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1. Barrier Effect of a New Topical Agent on Damaged Esophageal Mucosa: Experimental Study on an ex vivo Swine Model

Author

Salaroli R, Ventrella D, Bernardini C, Elmi A, Zannoni A, Bacci ML, Forni M, Calanni F, Ferrieri A, and Baldi F

Subjects
bioadhesion, evans blue dye (ebd), animal model, esophagus, gastroesophageal reflux disease (gerd), Diseases of the digestive system. Gastroenterology, RC799-869
Abstract

Roberta Salaroli,1 Domenico Ventrella,1 Chiara Bernardini,1 Alberto Elmi,1 Augusta Zannoni,1,2 Maria Laura Bacci,1,2 Monica Forni,1,2 Fiorella Calanni,3 Antonella Ferrieri,4 Fabio Baldi5 1Department of Veterinary Medical Science, University of Bologna, Ozzano Emilia, Bologna, Italy; 2Health Sciences and Technologies Interdepartmental Center for Industrial Research, University of Bologna, Bologna, Italy; 3Pre-Clinical Research Department, Alfasigma, Bologna, Italy; 4Division of Clinical Research, Department of Research and Development, Alfasigma, Bologna, Italy; 5Center for the Study of Diseases of the Esophagus, University of Bologna and Gruppo Villa Maria Care & Research, Ravenna, ItalyCorrespondence: Monica ForniDepartment of Veterinary Medical Science, University of Bologna, Via Tolara, 50, Ozzano Emilia 40064, Bologna, ItalyTel +39 051 20 9 7913Email monica.forni@unibo.itPurpose: AL2106 is a new medical device based on a mixture of chondroitin sulphate in a xyloglucan and glycerol solution made to maximize its bioadhesive capability to the esophageal mucosa. The aim of the present study was twofold to evaluate the AL2106 protective effect on the esophageal mucosa when exposed to an acidic solution mimicking gastric reflux and to assess the resilience of this effect to saline washing.Materials and Methods: A porcine ex vivo model was used and the effects of the new medical device were compared to a sodium alginate suspension (SAS) already present on the market which was assumed as reference. Mucosal damage was induced in 19 porcine esophagi by perfusion with an acidic solution added with pepsin, and Evans blue dye (EBD) tissue uptake was used as an indicator of mucosal permeability. The EBD penetration, expressed as EBD μg/g of dry tissue, was assessed in specimens of untreated damaged mucosa and in specimens treated with AL2106 or SAS. The same evaluation was carried out after washing with normal saline.Results: Both topical agents tested significantly reduced the EBD uptake by more than 60% (AL2106 8.4± 4.5, SAS 3.6± 2.7 vs control 23.2± 13.1, p< 0.01). The saline washing did not cause any significant reduction in the protective effect of AL2106 (8.6± 5.9), while it significantly reduced that of SAS (5.9± 4.3, p< 0.05).Conclusion: The new AL2106 medical device showed a good barrier effect against a reflux-like damaging solution and preserved this effect after the mucosal washing test, thus suggesting its possible relevance for the treatment of gastroesophageal reflux disease.Keywords: bioadhesion, Evans blue dye, EBD, animal model, esophagus, gastroesophageal reflux disease, GERD

Published
2020

2. Cost-effectiveness analysis of antiretroviral therapy in a cohort of HIV-infected patients starting first-line highly active antiretroviral therapy during 6 years of observation

Author

Maggiolo F, Colombo GL, Di Matteo S, Bruno GM, Astuti N, Di Filippo E, Masini G, and Bernardini C

Subjects
Medicine (General), R5-920
Abstract

Franco Maggiolo,1 Giorgio L Colombo,2,3 Sergio Di Matteo,3 Giacomo M Bruno,3 Noemi Astuti,1 Elisa Di Filippo,1 Giulia Masini,1 Claudia Bernardini1 1Division of Infectious Diseases, Azienda Ospedaliera Papa Giovanni XXIII, Bergamo, Italy; 2University of Pavia, Department of Drug Sciences, Pavia, Italy; 3SAVE Studi Analisi Valutazioni Economiche, Milan, Italy Objectives: Costs may play a role in deciding how and when to start highly active antiretroviral therapy (HAART) in a naïve patient. The aim of the present study was to assess the cost- effectiveness of treatment with HAART in a large clinical cohort of naïve adults to determine the potential role of single-tablet regimens in the management of patients with human immunodeficiency virus (HIV). An incremental cost-effectiveness ratio analysis was performed, including a quality-adjusted life year approach. Results: In total, 741 patients (females comprising 25.5%) were retrospectively included. The mean age was 39 years, the mean CD4 cell count was 266 cells/µL, and the mean viral load was 192,821 copies/mL. The most commonly used backbone was tenofovir + emtricitabine (77.6%); zidovudine + lamivudine was used in 10%, lamivudine + abacavir in 3%, and other nucleoside reverse transcriptase inhibitor (NRTI) or NRTI-free regimens in 9.4% of patients. NNRTIs were used in 52.8% of cases, boosted protease inhibitors in 44.1%, and unboosted protease inhibitors and integrase inhibitors in 0.7% and 2.4%, respectively. Starting therapy at CD4 >500 cells/µL and CD4 351–500 cells/µL rather than at 500 cells per µL); in this case, the incremental cost-effectiveness ratio value was €199,130 per quality-adjusted life year gained, a higher value than the one suggested in guidelines. The single-tablet regimen (STR) invariably dominated any other therapeutic approach. Sensitivity analysis was performed, and starting right away with an STR was cost-effective even when compared with therapeutic strategies contemplating STR as simplification. Conclusion: By integrating clinical data with economic variables, our study offers an estimate of the cost-effectiveness of the various first-line treatment strategies for patients infected with HIV and provides significant evidence to be used in future prospective pharmacoeconomic evaluations. Keywords: cost-effectiveness, quality-adjusted life years, highly active antiretroviral therapy, single-tablet regimen

