Your search keyword '"Zeng, Zhaoyang"' showing total 25 results

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

Author

Lan, Jiaoli, Zhang, Yuxin, Jin, Cuiyuan, Chen, Huan, Su, Zexiong, Wu, Jiaxing, Ma, Ni, Zhang, Xiaoyan, Lu, Yiyun, Chen, Yongxin, Zeng, Xiaolu, Zhang, Huiqiong, Zheng, Guilang, Sun, Yueyu, Wang, Chun, Hu, Yan, Wang, Yifei, Liu, Yumei, Zeng, Zhaoyang, and Shi, Liyun

Subjects

GLYCOGEN storage disease, INFLAMMATORY bowel diseases, GUT microbiome, PATHOGENIC bacteria, EPITHELIAL cells

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. [ABSTRACT FROM AUTHOR]

Published

2024

2. METTL14 promotes lipid metabolism reprogramming and sustains nasopharyngeal carcinoma progression via enhancing m6A modification of ANKRD22 mRNA.

Author

Li, Lvyuan, Tang, Qiling, Ge, Junshang, Wang, Dan, Mo, Yongzhen, Zhang, Yijie, Wang, Yumin, Xiong, Fang, Yan, Qijia, Liao, Qianjin, Guo, Can, Wang, Fuyan, Zhou, Ming, Xiang, Bo, Zeng, Zhaoyang, Shi, Lei, Chen, Pan, and Xiong, Wei

Subjects

MESSENGER RNA, METABOLIC reprogramming, GENE expression, LIPID metabolism, LIPID synthesis

Abstract

Background: N6‐methyladenosine (m6A) modification is essential for modulating RNA processing as well as expression, particularly in the context of malignant tumour progression. However, the exploration of m6A modification in nasopharyngeal carcinoma (NPC) remains very limited. Methods: RNA m6A levels were analysed in NPC using m6A dot blot assay. The expression level of methyltransferase‐like 14 (METTL14) within NPC tissues was analysed from public databases as well as RT‐qPCR and immunohistochemistry. The influences on METTL14 expression on NPC proliferation and metastasis were explored via in vitro as well as in vivo functional assays. Targeted genes of METTL14 were screened using the m6A and gene expression profiling microarray data. Actinomycin D treatment and polysome analysis were used to detect the half‐life and translational efficiency of ANKRD22. Flow cytometry, immunofluorescence and immunoprecipitation were used to validate the role of ANKRD22 on lipid metabolism in NPC cells. ChIP‐qPCR analysis of H3K27AC signalling near the promoters of METTL14, GINS3, POLE2, PLEK2 and FERMT1 genes. Results: We revealed METTL14, in NPC, correlating with poor patient prognosis. In vitro and in vivo assays indicated METTL14 actively promoted NPC cells proliferation and metastasis. METTL14 catalysed m6A modification on ANKRD22 messenger ribonucleic acid (mRNA), recognized by the reader IGF2BP2, leading to increased mRNA stability and higher translational efficiency. Moreover, ANKRD22, a metabolism‐related protein on mitochondria, interacted with SLC25A1 to enhance citrate transport, elevating intracellular acetyl‐CoA content. This dual impact of ANKRD22 promoted lipid metabolism reprogramming and cellular lipid synthesis while upregulating the expression of genes associated with the cell cycle (GINS3 and POLE2) and the cytoskeleton (PLEK2 and FERMT1) through heightened epigenetic histone acetylation levels in the nucleus. Intriguingly, our findings highlighted elevated ANKRD22‐mediated histone H3 lysine 27 acetylation (H3K27AC) signals near the METTL14 promoter, which contributes to a positive feedback loop perpetuating malignant progression in NPC. Conclusions: The identified METTL14‐ANKRD22‐SLC25A1 axis emerges as a promising therapeutic target for NPC, and also these molecules may serve as novel diagnostic biomarkers. [ABSTRACT FROM AUTHOR]

Published

2024

3. Viewing Soil Moisture Flash Drought Onset Mechanism and Their Changes Through XAI Lens: A Case Study in Eastern China.

Author

Feng, Jiajin, Li, Jun, Xu, Chong‐Yu, Wang, Zhaoli, Zhang, Zhenxing, Wu, Xushu, Lai, Chengguang, Zeng, Zhaoyang, Tong, Hongfu, and Jiang, Shijie

Subjects

SOIL moisture, DROUGHTS, WATER consumption, MACHINE learning, PLATEAUS

Abstract

Soil moisture flash droughts often pose significant challenges to humans and ecosystems, with wide‐ranging socioeconomic consequences. However, the underlying mechanisms of flash droughts and their changes remain unquantified. Taking China as a case study, we present a novel framework that combines machine learning with interpretable and cluster techniques to investigate flash drought mechanisms from 1980 to 2018. We first quantified the temporal contribution of drivers and further identified different mechanisms during drought onsets. We subsequently investigated the temporal changes in different mechanisms and classified drought event types. We identified four driving mechanism types triggering drought: Concurrent precipitation, Antecedent‐concurrent precipitation, Antecedent temperature‐concurrent precipitation, and Antecedent transpiration‐concurrent precipitation. The total effects from vegetation transpiration contributed to around 50% of the impacts for mechanisms involving antecedent transpiration and concurrent precipitation, highlighting the non‐neglectable role of vegetation water consumption in drought occurrences. Remarkably, about 60% of flash drought onsets exhibited close association with the antecedent anomalies, which contribute approximately 50% of overall effects, emphasizing the importance of the cumulative effects of drivers. Moreover, driving mechanisms associated with temperature and transpiration increased significantly over time, implying an elevated influence of these factors on droughts. Our classification of drought events reveals that nearly 70% of events were driven by at least two mechanisms, underscoring a complex time‐varying pattern of driving factors during drought events. The proposed holistic framework not only sheds insight into the multifaceted mechanisms driving flash droughts within China but also extends its potential applicability to broader geographical contexts. Key Points: A novel framework combining interpretable machine learning and cluster techniques was proposed to investigate flash drought mechanismFour distinct types of driving mechanisms of flash drought onset in eastern China were discoveredNearly 70% of flash drought events involve multiple mechanisms, emphasizing the time‐varying feature of drought drivers [ABSTRACT FROM AUTHOR]

