Your search keyword '"Viral receptor"' showing total 559 results

1. Receptor usage of Syncytin-1: ASCT2, but not ASCT1, is a functional receptor and effector of cell fusion in the human placenta.

Author

Štafl, Kryštof, Trávníček, Martin, Janovská, Anna, Kučerová, Dana, Pecnová, Ľubomíra, Zhiqi Yang, Stepanec, Vladimír, Jech, Lukáš, Salker, Madhuri S., Hejnar, Jiří, and Trejbalová, Kateřina

Abstract

Syncytin-1, a human fusogenic protein of retroviral origin, is crucial for placental syncytiotrophoblast formation. To mediate cell-to-cell fusion, Syncytin-1 requires specific interaction with its cognate receptor. Two trimeric transmembrane proteins, Alanine, Serine, Cysteine Transporters 1 and 2 (ASCT1 and ASCT2), were suggested and widely accepted as Syncytin-1 cellular receptors. To quantitatively assess the individual contributions of human ASCT1 and ASCT2 to the fusogenic activity of Syncytin-1, we developed a model system where the ASCT1 and ASCT2 double knockout was rescued by ectopic expression of either ASCT1 or ASCT2. We demonstrated that ASCT2 was required for Syncytin-1 binding, cellular entry, and cell-to-cell fusion, while ASCT1 was not involved in this receptor interaction. We experimentally validated the ASCT1-ASCT2 heterotrimers as a possible explanation for the previous misidentification of ASCT1 as a receptor for Syncytin-1. This redefinition of receptor specificity is important for proper understanding of Syncytin-1 function in normal and pathological pregnancy. [ABSTRACT FROM AUTHOR]

Published

2024

2. Both middle and large envelope proteins can mediate neutralization of hepatitis B virus infectivity by anti-preS2 antibodies: escape by naturally occurring preS2 deletions.

Author

Jing Zhang, Qianru Wang, Wenqing Yuan, Jing Li, Quan Yuan, Jiming Zhang, Ningshao Xia, Yongxiang Wang, Jisu Li, and Shuping Tong

Subjects

*HEPARAN sulfate proteoglycans, *VIRUS cloning, *HEPATITIS B virus, *HEPATITIS B, *VIRAL proteins, *GENETIC translation

Abstract

Hepatitis B virus (HBV) expresses co-terminal large (L), middle (M), and small (S) envelope proteins containing preS1/preS2/S, preS2/S, and S domain alone, respectively. S and preS1 domains mediate sequential virion attachment to heparan sulfate proteoglycans and sodium taurocholate cotransporting polypeptide (NTCP), respectively, which can be blocked by anti-S and anti-preS1 antibodies. How anti-preS2 antibodies neutralize HBV infectivity remains enigmatic. The late stage of chronic HBV infection often selects for mutated preS2 translation initiation codon to prevent M protein expression, or in-frame preS2 deletions to shorten both L and M proteins. When introduced to infectious clone of genotype C or D, both M-minus mutations and most 5’ preS2 deletions sustained virion production. Such mutant progeny viral particles were infectious in NTCP-reconstituted HepG2 cells. Neutralization experiments were performed on the genotype D clone. Although remaining susceptible to anti-preS1 and anti-S neutralizing antibodies, M-minus mutants were only partially neutralized by two anti-preS2 antibodies tested while preS2 deletion mutants were resistant. By infection experiments using viral particles with lost versus increased M protein expression, or a neutralization escaping preS2 deletion only present on L or M protein, we found that both full-length L and M proteins contributed to virus neutralization by the two anti-preS2 antibodies. Thus, immune escape could be a driving force for the selection of M-minus mutations, and especially preS2 deletions. The fact that both L and M proteins could mediate neutralization by anti-preS2 antibodies may shed light on the underlying molecular mechanism. IMPORTANCE The large (L), middle (M), and small (S) envelope proteins of hepatitis B virus (HBV) contain preS1/preS2/S, preS2/S, and S domain alone, respectively. The discovery of heparan sulfate proteoglycans and sodium taurocholate cotransporting polypeptide (NTCP) as the low- and high-affinity HBV receptors could explain neutralizing potential of anti-S and anti-preS1 antibodies, respectively, but how anti-preS2 neutralizing antibodies work remains enigmatic. In this study, we found two M-minus mutants in the context of genotype D partially escaped two anti-preS2 neutralizing antibodies in NTCP-reconstituted HepG2 cells, while several naturally occurring preS2 deletion mutants escaped both antibodies. By point mutations to eliminate or enhance M protein expression, and by introducing preS2 deletion selectively to L or M protein, we found binding of anti-preS2 antibodies to both L and M proteins contributed to neutralization of wild-type HBV infectivity. Our finding may shed light on the possible mechanism(s) whereby anti-preS2 antibodies neutralize HBV infectivity. [ABSTRACT FROM AUTHOR]

Published

2024

3. Effective inhibition of PDCoV infection in chimeric APN geneedited neonatal pigs.

Author

Jizong Li, Jian Zhou, Tianyi Zhang, Heyong Wu, Feng Li, Chunyun Qi, Liyuan Fan, Xuesong Yuan, Wei Wang, Rongli Guo, Baochao Fan, Xiaochun Tang, Daxin Pang, Hongsheng Ouyang, Zicong Xie, and Bin Li

Subjects

*ALANINE aminopeptidase, *DELTACORONAVIRUS, *CHIMERIC proteins, *CORONAVIRUSES, *VIRAL load

Abstract

Porcine deltacoronavirus (PDCoV), an emerging enteropathogenic coronavirus, is a serious threat to piglets and has zoonotic potential. Here, we aimed to further explore the role of aminopeptidase N (APN) as a receptor for PDCoV and test the inhibitory effect of a chimeric APN protein strategy on PDCoV infection. PK-15 cells and LLC-PK1 cells expressing chimeric APN were selected and infected with PDCoV. Viral replication was significantly decreased in these chimeric APN cells compared with that in control group cells. To further characterize the effect of the chimeric APN strategy on PDCoV infection in vitro, primary intestinal epithelial cells isolated from chimeric APN pigs were inoculated with PDCoV. Viral challenge of these cells led to decreased PDCoV infection. More importantly, virally challenged chimeric APN neonatal piglets displayed reduced viral load, significantly fewer microscopic lesions in the intestinal tissue, and no diarrhea. Taken together, these findings deepen our understanding of the mechanism of PDCoV infection and provide a valuable model for the production of disease-resistant animals. IMPORTANCE Porcine deltacoronavirus (PDCoV), an emerging enteropathogenic coronavirus, causes diarrhea in piglets and possesses the potential to infect humans. However, there are currently no effective measures for the prevention or control of PDCoV infection. Here, we have developed PK-15 cells, LLC-PK1 cells, and primary intestinal epithelial cells expressing chimeric APN, and viral challenge of these cells led to decreased PDCoV infection. Furthermore, virally challenged chimeric APN neonatal piglets displayed reduced viral load, significantly fewer microscopic lesions in the intestinal tissue, and no diarrhea. These data show that chimeric APN is a promising strategy to combat PDCoV infection. [ABSTRACT FROM AUTHOR]

Published

2024

4. Comparative Review of the State of the Art in Research on the Porcine Epidemic Diarrhea Virus and SARS-CoV-2, Scope of Knowledge between Coronaviruses.

Author

Rosas-Murrieta, Nora H., Rodríguez-Enríquez, Alan, Herrera-Camacho, Irma, Millán-Pérez-Peña, Lourdes, Santos-López, Gerardo, and Rivera-Benítez, José F.

Subjects

*PORCINE epidemic diarrhea virus, *CORONAVIRUSES, *SARS-CoV-2, *MIDDLE East respiratory syndrome, *SWINE farms, *SARS disease, *COVID-19

Abstract

This review presents comparative information corresponding to the progress in knowledge of some aspects of infection by the porcine epidemic diarrhea virus (PEDV) and severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2) coronaviruses. PEDV is an alphacoronavirus of great economic importance due to the million-dollar losses it generates in the pig industry. PEDV has many similarities to the SARS-CoV-2 betacoronavirus that causes COVID-19 disease. This review presents possible scenarios for SARS-CoV-2 based on the collected literature on PEDV and the tools or strategies currently developed for SARS-CoV-2 that would be useful in PEDV research. The speed of the study of SARS-CoV-2 and the generation of strategies to control the pandemic was possible due to the knowledge derived from infections caused by other human coronaviruses such as severe acute respiratory syndrome (SARS) and middle east respiratory syndrome (MERS). Therefore, from the information obtained from several coronaviruses, the current and future behavior of SARS-CoV-2 could be inferred and, with the large amount of information on the virus that causes COVID-19, the study of PEDV could be improved and probably that of new emerging and re-emerging coronaviruses. [ABSTRACT FROM AUTHOR]

Published

2024

5. Avian influenza A viruses exhibit plasticity in sialylglycoconjugate receptor usage in human lung cells.

Author

Chieh-Yu Liang, Huang, Iris, Han, Julianna, Sownthirarajan, Boopathi, Kulhankova, Katarina, Murray, Nathan B., Taherzadeh, Mehrnoush, Archer-Hartmann, Stephanie, Pepi, Lauren, Manivasagam, Senthamizharasi, Plung, Jesse, Sturtz, Miranda, Yolanda Yu, Vogel, Olivia A., Kandasamy, Matheswaran, Gourronc, Francoise A., Klingelhutz, Aloysius J., Choudhury, Biswa, Lijun Rong, and Perez, Jasmine T.

Subjects

*AVIAN influenza A virus, *GLYCOCALYX, *AVIAN influenza, *GLYCOCONJUGATES, *SIALIC acids, *LUNGS, *GLYCOLIPIDS

Abstract

Influenza A viruses (IAV) utilize sialic acid (Sia) containing cell surface glycoconjugates for host cell infection, and IAV strains from different host species show preferences for structurally distinct Sia at the termini of glycoconjugates. Various types of cell surface glycoconjugates (N-glycans, O-glycans, glycolipids) display significant diversity in both structure and carbohydrate composition. To define the types of sialylglycoconjugates that facilitate IAV infection, we utilized the CRISPR/Cas9 technique to truncate the three major types of glycoconjugates, either individually or in combination, by targeting glycosyltransferases essential to glycan biosynthesis in a human lung epithelial cell line. Our studies show that both human and avian IAV strains do not display strict preferences for a specific type of glycoconjugate. Interestingly, truncation of the three major types of glycoconjugates significantly decreased replication of human IAV strains, yet did not impact replication of avian IAV strains. Unlike human IAV strains, avian IAV strains were able to efficiently utilize other less prevalent shorter glycoconjugates such as sialyl Tn and sialyl T antigens. Taken together, our studies demonstrate that avian IAV strains utilize a broader repertoire of glycoconjugates for host cell infection as compared to human IAV strains. [ABSTRACT FROM AUTHOR]

Published

2023

6. Kidney cell culture Macaca fascicularis as a candidate for vaccine development and in vitro model.

Author

Yusni, Rahmat, Mariya, Silmi, Saepuloh, Uus, Mariya, Sela S., and Darusman, Huda S.

Subjects

*KIDNEY cell culture, *KRA, *VACCINE development, *CELL culture, *CELL morphology, *CELL populations

Abstract

Background: Cell culture is the proliferation of a cell population in vitro by isolating from the original tissue or growing from existing ones. One essential source is the monkey kidney cell cultures which have an essential role in biomedical study. This is due to the significant homology between the human and macaque genomes making these useful for cultivating human viruses, especially enteroviruses, and growing vaccines. Methods: This study developed cell cultures derived from the kidney of Macaca fascicularis (Mf) and validated its gene expression. Results: The primary cultures were successfully subcultured up to six passages, grew as monolayers, and exhibited epithelial‐like morphology. The cultured cells remained heterogeneous in phenotype and they expressed CD155 and CD46 as viral receptors, cell morphology (CD24, endosialin, and vWF), proliferation, also apoptosis markers (Ki67 and p53). Conclusions: These results indicated that the cell cultures can be used as in vitro model cells for vaccine development and bioactive compound. [ABSTRACT FROM AUTHOR]

Published

2023

7. The Structures and Functions of Parvovirus Capsids and Missing Pieces: the Viral DNA and Its Packaging, Asymmetrical Features, Nonprotein Components, and Receptor or Antibody Binding and Interactions.