Published
2015

3. Triple-combination rilpivirine, emtricitabine, and tenofovir (Complera™/Eviplera™) in the treatment of HIV infection

Author

Bernardini C and Maggiolo F

Subjects
Medicine (General), R5-920
Abstract

Claudia Bernardini, Franco MaggioloDivision of Infectious Diseases and Unit of Antiviral Therapy, AO Papa Giovanni XXIII, Bergamo, ItalyAbstract: The combination rilpivirine (RPV)/emtricitabine (FTC)/tenofovir (TDF) is a once-daily, single-tablet regimen (STR) containing one nonnucleoside reverse-transcriptase inhibitor associated with two nucleos(t)ide reverse transcriptase inhibitors. It is approved by regulatory agencies (eg, US Food and Drug Association, European Medicines Agency) in all countries in which it is manufactured, except Switzerland, as first-line highly active antiretroviral therapy (HAART) for the treatment of naïve patients with HIV infection and a viral load HIV-RNA level of ≤100,000 copies/mL. Two large trials (ECHO and THRIVE) comparing RPV with efavirenz, along with different background regimens, led to approval of the drug, while a more recent trial (STaR) explored the use of STR. RPV showed noninferiority to efavirenz in all the studies, including superiority as an STR in patients with HIV-RNA ≤100,000 copies/mL in the STaR study. A positive CD4 cell response was observed in all the studies, both in the RPV and efavirenz groups. The incidence of virologic failures was higher for RPV, but was mostly referred to patients with HIV-RNA >100,000 copies/mL. There were fewer adverse events (AEs) with the RPV-based regimens versus efavirenz-based regimens, with a lower discontinuation rate because of AEs, especially psychiatric–neurological AEs, and a significantly lower rate of blood-lipid abnormalities. In the SPIRIT study (a switch study), significantly greater improvements from baseline in serum total cholesterol, low-density lipoprotein cholesterol, and trygliceride were demonstrated in patients switching to RPV/FTC/TDF from a ritonavir-boosted protease inhibitor (PI/r)-based regimen, than in those who continued treatment with a PI/r regimen. RPV's better tolerability, associated with its once-daily STR formulation, is key to improving patients' adherence and quality of life, which are among the most important factors affecting the therapeutic efficacy of an antiretroviral regimen. In summary, RPV/FTC/TDF STR is a valuable treatment option for the majority of antiretroviral-naïve HIV-infected patients. Furthermore, the use of this STR in the therapeutic switch, like in the SPIRIT study, can result in another valuable option by which to reduce AEs and improve patients' quality of life.Keywords: rilpivirine or RPV, HIV, treatment-naïve, once-daily, single-tablet regimen

Published
2013

4. Efficacy and safety of darunavir and etravirine in an antiretroviral multi-experienced youth with vertically HIV-1 infection

Author

Rosso R, Bernardini C, Bruzzone B, Secondo G, Icardi G, Viscoli C, and Di Biagio A

Subjects
vertically acquired HIV-1 infection, multidrug resistance, adherence, darunavir, etravirine, Medicine
Abstract

Abstract Multiclass-drug resistance, often caused by poor treatment compliance, is a challenging problem in all categories of HIV-infected patients. Selective pressure is higher in youth for both biological and behavioral reasons. We report the case of a 15-year-old Caucasian male, with vertically acquired HIV-1 infection, who failed several lines of antiretroviral therapy and was successfully treated with darunavir/ritonavir and etravirine.

Published
2009
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5. Soft-approach to climate change adaptation. The active role of urban services

Author

Bernardini, C.

Subjects
Climate Change Adaptation, Health (social science), Cross-scale interactions, Architecture, Soft-resilience, Building and Construction, Adaptation services, Climate Change Adaptation, Soft-resilience, Urban services, Adaptation services, Cross-scale interactions, Urban services, Education
Abstract

Learning from the present polycrisis exacerbated by the global pandemic and applying these lessons to the issue of climate change could bring long-term benefits. This contribution offers a novel point of view on the active role of urban services (re-defined as adaptation services) in supporting human systems’ adaptation to climate change. Furthermore, it discusses the implications of cross-level and cross-scale interactions in the management of adaptation services’ systems. The convergence of information collected from different sources (data triangulation) by means of literature review, in-deep analysis of policy documents and a continuous dialogue with key stakeholders shall ensure the consistency of the point of view proposed.

Published
2022

7. The sieve-element endoplasmic reticulum: A focal point of phytoplasma-host plant interaction?

Author

Musetti, R., Pagliari, L., Mian, G., De Oliveira Cantao, F. R., Bernardini, C., Santi, S., and van Bel, A. J. E.

Subjects
phytoplasma-host interaction, Microbiology (medical), endoplasmic reticulum, pore-plasmodesma units, Arabidopsis, phytoplasma, sieve element, sieve-element ER docking sites, unfolded protein response, Arabidopsis, endoplasmic reticulum, phytoplasma, phytoplasma-host interaction, sieve element, pore-plasmodesma units, sieve-element ER docking sites, unfolded protein response, Microbiology
Abstract

The rough endoplasmic reticulum (r-ER) is of paramount importance for adaptive responses to biotic stresses due to an increased demand for de novo synthesis of immunity-related proteins and signaling components. In nucleate cells, disturbance of r-ER integrity and functionality leads to the “unfolded protein response” (UPR), which is an important component of innate plant immune signalling. In contrast to an abundance of reports on r-ER responses to biotic challenges, sieve-element endoplasmic reticulum (SE-ER) responses to phytoplasma infection have not been investigated. We found that morphological SE-ER changes, associated with phytoplasma infection, are accompanied by differential expression of genes encoding proteins involved in shaping and anchoring the reticulum. Phytoplasma infection also triggers an increased release of bZIP signals from the (SE-ER)/r-ER and consequent differential expression of UPR-related genes. The modified expression patterns seem to reflect a trade-off between survival of host cells, needed for the phytoplasmic biotrophic lifestyle, and phytoplasmas. Specialized plasmodesmata between sieve element and companion cell may provide a corridor for transfer of phytoplasma effectors inducing UPR-related gene expression in companion cells.

Published
2023
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9. Localization of the Serotonin Transporter in the Dog Intestine and Comparison to the Rat and Human Intestines

Author

Chiocchetti R., Galiazzo G., Giancola F., Tagliavia C., Bernardini C., Forni M., Pietra M., Chiocchetti R., Galiazzo G., Giancola F., Tagliavia C., Bernardini C., Forni M., and Pietra M.

