Your search keyword '"Vincenzo, Carafa"' showing total 90 results

1. Data from c-Myc Modulation and Acetylation Is a Key HDAC Inhibitor Target in Cancer

Author

Lucia Altucci, Hendrik G. Stunnenberg, Valeria Belsito Petrizzi, Concetta Ingenito, Gabriella Lania, Francesco Iovino, Guillermo Garcia-Manero, Saverio Minucci, Isabella Pallavicini, Rosaria Benedetti, Matthias Nees, Joost Martens, Ciro Abbondanza, Francesco Paolo Tambaro, Mariarosaria Conte, Vincenzo Carafa, and Angela Nebbioso

Abstract

Purpose: Histone deacetylase inhibitors (HDACi) are promising anticancer drugs. Although some HDACi have entered the clinic, the mechanism(s) underlying their tumor selectivity are poorly understood.Experimental Design and Results: Using gene expression analysis, we define a core set of six genes commonly regulated in acute myeloid leukemia (AML) blasts and cell lines. MYC, the most prominently modulated, is preferentially altered in leukemia. Upon HDACi treatment, c-Myc is acetylated at lysine 323 and its expression decreases, leading to TRAIL activation and apoptosis. c-Myc binds to the TRAIL promoter on the proximal GC box through SP1 or MIZ1, impairing TRAIL activation. HDACi exposure triggers TRAIL expression, altering c-Myc-TRAIL binding. These events do not occur in normal cells. Excitingly, this inverse correlation between TRAIL and c-Myc is supported by HDACi treatment ex vivo of AML blasts and primary human breast cancer cells. The predictive value of c-Myc to HDACi responsiveness is confirmed in vivo in AML patients undergoing HDACi-based clinical trials.Conclusions: Collectively, our findings identify a key role for c-Myc in TRAIL deregulation and as a biomarker of the anticancer action of HDACi in AML. The potential improved patient stratification could pave the way toward personalized therapies. Clin Cancer Res; 23(10); 2542–55. ©2016 AACR.

Published

2023

2. Supplementary note from RIP1–HAT1–SIRT Complex Identification and Targeting in Treatment and Prevention of Cancer

Author

Lucia Altucci, Antonello Mai, Hendrik G. Stunnenberg, Massimo Zollo, Rino Ragno, Adele Pirolli, Domenico Tarantino, Pasquale De Antonellis, Enrico Radaelli, Jani Shaik, Luca Maravigna, Paolo Ciana, Menotti Ruvo, Rosita Russo, Angela Chambery, Gennaro Citro, Enrico P. Spugnini, Alfonso Baldi, Paola Bontempo, Gilda Cobellis, Dante Rotili, Francesca Cuomo, Angela Nebbioso, and Vincenzo Carafa

Abstract

supplementary chemistry

Published

2023

3. Supplementary Figure 7 from c-Myc Modulation and Acetylation Is a Key HDAC Inhibitor Target in Cancer

Author

Lucia Altucci, Hendrik G. Stunnenberg, Valeria Belsito Petrizzi, Concetta Ingenito, Gabriella Lania, Francesco Iovino, Guillermo Garcia-Manero, Saverio Minucci, Isabella Pallavicini, Rosaria Benedetti, Matthias Nees, Joost Martens, Ciro Abbondanza, Francesco Paolo Tambaro, Mariarosaria Conte, Vincenzo Carafa, and Angela Nebbioso

Abstract

SAHA effects in different cell lines.

Published

2023

4. Supplementary Tables from RIP1–HAT1–SIRT Complex Identification and Targeting in Treatment and Prevention of Cancer

Author

Lucia Altucci, Antonello Mai, Hendrik G. Stunnenberg, Massimo Zollo, Rino Ragno, Adele Pirolli, Domenico Tarantino, Pasquale De Antonellis, Enrico Radaelli, Jani Shaik, Luca Maravigna, Paolo Ciana, Menotti Ruvo, Rosita Russo, Angela Chambery, Gennaro Citro, Enrico P. Spugnini, Alfonso Baldi, Paola Bontempo, Gilda Cobellis, Dante Rotili, Francesca Cuomo, Angela Nebbioso, and Vincenzo Carafa

Abstract

Supplementary Tables

Published

2023

5. Supplementary Table 1 from c-Myc Modulation and Acetylation Is a Key HDAC Inhibitor Target in Cancer

Author

Lucia Altucci, Hendrik G. Stunnenberg, Valeria Belsito Petrizzi, Concetta Ingenito, Gabriella Lania, Francesco Iovino, Guillermo Garcia-Manero, Saverio Minucci, Isabella Pallavicini, Rosaria Benedetti, Matthias Nees, Joost Martens, Ciro Abbondanza, Francesco Paolo Tambaro, Mariarosaria Conte, Vincenzo Carafa, and Angela Nebbioso

Abstract

Schematic representation of the TRAIL promoter, its analyzed regions and the occupancy of epi-marks analyzed under indicated conditions.

Published

2023

6. Supplementary Figure 4 from c-Myc Modulation and Acetylation Is a Key HDAC Inhibitor Target in Cancer

Author

Lucia Altucci, Hendrik G. Stunnenberg, Valeria Belsito Petrizzi, Concetta Ingenito, Gabriella Lania, Francesco Iovino, Guillermo Garcia-Manero, Saverio Minucci, Isabella Pallavicini, Rosaria Benedetti, Matthias Nees, Joost Martens, Ciro Abbondanza, Francesco Paolo Tambaro, Mariarosaria Conte, Vincenzo Carafa, and Angela Nebbioso

Abstract

Epigenetic status of the TRAIL promoter region after HDACi exposure.

Published

2023

7. On line Materials and Methods from RIP1–HAT1–SIRT Complex Identification and Targeting in Treatment and Prevention of Cancer

Author

Lucia Altucci, Antonello Mai, Hendrik G. Stunnenberg, Massimo Zollo, Rino Ragno, Adele Pirolli, Domenico Tarantino, Pasquale De Antonellis, Enrico Radaelli, Jani Shaik, Luca Maravigna, Paolo Ciana, Menotti Ruvo, Rosita Russo, Angela Chambery, Gennaro Citro, Enrico P. Spugnini, Alfonso Baldi, Paola Bontempo, Gilda Cobellis, Dante Rotili, Francesca Cuomo, Angela Nebbioso, and Vincenzo Carafa

Abstract

On line Materials and Methods

Published

2023

8. Supplementary Figure 3 from c-Myc Modulation and Acetylation Is a Key HDAC Inhibitor Target in Cancer

Author

Lucia Altucci, Hendrik G. Stunnenberg, Valeria Belsito Petrizzi, Concetta Ingenito, Gabriella Lania, Francesco Iovino, Guillermo Garcia-Manero, Saverio Minucci, Isabella Pallavicini, Rosaria Benedetti, Matthias Nees, Joost Martens, Ciro Abbondanza, Francesco Paolo Tambaro, Mariarosaria Conte, Vincenzo Carafa, and Angela Nebbioso

Abstract

c-Myc down-regulation modulates DR5 and p21 genes.

Published

2023

9. Supplementary Figure 8 from c-Myc Modulation and Acetylation Is a Key HDAC Inhibitor Target in Cancer

Author

Lucia Altucci, Hendrik G. Stunnenberg, Valeria Belsito Petrizzi, Concetta Ingenito, Gabriella Lania, Francesco Iovino, Guillermo Garcia-Manero, Saverio Minucci, Isabella Pallavicini, Rosaria Benedetti, Matthias Nees, Joost Martens, Ciro Abbondanza, Francesco Paolo Tambaro, Mariarosaria Conte, Vincenzo Carafa, and Angela Nebbioso

Abstract

SAHA effects in normal cells.

Published

2023

10. Suppl. Methods from c-Myc Modulation and Acetylation Is a Key HDAC Inhibitor Target in Cancer

Author

Lucia Altucci, Hendrik G. Stunnenberg, Valeria Belsito Petrizzi, Concetta Ingenito, Gabriella Lania, Francesco Iovino, Guillermo Garcia-Manero, Saverio Minucci, Isabella Pallavicini, Rosaria Benedetti, Matthias Nees, Joost Martens, Ciro Abbondanza, Francesco Paolo Tambaro, Mariarosaria Conte, Vincenzo Carafa, and Angela Nebbioso

Abstract

Suppl. Methods

Published

2023

11. Data from RIP1–HAT1–SIRT Complex Identification and Targeting in Treatment and Prevention of Cancer

Author

Lucia Altucci, Antonello Mai, Hendrik G. Stunnenberg, Massimo Zollo, Rino Ragno, Adele Pirolli, Domenico Tarantino, Pasquale De Antonellis, Enrico Radaelli, Jani Shaik, Luca Maravigna, Paolo Ciana, Menotti Ruvo, Rosita Russo, Angela Chambery, Gennaro Citro, Enrico P. Spugnini, Alfonso Baldi, Paola Bontempo, Gilda Cobellis, Dante Rotili, Francesca Cuomo, Angela Nebbioso, and Vincenzo Carafa

Abstract

Purpose: Alteration in cell death is a hallmark of cancer. A functional role regulating survival, apoptosis, and necroptosis has been attributed to RIP1/3 complexes.Experimental Design: We have investigated the role of RIP1 and the effects of MC2494 in cell death induction, using different methods as flow cytometry, transcriptome analysis, immunoprecipitation, enzymatic assays, transfections, mutagenesis, and in vivo studies with different mice models.Results: Here, we show that RIP1 is highly expressed in cancer, and we define a novel RIP1/3–SIRT1/2–HAT1/4 complex. Mass spectrometry identified five acetylations in the kinase and death domain of RIP1. The novel characterized pan-SIRT inhibitor, MC2494, increases RIP1 acetylation at two additional sites in the death domain. Mutagenesis of the acetylated lysine decreases RIP1-dependent cell death, suggesting a role for acetylation of the RIP1 complex in cell death modulation. Accordingly, MC2494 displays tumor-selective potential in vitro, in leukemic blasts ex vivo, and in vivo in both xenograft and allograft cancer models. Mechanistically, MC2494 induces bona fide tumor-restricted acetylated RIP1/caspase-8–mediated apoptosis. Excitingly, MC2494 displays tumor-preventive activity by blocking 7,12-dimethylbenz(α)anthracene–induced mammary gland hyperproliferation in vivo.Conclusions: These preventive features might prove useful in patients who may benefit from a recurrence-preventive approach with low toxicity during follow-up phases and in cases of established cancer predisposition. Thus, targeting the newly identified RIP1 complex may represent an attractive novel paradigm in cancer treatment and prevention. Clin Cancer Res; 24(12); 2886–900. ©2018 AACR.

Published

2023

12. Supplementary Figure 6 from c-Myc Modulation and Acetylation Is a Key HDAC Inhibitor Target in Cancer

Author

Lucia Altucci, Hendrik G. Stunnenberg, Valeria Belsito Petrizzi, Concetta Ingenito, Gabriella Lania, Francesco Iovino, Guillermo Garcia-Manero, Saverio Minucci, Isabella Pallavicini, Rosaria Benedetti, Matthias Nees, Joost Martens, Ciro Abbondanza, Francesco Paolo Tambaro, Mariarosaria Conte, Vincenzo Carafa, and Angela Nebbioso

Abstract

HDACI-specific effects on c-Myc acetylation.

