Your search keyword '"Dongyin Guan"' showing total 32 results

1. Hepatocyte SREBP signaling mediates clock communication within the liver

Author

Dongyin Guan, Hosung Bae, Dishu Zhou, Ying Chen, Chunjie Jiang, Cam Mong La, Yang Xiao, Kun Zhu, Wenxiang Hu, Trang Minh Trinh, Panpan Liu, Ying Xiong, Bishuang Cai, Cholsoon Jang, and Mitchell A. Lazar

Subjects

Hepatology, Metabolism, Medicine

Abstract

Rhythmic intraorgan communication coordinates environmental signals and the cell-intrinsic clock to maintain organ homeostasis. Hepatocyte-specific KO of core components of the molecular clock Rev-erbα and -β (Reverb-hDKO) alters cholesterol and lipid metabolism in hepatocytes as well as rhythmic gene expression in nonparenchymal cells (NPCs) of the liver. Here, we report that in fatty liver caused by diet-induced obesity (DIO), hepatocyte SREBP cleavage–activating protein (SCAP) was required for Reverb-hDKO–induced diurnal rhythmic remodeling and epigenomic reprogramming in liver macrophages (LMs). Integrative analyses of isolated hepatocytes and LMs revealed that SCAP-dependent lipidomic changes in REV-ERB–depleted hepatocytes led to the enhancement of LM metabolic rhythms. Hepatocytic loss of REV-ERBα and β (REV-ERBs) also attenuated LM rhythms via SCAP-independent polypeptide secretion. These results shed light on the signaling mechanisms by which hepatocytes regulate diurnal rhythms in NPCs in fatty liver disease caused by DIO.

Published

2023

2. Editorial: Tumor metabolism: From molecular mechanisms to clinical application

Author

Chunming Cheng, Si Zhang, Dongyin Guan, Yi Wang, and Nidhi Jyotsana

Subjects

tumor, metabolism, mechanism, clinical application, metabolic pathways, therapeutic strategies, Biology (General), QH301-705.5

Published

2023

3. In silico integrative analysis of multi-omics reveals regulatory layers for diurnal gene expression in mouse liver

Author

Chunjie Jiang, Panpan Liu, Cam Mong La, and Dongyin Guan

Subjects

diurnal rhythm, multi-omics analysis, liver, gene expression, regulatory layer, Diseases of the endocrine glands. Clinical endocrinology, RC648-665

Abstract

Diurnal oscillation persists throughout the body and plays an essential role in maintaining physiological homeostasis. Disruption of diurnal rhythm contributes to many diseases including type 2 diabetes. The regulatory mechanism of the transcription-translation feedback loop (TTFL) of core clock genes is well-established, while a systematic study across all regulatory layers of gene expression, including gene transcription, RNA translation, and DNA binding protein (DBP) activities, is still lacking. We comprehensively bioinformatics analyzed the rhythmicity of gene transcription, mature RNA abundance, protein abundance and DBP activity using publicly available omic-datasets from mouse livers. We found that the core clock genes, Bmal1 and Rev-erbα, persistently retained rhythmicity in all stages, which supported the essential rhythmic function along with the TTFL. Interestingly, there were many layer-specific rhythmic genes playing layer-specific rhythmic functions. The systematic analysis of gene transcription rate, RNA translation efficiency, and post-translation modification of DBP were incorporated to determine the potential mechanisms for layer-specific rhythmic genes. We observed the gene with rhythmic expression in both mature RNA and protein layers were largely due to relatively consistent translation rate. In addition, rhythmic translation rate induced the rhythms of protein whose mature RNA levels were not rhythmic. Further analysis revealed a phosphorylation-mediated and an enhancer RNA-mediated cycling regulation between the corresponding layers. This study presents a global view of the oscillating genes in multiple layers via a systematical analysis and indicates the complexity of regulatory mechanisms across different layers for further functional study.

Published

2022

4. Circadian Regulation of Gene Expression and Metabolism in the Liver

Author

Dongyin, Guan and Mitchell A, Lazar

Subjects

Gene Expression Regulation, Liver, Hepatology, Humans, Article, Circadian Rhythm

Abstract

Circadian rhythms are approximately 24-hour cycles of variation in physiological processes, gene expression, and behavior. They result from the interplay of internal biological clocks with daily environmental rhythms, including light/dark and feeding/fasting. Note that 24-hour rhythms of liver metabolic processes have been known for almost 100 years. Modern studies reveal that, like metabolism, hepatic gene expression is highly rhythmic. Genetic or environmental changes can disrupt the circadian rhythms of the liver, leading to metabolic disorders and hepatocellular carcinoma. In this review, we summarize the current understanding of mechanisms regulating rhythmic gene expression in the liver, highlighting the roles of transcription factors that comprise the core clock molecular as well as noncanonical regulators. We emphasize the plasticity of circadian rhythms in the liver as it responds to multiple inputs from the external and internal environments as well as the potential of circadian medicine to impact liver-related diseases.

Published

2022

5. Isoform-specific functions of PPARγ in gene regulation and metabolism

Author

Wenxiang Hu, Chunjie Jiang, Mindy Kim, Yang Xiao, Hannah J. Richter, Dongyin Guan, Kun Zhu, Brianna M. Krusen, Arielle N. Roberts, Jessica Miller, David J. Steger, and Mitchell A. Lazar

Subjects

PPAR gamma, Mice, Gene Expression Regulation, Adipocytes, Genetics, Animals, Protein Isoforms, Thiazolidinediones, Insulin Resistance, Developmental Biology

Abstract

Peroxisome proliferator-activated receptor γ (PPARγ) is a nuclear receptor that is a vital regulator of adipogenesis, insulin sensitivity, and lipid metabolism. Activation of PPARγ by antidiabetic thiazolidinediones (TZD) reverses insulin resistance but also leads to weight gain that limits the use of these drugs. There are two main PPARγ isoforms, but the specific functions of each are not established. Here we generated mouse lines in which endogenous PPARγ1 and PPARγ2 were epitope-tagged to interrogate isoform-specific genomic binding, and mice deficient in either PPARγ1 or PPARγ2 to assess isoform-specific gene regulation. Strikingly, although PPARγ1 and PPARγ2 contain identical DNA binding domains, we uncovered isoform-specific genomic binding sites in addition to shared sites. Moreover, PPARγ1 and PPARγ2 regulated a different set of genes in adipose tissue depots, suggesting distinct roles in adipocyte biology. Indeed, mice with selective deficiency of PPARγ1 maintained body temperature better than wild-type or PPARγ2-deficient mice. Most remarkably, although TZD treatment improved glucose tolerance in mice lacking either PPARγ1 or PPARγ2, the PPARγ1-deficient mice were protected from TZD-induced body weight gain compared with PPARγ2-deficient mice. Thus, PPARγ isoforms have specific and separable metabolic functions that may be targeted to improve therapy for insulin resistance and diabetes.

