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1. Development of a live attenuated trivalent porcine rotavirus A vaccine against disease caused by recent strains most prevalent in South Korea

Author

Jun-Gyu Park, Mia Madel Alfajaro, Eun-Hyo Cho, Ji-Yun Kim, Mahmoud Soliman, Yeong-Bin Baek, Chul-Ho Park, Ju-Hwan Lee, Kyu-Yeol Son, Kyoung-Oh Cho, and Mun-Il Kang

Subjects
Veterinary medicine, SF600-1100
Abstract

Abstract Porcine rotaviruses cause severe economic losses in the Korean swine industry due to G- and P-genotype mismatches between the predominant field and vaccine strains. Here, we developed a live attenuated trivalent porcine group A rotavirus vaccine using 80 cell culture passages of the representative Korean predominant strains G8P[7] 174-1, G9P[23] PRG942, and G5P[7] K71. Vaccination with the trivalent vaccine or its individual components induced no diarrhea during the first 2 weeks post-vaccination, i.e., the vaccines were attenuated. Challenge of trivalent-vaccinated or component-vaccinated piglets with homologous virulent strain(s) did not induce diarrhea for 2 weeks post-challenge. Immunization with the trivalent vaccine or its individual components also alleviated the histopathological lesions in the small intestines caused by challenge with the corresponding original virulent strain(s). Fecal secretory IgAs specific for each of vaccine strains were detected starting at 14 days post-vaccination (dpv), and IgA levels gradually increased up to 28 dpv. Oral immunization with the trivalent vaccine or its individual components induced high levels of serum virus-neutralizing antibody by 7 dpv. No diarrhea was observed in any experimental piglets during five consecutive passages of each vaccine strain. Our data indicated that the live attenuated trivalent vaccine was safe and effective at protecting piglets from diarrhea induced by challenge exposure of homologous virulent strains. This trivalent vaccine will potentially contribute toward controlling porcine rotavirus disease in South Korea and other countries where rotavirus infections with similar G and P genotypes are problematic.

Published
2019
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2. Porcine sapovirus Cowden strain enters LLC-PK cells via clathrin- and cholesterol-dependent endocytosis with the requirement of dynamin II

Author

Mahmoud Soliman, Deok-Song Kim, Chonsaeng Kim, Ja-Young Seo, Ji-Yun Kim, Jun-Gyu Park, Mia Madel Alfajaro, Yeong-Bin Baek, Eun-Hyo Cho, Sang-Ik Park, Mun-Il Kang, Kyeong-Ok Chang, Ian Goodfellow, and Kyoung-Oh Cho

Subjects
Veterinary medicine, SF600-1100
Abstract

Abstract Caliciviruses in the genus Sapovirus are a significant cause of viral gastroenteritis in humans and animals. However, the mechanism of their entry into cells is not well characterized. Here, we determined the entry mechanism of porcine sapovirus (PSaV) strain Cowden into permissive LLC-PK cells. The inhibition of clathrin-mediated endocytosis using chlorpromazine, siRNAs, and a dominant negative (DN) mutant blocked entry and infection of PSaV Cowden strain, confirming a role for clathrin-mediated internalization. Entry and infection were also inhibited by the cholesterol-sequestering drug methyl-β-cyclodextrin and was restored by the addition of soluble cholesterol, indicating that cholesterol also contributes to entry and infection of this strain. Furthermore, the inhibition of dynamin GTPase activity by dynasore, siRNA depletion of dynamin II, or overexpression of a DN mutant of dynamin II reduced the entry and infection, suggesting that dynamin mediates the fission and detachment of clathrin- and cholesterol-pits for entry of this strain. In contrast, the inhibition of caveolae-mediated endocytosis using nystatin, siRNAs, or a DN mutant had no inhibitory effect on entry and infection of this strain. It was further determined that cell entry of PSaV Cowden strain required actin rearrangements for vesicle internalization, endosomal trafficking from early to late endosomes through microtubules, and late endosomal acidification for uncoating. We conclude that PSaV strain Cowden is internalized into LLC-PK cells by clathrin- and cholesterol-mediated endocytosis that requires dynamin II and actin rearrangement, and that the uncoating occurs in the acidified late endosomes after trafficking from the early endosomes through microtubules.

Published
2018
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3. Activation of PI3K, Akt, and ERK during early rotavirus infection leads to V-ATPase-dependent endosomal acidification required for uncoating.

Author

Mahmoud Soliman, Ja-Young Seo, Deok-Song Kim, Ji-Yun Kim, Jun-Gyu Park, Mia Madel Alfajaro, Yeong-Bin Baek, Eun-Hyo Cho, Joseph Kwon, Jong-Soon Choi, Mun-Il Kang, Sang-Ik Park, and Kyoung-Oh Cho

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

The cellular PI3K/Akt and/or MEK/ERK signaling pathways mediate the entry process or endosomal acidification during infection of many viruses. However, their roles in the early infection events of group A rotaviruses (RVAs) have remained elusive. Here, we show that late-penetration (L-P) human DS-1 and bovine NCDV RVA strains stimulate these signaling pathways very early in the infection. Inhibition of both signaling pathways significantly reduced production of viral progeny due to blockage of virus particles in the late endosome, indicating that neither of the two signaling pathways is involved in virus trafficking. However, immunoprecipitation assays using antibodies specific for pPI3K, pAkt, pERK and the subunit E of the V-ATPase co-immunoprecipitated the V-ATPase in complex with pPI3K, pAkt, and pERK. Moreover, Duolink proximity ligation assay revealed direct association of the subunit E of the V-ATPase with the molecules pPI3K, pAkt, and pERK, indicating that both signaling pathways are involved in V-ATPase-dependent endosomal acidification. Acidic replenishment of the medium restored uncoating of the RVA strains in cells pretreated with inhibitors specific for both signaling pathways, confirming the above results. Isolated components of the outer capsid proteins, expressed as VP4-VP8* and VP4-VP5* domains, and VP7, activated the PI3K/Akt and MEK/ERK pathways. Furthermore, psoralen-UV-inactivated RVA and CsCl-purified RVA triple-layered particles triggered activation of the PI3K/Akt and MEK/ERK pathways, confirming the above results. Our data demonstrate that multistep binding of outer capsid proteins of L-P RVA strains with cell surface receptors phosphorylates PI3K, Akt, and ERK, which in turn directly interact with the subunit E of the V-ATPase to acidify the late endosome for uncoating of RVAs. This study provides a better understanding of the RVA-host interaction during viral uncoating, which is of importance for the development of strategies aiming at controlling or preventing RVA infections.

Published
2018
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4. Feline calicivirus- and murine norovirus-induced COX-2/PGE2 signaling pathway has proviral effects.

Author

Mia Madel Alfajaro, Eun-Hyo Cho, Jun-Gyu Park, Ji-Yun Kim, Mahmoud Soliman, Yeong-Bin Baek, Mun-Il Kang, Sang-Ik Park, and Kyoung-Oh Cho

Subjects
Medicine, Science
Abstract

Cyclooxygenases (COXs)/prostaglandin E2 (PGE2) signaling pathways are known to modulate a variety of homeostatic processes and are involved in various pathophysiological conditions. COXs/PGE2 signaling pathways have also been demonstrated to have proviral or antiviral effects, which appeared different even in the same virus family. A porcine sapovirus Cowden strain, a member of genus Sapovirus within the Caliciviridae family, induces strong COX-2/PGE2 but transient COX-1/PGE2 signaling to enhance virus replication. However, whether infections of other viruses in the different genera activate COXs/PGE2 signaling, and thus affect the replication of viruses, remains unknown. In the present study, infections of cells with the feline calicivirus (FCV) F9 strain in the genus Vesivirus and murine norovirus (MNV) CW-1 strain in the genus Norovirus only activated the COX-2/PGE2 signaling in a time-dependent manner. Treatment with pharmacological inhibitors or transfection of small interfering RNAs (siRNAs) against COX-2 enzyme significantly reduced the production of PGE2 as well as FCV and MNV replications. The inhibitory effects of these pharmacological inhibitors against COX-2 enzyme on the replication of both viruses were restored by the addition of PGE2. Silencing of COX-1 via siRNAs and inhibition of COX-1 via an inhibitor also decrease the production of PGE2 and replication of both viruses, which can be attributed to the inhibition COX-1/PGE2 signaling pathway. These data indicate that the COX-2/PGE2 signaling pathway has proviral effects for the replication of FCV and MNV, and pharmacological inhibitors against these enzymes serve as potential therapeutic candidates for treating FCV and MNV infections.

