Your search keyword '"Sarah Sebastian"' showing total 43 results

1. Systemic prime mucosal boost significantly increases protective efficacy of bivalent RSV influenza viral vectored vaccine

Author

Cameron Bissett, Sandra Belij-Rammerstorfer, Marta Ulaszewska, Holly Smith, Reshma Kailath, Susan Morris, Claire Powers, Sarah Sebastian, Hannah R. Sharpe, Elizabeth R. Allen, Ziyin Wang, Robert F. Cunliffe, Hadijatou J. Sallah, Alexandra J. Spencer, Sarah Gilbert, John S. Tregoning, and Teresa Lambe

Subjects

Immunologic diseases. Allergy, RC581-607, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282

Abstract

Abstract Although licensed vaccines against influenza virus have been successful in reducing pathogen-mediated disease, they have been less effective at preventing viral infection of the airways and current seasonal updates to influenza vaccines do not always successfully accommodate viral drift. Most licensed influenza and recently licensed RSV vaccines are administered via the intramuscular route. Alternative immunisation strategies, such as intranasal vaccinations, and “prime-pull” regimens, may deliver a more sterilising form of protection against respiratory viruses. A bivalent ChAdOx1-based vaccine (ChAdOx1-NP + M1-RSVF) encoding conserved nucleoprotein and matrix 1 proteins from influenza A virus and a modified pre-fusion stabilised RSV A F protein, was designed, developed and tested in preclinical animal models. The aim was to induce broad, cross-protective tissue-resident T cells against heterotypic influenza viruses and neutralising antibodies against RSV in the respiratory mucosa and systemically. When administered via an intramuscular prime-intranasal boost (IM-IN) regimen in mice, superior protection was generated against challenge with either RSV A, Influenza A H3N2 or H1N1. These results support further clinical development of a pan influenza & RSV vaccine administered in a prime-pull regimen.

Published

2024

2. Potent immunogenicity and protective efficacy of a multi-pathogen vaccination targeting Ebola, Sudan, Marburg and Lassa viruse.

Author

Amy Flaxman, Sarah Sebastian, Sofia Appelberg, Kuan M Cha, Marta Ulaszewska, Jyothi Purushotham, Ciaran Gilbride, Hannah Sharpe, Alexandra J Spencer, Sagida Bibi, Daniel Wright, Isabel Schmidt, Stuart Dowall, Linda Easterbrook, Stephen Findlay-Wilson, Sarah Gilbert, Ali Mirazimi, and Teresa Lambe

Subjects

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

Abstract

Viral haemorrhagic fevers (VHF) pose a significant threat to human health. In recent years, VHF outbreaks caused by Ebola, Marburg and Lassa viruses have caused substantial morbidity and mortality in West and Central Africa. In 2022, an Ebola disease outbreak in Uganda caused by Sudan virus resulted in 164 cases with 55 deaths. In 2023, a Marburg disease outbreak was confirmed in Equatorial Guinea and Tanzania resulting in over 49 confirmed or suspected cases; 41 of which were fatal. There are no clearly defined correlates of protection against these VHF, impeding targeted vaccine development. Any vaccine developed should therefore induce strong and preferably long-lasting humoral and cellular immunity against these viruses. Ideally this immunity should also cross-protect against viral variants, which are known to circulate in animal reservoirs and cause human disease. We have utilized two viral vectored vaccine platforms, an adenovirus (ChAdOx1) and Modified Vaccinia Ankara (MVA), to develop a multi-pathogen vaccine regime against three filoviruses (Ebola virus, Sudan virus, Marburg virus) and an arenavirus (Lassa virus). These platform technologies have consistently demonstrated the capability to induce robust cellular and humoral antigen-specific immunity in humans, most recently in the rollout of the licensed ChAdOx1-nCoV19/AZD1222. Here, we show that our multi-pathogen vaccines elicit strong cellular and humoral immunity, induce a diverse range of chemokines and cytokines, and most importantly, confers protection after lethal Ebola virus, Sudan virus and Marburg virus challenges in a small animal model.

Published

2024

3. Effect of Prior ChAdOx1 COVID-19 Immunisation on T-Cell Responses to ChAdOx1-HBV

Author

Charlotte Davis, Dave Singh, Katie Anderson, Antonella Vardeu, Jakub Kopycinski, Alice Bridges-Webb, Alice Trickett, Susanne O’Brien, Matthew Downs, Randip Kaur, Radka Kolenovska, Louise Bussey, Kathryn Rutkowski, Sarah Sebastian, Tamsin Cargill, Eleanor Barnes, Thomas G. Evans, and Paola Cicconi

Subjects

hepatitis B, vaccine, T cell, Vaxzevria, Medicine

Abstract

There are varying data concerning the effect of prior anti-vector immunity on the T-cell response induced by immunisation with an identical vectored vaccine containing a heterologous antigen insert. To determine whether prior exposure to ChAdOx1-SARS-CoV2 immunisation (Vaxzevria®) impacts magnitudes of antigen-specific T-cell responses elicited by subsequent administration of the same viral vector (encoding HBV antigens, ChAdOx1-HBV), healthy volunteers that had received Vaxzevria® (n = 15) or the Pfizer or Moderna mRNA COVID-19 vaccine (n = 11) between 10 and 18 weeks prior were recruited to receive a single intramuscular injection of ChAdOx1-HBV. Anti-ChAdOx1-neutralising antibody titers were determined, and vector or insert-specific T-cell responses were measured by a gamma-interferon ELISpot and intracellular cytokine staining (ICS) assay using multiparameter flow cytometry. Participants were followed for three months after the ChAdOx1-HBV injection, which was well-tolerated, and no dropouts occurred. The baseline ChAdOx1 neutralisation titers were higher in the Vaxzevria® cohort (median of 848) than in the mRNA cohort (median of 25). T-cell responses to HBV antigens, measured by ELISpot, were higher on day 28 in the mRNA group (p = 0.013) but were similar between groups on day 84 (p = 0.441). By ICS, these differences persisted at the last time point. There was no clear correlation between the baseline responses to the adenoviral hexon and the subsequent ELISpot responses. As vaccination within 3 months using the same viral vector backbone affected the insert-specific T-cell responses, a greater interval after prior adenoviral immunisation using heterologous antigens may be warranted in settings in which these cells play critical roles.

Published

2024

4. Effectiveness of an eHealth intervention for reducing psychological distress and increasing COVID-19 knowledge and protective behaviors among racialized sexual and gender minority adults: A quasi-experimental study (#SafeHandsSafeHearts).

Author

Peter A Newman, Venkatesan Chakrapani, Notisha Massaquoi, Charmaine C Williams, Wangari Tharao, Suchon Tepjan, Surachet Roungprakhon, Joelleann Forbes, Sarah Sebastian, Pakorn Akkakanjanasupar, and Muna Aden

Subjects

Medicine, Science

Abstract

PurposeSexual and gender minority and racialized populations experienced heightened vulnerability during the Covid-19 pandemic. Marginalization due to structural homophobia, transphobia and racism, and resulting adverse social determinants of health that contribute to health disparities among these populations, were exacerbated by the Covid-19 pandemic and public health measures to control it. We developed and tested a tailored online intervention (#SafeHandsSafeHearts) to support racialized lesbian, gay, bisexual, transgender, queer, and other persons outside of heteronormative and cisgender identities (LGBTQ+) in Toronto, Canada during the pandemic.MethodsWe used a quasi-experimental pre-test post-test design to evaluate the effectiveness of a 3-session, peer-delivered eHealth intervention in reducing psychological distress and increasing Covid-19 knowledge and protective behaviors. Individuals ≥18-years-old, resident in Toronto, and self-identified as sexual or gender minority were recruited online. Depressive and anxiety symptoms, and Covid-19 knowledge and protective behaviors were assessed at baseline, 2-weeks postintervention, and 2-months follow-up. We used generalized estimating equations and zero-truncated Poisson models to evaluate the effectiveness of the intervention on the four primary outcomes.ResultsFrom March to November 2021, 202 participants (median age, 27 years [Interquartile range: 23-32]) were enrolled in #SafeHandsSafeHearts. Over half (54.5%, n = 110) identified as cisgender lesbian or bisexual women or women who have sex with women, 26.2% (n = 53) cisgender gay or bisexual men or men who have sex with men, and 19.3% (n = 39) transgender or nonbinary individuals. The majority (75.7%, n = 143) were Black and other racialized individuals. The intervention led to statistically significant reductions in the prevalence of clinically significant depressive (25.4% reduction, p < .01) and anxiety symptoms (16.6% reduction, p < .05), and increases in Covid-19 protective behaviors (4.9% increase, p < .05), from baseline to postintervention.ConclusionWe demonstrated the effectiveness of a brief, peer-delivered eHealth intervention for racialized LGBTQ+ communities in reducing psychological distress and increasing protective behaviors amid the Covid-19 pandemic. Implementation through community-based organizations by trained peer counselors supports feasibility, acceptability, and the importance of engaging racialized LGBTQ+ communities in pandemic response preparedness. This trial is registered with ClinicalTrials.gov, number NCT04870723.

Published

2024

5. 665 Immunotherapeutic trial in men with biochemical recurrence after definitive local therapy for prostate cancer: A clinical trial in progress

Author

Neal Shore, Robert Dreicer, Matthew Zibelman, Mark N Stein, Ralph J Hauke, Russell Pachynski, Bethan Jones, Jessica Hawley, Charlotte Davis, Katie Anderson, Antonella Vardeu, Margaret A Marshall, Vicky Wheeler, Sarah Sebastian, Kevin Kayvan Zarrabi, Brian Miles, and Jennifer Bendall

Subjects

Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282

Published

2023

6. HBV001: Phase I study evaluating the safety and immunogenicity of the therapeutic vaccine ChAdOx1-HBV

Author

Tamsin Cargill, Paola Cicconi, Anthony Brown, Louise Holland, Benaka Karanth, Kathryn Rutkowski, Emily Ashwin, Reena Mehta, Senthil Chinnakannan, Sarah Sebastian, Louise Bussey, Henrik Sorensen, Paul Klenerman, Thomas Evans, and Eleanor Barnes

Subjects

Hepatitis B, Vaccine, Chimpanzee adenovirus, Shark invariant chain, Diseases of the digestive system. Gastroenterology, RC799-869

Abstract

Background & Aims: Millions of people worldwide are infected chronically with HBV, which results in significant morbidity and mortality. Therapeutic vaccination is a strategy that aims to induce functional cure by restoring cellular immunity to HBV. Previously we have shown the candidate HBV immunotherapeutic vaccine ChAdOx1-HBV, encoding all major HBV antigens and a genetic adjuvant (shark invariant chain), is highly immunogenic in mice. Methods: Here we report the results of HBV001, a first-in-human, phase I, non-randomised, dose-escalation trial of ChAdOx1-HBV assessed in healthy volunteers and patients with chronic HBV (CHB). Results: Vaccination with a single dose of ChAdOx1-HBV was safe and well tolerated in both healthy and CHB cohorts. Vaccination induced high magnitude HBV-specific T cell responses against all major HBV antigens (core, polymerase, and surface) in healthy volunteers. Responses were detected but lower in patients with CHB. T cells generated by vaccination were cross-reactive between HBV C and D genotypes. Conclusions: ChAdOx1-HBV is safe and immunogenic in healthy volunteers and patients with CHB. In further studies, ChAdOx1-HBV will be used in combination with other therapeutic strategies with an aim to overcome the attenuated immunogenicity in patients with CHB. Impact and implications: Therapeutic vaccine ChAdOx1-HBV, a novel treatment for chronic hepatitis B infection (CHB), has been shown to be immunogenic in preclinical studies. In HBV001, a first-in-human phase I study, we show vaccination with ChAdOx1-HBV is safe and generates high magnitude T cell responses in healthy volunteers and lower levels of responses in patients with CHB. This is an important first step in the development of ChAdOx1-HBV as part of a wider therapeutic strategy to induce hepatitis B functional cure, and is of great interest to patients CHB and clinicians treating the condition. Clinical Trials Registration: This study is registered at ClinicalTrials.gov (NCT04297917).

