Your search keyword '"Aaron Yun Chen"' showing total 27 results

1. Establishment of a reverse genetics system for studying human bocavirus in human airway epithelia.

Author

Qinfeng Huang, Xuefeng Deng, Ziying Yan, Fang Cheng, Yong Luo, Weiran Shen, Diana C M Lei-Butters, Aaron Yun Chen, Yi Li, Liang Tang, Maria Söderlund-Venermo, John F Engelhardt, and Jianming Qiu

Subjects

Immunologic diseases. Allergy, RC581-607, Biology (General), QH301-705.5

Abstract

Human bocavirus 1 (HBoV1) has been identified as one of the etiological agents of wheezing in young children with acute respiratory-tract infections. In this study, we have obtained the sequence of a full-length HBoV1 genome (including both termini) using viral DNA extracted from a nasopharyngeal aspirate of an infected patient, cloned the full-length HBoV1 genome, and demonstrated DNA replication, encapsidation of the ssDNA genome, and release of the HBoV1 virions from human embryonic kidney 293 cells. The HBoV1 virions generated from this cell line-based production system exhibits a typical icosahedral structure of approximately 26 nm in diameter, and is capable of productively infecting polarized primary human airway epithelia (HAE) from the apical surface. Infected HAE showed hallmarks of lung airway-tract injury, including disruption of the tight junction barrier, loss of cilia and epithelial cell hypertrophy. Notably, polarized HAE cultured from an immortalized airway epithelial cell line, CuFi-8 (originally derived from a cystic fibrosis patient), also supported productive infection of HBoV1. Thus, we have established a reverse genetics system and generated the first cell line-based culture system for the study of HBoV1 infection, which will significantly advance the study of HBoV1 replication and pathogenesis.

Published

2012

2. Productive parvovirus B19 infection of primary human erythroid progenitor cells at hypoxia is regulated by STAT5A and MEK signaling but not HIFα.

Author

Aaron Yun Chen, Steve Kleiboeker, and Jianming Qiu

Subjects

Immunologic diseases. Allergy, RC581-607, Biology (General), QH301-705.5

Abstract

Human parvovirus B19 (B19V) causes a variety of human diseases. Disease outcomes of bone marrow failure in patients with high turnover of red blood cells and immunocompromised conditions, and fetal hydrops in pregnant women are resulted from the targeting and destruction of specifically erythroid progenitors of the human bone marrow by B19V. Although the ex vivo expanded erythroid progenitor cells recently used for studies of B19V infection are highly permissive, they produce progeny viruses inefficiently. In the current study, we aimed to identify the mechanism that underlies productive B19V infection of erythroid progenitor cells cultured in a physiologically relevant environment. Here, we demonstrate an effective reverse genetic system of B19V, and that B19V infection of ex vivo expanded erythroid progenitor cells at 1% O(2) (hypoxia) produces progeny viruses continuously and efficiently at a level of approximately 10 times higher than that seen in the context of normoxia. With regard to mechanism, we show that hypoxia promotes replication of the B19V genome within the nucleus, and that this is independent of the canonical PHD/HIFα pathway, but dependent on STAT5A and MEK/ERK signaling. We further show that simultaneous upregulation of STAT5A signaling and down-regulation of MEK/ERK signaling boosts the level of B19V infection in erythroid progenitor cells under normoxia to that in cells under hypoxia. We conclude that B19V infection of ex vivo expanded erythroid progenitor cells at hypoxia closely mimics native infection of erythroid progenitors in human bone marrow, maintains erythroid progenitors at a stage conducive to efficient production of progeny viruses, and is regulated by the STAT5A and MEK/ERK pathways.

Published

2011

3. Chipmunk parvovirus is distinct from members in the genus Erythrovirus of the family Parvoviridae.

Author

Zhaojun Chen, Aaron Yun Chen, Fang Cheng, and Jianming Qiu

Subjects

Medicine, Science

Abstract

The transcription profile of chipmunk parvovirus (ChpPV), a tentative member of the genus Erythrovirus in the subfamily Parvovirinae of the family Parvoviridae, was characterized by transfecting a nearly full-length genome. We found that it is unique from the profiles of human parvovirus B19 and simian parvovirus, the members in the genus Erythrovirus so far characterized, in that the small RNA transcripts were not processed for encoding small non-structural proteins. However, like the large non-structural protein NS1 of the human parvovirus B19, the ChpPV NS1 is a potent inducer of apoptosis. Further phylogenetic analysis of ChpPV with other parvoviruses in the subfamily Parvovirinae indicates that ChpPV is distinct from the members in genus Erythrovirus. Thus, we conclude that ChpPV may represent a new genus in the family Parvoviridae.

Published

2010

4. Mechanism of dinitrochlorobenzene-induced dermatitis in mice: role of specific antibodies in pathogenesis.

Author

Elizabeth Yan Zhang, Aaron Yun Chen, and Bao Ting Zhu

Subjects

Medicine, Science

Abstract

Dinitrochlorobenzene-induced contact hypersensitivity is widely considered as a cell-mediated rather than antibody-mediated immune response. At present, very little is known about the role of antigen-specific antibodies and B cells in the development of dinitrochlorobenzene-induced hypersensitivity reactions, and this is the subject of the present investigation.Data obtained from multiple lines of experiments unequivocally showed that the formation of dinitrochlorobenzene-specific Abs played an important role in the development of dinitrochlorobenzene-induced contact hypersensitivity. The appearance of dinitrochlorobenzene-induced skin dermatitis matched in timing the appearance of the circulating dinitrochlorobenzene-specific antibodies. Adoptive transfer of sera containing dinitrochlorobenzene-specific antibodies from dinitrochlorobenzene-treated mice elicited a much stronger hypersensitivity reaction than the adoptive transfer of lymphocytes from the same donors. Moreover, dinitrochlorobenzene-induced contact hypersensitivity was strongly suppressed in B cell-deficient mice with no DNCB-specific antibodies. It was also observed that treatment of animals with dinitrochlorobenzene polarized Th cells into Th2 differentiation by increasing the production of Th2 cytokines while decreasing the production of Th1 cytokines.In striking contrast to the long-held belief that dinitrochlorobenzene-induced contact hypersensitivity is a cell-mediated immune response, the results of our present study demonstrated that the production of dinitrochlorobenzene-specific antibodies by activated B cells played an indispensible role in the pathogenesis of dinitrochlorobenzene-induced CHS. These findings may provide new possibilities in the treatment of human contact hypersensitivity conditions.

Published

2009

5. The 11-Kilodalton Nonstructural Protein of Human Parvovirus B19 Facilitates Viral DNA Replication by Interacting with Grb2 through Its Proline-Rich Motifs

Author

Aaron Yun Chen, Fang Cheng, Weiran Shen, Peng Xu, Steve Kleiboeker, Jianming Qiu, Safder S. Ganaie, Yi Li, and Xiaomei Wang

Subjects

MAPK/ERK pathway, DNA Replication, Proline, viruses, Immunology, Amino Acid Motifs, Viral Nonstructural Proteins, Virus Replication, Microbiology, Viral vector, Small hairpin RNA, Parvoviridae Infections, 03 medical and health sciences, Transduction (genetics), Virology, Parvovirus B19, Human, Humans, Phosphorylation, 030304 developmental biology, GRB2 Adaptor Protein, 0303 health sciences, Binding Sites, biology, 030306 microbiology, Cell growth, Parvovirus, DNA replication, biology.organism_classification, Cell biology, Virus-Cell Interactions, Molecular Weight, Lytic cycle, Insect Science, Mutation, Protein Binding

