Selective inhibition of HDAC3 targets synthetic vulnerabilities and activates immune surveillance in lymphoma

Mondello, Patrizia; Tadros, Saber; Teater, Matt; Fontán, Lorena; Chang, Amy; Jain, Nitin; Singh, Shailbala; J., M. C.; Yang, Haopeng; Toska, Eneda; Alig, Stefan; Durant, Matt; Stanchina, Elisa de; Mottok, Anja; Nastoupil, Loretta J.; Neelapu, Sattva S.; Weigert, Oliver; Inghirami, Giorgio; Baselga, José; Dhogan, A.; Younes, Anas; Yee, Cassian; Scheinberg, David A.; Melnick, Ari; Green, M.

doi:10.1101/531954

Cited by 12 publications

(23 citation statements)

References 41 publications

(61 reference statements)

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“…87 HDAC3 selective inhibitors yield transcriptional signatures in DLBCL cells consisting almost entirely of gene activation, consistent with their effects being truly epigenetic 165. HDAC3 is mostly contained in SMRT and NCOR corepressor complexes, which in GC B cells are almost uniquely associated with BCL6.…”

mentioning

confidence: 78%

“…81,150 By genetic DLBCL subtypes, SP1R2 and GNA13 are disrupted in 38% of EZB cases, 81 GNA13 is frequently altered in C3, and both GNA13 and its downstream mediators RHOA and SGK1 are disrupted in C4. 165 Somatic mutation of EZH2 is associated with profound silencing of both MHC I and MHC II genes, and EZH2-mutant lymphomas in both mouse and humans manifest reduced expression of these genes and a reduction in lymphoma infiltrating CD4 and CD8 T cells. MHC class II-dependent manner.…”

Section: Gα Migration Pathwaymentioning

confidence: 99%

“…165,186 Perhaps a more precise approach for targeting the epigenome is provided by specific EZH2 inhibitors, which are particularly effective in suppressing EZH2 mutant lymphoma cells and EZH2 mutant lymphomas in humans. 165,186 Perhaps a more precise approach for targeting the epigenome is provided by specific EZH2 inhibitors, which are particularly effective in suppressing EZH2 mutant lymphoma cells and EZH2 mutant lymphomas in humans.…”

Section: Epigenetic Therapymentioning

confidence: 99%

“…HDAC3 selective inhibitors are of interest for precision therapy of patients with CREBBP-mutant lymphomas. The major benefits of these compounds is expected to be in restoring anti-lymphoma immunity through induction of MHC I/II, with potential synergy in combination with checkpoint inhibitors, and in their ability to achieve full target suppression without invoking the toxicity associated with pan-HDAC inhibitors 165. 87 HDAC3 selective inhibitors yield transcriptional signatures in DLBCL cells consisting almost entirely of gene activation, consistent with their effects being truly epigenetic 165.…”

mentioning

confidence: 98%

“…IL-10 receptor is a therapeutic target in DLBCL171 and an IL-10 receptor-neutralizing antibody prevented STAT3 activation (phosphorylation) and induction of PD-L1 protein expression 170. Therefore, BTK inhibition, NFAT targeting, or IL-10 blocking could potentially be used to improve the efficacy of T cell-directed therapies.Finally, PD-L1 is co-regulated with MHC I/II through IFNγ response pathways, which are suppressed by BCL6 in GC B cells, an effect that is again reinforced by CREBBP mutation 165. Therefore, BTK inhibition, NFAT targeting, or IL-10 blocking could potentially be used to improve the efficacy of T cell-directed therapies.Finally, PD-L1 is co-regulated with MHC I/II through IFNγ response pathways, which are suppressed by BCL6 in GC B cells, an effect that is again reinforced by CREBBP mutation 165.…”

mentioning

confidence: 99%

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Germinal center‐derived lymphomas: The darkest side of humoral immunity

Mlynarczyk

Fontán

Melnick

2019

Immunological Reviews

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122

142

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Summary One of the unusual features of germinal center (GC) B cells is that they manifest many hallmarks of cancer cells. Accordingly, most B‐cell neoplasms originate from the GC reaction, and characteristically display abundant point mutations, structural genomic lesions, and clonal diversity from the genetic and epigenetic standpoints. The dominant biological theme of GC‐derived lymphomas is mutation of genes involved in epigenetic regulation and immune receptor signaling, which come into play at critical transitional stages of the GC reaction. Hence, mechanistic studies of these mutations reveal fundamental insight into the biology of the normal and malignant GC B cell. The BCL6 transcription factor plays a central role in establishing the GC phenotype in B cells, and most lymphomas are dependent on BCL6 to maintain survival, proliferation, and perhaps immune evasion. Many lymphoma mutations have the commonality of enhancing the oncogenic functions of BCL6, or overcoming some of its tumor suppressive effects. Herein, we discuss how unique features of the GC reaction create vulnerabilities that select for particular lymphoma mutations. We examine the interplay between epigenetic programming, metabolism, signaling, and immune regulatory mechanisms in lymphoma, and discuss how these are leading to novel precision therapy strategies to treat lymphoma patients.

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mentioning

confidence: 78%

Section: Gα Migration Pathwaymentioning

confidence: 99%

Section: Epigenetic Therapymentioning

confidence: 99%

mentioning

confidence: 98%

mentioning

confidence: 99%

See 3 more Smart Citations

Germinal center‐derived lymphomas: The darkest side of humoral immunity

Mlynarczyk

Fontán

Melnick

2019

Immunological Reviews

Self Cite

122

142

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Epi‐immunotherapy for cancers: rationales of epi‐drugs in combination with immunotherapy and advances in clinical trials

Liu

et al. 2022

Cancer Communications

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Over the last two decades, several epi‐drugs, immune checkpoint inhibitors (ICIs) and adoptive cell therapies have received clinical approval for use in certain types of cancer. However, monotherapy with epi‐drugs or ICIs has shown limited efficacy in most cancer patients. Epigenetic agents have been shown to regulate the crosstalk between the tumor and host immunity to alleviate immune evasion, suggesting that epi‐drugs can potentially synergize with immunotherapy. In this review, we discuss recent insights into the rationales of incorporating epigenetic therapy into immunotherapy, called epi‐immunotherapy, and focus on an update of current clinical trials in both hematological and solid malignancies. Furthermore, we outline the future challenges and strategies in the field of cancer epi‐immunotherapy.

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Vulnerabilities in the tumor and microenvironment in follicular lymphoma

Araujo-Ayala

Pérez-Galán

Campo

2021

Hematological Oncology

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Follicular lymphoma (FL) is a paradigm of tumors that require the interaction between tumor and microenvironment cells to foster their development from initial steps to progression. Recent large‐scale genome studies have uncovered multiple genetic alterations of FL that influence the microenvironment in two main directions, promoting tumor cell survival and proliferation and facilitating their evasion from immune antitumor signals. Understanding the crosstalk between tumor B‐cells and the microenvironment will facilitate the identification of vulnerabilities that may offer novel targets for treatment of the patients. This review highlights recent findings showing the effect of common genetic mutations modulating the cell composition of the tumor microenvironment and the novel therapeutic perspectives to target these interactions.

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Selective inhibition of HDAC3 targets synthetic vulnerabilities and activates immune surveillance in lymphoma

Cited by 12 publications

References 41 publications

Germinal center‐derived lymphomas: The darkest side of humoral immunity

Germinal center‐derived lymphomas: The darkest side of humoral immunity

Epi‐immunotherapy for cancers: rationales of epi‐drugs in combination with immunotherapy and advances in clinical trials

Vulnerabilities in the tumor and microenvironment in follicular lymphoma

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