Published

2023

7. Pre-Clinical Development of an Adenovirus Vector Based RSV and Shingles Vaccine Candidate

Author

Lawrence Petherbridge, Charlotte Davis, Angela Robinson, Thomas Evans, and Sarah Sebastian

Subjects

shingles, herpes zoster, chimpanzee adenovirus, glycoprotein E, prefusion F protein, viral vectored vaccine, Medicine

Abstract

Respiratory syncytial virus (RSV) infection and shingles are two viral diseases that affect older adults, and a combined vaccine to protect against both could be beneficial. RSV infection causes hospitalisations and significant morbidity in both children and adults and can be fatal in the elderly. The RSV fusion (F) envelope glycoprotein induces a strong RSV-neutralising antibody response and is the target of protective immunity in the first RSV vaccine for older adults, recently approved by the FDA. An initial childhood infection with the varicella zoster virus (VZV) results in chickenpox disease, but reactivation in older adults can cause shingles. This reactivation in sensory and autonomic neurons is characterized by a skin-blistering rash that can be accompanied by prolonged pain. The approved protein-in-adjuvant shingles vaccine induces VZV glycoprotein E (gE)-fspecific antibody and CD4+ T cell responses and is highly effective. Here we report the evaluation of RSV/shingles combination vaccine candidates based on non-replicating chimpanzee adenovirus (ChAd) vectors. We confirmed the cellular and humoral immunogenicity of the vaccine vectors in mice using T cell and antibody assays. We also carried out an RSV challenge study in cotton rats which demonstrated protective efficacy following a homologous prime-boost regimen with our preferred vaccine candidate.

Published

2023

8. Preclinical immunogenicity of an adenovirus-vectored vaccine for herpes zoster

Author

Marta Ulaszewska, Sarah Merelie, Sarah Sebastian, and Teresa Lambe

Subjects

herpes zoster, chimpanzee adenovirus, glycoprotein e, viral-vectored vaccine, varicella zoster virus, Immunologic diseases. Allergy, RC581-607, Therapeutics. Pharmacology, RM1-950

Abstract

Herpes zoster (HZ) results from waning immunity following childhood infection with varicella zoster virus (VZV) but is preventable by vaccination with recombinant HZ vaccine or live HZ vaccine (two doses or one dose, respectively). Vaccine efficacy declines with age, live HZ vaccine is contraindicated in immunosuppressed individuals, and severe local reactogenicity of recombinant HZ vaccine is seen in up to 20% of older adults, indicating a potential need for new vaccines. Nonreplicating chimpanzee adenovirus (ChAd) vectors combine potent immunogenicity with well-established reactogenicity and safety profiles. We evaluated the cellular and humoral immunogenicity of ChAdOx1 encoding VZV envelope glycoprotein E (ChAdOx1-VZVgE) in mice using IFN-γ ELISpot, flow cytometry with intracellular cytokine staining, and ELISA. In outbred CD-1 mice, one dose of ChAdOx1-VZVgE (1 × 107 infectious units) elicited higher gE-specific T cell responses than two doses of recombinant HZ vaccine (1 µg) or one dose of live HZ vaccine (1.3 × 103 plaque-forming units). Antibody responses were higher with two doses of recombinant HZ vaccine than with two doses of ChAdOx1-VZVgE or one dose of live HZ vaccine. ChAdOx1-VZVgE boosted T cell and antibody responses following live HZ vaccine priming. The frequencies of polyfunctional CD4+ and CD8+ T cells expressing more than one cytokine (IFN-γ, TNF-α and IL-2) were higher with ChAdOx1-VZVgE than with the conventional vaccines. Results were similar in young and aged BALB/c mice. These findings support the clinical development of ChAdOx1-VZVgE for prevention of HZ in adults aged 50 years or over, including those who have already received conventional vaccines.

Published

2023

9. Intravenous administration of viral vectors expressing prostate cancer antigens enhances the magnitude and functionality of CD8+ T cell responses

Author

Thomas Evans, Ian McDonald, Charlotte Davis, Katie Anderson, Antonella Vardeu, Guilherme Stahlberg, Barsha Thapa, Kinga Piotrowska, Margaret A Marshall, Vicky Wheeler, and Sarah Sebastian

Subjects

Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282

Abstract

Background The use of immunotherapeutic vaccination in prostate cancer is a promising approach that likely requires the induction of functional, cytotoxic T cells . The experimental approach described here uses a well-studied adenovirus-poxvirus heterologous prime-boost regimen, in which the vectors encode a combination of prostate cancer antigens, with the booster dose delivered by either the intravenous or intramuscular (IM) route. This prime-boost regimen was investigated for antigen-specific CD8+ T cell induction.Methods The coding sequences for four antigens expressed in prostate cancer, 5T4, PSA, PAP, and STEAP1, were inserted into replication-incompetent chimpanzee adenovirus Oxford 1 (ChAdOx1) and into replication-deficient modified vaccinia Ankara (MVA). In four strains of mice, ChAdOx1 prime was delivered intramuscularly, with an MVA boost delivered by either IM or intravenous routes. Immune responses were measured in splenocytes using ELISpot, multiparameter flow cytometry, and a targeted in vivo killing assay.Results The prime-boost regimen was highly immunogenic, with intravenous administration of the boost resulting in a sixfold increase in the magnitude of antigen-specific T cells induced and increased in vivo killing relative to the intramuscular boosting route. Prostate-specific antigen (PSA)-specific responses were dominant in all mouse strains studied (C57BL/6, BALBc, CD-1 and HLA-A2 transgenic).Conclusion This quadrivalent immunotherapeutic approach using four antigens expressed in prostate cancer induced high magnitude, functional CD8+ T cells in murine models. The data suggest that comparing the intravenous versus intramuscular boosting routes is worthy of investigation in humans.

Published

2022

10. ChAdOx1-vectored Lassa fever vaccine elicits a robust cellular and humoral immune response and protects guinea pigs against lethal Lassa virus challenge

Author

Robert J. Fischer, Jyothi N. Purushotham, Neeltje van Doremalen, Sarah Sebastian, Kimberly Meade-White, Kathleen Cordova, Michael Letko, M. Jeremiah Matson, Friederike Feldmann, Elaine Haddock, Rachel LaCasse, Greg Saturday, Teresa Lambe, Sarah C. Gilbert, and Vincent J. Munster

Subjects

Immunologic diseases. Allergy, RC581-607, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282

Abstract

Abstract Lassa virus (LASV) infects hundreds of thousands of individuals each year, highlighting the need for the accelerated development of preventive, diagnostic, and therapeutic interventions. To date, no vaccine has been licensed for LASV. ChAdOx1-Lassa-GPC is a chimpanzee adenovirus-vectored vaccine encoding the Josiah strain LASV glycoprotein precursor (GPC) gene. In the following study, we show that ChAdOx1-Lassa-GPC is immunogenic, inducing robust T-cell and antibody responses in mice. Furthermore, a single dose of ChAdOx1-Lassa-GPC fully protects Hartley guinea pigs against morbidity and mortality following lethal challenge with a guinea pig-adapted LASV (strain Josiah). By contrast, control vaccinated animals reached euthanasia criteria 10–12 days after infection. Limited amounts of LASV RNA were detected in the tissues of vaccinated animals. Viable LASV was detected in only one animal receiving a single dose of the vaccine. A prime-boost regimen of ChAdOx1-Lassa-GPC in guinea pigs significantly increased antigen-specific antibody titers and cleared viable LASV from the tissues. These data support further development of ChAdOx1-Lassa-GPC and testing in non-human primate models of infection.

Published

2021

11. Chimpanzee adenoviral vectors as vaccines for outbreak pathogens

Author

Katie Ewer, Sarah Sebastian, Alexandra J. Spencer, Sarah Gilbert, Adrian V. S. Hill, and Teresa Lambe

Subjects

vaccines, viral vectors, mers co-v, lassa fever, nipah, Immunologic diseases. Allergy, RC581-607, Therapeutics. Pharmacology, RM1-950

Abstract

The 2014–15 Ebola outbreak in West Africa highlighted the potential for large disease outbreaks caused by emerging pathogens and has generated considerable focus on preparedness for future epidemics. Here we discuss drivers, strategies and practical considerations for developing vaccines against outbreak pathogens. Chimpanzee adenoviral (ChAd) vectors have been developed as vaccine candidates for multiple infectious diseases and prostate cancer. ChAd vectors are safe and induce antigen-specific cellular and humoral immunity in all age groups, as well as circumventing the problem of pre-existing immunity encountered with human Ad vectors. For these reasons, such viral vectors provide an attractive platform for stockpiling vaccines for emergency deployment in response to a threatened outbreak of an emerging pathogen. Work is already underway to develop vaccines against a number of other outbreak pathogens and we will also review progress on these approaches here, particularly for Lassa fever, Nipah and MERS.

Published

2017

12. A single-dose ChAdOx1-vectored vaccine provides complete protection against Nipah Bangladesh and Malaysia in Syrian golden hamsters.

