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1. Coordinated expansion of memory T follicular helper and B cells mediates spontaneous clearance of HCV reinfection

Author

Mohamed Eisa, Elsa Gomez-Escobar, Nathalie Bédard, Nourtan F. Abdeltawab, Nicol Flores, Sabrina Mazouz, Alizée Fieffé-Bédard, Patrick Sakayan, John Gridley, Mohamed S. Abdel-Hakeem, Julie Bruneau, Arash Grakoui, and Naglaa H. Shoukry

Subjects
hepatitis C virus, B cells, neutralizing antibodies, Tfh and immunity, reinfection, Immunologic diseases. Allergy, RC581-607
Abstract

IntroductionFollicular helper T cells are essential for helping in the maturation of B cells and the production of neutralizing antibodies (NAbs) during primary viral infections. However, their role during recall responses is unclear. Here, we used hepatitis C virus (HCV) reinfection in humans as a model to study the recall collaborative interaction between circulating CD4 T follicular helper cells (cTfh) and memory B cells (MBCs) leading to the generation of NAbs.MethodsWe evaluated this interaction longitudinally in subjects who have spontaneously resolved primary HCV infection during a subsequent reinfection episode that resulted in either another spontaneous resolution (SR/SR, n = 14) or chronic infection (SR/CI, n = 8).ResultsBoth groups exhibited virus-specific memory T cells that expanded upon reinfection. However, early expansion of activated cTfh (CD4+CXCR5+PD-1+ICOS+FoxP3−) occurred in SR/SR only. The frequency of activated cTfh negatively correlated with time post-infection. Concomitantly, NAbs and HCV-specific MBCs (CD19+CD27+IgM−E2-Tet+) peaked during the early acute phase in SR/SR but not in SR/CI. Finally, the frequency of the activated cTfh1 (CXCR3+CCR6−) subset correlated with the neutralization breadth and potency of NAbs.ConclusionThese results underscore a key role for early activation of cTfh1 cells in helping antigen-specific B cells to produce NAbs that mediate the clearance of HCV reinfection.

Published
2024
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2. Activation-Induced Marker Assay to Identify and Isolate HCV-Specific T Cells for Single-Cell RNA-Seq Analysis

Author

Mohamed Eisa, Nicol Flores, Omar Khedr, Elsa Gomez-Escobar, Nathalie Bédard, Nourtan F. Abdeltawab, Julie Bruneau, Arash Grakoui, and Naglaa H. Shoukry

Subjects
hepatitis C virus, AIM assay, antigen-specific T cells, single-cell RNA sequencing, Microbiology, QR1-502
Abstract

Identification and isolation of antigen-specific T cells for downstream transcriptomic analysis is key for various immunological studies. Traditional methods using major histocompatibility complex (MHC) multimers are limited by the number of predefined immunodominant epitopes and MHC matching of the study subjects. Activation-induced markers (AIM) enable highly sensitive detection of rare antigen-specific T cells irrespective of the availability of MHC multimers. Herein, we have developed an AIM assay for the detection, sorting and subsequent single-cell RNA sequencing (scRNA-seq) analysis of hepatitis C virus (HCV)-specific T cells. We examined different combinations of the activation markers CD69, CD40L, OX40, and 4-1BB at 6, 9, 18 and 24 h post stimulation with HCV peptide pools. AIM+ CD4 T cells exhibited upregulation of CD69 and CD40L as early as 6 h post-stimulation, while OX40 and 4-1BB expression was delayed until 18 h. AIM+ CD8 T cells were characterized by the coexpression of CD69 and 4-1BB at 18 h, while the expression of CD40L and OX40 remained low throughout the stimulation period. AIM+ CD4 and CD8 T cells were successfully sorted and processed for scRNA-seq analysis examining gene expression and T cell receptor (TCR) usage. scRNA-seq analysis from this one subject revealed that AIM+ CD4 T (CD69+ CD40L+) cells predominantly represented Tfh, Th1, and Th17 profiles, whereas AIM+ CD8 T (CD69+ 4-1BB+) cells primarily exhibited effector and effector memory profiles. TCR analysis identified 1023 and 160 unique clonotypes within AIM+ CD4 and CD8 T cells, respectively. In conclusion, this approach offers highly sensitive detection of HCV-specific T cells that can be applied for cohort studies, thus facilitating the identification of specific gene signatures associated with infection outcome and vaccination.

Published
2024
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5. Phenotype and fate of liver-resident CD8 T cells during acute and chronic hepacivirus infection.

Author

Piyush Dravid, Satyapramod Murthy, Zayed Attia, Cole Cassady, Rahul Chandra, Sheetal Trivedi, Ashish Vyas, John Gridley, Brantley Holland, Anuradha Kumari, Arash Grakoui, John M Cullen, Christopher M Walker, Himanshu Sharma, and Amit Kapoor

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

Immune correlates of hepatitis C virus (HCV) clearance and control remain poorly defined due to the lack of an informative animal model. We recently described acute and chronic rodent HCV-like virus (RHV) infections in lab mice. Here, we developed MHC class I and class II tetramers to characterize the serial changes in RHV-specific CD8 and CD4 T cells during acute and chronic infection in C57BL/6J mice. RHV infection induced rapid expansion of T cells targeting viral structural and nonstructural proteins. After virus clearance, the virus-specific T cells transitioned from effectors to long-lived liver-resident memory T cells (TRM). The effector and memory CD8 and CD4 T cells primarily produced Th1 cytokines, IFN-γ, TNF-α, and IL-2, upon ex vivo antigen stimulation, and their phenotype and transcriptome differed significantly between the liver and spleen. Rapid clearance of RHV reinfection coincided with the proliferation of virus-specific CD8 TRM cells in the liver. Chronic RHV infection was associated with the exhaustion of CD8 T cells (Tex) and the development of severe liver diseases. Interestingly, the virus-specific CD8 Tex cells continued proliferation in the liver despite the persistent high-titer viremia and retained partial antiviral functions, as evident from their ability to degranulate and produce IFN-γ upon ex vivo antigen stimulation. Thus, RHV infection in mice provides a unique model to study the function and fate of liver-resident T cells during acute and chronic hepatotropic infection.

