A photo of a Nobel medal
BREAKING: The Nobel Prize in Physiology or Medicine has been awarded jointly to Mary E. Brunkow, Fred Ramsdell, and Shimon Sakaguchi "for their discoveries concerning peripheral immune tolerance"
Stay tuned for more.
#NobelPrize
06.10.2025 09:34
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8/ π Grateful to an outstanding team of collaborators and co-authors for their input to our project. @knollelab.bsky.social @jboettcherlab.bsky.social and all others that are not on social media
23.06.2025 07:51
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7/ π₯ Clinical implications:
The PUFAβlipid peroxide axis we have identified represents a targetable metabolic checkpoint to enhance immunotherapy in HCC.
23.06.2025 07:51
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6/ π‘ Conclusion:
MASLD generates a lipid-driven immunosuppressive microenvironment by inducing metabolic exhaustion-mediated dysfunction and ferroptosis in MAIT cells - an abundant intrahepatic T cell subset with anti-tumour properties.
23.06.2025 07:51
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β’ Interfering with lipid peroxide formation reverses MAIT dysfunction and restores anti-cancer activity.
β’ A PUFA-MAIT cell gene signature correlates with poor overall survival of patients with HCC.
23.06.2025 07:51
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β’ PUFAs induce intracellular lipid peroxidation, driving metabolic exhaustion β i.e. mitochondrial and glycolytic dysfunction β and triggering ferroptosis.
23.06.2025 07:51
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3/ π¬Core findings:
β’ In MASLD, MAIT cells exhibit profound functional exhaustion, including impaired cytokine production and anti-tumour activity.
β’ Mechanistically, PUFAs accumulate selectively in MAIT cells, not in conventional CD8βΊ or NK cells.
23.06.2025 07:51
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2/ In our study, we identify a previously unrecognised immunometabolic axis that links polyunsaturated fatty acids (PUFAs) to MAIT cell dysfunction in patients with MASLD.
23.06.2025 07:51
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1/ Our latest findings provide a possible mechanism on why patients with MASLD (metabolic dysfunction-associated steatotic liver disease) are more vulnerable to liver cancer.
23.06.2025 07:51
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I am more than happy that our study on MAIT cells in MASLD and their role in liver cancer immunity is now out in Journal of Hepatology!! π€©
β¬οΈ Here's a thread about:
𧬠Immunometabolic dysfunction of MAIT cells in MASLD: A novel barrier to liver cancer immunity π§¬
(led by Sebastian Deschler)
23.06.2025 07:51
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7/ π‘ Clinical implications:
Targeting the PUFAβlipid peroxide axis represents a targetable metabolic checkpoint to enhance immunotherapy in HCC.
23.06.2025 07:42
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6/ π§ Conclusion:
MASLD generates a lipid-driven immunosuppressive microenvironment by inducing metabolic exhaustion-mediated dysfunction and ferroptosis in MAIT cellsβan abundant intrahepatic T cell subset with anti-tumour properties.
23.06.2025 07:42
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5/
β’ Interfering with lipid peroxide formation reverses MAIT dysfunction and restores anti-cancer activity.
β’ A PUFA-MAIT cell gene signature correlates with poor overall survival of patients with HCC.
23.06.2025 07:42
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4/
β’ PUFAs induce intracellular lipid peroxidation, driving metabolic exhaustion β mitochondrial and glycolytic dysfunction β and triggering ferroptosis.
23.06.2025 07:42
π 0
π 0
π¬ 1
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3/ π¬Core findings:
β’ In MASLD, MAIT cells exhibit profound functional exhaustion, including impaired cytokine production and anti-tumor activity.
β’ Mechanistically, PUFAs accumulate selectively in MAIT cells, not in conventional CD8βΊ or NK cells.
23.06.2025 07:42
π 0
π 0
π¬ 1
π 0
2/ In our study, we identify a previously unrecognized immunometabolic axis that links polyunsaturated fatty acids (PUFAs) to MAIT cell dysfunction in patients with MASLD.
23.06.2025 07:42
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1/ Our latest findings provide a possible mechanism on why patients with MASLD (metabolic dysfunction-associated steatotic liver disease) are more vulnerable to liver cancer.
23.06.2025 07:42
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8/ π Grateful to an outstanding team of collaborators and co-authors for their input to our project. @knollelab.bsky.social @jboettcherlab.bsky.social
23.06.2025 07:35
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7/ π‘ Clinical implications:
Targeting the PUFAβlipid peroxide axis represents a targetable metabolic checkpoint to enhance immunotherapy in HCC.
23.06.2025 07:35
π 0
π 0
π¬ 1
π 0
6/ π§ Conclusion:
MASLD generates a lipid-driven immunosuppressive microenvironment by inducing metabolic exhaustion-mediated dysfunction and ferroptosis in MAIT cellsβan abundant intrahepatic T cell subset with anti-tumour properties.
23.06.2025 07:35
π 0
π 0
π¬ 1
π 0
5/
β’ Interfering with lipid peroxide formation reverses MAIT dysfunction and restores anti-cancer activity.
β’ A PUFA-MAIT cell gene signature correlates with poor overall survival of patients with HCC.
23.06.2025 07:35
π 0
π 0
π¬ 1
π 0
4/
β’ PUFAs induce intracellular lipid peroxidation, driving metabolic exhaustion β mitochondrial and glycolytic dysfunction β and triggering ferroptosis.
23.06.2025 07:35
π 0
π 0
π¬ 1
π 0
3/ π¬Core findings:
β’ In MASLD, MAIT cells exhibit profound functional exhaustion, including impaired cytokine production and anti-tumour activity.
β’ Mechanistically, PUFAs accumulate selectively in MAIT cells, not in conventional CD8βΊ or NK cells.
23.06.2025 07:35
π 0
π 0
π¬ 1
π 0
2/ In our study, we identify a previously unrecognised immunometabolic axis that links polyunsaturated fatty acids (PUFAs) to MAIT cell dysfunction in patients with MASLD.
23.06.2025 07:35
π 0
π 0
π¬ 1
π 0
1/ Our latest findings provide a possible mechanism on why patients with MASLD (metabolic dysfunction-associated steatotic liver disease) are more vulnerable to liver cancer.
23.06.2025 07:35
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PhD Student in Cancer Immunology
The team is growing - if youβre interested in doing a PhD in translational research at the interface of #immunology, #oncology and #Tcellengineering at the M3 Research Center in TΓΌbingen, follow the link below for more information and apply!
jobs.medizin.uni-tuebingen.de/Job/6357/PhD...
28.05.2025 09:27
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π€© Thrilled and honoured to talk MAIT cells at the Falk Experimental Days of Hepatology among a fantastic lineup of researchers in Lyon today π€©#MAITs #hepatology #translation #immunology
25.04.2025 09:57
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#MAITcells #Tcells #CARTcells #liverimmunology #MR1 #cancer #immunometabolism #Tcellengineering #immunotherapy #immuneoncology
04.03.2025 16:00
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