Elucidation of the transcriptional programme of memory T cells by a systems approach
Lead Research Organisation:
Imperial College London
Department Name: Life Sciences
Abstract
This project aims to reveal the fundamental molecular mechanisms of immunological memory at the gene level. Immunological memory is a unique attribute of the adaptive immune system and provides extremely efficient defense against pathogens. Because the immune system has this capacity, humans and animals (including mammals, birds, and fish) can efficiently eradicate life-threatening pathogens, especially viruses, that were once encountered in the past or for which they were immunised. Thus, immunological memory is essential for maintaining health and longevity, and the control of immunological memory will provide a mean for improving the prevention and treatment of infectious diseases, and for developing effective vaccines against pathogens such as HIV. It is, however, still unclear how immunological memory is determined and maintained in the immune system.
This study aims to reveal how immunological memory is provided by lymphocytes, especially in T cells. T cells coordinate the activities of other immune cells, and generate efficient and rapid responses to pathogens. Thus, not surprisingly, some viruses such as HIV target T cells, and thereby cause the major symptoms of acquired immune deficiency syndrome (AIDS). Memory T cells may play central roles both in immunity to pathogens and on vaccination. Research on memory T cells, however, has been difficult and will require multiple approaches, including immunology, molecular biology, and systems biology.
Thus, we will employ an integrated approach of immunology, molecular biology, genomics, and systems biology, and address how immunological memory is maintained in memory T cells at the gene level. Immunological and molecular approaches will identify which of already known molecules are involved in generation and function of memory T cells. Genomics will identify new molecular mechanisms for controlling memory T cells. The systems approach will identify the complex regulatory mechanisms between the molecules and thereby provide rigid frameworks to fully discover the mechanisms of the generation and function of memory T cells. These together will reveal the critical mechanisms that underlie T cell memory, which can then be exploited for the development of new immunosuppressive drugs and vaccine designs.
The project is designed to swiftly transfer knowledge and technology to industry, including the pharmaceutical industry. The understanding of the mechanism of T cell memory at the gene level is important not only for scientific progress but also for patency and for the development of new immunosuppressive drugs and vaccines. We also aim to use the findings of the project to improve the efficiency of the screening processes in the development of new drugs. The combined approach of experiments and mathematical modelling in this study can be directly used for screening processes for immunomodulative drugs, which can contribute to improve the cost performance of drug development at the preclinical stage.
This study is highly multidisciplinary. The applicant is an immunologist and molecular biologist, and has recently trained for genomics and systems biology. With this background, the applicant will coordinate collaborations with mathematical modellers, statisticians, and immunologists to provide the most efficient answers to this problem. The findings of this study will benefit broad scientific communities and contribute to health and well-being of humans and animals. In addition, this study will provide novel frameworks for systems biology, which can be used in many biological areas.
This study aims to reveal how immunological memory is provided by lymphocytes, especially in T cells. T cells coordinate the activities of other immune cells, and generate efficient and rapid responses to pathogens. Thus, not surprisingly, some viruses such as HIV target T cells, and thereby cause the major symptoms of acquired immune deficiency syndrome (AIDS). Memory T cells may play central roles both in immunity to pathogens and on vaccination. Research on memory T cells, however, has been difficult and will require multiple approaches, including immunology, molecular biology, and systems biology.
Thus, we will employ an integrated approach of immunology, molecular biology, genomics, and systems biology, and address how immunological memory is maintained in memory T cells at the gene level. Immunological and molecular approaches will identify which of already known molecules are involved in generation and function of memory T cells. Genomics will identify new molecular mechanisms for controlling memory T cells. The systems approach will identify the complex regulatory mechanisms between the molecules and thereby provide rigid frameworks to fully discover the mechanisms of the generation and function of memory T cells. These together will reveal the critical mechanisms that underlie T cell memory, which can then be exploited for the development of new immunosuppressive drugs and vaccine designs.
