Your search keyword '"Vescovi A. L."' showing total 11 results

1. Generation of induced pluripotent stem cells (CSSi017-A)(12862) from an ALS patient carrying a repeat expansion in the C9orf72 gene

Author

Ruotolo, G, D'Anzi, A, Casamassa, A, Mazzoni, M, Ferrari, D, Lombardi, I, Carletti, R, D'Asdia, C, Torrente, I, Frezza, K, Lattante, S, Sabatelli, M, Pennuto, M, Vescovi, A, Rosati, J, Ruotolo, G., D'Anzi, A., Casamassa, A., Mazzoni, M., Ferrari, D., Lombardi, I., Carletti, R. M., D'Asdia, C., Torrente, I., Frezza, K., Lattante, S., Sabatelli, M., Pennuto, M., Vescovi, A. L., Rosati, J., Ruotolo, G, D'Anzi, A, Casamassa, A, Mazzoni, M, Ferrari, D, Lombardi, I, Carletti, R, D'Asdia, C, Torrente, I, Frezza, K, Lattante, S, Sabatelli, M, Pennuto, M, Vescovi, A, Rosati, J, Ruotolo, G., D'Anzi, A., Casamassa, A., Mazzoni, M., Ferrari, D., Lombardi, I., Carletti, R. M., D'Asdia, C., Torrente, I., Frezza, K., Lattante, S., Sabatelli, M., Pennuto, M., Vescovi, A. L., and Rosati, J.

Abstract

Genetic expansions of the hexanucleotide repeats (GGGGCC) in the C9orf72 gene appear in approximately 40% of patients with familial ALS and 7% of patients with sporadic ALS in the European population, making this mutation one of the most prevalent genetic mutations in ALS. Here, we generated a human induced pluripotent stem cell (hiPSC) line from the dermal fibroblasts of a patient carrying a 56-repeat expansion in an ALS disease-causing allele of C9orf72. These iPSCs showed stable amplification in vitro with normal karyotype and high expression of pluripotent markers and differentiated spontaneously in vivo into three germ layers.

Published

2024

2. Stemness underpinning all steps of human colorectal cancer defines the core of effective therapeutic strategies

Author

Visioli, Alberto, Giani, Fabrizio, Trivieri, Nadia, Pracella, Riccardo, Miccinilli, Elide, Cariglia, Maria Grazia, Palumbo, Orazio, Arleo, Andrea, Dezi, Fabio, Copetti, Massimiliano, Cajola, Laura, Restelli, Silvia, Papa, Valerio, Sciuto, Antonio, Latiano, Tiziana Pia, Carella, Massimo, Amadori, Dino, Gallerani, Giulia, Ricci, Riccardo, Alfieri, Sergio, Pesole, Graziano, Vescovi, Angelo L., and Binda, Elena

Published

2019

3. Generation of an induced pluripotent stem cell line (CSS012-A (7672)) carrying the p.G376D heterozygous mutation in the TARDBP protein

Author

D'Anzi, A., Altieri, F., Perciballi, E., Ferrari, D., Torres, B., Bernardini, L., Lattante, Serena, Sabatelli, Mario, Vescovi, A. L., Rosati, J., Lattante S. (ORCID:0000-0003-2891-0340), Sabatelli M. (ORCID:0000-0001-6635-4985), D'Anzi, A., Altieri, F., Perciballi, E., Ferrari, D., Torres, B., Bernardini, L., Lattante, Serena, Sabatelli, Mario, Vescovi, A. L., Rosati, J., Lattante S. (ORCID:0000-0003-2891-0340), and Sabatelli M. (ORCID:0000-0001-6635-4985)

Abstract

Amyotrophic lateral sclerosis (ALS) is an incurable neurodegenerative condition with phenotypic and genetic heterogeneity. It is characterized by the selective vulnerability and the progressive loss of the neural population. Here, an induced pluripotent stem cell (iPSC) line was generated from dermal fibroblasts of an individual carrying the p.G376D mutation in the TDP-43 protein. Fibroblasts were reprogrammed using non-integrating episomal plasmids. There were no karyotype abnormalities, and iPSCs successfully differentiated into all three germ layers. This cell line may prove useful in the study of the pathogenic mechanisms that underpin ALS syndrome.