Published

2022

6. CSC Conference program from Cancer Stem Cells: Targeting the Roots of Cancer, Seeds of Metastasis, and Sources of Therapy Resistance

Author

Huiping Liu, Justin Lathia, Stanton L. Gerson, Jeremy Rich, Arnold I. Caplan, Alvaro Alvarado, Maksim Sinyuk, Erin Mulkearns-Hubert, Monica Venere, Chris Hubert, Dongyin Guan, Damian J. Junk, Mary Doherty, Xia Liu, Golam Kibria, and Valery Adorno-Cruz

Abstract

The list of talks, speaker names, and their affiliations.

Published

2023

7. Analysis and discussion on design points of sea discharge sewage pipeline project

Author

Lanfang Zhang and Dongyin Guan

Published

2023

8. Hepatocytes demarcated by EphB2 contribute to the progression of nonalcoholic steatohepatitis

Author

Yang Xiao, Kirill Batmanov, Wenxiang Hu, Kun Zhu, Alexander Y. Tom, Dongyin Guan, Chunjie Jiang, Lan Cheng, Sam J. McCright, Eric C. Yang, Matthew R. Lanza, Yifan Liu, David A. Hill, and Mitchell A. Lazar

Subjects

General Medicine

Abstract

Current therapeutic strategies for treating nonalcoholic steatohepatitis (NASH) have failed to alleviate liver fibrosis, which is a devastating feature leading to hepatic dysfunction. Here, we integrated single-nucleus transcriptomics and epigenomics to characterize all major liver cell types during NASH development in mice and humans. The bifurcation of hepatocyte trajectory with NASH progression was conserved between mice and humans. At the nonalcoholic fatty liver (NAFL) stage, hepatocytes exhibited metabolic adaptation, whereas at the NASH stage, a subset of hepatocytes was enriched for the signatures of cell adhesion and migration, which were mainly demarcated by receptor tyrosine kinase ephrin type B receptor 2 (EphB2). EphB2, acting as a downstream effector of Notch signaling in hepatocytes, was sufficient to induce cell-autonomous inflammation. Knockdown of Ephb2 in hepatocytes ameliorated inflammation and fibrosis in a mouse model of NASH. Thus, EphB2-expressing hepatocytes contribute to NASH progression and may serve as a potential therapeutic target.

Published

2023

9. Interconnections between circadian clocks and metabolism

Author

Mitchell A. Lazar and Dongyin Guan

Subjects

Artificial light, Core component, Review Series, Circadian clock, General Medicine, Metabolism, Biology, Unbalanced diet, Circadian Rhythm, Circadian Clocks, Animals, Humans, Circadian rhythm, Adaptation, Genetically modified animal, Neuroscience, Metabolism, Inborn Errors

Abstract

Circadian rhythms evolved through adaptation to daily light/dark changes in the environment; they are believed to be regulated by the core circadian clock interlocking feedback loop. Recent studies indicate that each core component executes general and specific functions in metabolism. Here, we review the current understanding of the role of these core circadian clock genes in the regulation of metabolism using various genetically modified animal models. Additionally, emerging evidence shows that exposure to environmental stimuli, such as artificial light, unbalanced diet, mistimed eating, and exercise, remodels the circadian physiological processes and causes metabolic disorders. This Review summarizes the reciprocal regulation between the circadian clock and metabolism, highlights remaining gaps in knowledge about the regulation of circadian rhythms and metabolism, and examines potential applications to human health and disease.

Published

2021

10. Using GRO-seq to Measure Circadian Transcription and Discover Circadian Enhancers

Author

Bin Fang, Mitchell A. Lazar, and Dongyin Guan

Subjects

Regulation of gene expression, 0303 health sciences, Circadian Rhythm Signaling Peptides and Proteins, Sequence Analysis, RNA, Enhancer RNAs, Computational biology, Biology, Article, Mice, Inbred C57BL, 03 medical and health sciences, Mice, 0302 clinical medicine, Enhancer Elements, Genetic, Transcription (biology), Gene expression, Animals, RNA, Small Untranslated, Circadian rhythm, Enhancer, Transcriptome, Gene, Transcription factor, 030217 neurology & neurosurgery, 030304 developmental biology

Abstract

Circadian gene transcription transmits timing information and drives cyclic physiological processes across various tissues. Recent studies indicate that oscillating enhancer activity is a major driving force of rhythmic gene transcription. Functional circadian enhancers can be identified in an unbiased manner by correlation with the rhythms of nearby gene transcription. Global Run-On sequencing (GRO-seq) measures nascent transcription of both pre-mRNAs and enhancer RNAs (eRNAs) at a genome-wide level, making it a unique tool for unraveling complex gene regulation mechanisms in vivo. Here, we describe a comprehensive protocol, ranging from wet lab to in silico analysis, for detecting and quantifying circadian transcription of genes and eRNAs. Moreover, using gene-eRNA correlation, we detail the steps necessary to identify functional enhancers and transcription factors (TFs) that control circadian gene expression in vivo. While we use mouse liver as an example, this protocol is applicable for multiple tissues.

Published

2021

11. The Hepatocyte Clock and Feeding Control Chronophysiology of Multiple Liver Cell Types

Author

Joshua D. Rabinowitz, Cholsoon Jang, Yang Xiao, Ying Xiong, Trang Minh Trinh, Mitchell A. Lazar, Chunjie Jiang, Wenxiang Hu, Pieterjan Dierickx, and Dongyin Guan

Subjects

Cell signaling, Cell type, Member 1, Nuclear Receptor Subfamily 1, Cytoplasmic and Nuclear, General Science & Technology, Knockout, 1.1 Normal biological development and functioning, Receptors, Cytoplasmic and Nuclear, Cell Communication, Biology, Inbred C57BL, Oral and gastrointestinal, Article, Transcriptome, Mice, Group D, Underpinning research, Circadian Clocks, Receptors, medicine, Animals, Circadian rhythm, Metabolic and endocrine, Nutrition, Mice, Knockout, Multidisciplinary, Liver cell, Liver Disease, Feeding Behavior, Cell biology, Circadian Rhythm, Mice, Inbred C57BL, Repressor Proteins, medicine.anatomical_structure, Gene Expression Regulation, Liver, Hepatocyte, Lipogenesis, Nuclear Receptor Subfamily 1, Group D, Member 1, Hepatocytes, Liver function, Sleep Research, Digestive Diseases, Gene Deletion

Abstract

Most cells of the body contain molecular clocks, but the requirement of peripheral clocks for rhythmicity, and their effects on physiology, are not well understood. Here we show that deletion of core clock components REV-ERBα and β in adult mouse hepatocytes disrupted diurnal rhythms of a subset of liver genes and altered the diurnal rhythm of de novo lipogenesis. Liver function is also influenced by non-hepatocytic cells, and the loss of hepatocyte REV-ERBs remodeled the rhythmic transcriptomes and metabolomes of multiple cell types within the liver. Finally, alteration of food availability demonstrated the hierarchy of the cell-intrinsic hepatocyte clock mechanism and the feeding environment. Together, these studies reveal previously unsuspected roles of the hepatocyte clock in the physiological coordination of nutritional signals and cell-cell communication controlling rhythmic metabolism.

