Your search keyword '"Vinci, Maria"' showing total 85 results

1. Pediatric brain tumor patients display altered immune activation and reduced lymphopoiesis at the onset of disease.

Author

Rosichini, Marco, Del Baldo, Giada, De Luca, Carmen Dolores, Benini, Francesca, Genah, Shirley, Vinci, Maria, Cerimele, Alfredo, Coccetti, Marianna, Flamini, Sara, Carsetti, Rita, Cacchione, Antonella, Carai, Andrea, Mastronuzzi, Angela, Locatelli, Franco, and Velardi, Enrico

Subjects

CENTRAL nervous system diseases, CHILD patients, TUMOR growth, BRAIN tumors, IMMUNOLOGIC memory

Abstract

Optimal immune function is crucial in preventing cancer development and growth and for the success of anti-cancer therapies. Here, we characterized the peripheral immunological status of 83 steroids-naïve pediatric patients with central nervous system neoplasia at the disease onset. Tumors were classified into low-grade gliomas (LGG), high-grade gliomas (HGG), medulloblastoma, and other tumors. We revealed that glioma patients showed an altered lymphocyte pool. T-cells of HGG patients shifted from naïve to effector memory phenotype. LGG patients exhibited T-cell central memory expansion and higher T-cell activation. Interestingly, HGG patients displayed reduced thymic function. Furthermore, LGG and HGG patients showed reduced activated B-cells and suboptimal B-cell formation. Our data demonstrate that glioma patients have reduced lymphopoiesis at the disease onset, which could contribute to the systemic lymphopenia characterizing these patients. This study offers novel insights into the immunological status of brain tumor patients which may help in designing more effective treatments. [ABSTRACT FROM AUTHOR]

Published

2024

2. The impact of vaccine hesitancy on psychological impairment among healthcare workers in a Total Worker Health© approach.

Author

Di Prinzio, Reparata Rosa, Ceresi, Bianca, Arnesano, Gabriele, Dosi, Alessia, Maimone, Mariarita, Vacca, Maria Eugenia, Vinci, Maria Rosaria, Camisa, Vincenzo, Santoro, Annapaola, Raponi, Massimiliano, Tomao, Paola, Vonesch, Nicoletta, Moscato, Umberto, Zaffina, Salvatore, and Dalmasso, Guendalina

Published

2024

3. Machine Learning Analysis in Diffusion Kurtosis Imaging for Discriminating Pediatric Posterior Fossa Tumors: A Repeatability and Accuracy Pilot Study.

Author

Voicu, Ioan Paul, Dotta, Francesco, Napolitano, Antonio, Caulo, Massimo, Piccirilli, Eleonora, D'Orazio, Claudia, Carai, Andrea, Miele, Evelina, Vinci, Maria, Rossi, Sabrina, Cacchione, Antonella, Vennarini, Sabina, Del Baldo, Giada, Mastronuzzi, Angela, Tomà, Paolo, and Colafati, Giovanna Stefania

Subjects

RANDOM forest algorithms, GLIOMAS, PILOT projects, MAGNETIC resonance imaging, INFRATENTORIAL brain tumors, RETROSPECTIVE studies, DESCRIPTIVE statistics, PEDIATRICS, RESEARCH bias, MACHINE learning, CANCER patient psychology, COMPARATIVE studies

Abstract

Simple Summary: Differentiating pediatric posterior fossa (PF) tumors such as medulloblastoma (MB), ependymoma (EP), and pilocytic astrocytoma (PA) remains relevant, due to important treatment and prognostic implications. Diffusion kurtosis imaging (DKI) has not been tested to date to distinguish between pediatric PF tumors. Estimating diffusion values from whole-tumor-based (VOI) segmentations may improve the repeatability of diffusion measurements compared to conventional region-of-interest (ROI) approaches. Our purpose was twofold: to assess the repeatability of VOI DKI-derived diffusion measurements and DKI accuracy in discriminating among pediatric PF tumors, by employing conventional statistical analyses and machine learning (ML) techniques. Background and purpose: Differentiating pediatric posterior fossa (PF) tumors such as medulloblastoma (MB), ependymoma (EP), and pilocytic astrocytoma (PA) remains relevant, because of important treatment and prognostic implications. Diffusion kurtosis imaging (DKI) has not yet been investigated for discrimination of pediatric PF tumors. Estimating diffusion values from whole-tumor-based (VOI) segmentations may improve diffusion measurement repeatability compared to conventional region-of-interest (ROI) approaches. Our purpose was to compare repeatability between ROI and VOI DKI-derived diffusion measurements and assess DKI accuracy in discriminating among pediatric PF tumors. Materials and methods: We retrospectively analyzed 34 children (M, F, mean age 7.48 years) with PF tumors who underwent preoperative examination on a 3 Tesla magnet, including DKI. For each patient, two neuroradiologists independently segmented the whole solid tumor, the ROI of the area of maximum tumor diameter, and a small 5 mm ROI. The automated analysis pipeline included inter-observer variability, statistical, and machine learning (ML) analyses. We evaluated inter-observer variability with coefficient of variation (COV) and Bland–Altman plots. We estimated DKI metrics accuracy in discriminating among tumor histology with MANOVA analysis. In order to account for class imbalances, we applied SMOTE to balance the dataset. Finally, we performed a Random Forest (RF) machine learning classification analysis based on all DKI metrics from the SMOTE dataset by partitioning 70/30 the training and testing cohort. Results: Tumor histology included medulloblastoma (15), pilocytic astrocytoma (14), and ependymoma (5). VOI-based measurements presented lower variability than ROI-based measurements across all DKI metrics and were used for the analysis. DKI-derived metrics could accurately discriminate between tumor subtypes (Pillai's trace: p < 0.001). SMOTE generated 11 synthetic observations (10 EP and 1 PA), resulting in a balanced dataset with 45 instances (34 original and 11 synthetic). ML analysis yielded an accuracy of 0.928, which correctly predicted all but one lesion in the testing set. Conclusions: VOI-based measurements presented improved repeatability compared to ROI-based measurements across all diffusion metrics. An ML classification algorithm resulted accurate in discriminating PF tumors on a SMOTE-generated dataset. ML techniques based on DKI-derived metrics are useful for the discrimination of pediatric PF tumors. [ABSTRACT FROM AUTHOR]

Published

2024

4. Evaluating cell culture reliability in pediatric brain tumor primary cells through DNA methylation profiling.

Author

Pedace, Lucia, Pizzi, Simone, Abballe, Luana, Vinci, Maria, Antonacci, Celeste, Patrizi, Sara, Nardini, Claudia, Del Bufalo, Francesca, Rossi, Sabrina, Pericoli, Giulia, Gianno, Francesca, Besharat, Zein Mersini, Tiberi, Luca, Mastronuzzi, Angela, Ferretti, Elisabetta, Tartaglia, Marco, Locatelli, Franco, Ciolfi, Andrea, and Miele, Evelina

Subjects

DNA methylation, CELL culture, GROWTH factors, BRAIN tumors

Abstract

In vitro models of pediatric brain tumors (pBT) are instrumental for better understanding the mechanisms contributing to oncogenesis and testing new therapies; thus, ideally, they should recapitulate the original tumor. We applied DNA methylation (DNAm) and copy number variation (CNV) profiling to characterize 241 pBT samples, including 155 tumors and 86 pBT-derived cell cultures, considering serum vs serum-free conditions, late vs early passages, and dimensionality (2D vs 3D cultures). We performed a t-SNE classification and identified differentially methylated regions in tumors compared to cell models. Early cell cultures recapitulate the original tumor, but serum media and 2D culturing were demonstrated to significantly contribute to the divergence of DNAm profiles from the parental ones. All divergent cells clustered together acquiring a common deregulated epigenetic signature suggesting a shared selective pressure. We identified a set of hypomethylated genes shared among unfaithful cells converging on response to growth factors and migration pathways, such as signaling cascade activation, tissue organization, and cellular migration. In conclusion, DNAm and CNV are informative tools that should be used to assess the recapitulation of pBT-cells from parental tumors. [ABSTRACT FROM AUTHOR]

Published

2024

5. Persistent epigenetic signals propel a senescence-associated secretory phenotype and trained innate immunity in CD34+ hematopoietic stem cells from diabetic patients.

Author

Vinci, Maria Cristina, Costantino, Sarah, Damiano, Giulia, Rurali, Erica, Rinaldi, Raffaella, Vigorelli, Vera, Sforza, Annalisa, Carulli, Ermes, Pirola, Sergio, Mastroiacovo, Giorgio, Raucci, Angela, El-Osta, Assam, Paneni, Francesco, and Pompilio, Giulio

Subjects

HEMATOPOIETIC stem cells, NATURAL immunity, PEOPLE with diabetes, RNA polymerase II, CELL physiology, HYPERGLYCEMIA, ATHEROSCLEROSIS

Abstract

Background: Diabetes-induced trained immunity contributes to the development of atherosclerosis and its complications. This study aimed to investigate in humans whether epigenetic signals involved in immune cell activation and inflammation are initiated in hematopoietic stem/progenitor cells (HSPCs) and transferred to differentiated progeny. Methods and results: High glucose (HG)-exposure of cord blood (CB)-derived HSPCs induced a senescent-associated secretory phenotype (SASP) characterized by cell proliferation lowering, ROS production, telomere shortening, up-regulation of p21 and p27genes, upregulation of NFkB-p65 transcription factor and increased secretion of the inflammatory cytokines TNFα and IL6. Chromatin immunoprecipitation assay (ChIP) of p65 promoter revealed that H3K4me1 histone mark accumulation and methyltransferase SetD7 recruitment, along with the reduction of repressive H3K9me3 histone modification, were involved in NFkB-p65 upregulation of HG-HSPCs, as confirmed by increased RNA polymerase II engagement at gene level. The differentiation of HG-HSPCs into myeloid cells generated highly responsive monocytes, mainly composed of intermediate subsets (CD14hiCD16+), that like the cells from which they derive, were characterized by SASP features and similar epigenetic patterns at the p65 promoter. The clinical relevance of our findings was confirmed in sternal BM-derived HSPCs of T2DM patients. In line with our in vitro model, T2DM HSPCs were characterized by SASP profile and SETD7 upregulation. Additionally, they generated, after myeloid differentiation, senescent monocytes mainly composed of proinflammatory intermediates (CD14hiCD16+) characterized by H3K4me1 accumulation at NFkB-p65 promoter. Conclusions: Hyperglycemia induces marked chromatin modifications in HSPCs, which, once transmitted to the cell progeny, contributes to persistent and pathogenic changes in immune cell function and composition. [ABSTRACT FROM AUTHOR]

Published

2024

6. Manipulating the tumor immune microenvironment to improve cancer immunotherapy: IGF1R, a promising target.

Author

Pellegrino, Marsha, Secli, Valerio, D’Amico, Silvia, Petrilli, Lucia Lisa, Caforio, Matteo, Folgiero, Valentina, Tumino, Nicola, Vacca, Paola, Vinci, Maria, Fruci, Doriana, and de Billy, Emmanuel

Subjects

TUMOR microenvironment, INSULIN-like growth factor receptors, SOMATOMEDIN C, IMMUNOTHERAPY, CELL physiology

Abstract

Cancer immunotherapy has made impressive advances in improving the outcome of patients affected by malignant diseases. Nonetheless, some limitations still need to be tackled to more efficiently and safely treat patients, in particular for those affected by solid tumors. One of the limitations is related to the immunosuppressive tumor microenvironment (TME), which impairs antitumor immunity. Efforts to identify targets able to turn the TME into a milieu more auspicious to current immuno-oncotherapy is a real challenge due to the high redundancy of the mechanisms involved. However, the insulin-like growth factor 1 receptor (IGF1R), an attractive drug target for cancer therapy, is emerging as an important immunomodulator and regulator of key immune cell functions. Here, after briefly summarizing the IGF1R signaling pathway in cancer, we review its role in regulating immune cells function and activity, and discuss IGF1R as a promising target to improve anti-cancer immunotherapy. [ABSTRACT FROM AUTHOR]

Published

2024

7. High Phosphate-Induced JAK-STAT Signalling Sustains Vascular Smooth Muscle Cell Inflammation and Limits Calcification.

