Your search keyword '"Keqin Kathy Li"' showing total 28 results

1. LncRNAs GIHCG and SPINT1-AS1 Are Crucial Factors for Pan-Cancer Cells Sensitivity to Lapatinib

Author

Zhen Xiang, Shuzheng Song, Zhenggang Zhu, Wenhong Sun, Jaron E. Gifts, Sam Sun, Qiushi Shauna Li, Yingyan Yu, and Keqin Kathy Li

Subjects

pan-cancer, computational analysis, LncRNAs, lapatinib, targeted therapy, Genetics, QH426-470

Abstract

Lapatinib is a small molecule inhibitor of EGFR (HER1) and ERBB2 (HER2) receptors, which is used for treatment of advanced or metastatic breast cancer. To find the drug resistance mechanisms of treatment for EGFR/ERBB2 positive tumors, we analyzed the possible effects of lncRNAs. In this study, using CCLE (Cancer Cell Line Encyclopedia) database, we explored the relationship between the lncRNAs and Lapatinib sensitivity/resistance, and then validated those findings through in vitro experiments. We found that the expression of EGFR/ERBB2 and activation of ERBB pathway was significantly related to Lapatinib sensitivity. GO (Gene Oncology) analysis of top 10 pathways showed that the sensitivity of Lapatinib was positively correlated with cell keratin, epithelial differentiation, and cell-cell junction, while negatively correlated with signatures of extracellular matrix. Forty-four differentially expressed lncRNAs were found between the Lapatinib sensitive and resistant groups (fold-change > 1.5, P < 0.01). Gene set variation analysis (GSVA) was performed based on 44 lncRNAs and genes in the top 10 pathways. Five lncRNAs were identified as hub molecules. Co-expression network was constructed by more than five lncRNAs and 199 genes in the top 10 pathways, and three lncRNAs (GIHCG, SPINT1-AS1, and MAGI2-AS3) and 47 genes were identified as close-related molecules. The three lncRNAs in epithelium-derived cancers were differentially expressed between sensitive and resistant groups, but no significance was found in non-epithelium-derived cancer cells. Correlation analysis showed that SPINT1-AS1 (R = −0.715, P < 0.001) and GIHCG (R = 0.557, P = 0.013) were correlated with the IC50 of epithelium-derived cancer cells. In further experiments, GIHCG knockdown enhanced cancer cell susceptibility to Lapatinib, while high level of SPINT1-AS1 was a sensitive biomarker of NCI-N87 and MCF7 cancer cells to Lapatinib. In conclusions, lncRNAs GIHCG and SPINT1-AS1 were involved in regulating Lapatinib sensitivity. Up-regulation of GIHCG was a drug-resistant biomarker, while up-regulation of SPINT1-AS1 was a sensitive indicator.

Published

2019

2. FTY720 induces apoptosis of M2 subtype acute myeloid leukemia cells by targeting sphingolipid metabolism and increasing endogenous ceramide levels.

Author

Limin Chen, Liu-Fei Luo, Junyan Lu, Lianchun Li, Yuan-Fang Liu, Jiang Wang, Hong Liu, Heng Song, Hualiang Jiang, Sai-Juan Chen, Cheng Luo, and Keqin Kathy Li

Subjects

Medicine, Science

Abstract

The M2 subtype Acute Myeloid Leukemia (AML-M2) with t(8;21) represents an unmet challenge because of poor clinical outcomes in a sizable portion of patients. In this study,we report that FTY720 (Fingolimod), a sphingosine analogue and an FDA approved drug for treating of multiple sclerosis, shows antitumorigenic activity against the Kasumi-1 cell line, xenograft mouse models and leukemic blasts isolated from AML-M2 patients with t(8;21) translocation. Primary investigation indicated that FTY720 caused cell apoptosis through caspases and protein phosphatase 2A (PP2A) activation. Transcriptomic profiling further revealed that FTY720 treatment could upregulate AML1 target genes and interfere with genes involved in ceramide synthesis. Treatment with FTY720 led to the elimination of AML1-ETO oncoprotein and caused cell cycle arrest. More importantly, FTY720 treatment resulted in rapid and significant increase of pro-apoptotic ceramide levels, determined by high-performance liquid chromatography-electrospray ionization tandem mass spectrometry based lipidomic approaches. Structural simulation model had also indicated that the direct binding of ceramide to inhibitor 2 of PP2A (I2PP2A) could reactivate PP2A and cause cell death. This study demonstrates, for the first time, that accumulation of ceramide plays a central role in FTY720 induced cell death of AML-M2 with t(8;21). Targeting sphingolipid metabolism by using FTY720 may provide novel insight for the drug development of treatment for AML-M2 leukemia.

Published

2014

3. Catalytic mechanism investigation of lysine-specific demethylase 1 (LSD1): a computational study.

Author

Xiangqian Kong, Sisheng Ouyang, Zhongjie Liang, Junyan Lu, Liang Chen, Bairong Shen, Donghai Li, Mingyue Zheng, Keqin Kathy Li, Cheng Luo, and Hualiang Jiang

Subjects

Medicine, Science

Abstract

Lysine-specific demethylase 1 (LSD1), the first identified histone demethylase, is a flavin-dependent amine oxidase which specifically demethylates mono- or dimethylated H3K4 and H3K9 via a redox process. It participates in a broad spectrum of biological processes and is of high importance in cell proliferation, adipogenesis, spermatogenesis, chromosome segregation and embryonic development. To date, as a potential drug target for discovering anti-tumor drugs, the medical significance of LSD1 has been greatly appreciated. However, the catalytic mechanism for the rate-limiting reductive half-reaction in demethylation remains controversial. By employing a combined computational approach including molecular modeling, molecular dynamics (MD) simulations and quantum mechanics/molecular mechanics (QM/MM) calculations, the catalytic mechanism of dimethylated H3K4 demethylation by LSD1 was characterized in details. The three-dimensional (3D) model of the complex was composed of LSD1, CoREST, and histone substrate. A 30-ns MD simulation of the model highlights the pivotal role of the conserved Tyr761 and lysine-water-flavin motif in properly orienting flavin adenine dinucleotide (FAD) with respect to substrate. The synergy of the two factors effectively stabilizes the catalytic environment and facilitated the demethylation reaction. On the basis of the reasonable consistence between simulation results and available mutagenesis data, QM/MM strategy was further employed to probe the catalytic mechanism of the reductive half-reaction in demethylation. The characteristics of the demethylation pathway determined by the potential energy surface and charge distribution analysis indicates that this reaction belongs to the direct hydride transfer mechanism. Our study provides insights into the LSD1 mechanism of reductive half-reaction in demethylation and has important implications for the discovery of regulators against LSD1 enzymes.

