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149 results on '"Bonanni, Alice"'

2. Inflammation and acute cardiotoxicity in adult hematological patients treated with CAR-T cells: results from a pilot proof-of-concept study

Author

Camilli, Massimiliano, Viscovo, Marcello, Felici, Tamara, Maggio, Luca, Ballacci, Federico, Carella, Giacomo, Bonanni, Alice, Lamendola, Priscilla, Tinti, Lorenzo, Di Renzo, Antonio, Coarelli, Giulia, Galli, Eugenio, Liuzzo, Giovanna, Burzotta, Francesco, Montone, Rocco Antonio, Sorà, Federica, Sica, Simona, Hohaus, Stefan, Lanza, Gaetano Antonio, Crea, Filippo, Lombardo, Antonella, and Minotti, Giorgio

Published
2024
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4. Microbial signature of plaque and gut in acute coronary syndrome

Author

Pisano, Eugenia, Bugli, Francesca, Severino, Anna, Pedicino, Daniela, Paroni Sterbini, Francesco, Martini, Cecilia, De Maio, Flavio, Vinci, Ramona, Sacconi, Andrea, Canonico, Francesco, D’Aiello, Alessia, Bonanni, Alice, Proto, Luca, Ciampi, Pellegrino, Ponzo, Myriana, Grimaldi, Maria Chiara, Urbani, Andrea, Primiano, Aniello, Gervasoni, Jacopo, Montone, Rocco, Crea, Filippo, Sanguinetti, Maurizio, and Liuzzo, Giovanna

Published
2023
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7. Early improvement of strain imaging parameters predicts long-term response to sacubitril/valsartan in patients with heart failure with reduced ejection fraction: An observational prospective study

Author

Camilli, Massimiliano, Iannaccone, Giulia, Russo, Michele, Meucci, Maria Chiara, Chiorazzo, Gisberta, Natali, Rosaria, Mango, Federica, Bonanni, Alice, Montone, Rocco Antonio, Graziani, Francesca, Locorotondo, Gabriella, Massetti, Massimo, Lanza, Gaetano Antonio, Aspromonte, Nadia, Crea, Filippo, and Lombardo, Antonella

Published
2023
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9. Coronary artery plaque rupture and erosion: Role of wall shear stress profiling and biological patterns in acute coronary syndromes

Author

Russo, Giulio, Pedicino, Daniela, Chiastra, Claudio, Vinci, Ramona, Lodi Rizzini, Maurizio, Genuardi, Lorenzo, Sarraf, Mohammad, d'Aiello, Alessia, Bologna, Marco, Aurigemma, Cristina, Bonanni, Alice, Bellantoni, Antonio, D'Ascenzo, Fabrizio, Ciampi, Pellegrino, Zambrano, Aniello, Mainardi, Luca, Ponzo, Myriana, Severino, Anna, Trani, Carlo, Massetti, Massimo, Gallo, Diego, Migliavacca, Francesco, Maisano, Francesco, Lerman, Amir, Morbiducci, Umberto, Burzotta, Francesco, Crea, Filippo, and Liuzzo, Giovanna

Published
2023
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12. Exposome in ischaemic heart disease: beyond traditional risk factors.

Author

Montone, Rocco A, Camilli, Massimiliano, Calvieri, Camilla, Magnani, Giulia, Bonanni, Alice, Bhatt, Deepak L, Rajagopalan, Sanjay, Crea, Filippo, and Niccoli, Giampaolo

Subjects
CARDIOVASCULAR diseases, HEART diseases, EMERGING infectious diseases, ENVIRONMENTAL exposure, POLLUTANTS, CARDIOVASCULAR diseases risk factors, PSYCHOLOGICAL factors
Abstract

Ischaemic heart disease represents the leading cause of morbidity and mortality, typically induced by the detrimental effects of risk factors on the cardiovascular system. Although preventive interventions tackling conventional risk factors have helped to reduce the incidence of ischaemic heart disease, it remains a major cause of death worldwide. Thus, attention is now shifting to non-traditional risk factors in the built, natural, and social environments that collectively contribute substantially to the disease burden and perpetuate residual risk. Of importance, these complex factors interact non-linearly and in unpredictable ways to often enhance the detrimental effects attributable to a single or collection of these factors. For this reason, a new paradigm called the 'exposome' has recently been introduced by epidemiologists in order to define the totality of exposure to these new risk factors. The purpose of this review is to outline how these emerging risk factors may interact and contribute to the occurrence of ischaemic heart disease, with a particular attention on the impact of long-term exposure to different environmental pollutants, socioeconomic and psychological factors, along with infectious diseases such as influenza and COVID-19. Moreover, potential mitigation strategies for both individuals and communities will be discussed. [ABSTRACT FROM AUTHOR]

Published
2024
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15. GLUT-1/PKM2 loop dysregulation in patients with non-ST-segment elevation myocardial infarction promotes metainflammation.

Author

Canonico, Francesco, Pedicino, Daniela, Severino, Anna, Vinci, Ramona, Flego, Davide, Pisano, Eugenia, d'Aiello, Alessia, Ciampi, Pellegrino, Ponzo, Myriana, Bonanni, Alice, Ciutiis, Astrid De, Russo, Sara, Sario, Marianna Di, Angelini, Giulia, Szczepaniak, Piotr, Baldi, Alfonso, Kapelak, Boguslaw, Wierzbicki, Karol, Montone, Rocco A, and D'Amario, Domenico

Subjects
MYOCARDIAL infarction, PYRUVATES, GLUCOSE transporters, PYRUVATE kinase, NON-ST elevated myocardial infarction, T cells, REGULATOR genes
Abstract

Aims The functional capacity of the immune cells is strongly dependent on their metabolic state and inflammatory responses are characterized by a greater use of glucose in immune cells. This study is aimed to establish the role of glucose metabolism and its players [glucose transporter 1 (GLUT-1) and pyruvate kinase isozyme M2 (PKM2)] in the dysregulation of adaptive immunity and inflammation observed in patients with non-ST-segment elevation myocardial infarction (NSTEMI). Methods and results We enrolled 248 patients allocated to three groups: NSTEMI patients, chronic coronary syndromes (CCS) patients, healthy subjects (HSs). NSTEMI patients showed higher expression of GLUT-1 and an enhanced glucose uptake in T cells when compared with CCS patients (P < 0.0001; P = 0.0101, respectively) and HSs (P = 0.0071; P = 0.0122, respectively). PKM2 had a prevalent nuclear localization in T lymphocytes in NSTEMI (P = 0.0005 for nuclear vs. cytoplasm localization), while in CCS and HS, it was equally distributed in both compartments. In addition, the nuclear fraction of PKM2 was significantly higher in NSTEMI compared with HS (P = 0.0023). In NSTEMI patients, treatment with Shikonin and Fasentin, which inhibits PKM2 enzyme activity and GLUT-1-mediated glucose internalization, respectively, led to a significant reduction in GLUT-1 expression along with the down-regulation of pro-inflammatory cytokine expression. Conclusion NSTEMI patients exhibit dysregulation of the GLUT-1/PKM2 metabolic loop characterized by nuclear translocation of PKM2, where it acts as a transcription regulator of pro-inflammatory genes. This detrimental loop might represent a new therapeutic target for personalized medicine. [ABSTRACT FROM AUTHOR]

Published
2023
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16. Targeting Collagen Pathways as an HFpEF Therapeutic Strategy.