Published
2018
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5. Development of a live attenuated trivalent porcine rotavirus A vaccine against disease caused by recent strains most prevalent in South Korea

Author

Ju-Hwan Lee, Mun-Il Kang, Yeong-Bin Baek, Eun-Hyo Cho, Chul-Ho Park, Ji-Yun Kim, Mahmoud Soliman, Kyoung-Oh Cho, Kyu-Yeol Son, Jun-Gyu Park, and Mia Madel Alfajaro

Subjects
0301 basic medicine, Rotavirus, 040301 veterinary sciences, Swine, [SDV]Life Sciences [q-bio], Virulence, Vaccines, Attenuated, Group A, Rotavirus Infections, 0403 veterinary science, 03 medical and health sciences, Republic of Korea, medicine, Animals, Feces, Swine Diseases, lcsh:Veterinary medicine, General Veterinary, biology, Viral Vaccines, 04 agricultural and veterinary sciences, Virology, Rotavirus vaccine, 3. Good health, Vaccination, Diarrhea, 030104 developmental biology, Immunization, biology.protein, lcsh:SF600-1100, medicine.symptom, Antibody, Research Article
Abstract

Porcine rotaviruses cause severe economic losses in the Korean swine industry due to G- and P-genotype mismatches between the predominant field and vaccine strains. Here, we developed a live attenuated trivalent porcine group A rotavirus vaccine using 80 cell culture passages of the representative Korean predominant strains G8P[7] 174-1, G9P[23] PRG942, and G5P[7] K71. Vaccination with the trivalent vaccine or its individual components induced no diarrhea during the first 2 weeks post-vaccination, i.e., the vaccines were attenuated. Challenge of trivalent-vaccinated or component-vaccinated piglets with homologous virulent strain(s) did not induce diarrhea for 2 weeks post-challenge. Immunization with the trivalent vaccine or its individual components also alleviated the histopathological lesions in the small intestines caused by challenge with the corresponding original virulent strain(s). Fecal secretory IgAs specific for each of vaccine strains were detected starting at 14 days post-vaccination (dpv), and IgA levels gradually increased up to 28 dpv. Oral immunization with the trivalent vaccine or its individual components induced high levels of serum virus-neutralizing antibody by 7 dpv. No diarrhea was observed in any experimental piglets during five consecutive passages of each vaccine strain. Our data indicated that the live attenuated trivalent vaccine was safe and effective at protecting piglets from diarrhea induced by challenge exposure of homologous virulent strains. This trivalent vaccine will potentially contribute toward controlling porcine rotavirus disease in South Korea and other countries where rotavirus infections with similar G and P genotypes are problematic. Electronic supplementary material The online version of this article (10.1186/s13567-018-0619-6) contains supplementary material, which is available to authorized users.

Published
2019

6. Dual Recognition of Sialic Acid and αGal Epitopes by the VP8* Domains of the Bovine Rotavirus G6P[5] WC3 and of Its Mono-reassortant G4P[5] RotaTeq Vaccine Strains

Author

Mahmoud Soliman, Jacques Le Pendu, Eun-Hyo Cho, Ji-Yun Kim, Sang-Ik Park, Soo Hyun Kim, Kyoung-Oh Cho, Yeong-Bin Baek, Laure Barbé, Geun-Joong Kim, Jun-Gyu Park, Mun-Il Kang, and Mia Madel Alfajaro

Subjects
Rotavirus, Immunology, Virus Attachment, Viral Nonstructural Proteins, medicine.disease_cause, Sialidase, Vaccines, Attenuated, Microbiology, Epitope, Rotavirus Infections, chemistry.chemical_compound, Epitopes, Antigen, Virology, medicine, Animals, Humans, Amino Acid Sequence, Pathogen, Infectivity, biology, ligands, Rotavirus Vaccines, αGal, N-Acetylneuraminic Acid, Sialic acid, Virus-Cell Interactions, chemistry, sialic acid, Insect Science, alpha-Galactosidase, biology.protein, Blood Group Antigens, Receptors, Virus, Capsid Proteins, Cattle, Neuraminidase
Abstract

Group A rotaviruses initiate infection through the binding of the VP8* domain of the VP4 protein to sialic acids (SAs) or histo-blood group antigens (HBGAs). Although the bovine G6P[5] WC3 strain is an important animal pathogen and is used as the backbone in the bovine-human reassortant RotaTeq vaccine, the receptor(s) for their P[5] VP8* domain has remained elusive. Using a variety of approaches, we demonstrated that the WC3 and bovine-human mono-reassortant G4P[5] vaccine strains recognize both α2,6-linked SA and αGal HBGA as ligands. Neither ligand is expressed on human small intestinal epithelial cells, explaining the absence of natural human infection by P[5]-bearing strains. However, we observed that the P[5]-bearing WC3 and G4P[5] RotaTeq vaccine strains could still infect human intestinal epithelial cells. Thus, the four P[5] RotaTeq vaccine strains potentially binding to additional alternative receptors may be efficient and effective in providing protection against severe rotavirus disease in human., Group A rotaviruses, an important cause of severe diarrhea in children and young animals, initiate infection via interactions of the VP8* domain of the VP4 spike protein with cell surface sialic acids (SAs) or histo-blood group antigens (HBGAs). Although the bovine G6P[5] WC3 strain is an important animal pathogen and is also used in the bovine-human reassortant RotaTeq vaccine, the receptor(s) for the VP8* domain of WC3 and its reassortant strains have not yet been identified. In the present study, HBGA- and saliva-binding assays showed that both G6P[5] WC3 and mono-reassortant G4P[5] strains recognized the αGal HBGA. The infectivity of both P[5]-bearing strains was significantly reduced in αGal-free MA-104 cells by pretreatment with a broadly specific neuraminidase or by coincubation with the α2,6-linked SA-specific Sambucus nigra lectin, but not by the α2,3-linked specific sialidase or by Maackia amurensis lectin. Free NeuAc and the αGal trisaccharide also prevented the infectivity of both strains. This indicated that both P[5]-bearing strains utilize α2,6-linked SA as a ligand on MA104 cells. However, the two strains replicated in differentiated bovine small intestinal enteroids and in their human counterparts that lack α2,6-linked SA or αGal HBGA, suggesting that additional or alternative receptors such as integrins, hsp70, and tight-junction proteins bound directly to the VP5* domain can be used by the P[5]-bearing strains to initiate the infection of human cells. In addition, these data also suggested that P[5]-bearing strains have potential for cross-species transmission. IMPORTANCE Group A rotaviruses initiate infection through the binding of the VP8* domain of the VP4 protein to sialic acids (SAs) or histo-blood group antigens (HBGAs). Although the bovine G6P[5] WC3 strain is an important animal pathogen and is used as the backbone in the bovine-human reassortant RotaTeq vaccine, the receptor(s) for their P[5] VP8* domain has remained elusive. Using a variety of approaches, we demonstrated that the WC3 and bovine-human mono-reassortant G4P[5] vaccine strains recognize both α2,6-linked SA and αGal HBGA as ligands. Neither ligand is expressed on human small intestinal epithelial cells, explaining the absence of natural human infection by P[5]-bearing strains. However, we observed that the P[5]-bearing WC3 and G4P[5] RotaTeq vaccine strains could still infect human intestinal epithelial cells. Thus, the four P[5] RotaTeq vaccine strains potentially binding to additional alternative receptors may be efficient and effective in providing protection against severe rotavirus disease in human.

