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3. In vitro extracellular vesicles' heterogeneity-related biological properties may be defined by a new method of separation and characterization

Author

Arnaboldi, L., primary, Accattatis, F., additional, Granata, A., additional, Carleo, A., additional, Francomano, F., additional, Rodolfo, M., additional, Vergani, E., additional, Romano, M., additional, Bergese, P., additional, Brucale, M., additional, Valle, F., additional, Corsini, A., additional, Bellosta, S., additional, and Bianchi, L., additional

Published
2023
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5. Kisspeptin-mediated improvement of sensitivity to BRAF inhibitors in vemurafenib resistant melanoma cells

Author

Guzzetti, C, Corno, C, Vergani, E, Mirra, L, Ciusani, E, Rodolfo, M, Perego, P, Beretta, G, Beretta, GL, Guzzetti, C, Corno, C, Vergani, E, Mirra, L, Ciusani, E, Rodolfo, M, Perego, P, Beretta, G, and Beretta, GL

Abstract

Metastatic dissemination is still one of the major causes of death of melanoma’s patients. KiSS1 is a metastasis suppressor originally identified in melanoma cells, known to play an important physiological role in mammals’ development and puberty. It has been previously shown that expression of KiSS1 could be increased in lung cancer cells using epigenetic agents, and that KiSS1 could have a pro-apoptotic action in combination with cisplatin. Thus, the aim of the present study was to examine in human melanoma vemurafenib sensitive- and -resistant BRAF mutant cells characterized by different mutational profiles and KiSS1, KiSS1 receptor and KiSS1 drug-induced release, if peptides derived from KiSS1 cleavage, i.e., kisspeptin 54, could increase the sensitivity to vemurafenib of human melanoma, using cellular, molecular and biochemical approaches. We found that kisspeptin 54 increases vemurafenib pro-apoptotic activity in a statistically significant manner, also in drug resistant cellular models. The efficacy of the combination appears to reflect the intrinsic susceptibility of each cell line to PLX4032-induced apoptosis, together with the different mutational profile as well as perturbation of proteins regulating the apoptotic pathway, The results presented here highlight the possibility to exploit KiSS1 to modulate the apoptotic response to therapeutically relevant agents, suggesting a multitasking function of this metastasis suppressor.

Published
2023

6. Increased levels of plasma neudesin in adult growth hormone deficiency and their relationship with plasma liver-expressed antimicrobial peptide-2 levels: a cross-sectional study

Author

Vergani, Edoardo, Bruno, Carmine, Gavotti, Cesare, Oliva, Alessandro, Curro', Diego, Mancini, Antonio, Vergani, E, Bruno, C, Gavotti, C, Oliva, A, Curro', D (ORCID:0000-0001-6726-6872), Mancini, A (ORCID:0000-0002-7707-4564), Vergani, Edoardo, Bruno, Carmine, Gavotti, Cesare, Oliva, Alessandro, Curro', Diego, Mancini, Antonio, Vergani, E, Bruno, C, Gavotti, C, Oliva, A, Curro', D (ORCID:0000-0001-6726-6872), and Mancini, A (ORCID:0000-0002-7707-4564)

Abstract

Purpose Adult growth hormone deficiency (aGHD) is characterized by an altered metabolic profile and increased cardiovascular risk. Neudesin is a newly discovered protein mainly secreted from adipose tissue and brain, under evaluation for its possible activity as a negative regulator of energy expenditure. Liver-expressed antimicrobial peptide (LEAP)-2 is a competitive antagonist of ghrelin on its receptor. An observational cross-sectional study was performed to test the hypothesis that plasma neudesin levels may be modified in aGHD. Given the role played in the energy balance, any possible relationships between neudesin, LEAP-2 and metabolic and anthropometric parameters were evaluated. Subjects and Methods Thirty-eight patients were included: 18 aGHD patients (7 females and 11 males, aged 59.7 & PLUSMN; 2.6 years, BMI 30.2 & PLUSMN; 2.2 kg/m(2)); 20 healthy controls (12 females and 8 males, aged 47.1 & PLUSMN; 2.5 years, BMI 24.1 & PLUSMN; 0.9 kg/m(2)). All patients were evaluated for glucose, insulin, HOMA and QUICKI index, total/LDL/HDL cholesterol, triglycerides, uric acid, and IGF-1. Plasma neudesin, LEAP-2, and ghrelin were measured by ELISA. Fat mass was evaluated by DEXA. Results Neudesin levels were significantly higher in aGHD versus controls. We confirmed the finding of significantly lower ghrelin levels and significantly higher LEAP-2/ghrelin ratio in aGHD patients and found a significant direct correlation between neudesin and LEAP-2 levels. A significant direct correlation between neudesin and fat mass percentage was found in the whole population. Conclusion These results suggest the onset of adaptive responses to an altered metabolic picture in aGHD. The changes in two distinct pathways that modulate food intake and the still limited knowledge about neudesin suggest future developments in this field.

Published
2023

7. SPTBN1 Mediates the Cytoplasmic Constraint of PTTG1, Impairing Its Oncogenic Activity in Human Seminoma

Author

Teveroni, Emanuela, Di Nicuolo, F., Vergani, Edoardo, Oliva, A., Vodola, Emanuele Pierpaolo, Bianchetti, Giada, Maulucci, Giuseppe, De Spirito, Marco, Cenci, Tonia, Pierconti, Francesco, Gulino, Gaetano, Iavarone, Federica, Urbani, Andrea, Milardi, Domenico, Pontecorvi, Alfredo, Mancini, F., Teveroni E., Vergani E., Vodola E. P., Bianchetti G., Maulucci G. (ORCID:0000-0002-2154-319X), De Spirito M. (ORCID:0000-0003-4260-5107), Cenci T., Pierconti F. (ORCID:0000-0003-0951-4131), Gulino G., Iavarone F. (ORCID:0000-0002-2074-5531), Urbani A. (ORCID:0000-0001-9168-3174), Milardi D., Pontecorvi A. (ORCID:0000-0003-0570-6865), Teveroni, Emanuela, Di Nicuolo, F., Vergani, Edoardo, Oliva, A., Vodola, Emanuele Pierpaolo, Bianchetti, Giada, Maulucci, Giuseppe, De Spirito, Marco, Cenci, Tonia, Pierconti, Francesco, Gulino, Gaetano, Iavarone, Federica, Urbani, Andrea, Milardi, Domenico, Pontecorvi, Alfredo, Mancini, F., Teveroni E., Vergani E., Vodola E. P., Bianchetti G., Maulucci G. (ORCID:0000-0002-2154-319X), De Spirito M. (ORCID:0000-0003-4260-5107), Cenci T., Pierconti F. (ORCID:0000-0003-0951-4131), Gulino G., Iavarone F. (ORCID:0000-0002-2074-5531), Urbani A. (ORCID:0000-0001-9168-3174), Milardi D., and Pontecorvi A. (ORCID:0000-0003-0570-6865)

Abstract

Seminoma is the most common testicular cancer. Pituitary tumor-transforming gene 1 (PTTG1) is a securin showing oncogenic activity in several tumors. We previously demonstrated that nuclear PTTG1 promotes seminoma tumor invasion through its transcriptional activity on matrix metalloproteinase 2 (MMP-2) and E-cadherin (CDH1). We wondered if specific interactors could affect its subcellular distribution. To this aim, we investigated the PTTG1 interactome in seminoma cell lines showing different PTTG1 nuclear levels correlated with invasive properties. A proteomic approach upon PTTG1 immunoprecipitation uncovered new specific securin interactors. Western blot, confocal microscopy, cytoplasmic/nuclear fractionation, sphere-forming assay, and Atlas database interrogation were performed to validate the proteomic results and to investigate the interplay between PTTG1 and newly uncovered partners. We observed that spectrin beta-chain (SPTBN1) and PTTG1 were cofactors, with SPTBN1 anchoring the securin in the cytoplasm. SPTBN1 downregulation determined PTTG1 nuclear translocation, promoting its invasive capability. Moreover, a PTTG1 deletion mutant lacking SPTBN1 binding was strongly localized in the nucleus. The Atlas database revealed that seminomas that contained higher nuclear PTTG1 levels showed significantly lower SPTBN1 levels in comparison to non-seminomas. In human seminoma specimens, we found a strong PTTG1/SPTBN1 colocalization that decreases in areas with nuclear PTTG1 distribution. Overall, these results suggest that SPTBN1, along with PTTG1, is a potential prognostic factor useful in the clinical management of seminoma.

Published
2023

9. The 'Adipo-Cerebral' Dialogue in Childhood Obesity: Focus on Growth and Puberty. Physiopathological and Nutritional Aspects

Author

Bruno, C, Vergani, E, Giusti, M, Oliva, A, Cipolla, C, Pitocco, D, Mancini, A, Vergani E, Cipolla C, Pitocco D (ORCID:0000-0002-6220-686X), Bruno, C, Vergani, E, Giusti, M, Oliva, A, Cipolla, C, Pitocco, D, Mancini, A, Vergani E, Cipolla C, and Pitocco D (ORCID:0000-0002-6220-686X)

Abstract

Overweight and obesity in children and adolescents are overwhelming problems in western countries. Adipocytes, far from being only fat deposits, are capable of endocrine functions, and the endocrine activity of adipose tissue, resumable in adipokines production, seems to be a key modulator of central nervous system function, suggesting the existence of an “adipo-cerebral axis.” This connection exerts a key role in children growth and puberty development, and it is exemplified by the leptin–kisspeptin interaction. The aim of this review was to describe recent advances in the knowledge of adipose tissue endocrine functions and their relations with nutrition and growth. The peculiarities of major adipokines are briefly summarized in the first paragraph; leptin and its interaction with kisspeptin are focused on in the second paragraph; the third paragraph deals with the regulation of the GH-IGF axis, with a special focus on the model represented by growth hormone deficiency (GHD); finally, old and new nutritional aspects are described in the last paragraph.

Published
2021

10. Size, fatty acid and protein characterization of different populations of extracellular vesicles obtained by sequential centrifugation. An useful tool to dissect their biological properties?

Author

Accattatis, F.M., primary, Mazza, S., additional, Bordonaro, F., additional, Granata, A., additional, Vergani, E., additional, Rodolfo, M., additional, Bianchi, L., additional, Francomano, F., additional, Carleo, A., additional, Bellosta, S., additional, Corsini, A., additional, and Arnaboldi, L., additional

Published
2022
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11. Pharmacological modulation of lipid metabolism in a human cell line alters protein content and signalling of secreted extracellular vesicles

Author

Mazza, S., primary, Accattatis, F.M., additional, Bordonaro, F., additional, Granata, A., additional, Bianchi, L., additional, Francomano, F., additional, Carleo, A., additional, Vergani, E., additional, Rodolfo, M., additional, Bellosta, S., additional, Corsini, A., additional, and Arnaboldi, L., additional

Published
2022
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12. miR-146a-5p impairs melanoma resistance to kinase inhibitors by targeting COX2 and regulating NFkB-mediated inflammatory mediators

Author

Vergani, E, Dugo, M, Cossa, M, Frigerio, S, Di Guardo, L, Gallino, G, Mattavelli, I, Vergani, B, Lalli, L, Tamborini, E, Valeri, B, Gargiuli, C, Shahaj, E, Ferrarini, M, Ferrero, E, Gomez Lira, M, Huber, V, Vecchio, M, Sensi, M, Leone, B, Santinami, M, Rivoltini, L, Rodolfo, M, Vallacchi, V, Vergani E., Dugo M., Cossa M., Frigerio S., Di Guardo L., Gallino G., Mattavelli I., Vergani B., Lalli L., Tamborini E., Valeri B., Gargiuli C., Shahaj E., Ferrarini M., Ferrero E., Gomez Lira M., Huber V., Vecchio M. D., Sensi M., Leone B. E., Santinami M., Rivoltini L., Rodolfo M., Vallacchi V., Vergani, E, Dugo, M, Cossa, M, Frigerio, S, Di Guardo, L, Gallino, G, Mattavelli, I, Vergani, B, Lalli, L, Tamborini, E, Valeri, B, Gargiuli, C, Shahaj, E, Ferrarini, M, Ferrero, E, Gomez Lira, M, Huber, V, Vecchio, M, Sensi, M, Leone, B, Santinami, M, Rivoltini, L, Rodolfo, M, Vallacchi, V, Vergani E., Dugo M., Cossa M., Frigerio S., Di Guardo L., Gallino G., Mattavelli I., Vergani B., Lalli L., Tamborini E., Valeri B., Gargiuli C., Shahaj E., Ferrarini M., Ferrero E., Gomez Lira M., Huber V., Vecchio M. D., Sensi M., Leone B. E., Santinami M., Rivoltini L., Rodolfo M., and Vallacchi V.

