Your search keyword '"Berrigan, Jacob"' showing total 18 results

1. Crimean-Congo hemorrhagic fever survivors elicit protective non-neutralizing antibodies that target 11 overlapping regions on glycoprotein GP38

Author

Shin, Olivia S., Monticelli, Stephanie R., Hjorth, Christy K., Hornet, Vladlena, Doyle, Michael, Abelson, Dafna, Kuehne, Ana I., Wang, Albert, Bakken, Russell R., Mishra, Akaash K., Middlecamp, Marissa, Champney, Elizabeth, Stuart, Lauran, Maurer, Daniel P., Li, Jiannan, Berrigan, Jacob, Barajas, Jennifer, Balinandi, Stephen, Lutwama, Julius J., Lobel, Leslie, Zeitlin, Larry, Walker, Laura M., Dye, John M., Chandran, Kartik, Herbert, Andrew S., Pauli, Noel T., and McLellan, Jason S.

Published

2024

2. Identification of potent inhibitors of SARS-CoV-2 infection by combined pharmacological evaluation and cellular network prioritization

Author

Patten, J.J., Keiser, Patrick T., Morselli-Gysi, Deisy, Menichetti, Giulia, Mori, Hiroyuki, Donahue, Callie J., Gan, Xiao, Valle, Italo do, Geoghegan-Barek, Kathleen, Anantpadma, Manu, Boytz, RuthMabel, Berrigan, Jacob L., Stubbs, Sarah H., Ayazika, Tess, O’Leary, Colin, Jalloh, Sallieu, Wagner, Florence, Ayehunie, Seyoum, Elledge, Stephen J., Anderson, Deborah, Loscalzo, Joseph, Zitnik, Marinka, Gummuluru, Suryaram, Namchuk, Mark N., Barabási, Albert-László, and Davey, Robert A.

Published

2022

3. Distinct pathways for evolution of enhanced receptor binding and cell entry in SARS-like bat coronaviruses.

Author

Tse, Alexandra L., Acreman, Cory M., Ricardo-Lax, Inna, Berrigan, Jacob, Lasso, Gorka, Balogun, Toheeb, Kearns, Fiona L., Casalino, Lorenzo, McClain, Georgia L., Chandran, Amartya Mudry, Lemeunier, Charlotte, Amaro, Rommie E., Rice, Charles M., Jangra, Rohit K., McLellan, Jason S., Chandran, Kartik, and Miller, Emily Happy

Subjects

PANDEMIC preparedness, VESICULAR stomatitis, COVID-19 pandemic, CELL receptors, CORONAVIRUSES

Abstract

Understanding the zoonotic risks posed by bat coronaviruses (CoVs) is critical for pandemic preparedness. Herein, we generated recombinant vesicular stomatitis viruses (rVSVs) bearing spikes from divergent bat CoVs to investigate their cell entry mechanisms. Unexpectedly, the successful recovery of rVSVs bearing the spike from SHC014-CoV, a SARS-like bat CoV, was associated with the acquisition of a novel substitution in the S2 fusion peptide-proximal region (FPPR). This substitution enhanced viral entry in both VSV and coronavirus contexts by increasing the availability of the spike receptor-binding domain to recognize its cellular receptor, ACE2. A second substitution in the S1 N–terminal domain, uncovered through the rescue and serial passage of a virus bearing the FPPR substitution, further enhanced spike:ACE2 interaction and viral entry. Our findings identify genetic pathways for adaptation by bat CoVs during spillover and host-to-host transmission, fitness trade-offs inherent to these pathways, and potential Achilles' heels that could be targeted with countermeasures. Author summary: The recent emergence of several highly virulent human coronaviruses, SARS-CoV, MERS-CoV and SARS-CoV-2, underscores the risk coronaviruses can pose to the human population. Bat coronaviruses (CoVs) are of particular concern due to their potential to adapt to new hosts. Here, we attempted to generate recombinant vesicular stomatitis viruses (rVSVs) bearing the spike glycoproteins from several SARS-like bat CoVs to study their cell entry mechanisms. We identified two mutations in the SHC014-CoV spike that afforded successful recovery of an rVSV bearing this spike by greatly increasing viral entry. Interestingly, these mutations occur outside the receptor-binding domain (RBD) but enhance spike-receptor interaction nevertheless. These and other results herein establish that these mutations serve to "open" the spike and thereby augment virus-receptor engagement. Our work uncovers new genetic pathways that could contribute to the adaptation of bat CoVs during host spillover. However, these mutations also render the spike more susceptible to neutralizing antibodies that recognize the RBD, pointing to fitness tradeoffs associated with these pathways. [ABSTRACT FROM AUTHOR]

