Search

Your search keyword '"Sorrentino, James T."' showing total 23 results
Start Over Author "Sorrentino, James T."
23 results on '"Sorrentino, James T."'

1. Preparing glycomics data for robust statistical analysis with GlyCompareCT

Author

Zhang, Yujie, Krishnan, Sridevi, Bao, Bokan, Chiang, Austin WT, Sorrentino, James T, Schinn, Song-Min, Kellman, Benjamin P, and Lewis, Nathan E

Subjects
Bioinformatics, Molecular Biology, Systems Biology
Abstract

GlyCompareCT is a portable command-line tool to facilitate downstream glycomic data analyses, by addressing data inherent sparsity and non-independence. Inputting glycan abundances, users can run GlyCompareCT with one line of code to obtain the abundances of a minimal substructure set, named glycomotif, thereby quantifying hidden biosynthetic relationships between measured glycans. Optional parameters tuning and annotation are supported for personal preference. For complete details on the use and execution of this protocol, please refer to Bao et al. (2021).1.

Published
2023

2. Vascular Proteome Responses Precede Organ Dysfunction in a Murine Model of Staphylococcus aureus Bacteremia

Author

Sorrentino, James T, Golden, Gregory J, Morris, Claire, Painter, Chelsea D, Nizet, Victor, Campos, Alexandre Rosa, Smith, Jeffrey W, Karlsson, Christofer, Malmström, Johan, Lewis, Nathan E, Esko, Jeffrey D, and Toledo, Alejandro Gómez

Subjects
Hematology, Emerging Infectious Diseases, Infectious Diseases, Sepsis, Aetiology, 2.1 Biological and endogenous factors, Infection, Inflammatory and immune system, Mice, Humans, Animals, Staphylococcus aureus, Proteome, Multiple Organ Failure, Disease Models, Animal, Bacteremia, vascular glycocalyx, proteome, sepsis, DIA mass spectrometry, glycocalyx, vascular
Abstract

Vascular dysfunction and organ failure are two distinct, albeit highly interconnected, clinical outcomes linked to morbidity and mortality in human sepsis. The mechanisms driving vascular and parenchymal damage are dynamic and display significant molecular cross talk between organs and tissues. Therefore, assessing their individual contribution to disease progression is technically challenging. Here, we hypothesize that dysregulated vascular responses predispose the organism to organ failure. To address this hypothesis, we have evaluated four major organs in a murine model of Staphylococcus aureus sepsis by combining in vivo labeling of the endothelial cell surface proteome, data-independent acquisition (DIA) mass spectrometry, and an integrative computational pipeline. The data reveal, with unprecedented depth and throughput, that a septic insult evokes organ-specific proteome responses that are highly compartmentalized, synchronously coordinated, and significantly correlated with the progression of the disease. These responses include abundant vascular shedding, dysregulation of the intrinsic pathway of coagulation, compartmentalization of the acute phase response, and abundant upregulation of glycocalyx components. Vascular cell surface proteome changes were also found to precede bacterial invasion and leukocyte infiltration into the organs, as well as to precede changes in various well-established cellular and biochemical correlates of systemic coagulopathy and tissue dysfunction. Importantly, our data suggest a potential role for the vascular proteome as a determinant of the susceptibility of the organs to undergo failure during sepsis. IMPORTANCE Sepsis is a life-threatening response to infection that results in immune dysregulation, vascular dysfunction, and organ failure. New methods are needed for the identification of diagnostic and therapeutic targets. Here, we took a systems-wide approach using data-independent acquisition (DIA) mass spectrometry to track the progression of bacterial sepsis in the vasculature leading to organ failure. Using a murine model of S. aureus sepsis, we were able to quantify thousands of proteins across the plasma and parenchymal and vascular compartments of multiple organs in a time-resolved fashion. We showcase the profound proteome remodeling triggered by sepsis over time and across these compartments. Importantly, many vascular proteome alterations precede changes in traditional correlates of organ dysfunction, opening a molecular window for the discovery of early markers of sepsis progression.

