, additional, Seesi, Sahar Al, additional, Mandoiu, Ion, additional, Pillai, Sambhu, additional, Hoffman, Maria, additional, O’Neill, Rachel, additional, Zinn, Steven, additional, Govoni, Kristen, additional, Reed, Sarah, additional, Jiang, Hesheng, additional, Jiang, Zongliang (Carl), additional, and Tian, Xiuchun (Cindy), additional

Published
2019
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36. Effects of maternal nutrition on the expression of genomic imprinted genes in ovine fetuses

Author

Duan, Jingyue (Ellie), primary, Zhang, Mingyuan, additional, Flock, Kaleigh, additional, Seesi, Sahar Al, additional, Mandoiu, Ion, additional, Jones, Amanda, additional, Johnson, Elizabeth, additional, Pillai, Sambhu, additional, Hoffman, Maria, additional, McFadden, Katelyn, additional, Jiang, Hesheng, additional, Reed, Sarah, additional, Govoni, Kristen, additional, Zinn, Steve, additional, Jiang, Zongliang, additional, and Tian, Xiuchun (Cindy), additional

Published
2018
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38. Production of Phytase Transgenic Porcine Blastocysts by Handmade Cloning

Author

Zhang, Mingyuan, primary, Yang, Haowen, additional, Gao, Jie, additional, Chen, Xiaoliang, additional, Chen, Shijin, additional, Huang, Yuemeng, additional, Wu, Yanjun, additional, Jiang, Qinyang, additional, Guo, Yafen, additional, Wei, Yingming, additional, Lin, Xiukun, additional, Lan, Ganqiu, additional, and Jiang, Hesheng, additional

Published
2018
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40. The role of government in tobacco leaf production in China: national and local interventions

Author

Hu, Teh-wei, Mao, Zhengzhong, Jiang, Hesheng, Tao, Ming, and Yurekli, Ayda

Subjects
China -- Economic policy, China -- Domestic policy, Administrative agencies -- Powers and duties, Tobacco products -- Usage, Market trend/market analysis, Government
Abstract

Byline: Teh-wei Hu, Zhengzhong Mao, Hesheng Jiang, Ming Tao, Ayda Yurekli China produces about one-third of the world's supply of tobacco leaf and is the largest consumer of cigarettes. Any discussion of tobacco control in China requires an understanding of the government's role in this sector because China's tobacco production and cigarette marketing are all under the control of the State Tobacco Monopoly Administration. Compared to other cash crops, tobacco leaf has the lowest economic rate of return. Currently, China has a large surplus of tobacco leaf. One of the factors contributing to this surplus is local governments' encouraging farmers to plant tobacco leaf, in part because of their incentive of collecting tax revenue from tobacco leaf sales.

Published
2007

47. Milk fat globule is an alternative to mammary epithelial cells for gene expression analysis in buffalo

Author

Chen, Qiuming, primary, Wu, Yanjun, additional, Zhang, Mingyuan, additional, Xu, Wenwen, additional, Guo, Xiaoping, additional, Yan, Xueyu, additional, Deng, Haiying, additional, Jiang, Qinyang, additional, Yang, Xiurong, additional, Lan, Ganqiu, additional, Guo, Yafen, additional, Qin, Guangsheng, additional, and Jiang, Hesheng, additional

Published
2016
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49. Assessment of M. longissimus fibre types and metabolic enzymes in Bama miniature pigs and Landrace swine.

Author

Chen, Baojian, Ao, Qiuwei, Chen, Shaomei, Wei, Yingming, Guo, Yafen, Lan, Ganqiu, Jiang, Qinyang, and Jiang, Hesheng

Subjects
LANDRACE swine, MEAT quality, SWINE breeding, LACTATE dehydrogenase, MESSENGER RNA
Abstract

Overt differences exist between Chinese local pigs and exotic pig breeds, especially in muscle growth rate and meat quality. However, the underlying molecular mechanisms remain unclear. This study aimed to assess muscle fibre types and metabolic enzymes in Bama miniature pigs and Landrace swine. Meat quality traits, including intramuscular fat content, and muscle colour, conductivity, and tenderness, were assessed in these pig breeds. Then, muscle fibre types were classified, and mRNA amounts and activities of lactate dehydrogenase (LDH), succinate dehydrogenase (SDH), and malate dehydrogenase (MDH) assessed, in M. longissimus from the two pig breeds, at various ages. Our data showed significantly higher back fat thickness, muscle conductivity, and intramuscular fat content in samples from Bama miniature pigs compared with the values obtained for Landrace pigs (p < .05). In addition, SDH activity was significantly higher, and LDH activity overtly lower in Bama pigs compared with Landrace swine (p < .05). Furthermore, myosin heavy-chain (MyHC) II A, II B, and II X mRNA levels in Bama miniature pigs at 180 were significantly higher than values obtained for Landrace pigs of the same age. Although MyHC I gene expression levels were similar in Bama miniature and Landrace pigs at 180 days of age, significantly higher amounts were obtained in 300 day old Bama miniature pigs compared with 180 day old Landrace pigs (p < .05). Collectively, these preliminary findings indicated that skeletal muscles from Bama miniature pigs may contain more oxidative fibres compared with those from Landrace pigs, which might explain the meat quality differences between the two pig breeds. [ABSTRACT FROM PUBLISHER]

Published
2018
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