HDAC and HDAC Inhibitor: From Cancer to Cardiovascular Diseases

Yoon, Somy; Eom, Gwang Hyeon

doi:10.4068/cmj.2016.52.1.1

Cited by 369 publications

(306 citation statements)

References 98 publications

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“…Both HAT and HDAC inhibitors are being tested for control of cancer cells in clinical trials, but they have also been shown to play a role in controlling cardiac hypertrophy in animal models. 26,27 The evidence that inhibiting both global activators and repressors has beneficial effects in cardiac stress strongly supports the hypothesis that control of transcription flexibility, and not the exact gene expression per se, may be an effective therapy to manage already progressing cardiac stress.…”

Section: Targeting Transcription In Left Ventricular Hypertrophymentioning

confidence: 74%

Timing and Targeting of Treatment in Left Ventricular Hypertrophy

Nam¹,

Reineke

2017

Methodist DeBakey Cardiovascular Journal

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Section: Targeting Transcription In Left Ventricular Hypertrophymentioning

confidence: 74%

Timing and Targeting of Treatment in Left Ventricular Hypertrophy

Nam¹,

Reineke

2017

Methodist DeBakey Cardiovascular Journal

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“…Preclinical atherosclerosis models have suggested that drugs modulating histone acetylation may be utilized to treat cardiovascular disease in the future 52. It is noteworthy that, to date, there are some debates on the effects of HDAC inhibitors in treating experimental atherosclerosis 50. Moreover, the side effects of HDAC inhibitor on the vascular system need to be systematically and closely monitored 50.…”

Section: Discussionmentioning

confidence: 99%

Suberanilohydroxamic Acid as a Pharmacological Kruppel‐Like Factor 2 Activator That Represses Vascular Inflammation and Atherosclerosis

Yang

Liu

et al. 2017

JAHA

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BackgroundKruppel‐like factor 2 (KLF2) is an important zinc‐finger transcription factor that maintains endothelial homeostasis by its anti‐inflammatory, ‐thrombotic, ‐oxidative, and ‐proliferative effects in endothelial cells. In light of the potent vasoprotective effects of KLF2, modulating KLF2 expression or function could give rise to new therapeutic strategies to treat cardiovascular diseases.Methods and ResultsHigh‐throughput drug screening based on KLF2 promoter luciferase reporter assay was performed to screen KLF2 activators. Real‐time PCR and western blot were used to detect gene and protein expression. Identified KLF2 activator was orally administered to ApoE−/− mice to evaluate anti‐atherosclerotic efficacy. By screening 2400 compounds in the Spectrum library, we identified suberanilohydroxamic (SAHA) acid, also known as vorinostat as a pharmacological KLF2 activator through myocyte enhancer factor 2. We found that SAHA exhibited anti‐inflammatory effects and attenuated monocyte adhesion to endothelial cells inflamed with tumor necrosis factor alpha. We further showed that the inhibitory effect of SAHA on endothelial inflammation and ensuing monocyte adhesion was KLF2 dependent using KLF2‐deficient mouse lung endothelial cells or KLF2 small interfering RNA– depleted human endothelial cells. Importantly, we observed that oral administration of SAHA reduced diet‐induced atherosclerotic lesion development in ApoE−/− mice without significant effect on serum lipid levels.ConclusionsThese results demonstrate that SAHA has KLF2‐dependent anti‐inflammatory effects in endothelial cells and provide the proof of concept that KLF2 activation could be a promising therapeutic strategy for treating atherosclerosis.

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“…HDAC inhibitors are becoming a well-known class of drugs for cancer treatment, in particular after the FDA approval of Vorinostat and Romidepsin for the treatment of hematologic cancers (2). At least 12 different HDACis are currently in use for clinical trials, and more are being sought to augment chemotherapy (4, 5, 7), immunotherapy/ cancer vaccines (14) and overcome multi-drug resistance which are common to diverse cytostatic or receptor-mediated drugs (3,8,9,(36)(37)(38) HDAC inhibitors were first isolated from microorganisms, and continue to be developed from microbial metabolites (39,40).…”

Section: Discussionmentioning

confidence: 99%

“…Elevated expression of HDACs are evident in advanced malignancy, where inhibitors (HDACis) antagonize tumor growth (2,3) antagonize tumor growth (2,3), augment chemotherapy (4-7), reverse chemoresistance (3,8,9), attenuate metastasis, halt epithelial-mesenchymal transition (10)(11)(12) and block tumor immune evasion (13,14). With the overwhelming surge of HDACis being sought worldwide for nearly every type of cancer (e.g.…”

mentioning

confidence: 99%