Author

López-Astacio, Robert A., Adu, Oluwafemi F., Hyunwook Lee, Hafenstein, Susan L., and Parrish, Colin R.

Subjects

*VIRAL DNA, *RECEPTOR antibodies, *CAPSIDS, *CANINE parvovirus, *ADENO-associated virus, *SINGLE-stranded DNA

Abstract

Parvoviruses are among the smallest and superficially simplest animal viruses, infecting a broad range of hosts, including humans, and causing some deadly infections. In 1990, the first atomic structure of the canine parvovirus (CPV) capsid revealed a 26-nm-diameter T=1 particle made up of two or three versions of a single protein, and packaging about 5,100 nucleotides of single-stranded DNA. Our structural and functional understanding of parvovirus capsids and their ligands has increased as imaging and molecular techniques have advanced, and capsid structures for most groups within the Parvoviridae family have now been determined. Despite those advances, significant questions remain unanswered about the functioning of those viral capsids and their roles in release, transmission, or cellular infection. In addition, the interactions of capsids with host receptors, antibodies, or other biological components are also still incompletely understood. The parvovirus capsid's apparent simplicity likely conceals important functions carried out by small, transient, or asymmetric structures. Here, we highlight some remaining open questions that may need to be answered to provide a more thorough understanding of how these viruses carry out their various functions. The many different members of the family Parvoviridae share a capsid architecture, and while many functions are likely similar, others may differ in detail. Many of those parvoviruses have not been experimentally examined in detail (or at all in some cases), so we, therefore, focus this minireview on the widely studied protoparvoviruses, as well as the most thoroughly investigated examples of adeno-associated viruses. [ABSTRACT FROM AUTHOR]

Published

2023

8. Comparative Review of the State of the Art in Research on the Porcine Epidemic Diarrhea Virus and SARS-CoV-2, Scope of Knowledge between Coronaviruses

Author

Nora H. Rosas-Murrieta, Alan Rodríguez-Enríquez, Irma Herrera-Camacho, Lourdes Millán-Pérez-Peña, Gerardo Santos-López, and José F. Rivera-Benítez

Subjects

PEDV, SARS-CoV-2, coronaviruses, viral receptor, innate immune response, vaccines, Microbiology, QR1-502

Abstract

This review presents comparative information corresponding to the progress in knowledge of some aspects of infection by the porcine epidemic diarrhea virus (PEDV) and severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2) coronaviruses. PEDV is an alphacoronavirus of great economic importance due to the million-dollar losses it generates in the pig industry. PEDV has many similarities to the SARS-CoV-2 betacoronavirus that causes COVID-19 disease. This review presents possible scenarios for SARS-CoV-2 based on the collected literature on PEDV and the tools or strategies currently developed for SARS-CoV-2 that would be useful in PEDV research. The speed of the study of SARS-CoV-2 and the generation of strategies to control the pandemic was possible due to the knowledge derived from infections caused by other human coronaviruses such as severe acute respiratory syndrome (SARS) and middle east respiratory syndrome (MERS). Therefore, from the information obtained from several coronaviruses, the current and future behavior of SARS-CoV-2 could be inferred and, with the large amount of information on the virus that causes COVID-19, the study of PEDV could be improved and probably that of new emerging and re-emerging coronaviruses.

Published

2024

9. Reduced Folate Carrier: an Entry Receptor for a Novel Feline Leukemia Virus Variant.

Author

Miyake, Ariko, Kawasaki, Junna, Ngo, Ha, Makundi, Isaac, Muto, Yutaro, Khan, Arshad H, Smith, Desmond J, and Nishigaki, Kazuo

Subjects

Medical Microbiology, Biomedical and Clinical Sciences, Biotechnology, Genetics, Prevention, Rare Diseases, Infectious Diseases, Aetiology, 2.2 Factors relating to the physical environment, 2.1 Biological and endogenous factors, Infection, Good Health and Well Being, Amino Acid Sequence, Animals, Cats, Cell Line, Cricetinae, Endogenous Retroviruses, Gene Products, env, Genes, env, HeLa Cells, Humans, Leukemia Virus, Feline, Leukemia, Feline, Phylogeny, Proviruses, RNA, Viral, Receptors, Virus, Reduced Folate Carrier Protein, Sequence Alignment, Viral Envelope Proteins, Virus Internalization, Virus Replication, cats, endogenous retrovirus, feline leukemia virus, retroviruses, viral envelope, viral infection, viral pathogenesis, viral receptor, Hela Cells, Biological Sciences, Agricultural and Veterinary Sciences, Medical and Health Sciences, Virology, Agricultural, veterinary and food sciences, Biological sciences, Biomedical and clinical sciences

Abstract

Feline leukemia virus (FeLV) is horizontally transmitted among cats and causes a variety of hematopoietic disorders. Five subgroups of FeLV, A to D and T, each with distinct receptor usages, have been described. Recently, we identified a new FeLV Env (TG35-2) gene from a pseudotyped virus that does not belong to any known subgroup. FeLV-A is the primary virus from which other subgroups have emerged via mutation or recombination of the subgroup A env gene. Retrovirus entry into cells is mediated by the interaction of envelope protein (Env) with specific cell surface receptors. Here, phenotypic screening of a human/hamster radiation hybrid panel identified SLC19A1, a feline reduced folate carrier (RFC) and potential receptor for TG35-2-phenotypic virus. RFC is a multipass transmembrane protein. Feline and human RFC cDNAs conferred susceptibility to TG35-2-pseudotyped virus when introduced into nonpermissive cells but did not render these cells permissive to other FeLV subgroups or feline endogenous retrovirus. Moreover, human cells with genomic deletion of RFC were nonpermissive for TG35-2-pseudotyped virus infection, but the introduction of feline and human cDNAs rendered them permissive. Mutation analysis of FeLV Env demonstrated that amino acid substitutions within variable region A altered the specificity of the Env-receptor interaction. We isolated and reconstructed the full-length infectious TG35-2-phenotypic provirus from a naturally FeLV-infected cat, from which the FeLV Env (TG35-2) gene was previously isolated, and compared the replication of the virus in hematopoietic cell lines with that of FeLV-A 61E by measuring the viral RNA copy numbers. These results provide a tool for further investigation of FeLV infectious disease.IMPORTANCE Feline leukemia virus (FeLV) is a member of the genus Gammaretrovirus, which causes malignant diseases in cats. The most prevalent FeLV among cats is FeLV subgroup A (FeLV-A), and specific binding of FeLV-A Env to its viral receptor, thiamine transporter feTHTR1, is the first step of infection. In infected cats, novel variants of FeLV with altered receptor specificity for viral entry have emerged by mutation or recombination of the env gene. A novel FeLV variant arose from a subtle mutation of FeLV-A Env, which altered the specific interaction of the virus with its receptor. RFC, a folate transporter, is a potential receptor for the novel FeLV variant. The perturbation of specific retrovirus-receptor interactions under selective pressure by the host results in the emergence of novel viruses.

Published

2019

10. Coxsackievirus and Adenovirus Receptor (CXADR): Recent Findings and Its Role and Regulation in Spermatogenesis

Author

Zhang, Yang, Lui, Wing-Yee, Crusio, Wim E., Series Editor, Dong, Haidong, Series Editor, Radeke, Heinfried H., Series Editor, Rezaei, Nima, Series Editor, Steinlein, Ortrud, Series Editor, Xiao, Junjie, Series Editor, Cheng, C.Yan, editor, and Sun, Fei, editor

Published

2021

11. Usutu virus escapes langerin-induced restriction to productively infect human Langerhans cells, unlike West Nile virus

Author

Marie-France Martin, Ghizlane Maarifi, Hervé Abiven, Marine Seffals, Nicolas Mouchet, Cécile Beck, Charles Bodet, Nicolas Lévèque, Nathalie J. Arhel, Fabien P. Blanchet, Yannick Simonin, and Sébastien Nisole

Subjects

west nile virus, usutu virus, langerhans cells, langerin, viral receptor, Infectious and parasitic diseases, RC109-216, Microbiology, QR1-502

Abstract

Usutu virus (USUV) and West Nile virus (WNV) are phylogenetically close emerging arboviruses transmitted by mosquitoes, and constitute a global public health threat. Since USUV and WNV enter the body through the skin, the first immune cells they encounter are skin-resident dendritic cells, the most peripheral outpost of immune defense. This unique network is composed of Langerhans cells (LCs) and dermal DCs, which reside in the epidermis and the dermis, respectively. Using human skin explants, we show that while both viruses can replicate in keratinocytes, they can also infect resident DCs with distinct tropism, since WNV preferentially infects DCs in the dermis, whereas USUV has a greater propensity to infect LCs. Using both purified human epidermal LCs (eLCs) and monocyte derived LCs (MoLCs), we confirm that LCs sustain a faster and more efficient replication of USUV compared with WNV and that this correlates with a more intense innate immune response to USUV compared with WNV. Next, we show that ectopic expression of the LC-specific C-type lectin receptor (CLR), langerin, in HEK293T cells allows WNV and USUV to bind and enter, but supports the subsequent replication of USUV only. Conversely, blocking or silencing langerin in MoLCs or eLCs made them resistant to USUV infection, thus demonstrating that USUV uses langerin to enter and replicate in LCs. Altogether, our results demonstrate that LCs constitute privileged target cells for USUV in human skin, because langerin favors its entry and replication. Intriguingly, this suggests that USUV efficiently escapes the antiviral functions of langerin, which normally safeguards LCs from most viral infections.

Published

2022

12. Role of CD163 in PRRSV infection.

Author

Rowland, Raymond R.R. and Brandariz-Nuñez, Alberto

Subjects

*PORCINE reproductive & respiratory syndrome, *ALVEOLAR macrophages, *SWINE industry, *VACCINE development, *INFECTION control

Abstract

Porcine reproductive and respiratory syndrome virus (PRRSV) is a highly infectious agent that poses a significant economic threat to the global swine industry. Efficient viral entry relies on interactions with cellular receptors, with CD163—a cysteine-rich scavenger receptor found on porcine alveolar macrophages (PAMs)—playing a critical role. Extensive evidence supports CD163's essential function in PRRSV infection. This review synthesizes current knowledge about CD163's role, examining its structure-function relationship and identifying specific regions crucial for viral entry. We evaluate the established role of CD163 in PRRSV pathogenesis and highlight areas requiring further investigation, along with the potential for targeted therapeutic interventions. Understanding the molecular determinants of CD163's function is vital for developing effective strategies to control PRRSV infection and mitigate its economic impact on swine production. Further research into the PRRSV-CD163 interactions will be crucial for creating novel antiviral strategies. • Recent advances show that CD163 is a key receptor for PRRSV infection. • Understanding CD163 and its function in PRRSV infection will improve PRRSV control. • Knowledge on PRRSV cell entry will aid in developing new vaccines and antivirals. [ABSTRACT FROM AUTHOR]

Published

2024

13. Neural precursor cells derived from induced pluripotent stem cells exhibit reduced susceptibility to infection with a neurotropic coronavirus.

Author

Mangale, Vrushali, Marro, Brett, Plaisted, Warren, Lane, Thomas, and Walsh, Craig

Subjects

Cytopathology, Mouse hepatitis virus, Neural progenitor cells, Viral receptor, Animals, Carcinoembryonic Antigen, Cell Differentiation, Gene Expression, Histocompatibility Antigens Class I, Histocompatibility Antigens Class II, Induced Pluripotent Stem Cells, Interferon-gamma, Mice, Mice, Transgenic, Murine hepatitis virus, Neural Stem Cells

Abstract

The present study examines the susceptibility of mouse induced pluripotent stem cell-derived neural precursor cells (iPSC-NPCs) to infection with the neurotropic JHM strain of mouse hepatitis virus (JHMV). Similar to NPCs derived from striatum of day 1 postnatal GFP-transgenic mice (GFP-NPCs), iPSC-derived NPCs (iPSC-NPCs) are able to differentiate into terminal neural cell types and express MHC class I and II in response to IFN-γ treatment. However, in contrast to postnatally-derived NPCs, iPSC-NPCs express low levels of carcinoembryonic antigen-cell adhesion molecule 1a (CEACAM1a), the surface receptor for JHMV, and are less susceptible to infection and virus-induced cytopathic effects. The relevance of this in terms of therapeutic application of NPCs resistant to viral infection is discussed.