The project is designed to swiftly transfer knowledge and technology to industry, including the pharmaceutical industry. The understanding of the mechanism of T cell memory at the gene level is important not only for scientific progress but also for patency and for the development of new immunosuppressive drugs and vaccines. We also aim to use the findings of the project to improve the efficiency of the screening processes in the development of new drugs. The combined approach of experiments and mathematical modelling in this study can be directly used for screening processes for immunomodulative drugs, which can contribute to improve the cost performance of drug development at the preclinical stage.
This study is highly multidisciplinary. The applicant is an immunologist and molecular biologist, and has recently trained for genomics and systems biology. With this background, the applicant will coordinate collaborations with mathematical modellers, statisticians, and immunologists to provide the most efficient answers to this problem. The findings of this study will benefit broad scientific communities and contribute to health and well-being of humans and animals. In addition, this study will provide novel frameworks for systems biology, which can be used in many biological areas.
Technical Summary
The memory response is the key feature of immunological memory, where the immune system responds to antigens in a more rapid and efficient way than during the primary response. T cells are central to such adaptive responses, and memory T cells show a more rapid and efficient response upon antigenic stimulation. It is, however, still obscure how memory T cells are generated by encounter with pathogens, and how memory T cells efficiently respond to antigens and propagate activation through interacting with other T cells and antigen-presenting cells. In addition, currently memory T cells lack specific markers and can be identified only by the expression of a set of markers or their situation, which hampers the analysis of the dynamic response of memory T cells.
The major objectives of this study are to understand T cell memory as a network of proteins/genes or as a cell population, by a systems approach using time course analysis and mathematical modelling: (1) analysis of the gene regulatory mechanisms of T cell activation-related molecules in memory T cells during the memory response; (2) analysis of the propagation of the activation from memory T cells through the naive T cell pool. The dynamics of the activation of T cells will be analysed at single cell level. This will identify physiological memory T cell populations; (3) identification of the transcriptional regulations that are specific to memory T cells by time course analysis of these cells during the memory response using a novel framework of microarray analysis with a multidimensional technique. These three stand-alone approaches will elucidate the mechanisms at different levels of T cell memory, and together strengthen the biological relevance of this study. In addition, these will define memory T cells and thereby provide the basis for future studies and applications. In addition, the modelling and multidimensional frameworks to analyse memory T cells can be used in other areas of biology.
The major objectives of this study are to understand T cell memory as a network of proteins/genes or as a cell population, by a systems approach using time course analysis and mathematical modelling: (1) analysis of the gene regulatory mechanisms of T cell activation-related molecules in memory T cells during the memory response; (2) analysis of the propagation of the activation from memory T cells through the naive T cell pool. The dynamics of the activation of T cells will be analysed at single cell level. This will identify physiological memory T cell populations; (3) identification of the transcriptional regulations that are specific to memory T cells by time course analysis of these cells during the memory response using a novel framework of microarray analysis with a multidimensional technique. These three stand-alone approaches will elucidate the mechanisms at different levels of T cell memory, and together strengthen the biological relevance of this study. In addition, these will define memory T cells and thereby provide the basis for future studies and applications. In addition, the modelling and multidimensional frameworks to analyse memory T cells can be used in other areas of biology.
Planned Impact
The project will benefit the following groups and thereby contribute to human well-being and health, and enhance the economic competitiveness of the UK.
1) Pharmaceutical industry
The project will contribute to pharmaceutical industry by providing drug targets as well as screening methods for candidate compounds. First, the molecular mechanism of memory T cells will provide targets for immunoregulatory drugs. Second, the combined system of experiments and theories that will be established in the project can be used at the preclinical stage of development of immunosuppressive drugs. We plan to start collaborations with pharmaceutical industry and aim to realise these benefits within 2-10 years thereafter.
2) Biotechnological industry
The antibodies to key molecules in T cell memory will be widely used in immunology and related areas and their commercialisation will benefit the biotechnological industry. I will use my informal connections with biotechnological companies, starting collaborations with them in the lifetime of the project and aiming to realise these benefits within 1-3 years thereafter.