Published

2024

4. Crimean-Congo Hemorrhagic Fever Survivors Elicit Protective Non-Neutralizing Antibodies that Target 11 Overlapping Regions on Viral Glycoprotein GP38

Author

Shin, Olivia S, primary, Monticelli, Stephanie R, additional, Hjorth, Christy K, additional, Hornet, Vladlena, additional, Doyle, Michael, additional, Abelson, Dafna, additional, Kuehne, Ana I, additional, Wang, Albert, additional, Bakken, Russell R, additional, Mishra, Akaash K, additional, Middlecamp, Marissa, additional, Champney, Elizabeth, additional, Stuart, Lauren, additional, Maurer, Daniel P, additional, Li, Jiannan, additional, Berrigan, Jacob L, additional, Balinandi, Stephen, additional, Lutwama, Julius J, additional, Lobel, Leslie, additional, Zeitlin, Larry, additional, Walker, Laura M, additional, Dye, John M, additional, Chandran, Kartik, additional, Herbert, Andrew S, additional, Pauli, Noel T, additional, and McLellan, Jason S, additional

Published

2024

5. Diminished Capsule Exacerbates Virulence, Blood–Brain Barrier Penetration, Intracellular Persistence, and Antibiotic Evasion of Hyperhemolytic Group B Streptococci

Author

Gendrin, Claire, Merillat, Sean, Vornhagen, Jay, Coleman, Michelle, Armistead, Blair, Ngo, Lisa, Aggarwal, Anjali, Quach, Phoenicia, Berrigan, Jacob, and Rajagopal, Lakshmi

Published

2018

6. CD169-mediated restrictive SARS-CoV-2 infection of macrophages induces pro-inflammatory responses

Author

Jalloh, Sallieu, primary, Olejnik, Judith, additional, Berrigan, Jacob, additional, Nisa, Annuurun, additional, Suder, Ellen L., additional, Akiyama, Hisashi, additional, Lei, Maohua, additional, Ramaswamy, Sita, additional, Tyagi, Sanjay, additional, Bushkin, Yuri, additional, Mühlberger, Elke, additional, and Gummuluru, Suryaram, additional

Published

2022

7. Identification of Druggable Host Targets Needed for SARS-CoV-2 Infection by Combined Pharmacological Evaluation and Cellular Network Directed Prioritization Both in vitro and in vivo

Author

Patten, J.J., primary, Keiser, Patrick T., additional, Gysi, Deisy, additional, Menichetti, Giulia, additional, Mori, Hiroyuki, additional, Donahue, Callie J., additional, Gan, Xiao, additional, do Valle, Italo, additional, Geoghegan-Barek, Kathleen, additional, Anantpadma, Manu, additional, Boytz, RuthMabel, additional, Berrigan, Jacob L., additional, Hulsey-Stubbs, Sarah, additional, Ayazika, Tess, additional, O’Leary, Colin, additional, Jalloh, Sallieu, additional, Wagner, Florence, additional, Ayehunie, Seyoum, additional, Elledge, Stephen J., additional, Anderson, Deborah, additional, Loscalzo, Joseph, additional, Zitnik, Marinka, additional, Gummuluru, Suryaram, additional, Namchuk, Mark N., additional, Barabási, Albert-László, additional, and Davey, Robert, additional