Published

2017

14. Cytolytic Recombinant Vesicular Stomatitis Viruses Expressing STLV-1 Receptor Specifically Eliminate STLV-1 Env-Expressing Cells in an HTLV-1 Surrogate Model In Vitro.

Author

Seki, Yohei, Kitamura, Tomoya, Tezuka, Kenta, Murata, Megumi, Akari, Hirofumi, Hamaguchi, Isao, and Okuma, Kazu

Subjects

*VESICULAR stomatitis, *HTLV-I, *VIRAL envelope proteins, *JAPANESE macaque, *GLUCOSE transporters

Abstract

Human T-cell leukemia virus type 1 (HTLV-1) causes serious and intractable diseases in some carriers after infection. The elimination of infected cells is considered important to prevent this onset, but there are currently no means by which to accomplish this. We previously developed "virotherapy", a therapeutic method that targets and kills HTLV-1-infected cells using a cytolytic recombinant vesicular stomatitis virus (rVSV). Infection with rVSV expressing an HTLV-1 primary receptor elicits therapeutic effects on HTLV-1-infected envelope protein (Env)-expressing cells in vitro and in vivo. Simian T-cell leukemia virus type 1 (STLV-1) is closely related genetically to HTLV-1, and STLV-1-infected Japanese macaques (JMs) are considered a useful HTLV-1 surrogate, non-human primate model in vivo. Here, we performed an in vitro drug evaluation of rVSVs against STLV-1 as a preclinical study. We generated novel rVSVs encoding the STLV-1 primary receptor, simian glucose transporter 1 (JM GLUT1), with or without an AcGFP reporter gene. Our data demonstrate that these rVSVs specifically and efficiently infected/eliminated the STLV-1 Env-expressing cells in vitro. These results indicate that rVSVs carrying the STLV-1 receptor could be an excellent candidate for unique anti-STLV-1 virotherapy; therefore, such antivirals can now be applied to STLV-1-infected JMs to determine their therapeutic usefulness in vivo. [ABSTRACT FROM AUTHOR]

Published

2022

15. Structural Insights into Rotavirus Entry

Author

Rodríguez, Javier M., Luque, Daniel, COHEN, IRUN R., Editorial Board Member, LAJTHA, ABEL, Editorial Board Member, LAMBRIS, JOHN D., Editorial Board Member, PAOLETTI, RODOLFO, Editorial Board Member, REZAEI, NIMA, Editorial Board Member, and Greber, Urs F., editor

Published

2019

16. Effective inhibition of PDCoV infection in chimeric APN gene-edited neonatal pigs.

Author

Li J, Zhou J, Zhang T, Wu H, Li F, Qi C, Fan L, Yuan X, Wang W, Guo R, Fan B, Tang X, Pang D, Ouyang H, Xie Z, and Li B

Subjects

Animals, Swine, Viral Load, Gene Editing methods, Cell Line, Epithelial Cells virology, Diarrhea virology, CD13 Antigens genetics, CD13 Antigens metabolism, Animals, Newborn, Virus Replication, Swine Diseases virology, Deltacoronavirus genetics, Coronavirus Infections virology, Coronavirus Infections veterinary, Coronavirus Infections prevention & control

Abstract

Porcine deltacoronavirus (PDCoV), an emerging enteropathogenic coronavirus, is a serious threat to piglets and has zoonotic potential. Here, we aimed to further explore the role of aminopeptidase N (APN) as a receptor for PDCoV and test the inhibitory effect of a chimeric APN protein strategy on PDCoV infection. PK-15 cells and LLC-PK1 cells expressing chimeric APN were selected and infected with PDCoV. Viral replication was significantly decreased in these chimeric APN cells compared with that in control group cells. To further characterize the effect of the chimeric APN strategy on PDCoV infection in vitro , primary intestinal epithelial cells isolated from chimeric APN pigs were inoculated with PDCoV. Viral challenge of these cells led to decreased PDCoV infection. More importantly, virally challenged chimeric APN neonatal piglets displayed reduced viral load, significantly fewer microscopic lesions in the intestinal tissue, and no diarrhea. Taken together, these findings deepen our understanding of the mechanism of PDCoV infection and provide a valuable model for the production of disease-resistant animals., Importance: Porcine deltacoronavirus (PDCoV), an emerging enteropathogenic coronavirus, causes diarrhea in piglets and possesses the potential to infect humans. However, there are currently no effective measures for the prevention or control of PDCoV infection. Here, we have developed PK-15 cells, LLC-PK1 cells, and primary intestinal epithelial cells expressing chimeric APN, and viral challenge of these cells led to decreased PDCoV infection. Furthermore, virally challenged chimeric APN neonatal piglets displayed reduced viral load, significantly fewer microscopic lesions in the intestinal tissue, and no diarrhea. These data show that chimeric APN is a promising strategy to combat PDCoV infection., Competing Interests: The authors declare no conflict of interest.

Published

2024

17. Both middle and large envelope proteins can mediate neutralization of hepatitis B virus infectivity by anti-preS2 antibodies: escape by naturally occurring preS2 deletions.

Author

Zhang J, Wang Q, Yuan W, Li J, Yuan Q, Zhang J, Xia N, Wang Y, Li J, and Tong S

Subjects

Humans, Hep G2 Cells, Sequence Deletion, Symporters immunology, Symporters genetics, Protein Precursors immunology, Protein Precursors genetics, Hepatitis B Antibodies immunology, Hepatitis B immunology, Hepatitis B virology, Genotype, Immune Evasion, Organic Anion Transporters, Sodium-Dependent genetics, Organic Anion Transporters, Sodium-Dependent immunology, Organic Anion Transporters, Sodium-Dependent metabolism, Virion immunology, Hepatitis B virus immunology, Hepatitis B virus genetics, Hepatitis B Surface Antigens immunology, Hepatitis B Surface Antigens genetics, Viral Envelope Proteins immunology, Viral Envelope Proteins genetics, Antibodies, Neutralizing immunology

Abstract

Hepatitis B virus (HBV) expresses co-terminal large (L), middle (M), and small (S) envelope proteins containing preS1/preS2/S, preS2/S, and S domain alone, respectively. S and preS1 domains mediate sequential virion attachment to heparan sulfate proteoglycans and sodium taurocholate cotransporting polypeptide (NTCP), respectively, which can be blocked by anti-S and anti-preS1 antibodies. How anti-preS2 antibodies neutralize HBV infectivity remains enigmatic. The late stage of chronic HBV infection often selects for mutated preS2 translation initiation codon to prevent M protein expression, or in-frame preS2 deletions to shorten both L and M proteins. When introduced to infectious clone of genotype C or D, both M-minus mutations and most 5' preS2 deletions sustained virion production. Such mutant progeny viral particles were infectious in NTCP-reconstituted HepG2 cells. Neutralization experiments were performed on the genotype D clone. Although remaining susceptible to anti-preS1 and anti-S neutralizing antibodies, M-minus mutants were only partially neutralized by two anti-preS2 antibodies tested while preS2 deletion mutants were resistant. By infection experiments using viral particles with lost versus increased M protein expression, or a neutralization escaping preS2 deletion only present on L or M protein, we found that both full-length L and M proteins contributed to virus neutralization by the two anti-preS2 antibodies. Thus, immune escape could be a driving force for the selection of M-minus mutations, and especially preS2 deletions. The fact that both L and M proteins could mediate neutralization by anti-preS2 antibodies may shed light on the underlying molecular mechanism.IMPORTANCEThe large (L), middle (M), and small (S) envelope proteins of hepatitis B virus (HBV) contain preS1/preS2/S, preS2/S, and S domain alone, respectively. The discovery of heparan sulfate proteoglycans and sodium taurocholate cotransporting polypeptide (NTCP) as the low- and high-affinity HBV receptors could explain neutralizing potential of anti-S and anti-preS1 antibodies, respectively, but how anti-preS2 neutralizing antibodies work remains enigmatic. In this study, we found two M-minus mutants in the context of genotype D partially escaped two anti-preS2 neutralizing antibodies in NTCP-reconstituted HepG2 cells, while several naturally occurring preS2 deletion mutants escaped both antibodies. By point mutations to eliminate or enhance M protein expression, and by introducing preS2 deletion selectively to L or M protein, we found binding of anti-preS2 antibodies to both L and M proteins contributed to neutralization of wild-type HBV infectivity. Our finding may shed light on the possible mechanism(s) whereby anti-preS2 antibodies neutralize HBV infectivity., Competing Interests: The authors declare no conflict of interest.

Published

2024

18. Effects of common mutations in the SARS-CoV-2 Spike RBD and its ligand, the human ACE2 receptor on binding affinity and kinetics

Author

Michael I Barton, Stuart A MacGowan, Mikhail A Kutuzov, Omer Dushek, Geoffrey John Barton, and P Anton van der Merwe

Subjects

COVID-19, SARS-CoV-2, ACE2, viral receptor, affinity, coronavirus, Medicine, Science, Biology (General), QH301-705.5

Abstract

The interaction between the SARS-CoV-2 virus Spike protein receptor binding domain (RBD) and the ACE2 cell surface protein is required for viral infection of cells. Mutations in the RBD are present in SARS-CoV-2 variants of concern that have emerged independently worldwide. For example, the B.1.1.7 lineage has a mutation (N501Y) in its Spike RBD that enhances binding to ACE2. There are also ACE2 alleles in humans with mutations in the RBD binding site. Here we perform a detailed affinity and kinetics analysis of the effect of five common RBD mutations (K417N, K417T, N501Y, E484K, and S477N) and two common ACE2 mutations (S19P and K26R) on the RBD/ACE2 interaction. We analysed the effects of individual RBD mutations and combinations found in new SARS-CoV-2 Alpha (B.1.1.7), Beta (B.1.351), and Gamma (P1) variants. Most of these mutations increased the affinity of the RBD/ACE2 interaction. The exceptions were mutations K417N/T, which decreased the affinity. Taken together with other studies, our results suggest that the N501Y and S477N mutations enhance transmission primarily by enhancing binding, the K417N/T mutations facilitate immune escape, and the E484K mutation enhances binding and immune escape.

Published

2021

19. Optical biosensors utilising viral receptors ACE2 and ACE2 mimics.

Author

Ow, Sian Yang, Sutarlie, Laura, Lim, Samuel Wei Yang, Salleh, Nur Asinah Binte Mohamed, Tanaka, Yuki, Tan, Chee Kiang Ivan, and Su, Xiaodi

Subjects

*BIOSENSORS, *VIRAL antigens, *SERS spectroscopy

Abstract

Common viral infections start from binding of the viral pathogens to the viral receptors on the host body, for example, SARS-CoV-2 infects cells by binding to human angiotensin converting enzyme 2 (ACE2). This review discusses optical biosensors that exploit ACE2 or ACE2 derived peptides (ACE2 mimics) as affinity ligands for detecting SARS-CoV-2. In these biosensors, the target analytes can include surrogate pseudoviruses, inactivated SARS-CoV-2 virus, spike proteins, or receptor binding domain (RBD) of the spike protein. The advantages of using ACE2 and/or ACE2 mimics over common affinity ligands (e.g. antibodies) against future virus mutations are highlighted. The advantages of the smaller sized ACE2 mimics relative to ACE2 protein for achieving more versatile sensor designs and higher selectivity are also discussed. In addition to SARS-CoV-2 detection, this review also discusses the expanded application of ACE2-based optical biosensors for the detection of non-viral targets, e.g., SARS-CoV-2 neutralising antibodies and anti-SARS-CoV-2 drugs. [Display omitted] • Designs of optical biosensors utilising viral receptor ACE2 are presented. • Use of ACE2 and ACE2 mimics opens new designs of optical viral biosensors. • Applications in detection of virus, viral antigens, neutralising antibodies, and drugs are discussed. • Sensing performance of different designs of optical biosensors are compared. • Advantages of optical biosensors utilising viral receptors are highlighted. [ABSTRACT FROM AUTHOR]

