Molecular regulation of NK cell functional maturation by the transcription factor BACH2
Lead Research Organisation:
Babraham Institute
Department Name: Immunology
Abstract
Natural killer (NK) cells are a specialised immune cell type that form a critical first line of defence against cancer and infection. NK cells recognise cancer cells and infections in a different way to CD8+ T cells. This makes them attractive as alternate targets for immunotherapy. Clinical responses to NK cell-targeted immunotherapies have thus far been modest identifying a need to better understand molecular processes that restrict their function.
NK cells exist in a variety of different states, called functional maturation states. These have important implications for their ability to control infections and cancer. We lack an understanding of how NK cell functional maturation is regulated, though identifying such mechanisms may provide new therapeutic targets in NK cell-based immune therapies. In people, genetic variations in a gene that encodes a transcription factor protein called BACH2 are associated with susceptibility to multiple autoimmune and allergic diseases, caused when the immune system undergoes excessive activation. Recent experiments conducted in our laboratories indicate that BACH2 is expressed in NK cells and negatively regulates their functional maturation with consequences for tumour immunity.
The purpose of this work is to establish the function of BACH2 in NK cells, testing the hypothesis that it is a critical negative regulator of NK cell functional maturation and testing its consequences for homeostasis and immune responses to infection and cancer.
Our proposed study is organised into three aims: Firstly, we will find out how BACH2 affects the behaviour of NK cells under normal conditions, and during infection with influenza, where NK cells can contribute to both viral clearance and excessive inflammation. Secondly, we will examine the effect of BACH2 in NK cell responses against cancer, both in NK cells existing within the body, and upon therapeutic transfer into tumour-bearing hosts. Finally, we will examine the molecular processes that underpin the function of BACH2, finding out where BACH2 binds in NK cell genomes and which genes it regulates.
Collectively, this research will enable a better understanding of how the function of the immune system is controlled to under normal conditions and during infections and cancer. This may enable development of new therapies that work by either restraining or enhancing immune responses in individuals with inflammation, infections and cancer.
NK cells exist in a variety of different states, called functional maturation states. These have important implications for their ability to control infections and cancer. We lack an understanding of how NK cell functional maturation is regulated, though identifying such mechanisms may provide new therapeutic targets in NK cell-based immune therapies. In people, genetic variations in a gene that encodes a transcription factor protein called BACH2 are associated with susceptibility to multiple autoimmune and allergic diseases, caused when the immune system undergoes excessive activation. Recent experiments conducted in our laboratories indicate that BACH2 is expressed in NK cells and negatively regulates their functional maturation with consequences for tumour immunity.
The purpose of this work is to establish the function of BACH2 in NK cells, testing the hypothesis that it is a critical negative regulator of NK cell functional maturation and testing its consequences for homeostasis and immune responses to infection and cancer.
Our proposed study is organised into three aims: Firstly, we will find out how BACH2 affects the behaviour of NK cells under normal conditions, and during infection with influenza, where NK cells can contribute to both viral clearance and excessive inflammation. Secondly, we will examine the effect of BACH2 in NK cell responses against cancer, both in NK cells existing within the body, and upon therapeutic transfer into tumour-bearing hosts. Finally, we will examine the molecular processes that underpin the function of BACH2, finding out where BACH2 binds in NK cell genomes and which genes it regulates.
Collectively, this research will enable a better understanding of how the function of the immune system is controlled to under normal conditions and during infections and cancer. This may enable development of new therapies that work by either restraining or enhancing immune responses in individuals with inflammation, infections and cancer.
Technical Summary
Natural killer (NK) cells are cytotoxic innate lymphocytes that form a critical first line of defence against cancer and infection. Unlike CD8+ T cells, recognition of cancer cells by NK cells is independent of neo-antigens and potentiated by defects in antigen presentation, making them attractive as mechanistically distinct targets to CD8+ T cells for cancer immunotherapy. Clinical responses to NK cell-targeted immunotherapies have thus far been modest identifying a need to better understand molecular mechanisms that restrict their function.