Published

2023

13. Supplementary Figure 2 from c-Myc Modulation and Acetylation Is a Key HDAC Inhibitor Target in Cancer

Author

Lucia Altucci, Hendrik G. Stunnenberg, Valeria Belsito Petrizzi, Concetta Ingenito, Gabriella Lania, Francesco Iovino, Guillermo Garcia-Manero, Saverio Minucci, Isabella Pallavicini, Rosaria Benedetti, Matthias Nees, Joost Martens, Ciro Abbondanza, Francesco Paolo Tambaro, Mariarosaria Conte, Vincenzo Carafa, and Angela Nebbioso

Abstract

Effects of c-Myc overexpression, p21shRNA and TRAILshRNA (A).

Published

2023

14. Supplementary Table 2 from c-Myc Modulation and Acetylation Is a Key HDAC Inhibitor Target in Cancer

Author

Lucia Altucci, Hendrik G. Stunnenberg, Valeria Belsito Petrizzi, Concetta Ingenito, Gabriella Lania, Francesco Iovino, Guillermo Garcia-Manero, Saverio Minucci, Isabella Pallavicini, Rosaria Benedetti, Matthias Nees, Joost Martens, Ciro Abbondanza, Francesco Paolo Tambaro, Mariarosaria Conte, Vincenzo Carafa, and Angela Nebbioso

Abstract

Primer sequence, location and product of amplification size.

Published

2023

15. Supplementary Figures from RIP1–HAT1–SIRT Complex Identification and Targeting in Treatment and Prevention of Cancer

Author

Lucia Altucci, Antonello Mai, Hendrik G. Stunnenberg, Massimo Zollo, Rino Ragno, Adele Pirolli, Domenico Tarantino, Pasquale De Antonellis, Enrico Radaelli, Jani Shaik, Luca Maravigna, Paolo Ciana, Menotti Ruvo, Rosita Russo, Angela Chambery, Gennaro Citro, Enrico P. Spugnini, Alfonso Baldi, Paola Bontempo, Gilda Cobellis, Dante Rotili, Francesca Cuomo, Angela Nebbioso, and Vincenzo Carafa

Abstract

Supplementary Figures

Published

2023

16. Supplementary Figure 5 from c-Myc Modulation and Acetylation Is a Key HDAC Inhibitor Target in Cancer

Author

Lucia Altucci, Hendrik G. Stunnenberg, Valeria Belsito Petrizzi, Concetta Ingenito, Gabriella Lania, Francesco Iovino, Guillermo Garcia-Manero, Saverio Minucci, Isabella Pallavicini, Rosaria Benedetti, Matthias Nees, Joost Martens, Ciro Abbondanza, Francesco Paolo Tambaro, Mariarosaria Conte, Vincenzo Carafa, and Angela Nebbioso

Abstract

HDACi effects in different cell lines.

Published

2023

17. Supplementary Figure 2 from Context-Selective Death of Acute Myeloid Leukemia Cells Triggered by the Novel Hybrid Retinoid-HDAC Inhibitor MC2392

Author

Lucia Altucci, Hendrik G. Stunnenberg, Antonello Mai, Angela Nebbioso, Hugues de Thé, Joost H.A. Martens, Amit Mandoli, Yves Collette, Armelle Goubard, Rèmy Castellano, Sergio Valente, Julien Ablain, Kees-Jan Françoijs, Filomena Matarese, Francesca Petraglia, Dante Rotili, Mariarosaria Conte, Vincenzo Carafa, and Floriana De Bellis

Abstract

PDF file - 147KB, Differences in gene expression between ATRA and MC2392.

Published

2023

18. Supplementary Figure 1 from Context-Selective Death of Acute Myeloid Leukemia Cells Triggered by the Novel Hybrid Retinoid-HDAC Inhibitor MC2392

Author

Lucia Altucci, Hendrik G. Stunnenberg, Antonello Mai, Angela Nebbioso, Hugues de Thé, Joost H.A. Martens, Amit Mandoli, Yves Collette, Armelle Goubard, Rèmy Castellano, Sergio Valente, Julien Ablain, Kees-Jan Françoijs, Filomena Matarese, Francesca Petraglia, Dante Rotili, Mariarosaria Conte, Vincenzo Carafa, and Floriana De Bellis

Abstract

PDF file - 187KB, MC2392 specificity and selectivity for PML-RARalpha binding sites.

Published

2023

19. Supplementary Materials and Methods, Tables 1 - 3 from Context-Selective Death of Acute Myeloid Leukemia Cells Triggered by the Novel Hybrid Retinoid-HDAC Inhibitor MC2392

Author

Lucia Altucci, Hendrik G. Stunnenberg, Antonello Mai, Angela Nebbioso, Hugues de Thé, Joost H.A. Martens, Amit Mandoli, Yves Collette, Armelle Goubard, Rèmy Castellano, Sergio Valente, Julien Ablain, Kees-Jan Françoijs, Filomena Matarese, Francesca Petraglia, Dante Rotili, Mariarosaria Conte, Vincenzo Carafa, and Floriana De Bellis

Abstract

PDF file - 160KB, Supplemental Materials and Methods. Supplemental Table 1. Primers. Supplemental Table 2. Analysis of the transcription level of the 148 genes associated with apoptosis revealed main differences between ATRA and MC2392. Supplemental Table 3. Primers used. Supplemental Table 4. Primers used in qPCR ChIP.

Published

2023

20. Data from Context-Selective Death of Acute Myeloid Leukemia Cells Triggered by the Novel Hybrid Retinoid-HDAC Inhibitor MC2392

Author

Lucia Altucci, Hendrik G. Stunnenberg, Antonello Mai, Angela Nebbioso, Hugues de Thé, Joost H.A. Martens, Amit Mandoli, Yves Collette, Armelle Goubard, Rèmy Castellano, Sergio Valente, Julien Ablain, Kees-Jan Françoijs, Filomena Matarese, Francesca Petraglia, Dante Rotili, Mariarosaria Conte, Vincenzo Carafa, and Floriana De Bellis

Abstract

HDAC inhibitors (HDACi) are widely used in the clinic to sensitize tumorigenic cells for treatment with other anticancer compounds. The major drawback of HDACi is the broad inhibition of the plethora of HDAC-containing complexes. In acute promyelocytic leukemia (APL), repression by the PML-RARα oncofusion protein is mediated by an HDAC-containing complex that can be dissociated by pharmacologic doses of all trans retinoic acid (ATRA) inducing differentiation and cell death at the expense of side effects and recurrence. We hypothesized that the context-specific close physical proximity of a retinoid and HDACi-binding protein in the repressive PML-RARα-HDAC complex may permit selective targeting by a hybrid molecule of ATRA with a 2-aminoanilide tail of the HDAC inhibitor MS-275, yielding MC2392. We show that MC2392 elicits weak ATRA and essentially no HDACi activity in vitro or in vivo. Genome-wide epigenetic analyses revealed that in NB4 cells expressing PML-RARα, MC2392 induces changes in H3 acetylation at a small subset of PML-RARα–binding sites. RNA-seq reveals that MC2392 alters expression of a number of stress-responsive and apoptotic genes. Concordantly, MC2392 induced rapid and massive, caspase-8–dependent cell death accompanied by RIP1 induction and ROS production. Solid and leukemic tumors are not affected by MC2392, but expression of PML-RARα conveys efficient MC2392-induced cell death. Our data suggest a model in which MC2392 binds to the RARα moiety and selectively inhibits the HDACs resident in the repressive complex responsible for the transcriptional impairment in APLs. Our findings provide proof-of-principle of the concept of a context-dependent targeted therapy. Cancer Res; 74(8); 2328–39. ©2014 AACR.

Published

2023

21. Supplementary Figure 3 from Context-Selective Death of Acute Myeloid Leukemia Cells Triggered by the Novel Hybrid Retinoid-HDAC Inhibitor MC2392

Author

Lucia Altucci, Hendrik G. Stunnenberg, Antonello Mai, Angela Nebbioso, Hugues de Thé, Joost H.A. Martens, Amit Mandoli, Yves Collette, Armelle Goubard, Rèmy Castellano, Sergio Valente, Julien Ablain, Kees-Jan Françoijs, Filomena Matarese, Francesca Petraglia, Dante Rotili, Mariarosaria Conte, Vincenzo Carafa, and Floriana De Bellis

Abstract

PDF file - 37KB, ChIP analysis for MC2392 specific target genes.

Published

2023

22. Supplementary Figure 4 from Context-Selective Death of Acute Myeloid Leukemia Cells Triggered by the Novel Hybrid Retinoid-HDAC Inhibitor MC2392

Author

Lucia Altucci, Hendrik G. Stunnenberg, Antonello Mai, Angela Nebbioso, Hugues de Thé, Joost H.A. Martens, Amit Mandoli, Yves Collette, Armelle Goubard, Rèmy Castellano, Sergio Valente, Julien Ablain, Kees-Jan Françoijs, Filomena Matarese, Francesca Petraglia, Dante Rotili, Mariarosaria Conte, Vincenzo Carafa, and Floriana De Bellis

Abstract

PDF file - 91KB, Death pathways modulation by MC2392.

Published

2023

23. Epi-Regulation of Cell Death in Cancer

Author

Antonio, Beato, Della, Torre, Laura, Vincenza, Capone, Daniela, Carannante, Gregorio, Favale, Giulia, Verrilli, Lucia, Altucci, and Vincenzo, Carafa

Abstract

How do organisms regulate the correct balance between the production of “new” cells and the elimination of the “old” ones, remains an important biology issue under investigation. Cell(s) death represents a fundamental process involved in organism development and cell homeostasis, whose alteration is considered one hallmark of cancer and lead to drug resistance and consequently treatment failure. The recent re-classification of cell death has identified new molecular programs in which several proteins have a pivotal role. Several studies have highlighted a direct link between epigenetic modifications and cell death mechanisms. Different epi-modifications have been described, capable of regulating diverse key players implicated in cell death, leading to uncontrolled proliferation of cancer cells. Scientific efforts are focused on the understanding the epigenetic regulation of cell death mechanisms by developing tools and/or new epi-molecules able to overcome cell death resistance. The development of new epi-molecular tools can overcome cell death deregulation thus potentially improving the sensitivity to the anti-tumor therapies. This chapter focuses on the main epigenetic deregulations in cell death mechanisms in cancer.

Published

2023

24. FASN multi-omic characterization reveals metabolic heterogeneity in pancreatic and prostate adenocarcinoma

Author

Ugo Chianese, Chiara Papulino, Ahmad Ali, Fortunato Ciardiello, Salvatore Cappabianca, Lucia Altucci, Vincenzo Carafa, Rosaria Benedetti, Chianese, Ugo, Papulino, Chiara, Ali, Ahmad, Ciardiello, Fortunato, Cappabianca, Salvatore, Altucci, Lucia, Carafa, Vincenzo, and Benedetti, Rosaria

Subjects

Metabolism, Prostate adenocarcinoma, Proliferation, General Medicine, FASN, Pancreatic adenocarcinoma, General Biochemistry, Genetics and Molecular Biology

Abstract

Background Pancreatic ductal adenocarcinoma (PDAC) and prostate cancer (PCa) are among the most prevalent malignant tumors worldwide. There is now a comprehensive understanding of metabolic reprogramming as a hallmark of cancer. Fatty acid synthase (FASN) is a key regulator of the lipid metabolic network, providing energy to favor tumor proliferation and development. Whereas the biological role of FASN is known, its response and sensitivity to inhibition have not yet been fully established in these two cancer settings. Methods To evaluate the association between FASN expression, methylation, prognosis, and mutational profile in PDAC and PCa, we interrogated public databases and surveyed online platforms using TCGA data. The STRING database was used to investigate FASN interactors, and the Gene Set Enrichment Analysis platform Reactome database was used to perform an enrichment analysis using data from RNA sequencing public databases of PDAC and PCa. In vitro models using PDAC and PCa cell lines were used to corroborate the expression of FASN, as shown by Western blot, and the effects of FASN inhibition on cell proliferation/cell cycle progression and mitochondrial respiration were investigated with MTT, colony formation assay, cell cycle analysis and MitoStress Test. Results The expression of FASN was not modulated in PDAC compared to normal pancreatic tissues, while it was overexpressed in PCa, which also displayed a different level of promoter methylation. Based on tumor grade, FASN expression decreased in advanced stages of PDAC, but increased in PCa. A low incidence of FASN mutations was found for both tumors. FASN was overexpressed in PCa, despite not reaching statistical significance, and was associated with a worse prognosis than in PDAC. The biological role of FASN interactors correlated with lipid metabolism, and GSEA indicated that lipid-mediated mitochondrial respiration was enriched in PCa. Following validation of FASN overexpression in PCa compared to PDAC in vitro, we tested TVB-2640 as a FASN inhibitor. PCa proliferation arrest was modulated by FASN inhibition in a dose- and time-dependent manner, whereas PDAC proliferation was not altered. In line with this finding, mitochondrial respiration was found to be more affected in PCa than in PDAC. FASN inhibition interfered with metabolic signaling causing lipid accumulation and affecting cell viability with an impact on the replicative processes. Conclusions FASN exhibited differential expression patterns in PDAC and PCa, suggesting a different evolution during cancer progression. This was corroborated by the fact that both tumors responded differently to FASN inhibition in terms of proliferative potential and mitochondrial respiration, indicating that its use should reflect context specificity.

