Your search keyword '"Ruth Cruz-cosme"' showing total 4 results

1. Zika Virus Infection Downregulates Connexin 43, Disrupts the Cardiomyocyte Gap Junctions and Induces Heart Diseases in A129 Mice

Author

Shuxuan Li, Najealicka Armstrong, Huan Zhao, Ruth Cruz-cosme, Hongwei Yang, Chunlian Zhong, Wenkun Fu, Wei Wang, Decheng Yang, Ningshao Xia, Tong Cheng, and Qiyi Tang

Subjects

Heart Failure, Adolescent, Heart Diseases, Zika Virus Infection, Immunology, Infant, Newborn, Gap Junctions, Zika Virus, Microbiology, Rats, Mice, Disease Models, Animal, Connexin 43, Virology, Insect Science, Animals, Humans, Paralysis, Myocytes, Cardiac, Child

Abstract

Zika virus (ZIKV) is transmitted mostly via mosquito bites and no vaccine is available, so it may reemerge. We and others previously demonstrated that neonatal infection of ZIKV results in heart failure and can be fatal. Animal models implicated ZIKV involvement in viral heart diseases. It is unknown whether and how ZIKV causes heart failure in adults. Herein, we studied the effects of ZIKV infection on the heart function of adult A129 mice. First, we found that ZIKV productively infects the rat-, mouse-, or human-originated heart cell lines and caused ubiquitination-mediated degradation of and distortive effects on connexin 43 (Cx43) protein that is important for communications between cardiomyocytes. Second, ZIKV infection caused 100% death of the A129 mice with decreasing body weight, worsening health score, shrugging fur, and paralysis. The viral replication was detected in multiple organs. In searching for the viral effects on heart of the A129 mice, we found that ZIKV infection resulted in the increase of cardiac muscle enzymes, implicating a viral acute myocardial injury. ZIKV-caused heart injury was also demonstrated by electrocardiogram (ECG) showing widened and fragmented QRS waves, prolonged PR interval, and slower heart rate. The intercalated disc (ICD) between two cardiomyocytes was destroyed, as shown by the electronic microscopy, and the Cx43 distribution in the ICDs was less organized in the ZIKV-infected mice compared to that in the phosphate-buffered saline (PBS)-treated mice. Consistently, ZIKV productively infected the heart of A129 mice and decreased Cx43 protein. Therefore, we demonstrated that ZIKV infection caused heart failure, which might lead to fatal sequelae in ZIKV-infected A129 mice.

Published

2022

2. Expression of Human Cytomegalovirus IE1 Leads to Accumulation of Mono-SUMOylated PML That Is Protected from Degradation by Herpes Simplex Virus 1 ICP0

Author

Ruth Cruz-Cosme, Jin-Hyun Ahn, Wangheng Hou, Qiyi Tang, Min-Hua Luo, Fayuan Wen, and Inez Reeves

Subjects

0301 basic medicine, Human cytomegalovirus, Ubiquitin-Protein Ligases, viruses, Immunology, SUMO protein, Cytomegalovirus, Herpesvirus 1, Human, Promyelocytic Leukemia Protein, Biology, Virus Replication, medicine.disease_cause, Microbiology, Immediate-Early Proteins, Mice, 03 medical and health sciences, Multiplicity of infection, Virology, medicine, Animals, Humans, Cells, Cultured, Protein PML, Mutation, Sumoylation, virus diseases, Herpes Simplex, Transfection, biochemical phenomena, metabolism, and nutrition, medicine.disease, Virus-Cell Interactions, 030104 developmental biology, Herpes simplex virus, Cell culture, Insect Science, Cytomegalovirus Infections, Proteolysis