Published
2023
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6. Regions of hepatitis C virus E2 required for membrane association

Author

Ashish Kumar, Tiana C. Rohe, Elizabeth J. Elrod, Abdul G. Khan, Altaira D. Dearborn, Ryan Kissinger, Arash Grakoui, and Joseph Marcotrigiano

Subjects
Science
Abstract

Hepatitis C virus (HCV) uses a hybrid entry mechanism. Upon exposure to low pH, envelope glycoprotein E2 releases an internal loop into the host membrane. Here we show the amino terminal region is a critical determinant for membrane interaction, providing insights into the HCV entry mechanism.

Published
2023
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7. Serum neutralization activity declines but memory B cells persist after cure of chronic hepatitis C

Author

Akira Nishio, Sharika Hasan, Heiyoung Park, Nana Park, Jordan H. Salas, Eduardo Salinas, Lela Kardava, Paul Juneau, Nicole Frumento, Guido Massaccesi, Susan Moir, Justin R. Bailey, Arash Grakoui, Marc G. Ghany, and Barbara Rehermann

Subjects
Science
Abstract

Long-term dynamics of the humoral response to HCV in cured individuals aren’t well understood. Here, Nishio et al. show that virus-neutralizing antibody levels decrease in potency and breadth after cure of chronic hepatitis C, while HCV-specific memory B cells persist.

Published
2022
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8. Coordinated expansion of memory T follicular helper and B cells mediates spontaneous clearance of HCV reinfection

Author

Eisa, Mohamed, primary, Gomez-Escobar, Elsa, additional, Bédard, Nathalie, additional, Abdeltawab, Nourtan F., additional, Flores, Nicol, additional, Mazouz, Sabrina, additional, Fieffé-Bédard, Alizée, additional, Sakayan, Patrick, additional, Gridley, John, additional, Abdel-Hakeem, Mohamed S., additional, Bruneau, Julie, additional, Grakoui, Arash, additional, and Shoukry, Naglaa H., additional

Published
2024
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9. Memory in repetitive protein–protein interaction series

Author

Aaron M. Rosado, Yan Zhang, Hyun-Kyu Choi, Yunfeng Chen, Samuel M. Ehrlich, Fengzhi Jin, Arash Grakoui, Brian D. Evavold, and Cheng Zhu

Subjects
Biotechnology, TP248.13-248.65, Medical technology, R855-855.5
Abstract

Interactions between proteins coordinate biological processes in an organism and may impact its responses to changing environments and diseases through feedback systems. Feedback systems function by using changes in the past to influence behaviors in the future, which we refer to here as memory. Here, we summarized several observations made, ideas conceptualized, and mathematical models developed for quantitatively analyzing memory effects in repetitive protein–protein interactions (PPIs). Specifically, we consider how proteins on the cell or in isolation retain information about prior interactions to impact current interactions. The micropipette, biomembrane force probe, and atomic force microscopic techniques were used to repeatedly assay PPIs. The resulting time series were analyzed by a previous and two new models to extract three memory indices of short (seconds), intermediate (minutes), and long (hours) timescales. We found that interactions of cell membrane, but not soluble, T cell receptor (TCR) with peptide-major histocompatibility complex (pMHC) exhibits short-term memory that impacts on-rate, but not off-rate of the binding kinetics. Peptide dissociation from MHC resulted in intermediate- and long-term memories in TCR–pMHC interactions. However, we observed no changes in kinetic parameters by repetitive measurements on living cells over intermediate timescales using stable pMHCs. Parameters quantifying memory effects in PPIs could provide additional information regarding biological mechanisms. The methods developed herein also provide tools for future research.

Published
2023
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12. Activation-Induced Marker Assay to Identify and Isolate HCV-Specific T Cells for Single-Cell RNA-Seq Analysis.

Author

Eisa, Mohamed, Flores, Nicol, Khedr, Omar, Gomez-Escobar, Elsa, Bédard, Nathalie, Abdeltawab, Nourtan F., Bruneau, Julie, Grakoui, Arash, and Shoukry, Naglaa H.

Subjects
T cells, MAJOR histocompatibility complex, HEPATITIS C virus, GENE expression, PEPTIDES
Abstract

Identification and isolation of antigen-specific T cells for downstream transcriptomic analysis is key for various immunological studies. Traditional methods using major histocompatibility complex (MHC) multimers are limited by the number of predefined immunodominant epitopes and MHC matching of the study subjects. Activation-induced markers (AIM) enable highly sensitive detection of rare antigen-specific T cells irrespective of the availability of MHC multimers. Herein, we have developed an AIM assay for the detection, sorting and subsequent single-cell RNA sequencing (scRNA-seq) analysis of hepatitis C virus (HCV)-specific T cells. We examined different combinations of the activation markers CD69, CD40L, OX40, and 4-1BB at 6, 9, 18 and 24 h post stimulation with HCV peptide pools. AIM+ CD4 T cells exhibited upregulation of CD69 and CD40L as early as 6 h post-stimulation, while OX40 and 4-1BB expression was delayed until 18 h. AIM+ CD8 T cells were characterized by the coexpression of CD69 and 4-1BB at 18 h, while the expression of CD40L and OX40 remained low throughout the stimulation period. AIM+ CD4 and CD8 T cells were successfully sorted and processed for scRNA-seq analysis examining gene expression and T cell receptor (TCR) usage. scRNA-seq analysis from this one subject revealed that AIM+ CD4 T (CD69+ CD40L+) cells predominantly represented Tfh, Th1, and Th17 profiles, whereas AIM+ CD8 T (CD69+ 4-1BB+) cells primarily exhibited effector and effector memory profiles. TCR analysis identified 1023 and 160 unique clonotypes within AIM+ CD4 and CD8 T cells, respectively. In conclusion, this approach offers highly sensitive detection of HCV-specific T cells that can be applied for cohort studies, thus facilitating the identification of specific gene signatures associated with infection outcome and vaccination. [ABSTRACT FROM AUTHOR]