Published

2023

25. Emerging Roles of SIRT5 in Metabolism, Cancer, and SARS-CoV-2 Infection

Author

Emanuele Fabbrizi, Francesco Fiorentino, Vincenzo Carafa, Lucia Altucci, Antonello Mai, Dante Rotili, Fabbrizi, Emanuele, Fiorentino, Francesco, Carafa, Vincenzo, Altucci, Lucia, Mai, Antonello, and Rotili, Dante

Subjects

sirtuins, HDAC, SIRT5 modulator, protein lysine desuccinylation, SIRT5, General Medicine, epigenetic

Abstract

Sirtuin 5 (SIRT5) is a predominantly mitochondrial enzyme catalyzing the removal of glutaryl, succinyl, malonyl, and acetyl groups from lysine residues through a NAD+-dependent deacylase mechanism. SIRT5 is an important regulator of cellular homeostasis and modulates the activity of proteins involved in different metabolic pathways such as glycolysis, tricarboxylic acid (TCA) cycle, fatty acid oxidation, electron transport chain, generation of ketone bodies, nitrogenous waste management, and reactive oxygen species (ROS) detoxification. SIRT5 controls a wide range of aspects of myocardial energy metabolism and plays critical roles in heart physiology and stress responses. Moreover, SIRT5 has a protective function in the context of neurodegenerative diseases, while it acts as a context-dependent tumor promoter or suppressor. In addition, current research has demonstrated that SIRT5 is implicated in the SARS-CoV-2 infection, although opposing conclusions have been drawn in different studies. Here, we review the current knowledge on SIRT5 molecular actions under both healthy and diseased settings, as well as its functional effects on metabolic targets. Finally, we revise the potential of SIRT5 as a therapeutic target and provide an overview of the currently reported SIRT5 modulators, which include both activators and inhibitors.

Published

2023

26. 763 ACTIVATION OF SIRT1 ATTENUATES VASCULAR DYSFUNCTION AND THROMBOSIS IN MTHFR DEFICIENCY

Author

Albino Carrizzo, Concetta Iside, Angela Nebbioso, Vincenzo Carafa, Antonio Damato, Michele Ciccarelli, Eleonora Venturini, Paola Di Pietro, Bruno Trimarco, Carmine Selleri, Lucia Altucci, and Carmine Vecchione

Subjects

Cardiology and Cardiovascular Medicine

Abstract

Beyond well-assessed risk factors, cardiovascular events could be also associated with the presence of epigenetic and genetic alterations, such as the methylenetetrahydrofolate-reductase (MTHFR) C677T polymorphism. This gene variant is related to increased circulating levels of homocysteine (Hcy) and cardiovascular risk. However, heterozygous carriers have an augmented risk of cardiovascular accidents independently from normal Hcy levels, suggesting the presence of additional deregulated processes in MTHFR C677T carriers. Here we hypothesize that targeting Sirtuin 1 (SIRT1) could be an alternative mechanism to control the cardiovascular risk associated to MTHFR deficiency condition. Flow Mediated Dilatation (FMD) and light transmission aggregometry assay were performed in subjects carrying MTHFR C677T allele after administration of resveratrol, the most powerful natural clinical usable compound that owns SIRT1 activating properties. MTHFR C677T carriers with normal Hcy levels revealed endothelial dysfunction and enhanced platelet aggregation associated with SIRT1 downregulation. SIRT1 activity stimulation by resveratrol intake was able to override these abnormalities without affecting Hcy levels. Impaired endothelial function, bleeding time, and wire-induced thrombus formation were rescued in a heterozygous Mthfr-deficient (Mthfr+/-) mouse model after resveratrol treatment. Using a cell-based high-throughput multiplexed screening (HTS) assay, a novel selective synthetic SIRT1 activator, namely ISIDE11, was identified. Ex vivo and in vivo treatment of Mthfr+/- mice with ISIDE11 rescues endothelial vasorelaxation and reduces wire-induced thrombus formation, effects that were abolished by SIRT1 inhibitor. Moreover, platelets from MTHFR C677T allele carriers treated with ISIDE11 showed normalization of their typical hyper-reactivity. These results candidate SIRT1 activation as a new therapeutic strategy to contain cardio and cerebrovascular events in MTHFR carriers.

Published

2022

27. Histone lysine demethylase inhibition reprograms prostate cancer metabolism and mechanics

Author

Ugo Chianese, Chiara Papulino, Eugenia Passaro, Tom MJ. Evers, Mehrad Babaei, Antonella Toraldo, Tommaso De Marchi, Emma Niméus, Vincenzo Carafa, Maria Maddalena Nicoletti, Nunzio Del Gaudio, Nunzia Iaccarino, Antonio Randazzo, Dante Rotili, Antonello Mai, Salvatore Cappabianca, Alireza Mashaghi, Fortunato Ciardiello, Lucia Altucci, Rosaria Benedetti, Chianese, Ugo, Papulino, Chiara, Passaro, Eugenia, Evers, Tom Mj, Babaei, Mehrad, Toraldo, Antonella, De Marchi, Tommaso, Niméus, Emma, Carafa, Vincenzo, Nicoletti, Maria Maddalena, Del Gaudio, Nunzio, Iaccarino, Nunzia, Randazzo, Antonio, Rotili, Dante, Mai, Antonello, Cappabianca, Salvatore, Mashaghi, Alireza, Ciardiello, Fortunato, Altucci, Lucia, Benedetti, Rosaria, Evers, Tom MJ., and Maddalena Nicoletti, Maria

Subjects

Histone Demethylases, Proteomics, Male, PCa, AR,Cell stiffness, KDMs, Lipid, Metabolism, PCa, Proteomic, Androgen Antagonists, Cell Biology, Cell stiffne, Lipid, Lipids, KDM, Androgen, Gene Expression Regulation, Neoplastic, Prostatic Neoplasms, Castration-Resistant, Metabolism, Androgens, Humans, Histone Demethylase, Androgen Antagonist, Molecular Biology, AR, Human

Abstract

Objective: Aberrant activity of androgen receptor (AR) is the primary cause underlying development and progression of prostate cancer (PCa) and castration-resistant PCa (CRPC). Androgen signaling regulates gene transcription and lipid metabolism, facilitating tumor growth and therapy resistance in early and advanced PCa. Although direct AR signaling inhibitors exist, AR expression and function can also be epigenetically regulated. Specifically, lysine (K)-specific demethylases (KDMs), which are often overexpressed in PCa and CRPC phenotypes, regulate the AR transcriptional program. Methods: We investigated LSD1/UTX inhibition, two KDMs, in PCa and CRPC using a multi-omics approach. We first performed a mitochondrial stress test to evaluate respiratory capacity after treatment with MC3324, a dual KDM-inhibitor, and then carried out lipidomic, proteomic, and metabolic analyses. We also investigated mechanical cellular properties with acoustic force spectroscopy. Results: MC3324 induced a global increase in H3K4me2 and H3K27me3 accompanied by significant growth arrest and apoptosis in androgen -responsive and-unresponsive PCa systems. LSD1/UTX inhibition downregulated AR at both transcriptional and non-transcriptional level, showing cancer selectivity, indicating its potential use in resistance to androgen deprivation therapy. Since MC3324 impaired metabolic activity, by modifying the protein and lipid content in PCa and CRPC cell lines. Epigenetic inhibition of LSD1/UTX disrupted mitochondrial ATP production and mediated lipid plasticity, which affected the phosphocholine class, an important structural element for the cell membrane in PCa and CRPC associated with changes in physical and mechanical properties of cancer cells. Conclusions: Our data suggest a network in which epigenetics, hormone signaling, metabolite availability, lipid content, and mechano-metabolic process are closely related. This network may be able to identify additional hotspots for pharmacological intervention and un-derscores the key role of KDM-mediated epigenetic modulation in PCa and CRPC.(c) 2022 The Author(s). Published by Elsevier GmbH. This is an open access article under the CC BY-NC-ND license (http://creativecommons.org/licenses/by-nc-nd/4.0/).

Published

2022

28. HAT1: Landscape of Biological Function and Role in Cancer

Author

Vincenza Capone, Laura Della Torre, Daniela Carannante, Mehrad Babaei, Lucia Altucci, Rosaria Benedetti, Vincenzo Carafa, Capone, V., Della Torre, L., Carannante, D., Babaei, M., Altucci, L., Benedetti, R., and Carafa, V.

Subjects

inflammation, cancer, General Medicine, HAT1, epigenetic, acetylation

Abstract

Histone modifications, as key chromatin regulators, play a pivotal role in the pathogenesis of several diseases, such as cancer. Acetylation, and more specifically lysine acetylation, is a reversible epigenetic process with a fundamental role in cell life, able to target histone and non-histone proteins. This epigenetic modification regulates transcriptional processes and protein activity, stability, and localization. Several studies highlight a specific role for HAT1 in regulating molecular pathways, which are altered in several pathologies, among which is cancer. HAT1 is the first histone acetyltransferase discovered; however, to date, its biological characterization is still unclear. In this review, we summarize and update the current knowledge about the biological function of this acetyltransferase, highlighting recent advances of HAT1 in the pathogenesis of cancer.