Author

Neeltje van Doremalen, Teresa Lambe, Sarah Sebastian, Trenton Bushmaker, Robert Fischer, Friederike Feldmann, Elaine Haddock, Michael Letko, Victoria A Avanzato, Ilona Rissanen, Rachel LaCasse, Dana Scott, Thomas A Bowden, Sarah Gilbert, and Vincent Munster

Subjects

Arctic medicine. Tropical medicine, RC955-962, Public aspects of medicine, RA1-1270

Abstract

Nipah virus (NiV) is a highly pathogenic re-emerging virus that causes outbreaks in South East Asia. Currently, no approved and licensed vaccine or antivirals exist. Here, we investigated the efficacy of ChAdOx1 NiVB, a simian adenovirus-based vaccine encoding NiV glycoprotein (G) Bangladesh, in Syrian hamsters. Prime-only as well as prime-boost vaccination resulted in uniform protection against a lethal challenge with NiV Bangladesh: all animals survived challenge and we were unable to find infectious virus either in oral swabs, lung or brain tissue. Furthermore, no pathological lung damage was observed. A single-dose of ChAdOx1 NiVB also prevented disease and lethality from heterologous challenge with NiV Malaysia. While we were unable to detect infectious virus in swabs or tissue of animals challenged with the heterologous strain, a very limited amount of viral RNA could be found in lung tissue by in situ hybridization. A single dose of ChAdOx1 NiVB also provided partial protection against Hendra virus and passive transfer of antibodies elicited by ChAdOx1 NiVB vaccination partially protected Syrian hamsters against NiV Bangladesh. From these data, we conclude that ChAdOx1 NiVB is a suitable candidate for further NiV vaccine pre-clinical development.

Published

2019

13. A Multi-Filovirus Vaccine Candidate: Co-Expression of Ebola, Sudan, and Marburg Antigens in a Single Vector

Author

Sarah Sebastian, Amy Flaxman, Kuan M. Cha, Marta Ulaszewska, Ciaran Gilbride, Hannah Sharpe, Edward Wright, Alexandra J. Spencer, Stuart Dowall, Roger Hewson, Sarah Gilbert, and Teresa Lambe

Subjects

Ebola, Marburg, filovirus, vaccine, viral vector, Medicine

Abstract

In the infectious diseases field, protective immunity against individual virus species or strains does not always confer cross-reactive immunity to closely related viruses, leaving individuals susceptible to disease after exposure to related virus species. This is a significant hurdle in the field of vaccine development, in which broadly protective vaccines represent an unmet need. This is particularly evident for filoviruses, as there are multiple family members that can cause lethal haemorrhagic fever, including Zaire ebolavirus, Sudan ebolavirus, and Marburg virus. In an attempt to address this need, both pre-clinical and clinical studies previously used mixed or co-administered monovalent vaccines to prevent filovirus mediated disease. However, these multi-vaccine and multi-dose vaccination regimens do not represent a practical immunisation scheme when considering the target endemic areas. We describe here the development of a single multi-pathogen filovirus vaccine candidate based on a replication-deficient simian adenoviral vector. Our vaccine candidate encodes three different filovirus glycoproteins in one vector and induces strong cellular and humoral immunity to all three viral glycoproteins after a single vaccination. Crucially, it was found to be protective in a stringent Zaire ebolavirus challenge in guinea pigs in a one-shot vaccination regimen. This trivalent filovirus vaccine offers a tenable vaccine product that could be rapidly translated to the clinic to prevent filovirus-mediated viral haemorrhagic fever.

Published

2020

14. The Design and Development of a Multi-HBV Antigen Encoded in Chimpanzee Adenoviral and Modified Vaccinia Ankara Viral Vectors; A Novel Therapeutic Vaccine Strategy against HBV

Author

Senthil K. Chinnakannan, Tamsin N. Cargill, Timothy A. Donnison, M. Azim Ansari, Sarah Sebastian, Lian Ni Lee, Claire Hutchings, Paul Klenerman, Mala K. Maini, Tom Evans, and Eleanor Barnes

Subjects

Hepatitis B virus (HBV), therapeutic HBV vaccine, T cell vaccine, chimpanzee adenovirus, ChAd, ChAdOx1, Medicine

Abstract

Chronic hepatitis B virus (HBV) infection affects 257 million people globally. Current therapies suppress HBV but viral rebound occurs on cessation of therapy; novel therapeutic strategies are urgently required. To develop a therapeutic HBV vaccine that can induce high magnitude T cells to all major HBV antigens, we have developed a novel HBV vaccine using chimpanzee adenovirus (ChAd) and modified vaccinia Ankara (MVA) viral vectors encoding multiple HBV antigens. ChAd vaccine alone generated very high magnitude HBV specific T cell responses to all HBV major antigens. The inclusion of a shark Invariant (SIi) chain genetic adjuvant significantly enhanced the magnitude of T-cells against HBV antigens. Compared to ChAd alone vaccination, ChAd-prime followed by MVA-boost vaccination further enhanced the magnitude and breadth of the vaccine induced T cell response. Intra-cellular cytokine staining study showed that HBV specific CD8+ and CD4+ T cells were polyfunctional, producing combinations of IFNγ, TNF-α, and IL-2. In summary, we have generated genetically adjuvanted ChAd and MVA vectored HBV vaccines with the potential to induce high-magnitude T cell responses through a prime-boost therapeutic vaccination approach. These pre-clinical studies pave the way for new studies of HBV therapeutic vaccination in humans with chronic hepatitis B infection.

Published

2020

15. Clinical Advances in Viral-Vectored Influenza Vaccines

Author

Sarah Sebastian and Teresa Lambe

Subjects

viral vectors, influenza, clinical trials, Medicine

Abstract

Influenza-virus-mediated disease can be associated with high levels of morbidity and mortality, particularly in younger children and older adults. Vaccination is the primary intervention used to curb influenza virus infection, and the WHO recommends immunization for at-risk individuals to mitigate disease. Unfortunately, influenza vaccine composition needs to be updated annually due to antigenic shift and drift in the viral immunogen hemagglutinin (HA). There are a number of alternate vaccination strategies in current development which may circumvent the need for annual re-vaccination, including new platform technologies such as viral-vectored vaccines. We discuss the different vectored vaccines that have been or are currently in clinical trials, with a forward-looking focus on immunogens that may be protective against seasonal and pandemic influenza infection, in the context of viral-vectored vaccines. We also discuss future perspectives and limitations in the field that will need to be addressed before new vaccines can significantly impact disease levels.

Published

2018

16. Phosphoinositide metabolism links cGMP-dependent protein kinase G to essential Ca²⁺ signals at key decision points in the life cycle of malaria parasites.

Author

Mathieu Brochet, Mark O Collins, Terry K Smith, Eloise Thompson, Sarah Sebastian, Katrin Volkmann, Frank Schwach, Lia Chappell, Ana Rita Gomes, Matthew Berriman, Julian C Rayner, David A Baker, Jyoti Choudhary, and Oliver Billker

Subjects

Biology (General), QH301-705.5

Abstract

Many critical events in the Plasmodium life cycle rely on the controlled release of Ca²⁺ from intracellular stores to activate stage-specific Ca²⁺-dependent protein kinases. Using the motility of Plasmodium berghei ookinetes as a signalling paradigm, we show that the cyclic guanosine monophosphate (cGMP)-dependent protein kinase, PKG, maintains the elevated level of cytosolic Ca²⁺ required for gliding motility. We find that the same PKG-dependent pathway operates upstream of the Ca²⁺ signals that mediate activation of P. berghei gametocytes in the mosquito and egress of Plasmodium falciparum merozoites from infected human erythrocytes. Perturbations of PKG signalling in gliding ookinetes have a marked impact on the phosphoproteome, with a significant enrichment of in vivo regulated sites in multiple pathways including vesicular trafficking and phosphoinositide metabolism. A global analysis of cellular phospholipids demonstrates that in gliding ookinetes PKG controls phosphoinositide biosynthesis, possibly through the subcellular localisation or activity of lipid kinases. Similarly, phosphoinositide metabolism links PKG to egress of P. falciparum merozoites, where inhibition of PKG blocks hydrolysis of phosphatidylinostitol (4,5)-bisphosphate. In the face of an increasing complexity of signalling through multiple Ca²⁺ effectors, PKG emerges as a unifying factor to control multiple cellular Ca²⁺ signals essential for malaria parasite development and transmission.

Published

2014

17. Effectiveness of an eHealth Intervention for Reducing Psychological Distress and Increasing COVID-19 Knowledge and Protective Behaviors among Ethnoracially Diverse Sexual and Gender Minority Adults: A Quasi-experimental Study (#SafeHandsSafeHearts)

Author

Peter A. Newman, Venkatesan Chakrapani, Notisha Massaquoi, Charmaine C. Williams, Wangari Tharao, Suchon Tepjan, Surachet Roungprakhon, Joelleann Forbes, Sarah Sebastian, Pakorn Akkakanjanasupar, and Muna Aden

Abstract

PurposeLesbian, gay, bisexual, transgender, queer, and other persons outside of heteronormative and cisgender identities (LGBTQ+) and ethnic/racial minority populations are at heightened vulnerability amid the Covid-19 pandemic. Systemic marginalization and resulting adverse social determinants of health contribute to health disparities among these populations that result in more severe consequences due to Covid-19 and the public health measures to control it. We developed and tested a tailored online intervention (#SafeHandsSafeHearts) to support ethnoracially diverse LGBTQ+ individuals in Toronto, Canada amid the pandemic.MethodsWe used a quasi-experimental pre-test post-test design to evaluate the effectiveness of a 3-session, peer-delivered eHealth intervention in reducing psychological distress and increasing Covid-19 knowledge and protective behaviors. Individuals ≥18-years-old, resident in Toronto, and self-identified as sexual or gender minority were recruited online. Depressive and anxiety symptoms, Covid-19 knowledge and protective behaviors were assessed at baseline, 2-weeks postintervention, and 2-months follow-up. We used generalized estimating equations and zero-truncated Poisson models to evaluate the effectiveness of the intervention on the four primary outcomes.ResultsFrom March to November 2021, 202 participants (median age, 27 years [Interquartile rage: 23-32]) were enrolled in #SafeHandsSafeHearts. Over half (54%, n=110) identified as cisgender lesbian or bisexual women or women who have sex with women, 26.2% (n=53) cisgender gay or bisexual men or men who have sex with men, and 19.3% (n=39) transgender or nonbinary individuals. The majority (75.7%, n=143) were Black and other people of color. The intervention led to statistically significant reductions in the prevalence of clinically significant depressive and anxiety symptoms, and increases in Covid-19 protective behaviors from baseline to postintervention.ConclusionWe demonstrated the effectiveness of a brief, peer-delivered eHealth intervention for ethnoracially diverse LGBTQ+ communities in reducing psychological distress and increasing protective behaviors amid the Covid-19 pandemic. Implementation through community-based health services with trained peer educators supports feasibility, acceptability, and the importance of engaging ethnoracially diverse LGBTQ+ communities in pandemic response preparedness. This trial is registered with ClinicalTrials.gov, numberNCT04870723.