Published
2024
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13. Structural insights into hepatitis C virus receptor binding and entry

Author

Kumar, Ashish, Hossain, Reafa A., Yost, Samantha A., Bu, Wei, Wang, Yuanyuan, Dearborn, Altaira D., and Grakoui, Arash

Subjects
Glycoproteins -- Physiological aspects, Protein binding -- Health aspects, Hepatitis C virus -- Physiological aspects, Proteins -- Conformation, Viral envelopes -- Physiological aspects, Environmental issues, Science and technology, Zoology and wildlife conservation
Abstract

Hepatitis C virus (HCV) infection is a causal agent of chronic liver disease, cirrhosis and hepatocellular carcinoma in humans, and afflicts more than 70 million people worldwide. The HCV envelope glycoproteins E1 and E2 are responsible for the binding of the virus to the host cell, but the exact entry process remains undetermined.sup.1. The majority of broadly neutralizing antibodies block interaction between HCV E2 and the large extracellular loop (LEL) of the cellular receptor CD81 (CD81-LEL).sup.2. Here we show that low pH enhances the binding of CD81-LEL to E2, and we determine the crystal structure of E2 in complex with an antigen-binding fragment (2A12) and CD81-LEL (E2-2A12-CD81-LEL); E2 in complex with 2A12 (E2-2A12); and CD81-LEL alone. After binding CD81, residues 418-422 in E2 are displaced, which allows for the extension of an internal loop consisting of residues 520-539. Docking of the E2-CD81-LEL complex onto a membrane-embedded, full-length CD81 places the residues Tyr529 and Trp531 of E2 proximal to the membrane. Liposome flotation assays show that low pH and CD81-LEL increase the interaction of E2 with membranes, whereas structure-based mutants of Tyr529, Trp531 and Ile422 in the amino terminus of E2 abolish membrane binding. These data support a model in which acidification and receptor binding result in a conformational change in E2 in preparation for membrane fusion. Crystal structures of the hepatitis C virus (HCV) glycoprotein E2 in complex with CD81 reveal the conformational changes that occur in E2 after binding of CD81 and the effects of pH on binding affinity., Author(s): Ashish Kumar [sup.1] , Reafa A. Hossain [sup.1] , Samantha A. Yost [sup.2] , Wei Bu [sup.3] , Yuanyuan Wang [sup.1] , Altaira D. Dearborn [sup.1] , Arash Grakoui [...]

Published
2021
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14. Differential immune transcriptomic profiles between vaccinated and resolved HCV reinfected subjects.

Author

Sabrina Mazouz, Eduardo Salinas, Nathalie Bédard, Ali Filali, Omar Khedr, Leo Swadling, Mohamed S Abdel-Hakeem, Asiyah Siddique, Eleanor Barnes, Julie Bruneau, Arash Grakoui, and Naglaa H Shoukry

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

Successive episodes of hepatitis C virus (HCV) infection represent a unique natural rechallenge experiment to define correlates of long-term protective immunity and inform vaccine development. We applied a systems immunology approach to characterize longitudinal changes in the peripheral blood transcriptomic signatures in eight subjects who spontaneously resolved two successive HCV infections. Furthermore, we compared these signatures with those induced by an HCV T cell-based vaccine regimen. We identified a plasma cell transcriptomic signature during early acute HCV reinfection. This signature was absent in primary infection and following HCV vaccine boost. Spontaneous resolution of HCV reinfection was associated with rapid expansion of glycoprotein E2-specifc memory B cells in three subjects and transient increase in E2-specific neutralizing antibodies in six subjects. Concurrently, there was an increase in the breadth and magnitude of HCV-specific T cells in 7 out of 8 subjects. These results suggest a cooperative role for both antibodies and T cells in clearance of HCV reinfection and support the development of next generation HCV vaccines targeting these two arms of the immune system.

Published
2022
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16. Erratum for Vanderheiden et al., 'CCR2 Signaling Restricts SARS-CoV-2 Infection'

Author

Abigail Vanderheiden, Jeronay Thomas, Allison L. Soung, Meredith E. Davis-Gardner, Katharine Floyd, Fengzhi Jin, David A. Cowan, Kathryn Pellegrini, Adrian Creanga, Amarendra Pegu, Alexandrine Derrien-Colemyn, Pei-Yong Shi, Arash Grakoui, Robyn S. Klein, Steven E. Bosinger, Jacob E. Kohlmeier, Vineet D. Menachery, and Mehul S. Suthar

Subjects
Microbiology, QR1-502
Published
2022
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17. BiliQML: a supervised machine-learning model to quantify biliary forms from digitized whole slide liver histopathological images.

Author

Hellen, Dominick J., Fay, Meredith E., Lee, David H., Klindt-Morgan, Caroline, Bennett, Ashley, Pachura, Kimberly J., Grakoui, Arash, Huppert, Stacey S., Dawson, Paul A., Lam, Wilbur A., and Karpen, Saul J.