Abstract

Background: Targeted therapy with BRAF and MEK inhibitors has improved the survival of patients with BRAF-mutated metastatic melanoma, but most patients relapse upon the onset of drug resistance induced by mechanisms including genetic and epigenetic events. Among the epigenetic alterations, microRNA perturbation is associated with the development of kinase inhibitor resistance. Here, we identified and studied the role of miR-146a-5p dysregulation in melanoma drug resistance. Methods: The miR-146a-5p-regulated NFkB signaling network was identified in drug-resistant cell lines and melanoma tumor samples by expression profiling and knock-in and knock-out studies. A bioinformatic data analysis identified COX2 as a central gene regulated by miR-146a-5p and NFkB. The effects of miR-146a-5p/COX2 manipulation were studied in vitro in cell lines and with 3D cultures of treatment-resistant tumor explants from patients progressing during therapy. Results: miR-146a-5p expression was inversely correlated with drug sensitivity and COX2 expression and was reduced in BRAF and MEK inhibitor-resistant melanoma cells and tissues. Forced miR-146a-5p expression reduced COX2 activity and significantly increased drug sensitivity by hampering prosurvival NFkB signaling, leading to reduced proliferation and enhanced apoptosis. Similar effects were obtained by inhibiting COX2 by celecoxib, a clinically approved COX2 inhibitor. Conclusions: Deregulation of the miR-146a-5p/COX2 axis occurs in the development of melanoma resistance to targeted drugs in melanoma patients. This finding reveals novel targets for more effective combination treatment. [MediaObject not available: see fulltext.] Graphical Abstract: [Figure not available: see fulltext.]

Published
2020

13. Oxidative stress and anabolic hormones in back pain: Current concept and preliminary analysis in male cohort

Author

Vergani, E., Bruno, C., Silvestrini, A., Meucci, E., Proietti, L., Perna, A., Tamburrelli, F. C., Mancini, A., Vergani E., Bruno C., Silvestrini A. (ORCID:0000-0002-2005-3746), Meucci E. (ORCID:0000-0002-8821-8041), Proietti L. (ORCID:0000-0003-2919-0381), Tamburrelli F. C. (ORCID:0000-0002-3140-5700), Mancini A. (ORCID:0000-0002-7707-4564), Vergani, E., Bruno, C., Silvestrini, A., Meucci, E., Proietti, L., Perna, A., Tamburrelli, F. C., Mancini, A., Vergani E., Bruno C., Silvestrini A. (ORCID:0000-0002-2005-3746), Meucci E. (ORCID:0000-0002-8821-8041), Proietti L. (ORCID:0000-0003-2919-0381), Tamburrelli F. C. (ORCID:0000-0002-3140-5700), and Mancini A. (ORCID:0000-0002-7707-4564)

Abstract

Back Pain (BP) is a common medical problem; anabolic hormones, through the modulation of oxidative stress (OS), could influence fracture risk. We evaluated the prevalence of anabolic hormonal deficiencies and their relationship with OS in males with BP, associated or not to nontraumatic fractures. 49 males with BP, from 36 to 80 years, were divided in two groups according to radiological evidence of nontraumatic fractures; group A (n=25): non-fractured; group B (n=24): fractured. A different prevalence of hormonal deficits was observed: 24% of hypotestosteronemia in A, 0% in B; 16% of GHD in A, 29% in B; Total Antioxidant Capacity (TAC) showed a trend toward higher levels in B. In A, despite lower TAC, a significant inverse correlation was present between TAC and IGF-1. A greater prevalence of GHD in patients with vertebral fractures was seen and, in a subgroup, OS could mediate the deleterious effects of hyposecretory GH state.

Published
2020

14. Progressive right ventricular dysfunction and exercise impairment in patients with heart failure and diabetes mellitus: insights from the T.O.S.CA. Registry

Author

Salzano, A, D'Assante, R, Iacoviello, M, Triggiani, V, Rengo, G, Cacciatore, F, Maiello, C, Limongelli, G, Masarone, D, Sciacqua, A, Perrone Filardi, P, Mancini, A, Volterrani, M, Vriz, O, Castello, R, Passantino, A, Campo, M, Modesti, Pa, De Giorgi, A, Arcopinto, M, Gargiulo, P, Perticone, M, Colao, A, Milano, S, Garavaglia, A, Napoli, R, Suzuki, T, Bossone, E, Marra, Am, Cittadini, A, Saccà, L, Monti, Mg, Matarazzo, M, Stagnaro, Fm, Piccioli, L, Lombardi, A, Panicara, V, Flora, M, Golia, L, Faga, V, Ruocco, A, Della Polla, D, Franco, R, Schiavo, A, Gigante, A, Spina, E, Sicuranza, M, Monaco, F, Apicella, M, Miele, C, Campanino, Ag, Mazza, L, Abete, R, Farro, A, Luciano, F, Polizzi, R, Ferrillo, G, De Luca, M, Crisci, G, Giardino, F, Barbato, M, Ranieri, B, Ferrara, F, Russo, V, Malinconico, M, Citro, R, Guastalamacchia, E, Leone, M, Giagulli, Va, Amarelli, C, Mattucci, I, Calabrò, P, Calabrò, R, D'Andrea, A, Maddaloni, V, Pacileo, G, Scarafile, R, Belfiore, A, Cimellaro, A, Casaretti, L, Paolillo, S, Favuzzi, Amr, Di Segni, C, Bruno, C, Vergani, E, Massaro, R, Grimaldi, F, Frigo, A, Sorrentino, Mr, Malandrino, D, Manfredini, R, Fabbian, F, Puzzo, A, Ragusa, L, Caliendo, L, Carbone, L, Frigiola, A, Generali, T, Giacomazzi, F, De Vincentiis, C, Ballotta, A, Garofalo, P, Malizia, G, Misiano, G, Israr, Mz, Bernieh, D, Cassambai, S, Yazaki, Y, Heaney, Lm, Eagle, Ka, Ventura, Ho, Bruzzese, D, Salzano, Andrea, D'Assante, Roberta, Iacoviello, Massimo, Triggiani, Vincenzo, Rengo, Giuseppe, Cacciatore, Francesco, Maiello, Ciro, Limongelli, Giuseppe, Masarone, Daniele, Sciacqua, Angela, Filardi, Pasquale Perrone, Mancini, Antonio, Volterrani, Maurizio, Vriz, Olga, Castello, Roberto, Passantino, Andrea, Campo, Michela, Modesti, Pietro A, De Giorgi, Alfredo, Arcopinto, Michele, Gargiulo, Paola, Perticone, Maria, Colao, Annamaria, Milano, Salvatore, Garavaglia, Agnese, Napoli, Raffaele, Suzuki, Toru, Bossone, Eduardo, Marra, Alberto M, Cittadini, Antonio, and Misiano, Gabriella

Subjects
Registrie, Heart Failure, Endocrinology, Diabetes and Metabolism, Ventricular Dysfunction, Right, Diabetes, Insulins, Socio-culturale, Stroke Volume, Insulin resistance, Diabete, Cardiopulmonary exercise test, Chronic heart failure, Diabetes, Insulin resistance, Right ventricle, TOSCA Registry, Chronic heart failure, Diabetes Mellitus, Type 2, TOSCA Registry, Exercise Test, Ventricular Function, Right, Humans, Insulin, Right ventricle, Registries, Cardiology and Cardiovascular Medicine, Cardiopulmonary exercise test, TOSCA, Human, LS4_7
Abstract

Background Findings from the T.O.S.CA. Registry recently reported that patients with concomitant chronic heart failure (CHF) and impairment of insulin axis (either insulin resistance—IR or diabetes mellitus—T2D) display increased morbidity and mortality. However, little information is available on the relative impact of IR and T2D on cardiac structure and function, cardiopulmonary performance, and their longitudinal changes in CHF. Methods Patients enrolled in the T.O.S.CA. Registry performed echocardiography and cardiopulmonary exercise test at baseline and at a patient-average follow-up of 36 months. Patients were divided into three groups based on the degree of insulin impairment: euglycemic without IR (EU), euglycemic with IR (IR), and T2D. Results Compared with EU and IR, T2D was associated with increased filling pressures (E/e′ratio: 15.9 ± 8.9, 12.0 ± 6.5, and 14.5 ± 8.1 respectively, p 2) in TD2 vs EU and IR patients was recorded (respectively, 15.8 ± 3.8 ml/Kg/min, 18.4 ± 4.3 ml/Kg/min and 16.5 ± 4.3 ml/Kg/min, p 2 in the T2D group (+ 13% increase in RV dimension, − 21% decline in TAPSE/PAPS ratio and − 20% decrease in peak VO2). Conclusion The higher risk of death and CV hospitalizations exhibited by HF-T2D patients in the T.O.S.CA. Registry is associated with progressive RV ventricular dysfunction and exercise impairment when compared to euglycemic CHF patients, supporting the pivotal importance of hyperglycaemia and right chambers in HF prognosis. Trial registration ClinicalTrials.gov identifier: NCT023358017

Published
2022

15. PTTG1/ZEB1 Axis Regulates E-Cadherin Expression in Human Seminoma

Author

Teveroni, Emanuela, Di Nicuolo, F., Vergani, Edoardo, Bianchetti, Giada, Bruno, C., Maulucci, Giuseppe, De Spirito, Marco, Cenci, Tonia, Pierconti, Francesco, Gulino, Gaetano, Bassi, Pierfrancesco, Pontecorvi, Alfredo, Milardi, D., Mancini, F., Teveroni E., Vergani E., Bianchetti G., Maulucci G. (ORCID:0000-0002-2154-319X), De Spirito M. (ORCID:0000-0003-4260-5107), Cenci T., Pierconti F. (ORCID:0000-0003-0951-4131), Gulino G., Bassi P. (ORCID:0000-0002-4313-8427), Pontecorvi A. (ORCID:0000-0003-0570-6865), Teveroni, Emanuela, Di Nicuolo, F., Vergani, Edoardo, Bianchetti, Giada, Bruno, C., Maulucci, Giuseppe, De Spirito, Marco, Cenci, Tonia, Pierconti, Francesco, Gulino, Gaetano, Bassi, Pierfrancesco, Pontecorvi, Alfredo, Milardi, D., Mancini, F., Teveroni E., Vergani E., Bianchetti G., Maulucci G. (ORCID:0000-0002-2154-319X), De Spirito M. (ORCID:0000-0003-4260-5107), Cenci T., Pierconti F. (ORCID:0000-0003-0951-4131), Gulino G., Bassi P. (ORCID:0000-0002-4313-8427), and Pontecorvi A. (ORCID:0000-0003-0570-6865)

Abstract

Simple Summary Seminoma represents one of the most common neoplasms in Caucasian males between 15 and 40 years old. The molecular pathways underlying its clinical behavior are far from being understood yet. We previously demonstrated that nuclear Pituitary-tumor transforming-gene 1 (PTTG1), overexpressed in several neoplasms, promotes invasiveness through its transcriptional target matrix-metalloproteinase-2 (MMP2). PTTG1 sustains the migratory and invasive properties of cancer cells through the induction of the epithelial-to-mesenchymal transition (EMT). E-Cadherin (E-CAD) repression is the first step of EMT. Therefore, we investigated the role of PTTG1 in EMT in human seminoma using an in vitro and in vivo model and through Atlas database interrogation. Our data showed a PTTG1-mediated E-CAD transcriptional repression through Zinc finger E-box binding homeobox 1 (ZEB1), a master regulator of the EMT process. Our data provide insights into the molecular characterization of seminoma, promoting PTTG1 as a prognostic marker useful in human seminoma clinical management. (1) Background: PTTG1 sustains the EMT process and the invasiveness of several neoplasms. We previously showed the role of nuclear PTTG1 in promoting invasiveness, through its transcriptional target MMP2, in seminoma in vitro models. Here, we investigated the key players involved in PTTG1-mediated EMT in human seminoma. (2) Methods: Two seminoma cell lines and four human seminoma tumor specimens were used. E-Cadherin gene regulation was investigated using Western blot, real-time PCR, and luciferase assay. Immunoprecipitation, ChIP, RE-ChIP, and confocal microscopy analysis were performed to evaluate the interplay between PTTG1 and ZEB1. Matrigel invasion and spheroid formation assays were applied to functionally investigate PTTG1 involvement in the EMT of seminoma cell lines. RNA depletion and overexpression experiments were performed to verify the role of PTTG1/ZEB1 in E-Cadherin repression and seminom

