3‐Deazaneplanocin A and Neplanocin A Analogues and Their Effects on Apoptotic Cell Death

Tam, Eric; Nguyen, Tuan Minh; Lim, Cheryl Zi Hui; Lee, Puay Leng; Li, Zhimei; Jiang, Xia; Santhanakrishnan, Sridhar; Tan, Tiong Wei; Goh, Yi Ling; Wong, Siew Yee; Yang, Haiyan; Ong, Esther; Hill, Jeffrey; Yu, Qiang; Chai, Christina L. L.

doi:10.1002/cmdc.201402315

Cited by 26 publications

(18 citation statements)

References 37 publications

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“…DZNep is a purine nucleoside analog (PNA), which is in a family of compounds, many of which are being used clinically and have been proven to be effective in the treatment of hematological malignancies and autoimmune disorders 33 . In a blinded fashion, we began by determining the ability of several chemically-related PNAs (designated compounds 1–9; Figure S1) to inhibit HSC expression of transcripts for the profibrogenic genes collagen 1A1, αSMA, and TIMP-1.…”

Section: Resultsmentioning

confidence: 99%

A Proof-of-Concept for Epigenetic Therapy of Tissue Fibrosis: Inhibition of Liver Fibrosis Progression by 3-Deazaneplanocin A

et al. 2017

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The progression of fibrosis in chronic liver disease is dependent upon hepatic stellate cells (HSCs) transdifferentiating to a myofibroblast-like phenotype. This pivotal process is controlled by enzymes that regulate histone methylation and chromatin structure, which may be targets for developing anti-fibrotics. There is limited pre-clinical experimental support for the potential to therapeutically manipulate epigenetic regulators in fibrosis. In order to learn if epigenetic treatment can halt the progression of pre-established liver fibrosis, we treated mice with the histone methyltransferase inhibitor 3-deazaneplanocin A (DZNep) in a naked form or by selectively targeting HSC-derived myofibroblasts via an antibody-liposome-DZNep targeting vehicle. We discovered that DZNep treatment inhibited multiple histone methylation modifications, indicative of a broader specificity than previously reported. This broad epigenetic repression was associated with the suppression of fibrosis progression as assessed both histologically and biochemically. The anti-fibrotic effect of DZNep was reproduced when the drug was selectively targeted to HSC-derived myofibroblasts. Therefore, the in vivo modulation of HSC histone methylation is sufficient to halt progression of fibrosis in the context of continuous liver damage. This discovery and our novel HSC-targeting vehicle, which avoids the unwanted effects of epigenetic drugs on parenchymal liver cells, represents an important proof-of-concept for epigenetic treatment of liver fibrosis.

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Section: Resultsmentioning

confidence: 99%

A Proof-of-Concept for Epigenetic Therapy of Tissue Fibrosis: Inhibition of Liver Fibrosis Progression by 3-Deazaneplanocin A

et al. 2017

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“…Not surprisingly, the inhibition of DNA methyltransferase activity by DZNep has been shown to have pleiotropic effects on anti-tumor responses as reported by several independent studies. 46,47,58,59 5-aza-2-deoxycytidine (5-AZA-dC) and DZNep have been shown to improve anti-tumor response by increasing CXCL9 and CXCL10 expression in cancer cells and tumor infiltration by T cells 60 or by inducing type I or III interferon responses through reactivation of endogenous retrovirus transcription. 61,62 On the other hand, EZH2 deletion or inhibition has been reported to negatively impact cytokine production and T cell survival.…”

Section: Discussionmentioning

confidence: 99%

“…45 It induces accumulation of S-adenosyl-L-homocysteine, a by-product of S-adenosyl methionine (SAM)-dependent methylation, thereby, inhibiting methyltransferases. 45,46 It has also been shown to deplete EZH2 levels, thereby, inhibiting trimethylation of lysine 27 on histone H3 by blocking the polycomb-repressive-complex 2 in primary AML cells in a dose-dependent manner (0.2-1 mM). 47,48 Although both RA and DZNep inhibit MDSC suppressive functions, they did so in a qualitative and quantitative different manner ( Fig.…”

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confidence: 99%

Identification of inhibitors of myeloid-derived suppressor cells activity through phenotypic chemical screening

et al. 2016

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Tumors are infiltrated by cells of the immune system that interact through complex regulatory networks. Although tumor-specific CD8 C T cells can be found in peripheral blood and tumor samples from cancer patients, their function is inhibited by immunosuppressive cells such as regulatory T cells, tumorassociated macrophages, and myeloid-derived suppressor cells (MDSC). Recent clinical successes have demonstrated that alleviating immunosuppression and T cell exhaustion translates into long-term clinical benefits. Although tremendous progress has been achieved, tools that afford unbiased approaches and screenings to uncover new potential inhibitors or gene targets are lacking. In this study, we describe a system based on immortalized progenitors that allows straightforward investigation of myeloid cells. We show that bone marrow progenitors immortalized through the transduction of NUP98-HOXB4 transgene can be differentiated into CD11b C Gr-1 C MDSC that express Arginase-1 and PD-L1, produce reactive oxygen and nitrogen species, and suppress T cell function in vitro. To uncover chemical probes that interfere with MDSC biology, we performed a chemical phenotypic screening and identified 3-deazaneplanocin A as a novel modulator of MDSC functions. We characterized and compared the effect of 3-deazaneplanocin-A and all-trans retinoic acid, a well-known modulator of MDSC activity, on the expression of effector molecules and immunosuppressive functions of MDSC. Altogether, this proof-ofprinciple opens new possibilities for the identification of drugs targeting myeloid cells with immunosuppressive activities.

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“…However, due to the unfavorable plasma pharmacokinetic (PK) properties of DZNep (half-life of 1.1 h in rats and 0.9 h in mice) (Peer et al, 2013;Sun et al, 2012), the antitumor studies on DZNep have been stuck in the preclinical phase. In order to ameliorate its plasma PK properties, recent efforts have led to the advent of novel nanoparticle carriers or analogous (Hung et al, 2013;Sun et al, 2012;Tam et al, 2015). Unfortunately, the pharmacological effects of the new formulations or analogues on cancer cell death or EZH2 modulation were not comparable to DZNep.…”

Section: -Deazaneplanocin a (Dznep)mentioning

confidence: 98%

Preclinical pharmacokinetic studies of 3-deazaneplanocin A, a potent epigenetic anticancer agent, and its human pharmacokinetic prediction using GastroPlus™

Sun

Lee

Zhang

et al. 2015

European Journal of Pharmaceutical Sciences

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3‐Deazaneplanocin A and Neplanocin A Analogues and Their Effects on Apoptotic Cell Death

Cited by 26 publications

References 37 publications

A Proof-of-Concept for Epigenetic Therapy of Tissue Fibrosis: Inhibition of Liver Fibrosis Progression by 3-Deazaneplanocin A

A Proof-of-Concept for Epigenetic Therapy of Tissue Fibrosis: Inhibition of Liver Fibrosis Progression by 3-Deazaneplanocin A

Identification of inhibitors of myeloid-derived suppressor cells activity through phenotypic chemical screening

Preclinical pharmacokinetic studies of 3-deazaneplanocin A, a potent epigenetic anticancer agent, and its human pharmacokinetic prediction using GastroPlus™

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