Author

Macrì, Federica, Vigorito, Ilaria, Castiglione, Stefania, Faggiano, Stefano, Casaburo, Manuel, Fanotti, Nadia, Piacentini, Luca, Vigetti, Davide, Vinci, Maria Cristina, and Raucci, Angela

Subjects

VASCULAR smooth muscle, MUSCLE cells, MYOSITIS, CALCIFICATION, JAK-STAT pathway, ARTERIAL calcification

Abstract

Vascular calcification (VC) is an age-related complication characterised by calcium-phosphate deposition in the arterial wall driven by the osteogenic transformation of vascular smooth muscle cells (VSMCs). The JAK-STAT pathway is an emerging target in inflammation. Considering the relationship between VC and inflammation, we investigated the role of JAK-STAT signalling during VSMC calcification. Human aortic smooth muscle cells (HASMCs) were cultured in high-inorganic phosphate (Pi) medium for up to 7 days; calcium deposition was determined via Alizarin staining and colorimetric assay. Inflammatory factor secretion was evaluated via ELISA and JAK-STAT members' activation using Western blot or immunohistochemistry on HASMCs or calcified aortas of Vitamin D-treated C57BL6/J mice, respectively. The JAK-STAT pathway was blocked by JAK Inhibitor I and Von Kossa staining was used for calcium deposits in murine aortic rings. During Pi-induced calcification, HASMCs released IL-6, IL-8, and MCP-1 and activated JAK1-JAK3 proteins and STAT1. Phospho-STAT1 was detected in murine calcified aortas. Blocking of the JAK-STAT cascade reduced HASMC proliferation and pro-inflammatory factor expression and release while increasing calcium deposition and osteogenic transcription factor RUNX2 expression. Consistently, JAK-STAT pathway inhibition exacerbates mouse aortic ring calcification ex vivo. Intriguingly, our results suggest an alternative link between VSMC inflammation and VC. [ABSTRACT FROM AUTHOR]

Published

2024

8. Association between sex hormones and anti-S/RBD antibody responses to COVID-19 vaccines in healthcare workers.

Author

Anticoli, Simona, Dorrucci, Maria, Iessi, Elisabetta, Chiarotti, Flavia, Di Prinzio, Reparata Rosa, Vinci, Maria Rosaria, Zaffina, Salvatore, Puro, Vincenzo, Colavita, Francesca, Mizzoni, Klizia, Meschi, Silvia, Vonesch, Nicoletta, Albano, Christian, Ortona, Elena, Ruggieri, Anna, and Tomao, Paola

Published

2023

9. Human Hematopoietic Stem/Progenitor Cells in Type One Diabetes Mellitus Treatment: Is There an Ideal Candidate?

Author

Carulli, Ermes, Pompilio, Giulio, and Vinci, Maria Cristina

Subjects

TYPE 1 diabetes, PROGENITOR cells, HEMATOPOIETIC stem cell transplantation, DIABETES, LIFE expectancy, OLDER patients, HEMATOPOIETIC stem cells

Abstract

Type 1 diabetes mellitus (T1DM) is a highly prevalent autoimmune disease causing the destruction of pancreatic islet β-cells. The resulting insulin production deficiency leads to a lifelong need for insulin re-placement therapy, systemic complications, and reduced life quality and expectancy. Cell therapy has been extensively attempted to restore insulin independence (IID), and autologous nonmyeloablative hematopoietic stem cell transplantation (AHST) has appeared to give the most promising results, but with a highly variable quote of patients achieving IID across the studies. We performed a comprehensive review of the trials involving stem cells, and in particular AHST, for the treatment of T1DM. We then pooled the patients enrolled in the different trials and looked for the patient characteristics that could be associated with the achievement of IID. We found a significantly higher probability of achieving IID in older patients (OR 1.17, 95%CI 1.06–1.33, p = 0.002) and a significantly lower probability in patients with a history of ketoacidosis (OR 0.23, 95%CI 0.06–0.78, p = 0.023). This suggests that there could be a population of patients more likely to benefit from AHST, but further data would be required to depict the profile of the ideal candidate. [ABSTRACT FROM AUTHOR]

Published

2023

10. Feasibility of a Stop Smoking Program for Healthcare Workers in an Italian Hospital: Econometric Analysis in a Total Worker Health® Approach.

Author

Di Prinzio, Reparata Rosa, Bondanini, Giorgia, De Falco, Federica, Vinci, Maria Rosaria, Camisa, Vincenzo, Santoro, Annapaola, Arnesano, Gabriele, Dalmasso, Guendalina, Raponi, Massimiliano, Di Brino, Eugenio, Cicchetti, Americo, Magnavita, Nicola, and Zaffina, Salvatore

Subjects

SMOKING cessation, STATISTICAL models, SICK leave, COST control, COST effectiveness, RESEARCH funding, JOB absenteeism, PROFIT, DATA analysis, HEALTH facility administration, EVALUATION of human services programs, INVESTMENTS, PILOT projects, SCIENTIFIC observation, KRUSKAL-Wallis Test, DESCRIPTIVE statistics, MANN Whitney U Test, PRE-tests & post-tests, STATISTICS, HEALTH promotion, HOSPITAL health promotion programs, DATA analysis software, INDUSTRIAL hygiene, NONPARAMETRIC statistics

Abstract

Background: Over 20% of healthcare workers (HCWs) are active smokers. Smoking is a targeted issue for workplace health promotion (WHP) programs. Objective: Our study aims to evaluate the effectiveness of the Stop Smoking Promotion (SSP) intervention, a 6-hour training course for HCWs, which took place from May 2018 to July 2019. Methods: We compared HCWs who successfully quit smoking (n = 15) to those who did not (n = 25) in terms of Sickness Absence Days (SADs). Moreover, we conducted an econometric analysis by calculating the return on investment and implementing a break-even analysis. Findings: Among the 40 enrolled workers, a success rate of 37.5% was observed after a span of over two years from the SSP intervention (with nurses and physicians showed the best success rate). Overall, participants showed a noticeable absenteeism reduction after the SSP intervention, with a reduction rate of 85.0% in a one-year period. The estimated ROI for the hospital was 1.90, and the break-even point was 7.85. In other words, the organization nearly doubled its profit from the investment, and the success of at least eight participants balanced costs and profits. Conclusion: Our pilot study confirms that WHP programs are simple and cost-saving tools which may help improve control over the smoking pandemic in healthcare settings. [ABSTRACT FROM AUTHOR]

Published

2023

11. The Long Telling Story of "Endothelial Progenitor Cells": Where Are We at Now?

Author

Vinci, Maria Cristina, Carulli, Ermes, Rurali, Erica, Rinaldi, Raffaella, Damiano, Giulia, Raucci, Angela, Pompilio, Giulio, and Genovese, Stefano

Subjects

PROGENITOR cells, ENDOTHELIAL cells, STORYTELLING, CELL populations, HEMATOPOIETIC stem cells, REGENERATIVE medicine

Abstract

Endothelial progenitor cells (EPCs): The name embodies years of research and clinical expectations, but where are we now? Do these cells really represent the El Dorado of regenerative medicine? Here, past and recent literature about this eclectic, still unknown and therefore fascinating cell population will be discussed. This review will take the reader through a temporal journey that, from the first discovery, will pass through years of research devoted to attempts at their definition and understanding their biology in health and disease, ending with the most recent evidence about their pathobiological role in cardiovascular disease and their recent applications in regenerative medicine. [ABSTRACT FROM AUTHOR]

Published

2023

12. The Management of Workplace Violence against Healthcare Workers: A Multidisciplinary Team for Total Worker Health ® Approach in a Hospital.

Author

Di Prinzio, Reparata Rosa, Bondanini, Giorgia, De Falco, Federica, Vinci, Maria Rosaria, Camisa, Vincenzo, Santoro, Annapaola, De Santis, Marcello, Raponi, Massimiliano, Dalmasso, Guendalina, and Zaffina, Salvatore

Published

2023

13. Developing a Predictive Grading Model for Children with Gliomas Based on Diffusion Kurtosis Imaging Metrics: Accuracy and Clinical Correlations with Patient Survival.

