Your search keyword '"Zhenghe Wang"' showing total 6 results

1. Liver Endothelium Promotes HER3-mediated Cell Survival in KRAS Wild-type and Mutant Colorectal Cancer Cells

Author

Moeez Rathore, Michel’le Wright, Rajat Bhattacharya, Fan Fan, Ali Vaziri-Gohar, Jordan Winter, Zhenghe Wang, Sanford D Markowitz, Joseph Willis, Lee M. Ellis, and Rui Wang

Subjects

Colorectal cancer, Cell growth, Seribantumab, Biology, medicine.disease, medicine.disease_cause, digestive system diseases, Receptor tyrosine kinase, Paracrine signalling, medicine, Cancer research, biology.protein, ERBB3, KRAS, Signal transduction, neoplasms

Abstract

We previously showed that liver endothelial cells (ECs) secreted soluble factors in a paracrine fashion and activated human epidermal growth factor receptor 3 (HER3, also known as ERBB3) for promoting colorectal cancer (CRC) growth and chemoresistance. However, RAS proteins play a critical role in receptor tyrosine kinase signaling pathways, and KRAS mutations mediate CRC resistance to therapies targeting EGFR, another HER protein. Therefore, the role of KRAS mutation status in EC-induced HER3 activation and CRC survival was investigated as it has therapeutic implications. We used CRC cell lines and patient-derived xenografts harboring KRAS wild-type or mutant genes and demonstrated that liver EC-secreted factors promoted HER3-mediated CRC cell growth independent of KRAS mutation status. Also, blocking HER3 in CRC cells by siRNAs or a HER3 antibody seribantumab blocked EC-induced CRC survival. Our findings highlight the potential of utilizing HER3 targeted therapies for treating patients with mCRC independent of RAS mutational status.

Published

2021

2. Modes of contact and risk of transmission in COVID-19 among close contacts

Author

Miaochun Cai, Jin-Ling Tang, Xian-Bo Wu, Xin-long Liao, Wei-Qi Song, Fanghua Liu, Xi-Ru Zhang, Qinlong Jing, Chen Mao, Dan Liu, Pei-Liang Chen, Bi Bi, Xin Cheng, Qing-Mei Huang, Zhi-gang Huang, Zhenghe Wang, Xin-fen Yang, Pei Yang, Shi-gui Yang, Jian-ping Liu, Wei Zhu, Huamin Liu, Jiazhen Zheng, Lei Luo, Yu Ma, and Zhi-Hao Li

Subjects

Pediatrics, medicine.medical_specialty, Coronavirus disease 2019 (COVID-19), business.industry, Incidence (epidemiology), Logistic regression, Throat swab, Asymptomatic, law.invention, Transmission (mechanics), Increased risk, Pcr test, law, medicine, medicine.symptom, business

Abstract

BackgroundRapid spread of SARS-CoV-2 in Wuhan prompted heightened surveillance in Guangzhou and elsewhere in China. Modes of contact and risk of transmission among close contacts have not been well estimated.MethodsWe included 4950 closes contacts from Guangzhou, and extracted data including modes of contact, laboratory testing, clinical characteristics of confirmed cases and source cases. We used logistic regression analysis to explore the risk factors associated with infection of close contacts.ResultsAmong 4950 closes contacts, the median age was 38.0 years, and males accounted for 50.2% (2484). During quarantine period, 129 cases (2.6%) were diagnosed, with 8 asymptomatic (6.2%), 49 mild (38.0%), and 5 (3.9%) severe to critical cases. The sensitivity of throat swab was 71.32% and 92.19% at first to second PCR test. Among different modes of contact, household contacts were the most dangerous in catching with infection of COVID-19, with an incidence of 10.2%. As the increase of age for close contacts and severity of source cases, the incidence of COVID-19 presented an increasing trend from 1.8% (0-17 years) to 4.2% (60 or over years), and from 0.33% for asymptomatic, 3.3% for mild, to 6.2% for severe and critical source cases, respectively. Manifestation of expectoration in source cases was also highly associated with an increased risk of infection in their close contacts (13.6%). Secondary cases were in general clinically milder and were less likely to have common symptoms than those of source cases.ConclusionsIn conclusion, the proportion of asymptomatic and mild infections account for almost half of the confirmed cases among close contacts. The household contacts were the main transmission mode, and clinically more severe cases were more likely to pass the infection to their close contacts. Generally, the secondary cases were clinically milder than those of source cases.