Abstract

The progress of research focused on cholangiocytes and the biliary tree during development and following injury is hindered by limited available quantitative methodologies. Current techniques include two-dimensional standard histological cell-counting approaches, which are rapidly performed, error prone, and lack architectural context or three-dimensional analysis of the biliary tree in opacified livers, which introduce technical issues along with minimal quantitation. The present study aims to fill these quantitative gaps with a supervised machine-learning model (BiliQML) able to quantify biliary forms in the liver of anti-keratin 19 antibody-stained whole slide images. Training utilized 5,019 researcher-labeled biliary forms, which following feature selection, and algorithm optimization, generated an F score of 0.87. Application of BiliQML on seven separate cholangiopathy models [genetic (Afp-CRE;Pkd1l1null/Fl, Alb-CRE;Rbp-jkfl/fl, and Albumin-CRE;ROSANICD), surgical (bile duct ligation), toxicological (3,5-diethoxycarbonyl-1,4-dihydrocollidine), and therapeutic (Cyp2c70−/− with ileal bile acid transporter inhibition)] allowed for a means to validate the capabilities and utility of this platform. The results from BiliQML quantification revealed biological and pathological differences across these seven diverse models, indicating a highly sensitive, robust, and scalable methodology for the quantification of distinct biliary forms. BiliQML is the first comprehensive machine-learning platform for biliary form analysis, adding much-needed morphologic context to standard immunofluorescence-based histology, and provides clinical and basic science researchers with a novel tool for the characterization of cholangiopathies. NEW & NOTEWORTHY: BiliQML is the first comprehensive machine-learning platform for biliary form analysis in whole slide histopathological images. This platform provides clinical and basic science researchers with a novel tool for the improved quantification and characterization of biliary tract disorders. [ABSTRACT FROM AUTHOR]

Published
2024
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18. CD4+ and CD8+ T cells are required to prevent SARS-CoV-2 persistence in the nasal compartment

Author

Kar, Meenakshi, primary, Johnson, Katherine E. E., additional, Vanderheiden, Abigail, additional, Elrod, Elizabeth J., additional, Floyd, Katharine, additional, Geerling, Elizabeth, additional, Stone, E. Taylor, additional, Salinas, Eduardo, additional, Banakis, Stephanie, additional, Wang, Wei, additional, Sathish, Shruti, additional, Shrihari, Swathi, additional, Davis-Gardner, Meredith E., additional, Kohlmeier, Jacob, additional, Pinto, Amelia, additional, Klein, Robyn, additional, Grakoui, Arash, additional, Ghedin, Elodie, additional, and Suthar, Mehul S., additional

Published
2024
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19. CCR2 Signaling Restricts SARS-CoV-2 Infection

Author

Abigail Vanderheiden, Jeronay Thomas, Allison L. Soung, Meredith E. Davis-Gardner, Katharine Floyd, Fengzhi Jin, David A. Cowan, Kathryn Pellegrini, Adrian Creanga, Amarendra Pegu, Alexandrine Derrien-Colemyn, Pei-Yong Shi, Arash Grakoui, Robyn S. Klein, Steven E. Bosinger, Jacob E. Kohlmeier, Vineet D. Menachery, and Mehul S. Suthar

Subjects
lung inflammation, monocytes, SARS-CoV-2, innate immunity, mouse model, Microbiology, QR1-502
Abstract

ABSTRACT Severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2) has caused a historic pandemic of respiratory disease (coronavirus disease 2019 [COVID-19]), and current evidence suggests that severe disease is associated with dysregulated immunity within the respiratory tract. However, the innate immune mechanisms that mediate protection during COVID-19 are not well defined. Here, we characterize a mouse model of SARS-CoV-2 infection and find that early CCR2 signaling restricts the viral burden in the lung. We find that a recently developed mouse-adapted SARS-CoV-2 (MA-SARS-CoV-2) strain as well as the emerging B.1.351 variant trigger an inflammatory response in the lung characterized by the expression of proinflammatory cytokines and interferon-stimulated genes. Using intravital antibody labeling, we demonstrate that MA-SARS-CoV-2 infection leads to increases in circulating monocytes and an influx of CD45+ cells into the lung parenchyma that is dominated by monocyte-derived cells. Single-cell RNA sequencing (scRNA-Seq) analysis of lung homogenates identified a hyperinflammatory monocyte profile. We utilize this model to demonstrate that mechanistically, CCR2 signaling promotes the infiltration of classical monocytes into the lung and the expansion of monocyte-derived cells. Parenchymal monocyte-derived cells appear to play a protective role against MA-SARS-CoV-2, as mice lacking CCR2 showed higher viral loads in the lungs, increased lung viral dissemination, and elevated inflammatory cytokine responses. These studies have identified a potential CCR2-monocyte axis that is critical for promoting viral control and restricting inflammation within the respiratory tract during SARS-CoV-2 infection. IMPORTANCE SARS-CoV-2 has caused a historic pandemic of respiratory disease (COVID-19), and current evidence suggests that severe disease is associated with dysregulated immunity within the respiratory tract. However, the innate immune mechanisms that mediate protection during COVID-19 are not well defined. Here, we characterize a mouse model of SARS-CoV-2 infection and find that early CCR2-dependent infiltration of monocytes restricts the viral burden in the lung. We find that SARS-CoV-2 triggers an inflammatory response in the lung characterized by the expression of proinflammatory cytokines and interferon-stimulated genes. Using RNA sequencing and flow cytometry approaches, we demonstrate that SARS-CoV-2 infection leads to increases in circulating monocytes and an influx of CD45+ cells into the lung parenchyma that is dominated by monocyte-derived cells. Mechanistically, CCR2 signaling promoted the infiltration of classical monocytes into the lung and the expansion of monocyte-derived cells. Parenchymal monocyte-derived cells appear to play a protective role against MA-SARS-CoV-2, as mice lacking CCR2 showed higher viral loads in the lungs, increased lung viral dissemination, and elevated inflammatory cytokine responses. These studies have identified that the CCR2 pathway is critical for promoting viral control and restricting inflammation within the respiratory tract during SARS-CoV-2 infection.