Published

2022

8. CD209L/L-SIGN and CD209/DC-SIGN Act as Receptors for SARS-CoV-2

Author

Amraei, Razie, primary, Yin, Wenqing, additional, Napoleon, Marc A., additional, Suder, Ellen L., additional, Berrigan, Jacob, additional, Zhao, Qing, additional, Olejnik, Judith, additional, Chandler, Kevin Brown, additional, Xia, Chaoshuang, additional, Feldman, Jared, additional, Hauser, Blake M., additional, Caradonna, Timothy M., additional, Schmidt, Aaron G., additional, Gummuluru, Suryaram, additional, Mühlberger, Elke, additional, Chitalia, Vipul, additional, Costello, Catherine E., additional, and Rahimi, Nader, additional

Published

2021

9. Identification of druggable host targets needed for SARS-CoV-2 infection by combined pharmacological evaluation and cellular network directed prioritization both in vitro and in vivo

Author

Patten, J.J., primary, Keiser, Patrick T., additional, Gysi, Deisy, additional, Menichetti, Giulia, additional, Mori, Hiroyuki, additional, Donahue, Callie J., additional, Gan, Xiao, additional, Valle, Italo do, additional, Geoghegan-Barek, Kathleen, additional, Anantpadma, Manu, additional, Boytz, RuthMabel, additional, Berrigan, Jacob L., additional, Hulsey-Stubbs, Sarah, additional, Ayazika, Tess, additional, O’Leary, Colin, additional, Jalloh, Sallieu, additional, Wagner, Florence, additional, Ayehunie, Seyoum, additional, Elledge, Stephen J., additional, Anderson, Deborah, additional, Loscalzo, Joseph, additional, Zitnik, Marinka, additional, Gummuluru, Suryaram, additional, Namchuk, Mark N., additional, Barabási, Albert-László, additional, and Davey, Robert A., additional

Published

2021

10. Novel ELISA Protocol Links Pre-Existing SARS-CoV-2 Reactive Antibodies With Endemic Coronavirus Immunity and Age and Reveals Improved Serologic Identification of Acute COVID-19 via Multi-Parameter Detection

Author

Yuen, Rachel R., primary, Steiner, Dylan, additional, Pihl, Riley M.F., additional, Chavez, Elizabeth, additional, Olson, Alex, additional, Smith, Erika L., additional, Baird, Lillia A., additional, Korkmaz, Filiz, additional, Urick, Patricia, additional, Sagar, Manish, additional, Berrigan, Jacob L., additional, Gummuluru, Suryaram, additional, Corley, Ronald B., additional, Quillen, Karen, additional, Belkina, Anna C., additional, Mostoslavsky, Gustavo, additional, Rifkin, Ian R., additional, Kataria, Yachana, additional, Cappione, Amedeo J., additional, Gao, Wenda, additional, Lin, Nina H., additional, Bhadelia, Nahid, additional, and Snyder-Cappione, Jennifer E., additional

Published

2021

11. SARS-CoV-2 reactive antibodies in unexposed individuals revealed by a high sensitivity, low noise serologic assay

Author

Yuen, Rachel R., primary, Steiner, Dylan, additional, Pihl, Riley M.F., additional, Chavez, Elizabeth, additional, Olson, Alex, additional, Baird, Lillia A., additional, Korkmaz, Filiz, additional, Urick, Patricia, additional, Sagar, Manish, additional, Berrigan, Jacob L., additional, Gummuluru, Suryaram, additional, Corley, Ronald B., additional, Quillen, Karen, additional, Belkina, Anna C., additional, Mostoslavsky, Gustavo, additional, Rifkin, Ian, additional, Kataria, Yachana, additional, Cappione, Amedeo J., additional, Lin, Nina H., additional, Bhadelia, Nahid, additional, and Snyder-Cappione, Jennifer E., additional