Published

2024

4. Spatial Transcriptomic and Metabolomic Landscapes of Oral Submucous Fibrosis‐Derived Oral Squamous Cell Carcinoma and its Tumor Microenvironment.

Author

Zhi, Yuan, Wang, Qian, Zi, Moxin, Zhang, Shanshan, Ge, Junshang, Liu, Keyue, Lu, Linsong, Fan, Chunmei, Yan, Qijia, Shi, Lei, Chen, Pan, Fan, Songqing, Liao, Qianjin, Guo, Can, Wang, Fuyan, Gong, Zhaojian, Xiong, Wei, and Zeng, Zhaoyang

Subjects

SQUAMOUS cell carcinoma, TUMOR microenvironment, ORAL submucous fibrosis, METABOLOMICS, METABOLIC reprogramming

Abstract

In South and Southeast Asia, the habit of chewing betel nuts is prevalent, which leads to oral submucous fibrosis (OSF). OSF is a well‐established precancerous lesion, and a portion of OSF cases eventually progress to oral squamous cell carcinoma (OSCC). However, the specific molecular mechanisms underlying the malignant transformation of OSCC from OSF are poorly understood. In this study, the leading‐edge techniques of Spatial Transcriptomics (ST) and Spatial Metabolomics (SM) are integrated to obtain spatial location information of cancer cells, fibroblasts, and immune cells, as well as the transcriptomic and metabolomic landscapes in OSF‐derived OSCC tissues. This work reveals for the first time that some OSF‐derived OSCC cells undergo partial epithelial–mesenchymal transition (pEMT) within the in situ carcinoma (ISC) region, eventually acquiring fibroblast‐like phenotypes and participating in collagen deposition. Complex interactions among epithelial cells, fibroblasts, and immune cells in the tumor microenvironment are demonstrated. Most importantly, significant metabolic reprogramming in OSF‐derived OSCC, including abnormal polyamine metabolism, potentially playing a pivotal role in promoting tumorigenesis and immune evasion is discovered. The ST and SM data in this study shed new light on deciphering the mechanisms of OSF‐derived OSCC. The work also offers invaluable clues for the prevention and treatment of OSCC. [ABSTRACT FROM AUTHOR]

Published

2024

5. Spatially Resolved Transcriptomics Technology Facilitates Cancer Research.

Author

Wang, Qian, Zhi, Yuan, Zi, Moxin, Mo, Yongzhen, Wang, Yumin, Liao, Qianjin, Zhang, Shanshan, Gong, Zhaojian, Wang, Fuyan, Zeng, Zhaoyang, Guo, Can, and Xiong, Wei

Subjects

CANCER research, STROMAL cells, NUCLEOTIDE sequencing, CELL physiology, RNA sequencing, GENE expression profiling

Abstract

Single cell RNA sequencing (scRNA‐seq) provides a great convenience for studying tumor occurrence and development for its ability to study gene expression at the individual cell level. However, patient‐derived tumor tissues are composed of multiple types of cells including tumor cells and adjacent non‐malignant cells such as stromal cells and immune cells. The spatial locations of various cells in situ tissues plays a pivotal role in the occurrence and development of tumors, which cannot be elucidated by scRNA‐seq alone. Spatially resolved transcriptomics (SRT) technology emerges timely to explore the unrecognized relationship between the spatial background of a particular cell and its functions, and is increasingly used in cancer research. This review provides a systematic overview of the SRT technologies that are developed, in particular the more widely used cutting‐edge SRT technologies based on next‐generation sequencing (NGS). In addition, the main achievements by SRT technologies in precisely unveiling the underappreciated spatial locations on gene expression and cell function with unprecedented high‐resolution in cancer research are emphasized, with the aim of developing more effective clinical therapeutics oriented to a deeper understanding of the interaction between tumor cells and surrounding non‐malignant cells. [ABSTRACT FROM AUTHOR]

Published

2023

6. Iron‐Rich Semiconducting Polymer Dots for the Combination of Ferroptosis–Starvation and Phototherapeutic Cancer Therapy.

Author

Chen, Mingjian, Yang, Yuxin, Tang, Le, He, Shuyi, Guo, Wanni, Ge, Guili, Zeng, Zhaoyang, Li, Xiaoling, Li, Guiyuan, Xiong, Wei, and Wu, Steven Xu

Published

2023

7. MYH10 Combines with MYH9 to Recruit USP45 by Deubiquitinating Snail and Promotes Serous Ovarian Cancer Carcinogenesis, Progression, and Cisplatin Resistance.