Abstract

Lytic infection of human parvovirus B19 (B19V) takes place exclusively in human erythroid progenitor cells of bone marrow and fetal liver, which disrupts erythropoiesis. During infection, B19V expresses three nonstructural proteins (NS1, 11-kDa, and 7.5-kDa) and two structural proteins (VP1 and VP2). While NS1 is essential for B19V DNA replication, 11-kDa enhances viral DNA replication significantly. In this study, we confirmed the enhancement role of 11-kDa in viral DNA replication and elucidated the underlying mechanism. We found that 11-kDa specially interacts with cellular growth factor receptor-bound protein 2 (Grb2) during virus infection and in vitro . We determined a high affinity interaction between 11-kDa and Grb2 that has an equilibrium dissociation constant ( K D ) value of 18.13 nM. In vitro , one proline-rich motif was sufficient for 11-kDa to sustain a strong interaction with Grb2. In consistence, in vivo during infection, one proline-rich motif was enough for 11-kDa to significantly reduce phosphorylation of extracellular signal-regulated kinase (ERK). Mutations of all three proline-rich motifs of 11-kDa abolished its capability to reduce ERK activity and, accordingly, decreased viral DNA replication. Transduction of a lentiviral vector encoding a short hairpin RNA (shRNA) targeting Grb2 decreased the expression of Grb2 as well as the level of ERK phosphorylation, which resulted in an increase of B19V replication. These results, in concert, indicate that the B19V 11-kDa protein interacts with cellular Grb2 to downregulate ERK activity, which upregulates viral DNA replication. IMPORTANCE Human parvovirus B19 (B19V) infection causes hematological disorders and is the leading cause of nonimmunological fetal hydrops during pregnancy. During infection, B19V expresses two structural proteins, VP1 and VP2, and three nonstructural proteins, NS1, 11-kDa, and 7.5-kDa. While NS1 is essential, 11-kDa plays an enhancing role in viral DNA replication. Here, we elucidated a mechanism underlying 11-kDa protein-regulated B19V DNA replication. 11-kDa is tightly associated with cellular growth factor receptor-bound protein 2 (Grb2) during infection. In vitro , 11-kDa interacts with Grb2 with high affinity through three proline-rich motifs, of which at least one is indispensable for the regulation of viral DNA replication. 11-kDa and Grb2 interaction disrupts extracellular signal-regulated kinase (ERK) signaling, which mediates upregulation of B19V replication. Thus, our study reveals a novel mechanism of how a parvoviral small nonstructural protein regulates viral DNA replication by interacting with a host protein that is predominately expressed in the cytoplasm.

Published

2018

6. Human Parvovirus B19 Utilizes Cellular DNA Replication Machinery for Viral DNA Replication

Author

Zekun Wang, Shui Qing Ye, Jianming Qiu, Wei Zou, Steve Kleiboeker, Peng Xu, Yomna Badawi, Hiroshi Nishimune, Aaron Yun Chen, Safder S. Ganaie, and Min Xiong

Subjects

CD36 Antigens, 0301 basic medicine, DNA Repair, DNA polymerase, Virus Replication, S Phase, chemistry.chemical_compound, Replication Protein A, Parvovirus B19, Human, Protein Interaction Maps, Phosphorylation, Erythroid Precursor Cells, biology, Cell Cycle, Genome Replication and Regulation of Viral Gene Expression, Cell biology, Host-Pathogen Interactions, Cell Division, DNA Replication, Gene Expression Regulation, Viral, DNA repair, DNA damage, Immunology, DNA viral genome, DNA, Single-Stranded, Genome, Viral, Red-Cell Aplasia, Pure, Microbiology, Cell Line, Parvoviridae Infections, 03 medical and health sciences, Virology, Humans, Viremia, Fetal Death, Replication protein A, DNA Polymerase beta, DNA Polymerase III, DNA replication, Cell Cycle Checkpoints, 030104 developmental biology, Bromodeoxyuridine, Viral replication, chemistry, Insect Science, DNA, Viral, biology.protein, Transcriptome, DNA, DNA Damage

Abstract

Human parvovirus B19 (B19V) infection of human erythroid progenitor cells (EPCs) induces a DNA damage response and cell cycle arrest at late S phase, which facilitates viral DNA replication. However, it is not clear exactly which cellular factors are employed by this single-stranded DNA virus. Here, we used microarrays to systematically analyze the dynamic transcriptome of EPCs infected with B19V. We found that DNA metabolism, DNA replication, DNA repair, DNA damage response, cell cycle, and cell cycle arrest pathways were significantly regulated after B19V infection. Confocal microscopy analyses revealed that most cellular DNA replication proteins were recruited to the centers of viral DNA replication, but not the DNA repair DNA polymerases. Our results suggest that DNA replication polymerase δ and polymerase α are responsible for B19V DNA replication by knocking down its expression in EPCs. We further showed that although RPA32 is essential for B19V DNA replication and the phosphorylated forms of RPA32 colocalized with the replicating viral genomes, RPA32 phosphorylation was not necessary for B19V DNA replication. Thus, this report provides evidence that B19V uses the cellular DNA replication machinery for viral DNA replication. IMPORTANCE Human parvovirus B19 (B19V) infection can cause transient aplastic crisis, persistent viremia, and pure red cell aplasia. In fetuses, B19V infection can result in nonimmune hydrops fetalis and fetal death. These clinical manifestations of B19V infection are a direct outcome of the death of human erythroid progenitors that host B19V replication. B19V infection induces a DNA damage response that is important for cell cycle arrest at late S phase. Here, we analyzed dynamic changes in cellular gene expression and found that DNA metabolic processes are tightly regulated during B19V infection. Although genes involved in cellular DNA replication were downregulated overall, the cellular DNA replication machinery was tightly associated with the replicating single-stranded DNA viral genome and played a critical role in viral DNA replication. In contrast, the DNA damage response-induced phosphorylated forms of RPA32 were dispensable for viral DNA replication.

Published

2018

7. RNA Binding Protein RBM38 Regulates Expression of the 11-Kilodalton Protein of Parvovirus B19, Which Facilitates Viral DNA Replication

Author

Safder S. Ganaie, Aaron Yun Chen, Peng Xu, Steve Kleiboeker, Chun Huang, Jianming Qiu, and Aifang Du

Subjects

0301 basic medicine, DNA Replication, Gene Expression Regulation, Viral, Viral nonstructural protein, viruses, Immunology, Down-Regulation, Erythema Infectiosum, RNA-binding protein, Biology, Viral Nonstructural Proteins, Virus Replication, Microbiology, 03 medical and health sciences, Virology, Parvovirus B19, Human, Humans, Gene knockdown, Messenger RNA, 030102 biochemistry & molecular biology, Alternative splicing, DNA replication, RNA-Binding Proteins, Cell biology, Genome Replication and Regulation of Viral Gene Expression, 030104 developmental biology, Viral replication, Insect Science, RNA splicing, DNA, Viral

Abstract

Human parvovirus B19 (B19V) expresses a single precursor mRNA (pre-mRNA), which undergoes alternative splicing and alternative polyadenylation to generate 12 viral mRNA transcripts that encode two structural proteins (VP1 and VP2) and three nonstructural proteins (NS1, 7.5-kDa protein, and 11-kDa protein). Splicing at the second 5′ donor site (D2 site) of the B19V pre-mRNA is essential for the expression of VP2 and the 11-kDa protein. We previously identified that cis -acting intronic splicing enhancer 2 (ISE2) that lies immediately after the D2 site facilitates the recognition of the D2 donor for its efficient splicing. In this study, we report that ISE2 is critical for the expression of the 11-kDa viral nonstructural protein. We found that ISE2 harbors a consensus RNA binding motif protein 38 (RBM38) binding sequence, 5′-UGUGUG-3′. RBM38 is expressed during the middle stage of erythropoiesis. We first confirmed that RBM38 binds specifically with the ISE2 element in vitro . The knockdown of RBM38 significantly decreases the level of spliced mRNA at D2 that encodes the 11-kDa protein but not that of the D2-spliced mRNA that encodes VP2. Importantly, we found that the 11-kDa protein enhances viral DNA replication and virion release. Accordingly, the knockdown of RBM38 decreases virus replication via downregulating 11-kDa protein expression. Taken together, these results suggest that the 11-kDa protein facilitates B19V DNA replication and that RBM38 is an essential host factor for B19V pre-mRNA splicing and for the expression of the 11-kDa protein. IMPORTANCE B19V is a human pathogen that can cause fifth disease, arthropathy, anemia in immunocompromised patients and sickle cell disease patients, myocarditis, and hydrops fetalis in pregnant women. Human erythroid progenitor cells (EPCs) are most susceptible to B19V infection and fully support viral DNA replication. The exclusive tropism of B19V for erythroid-lineage cells is dependent not only on the expression of viral receptors and coreceptors on the cell surface but also on the intracellular host factors that support B19V replication. Our present study shows that B19V uses a host factor, RNA binding motif protein 38 (RBM38), for the processing of its pre-mRNA during virus replication. Specifically, RBM38 interacts with the intronic splicing enhancer 2 (ISE2) element of B19V pre-mRNA and promotes 11-kDa protein expression, thereby regulating the 11-kDa protein-mediated augmentation of B19V replication. The identification of this novel host-pathogen interaction will provide mechanistic insights into B19V replication and aid in finding new targets for anti-B19V therapeutics.