Author

Bonanni, Alice, Vinci, Ramona, d'Aiello, Alessia, Grimaldi, Maria Chiara, Di Sario, Marianna, Tarquini, Dalila, Proto, Luca, Severino, Anna, Pedicino, Daniela, and Liuzzo, Giovanna

Subjects
*HEART failure, *ADVANCED glycation end-products, *TRANSFORMING growth factors, *COLLAGEN, *HEART fibrosis, *GLUCOSE transporters
Abstract

Heart failure with preserved ejection fraction (HFpEF) is a complex and heterogeneous clinical syndrome. The prevalence is expected to increase in the coming years, resulting in heart failure with reduced ejection fraction (HFrEF). This condition poses a burden to the global health care system as the number of patients affected by this condition is constantly increasing due to a rising average lifespan. The absence of validated drugs effective in reducing hospitalization rates and mortality may reflect the impossibility of applying a one size fits all approach as in HFrEF, heading for a personalized approach. Available evidence demonstrated the link between collagen quantity and quality alterations, and cardiac remodeling. In the context of fibrosis, collagen cross-linking is strictly involved, displaying two types of mechanisms: enzymatic and non-enzymatic. In the murine model, enzymatic inhibition of fibrosis-inducing protease-activated receptor-1 (PAR1) and transforming growth factor (TGF)-β signaling appeared to reduce cardiac fibrosis. On the other hand, in the case of non-enzymatic cross-linking, sodium glucose co-transporter type 2 inhibitors (SGLT2is), appeared to counteract the deposition of advanced glycation end-products (AGEs), which in turn contributed to ventricular remodeling. In this review, we address the mechanisms associated with collagen alterations to identify potential targets of cardiac fibrosis in HFpEF patients. [ABSTRACT FROM AUTHOR]

Published
2023
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17. Ofatumumab in two pediatric nephrotic syndrome patients allergic to rituximab

Author

Vivarelli, Marina, Colucci, Manuela, Bonanni, Alice, Verzani, Martina, Serafinelli, Jessica, Emma, Francesco, and Ghiggeri, Gianmarco

Subjects
Nephrotic syndrome -- Drug therapy -- Research, Rituximab -- Dosage and administration -- Complications and side effects, Ofatumumab -- Dosage and administration -- Complications and side effects, Health
Abstract

Background Rituximab, a chimeric anti-CD20 monoclonal antibody, is an effective treatment in steroid-dependent nephrotic syndrome (SDNS). However, some patients develop adverse reactions. Case-Diagnosis/Treatment Patient 1, a 14-year-old boy with SDNS since the age of 2, was treated with oral prednisone, cyclosporine A (CsA) and mycophenolate mofetil. A first infusion of rituximab at age 12 years was well tolerated, but this was followed by a prolonged relapse unresponsive to oral prednisone, mycophenolate mofetil and CsA. A second rituximab infusion was attempted, but treatment was interrupted due to severe dyspnea. Treatment with a humanized anti-CD20 monoclonal antibody, ofatumumab, was then attempted. The patient experienced a mild allergic reaction and maintained remission despite interruption of all treatment at >12 months of follow-up. Patient 2, a 3-year-old boy who presented at 18 months with nephrotic syndrome initially resistant to treatment with oral prednisone, was given with three intravenous boluses of methylprednisolone followed by CsA and achieved remission. Upon steroid discontinuation, the NS relapsed. Prednisone was restarted and treatment with a single dose of rituximab was never completed due to a severe allergic reaction. Ofatumumab infusion was uneventful, and he maintained remission during the follow-up period (>12 months) despite interruption of prednisone therapy. B cells reappeared at 7 months in both patients. Conclusions Ofatumumab may be a therapeutic option in severe forms of NS with allergy to rituximab., Author(s): Marina Vivarelli[sup.1] , Manuela Colucci[sup.1] , Alice Bonanni[sup.2] , Martina Verzani[sup.1] , Jessica Serafinelli[sup.1] , Francesco Emma[sup.1] , Gianmarco Ghiggeri[sup.2] Author Affiliations: (1) Division of Nephrology and Dialysis, IRCCS-Bambino [...]

Published
2017
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18. MINOCA Associated with a Myocardial Bridge: Pathogenesis, Diagnosis and Treatment.

Author

Rinaldi, Riccardo, Princi, Giuseppe, La Vecchia, Giulia, Bonanni, Alice, Chiariello, Giovanni Alfonso, Candreva, Alessandro, Gragnano, Felice, Calabrò, Paolo, Crea, Filippo, and Montone, Rocco A.

Subjects
SPONTANEOUS coronary artery dissection, ATHEROSCLEROTIC plaque, DIAGNOSIS, CORONARY arteries, CORONARY angiography, MYOCARDIAL ischemia
Abstract

Myocardial bridging (MB) is the most frequent congenital coronary anomaly characterized by a segment of an epicardial coronary artery that passes through the myocardium. MB is an important cause of myocardial ischemia and is also emerging as a possible cause of myocardial infarction with non-obstructed coronary arteries (MINOCA). There are multiple mechanisms underlying MINOCA in patients with MB (i.e., MB-mediated increased risk of epicardial or microvascular coronary spasm, atherosclerotic plaque disruption and spontaneous coronary artery dissection). The identification of the exact pathogenetic mechanism is crucial in order to establish a patient-tailored therapy. This review provides the most up-to-date evidence regarding the pathophysiology of MINOCA in patients with MB. Moreover, it focuses on the available diagnostic tools that could be implemented at the time of coronary angiography to achieve a pathophysiologic diagnosis. Finally, it focuses on the therapeutic implications associated with the different pathogenetic mechanisms of MINOCA in patients with MB. [ABSTRACT FROM AUTHOR]

Published
2023
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20. Meta-Inflammation and New Anti-Diabetic Drugs: A New Chance to Knock Down Residual Cardiovascular Risk.

Author

d'Aiello, Alessia, Bonanni, Alice, Vinci, Ramona, Pedicino, Daniela, Severino, Anna, De Vita, Antonio, Filomia, Simone, Brecciaroli, Mattia, and Liuzzo, Giovanna

Subjects
*EXENATIDE, *SODIUM-glucose cotransporter 2 inhibitors, *EMPAGLIFLOZIN, *TYPE 2 diabetes, *CARDIOVASCULAR diseases risk factors, *GLUCAGON-like peptide 1, *MAJOR adverse cardiovascular events
Abstract

Type 2 diabetes mellitus (DM) represents, with its macro and microvascular complications, one of the most critical healthcare issues for the next decades. Remarkably, in the context of regulatory approval trials, sodium-glucose cotransporter 2 inhibitors (SGLT2i) and glucagon-like peptide 1 receptor agonists (GLP-1 RAs) proved a reduced incidence of major adverse cardiovascular events (MACEs), i.e., cardiovascular death and heart failure (HF) hospitalizations. The cardioprotective abilities of these new anti-diabetic drugs seem to run beyond mere glycemic control, and a growing body of evidence disclosed a wide range of pleiotropic effects. The connection between diabetes and meta-inflammation seems to be the key to understanding how to knock down residual cardiovascular risk, especially in this high-risk population. The aim of this review is to explore the link between meta-inflammation and diabetes, the role of newer glucose-lowering medications in this field, and the possible connection with their unexpected cardiovascular benefits. [ABSTRACT FROM AUTHOR]

Published
2023
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25. Air pollution and plaque healing in acute coronary syndromes.

