Abstracts from the NIHR INVOLVE Conference 2017

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Mathematical models for immunology:current state of the art and future research directions

The advances in genetics and biochemistry that have taken place over the last 10 years led to significant advances in experimental and clinical immunology. In turn, this has led to the development of new mathematical models to investigate qualitatively and quantitatively various open questions in immunology. In this study we present a review of some research areas in mathematical immunology that evolved over the last 10 years. To this end, we take a step-by-step approach in discussing a range of models derived to study the dynamics of both the innate and immune responses at the molecular, cellular and tissue scales. To emphasise the use of mathematics in modelling in this area, we also review some of the mathematical tools used to investigate these models. Finally, we discuss some future trends in both experimental immunology and mathematical immunology for the upcoming years

Rapid Review of Equality, Diversity and Inclusion (EDI) in Global Health Literature

The National Institute for Health and Care Research (NIHR) has an ambitious programme for furthering inclusive research through their Equality Diversity and Inclusion (EDI) strategy and work plan. Part of this work includes work within low- and middle-income country (LMIC) settings for the Global Health Research (GHR) programmes, which are funded through Official Development Assistance (ODA) or UK International Development funding. It is recognised that the concepts of equality, diversity and inclusion in different geo-political, legal and cultural settings may differ to those of the United Kingdom. Having a good working understanding of how these concepts are understood and employed in different LMIC settings and in the wider literature in global health is crucial in understanding how the NIHR should position itself and how it should engage and tackle the most pressing obstacles to inclusive research within the LMIC settings. Funding for this work is internal to NIHR

Limiting dilution analysis of cytotoxic T lymphocytes to human immunodeficiency virus gag antigens in infected persons: in vitro quantitation of effector cell populations with p17 and p24 specificities

The presence of cytotoxic T lymphocytes (CTL) to the gag antigens of human immunodeficiency virus (HIV) has been described in infected populations. We found that the majority of this immune response as measured in bulk CTL assays of unstimulated peripheral blood mononuclear cells (PBMC) is directed against the p24 component of the p55 gag precursor protein. Using limiting dilution analysis of this effector cell population we confirm that the majority of activated gag-specific CTL circulating in the PBMC of infected hemophilic patients are directed at p24 determinants and are present at frequencies of 1/36,000 to 1/86,000 lymphocytes. By performing in vitro stimulation after limiting dilution, the precursor population of gag-specific CTL are characterized and quantitated. HIV gag-specific CTL precursors are identified at frequencies of 1/1700 to 1/17,000 lymphocytes and are made up of cells with both p17 and p24 specificities. No HIV gag-specific CTL precursor cells are identified in the PBMC of HIV-uninfected individuals. These studies demonstrate that CTL directed at both p17 and p24 determinants make up the cellular immune repertoire in HIV-infected individuals but that only the p24-specific CTL are routinely found in an activated state in the circulation