Published
2022

4. Endothelial Heparan Sulfate Mediates Hepatic Neutrophil Trafficking and Injury during Staphylococcus aureus Sepsis

Author

Golden, Gregory J, Toledo, Alejandro Gómez, Marki, Alex, Sorrentino, James T, Morris, Claire, Riley, Raquel J, Spliid, Charlotte, Chen, Qiongyu, Cornax, Ingrid, Lewis, Nathan E, Varki, Nissi, Le, Dzung, Malmström, Johan, Karlsson, Christofer, Ley, Klaus, Nizet, Victor, and Esko, Jeffrey D

Subjects
Liver Disease, Sepsis, Infectious Diseases, Hematology, Digestive Diseases, Emerging Infectious Diseases, Clinical Research, Chronic Liver Disease and Cirrhosis, 2.1 Biological and endogenous factors, Aetiology, Cardiovascular, Inflammatory and immune system, Animals, Disease Models, Animal, Endothelial Cells, Female, Glycocalyx, Heparitin Sulfate, Liver, Lung, Male, Mice, Mice, Inbred C57BL, Neutrophil Activation, Neutrophils, Staphylococcus aureus, heparan sulfate, intravital microscopy, liver, neutrophils, proteomics, sepsis, thrombosis, Microbiology
Abstract

Hepatic failure is an important risk factor for poor outcome in septic patients. Using a chemical tagging workflow and high-resolution mass spectrometry, we demonstrate that rapid proteome remodeling of the vascular surfaces precedes hepatic damage in a murine model of Staphylococcus aureus sepsis. These early changes include vascular deposition of neutrophil-derived proteins, shedding of vascular receptors, and altered levels of heparin/heparan sulfate-binding factors. Modification of endothelial heparan sulfate, a major component of the vascular glycocalyx, diminishes neutrophil trafficking to the liver and reduces hepatic coagulopathy and organ damage during the systemic inflammatory response to infection. Modifying endothelial heparan sulfate likewise reduces neutrophil trafficking in sterile hepatic injury, reflecting a more general role of heparan sulfate contribution to the modulation of leukocyte behavior during inflammation. IMPORTANCE Vascular glycocalyx remodeling is critical to sepsis pathology, but the glycocalyx components that contribute to this process remain poorly characterized. This article shows that during Staphylococcus aureus sepsis, the liver vascular glycocalyx undergoes dramatic changes in protein composition associated with neutrophilic activity and heparin/heparan sulfate binding, all before organ damage is detectable by standard circulating liver damage markers or histology. Targeted manipulation of endothelial heparan sulfate modulates S. aureus sepsis-induced hepatotoxicity by controlling the magnitude of neutrophilic infiltration into the liver in both nonsterile and sterile injury. These data identify an important vascular glycocalyx component that impacts hepatic failure during nonsterile and sterile injury.

Published
2021

5. Correcting for sparsity and interdependence in glycomics by accounting for glycan biosynthesis.

Author

Bao, Bokan, Kellman, Benjamin P, Chiang, Austin WT, Zhang, Yujie, Sorrentino, James T, York, Austin K, Mohammad, Mahmoud A, Haymond, Morey W, Bode, Lars, and Lewis, Nathan E

Subjects
Humans, Fucosyltransferases, Gangliosides, Polysaccharides, Erythropoietin, Mucins, Cluster Analysis, Biological Transport, Glycosylation, Biosynthetic Pathways, Glycomics, Gene Knockout Techniques, Data Analysis
Abstract

Glycans are fundamental cellular building blocks, involved in many organismal functions. Advances in glycomics are elucidating the essential roles of glycans. Still, it remains challenging to properly analyze large glycomics datasets, since the abundance of each glycan is dependent on many other glycans that share many intermediate biosynthetic steps. Furthermore, the overlap of measured glycans can be low across samples. We address these challenges with GlyCompare, a glycomic data analysis approach that accounts for shared biosynthetic steps for all measured glycans to correct for sparsity and non-independence in glycomics, which enables direct comparison of different glycoprofiles and increases statistical power. Using GlyCompare, we study diverse N-glycan profiles from glycoengineered erythropoietin. We obtain biologically meaningful clustering of mutant cell glycoprofiles and identify knockout-specific effects of fucosyltransferase mutants on tetra-antennary structures. We further analyze human milk oligosaccharide profiles and find mother's fucosyltransferase-dependent secretor-status indirectly impact the sialylation. Finally, we apply our method on mucin-type O-glycans, gangliosides, and site-specific compositional glycosylation data to reveal tissues and disease-specific glycan presentations. Our substructure-oriented approach will enable researchers to take full advantage of the growing power and size of glycomics data.