Author

Russo, Michele, Rinaldi, Riccardo, Camilli, Massimiliano, Bonanni, Alice, Caffè, Andrea, Basile, Mattia, Salzillo, Carmine, Colucci, Michele, Torre, Ilaria, Sanna, Tommaso, Liuzzo, Giovanna, Burzotta, Francesco, Trani, Carlo, Niccoli, Giampaolo, Crea, Filippo, and Montone, Rocco A

Subjects
ACUTE coronary syndrome, AIR pollution, ENDOTHELIUM diseases, ATHEROSCLEROTIC plaque, AIR quality monitoring stations, HEALING
Abstract

Keywords: Air pollution; Plaque healing; Acute coronary syndromes; Thrombosis; Inflammation EN Air pollution Plaque healing Acute coronary syndromes Thrombosis Inflammation 2403 2405 3 07/11/23 20230707 NES 230707 Introduction Plaque healing plays a key role in coronary atherosclerosis[1] and represents "the second hit" required to cause an acute coronary syndrome (ACS) after plaque destabilization, this latter being the "first hit".[[1], [3]] Moreover, an impaired plaque healing has been found in patients with recurrent ACS, suggesting its importance in preventing repeated symptomatic coronary thrombosis.[3] Nonetheless, mechanisms modulating plaque healing are unknown. In first acute coronary syndrome patients, particulate matter 2.5 chronic exposure levels were similar between patients with and without healed plaques in the culprit lesion, while particulate matter 2.5 was higher in those with macrophage infiltration and thin-cap fibroatheroma at the culprit plaque. Among recurrent ACS patients, 6 patients (20.7%) had TCFA at the culprit lesion, and these patients had higher PM2.5 (17.9 ± 3.6 vs. 13.6 ± 3.4 I µ i g/m SP 3 sp , I P i = 0.030) and PM10 (28.8 ± 3.2 vs. 24.2 ± 3.9 I µ i g/m SP 3 sp , I P i = 0.014) exposure levels compared to those without TCFA. [Extracted from the article]

Published
2023
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26. Myocardial Injury Portends a Higher Risk of Mortality and Long-Term Cardiovascular Sequelae after Hospital Discharge in COVID-19 Survivors.

Author

Rinaldi, Riccardo, Basile, Mattia, Salzillo, Carmine, Grieco, Domenico Luca, Caffè, Andrea, Masciocchi, Carlotta, Lilli, Livia, Damiani, Andrea, La Vecchia, Giulia, Iannaccone, Giulia, Bonanni, Alice, De Pascale, Gennaro, Murri, Rita, Fantoni, Massimo, Liuzzo, Giovanna, Sanna, Tommaso, Massetti, Massimo, Gasbarrini, Antonio, Valentini, Vincenzo, and Antonelli, Massimo

Subjects
HEART failure, MYOCARDIAL injury, HOSPITAL admission & discharge, DISEASE complications, COVID-19, TRANSIENT ischemic attack
Abstract

Background: Cardiovascular sequelae after COVID-19 are frequent. However, the predictors for their occurrence are still unknown. In this study, we aimed to assess whether myocardial injury during COVID-19 hospitalization is associated to CV sequelae and death after hospital discharge. Methods: In this prospective observational study, consecutive patients who were admitted for COVID-19 in a metropolitan COVID-19 hub in Italy, between March 2021 and January 2022, with a ≥ 1 assessment of high sensitivity cardiac troponin I (hs-cTnI) were included in the study, if they were alive at hospital discharge. Myocardial injury was defined as elevation hs-cTnI > 99th percentile of the upper reference limit. The incidence of all-cause mortality and major adverse cardiovascular and cerebrovascular events (MACCE, including cardiovascular death, admission for acute or chronic coronary syndrome, hospitalization for heart failure, and stroke/transient ischemic attack) at follow-up were the primary outcomes. Arrhythmias, inflammatory heart diseases, and/or thrombotic disorders were analyzed as well. Results: Among the 701 COVID-19 survivors (mean age 66.4 ± 14.4 years, 40.2% female), myocardial injury occurred in 75 (10.7%) patients. At a median follow-up of 270 days (IQR 165, 380), all-cause mortality (21.3% vs. 6.1%, p < 0.001), MACCE (25.3% vs. 4.5%, p < 0.001), arrhythmias (9.3% vs. 5.0%, p = 0.034), and inflammatory heart disease (8.0% vs. 1.1%, p < 0.001) were more frequent in patients with myocardial injury compared to those without. At multivariate analysis, myocardial injury (HR 1.95 [95% CI:1.05–3.61]), age (HR 1.09 [95% CI:1.06–1.12]), and chronic kidney disease (HR 2.63 [95% CI:1.33–5.21]) were independent predictors of death. Myocardial injury (HR 3.92 [95% CI:2.07–7.42]), age (HR 1.05 [95% CI:1.02–1.08]), and diabetes (HR 2.35 [95% CI:1.25–4.43]) were independent predictors of MACCE. Conclusion: In COVID-19 survivors, myocardial injury during the hospital stay portends a higher risk of mortality and cardiovascular sequelae and could be considered for the risk stratification of COVID-19 sequelae in patients who are successfully discharged. [ABSTRACT FROM AUTHOR]

Published
2022
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27. Molecular Hallmarks of Ischemia with Non-Obstructive Coronary Arteries: The "INOCA versus Obstructive CCS" Challenge.

Author

Bonanni, Alice, d'Aiello, Alessia, Pedicino, Daniela, Di Sario, Marianna, Vinci, Ramona, Ponzo, Myriana, Ciampi, Pellegrino, Lo Curto, Denise, Conte, Cristina, Cribari, Francesco, Canonico, Francesco, Russo, Giulio, Montone, Rocco Antonio, Trani, Carlo, Severino, Anna, Crea, Filippo, and Liuzzo, Giovanna

Subjects
*CORONARY arteries, *CELL adhesion molecules, *VASCULAR endothelial growth factors, *MONONUCLEAR leukocytes, *TUMOR necrosis factors
Abstract

Up to 4 million patients with signs of myocardial ischemia have no obstructive coronary artery disease (CAD). The absence of precise guidelines for diagnosis and treatment in non-obstructive CAD encourages the scientific community to fill the gap knowledge, to provide non-invasive and less expensive diagnostic tools. The aim of our study was to explore the biological profile of Ischemia with Non-Obstructive Coronary Arteries (INOCA) patients with microvascular dysfunction compared to patients presenting with obstructive chronic coronary syndrome (ObCCS) in order to find specific hallmarks of each clinical condition. We performed a gene expression array from peripheral blood mononuclear cells (PBMCs) isolated from INOCA (n = 18) and ObCCS (n = 20) patients. Our results showed a significantly reduced gene expression of molecules involved in cell adhesion, signaling, vascular motion, and inflammation in INOCA as compared to the ObCCS group. In detail, we found lower expression of Platelet and Endothelial Cell Adhesion Molecule 1 (CD31, p < 0.0001), Intercellular Adhesion Molecule-1 (ICAM1, p = 0.0004), Tumor Necrosis Factor (TNF p = 0.0003), Transferrin Receptor (TFRC, p = 0.002), and Vascular Endothelial Growth Factor A (VEGFA, p = 0.0006) in the INOCA group compared with ObCCS. Meanwhile, we observed an increased expression of Hyaluronidase (HYAL2, p < 0.0001) in INOCA patients in comparison to ObCCS. The distinct expression of molecular biomarkers might allow an early and non-invasive differential diagnosis between ObCCS and INOCA, improving clinical management and treatment options, in the era of personalized medicine. [ABSTRACT FROM AUTHOR]

Published
2022
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29. Platelet hyaluronidase 2 enrichment in acute coronary syndromes: a conceivable role in monocyte-platelet aggregate formation.