Published

2020

12. Nighttime light exposure enhances Rev-erbα-targeting microRNAs and contributes to hepatic steatosis

Author

Antonio C. Boschero, Patricia Cristine Borck, Gabriela Moreira Soares, Thiago M. Batista, Elaine Vieira, Jean Franciesco Vettorazzi, Dongyin Guan, Camila Lubaczeuski, Everardo M. Carneiro, and Mitchell A. Lazar

Subjects

Blood Glucose, Male, 0301 basic medicine, medicine.medical_specialty, Light, Endocrinology, Diabetes and Metabolism, Motor Activity, Biology, Article, Mice, 03 medical and health sciences, Endocrinology, Internal medicine, microRNA, medicine, Animals, Circadian rhythm, Chronobiology, Messenger RNA, Lipogenesis, medicine.disease, Circadian Rhythm, Fatty Liver, CLOCK, MicroRNAs, 030104 developmental biology, Liver, Steatosis, Metabolic syndrome, Energy Metabolism

Abstract

Objective The exposure to artificial light at night (ALAN) disrupts the biological rhythms and has been associated with the development of metabolic syndrome. MicroRNAs (miRNAs) display a critical role in fine-tuning the circadian system and energy metabolism. In this study, we aimed to assess whether altered miRNAs expression in the liver underlies metabolic disorders caused by disrupted biological rhythms. Results We found that C3H/HePas mice exposed to ALAN developed obesity, and hepatic steatosis, which was paralleled by decreased expression of Rev-erbα and up-regulation of its lipogenic targets ACL and FAS in liver. Furthermore, the expression of Rev-erbα-targeting miRNAs, miR-140-5p, 185-5p, 326-5p and 328-5p were increased in this group. Consistently, overexpression of these miRNAs in primary hepatocytes reduced Rev-erbα expression at the mRNA and protein levels. Importantly, overexpression of Rev-erbα-targeting miRNAs increased mRNA levels of Acly and Fasn. Conclusion Thus, altered miRNAs profile is an important mechanism underlying the disruption of the peripheral clock caused by exposure to ALAN, which could lead to hepatic steatosis.

Published

2018

13. Individual-specific functional epigenomics reveals genetic determinants of adverse metabolic effects of glucocorticoids

Author

Chunjie Jiang, Ching-Hon Pui, Mindy Kim, Jessica R. Wilson, Mary V. Relling, Wenjian Lv, Daniel J. Rader, Yang Xiao, Wenjian Yang, Kun Zhu, Mitchell A. Lazar, Wenxiang Hu, and Dongyin Guan

Subjects

Epigenomics, medicine.medical_specialty, Physiology, Endocrinology, Diabetes and Metabolism, Anti-Inflammatory Agents, MEDLINE, Adipose tissue, Single-nucleotide polymorphism, Biology, Bioinformatics, Dexamethasone, Article, Transcriptome, Receptors, Glucocorticoid, Endocrinology, Glucocorticoid receptor, Internal medicine, Genetic variation, Adipocytes, medicine, Humans, Induced pluripotent stem cell, Glucocorticoids, Molecular Biology, Regulation of gene expression, business.industry, Genetic Variation, Cell Biology, Chromatin, Action (philosophy), business, Glucocorticoid, hormones, hormone substitutes, and hormone antagonists, medicine.drug

Abstract

Glucocorticoids (GCs) are widely used as anti-inflammatory drugs, but their long-term use has severe metabolic side effects. Here, by treating multiple individual adipose stem cell-derived adipocytes and induced pluripotent stem cell-derived hepatocytes with the potent GC, dexamethasone (Dex), we uncovered cell-type-specific and individual-specific GC-dependent transcriptomes and glucocorticoid receptor (GR) cistromes. Individual-specific GR binding could be traced to single nucleotide polymorphisms (SNPs) that altered the binding motifs of GR or its cooperating factors. We also discovered another set of genetic variants that modulated Dex response through affecting chromatin accessibility or chromatin architecture. Several SNPs that altered Dex-regulated GR binding and gene expression controlled Dex-driven metabolic perturbations. Remarkably, these genetic variations were highly associated with increases in serum glucose, lipids, and body mass in subjects on GC therapy. Knowledge of the genetic variants that predispose individuals to metabolic side effects allows for a precision medicine approach to the use of clinically-relevant GCs.

Published

2021

14. The hepatic circadian clock fine-tunes the lipogenic response to feeding through RORα/γ

Author

Manashree Damle, Romeo Papazyan, Jennifer Jager, Zheng Sun, Mitchell A. Lazar, Yuxiang Zhang, Dongyin Guan, Lindsey C. Peed, Bin Fang, and Dan Feng

Subjects

Transcriptional Activation, 0301 basic medicine, Circadian clock, Biology, Gene Knockout Techniques, Mice, 03 medical and health sciences, 0302 clinical medicine, Time of day, Circadian Clocks, Genetics, Zeitgeber, medicine, Animals, Circadian rhythm, Lipogenesis, Membrane Proteins, Nuclear Receptor Subfamily 1, Group F, Member 1, Feeding Behavior, Metabolism, Nuclear Receptor Subfamily 1, Group F, Member 3, Lipid Metabolism, medicine.disease, Research Papers, Cell biology, Sterol regulatory element-binding protein, Mice, Inbred C57BL, 030104 developmental biology, Gene Expression Regulation, Liver, Nuclear receptor, Steatosis, 030217 neurology & neurosurgery, Sterol Regulatory Element Binding Protein 2, Developmental Biology

Abstract

Liver lipid metabolism is under intricate temporal control by both the circadian clock and feeding. The interplay between these two mechanisms is not clear. Here we show that liver-specific depletion of nuclear receptors RORα and RORγ, key components of the molecular circadian clock, up-regulate expression of lipogenic genes only under fed conditions at Zeitgeber time 22 (ZT22) but not under fasting conditions at ZT22 or ad libitum conditions at ZT10. RORα/γ controls circadian expression of Insig2, which keeps feeding-induced SREBP1c activation under check. Loss of RORα/γ causes overactivation of the SREBP-dependent lipogenic response to feeding, exacerbating diet-induced hepatic steatosis. These findings thus establish ROR/INSIG2/SREBP as a molecular pathway by which circadian clock components anticipatorily regulate lipogenic responses to feeding. This highlights the importance of time of day as a consideration in the treatment of liver metabolic disorders.