Subjects
enteric nervous system, General Veterinary, myenteric plexu, SERT, Veterinary medicine, SF600-1100, 5-HT, Veterinary Science, submucosal plexus, Original Research, myenteric plexus
Abstract

Serotonin is crucial in gastrointestinal functions, including motility, sensitivity, secretion, and the inflammatory response. The serotonin transporter (SERT), responsible for serotonin reuptake and signaling termination, plays a prominent role in gastrointestinal physiology, representing a promising therapeutic target in digestive disorders. Serotonin transporter expression has been poorly investigated in veterinary medicine, under both healthy and pathological conditions, including canine chronic enteropathy, in which the serotonin metabolism seems to be altered. The aim of the present study was to determine the distribution of SERT immunoreactivity (SERT-IR) in the dog intestine and to compare the findings with those obtained in the rat and human intestines. Serotonin transporter-IR was observed in canine enterocytes, enteric neurons, lamina propria cells and the tunica muscularis. Data obtained in dogs were consistent with those obtained in rats and humans. Since the majority of the serotonin produced by the body is synthesized in the gastrointestinal tract, SERT-expressing cells may exert a role in the mechanism of serotonin reuptake.

Published
2022

14. Increased susceptibility to Chrysanthemum Yellows phytoplasma infection in Atcals7 ko plants is accompanied by enhanced expression of carbohydrate transporters

Author

Simonetta Santi, Myrtho Pierre, Stacy Welker, Van Bel A, Joon Hyuk Suh, Bernardini C, Wang Y, Rita Musetti, Sara Buoso, Christopher Vincent, Amit Levy, Marta Martini, Alberto Loschi, and Bosetto F

Subjects
chemistry.chemical_compound, Photoassimilate, chemistry, biology, Phytoplasma, Arabidopsis, Callose, Gene expression, Mutant, Plasmodesma, Carbohydrate metabolism, biology.organism_classification, Microbiology
Abstract

Callose deposition around sieve pores, under control of callose synthase 7 (AtCALS7), has been interpreted as a mechanical response to limit pathogen spread in phytoplasma-infected plants. Wild-type and Atcals7ko mutants were therefore employed to unveil the mode of involvement of CALS7 in the plant’s response to phytoplasma infection. The fresh weights of healthy and CY-(Chrysanthemum Yellows) phytoplasma-infected Arabidopsis wild-type and mutant plants indicated two superimposed effects of the absence of CALS7: a partial impairment of photo-assimilate transport and a stimulated phytoplasma proliferation as illustrated by a significantly increased phytoplasma titre in Atcal7ko mutants. Further studies solely dealt with the effects of CALS7 absence on phytoplasma growth. Phytoplasma infection affected sieve-element substructure to a larger extent in mutants than in wild-type plants, which was also true for the levels of some free carbohydrates. Moreover, infection induced a similar upregulation of gene expression of enzymes involved in sucrose cleavage (AtSUS5, AtSUS6) and transmembrane transport (AtSWEET11) in mutants and wild-type plants, but an increased gene expression of carbohydrate transmembrane transporters (AtSWEET12, AtSTP13, AtSUC3) in infected mutants only. It remains still unclear how the absence of AtCALS7 leads to gene upregulation and how an increased intercellular mobility of carbohydrates and possibly effectors contributes to a higher susceptibility. It is also unclear if modified sieve-pore structures in mutants allow a better spread of phytoplasmas giving rise to higher titre.Author SummaryPhytoplasma infections are one of the most limiting factors for production of important crops all over the world. Phytoplasma disease epidemics can be handled mainly by insect-vector control using insecticides. Basic information about plant-phytoplasma interactions are still limited, nevertheless it is necessary to design new management and breeding strategies aimed to obtain more tolerant or resistant cultivars. Phytoplasmas are obligate intracellular parasites restricted to the phloem sieve tubes. Callose deposition at the sieve plates has been described since the ‘70s as a mechanical defence process to limit pathogen spread by occluding sieve pores. Studies reported 40 years later demonstrated that callose at the sieve pores is also involved in sieve-pore development and function and, hence, in mass-flow regulation, carbohydrate metabolism and distribution, and plant growth. Here, we reported on the role(s) of sieve-element callose in phytoplasma-infected Arabidopsis, using a mutant lacking AtCALS7, the enzyme responsible for callose synthesis in the sieve elements. The results indicate that loss of AtCAL7 appears to confer increased susceptibility to phytoplasma infection, due to alterations in expression of genes involved in sugar metabolism and membrane transport. In the long run, the identification of plant resistance or susceptibility traits against phytoplasmas will allow a complete re-organization of chemical control strategies, with obvious opportunities of reducing insecticide burden.

Published
2021

17. A comprehensive review on non-clinical methods to study transfer of medication into breast milk – A contribution from the ConcePTION project

Author

Nauwelaerts, N. (Nina), Deferm, N. (Neel), Smits, A., Bernardini, C. (Chiara), Lammens, B. (Bart), Gandia, P. (Peggy), Panchaud, A. (Alice), Nordeng, H. (Hedvig), Bacci, M.L. (Maria Laura), Forni, M. (Monica), Ventrella, D. (Domenico), Calsteren, K. (Kristel) van, DeLise, A. (Anthony), Huys, I. (Isabelle), Bouisset-Leonard, M. (Michele), Allegaert, K.M. (Karel), Annaert, P. (Pieter), Nauwelaerts, N. (Nina), Deferm, N. (Neel), Smits, A., Bernardini, C. (Chiara), Lammens, B. (Bart), Gandia, P. (Peggy), Panchaud, A. (Alice), Nordeng, H. (Hedvig), Bacci, M.L. (Maria Laura), Forni, M. (Monica), Ventrella, D. (Domenico), Calsteren, K. (Kristel) van, DeLise, A. (Anthony), Huys, I. (Isabelle), Bouisset-Leonard, M. (Michele), Allegaert, K.M. (Karel), and Annaert, P. (Pieter)