Author

Liu, Longyang, Chen, Chunlin, Liu, Ping, Li, Jing, Pang, Zhanjun, Zhu, Jiayu, Lin, Zhongqiu, Zhou, Haixu, Xie, Yingying, Lan, Tiancai, Chen, Zhe‐Sheng, Zeng, Zhaoyang, and Fang, Weiyi

Subjects

OVARIAN cancer, DEUBIQUITINATING enzymes, CISPLATIN, CARCINOGENESIS, PROTEIN domains, GLUTATHIONE transferase, MYOSIN

Abstract

The poor prognosis of serous ovarian cancer (SOC) is due to its high invasive capacity and cisplatin resistance of SOC cells, whereas the molecular mechanisms remain poorly understood. In the present study, the expression and function of non‐muscle myosin heavy chain IIB (MYH10) in SOC are identified by immunohistochemistry, in vitro, and in vivo studies, respectively. The mechanism of MYH10 is demonstrated by co‐immunoprecipitation, GST pull‐down, confocal laser assays, and so on. The results show that the knockdown of MYH10 suppressed SOC cell proliferation, migration, invasion, metastasis, and cisplatin resistance both in vivo and in vitro. Further studies confirm that the MYH10 protein functional domain combines with non‐muscle myosin heavy chain IIA (MYH9) to recruit the deubiquitinating enzyme Ubiquitin‐specific proteases 45 and deubiquitinates snail to inhibit snail degradation, eventually promoting tumorigenesis, progression, and cisplatin resistance in SOC. In clinical samples, MYH10 expression is significantly elevated in SOC samples compared to the paratumor samples. And the expression of MYH10 is positively correlated with MYH9 expression. MYH10+/MYH9+ co‐expression is an independent prognostic factor for predicting SOC patient survival. These findings uncover a key role of the MYH10‐MYH9‐snail axis in SOC carcinogenesis, progression, and cisplatin resistance, and provide potential novel therapeutic targets for SOC intervention. [ABSTRACT FROM AUTHOR]

Published

2023

8. LPLUNC1 reduces glycolysis in nasopharyngeal carcinoma cells through the PHB1‐p53/c‐Myc axis.

Author

Oyang, Linda, Ouyang, Lei, Yang, Lixia, Lin, Jinguan, Xia, Longzheng, Tan, Shiming, Wu, Nayiyuan, Han, Yaqian, Yang, Yiqing, Li, Jian, Chen, Xiaohui, Tang, Yanyan, Su, Min, Luo, Xia, Li, Jinyun, Xiong, Wei, Zeng, Zhaoyang, Liao, Qianjin, and Zhou, Yujuan

Abstract

Cancer cells prefer glycolysis to support their proliferation. Our previous studies have shown that the long palate, lung, and nasal epithelial cell clone 1 (LPLUNC1) can upregulate prohibitin 1 (PHB1) expression to inhibit the proliferation of nasopharyngeal carcinoma (NPC) cells. Given that PHB1 is an important regulator of cell energy metabolism, we explored whether and how LPLUNC1 regulated glucose glycolysis in NPC cells. LPLUNC1 or PHB1 overexpression decreased glycolysis and increased oxidative phosphorylation (OXPHOS)‐related protein expression in NPC cells, promoting phosphorylated PHB1 nuclear translocation through 14‐3‐3σ. LPLUNC1 overexpression also increased p53 but decreased c‐Myc expression in NPC cells, which were crucial for the decrease in glycolysis and increase in OXPHOS‐related protein expression induced by LPLUNC1 overexpression. Finally, we found that treatment with all‐trans retinoic acid (ATRA) reduced the viability and clonogenicity of NPC cells, decreased glycolysis, and increased OXPHOS‐related protein expression by enhancing LPLUNC1 expression in NPC cells. Therefore, the LPLUNC1‐PHB1‐p53/c‐Myc axis decreased glycolysis in NPC cells, and ATRA upregulated LPLUNC1 expression, ATRA maybe a promising drug for the treatment of NPC. [ABSTRACT FROM AUTHOR]

Published

2023

9. Potential applications of N6‐methyladenosine modification in the prognosis and treatment of cancers via modulating apoptosis, autophagy, and ferroptosis.

Author

Zhi, Yuan, Zhang, Shanshan, Zi, Moxin, Wang, Yian, Liu, Yuhang, Zhang, Mi, Shi, Lei, Yan, Qijia, Zeng, Zhaoyang, Xiong, Wei, Zhi, Keqian, and Gong, Zhaojian

Published

2022

10. Oxymatrine hydrazone (OMTH) synthesis and its protective effect for rheumatoid arthritis through downregulation of MEK/NF‐κB pathway.

Author

Zhang, Guangwen, Liu, Baojian, Zeng, Zhaoyang, Chen, Qinghai, Feng, Yiyun, and Ning, Xueqian

Subjects

RHEUMATOID arthritis, DOWNREGULATION, WESTERN immunoblotting, MATRIX metalloproteinases, PROTEIN expression

Abstract

Rheumatoid arthritis (RA) is one of the inflammatory diseases detected in more than 1% of the world population. In the present study, oxymatrine hydrazone (OMTH) was synthesized and investigated for treatment of RA in vitro in TNF‐α induced fibroblast‐like synoviocyte cell model. Cell viability and apoptosis were detected using MTT and flow cytometry assays, respectively. ELISA was used for determination of inflammatory cytokines and western blotting for evaluation of protein expression. Pretreatment of HFLS‐RA cells with 0.5, 1.0, 1.5, 2.0, and 2.5 μM doses of OMTH suppressed TNF‐α induced promotion of proliferative potential in dose‐based manner. The OMTH pretreatment of TNF‐α exposed HFLS‐RA cells significantly increased apoptotic cell proportion. In TNF‐α exposed HFLS‐RA cells OMTH pretreatment elevated Bax and suppressed Bcl‐2 expression. Treatment of HFLS‐RA cells with OMTH prevented TNF‐α mediated elevation of IL‐1β, IL‐6 and IL‐8. Moreover, OMTH treatment of HFLS‐RA cells effectively suppressed TNF‐α mediated elevated levels of MMP‐1 and MMP‐13. Pretreatment of HFLS‐RA cells with OMTH reversed TNF‐α mediated promotion of iNOS and COX‐2 levels. The MEK/1/2 and p65 phosphorylation in TNF‐α exposed HFLS‐RA cells was reduced by OMTH pre‐treatment in dose‐based manner. Thus, OMTH successfully inhibited TNF‐α‐mediated increased viability of RA synovial cells and activated apoptosis. Pretreatment of TNF‐α exposed synovial cells with OMTH targeted phosphorylation of MEK/NF‐κB. Therefore, OMTH may act as potential therapeutic agent for RA treatment. [ABSTRACT FROM AUTHOR]

