Branched-chain keto acids promote an immune-suppressive and neurodegenerative microenvironment in leptomeningeal disease

Author:

Khaled Mariam Lotfy,Ren Yuan,Kundalia Ronak,Alhaddad Hasan,Chen Zhihua,Wallace Gerald C.,Evernden Brittany,Ospina Oscar E.,Hall MacLean,Liu Min,Darville Lancia N.F.,Izumi Victoria,Chen Y. Ann,Pilon-Thomas Shari,Stewart Paul A.,Koomen John M.,Corallo Salvatore A.,Jain Michael D.,Robinson Timothy J.,Locke Fredrick L.,Forsyth Peter A.,Smalley InnaORCID

Abstract

AbstractLeptomeningeal disease (LMD) occurs when tumors seed into the leptomeningeal space and cerebrospinal fluid (CSF), leading to severe neurological deterioration and poor survival outcomes. We utilized comprehensive multi-omics analyses of CSF from patients with lymphoma LMD to demonstrate an immunosuppressive cellular microenvironment and identified dysregulations in proteins and lipids indicating neurodegenerative processes. Strikingly, we found a significant accumulation of toxic branched-chain keto acids (BCKA) in the CSF of patients with LMD. The BCKA accumulation was found to be a pan-cancer occurrence, evident in lymphoma, breast cancer, and melanoma LMD patients. Functionally, BCKA disrupted the viability and function of endogenous T lymphocytes, chimeric antigen receptor (CAR) T cells, neurons, and meningeal cells. Treatment of LMD mice with BCKA-reducing sodium phenylbutyrate significantly improved neurological function, survival outcomes, and efficacy of anti-CD19 CAR T cell therapy. This is the first report of BCKA accumulation in LMD and provides preclinical evidence that targeting these toxic metabolites improves outcomes.

Publisher

Cold Spring Harbor Laboratory

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