3) Immunisation practice and vaccine development
The monoclonal antibodies or molecular markers for memory T cells can be used for monitoring the effectiveness of immunisation, which will optimise immunisation plans. In addition, elucidation of the mechanisms of T cell memory will provide molecular targets for boosting the immune system, which can be exploited for vaccine development. These collectively will benefit public and global health and vaccine industry.
4) Governmental policy in public health regarding immunisation
The project will provide a modern understanding of the mechanisms of immunisation, which will make the governmental policy more effective in providing new plans for immunisation. We will liaise with the Research Council to transfer our knowledge to policy communities. This will be done within the lifetime of the project.
5) General Public
The project will benefit the health and the quality of life of the general public via three pathways: (a) improved healthcare service (see 6); (b) improved immunisation practice (see 3); and (c) in-depth understanding of immunisation. We will hold workshops to convey the frontline understanding of immunisation through educating pupils, which will improve their uptake of necessary vaccines at proper timings. We will publish the contents of these workshop to influence broad audience.
6) Health service
The project will contribute to improve health practice via three pathways. First, the findings of this project will promote studies in related clinical research areas to elucidate the molecular mechanism of immunity against pathogens. Second, the proposed project will identify drug target for controlling memory T cells to enhance immunity in aged people. The realisation of these benefits will be within 2- 10 years after the completion of the proposed project. Third, we will rapidly disseminate our findings to health and public health professionals by publishing our perspectives in medical journals for the successful development of the health service section.
7) Animal health
The project will contribute to improve health practice of animals, and thereby contribute to animal welfares, farming, and food production via three pathways: (i) effective development of vaccines (see 3); (ii) prevention and treatment of infectious disease including zoonosises. The realisation of these benefits will be within 2- 10 years after the completion of the proposed project.
8) Education and training of scientists
The project will nurture the involved post-doc and students to have a high quality research capacity by providing a wide range of skills and knowledge of experiments, modelling, and data analysis and their integration.
1) Pharmaceutical industry
The project will contribute to pharmaceutical industry by providing drug targets as well as screening methods for candidate compounds. First, the molecular mechanism of memory T cells will provide targets for immunoregulatory drugs. Second, the combined system of experiments and theories that will be established in the project can be used at the preclinical stage of development of immunosuppressive drugs. We plan to start collaborations with pharmaceutical industry and aim to realise these benefits within 2-10 years thereafter.
2) Biotechnological industry
The antibodies to key molecules in T cell memory will be widely used in immunology and related areas and their commercialisation will benefit the biotechnological industry. I will use my informal connections with biotechnological companies, starting collaborations with them in the lifetime of the project and aiming to realise these benefits within 1-3 years thereafter.
3) Immunisation practice and vaccine development
The monoclonal antibodies or molecular markers for memory T cells can be used for monitoring the effectiveness of immunisation, which will optimise immunisation plans. In addition, elucidation of the mechanisms of T cell memory will provide molecular targets for boosting the immune system, which can be exploited for vaccine development. These collectively will benefit public and global health and vaccine industry.
4) Governmental policy in public health regarding immunisation
The project will provide a modern understanding of the mechanisms of immunisation, which will make the governmental policy more effective in providing new plans for immunisation. We will liaise with the Research Council to transfer our knowledge to policy communities. This will be done within the lifetime of the project.
5) General Public
The project will benefit the health and the quality of life of the general public via three pathways: (a) improved healthcare service (see 6); (b) improved immunisation practice (see 3); and (c) in-depth understanding of immunisation. We will hold workshops to convey the frontline understanding of immunisation through educating pupils, which will improve their uptake of necessary vaccines at proper timings. We will publish the contents of these workshop to influence broad audience.
6) Health service
The project will contribute to improve health practice via three pathways. First, the findings of this project will promote studies in related clinical research areas to elucidate the molecular mechanism of immunity against pathogens. Second, the proposed project will identify drug target for controlling memory T cells to enhance immunity in aged people. The realisation of these benefits will be within 2- 10 years after the completion of the proposed project. Third, we will rapidly disseminate our findings to health and public health professionals by publishing our perspectives in medical journals for the successful development of the health service section.