Published

2023

18. Intravenous administration of viral vectors expressing prostate cancer antigens enhances the magnitude and functionality of CD8+ T cell responses

Author

Antonella Vardeu, Charlotte Davis, Ian McDonald, Guilherme Stahlberg, Barsha Thapa, Kinga Piotrowska, Margaret A Marshall, Thomas Evans, Vicky Wheeler, Sarah Sebastian, and Katie Anderson

Subjects

Male, Pharmacology, Cancer Research, Immunology, Prostatic Neoplasms, Vaccinia virus, Prostate-Specific Antigen, CD8-Positive T-Lymphocytes, Mice, Inbred C57BL, Mice, Oncology, Antigens, Neoplasm, Humans, Animals, Molecular Medicine, Immunology and Allergy, Administration, Intravenous, Oxidoreductases

Abstract

BackgroundThe use of immunotherapeutic vaccination in prostate cancer is a promising approach that likely requires the induction of functional, cytotoxic T cells . The experimental approach described here uses a well-studied adenovirus-poxvirus heterologous prime-boost regimen, in which the vectors encode a combination of prostate cancer antigens, with the booster dose delivered by either the intravenous or intramuscular (IM) route. This prime-boost regimen was investigated for antigen-specific CD8+ T cell induction.MethodsThe coding sequences for four antigens expressed in prostate cancer, 5T4, PSA, PAP, and STEAP1, were inserted into replication-incompetent chimpanzee adenovirus Oxford 1 (ChAdOx1) and into replication-deficient modified vaccinia Ankara (MVA). In four strains of mice, ChAdOx1 prime was delivered intramuscularly, with an MVA boost delivered by either IM or intravenous routes. Immune responses were measured in splenocytes using ELISpot, multiparameter flow cytometry, and a targeted in vivo killing assay.ResultsThe prime-boost regimen was highly immunogenic, with intravenous administration of the boost resulting in a sixfold increase in the magnitude of antigen-specific T cells induced and increased in vivo killing relative to the intramuscular boosting route. Prostate-specific antigen (PSA)-specific responses were dominant in all mouse strains studied (C57BL/6, BALBc, CD-1 and HLA-A2 transgenic).ConclusionThis quadrivalent immunotherapeutic approach using four antigens expressed in prostate cancer induced high magnitude, functional CD8+ T cells in murine models. The data suggest that comparing the intravenous versus intramuscular boosting routes is worthy of investigation in humans.

Published

2022

19. Revealing the voices of women living with IBD

Author

Susan Silver, Jordyn Perreault-Laird, and Sarah Sebastian

Subjects

digestive system diseases

Abstract

The purpose of this exploratory study is to center the voices of women who are living with inflammatory bowel disease (IBD) in order to understand their lived experiences and the kinds of support and resources they most value. Our review of the literature has indicated that studies which reveal the personal, lived, qualitative experiences with women with IBD are scarce. Instead, the existing body of research tends to be highly medicalized and expert-driven. In this study we constructed a sample of 20 YouTube videos posted by women living with Crohn's Disease and Ulcerative Colitis, who openly shared their experiences of living with the disease. Using phenomenology, coupled with an intersectional lens, we explored how living with IBD, was informed by gender, race, class and age. We hope to publish this exploratory work as a way to begin to address the gap in our understanding of the lived experiences with IBD.

Published

2021

20. ChAdOx1-vectored Lassa fever vaccine elicits a robust cellular and humoral immune response and protects guinea pigs against lethal Lassa virus challenge

Author

Sarah C. Gilbert, Vincent J. Munster, Greg Saturday, Neeltje van Doremalen, Rachel A. LaCasse, Elaine Haddock, Robert J. Fischer, Teresa Lambe, Jyothi N. Purushotham, Friederike Feldmann, Kathleen Cordova, Sarah Sebastian, Michael Letko, Kimberly Meade-White, and M. Jeremiah Matson

Subjects

0301 basic medicine, 2019-20 coronavirus outbreak, Severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2), viruses, 030231 tropical medicine, Immunology, Diseases, medicine.disease_cause, Microbiology, Article, 03 medical and health sciences, 0302 clinical medicine, Immune system, Virology, medicine, Pharmacology (medical), Lassa fever, RC254-282, Pharmacology, Vaccines, business.industry, Antibody titer, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, virus diseases, RC581-607, medicine.disease, 030104 developmental biology, Infectious Diseases, Lassa virus, Antibody response, Immunologic diseases. Allergy, business, Clearance

Abstract

Lassa virus (LASV) infects hundreds of thousands of individuals each year, highlighting the need for the accelerated development of preventive, diagnostic, and therapeutic interventions. To date, no vaccine has been licensed for LASV. ChAdOx1-Lassa-GPC is a chimpanzee adenovirus-vectored vaccine encoding the Josiah strain LASV glycoprotein precursor (GPC) gene. In the following study, we show that ChAdOx1-Lassa-GPC is immunogenic, inducing robust T-cell and antibody responses in mice. Furthermore, a single dose of ChAdOx1-Lassa-GPC fully protects Hartley guinea pigs against morbidity and mortality following lethal challenge with a guinea pig-adapted LASV (strain Josiah). By contrast, control vaccinated animals reached euthanasia criteria 10–12 days after infection. Limited amounts of LASV RNA were detected in the tissues of vaccinated animals. Viable LASV was detected in only one animal receiving a single dose of the vaccine. A prime-boost regimen of ChAdOx1-Lassa-GPC in guinea pigs significantly increased antigen-specific antibody titers and cleared viable LASV from the tissues. These data support further development of ChAdOx1-Lassa-GPC and testing in non-human primate models of infection.

Published

2020

21. A Multi-Filovirus Vaccine Candidate: Co-Expression of Ebola, Sudan, and Marburg Antigens in a Single Vector

Author

Stuart D. Dowall, Sarah Sebastian, Edward Wright, Sarah C. Gilbert, Hannah Sharpe, Marta Ulaszewska, Alexandra J. Spencer, Amy Flaxman, Roger Hewson, Teresa Lambe, Kuan M Cha, and Ciaran Gilbride

Subjects

0301 basic medicine, Zaire ebolavirus, filovirus, Immunology, Sudan ebolavirus, lcsh:Medicine, medicine.disease_cause, Article, Viral vector, Marburg virus, 03 medical and health sciences, Marburg, 0302 clinical medicine, Immunity, vaccine, Drug Discovery, medicine, Pharmacology (medical), 030212 general & internal medicine, Vector (molecular biology), Virus classification, Pharmacology, biology, viral vector, lcsh:R, biology.organism_classification, Virology, Vaccination, 030104 developmental biology, Infectious Diseases, Ebola

Abstract

In the infectious diseases field, protective immunity against individual virus species or strains does not always confer cross-reactive immunity to closely related viruses, leaving individuals susceptible to disease after exposure to related virus species. This is a significant hurdle in the field of vaccine development, in which broadly protective vaccines represent an unmet need. This is particularly evident for filoviruses, as there are multiple family members that can cause lethal haemorrhagic fever, including Zaire ebolavirus, Sudan ebolavirus, and Marburg virus. In an attempt to address this need, both pre-clinical and clinical studies previously used mixed or co-administered monovalent vaccines to prevent filovirus mediated disease. However, these multi-vaccine and multi-dose vaccination regimens do not represent a practical immunisation scheme when considering the target endemic areas. We describe here the development of a single multi-pathogen filovirus vaccine candidate based on a replication-deficient simian adenoviral vector. Our vaccine candidate encodes three different filovirus glycoproteins in one vector and induces strong cellular and humoral immunity to all three viral glycoproteins after a single vaccination. Crucially, it was found to be protective in a stringent Zaire ebolavirus challenge in guinea pigs in a one-shot vaccination regimen. This trivalent filovirus vaccine offers a tenable vaccine product that could be rapidly translated to the clinic to prevent filovirus-mediated viral haemorrhagic fever.

Published

2020

22. The Design and Development of a Multi-HBV Antigen Encoded in Chimpanzee Adenoviral and Modified Vaccinia Ankara Viral Vectors; A Novel Therapeutic Vaccine Strategy against HBV

Author

Mala K. Maini, Lian Ni Lee, Claire Hutchings, Eleanor Barnes, Tom Evans, M. Azim Ansari, Senthil Chinnakannan, Paul Klenerman, Sarah Sebastian, Timothy Donnison, and Tamsin Cargill

Subjects

0301 basic medicine, Modified vaccinia Ankara, T cell, Immunology, lcsh:Medicine, Virus, Article, Viral vector, 03 medical and health sciences, 0302 clinical medicine, Antigen, Drug Discovery, medicine, Pharmacology (medical), Hepatitis B virus (HBV), ChAdOx1, Pharmacology, T cell vaccine, ChAd, business.industry, lcsh:R, virus diseases, therapeutic HBV vaccine, MVA, Virology, chimpanzee adenovirus, digestive system diseases, Vaccination, 030104 developmental biology, Infectious Diseases, medicine.anatomical_structure, modified vaccinia Ankara, 030220 oncology & carcinogenesis, business, T-cell vaccine, CD8

Abstract

Chronic hepatitis B virus (HBV) infection affects 257 million people globally. Current therapies suppress HBV but viral rebound occurs on cessation of therapy; novel therapeutic strategies are urgently required. To develop a therapeutic HBV vaccine that can induce high magnitude T cells to all major HBV antigens, we have developed a novel HBV vaccine using chimpanzee adenovirus (ChAd) and modified vaccinia Ankara (MVA) viral vectors encoding multiple HBV antigens. ChAd vaccine alone generated very high magnitude HBV specific T cell responses to all HBV major antigens. The inclusion of a shark Invariant (SIi) chain genetic adjuvant significantly enhanced the magnitude of T-cells against HBV antigens. Compared to ChAd alone vaccination, ChAd-prime followed by MVA-boost vaccination further enhanced the magnitude and breadth of the vaccine induced T cell response. Intra-cellular cytokine staining study showed that HBV specific CD8+ and CD4+ T cells were polyfunctional, producing combinations of IFNγ, TNF-α, and IL-2. In summary, we have generated genetically adjuvanted ChAd and MVA vectored HBV vaccines with the potential to induce high-magnitude T cell responses through a prime-boost therapeutic vaccination approach. These pre-clinical studies pave the way for new studies of HBV therapeutic vaccination in humans with chronic hepatitis B infection.