Published

2017

8. TCF7L2 Variation and Proliferative Diabetic Retinopathy

Author

Srinivas R. Sadda, Yehong Zhuo, Jin Zhu, Jing Luo, Xiaohui Zhang, Aaron Yun Chen, Janet Lee, Yaojun Song, Kang Zhang, Hongrong Luo, Peter X. Shaw, Hong Ouyang, Sherrina Patel, Michael G. Rosenfeld, Jiagang Zhao, and Ling Zhao

Subjects

Vascular Endothelial Growth Factor A, endocrine system, medicine.medical_specialty, Genotype, endocrine system diseases, Endocrinology, Diabetes and Metabolism, 030209 endocrinology & metabolism, Retinal Neovascularization, Biology, Polymorphism, Single Nucleotide, Pathogenesis, Mice, 03 medical and health sciences, 0302 clinical medicine, Gene Frequency, Downregulation and upregulation, Internal medicine, Diabetes mellitus, Internal Medicine, medicine, Animals, Humans, Genetic Predisposition to Disease, Alleles, Genetic Association Studies, Original Research, 030304 developmental biology, 0303 health sciences, Diabetic Retinopathy, nutritional and metabolic diseases, Type 2 Diabetes Mellitus, Genetics/Genomes/Proteomics/Metabolomics, Diabetic retinopathy, Endoplasmic Reticulum Stress, medicine.disease, eye diseases, 3. Good health, Vascular endothelial growth factor A, Endocrinology, Diabetes Mellitus, Type 2, sense organs, Transcription Factor 7-Like 2 Protein, TCF7L2, Retinopathy

Abstract

Proliferative diabetic retinopathy (PDR) is the most severe vision-threatening complication of diabetes. For investigation of genetic association between TCF7L2 and PDR in Caucasian type 2 diabetes mellitus (T2DM) and its functional consequences, 383 T2DM patients with PDR (T2DM-PDR) and 756 T2DM patients without diabetic retinopathy (T2DM–no DR) were genotyped with rs7903146 in TCF7L2. We found that risk allele (T) frequency of rs7903146 was significantly higher in T2DM-PDR patients (allelic P = 2.52E-04). In lymphoblastoid cells induced to undergo endoplasmic reticulum (ER) stress by treatment of tunicamycin, higher fold change of TCF7L2 and VEGFA mRNA levels were observed in rs7903146-TT cells than in rs7903146-CC cells (P = 0.02 for TCF7L2; P = 0.004 for VEGFA), suggesting that ER stress plays a role in PDR pathogenesis. Silencing TCF7L2 resulted in decreased mRNA levels of both TCF7L2 and VEGFA (P < 0.001). Retinas of oxygen-induced retinopathy mice (a model for PDR) had higher TCF7L2 and VEGFA mRNA levels than those of controls (P = 2.9E-04 for TCF7L2; P = 1.9E-07 for VEGFA). Together, data from our study show that TCF7L2-rs7903146 is associated with PDR in Caucasian T2DM and suggest that TCF7L2 promotes pathological retinal neovascularization via ER stress–dependent upregulation of VEGFA.

Published

2013

9. Depletion and recovery of lymphoid subsets following morphine administration

Author

Thomas M. Yankee, J Qiu, Elizabeth Yan Zhang, Juan Xiong, Brooks L. Parker, P E Fields, Aaron Yun Chen, and Xiaochao Ma

Subjects

Pharmacology, medicine.medical_specialty, Lymphocyte, medicine.medical_treatment, Spleen, Immunosuppression, Biology, Endocrinology, medicine.anatomical_structure, Internal medicine, Precursor cell, Immunology, medicine, Morphine, Bone marrow, Lymph, Ex vivo, medicine.drug

Abstract

BACKGROUND AND PURPOSE Opioid use and abuse has been linked to significant immunosuppression, which has been attributed, in part, to drug-induced depletion of lymphocytes. We sought to define the mechanisms by which lymphocyte populations are depleted and recover following morphine treatment in mice. EXPERIMENTAL APPROACH Mice were implanted with morphine pellets and B- and T-cell subsets in the bone marrow, thymus, spleen and lymph nodes were analysed at various time points. We also examined the effects of morphine on T-cell development using an ex vivo assay. KEY RESULTS The lymphocyte populations most susceptible to morphine-induced depletion were the precursor cells undergoing selection. As the lymphocytes recovered, more lymphocyte precursors proliferated than in control mice. In addition, peripheral T-cells displayed evidence that they had undergone homeostatic proliferation during the recovery phase of the experiments. CONCLUSIONS AND IMPLICATIONS The recovery of lymphocytes following morphine-induced depletion occurred in the presence of morphine and via increased proliferation of lymphoid precursors and homeostatic proliferation of T-cells. LINKED ARTICLE This article is commented on by Eisenstein, pp. 1826–1828 of this issue. To view this commentary visit http://dx.doi.org/10.1111/j.1476-5381.2011.01513.x

Published

2011

10. Bocavirus Infection Induces Mitochondrion-Mediated Apoptosis and Cell Cycle Arrest at G 2 /M Phase

Author

Aaron Yun Chen, Yong Luo, Jianming Qiu, Fang Cheng, and Yuning Sun

Subjects

Programmed cell death, Cell cycle checkpoint, Cell division, Immunology, Apoptosis, Genome, Viral, Biology, Virus Replication, Microbiology, Cell Line, Bocavirus, Parvoviridae Infections, Dogs, Virology, Animals, Cytopathic effect, Cyclin-dependent kinase 1, Cell Cycle, Cell cycle, musculoskeletal system, Mitochondria, Virus-Cell Interactions, Cell biology, body regions, Viral replication, Insect Science, human activities, Cell Division

Abstract

Bocavirus is a newly classified genus of the family Parvovirinae . Infection with Bocavirus minute virus of canines (MVC) produces a strong cytopathic effect in permissive Walter Reed/3873D (WRD) canine cells. We have systematically characterized the MVC infection-produced cytopathic effect in WRD cells, namely, the cell death and cell cycle arrest, and carefully examined how MVC infection induces the cytopathic effect. We found that MVC infection induces an apoptotic cell death characterized by Bax translocalization to the mitochondrial outer membrane, disruption of the mitochondrial outer membrane potential, and caspase activation. Moreover, we observed that the activation of caspases occurred only when the MVC genome was replicating, suggesting that replication of the MVC genome induces apoptosis. MVC infection also induced a gradual cell cycle arrest from the S phase in early infection to the G 2 /M phase at a later stage, which was confirmed by the upregulation of cyclin B1 and phosphorylation of cdc2. Cell cycle arrest at the G 2 /M phase was reproduced by transfection of a nonreplicative NS1 knockout mutant of the MVC infectious clone, as well as by inoculation of UV-irradiated MVC. In contrast with other parvoviruses, only expression of the MVC proteins by transfection did not induce apoptosis or cell cycle arrest. Taken together, our results demonstrate that MVC infection induces a mitochondrion-mediated apoptosis that is dependent on the replication of the viral genome, and the MVC genome per se is able to arrest the cell cycle at the G 2 /M phase. Our results may shed light on the molecular pathogenesis of Bocavirus infection in general.