Published
2022

16. 3D tumor explant as a novel platform to investigate therapeutic pathways and predictive biomarkers in cancer patients

Author

Rodolfo, M, Huber, V, Cossa, M, Gallino, G, Leone, B, Vallacchi, V, Rivoltini, L, Vergani, E, Rodolfo, Monica, Huber, Veronica, Cossa, Mara, Gallino, Gianfrancesco, Leone, Biagio E, Vallacchi, Viviana, Rivoltini, Licia, Vergani, Elisabetta, Rodolfo, M, Huber, V, Cossa, M, Gallino, G, Leone, B, Vallacchi, V, Rivoltini, L, Vergani, E, Rodolfo, Monica, Huber, Veronica, Cossa, Mara, Gallino, Gianfrancesco, Leone, Biagio E, Vallacchi, Viviana, Rivoltini, Licia, and Vergani, Elisabetta

Abstract

Immunotherapy with immune checkpoint inhibitors can induce durable clinical responses in different human malignancies but the number of responding patients remains globally modest. The limited therapeutic efficacy of ICI depends on multiple factors, among which the immune suppressive features of the tumor microenvironment play a key role. For this reason, experimental models that enable dissection of the immune-hostile tumor milieu components are required to unravel how to overcome resistance and obtain full-fledged anti-tumor immunity. Recent evidence supports the usefulness of 3D ex vivo systems in retaining features of tumor microenvironment to elucidate molecular and immunologic mechanisms of response and resistance to immune checkpoint blockade. In this perspective article we discuss the recent advances in patient-derived 3D tumor models and their potential in support of treatment decision making in clinical setting. We will also share our experience with dynamic bioreactor tumor explant culture of samples from melanoma and sarcoma patients as a reliable and promising platform to unravel immune responses to immune checkpoint inhibitors.

Published
2022

17. Multiple hormonal and metabolic deficiency syndrome predicts outcome in heart failure: the T.O.S.CA. Registry

Author

Cittadini A., Salzano A., Iacoviello M., Triggiani V., Rengo G., Cacciatore F., Maiello C., Limongelli G., Masarone D., Perticone F., Cimellaro A., Filardi P. P., Paolillo S., Mancini A., Volterrani M., Vriz O., Castello R., Passantino A., Campo M., Modesti P. A., de Giorgi A., Monte I. P., Puzzo A., Ballotta A., D'Assante R., Arcopinto M., Gargiulo P., Sciacqua A., Bruzzese D., Colao A., Napoli R., Suzuki T., Eagle K. A., Ventura H. O., Marra A. M., Bossone E., Sacca L., Monti M. G., Matarazzo M., Stagnaro F. M., Piccioli L., Lombardi A., Panicara V., Flora M., Golia L., Faga V., Ruocco A., della Polla D., Franco R., Schiavo A., Gigante A., Spina E., Sicuranza M., Monaco F., Apicella M., Miele C., Campanino A. G., Mazza L., Abete R., Farro A., Luciano F., Polizzi R., Ferrillo G., de Luca M., Crisci G., Giardino F., Barbato M., Ranieri B., Ferrara F., Russo V., Malinconico M., Citro R., Guastalamacchia E., Leone M., Giagulli V. A., Amarelli C., Mattucci I., Calabro P., Calabro R., D'Andrea A., Maddaloni V., Pacileo G., Scarafile R., Belfiore A., Casaretti L., Favuzzi A. M. R., Di Segni C., Bruno C., Vergani E., Massaro R., Grimaldi F., Frigo A., Campo M. R., Sorrentino M. R., Malandrino D., Manfredini R., Fabbian F., Ragusa L., Caliendo L., Carbone L., Frigiola A., Generali T., Giacomazzi F., de Vincentiis C., Garofalo P., Malizia G., Milano S., Misiano G., Israr M. Z., Bernieh D., Cassambai S., Yazaki Y., Heaney L. M., Cittadini, Antonio, Salzano, Andrea, Iacoviello, Massimo, Triggiani, Vincenzo, Rengo, Giuseppe, Cacciatore, Francesco, Maiello, Ciro, Limongelli, Giuseppe, Masarone, Daniele, Perticone, Francesco, Cimellaro, Antonio, Perrone Filardi, Pasquale, Paolillo, Stefania, Mancini, Antonio, Volterrani, Maurizio, Vriz, Olga, Castello, Roberto, Passantino, Andrea, Campo, Michela, Modesti, Pietro A, De Giorgi, Alfredo, Monte, Ines P, Puzzo, Alfonso, Ballotta, Andrea, D'Assante, Roberta, Arcopinto, Michele, Gargiulo, Paola, Sciacqua, Angela, Bruzzese, Dario, Colao, Annamaria, Napoli, Raffaele, Suzuki, Toru, Eagle, Kim A, Ventura, Hector O, Marra, Alberto M, Bossone, Eduardo, Cittadini, A., Salzano, A., Iacoviello, M., Triggiani, V., Rengo, G., Cacciatore, F., Maiello, C., Limongelli, G., Masarone, D., Perticone, F., Cimellaro, A., Filardi, P. P., Paolillo, S., Mancini, A., Volterrani, M., Vriz, O., Castello, R., Passantino, A., Campo, M., Modesti, P. A., de Giorgi, A., Monte, I. P., Puzzo, A., Ballotta, A., D'Assante, R., Arcopinto, M., Gargiulo, P., Sciacqua, A., Bruzzese, D., Colao, A., Napoli, R., Suzuki, T., Eagle, K. A., Ventura, H. O., Marra, A. M., Bossone, E., Sacca, L., Monti, M. G., Matarazzo, M., Stagnaro, F. M., Piccioli, L., Lombardi, A., Panicara, V., Flora, M., Golia, L., Faga, V., Ruocco, A., della Polla, D., Franco, R., Schiavo, A., Gigante, A., Spina, E., Sicuranza, M., Monaco, F., Apicella, M., Miele, C., Campanino, A. G., Mazza, L., Abete, R., Farro, A., Luciano, F., Polizzi, R., Ferrillo, G., de Luca, M., Crisci, G., Giardino, F., Barbato, M., Ranieri, B., Ferrara, F., Russo, V., Malinconico, M., Citro, R., Guastalamacchia, E., Leone, M., Giagulli, V. A., Amarelli, C., Mattucci, I., Calabro, P., Calabro, R., D'Andrea, A., Maddaloni, V., Pacileo, G., Scarafile, R., Belfiore, A., Casaretti, L., Favuzzi, A. M. R., Di Segni, C., Bruno, C., Vergani, E., Massaro, R., Grimaldi, F., Frigo, A., Campo, M. R., Sorrentino, M. R., Malandrino, D., Manfredini, R., Fabbian, F., Ragusa, L., Caliendo, L., Carbone, L., Frigiola, A., Generali, T., Giacomazzi, F., de Vincentiis, C., Garofalo, P., Malizia, G., Milano, S., Misiano, G., Israr, M. Z., Bernieh, D., Cassambai, S., Yazaki, Y., and Heaney, L. M.

Subjects
medicine.medical_specialty, Multiple hormonal and metabolic deficiency syndrome, Epidemiology, Prognosi, Anabolic deficiency, Socio-culturale, Heart failure, 030204 cardiovascular system & hematology, Ventricular Function, Left, 03 medical and health sciences, 0302 clinical medicine, Insulin resistance, Diabetes mellitus, Internal medicine, Multiple hormonal, medicine, Clinical endpoint, Humans, 030212 general & internal medicine, Prospective Studies, Registries, TOSCA, LS4_7, Ejection fraction, business.industry, Hazard ratio, Metabolic deficiency syndrome, Heart failure • Anabolic deficiency • Multiple hormonal and metabolic deficiency syndrome • Hormones • Prognosis • TOSCA, Stroke Volume, medicine.disease, Prognosis, Hormone, Confidence interval, Heart failure, Anabolic deficiency, Multiple hormonal and metabolic deficiency syndrome, Hormones, Prognosis, TOSCA, Hormones, Hospitalization, Observational study, Cardiology and Cardiovascular Medicine, business
Abstract

Aims Recent evidence supports the occurrence of multiple hormonal and metabolic deficiency syndrome (MHDS) in chronic heart failure (CHF). However, no large observational study has unequivocally demonstrated its impact on CHF progression and outcome. The T.O.S.CA. (Trattamento Ormonale nello Scompenso CArdiaco; Hormone Treatment in Heart Failure) Registry has been specifically designed to test the hypothesis that MHDS affects morbidity and mortality in CHF patients. Methods and Results The T.O.S.CA. Registry is a prospective, multicentre, observational study involving 19 Italian centres. Thyroid hormones, insulin-like growth factor-1, total testosterone, dehydropianoandrosterone sulfate, insulin resistance, and the presence of diabetes were evaluated. A MHDS was defined as the presence of ≥2 hormone deficiencies (HDs). Primary endpoint was a composite of all-cause mortality and cardiovascular hospitalizations. Four hundred and eighty heart failure patients with ejection fraction ≤45% were enrolled. MHDS or diabetes was diagnosed in 372 patients (77.5%). A total of 271 events (97 deaths and 174 cardiovascular hospitalizations) were recorded, 41% in NO-MHDS and 62% in MHDS (P Conclusion MHDS is common in CHF and independently associated with increased all-cause mortality and cardiovascular hospitalization, representing a promising therapeutic target. Trial registration ClinicalTrials.gov identifier: NCT023358017

Published
2021

18. Non-thyroidal illness syndrome in chronic diseases: role of irisin as modulator of antioxidants.

Author

MANCINI, A., CAPOBIANCO, E., BRUNO, C., VERGANI, E., NICOLAZZI, M., FAVUZZI, A. M. R., PANOCCHIA, N., MEUCCI, E., MORDENTE, A., and SILVESTRINI, A.