Published

2020

23. Chimpanzee adenoviral vectors as vaccines for outbreak pathogens

Author

Adrian V. S. Hill, Sarah C. Gilbert, Alexandra J. Spencer, Sarah Sebastian, Katie J. Ewer, and Teresa Lambe

Subjects

0301 basic medicine, Pan troglodytes, viral vectors, viruses, Genetic Vectors, Immunology, Disease, Adenoviridae, West africa, Betacoronavirus, 03 medical and health sciences, parasitic diseases, Drug Discovery, medicine, Animals, Humans, Immunology and Allergy, Nipah, Lassa fever, Pharmacology, Drug Carriers, Vaccines, biology, Outbreak, medicine.disease, biology.organism_classification, Research Papers, MERS Co-V, Virology, 3. Good health, 030104 developmental biology, Geography, Preparedness

Abstract

The 2014–15 Ebola outbreak in West Africa highlighted the potential for large disease outbreaks caused by emerging pathogens and has generated considerable focus on preparedness for future epidemics. Here we discuss drivers, strategies and practical considerations for developing vaccines against outbreak pathogens. Chimpanzee adenoviral (ChAd) vectors have been developed as vaccine candidates for multiple infectious diseases and prostate cancer. ChAd vectors are safe and induce antigen-specific cellular and humoral immunity in all age groups, as well as circumventing the problem of pre-existing immunity encountered with human Ad vectors. For these reasons, such viral vectors provide an attractive platform for stockpiling vaccines for emergency deployment in response to a threatened outbreak of an emerging pathogen. Work is already underway to develop vaccines against a number of other outbreak pathogens and we will also review progress on these approaches here, particularly for Lassa fever, Nipah and MERS.

Published

2017

24. Pre-clinical development and assessment of viral vectors expressing a fusion antigen of P. falciparum LSA1 and LSAP2 for efficacy against liver-stage malaria

Author

Benedict R. Halbroth, Anita Gola, Adrian V. S. Hill, Chris J. Janse, Marta Ulaszewska, Ahmed M. Salman, Alexandra J. Spencer, Sarah Sebastian, Rhea J. Longley, and Shahid M. Khan

Subjects

0301 basic medicine, Recombinant Fusion Proteins, Immunology, T cells, malaria, Antigens, Protozoan, Vaccinia virus, Microbiology, Viral vector, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, Antigen, Malaria Vaccines, parasitic diseases, medicine, Animals, Humans, 030212 general & internal medicine, Vector (molecular biology), Drug Carriers, Immunity, Cellular, Mice, Inbred BALB C, Mice, Inbred ICR, Vaccines, Synthetic, biology, Malaria vaccine, liver stage, Plasmodium falciparum, vaccines, biology.organism_classification, medicine.disease, Virology, 3. Good health, Vaccination, Disease Models, Animal, Treatment Outcome, 030104 developmental biology, Infectious Diseases, chemistry, Vaccines, Subunit, Microbial Immunity and Vaccines, Adenoviruses, Simian, Female, Parasitology, Vaccinia, Malaria

Abstract

Despite promising progress in malaria vaccine development in recent years, an efficacious subunit vaccine against Plasmodium falciparum remains to be licensed and deployed. Cell-mediated protection from liver-stage malaria relies on a sufficient number of antigen-specific T cells reaching the liver during the time that parasites are present. A single vaccine expressing two antigens could potentially increase both the size and breadth of the antigen-specific response while halving vaccine production costs., Despite promising progress in malaria vaccine development in recent years, an efficacious subunit vaccine against Plasmodium falciparum remains to be licensed and deployed. Cell-mediated protection from liver-stage malaria relies on a sufficient number of antigen-specific T cells reaching the liver during the time that parasites are present. A single vaccine expressing two antigens could potentially increase both the size and breadth of the antigen-specific response while halving vaccine production costs. In this study, we investigated combining two liver-stage antigens, P. falciparum LSA1 (PfLSA1) and PfLSAP2, and investigated the induction of protective efficacy by coadministration of single-antigen vectors or vaccination with dual-antigen vectors, using simian adenovirus and modified vaccinia virus Ankara vectors. The efficacy of these vaccines was assessed in mouse malaria challenge models using chimeric P. berghei parasites expressing the relevant P. falciparum antigens and challenging mice at the peak of the T cell response. Vaccination with a combination of the single-antigen vectors expressing PfLSA1 or PfLSAP2 was shown to improve protective efficacy compared to vaccination with each single-antigen vector alone. Vaccination with dual-antigen vectors expressing both PfLSA1 and PfLSAP2 resulted in responses to both antigens, particularly in outbred mice, and most importantly, the efficacy was equivalent to that of vaccination with a mixture of single-antigen vectors. Based on these promising data, dual-antigen vectors expressing PfLSA1 and PfLSAP2 will now proceed to manufacturing and clinical assessment under good manufacturing practice (GMP) guidelines.

Published

2019

25. A single-dose ChAdOx1-vectored vaccine provides complete protection against Nipah Bangladesh and Malaysia in Syrian golden hamsters

Author

Sarah C. Gilbert, Rachel A. LaCasse, Vincent J. Munster, Ilona Rissanen, Dana P. Scott, Neeltje van Doremalen, Victoria A. Avanzato, Teresa Lambe, Elaine Haddock, Michael Letko, Thomas A. Bowden, Trenton Bushmaker, Robert S. Fischer, Friederike Feldmann, and Sarah Sebastian

Subjects

0301 basic medicine, Pulmonology, Physiology, RC955-962, Biochemistry, Geographical Locations, 0302 clinical medicine, Arctic medicine. Tropical medicine, Immune Physiology, Medicine and Health Sciences, Medicine, Public and Occupational Health, Enzyme-Linked Immunoassays, Henipavirus Infections, Mammals, Drug Carriers, Vaccines, Synthetic, Vaccines, Bangladesh, Immune System Proteins, biology, Immunogenicity, Viral Vaccine, Eukaryota, Vaccination and Immunization, 3. Good health, Vaccination, Infectious Diseases, Vertebrates, Hamsters, Female, Public aspects of medicine, RA1-1270, Research Article, Asia, Infectious Disease Control, 030231 tropical medicine, Immunology, Heterologous, Research and Analysis Methods, Rodents, Virus, Antibodies, 03 medical and health sciences, Animals, Hendra Virus, Immunoassays, Mesocricetus, business.industry, Public Health, Environmental and Occupational Health, Nipah Virus, Organisms, Malaysia, Outbreak, Animal Structures, Biology and Life Sciences, Proteins, Viral Vaccines, biology.organism_classification, Virology, Survival Analysis, Disease Models, Animal, 030104 developmental biology, Amniotes, People and Places, Respiratory Infections, Immunologic Techniques, Adenoviruses, Simian, Preventive Medicine, business

Abstract

Nipah virus (NiV) is a highly pathogenic re-emerging virus that causes outbreaks in South East Asia. Currently, no approved and licensed vaccine or antivirals exist. Here, we investigated the efficacy of ChAdOx1 NiVB, a simian adenovirus-based vaccine encoding NiV glycoprotein (G) Bangladesh, in Syrian hamsters. Prime-only as well as prime-boost vaccination resulted in uniform protection against a lethal challenge with NiV Bangladesh: all animals survived challenge and we were unable to find infectious virus either in oral swabs, lung or brain tissue. Furthermore, no pathological lung damage was observed. A single-dose of ChAdOx1 NiVB also prevented disease and lethality from heterologous challenge with NiV Malaysia. While we were unable to detect infectious virus in swabs or tissue of animals challenged with the heterologous strain, a very limited amount of viral RNA could be found in lung tissue by in situ hybridization. A single dose of ChAdOx1 NiVB also provided partial protection against Hendra virus and passive transfer of antibodies elicited by ChAdOx1 NiVB vaccination partially protected Syrian hamsters against NiV Bangladesh. From these data, we conclude that ChAdOx1 NiVB is a suitable candidate for further NiV vaccine pre-clinical development., Author summary Nipah virus was discovered in 1998 after an outbreak in Malaysia. Since then, several outbreaks have been reported in Bangladesh and India. Although most outbreaks are relatively small, a very high case-fatality rate is reported (75%). Furthermore, human-to-human transmission has been reported. Currently, no approved vaccine or countermeasure exist. In this manuscript, we discuss a vaccine based on a chimpanzee adenovirus. Importantly, the vaccine vector (ChAdOx1) is in clinical trials. In the work presented here, we show that this vaccine is fully protective against both genotypes of Nipah virus. Furthermore, we observe partial protection against Hendra virus, a related virus. Antibodies produced upon vaccination with our vaccine alone are partially protective against Nipah virus. This is an important step forwards towards the development of an approved vaccine for Nipah virus.

Published

2019

26. Development of a molecular adjuvant to enhance antigen-specific CD8+ T cell responses

Author

Benedict R. Halbroth, Sarah Sebastian, Hazel C. Poyntz, Migena Bregu, Matthew G. Cottingham, Adrian V. S. Hill, and Alexandra J. Spencer

Subjects

lcsh:R, lcsh:Medicine, lcsh:Q, lcsh:Science

Abstract

Despite promising progress in malaria vaccine development, an efficacious subunit vaccine against P. falciparum remains to be licensed and deployed. This study aimed to improve on the immunogenicity of the leading liver-stage vaccine candidate (ChAd63-MVA ME-TRAP), known to confer protection by eliciting high levels of antigen-specific CD8+ T cells. We previously showed fusion of ME-TRAP to the human MHC class II invariant chain (Ii) could enhance CD8+ T cell responses in non-human primates, but did not progress to clinical testing due to potential risk of auto-immunity by vaccination of humans with a self-antigen. Initial immunogenicity analyses of ME-TRAP fused to subdomains of the Ii showed that the Ii transmembrane domain alone can enhance CD8+ T cell responses. Subsequently, truncated Ii sequences with low homology to human Ii were developed and shown to enhance CD8+ T cell responses. By systematically mutating the TM domain sequence, multimerization of the Ii chain was shown to be important for immune enhancement. We subsequently identified several proteins from a variety of microbial pathogens with similar characteristics, that also enhance the CD8+ T cell response and could therefore be used in viral vector vaccines when potent cell mediated immunity is required.

Published

2018

27. The retroviral restriction factor TRIM5α

Author

Sarah Sebastian and Jeremy Luban

Subjects

Genetics, chemistry.chemical_classification, Apolipoprotein B, biology, Host (biology), Friend virus, Intracellular parasite, biology.organism_classification, Virology, Virus, Infectious Diseases, Enzyme, chemistry, biology.protein, Host factor, Restriction factor

Abstract

Retroviruses are obligate intracellular parasites that have coevolved with their hosts for millions of years. It is therefore not surprising that retroviruses take advantage of numerous host factors during their life cycle. In addition to positive cellular factors that are of use to the virus, host cells have also evolved intracellular proteins to antagonize the retroviral replication cycle. Such inhibitory cellular factors have been called retroviral restriction factors. Recently, several such restriction factors have been cloned, including Friend virus susceptibility factor 1, apolipoprotein B mRNA-editing enzyme catalytic proteins 3F and 3G, and ZAP. Here, we review the explosion of publications from the past 2 years concerning TRIM5, a host factor that potently inhibits HIV-1 and other retroviruses.