Author

Voicu, Ioan Paul, Napolitano, Antonio, Caulo, Massimo, Dotta, Francesco, Piccirilli, Eleonora, Vinci, Maria, Diomedi-Camassei, Francesca, Lattavo, Lorenzo, Carboni, Alessia, Miele, Evelina, Cacchione, Antonella, Carai, Andrea, Tomà, Paolo, Mastronuzzi, Angela, and Colafati, Giovanna Stefania

Subjects

PREDICTIVE tests, RESEARCH evaluation, THREE-dimensional imaging, CONFIDENCE intervals, GLIOMAS, MAGNETIC resonance imaging, RETROSPECTIVE studies, ACQUISITION of data, CANCER patients, SURVIVAL analysis (Biometry), MEDICAL records, KAPLAN-Meier estimator, DESCRIPTIVE statistics, PREDICTION models, PROGRESSION-free survival, RECEIVER operating characteristic curves, PROBABILITY theory, TUMOR grading, EVALUATION, CHILDREN

Abstract

Simple Summary: The most frequent brain tumors in children are solid tumors. A significant fraction of pediatric brain tumors is represented by gliomas, which are heterogeneous. Diffusion kurtosis imaging metrics (MK, AK, RK, FA, and ADC) have shown promising results for glioma grading in adult patients; however, it is unclear whether this technique is accurate for diagnosing high grade pediatric gliomas and if it is correlated with patient survival. In our study, we performed a retrospective whole-tumor analysis on 59 children affected by gliomas and tested (1) if DKI metrics are accurate for grading pediatric gliomas and (2) if DKI metrics are correlated with patient overall survival and progression-free survival. Purpose: To develop a predictive grading model based on diffusion kurtosis imaging (DKI) metrics in children affected by gliomas, and to investigate the clinical impact of the predictive model by correlating with overall survival and progression-free survival. Materials and methods: 59 patients with a histological diagnosis of glioma were retrospectively studied (33 M, 26 F, median age 7.2 years). Patients were studied on a 3T scanner with a standardized MR protocol, including conventional and DKI sequences. Mean kurtosis (MK), axial kurtosis (AK), radial kurtosis (RK), fractional anisotropy (FA), and apparent diffusion coefficient (ADC) maps were obtained. Whole tumour volumes (VOIs) were segmented semi-automatically. Mean DKI values were calculated for each metric. The quantitative values from DKI-derived metrics were used to develop a predictive grading model to develop a probability prediction of a high-grade glioma (pHGG). Three models were tested: DTI-based, DKI-based, and combined (DTI and DKI). The grading accuracy of the resulting probabilities was tested with a receiver operating characteristics (ROC) analysis for each model. In order to account for dataset imbalances between pLGG and pHGG, we applied a random synthetic minority oversampling technique (SMOTE) analysis. Lastly, the most accurate model predictions were correlated with progression-free survival (PFS) and overall survival (OS) using the Kaplan–Meier method. Results: The cohort included 46 patients with pLGG and 13 patients with pHGG. The developed model predictions yielded an AUC of 0.859 (95%CI: 0.752–0.966) for the DTI model, of 0.939 (95%CI: 0.879–1) for the DKI model, and of 0.946 (95%CI: 0.890–1) for the combined model, including input from both DTI and DKI metrics, which resulted in the most accurate model. Sample estimation with the random SMOTE analysis yielded an AUC of 0.98 on the testing set. Model predictions from the combined model were significantly correlated with PFS (25.2 months for pHGG vs. 40.0 months for pLGG, p < 0.001) and OS (28.9 months for pHGG vs. 44.9 months for pLGG, p < 0.001). Conclusions: a DKI-based predictive model was highly accurate for pediatric glioma grading. The combined model, derived from both DTI and DKI metrics, proved that DKI-based model predictions of tumour grade were significantly correlated with progression-free survival and overall survival. [ABSTRACT FROM AUTHOR]

Published

2022

14. Effects of RAGE Deletion on the Cardiac Transcriptome during Aging.

Author

Scavello, Francesco, Piacentini, Luca, Castiglione, Stefania, Zeni, Filippo, Macrì, Federica, Casaburo, Manuel, Vinci, Maria Cristina, Colombo, Gualtiero I., and Raucci, Angela

Subjects

ADVANCED glycation end-products, FATTY acid oxidation, TRANSCRIPTOMES, INTERFERON gamma, ANTIGEN processing, RECEPTOR for advanced glycation end products (RAGE)

Abstract

Cardiac aging is characterized by increased cardiomyocyte hypertrophy, myocardial stiffness, and fibrosis, which enhance cardiovascular risk. The receptor for advanced glycation end-products (RAGE) is involved in several age-related diseases. RAGE knockout (Rage−/−) mice show an acceleration of cardiac dimension changes and interstitial fibrosis with aging. This study identifies the age-associated cardiac gene expression signature induced by RAGE deletion. We analyzed the left ventricle transcriptome of 2.5-(Young), 12-(Middle age, MA), and 21-(Old) months-old female Rage−/− and C57BL/6N (WT) mice. By comparing Young, MA, and Old Rage−/− versus age-matched WT mice, we identified 122, 192, and 12 differently expressed genes, respectively. Functional inference analysis showed that RAGE deletion is associated with: (i) down-regulation of genes involved in antigen processing and presentation of exogenous antigen, adaptive immune response, and cellular responses to interferon beta and gamma in Young animals; (ii) up-regulation of genes related to fatty acid oxidation, cardiac structure remodeling and cellular response to hypoxia in MA mice; (iii) up-regulation of few genes belonging to complement activation and triglyceride biosynthetic process in Old animals. Our findings show that the age-dependent cardiac phenotype of Rage−/− mice is associated with alterations of genes related to adaptive immunity and cardiac stress pathways. [ABSTRACT FROM AUTHOR]

Published

2022

15. Pediatric Diffuse Midline Gliomas: An Unfinished Puzzle.

Author

Di Ruscio, Valentina, Del Baldo, Giada, Fabozzi, Francesco, Vinci, Maria, Cacchione, Antonella, de Billy, Emmanuel, Megaro, Giacomina, Carai, Andrea, and Mastronuzzi, Angela

Subjects

GLIOMAS, PROGRESSION-free survival, PROGNOSIS, SURVIVAL rate, OVERALL survival, BRAIN tumors

Abstract

Diffuse midline glioma (DMG) is a heterogeneous group of aggressive pediatric brain tumors with a fatal prognosis. The biological hallmark in the major part of the cases is H3K27 alteration. Prognosis remains poor, with median survival ranging from 9 to 12 months from diagnosis. Clinical and radiological prognostic factors only partially change the progression-free survival but they do not improve the overall survival. Despite efforts, there is currently no curative therapy for DMG. Radiotherapy remains the standard treatment with only transitory benefits. No chemotherapeutic regimens were found to significantly improve the prognosis. In the new era of a deeper integration between histological and molecular findings, potential new approaches are currently under investigation. The entire international scientific community is trying to target DMG on different aspects. The therapeutic strategies involve targeting epigenetic alterations, such as methylation and acetylation status, as well as identifying new molecular pathways that regulate oncogenic proliferation; immunotherapy approaches too are an interesting point of research in the oncology field, and the possibility of driving the immune system against tumor cells has currently been evaluated in several clinical trials, with promising preliminary results. Moreover, thanks to nanotechnology amelioration, the development of innovative delivery approaches to overcross a hostile tumor microenvironment and an almost intact blood–brain barrier could potentially change tumor responses to different treatments. In this review, we provide a comprehensive overview of available and potential new treatments that are worldwide under investigation, with the intent that patient- and tumor-specific treatment could change the biological inauspicious history of this disease. [ABSTRACT FROM AUTHOR]

Published

2022

16. Circulating levels of AGEs and soluble RAGE isoforms are associated with all-cause mortality and development of cardiovascular complications in type 2 diabetes: a retrospective cohort study.

Author

Sabbatinelli, Jacopo, Castiglione, Stefania, Macrì, Federica, Giuliani, Angelica, Ramini, Deborah, Vinci, Maria Cristina, Tortato, Elena, Bonfigli, Anna Rita, Olivieri, Fabiola, and Raucci, Angela

Subjects

TYPE 2 diabetes, MORTALITY, ADVANCED glycation end-products, CARDIOLOGICAL manifestations of general diseases, MAJOR adverse cardiovascular events

Abstract

Background: Advanced glycation end-products (AGEs) and their interaction with the receptor for advanced glycation end-products (RAGE) play a pivotal role in the development and progression of type 2 diabetes. In this retrospective cohort study, we explored the association of circulating levels of soluble RAGE (sRAGE) isoforms, i.e., endogenous secretory esRAGE and cleaved cRAGE, AGEs and their respective ratios with 15-year all-cause mortality in type 2 diabetes. Methods: Baseline AGEs and sRAGE isoforms concentration were measured by ELISA in 362 patients with type 2 diabetes and in 125 age- and gender-matched healthy control subjects (CTR). Independent predictors of mortality were determined using Cox proportional-hazards models and used to build and validate a nomogram for all-cause mortality prediction in type 2 diabetes. Results: AGEs, total sRAGE, cRAGE and the AGEs/sRAGE and AGEs/esRAGE ratios were significantly increased in patients with type 2 diabetes compared to CTR (p < 0.001). In CTR subjects, but not in type 2 diabetes patients, a significant negative correlation between cRAGE and age was confirmed (p = 0.003), whereas the AGEs/sRAGE (p = 0.032) and AGEs/cRAGE (p = 0.006) ratios were positively associated with age. At an average follow-up of 15 years (4,982 person-years), 130 deaths were observed. The increase in the AGEs/cRAGE ratio was accompanied by a higher risk of all-cause mortality in patients with type 2 diabetes (HR per each SD increment = 1.30, 95% CI 1.15–1.47; p < 0.001). Moreover, sRAGE was associated with the development of major adverse cardiovascular events (MACE) in type 2 diabetes patients without previous MACE (OR for each SD increase: 1.48, 95% CI 1.11–1.89). A nomogram based on age, sex, HbA1c, systolic blood pressure, and the AGEs/cRAGE ratio was built to predict 5-, 10- and 15-year survival in type 2 diabetes. Patients were categorized into quartiles of the monogram scores and Kaplan-Meier survival curves confirmed the prognostic accuracy of the model (log-rank p = 6.5 × 10− 13). Conclusions: The ratio between AGEs and the cRAGE isoform is predictive of 15-year survival in patients with type 2 diabetes. Our data support the assessment of circulating AGEs and soluble RAGE isoforms in patients with type 2 diabetes as predictors of MACE and all-cause mortality. [ABSTRACT FROM AUTHOR]

Published

2022

17. MET Inhibition Sensitizes Rhabdomyosarcoma Cells to NOTCH Signaling Suppression.

Author

Perrone, Clara, Pomella, Silvia, Cassandri, Matteo, Pezzella, Michele, Milano, Giuseppe Maria, Colletti, Marta, Cossetti, Cristina, Pericoli, Giulia, Di Giannatale, Angela, de Billy, Emmanuel, Vinci, Maria, Petrini, Stefania, Marampon, Francesco, Quintarelli, Concetta, Taulli, Riccardo, Roma, Josep, Gallego, Soledad, Camero, Simona, Mariottini, Paolo, and Cervelli, Manuela

Subjects

RHABDOMYOSARCOMA, SARCOMA, CELL communication, CELL migration, TUMOR growth, CHIMERIC proteins

Abstract

Rhabdomyosarcoma (RMS) is a pediatric myogenic soft tissue sarcoma. The Fusion-Positive (FP) subtype expresses the chimeric protein PAX3-FOXO1 (P3F) while the Fusion-Negative (FN) is devoid of any gene translocation. FP-RMS and metastatic FN-RMS are often unresponsive to conventional therapy. Therefore, novel therapeutic approaches are needed to halt tumor progression. NOTCH signaling has oncogenic functions in RMS and its pharmacologic inhibition through γ-secretase inhibitors blocks tumor growth in vitro and in vivo. Here, we show that NOTCH signaling blockade resulted in the up-regulation and phosphorylation of the MET oncogene in both RH30 (FP-RMS) and RD (FN-RMS) cell lines. Pharmacologic inhibition of either NOTCH or MET signaling slowed proliferation and restrained cell survival compared to control cells partly by increasing Annexin V and CASP3/7 activation. Co-treatment with NOTCH and MET inhibitors significantly amplified these effects and enhanced PARP1 cleavage in both cell lines. Moreover, it severely hampered cell migration, colony formation, and anchorage-independent growth compared to single-agent treatments in both cell lines and significantly prevented the growth of FN-RMS cells grown as spheroids. Collectively, our results unveil the overexpression of the MET oncogene by NOTCH signaling targeting in RMS cells and show that MET pathway blockade sensitizes them to NOTCH inhibition. [ABSTRACT FROM AUTHOR]

