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Dive into the research topics where G. Peloso is active.

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Featured researches published by G. Peloso.


International Journal of Legal Medicine | 2006

Subtyping mtDNA haplogroup H by SNaPshot minisequencing and its application in forensic individual identification

Pierangela Grignani; G. Peloso; Alessandro Achilli; Chiara Turchi; Adriano Tagliabracci; Milena Alù; Giovanni Beduschi; Ugo Ricci; L Giunti; Carlo Robino; Sarah Gino; C. Previderè

Sequence variation of the hypervariable segments (HVS) I/II of mitochondrial DNA (mtDNA) and the haplogroup affiliation were determined in a sample of 271 Italian subjects. This analysis showed that 42% of the individuals could be ascribed to H, the most frequent haplogroup in European Caucasian populations. This fraction was then screened for specific single nucleotide polymorphisms located in the coding region to identify H subclades H1–H15. We set up two multiplex polymerase chain reactions and specific SNaPshot assays to investigate the frequency distribution of these subgroups in our population sample and to examine their usefulness in discriminating among commonly shared HVS I/II sequences. This allowed the assignment of a large portion of the mtDNAs (∼70%) to specific subhaplogroups, with H1 and H5 being the most represented. About two-thirds of the individuals sharing common HVS I/II sequences were subdivided and ascribed to specific H subhaplogroups with a significant reduction of the frequencies of the most common mtDNA haplotypes. Haplogroup H subtyping could thus be extremely useful in forensic identification when many samples have to be analysed and compared, avoiding excessive time-consuming and labor-intensive sequencing analysis.


International Journal of Legal Medicine | 2000

Highly informative Y-chromosomal haplotypes by the addition of three new STRs DYS437, DYS438 and DYS439.

Pierangela Grignani; G. Peloso; Paolo Fattorini; C. Previderè

Abstract The Y chromosome STRs DYS437, DYS438 and DYS439 were selected from publicly available genome databases and used to analyse an Italian population sample. A tetraplex PCR reaction including the highly informative DYS385 locus, was set up and used for the analysis of 131 male samples to determine allele frequencies and STR diversity values. The number of different haplotypes and the haplotype diversity value found from the analysis of the STRs included in the tetraplex reaction were very similar to those found from the analysis of the basic set of 7 Y-STRs (DYS19, DYS389I/II, DYS390, DYS391, DYS392 and DYS393) previously carried out on the same population sample. By combining the allelic states of the 11 Y-chromosomal STRs we could construct highly informative haplotypes that allowed the discrimination of 93.8% (120 out of 128) of the samples tested. This approach represents a very powerful tool for individual identification and paternity testing in forensic medicine.


Clinical Cancer Research | 2010

Novel Models of Myxoid Liposarcoma Xenografts Mimicking the Biological and Pharmacologic Features of Human Tumors

Roberta Frapolli; Elena Tamborini; Emanuela Virdis; Ezia Bello; Eva Tarantino; Sergio Marchini; Federica Grosso; Roberta Sanfilippo; Alessandro Gronchi; Juan Carlos Tercero; G. Peloso; Paolo G. Casali; Silvana Pilotti; Maurizio D'Incalci

Purpose: Myxoid liposarcoma is a common subtype of liposarcoma. It is associated in more than 90% of cases with the chromosomal translocation t(12;16)(q13;p11) leading to the fusion FUS-CHOP gene that is responsible for the oncogenic transformation of preadipocytes. Recently the marine natural product trabectedin has shown highly selective activity for myxoid liposarcoma, even in the most aggressive round-cell subtype. Experimental Design: Fragments of 17 sarcomas were transplanted s.c. in female athymic NCr-nu/nu mice. Xenografts were established and characterized by morphology, fluorescence in situ hybridization analysis for the translocation and reverse transcriptase-PCR analysis for fusion transcripts. Trabectedin was injected i.v. Results: Seven of 17 tumors grew as continuous xenografts, five of them being myxoid liposarcoma of the round-cell subtype. The chromosomal rearrangement and fusion transcripts in different passages were the same as in the human tumors from which they were derived. The responsiveness to trabectedin in type II myxoid liposarcoma xenografts was as high as in patients. The pathologic response was associated with the presence of the FUS-CHOP fusion gene, indicating that the drug does not totally eradicate the disease. Type III myxoid liposarcoma xenografts seemed much less sensitive to trabectedin, confirming previous clinical observations. Conclusions: This study reports for the first time the characterization of human myxoid liposarcoma xenografts that adequately mimic the biological and pharmacologic features of the human tumor. These models offer a useful tool for investigating the mechanism of selectivity of trabectedin, testing new combinations with this drug and evaluating novel therapies for myxoid liposarcoma. Clin Cancer Res; 16(20); 4958–67. ©2010 AACR.