Published

2020

3. Deep proteomic analysis of Dnmt1 mutant/hypomorphic colorectal cancer cells reveals dys-regulation of Epithelial-Mesenchymal Transition and subcellular re-localization of Beta-Catenin

Author

Nullin Divecha, Alex Lester, Paul Skipp, Alex Smith-Vidal, Yihua Wang, Emily H Bowler, Zhenghe Wang, Christopher G. Bell, Joseph Bell, and Rob M. Ewing

Subjects

DNA (Cytosine-5-)-Methyltransferase 1, 0301 basic medicine, Cancer Research, Epithelial-Mesenchymal Transition, Proteome, Biology, DNA methyltransferase, environment and public health, Transcriptome, 03 medical and health sciences, 0302 clinical medicine, Cancer stem cell, Humans, Epithelial–mesenchymal transition, Molecular Biology, beta Catenin, urogenital system, Methylation, Epigenome, DNA Methylation, HCT116 Cells, Cell biology, Protein Transport, HEK293 Cells, 030104 developmental biology, CpG site, 030220 oncology & carcinogenesis, Mutation, Cancer cell, DNA methylation, embryonic structures, DNMT1, Colorectal Neoplasms, Research Paper, Signal Transduction

Abstract

BackgroundDNA methyltransferase I is the primary eukaryotic DNA methyltransferase engaged in maintenance of CpG DNA methylation patterns across the genome. Alteration of CpG methylation patterns and levels is a frequent and significant occurrence across many cancers, and targeted inhibition of Dnmt1 has become an approach of choice for select malignancies. There has been significant interest both in the methyltransferase activity as well as methylation-independent functions of Dnmt1. A previously generated hypomorphic allele of Dnmt1 in HCT116 colorectal cancer cells has become an important tool for understanding Dnmt1 function and how CpG methylation patterns are modulated across the genome. Colorectal cancer cells with the Dnmt1 hypomorphic allele carry a homozygous deletion of exons 3 to 5 of Dnmt1, resulting in greatly reduced Dnmt1 protein expression whilst still exhibiting a limited functional activity and methyltransferase ability. Although this cell model of reduced Dnmt1 levels and function have been used to study the downstream effects on the epigenome and transcriptome, the broader effects of the Dnmt1 hypomorph on the proteome and wider cell signalling are largely unknown.ResultsIn this study, we used quantitative proteomic analysis of nuclear-enriched samples of HCT116 Dnmt1 hypomorph cells to identify signalling pathways and processes dysregulated in the hypomorph cells as compared to wild-type HCT116 cells. Unexpectedly, we observed a clear signature of increased expression of Epithelial-to-Mesenchymal (EMT) in Dnmt1 hypomorph cells. We also observed reduced expression and sub-cellular re-localization of Beta-Catenin in Dnmt1 hypomorph cells. Expression of wild-type Dnmt1 in hypomorph cells or knock-down of wild-type Dnmt1 did not recapitulate or rescue the observed protein profiles in Dnmt1 hypomorph cells suggesting that hypomorphic Dnmt1 causes changes not solely attributableConclusionsIn summary we present the first comprehensive proteomic analysis of the widely studied Dnmt1 hypomorph colorectal cancer cells and identify redistribution of Dnmt1 and its interaction partner Beta-Catenin as well as the dysregulation of EMT related processes and signalling pathways related to the development of a cancer stem cell phenotype.

Published

2019

4. The PTPRT pseudo-phosphatase domain is a denitrase

Author

Zhenghe Wang, Shuliang Zhao, Yujun Hao, Yiqing Zhao, Masaru Miyagi, Sanford D. Markowitz, Rob M. Ewing, John J. Mieyal, Jing Song, Xiujing Feng, Yicheng Chen, Peng Zhang, Benlian Wang, and Ronald A. Conlon

Subjects

chemistry.chemical_classification, 0303 health sciences, biology, Chemistry, Phosphatase, Mutant, 3. Good health, law.invention, Cell biology, 03 medical and health sciences, 0302 clinical medicine, Enzyme, law, 030220 oncology & carcinogenesis, biology.protein, Suppressor, Tyrosine, Receptor, PTPRT, Paxillin, 030304 developmental biology

Abstract

Protein tyrosine nitration occurs under both physiological and pathological conditions1. However, enzymes that remove this protein modification have not yet been identified. Here we report that the pseudo-phosphatase domain of protein tyrosine receptor T (PTPRT) is a denitrase that removes nitro-groups from tyrosine residues in paxillin. PTPRT normally functions as a tumor suppressor and is frequently mutated in a variety of human cancers including colorectal cancer2,3. We demonstrate that some of the tumor-derived mutations located in the pseudophosphatase domain impair the denitrase activity. Moreover, PTPRT mutant mice that inactivate the denitrase activity are susceptible to carcinogen-induced colon tumor formation. This study uncovers a novel enzymatic activity that is involved in tumor suppression.

