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Your search keyword '"Valentina Agnese"' showing total 7 results
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3. Pediatric asthma control during the COVID‐19 pandemic.

Author

Ferraro, Valentina Agnese, Zamunaro, Andrea, Spaggiari, Silvia, Di Riso, Daniela, Zanconato, Stefania, and Carraro, Silvia

Subjects
*COVID-19 pandemic, *ASTHMA, *ASTHMA in children, *STAY-at-home orders, *CHILD support
Abstract

Background: The lockdown imposed by the COVID‐19 pandemic resulted in a completely different style of life with possible effects on the attitude toward their disease in patients with chronic lung disease, such as asthma. The aim of our study was to investigate in asthmatic children the level of asthma control and the maintenance therapy used during the lockdown. Methods: Among asthmatic children attending our clinic, we identified those who had been prescribed the same therapy in March‐April 2019 and March‐April 2020. The level of asthma control (GINA‐score) and the maintenance therapy used during the lockdown (March‐April 2020) were compared with those of March‐April 2019. We separately analyzed a small group of children with severe asthma treated with Omalizumab during the lockdown. Results: We enrolled 92 asthmatic children (67 males). Compared to 2019, in 2020 a higher proportion of children modified their maintenance therapy (38% vs. 15.2%, p <.001), with a significant increase in both the proportion of children who increased (p =.033) and in that of children who decreased their therapy (p =.026). The level of control resulted as significantly higher in 2020 (March p =.023; April p =.007). Also, the 13 children treated with Omalizumab showed a good level of control in 2020. Conclusions: In asthmatic children, the COVID‐19 pandemic lockdown had a significant impact on their asthma control and on their attitude toward maintenance therapy. [ABSTRACT FROM AUTHOR]

Published
2021
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4. Protecting youth from the vaping epidemic.

Author

Galderisi, Alfonso, Ferraro, Valentina Agnese, Caserotti, Marta, Quareni, Luca, Perilongo, Giorgio, Baraldi, Eugenio, and Eigenmann, Philippe

Subjects
*TOBACCO products, *ELECTRONIC cigarettes, *NICOTINE addiction, *ADOLESCENT smoking, *TOBACCO use, *SMOKING cessation, *ANTI-smoking campaigns
Abstract

E‐cigarettes (e‐cigs) have been initially proposed as an aid to smoke cessation in adults, whereas they turned into a paradoxical preferential gateway to tobacco and nicotine initiation for adolescents naïve to tobacco. More than 25% of US school‐age students is an e‐cigs user with a steep rise over the past years. A marketing strategy on media and social network targeting youths, in the absence of rules to protect the pediatric users, resulted in an unprecedented trend up in tobacco consumption among adolescents and gave rise to a new generation of nicotine‐addicted teenagers. Flavored e‐cigs liquids and aerosols contain airway irritants and toxicants, that, in turn, produced an increase in asthma prevalence and its exacerbations among adolescents. In addition, since August 2019 an outbreak of e‐cigarette, or vaping, product use‐associated lung injury (EVALI) has been described. In view of this, e‐cigs must no longer be considered harmless, especially in adolescents never used a tobacco product before. This is a call‐for‐action to establish effective rules and campaigns targeting youths aimed to limit their access to e‐cigs, thereby preserving the potential benefit in quitting tobacco addiction described in adults. Behavioral and educational actions, out of the conventional primary care setting, have been described as a model for a youth‐centered campaign. We call for stricter regulations on e‐cigs products, with respect to their marketing to the youngest ones, along with public health and primary care interventions that could curb the spread of this "vaping" epidemic. [ABSTRACT FROM AUTHOR]

Published
2020
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5. Pharmacogenomics in colorectal carcinomas: Future perspectives in personalized therapyThe authorship is shared equally by Antonio Russo and Simona Corsale.

Author

Antonio Russo, Simona Corsale, Patrizia Cammareri, Valentina Agnese, Sandra Cascio, Gaetana Di Fede, Marcella Macaluso, and Viviana Bazan

Subjects
PHARMACOLOGY, DRUG side effects, CANCER patients, DRUG metabolism -- Evaluation
Abstract

The recent introduction of new drugs such as capecitabine, irinotecan, and oxaliplatinum has greatly improved the clinical outcome of patients with advanced/metastatic colorectal cancer. Nevertheless, some patients may suffer from the adverse drug reactions which will probably be the main cause of chemotherapy failure. The goal of pharmacogenomics is to find correlations between therapeutic responses to drugs and the genetic profiles of patients; the different responses to a particular drug are due, in fact, not only to the specific clinico-pathological features of the patient or to environmental factors, but also to the ethnic origins and the particular individual's genetic profile. Genes which codify for the metabolism enzymes, receptor proteins, or protein targets of chemotherapy agents often present various genetic polymorphisms. The main aim of this review is to provide an overview of the known polymorphisms present in the genes which codify for factors (thymidylate synthase dihydropyrimidine dehydrogenase, uridine diphosphate (UDP)-glucuronosyl-transferase 1A1, enzymes implicated in DNA repair) involved in the action mechanisms of the drugs now utilized in chemotherapeutic treatment of colorectal carcinoma, such as fluoropyrimidines, irinotecan, and platinum agents. 2005 Wiley-Liss, Inc. [ABSTRACT FROM AUTHOR]

Published
2005
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6. Laser pressure catapulting (LPC): Optimization LPC‐system and genotyping of colorectal carcinomasThe authorship is shared equally by Viviana Bazan and Gaspare La Rocca.