Published

2010

11. The Capsid Proteins of Aleutian Mink Disease Virus Activate Caspases and Are Specifically Cleaved during Infection

Author

Aaron Yun Chen, Fang Cheng, Jianming Qiu, Sonja M. Best, David J. Pintel, and Marshall E. Bloom

Subjects

Recombinant Fusion Proteins, viruses, Molecular Sequence Data, Immunology, Aleutian Mink Disease, Microbiology, Virus, Cell Line, Virology, biology.animal, Aleutian Mink Disease Virus, Animals, Humans, Amino Acid Sequence, Mink, Peptide sequence, Caspase, Parvoviridae, biology, Parvovirus, Structure and Assembly, Temperature, biology.organism_classification, Molecular biology, Enzyme Activation, Isoenzymes, Capsid, Caspases, Insect Science, Cats, biology.protein, Capsid Proteins

Abstract

Aleutian mink disease virus (AMDV) is currently the only known member of the genus Amdovirus in the family Parvoviridae . It is the etiological agent of Aleutian disease of mink. We have previously shown that a small protein with a molecular mass of approximately 26 kDa was present during AMDV infection and following transfection of capsid expression constructs (J. Qiu, F. Cheng, L. R. Burger, and D. Pintel, J. Virol. 80:654-662, 2006). In this study, we report that the capsid proteins were specifically cleaved at aspartic acid residue 420 (D420) during virus infection, resulting in the previously observed cleavage product. Mutation of a single amino acid residue at D420 abolished the specific cleavage. Expression of the capsid proteins alone in Crandell feline kidney (CrFK) cells reproduced the cleavage of the capsid proteins in virus infection. More importantly, capsid protein expression alone induced active caspases, of which caspase-10 was the most active. Active caspases, in turn, cleaved capsid proteins in vivo . Our results also showed that active caspase-7 specifically cleaved capsid proteins at D420 in vitro . These results suggest that viral capsid proteins alone induce caspase activation, resulting in cleavage of capsid proteins. We also provide evidence that AMDV mutants resistant to caspase-mediated capsid cleavage increased virus production approximately 3- to 5-fold in CrFK cells compared to that produced from the parent virus AMDV-G at 37°C but not at 31.8°C. Collectively, our results indicate that caspase activity plays multiple roles in AMDV infection and that cleavage of the capsid proteins might have a role in regulating persistent infection of AMDV.

Published

2010

12. The small 11kDa nonstructural protein of human parvovirus B19 plays a key role in inducing apoptosis during B19 virus infection of primary erythroid progenitor cells

Author

Elizabeth Yan Zhang, Jianming Qiu, Steve Kleiboeker, Thomas M. Yankee, Wuxiang Guan, Aaron Yun Chen, and Fang Cheng

Subjects

Programmed cell death, Immunoblotting, Immunology, Apoptosis, Cysteine Proteinase Inhibitors, Viral Nonstructural Proteins, Transfection, Biochemistry, Amino Acid Chloromethyl Ketones, Cell Line, In Situ Nick-End Labeling, Parvovirus B19, Human, Humans, Caspase 10, Cells, Cultured, Erythroid Precursor Cells, Caspase, biology, Reverse Transcriptase Polymerase Chain Reaction, Cell Biology, Hematology, Flow Cytometry, Caspase Inhibitors, Molecular biology, Cell biology, Molecular Weight, Cell culture, Host-Pathogen Interactions, Quinolines, biology.protein, K562 Cells, HeLa Cells, K562 cells

Abstract

Human parvovirus B19 (B19V) infection shows a strong erythroid tropism and drastically destroys erythroid progenitor cells, thus leading to most of the disease outcomes associated with B19V infection. In this study, we systematically examined the 3 B19V nonstructural proteins, 7.5kDa, 11kDa, and NS1, for their function in inducing apoptosis in transfection of primary ex vivo–expanded erythroid progenitor cells, in comparison with apoptosis induced during B19V infection. Our results show that 11kDa is a more significant inducer of apoptosis than NS1, whereas 7.5kDa does not induce apoptosis. Furthermore, we determined that caspase-10, an initiator caspase in death receptor signaling, is the most active caspase in apoptotic erythroid progenitors induced by 11kDa and NS1 as well as during B19V infection. More importantly, cytoplasm-localized 11kDa is expressed at least 100 times more than nucleus-localized NS1 at the protein level in primary erythroid progenitor cells infected with B19V; and inhibition of 11kDa expression using antisense oligos targeting specifically to the 11kDa-encoding mRNAs reduces apoptosis significantly during B19V infection of erythroid progenitor cells. Taken together, these results demonstrate that the 11kDa protein contributes to erythroid progenitor cell death during B19V infection.

Published

2010

13. Molecular characterization of human parvovirus B19 genotypes 2 and 3

Author

Zhaojun Chen, Fang Cheng, Wuxiang Guan, Aaron Yun Chen, and Jianming Qiu

Subjects

Genotype, Replication, Apoptosis, Genome, Viral, Viral Nonstructural Proteins, Transfection, Genome, Article, Cell Line, Parvovirus, 03 medical and health sciences, Transcription (biology), Virology, Parvovirus B19, Human, Humans, RNA, Messenger, Gene, 030304 developmental biology, DNA Primers, Genetics, 0303 health sciences, biology, Base Sequence, 030306 microbiology, B19, Gene Expression Profiling, Intron, Terminal Repeat Sequences, RNA, Chromosome Mapping, biology.organism_classification, Molecular biology, Recombinant Proteins, 3. Good health, Gene expression profiling, RNA, Viral, Transcription

Abstract

We have characterized the transcription profiles of parvovirus B19 (B19V) genotype-2 A6 and genotype-3 V9 variants. The A6 RNA profile differs from that of the prototype B19V in both B19V non-permissive and permissive cells, whereas the overall profile of the V9 RNA in these cells is similar to that of the prototype. A unique feature we have identified is that the genotype-2 A6 variant used only one splice acceptor to remove the first intron. We also demonstrated that the inverted terminal repeats (ITRs) of the prototype B19V support replication of the V9 genome, which produces infectious virus, but not that of the A6 genome, in B19V-permissive cells. Similar to the proapoptotic nature of the prototype B19V large non-structural protein (NS1), the A6 and V9 NS1 proteins also are potent inducers of apoptosis in B19V-permissive cells.

Published

2009

14. Condensin I and II Complexes License Full Estrogen Receptor α-Dependent Enhancer Activation

Author

Daria Merkurjev, Wenbo Li, Xiang Zhou, Qi Ma, Michael G. Rosenfeld, Jie Zhang, Soohwan Oh, Yiren Hu, Aaron Yun Chen, Xiaoyuan Song, Kenny Ohgi, Bogdan Tanasa, Wen Liu, Zhijie Liu, and Xin He

Subjects

Condensin, Enhancer RNAs, Medical and Health Sciences, Models, 2.1 Biological and endogenous factors, RNA, Neoplasm, Aetiology, Promoter Regions, Genetic, Cancer, Regulation of gene expression, Adenosine Triphosphatases, biology, Estradiol, Adaptor Proteins, Nuclear Proteins, DNA, Neoplasm, Biological Sciences, Chromatin, Ubiquitin ligase, Cell biology, Nuclear Receptor Interacting Protein 1, DNA-Binding Proteins, Enhancer Elements, Genetic, Gene Knockdown Techniques, MCF-7 Cells, Female, Protein Binding, Enhancer Elements, Ubiquitin-Protein Ligases, 1.1 Normal biological development and functioning, Molecular Sequence Data, Breast Neoplasms, macromolecular substances, Models, Biological, Article, Promoter Regions, Condensin complex, Genetic, Underpinning research, Breast Cancer, Genetics, Humans, Enhancer, Molecular Biology, Interphase, Adaptor Proteins, Signal Transducing, Binding Sites, Base Sequence, Signal Transducing, Estrogen Receptor alpha, Ubiquitination, Cell Biology, DNA, Biological, Molecular biology, Estrogen, Multiprotein Complexes, biology.protein, Neoplasm, RNA, Generic health relevance, Estrogen receptor alpha, Developmental Biology

Abstract

Enhancers instruct spatio-temporally specific gene expression in a manner tightly linked to higher-order chromatin architecture. Critical chromatin architectural regulators condensin I and condensin II play non-redundant roles controlling mitotic chromosomes. But the chromosomal locations of condensins and their functional roles in interphase are poorly understood. Here we report that both condensin complexes exhibit an unexpected, dramatic estrogen-induced recruitment to estrogen receptor α (ER-α)-bound eRNA(+) active enhancers in interphase breast cancer cells, exhibiting non-canonical interaction with ER-α via its DNA-binding domain (DBD). Condensins positively regulate ligand-dependent enhancer activation at least in part by recruiting an E3 ubiquitin ligase, HECTD1, to modulate the binding of enhancer-associated coactivators/corepressors, including p300 and RIP140, permitting full eRNA transcription, formation of enhancer:promoter looping, and the resultant coding gene activation. Collectively, our results reveal an important, unanticipated transcriptional role of interphase condensins in modulating estrogen-regulated enhancer activation and coding gene transcriptional program.

