Your search keyword '"Verginelli, F"' showing total 7 results

1. Allele-specific loss and transcription of the miR-15a/16-1 cluster in chronic lymphocytic leukemia.

Author

Veronese, A, Veronese, A, Pepe, F, Chiacchia, J, Pagotto, S, Lanuti, P, Veschi, S, Di Marco, M, D'Argenio, A, Innocenti, I, Vannata, B, Autore, F, Marchisio, M, Wernicke, D, Verginelli, F, Leone, G, Rassenti, LZ, Kipps, TJ, Mariani-Costantini, R, Laurenti, L, Croce, CM, Visone, R, Veronese, A, Veronese, A, Pepe, F, Chiacchia, J, Pagotto, S, Lanuti, P, Veschi, S, Di Marco, M, D'Argenio, A, Innocenti, I, Vannata, B, Autore, F, Marchisio, M, Wernicke, D, Verginelli, F, Leone, G, Rassenti, LZ, Kipps, TJ, Mariani-Costantini, R, Laurenti, L, Croce, CM, and Visone, R

Abstract

Deregulation of the miR-15a/16-1 cluster has a key role in the pathogenesis of chronic lymphocytic leukemia (CLL), a clinically heterogeneous disease with indolent and aggressive forms. The miR-15a/16-1 locus is located at 13q14, the most frequently deleted region in CLL. Starting from functional investigations of a rare SNP upstream the miR cluster, we identified a novel allele-specific mechanism that exploits a cryptic activator region to recruit the RNA polymerase III for miR-15a/16-1 transcription. This regulation of the miR-15a/16- locus is independent of the DLEU2 host gene, which is often transcribed monoallellically by RPII. We found that normally one allele of miR-15a/16-1 is transcribed by RNAPII, the other one by RNAPIII. In our subset of CLL patients harboring 13q14 deletions, exclusive RNA polymerase III (RPIII)-driven transcription of the miR-15a/16-1 was the consequence of loss of the RPII-regulated allele and correlated with high expression of the poor prognostic marker ZAP70 (P=0.019). Thus, our findings point to a novel biological process, characterized by double allele-specific transcriptional regulation of the miR-15a/16-1 locus by alternative mechanisms. Differential usage of these mechanisms may distinguish at onset aggressive from indolent forms of CLL. This provides a basis for the clinical heterogeneity of the CLL patients carrying 13q14 deletions.

Published

2015

2. Allele-specific loss and transcription of the miR-15a/16-1 cluster in chronic lymphocytic leukemia.

Author

Veronese, A, Veronese, A, Pepe, F, Chiacchia, J, Pagotto, S, Lanuti, P, Veschi, S, Di Marco, M, D'Argenio, A, Innocenti, I, Vannata, B, Autore, F, Marchisio, M, Wernicke, D, Verginelli, F, Leone, G, Rassenti, LZ, Kipps, TJ, Mariani-Costantini, R, Laurenti, L, Croce, CM, Visone, R, Veronese, A, Veronese, A, Pepe, F, Chiacchia, J, Pagotto, S, Lanuti, P, Veschi, S, Di Marco, M, D'Argenio, A, Innocenti, I, Vannata, B, Autore, F, Marchisio, M, Wernicke, D, Verginelli, F, Leone, G, Rassenti, LZ, Kipps, TJ, Mariani-Costantini, R, Laurenti, L, Croce, CM, and Visone, R

Abstract

Deregulation of the miR-15a/16-1 cluster has a key role in the pathogenesis of chronic lymphocytic leukemia (CLL), a clinically heterogeneous disease with indolent and aggressive forms. The miR-15a/16-1 locus is located at 13q14, the most frequently deleted region in CLL. Starting from functional investigations of a rare SNP upstream the miR cluster, we identified a novel allele-specific mechanism that exploits a cryptic activator region to recruit the RNA polymerase III for miR-15a/16-1 transcription. This regulation of the miR-15a/16- locus is independent of the DLEU2 host gene, which is often transcribed monoallellically by RPII. We found that normally one allele of miR-15a/16-1 is transcribed by RNAPII, the other one by RNAPIII. In our subset of CLL patients harboring 13q14 deletions, exclusive RNA polymerase III (RPIII)-driven transcription of the miR-15a/16-1 was the consequence of loss of the RPII-regulated allele and correlated with high expression of the poor prognostic marker ZAP70 (P=0.019). Thus, our findings point to a novel biological process, characterized by double allele-specific transcriptional regulation of the miR-15a/16-1 locus by alternative mechanisms. Differential usage of these mechanisms may distinguish at onset aggressive from indolent forms of CLL. This provides a basis for the clinical heterogeneity of the CLL patients carrying 13q14 deletions.