7) Animal health
The project will contribute to improve health practice of animals, and thereby contribute to animal welfares, farming, and food production via three pathways: (i) effective development of vaccines (see 3); (ii) prevention and treatment of infectious disease including zoonosises. The realisation of these benefits will be within 2- 10 years after the completion of the proposed project.
8) Education and training of scientists
The project will nurture the involved post-doc and students to have a high quality research capacity by providing a wide range of skills and knowledge of experiments, modelling, and data analysis and their integration.
People |
ORCID iD |
| Masahiro Ono (Principal Investigator / Fellow) |
Publications
Yánez DC
(2019)
IFITM proteins drive type 2 T helper cell differentiation and exacerbate allergic airway inflammation.
in European journal of immunology
Whyte CE
(2022)
Correction: Context-dependent effects of IL-2 rewire immunity into distinct cellular circuits.
in The Journal of experimental medicine
Whyte CE
(2022)
Context-dependent effects of IL-2 rewire immunity into distinct cellular circuits.
in The Journal of experimental medicine
Van Logtestijn MD
(2016)
Water resistance profile as a marker of skin barrier damage in atopic dermatitis patients.
in Journal of dermatological science
Sinclair C
(2015)
A Zap70-dependent feedback circuit is essential for efficient selection of CD4 lineage thymocytes.
in Immunology and cell biology
Saldaña JI
(2016)
Sonic Hedgehog regulates thymic epithelial cell differentiation.
in Journal of autoimmunity
Sahni H
(2015)
A genome wide transcriptional model of the complex response to pre-TCR signalling during thymocyte differentiation.
in Oncotarget
Rattazzi L
(2016)
Impact of Enriched Environment on Murine T Cell Differentiation and Gene Expression Profile.
in Frontiers in immunology
Ono M
(2015)
Controversies concerning thymus-derived regulatory T cells: fundamental issues and a new perspective
in Immunology & Cell Biology
Kenefeck R
(2015)
Follicular helper T cell signature in type 1 diabetes.
in The Journal of clinical investigation
| Description | This project aimed to reveal the fundamental molecular mechanisms of immunological memory at the gene level. Specifically, it aimed to reveal how immunological memory is provided by lymphocytes, especially in T cells. To this end, we used an integrated approach of immunology, molecular biology, genomics, and systems biology, and developed new tools and thereby obtained new knowledge on the regulation of T cell memory responses. During the lifetime of the project, we successfully developed a new experimental tool, Timer-of-Cell-Kinetics-and-Activity (Tocky), which allows analysis of time-dependent changes in T cells during immune responses (e.g. infection) or during development (i.e. when T cells are produced in the thymus) (Bending et al, J Cell Biol, 2018). Tocky uses a new reporter system using Fluorescent Timer protein, which spontaneously changes colour from blue to red, and computer algorithms to analyse Timer fluorescence data in individual cells. Thus Tocky analyses time-dependent changes in individual T cells and allows tracking of T cells at the single cell level. In addition, using a systems biology approach, we established a new theoretical framework for understanding T cell memory and T cell regulation (which is currently understood as regulatory T cells) through analysing temporally-dynamic changes of T cell activities at single-cell level (Ono & Tanaka, Immunol Cell Biol, 2015). The understanding of the mechanism of T cell memory at the gene level is important not only for scientific progress but also for patency and for the development of new immunosuppressive drugs and vaccines. To this end, we showed how Tocky can be used to analyse effects of immunotherapy on T cells and thus established a proof-of-concept for Tocky as a new method for strategic design of immunotherapy (Bending et al, EMBO J, 2018; Bending & Ono, Clin Exp Immunol, 2018). In addition, we have successfully identified new mechanisms for parasite infection (precisely, nematode, which is a major health problem for humans and animals in developing countries) using