Published

2021

4. Generation of an induced pluripotent stem cell line (CSS012-A (7672)) carrying the p.G376D heterozygous mutation in the TARDBP protein

Author

D'Anzi, A, Altieri, F, Perciballi, E, Ferrari, D, Torres, B, Bernardini, L, Lattante, S, Sabatelli, M, Vescovi, A, Rosati, J, D'Anzi A., Altieri F., Perciballi E., Ferrari D., Torres B., Bernardini L., Lattante S., Sabatelli M., Vescovi A. L., Rosati J., D'Anzi, A, Altieri, F, Perciballi, E, Ferrari, D, Torres, B, Bernardini, L, Lattante, S, Sabatelli, M, Vescovi, A, Rosati, J, D'Anzi A., Altieri F., Perciballi E., Ferrari D., Torres B., Bernardini L., Lattante S., Sabatelli M., Vescovi A. L., and Rosati J.

Abstract

Amyotrophic lateral sclerosis (ALS) is an incurable neurodegenerative condition with phenotypic and genetic heterogeneity. It is characterized by the selective vulnerability and the progressive loss of the neural population. Here, an induced pluripotent stem cell (iPSC) line was generated from dermal fibroblasts of an individual carrying the p.G376D mutation in the TDP-43 protein. Fibroblasts were reprogrammed using non-integrating episomal plasmids. There were no karyotype abnormalities, and iPSCs successfully differentiated into all three germ layers. This cell line may prove useful in the study of the pathogenic mechanisms that underpin ALS syndrome.

Published

2021

5. Mechanisms of pathogenesis of missense mutations on the KDM6A-H3 interaction in type 2 Kabuki Syndrome

Author

Petrizzelli, F, Biagini, T, Barbieri, A, Parca, L, Panzironi, N, Castellana, S, Caputo, V, Vescovi, A, Carella, M, Mazza, T, Petrizzelli F., Biagini T., Barbieri A., Parca L., Panzironi N., Castellana S., Caputo V., Vescovi A. L., Carella M., Mazza T., Petrizzelli, F, Biagini, T, Barbieri, A, Parca, L, Panzironi, N, Castellana, S, Caputo, V, Vescovi, A, Carella, M, Mazza, T, Petrizzelli F., Biagini T., Barbieri A., Parca L., Panzironi N., Castellana S., Caputo V., Vescovi A. L., Carella M., and Mazza T.

Abstract

Mutations in genes encoding for histone methylation proteins are associated with several developmental disorders. Among them, KDM6A is the disease causative gene of type 2 Kabuki Syndrome, a rare multisystem disease. While nonsense mutations and short insertions/deletions are known to trigger pathogenic mechanisms, the functional effects of missense mutations are still uncharacterized. In this study, we demonstrate that a selected set of missense mutations significantly hamper the interaction between KDM6A and the histone H3, by modifying the dynamics of the linker domain, and then causing a loss of function effect.

Published

2020

6. Generation of an induced pluripotent stem cell line, CSSi011-A (6534), from an Amyotrophic lateral sclerosis patient with heterozygous L145F mutation in SOD1 gene

Author

D'Anzi, A, Altieri, F, Perciballi, E, Ferrari, D, Bernardini, L, Goldoni, M, Mazzini, L, De Marchi, F, Di Pierro, A, D'Alfonso, S, Gelati, M, Vescovi, A, Rosati, J, D'Anzi A., Altieri F., Perciballi E., Ferrari D., Bernardini L., Goldoni M., Mazzini L., De Marchi F., Di Pierro A., D'Alfonso S., Gelati M., Vescovi A. L., Rosati J., D'Anzi, A, Altieri, F, Perciballi, E, Ferrari, D, Bernardini, L, Goldoni, M, Mazzini, L, De Marchi, F, Di Pierro, A, D'Alfonso, S, Gelati, M, Vescovi, A, Rosati, J, D'Anzi A., Altieri F., Perciballi E., Ferrari D., Bernardini L., Goldoni M., Mazzini L., De Marchi F., Di Pierro A., D'Alfonso S., Gelati M., Vescovi A. L., and Rosati J.