Published

2022

18. Liraglutide preserves CD34+ stem cells from dysfunction Induced by high glucose exposure.

Author

Sforza, Annalisa, Vigorelli, Vera, Rurali, Erica, Perrucci, Gianluca Lorenzo, Gambini, Elisa, Arici, Martina, Metallo, Alessia, Rinaldi, Raffaella, Fiorina, Paolo, Barbuti, Andrea, Raucci, Angela, Sacco, Elena, Rocchetti, Marcella, Pompilio, Giulio, Genovese, Stefano, and Vinci, Maria Cristina

Subjects

STEM cells, TYPE 2 diabetes, HEMATOPOIETIC stem cells, LIRAGLUTIDE, GLUCOSE

Abstract

Background: Glucagon like peptide-1 receptor agonists (GLP-1RAs) have shown to reduce mortality and cardiovascular events in patients with type 2 diabetes mellitus (T2DM). Since the impairment in number and function of vasculotrophic circulating CD34+ hematopoietic stem progenitor cells (HSPCs) in T2D has been reported to increase cardiovascular (CV) risk, we hypothesized that one of the mechanisms whereby GLP-1 RAs exert CV protective effects may be related to the ability to improve CD34+ HSPC function. Methods: In cord blood (CB)-derived CD34+ HSPC, the expression of GLP-1 receptor (GLP-1R) mRNA, receptor protein and intracellular signaling was evaluated by RT-qPCR and Western Blot respectively. CD34+ HSPCs were exposed to high glucose (HG) condition and GLP-1RA liraglutide (LIRA) was added before as well as after functional impairment. Proliferation, CXCR4/SDF-1α axis activity and intracellular ROS production of CD34+ HSPC were evaluated. Results: CD34+ HSPCs express GLP-1R at transcriptional and protein level. LIRA treatment prevented and rescued HSPC proliferation, CXCR4/SDF-1α axis activity and metabolic imbalance from HG-induced impairment. LIRA stimulation promoted intracellular cAMP accumulation as well as ERK1/2 and AKT signaling activation. The selective GLP-1R antagonist exendin (9–39) abrogated LIRA-dependent ERK1/2 and AKT phosphorylation along with the related protective effects. Conclusion: We provided the first evidence that CD34+ HSPC express GLP-1R and that LIRA can favorably impact on cell dysfunction due to HG exposure. These findings open new perspectives on the favorable CV effects of GLP-1 RAs in T2DM patients. [ABSTRACT FROM AUTHOR]

Published

2022

19. Emergence and maintenance of actionable genetic drivers at medulloblastoma relapse.

Author

Richardson, Stacey, Hill, Rebecca M, Kui, Christopher, Lindsey, Janet C, Grabovksa, Yura, Keeling, Claire, Pease, Louise, Bashton, Matthew, Crosier, Stephen, Vinci, Maria, André, Nicolas, Figarella-Branger, Dominique, Hansford, Jordan R, Lastowska, Maria, Zakrzewski, Krzysztof, Jorgensen, Mette, Pickles, Jessica C, Taylor, Michael D, Pfister, Stefan M, and Wharton, Stephen B

Published

2022

20. MicroRNA-34a: the bad guy in age-related vascular diseases.

Author

Raucci, Angela, Macrì, Federica, Castiglione, Stefania, Badi, Ileana, Vinci, Maria Cristina, and Zuccolo, Estella

Subjects

VASCULAR diseases, PULMONARY arterial hypertension, ARTERIAL calcification, VASCULAR smooth muscle, OLDER people, HYPERGLYCEMIA, SIRTUINS

Abstract

The age-related vasculature alteration is the prominent risk factor for vascular diseases (VD), namely, atherosclerosis, abdominal aortic aneurysm, vascular calcification (VC) and pulmonary arterial hypertension (PAH). The chronic sterile low-grade inflammation state, alias inflammaging, characterizes elderly people and participates in VD development. MicroRNA34-a (miR-34a) is emerging as an important mediator of inflammaging and VD. miR-34a increases with aging in vessels and induces senescence and the acquisition of the senescence-associated secretory phenotype (SASP) in vascular smooth muscle (VSMCs) and endothelial (ECs) cells. Similarly, other VD risk factors, including dyslipidemia, hyperglycemia and hypertension, modify miR-34a expression to promote vascular senescence and inflammation. miR-34a upregulation causes endothelial dysfunction by affecting ECs nitric oxide bioavailability, adhesion molecules expression and inflammatory cells recruitment. miR-34a-induced senescence facilitates VSMCs osteoblastic switch and VC development in hyperphosphatemia conditions. Conversely, atherogenic and hypoxic stimuli downregulate miR-34a levels and promote VSMCs proliferation and migration during atherosclerosis and PAH. MiR34a genetic ablation or miR-34a inhibition by anti-miR-34a molecules in different experimental models of VD reduce vascular inflammation, senescence and apoptosis through sirtuin 1 Notch1, and B-cell lymphoma 2 modulation. Notably, pleiotropic drugs, like statins, liraglutide and metformin, affect miR-34a expression. Finally, human studies report that miR-34a levels associate to atherosclerosis and diabetes and correlate with inflammatory factors during aging. Herein, we comprehensively review the current knowledge about miR-34a-dependent molecular and cellular mechanisms activated by VD risk factors and highlight the diagnostic and therapeutic potential of modulating its expression in order to reduce inflammaging and VD burn and extend healthy lifespan. [ABSTRACT FROM AUTHOR]

Published

2021

21. Recurrence, Reactivation, or Inflammatory Rebound of SARS-CoV-2 Infection With Acute Vestibular Symptoms: A Case Report and Revision of Literature.

Author

Zaffina, Salvatore, Lanteri, Paola, Gilardi, Francesco, Garbarino, Sergio, Santoro, Annapaola, Vinci, Maria Rosaria, Carsetti, Rita, Scorpecci, Alessandro, Raponi, Massimiliano, Magnavita, Nicola, and Camisa, Vincenzo

Subjects

COVID-19, SARS-CoV-2, PHYSICIANS, MEDICAL personnel, ANTIBODY titer

Abstract

A case of recurrent coronavirus disease 2019 (COVID-19) with neurovestibular symptoms was reported. In March 2020, a physician working in an Italian pediatric hospital had flu-like symptoms with anosmia and dysgeusia, and following a reverse transcription PCR (RT/PCR) test with a nasopharyngeal swab tested positive for SARS-CoV-2. After home quarantine, 21 days from the beginning of the symptoms, the patient tested negative in two subsequent swabs and was declared healed and readmitted to work. Serological testing showed a low level of immunoglobulin G (IgG) antibody title and absence of immunoglobulin M (IgM). However, 2 weeks later, before resuming work, the patient complained of acute vestibular syndrome, and the RT/PCR test with mucosal swab turned positive. On the basis of the literature examined and reviewed for recurrence cases and vestibular symptoms during COVID-19, to our knowledge this case is the first case of recurrence with vestibular impairment as a neurological symptom, and we defined it as probably a viral reactivation. The PCR retest positivity cannot differentiate re-infectivity, relapse, and dead-viral RNA detection. Serological antibody testing and viral genome sequencing could be always performed in recurrence cases. [ABSTRACT FROM AUTHOR]

Published

2021

22. Evolution of Human Memory B Cells From Childhood to Old Age.

Author

Ciocca, Michela, Zaffina, Salvatore, Fernandez Salinas, Ane, Bocci, Chiara, Palomba, Patrizia, Conti, Maria Giulia, Terreri, Sara, Frisullo, Giuseppe, Giorda, Ezio, Scarsella, Marco, Brugaletta, Rita, Vinci, Maria Rosaria, Magnavita, Nicola, Carsetti, Rita, and Piano Mortari, Eva

Subjects

B cells, OLD age, HUMAN evolution, COVID-19 pandemic, OLDER people, PSYCHONEUROIMMUNOLOGY

Abstract

High quality medical assistance and preventive strategies, including pursuing a healthy lifestyle, result in a progressively growing percentage of older people. The population and workforce is aging in all countries of the world. It is widely recognized that older individuals show an increased susceptibility to infections and a reduced response to vaccination suggesting that the aged immune system is less able to react and consequently protect the organism. The SARS-CoV-2 pandemic is dramatically showing us that the organism reacts to novel pathogens in an age-dependent manner. The decline of the immune system observed in aging remains unclear. We aimed to understand the role of B cells. We analyzed peripheral blood from children (4-18 years); young people (23-60 years) and elderly people (65-91 years) by flow cytometry. We also measured antibody secretion by ELISA following a T-independent stimulation. Here we show that the elderly have a significant reduction of CD27dull memory B cells, a population that bridges innate and adaptive immune functions. In older people, memory B cells are mostly high specialized antigen-selected CD27bright. Moreover, after in vitro stimulation with CpG, B cells from older individuals produced significantly fewer IgM and IgA antibodies compared to younger individuals. Aging is a complex process characterized by a functional decline in multiple physiological systems. The immune system of older people is well equipped to react to often encountered antigens but has a low ability to respond to new pathogens. [ABSTRACT FROM AUTHOR]

Published

2021

23. Doxorubicin induces an alarmin-like TLR4-dependent autocrine/paracrine action of Nucleophosmin in human cardiac mesenchymal progenitor cells.