Published
2021

6. A consensus-based and readable extension of Linear Code for Reaction Rules (LiCoRR)

Author

Kellman, Benjamin P, Zhang, Yujie, Logomasini, Emma, Meinhardt, Eric, Godinez-Macias, Karla P, Chiang, Austin WT, Sorrentino, James T, Liang, Chenguang, Bao, Bokan, Zhou, Yusen, Akase, Sachiko, Sogabe, Isami, Kouka, Thukaa, Winzeler, Elizabeth A, Wilson, Iain BH, Campbell, Matthew P, Neelamegham, Sriram, Krambeck, Frederick J, Aoki-Kinoshita, Kiyoko F, and Lewis, Nathan E

Subjects
Organic Chemistry, Chemical Sciences, glycoinformatics, linear code, systems glycobiology, Organic chemistry
Abstract

Systems glycobiology aims to provide models and analysis tools that account for the biosynthesis, regulation, and interactions with glycoconjugates. To facilitate these methods, there is a need for a clear glycan representation accessible to both computers and humans. Linear Code, a linearized and readily parsable glycan structure representation, is such a language. For this reason, Linear Code was adapted to represent reaction rules, but the syntax has drifted from its original description to accommodate new and originally unforeseen challenges. Here, we delineate the consensuses and inconsistencies that have arisen through this adaptation. We recommend options for a consensus-based extension of Linear Code that can be used for reaction rule specification going forward. Through this extension and specification of Linear Code to reaction rules, we aim to minimize inconsistent symbology thereby making glycan database queries easier. With a clear guide for generating reaction rule descriptions, glycan synthesis models will be more interoperable and reproducible thereby moving glycoinformatics closer to compliance with FAIR standards. Here, we present Linear Code for Reaction Rules (LiCoRR), version 1.0, an unambiguous representation for describing glycosylation reactions in both literature and code.

Published
2020

9. Dissecting the properties of circulating IgG against Group A Streptococcus through a combined systems antigenomics-serology workflow

Author

Malmstrom, Johan, primary, Chowdhury, Sounak, additional, Gomez Toledo, Alejandro, additional, Hjortswang, Elisabeth, additional, Sorrentino, James T., additional, Lewis, Nathan E., additional, Blackberg, Anna, additional, Ekstrom, Simon, additional, Izadi, Arman, additional, Nordenfelt, Pontus, additional, Malmstrom, Lars, additional, and Rasmussen, Magnus, additional

Published
2023
Full Text
View/download PDF

10. Vascular Proteome Responses Precede Organ Dysfunction in a Murine Model of Staphylococcus aureus Bacteremia

Author

Sorrentino, James T., Golden, Gregory J., Morris, Claire, Painter, Chelsea D., Nizet, Victor, Campos, Alexandre Rosa, Smith, Jeffrey W., Karlsson, Christofer, Malmström, Johan, Lewis, Nathan E., Esko, Jeffrey D., Toledo, Alejandro Gómez, and Schmidt, Frank

Subjects
DIA mass spectrometry, Staphylococcus aureus, Proteome, Animal, Multiple Organ Failure, vascular glycocalyx, Inflammatory and immune system, Bacteremia, Hematology, sepsis, Mice, Emerging Infectious Diseases, Infectious Diseases, SDG 3 - Good Health and Well-being, vascular, Disease Models, Animals, Humans, 2.1 Biological and endogenous factors, Aetiology, Infection, glycocalyx
Abstract