Abstract

Among the known causative genes of familial ALS, SOD1 mutation is one of the most common. It encodes for the ubiquitous detoxifying copper/zinc binding SOD1 enzyme, whose mutations selectively cause motor neuron death, although the mechanisms are not as yet clear. What is known is that mutant-mediated toxicity is not caused by loss of its detoxifying activity but by a gain-of-function. In order to better understand the pathogenic mechanisms of SOD1 mutation, a human induced pluripotent stem cell (hiPSC) line was generated from the somatic cells of a female patient carrying a missense variation in SOD1 (L145F).

Published

2020

7. Stemness underpinning all steps of human colorectal cancer defines the core of effective therapeutic strategies

Author

Visioli, A, Giani, F, Trivieri, N, Pracella, R, Miccinilli, E, Cariglia, M, Palumbo, O, Arleo, A, Dezi, F, Copetti, M, Cajola, L, Restelli, S, Papa, V, Sciuto, A, Latiano, T, Carella, M, Amadori, D, Gallerani, G, Ricci, R, Alfieri, S, Pesole, G, Vescovi, A, Binda, E, Visioli A., Giani F., Trivieri N., Pracella R., Miccinilli E., Cariglia M. G., Palumbo O., Arleo A., Dezi F., Copetti M., Cajola L., Restelli S., Papa V., Sciuto A., Latiano T. P., Carella M., Amadori D., Gallerani G., Ricci R., Alfieri S., Pesole G., Vescovi A. L., Binda E., Visioli, A, Giani, F, Trivieri, N, Pracella, R, Miccinilli, E, Cariglia, M, Palumbo, O, Arleo, A, Dezi, F, Copetti, M, Cajola, L, Restelli, S, Papa, V, Sciuto, A, Latiano, T, Carella, M, Amadori, D, Gallerani, G, Ricci, R, Alfieri, S, Pesole, G, Vescovi, A, Binda, E, Visioli A., Giani F., Trivieri N., Pracella R., Miccinilli E., Cariglia M. G., Palumbo O., Arleo A., Dezi F., Copetti M., Cajola L., Restelli S., Papa V., Sciuto A., Latiano T. P., Carella M., Amadori D., Gallerani G., Ricci R., Alfieri S., Pesole G., Vescovi A. L., and Binda E.

Abstract

Background: Despite their lethality and ensuing clinical and therapeutic relevance, circulating tumor cells (CTCs) from colorectal carcinoma (CRC) remain elusive, poorly characterized biological entities. Methods and findings: We perfected a cell system of stable, primary lines from human CRC showing that they possess the full complement of ex- and in-vivo, in xenogeneic models, characteristics of CRC stem cells (CCSCs). Here we show how tumor-initiating, CCSCs cells can establish faithful orthotopic phenocopies of the original disease, which contain cells that spread into the circulatory system. While in the vascular bed, these cells retain stemness, thus qualifying as circulating CCSCs (cCCSCs). This is followed by the establishment of lesions in distant organs, which also contain resident metastatic CCSCs (mCCSCs). Interpretation: Our results support the concept that throughout all the stages of CRC, stemness is retained as a continuous property by some of their tumor cells. Importantly, we describe a useful standardized model that can enable isolation and stable perpetuation of human CRC's CCSCs, cCCSCs and mCCSCs, providing a useful platform for studies of CRC initiation and progression that is suitable for the discovery of reliable stage-specific biomarkers and the refinement of new patient-tailored therapies. Fund: This work was financially supported by grants from “Ministero della Salute Italiano”(GR-2011-02351534, RC1703IC36 and RC1803IC35) to Elena Binda and from “Associazione Italiana Cancro” (IG-14368) Angelo L. Vescovi. None of the above funders have any role in study design, data collection, data analysis, interpretation, writing the project.