Published

2011

4. Molecular basis of NDM-1, a new antibiotic resistance determinant.

Author

Zhongjie Liang, Lianchun Li, Yuanyuan Wang, Limin Chen, Xiangqian Kong, Yao Hong, Lefu Lan, Mingyue Zheng, Cai Guang-Yang, Hong Liu, Xu Shen, Cheng Luo, Keqin Kathy Li, Kaixian Chen, and Hualiang Jiang

Subjects

Medicine, Science

Abstract

The New Delhi Metallo-β-lactamase (NDM-1) was first reported in 2009 in a Swedish patient. A recent study reported that Klebsiella pneumonia NDM-1 positive strain or Escherichia coli NDM-1 positive strain was highly resistant to all antibiotics tested except tigecycline and colistin. These can no longer be relied on to treat infections and therefore, NDM-1 now becomes potentially a major global health threat.In this study, we performed modeling studies to obtain its 3D structure and NDM-1/antibiotics complex. It revealed that the hydrolytic mechanisms are highly conserved. In addition, the detailed analysis indicates that the more flexible and hydrophobic loop1, together with the evolution of more positive-charged loop2 leads to NDM-1 positive strain more potent and extensive in antibiotics resistance compared with other MBLs. Furthermore, through biological experiments, we revealed the molecular basis for antibiotics catalysis of NDM-1 on the enzymatic level. We found that NDM-1 enzyme was highly potent to degrade carbapenem antibiotics, while mostly susceptible to tigecycline, which had the ability to slow down the hydrolysis velocity of meropenem by NDM-1. Meanwhile, the mutagenesis experiments, including D124A, C208A, K211A and K211E, which displayed down-regulation on meropenem catalysis, proved the accuracy of our model.At present, there are no effective antibiotics against NDM-1 positive pathogen. Our study will provide clues to investigate the molecular basis of extended antibiotics resistance of NDM-1 and then accelerate the search for new antibiotics against NDM-1 positive strain in clinical studies.

Published

2011

5. Mutations and clinical significance of calcium voltage-gated channel subunit alpha 1E (CACNA1E) in non-small cell lung cancer

Author

San-Hui Gao, Gui-Zhen Wang, Li-Peng Wang, Lin Feng, Yong-Chun Zhou, Xian-Jun Yu, Fan Liang, Fu-Ying Yang, Zheng Wang, Bei-Bei Sun, Di Wang, Li-Jun Liang, Da-Wei Xie, Song Zhao, Hai-Ping Feng, Xueqing Li, Keqin Kathy Li, Tie-Shan Tang, Yun-Chao Huang, Shi-Qiang Wang, and Guang-Biao Zhou

Subjects

Lung Neoplasms, Physiology, Carcinoma, Non-Small-Cell Lung, Cell Line, Tumor, Mutation, Humans, Calcium, Calcium Channels, R-Type, Cell Biology, Cation Transport Proteins, Molecular Biology

Abstract

CACNA1E is a gene encoding the ion-conducting α1 subunit of R-type voltage-dependent calcium channels, whose roles in tumorigenesis remain to be determined. We previously showed that CACNA1E was significantly mutated in patients with non-small cell lung cancer (NSCLC) who were long-term exposed to household air pollution, with a mutation rate of 19% (15 of 79 cases). Here we showed that CACNA1E was also mutated in 207 (12.8%) of the 1616 patients with NSCLC in The Cancer Genome Atlas (TCGA) datasets. At mRNA and protein levels, CACNA1E was elevated in tumor tissues compared to counterpart non-tumoral lung tissues in NSCLCs of the public datasets and our settings, and its expression level was inversely associated with clinical outcome of the patients. Overexpression of wild type (WT) or A275S or R249G mutant CACNA1E transcripts promoted NSCLC cell proliferation with activation of epidermal growth factor receptor (EGFR) signaling pathway, whereas knockdown of this gene exerted inhibitory effects on NSCLC cells in vitro and in vivo. CACNA1E increased current density and Ca

Published

2022

6. Natural Product Micheliolide (MCL) Irreversibly Activates Pyruvate Kinase M2 and Suppresses Leukemia

Author

Keqin Kathy Li, Liuqing Wen, He Zhu, Ivaylo Ivanov, Qiuying Li, Yahui Ding, Shanshan Li, Jing Li, Peng George Wang, Jing Long, Yue Chen, Ming Luo, Quan Zhang, Cheng Ma, Ning Liu, Qingqing Xue, Rimo Xi, Haibo Long, Jianshuang Guo, Caili Zhao, Zhigang Wu, Chunli Yan, and Liangwei Li

Subjects

0301 basic medicine, Thyroid Hormones, Carcinogenesis, Cell, Active Transport, Cell Nucleus, Antineoplastic Agents, PKM2, medicine.disease_cause, Article, Substrate Specificity, Sesquiterpenes, Guaiane, 03 medical and health sciences, 0302 clinical medicine, Protein Domains, Cell Line, Tumor, Drug Discovery, medicine, Animals, Humans, Amino Acid Sequence, Phosphorylation, Protein Structure, Quaternary, Zebrafish, Cell Nucleus, Regulation of gene expression, Leukemia, Chemistry, Membrane Proteins, Acetylation, Xenograft Model Antitumor Assays, Cell biology, Enzyme Activation, Gene Expression Regulation, Neoplastic, 030104 developmental biology, medicine.anatomical_structure, Cell culture, 030220 oncology & carcinogenesis, Cancer cell, Molecular Medicine, Protein Multimerization, Carrier Proteins, Pyruvate kinase

Abstract

Metabolic reprogramming of cancer cells is essential for tumorigenesis in which pyruvate kinase M2 (PKM2), the low activity isoform of pyruvate kinase, plays a critical role. Herein, we describe the identification of a nature-product-derived micheliolide (MCL) that selectively activates PKM2 through the covalent binding at residue cysteine424 (C424), which is not contained in PKM1. This interaction promotes more tetramer formation, inhibits the lysine433 (K433) acetylation, and influences the translocation of PKM2 into the nucleus. In addition, the pro-drug dimethylaminomicheliolide (DMAMCL) with similar properties as MCL significantly suppresses the growth of leukemia cells and tumorigenesis in a zebrafish xenograft model. Cell-based assay with knock down PKM2 expression verifies that the effects of MCL are dependent on PKM2 expression. DMAMCL is currently in clinical trials in Australia. Our discovery may provide a valuable pharmacological mechanism for clinical treatment and benefit the development of new anticancer agents.

Published

2018

7. LncRNAs GIHCG and SPINT1-AS1 Are Crucial Factors for Pan-Cancer Cells Sensitivity to Lapatinib

Author

Shuzheng Song, Zhenggang Zhu, Jaron E. Gifts, Qiushi Shauna Li, Yingyan Yu, Wenhong Sun, Zhen Xiang, Sam Sun, and Keqin Kathy Li

Subjects

0301 basic medicine, lcsh:QH426-470, medicine.medical_treatment, Cell, pan-cancer, Biology, Lapatinib, Targeted therapy, 03 medical and health sciences, 0302 clinical medicine, ErbB, Genetics, medicine, lapatinib, LncRNAs, skin and connective tissue diseases, Genetics (clinical), Original Research, Gene knockdown, targeted therapy, medicine.disease, Metastatic breast cancer, lcsh:Genetics, 030104 developmental biology, medicine.anatomical_structure, computational analysis, 030220 oncology & carcinogenesis, Cancer cell, Cancer research, Molecular Medicine, Biomarker (medicine), medicine.drug