Tocky (manuscript in preparation), and this will have impacts on animal health and global health. Thus, the findings of this study will benefit broad scientific communities and contribute to health and well-being of humans and animals. Furthermore, we developed new analysis methods for genomic data using a multidimensional analysis (Canonical Correspondence Analysis, CCA). Firstly, we developed a CCA based method for cross-analysis of biological functions and gene expression (Ono et al, BMC Genomics, 2014). Subsequently, we adapted this method to single cell data analysis, thereby analysed single cell RNA-seq data from tumour-infiltrating T cells, and showed the dynamic generation of effector memory T cells and regulatory T cells in tumours (Bradley et al, Front Immunol, 2018). Thus, the project provided novel frameworks for systems biology, which can be used in many biological areas. |
| Exploitation Route | We have provided our new experimental tools to the research groups in the following areas on a collaboration basis: (1) Groups working on investigating human viral infections (2) Groups working on cancer immunology (3) Groups working on autophagy and molecular biology (4) Groups working on immunology Studies by ourselves and these collaborations are considered to benefit the following groups: (1) Groups working on developing vaccines (clinical, veterinary, and basic vaccinology). (2) Groups working on drug development (research sections of the pharmaceutical industry). (3) Groups working on cellular differentiation (genomicists, bioinformaticians, developmental biologists, stem cell research). (4) Groups working on analysing complex biological data (biostatisticians, bioinformaticians, biomathematicians, systems biologists) (5) Groups working on the activities of transcription factors (molecular biologists, biochemists, developmental biologists). (6) Groups working on mammalian (including humans) and bird pathogens (medical and agricultural/veterinary infectionologists, bacteriologists, virologists) |
| Sectors | Agriculture, Food and Drink,Healthcare,Pharmaceuticals and Medical Biotechnology |
| Description | Our research by the Tocky technology was communicated by several media: • Two news stories released by Imperial in 2018 - "Watching the immune system in action reveals what happens when things goes wrong", 25 June 2018, Imperial College website (news article for Bending et al, J Cell Biol, 2018) - Immune cells can switch from 'gang members' to 'police officers', 25 June 2018, Imperial College website (Bending et al, EMBO J, 2018 and Bradley et al, Front Immunol, 2018) • The online news, Multiple Sclerosis News Today, released two news stories: - "Overreactive T-cells Can Transition into T-cells That Control the Immune Response, Study Shows", 12th July 2018 - "New Fluorescent Imaging Tool Allows Researchers to Track Immune Cell Dynamics in MS Mouse Model", June 27, 2018 • My article about Tocky was published in Yahoo Japan News, and obtained 20k views to date. |
| First Year Of Impact | 2018 |
| Sector | Healthcare,Pharmaceuticals and Medical Biotechnology |
| Impact Types | Societal |
| Description | BBSRC Impact Acceleration Account 2015-2016 |
| Amount | £14,909 (GBP) |
| Funding ID | 4020012831 |
| Organisation | Biotechnology and Biological Sciences Research Council (BBSRC) |
| Sector | Public |
| Country | United Kingdom |
| Start | 11/2015 |
| End | 06/2016 |
| Description | CRCE pump priming collaborative pilot project grant |
| Amount | £29,913 (GBP) |
| Organisation | Imperial College London |
| Sector | Academic/University |
| Country | United Kingdom |
| Start | 09/2017 |
| End | 08/2018 |
| Description | Development of vaccine for gastrointestinal nematode parasite of livestock |
| Amount | £40,257 (GBP) |
| Organisation | Biotechnology and Biological Sciences Research Council (BBSRC) |
| Sector | Public |
| Country | United Kingdom |
| Start | 12/2016 |
| End | 03/2017 |
| Description | Elucidating molecular and cellular mechanisms underlying T-cell dysfunction and effective anti- cancer T-cell responses: towards the development of next-generation immunotherapy |
| Amount | £1,548,151 (GBP) |
| Funding ID | DCRPGF\100007 |
