Mitochondrial ABHD11 inhibition drives sterol metabolism to modulate T-cell effector function.

Jenkins, Benjamin J; Jenkins, Yasmin R; Ponce-Garcia, Fernando M; Moscrop, Chloe; Perry, Iain A; Hitchings, Matthew D; Uribe, Alejandro H; Bernuzzi, Federico; Eastham, Simon; Cronin, James G; Berisha, Ardena; Howell, Alexandra; Davies, Joanne; Blagih, Julianna; Williams, Marta; Marsden, Morgan; Veale, Douglas J; Davies, Luke C; Niphakis, Micah; Finlay, David K; Sinclair, Linda V; Cravatt, Benjamin F; Hogan, Andrew E; Nathan, James A; Humphreys, Ian R; Fearon, Ursula; Sumpton, David; Voorde, Johan Vande; do Vale, Goncalo Dias; McDonald, Jeffrey G; Jones, Gareth W; Pearson, James A; Vincent, Emma E; Jones, Nicholas

Mitochondrial ABHD11 inhibition drives sterol metabolism to modulate T-cell effector function.

https://hdl.handle.net/10779/crick.30581324

journal contribution

posted on 2025-11-10, 13:38 authored by Benjamin J Jenkins, Yasmin R Jenkins, Fernando M Ponce-Garcia, Chloe Moscrop, Iain A Perry, Matthew D Hitchings, Alejandro H Uribe, Federico Bernuzzi, Simon Eastham, James G Cronin, Ardena Berisha, Alexandra Howell, Joanne Davies, Julianna Blagih, Marta Williams, Morgan Marsden, Douglas J Veale, Luke C Davies, Micah Niphakis, David K Finlay, Linda V Sinclair, Benjamin F Cravatt, Andrew E Hogan, James A Nathan, Ian R Humphreys, Ursula Fearon, David Sumpton, Johan Vande Voorde, Goncalo Dias do Vale, Jeffrey G McDonald, Gareth W Jones, James A Pearson, Emma E Vincent, Nicholas Jones

α/β-hydrolase domain-containing protein 11 (ABHD11) is a mitochondrial hydrolase that maintains the catalytic function of α-ketoglutarate dehydrogenase (α-KGDH), and its expression in CD4 + T-cells has been linked to remission status in rheumatoid arthritis (RA). However, the importance of ABHD11 in regulating T-cell metabolism and function is yet to be explored. Here, we show that pharmacological inhibition of ABHD11 dampens cytokine production by human and mouse T-cells. Mechanistically, the anti-inflammatory effects of ABHD11 inhibition are attributed to increased 24,25-epoxycholesterol (24,25-EC) biosynthesis and subsequent liver X receptor (LXR) activation, which arise from a compromised TCA cycle. The impaired cytokine profile established by ABHD11 inhibition is extended to two patient cohorts of autoimmunity. Importantly, using murine models of accelerated type 1 diabetes (T1D), we show that targeting ABHD11 suppresses cytokine production in antigen-specific T-cells and delays the onset of diabetes in vivo in female mice. Collectively, our work provides pre-clinical evidence that ABHD11 is an encouraging drug target in T-cell-mediated inflammation.