Forensic Science International | 2003

Allele sharing in first-degree and unrelated pairs of individuals in the Ge.F.I. AmpFlSTR® Profiler Plus™ database

Silvano Presciuttini; Francesca Ciampini; Milena Alù; N. Cerri; M. Dobosz; Ranieri Domenici; G. Peloso; Susi Pelotti; A. Piccinini; E. Ponzano; Ugo Ricci; Adriano Tagliabracci; J.E Baley-Wilson; Francesco De Stefano; Vincenzo Lorenzo Pascali

Eleven Italian forensic laboratories participated in a population study based on the AB Profiler Plus loci with proficiency testing. The validated database, including 1340 individuals, is available on-line. Tests for Hardy-Weinberg equilibrium, gametic unbalance, and heterogeneity of gene frequency were generally not significant. Gene frequencies at each locus were consistent with those of two previously published Italian studies, but different from a third. Individuals of each subsample were paired, and the total number of alleles shared across the nine loci was determined in each pair. The analysis was replicated over the total sample. In addition, two samples of mother-child pairs (N=315) and full-sib pairs (N=91) were subjected to allele sharing analysis. The resulting distributions were sufficiently distinct from the sample of unrelated pairs as to be of practical usefulness.


International Congress Series | 2004

Allele distribution of five X-chromosome STR loci in an Italian population sample

G. Peloso; Pierangela Grignani; C. Previderè

Abstract Population genetic data for five X-chromosomal STR loci (DXS7423, DXS6789, DXS6795, DXS9898 and DXS8377) were generated by analysing a population sample from Northwest Italy. Intensive stutter bands were observed for the DXS8377 locus. The analysis of the 40 family trios segregation showed no new mutation.


Forensic Science International-genetics | 2009

Multiplex mtDNA coding region SNP assays for molecular dissection of haplogroups U/K and J/T.

Pierangela Grignani; Chiara Turchi; Alessandro Achilli; G. Peloso; Milena Alù; Ugo Ricci; Carlo Robino; Susi Pelotti; E. Carnevali; Ilaria Boschi; Adriano Tagliabracci; C. Previderè

Mitochondrial DNA (mtDNA) U/K and J/T are sister haplogroups within the superhaplogroup R. They are both common in Europe, with a combined overall frequency similar to the one reported for H, the most common European haplogroup (40-50%). In this study, we selected 159 Italian subjects, already ascribed to U/K and J/T by RFLP typing, and assigned each mtDNA to specific clades/subclades by investigating at least one diagnostic coding region SNP. For each sister haplogroup, one multiplex PCR and one SNaPshot minisequencing reaction were set up targeting 16 U/K and 7 J/T coding region SNPs. Each mtDNA sample was clearly assigned to a specific subclade, which could be further subdivided into several minor sub-branches according to peculiar HVS I/II motifs. Such a molecular dissection of haplogroups U/K and J/T could be extremely useful to reduce the overall analysis time and labor intensive sequencing procedures in high volume forensic casework, for example when it is important to rapidly exclude samples in order to restrict the number of suspects.


International Congress Series | 2003

Forensic evaluation of tetranucleotide STR instability in lung cancer

G. Peloso; Pierangela Grignani; R. Rosso; C. Previderè

Abstract The incidence of genetic instability affecting a set of STRs commonly used in forensic DNA analyses was assessed by performing a comparative study on 24 lung carcinomas with paired normal tissue samples. Out of 24 samples, 20 (83%) showed allele drop-out (ADO) in at least one STR locus. Allelic imbalance was detected at all the STR loci analysed. A small-cell carcinoma sample showed loss of heterozygosity (LOH), with complete deletion of one allele, at the D5S818 and D13S317 loci.


International Congress Series | 2003

A multicentric study of SE33 allele frequencies in the Italian population

Loredana Buscemi; Chiara Turchi; M. Pesaresi; Adriano Tagliabracci; Luciana Caenazzo; E. Ponzano; P. Cortivo; C. Previderè; G. Peloso; Pierangela Grignani; G. Pierucci; Chiara Toni; Isabella Spinetti; Silvano Presciuttini; Ranieri Domenici

Allele and genotype frequencies for STR SE33 were obtained for a sample of 419 Italians in view of application in personal identification and paternity. D 2003 Elsevier Science B.V. All rights reserved.


Forensic Science International | 2006

Validation of a large italian Database of 15 STR loci

Silvano Presciuttini; N. Cerri; Stefania Turrina; Benedetto Pennato; Milena Alù; Alessio Asmundo; Anna Barbaro; Ilaria Boschi; Loredana Buscemi; Luciana Caenazzo; E. Carnevali; Domenico De Leo; Cosimo Di Nunno; Ranieri Domenici; Michela Maniscalco; G. Peloso; Susi Pelotti; A. Piccinini; Daniele Podini; Ugo Ricci; Carlo Robino; Luigi Saravo; Andrea Verzeletti; M. Venturi; Adriano Tagliabracci


Forensic Science International: Genetics Supplement Series | 2008

Genetic characterisation of six miniSTR loci in an Italian population sample

G. Peloso; Pierangela Grignani; C. Previderè

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Adriano Tagliabracci

Marche Polytechnic University

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Milena Alù

University of Modena and Reggio Emilia

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Ugo Ricci

University of Florence

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