Published

2020

12. CD209L/L-SIGN and CD209/DC-SIGN act as receptors for SARS-CoV-2

Author

Amraei, Razie, primary, Yin, Wenqing, additional, Napoleon, Marc A., additional, Suder, Ellen L., additional, Berrigan, Jacob, additional, Zhao, Qing, additional, Olejnik, Judith, additional, Chandler, Kevin Brown, additional, Xia, Chaoshuang, additional, Feldman, Jared, additional, Hauser, Blake M., additional, Caradonna, Timothy M., additional, Schmidt, Aaron G., additional, Gummuluru, Suryaram, additional, Muhlberger, Elke, additional, Chitalia, Vipul, additional, Costello, Catherine E., additional, and Rahimi, Nader, additional

Published

2020

13. MPXV Infection Stimulates a More Robust and Durable Neutralizing Antibody Response Compared to MVA-BN Vaccination.

Author

Selverian CN, Monticelli SR, Jaleta YM, Lasso G, DeMouth ME, Meola A, Berrigan J, Batchelor TG, Battini L, Guardado-Calvo P, Herbert AS, Chandran K, Meyerowitz E, and Miller EH

Abstract

Monkeypox virus (MPXV) has recently caused a global disease outbreak in humans. Differences in the neutralizing antibody response to vaccination vs. MPXV infection remain poorly understood. Here, we examined the neutralization of MPXV and VACV by sera from a cohort of convalescent and vaccinated individuals at 1- and 8-months post-exposure. Convalescent individuals displayed higher neutralizing antibody titers against MPXV than vaccinated and MPXV-naïve persons at one-month post-exposure. Neutralizing antibody titers had waned significantly in both groups at 8 months. This study suggests additional vaccine strategies are needed to elicit a durable humoral response and prevent breakthrough infections., (© The Author(s) 2024. Published by Oxford University Press on behalf of Infectious Diseases Society of America. All rights reserved. For commercial re-use, please contact reprints@oup.com for reprints and translation rights for reprints. All other permissions can be obtained through our RightsLink service via the Permissions link on the article page on our site—for further information please contact journals.permissions@oup.com.)

Published

2024

14. Distinct pathway for evolution of enhanced receptor binding and cell entry in SARS-like bat coronaviruses.

Author

Tse AL, Acreman CM, Ricardo-Lax I, Berrigan J, Lasso G, Balogun T, Kearns FL, Casalino L, McClain GL, Chandran AM, Lemeunier C, Amaro RE, Rice CM, Jangra RK, McLellan JS, Chandran K, and Miller EH

Abstract

Understanding the zoonotic risks posed by bat coronaviruses (CoVs) is critical for pandemic preparedness. Herein, we generated recombinant vesicular stomatitis viruses (rVSVs) bearing spikes from divergent bat CoVs to investigate their cell entry mechanisms. Unexpectedly, the successful recovery of rVSVs bearing the spike from SHC014, a SARS-like bat CoV, was associated with the acquisition of a novel substitution in the S2 fusion peptide-proximal region (FPPR). This substitution enhanced viral entry in both VSV and coronavirus contexts by increasing the availability of the spike receptor-binding domain to recognize its cellular receptor, ACE2. A second substitution in the spike N-terminal domain, uncovered through forward-genetic selection, interacted epistatically with the FPPR substitution to synergistically enhance spike:ACE2 interaction and viral entry. Our findings identify genetic pathways for adaptation by bat CoVs during spillover and host-to-host transmission, fitness trade-offs inherent to these pathways, and potential Achilles' heels that could be targeted with countermeasures.

Published

2024

15. Crimean-Congo Hemorrhagic Fever Survivors Elicit Protective Non-Neutralizing Antibodies that Target 11 Overlapping Regions on Viral Glycoprotein GP38.