Author

Vinci, Ramona, Pedicino, Daniela, D'Aiello, Alessia, Ciampi, Pellegrino, Ponzo, Myriana, Bonanni, Alice, Russo, Giulio, Montone, Rocco Antonio, Massetti, Massimo, Crea, Filippo, and Liuzzo, Giovanna

Subjects
ACUTE coronary syndrome, HYALURONIDASES, BLOOD platelets, OPTICAL coherence tomography, EXTRACELLULAR matrix, MONOCYTES
Abstract

Acute Coronary Syndromes (ACS) with plaque erosion display dysregulated hyaluronan metabolism, with increased hyaluronidase-2 (HYAL2) expression. However, the expression and the role of this enzyme on platelets has never been explored. We evaluated the platelet's HYAL2 (pltHYAL2) levels on I) stable angina (SA) and II) ACS patients, furtherly sub-grouped in Intact-Fibrous-Cap (IFC) and Ruptured-Fibrous-Cap (RFC), according to Optical Coherence Tomography. We assessed the HYAL2 role through an in vitro model setting of co-cultured monocytes and platelets, before and after treatment with low-molecular-weight hyaluronic acid (HA) as pro-inflammatory stimulus and with or without HYAL2-antibody to inhibit HYAL2 activity. ACS patients exhibit higher pltHYAL2 levels comparing to SA, with the higher expression for IFC group. The addition of HYAL2-antibody significantly reduced the percentage of monocyte-platelet binding, suggesting that pltHYAL2 enrichment at the site of the culprit lesion is a key mediator in the systemic thrombo-inflammatory status of ACS presenting with plaque erosion. Representation of platelet Hyaluronidase 2 involvement in monocyte-platelet aggregates and pathogenesis of plaque erosion. (Ab, antibody; ECM, extracellular matrix; EC, endothelial cells, HYAL2, hyaluronidase 2; LMW-HA, low molecular weight-hyaluronan) [ABSTRACT FROM AUTHOR]

Published
2021
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31. Neutrophil Extracellular Traps Profiles in Patients with Incident Systemic Lupus Erythematosus and Lupus Nephritis.

Author

Bruschi, Maurizio, Bonanni, Alice, Petretto, Andrea, Vaglio, Augusto, Pratesi, Federico, Santucci, Laura, Migliorini, Paola, Bertelli, Roberta, Galetti, Maricla, Belletti, Silvana, Cavagna, Lorenzo, Moroni, Gabriella, Franceschini, Franco, Fredi, Micaela, Pazzola, Giulia, Allegri, Landino, Sinico, Renato Alberto, Pesce, Giampaola, Bagnasco, Marcello, and Manfredi, Angelo

Published
2020
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32. Adverse events linked with the use of chimeric and humanized anti‐CD20 antibodies in children with idiopathic nephrotic syndrome.

Author

Bonanni, Alice, Calatroni, Marta, D'Alessandro, Matteo, Signa, Sara, Bertelli, Enrica, Cioni, Michela, Di Marco, Eddi, Biassoni, Roberto, Caridi, Gianluca, Ingrasciotta, Giulia, Bertelli, Roberta, Di Donato, Armando, Bruschi, Maurizio, Canepa, Alberto, Piaggio, Giorgio, Ravani, Pietro, and Ghiggeri, Gian Marco

Subjects
*CHIMERIC proteins, *IMMUNOGLOBULINS, *NEPHROTIC syndrome, *JUVENILE diseases, *CALCINEURIN
Abstract

Aims: Anti‐CD20 antibodies are increasingly being used to treat idiopathic nephrotic syndrome (INS) in children. While they may allow steroid and calcineurin inhibitor withdrawal, repeated infusions of anti‐CD20 antibodies are often required to maintain remission. Data on their potential toxicity in INS are needed, to consider repeated infusions. Methods: We investigated the side effects associated with the use of rituximab (a chimeric antibody; 130 patients) and ofatumumab (a humanized antibody; 37 patients) in children with INS (steroid‐dependent and steroid/calcineurin inhibitor‐dependent disease) treated at a national referral centre over a 9‐year period (400 treatments; follow‐up 1–9 years). Results: Infusion reactions were mainly absent in children with steroid‐dependent disease. Rash, dyspnoea, fever, cough and itchy throat (5% and 18% following rituximab and ofatumumab infusion, respectively) were resolved by using premedication with salbutamol. Other short‐term reactions (up to 3 months), including arthritis (2%) and lung injury (1%), were more common with rituximab. Infections were observed 3–9 months following infusion, were similarly common in the two groups and resolved with targeted therapies [antibiotic, fluconazole, immunoglobulins (Igs), etc.]. The number of circulating CD19/20 cells fell to 0 at month 1 and were reconstituted at month 3; circulating IgG antibodies remained within the normal range for 1 year. Tetanus and hepatitis B virus immunization was not modified by either treatment; Epstein–Barr virus and John Cunningham virus activation markers were occasionally observed. Conclusion: Overall, the toxicity of anti‐CD20 monoclonal antibodies was limited to post‐infusion side effects in children with more complex disease. The relatively safe profile of anti‐CD20 antibodies supports their use as steroid‐sparing agents in children with INS. [ABSTRACT FROM AUTHOR]

Published
2018
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33. Remote ischaemic preconditioning for renal and cardiac protection in adult patients undergoing cardiac surgery with cardiopulmonary bypass: systematic review and meta-analysis of randomized controlled trials.