Author

Beji, Sara, D'Agostino, Marco, Gambini, Elisa, Sileno, Sara, Scopece, Alessandro, Vinci, Maria Cristina, Milano, Giuseppina, Melillo, Guido, Napolitano, Monica, Pompilio, Giulio, Capogrossi, Maurizio C., Avitabile, Daniele, and Magenta, Alessandra

Subjects

PROGENITOR cells, HUMAN behavior, NF-kappa B, DOUBLE-strand DNA breaks, DOXORUBICIN, NUCLEOPHOSMIN, ANTHRACYCLINES, AUTOPHAGY

Abstract

Background: Doxorubicin (Dox) is an anti-cancer anthracycline drug that causes double-stranded DNA breaks. It is highly effective against several types of tumours; however, it also has adverse effects on regenerative populations of normal cells, such as human cardiac mesenchymal progenitor cells (hCmPCs), and its clinical use is limited by cardiotoxicity. Another known effect of Dox is nucleolar disruption, which triggers the ubiquitously expressed nucleolar phosphoprotein Nucleophosmin (NPM) to be released from the nucleolus into the cell, where it participates in the orchestration of cellular stress responses. NPM has also been observed in the extracellular space in response to different stress stimuli; however, the mechanism behind this and its functional implications are as yet largely unexplored. The aim of this study was to establish whether Dox could elicit NPM secretion in the extracellular space and to elucidate the mechanism of secretion and the effect of extracellular NPM on hCmPCs. Results: We found that following the double-strand break formation in hCmPCs caused by Dox, NPM was rapidly secreted in the extracellular space by an active mechanism, in the absence of either apoptosis or necrosis. Extracellular release of NPM was similarly seen in response to ultraviolet radiation (UV). Furthermore, we observed an increase of NPM levels in the plasma of Dox-treated mice; thus, NPM release also occurred in vivo. The treatment of hCmPCs with extracellular recombinant NPM induced a decrease of cell proliferation and a response mediated through the Toll-like receptor (TLR)4. We demonstrated that NPM binds to TLR4, and via TLR4, and nuclear factor kappa B (NFkB) activation/nuclear translocation, exerts proinflammatory functions by inducing IL-6 and COX-2 gene expression. Finally, we found that in hCmPCs, NPM secretion could be driven by an autophagy-dependent unconventional mechanism that requires TLR4, since TLR4 inhibition dramatically reduced Dox-induced secretion. Conclusions: We hypothesise that the extracellular release of NPM could be a general response to DNA damage since it can be elicited by either a chemical agent such as Dox or a physical genotoxic stressor such as UV radiation. Following genotoxic stress, NPM acts similarly to an alarmin in hCmPCs, being rapidly secreted and promoting cell cycle arrest and a TLR4/NFκB-dependent inflammatory response. [ABSTRACT FROM AUTHOR]

Published

2021

24. Low influenza vaccination coverage in subjects with liver cirrhosis. An alert waiting for winter season 2020–2021 during the COVID‐19 pandemic.

Author

Stroffolini, Tommaso, Lombardi, Anna, Ciancio, Alessia, Niro, Grazia A., Colloredo, Guido, Marignani, Massimo, Vinci, Maria, Morisco, Filomena, Babudieri, Sergio, Ferrigno, Luigina, and Sagnelli, Evangelista

Subjects

COVID-19 pandemic, INFLUENZA vaccines, CIRRHOSIS of the liver, INFLUENZA, LOGISTIC regression analysis, MULTIPLE regression analysis

Abstract

We have evaluated flu vaccine coverage and variables associated with the lack of vaccination in cirrhotic subjects with particular attention to the cirrhosis etiology. Cirrhotic subjects consecutively referring to eight Italian centers were prospectively enrolled for a 6‐month period in 2019. Subjects were asked if they had received a flu vaccine in the last 12 months. Multiple logistic regression analysis was performed to identify independent predictors of lack of vaccination. A total of 818 cases were recruited. The overall vaccine coverage was 39.6% (26.9% in those younger than 65 years and 51.9% in those older than 64 years; p < 0.001). Age < 65 years (odds ratio [OR] = 2.38; 95% confidence interval [CI] = 1.68–3.36), alcoholic etiology (OR = 2.40; 95% CI = 1.49–3.85), birth abroad (OR = 2.7; 95% CI = 1.10–6.61), and residence in South/Sardinia island (OR = 1.66; 95% CI = 1.14–2.42) all resulted independent predictors of the likelihood of lack of vaccination. The lack of information regarding the vaccine as the reason for no vaccination was reported by 71.4% of foreigners and by 34.7% of natives (p < 0.001). In conclusion, much work still should be done to improve coverage among groups at higher risk of lack of vaccination identified in this survey. The ongoing SARS‐CoV‐2 pandemic may represent one more alert for improving seasonal flu vaccine coverage to avoid further stress to the National Health System. Highlights: Flu vaccine coverage is often perceived less beneficial in patients withliver disease resulting lower among cirrhotic subjects.Flu infection may cause collateral liver damage such as an usually mild and self‐limiting hepatitis and trigger hepatic decompensation in liver disease.Age (<65 years), birth abroad and alcoholic etiology resulted to be independent predictors of the likelihood of lack of flu vaccination in cirrhotic subjects. [ABSTRACT FROM AUTHOR]

Published

2021

25. Chronic hepatitis B virus infection in Italy during the twenty-first century: an updated survey in 2019.

Author

Stroffolini, Tommaso, Ciancio, Alessia, Furlan, Caterina, Vinci, Maria, Niro, Grazia Anna, Russello, Maurizio, Colloredo, Guido, Morisco, Filomena, Coppola, Nicola, Babudieri, Sergio, Ferrigno, Luigina, Sagnelli, Caterina, Sagnelli, Evangelista, Collaborating group, Verzon, Giulia, Latanza, Arianna, Picciotto, Viviana, Fontana, Rosanna, Benigno, Rosa Grazia, and Pontillo, Giuseppina

Subjects

HEPATITIS B virus, VIRUS diseases, TWENTY-first century, MULTIPLE regression analysis, LOGISTIC regression analysis, DRUG carriers

Abstract

The aim of this study is to provide updates on the characteristics of chronic HBsAg carriers in Italy before the advent of new drugs eliminating or functionally inactivating the genome HBV reservoirs. HBV endemicity has greatly decreased in Italy over the past decades. A not negligible number of chronic HBsAg carriers are still alive in the country. Chronic HBsAg carriers consecutively referring to 9 units in Italy were prospectively enrolled for a 6-month period in 2019. Multiple logistic regression analysis was performed to identify independent predictors of treatment. A total of 894 cases was recruited (sex ratio 1.6; mean age 53.7 ± 13.5 years). The proportion of subjects born abroad was 19.0%; only 1% of cases reported current heavy alcohol intake (> 4 units/day). Chronic HBV infection, chronic HBV hepatitis, and subjects with liver cirrhosis and/or HCC represented 24.8%, 55%, and 19.3% of cases, respectively. After exclusion of the 222 subjects with chronic HBV infection, the proportion of subjects under therapy was as high as 89.3%. A more severe liver disease (OR 2.52; 95% CI = 1.25–5.14) resulted an independent predictor of the likelihood of treatment; male sex was marginally associated (OR 1.67; 95% CI = 1.02–2.76) to the chance of treatment. People born abroad had same chance than Italians native to be treated (OR 2.12; 95% CI = 0.9–4.97). The high proportion of subjects under treatment and the absence of gender and ethnic barrier against treatment sound good news. These updated figures may represent reference data for evaluating the potential impact of forthcoming new therapy against HBV-related disease. [ABSTRACT FROM AUTHOR]

Published

2021

26. Digital PCR for high sensitivity viral detection in false-negative SARS-CoV-2 patients.

Author

Poggio, Paolo, Songia, Paola, Vavassori, Chiara, Ricci, Veronica, Banfi, Cristina, Barbieri, Silvia Stella, Garoffolo, Gloria, Myasoedova, Veronika A., Piacentini, Luca, Raucci, Angela, Scopece, Alessandro, Sommariva, Elena, Vinci, Maria Cristina, Carcione, Davide, Biondi, Maria Luisa, Mancini, Maria Elisabetta, Formenti, Alberto, Andreini, Daniele, Assanelli, Emilio M., and Agostoni, Piergiuseppe

Subjects

SARS-CoV-2, POLYMERASE chain reaction, GENETIC transcription, VIRAL genes, PATIENT management

Abstract

Patients requiring diagnostic testing for coronavirus disease 2019 (COVID-19) are routinely assessed by reverse-transcription quantitative polymerase chain reaction (RT-qPCR) amplification of Sars-CoV-2 virus RNA extracted from oro/nasopharyngeal swabs. Despite the good specificity of the assays certified for SARS-CoV-2 molecular detection, and a theoretical sensitivity of few viral gene copies per reaction, a relatively high rate of false negatives continues to be reported. This is an important challenge in the management of patients on hospital admission and for correct monitoring of the infectivity after the acute phase. In the present report, we show that the use of digital PCR, a high sensitivity method to detect low amplicon numbers, allowed us to correctly detecting infection in swab material in a significant number of false negatives. We show that the implementation of digital PCR methods in the diagnostic assessment of COVID-19 could resolve, at least in part, this timely issue. [ABSTRACT FROM AUTHOR]

Published

2021

27. SCA-1 micro-heterogeneity in the fate decision of dystrophic fibro/adipogenic progenitors.

Author

Giuliani, Giulio, Vumbaca, Simone, Fuoco, Claudia, Gargioli, Cesare, Giorda, Ezio, Massacci, Giorgia, Palma, Alessandro, Reggio, Alessio, Riccio, Federica, Rosina, Marco, Vinci, Maria, Castagnoli, Luisa, and Cesareni, Gianni

Published

2021

28. Different Innate and Adaptive Immune Responses to SARS-CoV-2 Infection of Asymptomatic, Mild, and Severe Cases.

Author

Carsetti, Rita, Zaffina, Salvatore, Piano Mortari, Eva, Terreri, Sara, Corrente, Francesco, Capponi, Claudia, Palomba, Patrizia, Mirabella, Mattia, Cascioli, Simona, Palange, Paolo, Cuccaro, Ilaria, Milito, Cinzia, Zumla, Alimuddin, Maeurer, Markus, Camisa, Vincenzo, Vinci, Maria Rosaria, Santoro, Annapaola, Cimini, Eleonora, Marchioni, Luisa, and Nicastri, Emanuele

Subjects

SARS-CoV-2, IMMUNE response, COVID-19, KILLER cells, ANTIBODY formation

Abstract

SARS-CoV-2 is a novel coronavirus, not encountered before by humans. The wide spectrum of clinical expression of SARS-CoV-2 illness suggests that individual immune responses to SARS-CoV-2 play a crucial role in determining the clinical course after first infection. Immunological studies have focused on patients with moderate to severe disease, demonstrating excessive inflammation in tissues and organ damage. In order to understand the basis of the protective immune response in COVID-19, we performed a longitudinal follow-up, flow-cytometric and serological analysis of innate and adaptive immunity in 64 adults with a spectrum of clinical presentations: 28 healthy SARS-CoV-2-negative contacts of COVID-19 cases; 20 asymptomatic SARS-CoV-2-infected cases; eight patients with Mild COVID-19 disease and eight cases of Severe COVID-19 disease. Our data show that high frequency of NK cells and early and transient increase of specific IgA, IgM and, to a lower extent, IgG are associated with asymptomatic SARS-CoV-2 infection. By contrast, monocyte expansion and high and persistent levels of IgA and IgG, produced relatively late in the course of the infection, characterize severe disease. Modest increase of monocytes and different kinetics of antibodies are detected in mild COVID-19. The importance of innate NK cells and the short-lived antibody response of asymptomatic individuals and patients with mild disease suggest that only severe COVID-19 may result in protective memory established by the adaptive immune response. [ABSTRACT FROM AUTHOR]