Published

2021

11. VPS33B interacts with NESG1 to suppress cell growth and cisplatin chemoresistance in ovarian cancer.

Author

Ning, Yingxia, Zeng, Zhaoyang, Deng, Yuao, Feng, Weifeng, Huang, Lun, Liu, Huiling, Lin, Jiazhi, Zhang, Chen, Fan, Yue, and Liu, Longyang

Abstract

The pathogenesis and cisplatin chemoresistance of ovarian cancer (OC) are still unclear. Vacuolar protein sorting‐associated 33B (VPS33B) has not been reported in OC to date. In this study, immunohistochemistry was used to detect VPS33B protein expression between OC and ovarian tissues. MTT, EdU, colony formation, cell cycle, in vivo tumorigenesis, western blot, ChIP, EMSA, co‐immunoprecipitation (CoIP), qRT‐PCR, and microconfocal microscopy were used to explore the function and molecular mechanisms of VPS33B in OC cells. The results of the present study demonstrated that VPS33B protein expression was obviously reduced in OC compared with that in ovarian tissues. Overexpressed VPS33B suppressed cell cycle transition, cell growth, and chemoresistance to cisplatin in vitro and in vivo. Analysis of the mechanism indicated that overexpressed VPS33B regulated the epidermal growth factor receptor (EGFR)/PI3K/AKT/c‐Myc/p53/miR‐133a‐3p feedback loop and reduced the expression of the cell cycle factor CDK4. Nasopharyngeal epithelium‐specific protein 1 (NESG1) as a tumor suppressor not only interacted with VPS33B, but was also induced by VPS33B by the attenuation of PI3K/AKT/c‐Jun‐mediated transcription inhibition. Overexpressed NESG1 further suppressed cell growth by mediating VPS33B‐modulated signals in VPS33B‐overexpressing OC cells. Finally, NESG1 induced VPS33B expression by reducing the inhibition of PI3K/AKT/c‐Jun‐mediated transcription. Our study is the first to demonstrate that VPS33B serves as a tumor suppressor, and VPS33B can interact with NESG1 to suppress cell growth and promote cisplatin sensitivity by regulating the EGFR/PI3K/AKT/c‐Myc/p53/miR‐133a‐3p feedback loop in OC cells. [ABSTRACT FROM AUTHOR]

Published

2021

12. EBV‐miR‐BART12 accelerates migration and invasion in EBV‐associated cancer cells by targeting tubulin polymerization‐promoting protein 1.

Author

Wu, Yingfen, Wang, Dan, Wei, Fang, Xiong, Fang, Zhang, Shanshan, Gong, Zhaojian, Shi, Lei, Li, Xiayu, Xiang, Bo, Ma, Jian, Deng, Hao, He, Yi, Liao, Qianjin, Zhang, Wenling, Li, Xiaoling, Li, Yong, Guo, Can, Zeng, Zhaoyang, Li, Guiyuan, and Xiong, Wei

Published

2020

13. LncRNA AATBC regulates Pinin to promote metastasis in nasopharyngeal carcinoma.

Author

Tang, Ting, Yang, Liting, Cao, Yujian, Wang, Maonan, Zhang, Shanshan, Gong, Zhaojian, Xiong, Fang, He, Yi, Zhou, Yujuan, Liao, Qianjin, Xiang, Bo, Zhou, Ming, Guo, Can, Li, Xiaoling, Li, Yong, Xiong, Wei, Li, Guiyuan, and Zeng, Zhaoyang

Abstract

Long noncoding RNA (lncRNA) have emerged as crucial regulators for a myriad of biological processes, and perturbations in their cellular expression levels have often been associated with cancer pathogenesis. In this study, we identified AATBC (apoptosis‐associated transcript in bladder cancer, LOC284837) as a novel lncRNA. AATBC was found to be highly expressed in nasopharyngeal carcinoma (NPC), and increased AATBC expression was associated with poor survival in patients with NPC. Furthermore, AATBC promoted migration and invasion of NPC cells in vitro, as well as metastasis in vivo. AATBC upregulated the expression of the desmosome‐associated protein pinin (PNN) through miR‐1237‐3p sponging. In turn, PNN interacted with the epithelial–mesenchymal transition (EMT) activator ZEB1 and upregulated ZEB1 expression to promote EMT in NPC cells. Collectively, our results indicate that AATBC promotes NPC progression through the miR‐1237‐3p–PNN–ZEB1 axis. Our findings indicate AATBC as a potential prognostic biomarker or therapeutic target in NPC. [ABSTRACT FROM AUTHOR]

Published

2020

14. Epstein‐Barr virus‐encoded miR‐BART6‐3p inhibits cancer cell proliferation through the LOC553103‐STMN1 axis.

Author

Wang, Dan, Zeng, Zhaoyang, Zhang, Shanshan, Xiong, Fang, He, Baoyu, Wu, Yingfen, Li, Weimin, Tang, Le, Wei, Fang, Xiang, Bo, Li, Zheng, Zhou, Yanhong, Zhou, Ming, Li, Xiaoling, Li, Yong, Li, Guiyuan, Xiong, Wei, and Guo, Can