Published

2023

29. SIRT1 pharmacological activation rescues vascular dysfunction and prevents thrombosis in MTHFR deficiency

Author

Albino Carrizzo, Concetta Iside, Angela Nebbioso, Vincenzo Carafa, Antonio Damato, Sebastiano Sciarretta, Giacomo Frati, Flavio Di Nonno, Valentina Valenti, Michele Ciccarelli, Eleonora Venturini, Mariarosaria Scioli, Paola Di Pietro, Tommaso Bucci, Valentina Giudice, Marianna Storto, Bianca Serio, Annibale Alessandro Puca, Giuseppe Giugliano, Valentina Trimarco, Raffaele Izzo, Bruno Trimarco, Carmine Selleri, Lucia Altucci, Carmine Vecchione, Carrizzo, Albino, Iside, Concetta, Nebbioso, Angela, Carafa, Vincenzo, Damato, Antonio, Sciarretta, Sebastiano, Frati, Giacomo, Di Nonno, Flavio, Valenti, Valentina, Ciccarelli, Michele, Venturini, Eleonora, Scioli, Mariarosaria, Di Pietro, Paola, Bucci, Tommaso, Giudice, Valentina, Storto, Marianna, Serio, Bianca, Puca, Annibale Alessandro, Giugliano, Giuseppe, Trimarco, Valentina, Izzo, Raffaele, Trimarco, Bruno, Selleri, Carmine, Altucci, Lucia, and Vecchione, Carmine

Subjects

Pharmacology, Endothelium, MTHFR, Nitric oxide, SIRT1, Vascular function, Animals, Genotype, Homocystinuria, Humans, Methylenetetrahydrofolate Reductase (NADPH2), Mice, Muscle Spasticity, Psychotic Disorders, Resveratrol, Sirtuin 1, Thrombosis, ndothelium, Cell Biology, Article, Cellular and Molecular Neuroscience, Molecular Medicine, Molecular Biology

Abstract

Beyond well-assessed risk factors, cardiovascular events could be also associated with the presence of epigenetic and genetic alterations, such as the methylenetetrahydrofolate-reductase (MTHFR) C677T polymorphism. This gene variant is related to increased circulating levels of homocysteine (Hcy) and cardiovascular risk. However, heterozygous carriers have an augmented risk of cardiovascular accidents independently from normal Hcy levels, suggesting the presence of additional deregulated processes in MTHFR C677T carriers. Here, we hypothesize that targeting Sirtuin 1 (SIRT1) could be an alternative mechanism to control the cardiovascular risk associated to MTHFR deficiency condition. Flow Mediated Dilatation (FMD) and light transmission aggregometry assay were performed in subjects carrying MTHFR C677T allele after administration of resveratrol, the most powerful natural clinical usable compound that owns SIRT1 activating properties. MTHFR C677T carriers with normal Hcy levels revealed endothelial dysfunction and enhanced platelet aggregation associated with SIRT1 downregulation. SIRT1 activity stimulation by resveratrol intake was able to override these abnormalities without affecting Hcy levels. Impaired endothelial function, bleeding time, and wire-induced thrombus formation were rescued in a heterozygous Mthfr-deficient (Mthfr+/–) mouse model after resveratrol treatment. Using a cell-based high-throughput multiplexed screening (HTS) assay, a novel selective synthetic SIRT1 activator, namely ISIDE11, was identified. Ex vivo and in vivo treatment of Mthfr+/– mice with ISIDE11 rescues endothelial vasorelaxation and reduces wire-induced thrombus formation, effects that were abolished by SIRT1 inhibitor. Moreover, platelets from MTHFR C677T allele carriers treated with ISIDE11 showed normalization of their typical hyper-reactivity. These results candidate SIRT1 activation as a new therapeutic strategy to contain cardio and cerebrovascular events in MTHFR carriers.

Published

2022

30. HIF3A Inhibition Triggers Browning of White Adipocytes via Metabolic Rewiring

Author

Francesca Cuomo, Carmela Dell’Aversana, Teresa Chioccarelli, Veronica Porreca, Francesco Manfrevola, Chiara Papulino, Vincenzo Carafa, Rosaria Benedetti, Lucia Altucci, Gilda Cobellis, Cuomo, F., Dell'Aversana, C., Chioccarelli, T., Porreca, V., Manfrevola, F., Papulino, C., Carafa, V., Benedetti, R., Altucci, L., and Cobellis, G.

Subjects

browning, Cell and Developmental Biology, QH301-705.5, Cell Biology, thermogenesis, Biology (General), sirts, CB1, HIF3α, Developmental Biology, Original Research, adipose tissue

Abstract

Maintenance of energy balance between intake and expenditure is a prerequisite of human health, disrupted in severe metabolic diseases, such as obesity and type 2 diabetes (T2D), mainly due to accumulation of white adipose tissue (WAT). WAT undergoes a morphological and energetic remodelling toward brown adipose tissue (BAT) and the BAT activation has anti-obesity potential. The mechanisms or the regulatory factors able to activate BAT thermogenesis have been only partially deciphered. Identifying novel regulators of BAT induction is a question of great importance for fighting obesity and T2D. Here, we evaluated the role of Hif3α in murine pre-adipocyte 3T3-L1 cell line, a versatile and well characterized biological model of adipogenesis, by gain- and loss-of function approaches and in thermogenesis-induced model in vivo. HIF3A is regulated by inflammation, it modulates lypolysis in adipose tissue of obese adults, but its role in energy metabolism has not previously been investigated. We characterized gene and protein expression patterns of adipogenesis and metabolic activity in vitro and mechanistically in vivo. Overexpression of Hif3α in differentiating adipocytes increases white fat cells, whereas silencing of Hif3α promotes “browning” of white cells, activating thermogenesis through upregulation of Ucp1, Elovl3, Prdm16, Dio2 and Ppargc1a genes. Investigating cell metabolism, Seahorse Real-Time Cell Metabolism Analysis showed that silencing of Hif3α resulted in a significant increase of mitochondrial uncoupling with a concomitant increase in acetyl-CoA metabolism and Sirt1 and Sirt3 expression. The causal Hif3α/Ucp1 inverse relation has been validated in Cannabinoid receptor 1 (CB1) knockout, a thermogenesis-induced model in vivo. Our data indicate that Hif3α inhibition triggers “browning” of white adipocytes activating the beneficial thermogenesis rewiring energy metabolism in vitro and in vivo. HIF3A is a novel player that controls the energy metabolism with potential applications in developing therapy to fight metabolic disorders, as obesity, T2D and ultimately cancer.

Published

2022

31. CBX2 shapes chromatin accessibility promoting AML via p38 MAPK signaling pathway

Author

Nunzio Del Gaudio, Antonella Di Costanzo, Ning Qing Liu, Lidio Conte, Carmela Dell’Aversana, Guglielmo Bove, Rosaria Benedetti, Liliana Montella, Fortunato Ciardiello, Vincenzo Carafa, Concetta Ambrosino, Valeria Tucci, Mariarosaria Conte, Joost H. A. Martens, Hendrik G. Stunnenberg, Angela Nebbioso, Lucia Altucci, Del Gaudio, Nunzio, Di Costanzo, Antonella, Liu, Ning Qing, Conte, Lidio, Dell’Aversana, Carmela, Bove, Guglielmo, Benedetti, Rosaria, Montella, Liliana, Ciardiello, Fortunato, Carafa, Vincenzo, Ambrosino, Concetta, Tucci, Valeria, Conte, Mariarosaria, Martens, Joost H. A., Stunnenberg, Hendrik G., Nebbioso, Angela, and Altucci, Lucia

Subjects

Polycomb Repressive Complex 1, Leukemia, Myeloid, Acute, Cancer Research, PcG, Leukemia, CBX2, Epigenetics, Oncology, Humans, Molecular Medicine, p38 Mitogen-Activated Protein Kinases, Molecular Biology, Chromatin, Signal Transduction

Abstract

Background The dynamic epigenome and proteins specialized in the interpretation of epigenetic marks critically contribute to leukemic pathogenesis but also offer alternative therapeutic avenues. Targeting newly discovered chromatin readers involved in leukemogenesis may thus provide new anticancer strategies. Accumulating evidence suggests that the PRC1 complex member CBX2 is overexpressed in solid tumors and promotes cancer cell survival. However, its role in leukemia is still unclear. Methods We exploited reverse genetic approaches to investigate the role of CBX2 in human leukemic cell lines and ex vivo samples. We also analyzed phenotypic effects following CBX2 silencing using cellular and molecular assays and related functional mechanisms by ATAC-seq and RNA-seq. We then performed bioinformatic analysis of ChIP-seq data to explore the influence of histone modifications in CBX2-mediated open chromatin sites. Lastly, we used molecular assays to determine the contribution of CBX2-regulated pathways to leukemic phenotype. Results We found CBX2 overexpressed in leukemia both in vitro and ex vivo samples compared to CD34+ cells. Decreased CBX2 RNA levels prompted a robust reduction in cell proliferation and induction of apoptosis. Similarly, sensitivity to CBX2 silencing was observed in primary acute myeloid leukemia samples. CBX2 suppression increased genome-wide chromatin accessibility followed by alteration of leukemic cell transcriptional programs, resulting in enrichment of cell death pathways and downregulation of survival genes. Intriguingly, CBX2 silencing induced epigenetic reprogramming at p38 MAPK-associated regulatory sites with consequent deregulation of gene expression. Conclusions Our results identify CBX2 as a crucial player in leukemia progression and highlight a potential druggable CBX2-p38 MAPK network in AML.

Published

2022

32. Characterization of Histone Acetyltransferase-1 in cancer cells

Author

Angelita Poziello, Angela Nebbioso, Hendrik G. Stunnenberg, Joost H. A. Martens, Lucia Altucci, Vincenzo Carafa, Angelita Poziello, Angela Nebbioso, Hendrik G. Stunnenberg, Joost H.A. Martens, Lucia Altucci, Vincenzo Carafa, Poziello, Angelita, Nebbioso, Angela, Stunnenberg, Hendrik G., Martens, Joost H. A., Altucci, Lucia, and Carafa, Vincenzo

Abstract

Introduction: Acetylation of histone and non-histone proteins is a post-translational modification mostly associated with activation of gene transcription. The first histone acetyltransferase (HAT) identified as modifying newly synthesized histone H4 at Lys5 and Lys12 was a type B HAT named HAT1. Although it was the first HAT to be discovered, it remains one of the most poorly studied enzymes in its class. In addition to its well-established role in the cytoplasm, recent findings have revealed new and intriguing aspects about the function of HAT1 in the nucleus. Purpose: Uncovering the non-canonical role of HAT1 first in DNA damage repair, then in chromatin assembly and chromatin maturation prompted in-depth investigations into the functional role of this protein in several biological processes. The involvement of HAT1 in regulating different pathways associated with a wide range of diseases, including cancer, and its contradictory role in carcinogenesis lead us to elucidate its role. Specifically, recent studies have shown that lower expression of HAT1 is associated with the pathogenesis of lung cancer 1, while in hepatocellular carcinoma, nasopharyngeal cancer, and pancreatic cancer 2–4 is highly expressed, acting as an oncogene, and linked to poor prognosis 4. Results and Conclusions: Immunoprecipitation experiment of overexpressed HAT1 combined with MS/MS analysis will be important to assess in which protein complexes HAT1 resides in breast cancer cell line. Moreover, genomics will be used for seeking possible molecular markers that can contribute at activating oncogenes or inactivating tumor suppressor genes. The main goal of this project is to understand HAT1 molecular mechanisms in cancer in order to develop novel strategy for cancer therapy. While efforts to identify molecules able to block its enzymatic activity are ongoing, the development of new compounds targeting one of its interactors could provide another entry point for HAT1 inhibition. REFERENCES

Published

2020

33. RIPK1-targeting in cancer: modulation of programmed cell death process for cancer treatment

Author

Laura Della Torre, Angela Nebbioso, Hendrik G. Stunnenberg, Joost H. A. Martens, Lucia Altucci, Vincenzo Carafa, Laura Della Torre, Angela Nebbioso, Hendrik G. Stunnenberg, Joost H.A. Martens, Lucia Altucci and Vincenzo Carafa, Della Torre, Laura, Nebbioso, Angela, Stunnenberg, Hendrik G., Martens, Joost H. A., Altucci, Lucia, and Carafa, Vincenzo

Subjects

CELL DEATH, NECROPTOSIS, CANCER

Abstract

PURPOSE: Programmed cell death (PCD) is an important cellular event responsible for the maintenance of cellular homeostasis. More studies have suggested that the imbalance between cell survival and cell death leads to tumorigenesis, a process in which cells escape from PCDs. INTRODUCTION: Among the well-known cell death pathways, necroptosis has been defined to be a regulated necrotic cell death, which mediators belong both to the apoptotic and necrotic pathways [1]. The process can be triggered by a variety of stimuli and requires the activation of receptor-interacting protein (RIP) kinases RIPK1 and RIPK3, as well as mixed lineage kinase domain-like protein (MLKL) [2]. RESULTS AND CONCLUSIONS: A recent study has correlated the acetylation of RIP to the tumorigenesis and cell death process. The molecular complex mediated by RIPK1 shows the co-presence of proteins with different enzymatic activities such as acetyltransferase, kinase and deacetylase elucidating cancer not only as a genetic but also an epigenetic disease [3]. Since RIPK1 is overexpressed in several cancer cell types and it is involved in either survival or apoptosis and necroptosis, one of the main goals of the project is to determine how to modulate the RIP1-complex, in order to lead malignant cells to cell death. To reach this aim, the interactome study in leukaemia cell line will be performed to clarify the involvement of RIPK1. While the roles of RIPK3 and MLKL in leukemogenesis are already known, the novelty is to understand “how” RIPK1 triggers different cellular pathways that leads cells to make a critical decision either to survive or die. Starting from the characterization of Necrostatins, the project includes the identification of new modulators of RIPK1 which could regulate the activated molecular complex in different cellular processes and eventually to make necroptosis a pharmacologically controllable event.