Abstract

OBJECTIVE: Non-thyroidal-illness syndrome (NTIS) refers to condition found in chronic diseases that is an adaptive mechanism. However, oxidative stress is related to NTIS in a vicious circle, due to deiodinases alteration and negative effects of low T3 on antioxidant levels or activity. Muscle is one of the main targets of thyroid hormones and it can secrete a myokine named irisin, which is able to induce the browning of white adipose tissue, energy expenditure and protect against insulin resistance. Inconclusive data have been reported about irisin role in chronic diseases. Moreover, no correlation with antioxidants has been investigated. Therefore, we performed a case-control study with the primary endpoint to evaluate irisin levels in two models of NTIS, such as chronic heart failure (CHF) and chronic kidney disease (CKD) during haemodialytic treatment. The secondary endpoint was the correlation with total antioxidant capacity (TAC) to establish a possible role of irisin in the modulation of antioxidant systems. PATIENTS AND METHODS: Three groups of subjects were enrolled. Group A included CHF patients (n=18; aged 70.22 ± 2.78 ys; BMI ± 27.75 ± 1.28 kg/m2); Group B included CKD patients (n=29; aged 67.03 ± 2.64; BMI 24.53 ± 1.01); finally, 11 normal subjects (Group C) have been enrolled as controls. Irisin has been evaluated by ELISA method and Total Antioxidant Capacity (TAC) by spectrophotometric method. RESULTS: Irisin was significantly higher in Group B vs. A and C groups (Mean ± SEM: 20.18 ± 0.61 ng/ml vs. 2.77 ± 0.77 and 13.06 ± 0.56, respectively; p<0.05); a significant correlation between irisin and TAC was observed in group B. CONCLUSIONS: These preliminary data suggest a possible role of irisin in the modulation of antioxidants in two chronic syndromes with low T3 (i.e., CHF and CKD) with differential pattern in these two models studied. Further insights are needed to confirm this pilot study, which could be the basis for a longitudinal investigation, to assess a prognostic role of irisin with possible therapeutic implications. [ABSTRACT FROM AUTHOR]

Published
2023

19. Oxidative stress and low-grade inflammation in polycystic ovary syndrome: Controversies and new insights

Author

Mancini, Antonio, Bruno, Carmine, Vergani, Edoardo, D'Abate, C., Giacchi, E., Silvestrini, Andrea, Mancini A. (ORCID:0000-0002-7707-4564), Bruno C., Vergani E., Silvestrini A. (ORCID:0000-0002-2005-3746), Mancini, Antonio, Bruno, Carmine, Vergani, Edoardo, D'Abate, C., Giacchi, E., Silvestrini, Andrea, Mancini A. (ORCID:0000-0002-7707-4564), Bruno C., Vergani E., and Silvestrini A. (ORCID:0000-0002-2005-3746)

Abstract

The pathophysiology of Polycystic Ovary Syndrome (PCOS) is quite complex and different mechanisms could contribute to hyperandrogenism and anovulation, which are the main features of the syndrome. Obesity and insulin-resistance are claimed as the principal factors contributing to the clinical presentation; in normal weight PCOS either, increased visceral adipose tissue has been described. However, their role is still debated, as debated are the biochemical markers linked to obesity per se. Oxidative stress (OS) and low-grade inflammation (LGI) have recently been a matter of researcher attention; they can influence each other in a reciprocal vicious cycle. In this review, we summarize the main mechanism of radical generation and the link with LGI. Furthermore, we discuss papers in favor or against the role of obesity as the first pathogenetic factor, and show how OS itself, on the contrary, can induce obesity and insulin resistance; in particular, the role of GH-IGF-1 axis is highlighted. Finally, the possible consequences on vitamin D synthesis and activation on the immune system are briefly discussed. This review intends to underline the key role of oxidative stress and low-grade inflammation in the physiopathology of PCOS, they can cause or worsen obesity, insulin-resistance, vitamin D deficiency, and immune dyscrasia, suggesting an inverse interaction to what is usually considered.

Published
2021

20. Evaluation of kisspeptin levels in prepubertal obese and overweight children: Sexual dimorphism and modulation of antioxidant levels

Author

Mancini, Antonio, Curro', Diego, Cipolla, C., Barini, Angelina, Bruno, Carmine, Vergani, Edoardo, Segni, C. D. I., Guidi, Francesco, Nicolotti, Nicola, Silvestrini, Andrea, Meucci Calabrese, Elisabetta, Valentini, Piero, Rossodivita, Aurora Natalia, Mancini A. (ORCID:0000-0002-7707-4564), Curro D. (ORCID:0000-0001-6726-6872), Barini A. (ORCID:0000-0002-1440-5581), Bruno C., Vergani E., Guidi F., Nicolotti N., Silvestrini A. (ORCID:0000-0002-2005-3746), Meucci E. (ORCID:0000-0002-8821-8041), Valentini P. (ORCID:0000-0001-6095-9510), Rossodivita A. N., Mancini, Antonio, Curro', Diego, Cipolla, C., Barini, Angelina, Bruno, Carmine, Vergani, Edoardo, Segni, C. D. I., Guidi, Francesco, Nicolotti, Nicola, Silvestrini, Andrea, Meucci Calabrese, Elisabetta, Valentini, Piero, Rossodivita, Aurora Natalia, Mancini A. (ORCID:0000-0002-7707-4564), Curro D. (ORCID:0000-0001-6726-6872), Barini A. (ORCID:0000-0002-1440-5581), Bruno C., Vergani E., Guidi F., Nicolotti N., Silvestrini A. (ORCID:0000-0002-2005-3746), Meucci E. (ORCID:0000-0002-8821-8041), Valentini P. (ORCID:0000-0001-6095-9510), and Rossodivita A. N.

Abstract

OBJECTIVE: Kisspeptin, neuropeptide involved in puberty beginning and regulation of pituitary-gonadal axis, has been shown to stimulate antioxidant defenses in murine models. Its levels are greater in females than males and also in obese prepubertal girls. Therefore, our aim was to evaluate sex-related differences in prepubertal obese patients and the relationships of Kisspeptin with metabolic/ hormonal parameters. PATIENTS AND METHODS: We studied Kisspeptin concentrations in 54 children (22 males and 32 females, Tanner stage 1), 5-12 ys, classified according to Cole’s criteria into 17 overweight and 37 obese; 25 normal-weight children, aged 6-12 years, were studied as controls. We evaluated metabolic (glucose and insulin levels after oral glucose load, total- LDL- HDL-cholesterol, triglycerides, uric acid) and hormonal (fT3, fT4, TSH, IGF-1, leptin) parameters. Moreover, total antioxidant capacity (TAC) was evaluated by spectrophotometric method, using the system H202-metmyoglobin-ABTS. Kisspeptin levels were measured by RIA. RESULTS: We did not find significant differences between obese and normal-weight children, but obese males presented significantly lower levels than females. Kisspeptin did not correlate with BMI, HOMA-IR, Insulin peak levels and TAC; a significant correlation was found between Kisspeptin and fT3 (r2=0.25; p=0.003) in the obese group; leptin levels, significantly greater in obese vs. overweight and control children, significantly correlated with TAC (r2=0.39; p=0.03). CONCLUSIONS: These data suggest that both hormones could modulate antioxidants, Kisspeptin indirectly via influence on thyroid hormones, and Leptin by a direct effect. This mechanism seems to be sex-related, not attributable to peripheral steroid levels. Further studies can clarify the complex interrelationship between central and peripheral Kisspeptin secretion and oxidative stress in children obesity.

Published
2021

21. Multiple hormonal and metabolic deficiency syndrome in chronic heart failure: rationale, design, and demographic characteristics of the T.O.S.CA. Registry

Author

Bossone, E., Arcopinto, M., Iacoviello, M., Triggiani, V., Cacciatore, F., Maiello, C., Limongelli, G., Masarone, D., Perticone, F., Sciacqua, A., Perrone-Filardi, P., Mancini, A., Volterrani, M., Vriz, O., Castello, R., Passantino, A., Campo, M., Modesti, P. A., de Giorgi, A., Monte, I., Puzzo, A., Ballotta, A., Caliendo, L., D’Assante, R., Marra, A. M., Salzano, A., Suzuki, T., Cittadini, A., Saccà, L., Monti, M. G., Napoli, R., Matarazzo, M., Stagnaro, F. M., Schiavo, A., Valente, P., Ferrara, F., Russo, V., Malinconico, M., Citro, R., Guastalamacchia, E., Leone, M., Amarelli, C., Mattucci, I., Calabrò, P., Calabrò, R., D’Andrea, A., Maddaloni, V., Pacileo, G., Scarafile, R., Belfiore, A., Cimellaro, A., Perrone Filardi, P., Casaretti, L., Paolillo, S., Gargiulo, P., Favuzzi, A. M. R., Di Segni, C., Bruno, C., Vergani, E., Massaro, R., Grimaldi, F., Frigo, A., Sorrentino, M. R., Malandrino, D., Manfredini, R., Fabbian, F., Ragusa, L., Carbone, L., Frigiola, A., Generali, T., Giacomazzi, F., de Vincentiis, C., Garofalo, P., Malizia, G., Milano, S., Misiano, G., Heaney, L. M., Bruzzese, D., Bossone E., Arcopinto M., Iacoviello M., Triggiani V., Cacciatore F., Maiello C., Limongelli G., Masarone D., Perticone F., Sciacqua A., Perrone-Filardi P., Mancini A., Volterrani M., Vriz O., Castello R., Passantino A., Campo M., Modesti P.A., De Giorgi A., Monte I., Puzzo A., Ballotta A., Caliendo L., D'Assante R., Marra A.M., Salzano A., Suzuki T., Cittadini A., Sacca L., Monti M.G., Napoli R., Matarazzo M., Stagnaro F.M., Schiavo A., Valente P., Ferrara F., Russo V., Malinconico M., Citro R., Guastalamacchia E., Leone M., Amarelli C., Mattucci I., Calabro P., Calabro R., D'Andrea A., Maddaloni V., Pacileo G., Scarafile R., Belfiore A., Cimellaro A., Casaretti L., Paolillo S., Gargiulo P., Favuzzi A.M.R., DiSegni C., Bruno C., Vergani E., Massaro R., Grimaldi F., Frigo A., Sorrentino M.R., Malandrino D., Manfredini R., DeGiorgi A., Fabbian F., Ragusa L., Carbone L., Frigiola A., Generali T., Giacomazzi F., DeVincentiis C., Garofalo P., Malizia G., Milano S., Misiano G., Heaney L.M., Bruzzese D., Bossone, E, Arcopinto, M, Iacoviello, M, Triggiani, V, Cacciatore, F, Maiello, C, Limongelli, G, Masarone, D, Perticone, F, Sciacqua, A, Perrone-Filardi, P, Mancini, A, Volterrani, M, Vriz, O, Castello, R, Passantino, A, Campo, M, A Modesti, P, De Giorgi, A, Monte, I, Puzzo, A, Ballotta, A, Caliendo, L, D'Assante, R, M Marra, A, Salzano, A, Suzuki, T, Cittadini, A, Investigators, Tosca, Bossone, E., Arcopinto, M., Iacoviello, M., Triggiani, V., Cacciatore, F., Maiello, C., Limongelli, G., Masarone, D., Perticone, F., Sciacqua, A., Perrone-Filardi, P., Mancini, A., Volterrani, M., Vriz, O., Castello, R., Passantino, A., Campo, M., Modesti, P. A., de Giorgi, A., Monte, I., Puzzo, A., Ballotta, A., Caliendo, L., D’Assante, R., Marra, A. M., Salzano, A., Suzuki, T., Cittadini, A., Saccà, L., Monti, M. G., Napoli, R., Matarazzo, M., Stagnaro, F. M., Schiavo, A., Valente, P., Ferrara, F., Russo, V., Malinconico, M., Citro, R., Guastalamacchia, E., Leone, M., Amarelli, C., Mattucci, I., Calabrò, P., Calabrò, R., D’Andrea, A., Maddaloni, V., Pacileo, G., Scarafile, R., Belfiore, A., Cimellaro, A., Perrone Filardi, P., Casaretti, L., Paolillo, S., Gargiulo, P., Favuzzi, A. M. R., Di Segni, C., Bruno, C., Vergani, E., Massaro, R., Grimaldi, F., Frigo, A., Sorrentino, M. R., Malandrino, D., Manfredini, R., Fabbian, F., Ragusa, L., Carbone, L., Frigiola, A., Generali, T., Giacomazzi, F., de Vincentiis, C., Garofalo, P., Malizia, G., Milano, S., Misiano, G., Heaney, L. M., and Bruzzese, D.