Published
2021
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20. T cell restoration and control of hepatitis C virus replication after childbirth

Author

Coss, Samantha L., Torres-Cornejo, Almudena, Prasad, Mona R., Moore-Clingenpeel, Melissa, Grakoui, Arash, Lauer, Georg M., Walker, Christopher M., and Honegger, Jonathan R.

Subjects
Delivery (Childbirth) -- Comparative analysis -- Health aspects, Virus diseases -- Comparative analysis -- Health aspects, Infection -- Comparative analysis -- Health aspects, Hepatitis C virus -- Comparative analysis -- Health aspects, Virus replication -- Comparative analysis -- Health aspects, T cells -- Comparative analysis -- Health aspects, Antigens, Pregnancy, Viremia, Health care industry
Abstract

Chronic hepatitis C virus (HCV) infection is characterized by persistent high-level viremia and defective cellular immunity, including a lack of functional HCV-specific [CD4.sup.+] T cells. We previously described an exceptional period of viral control that occurs in some chronically infected women after childbirth. Here, we investigated whether reduced HCV replication after pregnancy is associated with recovery of [CD4.sup.+] T cell immunity. Class II tetramer analysis revealed significantly greater frequencies of circulating HCV-specific [CD4.sup.+] T cells at 3 months postpartum in women with concurrent declines in viremia compared with those with stable viremia. These HCV-specific [CD4.sup.+] T cells had an effector-memory phenotype. Inhibitory coreceptor expression on these cells corresponded to the degree of viral control. Circulating [CD4.sup.+] T cells produced IL-2 and IFN-[[gamma]] after HCV antigen stimulation, demonstrating Th1 functionality. These data provide direct evidence that the profound loss of HCV-specific [CD4.sup.+] T cell help that results in chronic infection is reversible following pregnancy, and this recovery of [CD4.sup.+] T cells is associated with at least transient control of persistent viral replication., Introduction Hepatitis C virus (HCV) infections persist indefinitely in approximately three-quarters of infected individuals, predisposing to late complications, including hepatic cirrhosis and hepatocellular carcinoma (1). One of the strongest predictors [...]

Published
2020
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21. Phenotype and fate of liver-resident CD8 T cells during acute and chronic hepacivirus infection

Author

Dravid, Piyush, primary, Murthy, Satyapramod, additional, Attia, Zayed, additional, Cassady, Cole, additional, Chandra, Rahul, additional, Trivedi, Sheetal, additional, Vyas, Ashish, additional, Gridley, John, additional, Holland, Brantley, additional, Kumari, Anuradha, additional, Grakoui, Arash, additional, Cullen, John M., additional, Walker, Christopher M., additional, Sharma, Himanshu, additional, and Kapoor, Amit, additional

Published
2023
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22. Translocation of gut commensal bacteria to the brain

Author

Thapa, Manoj, primary, Kumari, Anuradha, additional, Chin, Chui-Yoke, additional, Choby, Jacob, additional, Jin, Fengzhi, additional, Bogati, Bikash, additional, Chopyk, Daniel, additional, Koduri, Nitya, additional, Pahnke, Andrew, additional, Elrod, Elizabeth, additional, Burd, Eileen M., additional, Weiss, David S, additional, and Grakoui, Arash, additional

Published
2023
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23. Acetaminophen Intoxication Rapidly Induces Apoptosis of Intestinal Crypt Stem Cells and Enhances Intestinal Permeability

Author

Daniel M. Chopyk, Johnasha D. Stuart, Matthew G. Zimmerman, Jing Wen, Sanjeev Gumber, Mehul S. Suthar, Manoj Thapa, Mark J. Czaja, and Arash Grakoui

Subjects
Diseases of the digestive system. Gastroenterology, RC799-869
Abstract

Acetaminophen (APAP)‐induced liver injury is the most common cause of acute liver failure (ALF) in the Western world. APAP toxicity progresses to multiorgan dysfunction and thus has broader whole‐body implications. Importantly, greater 30‐day mortality has been observed in liver transplant recipients following ALF due to APAP‐related versus non‐APAP‐related causes. Reasons for this discrepancy have yet to be determined. Extrahepatic toxicities of APAP overdose may represent underappreciated and unaddressed comorbidities within this patient population. In the present study, rapid induction of apoptosis following APAP overdose was observed in the intestine, an organ that greatly influences the physiology of the liver. Strikingly, apoptotic cells appeared to be strictly restricted to the intestinal crypts. The use of leucine‐rich repeat‐containing G protein–coupled receptor 5 (LGR5) reporter mice confirmed that the LGR5‐positive (+) crypt base stem cells were disproportionately affected by APAP‐induced cell death. Although the apoptotic cells were cleared within 24 hours after APAP treatment, potentially long‐lived consequences on the intestine due to APAP exposure were indicated by prolonged deficits in gut barrier function. Moreover, small intestinal cell death was found to be independent of tumor necrosis factor receptor signaling and may represent a direct toxic insult to the intestine by exposure to high concentrations of APAP. Conclusion: APAP induces intestinal injury through a regulated process of apoptotic cell death that disproportionately affects LGR5+ stem cells. This work advances our understanding of the consequences of APAP toxicity in a novel organ that was not previously considered as a significant site of injury and thus presents potential new considerations for patient management.

