Your search keyword '"Vincenza Morello"' showing total 3 results

1. Prognostic significance of p16INK4a alterations and 9p21 loss of heterozigosity in locally advanced laryngeal squamous cell carcinoma

Author

Manuela Migliavacca, Marcella Macaluso, M.L. Maestro, Nicola Gebbia, Sergio Salerno, Ricardo Bernaldez, Rosa Maria Tomasino, Corsale S, Ines Zanna, Viviana Bazan, Salvatore Restivo, Paloma López Quintela, G. Dardanoni, Antonio Russo, Vincenza Morello, Maria Teresa Sanz-Casla, Bazan V., Zanna I., Migliavacca M., Sanz-Casla M.T., Maestro M.L., Corsale S., Macaluso M., Dardanoni G., Restivo S., Quintela P.L., Bernaldez R., Salerno S., Morello V., Tomasino R.M., Gebbia N., and Russo A.

Subjects

Settore MED/06 - Oncologia Medica, Physiology, Clinical Biochemistry, Loss of Heterozygosity, Biology, Bioinformatics, S Phase, Loss of heterozygosity, p16INK4a, Humans, Point Mutation, Prospective Studies, Laryngeal Neoplasms, Gene, Proportional Hazards Models, Univariate analysis, Ploidies, Base Sequence, Proportional hazards model, Genes, p16, Point mutation, Single-strand conformation polymorphism, DNA, Neoplasm, Cell Biology, DNA Methylation, Cell cycle, Prognosis, Multivariate Analysis, DNA methylation, Carcinoma, Squamous Cell, Cancer research, Chromosomes, Human, Pair 9

Abstract

The p16INK4a gene, localized within chromosome 9p21, has been identified as a cyclin-dependent kinase inhibitor and may negatively regulate the cell cycle acting as a tumor suppressor. Genetic alterations involving the 9p21 region are common in human cancers. A consecutive series of 64 untreated patients (median of follow up 53 months) undergoing surgical resection for locally advanced laryngeal squamous-cell carcinomas (LSCCs) has been studied prospectively. Our purpose was to investigate p16 alterations (9p21 allelic loss, hypermethylation and point mutations) and their possible association with clinico-pathological data and flow cytometric variables (DNA-ploidy and S-phase fraction (SPF)), and to determine the possible prognostic role of this gene in these tumors. PCR-based techniques were used for investigating 9p21 loss of heterozygosity (LOH) and methylation promoter status of the p16 gene. p16 mutations were detected by PCR-SSCP (single strand conformation polymorphism) and sequencing. 9p21 LOH was detected in 16/62 (26%) informative tumors, point mutations in 5% (3/64) and hypermethylation in 9% (6/64) of the cases. p16 alterations were significantly associated with high SPF and DNA-aneuploidy. By univariate analysis, poor histologic differentiation, stage IV, DNA-aneuploidy and p16 point mutations proved to be significantly related to quicker relapse, whereas these same factors, and in addition high SPF, 9p21 LOH and any p16 alterations were significantly related to shorter overall survival. By Cox proportional hazards analysis only histologic grade (G3) and p16 point mutations were independently related to both disease relapse and death. Our study has identified p16 point mutations as important biomolecular indicators in LSCCs. © 2002 Wiley-Liss, Inc.

Published

2002

2. Havep53gene mutations and protein expression a different biological significance in colorectal cancer?*

Author

Ida Albanese, Valentina Calò, Ines Zanna, Marcella Macaluso, G. Dardanoni, Viviana Bazan, Rosa Maria Tomasino, Antonio Russo, Vincenza Morello, Corsale S, Antonella Amato, Nicola Gebbia, Mario La Farina, Carla Tubiolo, and Manuela Migliavacca

Subjects

Mutation, medicine.diagnostic_test, Physiology, Colorectal cancer, Clinical Biochemistry, Cell Biology, Gene mutation, Biology, medicine.disease, medicine.disease_cause, Molecular biology, Intestinal mucosa, DNA Mutational Analysis, medicine, Cancer research, Immunohistochemistry, Gene, Genetic testing

Abstract

p53 alterations are considered the most common genetic events in many types of neoplasms, including colorectal carcinoma (CRC). These alterations include mutations of the gene and/or overexpression of the protein. The aim of our study was to assess whether in 160 patients undergoing resective surgery for primary operable CRC there was an association between p53 mutations and protein overexpression and between these and other biological variables, such as cell DNA content (DNA-ploidy) and S-phase fraction (SPF), and the traditional clinicopathological variables. p53 mutations, identified by PCR-SSCP-sequencing analysis, were found in 68/160 patients (43%) and positive staining for p53 protein, detected with the monoclonal antibody DO-7, was present in 48% (77/160) of the cases, with agreement of 57% (91/160). In particular, a significant association was found between increased p53 expression and genetic alterations localized in the conserved regions of the gene or in the L3 DNA-binding domain and the specific type of mutation. Furthermore, both overexpression of p53 and mutations in the conserved areas of the gene were found more frequently in distal than in proximal CRCs, suggesting that they might be "biologically different diseases." Although p53 mutations in conserved areas were associated with flow cytometric variables, overexpression of p53 and mutations in its L3 domain were only related respectively to DNA-aneuploidy and high SPF. These data may reflect the complex involvement of p53 in the different pathways regulating cell-cycle progression. In conclusion, the combination of the mutational status and immunohistochemistry of p53, and flow cytometric data may provide an important insight into the biological features of CRCs.

Published

2002

3. 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