Subjects
Male, Anabolism, medicine.medical_treatment, 030204 cardiovascular system & hematology, law.invention, 0302 clinical medicine, Randomized controlled trial, law, Clinical endpoint, Medicine, Deficiency Disease, 030212 general & internal medicine, Prospective Studies, Registries, Prospective cohort study, Testosterone, Anabolic deficiency, Chronic heart failure, Heart failure metabolism, Multiple hormonal deficiency syndrome, Registry, Aged, Biomarkers, Chronic Disease, Deficiency Diseases, Disease Progression, Female, Heart Failure, Humans, Italy, Metabolic Diseases, Middle Aged, Internal Medicine, Emergency Medicine, Human, medicine.medical_specialty, Anabolic deficiency, Chronic heart failure, Heart failure metabolism, Multiple hormonal deficiency syndrome, Registry, Socio-culturale, 03 medical and health sciences, Internal medicine, business.industry, Settore MED/13 - ENDOCRINOLOGIA, Biomarker, medicine.disease, Metabolic Disease, Prospective Studie, Heart failure, Observational study, Hormone therapy, business
Abstract

Recent evidence supports the concept that progression of chronic heart failure (CHF) depends upon an imbalance of catabolic forces over the anabolic drive. In this regard, multiple hormonal deficiency syndrome (MHDS) significantly has impacts upon CHF progression, and is associated with a worse clinical status and increased mortality. The T.O.S.CA. (Trattamento Ormonale nello Scompenso CArdiaco; Hormone Therapy in Heart Failure) Registry (clinicaltrial.gov = NCT02335801) tests the hypothesis that anabolic deficiencies reduce survival in a large population of mild-to-moderate CHF patients. The T.O.S.CA. Registry is a prospective multicenter observational study coordinated by “Federico II” University of Naples, and involves 19 centers situated throughout Italy. Thyroid hormones, insulin-like growth factor-1, total testosterone, dehydroepiandrosterone , and insulin are measured at baseline and every year for a patient-average follow-up of 3years. Subjects with CHF are divided into two groups: patients with one or no anabolic deficiency, and patients with two or more anabolic deficiencies at baseline. The primary endpoint is the composite of all-cause mortality and cardiovascular hospitalization. Secondary endpoints include the composite of all-cause mortality and hospitalization, the composite of cardiovascular mortality and cardiovascular hospitalization, and change of VO 2 peak. Patient enrollment started in April 2013, and was completed in July 2017. Demographics and main clinical characteristics of enrolled patients are provided in this article. Detailed cross-sectional results will be available in late 2018. The T.O.S.CA. Registry represents the most robust prospective observational trial on MHDS in the field of CHF. The study findings will advance our knowledge with regard to the intimate mechanisms of CHF progression and hopefully pave the way for future randomized clinical trials of single or multiple hormonal replacement therapies in CHF.

Published
2017

22. The role of selenium in oxidative stress and in nonthyroidal illness syndrome (NTIS): An overview

Author

Silvestrini, Andrea, Mordente, Alvaro, Martino, G., Bruno, Carmine, Vergani, Edoardo, Meucci Calabrese, Elisabetta, Mancini, Antonio, Silvestrini A. (ORCID:0000-0002-2005-3746), Mordente A. (ORCID:0000-0003-3260-9796), Bruno C., Vergani E., Meucci E. (ORCID:0000-0002-8821-8041), Mancini A. (ORCID:0000-0002-7707-4564), Silvestrini, Andrea, Mordente, Alvaro, Martino, G., Bruno, Carmine, Vergani, Edoardo, Meucci Calabrese, Elisabetta, Mancini, Antonio, Silvestrini A. (ORCID:0000-0002-2005-3746), Mordente A. (ORCID:0000-0003-3260-9796), Bruno C., Vergani E., Meucci E. (ORCID:0000-0002-8821-8041), and Mancini A. (ORCID:0000-0002-7707-4564)

Abstract

Selenium is a trace element, nutritionally classified as an essential micronutrient, involved in maintaining the correct function of several enzymes incorporating the selenocysteine residue, namely the selenoproteins. The human selenoproteome including 25 proteins is extensively described here. The most relevant selenoproteins, including glutathione peroxidases, thioredoxin reductases and iodothyronine deiodinases are required for the proper cellular redox homeostasis as well as for the correct thyroid function, thus preventing oxidative stress and related diseases. This review summarizes the main advances on oxidative stress with a focus on selenium metabolism and transport. Moreover, thyroid-related disorders are discussed, considering that the thyroid gland contains the highest selenium amount per gram of tissue, also for future possible therapeutic implication.

Published
2020

23. Plasmatic lipocalin-2 levels in chronic low-grade inflammation syndromes: Comparison between metabolic syndrome, total and partial adult growth hormone deficiency

Author

Curro', Diego, Vergani, E., Bruno, C., Comi, S., D'Abate, C., Mancini, Antonio, Currò (ORCID:0000-0001-6726-6872), Mancini A. (ORCID:0000-0002-7707-4564), Curro', Diego, Vergani, E., Bruno, C., Comi, S., D'Abate, C., Mancini, Antonio, Currò (ORCID:0000-0001-6726-6872), and Mancini A. (ORCID:0000-0002-7707-4564)

Abstract

Lipocalin-2 (LCN2) is a secreted glycoprotein involved in several chronic inflammatory processes. Metabolic syndrome (MetS) and adult growth hormone deficiency (GHD) are known as chronic inflammatory conditions. The primary objective of this observational cross-sectional study was to compare LCN2 plasmatic levels in these clinical settings, whereas the secondary objective was to investigate any possible correlation between LCN2 and BMI and/or indexes of insulin sensitivity/resistance. Seventy-four patients were divided as follows: Group A, MetS (18 patients, 13 females and 5 males, mean ± SEM age 45.1 ± 4.11 years, BMI 31.22 ± 1.73 kg/m2); Group B, total GHD (18 patients, 8 females and 10 males, age 52.44 ± 2.61 years, BMI 30.49 ± 1.87 kg/m2); Group C, Partial GHD (pGHD; 19 patients, 13 females and 6 males, age 48.63 ± 2.19 years, BMI 29.11 ± 1.85 kg/m2); Group D, Controls (19 patients, 13 females and 6males, age 40.26 ± 2.87 years, BMI 23.25 ± 0.95 kg/m2). They were evaluated for glucose and insulin, HOMA-index, QUICKI-index, Total/low-density lipoprotein/high-density lipoprotein cholesterol, triglycerides, uric acid, IGF-1, and LCN2. LCN2 plasmatic levels were significantly increased in MetS, while no significant differences with controls were found in total and pGHD. LCN2 levels did not correlate with BMI. A significant positive correlation between LCN2 and HOMA-index was found in controls, while a trend-like, yet not significant, a positive correlation was observed in pGHD. Our data show an increase in LCN2 plasmatic levels in MetS. Different inflammatory patterns characterize MetS and GHD. The correlation between HOMA index and LCN2 in normal subjects and possibly in pGHD ones suggests a modulatory action of LCN2 on insulin resistance.

Published
2020

26. Circulating irisin levels in heart failure with preserved or reduced ejection fraction: A pilot study

Author

Silvestrini, Andrea, Bruno, Carmine, Vergani, E, Venuti, A, Favuzzi, Angela Maria Rita, Guidi, F, Nicolotti, Nicola, Meucci Calabrese, Elisabetta, Mordente, Alvaro, Mancini, Antonio, Silvestrini A (ORCID:0000-0002-2005-3746), Bruno C, Favuzzi AMR, Nicolotti N, Meucci E (ORCID:0000-0002-8821-8041), Mordente A (ORCID:0000-0003-3260-9796), Mancini A (ORCID:0000-0002-7707-4564), Silvestrini, Andrea, Bruno, Carmine, Vergani, E, Venuti, A, Favuzzi, Angela Maria Rita, Guidi, F, Nicolotti, Nicola, Meucci Calabrese, Elisabetta, Mordente, Alvaro, Mancini, Antonio, Silvestrini A (ORCID:0000-0002-2005-3746), Bruno C, Favuzzi AMR, Nicolotti N, Meucci E (ORCID:0000-0002-8821-8041), Mordente A (ORCID:0000-0003-3260-9796), and Mancini A (ORCID:0000-0002-7707-4564)

Abstract

Irisin, a recently discovered myokine, has been considered a prognostic factor in several cardiovascular diseases. Nevertheless, no data are available on the role of irisin in patients with heart failure (HF), both with preserved (HFpEF) or reduced (HFrEF) ejection fraction. We have therefore evaluated the circulating irisin levels in HFpEF and HFrEF patients, correlating them with metabolic parameters and total antioxidant capacity (TAC), as index of oxidative stress. Irisin was significantly higher in HFpEF than in HFrEF patients (7.72 ± 0.76 vs 2.77 ± 0.77 ng/ml, respectively). An inverse correlation between irisin and TAC was found in HFpEF, but not in HFrEF. Conversely, no correlation was present with HOMA index. These data support the hypothesis that a different pathophysiological mechanism is involved in the two HF subtypes, and oxidative stress modulates irisin secretion.

Published
2019

27. Saperi stretti e saperi larghi: per un’epistemologia del lavoro sociale ed educativo

Author

Tumminelli G., Vergani E., Tumminelli G., and Vergani E.

Subjects
Saperi stretti, saperi larghi, professioni d'aiuto, idea di scientificità, intervento sociale
Abstract

This contribution stems from the need to start a first theoretical reflection within social work. Therefore, the objective of our paper is the problematization of theknowledge that is associated with the helping professions, deconstructing them and rethinking them in a broader perspective, starting from the crisis of modernity and from the transformations triggered by globalization. This contribution wants to offer a track on which to start an epistemological reflection.

Published
2017

28. Evaluation of immunoglobulins subclasses and free-light chains in non-obese patients with polycystic ovary syndrome and correlations with hormonal and metabolic parameters: preliminary data.

Author

BASILE, U., BRUNO, C., NAPODANO, C., VERGANI, E., GULLI, F., PIUNNO, G., POCINO, K., STEFANILE, A., and MANCINI, A.

Abstract

OBJECTIVE: Polycystic ovary syndrome (PCOS) is characterized by hyperandrogenism and hyperinsulinemia thaontrol study to investigate inflammatory and immunological parameters, such as Igt contribute to create a state of chronic low-grade inflammation. We performed an observational case-cG subclasses and free light chains (FLCs) and hemolytic complement activity (CH50) in non-obese PCOS, evaluating their relations with metabolic and hormonal parameters. PATIENTS AND METHODS: 36 subjects were studied: 16 PCOS patients (mean±SEM 27.13±1.82 age; BMI 24.1±0.9 kg/m2); 20 controls (aged 26.05±0.73; BMI 20.8 ± 0.4 kg/m2). The blood sample was collected for metabolic and hormonal parameters, IgG subclasses, k and λ FLCs, CH50. Hormones were measured by immunochemiluminometric assays; metabolic parameters by enzymatic assays; subclasses of IgG, FLCs, and CH50 were evaluated by the turbidimetric method. RESULTS: PCOS patients showed vs. controls lower IgG1, IgG2, IgG3 (mean±SEM 3.76±0.29 g/l, 2.63±0.20, 0.62±0.06, 0.34±0.08 vs. 6.49±0.35, 4.28±0.25, 0.84±0.07, 0.33±0.04, respectively) and higher levels of FLCs (k 12.22±0.71 vs. 6.03±0.30, λ 10.10±0.79 vs. 8.04±0.48 g/l) and CH50 (48.64±2.65 vs. 36.51±1.38 U/ml); we found correlation between IgG2 and free-testosterone (r=0.72, p=0.005) and CH50 and vitamin D (r=0.54, p=0.04); an inverse correlation was found between IgG1 and, respectively, ACTH (r=-0.57, p=0.02) and cortisol (r=0.78, p=0.001) in PCOS. CONCLUSIONS: In the complex scenario of low-grade inflammation in non-obese PCOS, we showed lower levels of main subclasses of IgG and higher CH50 levels, suggesting the involvement of other mechanisms other than the "classical" pathway of complement activation; FLCs could be attractive to monitor inflammation degree, disease activity and influence on hormonal status. [ABSTRACT FROM AUTHOR]

Published
2021

29. Oxidative stress as a possible mechanism underlying multi-hormonal deficiency in chronic heart failure

Author

Mancini, Antonio, Vergani, E, Bruno, C, Olivieri, Giorgia, C Segni Di, Silvestrini, Andrea, Venuti, A, Favuzzi, Angela Maria Rita, and Meucci Calabrese, Elisabetta

Subjects
Heart Failure, Oxidative Stress, Myocardium, Chronic Disease, Animals, Humans, Settore MED/13 - ENDOCRINOLOGIA, Settore BIO/10 - BIOCHIMICA, Hormones
Abstract

Chronic Heart Failure (CHF) is associated with multi-hormonal derangement depicting a prevalence of catabolic vs. anabolic axes. Moreover, thyroid adaption is characterized by the reduced conversion of thyroxine to the active hormone triiodothyronine. On the other hand, hormones modulate synthesis and utilization of antioxidant systems. Therefore, hormonal failure can cause unbalance between reactive radical species and the defenses, resulting in oxidative stress (OS). OS is well described in CHF, but the relationship with the hormonal picture is not entirely known. In the present review, we firstly analyze the mechanisms of ROS production in the heart, discussing animal and human studies, and focusing on new discovered protective mechanisms such as sirtuins and fibroblast growth factor 21 (FGF21). The second section is dedicated to the role of main anabolic axes influencing antioxidant systems. Finally, we present some data supporting the hypothesis that OS could be the link between hormonal derangement and clinical outcome of CHF.