Published

2024

20. Structural basis of host ligand specificity change of GII porcine noroviruses from their closely related GII human noroviruses

Author

Yang Yang, Ming Xia, Leyi Wang, Sahaana Arumugam, Yajing Wang, Xianjin Ou, Chenlong Wang, Xi Jiang, Ming Tan, Yutao Chen, and Xuemei Li

Subjects

Emerging norovirus, viral evolution, crystal structure, viral receptor, virus-host interaction, viral attachment, Infectious and parasitic diseases, RC109-216, Microbiology, QR1-502

Abstract

ABSTRACTDiverse noroviruses infect humans and animals via the recognition of host-specific glycan ligands. Genogroup II (GII) noroviruses consist of human noroviruses (huNoVs) that generally bind histo-blood group antigens (HBGAs) as host factors and three porcine norovirus (porNoV) genotypes (GII.11/18/19) that form a genetic lineage lacking HBGA-binding ability. Thus, these GII porNoVs provide an excellent model to study norovirus evolution with host ligand specificity changes. Here we solved the crystal structures of a native GII.11 porNoV P protein and a closely-related GII.3 huNoV P protein complexed with an HBGA, focusing on the HBGA-binding sites (HBSs) compared with the previously known ones to understand the structural basis of the host ligand specificity change. We found that the GII.3 huNoV binds HBGAs via a conventional GII HBS that uses an arginine instead of the conserved aromatic residue for the required Van der Waals interaction, while the GII.11 porNoV HBS loses its HBGA-binding function because of two mutations (Q355/V451). A mutant that reversed the two mutated residues back to the conventional A355/Y451 restored the HBGA-binding function of the GII.11 porNoV P protein, which validated our observations. Similar mutations are also found in GII.19 porNoVs and a GII.19 P protein mutant with double reverse mutations restored the HBS function. This is the first reconstruction of a functional HBS based on one with new host specificity back to its parental one. These data shed light on the molecular basis of structural adaptation of the GII porNoVs to the pig hosts through mutations at their HBSs.

Published

2019

21. Cytolytic Recombinant Vesicular Stomatitis Viruses Expressing STLV-1 Receptor Specifically Eliminate STLV-1 Env-Expressing Cells in an HTLV-1 Surrogate Model In Vitro

Author

Yohei Seki, Tomoya Kitamura, Kenta Tezuka, Megumi Murata, Hirofumi Akari, Isao Hamaguchi, and Kazu Okuma

Subjects

HTLV-1, HTLV-1 surrogate model, STLV-1, recombinant VSV, viral receptor, envelope protein, Microbiology, QR1-502

Abstract

Human T-cell leukemia virus type 1 (HTLV-1) causes serious and intractable diseases in some carriers after infection. The elimination of infected cells is considered important to prevent this onset, but there are currently no means by which to accomplish this. We previously developed “virotherapy”, a therapeutic method that targets and kills HTLV-1-infected cells using a cytolytic recombinant vesicular stomatitis virus (rVSV). Infection with rVSV expressing an HTLV-1 primary receptor elicits therapeutic effects on HTLV-1-infected envelope protein (Env)-expressing cells in vitro and in vivo. Simian T-cell leukemia virus type 1 (STLV-1) is closely related genetically to HTLV-1, and STLV-1-infected Japanese macaques (JMs) are considered a useful HTLV-1 surrogate, non-human primate model in vivo. Here, we performed an in vitro drug evaluation of rVSVs against STLV-1 as a preclinical study. We generated novel rVSVs encoding the STLV-1 primary receptor, simian glucose transporter 1 (JM GLUT1), with or without an AcGFP reporter gene. Our data demonstrate that these rVSVs specifically and efficiently infected/eliminated the STLV-1 Env-expressing cells in vitro. These results indicate that rVSVs carrying the STLV-1 receptor could be an excellent candidate for unique anti-STLV-1 virotherapy; therefore, such antivirals can now be applied to STLV-1-infected JMs to determine their therapeutic usefulness in vivo.

Published

2022

22. Hijacking the Fusion Complex of Human Parainfluenza Virus as an Antiviral Strategy

Author

T. C. Marcink, E. Yariv, K. Rybkina, V. Más, F. T. Bovier, A. des Georges, A. L. Greninger, C. A. Alabi, M. Porotto, N. Ben-Tal, and A. Moscona

Subjects

antiviral agents, cryo-electron tomography, viral fusion protein, viral protein structure, viral receptor, Microbiology, QR1-502

Abstract

ABSTRACT The receptor binding protein of parainfluenza virus, hemagglutinin-neuraminidase (HN), is responsible for actively triggering the viral fusion protein (F) to undergo a conformational change leading to insertion into the target cell and fusion of the virus with the target cell membrane. For proper viral entry to occur, this process must occur when HN is engaged with host cell receptors at the cell surface. It is possible to interfere with this process through premature activation of the F protein, distant from the target cell receptor. Conformational changes in the F protein and adoption of the postfusion form of the protein prior to receptor engagement of HN at the host cell membrane inactivate the virus. We previously identified small molecules that interact with HN and induce it to activate F in an untimely fashion, validating a new antiviral strategy. To obtain highly active pretriggering candidate molecules we carried out a virtual modeling screen for molecules that interact with sialic acid binding site II on HN, which we propose to be the site responsible for activating F. To directly assess the mechanism of action of one such highly effective new premature activating compound, PAC-3066, we use cryo-electron tomography on authentic intact viral particles for the first time to examine the effects of PAC-3066 treatment on the conformation of the viral F protein. We present the first direct observation of the conformational rearrangement induced in the viral F protein. IMPORTANCE Paramyxoviruses, including human parainfluenza virus type 3, are internalized into host cells by fusion between viral and target cell membranes. The receptor binding protein, hemagglutinin-neuraminidase (HN), upon binding to its cell receptor, triggers conformational changes in the fusion protein (F). This action of HN activates F to reach its fusion-competent state. Using small molecules that interact with HN, we can induce the premature activation of F and inactivate the virus. To obtain highly active pretriggering compounds, we carried out a virtual modeling screen for molecules that interact with a sialic acid binding site on HN that we propose to be the site involved in activating F. We use cryo-electron tomography of authentic intact viral particles for the first time to directly assess the mechanism of action of this treatment on the conformation of the viral F protein and present the first direct observation of the induced conformational rearrangement in the viral F protein.

Published

2020

23. Molecular mechanism for antibody-dependent enhancement of coronavirus entry.

Author

Yushun Wan, Jian Shang, Shihui Sun, Wanbo Tai, Jing Chen, Qibin Geng, Lei He, Yuehong Chen, Jianming Wu, Zhengli Shi, Yusen Zhou, Lanying Du, and Fang Li

Subjects

*CELL receptors, *FC receptors, *MERS coronavirus, *VIRAL proteins, *VIRUS diseases, *MONOCLONAL antibodies

Abstract

Antibody-dependent enhancement (ADE) of viral entry has been a major concern for epidemiology, vaccine development and antibody-based drug therapy. However, the molecular mechanism behind ADE is still elusive. Coronavirus spike protein mediates viral entry into cells by first binding to a receptor on host cell surface and then fusing viral and host membranes. Here we investigated how a neutralizing monoclonal antibody (mAb), which targets the receptor-binding domain (RBD) of MERS coronavirus spike, mediates viral entry using pseudovirus entry and biochemical assays. Our results showed that mAb binds to the virus-surface spike, allowing it to undergo conformational changes and become prone to proteolytic activation. Meanwhile, mAb binds to cell-surface IgG Fc receptor, guiding viral entry through canonical viral-receptor-dependent pathways. Our data suggest that the antibody/Fc-receptor complex functionally mimics viral receptor in mediating viral entry. Moreover, we characterized mAb dosages in viral receptor-dependent, antibody-dependent, and both-receptors-dependent entry pathways, delineating guidelines on mAb usages in treating viral infections. Our study reveals a novel molecular mechanism for antibody-enhanced viral entry and can guide future vaccination and antiviral strategies. [ABSTRACT FROM AUTHOR]

Published

2020

24. The Impact of Angiotensin-Converting Enzyme 2 (ACE2) Expression Levels in Patients with Comorbidities on COVID-19 Severity: A Comprehensive Review

Author

Rui Rodrigues and Sofia Costa de Oliveira

Subjects

ACE2, SARS-CoV-2, COVID-19, comorbidity, viral receptor, Biology (General), QH301-705.5

Abstract

Angiotensin-Converting Enzyme 2 (ACE2) has been proved to be the main host cell receptor for the binding of the severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2), the virus responsible for the COVID-19 pandemic. The SARS-CoV-2 spike (S) protein binds to ACE2 to initiate the process of replication. This enzyme is widely present in human organ tissues, such as the heart and lung. The pathophysiology of ACE2 in SARS-CoV-2 infection is complex and may be associated with several factors and conditions that are more severe in COVID-19 patients, such as age, male gender, and comorbidities, namely, cardiovascular diseases, chronic respiratory diseases, obesity, and diabetes. Here we present a comprehensive review that aims to correlate the levels of expression of the ACE2 in patients with comorbidities and with a poor outcome in COVID-19 disease. Significantly higher levels of expression of ACE2 were observed in myocardial and lung tissues in heart failure and COPD patients, respectively. An age-dependent increase in SARS2-CoV-2 receptors in the respiratory epithelium may be also responsible for the increased severity of COVID-19 lung disease in elderly people. Although the role of ACE2 is highlighted regarding the damage that can arise upon the SARS-CoV-2 invasion, there was no association observed between renin-angiotensin-aldosterone system (RAAS) inhibitors and the severity of COVID-19.

Published

2021

25. CD155: A Key Receptor Playing Diversified Roles

Author

Snehasis Jana, Trupti Gohil, Upendra P. Lambe, Shyam Sundar Nandi, Sonali Ankush Sawant, and Sudip Ghosh

Subjects

Cell signaling, biology, Chemistry, General Medicine, Ligands, Biochemistry, Transmembrane protein, Hedgehog signaling pathway, Cell biology, TIGIT, Viral Receptor, Neoplasms, biology.protein, Humans, Receptors, Virus, Molecular Medicine, Hedgehog Proteins, CD155, Receptors, Immunologic, Receptor, Molecular Biology, Poliovirus Receptor

Abstract

Cluster of differentiation (CD155), formerly identified as poliovirus receptor (PVR) and later as immunoglobulin molecule, is involved in cell adhesion, proliferation, invasion and migration. It is a surface protein expressed mostly on normal and transformed malignant cells. The expression of the receptor varies based on the origin of tissue. The expression of the protein is determined by factors involved in the sonic hedgehog pathway, Ras-MEK-ERK pathway and during stressful conditions like DNA damage response. The protein uses an alternate splicing mechanism, producing four isoforms, two being soluble (CD155β and CD155γ) and two being transmembrane protein (CD155α and CD155δ). Apart from being a viral receptor, researchers have identified CD155 to play important roles in cancer research and the cell signaling field. The receptor is recognized as a biomarker for identifying cancerous tissue. The receptor interacts with molecules involved in the cells’ defense mechanism. The immunesurveillance role of CD155 is being deciphered to understand the mechanistic approach it utilizes as an onco-immunologic molecule. CD155 is a non-MHC-I ligand which helps in identifying non-self to NK cells via an inhibitory TIGIT ligand. The TIGIT–CD155 pathway is a novel MHC-I-independent education mechanism for cell tolerance and activation of NK cells. The receptor also has a role in metastasis of cancer and transendothelial mechanism. In this review, the authors discuss the virus-host interaction that occurs via a single transmembrane receptor, the poliovirus infection pathway, which is being exploited as a therapeutic pathway. The oncolytic virotherapy is now a promising modality for curing cancer.