NK cells exist in a variety of different states, called functional maturation states. These have important implications for their ability to control infections and cancer. We lack an understanding of negative regulators of NK cell functional maturation, though identifying such mechanisms may provide new therapeutic targets for NK cell-based immunotherapies. BACH2 is a transcriptional repressor whose expression is predominantly restricted to lymphocytes. New data indicates that BACH2 is an intrinsic negative regulator of NK cell functional maturation with consequences for homeostasis and anti-tumour immunity. The purpose of this work is to establish the function of BACH2 in NK cells, testing the hypothesis that it is a critical negative regulator of NK cell functional maturation and testing its consequences for homeostasis and immune responses to infection and cancer.
Our proposed study is organised into three aims: 1. We will determine how BACH2 affects NK cells function under normal conditions, and during influenza infection, where NK cells can contribute to both clearance and immunopathology. 2. We will examine the effect of BACH2 in restraining NK cell responses to cancer. 3. We will map the genome-wide epigenetic and transcriptional changes that occur with NK cell functional maturation and examine the component of the NK cell functional maturation programme controlled by BACH2.
NK cells exist in a variety of different states, called functional maturation states. These have important implications for their ability to control infections and cancer. We lack an understanding of negative regulators of NK cell functional maturation, though identifying such mechanisms may provide new therapeutic targets for NK cell-based immunotherapies. BACH2 is a transcriptional repressor whose expression is predominantly restricted to lymphocytes. New data indicates that BACH2 is an intrinsic negative regulator of NK cell functional maturation with consequences for homeostasis and anti-tumour immunity. The purpose of this work is to establish the function of BACH2 in NK cells, testing the hypothesis that it is a critical negative regulator of NK cell functional maturation and testing its consequences for homeostasis and immune responses to infection and cancer.
Our proposed study is organised into three aims: 1. We will determine how BACH2 affects NK cells function under normal conditions, and during influenza infection, where NK cells can contribute to both clearance and immunopathology. 2. We will examine the effect of BACH2 in restraining NK cell responses to cancer. 3. We will map the genome-wide epigenetic and transcriptional changes that occur with NK cell functional maturation and examine the component of the NK cell functional maturation programme controlled by BACH2.
Planned Impact
In addition to its immediate impact for basic and pre-clinical academic research (see Academic Beneficiaries), this work will be relevant for the following groups:
A) The biomedical industry: The proposed work will establish a critical molecular pathway that negatively regulates NK cell function. Identification of pathways that negatively regulate immune function is of interest to the industrial sector in their attempts to develop new treatments for patients with autoimmunity and allergy, chronic infections and cancer. Where relevant, we will pursue commercial opportunities generated from this research by developing projects with new and existing industrial collaborators, including CRUK Therapeutic Discovery Laboratories and F-Star Biotechnology (see Pathways to Impact for details). We will engage in industrial collaborations with the assistance of Babraham Institute Enterprise (BIE). BIE is the wholly owned trading arm of the Babraham Institute (BI) and manages, develops and commercialises the Institute's intellectual property portfolio, as well as facilitating collaborations between the Institute and industry. Successful commercial exploitation of the results will have impact by directly fostering UK and global economic growth.
B) The Babraham Institute and affiliates: Should the research lead directly to commercially exploitable outcomes, BIE has arrangements for protection and development of intellectual property and a track record in exploitation of the Institute's science. We will actively pursue commercial opportunities using an approach outlined in the Pathways to Impact section. Commercialisation of Babraham Institute science will directly benefit the Institute and affiliated parties by generating new revenue.