Vascular dysfunction and organ failure are two distinct, albeit highly interconnected, clinical outcomes linked to morbidity and mortality in human sepsis. The mechanisms driving vascular and parenchymal damage are dynamic and display significant molecular cross talk between organs and tissues. Therefore, assessing their individual contribution to disease progression is technically challenging. Here, we hypothesize that dysregulated vascular responses predispose the organism to organ failure. To address this hypothesis, we have evaluated four major organs in a murine model of Staphylococcus aureus sepsis by combining in vivo labeling of the endothelial cell surface proteome, data-independent acquisition (DIA) mass spectrometry, and an integrative computational pipeline. The data reveal, with unprecedented depth and throughput, that a septic insult evokes organ-specific proteome responses that are highly compartmentalized, synchronously coordinated, and significantly correlated with the progression of the disease. These responses include abundant vascular shedding, dysregulation of the intrinsic pathway of coagulation, compartmentalization of the acute phase response, and abundant upregulation of glycocalyx components. Vascular cell surface proteome changes were also found to precede bacterial invasion and leukocyte infiltration into the organs, as well as to precede changes in various well-established cellular and biochemical correlates of systemic coagulopathy and tissue dysfunction. Importantly, our data suggest a potential role for the vascular proteome as a determinant of the susceptibility of the organs to undergo failure during sepsis. IMPORTANCE Sepsis is a life-threatening response to infection that results in immune dysregulation, vascular dysfunction, and organ failure. New methods are needed for the identification of diagnostic and therapeutic targets. Here, we took a systems-wide approach using data-independent acquisition (DIA) mass spectrometry to track the progression of bacterial sepsis in the vasculature leading to organ failure. Using a murine model of S. aureus sepsis, we were able to quantify thousands of proteins across the plasma and parenchymal and vascular compartments of multiple organs in a time-resolved fashion. We showcase the profound proteome remodeling triggered by sepsis over time and across these compartments. Importantly, many vascular proteome alterations precede changes in traditional correlates of organ dysfunction, opening a molecular window for the discovery of early markers of sepsis progression.

Published
2022
Full Text
View/download PDF

12. Vascular proteome responses precede organ dysfunction in sepsis

Author

Sorrentino, James T., primary, Golden, Gregory J., additional, Morris, Claire, additional, Painter, Chelsea, additional, Nizet, Victor, additional, Campos, Alexandre Rosa, additional, Smith, Jeffrey W., additional, Karlsson, Christofer A.Q., additional, Malmström, Johan, additional, Lewis, Nathan E, additional, Esko, Jeffrey D, additional, and Gomez Toledo, Alejandro, additional

Published
2021
Full Text
View/download PDF

13. sj-pdf-1-jhc-10.1177_0022155420988661 – Supplemental material for A Systems View of the Heparan Sulfate Interactome

Author

Schaefer, Liliana, Frevert, Charles W., Toledo, Alejandro Gómez, Sorrentino, James T., Sandoval, Daniel R., Malmström, Johan, Lewis, Nathan E., and Esko, Jeffrey D.

Subjects
FOS: Biological sciences, FOS: Clinical medicine, Cell Biology, 69999 Biological Sciences not elsewhere classified, 111599 Pharmacology and Pharmaceutical Sciences not elsewhere classified
Abstract

Supplemental material, sj-pdf-1-jhc-10.1177_0022155420988661 for A Systems View of the Heparan Sulfate Interactome by Liliana Schaefer, Charles W. Frevert, Alejandro Gómez Toledo, James T. Sorrentino, Daniel R. Sandoval, Johan Malmström, Nathan E. Lewis and Jeffrey D. Esko in Journal of Histochemistry & Cytochemistry

Published
2021
Full Text
View/download PDF

14. Additional file 1 of Systems glycobiology for discovering drug targets, biomarkers, and rational designs for glyco-immunotherapy

Author

Chiang, Austin W. T., Baghdassarian, Hratch M., Kellman, Benjamin P., Bao, Bokan, Sorrentino, James T., Liang, Chenguang, Kuo, Chih-Chung, Masson, Helen O., and Lewis, Nathan E.

Subjects
surgical procedures, operative, digestive system, digestive system diseases
Abstract

Additional file 1: Appendix–A. Molecular mechanisms of cancer immunotherapies. Appendix–B. Novel targets to overcome tumor evasion. Appendix–C. Novel technologies to overcome tumor evasion. Appendix–D. Novel technologies to overcome graft-versus-host-disease. Appendix–E. The coming age of Systems Glycobiology in cancer research. Figure S1. The coming age of Systems Glycobiology in cancer research. (Top panel) Timeline of Nobel Prize or Milestone of cancer immunology (blue colors) and the FDA approved cancer immunotherapies (red colors). (Bottom panel) Timeline of systematic modelling of glycosylation machinery (purple colors) and the analytical methods and computational tool for study glycan epitopes (green colors).

Published
2021
Full Text
View/download PDF

15. Systems glycobiology for discovering drug targets, biomarkers, and rational designs for glyco-immunotherapy

Author

Chiang, Austin W.T., Baghdassarian, Hratch M., Kellman, Benjamin P., Bao, Bokan, Sorrentino, James T., Liang, Chenguang, Kuo, Chih Chung, Masson, Helen O., Lewis, Nathan E., Chiang, Austin W.T., Baghdassarian, Hratch M., Kellman, Benjamin P., Bao, Bokan, Sorrentino, James T., Liang, Chenguang, Kuo, Chih Chung, Masson, Helen O., and Lewis, Nathan E.