Published
2019

8. Porcine sapovirus Cowden strain enters LLC-PK cells via clathrin- and cholesterol-dependent endocytosis with the requirement of dynamin II

Author

Chonsaeng Kim, Deok-Song Kim, Mahmoud Soliman, Ja-Young Seo, Mun-Il Kang, Jun-Gyu Park, Yeong-Bin Baek, Kyoung-Oh Cho, Ji-Yun Kim, Ian Goodfellow, Eun-Hyo Cho, Sang-Ik Park, Mia Madel Alfajaro, and Kyeong-Ok Chang

Subjects
0301 basic medicine, Small interfering RNA, Swine, Endosome, media_common.quotation_subject, [SDV]Life Sciences [q-bio], 030106 microbiology, Endocytosis, Clathrin, Dynamin II, Sapovirus, Caliciviruses, 03 medical and health sciences, Dynasore, Animals, Humans, Cowden Strain, Internalization, Late Endosomal Acidification, Actin, Caliciviridae Infections, media_common, Dynamin, Swine Diseases, lcsh:Veterinary medicine, General Veterinary, biology, Gastroenteritis, Cell biology, Cholesterol, 030104 developmental biology, Porcine Sapovirus (PSaV), biology.protein, LLC-PK1 Cells, lcsh:SF600-1100, HeLa Cells
Abstract

International audience; AbstractCaliciviruses in the genus Sapovirus are a significant cause of viral gastroenteritis in humans and animals. However, the mechanism of their entry into cells is not well characterized. Here, we determined the entry mechanism of porcine sapovirus (PSaV) strain Cowden into permissive LLC-PK cells. The inhibition of clathrin-mediated endocytosis using chlorpromazine, siRNAs, and a dominant negative (DN) mutant blocked entry and infection of PSaV Cowden strain, confirming a role for clathrin-mediated internalization. Entry and infection were also inhibited by the cholesterol-sequestering drug methyl-β-cyclodextrin and was restored by the addition of soluble cholesterol, indicating that cholesterol also contributes to entry and infection of this strain. Furthermore, the inhibition of dynamin GTPase activity by dynasore, siRNA depletion of dynamin II, or overexpression of a DN mutant of dynamin II reduced the entry and infection, suggesting that dynamin mediates the fission and detachment of clathrin- and cholesterol-pits for entry of this strain. In contrast, the inhibition of caveolae-mediated endocytosis using nystatin, siRNAs, or a DN mutant had no inhibitory effect on entry and infection of this strain. It was further determined that cell entry of PSaV Cowden strain required actin rearrangements for vesicle internalization, endosomal trafficking from early to late endosomes through microtubules, and late endosomal acidification for uncoating. We conclude that PSaV strain Cowden is internalized into LLC-PK cells by clathrin- and cholesterol-mediated endocytosis that requires dynamin II and actin rearrangement, and that the uncoating occurs in the acidified late endosomes after trafficking from the early endosomes through microtubules.

Published
2018

9. Whole genomic characterization of Korean porcine G8P[7] reassortant rotaviruses

Author

Mia Madel Alfajaro, Deok-Song Kim, Mun-Il Kang, Jong-Soon Choi, Jun-Gyu Park, Ji-Yun Kim, Ja-Young Seo, Joseph Sang-Il Kwon, Mahmoud Soliman, Eun-Hyo Cho, Yeong-Bin Baek, Sang-Ik Park, Kyoung-Oh Cho, Nam-Il Woo, and Jelle Matthijnssens

Subjects
Rotavirus, 0301 basic medicine, Swine, Sequence analysis, viruses, Sequence Homology, Genome, Viral, Biology, medicine.disease_cause, Genome, Rotavirus Infections, 03 medical and health sciences, Viral genetics, Phylogenetics, Virology, Genotype, medicine, Animals, Cluster Analysis, Gene, Phylogeny, Swine Diseases, Genetics, Korea, Strain (biology), virus diseases, Sequence Analysis, DNA, General Medicine, biochemical phenomena, metabolism, and nutrition, 030104 developmental biology, RNA, Viral, Reassortant Viruses
Abstract

This study analyzed eleven genomic segments of three Korean porcine G8P[7] group A rotavirus (RVA) strains. Phylogenetically, these strains contained two bovine-like and nine porcine-like genomic segments. Eight genes (VP1, VP2, VP6 and NSP1-NSP5) of strains 156-1 and 42-1 and seven genes (VP1, VP2, VP6 and NSP2-NSP5) of strain C-1 clustered closely with porcine and porcine-like animal strains and distantly from typical human Wa-like strains. The VP3-M2 genotype of these strains clustered closely with bovine-like strains, but distantly with typical human DS-1-like strains. These data indicate that multiple reassortments involving porcine and bovine RVA strains in Korea must have occurred. ispartof: Archives of Virology vol:161 issue:10 pages:2835-2841 ispartof: location:Austria status: published

Published
2016

10. The Effects of Long-term Exercise on the Expression of SPARC and OSM in Colon Cancer-induced Mice

Author

Tae-Won Jeon, June-Hong Kim, and Eun-Hyo Cho

Subjects
medicine.medical_specialty, business.industry, Colorectal cancer, Significant difference, Exercise group, Public Health, Environmental and Occupational Health, Physical Therapy, Sports Therapy and Rehabilitation, Treadmill exercise, medicine.disease, digestive system diseases, Colon polyps, Andrology, Elisa kit, Physiology (medical), Cancer management, Physical therapy, Medicine, business
Abstract

PURPOSE: The purpose of this study was to investigate the impacts of long-term treadmill exercise on the expression of SPARC and OSM in muscle, blood and colon polyp of colon cancer-induced mice. METHODS: Thirty mice were randomly divided into two groups: Exercise group (EX, n=15), Control group (CON, n=15). Mice of EX, at 6-week of old, performed exercise at moderate intensity for 30 minutes, 5 days per week, during 12 weeks. At 17-week of old, all mice were injected AOM and DSS to induce colon cancer. Then EX kept doing exercise for another 12 weeks. The expression of OSM and SPARC in muscle, blood, colon polyp was analyzed using the ELISA kit. RESULTS: The OSM expression of EX was significantly higher than CON in muscle (p

Published
2016

11. Early Porcine Sapovirus Infection Disrupts Tight Junctions and Uses Occludin as a Coreceptor

Author

Jun-Gyu Park, Deok-Song Kim, Eun-Hyo Cho, Mun-Il Kang, Ji-Yun Kim, Mahmoud Soliman, Sang-Ik Park, Yeong-Bin Baek, Mia Madel Alfajaro, Chul-Ho Park, and Kyoung-Oh Cho

Subjects
Small interfering RNA, Endosome, Swine, tight junction, Immunology, CHO Cells, Endosomes, Biology, Occludin, Microbiology, Sapovirus, occludin, Tight Junctions, Cricetulus, Antigen, Virology, Animals, Receptor, cellular coreceptor, Tight junction, Chinese hamster ovary cell, Epithelial Cells, Cell biology, Gastroenteritis, Virus-Cell Interactions, Virus Diseases, Paracellular transport, Insect Science, LLC-PK1 Cells
Abstract

Sapoviruses (SaVs) cause severe acute gastroenteritis in humans and animals. Although they replicate in intestinal epithelial cells, which are tightly sealed by apical-junctional complexes, such as tight junctions (TJs), the mechanisms by which SaVs hijack TJs and their proteins for successful entry and infection remain largely unknown. Here, we demonstrate that porcine SaVs (PSaVs) induce early dissociation of TJs, allowing them to bind to the TJ protein occludin as a functional coreceptor. PSaVs then travel in a complex with occludin into late endosomes through Rab5- and Rab7-dependent trafficking. Claudin-1, another TJ protein, does not directly interact with PSaV but facilitates the entry of PSaV into cells as an entry factor. This work contributes to our understanding of the entry of SaV and other caliciviruses into cells and may aid in the development of efficient and affordable drugs to treat SaV infections., The genus Sapovirus belongs to the family Caliciviridae, and its members are common causative agents of severe acute gastroenteritis in both humans and animals. Some caliciviruses are known to use either terminal sialic acids or histo-blood group antigens as attachment factors and/or cell surface proteins, such as CD300lf, CD300ld, and junctional adhesion molecule 1 of tight junctions (TJs), as receptors. However, the roles of TJs and their proteins in sapovirus entry have not been examined. In this study, we found that porcine sapovirus (PSaV) significantly decreased transepithelial electrical resistance and increased paracellular permeability early in infection of LLC-PK cells, suggesting that PSaV dissociates TJs of cells. This led to the interaction between PSaV particles and occludin, which traveled in a complex into late endosomes via Rab5- and Rab7-dependent trafficking. Inhibition of occludin using small interfering RNA (siRNA), a specific antibody, or a dominant-negative mutant significantly blocked the entry of PSaV. Transient expression of occludin in nonpermissive Chinese hamster ovary (CHO) cells conferred susceptibility to PSaV, but only for a limited time. Although claudin-1, another TJ protein, neither directly interacted nor was internalized with PSaV particles, it facilitated PSaV entry and replication in the LLC-PK cells. We conclude that PSaV particles enter LLC-PK cells by binding to occludin as a coreceptor in PSaV-dissociated TJs. PSaV and occludin then form a complex that moves to late endosomes via Rab5- and Rab7-dependent trafficking. In addition, claudin-1 in the TJs opened by PSaV infection facilitates PSaV entry and infection as an entry factor. IMPORTANCE Sapoviruses (SaVs) cause severe acute gastroenteritis in humans and animals. Although they replicate in intestinal epithelial cells, which are tightly sealed by apical-junctional complexes, such as tight junctions (TJs), the mechanisms by which SaVs hijack TJs and their proteins for successful entry and infection remain largely unknown. Here, we demonstrate that porcine SaVs (PSaVs) induce early dissociation of TJs, allowing them to bind to the TJ protein occludin as a functional coreceptor. PSaVs then travel in a complex with occludin into late endosomes through Rab5- and Rab7-dependent trafficking. Claudin-1, another TJ protein, does not directly interact with PSaV but facilitates the entry of PSaV into cells as an entry factor. This work contributes to our understanding of the entry of SaV and other caliciviruses into cells and may aid in the development of efficient and affordable drugs to treat SaV infections.