Author

Viviana Bazan, Gaspare La Rocca, Simona Corsale, Valentina Agnese, Marcella Macaluso, Manuela Migliavacca, Valter Gregorio, Sandra Cascio, Pasqua Sandra Sisto, Gaetana Di Fede, Maria Buscemi, Eugenio Fiorentino, Rita Passantino, Vincenza Morello, Rosa Maria Tomasino, and Antonio Russo

Subjects
COLON cancer, CANCER prognosis, ELECTROPHORESIS, MICRODISSECTION
Abstract

Genotype analysis is becoming more and more useful in clinical practice, since specific mutations in tumors often correlate with prognosis and/or therapeutic response. Unfortunately, current molecular analytical techniques often require time‐consuming and costly steps of analysis, thus making their routine clinical use difficult. Moreover, one of the most difficult problems arising during tumor research is that of their cell heterogeneity, which depends on their clear molecular heterogeneity. SSCP analysis discriminates by means of aberrant electrophoresis migration bands, mutated alleles which may represent as little as 15–20% of their total number. Nevertheless, in order to identify by sequencing the type of alteration revealed by this technique, only the mutated allele must be isolated. The advent of laser microdissection is a procedure which easily solves these problems of accuracy, costs, and time. The aims of this study were to perfect the system of laser pressure catapulting (LPC) laser microdissection for the assessment of the mutational status of p53 and k‐ras genes in a consecutive series of 67 patients with colorectal carcinomas (CRC), in order to compare this technique with that involving hand‐dissection and to demonstrate that since the LPC system guarantees more accurate biomolecular analyses, it should become part of clinical routine in this field. The LPC‐system was perfected with the use of mineral oil and the LPC‐membrane. To compare the techniques of hand‐ and LPC‐microdissection, alcohol‐fixed, paraffin‐embedded tissue from 67 cases of CRC were both hand‐ and laser‐microdissected. In either case, dissected samples were analyzed by SSCP/sequencing and direct sequencing for k‐ras and p53 gene mutations. LPC‐microdissection made it possible to pick up mutations by direct sequencing or SSCP/sequencing, whereas hand‐microdissection mutations were identified only by means of SSCP followed by sequencing; direct sequencing did not reveal any mutation. In the 67 patients examined by either method, 36% (24/67) showed p53 mutations, 32 of which identified. Seventy‐eight percent (25/32) were found in the conserved areas of the gene, while 12% (4/32) were in the L2 loop, 50% (16/32) were in the L3 loop, and 12% (4/32) in the LSH motif of the protein. Moreover, of the 67 cases examined, 40% (27/67) showed mutations in k‐ras, with a total of 29 mutations identified. Of these, 14 (48%) were found in codon 12 and 15 (52%) in codon 13. The modifications which we brought to the LPC system led to a vast improvement of the technique, making it an ideal substitution for hand‐microdissection and guaranteeing a considerable number of advantages regarding facility, accuracy, time, and cost. Furthermore, the data obtained from the mutational analyses performed confirm that the LPC system is more efficient and rapid than hand‐microdissection for acquiring useful information regarding molecular profile and can therefore be used with success in clinical routine. © 2004 Wiley‐Liss, Inc. [ABSTRACT FROM AUTHOR]

Published
2005
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7. TP53 in gastric cancer: Mutations in the L3 loop and LSH motif DNA?binding domains of TP53 predict poor outcomeThe authorship is shared equally by Manuela Migliavacca and Laura Ottini, and their names are listed in alphabetical order.

Author

Manuela Migliavacca, Laura Ottini, Viviana Bazan, Valentina Agnese, Simona Corsale, Marcella Macaluso, Ramona Lupi, Gabriella Dardanoni, Maria Rosaria Valerio, Gianni Pantuso, Gaetana Di Fede, Rosa Maria Tomasino, Nicola Gebbia, Renato Mariani?Costantini, and Antonio Russo

Subjects
STOMACH cancer, CURATIVE medicine, ONCOLOGIC surgery, MICROSATELLITE repeats
Abstract

The aim of this study was to clarify whether specific p53 mutations may have biological relevance in terms of disease relapse or death in gastric carcinomas (GC). Resected specimens from a consecutive series of 62 patients with GC undergoing potentially curative surgery were prospectively studied. The mutational status of exons 5–8 of the p53 gene was investigated in 62 cases using the PCR?SSCP and sequencing. Presence of microsatellite instability (MSI) was evaluated in 56 cases by analyzing loci highly sensitive of MSI. Twenty mutations of p53 were detected in 17 of the 62 cases analyzed (27%). Ten mutations (50%) occurred in highly conserved domains. According to the p53 specific functional domains: 4/20 mutations (20%) were in the L3 loop and 3/20 (15%) in LSH motif. Eight of the 56 GC resulted MSI?H, 5 (9%) MSI?L, and 43 (77%) MSI stable (MSS). None of the 8 (14%) MSI?H GC showed p53 mutations. p53 mutations were associated with intestinal histotype. Moreover, specific mutations in functional domain (L3 and LSH), together with advanced TNM stage, node involvement, depth of invasion, diffuse histotype, proved to be significantly related to quicker relapse and to shorter overall survival. Specific mutations in p53 functional domains, rather than any mutations in this gene, may be biologically more significant in terms of patients outcome, indicating that these mutations might have biological relevance to identify subgroups of patients at higher risk of relapse or death who might benefit from a more aggressive therapeutic approach. © 2004 Wiley?Liss, Inc. [ABSTRACT FROM AUTHOR]

Published
2004
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