Abstract

Breastfeeding plays a major role in the health and wellbeing of mother and infant. However, information on the safety of maternal medication during breastfeeding is lacking for most medications. This leads to discontinuation of either breastfeeding or maternal therapy, although many medications are likely to be safe. Since human lactation studies are costly and challenging, validated non-clinical methods would offer an attractive alternative. This review gives an extensive overview of the non-clinical methods (in vitro, in vivo and in silico) to study the transfer of maternal medication into the human breast milk, and subsequent neonatal systemic exposure. Several in vitro models are available, but model characterization, including quantitative medication transport data across the in vitro blood-milk barrier, remains rather limited. Furthermore, animal in vivo models have been used successfully in the past. However, these models don't always mimic human physiology due to species-specific differences. Several efforts have been made to predict medication transfer into the milk based on physicochemical characteristics. However, the role of transporter proteins and several physiological factors (e.g., variable milk lipid content) are not accounted for by these methods. Physiologically-based pharmacokinetic (PBPK) modelling offers a mechanism-oriented strategy with bio-relevance. Recently, lactation PBPK models have been reported for some medications, showing at least the feasibility and value of PBPK

Published
2021
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18. Postfazione

Author

Bernardini, C, Dell’Avanzato, S, Fantacchiotti, T, Nofri F, Bertoni, Anna Marta Maria, Bertoni, A (ORCID:0000-0001-7228-8718), Bernardini, C, Dell’Avanzato, S, Fantacchiotti, T, Nofri F, Bertoni, Anna Marta Maria, and Bertoni, A (ORCID:0000-0001-7228-8718)

Abstract

Chi si occupa di ricerca, e soprattutto di ricerca-azione, sa che la ricerca scientifica si propone di “dare misura” e “dare valore” a un cambiamento che viene scientificamente valutato, che viene evidenziato come non casuale, ma specificamente legato a un intervento che, nel caso di Rondine, è un intervento formativo. Ci sono cambiamenti visibili (chi confronta il volto dei propri figli con quello nelle foto “da piccoli” sa cosa vuol dire), ma ci sono anche cambiamenti non immediatamente visibili. La ricerca si accorge prima di questi ultimi cambiamenti. E li racconta. Questo fanno le autrici di questo volume: evidenziano cambiamenti e cercano di rintracciarne la ratio, per comprendere se i cambiamenti mostrati dai giovani possano essere ricondotti al lavoro trasformativo portato avanti a Rondine. I risultati della ricerca ci dicono che molti mutamenti significativi sono legati ai contenuti trattati durante l’anno a Rondine. Possiamo davvero trovare nel nuovo sguardo che i giovani del QAR assumono a fine percorso una chiara sporgenza generativa del Metodo Rondine.

Published
2021

19. A comprehensive review on non-clinical methods to study transfer of medication into breast milk - A contribution from the ConcePTION project

Author

Nauwelaerts, N, Deferm, N, Smits, A, Bernardini, C, Lammens, B, Gandia, P, Panchaud, A, Nordeng, H, Bacci, ML, Forni, M, Ventrella, D, Van Calsteren, K, DeLise, A, Huys, I, Bouisset-Leonard, M, Allegaert, Karel, Annaert, P, Nauwelaerts, N, Deferm, N, Smits, A, Bernardini, C, Lammens, B, Gandia, P, Panchaud, A, Nordeng, H, Bacci, ML, Forni, M, Ventrella, D, Van Calsteren, K, DeLise, A, Huys, I, Bouisset-Leonard, M, Allegaert, Karel, and Annaert, P

Abstract

Breastfeeding plays a major role in the health and wellbeing of mother and infant. However, information on the safety of maternal medication during breastfeeding is lacking for most medications. This leads to discontinuation of either breastfeeding or maternal therapy, although many medications are likely to be safe. Since human lactation studies are costly and challenging, validated non-clinical methods would offer an attractive alternative. This review gives an extensive overview of the non-clinical methods (in vitro, in vivo and in silico) to study the transfer of maternal medication into the human breast milk, and subsequent neonatal systemic exposure. Several in vitro models are available, but model characterization, including quantitative medication transport data across the in vitro blood-milk barrier, remains rather limited. Furthermore, animal in vivo models have been used successfully in the past. However, these models don't always mimic human physiology due to species-specific differences. Several efforts have been made to predict medication transfer into the milk based on physicochemical characteristics. However, the role of transporter proteins and several physiological factors (e.g., variable milk lipid content) are not accounted for by these methods. Physiologically-based pharmacokinetic (PBPK) modelling offers a mechanism-oriented strategy with bio-relevance. Recently, lactation PBPK models have been reported for some medications, showing at least the feasibility and value of PBPK modelling to predict transfer of medication into the human milk. However, reliable data as input for PBPK models is often missing. The iterative development of in vitro, animal in vivo and PBPK modelling methods seems to be a promising approach. Human in vitro models will deliver essential data on the transepithelial transport of medication, whereas the combination of animal in vitro and in vivo methods will deliver information to establish accurate in vitro/in vivo extr

Published
2021

22. Corrigendum: Cellular Distribution of Canonical and Putative Cannabinoid Receptors in Canine Cervical Dorsal Root Ganglia (Frontiers in Veterinary Science, (2019), 6, (313), 10.3389/fvets.2019.00313)

Author

Chiocchetti R., Galiazzo G., Tagliavia C., Stanzani A., Giancola F., Menchetti M., Militerno G., Bernardini C., Forni M., Mandrioli L., Chiocchetti R., Galiazzo G., Tagliavia C., Stanzani A., Giancola F., Menchetti M., Militerno G., Bernardini C., Forni M., and Mandrioli L.