Author

Deferrari, Giacomo, Bonanni, Alice, Bruschi, Maurizio, Alicino, Cristiano, and Signori, Alessio

Subjects
*ISCHEMIC preconditioning, *KIDNEY disease prevention, *PREVENTION of heart diseases, *CARDIOPULMONARY bypass, CARDIAC surgery patients
Abstract

Background. The main aim of this systematic review was to assess whether remote ischaemic preconditioning (RIPC) protects kidneys and the heart in cardiac surgery with cardiopulmonary bypass (CPB) and to investigate a possible role of anaesthetic agents. Methods. Randomized clinical trials (RCTs) on the effects of RIPC through limb ischaemia in adult patients undergoing cardiac surgery with CPB were searched (1965-October 2016) in PubMed, Cochrane Library and article reference lists. A random effects model on standardized mean difference (SMD) for continuous outcomes and the Peto odds ratio (OR) for dichotomous outcomes were used to meta-analyse data. Subgroup analyses to evaluate the effects of different anaesthetic regimens were pre-planned. Results. Thirty-three RCTs (5999 participants) were included. In the whole group, RIPC did not significantly reduce the incidence of acute kidney injury (AKI), acute myocardial infarction, atrial fibrillation, mortality or length of intensive care unit (ICU) and hospital stays. On the contrary, RIPC significantly reduced the area under the curve for myocardial injury biomarkers (MIBs) {SMD -0.37 [95% confidence interval (CI) -0.53 to - 0.21]} and the composite endpoint incidence [OR 0.85 (95% CI 0.74-0.97)]. In the volatile anaesthetic group, RIPC significantly reduced AKI incidence [OR 0.57 (95% CI 0.41-0.79)] and marginally reduced ICU stay. Conversely, except for MIBs, RIPC had fewer non-significant effects under propofol with or without volatile anaesthetics. Conclusions. RIPC did not consistently reduce morbidity and mortality in adults undergoing cardiac surgery with CPB. In the subgroup on volatile anaesthetics only, RIPC markedly and significantly reduced the incidence of AKI and composite end-point as well as myocardial injury. [ABSTRACT FROM AUTHOR]

Published
2018
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34. ANCA-associated vasculitis in childhood: recent advances.

Author

Calatroni, Marta, Oliva, Elena, Gianfreda, Davide, Gregorini, Gina, Allinovi, Marco, Ramirez, Giuseppe A., Bozzolo, Enrica P., Monti, Sara, Bracaglia, Claudia, Marucci, Giulia, Bodria, Monica, Sinico, Renato A., Pieruzzi, Federico, Moroni, Gabriella, Pastore, Serena, Emmi, Giacomo, Esposito, Pasquale, Catanoso, Mariagrazia, Barbano, Giancarlo, and Bonanni, Alice

Subjects
VASCULITIS treatment, CHURG-Strauss syndrome, CHILDREN
Abstract

Anti-neutrophil cytoplasmic antibody (ANCA)-associated vasculitides are rare systemic diseases that usually occur in adulthood. They comprise granulomatosis with polyangiitis (GPA, Wegener's), microscopic polyangiitis (MPA) and eosinophilic granulomatosis with polyangiitis (EGPA, Churg-Strauss syndrome). Their clinical presentation is often heterogeneous, with frequent involvement of the respiratory tract, the kidney, the skin and the joints. ANCA-associated vasculitis is rare in childhood but North-American and European cohort studies performed during the last decade have clarified their phenotype, patterns of renal involvement and their prognostic implications, and outcome. Herein, we review the main clinical and therapeutic aspects of childhood-onset ANCA-associated vasculitis, and provide preliminary data on demographic characteristics and organ manifestations of an Italian multicentre cohort. [ABSTRACT FROM AUTHOR]

Published
2017
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35. Randomised controlled trial comparing ofatumumab to rituximab in children with steroid-dependent and calcineurin inhibitor-dependent idiopathic nephrotic syndrome: study protocol.

Author

Ravani, Pietro, Bonanni, Alice, and Ghiggeri, Gian Marco

Abstract

Introduction: Oral steroids induce remission in about 90% of children with idiopathic nephrotic syndrome (INS), which is characterised by severe proteinuria and hypoalbuminaemia. Some children become steroiddependent (SD) and require addition of calcineurin inhibitors (CNI) to maintain remission. Since these oral agents are toxic, alternative interventions are needed for long-term treatment. The anti-CD20 antibody rituximab has shown promising steroid-sparing properties in clinical trials, but benefits are less convincing in complicated forms of SD-INS. Ofatumumab, a new anti-CD20 antibody with stronger affinity to CD20, may be superior to rituximab in maintaining oral steroid-free and CNI-free disease remission in children with SD-INS. Methods and analysis: This open-label, twoparallel- arm, controlled, phase II randomised clinical trial will enrol children with SD-INS maintained in remission with oral steroids and CNI. Children will be randomised to either ofatumumab or rituximab infusion. After infusion of either antibody, steroids will be maintained for 30 days and then tapered off by 0.3 mg/kg/week until complete withdrawal. 1 week after complete steroid withdrawal, CNI will be decreased by 50% and withdrawn within 2 additional weeks. We will enrol 140 children to detect as significant at the 2-sided p value of 0.01 with a power of >0.8, a reduction in the risk of 1-year relapse (primary end point) of at least 0.3 (ie, from 0.65 to 0.35; (risk ratio 0.54)) in the ofatumumab arm when compared with the rituximab arm. We will compare the amount of steroids required to maintain complete disease remission at 6 and 24 months, relapse-free period, relapse rate per year as secondary end points. Circulating cell populations will be studied as biomarkers or predictors of the anti- CD20 response. Ethics and dissemination: The trial received ethics approval from the local ethics board. We will publish study results and present them at international scientific meetings. [ABSTRACT FROM AUTHOR]

Published
2017
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36. Interorgan handling of fibroblast growth factor-23 in humans.

Author

Verzola, Daniela, Ansaldo, Francesca, Milanesi, Samantha, Parodi, Emanuele Luigi, Rosa, Gian Marco, Sofia, Antonella, Bonanni, Alice, Viazzi, Francesca, Balbi, Manrico, and Garibotto, Giacomo

Subjects
FIBROBLAST growth factors, KIDNEY diseases, SPLANCHNIC nerves
Abstract

Fibroblast growth factor-23 (FGF-23) accumulates in blood of patients with chronic kidney disease (CKD) and is associated both with cardiovascular complications and disease progression. However, our knowledge of the sites and mechanisms that regulate plasma FGF-23 is still incomplete. We measured plasma intact FGF-23 across the kidney, splanchnic organs, and lung in 11 patients [estimated glomerular filtration rate (eGFR) 60 ± 6 ml/min] during elective diagnostic cardiac catheterizations. In these patients FGF-23 was removed by the kidney, with a fractional extraction (FE) of ∼22%. The FE of FGF-23 across the kidney was similar to that of creatinine (∼17%, P = NS). In addition, the FGF-23 FE by the kidney was significantly directly related to eGFR (r = 0.709 P = 0.018) and to kidney creatinine FE (r = 0.736 P = 0.013) but only as a trend to plasma phosphate levels (r = 0.55, P = 0.18). There was no difference in FGF-23 levels in blood perfusing splanchnic organs and cardiopulmonary bed. However, the arterial-venous difference of FGF-23 across the lung was directly related to FGF-23 pulmonary artery levels, suggesting that the lung, and possibly the heart, participate in the homeostasis of plasma FGF-23 when its systemic levels are increased. Our data show that the human kidney is the only site for FGF-23 removal from blood and suggest that FGF-23 is predominantly removed by glomerular filtration. The kidney ability to remove FGF-23 from the circulation likely accounts for the early increase in blood of FGF-23 in patients with CKD. [ABSTRACT FROM AUTHOR]

Published
2017
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37. A Pilot Study of IL2 in Drug-Resistant Idiopathic Nephrotic Syndrome.