Published
2018
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12. Phosphatidylinositol 3-Kinase/Akt and MEK/ERK Signaling Pathways Facilitate Sapovirus Trafficking and Late Endosomal Acidification for Viral Uncoating in LLC-PK Cells

Author

Eun-Hyo Cho, Chul-Ho Park, Mia Madel Alfajaro, Ji-Yun Kim, Sang-Ik Park, Mun-Il Kang, Mahmoud Soliman, Deok-Song Kim, Kyoung-Oh Cho, Jun-Gyu Park, and Yeong-Bin Baek

Subjects
0301 basic medicine, MAPK/ERK pathway, Endosome, MAP Kinase Signaling System, Swine, Immunology, Endosomes, Biology, Kidney, Microbiology, Sapovirus, Cell Line, 03 medical and health sciences, chemistry.chemical_compound, endosomal acidification, Virology, Virus Uncoating, Sf9 Cells, Animals, Phosphatidylinositol, Protein kinase B, PI3K/AKT/mTOR pathway, Caliciviridae Infections, PI3K/Akt, Kinase, Epithelial Cells, Virus Internalization, Cell biology, Virus-Cell Interactions, 030104 developmental biology, chemistry, Insect Science, Phosphorylation, viral entry, Signal transduction, Phosphatidylinositol 3-Kinase, Proto-Oncogene Proteins c-akt, MEK/ERK
Abstract

Sapoviruses cause acute gastroenteritis in both humans and animals. However, the host signaling pathway(s) that facilitates host cell entry by sapoviruses remains largely unknown. Here we demonstrate that porcine sapovirus (PSaV) activates both PI3K/Akt and MEK/ERK cascades at an early stage of infection. Removal of cell surface receptors decreased PSaV-induced early activation of both cascades. Moreover, blocking of PI3K/Akt and MEK/ERK cascades entrapped PSaV particles in early endosomes and prevented their trafficking to the late endosomes. PSaV-induced early activation of PI3K and ERK molecules further mediated V-ATPase-dependent late endosomal acidification for PSaV uncoating. This work unravels a new mechanism by which receptor-mediated early activation of both cascades may facilitate PSaV trafficking from early to late endosomes and late endosomal acidification for PSaV uncoating, which in turn can be a new target for treatment of sapovirus infection., Sapovirus, an important cause of acute gastroenteritis in humans and animals, travels from the early to the late endosomes and requires late endosomal acidification for viral uncoating. However, the signaling pathways responsible for these viral entry processes remain unknown. Here we demonstrate the receptor-mediated early activation of phosphatidylinositol 3-kinase (PI3K)/Akt and mitogen-activated protein extracellular signal-regulated kinase/extracellular signal-regulated kinase (MEK/ERK) signaling pathways involved in sapovirus entry processes. Both signaling pathways were activated during the early stage of porcine sapovirus (PSaV) infection. However, depletion of the cell surface carbohydrate receptors by pretreatment with sodium periodate or neuraminidase reduced the PSaV-induced early activation of these signaling pathways, indicating that PSaV binding to the cell surface carbohydrate receptors triggered these cascades. Addition of bile acid, known to be essential for PSaV escape from late endosomes, was also found to exert a stiffening effect to stimulate both pathways. Inhibition of these signaling pathways by use of inhibitors specific for PI3K or MEK or small interfering RNAs (siRNAs) against PI3K or MEK resulted in entrapment of PSaV particles in early endosomes and prevented their trafficking to late endosomes. Moreover, phosphorylated PI3K and ERK coimmunoprecipitated subunit E of the V-ATPase proton pump that is important for endosomal acidification. Based on our data, we conclude that receptor binding of PSaV activates both PI3K/Akt and MEK/ERK signaling pathways, which in turn promote PSaV trafficking from early to late endosomes and acidification of late endosomes for PSaV uncoating. These signaling cascades may provide a target for potent therapeutics against infections by PSaV and other caliciviruses. IMPORTANCE Sapoviruses cause acute gastroenteritis in both humans and animals. However, the host signaling pathway(s) that facilitates host cell entry by sapoviruses remains largely unknown. Here we demonstrate that porcine sapovirus (PSaV) activates both PI3K/Akt and MEK/ERK cascades at an early stage of infection. Removal of cell surface receptors decreased PSaV-induced early activation of both cascades. Moreover, blocking of PI3K/Akt and MEK/ERK cascades entrapped PSaV particles in early endosomes and prevented their trafficking to the late endosomes. PSaV-induced early activation of PI3K and ERK molecules further mediated V-ATPase-dependent late endosomal acidification for PSaV uncoating. This work unravels a new mechanism by which receptor-mediated early activation of both cascades may facilitate PSaV trafficking from early to late endosomes and late endosomal acidification for PSaV uncoating, which in turn can be a new target for treatment of sapovirus infection.

Published
2018

13. Rotavirus-Induced Early Activation of the RhoA/ROCK/MLC Signaling Pathway Mediates the Disruption of Tight Junctions in Polarized MDCK Cells

Author

Mahmoud Soliman, Jun-Gyu Park, Mun-Il Kang, Kyoung-Oh Cho, Ji-Yun Kim, Mia Madel Alfajaro, Yeong-Bin Baek, Eun-Hyo Cho, Sang-Ik Park, and Deok-Song Kim

Subjects
Rotavirus, 0301 basic medicine, Cytoplasm, Cell Membrane Permeability, RHOA, Myosin light-chain kinase, lcsh:Medicine, Cell Line, Madin Darby Canine Kidney Cells, Tight Junctions, 03 medical and health sciences, Dogs, Animals, Humans, lcsh:Science, Receptor, Myosin-Light-Chain Kinase, Protein kinase C, rho-Associated Kinases, Multidisciplinary, biology, Tight junction, Chemistry, lcsh:R, Membrane Proteins, Cell biology, 030104 developmental biology, Paracellular transport, biology.protein, lcsh:Q, Cattle, Signal transduction, rhoA GTP-Binding Protein, Signal Transduction
Abstract

Intestinal epithelial tight junctions (TJ) are a major barrier restricting the entry of various harmful factors including pathogens; however, they also represent an important entry portal for pathogens. Although the rotavirus-induced early disruption of TJ integrity and targeting of TJ proteins as coreceptors are well-defined, the precise molecular mechanisms involved remain unknown. In the present study, infection of polarized MDCK cells with the species A rotavirus (RVA) strains human DS-1 and bovine NCDV induced a redistribution of TJ proteins into the cytoplasm, a reversible decrease in transepithelial resistance, and an increase in paracellular permeability. RhoA/ROCK/MLC signaling was identified as activated at an early stage of infection, while inhibition of this pathway prevented the rotavirus-induced early disruption of TJ integrity and alteration of TJ protein distribution. Activation of pMYPT, PKC, or MLCK, which are known to participate in TJ dissociation, was not observed in MDCK cells infected with either rotavirus strain. Our data demonstrated that binding of RVA virions or cogent VP8* proteins to cellular receptors activates RhoA/ROCK/MLC signaling, which alters TJ protein distribution and disrupts TJ integrity via contraction of the perijunctional actomyosin ring, facilitating virion access to coreceptors and entry into cells.

