Novel Oligoamine Analogues Inhibit Lysine-Specific Demethylase 1 and Induce Reexpression of Epigenetically Silenced Genes

Huang, Yi; Murray-Stewart, Tracy; Wu, Yu; Baylin, Stephen B.; Marton, Laurence J.; Perkins, Brandy; Jones, Richard J.; Woster, Patrick M.; Casero, Robert A.

doi:10.1158/1078-0432.ccr-09-1293

Cited by 188 publications

(197 citation statements)

References 41 publications

Supporting

Mentioning

191

Contrasting

Unclassified

Order By: Relevance

“…LSD1 inhibited the proliferation of pluripotent cancer cells, including teratocarcinoma, embryonic carcinoma, seminoma or embryonic stem cells that express the stem cell markers Oct4 and Sox2, and colon cancer cells (Wang et al 2011). Treatment of the colon cancer cells with LSD1 inhibitors (such as SL11144) increases methylation at H3K4, decreases H3K9 methylation, and restores the expression of SFRP2, indicating the specificity of LSD1 and its inhibitors (Huang et al 2009). Its inhibition in neuroblastoma results in decreased proliferation in vitro and reduced xenograft growth (Schulte et al 2009).…”

Section: Polyphenolmentioning

confidence: 99%

Epigenetic Modifications: Therapeutic Potential in Cancer

Sachan

Kaur

2015

Braz. arch. biol. technol.

View full text Add to dashboard Cite

Epigenetic modifications and alterations in chromatin structure and function contribute to the cumulative changes observed as normal cells undergo malignant transformation. These modifications and enzymes (DNA methyltransferases, histone deacetylases, histone methyltransferases, and demethylases) related to them have been deeply studied to develop new drugs, epigenome-targeted therapies and new diagnostic tools. Epigenetic modifiers aim to restore normal epigenetic modification patterns through the inhibition of epigenetic modifier enzymes. Four of them (azacitidine, decitabine, vorinostat and romidepsin)

show abstract

Section: Polyphenolmentioning

confidence: 99%

Epigenetic Modifications: Therapeutic Potential in Cancer

Sachan

Kaur

2015

Braz. arch. biol. technol.

View full text Add to dashboard Cite

show abstract

“…17 One milligram peptide of histone H3 (residues [1][2][3][4][5][6][7][8][9][10][11][12][13][14][15][16][17][18][19][20] carrying one or two methyl groups at lysine 4 were incubated with 2 lg of GST-LSD1 in the absence or presence of Namoline. The reaction mixture was incubated in demethylation buffer for 4 hr at 37 C and analyzed by mass spectroscopy.…”

Section: Demethylase Assaymentioning

confidence: 99%

“…[7][8][9][10][11][12][13] However, these amine oxidase inhibitors including clorgyline, pargyline, tranylcypromine, polyamines and derivatives thereof, many of them do not selectively target LSD1 and therefore, limits their use as therapeutics owing to potential side effects. In this study, we found a novel and selective LSD1 inhibitor called Namoline by combining protein structure similarity clustering and in vitro screening.…”

mentioning

confidence: 99%

Impairment of prostate cancer cell growth by a selective and reversible lysine‐specific demethylase 1 inhibitor

Willmann

Lim

Wetzel

et al. 2012

Intl Journal of Cancer

129

108

View full text Add to dashboard Cite

Post-translational modifications of histones by chromatin modifying enzymes regulate chromatin structure and gene expression. As deregulation of histone modifications contributes to cancer progression, inhibition of chromatin modifying enzymes such as histone demethylases is an attractive therapeutic strategy to impair cancer growth. Lysine-specific demethylase 1 (LSD1) removes mono-and dimethyl marks from lysine 4 or 9 of histone H3. LSD1 in association with the androgen receptor (AR) controls androgen-dependent gene expression and prostate tumor cell proliferation, thus highlighting LSD1 as a drug target. By combining protein structure similarity clustering and in vitro screening, we identified Namoline, a cpyrone, as a novel, selective and reversible LSD1 inhibitor. Namoline blocks LSD1 demethylase activity in vitro and in vivo. Inhibition of LSD1 by Namoline leads to silencing of AR-regulated gene expression and severely impairs androgen-dependent proliferation in vitro and in vivo. Thus, Namoline is a novel promising starting compound for the development of therapeutics to treat androgen-dependent prostate cancer.Prostate cancer is the second leading cause of cancer deaths in Western countries. As long as tumors are prostate confined, they can be efficiently treated by surgery and/or radiation therapy in a curative intent. In cases, however, where the tumor has already disseminated an androgen ablation therapy has to be applied. 1 Patients initially respond to androgen ablation, but tumors become androgen resistant within a period of 12-18 months, 2 after which no curative treatment exists. Thus, the urgent need to identify novel therapeutic targets for the treatment of androgen-resistant prostate cancer is evident.We recently identified lysine-specific demethylase 1 (LSD1), an amine oxidase, as a novel target for prostate cancer therapy. 3 Expression of LSD1 positively correlates with the malignancy of prostate tumors. 3,4 LSD1 functions as a histone demethylase that removes mono-and dimethyl, but not trimethyl marks from either lysine 4 or lysine 9 of histone H3 (H3K4 and H3K9, respectively). 3,5 As a component of corepressor complexes, LSD1 demethylates active methyl marks at H3K4. 5,6 In comparison, when associated with the androgen receptor (AR), the enzyme removes repressive methyl marks from H3K9, thereby enhancing AR-dependent gene expression and prostate tumor cell proliferation. 3 Thus, we hypothesized that selective LSD1 inhibitors are useful precursors for the development of novel drugs for prostate cancer therapy.Previous studies showed that inhibitors of other members of the amine oxidase family also impair the activity of LSD1. 7-13 However, these amine oxidase inhibitors including clorgyline, pargyline, tranylcypromine, polyamines and derivatives thereof, many of them do not selectively target LSD1 and therefore, limits their use as therapeutics owing to potential side effects. In this study, we found a novel and selective LSD1 inhibitor called Namoline by combining protein structure similar...