Published

2020

34. SARS-CoV-2 spike protein detection through a plasmonic D-shaped plastic optical fiber aptasensor

Author

Lorenzo Lunelli, Francesco Arcadio, Lucia Altucci, Laura Pasquardini, Nunzio Cennamo, Vincenzo Carafa, Lia Vanzetti, Luigi Zeni, Cennamo, N., Pasquardini, L., Arcadio, F., Lunelli, L., Vanzetti, L., Carafa, V., Altucci, L., and Zeni, L.

Subjects

Aptamer, Biointerface, 02 engineering and technology, Plastic, 01 natural sciences, Article, Analytical Chemistry, Fluorescence microscope, Humans, Surface plasmon resonance, Plastic optical fiber, Plastic optical fiber (POF), Plasmon, Optical Fibers, Detection limit, Self assembled monolayer (SAM) Aptamer Sars-CoV-2 Plastic optical fiber (POF) Polyethyleneglycol (PEG) Surface plasmon resonance (SPR), Chemistry, SARS-CoV-2, 010401 analytical chemistry, technology, industry, and agriculture, COVID-19, 021001 nanoscience & nanotechnology, 0104 chemical sciences, Self assembled monolayer (SAM), Surface plasmon resonance (SPR), Spike Glycoprotein, Coronavirus, Polyethyleneglycol (PEG), Biophysics, 0210 nano-technology, Biosensor, Plastics, Spike Glycoprotein, Coronaviru, Human

Abstract

A specific aptameric sequence has been immobilized on short polyethyleneglycol (PEG) interface on gold nano-film deposited on a D-shaped plastic optical fiber (POFs) probe, and the protein binding has been monitored exploiting the very sensitive surface plasmon resonance (SPR) phenomenon. The receptor-binding domain (RBD) of the SARS-CoV-2 spike glycoprotein has been specifically used to develop an aptasensor. Surface analysis techniques coupled to fluorescence microscopy and plasmonic analysis have been utilized to characterize the biointerface. Spanning a wide protein range (25 ÷ 1000 nM), the SARS-Cov-2 spike protein was detected with a Limit of Detection (LoD) of about 37 nM. Different interferents (BSA, AH1N1 hemagglutinin protein and MERS spike protein) have been tested confirming the specificity of our aptasensor. Finally, a preliminary test in diluted human serum encouraged its application in a point-of-care device, since POF-based aptasensor represent a potentially low-cost compact biosensor, characterized by a rapid response, a small size and could be an ideal laboratory portable diagnostic tool., Graphical abstract Image 1

Published

2021

35. The Role of Necroptosis: Biological Relevance and Its Involvement in Cancer

Author

Laura Della Torre, Lucia Altucci, Hendrik G. Stunnenberg, Angela Nebbioso, Joost H.A. Martens, Vincenzo Carafa, Della Torre, Laura, Nebbioso, Angela, Stunnenberg, Hendrik G, Martens, Joost H A, Carafa, Vincenzo, and Altucci, Lucia

Subjects

0301 basic medicine, Cancer Research, Programmed cell death, RIPK1 mutation, RIPK1, RIPK1 mutations, Necroptosis, Cellular homeostasis, necroptosis, Review, Biology, medicine.disease_cause, lcsh:RC254-282, 03 medical and health sciences, 0302 clinical medicine, medicine, cancer, Molecular Biology, Kinase, Cancer, lcsh:Neoplasms. Tumors. Oncology. Including cancer and carcinogens, medicine.disease, 030104 developmental biology, Oncology, Apoptosis, 030220 oncology & carcinogenesis, Carcinogenesis, Neuroscience

Abstract

Simple Summary A new form of programmed necrosis called necroptosis has emerged. This new and well-documented type of programmed cell death is involved in several human diseases, including cancer. RIPK1, the main mediator of necroptosis, in response to different stimuli, activates several molecular pathways leading to inflammation, cell survival, or cell death. Targeting necroptosis could be a new strategy for advanced therapies. In this review, we focus on the biological relevance of this type of programmed cell death and its main executor RIPK1 in pathogenesis to find novel potential clinical intervention strategies. Abstract Regulated cell death mechanisms are essential for the maintenance of cellular homeostasis. Evasion of cell death is one of the most important hallmarks of cancer. Necroptosis is a caspase independent form of regulated cell death, investigated as a novel therapeutic strategy to eradicate apoptosis resistant cancer cells. The process can be triggered by a variety of stimuli and is controlled by the activation of RIP kinases family as well as MLKL. The well-studied executor, RIPK1, is able to modulate key cellular events through the interaction with several proteins, acting as strategic crossroads of several molecular pathways. Little evidence is reported about its involvement in tumorigenesis. In this review, we summarize current studies on the biological relevance of necroptosis, its contradictory role in cancer and its function in cell fate control. Targeting necroptosis might be a novel therapeutic intervention strategy in anticancer therapies as a pharmacologically controllable event.

Published

2021

36. The Two-Faced Role of SIRT6 in Cancer

Author

Lucia Altucci, Vincenzo Carafa, Dante Rotili, Antonello Mai, Francesco Fiorentino, Gregorio Favale, Fiorentino, F., Carafa, V., Favale, G., Altucci, L., Mai, A., and Rotili, D.

Subjects

0301 basic medicine, SIRT6, Cancer Research, Programmed cell death, Cancer, Cell death modulation, Epigenetics, NAD, +, dependent deacylases, SIRT6 modulators, Review, Cell fate determination, Biology, medicine.disease_cause, lcsh:RC254-282, 03 medical and health sciences, 0302 clinical medicine, NAD+-dependent deacylases, Survivin, medicine, Epigenetic, lcsh:Neoplasms. Tumors. Oncology. Including cancer and carcinogens, medicine.disease, Cell biology, 030104 developmental biology, Oncology, 030220 oncology & carcinogenesis, Sirtuin, biology.protein, dependent deacylase, Carcinogenesis

Abstract

Simple Summary Cancer therapy relies on the employment of different strategies aimed at inducing cancer cell death through different mechanisms, including DNA damage and apoptosis induction. One of the key regulators of these pathways is the epigenetic enzyme SIRT6, which has been shown to have a dichotomous function in cell fate determination and, consequently, cancer initiation and progression. In this review, we aim to summarize the current knowledge on the role of SIRT6 in cancer. We show that it can act as both tumor suppressor and promoter, even in the same cancer type, depending on the biological context. We then describe the most promising modulators of SIRT6 which, through enzyme activation or inhibition, may impair tumor growth. These molecules can also be used for the elucidation of SIRT6 function, thereby advancing the current knowledge on this crucial protein. Abstract Sirtuin 6 (SIRT6) is a NAD+-dependent nuclear deacylase and mono-ADP-ribosylase with a wide spectrum of substrates. Through its pleiotropic activities, SIRT6 modulates either directly or indirectly key processes linked to cell fate determination and oncogenesis such as DNA damage repair, metabolic homeostasis, and apoptosis. SIRT6 regulates the expression and activity of both pro-apoptotic (e.g., Bax) and anti-apoptotic factors (e.g., Bcl-2, survivin) in a context-depending manner. Mounting evidence points towards a double-faced involvement of SIRT6 in tumor onset and progression since the block or induction of apoptosis lead to opposite outcomes in cancer. Here, we discuss the features and roles of SIRT6 in the regulation of cell death and cancer, also focusing on recently discovered small molecule modulators that can be used as chemical probes to shed further light on SIRT6 cancer biology and proposed as potential new generation anticancer therapeutics.

Published

2021

37. Discovery of novel tetrahydrobenzo[b]thiophene-3-carbonitriles as histone deacetylase inhibitors

Author

Takashi Kurohara, Piyush Gediya, Varalakshmi Raguraman, Debarpan Ghosh, Manjunath Ghate, Lucia Altucci, Vincenzo Carafa, Nikum D. Sitwala, Vinod Sanna, K. Suthindhiran, Angelita Poziello, Laura Della Torre, Dhiraj Bhatia, Takayoshi Suzuki, Vivek K. Vyas, Gediya, P., Vyas, V. K., Carafa, V., Sitwala, N., Della Torre, L., Poziello, A., Kurohara, T., Suzuki, T., Sanna, V., Raguraman, V., Suthindhiran, K., Ghosh, D., Bhatia, D., Altucci, L., and Ghate, M. D.

Subjects

Cyclic linker, Stereochemistry, Antineoplastic Agents, Apoptosis, Thiophenes, 01 natural sciences, Biochemistry, Histone Deacetylases, chemistry.chemical_compound, Structure-Activity Relationship, HDAC inhibitors, Cell Line, Tumor, Drug Discovery, Humans, Molecular Biology, Cell Proliferation, chemistry.chemical_classification, Dose-Response Relationship, Drug, Molecular Structure, 010405 organic chemistry, Organic Chemistry, Cell Cycle Checkpoints, HDAC6, HDAC1, 0104 chemical sciences, Histone Deacetylase Inhibitors, 010404 medicinal & biomolecular chemistry, Piperazine, Enzyme, Anticancer agent, chemistry, Benzo[b]thiophene-3-carbonitrile, Histone deacetylase, Piperidine, Pharmacophore, Drug Screening Assays, Antitumor, Linker

Abstract

The discovery and development of isoform-selective histone deacetylase (HDAC) inhibitor is a challenging task because of the sequence homology among HDAC enzymes. In the present work, novel tetrahydro benzo[b]thiophene-3-carbonitrile based benzamides were designed, synthesized, and evaluated as HDAC inhibitors. Pharmacophore modeling was our main design strategy, and two novel series of tetrahydro benzo[b]thiophene-3-carbonitrile derivatives with piperidine linker (series 1) and piperazine linker (series 2) were identified as HDAC inhibitors. Among all the synthesised compounds, 9h with 4-(aminomethyl) piperidine linker and 14n with piperazine linker demonstrated good activity against human HDAC1 and HDAC6, respectively. Both the compounds also exhibited good antiproliferative activity against several human cancer cell lines. Both these compounds (9h and 14n) also induced cell cycle arrest and apoptosis in U937 and MDA-MB-231 cancer cells. Overall, for the first time, this research discovered potent isoform-selective HDAC inhibitors using cyclic linker instead of the aliphatic chain and aromatic ring system, which were reported in known HDAC inhibitors.