Subjects
cannabinoid receptor 2, cannabinoid receptor 1, nuclear peroxisome proliferator-activated receptor alpha, nervous system, transient receptor potential vanilloid type 1, endocannabinoid, satellite glial cell, G protein-coupled receptor 55
Abstract

In the original article, there was a mistake in the legend for Figure 3 as published. The legend of Figure 3 (g-l) is incorrect. The correct legend appears below. FIGURE 3 | Photomicrographs of cryosections of canine cervical (C8) dorsal root ganglion showing cannabinoid receptor 2- (CB2), glial fibrillary acidic protein- (GFAP), and CD31-immunoreactivity. (a–c) Stars indicate NeuroTrace labeled (a) dorsal root ganglion sensory neurons which were CB2 receptor negative (b), as well as the satellite glial cells (white arrows). (d–f) Stars indicate sensory neurons encircled by satellite glial cells (white arrows) which were GFAP-immunoreactive (e) and CB2 receptor negative. CB2 receptor immunoreactivity was expressed by Schwann cells and neuronal nuclei (open arrow). (g–i) The empty arrow indicates one neuronal axon that bifurcates (T-junction) in its central and peripheral portions (large white arrows). The small arrows indicate the nuclei of Schwann cells. (j–l) Open arrows indicate smooth muscle cells (vessel on the left) and pericyte-like cells (elongated and thin blood vessel on the right) showing CB2 receptor immunoreactivity (j).White arrows indicate endothelial cells showing CD31 immunoreactivity (k). Bar: a–f, j–l = 50μm; g–i = 100 μm. The authors apologize for this error and state that this does not change the scientific conclusions of the article in any way. The original article has been updated.

Published
2019

34. Echi della tradizione boitiana nella scuola italiana di architettura e design: ricordo di Luca Scacchetti

Author

Baila, A., Barbera, P., Basevi, B., Bernardini, C., Bordogna, E., Borella, M. A., Caramel, C., Chizzoniti, D., Colle, E., Contessi, Gianni, Crippa, M. A., Cusatelli, S., Dameri, A., Dellapiana, E., Dezzi Bardeschi, M., Fiore, I., Franchini, L., Giovannini, R., Grassi, L., Guarisco, M., Manoli, F., Massari, E., Monica, L., Nicoletti, B., Patetta, L., Pesando, A. B., Prescia, R., Rossi, M., Ruscio, R., Scarocchia, S., Serino, Roberto, Torricelli, A., Vettorata, G., and Zanzottera, F.

Published
2018

36. Skeletal Muscle MicroRNAs as Key Players in the Pathogenesis of Amyotrophic Lateral Sclerosis

Author

Di Pietro, Lorena, Lattanzi, Wanda, Bernardini, Camilla, Di Pietro, L (ORCID:0000-0001-5723-2169), Lattanzi, W (ORCID:0000-0003-3092-4936), Bernardini, C (ORCID:0000-0002-8869-6334), Di Pietro, Lorena, Lattanzi, Wanda, Bernardini, Camilla, Di Pietro, L (ORCID:0000-0001-5723-2169), Lattanzi, W (ORCID:0000-0003-3092-4936), and Bernardini, C (ORCID:0000-0002-8869-6334)

Abstract

Amyotrophic lateral sclerosis (ALS) is a fatal neurodegenerative disorder, for which, to date, no effective treatment to ameliorate the clinical manifestations is available. The long-standing view of ALS as affecting only motor neurons has been challenged by the finding that the skeletal muscle plays an active role in the disease pathogenesis and can be a valuable target for therapeutic strategies. In recent years, non-coding RNAs, including microRNAs, have emerged as important molecules that play key roles in several cellular mechanisms involved in the pathogenic mechanisms underlying various human conditions. In this review, we summarize how the expression of some microRNAs is dysregulated in the skeletal muscle of ALS mouse models and patients. Shedding light on the mechanisms underlying microRNAs dysregulation in the skeletal muscle could clarify some of the processes involved in the pathogenesis of ALS and especially identify new promising therapeutic targets in patients.

Published
2018

37. Effects of Class II-Selective Histone Deacetylase Inhibitor on Neuromuscular Function and Disease Progression in SOD1-ALS Mice

Author

Buonvicino, D, Felici, R, Ranieri, G, Caramelli, R, Lapucci, A, Cavone, L, Muzzi, M, Di Pietro, L, Bernardini, Camilla, Zwergel, C, Valente, S, Mai, A, Chiarugi, A, Bernardini, C (ORCID:0000-0002-8869-6334), Buonvicino, D, Felici, R, Ranieri, G, Caramelli, R, Lapucci, A, Cavone, L, Muzzi, M, Di Pietro, L, Bernardini, Camilla, Zwergel, C, Valente, S, Mai, A, Chiarugi, A, and Bernardini, C (ORCID:0000-0002-8869-6334)

Abstract

Emerging evidence indicates that transcriptome alterations due to epigenetic deregulation concur to ALS pathogenesis. Accordingly, pan-histone deacetylase (HDAC) inhibitors delay ALS development in mice, but these compounds failed when tested in ALS patients. Possibly, lack of selectivity toward specific classes of HDACs weakens the therapeutic effects of pan-HDAC inhibitors. Here, we tested the effects of the HDAC Class II selective inhibitor MC1568 on disease evolution, motor neuron survival as well as skeletal muscle function in SOD1G93A mice. We report that HDACs did not undergo expression changes during disease evolution in isolated motor neurons of adult mice. Conversely, increase in specific Class II HDACs (-4, -5 and -6) occurs in skeletal muscle of mice with severe neuromuscular impairment. Importantly, treatment with MC1568 causes early improvement of motor performances that vanishes at later stages of disease. Notably, motor improvement is not paralleled by reduced motor neuron degeneration but by increased skeletal muscle electrical potentials, reduced activation of mir206/FGFBP1-dependent muscle reinnervation signaling, and increased muscle expression of myogenic genes. (C) 2018 IBRO. Published by Elsevier Ltd. All rights reserved.

Published
2018

38. L'USPID

Author

Bernardini C., Colombetti G., Latella D., and Lenci F.

Subjects
Scienza e Disarmo, Scienza e Societa', Impegno Etico e Sociale degli Scienziati
Abstract

An introduction to the Historyof the Unione degli Scienziati Per Il Disarmo ONLUS is given. The major Achievements are presented and current Activities briefly discussed.

