Your search keyword '"Zafarana, Gaetano"' showing total 3 results

1. Defining minimum genomic regions of imbalance involved in testicular germ cell tumors of adolescents and adults through genome wide microarray analysis of cDNA clones.

Author

McIntyre, Alan, Summersgill, Brenda, Jafer, Osman, Rodriguez, Sandrine, Zafarana, Gaetano, Oosterhuis, J Wolter, Gillis, Ad JM, Looijenga, Leendert, Cooper, Colin, Huddart, Robert, Clark, Jeremy, and Shipley, Janet

Subjects

GERM cells, TUMORS, GENOMES, ONCOGENES, CHROMOSOMES, GERMPLASM

Abstract

Identifying changes in DNA copy number can pinpoint genes that may be involved in tumor development. Here we have defined the smallest overlapping regions of imbalance (SORI) in testicular germ cell tumors other than the 12p region, which has been previously investigated. Definition of the regions was achieved through comparative genomic hybridization (CGH) analysis of a 4559 cDNA clone microarray. A total of 14 SORI were identified, which involved at least five of the 11 samples analysed. Many of these refined regions were previously reported using chromosomal or allelic imbalance studies. The SORI included gain of material from the regions 4q12, 17q21.3, 22q11.23 and Xq22, and loss from 5q33, 11q12.1, 16q22.3 and 22q11. Comparison with parallel chromosomal CGH data supported involvement of most regions. The various SORI span between one and 20 genes and highlight potential oncogenes/tumor suppressor genes to be investigated further (Supplementary material is available at http://www.crukdmf.icr.ac.uk/array/array.html).Oncogene (2004) 23, 9142-9147. doi:10.1038/sj.onc.1208115 Published online 18 October 2004 [ABSTRACT FROM AUTHOR]

Published

2004

2. 12p-Amplicon structure analysis in testicular germ cell tumors of adolescents and adults by array CGH.

Author

Zafarana, Gaetano, Grygalewicz, Beata, Gillis, Ad J M, Vissers, Lisenka E L M, van de Vliet, Walter, van Gurp, Ruud J H L M, Stoop, Hans, Debiec-Rychter, Maria, Oosterhuis, Jan Wolter, van Kessel, Ad Geurts, Schoenmakers, Eric F P M, Looijenga, Leendert H J, and Veltman, Joris A

Subjects

*TESTIS, *GERM cells, *GERMPLASM, *TUMORS, *GENES

Abstract

All invasive testicular germ cell tumors of adolescents and adults (TGCTs), that is, seminomas and nonseminomas, show gain of 12p sequences, mostly as isochromosomes. Although several candidate genes have been suggested, the relevant gene(s) have not been identified yet. About 10% of testicular seminomas, however, show a more restricted amplification of the 12p11.2-p12.1 region, in which the various amplicons show an apparent overlap, allowing for the shortest region of amplification overlap approach, aiming at the identification of pathogenetically relevant sequences residing in this region. Here we report on a high-resolution 12p-amplicon architecture analysis using microarray-based comparative genomic hybridization, the results of which were subsequently confirmed by fluorescent in situ hybridization studies. The 12p-specific microarray contained 63 positionally selected BAC clones, which are more or less evenly distributed over the short arm of chromosome 12 (average spacing: less than 500?Kb), including 20 clones within the region of amplification. Out of a series of 17 seminomas, seven seminomas showed amplification of the whole amplicon region, of which three showed a dip in T/R value in the center of the amplified area. A more complex amplification pattern was found in the other 10 seminomas: three showed predominant amplification at the centromeric border; one mainly at the telomeric border; six showed a balanced amplification of both the centromeric and telomeric regions. The only nonseminoma investigated showed a structure in which the centromeric border was only amplified. These data support a mechanistic model in which at least two 12p genes, situated at the border regions of the amplicon, are positional candidates capable of actively supporting tumor progression in TGCTs.Oncogene (2003) 22, 7695-7701. doi:10.1038/sj.onc.1207011 [ABSTRACT FROM AUTHOR]

Published

2003

3. Role of gain of 12p in germ cell tumour development.

Author

LOOIJENGA, LEENDERT H. J, ZAFARANA, GAETANO, GRYGALEWICZ, BEATA, SUMMERSGILL, BRENDA, DEBIEC-RYCHTER, MARIA, VELTMAN, JORIS, SCHOENMAKERS, ERIC F. P. M, RODRIGUEZ, SANDRINE, JAFER, OSMAN, CLARK, JEREMY, VAN KESSEL, AD GEURTS, SHIPLEY, JANET, VAN GURP, RUUD J. H. L. M, GILLIS, AD J. M, and OOSTERHUIS, J. WOLTER

Subjects

*GERM cells, *TESTICULAR diseases, *TUMORS, *CANCER, *MEDICAL genetics

Abstract

Within the human testis, three entities of germ cell tumours are distinguished: the teratomas and yolk sac tumors of newborn and infants, the seminomas and nonseminomas of adolescents and young adults, referred to as testicular germ cell tumours (TGCT), and the spermatocytic seminomas. Characteristic chromosomal anomalies have been reported for each group, supporting their distinct pathogenesis. TGCT are the most common cancer in young adult men. The initiating pathogenetic event of these tumours occurs during embryonal development, affecting a primordial germ cell or gonocyte. Despite this intra-uterine initiation, the tumour will only be clinically manifest after puberty, with carcinoma in situ (IS) as the precursor. All invasive TGCT, both seminomas and nonseminomas, as well as CIS cells are aneuploid. The only consistent (structural) chromosomal abnormalities in invasive TGCT are gains of the short arm of chromosome 12, mostly due to isochromosome (i(12p)) formation. This suggests that an increase in copy number of a gene(s) on 12p is associated with the development of a clinically manifest TGCT. Despite the numerous (positional) candidate gene approaches that have been undertaken thus far, identification of a causative gene(s) has been hampered by the fact that most 12p gains involve rather large genomic intervals, containing unmanageable numbers of candidate genes. Several years ago, we initiated a search for 12p candidate genes using TGCT with a restricted 12p-amplification, cytogenetically identified as 12p11.2–p12.1. This approach is mainly based on identification of candidate genes mapped within the shortest region of overlap of amplification (SROA). In this review, data will be presented, which support the model that gain of 12p-sequences is associated with suppression of apoptosis and Sertoli cell-independence of CIS cells. So far, DAD-R is one of the most likely candidate genes involved in this process, possibly via N-glycosylation.... [ABSTRACT FROM AUTHOR]

Published

2003