Lactate reprograms glioblastoma immunity through CBX3-regulated histone lactylation
Shuai Wang, … , Dimitris G. Placantonakis, Jeremy N. Rich
Shuai Wang, … , Dimitris G. Placantonakis, Jeremy N. Rich
Published November 15, 2024
Citation Information: J Clin Invest. 2024;134(22):e176851. https://doi.org/10.1172/JCI176851.
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Research Article Metabolism Oncology

Lactate reprograms glioblastoma immunity through CBX3-regulated histone lactylation

Abstract

Glioblastoma (GBM), an aggressive brain malignancy with a cellular hierarchy dominated by GBM stem cells (GSCs), evades antitumor immunity through mechanisms that remain incompletely understood. Like most cancers, GBMs undergo metabolic reprogramming toward glycolysis to generate lactate. Here, we show that lactate production by patient-derived GSCs and microglia/macrophages induces tumor cell epigenetic reprogramming through histone lactylation, an activating modification that leads to immunosuppressive transcriptional programs and suppression of phagocytosis via transcriptional upregulation of CD47, a “don’t eat me” signal, in GBM cells. Leveraging these findings, pharmacologic targeting of lactate production augments efficacy of anti-CD47 therapy. Mechanistically, lactylated histone interacts with the heterochromatin component chromobox protein homolog 3 (CBX3). Although CBX3 does not possess direct lactyltransferase activity, CBX3 binds histone acetyltransferase (HAT) EP300 to induce increased EP300 substrate specificity toward lactyl-CoA and a transcriptional shift toward an immunosuppressive cytokine profile. Targeting CBX3 inhibits tumor growth by both tumor cell–intrinsic mechanisms and increased tumor cell phagocytosis. Collectively, these results suggest that lactate mediates metabolism-induced epigenetic reprogramming in GBM that contributes to CD47-dependent immune evasion, which can be leveraged to augment efficacy of immuno-oncology therapies.

Authors

Shuai Wang, Tengfei Huang, Qiulian Wu, Huairui Yuan, Xujia Wu, Fanen Yuan, Tingting Duan, Suchet Taori, Yingming Zhao, Nathaniel W. Snyder, Dimitris G. Placantonakis, Jeremy N. Rich

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Figure 6

CBX3 promotes histone lactylation by increasing catalytic ability of EP300.

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CBX3 promotes histone lactylation by increasing catalytic ability of EP3...
(A) Enrichment analysis by Metascape shows gene ontology terms enriched among lactylated proteins. (B) Top 10 proteins IP with an antibody against lactylated lysine (Kla). (C) Co-IP analysis of Kla and CBX3 in GSC23 and CW468 cells with either an IgG control or anti-CBX3 antibody. (D) Immunofluorescence staining of CBX3, EP300, and Kla in GSC23 and CW468. DAPI marks nuclei. Scale bars: 10 μm. (E) Western blot shows that His-CBX3 protein increases the lactyl-transferase of EP300. CBX3 has no effect on the acetyl-transferase function of EP300. (F) Western blot shows the levels of histone lactylation in GSC23 and CW468 cells transduced with either shCONT, shCBX3.295, or shCBX3.370. Histone 3 and Tubulin were used as loading controls.