Published

2015

15. RNA Binding Protein RBM38 Regulates Expression of the 11-Kilodalton Protein of Parvovirus B19, Which Facilitates Viral DNA Replication.

Author

Ganaie, Safder S., Aaron Yun Chen, Chun Huang, Peng Xu, Kleiboeker, Steve, Aifang Du, and Jianming Qiu

Subjects

*RNA-binding proteins, *PROTEIN expression, *PARVOVIRUS B19, *DNA replication, *ERYTHROPOIESIS

Abstract

Human parvovirus B19 (B19V) expresses a single precursor mRNA (pre-mRNA), which undergoes alternative splicing and alternative polyadenylation to generate 12 viral mRNA transcripts that encode two structural proteins (VP1 and VP2) and three nonstructural proteins (NS1, 7.5-kDa protein, and 11-kDa protein). Splicing at the second 5′ donor site (D2 site) of the B19V pre-mRNA is essential for the expression of VP2 and the 11-kDa protein. We previously identified that cis-acting intronic splicing enhancer 2 (ISE2) that lies immediately after the D2 site facilitates the recognition of the D2 donor for its efficient splicing. In this study, we report that ISE2 is critical for the expression of the 11-kDa viral nonstructural protein. We found that ISE2 harbors a consensus RNA binding motif protein 38 (RBM38) binding sequence, 5′-UGUGUG-3′. RBM38 is expressed during the middle stage of erythropoiesis. We first confirmed that RBM38 binds specifically with the ISE2 element in vitro. The knockdown of RBM38 significantly decreases the level of spliced mRNA at D2 that encodes the 11-kDa protein but not that of the D2-spliced mRNA that encodes VP2. Importantly, we found that the 11-kDa protein enhances viral DNA replication and virion release. Accordingly, the knockdown of RBM38 decreases virus replication via downregulating 11-kDa protein expression. Taken together, these results suggest that the 11-kDa protein facilitates B19V DNA replication and that RBM38 is an essential host factor for B19V pre-mRNA splicing and for the expression of the 11-kDa protein. IMPORTANCE B19V is a human pathogen that can cause fifth disease, arthropathy, anemia in immunocompromised patients and sickle cell disease patients, myocarditis, and hydrops fetalis in pregnant women. Human erythroid progenitor cells (EPCs) are most susceptible to B19V infection and fully support viral DNA replication. The exclusive tropism of B19V for erythroid-lineage cells is dependent not only on the expression of viral receptors and coreceptors on the cell surface but also on the intracellular host factors that support B19V replication. Our present study shows that B19V uses a host factor, RNA binding motif protein 38 (RBM38), for the processing of its pre-mRNA during virus replication. Specifically, RBM38 interacts with the intronic splicing enhancer 2 (ISE2) element of B19V pre-mRNA and promotes 11-kDa protein expression, thereby regulating the 11-kDa protein-mediated augmentation of B19V replication. The identification of this novel host-pathogen interaction will provide mechanistic insights into B19V replication and aid in finding new targets for anti-B19V therapeutics. [ABSTRACT FROM AUTHOR]

Published

2018

16. Establishment of a Reverse Genetics System for Studying Human Bocavirus in Human Airway Epithelia

Author

Jianming Qiu, Yi Li, Qinfeng Huang, Xuefeng Deng, John F. Engelhardt, Yong Luo, Fang Cheng, Ziying Yan, Liang Tang, Maria Söderlund-Venermo, Diana C.M. Lei-Butters, Weiran Shen, and Aaron Yun Chen

Subjects

Respiratory System, Virus Replication, Genome, Epithelium, Emerging Viral Diseases, Human bocavirus, Cell polarity, lcsh:QH301-705.5, Respiratory Tract Infections, 0303 health sciences, 3. Good health, Female, Research Article, lcsh:Immunologic diseases. Allergy, Immunology, Molecular Sequence Data, Genome, Viral, Biology, Transfection, Microbiology, Cell Line, Parvoviridae Infections, 03 medical and health sciences, Virology, Genetics, Viral Nucleic Acid, Humans, Molecular Biology, 030304 developmental biology, Base Sequence, 030306 microbiology, HEK 293 cells, Inverted Repeat Sequences, DNA replication, Epithelial Cells, Sequence Analysis, DNA, biology.organism_classification, Molecular biology, Reverse genetics, Viral Replication, Reverse Genetics, Viral replication, lcsh:Biology (General), Cell culture, DNA, Viral, Parasitology, lcsh:RC581-607

Abstract

Human bocavirus 1 (HBoV1) has been identified as one of the etiological agents of wheezing in young children with acute respiratory-tract infections. In this study, we have obtained the sequence of a full-length HBoV1 genome (including both termini) using viral DNA extracted from a nasopharyngeal aspirate of an infected patient, cloned the full-length HBoV1 genome, and demonstrated DNA replication, encapsidation of the ssDNA genome, and release of the HBoV1 virions from human embryonic kidney 293 cells. The HBoV1 virions generated from this cell line-based production system exhibits a typical icosahedral structure of approximately 26 nm in diameter, and is capable of productively infecting polarized primary human airway epithelia (HAE) from the apical surface. Infected HAE showed hallmarks of lung airway-tract injury, including disruption of the tight junction barrier, loss of cilia and epithelial cell hypertrophy. Notably, polarized HAE cultured from an immortalized airway epithelial cell line, CuFi-8 (originally derived from a cystic fibrosis patient), also supported productive infection of HBoV1. Thus, we have established a reverse genetics system and generated the first cell line-based culture system for the study of HBoV1 infection, which will significantly advance the study of HBoV1 replication and pathogenesis., Author Summary Human bocavirus 1 (HBoV1) has been identified as one of the etiological agents of wheezing in young children with acute respiratory-tract infections. HBoV1 productively infects polarized primary human airway epithelia. However, no cell lines permissive to HBoV1 infection have yet been established. More importantly, the sequences at both ends of the HBoV1 genome have remained unknown. We have resolved both of these issues in this study. We have sequenced a full-length HBoV1 genome and cloned it into a plasmid. We further demonstrated that this HBoV1 plasmid replicated and produced viruses in human embryonic kidney 293 cells. Infection of these HBoV1 progeny virions produced obvious cytopathogenic effects in polarized human airway epithelia, which were represented by disruption of the epithelial barrier. Moreover, we identified an airway epithelial cell line supporting HBoV1 infection, when it was polarized. This is the first study to obtain the full-length HBoV1 genome, to demonstrate pathogenesis of HBoV1 infection in human airway epithelia, and to identify the first cell line to support productive HBoV1 infection.