Published

2017

15. Dual regulation of Stat1 and Stat3 by the tumor suppressor protein PML contributes to interferon α-mediated inhibition of angiogenesis

Author

Kuo Sheng Hsu, Mukesh K. Jain, Yu Liu, Ernest Borden, Ganapati H. Mahabeleshwar, Xuan Zhao, Hung Ying Kao, Dongyin Guan, and Xiwen Cheng

Subjects

STAT3 Transcription Factor, 0301 basic medicine, Angiogenesis, viruses, Neovascularization, Physiologic, Alpha interferon, Promyelocytic Leukemia Protein, Biochemistry, Cell Line, 03 medical and health sciences, Promyelocytic leukemia protein, Endopeptidases, Human Umbilical Vein Endothelial Cells, Animals, Humans, STAT2, STAT3, Molecular Biology, Cells, Cultured, Mice, Knockout, Protein PML, Gene knockdown, Neovascularization, Pathologic, biology, Effector, Interferon-alpha, virus diseases, STAT2 Transcription Factor, Cell Biology, Recombinant Proteins, STAT1 Transcription Factor, 030104 developmental biology, biology.protein, Cancer research, RNA Interference, Endothelium, Vascular, Protein Processing, Post-Translational, Ubiquitin Thiolesterase, Signal Transduction

Abstract

IFNs are effective in inhibiting angiogenesis in preclinical models and in treating several angioproliferative disorders. However, the detailed mechanisms of IFNα-mediated anti-angiogenesis are not completely understood. Stat1/2/3 and PML are IFNα downstream effectors and are pivotal regulators of angiogenesis. Here, we investigated PML's role in the regulation of Stat1/2/3 activity. In Pml knock-out (KO) mice, ablation of Pml largely reduces IFNα angiostatic ability in Matrigel plug assays. This suggested an essential role for PML in IFNα's anti-angiogenic function. We also demonstrated that PML shared a large cohort of regulatory genes with Stat1 and Stat3, indicating an important role of PML in regulating Stat1 and Stat3 activity. Using molecular tools and primary endothelial cells, we demonstrated that PML positively regulates Stat1 and Stat2 isgylation, a ubiquitination-like protein modification. Accordingly, manipulation of the isgylation system by knocking down USP18 altered IFNα-PML axis-mediated inhibition of endothelial cell migration and network formation. Furthermore, PML promotes turnover of nuclear Stat3, and knockdown of PML mitigates the effect of LLL12, a selective Stat3 inhibitor, on IFNα-mediated anti-angiogenic activity. Taken together, we elucidated an unappreciated mechanism in which PML, an IFNα-inducible effector, possess potent angiostatic activity, doing so in part by forming a positive feedforward loop with Stat1/2 and a negative feedback loop with Stat3. The interplay between PML, Stat1/Stat2, and Stat3 contributes to IFNα-mediated inhibition of angiogenesis, and disruption of this network results in aberrant IFNα signaling and altered angiostatic activity.

Published

2017

16. Diet-induced circadian enhancer remodeling synchronizes opposing hepatic lipid metabolic processes

Author

Joshua D. Rabinowitz, Bin Fang, Cholsoon Jang, Erika R. Briggs, Chunjie Jiang, Yuxiang Zhang, David J. Steger, Dongyin Guan, Harry Ischiropoulos, Ying Xiong, Romeo Papazyan, Wenxiang Hu, Patricia Cristine Borck, Mitchell A. Lazar, and Paschalis-Thomas Doulias

Subjects

Male, 0301 basic medicine, Peroxisome proliferator-activated receptor, Endogeny, Inbred C57BL, PPAR, Medical and Health Sciences, Mice, 2.1 Biological and endogenous factors, Aetiology, Beta oxidation, fatty acid oxidation, chemistry.chemical_classification, Liver Disease, food and beverages, Biological Sciences, Circadian Rhythm, Cell biology, Liver, Lipogenesis, Sterol Regulatory Element Binding Protein 1, Sleep Research, diet-induced obesity, Biology, SREBP, General Biochemistry, Genetics and Molecular Biology, Article, 03 medical and health sciences, Overnutrition, medicine, Animals, PPAR alpha, Obesity, Circadian rhythm, Enhancer, lipogenesis, Metabolic and endocrine, fatty liver, Nutrition, chronotherapy, Lipid Metabolism, medicine.disease, Diet, Sterol regulatory element-binding protein, 030104 developmental biology, Gene Expression Regulation, chemistry, circadian rhythms, enhancers, Digestive Diseases, Developmental Biology

Abstract

Overnutrition disrupts circadian metabolic rhythms by mechanisms that are not well understood. Here, we show that diet-induced obesity (DIO) causes massive remodeling of circadian enhancer activity in mouse liver, triggering synchronous high-amplitude circadian rhythms of both fatty acid (FA) synthesis and oxidation. SREBP expression was rhythmically induced by DIO, leading to circadian FA synthesis and, surprisingly, FA oxidation (FAO). DIO similarly caused a high-amplitude circadian rhythm of PPARα, which was also required for FAO. Provision of a pharmacological activator of PPARα abrogated the requirement of SREBP for FAO (but not FA synthesis), suggesting that SREBP indirectly controls FAO via production of endogenous PPARα ligands. The high-amplitude rhythm of PPARα imparted time-of-day-dependent responsiveness to lipid-lowering drugs. Thus, acquisition of rhythmicity for non-core clock components PPARα and SREBP1 remodels metabolic gene transcription in response to overnutrition and enables a chronopharmacological approach to metabolic disorders.

Published

2018

17. Patient Adipose Stem Cell-Derived Adipocytes Reveal Genetic Variation that Predicts Antidiabetic Drug Response

Author

Chunjie Jiang, David J. Steger, Ruth J. F. Loos, Girish N. Nadkarni, Weiping Jia, Arden Moscati, Pieterjan Dierickx, Cheng Hu, Dongyin Guan, Raymond E. Soccio, Wenxiang Hu, Rong Zhang, and Mitchell A. Lazar

Subjects

Adult, medicine.medical_specialty, medicine.drug_class, Peroxisome proliferator-activated receptor, Adipose tissue, Biology, Polymorphism, Single Nucleotide, Cell Line, Rosiglitazone, 03 medical and health sciences, 0302 clinical medicine, Insulin resistance, Internal medicine, Adipocytes, Genetics, medicine, Humans, Hypoglycemic Agents, Thiazolidinedione, Aged, 030304 developmental biology, Gene Editing, chemistry.chemical_classification, 0303 health sciences, Base Sequence, Stem Cells, Genetic Variation, Cell Biology, Middle Aged, medicine.disease, PPAR gamma, NFI Transcription Factors, Cholesterol, Endocrinology, Adipose Tissue, Diabetes Mellitus, Type 2, chemistry, Genetic Loci, NFIA, ABCA1, biology.protein, Molecular Medicine, Stem cell, 030217 neurology & neurosurgery, ATP Binding Cassette Transporter 1, Protein Binding, medicine.drug

Abstract

Summary Thiazolidinedione drugs (TZDs) target the transcriptional activity of peroxisome proliferator activated receptor γ (PPARγ) to reverse insulin resistance in type 2 diabetes, but side effects limit their clinical use. Here, using human adipose stem cell-derived adipocytes, we demonstrate that SNPs were enriched at sites of patient-specific PPARγ binding, which correlated with the individual-specific effects of the TZD rosiglitazone (rosi) on gene expression. Rosi induction of ABCA1, which regulates cholesterol metabolism, was dependent upon SNP rs4743771, which modulated PPARγ binding by influencing the genomic occupancy of its cooperating factor, NFIA. Conversion of rs4743771 from the inactive SNP allele to the active one by clustered regularly interspaced short palindromic repeats (CRISPR)/Cas9-mediated editing rescued PPARγ binding and rosi induction of ABCA1 expression. Moreover, rs4743771 is a major determinant of undesired serum cholesterol increases in rosi-treated diabetics. These data highlight human genetic variation that impacts PPARγ genomic occupancy and patient responses to antidiabetic drugs, with implications for developing personalized therapies for metabolic disorders.