Published
2017

40. A method for uptake quantification of multiple fluorescent DNAs in boar semen as an alternative to radiolabeling

Author

De Cecco M, Zannoni A, Bernardini C, Lavitrano M, Maria Laura Bacci, Forni M, De Cecco M., Zannoni A., Bernardini C., Lavitrano M., Bacci M.L., Forni M., De Cecco, M, Zannoni, A, Bernardini, C, Lavitrano, M, Bacci, M, and Forni, M

Subjects
Male, Radioisotopes, Reverse Transcriptase Polymerase Chain Reaction, MED/04 - PATOLOGIA GENERALE, GENE TRANSFER TECHNIQUES, Uptake, DNA, Communications, DNA UPTAKE, Microscopy, Fluorescence, Semen, Isotope Labeling, Animals, Microscopy, Phase-Contrast, FLUORESCENCE, SPERMATOZOA, SWINE, Gene transfer technique, Fluorescent Dyes, Plasmids
Abstract

Sperm-mediated gene transfer (SMGT) is a simple and efficient method for producing multitransgenic organisms. Until now, the exogenous DNA uptake efficiencies have been quantified, performing coincubation of spermatozoa with (3)H-DNA. This method has significant limitations; from a researcher's point of view, radioactivity-based experiments are hazardous and require specialistic skills, and in technical analysis, the signal does not allow the simultaneous discrimination of two or more types of labeled constructs. Considering these remarkable points, the present work aims to develop a method for differential uptake quantification of various transgenes alternative to the use radioactive material. The main approach relies on fluorescent-specific peaks for each construct, and their diminution during the sperm--DNA-coincubation phase. The obtained results were confirmed by real-time PCR analysis and fluorescence microscopy imaging. This method becomes of primary importance when the SMGT technique has to be applied on various constructs, as it allows preliminary conclusions to be drawn about multiple transgenesis events and to approach further research about eventual sperm membrane preferences in sequences or structures for constructs.

Published
2010

41. Caching Strategies for Information Centric Networking: Opportunities and Challenges

Author

Bernardini, C��sar, Silverston, Thomas, and Vasilakos, Athanasios

Subjects
Networking and Internet Architecture (cs.NI), FOS: Computer and information sciences, Computer Science - Networking and Internet Architecture, Hardware_MEMORYSTRUCTURES
Abstract

Internet usage has shifted from host-centric end-to-end communication to a content-centric approach mainly used for content delivery. Information Centric Networking (ICN) was proposed as a promising novel content delivery architecture. ICN includes in-network caching features at every node which has a major impact on content retrieval. For instance, the ICN efficiency depends drastically on the management of the caching resources. The management of caching resources is achieved with caching strategies. Caching strategies decide what, where and when content is stored in the network. In this paper, we revisit the recent technical contributions on caching strategies, we compare them and discuss opportunities and challenges for improving content delivery in the upcoming years.

Published
2016

42. Radon contribution to single particle counts of the ARGO-YBJ detector

Author

B. Bartoli a, b, P. Bernardini c, d, X. J. Bi e, I. Bolognino n, o, P. Branchini f, A. Budano f, P. Camarri g, h, Z. Cao e, R. Cardarelli h, S. Catalanotti a, C. Cattaneo o, S. Z. Chen e, T. L. Chen i, P. Creti d, S. W. Cui j, B. Z. Dai k, A. D'Amone c, Danzengluobu i, I. De Mitri c, B. D'Ettorre Piazzoli a, T. Di Girolamo a, G. Di Sciascio h, C. F. Feng l, Zhaoyang Feng e, Zhenyong Feng m, E. Giroletti n, Q. B. Gou e, Y. Q. Guo e, H. H. He e, Haibing Hu i, Hongbo Hu e, M. Iacovacci a, R. Iuppa g, H. Y. Jia m, Labaciren i, H. J. Li i, G. Liguori n, C. Liu e, J. Liu k, M. Y. Liu i, H. Lu e, L. L. Ma e, X. H. Ma e, G. Mancarella c, f, p, G. Marsella c, D. Martello c, S. Mastroianni b, P. Montini f, p, C. C. Ning i, M. Panareo c, L. Perrone c, P. Pistilli f, F. Ruggieri f, P. Salvini o, R. Santonico g, P. R. Shen e, X. D. Sheng e, F. Shi e, A. Surdo d, Y. H. Tan e, P. Vallania q, r, S. Vernetto q, C. Vigorito r, s, H. Wang e, C. Y. Wu e, H. R. Wu e, L. Xue l, Q. Y. Yang k, X. C. Yang k, Z. G. Yao e, A. F. Yuan i, M. Zha e, H. M. Zhang e, L. Zhang k, X. Y. Zhang l, Y. Zhang e, J. Zhao e, Zhaxiciren i, Zhaxisangzhu i, X. X. Zhou m, F. R. Zhu m, Q. Q. Zhu e, G. Zizzi t, The ARGO YBJ Collaboration, MARI, Stefano Maria, B., Bartoli a, B, P., Bernardini c, D, X. J., Bi e, I., Bolognino n, O, P., Branchini f, A., Budano f, P., Camarri g, H, Z., Cao e, R., Cardarelli h, S., Catalanotti a, C., Cattaneo o, S. Z., Chen e, T. L., Chen i, P., Creti d, S. W., Cui j, B. Z., Dai k, A., D'Amone c, Danzengluobu, I, I., De Mitri c, B., D'Ettorre Piazzoli a, T., Di Girolamo a, G., Di Sciascio h, C. F., Feng l, Zhaoyang Feng, E, Zhenyong Feng, M, E., Giroletti n, Q. B., Gou e, Y. Q., Guo e, H. H., He e, Haibing Hu, I, Hongbo Hu, E, M., Iacovacci a, R., Iuppa g, H. Y., Jia m, Labaciren, I, H. J., Li i, G., Liguori n, C., Liu e, J., Liu k, M. Y., Liu i, H., Lu e, L. L., Ma e, X. H., Ma e, G., Mancarella c, Mari, Stefano Maria, F, P, G., Marsella c, D., Martello c, S., Mastroianni b, P., Montini f, P, C. C., Ning i, M., Panareo c, L., Perrone c, P., Pistilli f, F., Ruggieri f, P., Salvini o, R., Santonico g, P. R., Shen e, X. D., Sheng e, F., Shi e, A., Surdo d, Y. H., Tan e, P., Vallania q, R, S., Vernetto q, C., Vigorito r, S, H., Wang e, C. Y., Wu e, H. R., Wu e, L., Xue l, Q. Y., Yang k, X. C., Yang k, Z. G., Yao e, A. F., Yuan i, M., Zha e, H. M., Zhang e, L., Zhang k, X. Y., Zhang l, Y., Zhang e, J., Zhao e, Zhaxiciren, I, Zhaxisangzhu, I, X. X., Zhou m, F. R., Zhu m, Q. Q., Zhu e, G., Zizzi t, The ARGO YBJ, Collaboration, B., Bartoli, Bernardini, Paolo, X. J., Bi, I., Bolognino, P., Branchini, A., Budano, P., Camarri, Z., Cao, R., Cardarelli, S., Catalanotti, C., Cattaneo, S. Z., Chen, T. L., Chen, P., Creti, S. W., Cui, B. Z., Dai, D'Amone, Antonio, Danzengluobu, DE MITRI, Ivan, B., D'Ettorre Piazzoli, T., Di Girolamo, G., Di Sciascio, C. F., Feng, Zhaoyang, Feng, Zhenyong, Feng, E., Giroletti, Q. B., Gou, Y. Q., Guo, H. H., He, Haibing, Hu, Hongbo, Hu, M., Iacovacci, R., Iuppa, H. Y., Jia, Labaciren, H. J., Li, G., Liguori, C., Liu, J., Liu, M. Y., Liu, H., Lu, L. L., Ma, X. H., Ma, Mancarella, Giovanni, S. M., Mari, Marsella, Giovanni, Martello, Daniele, S., Mastroianni, P., Montini, C. C., Ning, Panareo, Marco, Perrone, Lorenzo, P., Pistilli, F., Ruggieri, P., Salvini, R., Santonico, P. R., Shen, X. D., Sheng, F., Shi, A., Surdo, Y. H., Tan, P., Vallania, S., Vernetto, C., Vigorito, H., Wang, C. Y., Wu, H. R., Wu, L., Xue, Q. Y., Yang, X. C., Yang, Z. G., Yao, A. F., Yuan, M., Zha, H. M., Zhang, L., Zhang, X. Y., Zhang, Y., Zhang, J., Zhao, Zhaxiciren, Zhaxisangzhu, X. X., Zhou, F. R., Zhu, Q. Q., Zhu, G., Zizzi, P., Bernardini, Catalanotti, Sergio, A., D'Amone, I., De Mitri, DI GIROLAMO, Tristano, Iacovacci, Michele, G., Mancarella, G., Marsella, D., Martello, M., Panareo, and L., Perrone

