Your search keyword '"Lei, Yuanyuan"' showing total 10 results

1. Gut microbiota alters host bile acid metabolism to contribute to intrahepatic cholestasis of pregnancy.

Author

Tang, Bo, Tang, Li, Li, Shengpeng, Liu, Shuang, He, Jialin, Li, Pan, Wang, Sumin, Yang, Min, Zhang, Longhui, Lei, Yuanyuan, Tu, Dianji, Tang, Xuefeng, Hu, Hua, Ouyang, Qin, Chen, Xia, and Yang, Shiming

Subjects

BACTEROIDES fragilis, BILE acids, FARNESOID X receptor, GUT microbiome, CHOLESTASIS, METABOLISM

Abstract

Intrahepatic cholestasis of pregnancy (ICP) is a female pregnancy-specific disorder that is characterized by increased serum bile acid and adverse fetal outcomes. The aetiology and mechanism of ICP are poorly understood; thus, existing therapies have been largely empiric. Here we show that the gut microbiome differed significantly between individuals with ICP and healthy pregnant women, and that colonization with gut microbiome from ICP patients was sufficient to induce cholestasis in mice. The gut microbiomes of ICP patients were primarily characterized by Bacteroides fragilis (B. fragilis), and B. fragilis was able to promote ICP by inhibiting FXR signaling via its BSH activity to modulate bile acid metabolism. B. fragilis-mediated FXR signaling inhibition was responsible for excessive bile acid synthesis and interrupted hepatic bile excretion to ultimately promote the initiation of ICP. We propose that modulation of the gut microbiota-bile acid-FXR axis may be of value for ICP treatment. Intrahepatic cholestasis of pregnancy (ICP) is a liver disease that sometimes develops during pregnancy and is characterized by increased serum bile acid levels. Here the authors report that the gut microbiome species B. fragilis is enriched in patients with ICP and promotes ICP development in mice via inhibition of signalling though the bile acid receptor FXR. [ABSTRACT FROM AUTHOR]

Published

2023

2. Disulfiram ameliorates nonalcoholic steatohepatitis by modulating the gut microbiota and bile acid metabolism.

Author

Lei, Yuanyuan, Tang, Li, Chen, Qiao, Wu, Lingyi, He, Wei, Tu, Dianji, Wang, Sumin, Chen, Yuyang, Liu, Shuang, Xie, Zhuo, Wei, Hong, Yang, Shiming, and Tang, Bo

Subjects

FARNESOID X receptor, NON-alcoholic fatty liver disease, BILE acids, DISULFIRAM, FECAL microbiota transplantation, HUMAN microbiota

Abstract

Nonalcoholic steatohepatitis (NASH) has been linked with the gut-liver axis. Here, we investigate the potential for repurposing disulfiram (DSF), a drug commonly used to treat chronic alcoholism, for NASH. Using a mouse model, we show that DSF ameliorates NASH in a gut microbiota-dependent manner. DSF modulates the gut microbiota and directly inhibits the growth of Clostridium. Administration of Clostridium abolishes the ameliorating effects of DSF on NASH. Mechanistically, DSF reduces Clostridium-mediated 7α-dehydroxylation activity to suppress secondary bile acid biosynthesis, which in turn activates hepatic farnesoid X receptor signaling to ameliorate NASH. To assess the effect of DSF on human gut microbiota, we performed a self-controlled clinical trial (ChiCTR2100048035), including 23 healthy volunteers who received 250 mg-qd DSF for 7 days. The primary objective outcomes were to assess the effects of the intervention on the diversity, composition and functional profile of gut microbiota. The pilot study shows that DSF also reduces Clostridium-mediated 7α-dehydroxylation activity. All volunteers tolerated DSF well and there were no serious adverse events in the 7-day follow-up period. Transferring fecal microbiota obtained from DSF-treated humans into germ-free mice ameliorates NASH. Collectively, the observations of similar ameliorating effects of DSF on mice and humans suggest that DSF ameliorates NASH by modulating the gut microbiota and bile acid metabolism. Nonalcoholic steatohepatitis (NASH) has been linked with the gut-liver axis. Here, the authors show that disulfiram (DSF) reduces Clostridium-mediated 7α-dehydroxylation activity to suppress secondary bile acid biosynthesis and ameliorate NASH in mice, and validate DSF regulation of the gut-liver axis in healthy men in a self-controlled clinical trial. [ABSTRACT FROM AUTHOR]