Abstract

Lapatinib is a small molecule inhibitor of EGFR (HER1) and ERBB2 (HER2) receptors, which is used for treatment of advanced or metastatic breast cancer. To find the drug resistance mechanisms of treatment for EGFR/ERBB2 positive tumors, we analyzed the possible effects of lncRNAs. In this study, using CCLE (Cancer Cell Line Encyclopedia) database, we explored the relationship between the lncRNAs and Lapatinib sensitivity/resistance, and then validated those findings through in vitro experiments. We found that the expression of EGFR/ERBB2 and activation of ERBB pathway was significantly related to Lapatinib sensitivity. GO (Gene Oncology) analysis of top 10 pathways showed that the sensitivity of Lapatinib was positively correlated with cell keratin, epithelial differentiation, and cell-cell junction, while negatively correlated with signatures of extracellular matrix. Forty-four differentially expressed lncRNAs were found between the Lapatinib sensitive and resistant groups (fold-change > 1.5, P < 0.01). Gene set variation analysis (GSVA) was performed based on 44 lncRNAs and genes in the top 10 pathways. Five lncRNAs were identified as hub molecules. Co-expression network was constructed by more than five lncRNAs and 199 genes in the top 10 pathways, and three lncRNAs (GIHCG, SPINT1-AS1, and MAGI2-AS3) and 47 genes were identified as close-related molecules. The three lncRNAs in epithelium-derived cancers were differentially expressed between sensitive and resistant groups, but no significance was found in non-epithelium-derived cancer cells. Correlation analysis showed that SPINT1-AS1 (R = −0.715, P < 0.001) and GIHCG (R = 0.557, P = 0.013) were correlated with the IC50 of epithelium-derived cancer cells. In further experiments, GIHCG knockdown enhanced cancer cell susceptibility to Lapatinib, while high level of SPINT1-AS1 was a sensitive biomarker of NCI-N87 and MCF7 cancer cells to Lapatinib. In conclusions, lncRNAs GIHCG and SPINT1-AS1 were involved in regulating Lapatinib sensitivity. Up-regulation of GIHCG was a drug-resistant biomarker, while up-regulation of SPINT1-AS1 was a sensitive indicator.

Published

2019

8. Structure based design, synthesis and activity studies of small hybrid molecules as HDAC and G9a dual inhibitors

Author

Keqin Kathy Li, Zhongying Xiao, Shanshan Li, Shameer M. Kondengadan, Xiaobo Li, Liuqing Wen, Peng George Wang, Lijuan Wang, Lanlan Zang, Qing Zhang, Dilep Kumar Sigalapalli, Fengyuan Che, Shukkoor Muhammed Kondengaden, Kenneth Huang, Hailiang Zhu, and Bathini Nagendra Babu

Subjects

0301 basic medicine, Multiple cancer, epigenetics, pharmacophore, business.industry, Dual inhibitor, 3. Good health, Central laboratory, 03 medical and health sciences, 030104 developmental biology, Oncology, Design synthesis, G9a inhibitors, HDAC inhibitors, Cancer research, Medicine, Structure based, PULMONARY CARCINOMA, Epigenetics, business, dual inhibitors, Research Paper

Abstract

// Lanlan Zang 1, * , Shukkoor M. Kondengaden 2, * , Qing Zhang 2, * , Xiaobo Li 5 , Dilep K. Sigalapalli 3 , Shameer M. Kondengadan 4 , Kenneth Huang 2 , Keqin Kathy Li 2 , Shanshan Li 2 , Zhongying Xiao 2 , Liuqing Wen 2 , Hailiang Zhu 2 , Bathini N. Babu 3 , Lijuan Wang 1 , Fengyuan Che 1 and Peng George Wang 2 1 Central Laboratory, Linyi People's Hospital, Linyi, Shandong 276003, P.R. China 2 Chemistry Department and Center for Diagnostics and Therapeutics, Georgia State University, Atlanta, GA 30303, USA 3 Department of Medicinal Chemistry, National Institute of Pharmaceutical Education and Research (NIPER), Hyderabad, Telangana 500037, India 4 Department of Medicinal Chemistry, National Institute of Pharmaceutical Education and Research (NIPER), Mohali, Punjab 160062, India 5 Department of Immunology, Collaborative Innovation Center of Tianjin for Medical Epigenetics, Tianjin Key Laboratory of Medical Epigenetics, Tianjin Medical University, Tianjin 300070, P.R. China * These authors have contributed equally to this work Correspondence to: Peng George Wang, email: pwang11@gsu.edu Fengyuan Che, email: che1971@126.com Lijuan Wang, email: lijian.wang730@outlook.com Keywords: epigenetics, pharmacophore, dual inhibitors, G9a inhibitors, HDAC inhibitors Received: April 14, 2017 Accepted: May 23, 2017 Published: June 28, 2017 ABSTRACT Aberrant enzymatic activities or expression profiles of epigenetic regulations are therapeutic targets for cancers. Among these, histone 3 lysine 9 methylation (H3K9Me2) and global de-acetylation on histone proteins are associated with multiple cancer phenotypes including leukemia, prostatic carcinoma, hepatocellular carcinoma and pulmonary carcinoma. Here, we report the discovery of the first small molecule capable of acting as a dual inhibitor targeting both G9a and HDAC. Our structure based design, synthesis, and screening for the dual activity of the small molecules led to the discovery of compound 14 which displays promising inhibition of both G9a and HDAC in low micro-molar range in cell based assays.

Published

2017

9. Discovery of novel small molecule inhibitors of lysine methyltransferase G9a and their mechanism in leukemia cell lines

Author

Keqin Kathy Li, Shukkoor Muhammed Kondengaden, Kenneth Huang, Runling Wang, Liu-Fei Luo, Cheng Luo, Eudoxie Bataba, Mengyuan Zhu, Binghe Wang, Peng George Wang, and Lanlan Zang

Subjects

0301 basic medicine, Methyltransferase, Protein Conformation, Apoptosis, Binding, Competitive, Small Molecule Libraries, 03 medical and health sciences, Histone H3, Mice, Drug Discovery, medicine, Animals, Humans, Cell Proliferation, Pharmacology, biology, Chemistry, Organic Chemistry, Cell Cycle, Myeloid leukemia, General Medicine, Methylation, Azepines, Histone-Lysine N-Methyltransferase, medicine.disease, Molecular Docking Simulation, Leukemia, 030104 developmental biology, Histone, Biochemistry, Histone methyltransferase, biology.protein, Quinazolines, K562 Cells, K562 cells

Abstract

Lysine methyltransferase G9a regulates the transcription of multiple genes by primarily catalyzing mono- and di-methylation of histone H3 lysine 9, as well as several non-histone lysine sites. An attractive therapeutic target in treating leukemia, knockout studies of G9a in mice have found dramatically slowed proliferation and self-renewal of acute myeloid leukemia (AML) cells due to the attenuation of HoxA9-dependent transcription. In this study, a series of compounds were identified as potential inhibitors through structure-based virtual screening. Among these compounds, a new G9a inhibitor, DCG066, was confirmed by in vitro biochemical, and cell based enzyme assays. DCG066 has a novel molecular scaffold unlike other G9a inhibitors presently available. Similar to G9a’s histone substrate, DCG066 can bind directly to G9a and inhibit methyltransferase activity in vitro. In addition to suppressing G9a methyltransferase activity and reducing histone H3 methylation levels, DCG066 displays low cytotoxicity in leukemia cell lines with high levels of G9a expression, including K562. This work presents DCG066 as an inhibitor of G9a with a novel structure, providing both a lead in G9a inhibitor design and a means for probing the functionality of G9a.