Author

Bonanni, Alice, Bertelli, Roberta, Rossi, Roberta, Bruschi, Maurizio, Di Donato, Armando, Ravani, Pietro, and Ghiggeri, Gian Marco

Subjects
*NEPHROTIC syndrome, *NEPHROTIC syndrome treatment, *INTERLEUKIN-21, *PROTEINURIA, *DRUG resistance, *PILOT projects, *PATIENTS
Abstract

Tregs infusion reverts proteinuria and reduces renal lesions in most animal models of nephrotic syndrome (i.e. Buffalo/Mna, Adriamycin, Promycin, LPS). IL2 up-regulates Tregs and may be an alternative to cell-therapy in this setting. To evaluate a potential role of IL2 as Tregs inducer and proteinuria lowering agent in human nephrotic syndrome we treated 5 nephrotic patients with 6 monthly cycles of low-dose IL2 (1x106 U/m2 first month, 1.5x106 U/m2 following months). The study cohort consisted of 5 children (all boys, 11–17 years) resistant to all the available treatments (i.e. steroids, calcineurin inhibitors, mycophenolate, Rituximab). Participants had Focal Segmental Glomerulosclerosis (3 cases) or Minimal Change Nephropathy (2 cases). IL2 was safe in all but one patient who had an acute asthma attack after the first IL2 dose and did not receive further doses. Circulating Tregs were stably increased (>10%) during the whole study period in 2 cases while were only partially modified in the other two children who started with very low levels and partially responded to single IL2 Proteinuria and renal function were not modified by IL2 at any phase of the study. We concluded that low-dose IL2 given in monthly pulses is safe and modifies the levels of circulating Tregs. This drug may not be able to lower proteinuria or affect renal function in children with idiopathic nephrotic syndrome. We were unable to reproduce in humans the effects of IL2 described in rats and mice reducing de facto the interest on this drug in nephrotic syndrome. Trial Registration: ClinicalTrials.gov [ABSTRACT FROM AUTHOR]

Published
2015
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38. Multi-antibody composition in lupus nephritis: Isotype and antigen specificity make the difference.

Author

Bonanni, Alice, Vaglio, Augusto, Bruschi, Maurizio, Sinico, Renato Alberto, Cavagna, Lorenzo, Moroni, Gabriella, Franceschini, Franco, Allegri, Landino, Pratesi, Federico, Migliorini, Paola, Candiano, Giovanni, Pesce, Giampaola, Ravelli, Angelo, Puppo, Francesco, Martini, Alberto, Tincani, Angela, and Ghiggeri, Gian Marco

Subjects
*IMMUNOGLOBULINS, *LUPUS nephritis, *ANTIGEN analysis, *AUTOIMMUNITY, *GLOMERULONEPHRITIS, *PROTEOMICS
Abstract

Research on autoimmune processes involved in glomerulonephritis has been for years based on experimental models. Recent progress in proteomics has radically modified perspectives: laser microdissection and proteomics were crucial for an in vivo analysis of autoantibodies eluted from human biopsies. Lupus nephritis has been the subject of recent independent researches. Main topics have been the definition of renal autoimmune components in human lupus biopsies; methods were laser capture of glomeruli and/or of single cells (CD38 + or Ki-67 +) from tubulointerstitial areas as starting step followed by elution and characterization of renal antibodies by proteomics. The innovative approach highlighted different panels of autoantibodies deposited in glomeruli and in tubulo-interstitial areas that actually represented the unique autoimmune components in these patients. IgG2 was the major isotype; new podocyte proteins (αenolase, annexin AI) and already known implanted molecules (DNA, histone 3, C1q) were their target antigens in glomeruli. Vimentin was the antigen in tubulo-interstitial areas. Matching renal autoantibodies with serum allowed the definition of a typical autoantibody serum map that included the same anti-αenolase, anti-annexin AI, anti-DNA, and anti-histone 3 IgG2 already detected in renal tissue. Serum levels of specific autoantibodies were tenfold increased in patients with lupus nephritis allowing a clear differentiation from both rheumatoid arthritis and other glomerulonephritis. In all cases, targeted antigens were characterized as components of lupus NETosis. Matching renal/serum autoantibody composition in vivo furnishes new insights on human lupus nephritis and allows to refine composition of circulating antibodies in patients with lupus. A thoughtful passage from bench to bedside of new knowledge would expand our clinical and therapeutic opportunities. [ABSTRACT FROM AUTHOR]

Published
2015
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39. LPS Nephropathy in Mice Is Ameliorated by IL-2 Independently of Regulatory T Cells Activity.

Author

Bertelli, Roberta, Di Donato, Armando, Cioni, Michela, Grassi, Fabio, Ikehata, Masami, Bonanni, Alice, Rastaldi, Maria Pia, and Ghiggeri, Gian Marco

Subjects
T cells, IMMUNOSUPPRESSION, MICE, CELLULAR control mechanisms, ANIMAL experimentation
Abstract

Immunosuppressive regulatory T cells (Tregs) have been hypothesized to exert a protective role in animal models of spontaneous (Buffalo/Mna) and/or drug induced (Adriamycin) nephrotic syndrome. In this study, we thought to define whether Tregs can modify the outcome of LPS nephropathy utilizing IL-2 as inducer of tissue and circulating Tregs. LPS (12 mg/Kg) was given as single shot in C57BL/6, p2rx7−/− and Foxp3EGFP; free IL-2 (18.000 U) or, in alternative, IL-2 coupled with JES6-1 mAb (IL-2/anti-IL-2) were injected before LPS. Peripheral and tissue Tregs/total CD4+ cell ratio, urinary parameters and renal histology were evaluated for 15 days. IL-2 administration to wild type mice had no effect on peripheral Tregs number, whereas a significant increase was induced by the IL-2/anti-IL-2 immunocomplex after 5 days. Spleen and lymph nodes Tregs were comparably increased. In p2rx7−/− mice, IL-2/anti-IL-2 treatment resulted in increase of peripheral Tregs but did not modify the spleen and lymph nodes quota. LPS induced comparable and transient proteinuria in both wild type and p2rx7−/− mice. Proteinuria was inhibited by co-infusion of human IL-2, with reduction at each phase of the disease (24 −48 and 72 hours) whereas IL-2/anti-IL-2 produced weaker effects. In all mice (wild type and p2rx7−/−) and irrespective of treatment (IL-2, IL-2/anti-IL-2), LPS was associated with progressive signs of renal pathologic involvement resulting in glomerulosclerosis. In conclusion, IL-2 plays a transient protective effect on proteinuria induced by LPS independent of circulating or tissue Tregs but does not modify the outcome of renal degenerative renal lesions. [ABSTRACT FROM AUTHOR]

Published
2014
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41. Ofatumumab-associated acute respiratory manifestations: clinical characteristics and treatment.

Author

Bonanni, Alice, Bertelli, Enrica, Moscatelli, Andrea, Lampugnani, Elisabetta, Bodria, Monica, Ravani, Pietro, and Ghiggeri, Gian Marco

Subjects
*SARS disease, *ADULT respiratory distress syndrome
Abstract

A letter to the editor is presented in response to the article "Ofatumumab-associated acute respiratory manifestations: clinical characteristics and treatment," by Alice Bonanni.