C) The UK skilled workforce: This will have immediate impact by enhancing skills within the UK workforce. Undertaking the proposed research will result in recruitment and training of a post-doctoral researcher at a world-class UK research institute in the fields of tumour immunology, NK cell biology and gene regulation and will enable the postdoctoral researcher to advance their career, potentially towards scientific independence. We encourage researchers to gain skills in bioinformatics and statistics through attendance of regularly held training sessions at the Babraham Institute. These research skills are relevant for both a career in academic or industrial science. The postdoctoral researcher will also gain presentation skills and the opportunity to expand their network of scientific and industrial contacts through the opportunity to attend an International conference, for which funding has been requested.
By being involved in this research, a variety of technical and scientific staff at the Babraham Institute, including Animal Facility technicians and managers, will gain new skills required to perform mouse tumour immunology and NK cell biology experiments. These technical skills will be relevant to a variety of academic and industrial research sectors.
D) Patients and the National Health Service: Immunotherapy is revolutionising the treatment of metastatic cancer. We will publish and present results of this work, thereby informing basic and translational research in NK cell-based cancer immunotherapy with the potential to generate mid- to long-term benefits to healthcare. Development of new treatments will benefit patients and the National Health Service. Such benefits would be realised in the mid- to long-term (5-20 years).
E) The general public: There is significant public interest in the interaction of cancer with the immune system and in development of new immunotherapies. We will engage public audiences with the results of our research through media communications and through presentations and open days (see Communications plan). Both the PIs and the PDRA will take part in Babraham's Annual Schools Days each year of the project.
A) The biomedical industry: The proposed work will establish a critical molecular pathway that negatively regulates NK cell function. Identification of pathways that negatively regulate immune function is of interest to the industrial sector in their attempts to develop new treatments for patients with autoimmunity and allergy, chronic infections and cancer. Where relevant, we will pursue commercial opportunities generated from this research by developing projects with new and existing industrial collaborators, including CRUK Therapeutic Discovery Laboratories and F-Star Biotechnology (see Pathways to Impact for details). We will engage in industrial collaborations with the assistance of Babraham Institute Enterprise (BIE). BIE is the wholly owned trading arm of the Babraham Institute (BI) and manages, develops and commercialises the Institute's intellectual property portfolio, as well as facilitating collaborations between the Institute and industry. Successful commercial exploitation of the results will have impact by directly fostering UK and global economic growth.
B) The Babraham Institute and affiliates: Should the research lead directly to commercially exploitable outcomes, BIE has arrangements for protection and development of intellectual property and a track record in exploitation of the Institute's science. We will actively pursue commercial opportunities using an approach outlined in the Pathways to Impact section. Commercialisation of Babraham Institute science will directly benefit the Institute and affiliated parties by generating new revenue.
C) The UK skilled workforce: This will have immediate impact by enhancing skills within the UK workforce. Undertaking the proposed research will result in recruitment and training of a post-doctoral researcher at a world-class UK research institute in the fields of tumour immunology, NK cell biology and gene regulation and will enable the postdoctoral researcher to advance their career, potentially towards scientific independence. We encourage researchers to gain skills in bioinformatics and statistics through attendance of regularly held training sessions at the Babraham Institute. These research skills are relevant for both a career in academic or industrial science. The postdoctoral researcher will also gain presentation skills and the opportunity to expand their network of scientific and industrial contacts through the opportunity to attend an International conference, for which funding has been requested.
By being involved in this research, a variety of technical and scientific staff at the Babraham Institute, including Animal Facility technicians and managers, will gain new skills required to perform mouse tumour immunology and NK cell biology experiments. These technical skills will be relevant to a variety of academic and industrial research sectors.
D) Patients and the National Health Service: Immunotherapy is revolutionising the treatment of metastatic cancer. We will publish and present results of this work, thereby informing basic and translational research in NK cell-based cancer immunotherapy with the potential to generate mid- to long-term benefits to healthcare. Development of new treatments will benefit patients and the National Health Service. Such benefits would be realised in the mid- to long-term (5-20 years).
E) The general public: There is significant public interest in the interaction of cancer with the immune system and in development of new immunotherapies. We will engage public audiences with the results of our research through media communications and through presentations and open days (see Communications plan). Both the PIs and the PDRA will take part in Babraham's Annual Schools Days each year of the project.
