Matt Coelho
@mattcoelho.bsky.social
Cancer Research UK Career Development Fellow at the Wellcome Sanger Institute - gene editing - drug resistance - cancer
A pleasure to talk about our research today with the amazing volunteers at St John’s ambulance in aid of @cancerresearchuk.org
October 10, 2025 at 8:51 PM
A pleasure to talk about our research today with the amazing volunteers at St John’s ambulance in aid of @cancerresearchuk.org
Finally, in patients, tumors with lower CHD1 and MAP3K7 expression responded better to cancer immunotherapy, suggesting that these genes could serve as biomarkers of response to ICB.
April 22, 2025 at 7:56 AM
Finally, in patients, tumors with lower CHD1 and MAP3K7 expression responded better to cancer immunotherapy, suggesting that these genes could serve as biomarkers of response to ICB.
In mice, knocking out these genes in tumour cells led to improved responses to immune-checkpoint blockade (ICB) and increased T cell numbers and activation in tumours.
April 22, 2025 at 7:56 AM
In mice, knocking out these genes in tumour cells led to improved responses to immune-checkpoint blockade (ICB) and increased T cell numbers and activation in tumours.
CHD1 and MAP3K7 KO additively sensitises cancer cells to IFN-g, TNF-a and T cells and are known activators of NF-kB signalling. RNA-seq revealed they regulate the transcriptional response to cytokines involving the TF CDX2, overall switching the cell response from apoptosis to cell survival.
April 22, 2025 at 7:56 AM
CHD1 and MAP3K7 KO additively sensitises cancer cells to IFN-g, TNF-a and T cells and are known activators of NF-kB signalling. RNA-seq revealed they regulate the transcriptional response to cytokines involving the TF CDX2, overall switching the cell response from apoptosis to cell survival.
We also identified known regulators of cytokine signalling as hits in our cytokine and T cells screens across multiple cell contexts (e.g. TBK1, SOCS1, ADAR), allowing us to compare the against CHD1 and MAP3K7 KO and unpick the signalling pathways involved in each case.
April 22, 2025 at 7:56 AM
We also identified known regulators of cytokine signalling as hits in our cytokine and T cells screens across multiple cell contexts (e.g. TBK1, SOCS1, ADAR), allowing us to compare the against CHD1 and MAP3K7 KO and unpick the signalling pathways involved in each case.
Through integrating these data, we identify CHD1 and MAP3K7 as key determinants of resistance to T cell attack. Our individual cytokine screens and the use of JAK1/2 KO isogenic cancer cell models allowed us to deconvolute different contributions of cytokines on T cell-mediated killing.
April 22, 2025 at 7:56 AM
Through integrating these data, we identify CHD1 and MAP3K7 as key determinants of resistance to T cell attack. Our individual cytokine screens and the use of JAK1/2 KO isogenic cancer cell models allowed us to deconvolute different contributions of cytokines on T cell-mediated killing.
These T cells are derived from the same patient as the tumoroids - endogenous neoantigen expression drives reactivity. Special thanks to our collaborators from the Voest lab for pioneering this sophisticated system for studying anti-tumour immunity.
April 22, 2025 at 7:56 AM
These T cells are derived from the same patient as the tumoroids - endogenous neoantigen expression drives reactivity. Special thanks to our collaborators from the Voest lab for pioneering this sophisticated system for studying anti-tumour immunity.
We used whole-genome CRISPR/Cas9 screens in autologous primary tumoroid T cell co-cultures to investigate genes that modulate cancer cell killing by T cells.
April 22, 2025 at 7:56 AM
We used whole-genome CRISPR/Cas9 screens in autologous primary tumoroid T cell co-cultures to investigate genes that modulate cancer cell killing by T cells.
We generated a large-scale dataset of context-specific dependencies in 4 cancer cell models, across 4 cytokines and autologous tumour-reactive T cells, collectively encompassing data from >150 whole-genome CRISPR-Cas9 screen samples.
April 22, 2025 at 7:56 AM
We generated a large-scale dataset of context-specific dependencies in 4 cancer cell models, across 4 cytokines and autologous tumour-reactive T cells, collectively encompassing data from >150 whole-genome CRISPR-Cas9 screen samples.
Excited to announce that we're recruiting a Staff scientist at the Sanger Institute to investigate drug resistance mechanisms in cancer using gene editing.
Interested?
Apply here:
sanger.wd103.myworkdayjobs.com/en-US/Wellco...
Interested?
Apply here:
sanger.wd103.myworkdayjobs.com/en-US/Wellco...
March 12, 2025 at 1:50 PM
Excited to announce that we're recruiting a Staff scientist at the Sanger Institute to investigate drug resistance mechanisms in cancer using gene editing.
Interested?
Apply here:
sanger.wd103.myworkdayjobs.com/en-US/Wellco...
Interested?
Apply here:
sanger.wd103.myworkdayjobs.com/en-US/Wellco...