Published

2019

8. Generation of induced pluripotent stem cell line CSSi008-A (4698) from a patient affected by advanced stage of Dentato-Rubral-Pallidoluysian atrophy (DRPLA)

Author

Bidollari, E, Rotundo, G, Altieri, F, Amicucci, M, Wiquel, D, Ferrari, D, Goldoni, M, Bernardini, L, Consoli, F, De Luca, A, Fanelli, S, Lamorte, G, D'Agruma, L, Vescovi, A, Squitieri, F, Rosati, J, Bidollari E., Rotundo G., Altieri F., Amicucci M., Wiquel D., Ferrari D., Goldoni M., Bernardini L., Consoli F., De Luca A., Fanelli S., Lamorte G., D'Agruma L., Vescovi A. L., Squitieri F., Rosati J., Bidollari, E, Rotundo, G, Altieri, F, Amicucci, M, Wiquel, D, Ferrari, D, Goldoni, M, Bernardini, L, Consoli, F, De Luca, A, Fanelli, S, Lamorte, G, D'Agruma, L, Vescovi, A, Squitieri, F, Rosati, J, Bidollari E., Rotundo G., Altieri F., Amicucci M., Wiquel D., Ferrari D., Goldoni M., Bernardini L., Consoli F., De Luca A., Fanelli S., Lamorte G., D'Agruma L., Vescovi A. L., Squitieri F., and Rosati J.

Abstract

Dentato-Rubral-pallidoluysian atrophy (DRPLA) is a rare autosomal, dominant, progressive neurodegenerative disease that causes involuntary movements, mental and emotional problems. DRPLA is caused by a mutation in the ATN1 gene that encodes for an abnormal polyglutamine stretch in the atrophin-1 protein. DRPLA is most common in the Japanese population, where it has an estimated incidence of 2 to 7 per million people. This condition has also been seen in families from North America and Europe. We obtained a reprogrammed iPSC line from a Caucasian patient with a juvenile onset of the disease, carrying 64 CAG repeat expansion in the ATN1 gene.

Published

2019

9. Production and characterization of human induced pluripotent stem cells (iPSC) CSSi007-A (4383) from Joubert Syndrome

Author

Altieri, F, D'Anzi, A, Martello, F, Tardivo, S, Spasari, I, Ferrari, D, Bernardini, L, Lamorte, G, Mazzoccoli, G, Valente, E, Vescovi, A, Rosati, J, Altieri F., D'Anzi A., Martello F., Tardivo S., Spasari I., Ferrari D., Bernardini L., Lamorte G., Mazzoccoli G., Valente E. M., Vescovi A. L., Rosati J., Altieri, F, D'Anzi, A, Martello, F, Tardivo, S, Spasari, I, Ferrari, D, Bernardini, L, Lamorte, G, Mazzoccoli, G, Valente, E, Vescovi, A, Rosati, J, Altieri F., D'Anzi A., Martello F., Tardivo S., Spasari I., Ferrari D., Bernardini L., Lamorte G., Mazzoccoli G., Valente E. M., Vescovi A. L., and Rosati J.

Abstract

Joubert syndrome (JS) is an autosomal recessive neurodevelopmental disorder, characterized by congenital cerebellar and brainstem defects, belonging to the group of disorders known as ciliopathies, which are caused by mutations in genes encoding proteins of the primary cilium and basal body. Human induced pluripotent stem cells (hiPSCs) from a patient carrying a homozygous missense mutation (c.2168G > A) in AHI1, the first gene to be associated with JS, were produced using a virus-free protocol.