Published

2016

10. Pharmacophore-Based Virtual Screening and Biological Evaluation of Small Molecule Inhibitors for Protein Arginine Methylation

Author

Keqin Kathy Li, Yu Wei Chou, Ming Fong Lin, You Feng, Hualiang Jiang, Chao Yang, Sarmistha Sinha, Sakthivel Muniyan, Zhongjie Liang, Hui-fang Chai, Leilei Yan, Juxian Wang, Limin Chen, Cheng Luo, and Yujun George Zheng

Subjects

Models, Molecular, Protein-Arginine N-Methyltransferases, Methyltransferase, Protein Conformation, Molecular Sequence Data, Drug Evaluation, Preclinical, P300-CBP Transcription Factors, Arginine, Methylation, Article, Chromatin remodeling, Small Molecule Libraries, User-Computer Interface, Cell Line, Tumor, Drug Discovery, Humans, p300-CBP Transcription Factors, Amino Acid Sequence, Enzyme Inhibitors, Histone Acetyltransferases, Virtual screening, Chemistry, Small molecule, Biochemistry, Molecular Medicine, Pharmacophore

Abstract

Protein arginine methyltransferases (PRMTs) are proved to play vital roles in chromatin remodeling, RNA metabolism and signal transduction. Aberrant regulation of PRMT activity is associated with various pathological states such as cancer and cardiovascular disorders. Development and application of small molecule PRMT inhibitors will provide new avenues for therapeutic discovery. We combined pharmacophore-based virtual screening methods with radioactive methylation assays, six hits were identified as inhibitors against the predominant arginine methyltransferase PRMT1 within micromolar potency. Two potent compounds, A9 and A36, exhibitting the inhibitory effect by directly targeting substrate H4 other than PRMT1 and displayed even higher inhibition activity than the well-known PRMT inhibitors AMI-1 and stilbamidine. A9 significantly inhibits proliferation of castrate-resistant prostate cancer cells. Together, A9 may be a potential inhibitor against advanced hormone-independent cancers and the work will provide clues for the future development of specific compounds that block the interaction of PRMTs with their targets.

Published

2012

11. Chemical and biochemical approaches in the study of histone methylation and demethylation

Author

Y. George Zheng, Hualiang Jiang, Dongxia Wang, Keqin Kathy Li, and Cheng Luo

Subjects

Pharmacology, biology, Chromatin remodeling, Histone, Biochemistry, Histone methyltransferase, Drug Discovery, Histone methylation, biology.protein, Molecular Medicine, Histone Demethylases, Epigenetics, Chromatin immunoprecipitation, Epigenomics

Abstract

Histone methylation represents one of the most critical epigenetic events in DNA function regulation in eukaryotic organisms. Classic molecular biology and genetics tools provide significant knowledge about mechanisms and physiological roles of histone methyltransferases and demethylases in various cellular processes. In addition to this stream line, development and application of chemistry and chemistry-related techniques are increasingly involved in biological study, and offer information otherwise difficult to obtain by standard molecular biology methods. Herein, we review recent achievements and progress in developing and applying chemical and biochemical approaches in the study of histone methylation, including chromatin immunoprecipitation, chemical ligation, mass spectrometry, biochemical methylation and demethylation assays, and inhibitor development. These technological advances allow histone methylation to be studied from genome-wide level to molecular and atomic levels. With ChIP technology, information can be obtained about precise mapping of histone methylation patterns at specific promoters, genes, or other genomic regions. MS is particularly useful in detecting and analyzing methylation marks in histone and nonhistone protein substrates. Chemical approaches that permit site-specific incorporation of methyl groups into histone proteins greatly facilitate the investigation of biological impacts of methylation at individual modification sites. Discovery and design of selective organic inhibitors of histone methyltransferases and demethylases provide chemical probes to interrogate methylation-mediated cellular pathways. Overall, these chemistry-related technological advances have greatly improved our understanding of the biological functions of histone methylation in normal physiology and diseased states, and also are of great potential to translate basic epigenetics research into diagnostic and therapeutic applications in the clinic.

Published

2012

12. Application of Epigenome-Modifying Small Molecules in Induced Pluripotent Stem Cells

Author

Keqin Kathy Li, Xiangqian Kong, Cheng Luo, and Junyan Lu

Subjects

Pharmacology, Genetics, Histone acetyltransferase, Epigenome, Biology, Cell biology, Histone methyltransferase, Drug Discovery, DNA methylation, biology.protein, Molecular Medicine, Epigenetics, Stem cell, Induced pluripotent stem cell, Reprogramming

Abstract

Recent breakthroughs in generating induced pluripotent stem cells (iPSCs) using four defined factors have revealed the potential utility of stem cells in biological research and clinical applications. However, the low efficiency and slow kinetics of reprogramming related to producing these cells and underlying safety issues, such as viral integration and genetic and epigenetic abnormalities of iPSCs, hamper the further application of iPSCs in laboratory and clinical settings. Previous studies have suggested that reprogramming efficiency can be enhanced and that reprogramming kinetics can be accelerated by manipulating epigenetic status. Herein, we review recent studies on the application of epigenome-modifying small molecules in enhancing reprogramming and functionally replacing some reprogramming factors. We mainly focus on studies that have used small molecules to interfere with epigenome-modifying enzymes, such as DNA methyltransferase, histone acetyltransferase, and histone methyltransferase. The potential use of these small molecules in inducing iPSCs and new ways to identify small molecules of higher potency and fewer side effects are also discussed.

Published

2012

13. As 4 S 4 targets RING-type E3 ligase c-CBL to induce degradation of BCR-ABL in chronic myelogenous leukemia

Author

Qun-Ye Zhang, Ping Liu, Quan Chen, Zhu Chen, Jian-Xiang Liu, Qiu-Hua Huang, Sai Juan Chen, Jian-Hua Mao, Xiao-Yan Sun, and Keqin Kathy Li

Subjects

Models, Molecular, Acute promyelocytic leukemia, Protein Conformation, Molecular Sequence Data, Fusion Proteins, bcr-abl, Sulfides, Biology, Arsenicals, Mice, Random Allocation, Leukemia, Myelogenous, Chronic, BCR-ABL Positive, hemic and lymphatic diseases, medicine, Animals, Humans, Amino Acid Sequence, Proto-Oncogene Proteins c-cbl, Multidisciplinary, Ubiquitination, Biological Sciences, medicine.disease, Ubiquitin ligase, RING finger domain, Multiprotein Complexes, biology.protein, Cancer research, Arsenic sulfide, K562 Cells, Tyrosine kinase, HeLa Cells, K562 cells, Chronic myelogenous leukemia

Abstract

Arsenic, a curative agent for acute promyelocytic leukemia, induces cell apoptosis and degradation of BCR-ABL in chronic myelogenous leukemia (CML). We demonstrated that ubiquitination and degradation of BCR-ABL was mediated by c-CBL, a RING-type E3 ligase that was also shown to be involved in ubiquitination for many other receptor/protein tyrosine kinases. Our data showed that c-CBL protein was considerably up-regulated by arsenic sulfide (As 4 S 4 ). Interestingly, arsenic directly bound the RING finger domain of c-CBL to inhibit its self-ubiquitination/degradation without interfering with the enhancement of ubiquitination and subsequent proteolysis of its substrate BCR-ABL. Degradation of BCR-ABL due to c-CBL induction as a result of arsenic treatment was also observed in vivo in CML mice. These findings provide insight into the molecular mechanisms of arsenic and further support its therapeutic applications in CML in combination with tyrosine kinase inhibitors and potentially also in other malignancies involving aberrant receptor/protein tyrosine kinase signaling.

