HDAC inhibiteurs/activateurs (HDAC Inhibitors/Activators)

Autre DNA Damage/DNA Repair Inhibiteurs

Produits sélectifs disoformes

• Inhibiteurs en vedette
• Inhibiteurs (91)
• Modulateur (1)
• Activateur (1)

N° Cat.	Nom du produit	Information	Citations dutilisation du produit	Validations de produits
S2170	ITF-2357 (Givinostat) Hydrochloride Monohydrate	Givinostat (ITF2357) est un puissant inhibiteur de HDAC pour le maïs HD2, HD1B et HD1A avec des IC50 de 10 nM, 7,5 nM et 16 nM dans des essais acellulaires. Phase 2.	J Leukoc Biol, 2024, qiae006 Sci Transl Med, 2022, 14(657):eabg3277 J Exp Clin Cancer Res, 2022, 41(1):325
S2759	Fimepinostat (CUDC-907)	Fimepinostat (CUDC-907) est un double inhibiteur de PI3K et HDAC ciblant PI3Kα et HDAC1/2/3/10 avec des valeurs d'IC50 de 19 nM et 1,7 nM/5 nM/1,8 nM/2,8 nM, respectivement. Ce composé induit l'arrêt du cycle cellulaire et l'apoptose dans les cellules de cancer du sein. Phase 1.	Cell Death Discov, 2025, 11(1):172 J Am Heart Assoc, 2025, 14(1):e037400 Viruses, 2024, 16(5)775
S1045	Trichostatin A (TSA)	TSA (Trichostatin A) est un inhibiteur de l'HDAC avec un IC50 d'environ 1,8 nM dans les essais sans cellules.	Nat Cell Biol, 2025, 27(1):73-86 Sci Bull (Beijing), 2025, S2095-9273(25)00472-4 Cell Rep Med, 2025, S2666-3791(25)00102-8
S1053	Entinostat (MS-275)	Entinostat (MS-275, SNDX-275) inhibe fortement HDAC1 et HDAC3 avec des IC50 de 0,51 μM et 1,7 μM dans des essais sans cellules, par rapport aux HDACs 4, 6, 8 et 10. Ce composé induit l'autophagie et l'apoptose. Phase 3.	Nat Commun, 2025, 16(1):2559 J Clin Invest, 2025, 135(11)e187490 Blood Cancer J, 2025, 15(1):108
S7229	RGFP966	RGFP966 est un inhibiteur de HDAC3 avec une IC50 de 0,08 μM dans un essai sans cellules, présentant une sélectivité > 200 fois supérieure aux autres HDAC.	Nat Commun, 2025, 16(1):2663 Nat Commun, 2025, 16(1):616 Cell Rep Med, 2025, S2666-3791(25)00102-8
S1030	Panobinostat (LBH589)	Le Panobinostat (LBH589, NVP-LBH589) est un nouvel inhibiteur de HDAC à large spectre avec une IC50 de 5 nM dans un essai sans cellule. Il induit l'autophagy et l'apoptosis, et perturbe efficacement la latence du HIV in vivo. Phase 3.	Cancer Cell, 2025, 43(4):776-796.e14 Signal Transduct Target Ther, 2025, 10(1):230 Nat Commun, 2025, 16(1):2173
S1085	Belinostat (PXD101)	Le Belinostat est un nouvel inhibiteur de l'HDAC avec un IC50 de 27 nM dans un essai sans cellules, avec une activité démontrée dans les tumeurs résistantes au cisplatine. Belinostat (PXD101) induit l'autophagy.	Cell Rep Med, 2025, S2666-3791(25)00102-8 Cell Death Dis, 2025, 16(1):743 Mol Oncol, 2025, 10.1002/1878-0261.70050
S1047	Vorinostat (SAHA)	Le Vorinostat (SAHA) est un inhibiteur de l'HDAC avec un IC50 d'environ 10 nM dans un test acellulaire et abroge l'amplification productive de l'ADN de HPV-18.	Mol Cancer, 2025, 24(1):154 Nat Commun, 2025, 16(1):28 Nucleic Acids Res, 2025, 53(20)gkaf1086
S3020	Romidepsin (FK228)	Romidepsin (FK228, Depsipeptide, FR 901228, NSC 630176) est un inhibiteur puissant de HDAC1 et HDAC2 avec des IC50 de 36 nM et 47 nM dans des essais sans cellules, respectivement. Ce composé contrôle la croissance et induit l'apoptose dans les cellules tumorales de neuroblastome.	J Extracell Vesicles, 2025, 14(2):e70042 Nucleic Acids Res, 2025, 53(20)gkaf1086 Cell Rep Med, 2025, S2666-3791(25)00102-8
S1096	Quisinostat (JNJ-26481585) Dihydrochloride	Quisinostat (JNJ-26481585) 2HCl est un nouvel inhibiteur de seconde génération de l'HDAC avec la plus forte puissance pour HDAC1 avec une IC50 de 0,11 nM dans un essai sans cellule, une puissance modérée pour les HDACs 2, 4, 10 et 11; une sélectivité supérieure à 30 fois contre les HDACs 3, 5, 8 et 9 et la plus faible puissance pour les HDACs 6 et 7. Phase 2.	Cell Discov, 2025, 11(1):81 iScience, 2024, 27(4):109366 iScience, 2024, 27(9):110775
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Classification of HDACs and HDAC Inhibitors

