Your search keyword '"Donnini, Sandra"' showing total 8 results

1. Targeting endothelial-to-mesenchymal transition: the protective role of hydroxytyrosol sulfate metabolite.

Author

Terzuoli E, Nannelli G, Giachetti A, Morbidelli L, Ziche M, and Donnini S

Subjects

Anti-Inflammatory Agents pharmacology, Antioxidants pharmacology, Cells, Cultured, In Vitro Techniques, Phenylethyl Alcohol pharmacology, Sulfates, Endothelium drug effects, Endothelium physiopathology, Inflammation physiopathology, Mesoderm drug effects, Mesoderm physiopathology, Phenylethyl Alcohol analogs & derivatives

Abstract

Purpose: Endothelial-to-mesenchymal transition (EndMT) plays an important role in pathogenesis of a number of inflammatory diseases. Hydroxytyrosol (HT) and, particularly, its major plasma metabolite HT-3O sulfate (HT-3Os) are known olive oil antioxidant and anti-inflammatory polyphenols which exert benefits against vascular diseases by improving endothelial function. However, to date the HT-3Os role in EndMT is not well known., Methods: To investigate the HT-3Os effects on EndMT in the inflamed endothelium, we used an in vitro model of endothelial dysfunction, challenging endothelial cells (EC), human umbilical EC (HUVEC) and human retinal EC (HREC) with Interleukin-1β (IL-1β), an inflammatory agent. HREC were used as a specific model to investigate HT-3Os effects on vascular retinal diseases., Results: We found that IL-1β treatment-induced EndMT phenotype in both cell models, also changing cell morphology. HT-3Os protected EC against IL-1β effects, recovering cell morphology and phenotype. Mechanistically, HT-3Os targeting fibroblast growth factor receptor 1 FGFR1 expression and let-7 miRNA, controlled transforming growth factor beta (TGF-β) signalling in EC, downregulating transcription factors expression (SNAI1 and ZEB2) and gene expression of late EndMT markers (FN1, VIM, NOTCH3, CNN1, MMP2 and MMP9)., Conclusion: These results demonstrate that HT-3Os blunts pathological EndMT in inflamed EC, maintaining high let-7 miRNA expression and preventing activation of TGF-β signalling.

Published

2020

2. Monitoring Endothelial and Tissue Responses to Cobalt Ferrite Nanoparticles and Hybrid Hydrogels.

Author

Finetti, Federica, Terzuoli, Erika, Donnini, Sandra, Uva, Marianna, Ziche, Marina, and Morbidelli, Lucia

Subjects

CANCER treatment, NANOMEDICINE, ENDOTHELIAL cells, COBALT, HYDROGELS, IRON oxide nanoparticles, DRUG delivery systems, STIMULUS & response (Biology)

Abstract

Iron oxide nanoparticles (NPs) have been proposed for many biomedical applications as in vivo imaging and drug delivery in cancer treatment, but their toxicity is an ongoing concern. When NPs are intravenously administered, the endothelium represents the first barrier to tissue diffusion/penetration. However, there is little information about the biological effects of NPs on endothelial cells. In this work we showed that cobalt-ferrite (CoFe2O4) NPs affect endothelial cell integrity by increasing permeability, oxidative stress, inflammatory profile and by inducing cytoskeletal modifications. To overcome these problems, NPs have be loaded into biocompatible gels to form nanocomposite hybrid material (polysaccharide hydrogels containing magnetic NPs) that can be further conjugated with anticancer drugs to allow their release close to the target. The organic part of hybrid biomaterials is a carboxymethylcellulose (CMC) polymer, while the inorganic part consists of CoFe2O4 NPs coated with (3-aminopropyl)trimethoxysilane. The biological activity of these hybrid hydrogels was evaluated in vitro and in vivo. Our findings showed that hybrid hydrogels, instead of NPs alone, were not toxic on endothelial, stromal and epithelial cells, safe and biodegradable in vivo. In conclusion, biohydrogels with paramagnetic NPs as cross-linkers can be further exploited for antitumor drug loading and delivery systems. [ABSTRACT FROM AUTHOR]

Published

2016

3. Hydrogen Peroxide Mediates Endothelium-Dependent Dilation of Coronary Arterioles in Obese Rats on a Low-Carbohydrate Diet.