Published
2019
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24. Alterations in Intestinal Microbiota Lead to Production of Interleukin 17 by Intrahepatic γδ T-Cell Receptor–Positive Cells and Pathogenesis of Cholestatic Liver Disease

Author

Tedesco, Dana, Thapa, Manoj, Chin, Chui Yoke, Ge, Yong, Gong, Minghao, Li, Jing, Gumber, Sanjeev, Speck, Patrick, Elrod, Elizabeth J., Burd, Eileen M., Kitchens, William H., Magliocca, Joseph F., Adams, Andrew B., Weiss, David S., Mohamadzadeh, Mansour, and Grakoui, Arash

Published
2018
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35. Western diet dampens T regulatory cell function to fuel hepatic inflammation in nonalcoholic fatty liver disease

Author

Chaudhary, Sudrishti, Rai, Ravi, Pal, Pabitra B., Tedesco, Dana, Singhi, Aatur D., Monga, Satdarshan P., Grakoui, Arash, Iyer, Smita S., and Raeman, Reben

Subjects
Article
Abstract

Background and aimsThe immunosuppressive T regulatory cells (Tregs) regulate immune responses and maintain immune homeostasis, yet their functions in nonalcoholic fatty liver disease (NAFLD) pathogenesis remains controversial.MethodsMice were fed a normal diet (ND) or a western diet (WD) for 16 weeks to induce NAFLD. Diphtheria toxin injection to deplete Tregs in Foxp3DTRmice or Treg induction therapy in WT mice to augment Treg numbers was initiated at twelve and eight weeks, respectively. Liver tissues from mice and NASH human subjects were analyzed by histology, confocal imaging, and qRT-PCR.ResultsWD triggered accumulation of adaptive immune cells, including Tregs and effector T cells, within the liver parenchyma. This pattern was also observed in NASH patients, where an increase in intrahepatic Tregs was noted. In the absence of adaptive immune cells in Rag1 KO mice, WD promoted accumulation of intrahepatic neutrophils and macrophages and exacerbated hepatic inflammation and fibrosis. Similarly, targeted Treg depletion exacerbated WD-induced hepatic inflammation and fibrosis. In Treg-depleted mice, hepatic injury was associated with increased accumulation of neutrophils, macrophages, and activated T cells within the liver. Conversely, induction of Tregs using recombinant IL2/αIL2 mAb cocktail reduced hepatic steatosis, inflammation, and fibrosis in WD-fed mice. Analysis of intrahepatic Tregs from WD-fed mice revealed a phenotypic signature of impaired Treg function in NAFLD.Ex vivofunctional studies showed that glucose and palmitate, but not fructose, impaired the immunosuppressive ability of Treg cells.ConclusionsOur findings indicate that the liver microenvironment in NAFLD impairs ability of Tregs to suppress effector immune cell activation, thus perpetuating chronic inflammation and driving NAFLD progression. These data suggest that targeted approaches aimed at restoring Treg function may represent a potential therapeutic strategy for treating NAFLD.Lay summaryIn this study, we elucidate the mechanisms contributing to the perpetuation of chronic hepatic inflammation in nonalcoholic fatty liver disease (NAFLD). We show that dietary sugar and fatty acids promote chronic hepatic inflammation in NAFLD by impairing immunosuppressive function of regulatory T cells. Finally, our preclinical data suggest that targeted approaches aimed at restoring T regulatory cell function have the potential to treat NAFLD.

Published
2023

36. Neutralization and receptor use of infectious culture–derived rat hepacivirus as a model for HCV

Author

Raphael Wolfisberg, Caroline E. Thorselius, Eduardo Salinas, Elizabeth Elrod, Sheetal Trivedi, Louise Nielsen, Ulrik Fahnøe, Amit Kapoor, Arash Grakoui, Charles M. Rice, Jens Bukh, Kenn Holmbeck, and Troels K. H. Scheel

Subjects
Mice, Viral Proteins, Hepatology, Animals, Hepacivirus, Mice, SCID, Hepatitis C Antibodies, Virus Replication, Hepatitis C, Rats
Abstract

Background and Aims: Lack of tractable immunocompetent animal models amenable to robust experimental challenge impedes vaccine efforts for HCV. Infection with rodent hepacivirus from Rattus norvegicus (RHV-rn1) in rats shares HCV-defining characteristics, including liver tropism, chronicity, and pathology. RHV in vitro cultivation would facilitate genetic studies on particle production, host factor interactions, and evaluation of antibody neutralization guiding HCV vaccine approaches. Approach and Results: We report an infectious reverse genetic cell culture system for RHV-rn1 using highly permissive rat hepatoma cells and adaptive mutations in the E2, NS4B, and NS5A viral proteins. Cell culture–derived RHV-rn1 particles (RHVcc) share hallmark biophysical characteristics of HCV and are infectious in mice and rats. Culture adaptive mutations attenuated RHVcc in immunocompetent rats, and the mutations reverted following prolonged infection, but not in severe combined immunodeficiency (SCID) mice, suggesting that adaptive immune pressure is a primary driver of reversion. Accordingly, sera from RHVcc-infected SCID mice or the early acute phase of immunocompetent mice and rats were infectious in culture. We further established an in vitro RHVcc neutralization assay, and observed neutralizing activity of rat sera specifically from the chronic phase of infection. Finally, we found that scavenger receptor class B type I promoted RHV-rn1 entry in vitro and in vivo. Conclusions: The RHV-rn1 infectious cell culture system enables studies of humoral immune responses against hepacivirus infection. Moreover, recapitulation of the entire RHV-rn1 infectious cycle in cell culture will facilitate reverse genetic studies and the exploration of tropism and virus–host interactions.