Published

2020

29. Migratory flow and hepatitis delta infection in Italy: A new challenge at the beginning of the third millennium.

Author

Stroffolini, Tommaso, Ciancio, Alessia, Furlan, Caterina, Vinci, Maria, Fontana, Rosanna, Russello, Maurizio, Colloredo, Guido, Morisco, Filomena, Coppola, Nicola, Babudieri, Sergio, Ferrigno, Luigina, Sagnelli, Caterina, Sagnelli, Evangelista, Verzon, Giulia, Latanza, Arianna, Picciotto, Viviana, Niro, Grazia Anna, Benigno, Rosa Grazia, Pontillo, Giuseppina, and Messina, Vincenzo

Subjects

MULTIPLE regression analysis, LOGISTIC regression analysis, OLDER people, PROGNOSIS, HEPATITIS

Abstract

In Italy, HDV infection endemicity has greatly decreased overtime. Migratory flow may change this scenario as migrants often come from high HDV endemicity areas. Here, we studied characteristics of HDV infection in Italy, particularly addressed to the birth area of subjects. Chronic HBsAg carriers consecutively referring to 9 units in Italy prospectively enrolled for a six‐month period in 2019 were tested for anti‐HDV by ELISA. Multiple logistic regression analysis was performed to identify anti‐HDV positivity independent predictors. A total of 894 HBsAg‐positive subjects were enrolled. Of them, 786 (87.9%) were tested for anti‐HDV. Anti‐HDV overall prevalence was 9.9% (6.4% in Italian natives and 26.4% in non‐natives; P <.001). HDV‐RNA was checked in 63 (80.8%) of the 78 anti–HDV+ subjects, and 49 (77.8%) tested positive. Compared to non‐natives, Italians were more likely males (male/female 1.6 vs 0.6; P <.05) and older (median age 57 years vs 46 years; P <.05). Multivariate analysis showed that non‐natives (OR = 6.02; CI 95% = 3.06‐11.84) and cirrhosis (OR 9.6; CI 95% = 5.39‐17.30) were independently associated with anti‐HDV positivity. A remarkable changing pattern in some characteristics of anti–HDV‐positive subjects was observed over 1987‐2019: a decreasing male/female ratio, an increasing mean age and proportion of cirrhotic subjects. Anti‐HDV prevalence decreased from 7.4% to 6.4% among Italians, increasing from 12.2% to 26.4% among non‐natives during 2001‐2019. Hence, HDV infection in Italians is further decreasing and mostly affects old people and subjects with advanced disease reflecting a survival effect. Conversely, non‐natives are sixfold more likely anti–HDV‐positive with an increasing trend. Migratory flow may be a new challenge for HDV infection at the beginning of the third millennium. [ABSTRACT FROM AUTHOR]

Published

2020

30. Advanced liver disease outcomes after hepatitis C eradication by human immunodeficiency virus infection in PITER cohort.

Author

Quaranta, Maria Giovanna, Ferrigno, Luigina, Monti, Monica, Filomia, Roberto, Biliotti, Elisa, Iannone, Andrea, Migliorino, Guglielmo, Coco, Barbara, Morisco, Filomena, Vinci, Maria, D'Ambrosio, Roberta, Chemello, Liliana, Massari, Marco, Ieluzzi, Donatella, Russo, Francesco Paolo, Blanc, Pierluigi, Verucchi, Gabriella, Puoti, Massimo, Rumi, Maria Grazia, and Barbaro, Francesco

Abstract

Background: Liver disease progression after Hepatitis C Virus (HCV) eradication following direct-acting antiviral (DAA) treatment in the real-life setting according to Human Immunodeficiency Virus (HIV) coinfection was evaluated. Methods: Patients consecutively enrolled in PITER between April 2014 and June 2019 and with at least 12-weeks follow-up following treatment were analysed. Cox regression analysis were used to evaluate HIV coinfection and factors independently associated with liver disease outcomes following viral eradication in DAA treated patients with pre-treatment liver cirrhosis. Results: 93 HIV/HCV coinfected and 1109 HCV monoinfected patients were evaluated during a median follow-up of 26.7 (range 6–44.6) and 24.6 (range 6.8–47.3) months, respectively. No difference in the cumulative HCC incidence and hepatic decompensation was observed between coinfected and monoinfected patients. Age (Hazard Ratio [HR] = 1.08; 95% CI 1.04–1.13), male sex (HR = 2.76; 95% CI 1.28–5.96), lower albumin levels (HR = 3.94; 95% CI 1.81–8.58), genotype 3 (HR = 5.05; 95% CI 1.75–14.57) and serum anti-HBc positivity (HR = 1.99, 95% CI 1.01–3.95) were independently associated with HCC incidence. Older age (HR = 1.03; 95% CI 1.00–1.07), male sex (HR = 2.13; 95% CI 1.06–4.26) and lower albumin levels (HR = 3.75; 95% CI 1.89–7.46) were independently associated with the appearance of a decompensating event after viral eradication. Conclusion: Different demographic, clinical and genotype distribution between HIV coinfected vs those monoinfected, was observed in a representative cohort of HCV infected patients in Italy. Once liver cirrhosis is established the disease progression is decreased, but still persists regardless of viral eradication in both coinfected and monoinfected patients. In patients with cirrhosis, HIV coinfection was not associated with a higher probability of liver complications, after viral eradication. [ABSTRACT FROM AUTHOR]

Published

2020

31. Abnormal DNA Methylation Induced by Hyperglycemia Reduces CXCR 4 Gene Expression in CD 34+ Stem Cells.

Author

Vigorelli, Vera, Resta, Jessica, Bianchessi, Valentina, Lauri, Andrea, Bassetti, Beatrice, Agrifoglio, Marco, Pesce, Maurizio, Polvani, Gianluca, Bonalumi, Giorgia, Cavallotti, Laura, Alamanni, Francesco, Genovese, Stefano, Pompilio, Giulio, and Vinci, Maria Cristina

Published

2019

32. Direct Involvement of Cranial Nerve V at Diagnosis in Patients With Diffuse Intrinsic Pontine Glioma: A Potential Magnetic Resonance Predictor of Short-Term Survival.

Author

Colafati, Giovanna Stefania, Voicu, Ioan Paul, Carducci, Chiara, Caulo, Massimo, Vinci, Maria, Diomedi-Camassei, Francesca, Merli, Pietro, Carai, Andrea, Miele, Evelina, Cacchione, Antonella, Tomà, Paolo, Locatelli, Franco, and Mastronuzzi, Angela

Subjects

GLIOMA treatment, CRANIAL nerve diseases, MAGNETIC resonance imaging of cancer, TUMOR markers, CANCER patients

Abstract

Background: Diffuse intrinsic pontine glioma (DIPG) has a dismal prognosis. Magnetic resonance imaging (MRI) remains the gold standard for non-invasive DIPG diagnosis. MRI features have been tested as surrogate biomarkers. We investigated the direct involvement of cranial nerve V (CN V) in DIPG at diagnosis and its utility as predictor of poor overall survival. Materials and Methods: We examined MRI scans of 35 consecutive patients with radiological diagnosis of DIPG. Direct involvement of CN V was assessed on the diagnostic scans. Differences in overall survival (OS) and time to progression (TTP) were analyzed for involvement of CN V, sex, age, tumor size, ring enhancement, and treatment regimen. Correlations between involvement of CN V and disease dissemination, magnet strength and slice thickness were analyzed. Statistical analyses included Kaplan-Meier curves, log-rank test and Spearman's Rho. Results: After excluding six long-term survivors, 29 patients were examined (15 M, 14 F). Four patients presented direct involvement of CN V. Histological data were available in 12 patients. Median OS was 11 months (range 3–23 months). Significant differences in OS were found for direct involvement of CN V (median OS: 7 months, 95% CI 1.1–12.9 months for involvement of CN V vs. 13 months, 95% CI 10.2–15.7 for lack of involvement of CN V, respectively, p < 0.049). Significant differences in TTP were found for the two treatment regimens (median TTP: 4 months, 95% CI 2.6–5.3 vs. 7 months, 95% CI 5.9–8.1, respectively, p < 0.027). No significant correlation was found between involvement of CN V and magnet strength or slice thickness (r = −0.201; p = NS). A trend toward positive correlation was found between direct involvement of CN V at diagnosis and dissemination of disease at follow-up (r = 0.347; p < 0.065). Conclusions: In our cohort, direct involvement of CN V correlated with poor prognosis. Based on our data, we suggest that in DIPG direct involvement of CN V should be routinely evaluated on diagnostic scans. [ABSTRACT FROM AUTHOR]

Published

2019

33. Seasonal influenza vaccination and absenteeism in health-care workers in two subsequent influenza seasons (2016/17 and 2017/18) in an Italian pediatric hospital.

Author

Zaffina, Salvatore, Gilardi, Francesco, Rizzo, Caterina, Sannino, Serena, Brugaletta, Rita, Santoro, Annapaola, Castelli Gattinara, Guido, Ciofi degli Atti, Marta Luisa, Raponi, Massimiliano, and Vinci, Maria Rosaria

Abstract

Background: Seasonal influenza in Health-Care Workers (HCWs) is a topic of growing interest in public health for its organizational implications. The study aims at measuring absenteeism due to influenza in HCWs of an Italian pediatric hospital. Research design and methods: A retrospective observational study on absenteeism for influenza and influenza-like illness was carried out on all hospital HCWs. Sickness absences up to 5 days and vaccination status of HCWs were recorded during the last two years (2016/2017, 2017/2018). Average sickness absenteeism rate in vaccinated and unvaccinated HCWs and total working days lost were estimated. Daily mean cost for HCW was calculated in order to define the non-vaccination costs. Results: In this study, the authors analyzed the overlapping between the trend of weekly sickness absenteeism and the morbidity rate associated with influenza epidemics in adults living in the Lazio region, Italy. An excess of 0.38 (p = 0.03) and 0.46 (p = 0.01) of average days lost was recorded in unvaccinated HCWs in the 2016/2017 and 2017/2018 epidemic seasons. The total amount of days lost in unvaccinated HCWs is 1.485,4 with a total cost of € 252.060,54. Conclusions: Seasonal influenza vaccination confirms its key role in preventing outbreaks of influenza and promoting HCWs health. [ABSTRACT FROM AUTHOR]

Published

2019

34. International experience in the development of patient-derived xenograft models of diffuse intrinsic pontine glioma.

Author

Tsoli, Maria, Shen, Han, Mayoh, Chelsea, Franshaw, Laura, Ehteda, Anahid, Upton, Danielle, Carvalho, Diana, Vinci, Maria, Meel, Michael H., van Vuurden, Dannis, Plessier, Alexander, Castel, David, Drissi, Rachid, Farrell, Michael, Cryan, Jane, Crimmins, Darach, Caird, John, Pears, Jane, Francis, Stephanie, and Ludlow, Louise E. A.

