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Overrepresentation of chromosome 12p sequences and karyotypic evolution in i(12p)-negative testicular germ-cell tumors revealed by fluorescence in situ hybridization
Authors:R. F. Suijkerbuijk   R. J. Sinke   A. M. Meloni   J. M. Parrington   J. van Echten   B. de Jong   J. W. Oosterhuis   A. A. Sandberg  A. Geurts van Kessel
Affiliation:

a Department of Human Genetics, University Hospital, Nijmegen, The Netherlands

b Cancer Center of the Southwest Biomedical Research Institute and Genetrix Inc., Scottsdale, Arizona, USA

c MRC Human Biochemical Genetics Unit, The Galton Laboratory, University College, London, UK

d Department of Medical Genetics, University of Groningen, The Netherlands

e Dr. Daniel den Hoed Cancer Center, Rotterdam, The Netherlands

Abstract:Human testicular germ-cell tumors (TGCTs) comprise a heterogeneous group of solid neoplasms. These tumors are characterized by the presence of a highly specific chromosomal abnormality, i.e., an isochromosome of the short arm of chromosome 12. At present, this i(12p) chromosome is found in more than 80% of TGCTs. Isochromosome 12p has also been observed in some ovarian and extragonadal germ cell tumors. In the remaining so-called i(12p)-negative TGCTs other abnormalities involving chromosome 12, mainly 12p, can be found. In order to establish whether 12p abnormalities other than i(12p) are a common phenomenon in TGCTs, a panel of 11 i(12p)-negative tumors was investigated using multicolor fluorescence in situ hybridization. All TGCTs examined appeared to contain chromosomal abnormalities involving 12p, resulting in a distinct overrepresentation of short arm sequences. In addition, indications were obtained for a clonal evolution in one of the tumors. Our data suggest that the occurrence of 12p abnormalities is a common phenomenon in i(12p)-negative TGCTs and that these abnormalities, analogous to i(12p), may contribute to the process of tumor development.
Keywords:
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