Abstract

Epstein‐Barr virus (EBV) is a tumorigenic virus that can cause various human malignancies such as nasopharyngeal carcinoma (NPC) and gastric cancer (GC). EBV encodes 44 mature micro (mi)RNAs, mostly exhibiting oncogenic properties and promoting cancer progression. However, we have previously found that one EBV‐encoded miRNA, namely EBV‐miR‐BART6‐3p, acts as a tumor suppressor by inhibiting metastasis and invasion. Here, we report that EBV‐miR‐BART6‐3p inhibits the proliferation of EBV‐associated cancers, NPC, and GC, by targeting and downregulating a long non‐coding RNA (lncRNA), LOC553103. Through proteomics analysis, we determined that stathmin (STMN1) is affected by EBV‐miR‐BART6‐3p and LOC553103. Further, via RNA immunoprecipitation and luciferase reporter assay, we confirmed that LOC553103 directly binds and stabilizes the 3′UTR region of STMN1 mRNA. These results indicate that the EBV‐miR‐BART6‐3p/LOC553103/STMN1 axis regulates the expression of cell cycle‐associated proteins, which then inhibit EBV‐associated tumor cell proliferation. These findings provide potential targets or strategies for novel EBV‐related cancer treatments, as well as contributes new insights into the understanding of EBV infection‐related carcinogenesis. [ABSTRACT FROM AUTHOR]

Published

2020

15. LNCAROD is stabilized by m6A methylation and promotes cancer progression via forming a ternary complex with HSPA1A and YBX1 in head and neck squamous cell carcinoma.

Author

Ban, Yuanyuan, Tan, Pingqing, Cai, Jing, Li, Junjun, Hu, Meng, Zhou, Ying, Mei, Yan, Tan, Yixin, Li, Xiaoling, Zeng, Zhaoyang, Xiong, Wei, Li, Guiyuan, Li, Xiayu, Yi, Mei, and Xiang, Bo

Abstract

Head and neck squamous cell carcinoma (HNSCC) constitute approximately 4% of all cancers worldwide. In this study, we analyzed the expression profile of the long noncoding RNA (lncRNA) of 502 HNSCC patients from The Cancer Genome Atlas database. Among the differentially expressed lncRNAs between HNSCC and normal samples, LNCAROD is overexpressed in HNSCC and associated with advanced T stage and shortened overall survival. The N6‐methyladenosine (m6A) modification mediated by METTL3 and METTL14 enhanced the stability of LNCAROD in HNSCC cells. Depletion of LNCAROD attenuated cell proliferation, mobility in vitro, and tumorigenicity in vivo, whereas overexpression of LNCAROD exerted opposite effects. LNCAROD is mainly distributed in nucleus and binds with YBX1 and HSPA1A proteins. Silencing either YBX1 or HSPA1A did not affect the level of LNCAROD. However, loss of LNCAROD led to shortened half‐life of YBX1 protein. Mechanistically, LNCAROD protected YBX1 from proteasomal degradation by facilitating YBX1‐HSPA1A protein–protein interaction. Depletion of HSPA1A in LNCAROD‐overexpressing cells resulted in accelerated proteasomal degradation of YBX1 protein. Moreover, re‐expression of Flag‐YBX1 in LNCAROD‐silenced cells rescued malignant behavior of HNSCC cells. Our study indicates that LNCAROD is an oncogenic lncRNA and dysregulation of m6A modification might account for aberrant expression of LNCAROD in HNSCC. LNCAROD acts as a scaffold for the interaction between YBX1 and HSPA1A, preventing proteasomal degradation of YBX1 in HNSCC cells. [ABSTRACT FROM AUTHOR]

Published

2020

16. Inhibin B suppresses anoikis resistance and migration through the transforming growth factor‐β signaling pathway in nasopharyngeal carcinoma.

Author

Zou, Guoying, Ren, Biqiong, Liu, Yi, Fu, Yin, Chen, Pan, Li, Xiayu, Luo, Shudi, He, Junyu, Gao, Ge, Zeng, Zhaoyang, Xiong, Wei, Li, Guiyuan, Huang, Yumei, Xu, Keqian, and Zhang, Wenling

Abstract

Inhibin B (INHBB), a heterodimer of a common α‐subunit and a βB‐subunit, is a glycoprotein belonging to the transforming growth factor‐β (TGF‐β) family. In this study, we observed INHBB expression was reduced in nasopharyngeal carcinoma (NPC) tissues compared to non‐tumor nasopharyngeal epithelium tissues, and INHBB was associated with lymph node metastasis, stage of disease, and clinical progress. Positive expression of INHBB in NPC predicted a better prognosis (overall survival, P = 0.038). However, the molecular mechanisms of INHBB have not been addressed in NPC. We induced anoikis‐resistant cells in NPC cell lines under anchorage‐independent conditions, then found epithelial‐mesenchymal transition markers changed, cell apoptosis decreased, cell cycle was modified, and invasion strengthened in anoikis‐resistant NPC cells. These anoikis‐resistant NPC cells showed decreased expression of INHBB compared with adhesion cells. Furthermore, INHBB was found to influence the above‐mentioned changes. In the anoikis‐resistant NPC cells with INHBB overexpression, apoptotic cells increased, S phase cells weakened, vimentin, matrix metallopeptidase‐9, and vascular endothelial growth factor A expression were downregulated, and E‐cadherin expression was upregulated, and vice versa in knockdown of INHBB (INHBB shRNA) anoikis‐resistant NPC cells. Diminished INHBB expression could activate the TGF‐β pathway to phosphorylate Smad2/3 and form complexes in the nucleus, which resulted in the above changes. Thus, our results revealed for the first time that INHBB could suppress anoikis resistance and migration of NPC cells by the TGF‐β signaling pathway, decrease p53 overexpression, and could serve as a potential biomarker for NPC metastasis and prognosis as well as a therapeutic application. Our results showed for the first time that inhibin B could suppress anoikis resistance and migration of nasopharyngeal carcinoma cells by the transforming growth factor‐β signaling pathway, and decrease p53 overexpression. Inhibin B could serve as a potential biomarker for nasopharyngeal carcinoma metastasis and prognosis, as well as a therapeutic application. [ABSTRACT FROM AUTHOR]