Published
2018

14. Feline calicivirus- and murine norovirus-induced COX-2/PGE2 signaling pathway has proviral effects

Author

Mun-Il Kang, Ji-Yun Kim, Mia Madel Alfajaro, Mahmoud Soliman, Yeong-Bin Baek, Kyoung-Oh Cho, Jun-Gyu Park, Eun-Hyo Cho, and Sang-Ik Park

Subjects
0301 basic medicine, RNA viruses, Small interfering RNA, Viral Diseases, Pulmonology, ved/biology.organism_classification_rank.species, lcsh:Medicine, Virus Replication, Pathology and Laboratory Medicine, Biochemistry, Mice, Proviruses, Medicine and Health Sciences, Small interfering RNAs, lcsh:Science, Feline calicivirus, Analgesics, Viral Genomics, Multidisciplinary, Mammalian Genomics, Drugs, Genomics, Nucleic acids, Infectious Diseases, Medical Microbiology, Viral Pathogens, Viruses, lipids (amino acids, peptides, and proteins), Signal transduction, Pathogens, Signal Transduction, Research Article, 030106 microbiology, Microbial Genomics, Biology, Microbiology, Virus, Dinoprostone, Sapovirus, COX-2 inhibitors, Caliciviruses, 03 medical and health sciences, Virology, Genetics, Gene silencing, Animals, Non-coding RNA, Microbial Pathogens, Pharmacology, Biology and life sciences, ved/biology, lcsh:R, Norovirus, Organisms, Membrane Proteins, Calicivirus Infection, biology.organism_classification, Caliciviridae, Viral Replication, Pain management, Gene regulation, 030104 developmental biology, RAW 264.7 Cells, Viral replication, Cyclooxygenase 2, Animal Genomics, Respiratory Infections, Cats, Cyclooxygenase 1, RNA, lcsh:Q, Gene expression, Murine norovirus, Calicivirus, Feline
Abstract

Cyclooxygenases (COXs)/prostaglandin E2 (PGE2) signaling pathways are known to modulate a variety of homeostatic processes and are involved in various pathophysiological conditions. COXs/PGE2 signaling pathways have also been demonstrated to have proviral or antiviral effects, which appeared different even in the same virus family. A porcine sapovirus Cowden strain, a member of genus Sapovirus within the Caliciviridae family, induces strong COX-2/PGE2 but transient COX-1/PGE2 signaling to enhance virus replication. However, whether infections of other viruses in the different genera activate COXs/PGE2 signaling, and thus affect the replication of viruses, remains unknown. In the present study, infections of cells with the feline calicivirus (FCV) F9 strain in the genus Vesivirus and murine norovirus (MNV) CW-1 strain in the genus Norovirus only activated the COX-2/PGE2 signaling in a time-dependent manner. Treatment with pharmacological inhibitors or transfection of small interfering RNAs (siRNAs) against COX-2 enzyme significantly reduced the production of PGE2 as well as FCV and MNV replications. The inhibitory effects of these pharmacological inhibitors against COX-2 enzyme on the replication of both viruses were restored by the addition of PGE2. Silencing of COX-1 via siRNAs and inhibition of COX-1 via an inhibitor also decrease the production of PGE2 and replication of both viruses, which can be attributed to the inhibition COX-1/PGE2 signaling pathway. These data indicate that the COX-2/PGE2 signaling pathway has proviral effects for the replication of FCV and MNV, and pharmacological inhibitors against these enzymes serve as potential therapeutic candidates for treating FCV and MNV infections.

Published
2018

15. MOESM1 of Porcine sapovirus Cowden strain enters LLC-PK cells via clathrin- and cholesterol-dependent endocytosis with the requirement of dynamin II

Author

Soliman, Mahmoud, Deok-Song Kim, Chonsaeng Kim, Seo, Ja-Young, Kim, Ji-Yun, Jun-Gyu Park, Alfajaro, Mia, Yeong-Bin Baek, Eun-Hyo Cho, Sang-Ik Park, Mun-Il Kang, Kyeong-Ok Chang, Goodfellow, Ian, and Kyoung-Oh Cho

Abstract

Additional file 1. Sequences of siRNAs against target molecules and scrambled siRNA used in this study.

Published
2018
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16. Activation of PI3K, Akt, and ERK during early rotavirus infection leads to V-ATPase-dependent endosomal acidification required for uncoating

Author

Mun-Il Kang, Kyoung-Oh Cho, Jun-Gyu Park, Jong-Soon Choi, Eun-Hyo Cho, Joseph Sang-Il Kwon, Sang-Ik Park, Mia Madel Alfajaro, Deok-Song Kim, Mahmoud Soliman, Ja-Young Seo, Yeong-Bin Baek, and Ji-Yun Kim

Subjects
0301 basic medicine, MAPK/ERK pathway, Rotavirus, Viral Diseases, Cell signaling, Physiology, viruses, Signal transduction, ERK signaling cascade, Biochemistry, Viral Packaging, Signaling Molecules, Phosphatidylinositol 3-Kinases, Immune Physiology, Virus Uncoating, Medicine and Health Sciences, Sf9 Cells, Small interfering RNAs, Extracellular Signal-Regulated MAP Kinases, lcsh:QH301-705.5, Late endosome, Cells, Cultured, Immune System Proteins, Chemistry, Signaling cascades, Haplorhini, Hydrogen-Ion Concentration, Cell biology, Precipitation Techniques, Nucleic acids, Infectious Diseases, Phosphorylation, Research Article, lcsh:Immunologic diseases. Allergy, Vacuolar Proton-Translocating ATPases, Signal Inhibition, Immunology, Endosomes, Research and Analysis Methods, Microbiology, Antibodies, Rotavirus Infections, 03 medical and health sciences, Virology, Genetics, Immunoprecipitation, Animals, Humans, Non-coding RNA, Molecular Biology, Protein kinase B, PI3K/AKT/mTOR pathway, Rotavirus Infection, Biology and life sciences, Proteins, Viral Replication, Gene regulation, Enzyme Activation, 030104 developmental biology, lcsh:Biology (General), RNA, Parasitology, Capsid Proteins, Cattle, Gene expression, Caco-2 Cells, lcsh:RC581-607, Acids, Proto-Oncogene Proteins c-akt
Abstract

The cellular PI3K/Akt and/or MEK/ERK signaling pathways mediate the entry process or endosomal acidification during infection of many viruses. However, their roles in the early infection events of group A rotaviruses (RVAs) have remained elusive. Here, we show that late-penetration (L-P) human DS-1 and bovine NCDV RVA strains stimulate these signaling pathways very early in the infection. Inhibition of both signaling pathways significantly reduced production of viral progeny due to blockage of virus particles in the late endosome, indicating that neither of the two signaling pathways is involved in virus trafficking. However, immunoprecipitation assays using antibodies specific for pPI3K, pAkt, pERK and the subunit E of the V-ATPase co-immunoprecipitated the V-ATPase in complex with pPI3K, pAkt, and pERK. Moreover, Duolink proximity ligation assay revealed direct association of the subunit E of the V-ATPase with the molecules pPI3K, pAkt, and pERK, indicating that both signaling pathways are involved in V-ATPase-dependent endosomal acidification. Acidic replenishment of the medium restored uncoating of the RVA strains in cells pretreated with inhibitors specific for both signaling pathways, confirming the above results. Isolated components of the outer capsid proteins, expressed as VP4-VP8* and VP4-VP5* domains, and VP7, activated the PI3K/Akt and MEK/ERK pathways. Furthermore, psoralen-UV-inactivated RVA and CsCl-purified RVA triple-layered particles triggered activation of the PI3K/Akt and MEK/ERK pathways, confirming the above results. Our data demonstrate that multistep binding of outer capsid proteins of L-P RVA strains with cell surface receptors phosphorylates PI3K, Akt, and ERK, which in turn directly interact with the subunit E of the V-ATPase to acidify the late endosome for uncoating of RVAs. This study provides a better understanding of the RVA-host interaction during viral uncoating, which is of importance for the development of strategies aiming at controlling or preventing RVA infections., Author summary Viral particles must transport their genome into the cytoplasm or the nucleus of host cells to initiate successful infection. Knowledge of how viruses may pirate host cell signaling cascades or molecules to promote their own replication can facilitate the development of antiviral drugs. Group A rotavirus (RVA) is a major etiological agent of acute gastroenteritis in young children and the young of various mammals. RVA enters cells by a complex multistep process. However, the cellular signaling cascades or molecules that facilitate these processes are incompletely understood. Here, we demonstrate that infection with late-penetration RVA strains results in phosphorylation of PI3K, Akt, and ERK signaling molecules at an early stage of infection, a process mediated by the multistep binding of RVAs outer capsid proteins. Specific inhibitors for PI3K/Akt and MEK/ERK signaling pathways trap the viral particles in late endosome, and acidic replenishment restores and releases them. Moreover, the RVA-induced phosphorylated PI3K, Akt, and ERK directly interact with the subunit E of the V-ATPase proton pump, required for endosomal acidification and RVA uncoating. Understanding how RVA-induced early activation of cellular signaling molecules mediates the V-ATPase-dependent endosomal acidification required for uncoating of viral particles opens up opportunities for targeted interventions against rotavirus entry.