Abstract

Cancer immunotherapy has revolutionized treatment and led to an unprecedented wave of immuno-oncology research during the past two decades. In 2018, two pioneer immunotherapy innovators, Tasuku Honjo and James P. Allison, were awarded the Nobel Prize for their landmark cancer immunotherapy work regarding “cancer therapy by inhibition of negative immune regulation” –CTLA4 and PD-1 immune checkpoints. However, the challenge in the coming decade is to develop cancer immunotherapies that can more consistently treat various patients and cancer types. Overcoming this challenge requires a systemic understanding of the underlying interactions between immune cells, tumor cells, and immunotherapeutics. The role of aberrant glycosylation in this process, and how it influences tumor immunity and immunotherapy is beginning to emerge. Herein, we review current knowledge of miRNA-mediated regulatory mechanisms of glycosylation machinery, and how these carbohydrate moieties impact immune cell and tumor cell interactions. We discuss these insights in the context of clinical findings and provide an outlook on modulating the regulation of glycosylation to offer new therapeutic opportunities. Finally, in the coming age of systems glycobiology, we highlight how emerging technologies in systems glycobiology are enabling deeper insights into cancer immuno-oncology, helping identify novel drug targets and key biomarkers of cancer, and facilitating the rational design of glyco-immunotherapies. These hold great promise clinically in the immuno-oncology field.

Published
2021

17. Bacterial modification of the host glycosaminoglycan heparan sulfate modulates SARS-CoV-2 infectivity

Author

Martino, Cameron, primary, Kellman, Benjamin P., additional, Sandoval, Daniel R., additional, Clausen, Thomas Mandel, additional, Marotz, Clarisse A., additional, Song, Se Jin, additional, Wandro, Stephen, additional, Zaramela, Livia S., additional, Salido Benítez, Rodolfo Antonio, additional, Zhu, Qiyun, additional, Armingol, Erick, additional, Vázquez-Baeza, Yoshiki, additional, McDonald, Daniel, additional, Sorrentino, James T., additional, Taylor, Bryn, additional, Belda-Ferre, Pedro, additional, Liang, Chenguang, additional, Zhang, Yujie, additional, Schifanella, Luca, additional, Klatt, Nichole R., additional, Havulinna, Aki S., additional, Jousilahti, Pekka, additional, Huang, Shi, additional, Haiminen, Niina, additional, Parida, Laxmi, additional, Kim, Ho-Cheol, additional, Swafford, Austin D., additional, Zengler, Karsten, additional, Cheng, Susan, additional, Inouye, Michael, additional, Niiranen, Teemu, additional, Jain, Mohit, additional, Salomaa, Veikko, additional, Esko, Jeffrey D., additional, Lewis, Nathan E., additional, and Knight, Rob, additional

Published
2020
Full Text
View/download PDF

18. A consensus-based and readable extension ofLinearCode forReactionRules (LiCoRR)

Author

Kellman, Benjamin P., primary, Zhang, Yujie, additional, Logomasini, Emma, additional, Meinhardt, Eric, additional, Chiang, Austin W. T., additional, Sorrentino, James T., additional, Liang, Chenguang, additional, Bao, Bokan, additional, Zhou, Yusen, additional, Akase, Sachiko, additional, Sogabe, Isami, additional, Kouka, Thukaa, additional, Wilson, Iain B.H., additional, Campbell, Matthew P., additional, Neelamegham, Sriram, additional, Krambeck, Frederick J., additional, Aoki-Kinoshita, Kiyoko F., additional, and Lewis, Nathan E., additional

Published
2020
Full Text
View/download PDF

21. A Systems View of the Heparan Sulfate Interactome

Author

Schaefer, Liliana, Frevert, Charles W., Gómez Toledo, Alejandro, Sorrentino, James T., Sandoval, Daniel R., Malmström, Johan, Lewis, Nathan E., and Esko, Jeffrey D.

