Your search keyword '"Scarpa, S"' showing total 6 results

1. Exploring the brain tissue proteome of TgCRND8 Alzheimer's Disease model mice under B vitamin deficient diet induced hyperhomocysteinemia by LC-MS top-down platform

Author

Delfino, Daniela, Rossetti, Dv, Martelli, C, Inserra, Ilaria, Vincenzoni, F, Castagnola, Massimo, Urbani, Andrea, Scarpa, S, Fuso, Paola, Cavallaro, Ra, Desiderio, Claudia, Delfino, D, Inserra, I, Castagnola, M (ORCID:0000-0002-0959-7259), Urbani, A (ORCID:0000-0001-9168-3174), Fuso, A, Desiderio, C, Delfino, Daniela, Rossetti, Dv, Martelli, C, Inserra, Ilaria, Vincenzoni, F, Castagnola, Massimo, Urbani, Andrea, Scarpa, S, Fuso, Paola, Cavallaro, Ra, Desiderio, Claudia, Delfino, D, Inserra, I, Castagnola, M (ORCID:0000-0002-0959-7259), Urbani, A (ORCID:0000-0001-9168-3174), Fuso, A, and Desiderio, C

Abstract

The multifactorial nature of Late Onset Alzheimer's Disease (LOAD), the AD form of major relevance on epidemiological and social aspects, has driven the original investigation by LC-MS and top-down proteomics approach of the protein repertoire of the brain tissue of TgCRND8 model mice fed with a diet deficient in B vitamins. The analysis of the acid-soluble fraction of brain tissue homogenates identified a list of proteins and peptides, proteoforms and PTMs. In order to disclose possible modulations, their relative quantification in wild type and AD model mice under both B vitamin deficient and control diets was performed. The levels of metallothionein III, guanine nucleotide-binding protein G(I)/G(S)/G(0) subunit gamma-2 and brain acid soluble protein 1 showed statistically significant alterations depending on genotype, diet or both effects, respectively. Particularly, metallothionein III exhibited increased levels in TgCRND8 mice under B vitamin deficient diet with respect to wild type mice under both diets. Brain acid soluble protein 1 showed the opposite, revealing decreased levels in all diet groups of AD model mice with respect to wild type mice in control diet. Lower levels of brain acid soluble protein 1 were also observed in wild type mice under deficiency of B vitamins. These results, besides contributing to increase the knowledge of AD at molecular level, give new suggestions for deeply investigating metallothionein III and brain acid soluble protein 1 in AD.

Published

2019

2. Infarct-related artery occlusion, tissue markers of ischemia, and increased apoptosis in the peri-infarct viable myocardium.

Author

Abbate, Antonio, Bussani, R, Biondi Zoccai, Giuseppe, Santini, D, Petrolini, A, De Giorgio, Fabio, Vasaturo, F, Scarpa, S, Severino, A, Liuzzo, G, Leone, Antonio Maria, Baldi, F, Sinagra, G, Silvestri, F, Vetrovec, Gw, Crea, Filippo, Biasucci, Luigi Marzio, Baldi, A., De Giorgio, Fabio (ORCID:0000-0002-9447-9707), Liuzzo, G (ORCID:0000-0002-5714-0907), Crea, Filippo (ORCID:0000-0001-9404-8846), Biasucci, Luigi Marzio (ORCID:0000-0002-6921-6497), Abbate, Antonio, Bussani, R, Biondi Zoccai, Giuseppe, Santini, D, Petrolini, A, De Giorgio, Fabio, Vasaturo, F, Scarpa, S, Severino, A, Liuzzo, G, Leone, Antonio Maria, Baldi, F, Sinagra, G, Silvestri, F, Vetrovec, Gw, Crea, Filippo, Biasucci, Luigi Marzio, Baldi, A., De Giorgio, Fabio (ORCID:0000-0002-9447-9707), Liuzzo, G (ORCID:0000-0002-5714-0907), Crea, Filippo (ORCID:0000-0001-9404-8846), and Biasucci, Luigi Marzio (ORCID:0000-0002-6921-6497)