Published

2019

18. HNF6 and Rev-erbα integrate hepatic lipid metabolism by overlapping and distinct transcriptional mechanisms

Author

Maureen Gannon, Manashree Damle, Bin Fang, Zhenghui Li, Mitchell A. Lazar, Yong Hoon Kim, Yuxiang Zhang, and Dongyin Guan

Subjects

0301 basic medicine, Male, Biology, 03 medical and health sciences, Gene Knockout Techniques, Mice, Hepatocyte Nuclear Factor 6, Genetics, medicine, Animals, Gene, Transcription factor, Lipid metabolism, Metabolism, medicine.disease, Lipid Metabolism, Cell biology, Fatty Liver, Mice, Inbred C57BL, 030104 developmental biology, Nuclear receptor, Gene Expression Regulation, Liver, Nuclear Receptor Subfamily 1, Group D, Member 1, Steatosis, Function (biology), Gene Deletion, Developmental Biology, Research Paper, Protein Binding

Abstract

Hepatocyte nuclear factor 6 (HNF6) is required for liver development, but its role in adult liver metabolism is not known. Here we show that deletion of HNF6 in livers of adult C57Bl/6 mice leads to hepatic steatosis in mice fed normal laboratory chow. Although HNF6 is known mainly as a transcriptional activator, hepatic loss of HNF6 up-regulated many lipogenic genes bound directly by HNF6. Many of these genes are targets of the circadian nuclear receptor Rev-erbα, and binding of Rev-erbα at these sites was lost when HNF6 was ablated in the liver. While HNF6 and Rev-erbα coordinately regulate hepatic lipid metabolism, each factor also affects additional gene sets independently. These findings highlight a novel mechanism of transcriptional repression by HNF6 and demonstrate how overlapping and distinct mechanisms of transcription factor function contribute to the integrated physiology of the liver.

Published

2016

19. HSP70 Protein Promotes Survival of C6 and U87 Glioma Cells by Inhibition of ATF5 Degradation

Author

Guangfu Li, Dongyin Guan, Yidi Xu, David Liu, and Zhengshan Liu

Subjects

Cell Survival, Activating transcription factor, Apoptosis, Protein degradation, Biology, Biochemistry, Cell Line, Cell Line, Tumor, Glioma, Heat shock protein, medicine, Animals, Humans, HSP70 Heat-Shock Proteins, Molecular Biology, Transcription factor, Early Growth Response Protein 1, Protein Stability, Cell Biology, medicine.disease, Activating Transcription Factors, Rats, Hsp70, Cell biology, Gene Expression Regulation, Neoplastic, Proto-Oncogene Proteins c-bcl-2, Proteasome, Cell culture, Protein Binding

Abstract

Although both the heat shock protein 70 (HSP70) and the activating transcription factor 5 (ATF5) have been shown to promote cell survival of transformed cells but not survival of non-transformed cells, the relationship of the two molecules is unknown. Here we show that HSP70 and ATF5 are concomitantly up-regulated upon transient but down-regulated over prolonged cellular stress and apoptotic stimulation in the rat C6 glioma and human U87 glioma cells. HSP70 interacts strongly with the N-terminal activation domain of ATF5, which is expected to be rigid and uniquely structured under physiological conditions because of extraordinary high concentration (over 25%) of proline residues. Binding of HSP70 to ATF5 is an ATP-driven process and requires functional ATPase on the nucleotide binding domain of the HSP70 molecule. Overexpression of HSP70 dramatically stabilizes the ATF5 protein, which is otherwise subject to rapid degradation, facilitated by both proteasome-dependent and caspase-dependent processes, whereas HSP70 depletion leads to acceleration of ATF5 degradation and transcription repression of Bcl-2 and Egr-1, which are downstream targets of ATF5 in C6 and U87 glioma cells. Our data reveal an essential role for HSP70 in maintaining high levels of ATF5 expression in glioma cells and support the conclusion that ATF5 is an important substrate protein of HSP70 that mediates HSP70-promoted cell survival in glioma cells.

Published

2011

20. ASK1-JNK signaling cascade mediates Ad-ST13-induced apoptosis in colorectal HCT116 cells

Author

Weiyun Wang, Yingying Xu, Zonghou Shen, Jinfa Gu, Min Yang, Mingcan Yu, Xin Cao, Dongyin Guan, Xinyuan Liu, and Shu Zheng

Subjects

Transcriptional Activation, MAPK/ERK pathway, MAP Kinase Kinase 4, p38 mitogen-activated protein kinases, Blotting, Western, Antineoplastic Agents, Apoptosis, Biology, Mitogen-activated protein kinase kinase, MAP Kinase Kinase Kinase 5, Transfection, Biochemistry, Heat shock protein, Humans, Immunoprecipitation, ASK1, Protein kinase A, Molecular Biology, Kinase, Tumor Suppressor Proteins, Genetic Therapy, Cell Biology, HCT116 Cells, Cell biology, Cancer research, Carrier Proteins, Colorectal Neoplasms, Signal Transduction

Abstract

ST13, a co-factor of heat shock protein, has shown potential antitumor efficacy for colorectal cancer in our previous study. However, the molecular mechanisms governing ST13-induced apoptosis are poorly understood. Here, we demonstrate that Ad-ST13 (ST13 mediated by adenovirus) activates apoptosis signal-regulated kinase (ASK I) and c-Jun N-terminal kinase (JNK) but not p38 (mitogen-activated protein kinase) in human colorectal HCT116 cells. Ad-ST13 also increases extracellular-regulated kinase (ERK) phosphorylation levels, but the change is due to adenovirus replication. Overexpression of ST13 also increases the transcription activity of AP-1. Blocking ASK1-JNK pathway affects Ad-ST13-mediated colorectal cell apoptosis, decreases the release of cytochrome c in cytoplasm and caspase activation. Because ASK! is known to contain a tetratricopeptide repeat (TPR)-acceptor site and ST13 has TPR domain, we found the interaction between ST13 and ASK1. These results strongly indicate Ad-ST13 triggers colorectal cell apoptosis via ASK1-JNK signaling cascade. J. Cell. Biochem. 110: 581-588, 2010. (C) 2010 Wiley-Liss, Inc.