Published
2018

17. Bovine Nebovirus Interacts with a Wide Spectrum of Histo-Blood Group Antigens

Author

Ja-Young Seo, Yeong-Bin Baek, Kyoung-Oh Cho, Mia Madel Alfajaro, Eun-Hyo Cho, Deok-Song Kim, Jacques Le Pendu, Sang-Ik Park, Mahmoud Soliman, Mun-Il Kang, Jun-Gyu Park, Ji-Yun Kim, Laboratory of Veterinary Pathology [Gwangju, Republic of Korea], Chonnam National University [Gwangju]-College of Veterinary Medicine [Gwangju, Republic of Korea], Host-Pathogen Interactions in the Regulation of Immune Responses (CRCINA-ÉQUIPE 5), Centre de Recherche en Cancérologie et Immunologie Nantes-Angers (CRCINA), Institut National de la Santé et de la Recherche Médicale (INSERM)-Université de Nantes - UFR de Médecine et des Techniques Médicales (UFR MEDECINE), Université de Nantes (UN)-Université de Nantes (UN)-Centre hospitalier universitaire de Nantes (CHU Nantes)-Centre National de la Recherche Scientifique (CNRS)-Université d'Angers (UA)-Institut National de la Santé et de la Recherche Médicale (INSERM)-Université de Nantes - UFR de Médecine et des Techniques Médicales (UFR MEDECINE), and Université de Nantes (UN)-Université de Nantes (UN)-Centre hospitalier universitaire de Nantes (CHU Nantes)-Centre National de la Recherche Scientifique (CNRS)-Université d'Angers (UA)

Subjects
0301 basic medicine, Saliva, Swine, Fucose, Epitope, Madin Darby Canine Kidney Cells, chemistry.chemical_compound, Epitopes, fucose, Intestinal Mucosa, Receptor, Caliciviridae Infections, biology, 3. Good health, Gastroenteritis, Virus-Cell Interactions, bovine calicivirus, HBGAs, Blood Group Antigens, Receptors, Virus, Caliciviridae, nebovirus, Protein Binding, 030106 microbiology, Immunology, Virus Attachment, [SDV.CAN]Life Sciences [q-bio]/Cancer, CHO Cells, Microbiology, 03 medical and health sciences, Cricetulus, Dogs, Antigen, binding spectrum, Virology, Cell Line, Tumor, attachment factor, Animals, Humans, Tropism, Binding selectivity, biology.organism_classification, 030104 developmental biology, chemistry, Insect Science, Cats, Sialic Acids, Caco-2 Cells, HeLa Cells
Abstract

Some viruses within the Caliciviridae family initiate their replication cycle by attachment to cell surface carbohydrate moieties, histo-blood group antigens (HBGAs), and/or terminal sialic acids (SAs). Although bovine nebovirus (BNeV), one of the enteric caliciviruses, is an important causative agent of acute gastroenteritis in cattle, its attachment factors and possibly other cellular receptors remain unknown. Using a comprehensive series of protein-ligand biochemical assays, we sought to determine whether BNeV recognizes cell surface HBGAs and/or SAs as attachment factors. It was found that BNeV virus-like particles (VLPs) bound to A type/H type 2/Le y HBGAs expressed in the bovine digestive tract and are related to HBGAs expressed in humans and other host species, suggesting a wide spectrum of HBGA recognition by BNeV. BNeV VLPs also bound to a large variety of different bovine and human saliva samples of all ABH and Lewis types, supporting previously obtained results and suggesting a zoonotic potential of BNeV transmission. Removal of α1,2-linked fucose and α1,3/4-linked fucose epitopes of target HBGAs by confirmation-specific enzymes reduced the binding of BNeV VLPs to synthetic HBGAs, bovine and human saliva, cultured cell lines, and bovine small intestine mucosa, further supporting a wide HBGA binding spectrum of BNeV through recognition of α1,2-linked fucose and α1,3/4-linked fucose epitopes of targeted HBGAs. However, removal of terminal α2,3- and α2,6-linked SAs by their specific enzyme had no inhibitory effects on binding of BNeV VLPs, indicating that BNeV does not use terminal SAs as attachment factors. Further details of the binding specificity of BNeV remain to be explored. IMPORTANCE Enteric caliciviruses such as noroviruses, sapoviruses, and recoviruses are the most important etiological agents of severe acute gastroenteritis in humans and many other mammalian host species. They initiate infection by attachment to cell surface carbohydrate moieties, HBGAs, and/or terminal SAs. However, the attachment factor(s) for BNeV, a recently classified enteric calicivirus genus/type species, remains unexplored. Here, we demonstrate that BNeV VLPs have a wide spectrum of binding to synthetic HBGAs, bovine and human saliva samples, and bovine duodenal sections. We further discovered that α1,2-linked fucose and α1,3/4-linked fucose epitopes are essential for binding of BNeV VLPs. However, BNeV VLPs do not bind to terminal SAs on cell carbohydrates. Continued investigation regarding the proteinaceous receptor(s) will be necessary for better understanding of the tropism, pathogenesis, and host range of this important viral genus.

Published
2017

18. Glycan-specificity of four neuraminidase-sensitive animal rotavirus strains

Author

Mun-Il Kang, Mia Madel Alfajaro, Hyung-Jun Kwon, Kyoung-Oh Cho, Ja-Young Seo, Su-Jin Park, Ji-Yun Kim, Yeong-Bin Baek, Jun-Gyu Park, Deok-Song Kim, Mahmoud Soliman, and Eun-Hyo Cho

Subjects
0301 basic medicine, Rotavirus, Glycan, 030106 microbiology, Cell, Neuraminidase, Virus Attachment, Biology, Sialidase, medicine.disease_cause, Microbiology, Cell Line, 03 medical and health sciences, Glycolipid, medicine, Animals, Humans, chemistry.chemical_classification, Infectivity, Membrane Glycoproteins, General Veterinary, General Medicine, Fibroblasts, Molecular biology, 030104 developmental biology, medicine.anatomical_structure, chemistry, biology.protein, Glycoprotein
Abstract

Group A rotaviruses (RVAs) are divided into neuraminidase (NA)-sensitive and NA-insensitive strains depending upon their binding affinity to the VP8* domain in the terminal sialic acids (SAs) of cell surface carbohydrates. Although NA-sensitive strains are known to use terminal SAs as an attachment factor, the exact nature of this attachment factor is largely unknown. Here we show that the specific linkage of SA-containing glycan to glycoprotein or glycolipid is an attachment factor used by NA-sensitive porcine G9P[7] PRG9121 and G9P[23] PRG942, bovine G6P[1] NCDV, and canine G3P[3] strains. Infectivity of porcine G9P[7] and G9P[23] strains was markedly blocked by α2,3-linkage and α2,6-linkage inhibitors, indicating that these strains bind to both α2,3- and α2,6-linked SAs. However, the infectivity of bovine G6P[1] and canine G3P[3] strains was significantly reduced by α2,6-linkage inhibitor but not by α2,3-linkage blockers, demonstrating a predilection of these strains for α2,6-linked SAs. The infectivity of four NA-sensitive strains was equally reduced by inhibitors of lipid membrane and N-linked glycoprotein but not by an inhibitor of O-linked glycoprotein, indicating that these strains utilize both glycolipid and N-linked glycoprotein. Our study demonstrates that four NA-sensitive animal strains could have a strain-dependent binding preference toward α2,6-linked SAs (P[1] NCDV and P[3] CU-1 strains) or both α2,3- and α2,6-linked SAs (P[7] PRG9121 and P[23] PRG942 strains) to the glycolipid and N-linked glycoprotein.