Published

2010

14. Histone Methyltransferase Inhibitors for Cancer Therapy

Author

Peng George Wang, Shukkoor Muhammed Kondengaden, Bingxue Chris Zhai, Kenneth Huang, Zhang Qing, Hamed Reyhanfard, Jonathan Wooten, and Keqin Kathy Li

Subjects

Genetics, Histone, Methyltransferase, biology, Histone methyltransferase, EZH2, biology.protein, Epigenetics, DOT1L, Cancer epigenetics, Epigenomics

Abstract

Epigenetics is the study of heritable changes in gene expression without alterations in the underlying DNA sequence. Efforts have been made to understand aspects of epigenetic regulation in normal and cancer cells. With the recent discoveries of key histone methyltransferases, it is an exciting time for the field of epigenetics, particularly for enzymes that have been shown to be the writers of epigenetic markers on genes coding for proteins in cancer. Thus, the development of highly potent and specific small-molecule inhibitors to cancer-related histone methyltransferases shows great promise as a therapeutic option. In this review, we focus on the cancer-related histone methyltransferases, including lysine methyltransferases such as DOT1L, EZH2, G9a, and MLL, as well as arginine methyltransferases. We summarize the enzyme characters, their relations to different cancers, and the drug discoveries targeted to these key enzymes.

Published

2015

15. List of Contributors

Author

Alison I. Bernstein, Kelly M. Biette, Joshua C. Black, Champak Chatterjee, Aili Chen, Xiangyun Amy Chen, Abhinav Dhall, Alfonso Dueñas-González, Yuhong Fan, Benjamin A. Garcia, Zhen Han, Alexander-Thomas Hauser, Gang Huang, Kenneth Huang, Peng Jin, Manfred Jung, Shukkoor Kondengaden, James R. Kornacki, Haitao Li, Keqin Kathy Li, Junyan Lu, Yepeng Luan, Cheng Luo, Minkui Luo, Antonia Masch, José L. Medina-Franco, Milan Mrksich, Liza Ngo, Adegboyega K. Oyelere, Chenyi Pan, Sriharsa Pradhan, Zhang Qing, Meihua Qu, Ulf Reimer, Hamed Reyhanfard, Martin Roatsch, Dina Robaa, Johannes Schulz-Fincke, Mike Schutkowski, Simone Sidoli, Wolfgang Sippl, Quaovi H. Sodji, Jinquan Sun, Jolyon Terragni, Xiao-Jun Tian, Peng George Wang, Xiaoshi Wang, Xuejian Wang, Yanming Wang, Johnathan R. Whetstine, Jonathan Wooten, Jianhua Xing, Wei Xu, Jakyung Yoo, Jin Yu, Hao Zeng, Johannes Zerweck, Bingxue Chris Zhai, Hang Zhang, Hao Zhang, Liyi Zhang, Yunzhe Zhang, Shuai Zhao, and Y. George Zheng

Published

2015

16. An Arginine-rich Motif of Ring Finger Protein 4 (RNF4) Oversees the Recruitment and Degradation of the Phosphorylated and SUMOylated Krüppel-associated Box Domain-associated Protein 1 (KAP1)/TRIM28 Protein during Genotoxic Stress*

Author

Xiang Qian Kong, Cheng Luo, Che Chang Chang, Xu Li, Hsiu Ming Shih, Yiyin Chung, Ching Ying Kuo, David K. Ann, and Keqin Kathy Li

Subjects

SUMO-1 Protein, Amino Acid Motifs, SUMO protein, Tripartite Motif-Containing Protein 28, Biochemistry, Protein–protein interaction, Bimolecular fluorescence complementation, Ubiquitin, Humans, Nuclear protein, Molecular Biology, biology, RNF4, Nuclear Proteins, Sumoylation, Cell Biology, Molecular biology, Ubiquitin ligase, Cell biology, Repressor Proteins, HEK293 Cells, Protein Synthesis and Degradation, Proteolysis, biology.protein, DNA Damage, HeLa Cells, Transcription Factors

Abstract

Kruppel-associated box domain-associated protein 1 (KAP1) is a universal transcriptional corepressor that undergoes multiple posttranslational modifications (PTMs), including SUMOylation and Ser-824 phosphorylation. However, the functional interplay of KAP1 PTMs in regulating KAP1 turnover during DNA damage response remains unclear. To decipher the role and cross-talk of multiple KAP1 PTMs, we show here that DNA double strand break-induced KAP1 Ser-824 phosphorylation promoted the recruitment of small ubiquitin-like modifier (SUMO)-targeted ubiquitin E3 ligase, ring finger protein 4 (RNF4), and subsequent RNF4-mediated, SUMO-dependent degradation. Besides the SUMO interacting motif (SIM), a previously unrecognized, but evolutionarily conserved, arginine-rich motif (ARM) in RNF4 acts as a novel recognition motif for selective target recruitment. Results from combined mutagenesis and computational modeling studies suggest that RNF4 utilizes concerted bimodular recognition, namely SIM for Lys-676 SUMOylation and ARM for Ser(P)-824 of simultaneously phosphorylated and SUMOylated KAP1 (Ser(P)-824-SUMO-KAP1). Furthermore, we proved that arginines 73 and 74 within the ARM of RNF4 are required for efficient recruitment to KAP1 or accelerated degradation of promyelocytic leukemia protein (PML) under stress. In parallel, results of bimolecular fluorescence complementation assays validated the role of the ARM in recognizing Ser(P)-824 in living cells. Taken together, we establish that the ARM is required for RNF4 to efficiently target Ser(P)-824-SUMO-KAP1, conferring ubiquitin Lys-48-mediated proteasomal degradation in the context of double strand breaks. The conservation of such a motif may possibly explain the requirement for timely substrate selectivity determination among a myriad of SUMOylated proteins under stress conditions. Thus, the ARM dynamically regulates the SIM-dependent recruitment of targets to RNF4, which could be critical to dynamically fine-tune the abundance of Ser(P)-824-SUMO-KAP1 and, potentially, other SUMOylated proteins during DNA damage response.