Published

2022

3. Prognostic significance of abdominal obesity and its post-diagnosis change in a Chinese breast cancer cohort.

Author

Chung, Gary K. K., Yeo, Winnie, Cheng, Ashley, Kwok, Carol, Lei, Yuanyuan, Cheung, Ka Li, Lee, Roselle, and Ho, Suzanne C.

Abstract

Purpose: It is well-known that obesity has an adverse impact on breast cancer prognosis; nonetheless, the prognostic role of abdominal obesity, especially its post-diagnosis change, has been understudied. This study aims to examine the prospective associations of general and abdominal obesity and their post-diagnosis changes with all-cause mortality, breast cancer-specific mortality, and breast cancer recurrence in Chinese breast cancer patients. Methods: From 2011 to 2014, 1460 Chinese breast cancer patients were recruited and followed up at 18, 36, and 60 months after diagnosis. Body mass index (BMI), waist-to-hip ratio (WHR), and their changes between baseline and 18-month follow-up were derived. Clinical records on diagnosis, treatment, and death were also obtained. In total, 1309 women who completed the 18-month follow-up were included for Cox regression analyses, stratified by follow-up periods. Results: Within 18–48 months post-diagnosis, substantial WHR loss (5% or above) had reduced risk of all-cause (HR = 0.21 [95% CI 0.06–0.75]) and breast cancer-specific mortality (0.21 [0.06–0.77]) relative to stable WHR; whereas after 48 months post-diagnosis, substantial WHR gain showed elevated risks of all-cause mortality (2.67 [1.22–5.85])). Higher baseline WHR was also associated with both mortality outcomes. Nonetheless, no such associations were observed for BMI measures. Also, the effects of obesity measures on breast recurrence were less apparent. Conclusion: Abdominal obesity, rather than general obesity, was linked to worse survival in Chinese breast cancer patients. Prevention on abdominal obesity and waist gain following breast cancer diagnosis may have a beneficial effect on longer-term survival over and above conventional weight management. Waist assessment and abdominal obesity control should therefore be incorporated as a vital component of the evaluation and interventions of breast cancer prognosis. [ABSTRACT FROM AUTHOR]

Published

2022

4. Human telomerase reverse transcriptase (hTERT) synergistic with Sp1 upregulate Gli1 expression and increase gastric cancer invasion and metastasis.

Author

Wu, Lingyi, Wang, Sumin, Tang, Bo, Tang, Li, Lei, Yuanyuan, Liu, Yaojiang, Yang, Min, Yang, Guodong, Zhang, Dan, and Liu, En

Abstract

Abnormal expression of human telomerase reverse transcriptase (hTERT) has been widely identified in tumors, but the relevant mechanism is not well known. This study aims to investigate the role and mechanism of hTERT in gastric cancer metastasis. Gastric cancer and adjacent non-tumor tissues were collected and the expression levels of hTERT and Gli1 were detected by immunohistochemistry. The results demonstrated that hTERT and Gli1 expression levels in gastric cancer tissue were significantly higher than adjacent non-tumor tissues. Western blot and quantitative real-time PCR were used to an identified expression of the related protein in BGC-823 and SGC-7901 cells. The interactions between hTERT and Sp1 were tested by co-immunoprecipitation experiments. Chromatin immunoprecipitation was performed to confirm that Sp1 and hTERT could bind to the Gli1 promoter. Chromatin reimmunoprecipitation assay further demonstrated that both hTERT and Sp1 bind to the Sp1 site of the Gli1 promoter. Moreover, the hTERT, Sp1, and Gli1 were upregulate was verified in human gastric cancer tissues. These results showed that the expression levels of hTERT in GC tissues were strongly closed to the depth of invasion, lymph node metastasis, TNM (tumor, node, metastasis) stage, and distant metastasis. By combining Sp1 and Gli1 promoter, hTERT upregulated Gli1 expression and promoted invasion and metastasis of GC cells. Overall, these data provide a new molecular mechanism of hTERT to promotes gastric cancer progression. Targeting the hTERT/Sp1/Gli1 axis may represent a new therapeutic strategy. [ABSTRACT FROM AUTHOR]