Published

2022

26. GII.13/21 noroviruses recognize glycans with a terminal β-galactose via an unconventional glycan binding site.

Author

Xin Cong, Xiao-man Sun, Jian-xun Qi, Han-bo Li, Wen-gang Chai, Qing Zhang, Hong Wang, Xiang-yu Kong, Jiao Song, Li-li Pang, Miao Jin, Dan-di Li, Ming Tan, and Zhao-jun Duan

Subjects

*BINDING sites, *NOROVIRUSES, *GLYCANS, *CRYSTAL structure, *PROTEIN domains, *SACCHARIDES

Abstract

Human noroviruses (huNoVs) recognize histo-blood group antigens (HBGAs) as host susceptibility factors. GII.13 and GII.21 huNoVs form a unique genetic lineage that emerged from mainstream GII NoVs via development of a new, nonconventional glycan binding site (GBS) that binds Lea antigen. This previous finding raised the question of whether the new GII.13/21 GBS really has such a narrow glycan binding spectrum. In this study, we provide solid phenotypic and structural evidence indicating that this new GBS recognizes a group of glycans with a common terminal β-galactose (β-Gal). First, we found that P domain proteins of GII.13/21 huNoVs circulating at different times bound three glycans sharing a common terminal β-Gal, including Lec, lactose, and mucin core 2. Second, we solved the crystal structures of the GII.13 P dimers in complex with Lec and mucin core 2, which showed that β-Gal is the major binding saccharide. Third, nonfat milk and lactose blocked the GII.13/21 P domain-glycan binding, which may explain the low prevalence of GII.13/21 viruses. Our data provide new insight into the host interactions and epidemiology of huNoVs, which would help in the control and prevention of NoV-associated diseases. [ABSTRACT FROM AUTHOR]

Published

2019

27. Resistance to coronavirus infection in amino peptidase N-deficient pigs.

Author

Whitworth, Kristin M., Rowland, Raymond R. R., Petrovan, Vlad, Sheahan, Maureen, Cino-Ozuna, Ada G., Fang, Ying, Hesse, Richard, Mileham, Alan, Samuel, Melissa S., Wells, Kevin D., and Prather, Randall S.

Abstract

The alphacoronaviruses, transmissible gastroenteritis virus (TGEV) and Porcine epidemic diarrhea virus (PEDV) are sources of high morbidity and mortality in neonatal pigs, a consequence of dehydration caused by the infection and necrosis of enterocytes. The biological relevance of amino peptidase N (ANPEP) as a putative receptor for TGEV and PEDV in pigs was evaluated by using CRISPR/Cas9 to edit exon 2 of ANPEP resulting in a premature stop codon. Knockout pigs possessing the null ANPEP phenotype and age matched wild type pigs were challenged with either PEDV or TGEV. Fecal swabs were collected daily from each animal beginning 1 day prior to challenge with PEDV until the termination of the study. The presence of virus nucleic acid was determined by PCR. ANPEP null pigs did not support infection with TGEV, but retained susceptibility to infection with PEDV. Immunohistochemistry confirmed the presence of PEDV reactivity and absence of TGEV reactivity in the enterocytes lining the ileum in ANPEP null pigs. The different receptor requirements for TGEV and PEDV have important implications in the development of new genetic tools for the control of enteric disease in pigs. [ABSTRACT FROM AUTHOR]

Published

2019

28. Structural Adaptations of Norovirus GII.17/13/21 Lineage through Two Distinct Evolutionary Paths.

Author

Ying Qian, Song, Mohan, Xi Jiang, Ming Xia, Meller, Jarek, Ming Tan, Yutao Chen, Xuemei Li, and Zihe Rao

Subjects

*NOROVIRUSES, *GASTROENTERITIS, *VIRAL antigens, *DISEASE susceptibility, *GLYCANS

Abstract

Human noroviruses (huNoVs), which cause epidemic acute gastroenteritis, recognize histo-blood group antigens (HBGAs) as host attachment factors affecting host susceptibility. HuNoVs are genetically diverse, containing at least 31 genotypes in the two major genogroups (genogroup I [GI] and GII). Three GII genotypes, GII genotype 17 (GII.17), GII.13, and GII.21, form a unique genetic lineage, in which the GII.17 genotype retains the conventional GII HBGA binding site (HBS), while the GII.13/21 genotypes acquire a completely new HBS. To understand the molecular bases behind these evolutionary changes, we solved the crystal structures of the HBGA binding protruding domains of (i) an early GII.17 variant (the 1978 variant) that does not bind or binds weakly to HBGAs, (ii) the new GII.17 variant (the 2014/15 variant) that binds A/B/H antigens strongly via an optimized GII HBS, and (iii) a GII.13 variant (the 2010 variant) that binds the Lewis a (Lea) antigen via the new HBS. These serial, high-resolution structural data enable a comprehensive structural comparison to understand the evolutionary changes of the GII.17/13/21 lineage, including the emergence of the new HBS of the GII.13/21 sublineage and the possible HBS optimization of the recent GII.17 variant for an enhanced HBGA binding ability. Our study elucidates the structural adaptations of the GII.17/13/21 lineage through distinct evolutionary paths, which may allow a theory explaining huNoV adaptations and evolutions to be put forward. IMPORTANCE Our understanding of the molecular bases behind the interplays between human noroviruses and their host glycan ligands, as well as their evolutionary changes over time with alterations in their host ligand binding capability and host susceptibility, remains limited. By solving the crystal structures of the glycan ligand binding protruding (P) domains with or without glycan ligands of three representative noroviruses of the GII.17/13/21 genetic lineage, we elucidated the molecular bases of the human norovirus-glycan interactions of this special genetic lineage. We present solid evidence on how noroviruses of this genetic lineage evolved via different evolutionary paths to (i) optimize their glycan binding site for higher glycan binding function and (ii) acquire a completely new glycan binding site for new ligands. Our data shed light on the mechanism of the structural adaptations of human noroviruses through different evolutionary paths, facilitating our understanding of human norovirus adaptations, evolutions, and epidemiology. [ABSTRACT FROM AUTHOR]

Published

2019

29. Adenovirus and the Cornea: More Than Meets the Eye

Author

Jaya Rajaiya, Amrita Saha, Ashrafali M. Ismail, Xiaohong Zhou, Ting Su, and James Chodosh

Subjects

adenovirus, epidemic keratoconjunctivitis, human corneal epithelium, viral receptor, Microbiology, QR1-502

Abstract

Human adenoviruses cause disease at multiple mucosal sites, including the respiratory, gastrointestinal, and genitourinary tracts, and are common agents of conjunctivitis. One site of infection that has received sparse attention is the cornea, a transparent tissue and the window of the eye. While most adenovirus infections are self-limited, corneal inflammation (keratitis) due to adenovirus can persist or recur for months to years after infection, leading to reduced vision, discomfort, and light sensitivity. Topical corticosteroids effectively suppress late adenovirus keratitis but are associated with vision-threatening side effects. In this short review, we summarize current knowledge on infection of the cornea by adenoviruses, including corneal epithelial cell receptors and determinants of corneal tropism. We briefly discuss mechanisms of stromal keratitis due to adenovirus infection, and review an emerging therapy to mitigate adenovirus corneal infections based on evolving knowledge of corneal epithelial receptor usage.

Published

2021

30. Single-Molecule Super-Resolution Imaging of T-Cell Plasma Membrane CD4 Redistribution upon HIV-1 Binding

Author

Yue Yuan, Caron A. Jacobs, Isabel Llorente Garcia, Pedro M. Pereira, Scott P. Lawrence, Romain F. Laine, Mark Marsh, and Ricardo Henriques

Subjects

HIV-1 entry, viral receptor, nanoscale cluster, super-resolution microscopy, CD4, STORM, Microbiology, QR1-502

Abstract

The first step of cellular entry for the human immunodeficiency virus type-1 (HIV-1) occurs through the binding of its envelope protein (Env) with the plasma membrane receptor CD4 and co-receptor CCR5 or CXCR4 on susceptible cells, primarily CD4+ T cells and macrophages. Although there is considerable knowledge of the molecular interactions between Env and host cell receptors that lead to successful fusion, the precise way in which HIV-1 receptors redistribute to sites of virus binding at the nanoscale remains unknown. Here, we quantitatively examine changes in the nanoscale organisation of CD4 on the surface of CD4+ T cells following HIV-1 binding. Using single-molecule super-resolution imaging, we show that CD4 molecules are distributed mostly as either individual molecules or small clusters of up to 4 molecules. Following virus binding, we observe a local 3-to-10-fold increase in cluster diameter and molecule number for virus-associated CD4 clusters. Moreover, a similar but smaller magnitude reorganisation of CD4 was also observed with recombinant gp120. For one of the first times, our results quantify the nanoscale CD4 reorganisation triggered by HIV-1 on host CD4+ T cells. Our quantitative approach provides a robust methodology for characterising the nanoscale organisation of plasma membrane receptors in general with the potential to link spatial organisation to function.

Published

2021

31. Viral Infections and Sphingolipids

Author

Schneider-Schaulies, Jürgen, Schneider-Schaulies, Sibylle, Gulbins, Erich, editor, and Petrache, Irina, editor

Published

2013

32. Na+-Taurocholate Co-Transporting Polypeptide (NTCP) in Livers, Function, Expression Regulation, and Potential in Hepatitis B Treatment

Author

Xiaoyu Zhao, Xiaoling Zhou, Pingnan Sun, and Waqas Iqbal

Subjects

Medicine (General), Cirrhosis, business.industry, viruses, virus diseases, NTCP, Hepatitis B, medicine.disease, digestive system, Virology, digestive system diseases, Virus, Solute carrier family, R5-920, Viral Receptor, Hepatocellular carcinoma, HBV, Medicine, Hepatitis D virus, business, Receptor, anti-HBV drugs

Abstract

Chronic hepatitis B virus (HBV) infection has become one of the leading causes of liver cirrhosis and hepatocellular carcinoma globally. The discovery of sodium taurocholate co-transporting polypeptide (NTCP), a solute carrier, as a key receptor for HBV and hepatitis D virus (HDV) has opened new avenues for HBV treatment. Additionally, it has led researchers to generate hepatoma cell lines (including HepG2-NTCP and Huh-7-NTCP) susceptible to HBV infection in vitro, hence, paving the way to develop and efficiently screen new and novel anti-HBV drugs. This review summarizes the history, function and critical findings regarding NTCP as a viral receptor for HBV/HDV, and it also discusses recently developed drugs targeting NTCP.

Published

2021

33. Diversity of ACE2 and its interaction with SARS-CoV-2 receptor binding domain

Author

Ruiqi Huang, Jessie Low-Gan, Gabrielle Warner, Abigail Kelley, Duncan McGregor, and Vaughn V. Smider

Subjects

Coronavirus disease 2019 (COVID-19), Sequence analysis, viruses, Severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2), Protein domain, Hamster, Plasma protein binding, Biology, medicine.disease_cause, Horseshoe bat, Biochemistry, Article, Virus, Homology (biology), Mice, Dogs, Protein Domains, Species Specificity, medicine, Animals, Humans, Molecular Biology, Coronavirus, Genetics, SARS-CoV-2, fungi, COVID-19, Cell Biology, Entry into host, biology.organism_classification, Receptor–ligand kinetics, Viral Tropism, Viral Receptor, Spike Glycoprotein, Coronavirus, Cats, Tissue tropism, Angiotensin-Converting Enzyme 2, hormones, hormone substitutes, and hormone antagonists, Protein Binding

Abstract

COVID-19, the clinical syndrome caused by the SARS-CoV-2 virus, has rapidly spread globally causing tens of millions of infections and over a million deaths. The potential animal reservoirs for SARS-CoV-2 are currently unknown, however sequence analysis has provided plausible potential candidate species. SARS-CoV-2 binds to the angiotensin I converting enzyme 2 (ACE2) to enable its entry into host cells and establish infection. We analyzed the binding surface of ACE2 from several important animal species to begin to understand the parameters for the ACE2 recognition by the SARS-CoV-2 spike protein receptor binding domain (RBD). We employed Shannon entropy analysis to determine the variability of ACE2 across its sequence and particularly in its RBD interacting region, and assessed differences between various species’ ACE2 and human ACE2. As cattle are a known reservoir for coronaviruses with previous human zoonotic transfer, and has a relatively divergent ACE2 sequence, we compared the binding kinetics of bovine and human ACE2 to SARS-CoV-2 RBD. This revealed a nanomolar binding affinity for bovine ACE2 but an approximate ten-fold reduction of binding compared to human ACE2. Since cows have been experimentally infected by SARS-CoV-2, this lower affinity sets a threshold for sequences with lower homology to human ACE2 to be able to serve as a productive viral receptor for SARS-CoV-2.