Published

2015

3. Allele-specific loss and transcription of the miR-15a/16-1 cluster in chronic lymphocytic leukemia.

Author

Veronese, A, Pepe, F, Chiacchia, J, Pagotto, S, Lanuti, P, Veschi, S, Di Marco, M, D'Argenio, A, Innocenti, I, Vannata, B, Autore, Francesco, Marchisio, M, Wernicke, D, Verginelli, F, Leone, G, Rassenti, Lz, Kipps, Tj, Mariani-Costantini, R, Laurenti, Luca, Croce, Cm, Visone, R., Autore F, Laurenti L (ORCID:0000-0002-8327-1396), Veronese, A, Pepe, F, Chiacchia, J, Pagotto, S, Lanuti, P, Veschi, S, Di Marco, M, D'Argenio, A, Innocenti, I, Vannata, B, Autore, Francesco, Marchisio, M, Wernicke, D, Verginelli, F, Leone, G, Rassenti, Lz, Kipps, Tj, Mariani-Costantini, R, Laurenti, Luca, Croce, Cm, Visone, R., Autore F, and Laurenti L (ORCID:0000-0002-8327-1396)

Abstract

X

Published

2015

4. Pharmacological inhibition of EZH2 as a promising differentiation therapy in embryonal RMS

Author

Ciarapica, R., Carcarino, E., Adesso, L., De Salvo, M., Bracaglia, G., Leoncini, P. P., Dall'Agnese, A., Verginelli, F., Milano, G. M., Boldrini, R., Inserra, A., Stifani, S., Screpanti, I., Marquez, V. E., Valente, S., Mai, A., Puri, P. L., Locatelli, Franco, Palacios, Daniela, Rota, R., Locatelli F. (ORCID:0000-0002-7976-3654), Palacios D. (ORCID:0000-0002-2207-2369), Ciarapica, R., Carcarino, E., Adesso, L., De Salvo, M., Bracaglia, G., Leoncini, P. P., Dall'Agnese, A., Verginelli, F., Milano, G. M., Boldrini, R., Inserra, A., Stifani, S., Screpanti, I., Marquez, V. E., Valente, S., Mai, A., Puri, P. L., Locatelli, Franco, Palacios, Daniela, Rota, R., Locatelli F. (ORCID:0000-0002-7976-3654), and Palacios D. (ORCID:0000-0002-2207-2369)

Abstract

Background: Embryonal Rhabdomyosarcoma (RMS) is a pediatric soft-tissue sarcoma derived from myogenic precursors that is characterized by a good prognosis in patients with localized disease. Conversely, metastatic tumors often relapse, leading to a dismal outcome. The histone methyltransferase EZH2 epigenetically suppresses skeletal muscle differentiation by repressing the transcription of myogenic genes. Moreover, de-regulated EZH2 expression has been extensively implied in human cancers. We have previously shown that EZH2 is aberrantly over-expressed in RMS primary tumors and cell lines. Moreover, it has been recently reported that EZH2 silencing in RD cells, a recurrence-derived embryonal RMS cell line, favors myofiber-like structures formation in a pro-differentiation context. Here we evaluate whether similar effects can be obtained also in the presence of growth factor-supplemented medium (GM), that mimics a pro-proliferative microenvironment, and by pharmacological targeting of EZH2 in RD cells and in RD tumor xenografts.Methods: Embryonal RMS RD cells were cultured in GM and silenced for EZH2 or treated with either the S-adenosylhomocysteine hydrolase inhibitor 3-deazaneplanocin A (DZNep) that induces EZH2 degradation, or with a new class of catalytic EZH2 inhibitors, MC1948 and MC1945, which block the catalytic activity of EZH2. RD cell proliferation and myogenic differentiation were evaluated both in vitro and in vivo.Results: Here we show that EZH2 protein was abnormally expressed in 19 out of 19 (100%) embryonal RMS primary tumors and cell lines compared to their normal counterparts. Genetic down-regulation of EZH2 by silencing in GM condition reduced RD cell proliferation up-regulating p21Cip1. It also resulted in myogenic-like differentiation testified by the up-regulation of myogenic markers Myogenin, MCK and MHC. These effects were reverted by enforced over-expression of a murine Ezh2, highlighting an EZH2-specific effect. Pharmacological inhibition o