Author

Shin OS, Monticelli SR, Hjorth CK, Hornet V, Doyle M, Abelson D, Kuehne AI, Wang A, Bakken RR, Mishra A, Middlecamp M, Champney E, Stuart L, Maurer DP, Li J, Berrigan J, Barajas J, Balinandi S, Lutwama JJ, Lobel L, Zeitlin L, Walker LM, Dye JM, Chandran K, Herbert AS, Pauli NT, and McLellan JS

Abstract

Crimean-Congo hemorrhagic fever virus can cause lethal disease in humans yet there are no approved medical countermeasures. Viral glycoprotein GP38, unique to Nairoviridae , is a target of protective antibodies, but extensive mapping of the human antibody response to GP38 has not been previously performed. Here, we isolated 188 GP38-specific antibodies from human survivors of infection. Competition experiments showed that these antibodies bind across five distinct antigenic sites, encompassing eleven overlapping regions. Additionally, we reveal structures of GP38 bound with nine of these antibodies targeting different antigenic sites. Although GP38-specific antibodies were non-neutralizing, several antibodies were found to have protection equal to or better than murine antibody 13G8 in two highly stringent rodent models of infection. Together, these data expand our understanding regarding this important viral protein and inform the development of broadly effective CCHFV antibody therapeutics., Competing Interests: DECLARATION OF INTERESTS N.T.P., E.C., and J.L. are employees and shareholders of Adimab, LLC. D.P.M., L.M.W., O.S.S., V.H., and M.D. are shareholders of Adimab.

Published

2024

16. CD169-mediated restrictive SARS-CoV-2 infection of macrophages induces pro-inflammatory responses.

Author

Jalloh S, Olejnik J, Berrigan J, Nisa A, Suder EL, Akiyama H, Lei M, Tyagi S, Bushkin Y, Mühlberger E, and Gummuluru S

Abstract

Exacerbated and persistent innate immune response marked by pro-inflammatory cytokine expression is thought to be a major driver of chronic COVID-19 pathology. Although macrophages are not the primary target cells of SARS-CoV-2 infection in humans, viral RNA and antigens in activated monocytes and macrophages have been detected in post-mortem samples, and dysfunctional monocytes and macrophages have been hypothesized to contribute to a protracted hyper-inflammatory state in COVID-19 patients. In this study, we demonstrate that CD169, a myeloid cell specific I-type lectin, facilitated ACE2-independent SARS-CoV-2 fusion and entry in macrophages. CD169- mediated SARS-CoV-2 entry in macrophages resulted in expression of viral genomic and sub-genomic (sg) RNAs with minimal viral protein expression and no infectious viral particle release, suggesting a post-entry restriction of the SARS-CoV-2 replication cycle. Intriguingly this post-entry replication block was alleviated by exogenous ACE2 expression in macrophages. Restricted expression of viral gRNA and sgRNA in CD169 + macrophages elicited a pro-inflammatory cytokine expression (TNFα, IL-6 and IL-1β) in a RIG-I, MDA-5 and MAVS-dependent manner, which was suppressed by remdesivir pre- treatment. These findings suggest that de novo expression of SARS-CoV-2 RNA in macrophages contributes to the pro-inflammatory cytokine signature and that blocking CD169-mediated ACE2 independent infection and subsequent activation of macrophages by viral RNA might alleviate COVID-19-associated hyperinflammatory response., Author Summary: Over-exuberant production of pro-inflammatory cytokine expression by macrophages has been hypothesized to contribute to severity of COVID-19 disease. Molecular mechanisms that contribute to macrophage-intrinsic immune activation during SARS- CoV-2 infection are not fully understood. Here we show that CD169, a macrophage- specific sialic-acid binding lectin, facilitates abortive SARS-CoV-2 infection of macrophages that results in innate immune sensing of viral replication intermediates and production of proinflammatory responses. We identify an ACE2-independent, CD169- mediated endosomal viral entry mechanism that results in cytoplasmic delivery of viral capsids and initiation of virus replication, but absence of infectious viral production. Restricted viral replication in CD169 + macrophages and detection of viral genomic and sub-genomic RNAs by cytoplasmic RIG-I-like receptor family members, RIG-I and MDA5, and initiation of downstream signaling via the adaptor protein MAVS, was required for innate immune activation. These studies uncover mechanisms important for initiation of innate immune sensing of SARS-CoV-2 infection in macrophages, persistent activation of which might contribute to severe COVID-19 pathophysiology.