Published

2021

38. Searching for a Putative Mechanism of RIZ2 Tumor-Promoting Function in Cancer Models

Author

Vincenzo Carafa, Lucia Altucci, Anna Sorrentino, Marzia Di Donato, Erika Di Zazzo, Gabriella Castoria, Ciro Abbondanza, Maria Michela Marino, Patrizia Gazzerro, Monica Rienzo, Amelia Casamassimi, and Caterina De Rosa

Subjects

Cancer Research, Oncogene, Microarray analysis techniques, Cell growth, PRDM2, apoptosis, 3D models, Biology, medicine.disease_cause, lcsh:Neoplasms. Tumors. Oncology. Including cancer and carcinogens, lcsh:RC254-282, Cell biology, cell proliferation, Oncology, medicine, microarray, RIZ2 overexpression, Gene silencing, Epigenetics, Viability assay, Carcinogenesis, Mitosis, Original Research

Abstract

Positive Regulatory Domain (PRDM) gene family members commonly express two main molecular variants, the PR-plus isoform usually acting as tumor suppressor and the PR-minus one functioning as oncogene. Accordingly, PRDM2/RIZ encodes for RIZ1 (PR-plus) and RIZ2 (PR-minus). In human cancers, genetic or epigenetic modifications induce RIZ1 silencing with an expression level imbalance in favor of RIZ2 that could be relevant for tumorigenesis. Additionally, in estrogen target cells and tissues, estradiol increases RIZ2 expression level with concurrent increase of cell proliferation and survival. Several attempts to study RIZ2 function in HeLa or MCF-7 cells by its over-expression were unsuccessful. Thus, we over-expressed RIZ2 in HEK-293 cells, which are both RIZ1 and RIZ2 positive but unresponsive to estrogens. The forced RIZ2 expression increased cell viability and growth, prompted the G2-to-M phase transition and organoids formation. Accordingly, microarray analysis revealed that RIZ2 regulates several genes involved in mitosis. Consistently, RIZ silencing in both estrogen-responsive MCF-7 and -unresponsive MDA-MB-231 cells induced a reduction of cell proliferation and an increase of apoptosis rate. Our findings add novel insights on the putative RIZ2 tumor-promoting functions, although additional attempts are warranted to depict the underlying molecular mechanism.

Published

2021

39. Different Approaches to Unveil Biomolecule Configurations and Their Mutual Interactions

Author

Lucia Altucci, Vincenzo Carafa, Mariarosaria Conte, M. R. Del Sorbo, Francesco Bajardi, Salvatore Capozziello, Angela Nebbioso, Rosaria Benedetti, Carlo Altucci, Hendrik G. Stunnenberg, Benedetti, R., Bajardi, F., Capozziello, S., Carafa, V., Conte, M., Del Sorbo, M. R., Nebbioso, A., Singh, M., Stunnenberg, H. G., Valadan, M., Altucci, L., and Altucci, C.

Subjects

Novel technique, Chern-Simons current, Clinical Biochemistry, optical physics, Nanotechnology, 02 engineering and technology, medicine.disease_cause, 01 natural sciences, Biochemistry, Analytical Chemistry, law.invention, law, Electrochemistry, medicine, Chromatin analysi, Irradiation, Molecular Biology, Spectroscopy, chemistry.chemical_classification, Chemistry, Biomolecule, 010401 analytical chemistry, Biochemistry (medical), Molecular biophysics, Optical physics, Biomolecules (q-bio.BM), 021001 nanoscience & nanotechnology, Laser, 0104 chemical sciences, genetic code, Quantitative Biology - Biomolecules, molecular biophysic, FOS: Biological sciences, 0210 nano-technology, Ultraviolet

Abstract

A novel technique was demonstrated that overcome important drawbacks to crosslink cells by irradiation with ultrashort UV laser pulses (L-crosslinking). To use this technique coupled to Chromatin ImmunoPrecipitation (ChIP) in a high throughput context, a pre-screening fast method needs to be implemented to set up suitable irradiation conditions of the cell sample for efficient L-crosslinking with no final and long ChIP analysis. Here a fast method is reported where living human cells have been first transfected with a vector coding for Estrogen Receptor {\alpha} (ER{\alpha}), linked to Green Florescent protein (ER{\alpha}-GFP), so that the well-known interaction between the Estrogen Receptor Elements (ERE) region of the cell DNA and the ER{\alpha} protein can be detected by studying the fluorometric response of the irradiated cells. The damage induced to cells by UV irradiation is characterized by looking at DNA integrity, proteins stability and cellular viability. A second novel approach is presented to analyze or re-visit DNA and RNA sequences and their molecular configurations. This approach is based on methods derived from Chern-Simons super-gravity adapted to describe mutations in DNA/RNA strings, as well as interactions between nucleic acids. As a preliminary case we analyze the KRAS human gene sequence and some of its mutations. Interestingly, our model shows how the Chern-Simons current are capable to characterize the mutations within a sequence, in particular giving a quantitative indication of the mutation likelihood., Comment: 33 pages, 5 figures

Published

2021

40. Trifolium Repens Blocks Proliferation in Chronic Myelogenous Leukemia via the BCR-ABL/STAT5 Pathway

Author

Angela Nebbioso, Fabrizio Merciai, Lucia Altucci, Vincenzo Carafa, Crescenzo Massaro, Pasquale Termolino, Federica Sarno, Pietro Campiglia, Giacomo Pepe, Sarno, Federica, Pepe, Giacomo, Termolino, Pasquale, Carafa, Vincenzo, Massaro, Crescenzo, Merciai, Fabrizio, Campiglia, Pietro, Nebbioso, Angela, and Altucci, Lucia

Subjects

Trifolium repens, Pharmacology, Repens, Article, medicine, Trifolium repen, Cytotoxic T cell, cancer, MTT assay, lcsh:QH301-705.5, polyphenols, K562 cells, BCR-ABL/STAT5, chronic myelogenous leukemia, isoflavonoids, K562 cell, biology, Chemistry, Cell growth, Cancer, General Medicine, biology.organism_classification, medicine.disease, lcsh:Biology (General), isoflavonoid, Chronic myelogenous leukemia

Abstract

Some species of clover are reported to have beneficial effects in human diseases. However, little is known about the activity of the forage plant Trifolium repens, or white clover, which has been recently found to exert a hepatoprotective action. Scientific interest is increasingly focused on identifying new drugs, especially natural products and their derivatives, to treat human diseases including cancer. We analyzed the anticancer effects of T. repens in several cancer cell lines. The phytochemical components of T. repens were first extracted in a methanol solution and then separated into four fractions by ultra-high-performance liquid chromatography. The effects of the total extract and each fraction on cancer cell proliferation were analyzed by MTT assay and Western blotting. T. repens and, more robustly, its isoflavonoid-rich fraction showed high cytotoxic effects in chronic myelogenous leukemia (CML) K562 cells, with IC50 values of 1.67 and 0.092 mg/mL, respectively. The block of cell growth was associated with a total inhibition of BCR-ABL/STAT5 and activation of the p38 signaling pathways. In contrast, these strongly cytotoxic effects did not occur in normal cells. Our findings suggest that the development of novel compounds derived from phytochemical molecules contained in Trifolium might lead to the identification of new therapeutic agents active against CML.

Published

2020

41. Two novel SIRT1 activators, SCIC2 and SCIC2.1, enhance SIRT1-mediated effects in stress response and senescence

Author

Sandro Cosconati, Paola Stiuso, Federica Sarno, Alessandra Feoli, Vincenzo Carafa, Gianluca Sbardella, Loreta Pia Ciuffreda, Salvatore Di Maro, Lucia Scisciola, Antonella De Angelis, Angela Nebbioso, Lucia Altucci, Scisciola, Lucia, Sarno, Federica, Carafa, Vincenzo, Cosconati, Sandro, Di Maro, Salvatore, Ciuffreda, Loreta, De Angelis, Antonella, Stiuso, Paola, Feoli, Alessandra, Sbardella, Gianluca, Altucci, Lucia, and Nebbioso, Angela

Subjects

0301 basic medicine, Senescence, Cancer Research, senescence, epigenetic modulator, Class iii, Biology, drug discovery, Epigenesis, Genetic, Small Molecule Libraries, Fight-or-flight response, 03 medical and health sciences, 0302 clinical medicine, Sirtuin 1, Stress, Physiological, Sirtuin, Sirtuins, Animals, Humans, Molecular Biology, Cellular Senescence, chemistry.chemical_classification, epigenetic modulators, Binding Sites, Drug discovery, Substrate (chemistry), stress response, Hep G2 Cells, Rats, Cell biology, Histone Deacetylase Inhibitors, Molecular Docking Simulation, 030104 developmental biology, Histone, Enzyme, chemistry, 030220 oncology & carcinogenesis, biology.protein, NAD+ kinase, Caco-2 Cells, Research Article, Research Paper, Protein Binding

Abstract

SIRT1, a NAD+-dependent deacetylase, is the most well-studied member of class III histone deacetylases. Due to its wide range of activities and substrate targets, this enzyme has emerged as a major regulator of different physiological processes. However, SIRT1-mediated alterations are also implicated in the pathogenesis of several conditions, including metabolic and neurodegenerative disorders, and cancer. Current evidence highlights the potential role of SIRT1 as an attractive therapeutic target for disease prevention and treatment strategies, thus propelling the development of new pharmacological agents. By high-throughput screening of a large library of compounds, we identified SCIC2 as an effective SIRT1 activator. This small molecule showed enzymatic activity of 135.8% at 10μM, an AC50 value of 50±1.8µM, and bound SIRT1 with a KD of 26.4±0.6μM. In order to potentiate its SIRT1-activating ability, SCIC2 was subjected to modelling studies, leading to the identification of a more potent derivative, SCIC2.1. SCIC2.1 displayed higher SIRT1 activity (175%; AC50=36.83±2.23µM), stronger binding to SIRT1, and greater cell permeability than SCIC2. At cellular level, both molecules did not alter the cell cycle progression of cancer cells and normal cells, and were able to strengthen SIRT1-mediated effects in stress response. Finally, SCIC2 and SCIC2.1 attenuated induction of senescence by reducing senescence-associated β-galactosidase activity. Our findings warrant further investigation of these two novel SIRT1 activators in in vivo and human studies. SIRT1, a NAD+-dependent deacetylase, is the most well-studied member of class III histone deacetylases. Due to its wide range of activities and substrate targets, this enzyme has emerged as a major regulator of different physiological processes. However, SIRT1-mediated alterations are also implicated in the pathogenesis of several conditions, including metabolic and neurodegenerative disorders, and cancer. Current evidence highlights the potential role of SIRT1 as an attractive therapeutic target for disease prevention and treatment strategies, thus propelling the development of new pharmacological agents. By high-throughput screening of a large library of compounds, we identified SCIC2 as an effective SIRT1 activator. This small molecule showed enzymatic activity of 135.8% at 10μM, an AC50 value of 50±1.8µM, and bound SIRT1 with a KD of 26.4±0.6μM. In order to potentiate its SIRT1-activating ability, SCIC2 was subjected to modelling studies, leading to the identification of a more potent derivative, SCIC2.1. SCIC2.1 displayed higher SIRT1 activity (175%; AC50=36.83±2.23µM), stronger binding to SIRT1, and greater cell permeability than SCIC2. At cellular level, both molecules did not alter the cell cycle progression of cancer cells and normal cells, and were able to strengthen SIRT1-mediated effects in stress response. Finally, SCIC2 and SCIC2.1 attenuated induction of senescence by reducing senescence-associated β-galactosidase activity. Our findings warrant further investigation of these two novel SIRT1 activators in in vivo and human studies.