Published
2016
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42. Ofatumumab-associated acute pneumonitis: Not new but still the first case.

Author

Bonanni, Alice, Bertelli, Enrica, Panicucci, Chiara, D'Alessandro, Matteo, Moscatelli, Andrea, Lampugnani, Elisabetta, Sacco, Oliviero, Magnano, Gian Michele, Ravani, Pietro, and Ghiggeri, Gian Marco

Subjects
*PNEUMONIA, *RITUXIMAB, *DRUG side effects, *MONOCLONAL antibodies, *DYSPNEA
Abstract

Ofatumumab is an anti- CD20 humanized monoclonal antibody utilized in the treatment of several clinical conditions resistant to other treatments. In spite there was a general expectation that ofatumumab was less toxic compared to rituximab, side effects have been reported that resemble those of its anti- CD20 chimeric precursor. Here, we describe the first case of Ofatumumab associate lung injury occurring in a 14-year-old boy affected by nephrotic syndrome dependent to prednisone plus cyclosporine A who had been treated with the dose of drug utilized in nephrotic syndrome (1500 mg/173 m2). The patient developed the full blown picture of rituximab associated lung injury ( RALI) after 45 days from ofatumumab infusion at the end of the steroid tapering: severe exertional dyspnea, mild fever and cyanosis, with CT scan showing diffuse ground glass areas in both lungs and DLCO (diffusing capacity of transfer factor of the lung for carbon monoxide) test suggestive for reduction of CO diffusion. Clinical outcome was good with rapid improvement and normalization of all parameters without any specific therapy. After 60 days, chest CT and CO diffusion tests were normal. In conclusion, we describe here the first case of acute pneumonitis associated with ofatumumab that presents the same clinical, laboratory, and radiology features of the lung injury reported for rituximab. Like RALI occurring in patients treated for nephrotic syndrome, this case had a mild clinical expression and recovered in a few months. [ABSTRACT FROM AUTHOR]

Published
2017
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44. Post-translational modified proteins are biomarkers of autoimmune-processes: NETosis and the inflammatory–autoimmunity connection.

Author

Bruschi, Maurizio, Petretto, Andrea, Bertelli, Roberta, Galetti, Maricla, Bonanni, Alice, Pratesi, Federico, Migliorini, Paola, Candiano, Giovanni, Vaglio, Augusto, and Ghiggeri, Gian Marco

Subjects
*BIOMARKERS, *POST-translational modification, *PROTEIN expression, *NEUTROPHILS, *IMMUNE response, *AUTOIMMUNITY
Abstract

Basic research is showing new mechanisms involved in early immune responses and Neutrophil Extracellular Trap (NET) formation (or NETosis) is of key importance as first line defense against bacteria, virus and protozoa. Enzymatic modification of arginine in citrulline in histones is the prerequisite of NETosis being it necessary for decondensation and extrusion of DNA from cells; it is conceivable that other post translational modifications may occur during this event. There is consensus in considering that post translational modified proteins may elicit an autoimmune response that leads to the formation of autoantibodies. Several autoimmune diseases seem to share these pathogenic mechanisms, in particular Rheumatoid arthritis, Systemic Lupus Erythematosus, Small Vessel Vasculitis and Anti-Phospholipid Syndrome, which are all characterized by high levels of circulating autoantibodies. Autoimmunity has, however, different targets and elicits different clinical responses. It seems reasonable to hypothesize that although NETosis is common to all the conditions above, NET components are different and potentially responsible for different autoimmune responses. On the other hand also showing whether circulating NET remnants are present as free structures in blood/biological fluids and determine their levels is relevant to autoimmunity. This review is intended to discuss the rationale for utilizing new discoveries that could be of rapid clinical application and lead to the development of early biomarkers of autoimmunity to predict and treat otherwise serious conditions. [ABSTRACT FROM AUTHOR]

Published
2017
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45. FCGR2A single nucleotide polymorphism confers susceptibility to childhood-onset idiopathic nephrotic syndrome.

Author

Rossi, Giovanni M., Bonatti, Francesco, Adorni, Alessia, Alberici, Federico, Bodria, Monica, Bonanni, Alice, Ghiggeri, Gian M., Martorana, Davide, and Vaglio, Augusto

Subjects
*NEPHROTIC syndrome in children, *T cells, *SINGLE nucleotide polymorphisms, *FC receptors, *RITUXIMAB
Abstract

Childhood-onset idiopathic nephrotic syndrome affects 1.15–3.4 children/100,000 children/year in Western Countries. Immune-mediated mechanisms, particularly T cell-mediated, are thought to play a key pathogenic role. The genetic basis of the disease is still poorly understood. We tested the association between single nucleotide polymorphisms (SNPs) of four genes encoding Fc gamma receptors ( FCGR2A , FCGR2B , FCGR3A , FCGR3B ) and idiopathic nephrotic syndrome in a case-control study of paediatric patients. Children with idiopathic nephrotic syndrome (aged 1–16 years) were included. FCGR2A rs1801274 and FCGR3A rs396991 SNPs were genotyped using real-time PCR with the TaqMan method, while FCGR2B rs1050501 and FCGR3B NA1/NA2 were genotyped using Sanger sequencing. Fisher’s exact test was used to explore genetic association. We enrolled 103 idiopathic nephrotic syndrome patients and 181 healthy controls. A significant association was found between idiopathic nephrotic syndrome and FCGR2A rs1801274 SNP (both with the T allele and the TT genotype, p value = 0.0009, OR 1.81, 95% CI 1.27–2.59 and p value = 0.0007, OR 2.39, 95% CI 1.44–3.99, respectively). No associations were found for the remaining SNPs. Fc gamma receptors might modulate response to rituximab; since 60 of the enrolled patients were treated with rituximab, we also tested the association between the studied SNPs and rituximab efficacy in this patient subgroup, but found only a weak association with FCGR2A CC genotype (p value = 0.03). The FCGR2A rs1801274 SNP in the gene encoding the activating receptor CD32A confers susceptibility to idiopathic nephrotic syndrome. [ABSTRACT FROM AUTHOR]

Published
2018
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46. UPREGULATED MONOCYTE EXPRESSION OF PLIN2 IS ASSOCIATED WITH PLAQUE INSTABILITY IN CORONARY ARTERY DISEASE.

Author

Canonico, Francesco, Severino, Anna, Camilli, Massimiliano, Migliaro, Stefano, Vinci, Ramona, Galli, Mattia, Pisano, Eugenia, Arcudi, Alessandra, Bonanni, Alice, Sario, Marianna Di, Ciutiis, Astrid De, Russo, Sara, Angelini, Giulia, Pedicino, Daniela, Montone, Rocco, Niccoli, Giampaolo, Liuzzo, Giovanna, Crea, Filippo, and D'Amario, Domenico

Subjects
*CORONARY artery disease
Published
2022
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47. Apoptosis and myostatin mRNA are upregulated in the skeletal muscle of patients with chronic kidney disease.