Abstract

AIMS: Unfavourable cardiac remodelling often complicates acute myocardial infarction (AMI) as a result of increased cardiomyocyte apoptosis. It is currently unclear whether ongoing or recurrent ischaemia is an independent determinant for increased apoptosis in peri-infarct viable myocardium. METHODS AND RESULTS: In order to assess the link between infarct-related artery (IRA) occlusion, ischaemia, and apoptosis, 30 subjects dying 7-120 days after AMI (16 with IRA occlusion and 14 with patent IRA) and five control subjects were selected at autopsy. Cardiomyocytes were defined as apoptotic if co-expressing TUNEL and activated caspase-3. Expression of both hypoxia-inducible factor-1 and cyclo-oxygenase-2 was assessed in the peri-infarct myocardium and considered as tissue markers of ischaemia. Evidence of ischaemia was significantly more frequent in cases with IRA occlusion (53%) than in cases with patent IRA (15%) or control hearts (0%, P=0.026). The finding of IRA occlusion and markers of ischaemia identified cases with higher apoptotic rates (ARs) in the peri-infarct viable myocardium [12.2% (8.2-14.0), P<0.001 vs. others], whereas IRA occlusion without ischaemia was associated with lower AR, not significantly different from patent IRA [3.0% (1.0-7.9) vs. 2.2% (1.0-5.8), respectively, P=0.42] CONCLUSION: Ischaemia in the peri-infarct viable myocardium is present in over 50% of subjects dying late after AMI with IRA occlusion, and it is associated with increased apoptosis. Relief of ischaemia after AMI may prove of benefit in preventing apoptosis and its consequences.

Published

2005

3. Increased apoptosis in remote non-infarcted myocardium in multivessel coronary disease

Author

Biondi Zoccai, Giuseppe, Abbate, Antonio, Vasaturo, F, Scarpa, S, Santini, D, Leone, Antonio Maria, Parisi, Q, De Giorgio, Fabio, Bussani, Rossana, Baldi, F, Silvestri, F, Biasucci, Luigi Marzio, Baldi, A., De Giorgio, Fabio (ORCID:0000-0002-9447-9707), Biasucci, Luigi Marzio (ORCID:0000-0002-6921-6497), Biondi Zoccai, Giuseppe, Abbate, Antonio, Vasaturo, F, Scarpa, S, Santini, D, Leone, Antonio Maria, Parisi, Q, De Giorgio, Fabio, Bussani, Rossana, Baldi, F, Silvestri, F, Biasucci, Luigi Marzio, Baldi, A., De Giorgio, Fabio (ORCID:0000-0002-9447-9707), and Biasucci, Luigi Marzio (ORCID:0000-0002-6921-6497)

Abstract

BACKGROUND: Multivessel coronary disease after myocardial infarction is a major risk factor for unfavorable cardiac remodeling and death due to pump failure, but underlying pathophysiologic mechanisms are still uncompletely established. Post-infarction myocardial apoptosis has been recently implicated as a cause of ongoing cell loss leading to cardiac failure. Our aim was to assess the role of post-infarction myocardial apoptosis and pro-apoptotic factor expression in the non-infarcted remote myocardium of subjects with multivessel coronary disease. METHODS: Twenty-one males dying after recent myocardial infarction with permanent occlusion of the infarct-related artery were selected at autopsy. Apoptosis was assessed at viable myocardial regions remote from infarction by co-staining for in situ end-labeling of DNA fragmentation and cleaved caspase-3. Expression of pro-apoptotic factor bax and hypoxia-induced factor-1alpha was evaluated by immunohistochemistry. RESULTS: Subjects with multivessel disease (N=11) showed a significantly two-fold higher myocardial apoptosis in comparison to subjects with single vessel disease (N=10) (0.9% vs. 0.5%, p=0.013). Similarly, myocardial bax expression was increased in patients with multivessel disease (3.0% vs. 1.4%, p=0.029). Stratification for the number of diseased coronary vessels confirmed the association between extent of coronary disease and apoptotic rates (p=0.022). Even in subjects dying over 30 days after infarction multivessel disease remained predictive of enhanced myocardiocyte apoptosis at remote regions (p=0.033). CONCLUSIONS: Post-infarction myocardial apoptosis and bax expression in remote left ventricular regions are significantly increased in male patients with multivessel coronary disease in comparison to those with isolated infarct-related artery occlusion. These findings suggest that apoptotic cell loss in the viable non-infarcted myocardium, possibly due ongoing ischemia, may play a relevant role in the u

Published

2004

4. Surviving acute myocardial infarction: survivin expression in viable cardiomyoctes after infarction

Author

Santini, D, Abbate, Antonio, Scarpa, S, Vasaturo, F, Biondi Zoccai, Giuseppe, Bussani, Rossana, De Giorgio, Fabio, Bassan, F, Camilot, D, Di Marino, Mp, Feroce, F, Baldi, F, Silvestri, Furio, Crea, Filippo, Baldi, A., De Giorgio, Fabio (ORCID:0000-0002-9447-9707), Crea, Filippo (ORCID:0000-0001-9404-8846), Santini, D, Abbate, Antonio, Scarpa, S, Vasaturo, F, Biondi Zoccai, Giuseppe, Bussani, Rossana, De Giorgio, Fabio, Bassan, F, Camilot, D, Di Marino, Mp, Feroce, F, Baldi, F, Silvestri, Furio, Crea, Filippo, Baldi, A., De Giorgio, Fabio (ORCID:0000-0002-9447-9707), and Crea, Filippo (ORCID:0000-0001-9404-8846)