Published

2010

21. N-glycosylation of ATF6β is essential for its proteolytic cleavage and transcriptional repressor function to ATF6α

Author

Hao Wang, Zonghou Shen, Dongyin Guan, Min Yang, Yingying Xu, and Veronica E. Li

Subjects

Glycosylation, Transcription, Genetic, Activating transcription factor, Repressor, Endoplasmic Reticulum, CREB, Biochemistry, Mice, chemistry.chemical_compound, N-linked glycosylation, Animals, Humans, Promoter Regions, Genetic, Molecular Biology, Transcription factor, Glycoproteins, Cell Nucleus, Models, Genetic, biology, ATF6, Endoplasmic reticulum, Cell Membrane, Cell Biology, Activating Transcription Factor 6, Dithiothreitol, chemistry, biology.protein, HeLa Cells, Plasmids

Abstract

Activating transcription factor 6 (ATF6), a member of the ATF/CREB family of transcription factors, has two isoforms of 90-kDa (p90ATF6alpha) and 110-kDa (p110 ATF6beta) as endoplasmic reticulum (ER) transmembrane glycoprotein. ATF6beta contains five evolutionarily conserved N-linked glycosylation sites and is a key transcriptional repressor of ATF6alpha, which contribute to regulating the strength and duration of ATF6-dependent ER stress response (ERSR) gene induction. Although it is well established that p110ATF6beta can be cleaved and generate a nuclear form of 60-kDa (p60ATF6beta) that inhibits ATF6alpha-mediated ERSR genes activation, the functional significance of p110 ATF6beta N-linked glycosylation is unknown. Herein, we found that the fully unglycosylated ATF6beta cannot be proteolytic cleaved, be detectable in nucleus after dithiothreitol treatment, and repress the transcriptional activity of ATF6alpha. These results provide the first evidence that unglycosylated ATF6beta may directly facilitate the expression of ERSR genes by losing its repressor function to ATF6alpha.

Published

2009

22. N-acetyl cysteine and penicillamine induce apoptosis via the ER stress response-signaling pathway

Author

Dongyin Guan, Yingying Xu, Hao Wang, Min Yang, Zonghou Shen, and Xiaoming Wang

Subjects

Cancer Research, Small interfering RNA, XBP1, genetic structures, ATF6, Endoplasmic reticulum, CHOP, Biology, Molecular biology, Cell biology, Apoptosis, Unfolded protein response, Signal transduction, Molecular Biology

Abstract

N-acetyl cysteine (NAC) and penicillamine (PEN) have been shown to induce apoptosis in multiple types of human cancer cells; however, the molecular mechanism underlying this activity is unclear. This study was designed to identify the genes responsible for apoptosis induction by NAC and PEN. We found that glucose-regulated protein 78 (GRP78) was upregulated in HeLa cells following treatment with NAC or PEN. GRP78 is a central regulator of endoplasmic reticulum (ER) stress and has been used as a marker of ER stress. Additionally, both the activating transcription factor 6 (ATF6) protein and X box-binding protein 1 (XBP1) mRNA were processed, which facilitates the expression of C/EBP homologous protein (CHOP), a key-signaling component of ER stress-induced apoptosis. Furthermore, the PERK-ATF4 pathway, which also induces the expression of CHOP, was activated in NAC-treated cells. The role of the ER stress pathway was further confirmed through the small interfering RNA (siRNA)-mediated knockdown of CHOP, which attenuated NAC and PEN-induced apoptosis. These results demonstrate that NAC- and PEN-induced apoptosis in HeLa cells is mediated by the ER stress pathway.

Published

2009

23. Involvement of the role of Chk1 in lithium‐induced G2/M phase cell cycle arrest in hepatocellular carcinoma cells

Author

Xiao-Cheng Feng, Zonghou Shen, Jiao Li, Dongyin Guan, Xiaoming Wang, and Qiong Wang

Subjects

G2 Phase, Carcinoma, Hepatocellular, animal structures, Cell cycle checkpoint, Lithium (medication), Inositol monophosphatase, Cyclin B, Lithium, Biology, environment and public health, Biochemistry, Cyclin-dependent kinase, Cell Line, Tumor, CDC2 Protein Kinase, medicine, Humans, CHEK1, Phosphorylation, Molecular Biology, Cyclin-dependent kinase 1, Kinase, Cell Cycle, Cell Biology, Cyclin-Dependent Kinases, Cell biology, enzymes and coenzymes (carbohydrates), Checkpoint Kinase 1, embryonic structures, biology.protein, Cancer research, biological phenomena, cell phenomena, and immunity, Protein Kinases, Cell Division, medicine.drug

Abstract

Lithium, a therapeutic agent for bipolar disorder, can induce G2/M arrest in various cells, but the mechanism is unclear. In this article, we demonstrated that lithium arrested hepatocellular carcinoma cell SMMC-7721 at G2/M checkpoint by inducing the phosphorylation of cdc2 (Tyr-15). This effect was p53 independent and not concerned with the inhibition of glycogen synthase kinase-3 and inositol monophosphatase, two well-documented targets of lithium. Checkpoint kinase 1 (Chk1), a critical enzyme in DNA damage-induced G2/M arrest, was at least partially responsible for the lithium action. The lithium-induced phosphorylation of cdc2 and G2/M arrest was abrogated largely by SB218078, a potent Chk1 inhibitor, as well as by Chk1 siRNA or the over-expression of kinase dead Chk1. Furthermore, lithium-induced cdc25C phosphorylation in 7721 cells and in vitro kinase assay showed that the activity of Chk1 was enhanced after lithium treatment. Interestingly, the increase of Chk1 activity by lithium may be independent of ataxia telangiectasia mutated (ATM)/ATM and Rad3-related (ATR) kinase. This is because no elevated phosphorylation on Chk1 (Ser-317 and Ser-345) was observed after lithium treatment. Moreover, caffeine, a known ATM/ATR kinase inhibitor, relieved the phosphorylation of cdc2 (Tyr-15) by hydroxyurea, but not that by lithium. Our study's results revealed the role of Chk1 in lithium-induced G2/M arrest. Given that Chk1 has been proposed to be a novel tumor suppressor, we suggest that the effect of lithium on Chk1 and cell cycle is useful in tumor prevention and therapy.

Published

2008

24. Post‐transcriptional Regulation of PML Protein by Distinct Mechanisms

Author

Dongyin Guan, Hung Ying Kao, Andrea Putnam, and Eckhard Jankowsky

Subjects

Acute promyelocytic leukemia, Untranslated region, Messenger RNA, biology, Chemistry, medicine.disease, medicine.disease_cause, Biochemistry, Ubiquitin ligase, Cell biology, Promyelocytic leukemia protein, Ubiquitin, Genetics, medicine, biology.protein, Carcinogenesis, Molecular Biology, Post-transcriptional regulation, Biotechnology

Abstract

The promyelocytic leukemia (PML) protein is a tumor suppressor originally identified in acute promyelocytic leukemia and implicated in tumorigenesis in multiple forms of cancer. PML protein is frequently down-regulated in various cancers, but PML mRNA levels are relatively similar between normal and cancerous tissues (1). These observations indicate that PML protein levels are tightly regulated, in part, through post-transcriptional modification. We previously demonstrated that the PML protein undergoes ubiquitination (Ub)-mediated degradation facilitated by an E3 ligase UHRF1 (2), and that SIRT1/SIRT5 promotes deacetylation and SUMO1 conjugation of PML (3) in response to oxidative stress. Here, we found that the small noncoding RNA miR-24 and miR-133 target 3' UTR of PML1 mRNA, the major PML isoform in primary human endothelial cells (ECs). In normal culture condition, miR-24 and miR-133 down-regulate PML1 protein expression in primary human ECs. However, miR-24 but not miR-133 up-regulates PML1 protein ...