Published
2018

30. Multiple hormonal and metabolic deficiency syndrome in chronic heart failure: rationale, design, and demographic characteristics of the T.O.S.CA. Registry

Author

Bossone, E., Arcopinto, M., Iacoviello, M., Triggiani, V., Cacciatore, F., Maiello, C., Limongelli, G., Masarone, D., Perticone, F., Sciacqua, A., Perrone-Filardi, P., Mancini, Antonio, Volterrani, M., Vriz, O., Castello, R., Passantino, A., Campo, Marco, Modesti, P. A., De Giorgi, A., Monte, I., Puzzo, A., Ballotta, A., Caliendo, L., D'Assante, R., Marra, A. M., Salzano, A., Suzuki, T., Cittadini, Achille Renato Maria, Sacca, L., Monti, M. G., Napoli, R., Matarazzo, M., Stagnaro, F. M., Schiavo, A., Valente, P., Ferrara, F., Russo, V., Malinconico, M., Citro, R., Guastalamacchia, E., Leone, M., Amarelli, C., Mattucci, I., Calabro, P., Calabro, R., D'Andrea, A., Maddaloni, V., Pacileo, G., Scarafile, R., Belfiore, A., Cimellaro, A., Casaretti, L., Paolillo, S., Gargiulo, P., Favuzzi, Angela Maria Rita, Disegni, C., Bruno, C., Vergani, Edoardo, Massaro, R., Grimaldi, F., Frigo, A., Sorrentino, M. R., Malandrino, D., Manfredini, R., Fabbian, F., Ragusa, L., Carbone, Luigi, Frigiola, A., Generali, T., Giacomazzi, F., Devincentiis, C., Garofalo, P., Malizia, G., Milano, S., Misiano, G., Heaney, L. M., Bruzzese, D., Mancini A. (ORCID:0000-0002-7707-4564), Campo M., Cittadini A., Favuzzi A. M. R., Vergani E., Carbone L., Bossone, E., Arcopinto, M., Iacoviello, M., Triggiani, V., Cacciatore, F., Maiello, C., Limongelli, G., Masarone, D., Perticone, F., Sciacqua, A., Perrone-Filardi, P., Mancini, Antonio, Volterrani, M., Vriz, O., Castello, R., Passantino, A., Campo, Marco, Modesti, P. A., De Giorgi, A., Monte, I., Puzzo, A., Ballotta, A., Caliendo, L., D'Assante, R., Marra, A. M., Salzano, A., Suzuki, T., Cittadini, Achille Renato Maria, Sacca, L., Monti, M. G., Napoli, R., Matarazzo, M., Stagnaro, F. M., Schiavo, A., Valente, P., Ferrara, F., Russo, V., Malinconico, M., Citro, R., Guastalamacchia, E., Leone, M., Amarelli, C., Mattucci, I., Calabro, P., Calabro, R., D'Andrea, A., Maddaloni, V., Pacileo, G., Scarafile, R., Belfiore, A., Cimellaro, A., Casaretti, L., Paolillo, S., Gargiulo, P., Favuzzi, Angela Maria Rita, Disegni, C., Bruno, C., Vergani, Edoardo, Massaro, R., Grimaldi, F., Frigo, A., Sorrentino, M. R., Malandrino, D., Manfredini, R., Fabbian, F., Ragusa, L., Carbone, Luigi, Frigiola, A., Generali, T., Giacomazzi, F., Devincentiis, C., Garofalo, P., Malizia, G., Milano, S., Misiano, G., Heaney, L. M., Bruzzese, D., Mancini A. (ORCID:0000-0002-7707-4564), Campo M., Cittadini A., Favuzzi A. M. R., Vergani E., and Carbone L.

Abstract

Recent evidence supports the concept that progression of chronic heart failure (CHF) depends upon an imbalance of catabolic forces over the anabolic drive. In this regard, multiple hormonal deficiency syndrome (MHDS) significantly has impacts upon CHF progression, and is associated with a worse clinical status and increased mortality. The T.O.S.CA. (Trattamento Ormonale nello Scompenso CArdiaco; Hormone Therapy in Heart Failure) Registry (clinicaltrial.gov = NCT02335801) tests the hypothesis that anabolic deficiencies reduce survival in a large population of mild-to-moderate CHF patients. The T.O.S.CA. Registry is a prospective multicenter observational study coordinated by “Federico II” University of Naples, and involves 19 centers situated throughout Italy. Thyroid hormones, insulin-like growth factor-1, total testosterone, dehydroepiandrosterone , and insulin are measured at baseline and every year for a patient-average follow-up of 3 years. Subjects with CHF are divided into two groups: patients with one or no anabolic deficiency, and patients with two or more anabolic deficiencies at baseline. The primary endpoint is the composite of all-cause mortality and cardiovascular hospitalization. Secondary endpoints include the composite of all-cause mortality and hospitalization, the composite of cardiovascular mortality and cardiovascular hospitalization, and change of VO2 peak. Patient enrollment started in April 2013, and was completed in July 2017. Demographics and main clinical characteristics of enrolled patients are provided in this article. Detailed cross-sectional results will be available in late 2018. The T.O.S.CA. Registry represents the most robust prospective observational trial on MHDS in the field of CHF. The study findings will advance our knowledge with regard to the intimate mechanisms of CHF progression and hopefully pave the way for future randomized clinical trials of single or multiple hormonal replacement therapies in CHF.

Published
2018

31. Evaluation of kisspeptin levels in prepubertal obese and overweight children: sexual dimorphism and modulation of antioxidant levels.

Author

MANCINI, A., CURRÒ, D., CIPOLLA, C., BARINI, A., BRUNO, C., VERGANI, E., DI SEGNI, C., GUIDI, F., NICOLOTTI, N., SILVESTRINI, A., MEUCCI, E., VALENTINI, P., and ROSSODIVITA, A. N.

Abstract

OBJECTIVE: Kisspeptin, neuropeptide involved in puberty beginning and regulation of pituitary-gonadal axis, has been shown to stimulate antioxidant defenses in murine models. Its levels are greater in females than males and also in obese prepubertal girls. Therefore, our aim was to evaluate sex-related differences in prepubertal obese patients and the relationships of Kisspeptin with metabolic/hormonal parameters. PATIENTS AND METHODS: We studied Kisspeptin concentrations in 54 children (22 males and 32 females, Tanner stage 1), 5-12 ys, classified according to Cole's criteria into 17 overweight and 37 obese; 25 normal-weight children, aged 6-12 years, were studied as controls. We evaluated metabolic (glucose and insulin levels after oral glucose load, total- LDL- HDL-cholesterol, triglycerides, uric acid) and hormonal (fT3, fT4, TSH, IGF-1, leptin) parameters. Moreover, total antioxidant capacity (TAC) was evaluated by spectrophotometric method, using the system H202-metmyoglobin-ABTS. Kisspeptin levels were measured by RIA. RESULTS: We did not find significant differences between obese and normal-weight children, but obese males presented significantly lower levels than females. Kisspeptin did not correlate with BMI, HOMA-IR, Insulin peak levels and TAC; a significant correlation was found between Kisspeptin and fT3 (r2=0.25; p=0.003) in the obese group; leptin levels, significantly greater in obese vs. overweight and control children, significantly correlated with TAC (r2=0.39; p=0.03). CONCLUSIONS: These data suggest that both hormones could modulate antioxidants, Kisspeptin indirectly via influence on thyroid hormones, and Leptin by a direct effect. This mechanism seems to be sex-related, not attributable to peripheral steroid levels. Further studies can clarify the complex interrelationship between central and peripheral Kisspeptin secretion and oxidative stress in children obesity. [ABSTRACT FROM AUTHOR]

Published
2021

32. Recurrent hepatocellular carcinoma and non-classic adreno-genital syndrome.

Author

VERGANI, E., BRUNO, C., RAIMONDO, S., MACIS, G., VECCHIO, F. M., RICCARDI, L., PONZIANI, F. R., POMPILI, M., and MANCINI, A.

Abstract

OBJECTIVE: Hepatocellular carcinoma (HCC) is one of the most common fatal cancer in the world and androgens are among the possible etiological factors. Congenital adrenal hyperplasia (CAH) is a group of inherited diseases caused by enzyme failure in the steroid biosynthesis of the adrenal cortex, resulting in an augmented 17-hydroxyprogesterone, androstenedione and testosterone production. While the occurrence of testicular adrenal rest tumors and adrenocortical tumors in congenital adrenal hyperplasia is well described in the literature, no data on HCC occurrence are available. CASE PRESENTATION: A 35-years-old Italian man of Caucasian origin, affected by non-classic CAH due to partial 21-hydroxylase deficiency came to observation for revaluation of his adrenal picture. Besides common hormonal and biochemical analysis, an abdomen Magnetic Resonance Imaging was performed, resulting in an 18 mm large nodular lesion between liver segments VII and VIII. Radiological reports matched with an increased serum a-fetoprotein level. A surgical removal of the lesion was performed. After that, several recurrences of the lesion, which was consequently treated by radiofrequency ablation, occurred. Every recurrence was accompanied by an increase in testosterone and steroid hormone binding globulin serum levels. CONCLUSIONS: Our report suggests the need for screening of liver lesions in males affected by this syndrome. [ABSTRACT FROM AUTHOR]

Published
2020

33. Ricostruzione delle caratteristiche tessiturali e dei parametri idraulici nella bassa pianura lombarda (Lodi e Cremona)

Author

Bonomi, T, Canepa, P, DEL ROSSO, F, Crestana, B, Vergani, E, BONOMI, TULLIA, CANEPA, PAOLA, DEL ROSSO, FRANCESCA, Vergani, E., Bonomi, T, Canepa, P, DEL ROSSO, F, Crestana, B, Vergani, E, BONOMI, TULLIA, CANEPA, PAOLA, DEL ROSSO, FRANCESCA, and Vergani, E.

Abstract

The suggested methodology concerns the structural reconstruction of the shallow aquifer in the distal meander plain of Lombardy region. The aim of the work is to reproduce the heterogeneity of the fluvial and the glacio-fluvial sediments in the subsoil and the heterogeneity of hydraulic conductivity and effective porosity, that may be the input of a groundwater flow model. We would like to exceed the strong subdivision into aquifers and aquitards and to introduce the concept of textural changing inside an aquifer. The first step is a detailed quantitative reconstruction of subsoil textural characteristics in the study area. It is necessary to collect and store in a specific hydrologic database, TANGRAM, the highest and the most reliable number of georeferenced water wells with their own stratigraphic data: each stratigraphic level is codified and, during the extraction step, is translated in textural percentage classes (gravel, sand and clay) according to a vertical subdivision, chosen by the user. The second step is to estimate the hydraulic conductivity and effective porosity values, used a linked database module. Literature values for the parameters of cobbles, gravel, sand and clay are taken into account. The idea is to associate a value of hydraulic conductivity or effective porosity with different textural percentages, weighted by the scaling described approach. The last step is to link the specific hydrologic database and a three-dimensional modelling software GOCAD (Geological Object Computer Aided Design). The data, extracted from Tangram, are elaborated within a three-dimensional grid, built according to the boundary surfaces of the hydrogeological system (the topographic surface and the aquifer bottom): the properties are interpolated, using the powerful three-dimensional interpolator inside Gocad. Results are a three-dimensional rebuilding of the heterogeneous distribution of textural percentages or hydraulic parameters into the whole studied volume of t

Published
2009

34. TNF-related apoptosis-inducing ligand (trail)-armed exosomes deliver proapoptotic signals to tumor site

Author

Rivoltini, L, Chiodoni, C, Squarcina, P, Tortoreto, M, Villa, A, Vergani, B, Bürdek, M, Botti, L, Arioli, I, Cova, A, Mauri, G, Vergani, E, Bianchi, B, Della Mina, P, Cantone, L, Bollati, V, Zaffaroni, N, Gianni, A, Colombo, M, Huber, V, Rivoltini, L, Chiodoni, C, Squarcina, P, Tortoreto, M, Villa, A, Vergani, B, Bürdek, M, Botti, L, Arioli, I, Cova, A, Mauri, G, Vergani, E, Bianchi, B, Della Mina, P, Cantone, L, Bollati, V, Zaffaroni, N, Gianni, A, Colombo, M, and Huber, V

