Your search keyword '"Cargill, Tamsin"' showing total 3 results

1. NK cells limit therapeutic vaccine–induced CD8+T cell immunity in a PD-L1–dependent manner.

Author

Diniz, Mariana O., Schurich, Anna, Chinnakannan, Senthil K., Duriez, Marion, Stegmann, Kerstin A., Davies, Jessica, Kucykowicz, Stephanie, Suveizdyte, Kornelija, Amin, Oliver E., Alcock, Frances, Cargill, Tamsin, Barnes, Eleanor, and Maini, Mala K.

Subjects

KILLER cells, CHRONIC hepatitis B, VACCINE effectiveness, T cells, HEPATITIS B virus, IMMUNITY, NUDGE theory

Abstract

A better understanding of mechanisms that regulate CD8+T cell responses to therapeutic vaccines is needed to develop approaches to enhance vaccine efficacy for chronic viral infections and cancers. We show here that NK cell depletion enhanced antigen-specific T cell responses to chimp adenoviral vector (ChAdOx) vaccination in a mouse model of chronic HBV infection (CHB). Probing the mechanism underlying this negative regulation, we observed that CHB drove parallel up-regulation of programmed cell death ligand 1 (PD-L1) on liver-resident NK cells and programmed cell death 1 (PD-1) on intrahepatic T cells. PD-L1–expressing liver-resident NK cells suppressed PD-1hiCD8+T cells enriched within the HBV-specific response to therapeutic vaccination. Cytokine activation of NK cells also induced PD-L1, and combining cytokine activation with PD-L1 blockade resulted in conversion of NK cells into efficient helpers that boosted HBV-specific CD8+T cell responses to therapeutic vaccination in mice and to chronic infection in humans. Our findings delineate an immunotherapeutic combination that can boost the response to therapeutic vaccination in CHB and highlight the broader importance of PD-L1–dependent regulation of T cells by cytokine-activated NK cells. NK cells nudge vaccine response: Therapeutic vaccines for chronic infections have reduced efficacy because of the presence of exhausted T cells and a tolerogenic environment that limits vaccine responses. Diniz et al. observed that NK cell depletion enhanced T cell responses to a chimp adenoviral vectored hepatitis B virus (HBV) vaccine in a mouse model of chronic hepatitis B virus (CHB) infection. CHB was associated with up-regulation of PD-1 on intrahepatic CD8+T cells and PD-L1 on liver-resident NK cells. These NK cells suppressed HBV-specific responses of PD-1hiCD8+T cells upon vaccination. Stimulation of NK cells with activating cytokines also induced PD-L1 expression, but cytokine activation combined with PD-L1 blockade altered NK cells to function as enhancers of HBV-specific CD8+T cell responses. These findings highlight a strategy by which therapeutic vaccine responses can be restored even in tolerogenic settings. [ABSTRACT FROM AUTHOR]

Published

2022

2. Therapeutic vaccination for treatment of chronic hepatitis B.

Author

Cargill, Tamsin and Barnes, Eleanor

Subjects

*CHRONIC hepatitis B, *VACCINE effectiveness, *HEPATITIS B, *VACCINATION, *VIRAL antigens

Abstract

Summary: Chronic hepatitis B infection remains a serious global health threat, contributing to a large number of deaths through liver cirrhosis and hepatocellular carcinoma. Current treatment does not eradicate disease, and therefore new treatments are urgently needed. In acute hepatitis B virus (HBV) a strong immune response is necessary to clear the virus, but in chronic infection the immune response is weakened and dysfunctional. Therapeutic vaccination describes the process of inoculating individuals with a non‐infective form of viral antigen with the aim of inducing or boosting existing HBV‐specific immune responses, resulting in sustained control of HBV infection. In this review we outline the rationale for therapeutic vaccination in chronic HBV infection, discuss previous and ongoing trials of novel HBV therapeutic vaccine candidates and outline strategies to improve vaccine efficacy going forward. [ABSTRACT FROM AUTHOR]

Published

2021

3. 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

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

Subjects

GENETIC vectors, VACCINIA, CHRONIC hepatitis B, CHIMPANZEES, HEPATITIS B virus

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. [ABSTRACT FROM AUTHOR]

Published

2020