Published

2017

5. Inhibition of Intracellular Lipolysis Promotes Cancer Cell Adaptation to Hypoxia

Author

Alicia M. Saarinen, Zhenghe Wang, Thai H. Ho, Liguo Wang, Xiaodong Zhang, Jun Liu, and Taro Hitosugi

Subjects

Apoptosis, Catabolism, Chemistry, Lipid droplet, Cancer cell, Adipose triglyceride lipase, medicine, Lipolysis, Hypoxia (medical), medicine.symptom, Intracellular, Cell biology

Abstract

Tumor tissues are chronically exposed to hypoxia owing to aberrant vascularity. Lipid droplet (LD) accumulation is a hallmark of hypoxic cancer cells, yet how LDs form and function during hypoxia remains poorly understood. Herein, we report that in various cancer cells upon oxygen deprivation, HIF-1 activation down-modulates LD catabolism mediated by adipose triglyceride lipase (ATGL), the key enzyme for intracellular lipolysis. Proteomics and functional analyses identified hypoxia-inducible gene 2 (HIG2), a HIF-1 target, as a new inhibitor of ATGL. Knockout of HIG2 enhanced LD breakdown and fatty acid (FA) oxidation, leading to increased ROS production and apoptosis in hypoxic cancer cells as well as impaired growth of tumor xenografts. All of these effects were reversed by co-ablation of ATGL. Thus, by inhibiting ATGL, HIG2 acts downstream of HIF-1 to sequester FAs in LDs away from the mitochondrial pathways for oxidation and ROS generation, thereby sustaining cancer cell survival in hypoxia.

Published

2017

6. Genomic distribution of CHD7 on chromatin tracks H3K4 methylation patterns

Author

Dheepa Balasubramanian, Lingyun Song, Michael P. Schnetz, Ravishankar Balaji, Kuntal Shastri, Gabriel E. Zentner, Xiao-Dong Zhang, Zhenghe Wang, Cynthia F. Bartels, Peter C. Scacheri, Gregory E. Crawford, and Thomas LaFramboise

Subjects

Chromatin Immunoprecipitation, Letter, Transcription, Genetic, Biology, Chromatin remodeling, Histones, Mice, Neuroblastoma, Genetics, Animals, Humans, Luciferases, Cells, Cultured, Embryonic Stem Cells, Genetics (clinical), ChIA-PET, Oligonucleotide Array Sequence Analysis, Neurons, Lysine, Pioneer factor, DNA Helicases, Cell Differentiation, DNA Methylation, Molecular biology, Chromatin, ChIP-sequencing, DNA-Binding Proteins, Enhancer Elements, Genetic, DNase I hypersensitive site, Transcription Initiation Site, Colorectal Neoplasms, Chromatin immunoprecipitation, Bivalent chromatin

Abstract

CHD7 is a member of the chromodomain helicase DNA binding domain family of ATP-dependent chromatin remodeling enzymes. De novo mutation of the CHD7 gene is a major cause of CHARGE syndrome, a genetic disease characterized by a complex constellation of birth defects (Coloboma of the eye, Heart defects, Atresia of the choanae, severe Retardation of growth and development, Genital abnormalities, and Ear abnormalities). To gain insight into the function of CHD7, we mapped the distribution of the CHD7 protein on chromatin using the approach of chromatin immunoprecipitation on tiled microarrays (ChIP-chip). These studies were performed in human colorectal carcinoma cells, human neuroblastoma cells, and mouse embryonic stem (ES) cells before and after differentiation into neural precursor cells. The results indicate that CHD7 localizes to discrete locations along chromatin that are specific to each cell type, and that the cell-specific binding of CHD7 correlates with a subset of histone H3 methylated at lysine 4 (H3K4me). The CHD7 sites change concomitantly with H3K4me patterns during ES cell differentiation, suggesting that H3K4me is part of the epigenetic signature that defines lineage-specific association of CHD7 with specific sites on chromatin. Furthermore, the CHD7 sites are predominantly located distal to transcription start sites, most often contained within DNase hypersensitive sites, frequently conserved, and near genes expressed at relatively high levels. These features are similar to those of gene enhancer elements, raising the possibility that CHD7 functions in enhancer mediated transcription, and that the congenital anomalies in CHARGE syndrome are due to alterations in transcription of tissue-specific genes normally regulated by CHD7 during development.

Published

2009