| Organisation | Cancer Research UK |
| Sector | Charity/Non Profit |
| Country | United Kingdom |
| Start | 11/2021 |
| End | 10/2027 |
| Description | Facility usage at the University of Tokushima, Japan |
| Amount | ¥500,000 (JPY) |
| Organisation | University of Tokushima |
| Sector | Academic/University |
| Country | Japan |
| Start | 09/2016 |
| End | 03/2017 |
| Description | Investigating the molecular mechanisms downstream of T cell receptor signalling during T cell differentiation and response. |
| Amount | £8,541,424 (GBP) |
| Funding ID | 1814289 |
| Organisation | Biotechnology and Biological Sciences Research Council (BBSRC) |
| Sector | Public |
| Country | United Kingdom |
| Start | 10/2016 |
| End | 09/2020 |
| Description | Investigation of the generation and functional maturation of regulatory T cells in vivo |
| Amount | £492,938 (GBP) |
| Funding ID | MR/S000208/1 |
| Organisation | Imperial College London |
| Sector | Academic/University |
| Country | United Kingdom |
| Start | 02/2019 |
| End | 01/2022 |
| Description | Repurposing computational tools to evaluate anti-cancer immunity for development of cancer immunotherapy |
| Amount | £21,476 (GBP) |
| Organisation | Engineering and Physical Sciences Research Council (EPSRC) |
| Sector | Public |
| Country | United Kingdom |
| Start | 10/2016 |
| End | 03/2017 |
| Title | Single cell RNA-seq analysis method |
| Description | Our multidimensional methods Canonical Correspondence Analysis (CCA) was adapted to single cell RNA-seq data analysis, and designated as Single Cell Combinatorial CCA (SC4A) (Bradley et al, Frontiers in Immunology, 2018) |
| Type Of Material | Technology assay or reagent |
| Year Produced | 2018 |
| Provided To Others? | Yes |
| Impact | The paper obtained a good online attention (Altemetric score 50), and this led to (1) an award of a JSPS grant from the Japanese government; and (2) a new collaboration with Prof Kinya Otsu, Kings College London. |
| Title | Timer of Cell Kinetics and Activity (Tocky) |
| Description | A novel transgenic reporter method, Timer of Cell Kinetics and Activity (Tocky) was established for analysing in vivo temporal dynamics of transcriptional activities and cellular differentiation in vivo. This system uses transgenic reporter mice using Fluorescent Timer protein and computational algorithms to analyse Timer fluorescence data. |
| Type Of Material | Model of mechanisms or symptoms - mammalian in vivo |
| Year Produced | 2018 |
| Provided To Others? | No |
| Impact | Our tool paper (Bending et al, J Cell Biol, 2018) received a high online attention (Altmetric score >100; F1000 recommendation). • Seven new collaborations were established for sharing the Tocky tools. • Seminar invitations (including Oxford, Kings College London, UCL, University of Birmingham, Technical University of Munich, Kyoto University [by Prof Tasuku Honjo, the Nobel Laureate 2018]) • Invitations to conference key note talk (Japanese Biochemical Society) |
| Title | Canonical Correspondence Analysis |
| Description | We have adapted Canonical Correspondence Analysis to analyse immunological genomic data including microarray and RNA-sequencing data. |
| Type Of Material | Data analysis technique |
| Year Produced | 2014 |
| Provided To Others? | Yes |
| Impact | The data analysis tool has been used by the following publications: Kenefeck et al, J Clin Inv, 2015; Sahni et al, Oncotarget, 2015; Sinclair et al, Immunol Cell Biol, 2015. |
| URL | http://bmcgenomics.biomedcentral.com/articles/10.1186/1471-2164-15-1028 |
| Description | Collaboration, Dr David Withers, University of Birmingham |
| Organisation | University of Birmingham |
| Country | United Kingdom |
| Sector | Academic/University |
| PI Contribution | To provide the new tool Tocky mice to the Dr David Withers group at University of Birmingham on a collaboration basis. |
| Collaborator Contribution | To provide their transgenic mouse strains, write a manuscript, on which I will be coauthored. |
| Impact | NA |
| Start Year | 2019 |
| Description | Julie Josse |
| Organisation | Agrocampus Ouest |
| Department | Laboratory of Applied Mathematics Agrocampus (LMA) |
| Country | France |