Abstract

To countermeasure the host cellular intrinsic defense, cytomegalovirus (CMV) and herpes simplex viruses (HSV) have evolved the ability to disperse nuclear domain 10 (ND10, aka PML body). However, mechanisms underlying their action on ND10 differ. HSV infection produces ICP0, which degrades the ND10-forming protein PML. Human CMV (HCMV) infection expresses IE1 that deSUMOylates PML to result in dispersion of ND10. It has been demonstrated that HSV ICP0 degraded only the SUMOylated PML, so we hypothesized that HCMV IE1 can protect PML from degradation by ICP0. HCMV IE1-expressing cell lines (U-251 MG-IE1 and HELF-IE1) were used for infection of HSV-1 or transfection of ICP0-expressing plasmid. Multilabeling by immunocytochemistry assay and protein examination by Western blot assay were performed to determine the resultant fate of PML caused by ICP0 in the presence or absence of HCMV IE1. Here, we report that deSUMOylation of human PML (hPML) by HCMV IE1 was incomplete, as mono-SUMOylated PML remained in the IE1-expressing cells, which is consistent with the report by E. M. Schilling, M. Scherer, N. Reuter, J. Schweininger, et al. (J Virol 91:e02049-16, 2017, https://doi.org/10.1128/JVI.02049-16). As expected, we found that IE1 protected PML from degradation by ICP0 or HSV-1 infection. An in vitro study found that IE1 with mutation of L174P failed to deSUMOylate PML and did not protect PML from degradation by ICP0; hence, we conclude that the deSUMOylation of PML is important for IE1 to protect PML from degradation by ICP0. In addition, we revealed that murine CMV failed to deSUMOylate and to protect the HSV-mediated degradation of hPML, and that HCMV failed to deSUMOylate and protect the HSV-mediated degradation of mouse PML. However, IE1-expressing cells did not enhance wild-type HSV-1 replication but significantly increased ICP0-defective HSV-1 replication at a low multiplicity of infection. Therefore, our results uncovered a host-virus functional interaction at the posttranslational level. IMPORTANCE Our finding that HCMV IE1 protected hPML from degradation by HSV ICP0 is important, because the PML body (aka ND10) is believed to be the first line of host intrinsic defense against herpesviral infection. How the infected viruses overcome the nuclear defensive structure (PML body) has not been fully understood. Herpesviral proteins, ICP0 of HSV and IE1 of CMV, have been identified to interact with PML. Here, we report that HCMV IE1 incompletely deSUMOylated PML, resulting in the mono-SUMOylated PML, which is consistent with the report of Schilling et al. (J Virol 91:e02049-16, 2017, https://doi.org/10.1128/JVI.02049-16). The mono-SUMOylated PML was subjected to degradation by HSV ICP0. However, it was protected by IE1 from degradation by ICP0 or HSV-1 infection. In contrast, IE1 with L174P mutation lost the function of deSUMOylating PML and failed to protect the degradation of the mono-SUMOylated PML. Whether the mono-SUMOylated PML has any defensive function against viral infection will be further investigated.

Published

2018

3. Two Polypyrimidine Tracts in Intron 4 of the Major Immediate Early Gene Are Critical for Gene Expression Switching from IE1 to IE2 and for Replication of Human Cytomegalovirus

Author

Dalia Luciano, Qiyi Tang, Min-Hua Luo, Luis Irizarry, Lilith Torres, Leslie L. Rivera, Wangheng Hou, Antonio L. Sala, Fernando Arroyo, Arturo Márquez, and Ruth Cruz-Cosme

Subjects

0301 basic medicine, Gene Expression Regulation, Viral, Small RNA, Transcription, Genetic, viruses, Immunology, Cytomegalovirus, Electrophoretic Mobility Shift Assay, Biology, Virus Replication, Microbiology, Immediate-Early Proteins, 03 medical and health sciences, Exon, Splicing factor, Virology, Gene expression, Humans, Gene, Regulation of gene expression, Genetics, Intron, virus diseases, Introns, Virus-Cell Interactions, 030104 developmental biology, Pyrimidines, Insect Science, RNA splicing, Trans-Activators, RNA Splicing Factors, Protein Binding