Subjects
Physics, Radiation, Atmospheric pressure, Astrophysics::High Energy Astrophysical Phenomena, Settore FIS/01 - Fisica Sperimentale, Detector, Extensive air shower, Radon - natural radioactivity, Gamma ray, chemistry.chemical_element, Cosmic ray, Radon, Gamma-ray astronomy, Extensive air shower, Low energy cosmic instrumentation, Natural radioactivity, Radon, Nuclear physics, Air shower, chemistry, Low energy cosmic instrumentation, Natural radioactivity, Instrumentation, Radioactive decay, Physics::Atmospheric and Oceanic Physics
Abstract

The ARGO-YBJ experiment is an air shower detector for gamma ray astronomy and cosmic ray studies with an energy threshold of ∼500 GeV. Working in “single particle mode”, i.e. counting the single particles hitting the detector at fixed time intervals, ARGO-YBJ can monitor cosmic ray and gamma ray transients at energies of a few GeV. The single particle counting rate is modulated by the atmospheric pressure and temperature, and is affected by the local radioactivity from soil and air. Among the radioactive elements, radon gas is of particular importance since its concentration in air can vary significantly, according to environmental conditions. In this paper we evaluate the contribution of the radon daughter gamma ray emitters to the single particle counting rate measured by ARGO-YBJ. According to our analysis, the radon gas contribution is roughly 1–2%, producing a counting rate modulation of the same order of magnitude of the atmospheric effects.

Published
2014

45. Effectiveness of a project to prevent HIV vertical transmission in the Republic of Congo

Author

Bisio, F., Masini, G., Vacca, E. B., Calzi, A., Cardinale, F., Bruzzone, B., Bruzzi, P., Viscoli, C., Kento-Mwana, K., Nkouendolo, J. P., Moutou, J., Banguissa, H., Nicolini, L., Schenone, E., Repetto, E., Montaldo, C., Ferrando, S., Righi, E., Dentone, C., Farinella, S. T., Vitale, F., Izzo, M., Mularoni, A., Mikulska, M., Di Stefano, L., Malfatto, E., Bernardini, C., Ginocchio, F., Secondo, G., Delfino, E., Nicco, E., Prinapori, R., Parisini, A., De Hoffer, L., Mesini, A., Grignolo, S., Taramasso, L., Giacobbe, D. R., Artom, F., Dini, S., Beltrame, A., Ratto, S., Mbongou, F. A. M., Miguel, L. M., Nzagou, A. C., Mayembo, P., Ibata, D., Ventura, A., Nigro, N., Andrei, C., Icardi, G., Bisio, F, Masini, G, Blasi Vacca, E, Calzi, A, Cardinale, F, Bruzzone, B, Bruzz, P, Viscoli, C, Kento-Mwana group. Collaborators: Nkouendolo, JP, Moutou, J, Banguissa, H, Nicolini, L, Schenone, E, Repetto, E, Montaldo, C, Ferrando, S, Righi, E, Dentone, C, Farinella, ST, Vitale, F, Izzo, M, Mularoni, A, Mikulska, M, Di Stefano, L, Malfatto, E, Bernardini, C, Ginocchio,F, Secondo, G, Delfino, E, Nicco, E, Prinapori, R, Parisini, A, De Hoffer, L, and esini A, Grignolo S, Taramasso L, Giacobbe DR, Artom F, Dini S, Beltrame A, Ratto S, Mbongou FA, Miguel LM, Nzagou AC, Mayembo P, Ibata D, Ventura A, Nigro N, Andrei C, Icardi G.