Published

2015

25. Cancer stem cells: targeting the roots of cancer, seeds of metastasis, and sources of therapy resistance

Author

Golam Kibria, Justin D. Lathia, Jeremy N. Rich, Stanton L. Gerson, Dongyin Guan, Xia Liu, Huiping Liu, Valery Adorno-Cruz, Damian J. Junk, Maksim Sinyuk, Mary R. Doherty, Erin E. Mulkearns-Hubert, Alvaro G. Alvarado, Arnold I. Caplan, Monica Venere, and Christopher G. Hubert

Subjects

Cancer Research, Tumor microenvironment, Pathology, medicine.medical_specialty, business.industry, Cancer, medicine.disease, Microvesicles, Article, Metastasis, Epigenesis, Genetic, Clinical trial, Oncology, Cancer stem cell, Drug Resistance, Neoplasm, Cancer research, Neoplastic Stem Cells, Tumor Microenvironment, Medicine, Humans, Epigenetics, Neoplasm Metastasis, business, Reprogramming

Abstract

With the goal to remove the roots of cancer, eliminate metastatic seeds, and overcome therapy resistance, the 2014 inaugural International Cancer Stem Cell (CSC) Conference at Cleveland, OH, convened together over 320 investigators, including 55 invited world-class speakers, 25 short oral presenters, and 100 poster presenters, to gain an in-depth understanding of CSCs and explore therapeutic opportunities targeting CSCs. The meeting enabled intriguing discussions on several topics including: genetics and epigenetics; cancer origin and evolution; microenvironment and exosomes; metabolism and inflammation; metastasis and therapy resistance; single cell and heterogeneity; plasticity and reprogramming; as well as other new concepts. Reports of clinical trials targeting CSCs emphasized the urgent need for strategically designing combinational CSC-targeting therapies against cancer. Cancer Res; 75(6); 924–9. ©2015 AACR.

Published

2015

26. The epigenetic regulator UHRF1 promotes ubiquitination-mediated degradation of the tumor-suppressor protein promyelocytic leukemia protein

Author

Dongyin Guan, Hung Ying Kao, Daniel C. Factor, Zhong Lin Wang, and Yu Liu

Subjects

Acute promyelocytic leukemia, Cancer Research, Immunoprecipitation, Ubiquitin-Protein Ligases, viruses, Blotting, Western, Promyelocytic Leukemia Protein, Transfection, medicine.disease_cause, Article, Epigenesis, Genetic, Promyelocytic leukemia protein, Ubiquitin, Neoplasms, Genetics, medicine, Humans, RNA, Small Interfering, Molecular Biology, biology, Reverse Transcriptase Polymerase Chain Reaction, Tumor Suppressor Proteins, HEK 293 cells, Ubiquitination, Endothelial Cells, Nuclear Proteins, virus diseases, medicine.disease, Molecular biology, Ubiquitin ligase, Cell biology, HEK293 Cells, Microscopy, Fluorescence, Gene Knockdown Techniques, Cancer cell, CCAAT-Enhancer-Binding Proteins, biology.protein, Carcinogenesis, Transcription Factors

Abstract

The promyelocytic leukemia (PML) protein is a tumor suppressor originally identified in acute promyelocytic leukemia and implicated in tumorigenesis in multiple forms of cancer. Here, we demonstrate that the PML protein undergoes ubiquitination-mediated degradation facilitated by an E3 ligase UHRF1 (ubiquitin-like with PHD and RING finger domains 1), which is commonly upregulated in various human malignancies. Furthermore, UHRF1 negatively regulates PML protein accumulation in primary human umbilical vein endothelial cells (HUVECs), HEK 293 cells and cancer cells. Knockdown of UHRF1 upregulates whereas ectopic overexpression of UHRF1 downregulates protein abundance of endogenous or exogenous PML, doing so through its binding to the N-terminus of PML. Overexpression of wild-type UHRF1 shortens PML protein half-life and promotes PML polyubiquitination, whereas deletion of the RING domain or coexpression of the dominant-negative E2 ubiquitin-conjugating enzyme, E2D2, attenuates this modification to PML. Finally, knockdown of UHRF1 prolongs PML half-life and increases PML protein accumulation, yet inhibits cell migration and in vitro capillary tube formation, whereas co-knockdown of PML compromises this inhibitory effect. These findings suggest that UHRF1 promotes the turnover of PML protein, and thus targeting UHRF1 to restore PML-mediated tumor suppression represents a promising, novel, anticancer strategy.

Published

2012

27. Identification of a Novel LXXLL Motif in α-Actinin 4-spliced Isoform That Is Critical for Its Interaction with Estrogen Receptor α and Co-activators*

Author

Sharmistha Chakraborty, Yu Liu, Minh Lam, Sichun Yang, Wei Huang, Dongyin Guan, Xuan Zhao, Hung Ying Kao, and Simran Khurana

Subjects

Gene isoform, Transcription, Genetic, Amino Acid Motifs, Estrogen receptor, P300-CBP Transcription Factors, Biology, Biochemistry, Nuclear Receptor Coactivator 1, Cell Line, Tumor, Humans, Protein Isoforms, Gene Regulation, Actinin, p300-CBP Transcription Factors, Molecular Biology, Estrogen receptor beta, Estrogen Receptor alpha, Cell Biology, Molecular biology, Cell biology, Nuclear receptor coactivator 1, Alternative Splicing, Nuclear receptor, Estrogen-related receptor gamma, Estrogen receptor alpha, Protein Binding

Abstract

α-Actinins (ACTNs) are a family of proteins cross-linking actin filaments that maintain cytoskeletal organization and cell motility. Recently, it has also become clear that ACTN4 can function in the nucleus. In this report, we found that ACTN4 (full length) and its spliced isoform ACTN4 (Iso) possess an unusual LXXLL nuclear receptor interacting motif. Both ACTN4 (full length) and ACTN4 (Iso) potentiate basal transcription activity and directly interact with estrogen receptor α, although ACTN4 (Iso) binds ERα more strongly. We have also found that both ACTN4 (full length) and ACTN4 (Iso) interact with the ligand-independent and the ligand-dependent activation domains of estrogen receptor α. Although ACTN4 (Iso) interacts efficiently with transcriptional co-activators such as p300/CBP-associated factor (PCAF) and steroid receptor co-activator 1 (SRC-1), the full length ACTN4 protein either does not or does so weakly. More importantly, the flanking sequences of the LXXLL motif are important not only for interacting with nuclear receptors but also for the association with co-activators. Taken together, we have identified a novel extended LXXLL motif that is critical for interactions with both receptors and co-activators. This motif functions more efficiently in a spliced isoform of ACTN4 than it does in the full-length protein.