Published

2012

17. Functional roles of enhancer RNAs for oestrogen-dependent transcriptional activation

Author

Daria Merkurjev, Wenbo Li, Xiaoyuan Song, Qi Ma, Soohwan Oh, Christopher K. Glass, Dimple Notani, Bogdan Tanasa, Hong-Sook Kim, Michael G. Rosenfeld, Jie Zhang, Aaron Yun Chen, Kenneth A. Ohgi, and Esperanza Nunez

Subjects

Transcriptional Activation, RNA, Untranslated, Transcription, Genetic, Chromosomal Proteins, Non-Histone, Enhancer RNAs, Cell Cycle Proteins, Biology, Ligands, Article, Transcription (biology), Gene expression, Humans, Enhancer, Promoter Regions, Genetic, Gene, Genetics, Regulation of gene expression, Multidisciplinary, Estradiol, Estrogen Receptor alpha, RNA, Estrogens, Research Highlight, Enhancer Elements, Genetic, MCF-7 Cells, Nucleic Acid Conformation, Estrogen receptor alpha

Abstract

The functional importance of gene enhancers in regulated gene expression is well established. In addition to widespread transcription of long non-coding RNAs (lncRNAs) in mammalian cells, bidirectional ncRNAs are transcribed on enhancers, and are thus referred to as enhancer RNAs (eRNAs). However, it has remained unclear whether these eRNAs are functional or merely a reflection of enhancer activation. Here we report that in human breast cancer cells 17β-oestradiol (E2)-bound oestrogen receptor α (ER-α) causes a global increase in eRNA transcription on enhancers adjacent to E2-upregulated coding genes. These induced eRNAs, as functional transcripts, seem to exert important roles for the observed ligand-dependent induction of target coding genes, increasing the strength of specific enhancer-promoter looping initiated by ER-α binding. Cohesin, present on many ER-α-regulated enhancers even before ligand treatment, apparently contributes to E2-dependent gene activation, at least in part by stabilizing E2/ER-α/eRNA-induced enhancer-promoter looping. Our data indicate that eRNAs are likely to have important functions in many regulated programs of gene transcription.

Published

2012

18. Parvovirus infection-induced cell death and cell cycle arrest

Author

Jianming Qiu and Aaron Yun Chen

Subjects

Programmed cell death, Cell cycle checkpoint, biology, Parvovirus, animal diseases, viruses, Cell, Parvovirus infection, virus diseases, Bovine parvovirus, biology.organism_classification, medicine.disease, Virology, Article, medicine.anatomical_structure, Apoptosis, medicine, Minute virus of mice

Abstract

The cytopathic effects induced during parvovirus infection have been widely documented. Parvovirus infection-induced cell death is often directly associated with disease outcomes (e.g., anemia resulting from loss of erythroid progenitors during parvovirus B19 infection). Apoptosis is the major form of cell death induced by parvovirus infection. However, nonapoptotic cell death, namely necrosis, has also been reported during infection of the minute virus of mice, parvovirus H-1 and bovine parvovirus. Recent studies have revealed multiple mechanisms underlying the cell death during parvovirus infection. These mechanisms vary in different parvoviruses, although the large nonstructural protein (NS)1 and the small NS proteins (e.g., the 11 kDa of parvovirus B19), as well as replication of the viral genome, are responsible for causing infection-induced cell death. Cell cycle arrest is also common, and contributes to the cytopathic effects induced during parvovirus infection. While viral NS proteins have been indicated to induce cell cycle arrest, increasing evidence suggests that a cellular DNA damage response triggered by an invading single-stranded parvoviral genome is the major inducer of cell cycle arrest in parvovirus-infected cells. Apparently, in response to infection, cell death and cell cycle arrest of parvovirus-infected cells are beneficial to the viral cell lifecycle (e.g., viral DNA replication and virus egress). In this article, we will discuss recent advances in the understanding of the mechanisms underlying parvovirus infection-induced cell death and cell cycle arrest.

Published

2011

19. Bocavirus infection induces a DNA damage response that facilitates viral DNA replication and mediates cell death

Author

Aaron Yun Chen, Yong Luo, and Jianming Qiu

Subjects

DNA Replication, Programmed cell death, Small interfering RNA, DNA damage, Immunology, Cell Cycle Proteins, Ataxia Telangiectasia Mutated Proteins, Protein Serine-Threonine Kinases, Virus Replication, Microbiology, Cell Line, Bocavirus, Histones, Dogs, Virology, Replication Protein A, Animals, Replication protein A, biology, Cell Death, Parvovirus, Tumor Suppressor Proteins, DNA replication, biology.organism_classification, Molecular biology, Virus-Cell Interactions, DNA-Binding Proteins, Viral replication, Apoptosis, Insect Science, DNA Damage

Abstract

Minute virus of canines (MVC) is an autonomous parvovirus that replicates efficiently without helper viruses in Walter Reed/3873D (WRD) canine cells. We previously showed that MVC infection induces mitochondrion-mediated apoptosis and G 2 /M-phase arrest in infected WRD cells. However, the mechanism responsible for these effects has not been established. Here, we report that MVC infection triggers a DNA damage response in infected cells, as evident from phosphorylation of H2AX and RPA32. We discovered that both ATM (ataxia telangiectasia-mutated kinase) and ATR (ATM- and Rad3-related kinase) were phosphorylated in MVC-infected WRD cells and confirmed that ATM activation was responsible for the phosphorylation of H2AX, whereas ATR activation was required for the phosphorylation of RPA32. Both pharmacological inhibition of ATM activation and knockdown of ATM in MVC-infected cells led to a significant reduction in cell death, a moderate correction of cell cycle arrest, and most importantly, a reduction in MVC DNA replication and progeny virus production. Parallel experiments with an ATR-targeted small interfering RNA (siRNA) had no effect. Moreover, we identified that this ATM-mediated cell death is p53 dependent. In addition, we localized the Mre11-Rad50-Nbs1 (MRN) complex, the major mediator as well as a substrate of the ATM-mediated DNA damage response pathway to MVC replication centers during infection, and show that Mre11 knockdown led to a reduction in MVC DNA replication. Our findings are the first to support the notion that an autonomous parvovirus is able to hijack the host DNA damage machinery for its own replication and for the induction of cell death.

Published

2010

20. Role of Erythropoietin Receptor Signaling in Parvovirus B19 Replication in Human Erythroid Progenitor Cells▿

Author

Wuxiang Guan, Steve Kleiboeker, Zhengwen Liu, Sai Lou, Aaron Yun Chen, and Jianming Qiu

Subjects

CD36 Antigens, Receptor expression, Immunology, Blotting, Western, Genetic Vectors, Fluorescent Antibody Technique, Biology, Virus Replication, Microbiology, Parvoviridae Infections, Virology, hemic and lymphatic diseases, medicine, Parvovirus B19, Human, Receptors, Erythropoietin, Humans, Progenitor cell, Phosphorylation, RNA, Small Interfering, Tropism, Erythroid Precursor Cells, Janus kinase 2, Reverse Transcriptase Polymerase Chain Reaction, Lentivirus, Janus Kinase 2, Tyrphostins, Flow Cytometry, Molecular biology, Cell biology, Erythropoietin receptor, Virus-Cell Interactions, Haematopoiesis, Blotting, Southern, Viral Tropism, Erythropoietin, Insect Science, embryonic structures, biology.protein, medicine.drug, circulatory and respiratory physiology, Signal Transduction

Abstract

Parvovirus B19 (B19V) infection is highly restricted to human erythroid progenitor cells. Although previous studies have led to the theory that the basis of this tropism is receptor expression, this has been questioned by more recent observation. In the study reported here, we have investigated the basis of this tropism, and a potential role of erythropoietin (Epo) signaling, in erythroid progenitor cells (EPCs) expanded ex vivo from CD34 + hematopoietic cells in the absence of Epo (CD36 + /Epo − EPCs). We show, first, that CD36 + /Epo − EPCs do not support B19V replication, in spite of B19V entry, but Epo exposure either prior to infection or after virus entry enabled active B19V replication. Second, when Janus kinase 2 (Jak2) phosphorylation was inhibited using the inhibitor AG490, phosphorylation of the Epo receptor (EpoR) was also inhibited, and B19V replication in ex vivo -expanded erythroid progenitor cells exposed to Epo (CD36 + /Epo + EPCs) was abolished. Third, expression of constitutively active EpoR in CD36 + /Epo − EPCs led to efficient B19V replication. Finally, B19V replication in CD36 + /Epo + EPCs required Epo, and the replication response was dose dependent. Our findings demonstrate that EpoR signaling is absolutely required for B19V replication in ex vivo -expanded erythroid progenitor cells after initial virus entry and at least partly accounts for the remarkable tropism of B19V infection for human erythroid progenitors.