Published

2020

42. The Pan-Sirtuin Inhibitor MC2494 Regulates Mitochondrial Function in a Leukemia Cell Line

Author

Gilda Cobellis, Marzia Di Donato, Giulia Sgueglia, Dante Rotili, Antonello Mai, Laura Della Torre, Vincenzo Carafa, Angela Nebbioso, Angela Chambery, Carmela Dell'Aversana, Rosita Russo, Federica Sarno, Francesca Cuomo, Lucia Altucci, Carafa, V, Russo, R, Della Torre, L, Cuomo, F, Dell'Aversana, C, Sarno, F, Sgueglia, G, Di Donato, M, Rotili, D, Mai, A, Nebbioso, A, Cobellis, G, Chambery, A, Altucci, L, Carafa, Vincenzo, Russo, Rosita, Della Torre, Laura, Cuomo, Francesca, Dell'Aversana, Carmela, Sarno, Federica, Sgueglia, Giulia, Di Donato, Marzia, Rotili, Dante, Mai, Antonello, Nebbioso, Angela, Cobellis, Gilda, Chambery, Angela, and Altucci, Lucia

Subjects

0301 basic medicine, Cancer Research, Mitochondrion, lcsh:RC254-282, energy production, 03 medical and health sciences, 0302 clinical medicine, sirtuins, Organelle, medicine, cancer, epigenetic, leukemia, mitochondria, proteomic analysis, Epigenetics, cancer, leukemia, Original Research, ATP synthase, biology, proteomic analysi, Cancer, medicine.disease, lcsh:Neoplasms. Tumors. Oncology. Including cancer and carcinogens, Cell biology, 030104 developmental biology, Oncology, Mitochondrial biogenesis, 030220 oncology & carcinogenesis, Sirtuin, biology.protein, Function (biology)

Abstract

The involvement of sirtuins (SIRTs) in modulating metabolic and stress response pathways is attracting growing scientific interest. Some SIRT family members are located in mitochondria, dynamic organelles that perform several crucial functions essential for eukaryotic life. Mitochondrial dysfunction has emerged as having a key role in a number of human diseases, including cancer. Here, we investigated mitochondrial damage resulting from treatment with a recently characterized pan-SIRT inhibitor, MC2494. MC2494 was able to block mitochondrial biogenesis and function in terms of ATP synthesis and energy metabolism, suggesting that it might orchestrate cell response to metabolic stress and thereby interfere with cancer promotion and progression. Targeting mitochondrial function could thus be considered a potential anticancer strategy for use in clinical therapy.

Published

2020

43. Recent insights into Histone Acetyltransferase-1: biological function and involvement in pathogenesis

Author

Hendrik G. Stunnenberg, Lucia Altucci, Joost H.A. Martens, Angela Nebbioso, Angelita Poziello, Vincenzo Carafa, Poziello, Angelita, Nebbioso, Angela, Stunnenberg, Hendrik G, Martens, Joost H A, Carafa, Vincenzo, and Altucci, Lucia

Subjects

0301 basic medicine, Cancer Research, Histone Acetyltransferase-1, Review, Biology, Histone H4, Histones, 03 medical and health sciences, 0302 clinical medicine, Gene expression, Epigenetics, Molecular Biology, HAT1 inhibitor, Histone Acetyltransferases, acetylation, histones H3-H4, Histone acetyltransferase, DNA Methylation, Chromatin, Cell biology, 030104 developmental biology, Histone, Acetylation, 030220 oncology & carcinogenesis, biology.protein, HAT1, epigenetic

Abstract

Acetylation of histone and non-histone proteins is a post-translational modification mostly associated with activation of gene transcription. The first histone acetyltransferase (HAT) identified as modifying newly synthesized histone H4 in yeast was a type B HAT named HAT1. Although it was the first HAT to be discovered, HAT1 remains one of the most poorly studied enzymes in its class. In addition to its well-established role in the cytoplasm, recent findings have revealed new and intriguing aspects of the function of HAT1 in the nucleus. Several studies have described its involvement in regulating different pathways associated with a wide range of diseases, including cancer. This review focuses on our current understanding of HAT1, highlighting its importance in regulating chromatin replication and gene expression. This previously unknown role for HAT1 opens up novel scenarios in which further studies will be required to better understand its function.

Published

2020

44. Comparative phytochemical characterization, genetic profile, and antiproliferative activity of polyphenol-rich extracts from pigmented tubers of different solanum tuberosum varieties

Author

Luigi De Masi, Paola Stiuso, Paola Bontempo, Vincenzo Carafa, Paola Montoro, Riccardo Aversano, Daniela Rigano, Domenico Carputo, Lucia Altucci, Angela Nebbioso, Sonia Piacente, Vincenzo D'Amelia, De Masi, L., Bontempo, P., Rigano, D., Stiuso, P., Carafa, V., Nebbioso, A., Piacente, S., Montoro, P., Aversano, R., D'Amelia, V., Carputo, D., and Altucci, L.

Subjects

0106 biological sciences, Pigmented potatoes, Phytochemicals, Pharmaceutical Science, Bioactive molecules, Apoptosis, Tandem mass spectrometry, 01 natural sciences, Analytical Chemistry, chemistry.chemical_compound, Bioactive molecule, Phytogenic, Drug Discovery, Genotype, 0303 health sciences, Tumor, Electrospray Ionization, food and beverages, Genetic Profile, Plant Tubers, Leukemia cell, Biochemistry, Phytochemical, Chemistry (miscellaneous), Molecular Medicine, Potato genotyping, animal structures, Electrospray ionization, Pigmented potatoe, Antineoplastic Agents, Biology, Cell Line, lcsh:QD241-441, 03 medical and health sciences, lcsh:Organic chemistry, Cell cycle modulation, Humans, Physical and Theoretical Chemistry, Potato tuber extract, Transcription factor, 030304 developmental biology, Solanum tuberosum, Plant Extracts, Spectrometry, Organic Chemistry, fungi, Polyphenols, Mass, chemistry, Polyphenol, Leukemia cells, Antineoplastic Agents, Phytogenic, Cell Line, Tumor, Spectrometry, Mass, Electrospray Ionization, DNA, 010606 plant biology & botany

Abstract

Plants produce a vast array of biomolecules with beneficial effects for human health. In this study, polyphenol and anthocyanin-rich extracts (PAE) from pigmented tubers of Solanum tuberosum L. varieties &ldquo, Blue Star&rdquo, &ldquo, Magenta Love&rdquo, and &ldquo, Double Fun&rdquo, in comparison with the more extensively studied &ldquo, Vitelotte&rdquo, were evaluated and compared for antiproliferative effects in human leukemia cells, and their phytochemical and genetic profiles were determined. In U937 cells, upon treatment with PAE, it was possible to reveal the expression of specific apoptotic players, such as caspase 8, 9, 3, and poly (ADP-ribose) polymerase (PARP), as well as the induction of monocyte and granulocyte differentiation. A liquid chromatography/electrospray ionization tandem mass spectrometry (LC-ESI-MS/MS) investigation revealed the presence of polyphenolic compounds in all the varieties of potatoes analyzed, among which caffeoyl and feruloyl quinic acid derivatives were the most abundant, as well as several acylated anthocyanins. Each pigmented variety was genotyped by DNA-based molecular markers, and flavonoid-related transcription factors were profiled in tubers in order to better characterize these outstanding resources and contribute to their exploitation in breeding. Interesting biological activities were observed for &ldquo, varieties with respect to the minor or no effect of the &ldquo, variety.

Published

2020

45. Deregulation of cell death in cancer: Recent highlights

Author

Vincenzo Carafa, Lucia Altucci, Carafa, V., and Altucci, L.

Subjects

0301 basic medicine, cell death, cancer, Cancer Research, Programmed cell death, business.industry, Cancer, medicine.disease, medicine.disease_cause, lcsh:Neoplasms. Tumors. Oncology. Including cancer and carcinogens, lcsh:RC254-282, 03 medical and health sciences, Deregulation, 030104 developmental biology, 0302 clinical medicine, n/a, Editorial, Oncology, 030220 oncology & carcinogenesis, medicine, Cancer research, otorhinolaryngologic diseases, Carcinogenesis, business

Abstract

The aim of this Special Issue on the deregulation of cell death in cancer is to bring together recent perspectives on the relationship between tumorigenesis and programmed cell death (PCD) [...]

Published

2020

46. Combined HAT/EZH2 modulation leads to cancer-selective cell death

Author

Valeria Cicatiello, Alfonso Baldi, Eva M. Janssen-Megens, Simon Heath, Olivier A. Bernard, Mariarosaria Conte, Edo Vellenga, Gianluca Sbardella, Alessandra Feoli, Antonello Mai, Francesca Petraglia, Concetta Ingenito, Bowon Kim, Valeria Belsito Petrizzi, Guoqiang Yi, Stefano Tomassi, Abhishek Singh, Angela Nebbioso, Ivo Gut, Paul Flicek, Albertus T. J. Wierenga, Marie-Laure Yaspo, Joost H.A. Martens, Hendrik G. Stunnenberg, Ivana Apicella, Lucia Scisciola, Sergio Valente, Ettore Novellino, Véronique Della Valle, Menotti Ruvo, Sandro De Falco, Amit Mandoli, Colin Logie, Vincenzo Carafa, Lucia Altucci, Università degli studi della Campania 'Luigi Vanvitelli', Radboud university [Nijmegen], Institut de Recherche Vétérinaire de Tunisie (IRVT), Università degli Studi di Roma 'La Sapienza' = Sapienza University [Rome], Ospedale Umberto I, Istituto di Biofisica e Genetica 'Adriano Buzzati Traverso', Consiglio Nazionale delle Ricerche (CNR), Centro Nacional de Analisis Genomico [Barcelona] (CNAG), CNR – Istituto di Biostrutture e Bioimmagini, University Medical Center Groningen [Groningen] (UMCG), European Bioinformatics Institute [Hinxton] (EMBL-EBI), EMBL Heidelberg, Max Planck Institute for Molecular Genetics (MPIMG), Max-Planck-Gesellschaft, Hématopoïèse normale et pathologique (U1170 Inserm), Institut National de la Santé et de la Recherche Médicale (INSERM)-Université Paris-Sud - Paris 11 (UP11)-Institut Gustave Roussy (IGR), Department of Medicinal Chemistry and Technologies, Institut Pasteur, Fondation Cenci Bolognetti - Istituto Pasteur Italia, Fondazione Cenci Bolognetti, Réseau International des Instituts Pasteur (RIIP)-Réseau International des Instituts Pasteur (RIIP)-Università degli Studi di Roma 'La Sapienza' = Sapienza University [Rome], Università degli studi di Napoli Federico II, Università degli Studi di Salerno (UNISA), Centro Nacional de Análisi Genómico (CNAG), Centro Nacional de Análisis Genómico, This work was supported by BLUEPRINT (282510), Programma VALERE: Vanvitelli per la Ricerca, the Italian-Flag Project-EPIGEN, PRIN-20152TE5PK, the Italian association against cancer (AIRC-17217), the Dutch Cancer Foundation (KWF kun 2011–4937) and Netherlands organization for Scientific Research (NWO-VIDI)., Petraglia, Francesca, Singh, Abhishek A., Carafa, Vincenzo, Nebbioso, Angela, Conte, Mariarosaria, Scisciola, Lucia, Valente, Sergio, Baldi, Alfonso, Mandoli, Amit, Petrizzi, Valeria Belsito, Ingenito, Concetta, De Falco, Sandro, Cicatiello, Valeria, Apicella, Ivana, Janssen-Megens, Eva M., Kim, Bowon, Yi, Guoqiang, Logie, Colin, Heath, Simon, Ruvo, Menotti, Wierenga, Albertus T. J., Flicek, Paul, Yaspo, Marie Laure, Della Valle, Veronique, Bernard, Olivier, Tomassi, Stefano, Novellino, Ettore, Feoli, Alessandra, Sbardella, Gianluca, Gut, Ivo, Vellenga, Edo, Stunnenberg, Hendrik G., Mai, Antonello, Martens, Joost H. A., Altucci, Lucia, Guided Treatment in Optimal Selected Cancer Patients (GUTS), and Stem Cell Aging Leukemia and Lymphoma (SALL)