Published

2021

34. Emergence and Re-emergence of Human Coronaviruses: Spike Protein as the Potential Molecular Switch and Pharmaceutical Target

Author

Mohammad Amjad Kamal, Babu L. Tekwani, and Fahim Ahmad

Subjects

Pharmacology, Genetics, SARS-CoV-2, viruses, COVID-19, Virulence, Outbreak, Disease, Biology, Phenotype, Virus, Pharmaceutical Preparations, Viral entry, Viral Receptor, Spike Glycoprotein, Coronavirus, Drug Discovery, Animals, Humans, Prospective Studies, Gene

Abstract

Background: Recent emergence of COVID-19 caused by a new human coronavirus (CoV) strain (SARS-CoV-2), which originated from China, poses the future emergence of additional CoVs. In most of the cases of emergence of human CoVs, bats, palm civets, raccoon dogs and camels have been identified as the sources of human infections and as reservoir hosts. A review of comparative genomic and phenotypic characteristics of human CoV strains vis-à-vis their comparison with the corresponding animal isolates shall provide clues regarding the potential genomic, phenotypic and molecular factors responsible for host-switching, which may lead to prospective emergence and re-emergence of human CoV outbreaks in the future. Methods: The seven known human strains of CoV were analyzed for the host and viral factors responsible for human outbreaks. The molecular factors responsible for host-susceptibility, virulence and pathogenesis were reviewed to predict the emergence and re-emergence of additional human CoV strains. CoV spike protein was evaluated as a potential viral receptor for host switching and the target for pharmaceutical design. Results: A review of the factors associated with host-susceptibility, virulence and pathogenesis of seven known human CoV strains presents significant possibilities for the emergence of new CoV strain(s), leading to more human outbreaks. Continuous exposure of animals’ handlers to the infected animals, environmental changes, improper sanitations, non-disposal of the solid waste and resumption of exotic animals markets provides favorable conditions for “host switching” and the emergence of new and potentially more virulent human CoV strains. Mutations in target genes (like spike protein), which facilitate the viral entry into the host-cells, provide a potential “molecular switch” for preferences of new host-receptors, genetic diversity, genetic-recombination and high virulence. Additionally, the clinical and environmental factors, asymptomatic carriers, the paucity of efficacious vaccines & therapeutics, inefficient disease management and infection control measures, lack of public awareness, and effective communication of information about more virulent human-adapted virus isolates are critical for the emergence of new and virulent SARS-CoV strains with high mortality and varied incubation period in the near future. Small molecules binding with conserved druggable regions of the CoV spike proteins may be effective against multiple strains of CoVs. Conclusions: High propensity of mutations and “molecular adaptations” in coronaviruses creates the hot spots and high potential for “host switching”, leading to the emergence of more virulent strains of human CoVs. The public/global health agencies, medical communities and research scientists should be prepared for the emergence and re-emergence of new human CoV strain(s) leading to potential disease outbreaks. The inhibitors binding with conserved druggable regions of spike proteins from multiple strains CoV may have utility as broad-spectrum antiviral drugs to combat future emergence of CoVs.

Published

2021

35. Avian influenza A viruses exhibit plasticity in sialylglycoconjugate receptor usage in human lung cells.

Author

Liang C-Y, Huang I, Han J, Sownthirarajan B, Kulhankova K, Murray NB, Taherzadeh M, Archer-Hartmann S, Pepi L, Manivasagam S, Plung J, Sturtz M, Yu Y, Vogel OA, Kandasamy M, Gourronc FA, Klingelhutz AJ, Choudhury B, Rong L, Perez JT, Azadi P, McCray PB Jr, Neelamegham S, and Manicassamy B

Subjects

Animals, Humans, Carrier Proteins metabolism, Glycoconjugates metabolism, N-Acetylneuraminic Acid metabolism, Polysaccharides metabolism, Sugars metabolism, Influenza in Birds metabolism, Receptors, Virus metabolism, Influenza A virus metabolism, Influenza, Human, Lung virology, Receptors, Cell Surface metabolism

Abstract

Importance: It is well known that influenza A viruses (IAV) initiate host cell infection by binding to sialic acid, a sugar molecule present at the ends of various sugar chains called glycoconjugates. These sugar chains can vary in chain length, structure, and composition. However, it remains unknown if IAV strains preferentially bind to sialic acid on specific glycoconjugate type(s) for host cell infection. Here, we utilized CRISPR gene editing to abolish sialic acid on different glycoconjugate types in human lung cells, and evaluated human versus avian IAV infections. Our studies show that both human and avian IAV strains can infect human lung cells by utilizing any of the three major sialic acid-containing glycoconjugate types, specifically N-glycans, O-glycans, and glycolipids. Interestingly, simultaneous elimination of sialic acid on all three major glycoconjugate types in human lung cells dramatically decreased human IAV infection, yet had little effect on avian IAV infection. These studies show that avian IAV strains effectively utilize other less prevalent glycoconjugates for infection, whereas human IAV strains rely on a limited repertoire of glycoconjugate types. The remarkable ability of avian IAV strains to utilize diverse glycoconjugate types may allow for easy transmission into new host species., Competing Interests: The authors declare no conflict of interest.

Published

2023

36. A bioengineered pseudovirus nanoparticle displaying SARS-CoV 2 RBD fully protects mice from mortality and weight loss caused by SARS-CoV 2 challenge.

Author

Xia M, López K, Vago FS, Huang P, Auguste DI, Jiang W, Auguste AJ, and Tan M

Subjects

Animals, Humans, Mice, SARS-CoV-2 genetics, COVID-19 Vaccines genetics, Pandemics, Weight Loss, COVID-19 prevention & control, Nanoparticles

Abstract

The COVID-19 pandemic caused by severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2) has caused considerable morbidity and mortality worldwide. Although authorized COVID-19 vaccines have been shown highly effective, their significantly lower efficacy against heterologous variants, and the rapid decrease of vaccine-elicited immunity raises serious concerns, calling for improved vaccine tactics. To this end, a pseudovirus nanoparticle (PVNP) displaying the receptor binding domains (RBDs) of SARS-CoV-2 spike, named S-RBD, was generated and shown it as a promising COVID-19 vaccine candidate. The S-RBD PVNP was produced using both prokaryotic and eukaryotic systems. A 3D structural model of the S-RBD PVNPs was built based on the known structures of the S 60 particle and RBDs, revealing an S 60 particle-based icosahedral symmetry with multiple surface-displayed RBDs that retain authentic conformations and receptor-binding functions. The PVNP is highly immunogenic, eliciting high titers of RBD-specific IgG and neutralizing antibodies in mice. The S-RBD PVNP demonstrated exceptional protective efficacy, and fully (100%) protected K18-hACE2 mice from mortality and weight loss after a lethal SARS-CoV-2 challenge, supporting the S-RBD PVNPs as a potent COVID-19 vaccine candidate. By contrast, a PVNP displaying the N-terminal domain (NTD) of SARS-CoV-2 spike exhibited only 50% protective efficacy. Since the RBD antigens of our PVNP vaccine are adjustable as needed to address the emergence of future variants, and various S-RBD PVNPs can be combined as a cocktail vaccine for broad efficacy, these non-replicating PVNPs offer a flexible platform for a safe, effective COVID-19 vaccine with minimal manufacturing cost and time., (© 2023 The Authors. Biotechnology Journal published by Wiley-VCH GmbH.)

Published

2023

37. Amino acid variation at VP1-145 of Enterovirus A71 determines the viral infectivity and receptor usage in a primary human intestinal model

Author

Aknouch, Ikrame, García-Rodríguez, Inés, Giugliano, Francesca, Calitz, Carlemi, Koen, Gerrit, van Eijk, Hetty, Johannesson, Nina, Rebers, Sjoerd, Brouwer, Lieke, Muncan, Vanesa, Stittelaar, Koert, Pajkrt, Dasja, Wolthers, Katja, Sridhar, Adithya, Medical Microbiology and Infection Prevention, Graduate School, AII - Infectious diseases, AGEM - Amsterdam Gastroenterology Endocrinology Metabolism, Tytgat Institute for Liver and Intestinal Research, Paediatric Infectious Diseases / Rheumatology / Immunology, and ARD - Amsterdam Reproduction and Development

Subjects

Microbiology (medical), heparin sulfate proteoglycan, viruses, Enterovirus A71, Transwell, VP1-145, Heparan sulfate, Microbiology, EV-A71, Organoids, polarized epithelium, Viral receptor, human inestinal organoids

Abstract

Enterovirus A71 (EV-A71) can elicit a wide variety of human diseases such as hand, foot, and mouth disease and severe or fatal neurological complications. It is not clearly understood what determines the virulence and fitness of EV-A71. It has been observed that amino acid changes in the receptor binding protein, VP1, resulting in viral binding to heparan sulfate proteoglycans (HSPGs) may be important for the ability of EV-A71 to infect neuronal tissue. In this study, we identified that the presence of glutamine, as opposed to glutamic acid, at VP1-145 is key for viral infection in a 2D human fetal intestinal model, consistent with previous findings in an airway organoid model. Moreover, pre-treatment of EV-A71 particles with low molecular weight heparin to block HSPG-binding significantly reduced the infectivity of two clinical EV-A71 isolates and viral mutants carrying glutamine at VP1-145. Our data indicates that mutations in VP1 leading to HSPG-binding enhances viral replication in the human gut. These mutations resulting in increased production of viral particles at the primary replication site could lead to a higher risk of subsequent neuroinfection.ImportanceWith the near eradication of polio worldwide, polio-like illness (as is increasingly caused by EV-A71 infections) is of emerging concern. EV-A71 is indeed the most neurotropic enterovirus that poses a major threat globally to public health and specifically in infants and young children. Our findings will contribute to the understanding of the virulence and the pathogenicity of this virus. Further, our data also supports the identification of potential therapeutic targets against severe EV-A71 infection especially among infants and young children. Furthermore, our work highlights the key role of HSPG-binding mutations in the disease outcome of EV-A71. Additionally, EV-A71 is not able to infect the gut (the primary replication site in humans) in traditionally used animal models. Thus, our research highlights the need for human-based models to study human viral infections.

Published

2022

38. The p.Ser267Phe variant of sodium taurocholate cotransporting polypeptide (NTCP) supports HBV infection with a low efficiency.

Author

Liu, Chenxuan, Xu, Guangwei, Gao, Zhenchao, Zhou, Zhongmin, Guo, Guilan, Li, Dan, Jing, Zhiyi, Sui, Jianhua, and Li, Wenhui

Subjects

*SINGLE nucleotide polymorphisms, *TAUROCHOLIC acid, *CHRONIC hepatitis B, *GENETIC mutation, *POLYPEPTIDES, *GENETICS

Abstract

Sodium taurocholate cotransporting polypeptide (NTCP) is a functional receptor for human hepatitis B virus (HBV) and its satellite virus Hepatitis D virus (HDV). Physiologically, NTCP is responsible for the majority of sodium-dependent bile acids uptake by hepatocytes. The p.Ser267Phe (S267F) variant of NTCP is a single nucleotide polymorphism (SNP) previously found to cause substantial loss of ability to support HBV and HDV infection and its taurocholic acid uptake function in vitro . Intriguingly, ten individuals were identified as S267F homozygotes in population studies of chronic hepatitis B (CHB) patients. In this study, we identified new HBV isolates from one homozygous S267F mutation carrier and confirmed new isolates also use wildtype-NTCP as a cellular receptor. Furthermore, we demonstrated S267F variant of NTCP, though inefficient, is still a functional receptor for HBV entry. This study advances our understanding of NTCP-mediated HBV infection. [ABSTRACT FROM AUTHOR]

Published

2018

39. Immunohistochemical and qPCR Detection of SARS-CoV-2 in the Human Middle Ear Versus the Nasal Cavity: Case Series

Author

Adam S. DeConde, Kwang Pak, Arwa Kurabi, Allen F. Ryan, and Carol H. Yan

Subjects

Nasal cavity, Pathology, medicine.medical_specialty, Middle ear, Ear, Middle, Case Reports, medicine.disease_cause, Pathology and Forensic Medicine, chemistry.chemical_compound, otorhinolaryngologic diseases, medicine, Humans, Coronavirus, SARS-CoV-2, business.industry, COVID-19, Epithelial cell adhesion molecule, Immunohistochemistry, Epithelium, qPCR, medicine.anatomical_structure, Otitis, Oncology, Otorhinolaryngology, chemistry, Viral Receptor, Angiotensin-Converting Enzyme 2, Nasal Cavity, medicine.symptom, business, Viral load

Abstract

Viral infections have already been implicated with otitis media and sudden sensorineural hearing loss. However, the pathophysiology of COVID-19 as it relates to otologic disorders is not well-defined. With the spread of SARS-CoV-2, it is important to evaluate its colonization of middle ear mucosa. Middle ear and nasal tissue samples for quantitative RT-PCR and histologic evaluations were obtained from post-mortem COVID-19 patients and non-diseased control patients. Here we present evidence that SARS-CoV-2 colonizes the middle ear epithelium and co-localizes with the primary viral receptor, angiotensin-converting enzyme 2 (ACE2). Both middle ear and nasal epithelial cells show relatively high expression of ACE2, required for SARS-CoV-2 entry. The epithelial cell adhesion molecule (EpCAM) was use as a biomarker of epithelia. Furthermore, we found that the viral load in the middle ear is lower than that present in the nasal cavity.