Author

Focardi, Marta, Picchi, Andrea, Donnini, Sandra, Cameli, Matteo, Ziche, Marina, Marzilli, Mario, and Mondillo, Sergio

Subjects

HYDROGEN peroxide, ENDOTHELIUM, LOW-carbohydrate diet, VASODILATION, MESSENGER RNA, GENE expression, LABORATORY rats

Abstract

Objective Endothelium-dependent vasodilation of coronary arterioles is impaired in obese rats and may be improved by a LCD. The aim of this study is to elucidate the mechanism by which this improvement occurs. Methods We used four groups of male Zucker rats: lean and obese on either SD or LCD. Coronary arterioles were cannulated and pressurized for diameter measurements during administration of acetylcholine or sodium nitroprusside or during flow. Real-time PCR was performed to quantify mRNA expression of CuZnSOD and catalase. Results The LCD significantly increased endothelium-dependent dilation in the obese rats. l-NAME and indomethacin reduced responses to flow and acetylcholine in the lean rats without any effect on the obese on either diet. In contrast, TEA and catalase blocked flow-dependent and acetylcholine-induced dilation in the obese on either diet, while no effect was observed on the lean. The LCD in the obese significantly up-regulated catalase mRNA expression and slightly increased CuZnSOD mRNA levels. Conclusions A LCD improves endothelium-dependent vasodilation of coronary arterioles in obese rats through the production of H2O2 which acts as a hyperpolarizing factor, independent of nitric oxide and PGI2. [ABSTRACT FROM AUTHOR]

Published

2013

4. Aβ peptides accelerate the senescence of endothelial cells in vitro and in vivo, impairing angiogenesis.

Author

Donnini, Sandra, Solito, Raffaella, Cetti, Elisa, Corti, Federico, Giachetti, Antonio, Carra, Silvia, Beltrame, Monica, Cotelli, Franco, and Ziche, Marina

Subjects

*AMYLOID, *AMYLOID beta-protein, *NEURODEGENERATION, *PEPTIDES, *AGING, *CELLS, *ENDOTHELIUM

Abstract

Cerebral amyloid angiopathy (CAA) caused by amyloid β (Aβ) deposition around brain microvessels results in vascular degenerative changes. Antiangiogenic Aβ properties are known to contribute to the compromised cerebrovascular architecture. Here we hypothesize that Aβ peptides impair angiogenesis by causing endothelial cells to enter senescence at an early stage of vascular development. Wild-type (WT) Aβ and its mutated variant E22Q peptide, endowed with marked vascular tropism, were used in this study. In vivo, in zebrafish embryos, the WT or E22Q peptides reduced embryo survival with an IC50 of 6.1 and 4.7 βM, respectively. The 2.5 βM concentration, showing minimal toxicity, was chosen. Alkaline phosphatase staining revealed disorganized vessel patterning, narrowing, and reduced branching of vessels. β-Galactosidase staining and the cyclindependent kinase inhibitor p21 expression, indicative of senescence, were increased. In vitro, WT and E22Q reduced endothelial cell survival with an IC50 of 12.3 and 8.8 µM, respectively. The 5 µM concentration, devoid of acute effects on the endothelium, was applied chronically to long-term cultured human umbilical vein endothelial cells (HUVECs). We observed reduced cumulative population doubling, which coincided with β-galactosidase accumulation, down-regulation of telomerase reverse-transcriptase mRNA expression, decreased telomerase activity, and p21 activation. Senescent HUVECs showed marked angiogenesis impairment, as Aβ treatment reduced tube sprouting. The endothelial injuries caused by the E22Q peptide were much more aggressive than those induced by the WT peptide. Premature Aβ-induced senescence of the endothelium, producing progressive alterations of microvessel morphology and functions, may represent one of the underlying mechanisms for sporadic or heritable CAA. [ABSTRACT FROM AUTHOR]

Published

2010

5. δPKC inhibition or ɛPKC activation repairs endothelial vascular dysfunction by regulating eNOS post-translational modification

Author

Monti, Martina, Donnini, Sandra, Giachetti, Antonio, Mochly-Rosen, Daria, and Ziche, Marina

Subjects

*PROTEIN kinase C, *ENZYME regulation, *ENZYME activation, *ENDOTHELIUM, *NITRIC-oxide synthases, *POST-translational modification, *HOMEOSTASIS, *MYOCARDIAL infarction

Abstract

Abstract: The balance between endothelial nitric oxide synthase (eNOS)-derived nitric oxide (NO) and reactive oxygen species (ROS) production determines endothelial-mediated vascular homeostasis. Activation of protein kinase C (PKC) has been linked to imbalance of the eNOS/ROS system, which leads to endothelial dysfunction. We previously found that selective inhibition of delta PKC (δPKC) or selective activation of epsilon PKC (ɛPKC) reduces oxidative damage in the heart following myocardial infarction. In this study we determined the effect of these PKC isozymes in the survival of coronary endothelial cells (CVEC). We demonstrate here that serum deprivation of CVEC increased eNOS-mediated ROS levels, activated caspase-3, reduced Akt phosphorylation and cell number. Treatment with either the δPKC inhibitor, δV1-1, or the ɛPKC activator, ψɛRACK, inhibited these effects, restoring cell survival through inhibition of eNOS activity. The decrease in eNOS activity coincided with specific de-phosphorylation of eNOS at Ser1179, and eNOS phosphorylation at Thr497 and Ser116. Furthermore, δV1-1 or ψɛRACK induced physical association of eNOS with caveolin-1, an additional marker of eNOS inhibition, and restored Akt activation by inhibiting its nitration. Together our data demonstrate that (1) in endothelial dysfunction, ROS and reactive nitrogen species (RNS) formation result from uncontrolled eNOS activity mediated by activation of δPKC or inhibition of ɛPKC; (2) inhibition of δPKC or activation of ɛPKC corrects the perturbed phosphorylation state of eNOS, thus increasing cell survival. Since endothelial health ensures better tissue perfusion and oxygenation, treatment with a δPKC inhibitor and/or an ɛPKC activator in diseases of endothelial dysfunction should be considered. [Copyright &y& Elsevier]