Published

2018

17. Rediscovery of NF‐κB signaling in nasopharyngeal carcinoma: How genetic defects of NF‐κB pathway interplay with EBV in driving oncogenesis?

Author

Yi, Mei, Cai, Jing, Li, Junjun, Chen, Shengnan, Zeng, Zhaoyang, Peng, Qian, Ban, Yuanyuan, Zhou, Ying, Li, Xiaoling, Xiong, Wei, Li, Guiyuan, and Xiang, Bo

Subjects

NF-kappa B, CELLULAR signal transduction, NASOPHARYNX cancer, NEOPLASTIC cell transformation, DISEASE incidence

Abstract

Nasopharyngeal carcinoma (NPC) is a unique EBV‐associated subtype of head and neck cancer, which has the highest incidence in Southern China and eastern South Asia. The interaction between genetic risk factors and environmental challenge, have been considered to contribute to the development of nasopharyngeal carcinogenesis. Constitutive activation of NF‐κB signaling has been seen in NPC tissues and is associated with unfavorable prognosis. Recently, several whole exome sequencing study consistently revealed that high frequency mutations of NF‐κB pathway negative regulators is common in nasopharyngeal carcinoma, which reinforce the importance of NF‐κB driving oncogenesis. This review focuses on the current state of research in role of NF‐κB in NPC carcinogenesis. We summarized the newly identified loss of function (LOF) mutations on NF‐κB negative regulators leading to it's activation bypass LMP‐1 stimulation. We discussed the critical role of NF‐κB activation in immortalization and transformation of nasopharygeal epithelium. We also depicted how NF‐κB signaling mediated chronic inflammation contribute to persistent EBV infection, immune evasion of EBV infected cells, metabolic reprogramming, and cancer stem cells (CSCs) formation in NPC. Lastly, we discussed the clinical resonance of targeting NF‐κB for NPC precise therapy. [ABSTRACT FROM AUTHOR]

Published

2018

18. Abberent expression of NOR1 protein in tumor associated macrophages contributes to the development of DEN‐induced hepatocellular carcinoma.

Author

Chen, Shengnan, Zheng, Pan, Wang, Wei, Yi, Mei, Chen, Pan, Cai, Jing, Li, Junjun, Peng, Qian, Ban, Yuanyuan, Zhou, Ying, Zeng, Zhaoyang, Li, Xiaoling, Xiong, Wei, Li, Guiyuan, and Xiang, Bo

Subjects

LIVER cancer, PROTEIN domains, MACROPHAGES, GENETIC overexpression, TUMOR suppressor genes, GENETICS

Abstract

Hepatocellular carcinoma (HCC) is the most common primary tumor of the liver and the sixth most common lethal cancer worldwide. Recent evidences demonstrated that oxidored nitro domain containing protein 1 (NOR1), a putative tumor suppressor gene, is overexpressed in human HCC tissues. However, the role of NOR1 in HCC development remains unclear. Here, we described that NOR1 protein level is elevated in HCC and is associated with poorer clinical outcome. However, ecotopic overexpression of NOR1 protein in human HCC cell line HepG2 cells had no effect on cells proliferation, migration, and clonality. Immunofluoresence assay indicates NOR1 protein is mainly expressed at CD163 positive M2 tumor associated macrophages (TAMs). To explore the role of NOR1 in the development of HCC, we interrogated the susceptibility of mice lacking the NOR1 gene to DEN‐induced hepatocarcinogenesis. NOR1 deficient mice displayed resistance to DEN‐induced HCC. We also demonstrate that mNOR1 protein is enriched in F4/80 positive Kupffer cells (KCs) infiltrated in DEN induced murine HCC tissues. Loss of NOR1 led to increase of iNOS whereas decrease of Arg1, Ym1 expression in KCs. Overexpression of NOR1 in THP‐1 macrophages led to decrease of iNOS but increase of Arg1. Mechanistic investigations showed that inflammatory cytokines IL‐6, TNF‐α production, and NF‐κB activation were also decreased in NOR1 knockout mice exposed to DEN treatment. Our data suggested that NOR1 is overexpressed in HCC associated TAMs and promotes M2 alternative polarization. Genetic deletion of NOR1 in mice leads to impairment of IL‐6 production and NF‐κB activation, which in turn attenuates DEN‐induced HCC development. [ABSTRACT FROM AUTHOR]

Published

2018

19. CD38 enhances the proliferation and inhibits the apoptosis of cervical cancer cells by affecting the mitochondria functions.