Published

2012

28. All-trans-retinoic acid intensifies endoplasmic reticulum stress inN-acetylglucosaminyltransferase V repressed human hepatocarcinoma cells by perturbing homocysteine metabolism

Author

Zonghou Shen, Hao Wang, Yingying Xu, Dongyin Guan, and Min Yang

Subjects

medicine.medical_specialty, Carcinoma, Hepatocellular, XBP1, Homocysteine, Retinoic acid, Cystathionine beta-Synthase, Antineoplastic Agents, Apoptosis, Tretinoin, Biology, Endoplasmic Reticulum, N-Acetylglucosaminyltransferases, Biochemistry, chemistry.chemical_compound, Cell Line, Tumor, Internal medicine, medicine, Humans, Endoplasmic Reticulum Chaperone BiP, Molecular Biology, organic chemicals, Endoplasmic reticulum, Liver Neoplasms, Cell Biology, Glutathione, Cell biology, Endocrinology, Betaine-Homocysteine S-Methyltransferase, chemistry, Unfolded protein response, Intracellular

Abstract

We previously reported that all-trans-retinoic acid (ATRA) induced apoptosis in N-acetylglucosaminyltransferase V (GnT-V) repressed human hepatocarcinoma 7721 (GnT-V-AS/7721) cells via endoplasmic reticulum (ER) stress. In addition to confirming these findings, we further found that ATRA repressed the expression of betaine-homocysteine methyltransferase (BHMT) and cystathionine-β-synthase (CBS), which are key enzymes that are involved in homocysteine metabolism, increased the level of intracellular homocysteine, and decreased the glutathione (GSH) level in GnT-V-AS/7721 cells. To investigate the effect of ATRA on homocysteine metabolism, cells were challenged with exogenous homocysteine. In GnT-V-AS/7721 cells with ATRA treatment, a significant elevation of intracellular homocysteine levels suggests that ATRA perturbs homocysteine metabolism in GnT-V-AS/7721 cells and, therefore, sensitizes the cells to homocysteine-induced ER stress. An obvious increase in the levels of GRP78/Bip protein and spliced XBP1 mRNA were observed. Furthermore, we observed that ATRA blunted the homocysteine-induced increase of GSH only in GnT-V-AS/7721 cells. These results demonstrate that ATRA intensifies ER stress and induces apoptosis in GnT-V-AS/7721 cells by disturbing homocysteine metabolism through the down-regulation of CBS and BHMT, depleting the cellular GSH and, in turn, altering the cellular redox status. In addition, we showed that ATRA did not trigger ER stress, induce apoptosis, or affect homocysteine metabolism in L02 cells, which is a cell type that is derived from normal liver tissue. These results provide support for the hypothesis that ATRA is an anticancer agent. J. Cell. Biochem. 109: 468–477, 2010. © 2009 Wiley-Liss, Inc.

Published

2009

29. Erratum: The epigenetic regulator UHRF1 promotes ubiquitination-mediated degradation of the tumor-suppressor protein promyelocytic leukemia protein

Author

D. Factor, Dongyin Guan, Zhong Lin Wang, Yu Liu, and Hung Ying Kao

Subjects

Cancer Research, Oncogene, biology, Regulator, law.invention, Promyelocytic leukemia protein, Ubiquitin, law, Genetics, biology.protein, Cancer research, Suppressor, Epigenetics, Molecular Biology

Published

2015

30. The function, regulation and therapeutic implications of the tumor suppressor protein, PML.

Author

Dongyin Guan and Hung-Ying Kao

Subjects

*TUMOR suppressor proteins, *ACUTE promyelocytic leukemia, *CELL cycle regulation

Abstract

The tumor suppressor protein, promyelocytic leukemia protein (PML), was originally identified in acute promyelocytic leukemia due to a chromosomal translocation between chromosomes 15 and 17. PML is the core component of subnuclear structures called PML nuclear bodies (PML-NBs), which are disrupted in acute promyelocytic leukemia cells. PML plays important roles in cell cycle regulation, survival and apoptosis, and inactivation or down-regulation of PML is frequently found in cancer cells. More than 120 proteins have been experimentally identified to physically associate with PML, and most of them either transiently or constitutively co-localize with PML-NBs. These interactions are associated with many cellular processes, including cell cycle arrest, apoptosis, senescence, transcriptional regulation, DNA repair and intermediary metabolism. Importantly, PML inactivation in cancer cells can occur at the transcriptional-, translational- or post-translational-levels. However, only a few somatic mutations have been found in cancer cells. A better understanding of its regulation and its role in tumor suppression will provide potential therapeutic opportunities. In this review, we discuss the role of PML in multiple tumor suppression pathways and summarize the players and stimuli that control PML protein expression or subcellular distribution. [ABSTRACT FROM AUTHOR]

Published

2015

31. The function, regulation and therapeutic implications of the tumor suppressor protein, PML

Author

Hung Ying Kao and Dongyin Guan

Subjects

Acute promyelocytic leukemia, Protein PML, PML, Cell cycle checkpoint, DNA repair, viruses, PML nuclear bodies, virus diseases, Review, Biology, Bioinformatics, medicine.disease, Tumor suppressor protein, General Biochemistry, Genetics and Molecular Biology, Cell biology, Promyelocytic leukemia protein, Cancer cell, biology.protein, medicine, Transcriptional regulation, Therapy, Stem cell

Abstract

The tumor suppressor protein, promyelocytic leukemia protein (PML), was originally identified in acute promyelocytic leukemia due to a chromosomal translocation between chromosomes 15 and 17. PML is the core component of subnuclear structures called PML nuclear bodies (PML-NBs), which are disrupted in acute promyelocytic leukemia cells. PML plays important roles in cell cycle regulation, survival and apoptosis, and inactivation or down-regulation of PML is frequently found in cancer cells. More than 120 proteins have been experimentally identified to physically associate with PML, and most of them either transiently or constitutively co-localize with PML-NBs. These interactions are associated with many cellular processes, including cell cycle arrest, apoptosis, senescence, transcriptional regulation, DNA repair and intermediary metabolism. Importantly, PML inactivation in cancer cells can occur at the transcriptional-, translational- or post-translational- levels. However, only a few somatic mutations have been found in cancer cells. A better understanding of its regulation and its role in tumor suppression will provide potential therapeutic opportunities. In this review, we discuss the role of PML in multiple tumor suppression pathways and summarize the players and stimuli that control PML protein expression or subcellular distribution.

32. HNF6 and Rev-erbα integrate hepatic lipid metabolism by overlapping and distinct transcriptional mechanisms.

Author

Yuxiang Zhang, Bin Fang, Damle, Manashree, Dongyin Guan, Zhenghui Li, Yong Hoon Kim, Gannon, Maureen, and Lazar, Mitchell A.

Subjects

*HEPATOCYTE nuclear factors, *LIVER physiology, *FATTY degeneration, *LIPID metabolism, *NUCLEAR receptors (Biochemistry)

Abstract

Hepatocyte nuclear factor 6 (HNF6) is required for liver development, but its role in adult liver metabolism is not known. Here we show that deletion of HNF6 in livers of adult C57Bl/6 mice leads to hepatic steatosis in mice fed normal laboratory chow. Although HNF6 is known mainly as a transcriptional activator, hepatic loss of HNF6 up-regulated many lipogenic genes bound directly by HNF6. Many of these genes are targets of the circadian nuclear receptor Rev-erbα, and binding of Rev-erbα at these sites was lost when HNF6 was ablated in the liver. While HNF6 and Rev-erbα coordinately regulate hepatic lipid metabolism, each factor also affects additional gene sets independently. These findings highlight a novel mechanism of transcriptional repression by HNF6 and demonstrate how overlapping and distinct mechanisms of transcription factor function contribute to the integrated physiology of the liver. [ABSTRACT FROM AUTHOR]

Published

2016