Abstract

Purpose: Exosomes deliver signals to target cells and could thus be exploited as an innovative therapeutic tool. We investigated the ability of membrane TRAIL-armed exosomes to deliver proapoptotic signals to cancer cells and mediate growth inhibition in different tumor models. Experimental Methods and Results: K562 cells, transduced with lentiviral human membrane TRAIL, were used for the production of TRAIL+ exosomes, which were studied by nanoparticle tracking analysis, cytofluorimetry, immunoelectronmicroscopy, Western blot, and ELISA. In vitro, TRAIL+ exosomes induced more pronounced apoptosis (detected by Annexin V/ propidium iodide and activated caspase-3) in TRAIL-death receptor (DR)5+ cells (SUDHL4 lymphoma and INT12 melanoma), with respect to the DR5 - DR4+ KMS11 multiple myeloma. Intratumor injection of TRAIL+ exosomes, but not mock exosomes, induced growth inhibition of SUDHL4 (68%) and INT12 (51%), and necrosis in KMS11 tumors. After rapid blood clearance, systemically administered TRAIL+ exosomes accumulatedintheliver,lungs,andspleenandhomedtothetumor site, leading to a significant reduction of tumor growth (58%) in SUDHL4-bearing mice. The treatment of INT12-bearing animals promoted tumor necrosis and a not statistically significant tumor volume reduction. In KMS11-bearing mice, despite massive perivascular necrosis, no significant tumor growth inhibition was detected. Conclusions: TRAIL-armed exosomes can induce apoptosis in cancer cells and control tumor progression in vivo. Therapeutic efficacy was particularly evident in intratumor setting, while depended on tumor model upon systemic administration. Thanks to their ability to deliver multiple signals, exosomes thus represent a promising therapeutic tool in cancer.

Published
2016

35. Overcoming melanoma resistance to vemurafenib by targeting CCL2-induced miR-34a, miR-100 and miR-125b

Author

Vergani, E, Di Guardo, L, Dugo, M, Rigoletto, S, Tragni, G, Ruggeri, R, Perrone, F, Tamborini, E, Gloghini, A, Arienti, F, Vergani, B, Deho, P, De Cecco, L, Vallacchi, V, Frati, P, Shahaj, E, Villa, A, Santinami, M, De Braud, F, Rivoltini, L, Rodolfo, M, Rodolfo, M., VERGANI, BARBARA, VILLA, ANTONELLO, Vergani, E, Di Guardo, L, Dugo, M, Rigoletto, S, Tragni, G, Ruggeri, R, Perrone, F, Tamborini, E, Gloghini, A, Arienti, F, Vergani, B, Deho, P, De Cecco, L, Vallacchi, V, Frati, P, Shahaj, E, Villa, A, Santinami, M, De Braud, F, Rivoltini, L, Rodolfo, M, Rodolfo, M., VERGANI, BARBARA, and VILLA, ANTONELLO

Abstract

In melanoma, the adaptative cell response to BRAF inhibitors includes altered patterns of cytokine production contributing to tumor progression and drug resistance. Among the factors produced by PLX4032-resistant melanoma cell lines, CCL2 was higher compared to the sensitive parental cell lines and increased upon drug treatment. CCL2 acted as an autocrine growth factor for melanoma cells, stimulating the proliferation and resistance to apoptosis. In patients, CCL2 is detected in melanoma cells in tumors and in plasma at levels that correlate with tumor burden and lactate dehydrogenase. Vemurafenib treatment increased the CCL2 levels in plasma, whereas the long-term clinical response was associated with low CCL2 levels. Increased CCL2 production was associated with miRNA deregulation in the resistant cells. miR-34a, miR-100 and miR-125b showed high expression in both resistant cells and in tumor biopsies that were obtained from treated patients, and they were involved in the control of cell proliferation and apoptosis. Inhibition of CCL2 and of the selected miRNAs restored both the cell apoptosis and the drug efficacy in resistant melanoma cells. Therefore, CCL2 and miRNAs are potential prognostic factors and attractive targets for counteracting treatment resistance in metastatic melanoma.

Published
2016

36. Ricostruzione delle caratteristiche tessiturali e dei parametri idraulici nella bassa pianura lombarda (Lodi e Cremona)

Author

BONOMI, TULLIA, CANEPA, PAOLA, DEL ROSSO, FRANCESCA, Crestana, B, Vergani, E., Bonomi, T, Canepa, P, DEL ROSSO, F, Crestana, B, and Vergani, E

Subjects
Heterogeneity, hydrologic database, three-dimensional rebuilding, GEO/05 - GEOLOGIA APPLICATA
Abstract

The suggested methodology concerns the structural reconstruction of the shallow aquifer in the distal meander plain of Lombardy region. The aim of the work is to reproduce the heterogeneity of the fluvial and the glacio-fluvial sediments in the subsoil and the heterogeneity of hydraulic conductivity and effective porosity, that may be the input of a groundwater flow model. We would like to exceed the strong subdivision into aquifers and aquitards and to introduce the concept of textural changing inside an aquifer. The first step is a detailed quantitative reconstruction of subsoil textural characteristics in the study area. It is necessary to collect and store in a specific hydrologic database, TANGRAM, the highest and the most reliable number of georeferenced water wells with their own stratigraphic data: each stratigraphic level is codified and, during the extraction step, is translated in textural percentage classes (gravel, sand and clay) according to a vertical subdivision, chosen by the user. The second step is to estimate the hydraulic conductivity and effective porosity values, used a linked database module. Literature values for the parameters of cobbles, gravel, sand and clay are taken into account. The idea is to associate a value of hydraulic conductivity or effective porosity with different textural percentages, weighted by the scaling described approach. The last step is to link the specific hydrologic database and a three-dimensional modelling software GOCAD (Geological Object Computer Aided Design). The data, extracted from Tangram, are elaborated within a three-dimensional grid, built according to the boundary surfaces of the hydrogeological system (the topographic surface and the aquifer bottom): the properties are interpolated, using the powerful three-dimensional interpolator inside Gocad. Results are a three-dimensional rebuilding of the heterogeneous distribution of textural percentages or hydraulic parameters into the whole studied volume of the subsoil. This procedure has been used within some different province in Lombardy, like Lodi and Cremona, where more than 1000 stratigraphic data were collected, codified and stored. In this work the first results are shown.

Published
2009

40. Transcriptional profiling of melanoma sentinel nodes identify patients with poor outcome and reveal an association of CD30(+) T lymphocytes with progression

Author

Vallacchi, V, Vergani, E, Camisaschi, C, Deho, P, Cabras, A, Sensi, M, De Cecco, L, Bassani, N, Ambrogi, F, Carbone, A, Crippa, F, Vergani, B, Frati, P, Arienti, F, Patuzzo, R, Villa, A, Biganzoli, E, Canevari, S, Santinami, M, Castelli, C, Rivoltini, L, Rodolfo, M, VERGANI, BARBARA, VILLA, ANTONELLO, Rodolfo, M., Vallacchi, V, Vergani, E, Camisaschi, C, Deho, P, Cabras, A, Sensi, M, De Cecco, L, Bassani, N, Ambrogi, F, Carbone, A, Crippa, F, Vergani, B, Frati, P, Arienti, F, Patuzzo, R, Villa, A, Biganzoli, E, Canevari, S, Santinami, M, Castelli, C, Rivoltini, L, Rodolfo, M, VERGANI, BARBARA, VILLA, ANTONELLO, and Rodolfo, M.

Abstract

Sentinel lymph nodes set the stance of the immune system to a localized tumor and are often the first site to be colonized by neoplastic cells that metastasize. To investigate how the presence of neoplastic cells in sentinel lymph nodes may trigger pathways associated with metastatic progression, we analyzed the transcriptional profiles of archival sentinel node biopsy specimens obtained from melanoma patients. Biopsies from positive nodes were selected for comparable tumor infiltration, presence or absence of further regional node metastases, and relapse at 5-year follow-up. Unsupervised analysis of gene expression profiles revealed immune response to be a major gene ontogeny represented. Among genes upregulated in patients with progressing disease, the TNF receptor family member CD30/TNFRSF8 was confirmed in biopsy specimens from an independent group of patients. Immunohistochemical analysis revealed higher numbers of CD30(+) lymphocytes in nodes from progressing patients compared with nonprogressing patients. Phenotypic profiling demonstrated that CD30(+) lymphocytes comprised a broad population of suppressive or exhausted immune cells, such as CD4(+)Foxp3(+) or PD1(+) subpopulations and CD4(-)CD8(-) T cells. CD30(+) T lymphocytes were increased in peripheral blood lymphocytes of melanoma patients at advanced disease stages. Our findings reinforce the concept that sentinel nodes act as pivotal sites for determining progression patterns, revealing that the presence of CD30(+) lymphocytes at those sites associate positively with melanoma progression.

Published
2014

41. How did al-Gazali conceptualize philosophy?

Author

Baffioni, Carmela, Finazzi, Rosa, Dell'Acqua, Anna, Vergani, Emidio, Baffioni, C ( Carmela ), Finazzi, R ( Rosa ), Dell'Acqua, A ( Anna ), Vergani, E ( Emidio ), Rudolph, Ulrich, Baffioni, Carmela, Finazzi, Rosa, Dell'Acqua, Anna, Vergani, Emidio, Baffioni, C ( Carmela ), Finazzi, R ( Rosa ), Dell'Acqua, A ( Anna ), Vergani, E ( Emidio ), and Rudolph, Ulrich

Published
2013

45. 3D tumor explant as a novel platform to investigate therapeutic pathways and predictive biomarkers in cancer patients

Author

Rodolfo, Monica, Huber, Veronica, Cossa, Mara, Gallino, Gianfrancesco, Leone, Biagio E., Vallacchi, Viviana, Rivoltini, Licia, Vergani, Elisabetta, Rodolfo, M, Huber, V, Cossa, M, Gallino, G, Leone, B, Vallacchi, V, Rivoltini, L, and Vergani, E

Subjects
bioreactor, sarcoma, Immunology, melanoma, Immunology and Allergy, immunotherapy, patient-derived 3D tumor explant
Abstract

Immunotherapy with immune checkpoint inhibitors can induce durable clinical responses in different human malignancies but the number of responding patients remains globally modest. The limited therapeutic efficacy of ICI depends on multiple factors, among which the immune suppressive features of the tumor microenvironment play a key role. For this reason, experimental models that enable dissection of the immune-hostile tumor milieu components are required to unravel how to overcome resistance and obtain full-fledged anti-tumor immunity. Recent evidence supports the usefulness of 3D ex vivo systems in retaining features of tumor microenvironment to elucidate molecular and immunologic mechanisms of response and resistance to immune checkpoint blockade. In this perspective article we discuss the recent advances in patient-derived 3D tumor models and their potential in support of treatment decision making in clinical setting. We will also share our experience with dynamic bioreactor tumor explant culture of samples from melanoma and sarcoma patients as a reliable and promising platform to unravel immune responses to immune checkpoint inhibitors.