Subjects

0301 basic medicine, acetylation, apoptosis, cancer, epigenetics, methylation, oncology, Programmed cell death, [SDV.CAN]Life Sciences [q-bio]/Cancer, 03 medical and health sciences, In vivo, medicine, Molecular Biology, business.industry, Cancer, Epigenetics, Apoptosis, Acetylation, Methylation, EZH2, Apoptosi, Epigenetic, Epigenome, medicine.disease, 3. Good health, Leukemia, 030104 developmental biology, Oncology, Cancer research, business, Ex vivo, Research Paper

Abstract

Contains fulltext : 197351.pdf (Publisher’s version ) (Open Access) Epigenetic alterations have been associated with both pathogenesis and progression of cancer. By screening of library compounds, we identified a novel hybrid epi-drug MC2884, a HAT/EZH2 inhibitor, able to induce bona fide cancer-selective cell death in both solid and hematological cancers in vitro, ex vivo and in vivo xenograft models. Anticancer action was due to an epigenome modulation by H3K27me3, H3K27ac, H3K9/14ac decrease, and to caspase-dependent apoptosis induction. MC2884 triggered mitochondrial pathway apoptosis by up-regulation of cleaved-BID, and strong down-regulation of BCL2. Even aggressive models of cancer, such as p53(-/-) or TET2(-/-) cells, responded to MC2884, suggesting MC2884 therapeutic potential also for the therapy of TP53 or TET2-deficient human cancers. MC2884 induced massive apoptosis in ex vivo human primary leukemia blasts with poor prognosis in vivo, by targeting BCL2 expression. MC2884-treatment reduced acetylation of the BCL2 promoter at higher level than combined p300 and EZH2 inhibition. This suggests a key role for BCL-2 reduction in potentiating responsiveness, also in combination therapy with BCL2 inhibitors. Finally, we identified both the mechanism of MC2884 action as well as a potential therapeutic scheme of its use. Altogether, this provides proof of concept for the use of epi-drugs coupled with epigenome analyses to 'personalize' precision medicine.

Published

2018

47. c-Myc modulation & acetylation is a key HDAC inhibitor target in cancer

Author

Ciro Abbondanza, Mariarosaria Conte, Angela Nebbioso, Vincenzo Carafa, Lucia Altucci, Gabriella Lania, Valeria Belsito Petrizzi, Francesco Iovino, Francesco Paolo Tambaro, Hendrik G. Stunnenberg, Concetta Ingenito, Isabella Pallavicini, Rosaria Benedetti, Matthias Nees, Guillermo Garcia-Manero, Joost H.A. Martens, Saverio Minucci, Nebbioso, Angela, Carafa, Vincenzo, Conte, Mariarosaria, Tambaro, Francesco Paolo, Abbondanza, Ciro, Martens, Joost H. A, Nees, Matthia, Benedetti, Rosaria, Pallavicini, Isabella, Minucci, Saverio, Garcia Manero, G, Iovino, Francesco, Lania, Gabriella, Ingenito, Concetta, Belsito Petrizzi, Valeria, Stunnenberg, Hendrik G, and Altucci, Lucia

Subjects

0301 basic medicine, Cancer Research, Sp1 Transcription Factor, Kruppel-Like Transcription Factors, Histone Deacetylase 1, Proto-Oncogene Proteins c-myc, TNF-Related Apoptosis-Inducing Ligand, 03 medical and health sciences, Cell Line, Tumor, Neoplasms, hemic and lymphatic diseases, medicine, Humans, Molecular Biology, Regulation of gene expression, Clinical Trials as Topic, Gene Expression Regulation, Leukemic, business.industry, Myeloid leukemia, Cancer, Acetylation, medicine.disease, c-Myc modulation, 3. Good health, Histone Deacetylase Inhibitors, Leukemia, 030104 developmental biology, Oncology, Apoptosis, Immunology, Cancer cell, Cancer research, Histone deacetylase, business, Ex vivo, Protein Binding, Signal Transduction

Abstract

Histone deacetylase inhibitors (HDACi) are promising anticancer drugs. Although some HDACi have entered the clinic, the mechanism(s) underlying their tumor selectivity are poorly understood. Experimental Design/Results: Using gene expression analysis, we define a core set of 6 genes commonly regulated in acute myeloid leukemia (AML) blasts and cell lines. c-Myc, the most prominently modulated, is preferentially altered in leukemia. Upon HDACi treatment, c-Myc is acetylated at lysine 323 and its expression decreases, leading to TRAIL activation and apoptosis. c-Myc binds to the TRAIL promoter on the proximal GC box through Sp1 or Miz1, impairing TRAIL activation. HDACi exposure triggers TRAIL expression, altering c-Myc-TRAIL binding. These events do not occur in normal cells. Excitingly, this inverse correlation between TRAIL and c-Myc is supported by HDACi treatment ex vivo of AML blasts and primary human breast cancer cells. The predictive value of c-Myc to HDACi responsiveness is confirmed in vivo in AML patients undergoing HDACi-based clinical trials. Purpose: Histone deacetylase inhibitors (HDACi) are promising anticancer drugs. Although some HDACi have entered the clinic, the mechanism(s) underlying their tumor selectivity are poorly understood. Experimental Design and Results: Using gene expression analysis, we define a core set of six genes commonly regulated in acute myeloid leukemia (AML) blasts and cell lines. MYC, the most prominently modulated, is preferentially altered in leukemia. Upon HDACi treatment, c-Myc is acetylated at lysine 323 and its expression decreases, leading to TRAIL activation and apoptosis. c-Myc binds to the TRAIL promoter on the proximal GC box through SP1 or MIZ1, impairing TRAIL activation. HDACi exposure triggers TRAIL expression, altering c-Myc-TRAIL binding. These events do not occur in normal cells. Excitingly, this inverse correlation between TRAIL and c-Myc is supported by HDACi treatment ex vivo of AML blasts and primary human breast cancer cells. The predictive value of c-Myc to HDACi responsiveness is confirmed in vivo in AML patients undergoing HDACi-based clinical trials. Conclusions: Collectively, our findings identify a key role for c-Myc in TRAIL deregulation and as a biomarker of the anticancer action of HDACi in AML. The potential improved patient stratification could pave the way toward personalized therapies.

Published

2017

48. Effect of the Sirtuin Inhibitor MC2494 on RIPK1 Expression

Author

Laura Della Torre, Angelita Poziello, Federica Sarno, Alessandro Paiardini, Antonello Mai, Dante Rotili, Angela Nebbioso, Lucia Altucci, Vincenzo Carafa, Della Torre, Laura, Poziello, Angelita, Sarno, Federica, Paiardini, Alessandro, Mai, Antonello, Rotili, Dante, Nebbioso, Angela, Altucci, Lucia, and Carafa, Vincenzo

Subjects

RIPK1, Programmed cell death, biology, Chemistry, Necroptosis, Sirtuin, otorhinolaryngologic diseases, biology.protein, Cellular homeostasis, General Medicine, Animal development, Metabolism, Cell biology

Abstract

Programmed cell death (PCD) is a fundamental process involved in animal development and in maintaining cellular homeostasis...

Published

2019

49. Comparative Phytochemical Characterization, Genetic Profile, and Antiproliferative Activity of Polyphenol-Rich Extracts from Pigmented Tubers of Different

Author

Luigi, De Masi, Paola, Bontempo, Daniela, Rigano, Paola, Stiuso, Vincenzo, Carafa, Angela, Nebbioso, Sonia, Piacente, Paola, Montoro, Riccardo, Aversano, Vincenzo, D'Amelia, Domenico, Carputo, and Lucia, Altucci

Subjects

Spectrometry, Mass, Electrospray Ionization, potato tuber extract, pigmented potatoes, Genotype, Plant Extracts, potato genotyping, fungi, Phytochemicals, leukemia cells, food and beverages, Polyphenols, Apoptosis, Genetic Profile, Antineoplastic Agents, Phytogenic, Article, Plant Tubers, Cell Line, Tumor, bioactive molecules, cell cycle modulation, Humans, Solanum tuberosum

Abstract

Plants produce a vast array of biomolecules with beneficial effects for human health. In this study, polyphenol and anthocyanin-rich extracts (PAE) from pigmented tubers of Solanum tuberosum L. varieties “Blue Star”, “Magenta Love”, and “Double Fun” in comparison with the more extensively studied “Vitelotte” were evaluated and compared for antiproliferative effects in human leukemia cells, and their phytochemical and genetic profiles were determined. In U937 cells, upon treatment with PAE, it was possible to reveal the expression of specific apoptotic players, such as caspase 8, 9, 3, and poly (ADP-ribose) polymerase (PARP), as well as the induction of monocyte and granulocyte differentiation. A liquid chromatography/electrospray ionization tandem mass spectrometry (LC-ESI-MS/MS) investigation revealed the presence of polyphenolic compounds in all the varieties of potatoes analyzed, among which caffeoyl and feruloyl quinic acid derivatives were the most abundant, as well as several acylated anthocyanins. Each pigmented variety was genotyped by DNA-based molecular markers, and flavonoid-related transcription factors were profiled in tubers in order to better characterize these outstanding resources and contribute to their exploitation in breeding. Interesting biological activities were observed for “Blue Star” and “Vitelotte” varieties with respect to the minor or no effect of the “Double Fun” variety.

Published

2019

50. Dual Tumor Suppressor and Tumor Promoter Action of Sirtuins in Determining Malignant Phenotype

Author

Vincenzo Carafa, Lucia Altucci, Angela Nebbioso, Carafa, Vincenzo, Altucci, Lucia, and Nebbioso, Angela

Subjects

0301 basic medicine, Programmed cell death, Context (language use), Review, Metastasis, law.invention, 03 medical and health sciences, 0302 clinical medicine, law, medicine, Sirtuin, Sirtuins, cancer, Pharmacology (medical), Epigenetics, Pharmacology, epigenetics, biology, lcsh:RM1-950, EMT, Cancer, medicine.disease, 3. Good health, lcsh:Therapeutics. Pharmacology, 030104 developmental biology, Histone, 030220 oncology & carcinogenesis, biology.protein, Cancer research, cancer therapy, Suppressor

Abstract

Sirtuins, class III histone deacetylases, are differentially expressed in several human cancers, where they display both oncogenic and tumor-suppressive properties depending on cellular context and experimental conditions. Sirtuins are involved in many important biological processes and play a critical role in cancer initiation, promotion and progression. A growing body of evidence indicates the involvement of sirtuins in regulating three important tumor processes: epithelial-to-mesenchymal transition (EMT), invasion and metastasis. Many sirtuins are responsible for cellular metabolic reprogramming and drug resistance by inactivating cell death pathways and promoting uncontrolled proliferation. In this review, we summarize current knowledge on the role of sirtuins in cancer and discuss their puzzling dual function as tumor suppressors and tumor promoters, important for the future development of novel tailored sirtuin-based cancer therapies.

Published

2019