Abstract

Purpose: Diffuse intrinsic pontine glioma is the most aggressive form of high grade glioma in children with no effective therapies. There have been no improvements in survival in part due poor understanding of underlying biology, and lack of representative in vitro and in vivo models. Recently, it has been found feasible to use both biopsy and autopsy tumors to generate cultures and xenograft models.Methods: To further model development, we evaluated the collective international experience from 8 collaborating centers to develop DIPG pre-clinical models from patient-derived autopsies and biopsies. Univariate and multivariate analysis was performed to determine key factors associated with the success of in vitro and in vivo PDX development.Results: In vitro cultures were successfully established from 57% of samples (84.2% of biopsies and 38.2% of autopsies). Samples transferred in DMEM media were more likely to establish successful culture than those transported in Hibernate A. In vitro cultures were more successful from biopsies (84.2%) compared with autopsies (38.2%) and as monolayer on laminin-coated plates than as neurospheres. Primary cultures successfully established from autopsy samples were more likely to engraft in animal models than cultures established from biopsies (86.7% vs. 47.4%). Collectively, tumor engraftment was more successful when DIPG samples were directly implanted in mice (68%), rather than after culturing (40.7%).Conclusion: This multi-center study provides valuable information on the success rate of establishing patient-derived pre-clinical models of DIPG. The results can lead to further optimization of DIPG model development and ultimately assist in the investigation of new therapies for this aggressive pediatric brain tumor. [ABSTRACT FROM AUTHOR]

Published

2019

35. Forecasting Hepatitis C liver disease burden on real‐life data. Does the hidden iceberg matter to reach the elimination goals?

Author

Kondili, Loreta A., Quaranta, Maria G., Vella, Stefano, Zuin, Massimo, Chessa, Luchino, Blanc, Pierluigi, Puoti, Massimo, Vinci, Maria, Erne, Elke M., Strazzabosco, Mario, Massari, Marco, Lampertico, Pietro, Rumi, Maria G., Robbins, Sarah, Blach, Sarah, Gamkrelidze, Ivane, Razavi, Homie, Federico, Alessandro, Orlandini, Alessandra, and Ciancio, Alessia

Abstract

Background & Aims: Advances in direct‐acting antiviral treatment of HCV have reinvigorated public health initiatives aimed at identifying affected individuals. We evaluated the possible impact of only diagnosed and linked‐to‐care individuals on overall HCV burden estimates and identified a possible strategy to achieve the WHO targets by 2030. Methods: Using a modelling approach grounded in Italian real‐life data of diagnosed and treated patients, different linkage‐to‐care scenarios were built to evaluate potential strategies in achieving the HCV elimination goals. Results: Under the 40% linked‐to‐care scenario, viraemic burden would decline (60%); however, eligible patients to treat will be depleted by 2025. Increased case finding through a targeted screening strategy in 1948‐1978 birth cohorts could supplement the pool of diagnosed patients by finding 75% of F0‐F3 cases. Under the 60% linked‐to‐care scenario, viraemic infections would decline by 70% by 2030 but the patients eligible for treatment will run out by 2028. If treatment is to be maintained, a screening strategy focusing on 1958‐1978 birth cohorts could capture 55% of F0‐F3 individuals. Under the 80% linked‐to‐care scenario, screening limited in 1968‐1978 birth cohorts could sustain treatment at levels required to achieve the HCV elimination goals. Conclusion: In Italy, which is an HCV endemic country, the eligible pool of patients to treat will run out between 2025 and 2028. To maintain the treatment rate and achieve the HCV elimination goals, increased case finding in targeted, high prevalence groups is required. [ABSTRACT FROM AUTHOR]

Published

2018

36. Near‐infrared photoimmunotherapy targeting EGFR—Shedding new light on glioblastoma treatment.

Author

Burley, Thomas A., Mączyńska, Justyna, Shah, Anant, Szopa, Wojciech, Harrington, Kevin J., Boult, Jessica K. R., Mrozek‐Wilczkiewicz, Anna, Vinci, Maria, Bamber, Jeffrey C., Kaspera, Wojciech, and Kramer‐Marek, Gabriela

Abstract

Glioblastomas (GBMs) are high‐grade brain tumors, differentially driven by alterations (amplification, deletion or missense mutations) in the epidermal growth factor receptor (EGFR), that carry a poor prognosis of just 12–15 months following standard therapy. A combination of interventions targeting tumor‐specific cell surface regulators along with convergent downstream signaling pathways may enhance treatment efficacy. Against this background, we investigated a novel photoimmunotherapy approach combining the cytotoxicity of photodynamic therapy with the specificity of immunotherapy. An EGFR‐specific affibody (ZEGFR:03115) was conjugated to the phthalocyanine dye, IR700DX, which when excited with near‐infrared light produces a cytotoxic response. ZEGFR:03115–IR700DX EGFR‐specific binding was confirmed by flow cytometry and confocal microscopy. The conjugate showed effective targeting of EGFR positive GBM cells in the brain. The therapeutic potential of the conjugate was assessed both in vitro, in GBM cell lines and spheroids by the CellTiter‐Glo® assay, and in vivo using subcutaneous U87‐MGvIII xenografts. In addition, mice were imaged pre‐ and post‐PIT using the IVIS/Spectrum/CT to monitor treatment response. Binding of the conjugate correlated to the level of EGFR expression in GBM cell lines. The cell proliferation assay revealed a receptor‐dependent response between the tested cell lines. Inhibition of EGFRvIII+ve tumor growth was observed following administration of the immunoconjugate and irradiation. Importantly, this response was not seen in control tumors. In conclusion, the ZEGFR:03115–IR700DX showed specific uptake in vitro and enabled imaging of EGFR expression in the orthotopic brain tumor model. Moreover, the proof‐of‐concept in vivo PIT study demonstrated therapeutic efficacy of the conjugate in subcutaneous glioma xenografts. [ABSTRACT FROM AUTHOR]

Published

2018

37. Technological solutions for an innovative fruition the “museo delle terme di diocleziano” project.

Author

Armone, Giulia, De Sanctis, Elisabetta, Esposito, Sara, Ventura, Maximilian, and Vinci, Maria Letizia

Published

2015

38. Disability Management in una struttura sanitaria complessa: attività manageriali del medico competente.

Author

Camisa, Vincenzo, Vinci, Maria Rosaria, Santoro, Annapaola, Guendalina Dalmasso, Bianchi, Natalia, Raponi, Massimiliano, Brugaletta, Rita, Derrico, Pietro, and Zaffina, Salvatore

Published

2016

39. Disability Management: contesto internazionale e nazionale.

Author

Camisa, Vincenzo, Vinci, Maria Rosaria, Santoro, Annapaola, Brugaletta, Rita, Zaffina, Salvatore, and Apostoli, Pietro

Published

2016

40. Feasibility of pig and human-derived aortic valve interstitial cells seeding on fixative-free decellularized animal pericardium.

Author

Santoro, Rosaria, Consolo, Filippo, Spiccia, Marco, Piola, Marco, Kassem, Samer, Prandi, Francesca, Vinci, Maria Cristina, Forti, Elisa, Polvani, Gianluca, Fiore, Gianfranco Beniamino, Soncini, Monica, and Pesce, Maurizio

Abstract

Glutaraldehyde-fixed pericardium of animal origin is the elective material for the fabrication of bio-prosthetic valves for surgical replacement of insufficient/stenotic cardiac valves. However, the pericardial tissue employed to this aim undergoes severe calcification due to chronic inflammation resulting from a non-complete immunological compatibility of the animal-derived pericardial tissue resulting from failure to remove animal-derived xeno-antigens. In the mid/long-term, this leads to structural deterioration, mechanical failure, and prosthesis leaflets rupture, with consequent need for re-intervention. In the search for novel procedures to maximize biological compatibility of the pericardial tissue into immunocompetent background, we have recently devised a procedure to decellularize the human pericardium as an alternative to fixation with aldehydes. In the present contribution, we used this procedure to derive sheets of decellularized pig pericardium. The decellularized tissue was first tested for the presence of 1,3 α-galactose (αGal), one of the main xenoantigens involved in prosthetic valve rejection, as well as for mechanical tensile behavior and distensibility, and finally seeded with pig- and human-derived aortic valve interstitial cells. We demonstrate that the decellularization procedure removed the αGAL antigen, maintained the mechanical characteristics of the native pig pericardium, and ensured an efficient surface colonization of the tissue by animal- and human-derived aortic valve interstitial cells. This establishes, for the first time, the feasibility of fixative-free pericardial tissue seeding with valve competent cells for derivation of tissue engineered heart valve leaflets. © 2015 Wiley Periodicals, Inc. J Biomed Mater Res Part B: Appl Biomater, 104B: 345-356, 2016. [ABSTRACT FROM AUTHOR]

Published

2016

41. Adventitial Vessel Growth and Progenitor Cells Activation in an Ex Vivo Culture System Mimicking Human Saphenous Vein Wall Strain after Coronary Artery Bypass Grafting.

Author

Prandi, Francesca, Piola, Marco, Soncini, Monica, Colussi, Claudia, D’Alessandra, Yuri, Penza, Eleonora, Agrifoglio, Marco, Vinci, Maria Cristina, Polvani, Gianluca, Gaetano, Carlo, Fiore, Gianfranco Beniamino, and Pesce, Maurizio

Subjects

PROGENITOR cells, CORONARY artery bypass, TRANSPLANTATION of organs, tissues, etc., MUSCLE cells, MATRIX metalloproteinases

Abstract

Saphenous vein graft disease is a timely problem in coronary artery bypass grafting. Indeed, after exposure of the vein to arterial blood flow, a progressive modification in the wall begins, due to proliferation of smooth muscle cells in the intima. As a consequence, the graft progressively occludes and this leads to recurrent ischemia. In the present study we employed a novel ex vivo culture system to assess the biological effects of arterial-like pressure on the human saphenous vein structure and physiology, and to compare the results to those achieved in the presence of a constant low pressure and flow mimicking the physiologic vein perfusion. While under both conditions we found an activation of Matrix Metallo-Proteases 2/9 and of microRNAs-21/146a/221, a specific effect of the arterial-like pressure was observed. This consisted in a marked geometrical remodeling, in the suppression of Tissue Inhibitor of Metallo-Protease-1, in the enhanced expression of TGF-β1 and BMP-2 mRNAs and, finally, in the upregulation of microRNAs-138/200b/200c. In addition, the veins exposed to arterial-like pressure showed an increase in the density of the adventitial vasa vasorum and of cells co-expressing NG2, CD44 and SM22α markers in the adventitia. Cells with nuclear expression of Sox-10, a transcription factor characterizing multipotent vascular stem cells, were finally found in adventitial vessels. Our findings suggest, for the first time, a role of arterial-like wall strain in the activation of pro-pathologic pathways resulting in adventitial vessels growth, activation of vasa vasorum cells, and upregulation of specific gene products associated to vascular remodeling and inflammation. [ABSTRACT FROM AUTHOR]

Published

2015

42. Tumor Spheroid-Based Migration Assays for Evaluation of Therapeutic Agents.

Author

Vinci, Maria, Box, Carol, Zimmermann, Miriam, and Eccles, Suzanne A.