Published

2021

40. ACE2 and TMPRSS2 Expression in Hepatocytes of Chronic HBV Infection Patients

Author

Yao-Xiang Lin, Jing Wu, Xiang-Ji Wu, Xiao-Ben Pan, Xiao-Xiao Hu, Hui Ma, Gong-Yin Chen, Sheng-Zhang Lin, and Yan-Xiu Ma

Subjects

chemistry.chemical_classification, Serine protease, biology, SARS-CoV-2, business.industry, viruses, ACE2, medicine.disease, TMPRSS2, Transmembrane protein, Liver disease, Enzyme, chemistry, Viral Receptor, Hepatocellular carcinoma, Immunology, biology.protein, Medicine, Original Article, Risk factor, business, hormones, hormone substitutes, and hormone antagonists, Liver diseases

Abstract

Background: Pre-existing liver disease is a risk factor for the worse prognosis of severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2) infection. We aimed to evaluate whether chronic hepatitis B (CHB) and hepatocellular carcinoma (HCC) affect the expression of viral receptor angiotensin-converting enzyme 2 (ACE2) and transmembrane serine protease 2 (TMPRSS2) in the liver. Methods: Twelve pairs of matched liver tissues of HCC and para-carcinoma were collected from the First Affiliated Hospital of Zhejiang University School of Medicine. And 20 liver biopsies from CHB patients were collected from Peking University People's Hospital. The expression of ACE2 and TMRPSS2 were detected using immunofluorescence staining, western blot, and RT-qPCR. The effects of hepatitis B virus (HBV) replication or interferon on ACE2 and TMPRSS2 expression were tested in hepatic cell lines. Results: The mRNA expression of TMPRSS2 in HCC tissues was six-fold higher than that of para-carcinoma tissues (P = 0.002), whereas that of ACE2 was not statistically different between HCC and para-carcinoma tissues. Hepatocellular ACE2 expression was detected in 35% (7/20) of CHB patients and mostly distributed in the inflammatory areas. However, there was no difference in TMPRSS2 expression between areas with or without inflammation. IFN-α2b slightly induced ACE2 expression (2.4-fold, P = 0.033) in HepG2 cells but not in Huh-7, QSG-7701, and L-02 cells. IFN-α2b did not affect TMPRSS2 expression in these cell lines. In addition, HBV replication did not alter ACE2 expression in HepAD38 cells. Conclusions: Although HBV replication does not directly affect the expression of ACE2 and TMPRSS2, intrahepatic inflammation and carcinogenesis may increase their expression in some patients, which, in turn, may facilitate SARS-CoV-2 infection in hepatocytes.

Published

2021

41. Rapid seroconversion and persistent functional IgG antibodies in severe COVID-19 patients correlates with an IL-12p70 and IL-33 signature

Author

Michael Mor, Ariel Munitz, Michal Itan, Michal Stein, Shaul Lev, Moran G. Goren, Liat Edry-Botzer, Udi Qimron, Ran Tur-Kaspa, Natalia T. Freund, Dani Cohen, Motti Gerlic, Yariv Wine, Dror Dicker, Tamar Gottesman, D. Marcoviciu, and Khitam Muhsen

Subjects

0301 basic medicine, Science, Disease, Severity of Illness Index, Article, 03 medical and health sciences, 0302 clinical medicine, Antigen, Severity of illness, Medicine, Humans, Seroconversion, Multidisciplinary, biology, business.industry, COVID-19, Interleukin-33, Interleukin-12, 3. Good health, Interleukin 33, 030104 developmental biology, Viral Receptor, Viral infection, 030220 oncology & carcinogenesis, Immunoglobulin G, Immunology, Antibody Formation, biology.protein, Infectious diseases, Antibody, business, Binding domain

Abstract

Despite ongoing efforts to characterize the host response toward SARS-CoV-2, a major gap in our knowledge still exists regarding the magnitude and duration of the humoral response. Analysis of the antibody response in mild versus moderate/severe patients, using our new developed quantitative electrochemiluminescent assay for detecting IgM/IgA/IgG antibodies toward SARS-CoV-2 antigens, revealed a rapid onset of IgG/IgA antibodies, specifically in moderate/severe patients. IgM antibodies against the viral receptor binding domain, but not against nucleocapsid protein, were detected at early stages of the disease. Furthermore, we observed a marked reduction in IgM/IgA antibodies over-time. Adapting our assay for ACE2 binding-competition, demonstrated that the presence of potentially neutralizing antibodies is corelated with IgG/IgA. Finally, analysis of the cytokine profile in COVID-19 patients revealed unique correlation of an IL-12p70/IL33 and IgG seroconversion, which correlated with disease severity. In summary, our comprehensive analysis has major implications on the understanding and monitoring of SARS-CoV-2 infections.

Published

2021

42. Docked severe acute respiratory syndrome coronavirus 2 proteins within the cutaneous and subcutaneous microvasculature and their role in the pathogenesis of severe coronavirus disease 2019

Author

A. Neil Crowson, J. Justin Mulvey, Steven P. Salvatore, Cynthia M. Magro, Jeffrey Laurence, Andrew J. Dannenberg, Gerard J. Nuovo, Surya V. Seshan, and Joanna Harp

Subjects

Adult, Male, 0301 basic medicine, skin, Pathology, medicine.medical_specialty, Viral protein, viruses, ACE2, Peptidyl-Dipeptidase A, medicine.disease_cause, Pathology and Forensic Medicine, Pathogenesis, 03 medical and health sciences, 0302 clinical medicine, Atypical hemolytic uremic syndrome, medicine, Humans, complement, Receptor, Complement Activation, Aged, deltoid biopsy, medicine.diagnostic_test, SARS-CoV-2, business.industry, COVID-19, Endothelial Cells, Original Contribution, Middle Aged, medicine.disease, Complement system, Endothelial stem cell, 030104 developmental biology, Viral Receptor, 030220 oncology & carcinogenesis, Microvessels, Skin biopsy, RNA, Viral, Female, Angiotensin-Converting Enzyme 2, business

Abstract

The purpose of this study was to examine the deltoid skin biopsy in twenty-three patients with coronavirus disease 2019 (COVID-19), most severely ill, for vascular complement deposition and correlate this with severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2) viral RNA and protein localization and ACE2 expression. Deltoid skin microvascular complement screening has been applied to patients with various systemic complement-mediated microvascular syndromes, best exemplified by atypical hemolytic uremic syndrome. In 21 of 23 cases, substantial microvascular deposition of complement components was identified. The two patients without significant complement deposition included one patient with moderate disease and a severely ill patient who although on a ventilator for a day was discharged after 3 days. The dominant microvascular complement immunoreactant identified was the terminal membranolytic attack complex C5b-9. Microvascular complement deposition strongly colocalized in situ with the SARS-CoV-2 viral proteins including spike glycoproteins in the endothelial cells as well as the viral receptor ACE2 in lesional and nonlesional skin; viral RNA was not evident. Microvascular SARS-CoV-2 viral protein, complement, and ACE2 expression was most conspicuous in the subcutaneous fat. Although the samples from severely ill patients with COVID-19 were from grossly normal skin, light microscopically focal microvascular abnormalities were evident that included endothelial cell denudement, basement membrane zone reduplication, and small thrombi. It is concluded that complement activation is common in grossly normal skin, especially in the subcutaneous fat which may provide a link between severe disease and obesity, in people with severe COVID-19, and the strong colocalization with the ACE2 receptor and viral capsid proteins without viral RNA suggests that circulating viral proteins (ie, pseudovirions) may dock onto the endothelial of these microvessels and induce complement activation.

Published

2020

43. Adeno-associated Virus (AAV) Serotypes Have Distinctive Interactions with Domains of the Cellular AAV Receptor.

Author

Pillay, Sirika, Wei Zou, Fang Cheng, Puschnik, Andreas S., Meyer, Nancy L., Ganaie, Safder S., Xuefeng Deng, Wosen, Jonathan E., Davulcu, Omar, Ziying Yan, Engelhardt, John F., Brown, Kevin E., Chapman, Michael S., Jianming Qiu, and Carette, Jan E.

Subjects

*ADENO-associated virus, *SEROTYPES, *PRIONS, *GLYCANS, *VIRAL receptors

Abstract

Adeno-associated virus (AAV) entry is determined by its interactions with specific surface glycans and a proteinaceous receptor(s). Adeno-associated virus receptor (AAVR) (also named KIAA0319L) is an essential cellular receptor required for the transduction of vectors derived from multiple AAV serotypes, including the evolutionarily distant serotypes AAV2 and AAV5. Here, we further biochemically characterize the AAV-AAVR interaction and define the domains within the ectodomain of AAVR that facilitate this interaction. By using a virus overlay assay, it was previously shown that the major AAV2 binding protein in membrane preparations of human cells corresponds to a glycoprotein with a molecular mass of 150 kDa. By establishing a purification procedure, performing further protein separation by two-dimensional electrophoresis, and utilizing mass spectrometry, we now show that this glycoprotein is identical to AAVR. While we find that AAVR is an N-linked glycosylated protein, this glycosylation is not a strict requirement for AAV2 binding or functional transduction. Using a combination of genetic complementation with deletion constructs and virus overlay assays with individual domains, we find that AAV2 functionally interacts predominantly with the second Ig-like polycystic kidney disease (PKD) repeat domain (PKD2) present in the ectodomain of AAVR. In contrast, AAV5 interacts primarily through the first, most membrane-distal, PKD domain (PKD1) of AAVR to promote transduction. Furthermore, other AAV serotypes, including AAV1 and -8, require a combination of PKD1 and PKD2 for optimal transduction. These results suggest that despite their shared dependence on AAVR as a critical entry receptor, different AAV serotypes have evolved distinctive interactions with the same receptor. [ABSTRACT FROM AUTHOR]

Published

2017

44. Three cysteine residues of SLC52A1, a receptor for the porcine endogenous retrovirus-A (PERV-A), play a critical role in cell surface expression and infectivity.

Author

Colon-Moran, Winston, Argaw, Takele, and Wilson, Carolyn A.