show abstract

“…Further evidences on collaborative actions of LSD1 and DNMTs in epigenetic silencing of tumor suppressor genes were provided by Huang et al They showed that a combination of LSD1 inhibitors and a DNMT inhibitor has proven to be highly efficient in reactivating aberrantly silenced genes in cancer and led to profound inhibition of the growth of human colon cancer xenografts in nude mice. 21 The oncogenic potential of LSD1 could also be the result of the p53 antagonizing action of LSD1. LSD1 can control the tumor suppressor activity of p53 by directly demethylating a specific p53 lysine (Lys370me2/1), which is required for efficient binding to the transcriptional coactivator p53-binding protein-1.…”

Section: Lsd1/kdm1amentioning

confidence: 99%

Epigenetic regulation of cancer growth by histone demethylases

Lim

Metzger

Schüle

et al. 2010

Intl Journal of Cancer

View full text Add to dashboard Cite

Cancer is traditionally viewed as a primarily genetic disorder. However, it is now increasingly apparent that epigenetic abnormalities play a fundamental role in cancer development. Aberrant expression of histone-modifying enzymes has been implicated in the course of tumor initiation and progression. The discovery of a large number of histone demethylases suggests an important role for dynamic regulation of histone methylation in biological processes. The observation that overexpression, amplification or mutations of several histone demethylases have been found in many types of tumors, raise the possibility of using these enzymes as diagnostic tools as well as pave a way for the discovery of novel therapeutic targets and treatment modalities. Here, we review the current knowledge of the potential role of H3K4, H3K9 and H3K27 histone demethylases in tumorigenesis.Recently, it has become apparent that not only genetic mutations but also epigenetic alterations lead to the activation of oncogenes and the loss of function of tumor-suppressor genes. Since epigenetic abnormalities in DNA methylation patterns as well as histone modifications are potentially reversible in contrast to gene mutations, much effort has been directed toward understanding the mechanism of epigenetic aberration to develop epigenetic therapies. Indeed, inhibitors of histone deacetylases (HDACs) and DNA methyltransferases (DNMTs) have been approved for treatment of certain types of cancers. Recently, overexpression, amplification or mutations of several histone demethylases have been linked to many types of tumor, raising the possibility of using these enzymes as diagnostic tools and therapeutic targets. Here, we focus mainly on the potential role of some selected histone lysine demethylases in tumorigenesis.The N-terminal tails of histones are subjected to several types of post-translational modifications, including acetylation, methylation, phosphorylation and ubiquitination. The combination of these modifications determines chromatin structure and transcriptional activation or repression of genes. In contrast to other histone modifications, the importance of histone methylations is highlighted because of their enormously specific dynamics with respect to gene regulation. Histone lysine residues on histone H3 and H4 (H3K4, H3K9, H3K27, H3K36, H3K79 and H4K20) can become mono-, dior trimethylated. These modifications are regulated by two classes of enzymes with opposing activities: histone methyltransferases and histone lysine demethylases. LSD1, also known as AOF2 and KDM1, is the first discovered histone lysine demethylase that belongs to the flavin adenine dinucleotide-dependent enzyme family. 1 Subsequently, another family of histone lysine demethylases structurally different from LSD1 was described, all of which sharing the conserved jumonji C (JmjC) domain (Table 1). H3K4 Demethylases in Cancer LSD1/KDM1ATri-and dimethylated H3K4 (H3K4me3/2) are often found at actively transcribed genes. Although H3K4me3 is highly enriched around transcrip...

show abstract

Novel Oligoamine Analogues Inhibit Lysine-Specific Demethylase 1 and Induce Reexpression of Epigenetically Silenced Genes

Cited by 188 publications

References 41 publications

Epigenetic Modifications: Therapeutic Potential in Cancer

Epigenetic Modifications: Therapeutic Potential in Cancer

Impairment of prostate cancer cell growth by a selective and reversible lysine‐specific demethylase 1 inhibitor

Epigenetic regulation of cancer growth by histone demethylases

Contact Info

Product

Resources

About