Published

2018

28. Clinical Advances in Viral-Vectored Influenza Vaccines

Author

Teresa Lambe and Sarah Sebastian

Subjects

0301 basic medicine, medicine.medical_specialty, viral vectors, Influenza vaccine, Immunology, Hemagglutinin (influenza), lcsh:Medicine, Context (language use), Disease, Review, Viral vector, 03 medical and health sciences, Drug Discovery, medicine, Pharmacology (medical), Intensive care medicine, Pharmacology, clinical trials, biology, business.industry, lcsh:R, Antigenic shift, Vaccination, 030104 developmental biology, Infectious Diseases, Immunization, biology.protein, business, influenza

Abstract

Influenza-virus-mediated disease can be associated with high levels of morbidity and mortality, particularly in younger children and older adults. Vaccination is the primary intervention used to curb influenza virus infection, and the WHO recommends immunization for at-risk individuals to mitigate disease. Unfortunately, influenza vaccine composition needs to be updated annually due to antigenic shift and drift in the viral immunogen hemagglutinin (HA). There are a number of alternate vaccination strategies in current development which may circumvent the need for annual re-vaccination, including new platform technologies such as viral-vectored vaccines. We discuss the different vectored vaccines that have been or are currently in clinical trials, with a forward-looking focus on immunogens that may be protective against seasonal and pandemic influenza infection, in the context of viral-vectored vaccines. We also discuss future perspectives and limitations in the field that will need to be addressed before new vaccines can significantly impact disease levels.

Published

2018

29. Recombinant modified vaccinia virus Ankara-based malaria vaccines

Author

Sarah C. Gilbert and Sarah Sebastian

Subjects

0301 basic medicine, viruses, Genetic Vectors, Immunology, Heterologous, Vaccinia virus, Biology, complex mixtures, Virus, law.invention, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, law, Malaria elimination, Malaria Vaccines, Drug Discovery, medicine, Humans, Pharmacology, Clinical Trials as Topic, Drug Carriers, Vaccines, Synthetic, Malaria vaccine, medicine.disease, Virology, 030104 developmental biology, chemistry, Recombinant DNA, Molecular Medicine, Vaccinia, Malaria, 030215 immunology

Abstract

A safe and effective malaria vaccine is a crucial part of the roadmap to malaria elimination/eradication by the year 2050. Viral-vectored vaccines based on adenoviruses and modified vaccinia virus Ankara (MVA) expressing malaria immunogens are currently being used in heterologous prime-boost regimes in clinical trials for induction of strong antigen-specific T-cell responses and high-titer antibodies. Recombinant MVA is a safe and well-tolerated attenuated vector that has consistently shown significant boosting potential. Advances have been made in large-scale MVA manufacture as high-yield producer cell lines and high-throughput purification processes have recently been developed. This review describes the use of MVA as malaria vaccine vector in both preclinical and clinical studies in the past 5 years.

Published

2015

30. Generation and Production of Modified Vaccinia Virus Ankara (MVA) as a Vaccine Vector

Author

Vincent, Pavot, Sarah, Sebastian, Alison V, Turner, Jake, Matthews, and Sarah C, Gilbert

Subjects

Recombination, Genetic, Cricetinae, Vaccines, DNA, Animals, Viral Vaccines, Chick Embryo, Fibroblasts, Vaccines, Attenuated, Cell Line

Abstract

The smallpox vaccine based on the vaccinia virus was successfully used to eradicate smallpox, but although very effective, it was a very reactogenic vaccine and responsible for the deaths of one to two people per million vaccinated. Modified Vaccinia virus Ankara (MVA) is an attenuated derivative, also used in the smallpox eradication campaign and now being developed as a recombinant viral vector to produce vaccines against infectious diseases and cancer. MVA can encode one or more foreign antigens and thus can function as a multivalent vaccine. The vector can be used at biosafety level 1, has intrinsic adjuvant properties, and induces humoral and cellular immune responses. Many clinical trials of these new vaccines have been conducted, and the safety of MVA is now well documented. Immunogenicity is influenced by the dose and vaccination regimen, and information on the efficacy of MVA-vectored vaccines is now beginning to accumulate. In this chapter, we provide protocols for generation, isolation, amplification, and purification of recombinant MVA for preclinical and clinical evaluation.

Published

2017

31. Generation and Production of Modified Vaccinia Virus Ankara (MVA) as a Vaccine Vector

Author

Sarah Sebastian, Sarah C. Gilbert, A Turner, Vincent Pavot, and Jake Matthews

Subjects

0301 basic medicine, business.industry, viruses, medicine.medical_treatment, Immunogenicity, medicine.disease, complex mixtures, Virology, Virus, Viral vector, Vaccination, 03 medical and health sciences, chemistry.chemical_compound, 030104 developmental biology, 0302 clinical medicine, chemistry, Medicine, Smallpox, 030212 general & internal medicine, Vaccinia, business, Smallpox vaccine, Adjuvant

Abstract

The smallpox vaccine based on the vaccinia virus was successfully used to eradicate smallpox, but although very effective, it was a very reactogenic vaccine and responsible for the deaths of one to two people per million vaccinated. Modified Vaccinia virus Ankara (MVA) is an attenuated derivative, also used in the smallpox eradication campaign and now being developed as a recombinant viral vector to produce vaccines against infectious diseases and cancer. MVA can encode one or more foreign antigens and thus can function as a multivalent vaccine. The vector can be used at biosafety level 1, has intrinsic adjuvant properties, and induces humoral and cellular immune responses. Many clinical trials of these new vaccines have been conducted, and the safety of MVA is now well documented. Immunogenicity is influenced by the dose and vaccination regimen, and information on the efficacy of MVA-vectored vaccines is now beginning to accumulate. In this chapter, we provide protocols for generation, isolation, amplification, and purification of recombinant MVA for preclinical and clinical evaluation.

Published

2017

32. A Plasmodium Calcium-Dependent Protein Kinase Controls Zygote Development and Transmission by Translationally Activating Repressed mRNAs

Author

Matthew L. Jones, Oliver Billker, Frank Schwach, Julian C. Rayner, David Goulding, Jyoti S. Choudhary, Mathieu Brochet, Sarah Sebastian, and Mark O. Collins

Subjects

Male, Cancer Research, Plasmodium berghei, Zygote, Cell- och molekylärbiologi, Protozoan Proteins, Motility, Myosins, Microbiology, Mice, 03 medical and health sciences, Immunology and Microbiology(all), Virology, parasitic diseases, Protein biosynthesis, Animals, RNA, Messenger, Promoter Regions, Genetic, 3' Untranslated Regions, Molecular Biology, 030304 developmental biology, 0303 health sciences, Messenger RNA, Gene knockdown, biology, Three prime untranslated region, Kinase, 030302 biochemistry & molecular biology, biology.organism_classification, Molecular biology, 3. Good health, Cell biology, Culicidae, Gene Knockdown Techniques, Protein Biosynthesis, Female, Parasitology, 5' Untranslated Regions, Protein Kinases, Cell and Molecular Biology

Abstract

SummaryCalcium-dependent protein kinases (CDPKs) play key regulatory roles in the life cycle of the malaria parasite, but in many cases their precise molecular functions are unknown. Using the rodent malaria parasite Plasmodium berghei, we show that CDPK1, which is known to be essential in the asexual blood stage of the parasite, is expressed in all life stages and is indispensable during the sexual mosquito life-cycle stages. Knockdown of CDPK1 in sexual stages resulted in developmentally arrested parasites and prevented mosquito transmission, and these effects were independent of the previously proposed function for CDPK1 in regulating parasite motility. In-depth translational and transcriptional profiling of arrested parasites revealed that CDPK1 translationally activates mRNA species in the developing zygote that in macrogametes remain repressed via their 3′ and 5′UTRs. These findings indicate that CDPK1 is a multifunctional protein that translationally regulates mRNAs to ensure timely and stage-specific protein expression.

Published

2012

33. A Tetracycline-Repressible Transactivator System to Study Essential Genes in Malaria Parasites

Author

EunBin Arin Kim, Elyse Kozlowski, Manuel Llinás, Katrin Volkmann, Sarah Sebastian, Oliver Billker, Mathieu Brochet, Paco Pino, Erin C. Bush, and Dominique Soldati-Favre

Subjects

Resource, Genetics, Microbial, Cancer Research, Plasmodium berghei, Cell- och molekylärbiologi, Genes, Protozoan, Plasmodium falciparum, Microbiology, 03 medical and health sciences, Transactivation, Protein acylation, Immunology and Microbiology(all), Virology, parasitic diseases, Gene, Transcription factor, Molecular Biology, 030304 developmental biology, Regulation of gene expression, Genetics, ddc:616, 0303 health sciences, Genes, Essential, biology, 030306 microbiology, Tetracycline, biology.organism_classification, 3. Good health, Profilin, Gene Expression Regulation, biology.protein, Trans-Activators, Parasitology, Toxoplasma, Cell and Molecular Biology

Abstract

Summary A major obstacle in analyzing gene function in apicomplexan parasites is the absence of a practical regulatable expression system. Here, we identified functional transcriptional activation domains within Apicomplexan AP2 (ApiAP2) family transcription factors. These ApiAP2 transactivation domains were validated in blood-, liver-, and mosquito-stage parasites and used to create a robust conditional expression system for stage-specific, tetracycline-dependent gene regulation in Toxoplasma gondii, Plasmodium berghei, and Plasmodium falciparum. To demonstrate the utility of this system, we created conditional knockdowns of two essential P. berghei genes: profilin (PRF), a protein implicated in parasite invasion, and N-myristoyltransferase (NMT), which catalyzes protein acylation. Tetracycline-induced repression of PRF and NMT expression resulted in a dramatic reduction in parasite viability. This efficient regulatable system will allow for the functional characterization of essential proteins that are found in these important parasites., Highlights ► Transactivating regions within Apicomplexan AP2 family transcription factors identified ► Design of a TetRep-inducible system based on ApiAP2-derived activating domains ► Conditional disruption of the essential profilin gene validates the inducible system ► Depletion of N-myristoyltransferase activity severely hampers parasite development

Published

2012

34. The role of lysine 186 in HIV-1 integrase multimerization

Author

Mark A. Muesing, Lionel Berthoux, Sarah Sebastian, and Jeremy Luban

Subjects

Models, Molecular, Mutant, HIV Integrase, In Vitro Techniques, Virus Replication, Article, Cell Line, Jurkat Cells, chemistry.chemical_compound, Protein structure, Tetramer, Two-Hybrid System Techniques, Complementary DNA, Virology, Humans, Protein Structure, Quaternary, Base Sequence, biology, Lysine, Mutagenesis, Molecular biology, Integrase, Cell biology, Amino Acid Substitution, chemistry, Viral replication, DNA, Viral, HIV-1, Mutagenesis, Site-Directed, biology.protein, DNA, HeLa Cells

Abstract

HIV-1 integrase (IN) catalyzes biochemical reactions required for viral cDNA insertion into host cell chromosomal DNA, an essential step in the HIV-1 replication cycle. In one of these reactions, the two ends of the linear viral cDNA are believed to be simultaneously ligated to chromosomal DNA by a tetrameric form of IN. The structure of the full-length IN tetramer is not known but a model consisting of the N-terminal domain and the catalytic core revealed basic residues 186 to 188 at the interface between the two IN dimers. We found that alteration of these residues, in particular changing IN lysine residue 186 to glutamate (K186Q), impairs IN oligomerization in the yeast two-hybrid system and decreases oligomeric forms of IN within virions. When expressed independently of other viral proteins in human cells, IN-K186Q did not concentrate in the nucleus as did wild-type IN. Co-expression of wild-type IN restored the multimerization defects of IN-K186Q, in both the two-hybrid system and in virions, and also rescued the nuclear targeting defects. Virions bearing IN-K186Q were not infectious in a single cycle of replication but when mixed virions containing two different IN mutants were produced, IN-K186Q was capable of complementing the catalytically inactive mutant IN-D116A. Our biochemical and functional data support the crystallographic model in which IN residue K186 lies at the interface between IN dimers and suggest that tetramerization is important, not only for concerted integration, but also for IN nuclear targeting.

