LSD1 mediates MYCN control of epithelial-mesenchymal transition through silencing of metastatic suppressor NDRG1 gene

Ambrosio, Susanna; Amente, Stefano; Saccà, Carmen D.; Capasso, Mario; Calogero, Raffaele; Lania, Luigi; Majello, Barbara

doi:10.18632/oncotarget.12924

Cited by 40 publications

(43 citation statements)

References 45 publications

(61 reference statements)

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“…Again, we used bioinformatics tools to explore such putative links and performed a meta-analysis of the protein interactants potentially linking the identified candidate cytokines with N-Myc. Indeed, a well identified mechanism of NDRG1 repression relies on the binding of N-Myc to the promoter region of NDRG1 and the subsequent recruitment of histone deacetylases leading to promoter hypermethylation and an epigenetic silencing of NDRG1 [47][48][49][50][51][52]. Our meta-analysis showed that only TGFBR1 (an oligodendrocyte-expressed receptor to TGFB1) and PDGRA (an oligodendrocyte-expressed receptor to PDGFC) formed a close (second shell) protein network with N-MyC.…”

Section: Discussionmentioning

confidence: 98%

“…Since then, in multiple cell types, MYCN was shown to silence NDRG1 gene expression via a process involving a hypermethylation of the NDRG1 promoter [47][48][49][50][51][52] . On this basis, we performed a meta-analysis of the human interactome to determine whether signaling pathways could link MYCN to the identified candidate molecules (i.e IL17D, IL33, IL12A, PDGF-C and TGFB1).…”

Section: Identification Of a Molecular Pathway Linking Mycn To Pdgfc mentioning

confidence: 99%

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A Unique TGFB1-Driven Genomic Program Links Astrocytosis, Low-Grade Inflammation and Partial Demyelination in Periplaques of Spinal Cords from Progressive Multiple Sclerosis Patients

Nataf¹,

Barritault²,

Pays³

2017

Preprint

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Abstract:We previously reported that in multiple sclerosis (MS) patients with a progressive form of the disease, spinal cord periplaques extend distance away from plaque borders and are characterized by the co-occurrence of partial demyelination, astrocytosis and low-grade inflammation. However, transcriptomic analyses comparing periplaques to adjacent normal-appearing white matter (NAWM) areas did not allow providing a comprehensive view of molecular events in astrocytes vs oligodendrocytes. Here, we re-assessed our transcriptomic data with the aim of identifying functionally-relevant co-expression networks that would reflect astrocyte vs oligodendrocyte molecular signatures in periplaques. We identified an astrocytosis-related gene module comprising GFAP, the hub gene CX43/GJA1 and a set of transcripts forming a TGFB/SMAD1/SMAD2 genomic signature. Partial demyelination was characterized by a co-expression network which, besides myelin genes, comprised a highly significant number of translation/elongation-related genes. Interestingly, the main oligodendrocyte-related hub we identified was NDRG1, a gene previously shown to be specifically silenced in the NAWM of MS patients. This result indicated that NDRG1 down-regulation could be an important event in the process of periplaque partial demyelination. To establish a putative link between NDRG1 down-regulation and a cytokine/chemokine signature, we then sought to identify cytokine/chemokine genes whose mRNA levels inversely correlated with those of NDRG1. Following this approach we found 5 candidate immune-related genes whose up-regulation associated with NDRG1 down-regulation: TGFB1, PDGFC, . From these results we propose that in the spinal cord of MS patients with progressive forms of the disease, TGFB1 may Preprints (www.preprints.org) | NOT PEER-REVIEWED | Posted:

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Section: Discussionmentioning

confidence: 98%

Section: Identification Of a Molecular Pathway Linking Mycn To Pdgfc mentioning

confidence: 99%

A Unique TGFB1-Driven Genomic Program Links Astrocytosis, Low-Grade Inflammation and Partial Demyelination in Periplaques of Spinal Cords from Progressive Multiple Sclerosis Patients

Nataf¹,

Barritault²,

Pays³

2017

Preprint

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“…Additionally, we observed that the half‐life of LSD1 is decreased from an initial 30 h to 21 h after HCI‐2509 treatment. This is in agreement with previous studies with respect to neuroblastoma and prostate cancer (Ambrosio et al ., ; Sehrawat et al ., ).…”