Author

Verzola, Daniela, Procopio, Vanessa, Sofia, Antonella, Villaggio, Barbara, Tarroni, Alice, Bonanni, Alice, Mannucci, Irene, De Cian, Franco, Gianetta, Ezio, Saffioti, Stefano, and Garibotto, Giacomo

Subjects
*APOPTOSIS, *MUSCULAR atrophy, *INTERLEUKIN-6, *GENE expression, *GROWTH factors, *RNA
Abstract

Apoptosis and myostatin are major mediators of muscle atrophy and might therefore be involved in the wasting of uremia. To examine whether they are expressed in the skeletal muscle of patients with chronic kidney disease (CKD), we measured muscle apoptosis and myostatin mRNA and their related intracellular signal pathways in rectus abdominis biopsies obtained from 22 consecutive patients with stage 5 CKD scheduled for peritoneal dialysis. Apoptotic loss of myonuclei, determined by anti-single-stranded DNA antibody and terminal deoxynucleotidyl transferase-mediated dUTP nick-end labeling assays, was significantly increased three to fivefold, respectively. Additionally, myostatin and interleukin (IL)-6 gene expressions were significantly upregulated, whereas insulin-like growth factor-I mRNA was significantly lower than in controls. Phosphorylated JNK (c-Jun amino-terminal kinase) and its downstream effector, phospho-c-Jun, were significantly upregulated, whereas phospho-Akt was markedly downregulated. Multivariate analysis models showed that phospho-Akt and IL-6 contributed individually and significantly to the prediction of apoptosis and myostatin gene expression, respectively. Thus, our study found activation of multiple pathways that promote muscle atrophy in the skeletal muscle of patients with CKD. These pathways appear to be associated with different intracellular signals, and are likely differently regulated in patients with CKD. [ABSTRACT FROM AUTHOR]

Published
2011
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48. Vaccines and Myocardial Injury in Patients Hospitalized for COVID-19 Infection: the CardioCOVID-Gemelli Study.

Author

Montone RA, Rinaldi R, Masciocchi C, Lilli L, Damiani A, La Vecchia G, Iannaccone G, Basile M, Salzillo C, Caffè A, Bonanni A, De Pascale G, Grieco DL, Tanzarella ES, Buonsenso D, Murri R, Fantoni M, Liuzzo G, Sanna T, Richeldi L, Sanguinetti M, Massetti M, Trani C, Tshomba Y, Gasbarrini A, Valentini V, Antonelli M, and Crea F

Abstract

Background: Myocardial injury is prevalent among patients hospitalized for COVID-19. However, the role of COVID-19 vaccines in modifying the risk of myocardial injury is unknown., Objectives: To assess the role of vaccines in modifying the risk of myocardial injury in COVID-19., Methods: We enrolled COVID-19 patients admitted from March 2021 to February 2022 with known vaccination status and ≥1 assessment of hs-cTnI within 30 days from the admission. The primary endpoint was the occurrence of myocardial injury (hs-cTnI levels >99th percentile upper reference limit)., Results: 1019 patients were included (mean age 67.7±14.8 years, 60.8% male, 34.5% vaccinated against COVID-19). Myocardial injury occurred in 145 (14.2%) patients. At multivariate logistic regression analysis, advanced age, chronic kidney disease and hypertension, but not vaccination status, were independent predictors of myocardial injury. In the analysis according to age tertiles distribution, myocardial injury occurred more frequently in the III tertile (≥76 years) compared to other tertiles (I tertile:≤60 years;II tertile:61-75 years) (p<0.001). Moreover, in the III tertile, vaccination was protective against myocardial injury (OR 0.57, CI 95% 0.34-0.94; p=0.03), while a previous history of coronary artery disease was an independent positive predictor. In contrast, in the I tertile, chronic kidney disease (OR 6.94, 95% CI 1.31-36.79, p=0.02) and vaccination (OR 4.44, 95% CI 1.28-15.34, p=0.02) were independent positive predictors of myocardial injury., Conclusions: In patients ≥76 years, COVID-19 vaccines were protective for the occurrence of myocardial injury, while in patients ≤60 years, myocardial injury was associated with previous COVID-19 vaccination. Further studies are warranted to clarify the underlying mechanisms., (© The Author(s) 2024. Published by Oxford University Press on behalf of the European Society of Cardiology.)

Published
2024
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49. Impact of the exposome on cardiovascular disease.

Author

Bonanni A, Basile M, Montone RA, and Crea F

Abstract

Air pollution, noise pollution, and light pollution have emerged as important but often overlooked risk factors for cardiovascular disease. In this review, we examine the emerging concept of the exposome, highlighting the close relationship between environmental exposure (e.g. PM 2.5 , traffic noise, and night light) and cardiovascular disease, finally addressing the possible mitigation strategies that should be implemented to reduce the impact of air, noise, and light pollution on cardiovascular morbidity and mortality., Competing Interests: Conflict of interest: None declared., (© The Author(s) 2023. Published by Oxford University Press on behalf of the European Society of Cardiology.)

Published
2023
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50. Monocyte-Platelet Aggregates Triggered by CD31 Molecule in Non-ST Elevation Myocardial Infarction: Clinical Implications in Plaque Rupture.

Author

Vinci R, Pedicino D, Bonanni A, d'Aiello A, Pisano E, Ponzo M, Severino A, Ciampi P, Canonico F, Russo G, Di Sario M, Vergallo R, Filomia S, Montone RA, Flego D, Stefanini L, Piacentini R, Conte C, Cribari F, Massetti M, Crea F, and Liuzzo G

Abstract

Despite the recent innovations in cardiovascular care, atherothrombosis is still a major complication of acute coronary syndromes (ACS). We evaluated the involvement of the CD31 molecule in thrombotic risk through the formation of monocyte-platelet (Mo-Plt) aggregates in patients with ACS with no-ST-segment elevation myocardial infarction (NSTEMI) on top of dual anti-platelet therapy (DAPT). We enrolled 19 control (CTRL) subjects, 46 stable angina (SA), and 86 patients with NSTEMI, of which, 16 with Intact Fibrous Cap (IFC) and 19 with Ruptured Fibrous Cap (RFC) as assessed by the Optical Coherence Tomography (OCT). The expression of CD31 on monocytes and platelets was measured. Following the coronary angiography, 52 NSTEMIs were further stratified according to thrombus grade (TG) evaluation. Finally, a series of ex vivo experiments verified whether the CD31 participates in Mo-Plt aggregate formation. In patients with NSTEMI, CD31 was reduced on monocytes and was increased on platelets, especially in NSTEMI presented with RFC plaques compared to those with IFC lesions, and in patients with high TG compared to those with zero/low TG. Ex vivo experiments documented an increase in Mo-Plt aggregates among NSTEMI, which significantly decreased after the CD31 ligation, particularly in patients with RFC plaques. In NSTEMI, CD31 participates in Mo-Plt aggregate formation in spite of optimal therapy and DAPT, suggesting the existence of alternative thrombotic pathways, as predominantly displayed in patients with RFC., Competing Interests: The authors declare that the research was conducted in the absence of any commercial or financial relationships that could be construed as a potential conflict of interest., (Copyright © 2022 Vinci, Pedicino, Bonanni, d'Aiello, Pisano, Ponzo, Severino, Ciampi, Canonico, Russo, Di Sario, Vergallo, Filomia, Montone, Flego, Stefanini, Piacentini, Conte, Cribari, Massetti, Crea and Liuzzo.)

Published
2022
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