Published

2021

5. PLAU directs conversion of fibroblasts to inflammatory cancer-associated fibroblasts, promoting esophageal squamous cell carcinoma progression via uPAR/Akt/NF-κB/IL8 pathway.

Author

Fang, Lingling, Che, Yun, Zhang, Chaoqi, Huang, Jianbing, Lei, Yuanyuan, Lu, Zhiliang, Sun, Nan, and He, Jie

Published

2021

6. The membrane-bound and soluble form of melanotransferrin function independently in the diagnosis and targeted therapy of lung cancer.

Author

Lei, Yuanyuan, Lu, Zhiliang, Huang, Jianbing, Zang, Ruochuan, Che, Yun, Mao, Shuangshuang, Fang, Lingling, Liu, Chengming, Wang, Xinfeng, Zheng, Sufei, Sun, Nan, and He, Jie

Published

2020

7. Systematic profiling of immune signatures identifies prognostic predictors in lung adenocarcinoma.

Author

Mao, Shuangshuang, Li, Yuan, Lu, Zhiliang, Che, Yun, Huang, Jianbing, Lei, Yuanyuan, Wang, Yalong, Wang, Xinfeng, Liu, Chengming, Zheng, Sufei, Li, Ning, Li, Jiagen, Sun, Nan, and He, Jie

Subjects

LUNGS, UNIVARIATE analysis, MULTIVARIATE analysis, LUNG cancer, DRUG resistance

Abstract

Purpose: Lung adenocarcinoma (LUAD) is the predominant subtype of lung cancer, with increasing evidence showing clinical benefits of immunotherapy. However, a lack of integrated profiles of complex LUAD immune microenvironments hampers the application of immunotherapy, resulting in limited eligible patient populations as well as drug resistance problems. Here, we aimed to systematically profile the immune signatures of LUADs and to assess the role of the immune microenvironment in patient outcome. Methods: We systematically profiled the immune signatures of LUADs deposited in the TCGA and GEO databases using a total of 730 immune-related genes. Differential expression analysis was used to identify dysregulated genes. Univariate Cox analysis followed by robust likelihood-based survival analysis and multivariate Cox analysis were applied to construct an immune-related prognostic model. Results: We found that differentially expressed immune genes were mainly enriched in immune cell proliferation, migration, activation and the NF-κB and TNF signaling pathways. The 10-immune gene predictive model that we constructed could differentiate LUAD patients with different overall survival times in several datasets, with areas under the curve (AUCs) of 0.67, 0.69, 0.72 and 0.74. LUAD patients with high- or low-risk scores exhibited distinct immune cell compositions, which may explain the prognostic significance of our model. Conclusions: Our results add to the current knowledge of immune processes in LUADs and underscore the critical role of the immune microenvironment in LUAD patient outcome. [ABSTRACT FROM AUTHOR]

Published

2020

8. Analysis of functional hub genes identifies CDC45 as an oncogene in non-small cell lung cancer - a short report.

Author

Huang, Jianbing, Li, Yuan, Lu, Zhiliang, Che, Yun, Sun, Shouguo, Mao, Shuangshuang, Lei, Yuanyuan, Zang, Ruochuan, Li, Ning, Zheng, Sufei, Liu, Chengming, Wang, Xinfeng, Sun, Nan, and He, Jie

Subjects

NON-small-cell lung carcinoma, FUNCTIONAL analysis, GENE regulatory networks, GENES, CELL division