Published

2014

17. Functional and molecular features of the calmodulin-interacting protein IQCG required for haematopoiesis in zebrafish

Author

Ren-Ke Li, Wen-Xue Liang, Sai-Juan Chen, Lei Wang, Ting Xi Liu, Jue-Ling Tan, Liu-Fei Luo, Shan-He Yu, Guoyu Meng, Peng-Fei Xu, Keqin Kathy Li, Zhu Chen, Li-Ting Chen, and Shuo Chen

Subjects

Calmodulin, Regulator, General Physics and Astronomy, General Biochemistry, Genetics and Molecular Biology, Animals, HSP70 Heat-Shock Proteins, Transcriptional expression, Zebrafish, Calcium signaling, Cell Proliferation, Multidisciplinary, biology, Kinase, General Chemistry, Zebrafish Proteins, biology.organism_classification, Fusion protein, Cell biology, Hematopoiesis, Haematopoiesis, Gene Knockdown Techniques, biology.protein, Cancer research, Calcium-Calmodulin-Dependent Protein Kinase Type 4

Abstract

We previously reported a fusion protein NUP98-IQCG in an acute leukaemia, which functions as an aberrant regulator of transcriptional expression, yet the structure and function of IQCG have not been characterized. Here we use zebrafish to investigate the role of iqcg in haematopoietic development, and find that the numbers of haematopoietic stem cells and multilineage-differentiated cells are reduced in iqcg-deficient embryos. Mechanistically, IQCG binds to calmodulin (CaM) and acts as a molecule upstream of CaM-dependent kinase IV (CaMKIV). Crystal structures of complexes between CaM and IQ domain of IQCG reveal dual CaM-binding footprints in this motif, and provide a structural basis for a higher CaM-IQCG affinity when deprived of calcium. The results collectively allow us to understand IQCG-mediated calcium signalling in haematopoiesis, and propose a model in which IQCG stores CaM at low cytoplasmic calcium concentrations, and releases CaM to activate CaMKIV when calcium level rises.

Published

2013

18. DNA methyltransferases in hematologic malignancies

Author

Liu-Fei Luo, Keqin Kathy Li, Sai-Juan Chen, Jie Xu, Zhu Chen, and Yang Shen

Subjects

Genetics, Models, Molecular, Methyltransferase, Myelodysplastic syndromes, Myeloid leukemia, Hematology, Methylation, Biology, DNA Methylation, medicine.disease, DNA methyltransferase, DNA Methyltransferase 3A, Epigenesis, Genetic, Hematologic Neoplasms, DNA methylation, Mutation, DNMT1, medicine, Cancer research, Animals, Humans, Epigenetics, DNA (Cytosine-5-)-Methyltransferases, Molecular Targeted Therapy, Enzyme Inhibitors

Abstract

DNA methyltransferases (DNMTs) are the key enzymes for genome methylation, which plays an important role in epigenetically regulated gene expression and repression. Mouse models with conditional knockout of the DNA methyltransferase 1 (DNMT1) and DNA methyltransferase 3A (DNMT3A) genes have revealed a role of DNA methylation in mediating the self-renewal and differentiation of normal hematopoietic stem cells (HSCs) and the leukemia stem cells (LSCs). Recently, various mutations of DNMT3A and other DNA methylation regulators have been identified in hematologic malignancies. Functional analysis of these mutations may lead to a better understanding of the disease mechanisms, and even the discovery of new biomarkers and/or drug targets, as well as more rational design of therapeutic regimens. Moreover, DNMTs inhibitors as epigenetic drugs have already been approved by US Food and Drug Administration for clinical use and some clinical trials are currently underway in patients with myelodysplastic syndromes (MDS) and acute myeloid leukemia (AML). This review focuses on the biology of DNMTs with regard to epigenetic regulation, HSC renewal/differentiation, and drug discovery for targeted therapy, and delineates the latest studies that have been conducted to unfold the relationship between aberrant DNMTs and hematologic malignancies.

Published

2013

19. Natural Product Micheliolide (MCL) Irreversibly Activates Pyruvate Kinase M2 and Suppresses Leukemia.

Author

Jing Li, Shanshan Li, Jianshuang Guo, Qiuying Li, Jing Long, Cheng Ma, Yahui Ding, Chunli Yan, Liangwei Li, Zhigang Wu, He Zhu, Keqin Kathy Li, Liuqing Wen, Quan Zhang, Qingqing Xue, Caili Zhao, Ning Liu, Ivaylo Ivanov, Ming Luo, and Rimo Xi

Published

2018

20. Chemical and Biochemical Approaches in the Study of Histone Methylation and Demethylation

Author

Keqin Kathy Li, Cheng Luo, Dongxia Wang, Hualiang Jiang, and Y. George Zheng

Subjects

Pharmacology, Epigenomics, Histone Demethylases, Protein-Arginine N-Methyltransferases, Genome, Histone-Lysine N-Methyltransferase, Methylation, Article, Histones, Drug Discovery, Histone Methyltransferases, Molecular Medicine, Animals, Humans, Enzyme Inhibitors

Abstract

Histone methylation represents one of the most critical epigenetic events in DNA function regulation in eukaryotic organisms. Classic molecular biology and genetics tools provide significant knowledge about mechanisms and physiological roles of histone methyltransferases and demethylases in various cellular processes. In addition to this stream line, development and application of chemistry and chemistry-related techniques are increasingly involved in biological study, and offer information otherwise difficult to obtain by standard molecular biology methods. Herein, we review recent achievements and progress in developing and applying chemical and biochemical approaches in the study of histone methylation, including chromatin immunoprecipitation, chemical ligation, mass spectrometry, biochemical methylation and demethylation assays, and inhibitor development. These technological advances allow histone methylation to be studied from genome-wide level to molecular and atomic levels. With ChIP technology, information can be obtained about precise mapping of histone methylation patterns at specific promoters, genes, or other genomic regions. MS is particularly useful in detecting and analyzing methylation marks in histone and nonhistone protein substrates. Chemical approaches that permit site-specific incorporation of methyl groups into histone proteins greatly facilitate the investigation of biological impacts of methylation at individual modification sites. Discovery and design of selective organic inhibitors of histone methyltransferases and demethylases provide chemical probes to interrogate methylation-mediated cellular pathways. Overall, these chemistry-related technological advances have greatly improved our understanding of the biological functions of histone methylation in normal physiology and diseased states, and also are of great potential to translate basic epigenetics research into diagnostic and therapeutic applications in the clinic.

Published

2012

21. Application of epigenome-modifying small molecules in induced pluripotent stem cells

Author

Junyan, Lu, Xiangqian, Kong, Cheng, Luo, and Keqin Kathy, Li

Subjects

Epigenomics, Histones, Small Molecule Libraries, Induced Pluripotent Stem Cells, Drug Evaluation, Preclinical, Animals, Humans

Abstract

Recent breakthroughs in generating induced pluripotent stem cells (iPSCs) using four defined factors have revealed the potential utility of stem cells in biological research and clinical applications. However, the low efficiency and slow kinetics of reprogramming related to producing these cells and underlying safety issues, such as viral integration and genetic and epigenetic abnormalities of iPSCs, hamper the further application of iPSCs in laboratory and clinical settings. Previous studies have suggested that reprogramming efficiency can be enhanced and that reprogramming kinetics can be accelerated by manipulating epigenetic status. Herein, we review recent studies on the application of epigenome-modifying small molecules in enhancing reprogramming and functionally replacing some reprogramming factors. We mainly focus on studies that have used small molecules to interfere with epigenome-modifying enzymes, such as DNA methyltransferase, histone acetyltransferase, and histone methyltransferase. The potential use of these small molecules in inducing iPSCs and new ways to identify small molecules of higher potency and fewer side effects are also discussed.