Published
2017

21. Occurrence and molecular characterization of Sapelovirus A in diarrhea and non-diarrhea feces of different age group pigs in one Korean pig farm

Author

Mahmoud Soliman, Mia Madel Alfajaro, Ja-Young Seo, Yeong-Bin Baek, Eun-Hyo Cho, Sang-Ik Park, Ji-Yun Kim, Jun-Gyu Park, Jong-Soon Choi, Mun-Il Kang, Joseph Sang-Il Kwon, Kyoung-Oh Cho, Kyu-Yeol Son, Deok-Song Kim, and Geon-Yong Bak

Subjects
0301 basic medicine, Diarrhea, Male, Veterinary medicine, food.ingredient, Swine, Picornaviridae, Biology, Disease cluster, occurrence, 03 medical and health sciences, Feces, Animal science, food, Age groups, Sapelovirus A, Virology, Genetic variation, Republic of Korea, medicine, Animals, Picornaviridae Infections, Swine Diseases, Genetic diversity, General Veterinary, Age Factors, Genetic Variation, genetic diversity, Note, porcine, 030104 developmental biology, Female, medicine.symptom, Sapelovirus
Abstract

To determine the occurrence and genetic diversity of Sapelovirus A (SV-A) in diarrhea and non-diarrhea feces of Korean pigs, 110 specimens from different age groups of pigs in the same farm were analyzed by RT-nested PCR. SV-As were detected in 60% of both diarrhea and non-diarrhea specimens regardless of age groups with primer pairs for 2C region, in which all diarrhea samples were co-infected by other enteric pathogens. Phylogenetical analysis of partial VP1 region showed that our strains and several other Korean strains belonged to cluster I, distinct from some strains reported in Korea and other countries. These data indicate that genetically distinct SV-As are frequently detected in Korean pigs irrespective of diarrhea and age.

Published
2016

22. Early Porcine Sapovirus Infection Disrupts Tight Junctions and Uses Occludin as a Coreceptor.

Author

Alfajaro, Mia Madel, Eun-Hyo Cho, Deok-Song Kim, Ji-Yun Kim, Jun-Gyu Park, Soliman, Mahmoud, Yeong-Bin Baek, Chul-Ho Park, Mun-Il Kang, Sang-Ik Park, and Kyoung-Oh Cho

Subjects
*CALICIVIRUSES, *VIRUS diseases, *OCCLUDINS, *TIGHT junctions, *SIALIC acids
Abstract

The genus Sapovirus belongs to the family Caliciviridae, and its members are common causative agents of severe acute gastroenteritis in both humans and animals. Some caliciviruses are known to use either terminal sialic acids or histoblood group antigens as attachment factors and/or cell surface proteins, such as CD300lf, CD300ld, and junctional adhesion molecule 1 of tight junctions (TJs), as receptors. However, the roles of TJs and their proteins in sapovirus entry have not been examined. In this study, we found that porcine sapovirus (PSaV) significantly decreased transepithelial electrical resistance and increased paracellular permeability early in infection of LLC-PK cells, suggesting that PSaV dissociates TJs of cells. This led to the interaction between PSaV particles and occludin, which traveled in a complex into late endosomes via Rab5- and Rab7-dependent trafficking. Inhibition of occludin using small interfering RNA (siRNA), a specific antibody, or a dominantnegative mutant significantly blocked the entry of PSaV. Transient expression of occludin in nonpermissive Chinese hamster ovary (CHO) cells conferred susceptibility to PSaV, but only for a limited time. Although claudin-1, another TJ protein, neither directly interacted nor was internalized with PSaV particles, it facilitated PSaV entry and replication in the LLC-PK cells. We conclude that PSaV particles enter LLC-PK cells by binding to occludin as a coreceptor in PSaV-dissociated TJs. PSaV and occludin then form a complex that moves to late endosomes via Rab5- and Rab7- dependent trafficking. In addition, claudin-1 in the TJs opened by PSaV infection facilitates PSaV entry and infection as an entry factor. [ABSTRACT FROM AUTHOR]

Published
2019
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23. Bovine Nebovirus Interacts with a Wide Spectrum of Histo-Blood Group Antigens.

Author

Eun-Hyo Cho, Soliman, Mahmoud, Alfajaro, Mia Madel, Ji-Yun Kim, Ja-Young Seo, Jun-Gyu Park, Deok-Song Kim, Yeong-Bin Baek, Mun-Il Kang, Sang-Ik Park, Pendu, Jacques Le, and Kyoung-Oh Choa

Subjects
*CALICIVIRUSES, *CARBOHYDRATES, *BLOOD group antigens, *FUCOSE, *BOVINE anatomy
Abstract

Some viruses within the Caliciviridae family initiate their replication cycle by attachment to cell surface carbohydrate moieties, histo-blood group antigens (HBGAs), and/or terminal sialic acids (SAs). Although bovine nebovirus (BNeV), one of the enteric caliciviruses, is an important causative agent of acute gastroenteritis in cattle, its attachment factors and possibly other cellular receptors remain unknown. Using a comprehensive series of protein-ligand biochemical assays, we sought to determine whether BNeV recognizes cell surface HBGAs and/or SAs as attachment factors. It was found that BNeV virus-like particles (VLPs) bound to A type/H type 2/Ley HBGAs expressed in the bovine digestive tract and are related to HBGAs expressed in humans and other host species, suggesting a wide spectrum of HBGA recognition by BNeV. BNeV VLPs also bound to a large variety of different bovine and human saliva samples of all ABH and Lewis types, supporting previously obtained results and suggesting a zoonotic potential of BNeV transmission. Removal of α1,2-linked fucose and α1,3/4-linked fucose epitopes of target HBGAs by confirmation-specific enzymes reduced the binding of BNeV VLPs to synthetic HBGAs, bovine and human saliva, cultured cell lines and bovine small intestine mucosa, further supporting a wide HBGA binding spectrum of BNeV through recognition of α1,2- linked fucose and α1,3/4-linked fucose epitopes of targeted HBGAs. However, removal of terminal α2,3- and α2,6-linked SAs by their specific enzyme had no inhibitory effects on binding of BNeV VLPs, indicating that BNeV does not use terminal SAs as attachment factors. Further details of the binding specificity of BNeV remain to be explored. IMPORTANCE Enteric caliciviruses such as noroviruses, sapoviruses, and recoviruses are the most important etiological agents of severe acute gastroenteritis in humans and many other mammalian host species. They initiate infection by attachment to cell surface carbohydrate moieties, HBGAs, and/or terminal SAs. However, the attachment factor(s) for BNeV, a recently classified enteric calicivirus genus/type species, remains unexplored. Here, we demonstrate that BNeV VLPs have a wide spectrum of binding to synthetic HBGAs, bovine and human saliva samples and bovine duodenal sections. We further discovered that α1,2-linked fucose and α1,3/4-linked fucose epitopes are essential for binding of BNeV VLPs. However, BNeV VLPs do not bind to terminal SAs on cell carbohydrates. Continued investigation regarding the proteinaceous receptor(s) will be necessary for better understanding of the tropism, pathogenesis, and host range of this important viral genus. [ABSTRACT FROM AUTHOR]

Published
2018
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25. Occurrence and molecular characterization of Sapelovirus A in diarrhea and non-diarrhea feces of different age group pigs in one Korean pig farm.