Publications
Alvisi G
(2020)
IRF4 instructs effector Treg differentiation and immune suppression in human cancer.
in The Journal of clinical investigation
Alvisi G
(2020)
IRF4 instructs effector Treg differentiation and immune suppression in human cancer.
in The Journal of clinical investigation
Gallimore A
(2019)
Regulatory T cells in cancer: where are we now?
in Immunology
Gautam S
(2019)
The transcription factor c-Myb regulates CD8+ T cell stemness and antitumor immunity.
in Nature immunology
Grant FM
(2020)
BACH2 drives quiescence and maintenance of resting Treg cells to promote homeostasis and cancer immunosuppression.
in The Journal of experimental medicine
Imianowski CJ
(2022)
BACH2 restricts NK cell maturation and function, limiting immunity to cancer metastasis.
in The Journal of experimental medicine
Nasrallah R
(2020)
A distal enhancer at risk locus 11q13.5 promotes suppression of colitis by Treg cells.
in Nature
Sadiyah MF
(2019)
Genome-Wide Measurement and Computational Analysis of Transcription Factor Binding and Chromatin Accessibility in Lymphocytes.
in Current protocols in immunology
Stockis J
(2019)
Regulation of regulatory T cells in cancer
in Immunology
Vardaka P
(2020)
A cell-based bioluminescence assay reveals dose-dependent and contextual repression of AP-1-driven gene expression by BACH2.
in Scientific reports
| Description | AstraZeneca Postdoctoral Research Grant (2 years) |
| Amount | £468,000 (GBP) |
| Organisation | AstraZeneca |
| Sector | Private |
| Country | United Kingdom |
| Start | 04/2022 |
| End | 03/2024 |
| Title | Development of a cell-based reporter assay for high-throughput screening of small molecule inhibitors of BACH2 function |
| Description | A cell-based reporter assay for high-throughput screening of small molecule inhibitors of BACH2 function as was a major aim of the funded work |
| Type Of Material | Cell line |
| Year Produced | 2008 |
| Provided To Others? | No |
| Impact | This is now enabling high-throughput screening which is planned for later this year. |
| Title | Generation of a NK cell-specific Bach2 conditional knockout mouse |
| Description | Generation of a NK cell-specific Bach2 conditional knockout mouse |
| Type Of Material | Model of mechanisms or symptoms - mammalian in vivo |
| Year Produced | 2020 |
| Provided To Others? | No |
| Impact | This will enable the molecular mechanisms that control natural killer cell function in the context of homeostasis, infection and tumour immunity to be determined. |
| Title | Methods for Genome-Wide Measurement and Computational Analysis of Transcription Factor Binding and Chromatin Accessibility in Lymphocytes |
| Description | Cells of the adaptive immune system, including CD4+ and CD8+ T cells, as well as B cells, possess the ability to undergo dynamic changes in population size, differentiation state, and function to counteract diverse and temporally stochastic threats from the external environment. To achieve this, lymphocytes must be able to rapidly control their gene-expression programs in a cell-type-specific manner and in response to extrinsic signals. Such capacity is provided by transcription factors (TFs), which bind to the available repertoire of regulatory DNA elements in distinct lymphocyte subsets to program cell-type-specific gene expression. Here we provide a set of protocols that utilize massively parallel sequencing-based approaches to map genome-wide TF-binding sites and accessible chromatin, with consideration of the unique aspects and technical issues facing their application to lymphocytes. We show how to computationally validate and analyze aligned data to map differentially enriched/accessible sites, identify enriched DNA sequence motifs, and detect the position of nucleosomes adjacent to accessible DNA elements. |
| Type Of Material | Technology assay or reagent |
| Year Produced | 2019 |
| Provided To Others? | Yes |
| Impact | These techniques, when applied to immune cells, can enhance our understanding of how gene-expression programs are controlled within lymphocytes to coordinate immune function in homeostasis and disease. |
| URL | https://pubmed.ncbi.nlm.nih.gov/31483104/ |