Published

2007

35. Arsenic Counteracts Human Immunodeficiency Virus Type 1 Restriction by Various TRIM5 Orthologues in a Cell Type-Dependent Manner

Author

Jeremy Luban, Sarah Sebastian, and Elena Sokolskaja

Subjects

Cell type, DNA, Complementary, Ubiquitin-Protein Ligases, Immunology, Context (language use), Biology, Microbiology, Cercopithecus aethiops, Arsenicals, Virus, Cell Line, Antiviral Restriction Factors, Tripartite Motif Proteins, Arsenic Trioxide, Transduction, Genetic, RNA interference, Virology, Chlorocebus aethiops, Animals, Humans, Gene Silencing, Infectivity, Gene knockdown, virus diseases, Oxides, Fibroblasts, Macaca mulatta, Molecular biology, Virus-Cell Interactions, Aotus trivirgatus, Cell culture, Insect Science, Cats, HIV-1, RNA Interference, Carrier Proteins

Abstract

Arsenic trioxide (As 2 O 3 ) increased human immunodeficiency virus type 1 (HIV-1) infectivity when particular Homo sapiens and Cercopithecus aethiops cell lines were used as targets. Knockdown of human TRIM5α by RNA interference eliminated the As 2 O 3 effect, demonstrating that the drug acts by modulating the activity of this retroviral restriction factor. In contrast, HIV-1 infectivity in target cell lines from other primate species ( Cercopithecus tantalus , Macaca mulatta , and Aotus trivirgatus ) was not increased by As 2 O 3 , despite the potent TRIM5-dependent HIV-1 restriction activity that these cells exhibit. To determine if As 2 O 3 responsiveness is characteristic of particular TRIM5 orthologues and not others, TRIM5 cDNAs from these five primate species were transduced into cat fibroblasts, which lack endogenous HIV-1 restriction activity and, therefore, responsiveness to As 2 O 3 . In this context, the HIV-1 restriction activity conferred by all TRIM5 orthologues was largely eliminated by As 2 O 3 . The effect of As 2 O 3 on HIV-1 restriction is thus shared by different TRIM5 orthologues but dependent on factors specific to the cell line in which TRIM5 is expressed.

Published

2006

36. Disruption of Human TRIM5α Antiviral Activity by Nonhuman Primate Orthologues

Author

Jeremy Luban, David M. Sayah, Sarah Sebastian, and Lionel Berthoux

Subjects

Gene isoform, Recombinant Fusion Proteins, Ubiquitin-Protein Ligases, viruses, Immunology, Cellular Response to Infection, Biology, Transfection, Antiviral Agents, Microbiology, Virus, Antiviral Restriction Factors, Tripartite Motif Proteins, Mice, Cyclophilin A, Cell Line, Tumor, Virology, Murine leukemia virus, Animals, Humans, Gene, Cyclophilin, Proteins, Haplorhini, biology.organism_classification, Macaca mulatta, Leukemia Virus, Murine, Insect Science, HIV-1, biology.protein, Aotidae, TRIM5alpha, Heterologous expression, Carrier Proteins, Dimerization

Abstract

TRIM5 is a determinant of species-specific differences in susceptibility to infection by retroviruses bearing particular capsids. Human immunodeficiency virus type 1 (HIV-1) infection is blocked by the alpha isoform of macaque TRIM5 (TRIM5α rh ) or by the product of the owl monkey TRIM5-cyclophilin A gene fusion (TRIMCyp). Human TRIM5α potently restricts specific strains of murine leukemia virus (N-MLV) but has only a modest effect on HIV-1. The amino termini of TRIM5 orthologues are highly conserved and possess a coiled-coil domain that promotes homomultimerization. Here we show that heterologous expression of TRIM5α rh or TRIMCyp in human cells interferes with the anti-N-MLV activity of endogenous human TRIM5α (TRIM5α hu ). Deletion of the cyclophilin domain from TRIMCyp has no effect on heteromultimerization or colocalization with TRIM5α hu but prevents interference with anti-N-MLV activity. These data demonstrate that TRIM5 orthologues form heteromultimers and indicate that C-terminal extensions alter virus recognition by multimers of these proteins.

Published

2005

37. HIV-1 Vpr Induces Defects in Mitosis, Cytokinesis, Nuclear Structure, and Centrosomes

Author

Fred Chang, Sarah Sebastian, Fabio Re, Jeremy Luban, and Shelley Sazer

Subjects

G2 Phase, Umbilical Veins, Saccharomyces cerevisiae Proteins, Time Factors, viruses, Mitosis, Cell Cycle Proteins, Spindle Apparatus, Polo-like kinase, Protein Serine-Threonine Kinases, Biology, Transfection, Spindle pole body, Schizosaccharomyces, Drosophila Proteins, Humans, Molecular Biology, Cells, Cultured, Cell Nucleus, Centrosome, Gene Products, vpr, Cell Cycle, Polo kinase, Articles, Cell Biology, Cell cycle, Spindle apparatus, Cell biology, Checkpoint Kinase 2, Mutation, Cell Division, Cytokinesis, HeLa Cells, Plasmids

Abstract

Human immunodeficiency virus type 1 (HIV-1) Vpr is a 15-kDa accessory protein that contributes to several steps in the viral replication cycle and promotes virus-associated pathology. Previous studies demonstrated that Vpr inhibits G2/M cell cycle progression in both human cells and in the fission yeast Schizosaccharomyces pombe. Here, we report that, upon induction of vpr expression, fission yeast exhibited numerous defects in the assembly and function of the mitotic spindle. In particular, two spindle pole body proteins, sad1p and the polo kinase plo1p, were delocalized in vpr-expressing yeast cells, suggesting that spindle pole body integrity was perturbed. In addition, nuclear envelope structure, contractile actin ring formation, and cytokinesis were also disrupted. Similar Vpr-induced defects in mitosis and cytokinesis were observed in human cells, including aberrant mitotic spindles, multiple centrosomes, and multinucleate cells. These defects in cell division and centrosomes might account for some of the pathological effects associated with HIV-1 infection.

Published

2004

38. Phosphoinositide Metabolism Links cGMP-Dependent Protein Kinase G to Essential Ca2+ Signals at Key Decision Points in the Life Cycle of Malaria Parasites

Author

Mark O. Collins, Jyoti S. Choudhary, Frank Schwach, David A. Baker, Oliver Billker, Mathieu Brochet, Sarah Sebastian, Eloise Thompson, Terry K. Smith, Julian C. Rayner, Katrin Volkmann, Lia Chappell, Ana Rita Gomes, and Matthew Berriman

Subjects

Gliding motility, Pathogenesis, Signal transduction, Phosphatidylinositols, Molecular cell biology, Crosstalk, Second Messenger System, Calcium signaling, biology, Protein Kinase Signaling Cascade, Kinase, General Neuroscience, Mechanisms of Signal Transduction, Signaling Cascades, 3. Good health, Cell biology, Cyclic GMP-Dependent Protein Kinases, Host-Pathogen Interaction, Biochemistry, cardiovascular system, General Agricultural and Biological Sciences, Research Article, Signaling in cellular processes, Plasmodium falciparum, Phosphoinositide Signal Transduction, Microbiology, Signaling Pathways, Models, Biological, General Biochemistry, Genetics and Molecular Biology, Host-Parasite Interactions, parasitic diseases, Calcium-Mediated Signal Transduction, Animals, Humans, Plasmodium berghei, Calcium Signaling, Protein kinase A, Biology, Life Cycle Stages, General Immunology and Microbiology, Parasite Physiology, biology.organism_classification, Malaria, Culicidae, Cell movement signaling, Phospholipid Signaling Cascade, Calcium Signaling Cascade, cGMP signaling, Parasitology, cGMP-dependent protein kinase

Abstract

Chemical genetics and a global comparative analysis of phosphorylation and phospholipids in vivo shows that PKG is the upstream regulator that induces calcium signals that enables Plasmodium to progress through its complex life cycle., Many critical events in the Plasmodium life cycle rely on the controlled release of Ca2+ from intracellular stores to activate stage-specific Ca2+-dependent protein kinases. Using the motility of Plasmodium berghei ookinetes as a signalling paradigm, we show that the cyclic guanosine monophosphate (cGMP)-dependent protein kinase, PKG, maintains the elevated level of cytosolic Ca2+ required for gliding motility. We find that the same PKG-dependent pathway operates upstream of the Ca2+ signals that mediate activation of P. berghei gametocytes in the mosquito and egress of Plasmodium falciparum merozoites from infected human erythrocytes. Perturbations of PKG signalling in gliding ookinetes have a marked impact on the phosphoproteome, with a significant enrichment of in vivo regulated sites in multiple pathways including vesicular trafficking and phosphoinositide metabolism. A global analysis of cellular phospholipids demonstrates that in gliding ookinetes PKG controls phosphoinositide biosynthesis, possibly through the subcellular localisation or activity of lipid kinases. Similarly, phosphoinositide metabolism links PKG to egress of P. falciparum merozoites, where inhibition of PKG blocks hydrolysis of phosphatidylinostitol (4,5)-bisphosphate. In the face of an increasing complexity of signalling through multiple Ca2+ effectors, PKG emerges as a unifying factor to control multiple cellular Ca2+ signals essential for malaria parasite development and transmission., Author Summary Malaria, caused by Plasmodium spp. parasites, is a profound human health problem. Plasmodium parasites progress through a complex life cycle as they move between infected humans and blood-feeding mosquitoes. We know that tight regulation of calcium ion levels within the cytosol of the parasite is critical to control multiple signalling events in their life cycle. However, how these calcium levels are controlled remains a mystery. Here, we show that a single protein kinase, the cGMP-dependent protein kinase G (PKG), controls the calcium signals that are critical at three different points of the life cycle: (1) for the exit of the merozoite form of the parasite from human erythrocytes (red blood cells), (2) for the cellular activation that happens when Plasmodium sexual transmission stages are ingested by a blood-feeding mosquito, and (3) for the productive gliding of the ookinete, which is the parasite stage that invades the mosquito midgut. We provide initial evidence that the universal role of PKG relies on the production of lipid precursors which then give rise to inositol (1,4,5)-trisphosphate (IP3), a messenger molecule that serves as a signal for the release of calcium from stores within the parasite. This signalling pathway provides a potential target to block both malaria development in the human host and transmission to the mosquito vector.