Published

2012

22. DNA methylation as a target of epigenetic therapeutics in cancer

Author

Fangcheng Li, Keqin Kathy Li, Kun Yang, Bilian Jin, and Qiushi Shawna Li

Subjects

DNA (Cytosine-5-)-Methyltransferase 1, Cancer Research, Methyltransferase, DNMT3B, Antineoplastic Agents, Biology, Bioinformatics, medicine.disease_cause, DNA methyltransferase, Gene Expression Regulation, Enzymologic, DNA Methyltransferase 3A, Epigenesis, Genetic, Neoplasms, medicine, Humans, Epigenetics, Cancer epigenetics, DNA (Cytosine-5-)-Methyltransferases, Pharmacology, Genetic Therapy, DNA Methylation, Gene Expression Regulation, Neoplastic, DNA methylation, Molecular Medicine, Carcinogenesis, Epigenetic therapy

Abstract

Epigenetic alterations have been implicated in the development and progression of human cancer. It is noteworthy that epigenetic modifications, in contrast to genetic mutations, are intrinsically reversible. This triggers an impressive interest of researchers in treatment of cancer patients via targeting epigenetic mechanisms, leading to subsequent intensive investigations of epigenetic drugs as a novel therapeutic intervention. DNA methylation, the major form of epigenetic modifications, is catalyzed by the maintenance DNA methyltransferase (DNMT) 1 and/or the de novo methyltransferases DNMT3A and DNMT3B. Aberrant expression of DNMTs and disruption of DNA methylation are closely associated with multiple forms of cancer, although the exact mechanisms underlying this link remain elusive. An array of tumor suppressor genes (TSGs) frequently sustain promoter hypermethylation, which results in epigenetic silencing of these genes and makes cancer cells acquire growth advantages. DNA demethylating agents, re-activating TSGs via inhibiting hypermethylation of their promoter regions, are currently being tested in clinical trials, and several of them are already applied in clinics. DNA demethylating agents, used either alone or in combination with other agents, such as chemotherapeutic drugs and the histone deacetylase inhibitors, have shown to be effective in treatment of cancer, although only in a small set of patients. In this review, we examine and discuss the most recent advances in epigenetic therapy of cancer, with a focus on DNA demethylating agents.

Published

2012

23. Targeting of AML1-ETO in t(8;21) Leukemia by Oridonin Generates a Tumor Suppressor–Like Protein

Author

Haiyan Wu, Zhu Chen, Limin Chen, Ping Liu, Kevin Petrie, Keqin Kathy Li, Yin-Yin Xie, Yue-Ying Wang, Huang-Ming Cao, Tao Zhen, Jian-Xiang Liu, Ying Lu, Miao-Miao He, Sai-Juan Chen, Yang Liang, Guang-Biao Zhou, Chuanfeng Wu, and Wei-Na Zhang

Subjects

Myeloid, Oncogene Proteins, Fusion, Chromosomes, Human, Pair 21, Thioredoxin reductase, Intracellular Space, Chromosomal translocation, Pharmacology, Models, Biological, Translocation, Genetic, Mice, RUNX1 Translocation Partner 1 Protein, hemic and lymphatic diseases, medicine, Animals, Humans, Molecular Targeted Therapy, sub_healthsciences, Caspase 3, Protein Stability, business.industry, Tumor Suppressor Proteins, Myeloid leukemia, General Medicine, medicine.disease, Enzyme Activation, Mice, Inbred C57BL, Leukemia, Myeloid, Acute, Leukemia, medicine.anatomical_structure, Apoptosis, Core Binding Factor Alpha 2 Subunit, Neoplastic Stem Cells, Cancer research, Thioredoxin, Diterpenes, Kaurane, Reactive Oxygen Species, business, sub_biomedicalsciences, Chromosomes, Human, Pair 8

Abstract

Nearly 60% of acute myeloid leukemia (AML) patients with the t(8;21)(q22;q22) translocation fail to achieve long-term disease-free survival. Our previous studies demonstrated that oridonin selectively induces apoptosis of t(8;21) leukemia cells and causes cleavage of AML1-ETO oncoprotein resulting from t(8;21), but the underlying mechanisms remain unclear. We show that oridonin interacted with glutathione and thioredoxin/thioredoxin reductase to increase intracellular reactive oxygen species, which in turn activated caspase-3 in t(8;21) cells. Moreover, oridonin bound AML1-ETO, directing the enzymatic cleavage at aspartic acid 188 via caspase-3 to generate a truncated AML1-ETO (ΔAML1-ETO) and preventing the protein from further proteolysis. ΔAML1-ETO interacted with AML1-ETO and interfered with the trans-regulatory functions of remaining AML1-ETO oncoprotein, thus acting as a tumor suppressor that mediates the anti-leukemia effect of oridonin. Furthermore, oridonin inhibited the activity of c-Kit(+) leukemia-initiating cells. Therefore, oridonin is a potential lead compound for molecular target-based therapy of leukemia.

Published

2012

24. Molecular basis of NDM-1, a new antibiotic resistance determinant

Author

Mingyue Zheng, Cai Guang-Yang, Hualiang Jiang, Limin Chen, Kaixian Chen, Zhongjie Liang, Hong Liu, Yuanyuan Wang, Yao Hong, Keqin Kathy Li, Xu Shen, Xiangqian Kong, Cheng Luo, Lianchun Li, and Lefu Lan

Subjects

Models, Molecular, Antibiotics, lcsh:Medicine, Tigecycline, Drug resistance, Biophysics Simulations, Biochemical Simulations, Macromolecular Structure Analysis, Biomacromolecule-Ligand Interactions, lcsh:Science, Conserved Sequence, Multidisciplinary, Hydrolysis, Drug Resistance, Microbial, Bacterial Pathogens, Anti-Bacterial Agents, Zinc, Biophysic Al Simulations, Sequence Analysis, Research Article, Computer Modeling, Protein Binding, medicine.drug, medicine.drug_class, Biophysics, Biology, Microbiology, Meropenem, beta-Lactamases, Antibiotic resistance, Microbial Control, medicine, Point Mutation, Microbial Pathogens, Enzyme Assays, Thienamycins, lcsh:R, Computational Biology, medicine.disease, Carbapenems, Structural Homology, Protein, Computer Science, Biocatalysis, Colistin, lcsh:Q, Klebsiella pneumonia, Sequence Alignment

Abstract

The New Delhi Metallo-β-lactamase (NDM-1) was first reported in 2009 in a Swedish patient. A recent study reported that Klebsiella pneumonia NDM-1 positive strain or Escherichia coli NDM-1 positive strain was highly resistant to all antibiotics tested except tigecycline and colistin. These can no longer be relied on to treat infections and therefore, NDM-1 now becomes potentially a major global health threat. In this study, we performed modeling studies to obtain its 3D structure and NDM-1/antibiotics complex. It revealed that the hydrolytic mechanisms are highly conserved. In addition, the detailed analysis indicates that the more flexible and hydrophobic loop1, together with the evolution of more positive-charged loop2 leads to NDM-1 positive strain more potent and extensive in antibiotics resistance compared with other MBLs. Furthermore, through biological experiments, we revealed the molecular basis for antibiotics catalysis of NDM-1 on the enzymatic level. We found that NDM-1 enzyme was highly potent to degrade carbapenem antibiotics, while mostly susceptible to tigecycline, which had the ability to slow down the hydrolysis velocity of meropenem by NDM-1. Meanwhile, the mutagenesis experiments, including D124A, C208A, K211A and K211E, which displayed down-regulation on meropenem catalysis, proved the accuracy of our model. At present, there are no effective antibiotics against NDM-1 positive pathogen. Our study will provide clues to investigate the molecular basis of extended antibiotics resistance of NDM-1 and then accelerate the search for new antibiotics against NDM-1 positive strain in clinical studies.