Author

Liao, Shan, Xiao, Songshu, Chen, Hongxiang, Zhang, Manying, Chen, Zhifang, Long, Yuehua, Gao, Lu, Zhu, Guangchao, He, Junyu, Peng, Shuping, Xiong, Wei, Zeng, Zhaoyang, Li, Zheng, Zhou, Ming, Li, Xiaoling, Ma, Jian, Wu, Minghua, Xiang, Juanjuan, Li, Guiyuan, and Zhou, Yanhong

Published

2017

20. A regional frequency analysis of precipitation extremes in Mainland China with fuzzy c-means and L-moments approaches.

Author

Wang, Zhaoli, Zeng, Zhaoyang, Lai, Chengguang, Lin, Wenxin, Wu, Xushu, and Chen, Xiaohong

Subjects

*METEOROLOGICAL precipitation, *DISASTERS & the environment, *SPATIO-temporal variation, *L-moments

Abstract

ABSTRACT Owing to their essential influence on human society and natural environment exerted by inducing disasters, such as floods and droughts, further studies on precipitation extremes in China are needed. This study presents the regional frequency and spatial-temporal patterns of precipitation extremes in China based on a high-resolution (0.5° × 0.5°) daily precipitation dataset from 1961 to 2013. With fuzzy c-means, L-moments methods and other scientific statistical tests, a regional frequency analysis ( RFA) is conducted, aiming to further understand the regional and spatial distribution of precipitation extremes across China. The results show that: (1) the whole Mainland China can be divided into 50 homogeneous regions on the basis of the characteristics of mean annual precipitation and location indices. (2) For most of the regions, Generalized Extreme Value ( GEV), Generalized Normal ( GNO) and Pearson type III ( PE3) distributions of precipitation extremes fit well, according to the results of goodness-of-fit ( GOF) test. (3) For RX1DAY, GEV has the best-fit distribution in the east, northeast and southwest of China, whereas GNO distribution mostly fits the northern and parts of southwest and southeast; in addition, regions which fit PE3 and Generalized Logistic ( GLO) distribute dispersedly across the country. (4) For RX5DAY, GEV mainly fits in the middle, southwestern and southern; GNO and PE3 apply best to the northeastern and northern, respectively. (5) Return periods of 20, 50 and 100 years for their best-fit distributions decrease gradually from southeastern China to northwestern China. Compared with the results of GEV distribution fitted to each grid, RFA may provide more accurate estimates of rainfall quantiles. Definitely, the study results will not only benefit further understanding of the unique and complex features of extreme precipitation in the whole Mainland China but also contribute to the nation-scale flood prevention, control and management in the backdrop of the changing climate. [ABSTRACT FROM AUTHOR]

Published

2017

21. SPLUNC1 is associated with nasopharyngeal carcinoma prognosis and plays an important role in all-trans-retinoic acid-induced growth inhibition and differentiation in nasopharyngeal cancer cells.

Author

Zhang, Wenling, Zeng, Zhaoyang, Wei, Fang, Chen, Pan, Schmitt, David C., Fan, Songqing, Guo, Xiaofang, Liang, Fang, Shi, Lei, Liu, Zixin, Zhang, Zuping, Xiang, Bo, Zhou, Ming, Huang, Donghai, Tang, Ke, Li, Xiaoling, Xiong, Wei, Tan, Ming, Li, Guiyuan, and Li, Xiayu

Subjects

*NASOPHARYNX cancer, *NASOPHARYNX cancer patients, *TRETINOIN, *CANCER cell differentiation, *ENZYME inhibitors, *PREDICTION theory, *RETINOID X receptors, *BIOINFORMATICS, *PROGNOSIS

Abstract

Human SPLUNC1 can suppress nasopharyngeal carcinoma ( NPC) tumor formation; however, the correlation between SPLUNC1expression and NPC patient prognosis has not been reported. In the present study, we used a large-scale sample of 1015 tissue cores to detect SPLUNC1 expression and its association with patient prognosis. SPLUNC1 expression was reduced in NPC samples compared to nontumor nasopharyngeal epithelium tissues. Positive expression of SPLUNC1 in NPC predicted a better prognosis (disease-free survival, P = 0.034; overall survival, P = 0.048). Cox's proportional hazards model revealed that SPLUNC1 could be a significant prognostic factor affecting disease-free survival ( P = 0.027). A c DNA micro-array analyzed by significant analysis of micro-array (SAM) and ingenuity pathway analysis (IPA) revealed that an indirect interaction existed between SPLUNC1 and retinoic acid (RA) in the cancer regulatory network. To further investigate the molecular mechanisms involved, we utilized several bioinformatics tools and identified 12 retinoid X receptors heterodimer binding sites in the promoter region of the SPLUNC1 gene. The transcriptional activity of the SPLUNC1 promoter was up-regulated significantly by all-trans-retinoic acid ( ATRA). SPLUNC1 and retinoic acid receptor expression were induced significantly by ATRA, and removal of ATRA led to a progressive loss of SPLUNC1 and retinoic acid receptor expression. ATRA inhibited proliferation and induced the differentiation of NPC cells. Interestingly, over-expression of SPLUNC1 sensitized NPC cells to ATRA, whereas knockdown of SPLUNC1 in HNE1 cells increased cell viability. Under SPLUNC1 knockdown conditions, differentiation was reversed by ATRA treatment. We concluded that SPLUNC1 could potentially predict prognosis for NPC patients and play an important role in ATRA-induced growth inhibition and differentiation in NPC cells. [ABSTRACT FROM AUTHOR]