Section: Discussionmentioning

confidence: 99%

Preclinical studies reveal that LSD1 inhibition results in tumor growth arrest in lung adenocarcinoma independently of driver mutations

et al. 2018

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Lung adenocarcinoma (LUAD) is the most prevalent subtype of non‐small cell lung cancer. Despite the development of novel targeted and immune therapies, the 5‐year survival rate is still only 21%, indicating the need for more efficient treatment regimens. Lysine‐specific demethylase 1 (LSD1) is an epigenetic eraser that modifies histone 3 methylation status, and is highly overexpressed in LUAD. Using representative human cell culture systems and two autochthonous transgenic mouse models, we investigated inhibition of LSD1 as a novel therapeutic option for treating LUAD. The reversible LSD1 inhibitor HCI‐2509 significantly reduced cell growth with an IC 50 of 0.3–5 μm in vitro, which was linked to an enhancement of histone 3 lysine methylation. Most importantly, growth arrest, as well as inhibition of the invasion capacities, was independent of the underlying driver mutations. Subsequent expression profiling revealed that the cell cycle and replication machinery were prominently affected after LSD1 inhibition. In addition, our data provide evidence that LSD1 blockade significantly interferes with EGFR downstream signaling. Finally, our in vitro results were confirmed by preclinical therapeutic approaches, including the use of two autochthonous transgenic LUAD mouse models driven by either EGFR or KRAS mutations. Importantly, LSD1 inhibition resulted in significantly lower tumor formation and a strong reduction in tumor progression, which were independent of the underlying mutational background of the mouse models. Hence, our findings provide substantial evidence indicating that tumor growth of LUAD can be markedly decreased by HCI‐2509 treatment, suggesting its use as a single agent maintenance therapy or combined therapeutical application in novel concerted drug approaches.

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“…There is evidence that demonstrates that 8-oxoGua generation may regulate transcriptional activation, derived from experiments involving estrogen-responsive genes, Myc targeted genes and hypoxia-inducible genes [48][49][50][51]. It was demonstrated that exposure of cells to estrogen substantially increases 8-oxoGua in the promoter region of estrogen-responsive genes, which in turn recruits OGG1 and topoisomerase IIβ.…”

Section: Potential Regulatory Role Of 8-oxoguamentioning

confidence: 99%

“…OGG1 generates transient nicks, which allows entry of the topoisomerase, the activity of which relaxes the DNA strand, triggering chromatin conformational changes essential for estrogen-induced transcription [48]. It has been shown that a similar mechanism is responsible for Myc-induced transcription activation [50]. It is proposed that upon binding of above mentioned transcription factors to the specific sequences, demethylating enzyme lysine-specific demethylase 1 (LSD1) is recruiting.…”

Section: Potential Regulatory Role Of 8-oxoguamentioning

confidence: 99%

Endogenously generated DNA nucleobase modifications source, and significance as possible biomarkers of malignant transformation risk, and role in anticancer therapy

Oliński

Gackowski

Cooke

2018

Biochimica et Biophysica Acta (BBA) - Reviews on Cancer

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The DNA of all living cells undergoes continuous structural and chemical alteration, which may be derived from exogenous sources, or endogenous, metabolic pathways, such as cellular respiration, replication and DNA demethylation. It has been estimated that approximately 70,000 DNA lesions may be generated per day in a single cell, and this has been linked to a wide variety of diseases, including cancer. However, it is puzzling why potentially mutagenic DNA modifications, occurring at a similar level in different organs/tissue, may lead to organ/tissue specific cancers, or indeed non-malignant disease - what is the basis for this differential response? We suggest that it is perhaps the precise location of damage, within the genome, that is a key factor. Finally, we draw attention to the requirement for reliable methods for identification and quantification of DNA adducts/modifications, and stress the need for these assays to be fully validated. Once these prerequisites are satisfied, measurement of DNA modifications may be helpful as a clinical parameter for treatment monitoring, risk group identification and development of prevention strategies.

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LSD1 mediates MYCN control of epithelial-mesenchymal transition through silencing of metastatic suppressor NDRG1 gene

Cited by 40 publications

References 45 publications

A Unique TGFB1-Driven Genomic Program Links Astrocytosis, Low-Grade Inflammation and Partial Demyelination in Periplaques of Spinal Cords from Progressive Multiple Sclerosis Patients

A Unique TGFB1-Driven Genomic Program Links Astrocytosis, Low-Grade Inflammation and Partial Demyelination in Periplaques of Spinal Cords from Progressive Multiple Sclerosis Patients

Preclinical studies reveal that LSD1 inhibition results in tumor growth arrest in lung adenocarcinoma independently of driver mutations

Endogenously generated DNA nucleobase modifications source, and significance as possible biomarkers of malignant transformation risk, and role in anticancer therapy

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