Subjects

*ENDOGENOUS retroviruses, *XENOTRANSPLANTATION, *CYSTEINE, *ZOONOSES, *ANTISENSE DNA, *GLYCOSYLATION, *PREVENTION

Abstract

Porcine endogenous retrovirus-A (PERV-A), a gammaretrovirus, infects human cells in vitro, thus raising the potential risk of cross-species transmission in xenotransplantation. Two members of the solute carrier family 52 (SLC52A1 and SLC52A2) are PERV-A receptors. Site-directed mutagenesis of the cDNA encoding SLC52A1 identified that only one of two putative glycosylation signals is occupied by glycans. In addition, we showed that glycosylation of SLC52A1 is not necessary for PERV-A receptor function. We also identified that at a minimum, three cysteine residues are sufficient for SLC52A1 cell surface expression. Mutation of cysteine at position 365 and either of the two cysteine residues in the C-terminal tail at positions 442 or 446 reduced SLC52A1 surface expression and PERV-A infection suggesting that these residues may contribute to overall structural stability and receptor function. Understanding interactions between PERV-A and its cellular receptor may provide novel strategies to prevent zoonotic infection in the setting of xenotransplantation. [ABSTRACT FROM AUTHOR]

Published

2017

45. Beyond attachment: Roles of DC-SIGN in dengue virus infection.

Author

Liu, Ping, Ridilla, Marc, Patel, Pratik, Betts, Laurie, Gallichotte, Emily, Shahidi, Lidea, Thompson, Nancy L., and Jacobson, Ken

Subjects

*DENGUE, *DIAGNOSIS of fever, *CELL adhesion, *INTEGRINS, *CELL membranes, *MUTANT proteins

Abstract

Dendritic cell-specific intercellular adhesion molecule-3-grabbing non-integrin ( DC-SIGN), a C-type lectin expressed on the plasma membrane by human immature dendritic cells, is a receptor for numerous viruses including Ebola, SARS and dengue. A controversial question has been whether DC-SIGN functions as a complete receptor for both binding and internalization of dengue virus ( DENV) or whether it is solely a cell surface attachment factor, requiring either hand-off to another receptor or a co-receptor for internalization. To examine this question, we used 4 cell types: human immature dendritic cells and NIH3T3 cells expressing either wild-type DC-SIGN or 2 internalization-deficient DC-SIGN mutants, in which either the 3 cytoplasmic internalization motifs are silenced by alanine substitutions or the cytoplasmic region is truncated. Using confocal and super-resolution imaging and high content single particle tracking, we investigated DENV binding, DC-SIGN surface transport, endocytosis, as well as cell infectivity. DC-SIGN was found colocalized with DENV inside cells suggesting hand-off at the plasma membrane to another receptor did not occur. Moreover, all 3 DC-SIGN molecules on NIH3T3 cells supported cell infection. These results imply the involvement of a co-receptor because cells expressing the internalization-deficient mutants could still be infected. [ABSTRACT FROM AUTHOR]

Published

2017

46. Structures of Echovirus 30 in complex with its receptors inform a rational prediction for enterovirus receptor usage

Author

Lunbiao Cui, Zihe Rao, Xin Zhao, Weiwei Zhai, Xiangxi Wang, Minhao Li, Yao Sun, Ling Zhu, Fengcai Zhu, Li Zhang, Kang Wang, and George F. Gao

Subjects

0301 basic medicine, Echovirus, Science, In silico, viruses, General Physics and Astronomy, Antigen-Antibody Complex, Receptors, Fc, 02 engineering and technology, Computational biology, Biology, medicine.disease_cause, Biochemistry, Article, General Biochemistry, Genetics and Molecular Biology, Epitope, Epitopes, 03 medical and health sciences, Antigen, Virology, Electron microscopy, medicine, Humans, Receptor, lcsh:Science, Antigens, Viral, Tropism, Multidisciplinary, CD55 Antigens, Cryoelectron Microscopy, Virion, General Chemistry, 021001 nanoscience & nanotechnology, Enterovirus B, Human, 030104 developmental biology, Viral Receptor, Enterovirus, lcsh:Q, 0210 nano-technology

Abstract

Receptor usage that determines cell tropism and drives viral classification closely correlates with the virus structure. Enterovirus B (EV-B) consists of several subgroups according to receptor usage, among which echovirus 30 (E30), a leading causative agent for human aseptic meningitis, utilizes FcRn as an uncoating receptor. However, receptors for many EVs remain unknown. Here we analyzed the atomic structures of E30 mature virion, empty- and A-particles, which reveals serotype-specific epitopes and striking conformational differences between the subgroups within EV-Bs. Of these, the VP1 BC loop markedly distinguishes E30 from other EV-Bs, indicative of a role as a structural marker for EV-B. By obtaining cryo-electron microscopy structures of E30 in complex with its receptor FcRn and CD55 and comparing its homologs, we deciphered the underlying molecular basis for receptor recognition. Together with experimentally derived viral receptor identifications, we developed a structure-based in silico algorithm to inform a rational prediction for EV receptor usage., Echovirus 30 (E30) belongs to the Enterovirus-B group and causes aseptic meningitis in humans. Here, the authors present the cryo-EM structures of the E30 E-particle, A-particle and the mature virion, as well as structures of E30 in complex with its receptor FcRn and CD55, and furthermore they describe a structure-based algorithm that allows the prediction of EV receptor usage.

Published

2020

47. The constitutive activity of the viral-encoded G protein-coupled receptor US28 supports a complex signalling network contributing to cancer development

Author

Martine J. Smit, Bianca Plouffe, Carole A. Daly, Medicinal chemistry, and AIMMS

Subjects

Human cytomegalovirus, Chemokine, Protein Conformation, Cytomegalovirus, Biology, Biochemistry, Organelles & Localization, Molecular Bases of Health & Disease, 03 medical and health sciences, Chemokine receptor, 0302 clinical medicine, Viral Envelope Proteins, SDG 3 - Good Health and Well-being, GTP-Binding Proteins, US28, Neoplasms, medicine, Humans, cancer, Receptor, Review Articles, constitutive activity, 030304 developmental biology, G protein-coupled receptor, 0303 health sciences, signalling network, viral GCPR, chemokine receptor, medicine.disease, Therapeutics & Molecular Medicine, Signaling, Cell biology, Signalling, Lytic cycle, Viral Receptor, 030220 oncology & carcinogenesis, biology.protein, Signal Transduction

Abstract

US28 is a viral G protein-coupled receptor (GPCR) encoded by the human cytomegalovirus (HCMV). This receptor, expressed both during lytic replication and viral latency, is required for latency. US28 is binding to a wide variety of chemokines but also exhibits a particularly high constitutive activity robustly modulating a wide network of cellular pathways altering the host cell environment to benefit HCMV infection. Several studies suggest that US28-mediated signalling may contribute to cancer progression. In this review, we discuss the unique structural characteristics that US28 acquired through evolution that confer a robust constitutive activity to this viral receptor. We also describe the wide downstream signalling network activated by this constitutive activation of US28 and discuss how these signalling pathways may promote and support important cellular aspects of cancer.

Published

2020

48. Susceptibility of the Iranian population to severe acute respiratory syndrome coronavirus 2 infection based on variants of angiotensin I converting enzyme 2

Author

Hanieh Bagheri, Mohammad Yasaghi, Mohsen Ebrahimi, Naeme Javid, Fatemeh Sana Askari, Mana Zakeri, and Alireza Mohebbi

Subjects

0301 basic medicine, Population, Mutant, Single-nucleotide polymorphism, 030204 cardiovascular system & hematology, Biology, medicine.disease_cause, Virus, human angiotensin-converting enzyme 2, 03 medical and health sciences, 0302 clinical medicine, Virology, medicine, Missense mutation, natural resistance variant, education, chemistry.chemical_classification, education.field_of_study, Mutation, SARS-CoV-2, molecular docking, SARS-CoV-2 spike glycoprotein, 030104 developmental biology, chemistry, Viral Receptor, Glycoprotein, hormones, hormone substitutes, and hormone antagonists, Research Article

Abstract

Background: Variations in the viral receptor human angiotensin-converting enzyme 2 (ACE2) may specify the susceptibility of a certain population to severe acute respiratory syndrome coronavirus 2. Objective: Evaluation of the affinity of severe acute respiratory syndrome coronavirus 2 spike glycoprotein to the Iranian genetic variants of ACE2. Materials & methods: Single nucleotide polymorphisms of ACE2 among the Iranian population were collected from the Iranome database. Missense mutations in the N-terminal peptidase domain were selected for in silico analysis. Results: 17 missense single nucleotide polymorphisms were found at ACE2. Viral glycoprotein had the lowest affinity to ACE2 mutant V485L. Discussion: The V485L variant of ACE2 could be a natural resistance mutation among the Iranian population. In addition, variant S331F can increase slightly the susceptibility to infection with the virus.

Published

2020

49. The coxsackievirus and adenovirus receptor: virological and biological beauty

Author

Katherine J. D. A. Excoffon

Subjects

Coxsackie and Adenovirus Receptor-Like Membrane Protein, Adenoviridae Infections, viruses, Genetic enhancement, PDZ domain, Biophysics, Biology, Coxsackievirus, Biochemistry, Mice, 03 medical and health sciences, Structural Biology, Genetics, Animals, Humans, Protein Isoforms, Receptor, Molecular Biology, 030304 developmental biology, 0303 health sciences, 030302 biochemistry & molecular biology, Gene Expression Regulation, Developmental, Cell Biology, biology.organism_classification, Cell biology, Alternative Splicing, Swine Vesicular Disease Virus, Viral Receptor, Knockout mouse, Function (biology)

Abstract

The coxsackievirus and adenovirus receptor (CAR) is an essential multifunctional cellular protein that is only beginning to be understood. CAR serves as a receptor for many adenoviruses, human group B coxsackieviruses, swine vesicular disease virus, and possibly other viruses. While named for its function as a viral receptor, CAR is also involved in cell adhesion, immune cell activation, synaptic transmission, and signaling. Knockout mouse models were first to identify some of these biological functions; however, tissue-specific model systems have shed light on the complexity of different CAR isoforms and their specific activities. Many of these functions are mediated by the large number of interacting proteins described so far, and several new putative interactions have recently been discovered. As antiviral and gene therapy strategies that target CAR continue to emerge, future work poised to understand the biological implications of manipulating CAR in vivo is critical.

Published

2020

50. Discovery of potential multi-target-directed ligands by targeting host-specific SARS-CoV-2 structurally conserved main protease

Author

Rakesh Joshi, Sneha B. Bansode, Anita Chugh, Mahesh J. Kulkarni, Shounak S. Jagdale, S. Shiva Shankar, Vaibhav Kumar Pandya, Meenakshi B. Tellis, and Ashok P. Giri

Subjects

RdRp, viruses, medicine.medical_treatment, RNA-dependent RNA polymerase, SARS-CoV-2 virus, Computational biology, Biology, Ligands, medicine.disease_cause, protease inhibitor, multi-target-directed ligand, Structural Biology, medicine, Humans, Coronaviridae, Protease Inhibitors, Protease inhibitor (pharmacology), Pandemics, Molecular Biology, Phylogeny, MPro, Coronavirus, Protease, SARS-CoV-2, Drug discovery, COVID-19, General Medicine, hACE-2, biology.organism_classification, Pharmaceutical Preparations, Viral replication, Viral Receptor, Peptide Hydrolases, Research Article

Abstract

Severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2) infection has resulted in the current COVID-19 pandemic. Worldwide this disease has infected over 2.5 million individuals with a mortality rate ranging from 5 to 10%. There are several efforts going on in the drug discovery to control the SARS-CoV-2 viral infection. The main protease (MPro) plays a critical role in viral replication and maturation, thus can serve as the primary drug target. To understand the structural evolution of MPro, we have performed phylogenetic and Sequence Similarity Network analysis, that depicted divergence of Coronaviridae MPro in five clusters specific to viral hosts. This clustering was corroborated with the comparison of MPro structures. Furthermore, it has been observed that backbone and binding site conformations are conserved despite variation in some of the residues. These attributes can be exploited to repurpose available viral protease inhibitors against SARS-CoV-2 MPro. In agreement with this, we performed screening of ∼7100 molecules including active ingredients present in the Ayurvedic anti-tussive medicines, anti-viral phytochemicals and synthetic anti-virals against SARS-CoV-2 MPro as the primary target. We identified several natural molecules like δ-viniferin, myricitrin, taiwanhomoflavone A, lactucopicrin 15-oxalate, nympholide A, afzelin, biorobin, hesperidin and phyllaemblicin B that strongly binds to SARS-CoV-2 MPro. Intrestingly, these molecules also showed strong binding with other potential targets of SARS-CoV-2 infection like viral receptor human angiotensin-converting enzyme 2 (hACE-2) and RNA dependent RNA polymerase (RdRp). We anticipate that our approach for identification of multi-target-directed ligand will provide new avenues for drug discovery against SARS-CoV-2 infection. Communicated by Ramaswamy H. Sarma

Published

2020