To understand HDACis, it is first critical to categorize their targets: HDACs are divided into four classes based on sequence homology and cofactor requirements. Class I HDACs (HDAC1, 2, 3, 8) are primarily localized in the nucleus and are ubiquitously expressed, playing essential roles in cell cycle regulation and proliferation. Class II HDACs (subdivided into IIa: HDAC4, 5, 7, 9; IIb: HDAC6, 10) shuttle between the nucleus and cytoplasm, with Class IIa involved in developmental signaling and Class IIb regulating cytoskeletal dynamics and protein degradation. Class III HDACs, also called sirtuins (SIRT1–7), depend on NAD+ as a cofactor and are implicated in metabolism, aging, and stress responses. Class IV HDAC (HDAC11) is the smallest family member, with functions in immune cell activation and lipid metabolism. HDACis are correspondingly classified based on their chemical structure and HDAC class selectivity:

1.1 Pan-HDACis:

Inhibit multiple HDAC classes, particularly Class I and II. Examples include vorinostat (SAHA) and trichostatin A (TSA). Vorinostat, the first FDA-approved HDACi (2006), targets Class I (HDAC1, 2, 3) and Class IIb (HDAC6) and is used to treat cutaneous T-cell lymphoma (CTCL).

1.2 Class I-Selective HDACis:

Preferentially inhibit Class I HDACs, reducing off-target effects on Class II enzymes. Romidepsin, a cyclic peptide HDACi, selectively targets HDAC1 and 2 and is approved for relapsed CTCL and peripheral T-cell lymphoma (PTCL).

1.3 Class II-Selective HDACis:

Focus on Class II HDACs, with potential applications in neurodegeneration and cardiovascular disease. For example, MC1568 inhibits Class IIa HDACs (HDAC4, 5, 7) and has shown promise in preclinical models of Huntington’s disease.

1.4 Class III HDAC (Sirtuin) Modulators:

Unlike other HDACis, sirtuin-targeting compounds often act as activators (e.g., resveratrol, which activates SIRT1) due to the unique NAD+-dependent mechanism of sirtuins. These modulators are studied for their roles in aging and metabolic disorders.

2. Mechanisms of Action: Beyond Histone Acetylation

The canonical mechanism of HDACis involves histone acetylation, but their biological effects extend far beyond this epigenetic regulation, driven by the modulation of non-histone proteins.

2.1 Histone-Mediated Epigenetic Regulation

HDACs remove acetyl groups from the ε-amino groups of lysine residues on histone tails (e.g., H3K9, H3K14, H4K8). This deacetylation increases the positive charge of histones, strengthening their electrostatic interaction with negatively charged DNA and forming a condensed chromatin structure (heterochromatin) that blocks transcription. HDACis bind to the catalytic site of HDACs, preventing deacetylation and accumulating acetylated histones. This relaxed chromatin (euchromatin) allows transcription factors, such as p53 and E2F, to bind to promoter regions, activating the expression of tumor suppressor genes (e.g., p21 Bax) and genes involved in cell cycle arrest and apoptosis. In cancer cells, this reactivation reverses the oncogenic silencing of critical pathways, suppressing proliferation and inducing cell death.