Published
2022

37. Early T follicular helper cell activity accelerates hepatitis C virus-specific B cell expansion

Author

Salinas, Eduardo, Boisvert, Maude, Upadhyay, Amit A., Bedard, Nathalie, Nelson, Sydney A., Bruneau, Julie, Derdeyn, Cynthia A., Marcotrigiano, Joseph, Evans, Matthew J., Bosinger, Steven E., Shoukry, Naglaa H., and Grakoui, Arash

Subjects
Glycoproteins -- Physiological aspects -- Health aspects, T cells -- Health aspects -- Physiological aspects, B cells -- Physiological aspects -- Health aspects, Hepatitis C -- Physiological aspects, Health care industry
Abstract

Early appearance of neutralizing antibodies during acute hepatitis C virus (HCV) infection is associated with spontaneous viral clearance. However, the longitudinal changes in antigen-specific memory B cell (MBCs) associated with divergent HCV infection outcomes remain undefined. We characterized longitudinal changes in E2 glycoprotein-specific MBCs from subjects who either spontaneously resolved acute HCV infection or progressed to chronic infection, using single-cell RNA-seq and functional assays. HCV-specific antibodies in plasma from chronically infected subjects recognized multiple E2 genotypes, while those from spontaneous resolvers exhibited variable cross-reactivity to heterotypic E2. E2-specific MBCs from spontaneous resolvers peaked early after infection (4-6 months), following expansion of activated circulating T follicular helper cells (cTfh) expressing interleukin 21. In contrast, E2-specific MBCs from chronically infected subjects, enriched in VH1-69, expanded during persistent infection (> 1 year), in the absence of significantly activated cTfh expansion. Early E2- specific MBCs from spontaneous resolvers produced monoclonal antibodies (mAbs) with fewer somatic hypermutations and lower E2 binding but similar neutralization as mAbs from late E2-specific MBCs of chronically infected subjects. These findings indicate that early cTfh activity accelerates expansion of E2-specific MBCs during acute infection, which might contribute to spontaneous clearance of HCV., Introduction Mechanisms of immune protection are not well defined for many rapidly evolving RNA viruses, such as HIV and hepatitis C virus (HCV), which affect millions worldwide without effective vaccines [...]

Published
2021
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39. Mechanotransduction in T Cell Development, Differentiation and Function

Author

Muaz Rushdi, Kaitao Li, Zhou Yuan, Stefano Travaglino, Arash Grakoui, and Cheng Zhu

Subjects
t cell antigen receptor, lymphocytes, thymocytes, catch bond, force, stiffness, Cytology, QH573-671
Abstract

Cells in the body are actively engaging with their environments that include both biochemical and biophysical aspects. The process by which cells convert mechanical stimuli from their environment to intracellular biochemical signals is known as mechanotransduction. Exemplifying the reliance on mechanotransduction for their development, differentiation and function are T cells, which are central to adaptive immune responses. T cell mechanoimmunology is an emerging field that studies how T cells sense, respond and adapt to the mechanical cues that they encounter throughout their life cycle. Here we review different stages of the T cell’s life cycle where existing studies have shown important effects of mechanical force or matrix stiffness on a T cell as sensed through its surface molecules, including modulating receptor−ligand interactions, inducing protein conformational changes, triggering signal transduction, amplifying antigen discrimination and ensuring directed targeted cell killing. We suggest that including mechanical considerations in the immunological studies of T cells would inform a more holistic understanding of their development, differentiation and function.

Published
2020
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40. Resolution of hepatitis E virus infection in CD8+ T cell-depleted rhesus macaques

Author

William G. Bremer, Xin Yin, Arash Grakoui, Zongdi Feng, Eduardo Salinas, Heather Blasczyk, and Christopher M. Walker

Subjects
0301 basic medicine, viruses, T cell, CD8-Positive T-Lymphocytes, Biology, medicine.disease_cause, Article, Virus, 03 medical and health sciences, 0302 clinical medicine, Immune system, Hepatitis E virus, medicine, Animals, Cytotoxic T cell, Hepatology, virus diseases, Haplorhini, Macaca mulatta, Virology, digestive system diseases, Hepatitis E, Disease Models, Animal, Chronic infection, 030104 developmental biology, medicine.anatomical_structure, Liver, Immunoglobulin G, biology.protein, 030211 gastroenterology & hepatology, Antibody, CD8
Abstract

Background & Aims HEV is a significant cause of acute hepatitis globally. Some genotypes establish persistent infection when immunity is impaired. Adaptive immune mechanisms that mediate resolution of infection have not been identified. Herein, the requirement for CD8+ T cells to control HEV infection was assessed in rhesus macaques, a model of acute and persistent HEV infection in humans. Methods Rhesus macaques were untreated or treated with depleting anti-CD8α monoclonal antibodies before challenge with an HEV genotype (gt)3 isolate derived from a chronically infected human patient. HEV replication, alanine aminotransferase, anti-capsid antibody and HEV-specific CD4+ and CD8+ T cell responses were assessed after infection. Results HEV control in untreated macaques coincided with the onset of a neutralizing IgG response against the ORF2 capsid and liver infiltration of functional HEV-specific CD4+ and CD8+ T cells. Virus control was delayed by 1 week in CD8+ T cell-depleted macaques. Infection resolved with onset of a neutralizing IgG antibody response and a much more robust expansion of CD4+ T cells with antiviral effector function. Conclusions Liver infiltration of functional CD8+ T cells coincident with HEV clearance in untreated rhesus macaques, and a 1-week delay in HEV clearance in CD8+ T cell-depleted rhesus macaques, support a role for this subset in timely control of virus replication. Resolution of infection in the absence of CD8+ T cells nonetheless indicates that neutralizing antibodies and/or CD4+ T cells may act autonomously to inhibit HEV replication. HEV susceptibility to multiple adaptive effector mechanisms may explain why persistence occurs only with generalized immune suppression. The findings also suggest that neutralizing antibodies and/or CD4+ T cells should be considered as a component of immunotherapy for chronic infection. Lay summary The hepatitis E virus (HEV) is a major cause of liver disease globally. Some genetic types (genotypes) of HEV persist in the body if immunity is impaired. Our objective was to identify immune responses that promote clearance of HEV. Findings indicate that HEV may be susceptible to multiple arms of the immune response that can act independently to terminate infection. They also provide a pathway to assess immune therapies for chronic HEV infection.