Published

2014

5. The Polycomb group (PcG) protein EZH2 supports the survival of PAX3-FOXO1 alveolar rhabdomyosarcoma by repressing FBXO32 (Atrogin1/MAFbx)

Author

Ciarapica, R., De Salvo, M., Carcarino, E., Bracaglia, G., Adesso, L., Leoncini, P. P., Dall'Agnese, A., Walters, Z. S., Verginelli, F., De Sio, L., Boldrini, R., Inserra, A., Bisogno, G., Rosolen, A., Alaggio, R., Ferrari, A., Collini, P., Locatelli, M., Stifani, S., Screpanti, I., Rutella, S., Yu, Q., Marquez, V. E., Shipley, J., Valente, S., Mai, A., Miele, L., Puri, P. L., Locatelli, Franco, Palacios, Daniela, Rota, R., Locatelli F. (ORCID:0000-0002-7976-3654), Palacios D. (ORCID:0000-0002-2207-2369), Ciarapica, R., De Salvo, M., Carcarino, E., Bracaglia, G., Adesso, L., Leoncini, P. P., Dall'Agnese, A., Walters, Z. S., Verginelli, F., De Sio, L., Boldrini, R., Inserra, A., Bisogno, G., Rosolen, A., Alaggio, R., Ferrari, A., Collini, P., Locatelli, M., Stifani, S., Screpanti, I., Rutella, S., Yu, Q., Marquez, V. E., Shipley, J., Valente, S., Mai, A., Miele, L., Puri, P. L., Locatelli, Franco, Palacios, Daniela, Rota, R., Locatelli F. (ORCID:0000-0002-7976-3654), and Palacios D. (ORCID:0000-0002-2207-2369)

Abstract

The Polycomb group (PcG) proteins regulate stem cell differentiation via the repression of gene transcription, and their deregulation has been widely implicated in cancer development. The PcG protein Enhancer of Zeste Homolog 2 (EZH2) works as a catalytic subunit of the Polycomb Repressive Complex 2 (PRC2) by methylating lysine 27 on histone H3 (H3K27me3), a hallmark of PRC2-mediated gene repression. In skeletal muscle progenitors, EZH2 prevents an unscheduled differentiation by repressing muscle-specific gene expression and is downregulated during the course of differentiation. In rhabdomyosarcoma (RMS), a pediatric soft-tissue sarcoma thought to arise from myogenic precursors, EZH2 is abnormally expressed and its downregulation in vitro leads to muscle-like differentiation of RMS cells of the embryonal variant. However, the role of EZH2 in the clinically aggressive subgroup of alveolar RMS, characterized by the expression of PAX3-FOXO1 oncoprotein, remains unknown. We show here that EZH2 depletion in these cells leads to programmed cell death. Transcriptional derepression of F-box protein 32 (FBXO32) (Atrogin1/MAFbx), a gene associated with muscle homeostasis, was evidenced in PAX3-FOXO1 RMS cells silenced for EZH2. This phenomenon was associated with reduced EZH2 occupancy and H3K27me3 levels at the FBXO32 promoter. Simultaneous knockdown of FBXO32 and EZH2 in PAX3-FOXO1 RMS cells impaired the pro-apoptotic response, whereas the overexpression of FBXO32 facilitated programmed cell death in EZH2-depleted cells. Pharmacological inhibition of EZH2 by either 3-Deazaneplanocin A or a catalytic EZH2 inhibitor mirrored the phenotypic and molecular effects of EZH2 knockdown in vitro and prevented tumor growth in vivo. Collectively, these results indicate that EZH2 is a key factor in the proliferation and survival of PAX3-FOXO1 alveolar RMS cells working, at least in part, by repressing FBXO32. They also suggest that the reducing activity of EZH2 could represent a novel a

Published

2014

6. Inhibition of Notch3 signalling induces rhabdomyosarcoma cell differentiation promoting p38 phosphorylation and p21(Cip1) expression and hampers tumour cell growth in vitro and in vivo