Abstract

Purpose: Hub genes are good molecular candidates for targeted cancer therapy. As yet, however, there is little information on the clinical implications and functional characteristics of hub genes in the development of non-small cell lung cancer (NSCLC). In this study, we set out to analyze the role of hub genes in NSCLC. Methods: We performed weighted gene co-expression network analysis (WGCNA) to analyze gene networks during NSCLC development using transcriptomic data from normal, pre-cancer and cancer tissues. Both in vitro and in vivo expression knockdown assays were used to evaluate the biological function of candidate hub gene CDC45 (cell division cycle 45) in NSCLC. Results: We identified 14 gene networks associated with NSCLC development, in which two modules (turquoise and green) correlated with tumorigenesis most positively and negatively, respectively. Gene enrichment analysis showed that the turquoise module was associated with cell cycle/mitosis, and that the green module was associated with development/morphogenesis. We found that the expression levels of the hub genes CDC45, CDCA5, GINS2, RAD51 and TROAP in the turquoise module increased gradually during tumorigenesis, whereas those of MAGI2-AS3 and RBMS3 in the green module decreased during tumorigenesis. Functionally, we found that expression knockdown of CDC45 inhibited NSCLC cell proliferation both in vitro and in vivo, and arrested the cells in the G2/M phase of the cell cycle, supporting an oncogenic role of CDC45. Conclusion: Through gene co-expression network analysis and subsequent functional analyses we identified hub gene CDC45 as a putative novel therapeutic target in NSCLC. [ABSTRACT FROM AUTHOR]

Published

2019

9. Cisplatin-activated PAI-1 secretion in the cancer-associated fibroblasts with paracrine effects promoting esophageal squamous cell carcinoma progression and causing chemoresistance.

Author

Che, Yun, Wang, Jingnan, Li, Yuan, Lu, Zhiliang, Huang, Jianbing, Sun, Shouguo, Mao, Shuangshuang, Lei, Yuanyuan, Zang, Ruochuan, Sun, Nan, and He, Jie

Published

2018

10. TGF-β-induced NKILA inhibits ESCC cell migration and invasion through NF-κB/MMP14 signaling.

Author

Lu, Zhiliang, Chen, Zhaoli, Li, Yuan, Wang, Jingnan, Zhang, Zhirong, Che, Yun, Huang, Jianbing, Sun, Shouguo, Mao, Shuangshuang, Lei, Yuanyuan, Gao, Yibo, and He, Jie

Subjects

TRANSFORMING growth factors-beta, CELL migration, NON-coding RNA, SQUAMOUS cell carcinoma, PHOSPHORYLATION

Abstract

Abstract: The transforming growth factor β (TGF-β) signaling pathway plays anti- and pro-tumoral roles in the vast majority of cancers, and long noncoding RNAs have been reported to play key roles in the highly contextual response process. However, the roles of long noncoding RNAs (lncRNAs) in TGF-β signaling in esophageal squamous cell carcinoma (ESCC) remain unknown. In this study, we performed RNA-seq to compare lncRNAs expression levels between TGF-β1-treated and untreated ESCC cells and observed that NF-kappaB-interacting lncRNA (NKILA) was remarkably upregulated by the classical TGF-β signaling pathway. RNA profiling of 39 pairs ESCC tumor and adjacent nontumor samples using RT-qPCR demonstrated that NKILA is significantly downregulated in ESCC tumor tissues, and NKILA expression levels were significantly decreased in advanced tumor tissues (III and IV) compared to early stages (I and II) (p < 0.01). Gain- and loss-of-function assays showed that NKILA inhibited ESCC cell metastasis in vitro and in vivo, and mechanism studies showed that NKILA repressed MMP14 expression by inhibiting IκBα phosphorylation and NF-κB activation. Collectively, these findings suggest that the TGF-β-induced lncRNA NKILA has potential as an antimetastasis therapy.Key messages: Long noncoding RNA NKILA could be remarkably upregulated by classical TGF-β signal pathway in ESCC.NKILA was significantly downregulated in esophageal squamous cell carcinoma and negatively correlated with TNM stage.NKILA inhibits ESCC cell metastasis via repressing MMP14 expression by suppressing the phosphorylation of IκBα and NF-κB activation. [ABSTRACT FROM AUTHOR]

Published

2018