Published

2011

25. Recurrent Mutations Found In Acute Monocytic Leukemia by Exomes Sequencing

Author

Chun-Ming Pan, Jie Xu, Jian-Qing Mi, Keqin Kathy Li, Sai-Juan Chen, Xiaojing Yan, Zhu Chen, Zhaohui Gu, Huai-Dong Song, Gang Lv, and Shen Yang

Subjects

Neuroblastoma RAS viral oncogene homolog, Genetics, NPM1, Point mutation, Immunology, Myeloid leukemia, Cell Biology, Hematology, Biology, Gene mutation, medicine.disease, Biochemistry, hemic and lymphatic diseases, Acute myelomonocytic leukemia, medicine, Acute monocytic leukemia, neoplasms, Exome sequencing

Abstract

Abstract 2490 Acute monocytic leukemia, the M5 subtype of acute myeloid leukemia (AML-M5), is a distinct group with characteristic clinical features and has been reported to have a poor prognosis. A subset of AML-M5 is associated with various chromosomal translocations involving the MLL locus at 11q23, while mutations are also reported in genes such as NPM1, FLT3, NRAS at different frequencies in this disease. However, these genetic changes occur only in a part of AML-M5 patients and some of them lack specificity due to the presence in other AML subtypes. To address the important genetic and molecular factors for the pathogenesis of M5 in a comprehensive manner, we sequenced exomes from nine AML-M5 initial bone marrow (BM) samples and matched control samples. We identified 64 somatic mutations within the coding sequences of 61 genes including 57 point mutations and 7 insertions or deletions (indels), among which 17 genes had at least 2 cases of mutations in 100 validated AML-M5 BM samples. We tested a part of these gene mutations in different subtypes of AML and found that some mutations are restricted to AML-M5 and AML-M4 (acute myelomonocytic leukemia) with more than 15% and 10% frequency, respectively. Thus, by systemic sequencing of exomes from a group of AML-M5 cases, we discovered recurring mutations that may play an essential role in the pathogenesis of AML with monocytic features.The prognostic significance of the mutations will be present in details. Disclosures: No relevant conflicts of interest to declare.

Published

2010

26. Targeting of AML1-ETO in t(8;21) Leukemia by Oridonin Generates a Tumor Suppressor-Like Protein.

Author

Tao Zhen, Chuan-Feng Wu, Ping Liu, Hai-Yan Wu, Guang-Biao Zhou, Ying Lu, Jian-Xiang Liu, Yang Liang, Keqin Kathy Li, Yue-Ying Wang, Yin-Yin Xie, Miao-Miao He, Huang-Ming Cao, Wei-Na Zhang, Li-Min Chen, Kevin Petrie, Sai-Juan Chen, and Zhu Chen

Published

2012

27. As4S4 targets RING-type E3 ligase c-CBL to induce degradation of BCR-ABL in chronic myelogenous leukemia.

Author

Jian-Hua Mao, Xiao-Yan Sun, Jian-Xiang Liu, Qun-Ye Zhang, Ping Lju, Qiu-Hua Huang, Keqin Kathy Li, Quan Chen, Zhu Chen, and Sai-Juan Chen

Subjects

NONMETALS, PRELEUKEMIA, ANEMIA, CANCER, APOPTOSIS

Abstract

Arsenic, a curative agent for acute promyelocytic leukemia, induces cell apoptosis and degradation of BCR-ABL in chronic myelogenous leukemia (CML). We demonstrated that ubiquitination and degradation of BCR-ABL was mediated by c-CBL a RING-type E3 ligase that was also shown to be involved in ubiquitination for many other receptor/protein tyrosine kinases. Our data showed that c-CBL protein was considerably up-regulated by arsenic sulfide (As454). Interestingly, arsenic directly bound the RING finger domain of c-CBL to inhibit its self-ubiquitination/degradation without interfering with the enhancement of ubiquitination and subsequent proteolysis of its substrate BCR-ABL. Degradation of BCR-ABL due to c-CBL induction as a result of arsenic treatment was also observed in vivo in CML mice. These findings provide insight into the molecular mechanisms of arsenic and further support its therapeutic applications in CML in combination with tyrosine kinase inhibitors and potentially also in other malignancies involving aberrant receptor/protein tyrosine kinase signaling. [ABSTRACT FROM AUTHOR]

Published

2010

28. An Arginine-rich Motif of Ring Finger Protein 4 (RNF4) Oversees the Recruitment and Degradation of the Phosphorylated and SUMOylated Krüppel-associated Box Domain-associated Protein 1 (KAP1)/TRIM28 Protein during Genotoxic Stress.

Author

Ching-Ying Kuo, Xu Li, Xiang-Qian Kong, Cheng Luo, Che-Chang Chang, Yiyin Chung, Hsiu-Ming Shih, Keqin Kathy Li, and Ann, David K.

Subjects

*ARGININE, *TRANSCRIPTION factors, *PHOSPHORYLATION, *DNA damage, *MUTAGENESIS, *GENETIC mutation

Abstract

Krüppel-associated box domain-associated protein 1 (KAP1) is a universal transcriptional corepressor that undergoes multiple posttranslational modifications (PTMs), including SUMOylation and Ser-824 phosphorylation. However, the functional interplay of KAP1 PTMs in regulating KAP1 turnover during DNA damage response remains unclear. To decipher the role and cross-talk of multiple KAP1 PTMs, we show here that DNA double strand break-induced KAP1 Ser-824 phosphorylation promoted the recruitment of small ubiquitin-like modifier (SUMO)-targeted ubiquitin E3 ligase, ring finger protein 4 (RNF4), and subsequent RNF4-mediated, SUMO-dependent degradation. Besides the SUMO interacting motif (SIM), a previously unrecognized, but evolutionarily conserved, argininerich motif (ARM) in RNF4 acts as a novel recognition motif for selective target recruitment. Results from combined mutagenesis and computational modeling studies suggest that RNF4 utilizes concerted bimodular recognition, namely SIM for Lys-676 SUMOylation and ARM for Ser(P)-824 of simultaneously phosphorylated and SUMOylated KAP1 (Ser(P)-824-SUMO-KAP1). Furthermore, we proved that arginines 73 and 74 within the ARM of RNF4 are required for efficient recruitment to KAP1 or accelerated degradation of promyelocytic leukemia protein (PML) under stress. In parallel, results of bimolecular fluorescence complementation assays validated the role of the ARM in recognizing Ser(P)-824 in living cells. Taken together, we establish that the ARM is required for RNF4 to efficiently target Ser(P)-824-SUMO-KAP1, conferring ubiquitin Lys-48-mediated proteasomal degradation in the context of double strand breaks. The conservation of such a motif may possibly explain the requirement for timely substrate selectivity determination among a myriad of SUMOylated proteins under stress conditions. Thus, the ARM dynamically regulates the SIM-dependent recruitment of targets to RNF4, which could be critical to dynamically fine-tune the abundance of Ser(P)-824-SUMOKAP1and, potentially, other SUMOylated proteins during DNA damage response. [ABSTRACT FROM AUTHOR]

Published

2014