2.2 Regulation of Non-Histone Substrates

Non-histone proteins constitute a large fraction of HDAC substrates, and their acetylation status controls protein function, localization, and stability. HDACis modulate key non-histone targets, including:
p53: A master tumor suppressor. Acetylation of p53 (at lysine residues 373 and 382) by HDAC inhibition enhances its stability and DNA-binding activity, promoting cell cycle arrest and apoptosis in cancer cells.
NF-κB: A transcription factor central to inflammation and immune responses. HDACs deacetylate the p65 subunit of NF-κB, enhancing its transcriptional activity. HDACis block this deacetylation, inhibiting NF-κB-mediated expression of pro-inflammatory cytokines (e.g., TNF-α, IL-6) and reducing tumor cell survival.
α-Tubulin: A component of the cytoskeleton. HDAC6 (a Class IIb HDAC) deacetylates α-tubulin, regulating microtubule dynamics. HDACis targeting HDAC6 increase α-tubulin acetylation, disrupting mitosis and inhibiting cancer cell migration and invasion.
These non-histone effects expand the therapeutic potential of HDACis beyond cancer, as seen in their ability to reduce inflammation in autoimmune diseases and protect neurons in neurodegenerative disorders.

3. Key Research Advances in HDAC Inhibitor Development

Recent research has advanced HDACi development in three major directions: optimizing efficacy in cancer therapy, exploring applications in non-oncological diseases, and improving selectivity to reduce side effects.

3.1 Cancer Therapy: From Monotherapy to Combination Strategies

While single-agent HDACis have shown efficacy in hematological malignancies (e.g., CTCL, PTCL), their performance in solid tumors has been limited due to tumor heterogeneity and drug resistance. To address this, researchers have focused on combination therapies that synergize with HDACis:
Immune Checkpoint Inhibitors: HDAC is modulate the tumor microenvironment by increasing the expression of tumor-associated antigens (TAAs) and MHC class I molecules, enhancing T-cell recognition of cancer cells. Preclinical studies have shown that combining vorinostat with anti-PD-1 antibodies (e.g., pembrolizumab) improves T-cell infiltration and tumor regression in melanoma and non-small cell lung cancer (NSCLC). A 2023 clinical trial (NCT03123096) reported that the combination of romidepsin and (e.g., nivolumab) achieved a 35% objective response rate in relapsed PTCL, significantly higher than romidepsin monotherapy (15%).
Targeted Therapies: HDACis synergize with inhibitors of oncogenic pathways, such as the PI3K/Akt/mTOR pathway. In breast cancer models, combining the Class I HDACi entinostat with the PI3K inhibitor (e.g., alpelisib) enhances apoptosis by blocking mTOR-mediated survival signals. Similarly, in glioblastoma, HDACis reverse the resistance to EGFR inhibitors by reactivating silenced tumor suppressor genes (e.g., PTEN).

3.2 Non-Oncological Applications: Neurodegeneration and Autoimmunity

HDACis have gained traction in non-cancer research, particularly in neurodegenerative diseases where epigenetic dysregulation contributes to pathogenesis:
3.2.1 Alzheimer’s Disease (AD): HDACis increase the acetylation of histones and tau protein (a key component of neurofibrillary tangles in AD). Preclinical studies with vorinostat and panobinostat have shown reduced tau hyperphosphorylation and improved cognitive function in AD mouse models. A 2022 study in Nature Communications reported that a Class IIa HDACi (HDAC4/5 inhibitor) enhances the clearance of amyloid-beta (Aβ) plaques by activating microglia, a critical step in reducing neuroinflammation in AD.
3.2.2 Autoimmune Diseases: HDACis suppress immune cell activation by inhibiting NF-κB and reducing cytokine production. In rheumatoid arthritis (RA), HDACis (e.g., givinostat) have been tested in phase II trials, showing reduced joint inflammation and improved disease activity scores by inhibiting the proliferation of synovial fibroblasts and the production of IL-6 and TNF-α.