Published
2022

46. miR-146a-5p impairs melanoma resistance to kinase inhibitors by targeting COX2 and regulating NFkB-mediated inflammatory mediators

Author

Elisabetta Ferrero, Marina Ferrarini, Chiara Gargiuli, Viviana Vallacchi, Michele Del Vecchio, Macarena Gomez Lira, Eriomina Shahaj, Mara Cossa, Elena Tamborini, Barbara Vergani, Luca Lalli, Mario Santinami, Barbara Valeri, Monica Rodolfo, Gianfrancesco Gallino, Simona Frigerio, Veronica Huber, Marialuisa Sensi, Licia Rivoltini, Elisabetta Vergani, Lorenza Di Guardo, Matteo Dugo, Ilaria Mattavelli, Biagio Eugenio Leone, Vergani, E, Dugo, M, Cossa, M, Frigerio, S, Di Guardo, L, Gallino, G, Mattavelli, I, Vergani, B, Lalli, L, Tamborini, E, Valeri, B, Gargiuli, C, Shahaj, E, Ferrarini, M, Ferrero, E, Gomez Lira, M, Huber, V, Vecchio, M, Sensi, M, Leone, B, Santinami, M, Rivoltini, L, Rodolfo, M, and Vallacchi, V

Subjects
Proto-Oncogene Proteins B-raf, BRAF/MEK inhibitors, medicine.medical_treatment, lcsh:Medicine, Drug resistance, Models, Biological, Biochemistry, Targeted therapy, 03 medical and health sciences, 0302 clinical medicine, miR-146a-5p, Cell Line, Tumor, microRNA, medicine, Humans, Epigenetics, BRAF/MEK inhibitor, lcsh:QH573-671, Extracellular Signal-Regulated MAP Kinases, Melanoma, Protein Kinase Inhibitors, Molecular Biology, 030304 developmental biology, Mitogen-Activated Protein Kinase Kinases, 0303 health sciences, Kinase, business.industry, lcsh:Cytology, Research, lcsh:R, NF-kappa B, Cell Biology, medicine.disease, Gene Expression Regulation, Neoplastic, Gene expression profiling, MicroRNAs, Cyclooxygenase 2, Drug Resistance, Neoplasm, Apoptosis, 030220 oncology & carcinogenesis, Cancer research, Inflammation Mediators, Melanoma resistance, business, Proto-Oncogene Proteins c-akt, COX2, Signal Transduction
Abstract

Background Targeted therapy with BRAF and MEK inhibitors has improved the survival of patients with BRAF-mutated metastatic melanoma, but most patients relapse upon the onset of drug resistance induced by mechanisms including genetic and epigenetic events. Among the epigenetic alterations, microRNA perturbation is associated with the development of kinase inhibitor resistance. Here, we identified and studied the role of miR-146a-5p dysregulation in melanoma drug resistance. Methods The miR-146a-5p-regulated NFkB signaling network was identified in drug-resistant cell lines and melanoma tumor samples by expression profiling and knock-in and knock-out studies. A bioinformatic data analysis identified COX2 as a central gene regulated by miR-146a-5p and NFkB. The effects of miR-146a-5p/COX2 manipulation were studied in vitro in cell lines and with 3D cultures of treatment-resistant tumor explants from patients progressing during therapy. Results miR-146a-5p expression was inversely correlated with drug sensitivity and COX2 expression and was reduced in BRAF and MEK inhibitor-resistant melanoma cells and tissues. Forced miR-146a-5p expression reduced COX2 activity and significantly increased drug sensitivity by hampering prosurvival NFkB signaling, leading to reduced proliferation and enhanced apoptosis. Similar effects were obtained by inhibiting COX2 by celecoxib, a clinically approved COX2 inhibitor. Conclusions Deregulation of the miR-146a-5p/COX2 axis occurs in the development of melanoma resistance to targeted drugs in melanoma patients. This finding reveals novel targets for more effective combination treatment. Graphical Abstract

Published
2020

47. Anabolic Hormone Deficiencies in Heart Failure with Reduced or Preserved Ejection Fraction and Correlation with Plasma Total Antioxidant Capacity

Author

Antonio Mancini, Antonio Cittadini, Andrea Silvestrini, Nunzia Ciferri, Carmine Bruno, Edoardo Vergani, Maria Anna Nicolazzi, Roberta D'Assante, Nicola Nicolotti, Angela Maria Rita Fuvuzzi, Elisabetta Meucci, Mancini, A., Fuvuzzi, A. M. R., Bruno, C., Nicolazzi, M. A., Vergani, E., Ciferri, N., Silvestrini, A., Meucci, E., Nicolotti, N., D'Assante, R., and Cittadini, A.

Subjects
medicine.medical_specialty, Anabolism, Article Subject, Endocrinology, Diabetes and Metabolism, Diseases of the endocrine glands. Clinical endocrinology, chemistry.chemical_compound, Endocrinology, Internal medicine, medicine, Settore BIO/10 - BIOCHIMICA, Testosterone, Creatinine, Ejection fraction, Endocrine and Autonomic Systems, Cholesterol, business.industry, Settore MED/13 - ENDOCRINOLOGIA, medicine.disease, anabolic hormone, RC648-665, chemistry, Heart failure, Heart failure with preserved ejection fraction, business, Hormone, Research Article
Abstract

Background. While anabolic hormone deficit is a common finding in heart failure with reduced ejection fraction (HFrEF), few data are available in heart failure with preserved ejection fraction (HFpEF). Methods. Blood samples were collected for metabolic (total cholesterol, HDL cholesterol, LDL cholesterol, creatinine, and glucose) and hormonal (IGF-1, DHEA-S, TSH, fT3, fT4, and T) determination, comparing 30 patients with HFpEF and 20 patients with HFrEF. Total antioxidant capacity was evaluated by using the spectrophotometric method using the latency time in the appearance of the radical species of a chromogen (LAG, sec) as a parameter proportional to antioxidant content of the sample. Echocardiographic parameters were also assessed in the two groups. Results. A high prevalence of testosterone (32% in HFrEF and 72% in HFpEF, p<0.05) and DHEA-S deficiencies was observed in HFpEF patients. Echocardiographic parameters did not correlate with hormone values. A significant direct correlation between T (r2 = 0.25, p<0.05) and DHEA-S (r2 = 0.19, p<0.05) with LAG was observed only in HFpEF. Conclusion. Anabolic hormone deficiency is clearly shown in HFpEF, as already known in HFrEF. Although longitudinal studies are required to confirm the prognostic value of this observation, our data suggest different mechanisms in modulating antioxidants in the two conditions, with possible therapeutic implications.

Published
2020

48. Transcriptional Profiling of Melanoma Sentinel Nodes Identify Patients with Poor Outcome and Reveal an Association of CD30+ T Lymphocytes with Progression

Author

Antonello Domenico Cabras, Paola Deho, Chiara Camisaschi, Monica Rodolfo, Barbara Vergani, Federica Crippa, Niccolò Bassani, Antonino Carbone, Roberto Patuzzo, Silvana Canevari, Paola Frati, Flavio Arienti, Mario Santinami, Loris De Cecco, Licia Rivoltini, Viviana Vallacchi, Elia Biganzoli, Federico Ambrogi, Chiara Castelli, Antonello Villa, Marialuisa Sensi, Elisabetta Vergani, Vallacchi, V, Vergani, E, Camisaschi, C, Deho, P, Cabras, A, Sensi, M, De Cecco, L, Bassani, N, Ambrogi, F, Carbone, A, Crippa, F, Vergani, B, Frati, P, Arienti, F, Patuzzo, R, Villa, A, Biganzoli, E, Canevari, S, Santinami, M, Castelli, C, Rivoltini, L, and Rodolfo, M

Subjects
Cancer Research, Pathology, medicine.medical_specialty, CD30, T-Lymphocytes, Population, Ki-1 Antigen, Antigens, CD30, Immune system, Biopsy, medicine, Humans, education, Melanoma, education.field_of_study, medicine.diagnostic_test, Sentinel Lymph Node Biopsy, business.industry, Computational Biology, FOXP3, Sentinel node, medicine.disease, Immunohistochemistry, Treatment Outcome, T-Lymphocyte, Oncology, Disease Progression, Transcriptome, business, CD8, Human
Abstract

Sentinel lymph nodes set the stance of the immune system to a localized tumor and are often the first site to be colonized by neoplastic cells that metastasize. To investigate how the presence of neoplastic cells in sentinel lymph nodes may trigger pathways associated with metastatic progression, we analyzed the transcriptional profiles of archival sentinel node biopsy specimens obtained from melanoma patients. Biopsies from positive nodes were selected for comparable tumor infiltration, presence or absence of further regional node metastases, and relapse at 5-year follow-up. Unsupervised analysis of gene expression profiles revealed immune response to be a major gene ontogeny represented. Among genes upregulated in patients with progressing disease, the TNF receptor family member CD30/TNFRSF8 was confirmed in biopsy specimens from an independent group of patients. Immunohistochemical analysis revealed higher numbers of CD30+ lymphocytes in nodes from progressing patients compared with nonprogressing patients. Phenotypic profiling demonstrated that CD30+ lymphocytes comprised a broad population of suppressive or exhausted immune cells, such as CD4+Foxp3+ or PD1+ subpopulations and CD4−CD8− T cells. CD30+ T lymphocytes were increased in peripheral blood lymphocytes of melanoma patients at advanced disease stages. Our findings reinforce the concept that sentinel nodes act as pivotal sites for determining progression patterns, revealing that the presence of CD30+ lymphocytes at those sites associate positively with melanoma progression. Cancer Res; 74(1); 130–40. ©2014 AACR.

Published
2014

50. TNF-related apoptosis-inducing ligand (trail)-armed exosomes deliver proapoptotic signals to tumor site

Author

Mario P. Colombo, Alessandro Massimo Gianni, Veronica Huber, Agata Cova, Paola Squarcina, Pamela Della Mina, Elisabetta Vergani, Nadia Zaffaroni, Claudia Chiodoni, Giorgio Mauri, Antonello Villa, Valentina Bollati, Beatrice Bianchi, Maja Bürdek, Ivano Arioli, Licia Rivoltini, Barbara Vergani, Laura Cantone, Monica Tortoreto, Laura Botti, Rivoltini, L, Chiodoni, C, Squarcina, P, Tortoreto, M, Villa, A, Vergani, B, Bürdek, M, Botti, L, Arioli, I, Cova, A, Mauri, G, Vergani, E, Bianchi, B, Della Mina, P, Cantone, L, Bollati, V, Zaffaroni, N, Gianni, A, Colombo, M, and Huber, V

Subjects
0301 basic medicine, Cancer Research, Apoptosis, Mice, SCID, Exosomes, TNF-Related Apoptosis-Inducing Ligand, 03 medical and health sciences, chemistry.chemical_compound, Mice, Necrosis, Cell Line, Tumor, TRAIL, Exosomes, Tumor, Medicine, Animals, Humans, Propidium iodide, Melanoma, business.industry, Caspase 3, Tumor Necrosis Factor-alpha, medicine.disease, Microvesicles, Receptors, TNF-Related Apoptosis-Inducing Ligand, 030104 developmental biology, Oncology, chemistry, Tumor progression, Immunology, Cancer cell, Cancer research, Tumor necrosis factor alpha, Female, Growth inhibition, business, Apoptosis Regulatory Proteins, K562 Cells
Abstract

Purpose: Exosomes deliver signals to target cells and could thus be exploited as an innovative therapeutic tool. We investigated the ability of membrane TRAIL-armed exosomes to deliver proapoptotic signals to cancer cells and mediate growth inhibition in different tumor models. Experimental Methods and Results: K562 cells, transduced with lentiviral human membrane TRAIL, were used for the production of TRAIL+ exosomes, which were studied by nanoparticle tracking analysis, cytofluorimetry, immunoelectronmicroscopy, Western blot, and ELISA. In vitro, TRAIL+ exosomes induced more pronounced apoptosis (detected by Annexin V/propidium iodide and activated caspase-3) in TRAIL-death receptor (DR)5+ cells (SUDHL4 lymphoma and INT12 melanoma), with respect to the DR5−DR4+KMS11 multiple myeloma. Intratumor injection of TRAIL+ exosomes, but not mock exosomes, induced growth inhibition of SUDHL4 (68%) and INT12 (51%), and necrosis in KMS11 tumors. After rapid blood clearance, systemically administered TRAIL+ exosomes accumulated in the liver, lungs, and spleen and homed to the tumor site, leading to a significant reduction of tumor growth (58%) in SUDHL4-bearing mice. The treatment of INT12-bearing animals promoted tumor necrosis and a not statistically significant tumor volume reduction. In KMS11-bearing mice, despite massive perivascular necrosis, no significant tumor growth inhibition was detected. Conclusions: TRAIL-armed exosomes can induce apoptosis in cancer cells and control tumor progression in vivo. Therapeutic efficacy was particularly evident in intratumor setting, while depended on tumor model upon systemic administration. Thanks to their ability to deliver multiple signals, exosomes thus represent a promising therapeutic tool in cancer. Clin Cancer Res; 22(14); 3499–512. ©2016 AACR.

Published
2016

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