Published

2014

39. TRIM5α associates with proteasomal subunits in cells while in complex with HIV-1 virions

Author

Jaya Sastri, Zana Lukic, Edward M. Campbell, Seth L. Robia, Stéphane Hausmann, Justin Rucci, Jeremy Luban, and Sarah Sebastian

Subjects

lcsh:Immunologic diseases. Allergy, Cytoplasm, Proteasome Endopeptidase Complex, PSMC2, viruses, Protein subunit, Ubiquitin-Protein Ligases, DNA, Recombinant, HIV Infections, Plasma protein binding, Biology, Transfection, Antiviral Restriction Factors, Tripartite Motif Proteins, 03 medical and health sciences, Ubiquitin, Species Specificity, TRIM5α, Virology, Two-Hybrid System Techniques, Protein Interaction Mapping, Fluorescence Resonance Energy Transfer, Humans, Immunoprecipitation, immunofluorescence, 030304 developmental biology, Gene Library, cytoplasmic bodies, 0303 health sciences, Research, 030302 biochemistry & molecular biology, HEK 293 cells, Ubiquitination, proteasomal subunits, 3. Good health, Cell biology, Infectious Diseases, Förster resonance energy transfer, HEK293 Cells, Proteasome, Microscopy, Fluorescence, biology.protein, HIV-1, ATPases Associated with Diverse Cellular Activities, Carrier Proteins, lcsh:RC581-607, Protein Binding

Abstract

Background The TRIM5 proteins are cellular restriction factors that prevent retroviral infection in a species-specific manner. Multiple experiments indicate that restriction activity requires accessory host factors, including E2-enzymes. To better understand the mechanism of restriction, we conducted yeast-two hybrid screens to identify proteins that bind to two TRIM5 orthologues. Results The only cDNAs that scored on repeat testing with both TRIM5 orthologues were the proteasome subunit PSMC2 and ubiquitin. Using co-immunoprecipitation assays, we demonstrated an interaction between TRIM5α and PSMC2, as well as numerous other proteasome subunits. Fluorescence microscopy revealed co-localization of proteasomes and TRIM5α cytoplasmic bodies. Forster resonance energy transfer (FRET) analysis indicated that the interaction between TRIM5 and PSMC2 was direct. Previous imaging experiments demonstrated that, when cells are challenged with fluorescently-labeled HIV-1 virions, restrictive TRIM5α orthologues assemble cytoplasmic bodies around incoming virion particles. Following virus challenge, we observed localization of proteasome subunits to rhTRIM5α cytoplasmic bodies that contained fluorescently labeled HIV-1 virions. Conclusions Taken together, the results presented here suggest that localization of the proteasome to TRIM5α cytoplasmic bodies makes an important contribution to TRIM5α-mediated restriction.

Published

2011

40. An invariant surface patch on the TRIM5alpha PRYSPRY domain is required for retroviral restriction but dispensable for capsid binding

Author

Sarah Sebastian, Jeremy Luban, Thomas Pertel, Silvia Olivari, Markus G. Grütter, Christian Grütter, Caterina Strambio De Castillia, University of Zurich, and Luban, J

Subjects

Models, Molecular, Capsid Proteins/*metabolism, 1109 Insect Science, Protein Conformation, Ubiquitin-Protein Ligases, viruses, Molecular Sequence Data, Immunology, Mutant, Mutation, Missense, Biology, Microbiology, Cell Line, Antiviral Restriction Factors, Tripartite Motif Proteins, Retrovirus, Virology, 10019 Department of Biochemistry, Humans, Amino Acid Sequence, Amino Acid Substitution/genetics, Carrier Proteins/genetics/*metabolism, Binding site, Peptide sequence, ddc:616, Genetics, 2403 Immunology, Binding Sites, 2404 Microbiology, Leukemia Virus, Murine/*immunology, Provirus, biology.organism_classification, Virus-Cell Interactions, Protein Structure, Tertiary, Leukemia Virus, Murine, Amino Acid Substitution, Capsid, Insect Science, Host cell cytoplasm, Mutagenesis, Site-Directed, biology.protein, 2406 Virology, TRIM5alpha, 570 Life sciences, biology, Capsid Proteins, Infectious Anemia Virus, Equine/*immunology, Carrier Proteins, Infectious Anemia Virus, Equine, Protein Binding

Abstract

TRIM5α is a retrovirus restriction factor in the host cell cytoplasm that blocks infection before provirus establishment. Restriction activity requires capsid (CA)-specific recognition by the PRYSPRY domain of TRIM5α. To better understand the restriction mechanism, nine charge-cluster-to-triple-alanine mutants in the TRIM5α PRYSPRY domain were assessed for CA-specific restriction activity. Five mutants distributed along the TRIM5α PRYSPRY primary sequence disrupted restriction activity against N-tropic murine leukemia virus and equine infectious anemia virus. Modeling of the TRIM5α PRYSPRY domain based on the crystal structures of PRYSPRY-19q13.4.1, GUSTAVUS, and TRIM21 identified a surface patch where disruptive mutants clustered. All mutants in this patch retained CA-binding activity, a reticular distribution in the cytoplasm, and steady-state protein levels comparable to those of the wild type. Residues in the essential patch are conserved in TRIM5α orthologues and in closely related paralogues. The same surface patch in the TRIM18 and TRIM20 PRYSPRY domains is the site of mutants causing Opitz syndrome and familial Mediterranean fever. These results indicate that, in addition to CA-specific binding, the PRYSPRY domain possesses a second function, possibly binding of a cofactor, that is essential for retroviral restriction activity by TRIM5α.

Published

2009

41. Cyclophilin A is required for TRIM5α-mediated resistance to HIV-1 in Old World monkey cells

Author

Lionel Berthoux, Elena Sokolskaja, Sarah Sebastian, and Jeremy Luban

Subjects

Ubiquitin-Protein Ligases, Cypa, HIV Infections, Old World monkey, Cell Line, Cyclophilin A, RNA interference, Cyclosporin a, Chlorocebus aethiops, Animals, DNA Primers, Multidisciplinary, biology, Proteins, Biological Sciences, biology.organism_classification, Virology, Macaca mulatta, Reverse transcriptase, Immunity, Innate, Titer, Cell culture, Cats, HIV-1, RNA Interference

Abstract

The peptidyl-prolyl isomerase cyclophilin A (CypA) embraces an exposed, proline-rich loop on HIV-1 capsid (CA) and renders reverse transcription complexes resistant to an antiviral activity in human cells. A CypA fusion with TRIM5 that is unique to New World owl monkeys also targets HIV-1 CA, but this interaction potently inhibits infection. A similar block to HIV-1 infection in Old World monkeys is attributable to the alpha isoform of the TRIM5 orthologue in these species. To determine whether HIV-1 restriction by Old World monkey TRIM5alpha is modulated by the CA-CypA interaction, RNA interference was used to disrupt CypA in cells from African green monkeys and rhesus macaques. HIV-1 infectivity increased in response to CypA knock-down to the same extent that it increased in response to TRIM5 knock-down. CypA knock-down eliminated the HIV-1 stimulatory effect of cyclosporin A (CsA), a competitive inhibitor of the CypA-CA interaction, or of CA mutants that block binding to CypA but caused no change in titer of retroviruses that don't interact with CypA. Simultaneous knock-down of both CypA and TRIM5 caused minimal additional increase in titer, suggesting that CypA inhibits HIV-1 replication in these cells because it is required for CA recognition by TRIM5alpha. Finally, CsA increased HIV-1 titer in otherwise nonrestrictive feline cells but only after these cells were transduced with Old World monkey TRIM5alpha. Thus, CypA is required for HIV-1 restriction by Old World monkey orthologues of TRIM5alpha.

Published

2005

42. TRIM5α selectively binds a restriction-sensitive retroviral capsid

Author

Jeremy Luban and Sarah Sebastian

Subjects

lcsh:Immunologic diseases. Allergy, 0303 health sciences, Viral Reverse Transcription, biology, 030306 microbiology, viruses, Short Report, Plasma protein binding, biology.organism_classification, Virology, 3. Good health, 03 medical and health sciences, Infectious Diseases, Retrovirus, Protein structure, Capsid, Murine leukemia virus, biology.protein, Tripartite Motif Proteins, TRIM5alpha, lcsh:RC581-607, 030304 developmental biology

Abstract

TRIM5 is a potent retrovirus inhibitor that targets viruses bearing particular capsid (CA) residues. In most primate species, retroviral restriction requires the C-terminal SPRY domain unique to the α-isoform of TRIM5, but the mechanism by which susceptible viruses are recognized and targeted for restriction is unknown. Here we show that TRIM5α binds retroviral CA from detergent-stripped virions in a SPRY-dependent manner with sufficient discrimination to account for the exquisite specificity of restriction.

Published

2005

43. Cultivated systems

Author

Cassman, Kenneth G.; Wood, Stanley; Choo, Poh Sze; Cooper, H. David; Devendra, C.; Dixon, John; Gaskell, Joanne; Khan, Shabaz; Lal, Rattan; Lipper, Leslie; Pretty, Jules N.; Primavera, Jurgenna; Ramankutty, Navin; Viglizzo, Ernesto; Wiebe, Keith D. D.; Kadungure, Sandra; Kanbar, Nancy; Zahia Khan,; Leakey, Roger; Porter, Sarah; Sebastian, Kate; Tharme, Rebecca, http://orcid.org/0000-0001-6035-620X Wiebe, Keith, Cassman, Kenneth G.; Wood, Stanley; Choo, Poh Sze; Cooper, H. David; Devendra, C.; Dixon, John; Gaskell, Joanne; Khan, Shabaz; Lal, Rattan; Lipper, Leslie; Pretty, Jules N.; Primavera, Jurgenna; Ramankutty, Navin; Viglizzo, Ernesto; Wiebe, Keith D. D.; Kadungure, Sandra; Kanbar, Nancy; Zahia Khan,; Leakey, Roger; Porter, Sarah; Sebastian, Kate; Tharme, Rebecca, and http://orcid.org/0000-0001-6035-620X Wiebe, Keith

Abstract

PR, IFPRI4; GRP38, EPTD

Published

2005