Author

Geon-Yong BAK, Mun-Il KANG, Kyu-Yeol SON, Jun-Gyu PARK, Deok-Song KIM, Ja-Young SEO, Ji-Yun KIM, Mia Madel ALFAJARO, SOLIMAN, Mahmoud, Yeong-Bin BAEK, Eun-Hyo CHO, KWON, Joseph, Jong-Soon CHOI, Sang-Ik PARK, and Kyoung-Oh CHO

Subjects
SWINE, SWINE diseases, DIARRHEA, SWINE farms, ANIMALS, AGE, ANIMAL health
Abstract

To determine the occurrence and genetic diversity of Sapelovirus A (SV-A) in diarrhea and non-diarrhea feces of Korean pigs, 110 specimens from different age groups of pigs in the same farm were analyzed by RT-nested PCR. SV-As were detected in 60% of both diarrhea and non-diarrhea specimens regardless of age groups with primer pairs for 2C region, in which all diarrhea samples were co-infected by other enteric pathogens. Phylogenetical analysis of partial VP1 region showed that our strains and several other Korean strains belonged to cluster I, distinct from some strains reported in Korea and other countries. These data indicate that genetically distinct SV-As are frequently detected in Korean pigs irrespective of diarrhea and age. [ABSTRACT FROM AUTHOR]

Published
2016
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26. Dual Recognition of Sialic Acid and αGal Epitopes by the VP8 Domains of the Bovine Rotavirus G6P[5] WC3 and of Its Mono-reassortant G4P[5] RotaTeq Vaccine Strains.

Author

Alfajaro, Mia Madel, Ji-Yun Kim, Barbé, Laure, Eun-Hyo Cho, Jun-Gyu Park, Soliman, Mahmoud, Yeong-Bin Baek, Mun-Il Kang, Soo Hyun Kim, Geun-Joong Kim, Sang-Ik Park, Le Pendu, Jacques, and Kyoung-Oh Cho

Subjects
*SIALIC acids, *NEURAMINIDASE, *ROTAVIRUSES, *EPITOPES, *TIGHT junctions, *INTEGRINS, *VACCINES, *PROTEIN binding
Abstract

Group A rotaviruses, an important cause of severe diarrhea in children and young animals, initiate infection via interactions of the VP8* domain of the VP4 spike protein with cell surface sialic acids (SAs) or histo-blood group antigens (HBGAs). Although the bovine G6P[5] WC3 strain is an important animal pathogen and is also used in the bovine-human reassortant RotaTeq vaccine, the receptor(s) for the VP8* domain of WC3 and its reassortant strains have not yet been identified. In the present study, HBGA- and saliva-binding assays showed that both G6P[5] WC3 and mono-reassortant G4P[5] strains recognized the αGal HBGA. The infectivity of both P[5]-bearing strains was significantly reduced in αGal-free MA-104 cells by pretreatment with a broadly specific neuraminidase or by coincubation with the α2,6- linked SA-specific Sambucus nigra lectin, but not by the α2,3-linked specific sialidase or by Maackia amurensis lectin. Free NeuAc and the αGal trisaccharide also prevented the infectivity of both strains. This indicated that both P[5]-bearing strains utilize α2,6-linked SA as a ligand on MA104 cells. However, the two strains replicated in differentiated bovine small intestinal enteroids and in their human counterparts that lack α2,6-linked SA or αGal HBGA, suggesting that additional or alternative receptors such as integrins, hsp70, and tight-junction proteins bound directly to the VP5* domain can be used by the P[5]-bearing strains to initiate the infection of human cells. In addition, these data also suggested that P[5]-bearing strains have potential for cross-species transmission. [ABSTRACT FROM AUTHOR]

Published
2019
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27. Activation of COX-2/PGE2 Promotes Sapovirus Replication via the Inhibition of Nitric Oxide Production.

Author

Alfajaro, Mia Madel, Jong-Soon Choi, Deok-Song Kim, Ja-Young Seo, Ji-Yun Kim, Jun-Gyu Park, Soliman, Mahmoud, Yeong-Bin Baek, Eun-Hyo Cho, Kwon, Joseph, Hyung-Jun Kwon, Su-Jin Park, Woo Song Lee, Mun-Il Kang, Hosmillo, Myra, Goodfellow, Ian, and Kyoung-Oh Cho

Subjects
*CYCLOOXYGENASE 2, *ENZYME activation, *CALICIVIRUSES, *VIRAL replication, *NITRIC oxide
Abstract

Enteric caliciviruses in the genera Norovirus and Sapovirus are important pathogens that cause severe acute gastroenteritis in both humans and animals. Cyclooxygenases (COXs) and their final product, prostaglandin E2 (PGE2), are known to play important roles in the modulation of both the host response to infection and the replicative cycles of several viruses. However, the precise mechanism(s) by which the COX/PGE2 pathway regulates sapovirus replication remains largely unknown. In this study, infection with porcine sapovirus (PSaV) strain Cowden, the only cultivable virus within the genus Sapovirus, markedly increased COX-2 mRNA and protein levels at 24 and 36 h postinfection (hpi), with only a transient increase in COX-1 levels seen at 24 hpi. The treatment of cells with pharmacological inhibitors, such as nonsteroidal anti-inflammatory drugs or small interfering RNAs (siRNAs) against COX-1 and COX-2, significantly reduced PGE2 production, as well as PSaV replication. Expression of the viral proteins VPg and ProPol was associated with activation of the COX/PGE2 pathway. We observed that pharmacological inhibition of COX-2 dramatically increased NO production, causing a reduction in PSaV replication that could be restored by inhibition of nitric oxide synthase via the inhibitor N-nitro-L-methylarginine ester. This study identified a pivotal role for the COX/PGE2 pathway in the regulation of NO production during the sapovirus life cycle, providing new insights into the life cycle of this poorly characterized family of viruses. Our findings also reveal potential new targets for treatment of sapovirus infection. [ABSTRACT FROM AUTHOR]

Published
2017
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28. Porcine Sapelovirus Uses α2,3-Linked Sialic Acid on GD1a Ganglioside as a Receptor.

Author

Deok-Song Kim, Kyu-Yeol Son, Kyung-Min Koo, Ji-Yun Kim, Alfajaro, Mia Madel, Jun-Gyu Park, Hosmillo, Myra, Soliman, Mahmoud, Yeong-Bin Baek, Eun-Hyo Cho, Ju-Hwan Lee, Mun-Il Kang, Ian Goodfellow, and Kyoung-Oh Cho

Subjects
*SIALIC acids, *GANGLIOSIDES, *PICORNAVIRUSES, *DIARRHEA, *PNEUMONIA, *NEURAMINIDASE, *OLIGOSACCHARIDES, *THERAPEUTICS
Abstract

The receptor(s) for porcine sapelovirus (PSV), which causes diarrhea, pneumonia, polioencephalomyelitis, and reproductive disorders in pigs, remains largely unknown. Given the precedent for other picornaviruses which use terminal sialic acids (SAs) as receptors, we examined the role of SAs in PSV binding and infection. Using a variety of approaches, including treating cells with a carbohydrate-destroying chemical (NaIO4), mono- or oligosaccharides (N-acetylneuraminic acid, galactose, and 6'-sialyllactose), linkage-specific sialidases (neuraminidase and sialidase S), lectins (Maakia amurensis lectin and Sambucus nigra lectin), proteases (trypsin and chymotrypsin), and glucosylceramide synthase inhibitors (DL-threo-1-phenyl-2-decanoylamino-3-morpholino-1-propanol and phospholipase C), we demonstrated that PSV could recognize α2,3-linked SA on glycolipids as a receptor. On the other hand, PSVs had no binding affinity for synthetic histo-blood group antigens (HBGAs), suggesting that PSVs could not use HBGAs as receptors. Depletion of cell surface glycolipids followed by reconstitution studies indicated that GD1a ganglioside, but not other gangliosides, could restore PSV binding and infection, further confirming α2,3-linked SA on GD1a as a PSV receptor. Our results could provide significant information on the understanding of the life cycle of sapelovirus and other picornaviruses. For the broader community in the area of pathogens and pathogenesis, these findings and insights could contribute to the development of affordable, useful, and efficient drugs for anti-sapelovirus therapy. [ABSTRACT FROM AUTHOR]

Published
2016
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