Abstract

The human cytomegalovirus (HCMV) major immediate early (MIE) gene is essential for viral replication. The most abundant products encoded by the MIE gene include IE1 and IE2. Genes of IE1 and IE2 share the MIE promoter (MIEP), the first 3 exons, and the first 2 introns. IE1 is expressed earlier than IE2 after CMV infection or MIE gene transfection. In this study, we identified 2 polypyrimidine (Py) tracts in intron 4 (between exons 4 and 5) that are responsible for transcriptional switching from IE1 to IE2. The first Py is important and the second one is essential for the splicing and expression of IE2. In searching for the mechanisms of MIE gene switching from IE1 to IE2, we found that the second Py was required for the IE2's fourth intron to bind to a splicing factor such as U2AF65, as determined by an RNA electrophoretic mobility shift assay and a chromatin immunoprecipitation (ChIP) assay, while the first Py enhanced the binding of U2AF65 with the intron. An HCMV BACmid with the second Py mutated failed to produce any virus, while the HCMV with the first Py mutated replicated with a defective phenotype. Furthermore, we designed a small RNA (scRNAPy) that is complementary to the intron RNA covering the two Pys. The scRNAPy interfered with the interaction of U2AF65 with the intron and repressed the IE2 expression. Therefore, our studies implied that IE2 gene splicing might be an anti-CMV target. IMPORTANCE CMV is a ubiquitous herpesvirus and a significant cause of disease and death in the immunocompromised and elderly. Insights into its gene regulation will provide clues in designing anti-CMV strategies. The MIE gene is one of the earliest genes of CMV and is essential for CMV replication. It is known that the MIE gene needs to be spliced to produce more than two proteins; however, how MIE gene splicing is regulated remains elusive. In the present studies, we identified two Pys in intron 4 and found that the first Py is important and the second is required for the splicing and expression of IE2. We further investigated the mechanisms of gene switching from IE1 to IE2 and found that the two Pys are responsible for U2AF65's binding with intron 4. Therefore, the Pys in intron 4 are the cis elements that determine the fate of IE2 splicing. Furthermore, we found that a small RNA that is complementary to intron 4 repressed IE2 expression. Hence, we provide the first piece of evidence for a unique mechanism of MIE gene regulation at the splicing level.

Published

2016

4. ORF7 of Varicella-Zoster Virus Is a Neurotropic Factor

Author

Ruth Cruz-Cosme, Ying Huang, Amos Markus, Ningshao Xia, Jinle Han, Xiangzhong Ye, Qiyi Tang, Benjamin Silver, Yimin Li, Kalpana Dulal, Lanling Wen, Hongliu Qian, Tong Cheng, Hua Zhu, Ronald S. Goldstein, Lianwei Yang, Yanzhen Lin, Che Liu, and Anca Selariu

Subjects

Herpesvirus 3, Human, Varicella vaccine, Virulence Factors, viruses, Neurotropism, Immunology, Biology, medicine.disease_cause, Herpes Zoster, Microbiology, Virus, Mice, Viral Proteins, Organ Culture Techniques, Immune system, Virology, medicine, Animals, Humans, Neurons, Chickenpox, integumentary system, Virulence, Varicella zoster virus, virus diseases, medicine.disease, Disease Models, Animal, Herpes simplex virus, Insect Science, Pathogenesis and Immunity, Gene Deletion, Shingles

Abstract

Varicella-zoster virus (VZV) is the causative agent of chickenpox and herpes zoster (shingles). After the primary infection, the virus remains latent in sensory ganglia and reactivates upon weakening of the cellular immune system due to various conditions, erupting from sensory neurons and infecting the corresponding skin tissue. The current varicella vaccine is highly attenuated in the skin and yet retains its neurovirulence and may reactivate and damage sensory neurons. The factors involved in neuronal invasion and establishment of latency are still elusive. Previously, we constructed a library of whole-gene deletion mutants carrying a bacterial artificial chromosome sequence and a luciferase marker in order to perform a comprehensive VZV genome functional analysis. Here, screening of dispensable gene deletion mutants in differentiated neuronal cells led to the identification of ORF7 as the first known, likely a main, VZV neurotropic factor. ORF7 is a virion component localized to the Golgi compartment in infected cells, whose deletion causes loss of polykaryon formation in epithelial cell culture. Interestingly, ORF7 deletion completely abolishes viral spread in human nervous tissue ex vivo and in an in vivo mouse model. This finding adds to our previous report that ORF7 is also a skin-tropic factor. The results of our investigation will not only lead to a better understanding of VZV neurotropism but could also contribute to the development of a neuroattenuated vaccine candidate against shingles or a vector for delivery of other antigens.

Published

2012