Published

2022

17. Identification of druggable host targets needed for SARS-CoV-2 infection by combined pharmacological evaluation and cellular network directed prioritization both in vitro and in vivo.

Author

Patten JJ, Keiser PT, Gysi D, Menichetti G, Mori H, Donahue CJ, Gan X, do Valle I, Geoghegan-Barek K, Anantpadma M, Boytz R, Berrigan JL, Hulsey-Stubbs S, Ayazika T, O'Leary C, Jalloh S, Wagner F, Ayehunie S, Elledge SJ, Anderson D, Loscalzo J, Zitnik M, Gummuluru S, Namchuk MN, Barabási AL, and Davey RA

Abstract

Identification of host factors contributing to replication of viruses and resulting disease progression remains a promising approach for development of new therapeutics. Here, we evaluated 6710 clinical and preclinical compounds targeting 2183 host proteins by immunocytofluorescence-based screening to identify SARS-CoV-2 infection inhibitors. Computationally integrating relationships between small molecule structure, dose-response antiviral activity, host target and cell interactome networking produced cellular networks important for infection. This analysis revealed 389 small molecules, >12 scaffold classes and 813 host targets with micromolar to low nanomolar activities. From these classes, representatives were extensively evaluated for mechanism of action in stable and primary human cell models, and additionally against Beta and Delta SARS-CoV-2 variants and MERS-CoV. One promising candidate, obatoclax, significantly reduced SARS-CoV-2 viral lung load in mice. Ultimately, this work establishes a rigorous approach for future pharmacological and computational identification of novel host factor dependencies and treatments for viral diseases.

Published

2022

18. CD209L/L-SIGN and CD209/DC-SIGN act as receptors for SARS-CoV-2.

Author

Amraei R, Yin W, Napoleon MA, Suder EL, Berrigan J, Zhao Q, Olejnik J, Chandler KB, Xia C, Feldman J, Hauser BM, Caradonna TM, Schmidt AG, Gummuluru S, Muhlberger E, Chitalia V, Costello CE, and Rahimi N

Abstract

As the COVID-19 pandemic continues to spread, investigating the processes underlying the interactions between SARS-CoV-2 and its hosts is of high importance. Here, we report the identification of CD209L/L-SIGN and the related protein CD209/DC-SIGN as receptors capable of mediating SARS-CoV-2 entry into human cells. Immunofluorescence staining of human tissues revealed prominent expression of CD209L in the lung and kidney epithelium and endothelium. Multiple biochemical assays using a purified recombinant SARS-CoV-2 spike receptor binding domain (S-RBD) or S1 encompassing both NTB and RBD and ectopically expressed CD209L and CD209 revealed that CD209L and CD209 interact with S-RBD. CD209L contains two N- glycosylation sequons, at sites N92 and N361, but we determined that only site N92 is occupied. Removal of the N -glycosylation at this site enhances the binding of S-RBD with CD209L. CD209L also interacts with ACE2, suggesting a role for heterodimerization of CD209L and ACE2 in SARS-CoV-2 entry and infection in cell types where both are present. Furthermore, we demonstrate that human endothelial cells are permissive to SARS-CoV-2 infection and interference with CD209L activity by knockdown strategy or with soluble CD209L inhibits virus entry. Our observations demonstrate that CD209L and CD209 serve as alternative receptors for SARS-CoV-2 in disease-relevant cell types, including the vascular system. This property is particularly important in tissues where ACE2 has low expression or is absent, and may have implications for antiviral drug development., Competing Interests: Conflict of interest: Authors declare no conflict of interest.

Published

2021