Published

2010

21. Molecular Characterization of Infectious Clones of the Minute Virus of Canines Reveals Unique Features of Bocaviruses▿

Author

Wuxiang Guan, Fang Cheng, Aaron Yun Chen, F. Brent Johnson, Jianming Qiu, and Yuning Sun

Subjects

clone (Java method), Bocaparvovirus, Transcription, Genetic, Immunology, DNA Mutational Analysis, Molecular Sequence Data, Molecular cloning, Virus Replication, Microbiology, Genome, Virus, Cell Line, Bocavirus, Open Reading Frames, Viral Proteins, Dogs, Virology, Sequence Homology, Nucleic Acid, RNA Precursors, Animals, Cloning, Molecular, Genetics, biology, Human bocavirus, Inverted Repeat Sequences, Bovine parvovirus, Sequence Analysis, DNA, biology.organism_classification, Viral replication, Genetic Diversity and Evolution, Insect Science, DNA, Viral

Abstract

Minute virus of canines (MVC) is a member of the genus Bocavirus in the family Parvoviridae . We have molecularly cloned and sequenced the 5′- and 3′-terminal palindromes of MVC. The MVC genome, 5,404 nucleotides (nt) in length, shared an identity of 52.6% and 52.1% with that of human bocavirus and bovine parvovirus, respectively. It had distinct palindromic hairpins of 183 nt and 198 nt at the left-end and right-end termini of the genome, respectively. The left-end terminus was also found in two alternative orientations (flip or flop). Both termini shared extensive similarities with those of bovine parvovirus. Four full-length molecular clones constructed with different orientations of the left-end terminus proved to be infectious in Walter Reed canine cell/3873D (WRD) canine cells. Both MVC infection and transfection of the infectious clone in WRD cells revealed an identical RNA transcription profile that was similar to that of bovine parvovirus. Mutagenesis of the infectious clone demonstrated that the middle open reading frame encodes the NP1 protein. This protein, unique to the genus Bocavirus , was essential for MVC DNA replication. Moreover, the phospholipase A2 motif in the VP1 unique region was also critical for MVC infection. Thus, our studies revealed important information about the genus Bocavirus that may eventually help us to clone the human bocavirus and study its pathogenesis.

Published

2009

22. Chemical synthesis of six novel 17beta-estradiol and estrone dimers and study of their formation catalyzed by human cytochrome P450 isoforms

Author

Aaron Yun Chen, Anthony J. Lee, Bao Ting Zhu, and Xiang-Rong Jiang

Subjects

Stereochemistry, Estrone, Dimer, Metabolite, In Vitro Techniques, Cofactor, Catalysis, chemistry.chemical_compound, Cytochrome P-450 Enzyme System, Drug Discovery, Cytochrome P-450 CYP3A, Humans, Unspecific monooxygenase, biology, Estradiol, Chemistry, Cytochrome P450, Estrogens, Recombinant Proteins, Isoenzymes, Biochemistry, biology.protein, Microsome, Microsomes, Liver, Molecular Medicine, Dimerization, hormones, hormone substitutes, and hormone antagonists

Abstract

Our earlier studies have shown that over 20 nonpolar 17beta-estradiol metabolite peaks were detected following incubations of radioactive 17beta-estradiol with human liver microsomes or recombinant human cytochrome P450 isoforms in the presence of NADPH as a cofactor. The structures of two representative nonpolar metabolites were identified earlier as dimers of 17beta-estradiol linked through a diaryl ether bond between the C-3 phenolic oxygen of one molecule and the C-2 or C-4 aromatic carbon of another. Six additional putative dimers between estrone and 17beta-estradiol with structures similar to the two identified ones were synthesized in this study. Using these newly synthesized estrogen dimers as reference standards, we demonstrated that incubations of human liver microsomes or various human cytochrome P450 isoforms with estrone or 17beta-estradiol alone or two estrogens in combination in the presence of NADPH as a cofactor resulted in the formation of all eight estrogen dimers in varying quantities.

Published

2007

23. Productive Parvovirus B19 Infection of Primary Human Erythroid Progenitor Cells at Hypoxia Is Regulated by STAT5A and MEK Signaling but not HIFα

Author

Steve Kleiboeker, Jianming Qiu, and Aaron Yun Chen

Subjects

CD36 Antigens, MAPK/ERK pathway, Cellular differentiation, Virus Replication, 0302 clinical medicine, Parvovirus B19, Human, STAT5 Transcription Factor, Biology (General), Hypoxia, Cells, Cultured, Erythroid Precursor Cells, 0303 health sciences, Cell Differentiation, MAP Kinase Kinase Kinases, 3. Good health, Cell biology, 030220 oncology & carcinogenesis, medicine.symptom, Research Article, DNA Replication, MAP Kinase Signaling System, QH301-705.5, Immunology, Erythema Infectiosum, Biology, Models, Biological, Microbiology, 03 medical and health sciences, Downregulation and upregulation, Virology, Genetics, medicine, Humans, Molecular Biology, Cell Proliferation, 030304 developmental biology, Tumor Suppressor Proteins, Host Cells, Bone marrow failure, RC581-607, Hypoxia (medical), Hypoxia-Inducible Factor 1, alpha Subunit, medicine.disease, Viral Replication, Viral replication, Parasitology, Immunologic diseases. Allergy, Viral Transmission and Infection, Ex vivo

Abstract

Human parvovirus B19 (B19V) causes a variety of human diseases. Disease outcomes of bone marrow failure in patients with high turnover of red blood cells and immunocompromised conditions, and fetal hydrops in pregnant women are resulted from the targeting and destruction of specifically erythroid progenitors of the human bone marrow by B19V. Although the ex vivo expanded erythroid progenitor cells recently used for studies of B19V infection are highly permissive, they produce progeny viruses inefficiently. In the current study, we aimed to identify the mechanism that underlies productive B19V infection of erythroid progenitor cells cultured in a physiologically relevant environment. Here, we demonstrate an effective reverse genetic system of B19V, and that B19V infection of ex vivo expanded erythroid progenitor cells at 1% O2 (hypoxia) produces progeny viruses continuously and efficiently at a level of approximately 10 times higher than that seen in the context of normoxia. With regard to mechanism, we show that hypoxia promotes replication of the B19V genome within the nucleus, and that this is independent of the canonical PHD/HIFα pathway, but dependent on STAT5A and MEK/ERK signaling. We further show that simultaneous upregulation of STAT5A signaling and down-regulation of MEK/ERK signaling boosts the level of B19V infection in erythroid progenitor cells under normoxia to that in cells under hypoxia. We conclude that B19V infection of ex vivo expanded erythroid progenitor cells at hypoxia closely mimics native infection of erythroid progenitors in human bone marrow, maintains erythroid progenitors at a stage conducive to efficient production of progeny viruses, and is regulated by the STAT5A and MEK/ERK pathways., Author Summary Human parvovirus B19 (B19V) is the etiological agent of fifth disease seen in children, aplastic crisis in sickle cell disease patients, chronic anemia in immunocompromised patients, and hydrops fetalis in pregnant women. After more than 35 years since its discovery, B19V was still unable to be propagated in vitro in a productive and sustainable manner, which directly delayed the progress of B19V pathogenesis study and consequently finding ways to treat patients infected with B19V. We cultured human erythroid progenitor cells at a hypoxic condition by mimicking the natural niches of human bone marrow. Our current work reveals, for the first time, a long-term B19V infection of ex vivo expanded erythroid progenitor cells at hypoxia. Thus, this finding will largely facilitate the study of the mechanisms underlying B19V infection and more importantly identification of approaches to treat B19V infection. Finally, the identification of the cellular signaling pathways in regulating B19V replication sheds light on the virus-host interaction and will nominate potential candidates for anti-virus drug targeting.