Published

2014

22. Multivalent Functionalization of Cyclodextrins by Photochemical Thiol-Ene Addition Reaction.

Author

Becker, Maria M., Zeng, Zhaoyang, and Ravoo, Bart Jan

Subjects

*CYCLODEXTRINS, *ADDITION reactions, *THIOLS, *ALKENES, *ALKANETHIOLS, *CARBOXYLIC acids, *ESTERS, *AMINES

Abstract

Cyclodextrins are among the most popular host compounds in supramolecular chemistry. In this paper we describe a versatile approach to the multivalent functionalization of cyclodextrins by using photochemical thiol-alkene addition reactions ('thiol-ene click chemistry'). Starting from cyclodextrins allylated at the 2-OH, 3-OH and/or 6-OH positions, a range of thiols could be introduced in good to excellent yields. By using alkanethiols substituted with hydroxy, carboxylic acid, ester, protected amine, and tetraethyleneglycol groups, a broad variety of functionalized cyclodextrins was obtained. By using fluorinated alkanethiols, highly fluorinated cyclodextrins (up to 56 wt.-% of fluorine) were obtained in excellent yield. [ABSTRACT FROM AUTHOR]

Published

2013

23. Capacitance Effects Superimposed on Redox Processes in Molecular-Cluster Batteries: A Synergic Route to High-Capacity Energy Storage.

Author

Wang, Heng, Zeng, Zhaoyang, Kawasaki, Naoya, Eckert, Hellmut, Yoshikawa, Hirofumi, and Awaga, Kunio

Subjects

*OXIDATION-reduction reaction, *ELECTRIC batteries, *MANGANESE clusters, *CHEMICAL reduction, *CYCLIC voltammetry, *CARBON electrodes, *ENERGY storage

Abstract

Rechargeable molecular-cluster batteries (MCBs) based on the manganese cluster complex [Mn12O12(CH3CH2C(CH3)2COO)16(H2O)4] ([Mn12]) that exhibited a capacity of approximately 200 A h kg−1 in the battery voltage range of 4.0 to 2.0 V were developed. In these batteries, the capacity of approximately 100 A h kg−1 in the range of 4.0-3.0 V is caused by a chemical reduction from [Mn12]0 to [Mn12]8−, whereas the other half in the range of 3.0-2.0 V cannot be explained by a redox change of the Mn ions. We performed the cyclic voltammetry (CV) and 7Li solid-state NMR measurements on the Mn12-MCBs to investigate the origin of the capacity below 3.0 V. Pseudo-rectangular-shaped CV curves in the range of 3.0-2.0 V demonstrate the presence of an electrical double-layer (EDL) capacitance in Mn12-MCBs, which corresponds to approximately 100 A h kg−1. 7Li NMR studies suggest that Li ions form an EDL with electrons in carbon black electrodes in the capacitance voltage range. The capacitance effects are not formed by the single-carbon electrodes alone, but appear only in the mixture of Mn12 and the carbon black electrodes. This type of coexistence of capacitance effects and redox reaction in one electrochemical cell is quite unusual and can serve as a new working principle for high-performance energy-storage devices. [ABSTRACT FROM AUTHOR]

Published

2013

24. Lactotransferrin: A candidate tumor suppressor-Deficient expression in human nasopharyngeal carcinoma and inhibition of NPC cell proliferation by modulating the mitogen-activated protein kinase pathway.

Author

Zhou, Yanhong, Zeng, Zhaoyang, Zhang, Wenling, Xiong, Wei, Wu, Minghua, Tan, Yixin, Yi, Wei, Xiao, Lan, Li, Xiaoling, Huang, Chen, Cao, Li, Tang, Ke, Li, Xiayu, Shen, Shourong, and Li, Guiyuan

Abstract

Lactotransferrin (LTF) has been shown to regulate tumorogenesis. However, little is known about the role of LTF in regulating the development of human nasopharyngeal carcinoma (NPC). The aim of our study was to investigate whether LTF could regulate the development of NPC by characterizing the pattern of LTF expression in human NPC tissues using cDNA and tissue microarrays. Loss of LTF expression was observed in a significantly higher frequency of NPC tissues compared to that in nontumor nasopharyngeal epithelial tissues. While 61.25% of NPC tissues at the T1/T2 stage were positive for LTF expression, only 40.82% of NPC at the T3/T4 stage were stained by anti-LTF. Similarly, 41.58% of NPC with local lymph node metastasis displayed LTF expression, a value significantly lower than the 46.36% in primary tumors ( p < 0.05). These findings suggest that LTF may negatively regulate the development and metastasis of NPC in vivo. Furthermore, overexpression of or treatment with LTF inhibited the proliferation of NPC cells and promoted cell cycle arrest at the G [ABSTRACT FROM AUTHOR]

Published

2008

25. Amino acid metabolic reprogramming in the tumor microenvironment and its implication for cancer therapy.

Author

Zhang, Jiarong, Chen, Mingjian, Yang, Yuxin, Liu, Ziqi, Guo, Wanni, Xiang, Pingjuan, Zeng, Zhaoyang, Wang, Dan, and Xiong, Wei

Subjects

*METABOLIC reprogramming, *TUMOR microenvironment, *AMINO acid metabolism, *CANCER treatment, *ESSENTIAL amino acids, *AMINO acids

Abstract

Amino acids are essential building blocks for proteins, crucial energy sources for cell survival, and key signaling molecules supporting the resistant growth of tumor cells. In tumor cells, amino acid metabolic reprogramming is characterized by the enhanced uptake of amino acids as well as their aberrant synthesis, breakdown, and transport, leading to immune evasion and malignant progression of tumor cells. This article reviews the altered amino acid metabolism in tumor cells and its impact on tumor microenvironment, and also provides an overview of the current clinical applications of amino acid metabolism. Innovative drugs targeting amino acid metabolism hold great promise for precision and personalized cancer therapy. [ABSTRACT FROM AUTHOR]

Published

2024