Published

2010

6. ERK1-2 and p38 MAPK regulate MMP/TIMP balance and function in response to thrombospondin-1 fragments in the microvascular endothelium

Author

Donnini, Sandra, Morbidelli, Lucia, Taraboletti, Giulia, and Ziche, Marina

Subjects

*THROMBOSPONDINS, *NEOVASCULARIZATION, *ENDOTHELIUM, *METALLOPROTEINASES

Abstract

We found that thrombospondin-1 (TSP-1) has opposite functions on angiogenesis depending on the nature of the proteolytic fragment released in vivo by the action of proteases. We studied the effect of the 25 and 140 kDa fragments of TSP-1 generated by its proteolytic cleavage on the cascade of mitogen activated protein kinase (MAPK) activation and matrix-metalloproteinase (MMP)/tissue inhibitor of metalloproteinase (TIMP) function and expression in microvascular endothelium. Post-capillary endothelial cells (CVEC) isolated from bovine heart were used. The 25 kDa fragment enhanced the upregulation of MMP-2 and -9 and reduced TIMP-2 expression leading to CVEC chemoinvasion. Conversely, the 140 kDa fragment blocked MMP-2 and -9 stimulation and doubled TIMP-2 expression, leading to inhibition of endothelial chemoinvasion induced by fibroblast growth factor-2 (FGF-2). MAPK activity (ERK1-2) was induced by TSP-1 and by the 25 kDa fragment, but not by the 140 kDa fragment which, however, promoted MAPK p38 activation. This evidence indicates that fragments originating from TSP-1 switch the pro- or anti-angiogenic phenotype in endothelium by targeting MAPK cascades with opposite functions on MMP/TIMP balance. [Copyright &y& Elsevier]

Published

2004

7. Physiological levels of amyloid peptides stimulate the angiogenic response through FGF-2.

Author

Cantara, Silvia, Donnini, Sandra, Morbidelli, Lucia, Giachetti, Antonio, Schulz, Richard, Memo, Maurizio, and Ziche, Marina

Subjects

*AMYLOID beta-protein, *PEPTIDES, *ENDOTHELIUM, *CELLS, *NEOVASCULARIZATION

Abstract

Focuses on a study on the effects of amyloid β peptides on endothelial cell functions required for angiogenesis. Findings of the study; Conclusions of the study.

Published

2004

8. Dutch and arctic mutant peptides of β amyloid1–40 differentially affect the FGF-2 pathway in brain endothelium

Author

Solito, Raffaella, Corti, Federico, Fossati, Silvia, Mezhericher, Emiliya, Donnini, Sandra, Ghiso, Jorge, Giachetti, Antonio, Rostagno, Agueda, and Ziche, Marina

Subjects

*PEPTIDES, *AMYLOID, *FIBROBLAST growth factors, *ENDOTHELIUM, *CELLULAR signal transduction, *BRAIN physiology, *GENE expression, *NEOVASCULARIZATION

Abstract

Abstract: Single point mutations of the amyloid precursor protein generate Aβ variants bearing amino acid substitutions at positions 21–23. These mutants are associated with distinct hereditary phenotypes of cerebral amyloid angiopathy, manifesting varying degrees of tropism for brain vessels, and impaired microvessel remodeling and angiogenesis. We examined the differential effects of E22Q (Dutch), and E22G (Arctic) variants in comparison to WT Aβ on brain endothelial cell proliferation, angiogenic phenotype expression triggered by fibroblast growth factor (FGF-2), pseudo-capillary sprouting, and induction of apoptosis. E22Q exhibited a potent anti-angiogenic profile in contrast to E22G, which had a much weaker effect. Investigations on the FGF-2 signaling pathway revealed the greatest differences among the peptides: E22Q and WT peptides suppressed FGF-2 expression while E22G had barely any effect. Phosphorylation of the FGF-2 receptor, FGFR-1, and the survival signal Akt were abolished by E22Q and WT peptides, but not by E22G. The biological dissimilar effect of the mutant and WT peptides on cerebral EC cannot be assigned to a particular Aβ structure, suggesting that the toxic effect of the Aβ assemblies goes beyond mere multimerization. [Copyright &y& Elsevier]

Published

2009