Abstract

BACKGROUND: Apoptosis is a key feature in postinfarction remodelling leading to progressive myocyte loss. Both proapoptotic and antiapoptotic factors contribute to the delicate balance between death and survival. The survivin pathway has emerged as essential in the control of apoptosis, although its role in heart disease is unknown. AIM: To evaluate survivin expression after acute myocardial infarction (AMI). METHODS: Survivin expression was assessed immunohistochemically in the peri-infarct and remote viable myocardium in 17 consecutive patients who died 1-30 weeks after AMI and in four control hearts. RESULTS: Survivin was expressed by myocytes in the peri-infarct area in eight patients and in the remote region in 13 patients. The rate of survivin expression after AMI was significantly higher in the remote versus peri-infarct regions and compared with control hearts. Its expression was inversely associated with the presence of dilated cardiopathy and of apoptosis, independently from the gross pathology infarct size. CONCLUSIONS: Survivin myocardial expression after AMI may be associated with the survival of at risk myocardium and may be indicative of more favourable remodelling after AMI. These findings identify a potential new target for the treatment of postinfarction remodelling.

Published

2004

5. Nicotine regulates basic fibroblastic growth factor and transforming growth factor beta1 production in endothelial cells.

Author

Cucina, A, Corvino, Valentina, Sapienza, P, Borrelli, V, Lucarelli, M, Scarpa, S, Strom, R, Santoro D'Angelo, L, Cavallaro, A., Corvino, Valentina (ORCID:0000-0001-8391-442X), Cucina, A, Corvino, Valentina, Sapienza, P, Borrelli, V, Lucarelli, M, Scarpa, S, Strom, R, Santoro D'Angelo, L, Cavallaro, A., and Corvino, Valentina (ORCID:0000-0001-8391-442X)

Abstract

Nicotine, a constituent of cigarette smoking, may induce atherosclerosis through the production of growth factors. The pattern of bFGF and TGF b1 production and release by bovine aortic endothelial cells (EC) stimulated with nicotine (from 6 3 1024 to 6 3 1028 M) was studied. EC viability and count were assessed. The presence of bFGF and TGF b1 in serum-free conditioned media was determined by the inhibition antibody-binding assay and Western blot analysis. Mitogenic activity of nicotine on EC was also determined. Polymerase chain reaction (PCR) was used to study the expression of bFGF and TGF b1. The bFGF release after nicotine stimulation was greater than controls, whereas TGF b1 release was lower. At a nicotine concentration of 6 3 1026 Mwe noted the greatest mitogenic activity. The addition of monoclonal antibody anti-bFGF decreased the tritiated thymidine uptake of EC exposed to nicotine but the addition of monoclonal antibody anti-TGF b1 had no significant effect. bFGF mRNA expression was significantly higher in EC exposed to nicotine than in controls, whereas TGF b1 mRNA expression was not modified. From these data we concluded that nicotine regulates bFGF production and release and TGF b1 release and may have a key role in the development and progression of atherosclerosis

Published

1999

6. Vasopressin and insulin-like growth factors synergistically induce myogenesis in serum-free medium

Author

Minotti, S, Scicchitano, Bianca Maria, Nervi, C, Scarpa, S, Lucarelli, M, Molinaro, M, Adamo, S., Scicchitano, Bianca Maria (ORCID:0000-0002-9599-6642), Minotti, S, Scicchitano, Bianca Maria, Nervi, C, Scarpa, S, Lucarelli, M, Molinaro, M, Adamo, S., and Scicchitano, Bianca Maria (ORCID:0000-0002-9599-6642)

Abstract

erminal differentiation of myogenic cells has long been known to be positively regulated by insulin-like growth factors (IGFs). Arg8-vasopressin (AVP) has been recently reported to potently induce myogenic differentiation. In the present study, the effects and the mechanisms of action of AVP and IGFs on myogenic cells have been investigated under conditions allowing growth and differentiation of myogenic cells in a simple serum-free medium. Under these conditions, L6 and L5 myogenic cells slowly proliferate and do not undergo differentiation (less than 1% fusion up to 7 days). AVP rapidly (2-3 days) and dose-dependently induces the formation of multinucleated myotubes. Creatine kinase activity and myosin accumulation are strongly up-regulated by AVP. Insulin or IGF-I or IGF-II, at concentrations that cause extensive differentiation in serum-containing medium, induces a modest degree of differentiation in serum-free medium. The simultaneous presence of AVP and of one of the IGFs in the synthetic medium induces maximal differentiation of L6, L5, and satellite cells. The expression of both myogenin and Myf-5 is dramatically stimulated by AVP. Our results indicate that AVP induces a significant level of myogenic differentiation in the absence of other factors. Furthermore, they suggest that to express their full myogenic potential, IGFs require the presence of other factors normally present in serum and fully mimicked by AVP. These studies support the conclusion that terminal myogenic differentiation may depend on the presence of differentiation factors rather than the absence of growth factors.

Published

1998