Published

2011

24. Molecular Characterization of Infectious Clones of the Minute Virus of Canines Reveals Unique Features of Bocaviruses.

Author

Yuning Sun, Aaron Yun Chen, Fang Cheng, Wuxiang Guan, Johnson, F. Brent, and Jianming Qiu

Subjects

*PLANT clones, *CUSPIDS, *PARVOVIRUSES, *PALINDROMES, *NUCLEOTIDES, *GENOMES, *PHOSPHOLIPASES

Abstract

Minute virus of canines (MVC) is a member of the genus Bocavirus in the family Parvoviridae. We have molecularly cloned and sequenced the 5'- and 3'-terminal palindromes of MVC. The MVC genome, 5,404 nucleotides (nt) in length, shared an identity of 52.6% and 52.1% with that of human bocavirus and bovine parvovirus, respectively. It had distinct palindromic hairpins of 183 nt and 198 nt at the left-end and right-end termini of the genome, respectively. The left-end terminus was also found in two alternative orientations (flip or flop). Both termini shared extensive similarities with those of bovine parvovirus. Four full-length molecular clones constructed with different orientations of the left-end terminus proved to be infectious in Walter Reed canine cell/3873D (WRD) canine cells. Both MVC infection and transfection of the infectious clone in WRD cells revealed an identical RNA transcription profile that was similar to that of bovine parvovirus. Mutagenesis of the infectious clone demonstrated that the middle open reading frame encodes the NP1 protein. This protein, unique to the genus Bocavirus, was essential for MVC DNA replication. Moreover, the phospholipase A2 motif in the VP1 unique region was also critical for MVC infection. Thus, our studies revealed important information about the genus Bocavirus that may eventually help us to clone the human bocavirus and study its pathogenesis. [ABSTRACT FROM AUTHOR]

Published

2009

25. Characterization of the gene expression profile of human bocavirus

Author

Aaron Yun Chen, Eric Delwart, Jianming Qiu, David J. Pintel, Yong Luo, Zhengwen Liu, Fang Cheng, and Sai Lou

Subjects

RNA Splicing, viruses, Biology, Article, Cell Line, Bocavirus, 03 medical and health sciences, Virology, Human bocavirus, Gene expression, Humans, RNA, Messenger, Gene, 030304 developmental biology, A549 cell, 0303 health sciences, 030306 microbiology, Gene Expression Profiling, Protein, HEK 293 cells, Transfection, Bovine parvovirus, biology.organism_classification, Molecular biology, 3. Good health, respiratory tract diseases, Gene expression profiling, RNA, Viral

Abstract

We have generated a quantitative transcription profile of human bocavirus type 1 (HBoV1) by transfecting a nearly full-length clone in human lung epithelial A549 cells as well as in a replication competent system in 293 cells. The overall transcription profile of HBoV1 is similar to that of two other members of genus Bocavirus, minute virus of canines and bovine parvovirus 1. In particular, a spliced NS1-transcript that was not recognized previously expressed the large non-structural protein NS1 at approximately 100kDa; and the NP1-encoding transcripts were expressed abundantly. In addition, the protein expression profile of human bocavirus type 2 (HBoV2) was examined in parallel by transfection of a nearly full-length clone in A549 cells, which is similar to that of HBoV1. Moreover, our results showed that, unlike human parvovirus B19 infection, expression of the HBoV1 proteins only does not induce cell cycle arrest and apoptosis of A549 cells.

26. The Capsid Proteins of Aleutian Mink Disease Virus Activate Caspases and Are Specifically Cleaved during Infection.

Author

Fang Cheng, Aaron Yun Chen, Best, Sonja M., Bloom, Marshall E., Pintel, David, and Jianming Qiu

Subjects

*MINK Aleutian disease, *VIRUS diseases, *PARVOVIRUSES, *GENE transfection, *ASPARTIC acid, *MIRIDAE

Abstract

Aleutian mink disease virus (AMDV) is currently the only known member of the genus Amdovirus in the family Parvoviridae. It is the etiological agent of Aleutian disease of mink. We have previously shown that a small protein with a molecular mass of approximately 26 kDa was present during AMDV infection and following transfection of capsid expression constructs (J. Qiu, F. Cheng, L. R. Burger, and D. Pintel, J. Virol. 80:654-662, 2006). In this study, we report that the capsid proteins were specifically cleaved at aspartic acid residue 420 (D420) during virus infection, resulting in the previously observed cleavage product. Mutation of a single amino acid residue at D420 abolished the specific cleavage. Expression of the capsid proteins alone in Crandell feline kidney (CrFK) cells reproduced the cleavage of the capsid proteins in virus infection. More importantly, capsid protein expression alone induced active caspases, of which caspase-10 was the most active. Active caspases, in turn, cleaved capsid proteins in vivo. Our results also showed that active caspase-7 specifically cleaved capsid proteins at D420 in vitro. These results suggest that viral capsid proteins alone induce caspase activation, resulting in cleavage of capsid proteins. We also provide evidence that AMDV mutants resistant to caspase-mediated capsid cleavage increased virus production approximately 3- to 5-fold in CrFK cells compared to that produced from the parent virus AMDV-G at 37°C but not at 31.8°C. Collectively, our results indicate that caspase activity plays multiple roles in AMDV infection and that cleavage of the capsid proteins might have a role in regulating persistent infection of AMDV. [ABSTRACT FROM AUTHOR]

Published

2010

27. Human Parvovirus B19 Utilizes Cellular DNA Replication Machinery for Viral DNA Replication.

Author

Wei Zou, Zekun Wang, Min Xiong, Aaron Yun Chen, Peng Xu, Ganaie, Safder S., Badawi, Yomna, Kleiboeker, Steve, Hiroshi Nishimune, Shui Qing Ye, and Jianming Qiu

Subjects

*PARVOVIRUSES, *PROGENITOR cells, *DNA replication, *DNA metabolism, *DNA polymerases, *PHOSPHORYLATION

Abstract

Human parvovirus B19 (B19V) infection of human erythroid progenitor cells (EPCs) induces a DNA damage response and cell cycle arrest at late S phase, which facilitates viral DNA replication. However, it is not clear exactly which cellular factors are employed by this single-stranded DNA virus. Here, we used microarrays to systematically analyze the dynamic transcriptome of EPCs infected with B19V. We found that DNA metabolism, DNA replication, DNA repair, DNA damage response, cell cycle, and cell cycle arrest pathways were significantly regulated after B19V infection. Confocal microscopy analyses revealed that most cellular DNA replication proteins were recruited to the centers of viral DNA replication, but not the DNA repair DNA polymerases. Our results suggest that DNA replication polymerase δ and polymerase α are responsible for B19V DNA replication by knocking down its expression in EPCs. We further showed that although RPA32 is essential for B19V DNA replication and the phosphorylated forms of RPA32 colocalized with the replicating viral genomes, RPA32 phosphorylation was not necessary for B19V DNA replication. Thus, this report provides evidence that B19V uses the cellular DNA replication machinery for viral DNA replication. IMPORTANCE Human parvovirus B19 (B19V) infection can cause transient aplastic crisis, persistent viremia, and pure red cell aplasia. In fetuses, B19V infection can result in nonimmune hydrops fetalis and fetal death. These clinical manifestations of B19V infection are a direct outcome of the death of human erythroid progenitors that host B19V replication. B19V infection induces a DNA damage response that is important for cell cycle arrest at late S phase. Here, we analyzed dynamic changes in cellular gene expression and found that DNA metabolic processes are tightly regulated during B19V infection. Although genes involved in cellular DNA replication were downregulated overall, the cellular DNA replication machinery was tightly associated with the replicating single-stranded DNA viral genome and played a critical role in viral DNA replication. In contrast, the DNA damage response-induced phosphorylated forms of RPA32 were dispensable for viral DNA replication. [ABSTRACT FROM AUTHOR]

Published

2018