Author

Raimondi, L, Ciarapica, R, De Salvo, M, Verginelli, Flavia, Gueguen, M, Martini, C, De Sio, L, Cortese, G, Locatelli, M, Dang, T P, Carlesso, N, Miele, Luca, Stifani, S, Limon, I, Locatelli, Franco, Rota, R, Verginelli, F, Miele, L (ORCID:0000-0003-3464-0068), Locatelli, F (ORCID:0000-0002-7976-3654), Raimondi, L, Ciarapica, R, De Salvo, M, Verginelli, Flavia, Gueguen, M, Martini, C, De Sio, L, Cortese, G, Locatelli, M, Dang, T P, Carlesso, N, Miele, Luca, Stifani, S, Limon, I, Locatelli, Franco, Rota, R, Verginelli, F, Miele, L (ORCID:0000-0003-3464-0068), and Locatelli, F (ORCID:0000-0002-7976-3654)

Abstract

Rhabdomyosarcoma (RMS) is a paediatric soft-tissue sarcoma arising from skeletal muscle precursors coexpressing markers of proliferation and differentiation. Inducers of myogenic differentiation suppress RMS tumourigenic phenotype. The Notch target gene HES1 is upregulated in RMS and prevents tumour cell differentiation in a Notch-dependent manner. However, Notch receptors regulating this phenomenon are unknown. In agreement with data in RMS primary tumours, we show here that the Notch3 receptor is overexpressed in RMS cell lines versus normal myoblasts. Notch3-targeted downregulation in RMS cells induces hyper-phosphorylation of p38 and Akt essential for myogenesis, resulting in the differentiation of tumour cells into multinucleated myotubes expressing Myosin Heavy Chain. These phenomena are associated to a marked decrease in HES1 expression, an increase in p21(Cip1) level and the accumulation of RMS cells in the G1 phase. HES1-forced overexpression in RMS cells reverses, at least in part, the pro-differentiative effects of Notch3 downregulation. Notch3 depletion also reduces the tumourigenic potential of RMS cells both in vitro and in vivo. These results indicate that downregulation of Notch3 is sufficient to force RMS cells into completing a correct full myogenic program providing evidence that it contributes, partially through HES1 sustained expression, to their malignant phenotype. Moreover, they suggest Notch3 as a novel potential target in human RMS. Cell Death and Differentiation (2012) 19, 871-881; doi:10.1038/cdd.2011.171; published online 25 November 2011

Published

2012

7. The analysis of variation of mtDNA hypervariable region 1 suggests that Eastern and Western Pygmies diverged before the Bantu expansion

Author

Destro Bisol, G, Coia, Valentina, Boschi, Ilaria, Verginelli, F, Caglià, A, Pascali, Vincenzo Lorenzo, Spedini, G, Calafell, F., Pascali, Vincenzo Lorenzo (ORCID:0000-0001-6520-5224), Destro Bisol, G, Coia, Valentina, Boschi, Ilaria, Verginelli, F, Caglià, A, Pascali, Vincenzo Lorenzo, Spedini, G, Calafell, F., and Pascali, Vincenzo Lorenzo (ORCID:0000-0001-6520-5224)

Abstract

The Eastern Pygmies from Zaire and Western Pygmies from Cameroon, Congo, and the Central African Republic represent the two principal groups of African Pygmies. In the "recent divergence" hypothesis in which Western Pygmies are thought to be the result of hybridization between the ancestors of Eastern Pygmies and Bantu farmers who penetrated the equatorial belt and came into contact with Pygmies around 2-3 kiloyears ago. On the basis of recent archaeological research in the tropical rain forest, we propose a "pre-Bantu divergence" hypothesis, which posits the separation between the ancestors of Eastern and Western Pygmies earlier than 18 kiloyears ago. In order to test the two hypotheses, we analyzed the variation of the hypervariable region 1 of the mitochondrial DNA in the Mbenzele, Western Pygmies of the Central African Republic, and compared our results with those of previous mtDNA and Y chromosome studies. Distribution, sequence variation, and age of haplogroups along with genetic distances among populations, estimates of divergence times, and simulations based on the coalescent approach were found to be congruent with the pre-Bantu divergence but failed to support the recent divergence hypothesis

Published

2004