| Sector | Academic/University |
| PI Contribution | To lead a collaborative project, providing experimental data and performing data analysis. |
| Collaborator Contribution | To provide statistical knowledge. |
| Impact | One publication (Fujii et al, J Immunol, 2016). We have applied for a BBSRC funding with Julie Josse in Agrocampus Ouest as a collaborator. |
| Start Year | 2013 |
| Description | Reiko J Tanaka |
| Organisation | Imperial College London |
| Department | Department of Bioengineering |
| Country | United Kingdom |
| Sector | Academic/University |
| PI Contribution | To lead a collaborative project, provide experimental data and data anlaysis. |
| Collaborator Contribution | To provide mathematical analysis. |
| Impact | With Dr Reiko J Tanaka in the organisation as a co-PI, I have been awarded a BBSRC IAA. The collaboration is multi-disciplinary involving immunology, molecular biology, mathematical modelling, multidimensional data analysis. |
| Start Year | 2013 |
| Description | Visiting Associate Professorship, University of Kumamoto |
| Organisation | University of Kumamoto |
| Department | International Research Center for Medical Sciences |
| Country | Japan |
| Sector | Academic/University |
| PI Contribution | Dr Yorifumi Satou is a collaborator at the institute of the University. I have provided my data analysis skills to their research. |
| Collaborator Contribution | The institute has offered me a visiting associate professorship, so that the collaboration can be further deepened to enable research visits and also apply for funding. |
| Impact | This is a multidisciplinary collaboration between immunology and haematology. |
| Start Year | 2017 |
| Description | Immuno-dancing |
| Form Of Engagement Activity | Participation in an activity, workshop or similar |
| Part Of Official Scheme? | No |
| Geographic Reach | Local |
| Primary Audience | Schools |
| Results and Impact | Immuno-dancing: I have established a novel way to convey immunology to primary school pupils by combining immunology with dancing (which I have named Immuno-dancing). The session is composed of two activities: (1) 14~15 pupils dance in a ring, and thereby become a big macrophage, which is a special immune cell dedicated for eating germs; (2) to learn Division of Labour of the immune system. We make 3 groups (dendritic cells, B cells, macrophages), and each of which has 5-6 pupils. The roles are given to each groups, to understand how immune cells coordinate an immune response. We have done the Immuno-dancing in a local primary school with a great success, and will continue developing the method. |
| Year(s) Of Engagement Activity | 2016,2018 |
| Description | Immunology workshop for primary school 2018 |
| Form Of Engagement Activity | Participation in an activity, workshop or similar |
| Part Of Official Scheme? | No |
| Geographic Reach | Local |
| Primary Audience | Schools |
| Results and Impact | We delivered a workshop for immunological memory and vaccination to a primary school (St Clemant Danes CoE primary school, London). |
| Year(s) Of Engagement Activity | 2018 |
| Description | Powys Dance CELL Project |
| Form Of Engagement Activity | Participation in an activity, workshop or similar |
| Part Of Official Scheme? | No |
| Geographic Reach | Local |
| Primary Audience | Other audiences |
| Results and Impact | On behalf of Imperial's Outreach Department, I have been collaborating with a Welsh dance company (Powys Dance) for the production of the show CELL DANCE. We have given scientific inputs to the choreographer, dancers, music composer, and inflatable artist. The show will visualise (1) the research life and lab; (2) cells; (3) T cell response; and DNA and chromatin. The first show will be at Imperial in July 2019, and Powys Dance will do a tour in Wales. We will also produce a website (will be hosted by Imperial) to provide scientific backgrounds to children and teachers. Furthermore, we are preparing to produce a comic for the show. The impact is so far ~10 artists involved (since the show is still being prepared) but after the release of website and the tour, we expect that we can reach more than 500 people. |
| Year(s) Of Engagement Activity | 2018 |