| Title | Molecular profiles of mature NK subsets and effect of transcriptional regulator BACH2 on NK cell transcriptional profiles |
| Description | RNA-Seq of Bach2-deficient and WT NK cells RNA-Seq of NK cells in diverse maturation states |
| Type Of Material | Database/Collection of data |
| Year Produced | 2022 |
| Provided To Others? | No |
| Impact | This has shed light on how NK cells develop and contribute to cancer immunosurveillance in tissues |
| Description | Collaboration between the University of Cambridge Department of Pathology and CRUK Cambridge Cancer Institute |
| Organisation | Cancer Research UK Cambridge Institute |
| Country | United Kingdom |
| Sector | Academic/University |
| PI Contribution | Describing the transcriptional changes associated with NK cell maturation |
| Collaborator Contribution | The research on NK cell maturation and function has fostered a collaboration between my group at the University of Cambridge and that of Dr Tim Halim at CRUK Cambridge Institute, enabling exchange of ideas and reagents |
| Impact | Scientific results (manuscript presently under review); High-content data |
| Start Year | 2020 |
| Description | Collaboration with Crescendo Biologics to develop ways of improving the anti-cancer activity of NK cells |
| Organisation | Crescendo Biologics |
| Country | United Kingdom |
| Sector | Private |
| PI Contribution | By studying negative regulators of NK cell function in tumours, we have discovered an inhibitory pathway that is a potential drug target for augmentation of NK cell function. We are exploring the therapeutic potential of this pathway as part of a collaboration with Crescendo Biologics |
| Collaborator Contribution | Antibody development pipeline. The company will host a member of the laboratory in their organisation to conduct research |
| Impact | None yet |
| Start Year | 2019 |
| Description | Contribution to Cambridge Festival of Ideas public event on cancer immunology |
| Form Of Engagement Activity | A talk or presentation |
| Part Of Official Scheme? | No |
| Geographic Reach | Regional |
| Primary Audience | Public/other audiences |
| Results and Impact | The inaugural Cambridge Festival, which runs from 26 March - 4 April, brings together the hugely popular Cambridge Science Festival and the Cambridge Festival of Ideas. It hosts an extensive programme of over 350 events that tackle many of the critical global challenges affecting us all, and features hundreds of renowned experts in the field of health and medicine. The key themes are health, society, environment and explore. Over 120 events focus on health. We held a public event on how cancer immunotherapy harnesses the power of our immune system in the fight against cancer: Innovation from Laboratory Bench to Bedside |
| Year(s) Of Engagement Activity | 2021 |
| Description | Participation in an activity, workshop or similar - School visit to the Roychoudhuri laboratory for hands-on experience in flow cytometry and cellular immunology |
| Form Of Engagement Activity | Participation in an open day or visit at my research institution |
| Part Of Official Scheme? | No |
| Geographic Reach | Regional |
| Primary Audience | Schools |
| Results and Impact | The laboratory hosted a group of 6 sixth form school students to undertake a flow cytometry experiment in cellular immunology with bench research, teaching from PhD and Postdocs in the group |
| Year(s) Of Engagement Activity | 2020 |
| Description | School visit to the Roychoudhuri laboratory for hands-on experience in flow cytometry and cellular immunology |
| Form Of Engagement Activity | Participation in an activity, workshop or similar |
| Part Of Official Scheme? | No |
| Geographic Reach | National |
| Primary Audience | Schools |
| Results and Impact | Two groups of six school children were hosted in the laboratory and were provided hands-on experience processing tissues and using flow cytometry to distinguish populations of lymphoid cells in secondary lymphoid organs using multiparameter flow cytometry. Students were also taught basic scientific background relating to the adaptive immune system |
| Year(s) Of Engagement Activity | 2019 |