Abstract

Heparan sulfate proteoglycans consist of a small family of proteins decorated with one or more covalently attached heparan sulfate glycosaminoglycan chains. These chains have intricate structural patterns based on the position of sulfate groups and uronic acid epimers, which dictate their ability to engage a large repertoire of heparan sulfate–binding proteins, including extracellular matrix proteins, growth factors and morphogens, cytokines and chemokines, apolipoproteins and lipases, adhesion and growth factor receptors, and components of the complement and coagulation system. This review highlights recent progress in the characterization of the so-called “heparan sulfate interactome,” with a major focus on systems-wide strategies as a tool for discovery and characterization of this subproteome. In addition, we compiled all heparan sulfate–binding proteins reported in the literature to date and grouped them into a few major functional classes by applying a networking approach.

Published
2021
Full Text
View/download PDF

22. A consensus-based and readable extension of Li near Co de for R eaction R ules (LiCoRR).

Author

Kellman BP, Zhang Y, Logomasini E, Meinhardt E, Godinez-Macias KP, Chiang AWT, Sorrentino JT, Liang C, Bao B, Zhou Y, Akase S, Sogabe I, Kouka T, Winzeler EA, Wilson IBH, Campbell MP, Neelamegham S, Krambeck FJ, Aoki-Kinoshita KF, and Lewis NE

Abstract

Systems glycobiology aims to provide models and analysis tools that account for the biosynthesis, regulation, and interactions with glycoconjugates. To facilitate these methods, there is a need for a clear glycan representation accessible to both computers and humans. Linear Code, a linearized and readily parsable glycan structure representation, is such a language. For this reason, Linear Code was adapted to represent reaction rules, but the syntax has drifted from its original description to accommodate new and originally unforeseen challenges. Here, we delineate the consensuses and inconsistencies that have arisen through this adaptation. We recommend options for a consensus-based extension of Linear Code that can be used for reaction rule specification going forward. Through this extension and specification of Linear Code to reaction rules, we aim to minimize inconsistent symbology thereby making glycan database queries easier. With a clear guide for generating reaction rule descriptions, glycan synthesis models will be more interoperable and reproducible thereby moving glycoinformatics closer to compliance with FAIR standards. Here, we present Linear Code for Reaction Rules (LiCoRR), version 1.0, an unambiguous representation for describing glycosylation reactions in both literature and code., (Copyright © 2020, Kellman et al.; licensee Beilstein-Institut.)

Published
2020
Full Text
View/download PDF

23. Bacterial modification of the host glycosaminoglycan heparan sulfate modulates SARS-CoV-2 infectivity.

Author

Martino C, Kellman BP, Sandoval DR, Clausen TM, Marotz CA, Song SJ, Wandro S, Zaramela LS, Salido Benítez RA, Zhu Q, Armingol E, Vázquez-Baeza Y, McDonald D, Sorrentino JT, Taylor B, Belda-Ferre P, Liang C, Zhang Y, Schifanella L, Klatt NR, Havulinna AS, Jousilahti P, Huang S, Haiminen N, Parida L, Kim HC, Swafford AD, Zengler K, Cheng S, Inouye M, Niiranen T, Jain M, Salomaa V, Esko JD, Lewis NE, and Knight R

Abstract

The human microbiota has a close relationship with human disease and it remodels components of the glycocalyx including heparan sulfate (HS). Studies of the severe acute respiratory syndrome coronavirus (SARS-CoV-2) spike protein receptor binding domain suggest that infection requires binding to HS and angiotensin converting enzyme 2 (ACE2) in a codependent manner. Here, we show that commensal host bacterial communities can modify HS and thereby modulate SARS-CoV-2 spike protein binding and that these communities change with host age and sex. Common human-associated commensal bacteria whose genomes encode HS-modifying enzymes were identified. The prevalence of these bacteria and the expression of key microbial glycosidases in bronchoalveolar lavage fluid (BALF) was lower in adult COVID-19 patients than in healthy controls. The presence of HS-modifying bacteria decreased with age in two large survey datasets, FINRISK 2002 and American Gut, revealing one possible mechanism for the observed increase in COVID-19 susceptibility with age. In vitro , bacterial glycosidases from unpurified culture media supernatants fully blocked SARS-CoV-2 spike binding to human H1299 protein lung adenocarcinoma cells. HS-modifying bacteria in human microbial communities may regulate viral adhesion, and loss of these commensals could predispose individuals to infection. Understanding the impact of shifts in microbial community composition and bacterial lyases on SARS-CoV-2 infection may lead to new therapeutics and diagnosis of susceptibility.

Published
2020
Full Text
View/download PDF

Catalog

Books, media, physical & digital resources
See catalog results