UHRF1 coordinates peroxisome proliferator activated receptor gamma (PPARG) epigenetic silencing and mediates colorectal cancer progression

Sabatino, Lina; Fucci, Alessandra; Pancione, Massimo; Carafa, Vincenzo; Nebbioso, Angela; Pistore, Christian; Babbio, Federica; Votino, Carolina; Laudanna, Carmelo; Ceccarelli, Michele; Altucci, Lucia; Bonapace, Ian Marc; Colantuoni, Vittorio

doi:10.1038/onc.2012.3

Cited by 84 publications

(86 citation statements)

References 40 publications

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“…In addition, it stimulates E-cadherin gene transcription, further supporting the anti-metastatic activity of this compound [8]. These results are consistent with the data from literature disclosing for PPARc a protective role in in vitro and in vivo colorectal cancer (CRC) models [9][10][11][12][13]. In the gastrointestinal tract, in fact, PPARc impairs cellular proliferation, stimulates differentiation and induces apoptosis [14].…”

Section: Introductionsupporting

confidence: 85%

The antiproliferative and proapoptotic effects of cladosporols A and B are related to their different binding mode as PPARγ ligands

Zurlo

Ziccardi

Votino

et al. 2016

Biochemical Pharmacology

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a b s t r a c tCladosporols are secondary metabolites from Cladosporium tenuissimum characterized for their ability to control cell proliferation. We previously showed that cladosporol A inhibits proliferation of human colon cancer cells through a PPARc-mediated modulation of gene expression. In this work, we investigated cladosporol B, an oxidate form of cladosporol A, and demonstrate that it is more efficient in inhibiting HT-29 cell proliferation due to a robust G0/G1-phase arrest and p21 waf1/cip1 overexpression. Cladosporol B acts as a PPARc partial agonist with lower affinity and reduced transactivation potential in transient transfections as compared to the full agonists cladosporol A and rosiglitazone. Site-specific PPARc mutants and surface plasmon resonance (SPR) experiments confirm these conclusions. Cladosporol B in addition displays a sustained proapoptotic activity also validated by p21 waf1/cip1 expression analysis in the presence of the selective PPARc inhibitor GW9662. In the DMSO/H 2 O system, cladosporols A and B are unstable and convert to the ring-opened compounds 2A and 2B. Finally, docking experiments provide the structural basis for full and partial PPARc agonism of 2A and 2B, respectively. In summary, we report here, for the first time, the structural characteristics of the binding of cladosporols, two natural molecules, to PPARc. The binding of compound 2B is endowed with a lower transactivation potential, higher antiproliferative and proapoptotic activity than the two full agonists as compound 2A and rosiglitazone (RGZ).

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Section: Introductionsupporting

confidence: 85%

The antiproliferative and proapoptotic effects of cladosporols A and B are related to their different binding mode as PPARγ ligands

Zurlo

Ziccardi

Votino

et al. 2016

Biochemical Pharmacology

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show abstract

“…62 Similarly, alterations in the methylation of peroxisome proliferatoractivated receptor (PPARγ) due to UHRF1-mediated DNMT3b recruitment on its promoter region resulted in progression of colorectal cancer. 63 In bladder cancer cells, UHRF1 suppressed regulator of G-protein signaling 2 (RGS2) gene expression via promoter hypermethylation resulting in cellular proliferation. 64 Role of UHRF1 in carcinogenesis was also supported by the observation that its downregulation in MKN45 Catalyzes di-/tri-methylation of H3 at lysine 9 which represses the transcription of its target genes Kim et al 1 …”

Section: Uhrf1-mediated Silencing Of Tumor Suppressor Genesmentioning

confidence: 99%

UHRF1: The key regulator of epigenetics and molecular target for cancer therapeutics

Sidhu

Capalash

2017

Tumour Biol.

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UHRF1 is a master regulator of epigenome as it coordinates DNA methylation and histone modifications. Compelling evidence suggests a strong link between UHRF1 overexpression and tumorigenesis, substantiating its ability to act as a potential biomarker for cancer diagnosis and prognosis. UHRF1 also mediates repair of damaged DNA that makes cancer cells resistant toward cytocidal drugs. Hence, understanding the molecular mechanism of UHRF1 regulation would help in developing cancer therapeutics. Natural compounds have shown applicability to downregulate UHRF1 leading to growth arrest and apoptosis in cancer cells.

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“…Recently UHRF1 overexpression has been linked to tumor progression and poor prognosis in prostate cancer and colorectal cancer (37,38). UHRF1 function in heterochromatin formation and inheritance of genomic DNA methylation patterns has long been implicated as its major oncogenic role.…”

Section: Discussionmentioning

confidence: 99%

“…Recent studies demonstrated correlation of UHRF1 overexpression with tumor growth and aggressiveness and poor prognosis in prostate cancer and colorectal cancer (37,38). The oncogenic role of UHRF1 has long been implicated through epigenetic regulation, however recent indication of coexistence of UHRF1 in the same multi-protein complex with the TIP60 acetyltransferase (16,17) that modulates p53-dependent growth arrest and apoptosis leads to the attractive hypothesis that UHRF1 may be linked to the TIP60-p53 interplay and modulate the p53-dependent damage response pathway.…”

Section: Uhrf1 Interacts With Tip60 Both In Vitro and In Vivo-mentioning

confidence: 99%

Negative Regulation of the Acetyltransferase TIP60-p53 Interplay by UHRF1 (Ubiquitin-like with PHD and RING Finger Domains 1)

Dai

Shi

2013

Journal of Biological Chemistry

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Background:The TIP60 acetyltransferase mediates p53 acetylation at K120 and is required for p53-dependent growth arrest and apoptosis. Results: UHRF1 suppresses TIP60 interaction with p53 and TIP60-mediated p53 acetylation. UHRF1 depletion significantly enhances p53 and Tip60-dependent transactivation of growth arrest and apoptotic targets. Conclusion: UHRF1 negatively regulates p53 transactivity upstream of the TIP60-p53 interplay. Significance: Inhibition of the TIP60-p53 interplay contributes to the oncogenic functions of UHRF1.

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UHRF1 coordinates peroxisome proliferator activated receptor gamma (PPARG) epigenetic silencing and mediates colorectal cancer progression

Cited by 84 publications

References 40 publications

The antiproliferative and proapoptotic effects of cladosporols A and B are related to their different binding mode as PPARγ ligands

The antiproliferative and proapoptotic effects of cladosporols A and B are related to their different binding mode as PPARγ ligands

UHRF1: The key regulator of epigenetics and molecular target for cancer therapeutics

Negative Regulation of the Acetyltransferase TIP60-p53 Interplay by UHRF1 (Ubiquitin-like with PHD and RING Finger Domains 1)

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