Analysis of chromosome 12 aneuploidy in interphase cells from human male germ cell tumors by fluorescence in situ hybridization

Rodríguez, Eduardo; Mathew, Susan; Mukherjee, Asit B.; Reuter, Victor E.; Bosl, George J.; Chaganti, R. S. K.

doi:10.1002/gcc.2870050104

Cited by 47 publications

(26 citation statements)

References 8 publications

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“…Since the formation of the isochromosome includes the centromeric/pericentromeric region of chromosome 12, the abnormality can be detected using commercially available chromosome 12 centromeric fluorescent in situ hybridization (FISH) probes. 67,68,71 In a metaphase spread these will show the isochromosome nicely. In interphase cells one can detect a numerical abnormality (normal chromosome 12 plus the number of isochromosomes present) but it is more difficult if not impossible to state that an isochromosome is indeed present.…”

Section: Molecular Biology Of Germ Cell Tumorsmentioning

confidence: 97%

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Origins and molecular biology of testicular germ cell tumors

2005

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Section: Molecular Biology Of Germ Cell Tumorsmentioning

confidence: 97%

“…This genetic abnormality occurs in all primary sites and histologic types. 66,67 Approximately 80% of cases have i(12p) and the remainder have excess 12p genetic material in derivative chromosomes. 68 The consistent gain of 12p genetic material is supported by gene array and comparative genomic hybridization data.…”

Section: Molecular Biology Of Germ Cell Tumorsmentioning

confidence: 99%

Origins and molecular biology of testicular germ cell tumors

2005

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“…This anomaly is found less frequently in seminomas (SE), composed of malignant counterparts of early germ cells, than in nonseminomatous TGCT (NS), which are caricatures of early embryonal development composed of embryonal (embryonal carcinoma (EC] and teratoma (TE)) and/or extraembryonal (yolk sac (YS) and choriocarcinoma (CH)) components [9,10], Fluorescence in situ hybridization (FISH) using region-specific probes showed that also i(l2p)-negative TGCT invariably exhibit overrepresentations of 12p-sequences [11,12], Because conventional cytogenetic information is derived from mitotic cells, such data may be biased due to selection of 0165-4608/96/$15.00 PII S0165-4608(96)00043-X subpopulations of cells by the methods of direct harvest ing or short-term in vitro culture. This has recently been suggested for SE with respect to the presence of i(12p) [13]. Also the presence of markers of which, by definition, the chromosomal origin can not be determined, may ham per the identification of certain chromosomal regions important for the development of this cancer.…”

Section: Introductionmentioning

confidence: 99%

Comparative genomic hybridization of germ cell tumors of the adult testis: Confirmation of karyotypic findings and identification of a 12p-amplicon

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Pol

Weghuis

et al. 1996

Cancer Genetics and Cytogenetics

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Comparative genomic hybridization (CGH) was carried out on 15 primary testicular germ cell tumors (TGCT) o f adolescents and adults and two metastatic residual tumors after chemotherapeu tic treatment. The results were compared with karyotypic data obtained form the same tum or specimens after direct harvesting o f metaphases or short-term in vitro culture. .Both techniques revealed that the m ost consistent abnormality in prim ary TGCT is gain o f 12p-sequences. Although In m o st cases over representation o f the complete short arm was observed, CGH revealed a specific amplification of 1 2 p ll.l-p l2 ,l region in two independent primary tumors. In additiont loss of (parts of) chromosome 13 (always involving q31-qter), and gain o f (parts of) chromosome 7 (mostly involving q ll), (parts of) chro mosome 8, and the X chromosome were detected in more than 25% o f the tumors by this latter tech nique. Loss of 6ql5-q21 in both residual tumors analyzed m a y suggest a role for this anomaly in acquired resistance to chemotherapeutic treatm ent Overall, the CGH analyses confirmed gains and losses o f certain chromosomal regions in TGCT as

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“…In contrast, other groups have reported that 12p gain is not an early event, but rather relates to the invasive growth of TGCTs (Rosenberg et al, 2000;Summersgill et al, 2001). An isochromosome of the short arm of chromosome 12, i(12p), has been proposed as a specific genetic marker of human TGCTs (Rodriguez et al, 1992). The same group recently reported that among 101 TGCT specimens, stem cell-associated genes that localize on chromosome 12p13.3 are overexpressed in seminomas and embryonal carcinomas (Korkola et al, 2006).…”

Section: Introductionmentioning

confidence: 99%

DDX1 is required for testicular tumorigenesis, partially through the transcriptional activation of 12p stem cell genes

et al. 2009

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Cytogenetic analysis has identified 12p gain as the most frequent abnormality in human testicular germ cell tumors (TGCTs). It has been suggested that amplification and overexpression of stem cell-associated genes, including cyclin-D2, on the human chromosome 12p region are involved in germ cell tumorigenesis. By subtractive cDNA analysis, we identified Ddx1, a member of the DEAD-box protein family, as a gene predominantly expressed in the primordial germ cells of mouse embryos. Knockdown of Ddx1 in a mouse spermatogonia-derived cell line, GC-1spg, by short interference RNA repressed the expression of cyclin-D2, CD9 and GDF3 genes. In the mouse cyclin-D2 gene, a genomic DNA region between À348 and À329 was responsible for transcriptional activation by DDX1 based on reporter and gel shift assays. Similarly, DDX1 knockdown in the human TGCT cell line NEC8 repressed the expression of stem cell-associated genes localized on chromosome 12p13.3, including cyclin-D2, CD9 and NANOG. DDX1-knockeddown TGCT cells could not form solid tumors in nude mice. Furthermore, in situ hybridization revealed that DDX1 mRNA was produced in both seminoma and nonseminoma types of human TGCT samples. We conclude that DDX1 is a critical factor for testicular tumorigenesis.

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Analysis of chromosome 12 aneuploidy in interphase cells from human male germ cell tumors by fluorescence in situ hybridization

Cited by 47 publications

References 8 publications

Origins and molecular biology of testicular germ cell tumors

Origins and molecular biology of testicular germ cell tumors

Comparative genomic hybridization of germ cell tumors of the adult testis: Confirmation of karyotypic findings and identification of a 12p-amplicon

DDX1 is required for testicular tumorigenesis, partially through the transcriptional activation of 12p stem cell genes

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