Published

2019

10. Stemness underpinning all steps of human colorectal cancer defines the core of effective therapeutic strategies

Author

Visioli, A., Giani, F., Trivieri, N., Pracella, R., Miccinilli, E., Cariglia, M. G., Palumbo, O., Arleo, A., Dezi, F., Copetti, M., Cajola, L., Restelli, S., Papa, Valerio, Sciuto, A., Latiano, T. P., Carella, M., Amadori, D., Gallerani, G., Ricci, Riccardo, Alfieri, Sergio, Pesole, G., Vescovi, A. L., Binda, E., Papa V. (ORCID:0000-0002-3709-8924), Ricci R. (ORCID:0000-0002-9089-5084), Alfieri S. (ORCID:0000-0002-0404-724X), Visioli, A., Giani, F., Trivieri, N., Pracella, R., Miccinilli, E., Cariglia, M. G., Palumbo, O., Arleo, A., Dezi, F., Copetti, M., Cajola, L., Restelli, S., Papa, Valerio, Sciuto, A., Latiano, T. P., Carella, M., Amadori, D., Gallerani, G., Ricci, Riccardo, Alfieri, Sergio, Pesole, G., Vescovi, A. L., Binda, E., Papa V. (ORCID:0000-0002-3709-8924), Ricci R. (ORCID:0000-0002-9089-5084), and Alfieri S. (ORCID:0000-0002-0404-724X)

Abstract

Background: Despite their lethality and ensuing clinical and therapeutic relevance, circulating tumor cells (CTCs) from colorectal carcinoma (CRC) remain elusive, poorly characterized biological entities. Methods and findings: We perfected a cell system of stable, primary lines from human CRC showing that they possess the full complement of ex- and in-vivo, in xenogeneic models, characteristics of CRC stem cells (CCSCs). Here we show how tumor-initiating, CCSCs cells can establish faithful orthotopic phenocopies of the original disease, which contain cells that spread into the circulatory system. While in the vascular bed, these cells retain stemness, thus qualifying as circulating CCSCs (cCCSCs). This is followed by the establishment of lesions in distant organs, which also contain resident metastatic CCSCs (mCCSCs). Interpretation: Our results support the concept that throughout all the stages of CRC, stemness is retained as a continuous property by some of their tumor cells. Importantly, we describe a useful standardized model that can enable isolation and stable perpetuation of human CRC's CCSCs, cCCSCs and mCCSCs, providing a useful platform for studies of CRC initiation and progression that is suitable for the discovery of reliable stage-specific biomarkers and the refinement of new patient-tailored therapies. Fund: This work was financially supported by grants from “Ministero della Salute Italiano”(GR-2011-02351534, RC1703IC36 and RC1803IC35) to Elena Binda and from “Associazione Italiana Cancro” (IG-14368) Angelo L. Vescovi. None of the above funders have any role in study design, data collection, data analysis, interpretation, writing the project.

Published

2019

11. The EphA2 Receptor Drives Self-Renewal and Tumorigenicity in Stem-like Tumor-Propagating Cells from Human Glioblastomas

Author

Binda, Elena, Visioli, Alberto, Giani, Fabrizio, Lamorte, Giuseppe, Copetti, Massimiliano, Pitter, Ken L., Huse, Jason T., Cajola, Laura, Zanetti, Nadia, DiMeco, Francesco, De Filippis, Lidia, Mangiola, Annunziato, Maira, Giulio, Anile, Carmelo, De Bonis, Pasquale, Reynolds, Brent A., Pasquale, Elena B., and Vescovi, Angelo L.

Subjects

*EPHRIN receptors, *CELL proliferation, *CARCINOGENICITY, *STEM cells, *TUMOR growth, *GLIOBLASTOMA multiforme, *PROTEIN-tyrosine kinases, *GENE expression

Abstract

Summary: In human glioblastomas (hGBMs), tumor-propagating cells with stem-like characteristics (TPCs) represent a key therapeutic target. We found that the EphA2 receptor tyrosine kinase is overexpressed in hGBM TPCs. Cytofluorimetric sorting into EphA2High and EphA2Low populations demonstrated that EphA2 expression correlates with the size and tumor-propagating ability of the TPC pool in hGBMs. Both ephrinA1-Fc, which caused EphA2 downregulation in TPCs, and siRNA-mediated knockdown of EPHA2 expression suppressed TPCs self-renewal ex vivo and intracranial tumorigenicity, pointing to EphA2 downregulation as a causal event in the loss of TPCs tumorigenicity. Infusion of ephrinA1-Fc into intracranial xenografts elicited strong tumor-suppressing effects, suggestive of therapeutic applications. [ABSTRACT FROM AUTHOR]

Published

2012