Published
2021

41. Memory in Repetitive Protein–Protein Interaction Series – in Memory of the Late Professor Robert M. Nerem

Author

Aaron M. Rosado, Yan Zhang, Hyun-Kyu Choi, Samuel M. Ehrlich, Fengzhi Jin, Arash Grakoui, Brian D. Evavold, and Cheng Zhu

Abstract

Over the past three decades, the senior author had interacted with and been mentored by the late Professor Robert M. Nerem. In his memory, the authors summarized several observations made, ideas conceptualized, and mathematical models developed during this period for quantitatively analyzing memory effects in repetitive protein–protein interactions (PPI). Interactions between proteins in an organism coordinate its biological processes and may impact its responses to changing environment and diseases through feedback systems. Feedback systems function by using changes in the past to influence behaviors in the future, which we refer here as memory. Specifically, we consider how proteins on cell or in isolation retain information about prior interactions to impact current interactions. The micropipette, biomembrane force probe and atomic force microscopic techniques were used to repeatedly assay several PPIs. The resulting time series were analyzed by a previous and two new models to extract three memory indices of short (seconds), intermediate (minutes), and long (hours) timescales. We found that interactions of cell membrane, but not soluble, T cell receptor (TCR) with peptide-major histocompatibility complex (pMHC) exhibits short-term memory that impacts on-rate, but not off-rate of the binding kinetics. Peptide dissociation from MHC resulted in intermediate- and long-term memories in TCR–pMHC interactions. However, we observed no changes in kinetic parameters by repetitive measurements on living cells over intermediate timescale using stable pMHCs. Parameters quantifying memory effects in PPIs could provide additional information regarding biological mechanisms. The methods developed herein also provide tools for future research.

Published
2022

42. Differential immune transcriptomic profiles between vaccinated and resolved HCV reinfected subjects

Author

Mazouz, Sabrina, primary, Salinas, Eduardo, additional, Bédard, Nathalie, additional, Filali, Ali, additional, Khedr, Omar, additional, Swadling, Leo, additional, Abdel-Hakeem, Mohamed S., additional, Siddique, Asiyah, additional, Barnes, Eleanor, additional, Bruneau, Julie, additional, Grakoui, Arash, additional, and Shoukry, Naglaa H., additional

Published
2022
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45. Erratum for Vanderheiden et al., “CCR2 Signaling Restricts SARS-CoV-2 Infection”

Author

Vanderheiden, Abigail, primary, Thomas, Jeronay, additional, Soung, Allison L., additional, Davis-Gardner, Meredith E., additional, Floyd, Katharine, additional, Jin, Fengzhi, additional, Cowan, David A., additional, Pellegrini, Kathryn, additional, Creanga, Adrian, additional, Pegu, Amarendra, additional, Derrien-Colemyn, Alexandrine, additional, Shi, Pei-Yong, additional, Grakoui, Arash, additional, Klein, Robyn S., additional, Bosinger, Steven E., additional, Kohlmeier, Jacob E., additional, Menachery, Vineet D., additional, and Suthar, Mehul S., additional

Published
2022
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48. Neutralization and receptor use of infectious culture–derived rat hepacivirus as a model for HCV

Author

Wolfisberg, Raphael, Thorselius, Caroline E., Salinas, Eduardo, Elrod, Elizabeth, Trivedi, Sheetal, Nielsen, Louise, Fahnøe, Ulrik, Kapoor, Amit, Grakoui, Arash, Rice, Charles M., Bukh, Jens, Holmbeck, Kenn, Scheel, Troels K.H., Wolfisberg, Raphael, Thorselius, Caroline E., Salinas, Eduardo, Elrod, Elizabeth, Trivedi, Sheetal, Nielsen, Louise, Fahnøe, Ulrik, Kapoor, Amit, Grakoui, Arash, Rice, Charles M., Bukh, Jens, Holmbeck, Kenn, and Scheel, Troels K.H.

Abstract

Background and Aims: Lack of tractable immunocompetent animal models amenable to robust experimental challenge impedes vaccine efforts for HCV. Infection with rodent hepacivirus from Rattus norvegicus (RHV-rn1) in rats shares HCV-defining characteristics, including liver tropism, chronicity, and pathology. RHV in vitro cultivation would facilitate genetic studies on particle production, host factor interactions, and evaluation of antibody neutralization guiding HCV vaccine approaches. Approach and Results: We report an infectious reverse genetic cell culture system for RHV-rn1 using highly permissive rat hepatoma cells and adaptive mutations in the E2, NS4B, and NS5A viral proteins. Cell culture–derived RHV-rn1 particles (RHVcc) share hallmark biophysical characteristics of HCV and are infectious in mice and rats. Culture adaptive mutations attenuated RHVcc in immunocompetent rats, and the mutations reverted following prolonged infection, but not in severe combined immunodeficiency (SCID) mice, suggesting that adaptive immune pressure is a primary driver of reversion. Accordingly, sera from RHVcc-infected SCID mice or the early acute phase of immunocompetent mice and rats were infectious in culture. We further established an in vitro RHVcc neutralization assay, and observed neutralizing activity of rat sera specifically from the chronic phase of infection. Finally, we found that scavenger receptor class B type I promoted RHV-rn1 entry in vitro and in vivo. Conclusions: The RHV-rn1 infectious cell culture system enables studies of humoral immune responses against hepacivirus infection. Moreover, recapitulation of the entire RHV-rn1 infectious cycle in cell culture will facilitate reverse genetic studies and the exploration of tropism and virus–host interactions.

Published
2022

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