Published

2013

43. Quantification of spatial subclonal interactions enhancing the invasive phenotype of pediatric glioma.

Author

Tari, Haider, Kessler, Ketty, Trahearn, Nick, Werner, Benjamin, Vinci, Maria, Jones, Chris, and Sottoriva, Andrea

Abstract

Diffuse midline gliomas (DMGs) are highly aggressive, incurable childhood brain tumors. They present a clinical challenge due to many factors, including heterogeneity and diffuse infiltration, complicating disease management. Recent studies have described the existence of subclonal populations that may co-operate to drive pro-tumorigenic processes such as cellular invasion. However, a precise quantification of subclonal interactions is lacking, a problem that extends to other cancers. In this study, we combine spatial computational modeling of cellular interactions during invasion with co-evolution experiments of clonally disassembled patient-derived DMG cells. We design a Bayesian inference framework to quantify spatial subclonal interactions between molecular and phenotypically distinct lineages with different patterns of invasion. We show how this approach could discriminate genuine interactions, where one clone enhanced the invasive phenotype of another, from those apparently only due to the complex dynamics of spatially restricted growth. This study provides a framework for the quantification of subclonal interactions in DMG. [Display omitted] • Explored the effects of interactions between cancer cells and their ability to spread • Developed a computational and experimental framework to study spatial interactions • Classified and quantified interactions present between two independent patient models • Identified the presence of a commensalism interaction between DIPG subclones Tari et al. explore interactions present between cancer cells and develop a methodology for their identification and quantification. Using a combination of computational modeling and experimental investigations, these interactions are demonstrated in pairs of single-cell-derived subclones isolated from independent patient tumors. [ABSTRACT FROM AUTHOR]

Published

2022

44. Endothelial progenitor cells augment collateralization and hemodynamic rescue in a model of chronic cerebral ischemia.

Author

Hecht, Nils, Schneider, Ulf C, Czabanka, Marcus, Vinci, Maria, Hatzopoulos, Antonis K, Vajkoczy, Peter, and Woitzik, Johannes

Subjects

PROGENITOR cells, HEMODYNAMICS, CEREBRAL ischemia treatment, LABORATORY rats, IMMUNOHISTOCHEMISTRY, CLINICAL trials

Abstract

Surgical flow augmentation for treatment of cerebral hemodynamic impairment remains controversial. Here, we investigated the benefit of endothelial progenitor cell (EPC) treatment in a rat model of chronic cerebral hypoperfusion. At repeated time points after 3-vessel occlusion (3-VO), animals were treated with 1 × 106 DiI-labeled (a) ex vivo-expanded embryonic-EPC (e-EPC), (b) cyclic AMP-differentiated embryonic-endothelial progenitor-derived cells (e-EPDC as biologic control) or, (c) saline. The cerebrovascular reserve capacity (CVRC) was assessed immediately before and on days 7 and 21 after 3-VO. Structural effects were assessed by latex perfusion, immunohistochemistry, and intravital fluorescence video microscopy on day 21. Three-vessel occlusion resulted in a significant impairment of the CVRC with better functional recovery after treatment with e-EPC (16.4±8%) compared with e-EPDC (3.7±8%) or saline (6.4±9%) by day 21 (P<0.05), which was paralleled by a significant increase in the vessel diameters of the anterior Circle of Willis, a significantly higher number of leptomeningeal anastomoses and higher parenchymal capillary density in e-EPC-treated animals. Interestingly, despite in vivo interaction of e-EPC with the cerebral endothelium, e-EPC incorporation into the cerebral vasculature was not observed. Our results suggest that EPC may serve as a novel therapeutic agent in clinical trials for nonsurgical treatment of chronic cerebral hemodynamic impairment. [ABSTRACT FROM AUTHOR]

Published

2014

45. Recurrent activating ACVR1 mutations in diffuse intrinsic pontine glioma.

Author

Taylor, Kathryn R, Mackay, Alan, Truffaux, Nathalène, Butterfield, Yaron S, Morozova, Olena, Philippe, Cathy, Castel, David, Grasso, Catherine S, Vinci, Maria, Carvalho, Diana, Carcaboso, Angel M, de Torres, Carmen, Cruz, Ofelia, Mora, Jaume, Entz-Werle, Natacha, Ingram, Wendy J, Monje, Michelle, Hargrave, Darren, Bullock, Alex N, and Puget, Stéphanie

Subjects

GLIOMAS, SERINE, FIBRODYSPLASIA ossificans progressiva, INCURABLE diseases, NERVOUS system tumors, CLINICAL trials

Abstract

Diffuse intrinsic pontine gliomas (DIPGs) are highly infiltrative malignant glial neoplasms of the ventral pons that, due to their location within the brain, are unsuitable for surgical resection and consequently have a universally dismal clinical outcome. The median survival time is 9-12 months, with neither chemotherapeutic nor targeted agents showing substantial survival benefit in clinical trials in children with these tumors. We report the identification of recurrent activating mutations in the ACVR1 gene, which encodes a type I activin receptor serine/threonine kinase, in 21% of DIPG samples. Strikingly, these somatic mutations (encoding p.Arg206His, p.Arg258Gly, p.Gly328Glu, p.Gly328Val, p.Gly328Trp and p.Gly356Asp substitutions) have not been reported previously in cancer but are identical to mutations found in the germ line of individuals with the congenital childhood developmental disorder fibrodysplasia ossificans progressiva (FOP) and have been shown to constitutively activate the BMP-TGF-β signaling pathway. These mutations represent new targets for therapeutic intervention in this otherwise incurable disease. [ABSTRACT FROM AUTHOR]

Published

2014

46. Hypoxia-resistant profile implies vulnerability of cancer stem cells to physiological agents, which suggests new therapeutic targets.

Author

Cipolleschi, Maria Grazia, Marzi, Ilaria, Santini, Roberta, Fredducci, David, Vinci, Maria Cristina, D'Amico, Massimo, Rovida, Elisabetta, Stivarou, Theodora, Torre, Eugenio, Sbarba, Persio Dello, Stecca, Barbara, and Olivotto, Massimo

Published

2014

47. MENTAL HEALTH DURING AND AFTER THE COVID-19 PANDEMIC AMONG HEALTHCARE WORKERS. PSYCHOLOGICAL PRELIMINARY FINDINGS BY AN ITALIAN OCCUPATIONAL HEALTH SERVICE.

Author

Bondanini, Giorgia, Di Prinzio, Reparata Rosa, De Falco, Federica, Vinci, Maria Rosaria, Camisa, Vincenzo, Santoro, Annapaola, Dalmasso, Guendalina, Santo, Arianna, Ceresi, Bianca, Gnocchi, Francesca, Coscia, Emanuele, and Zaffina, Salvatore

Published

2022

48. Epigenetic Programming and Risk: The Birthplace of Cardiovascular Disease?

Author

Vinci, Maria, Polvani, Gianluca, and Pesce, Maurizio

Subjects

EPIGENETICS, CARDIOVASCULAR diseases risk factors, GENE expression, DNA, CELL differentiation, STEM cells, EMBRYOLOGY, TISSUES

Abstract

Epigenetics, through control of gene expression circuitries, plays important roles in various physiological processes such as stem cell differentiation and self renewal. This occurs during embryonic development, in different tissues, and in response to environmental stimuli. The language of epigenetic program is based on specific covalent modifications of DNA and chromatin. Thus, in addition to the individual identity, encoded by sequence of the four bases of the DNA, there is a cell type identity characterized by its positioning in the epigenetic 'landscape'. Aberrant changes in epigenetic marks induced by environmental cues may contribute to the development of abnormal phenotypes associated with different human diseases such as cancer, neurological disorders and inflammation. Most of the epigenetic studies have focused on embryonic development and cancer biology, while little has been done to explore the role of epigenetic mechanisms in the pathogenesis of cardiovascular disease. This review highlights our current knowledge of epigenetic gene regulation and the evidence that chromatin remodeling and histone modifications play key roles in the pathogenesis of cardiovascular disease through (re)programming of cardiovascular (stem) cells commitment, identity and function. [ABSTRACT FROM AUTHOR]

Published

2013

49. Mechanical Compliance and Immunological Compatibility of Fixative-Free Decellularized/Cryopreserved Human Pericardium

Author

Vinci, Maria Cristina, Tessitore, Giulio, Castiglioni, Laura, Prandi, Francesca, Soncini, Monica, Santoro, Rosaria, Consolo, Filippo, Colazzo, Francesca, Micheli, Barbara, Sironi, Luigi, Polvani, Gianluca, and Pesce, Maurizio

Subjects

PERICARDIUM, BIOCOMPATIBILITY, HEART valves, CARDIAC surgery, ALDEHYDES, CALCIFICATION, THERAPEUTICS

Abstract

Background: The pericardial tissue is commonly used to produce bio-prosthetic cardiac valves and patches in cardiac surgery. The procedures adopted to prepare this tissue consist in treatment with aldehydes, which do not prevent post-graft tissue calcification due to incomplete xeno-antigens removal. The adoption of fixative-free decellularization protocols has been therefore suggested to overcome this limitation. Although promising, the decellularized pericardium has not yet used in clinics, due to the absence of proofs indicating that the decellularization and cryopreservation procedures can effectively preserve the mechanical properties and the immunologic compatibility of the tissue. Principal Findings: The aim of the present work was to validate a procedure to prepare decellularized/cryopreserved human pericardium which may be implemented into cardiovascular homograft tissue Banks. The method employed to decellularize the tissue completely removed the cells without affecting ECM structure; furthermore, uniaxial tensile loading tests revealed an equivalent resistance of the decellularized tissue to strain, before and after the cryopreservation, in comparison with the fresh tissue. Finally, immunological compatibility, showed a minimized host immune cells invasion and low levels of systemic inflammation, as assessed by tissue transplantation into immune-competent mice. Conclusions: Our results indicate, for the first time, that fixative-free decellularized pericardium from cadaveric tissue donors can be banked according to Tissue Repository-approved procedures without compromising its mechanical properties and immunological tolerance. This tissue can be therefore treated as a safe homograft for cardiac surgery. [ABSTRACT FROM AUTHOR]

Published

2013

50. The involvement of a Nanog, Klf4 and c-Myc transcriptional circuitry in the intertwining between neoplastic progression and reprogramming.

Author

Marzi, Ilaria, Cipolleschi, Maria Grazia, D'Amico, Massimo, Stivarou, Theodora, Rovida, Elisabetta, Vinci, Maria Cristina, Pandolfi, Silvia, Sbarba, Persio Dello, Stecca, Barbara, and Olivotto, Massimo

Published

2013