Subjects
Male, Infectious Disease Transmission, PMTCT, Human immunodeficiency virus (HIV), HIV Infections, medicine.disease_cause, Settore MED/42 - Igiene Generale E Applicata, law.invention, law, Pregnancy, Vertical, Pharmacology (medical), Prospective Studies, Pregnancy Complications, Infectious, Prospective cohort study, Attrition, Drop-out, Lost to follow-up, Mother-to-child transmission, Congo, Female, Humans, Infant, Infant, Newborn, Infectious Disease Transmission, Vertical, Patient Acceptance of Health Care, Patient Compliance, Health Services Research, Pharmacology, Infectious Diseases, Infectious, drop-out, Transmission (mechanics), Microbiology (medical), attrition, HIV prevention, vertical transmission, republic of Congo, Transmission rate, Target population, Prenatal care, medicine, lost to follow-up, business.industry, mother-to-child transmission, medicine.disease, Newborn, Pregnancy Complications, Immunology, business, Demography
Abstract

OBJECTIVES: To evaluate the effectiveness of a prevention programme against the vertical transmission of HIV in a resource-limited setting and to investigate variables associated with compliance. PATIENTS AND METHODS: The Kento-Mwana project (2005-2008) provided counselling, serological and biomolecular testing and prophylaxis/therapy to HIV-positive pregnant women and their children attending four antenatal clinics in Pointe Noire, Republic of Congo. Expected and actual rates of vertical transmission of HIV were compared. Univariate and multivariate analyses were performed in order to identify variables associated with non-compliance. RESULTS: The observed transmission rate in the group who completed follow-up was 5/290 (1.7%, 95% CI 0.6%-4.1%). The overall estimated transmission rate in the target population, computed taking into account the expected vertical transmission of HIV among drop-outs, was 67-115/638 (10.5%-18.0%). A comparison between this rate and the expected transmission rate in the absence of intervention (25%-40%) showed that the programme was able to prevent approximately 50% of vertical transmissions. Older age (OR 0.33, 95% CI 0.16-0.66, P = 0.002), telephone availability (OR 0.42, 95% CI 0.24-0.72, P = 0.002) and occupation (OR 0.57, 95% CI 0.29-1.10, P = 0.092) were associated with better compliance. CONCLUSIONS: Despite the vast majority of women accepting counselling and testing, many of them refused prophylaxis or dropped out, thus reducing the effectiveness of the intervention from an ideal 2% to a still important but less impressive median transmission rate of 15% (range 10.5%-18%). Promoting participation and compliance, rather than increasing the potency of antiretroviral regimens, is crucial for preventing the vertical transmission of HIV in Africa

Published
2013

46. Molecular and functional characterization of calvarial stem cells in nonsyndromic craniosynostosis: role of the primary cilium-related signaling in the abnormal osteogenic niche

Author

Lattanzi, W., Bernardini, C., Barba, M., Geloso, M.C., Massimi, L., Tamburrini, G., Caldarelli, M., and Michetti, F.

Subjects
Craniosynostosis, primary cilium, osteogenic niche, bone, cranial vault
Abstract

Nonsyndromic craniosynostosis (NSC) is a congenital malformation due to the premature ossification of calvarial sutures, representing a paradigm of aberrant osteogenesis, with an unclear multifactorial etiopathogenesis. Through comparative analyses of fused-versus-patent sutures of affected patients, we demonstrated that calvarial stem cells (CSCs) display a constitutively overactive osteogenic potential at the site of premature synostosis, driven by the activation of intracellular osteogenic pathways. Microarray profiling allowed evidencing the significant differential expression of genes involved in the structure and function of the primary cilium, a key sensing organelle involved in cell differentiation and development. Indeed, the Bardet Biedl Syndrome-associated gene 9 (BBS9), encoding a structural component of the primary cilium, has been associated to the NSC phenotype in a recent GWAS. The expression of BBS9 appeared to be increased in CSCs from fused- versus unfused-sutures; moreover, confocal microscopy indicated that BBS9 expression in fused suture-CSCs tended to be scattered within the cytoplasm rather than localized at the transition zone of the primary cilium, as in control cells, indicating a reduced cell polarization. We performed in vitro gene silencing, co-culture assays and in vivo expression analysis in the rat calvarium, to confirm the role of BBS9 and related signaling in the osteogenic differentiation of CSCs and in the ossification of calvarial sutures. Overall our original data point towards the identification of the primary cilium as a key player involved in the abnormal communication of calvarial stem cells with surrounding cells and extracellular matrix within the abnormal osteogenic niche orchestrating the NSC phenotype., Italian Journal of Anatomy and Embryology, Vol 119, No 1 (Supplement) 2014

Published
2015
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49. Undifferentiated Human Adipose Tissue-Derived Stromal Cells Induce Mandibular Bone Healing in Rats

Author

Parrilla C, Saulnier N, Bernardini C, Patti R, Tartaglione T, Fetoni AR, Pola E, Paludetti G, Michetti F, Lattanzi W, Parrilla, C, Saulnier, N, Bernardini, C, Patti, R, Tartaglione, T, Fetoni, Ar, Pola, E, Paludetti, G, Michetti, F, and Lattanzi, W

Subjects
mandible, atsc
Abstract

OBJECTIVE: To test the osteo-regenerative potential of adipose tissue-derived stromal cells (ATSCs), an attractive human source for tissue engineering, in a rat model of mandibular defect. Human dermal fibroblasts (HDFs) were used as a differentiated cellular control in the study. DESIGN: The ATSCs and HDFs were isolated from human lipoaspirate and skin biopsy specimens, respectively. Cells were characterized in vitro and then adsorbed on an osteo-conductive scaffold to be transplanted in a mandibular defect of immunosuppressed rats. Naked unseeded scaffold was used as a negative control. MAIN OUTCOME MEASURES: Bone healing was studied by computerized tomography and histologic analysis after 4, 8, and 12 weeks. RESULTS: Computed tomography showed that undifferentiated ATSCs induced successful bone healing of the mandible defect when transplanted in animals, compared with HDFs and negative controls. Histologic analysis demonstrated that the newly formed tissue in the surgical defect retained the features of compact bone. CONCLUSION: Undifferentiated human ATSCs are suitable for cell-based treatment of mandibular defects, even in the absence of previous osteogenic induction in vitro.

Published
2011

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