Literature DB >> 7777541

A region of consistent deletion in neuroblastoma maps within human chromosome 1p36.2-36.3.

P S White1, J M Maris, C Beltinger, E Sulman, H N Marshall, M Fujimori, B A Kaufman, J A Biegel, C Allen, C Hilliard, M B Valentine, A T Look, H Enomoto, S Sakiyama, G M Brodeur.   

Abstract

Deletion of the short arm of human chromosome 1 is the most common cytogenetic abnormality observed in neuroblastoma. To characterize the region of consistent deletion, we performed loss of heterozygosity (LOH) studies on 122 neuroblastoma tumor samples with 30 distal chromosome 1p polymorphisms. LOH was detected in 32 of the 122 tumors (26%). A single region of LOH, marked distally by D1Z2 and proximally by D1S228, was detected in all tumors demonstrating loss. Also, cells from a patient with a constitutional deletion of 1p36, and from a neuroblastoma cell line with a small 1p36 deletion, were analyzed by fluorescence in situ hybridization. Cells from both sources had interstitial deletions of 1p36.2-36.3 which overlapped the consensus region of LOH defined by the tumors. Interstitial deletion in the constitutional case was confirmed by allelic loss studies using the panel of polymorphic markers. Four proposed candidate genes--DAN, ID3 (heir-1), CDC2L1 (p58), and TNFR2--were shown to lie outside of the consensus region of allelic loss, as defined by the above deletions. These results more precisely define the location of a neuroblastoma suppressor gene within 1p36.2-36.3, eliminating 33 centimorgans of proximal 1p36 from consideration. Furthermore, a consensus region of loss, which excludes the four leading candidate genes, was found in all tumors with 1p36 LOH.

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Year:  1995        PMID: 7777541      PMCID: PMC41727          DOI: 10.1073/pnas.92.12.5520

Source DB:  PubMed          Journal:  Proc Natl Acad Sci U S A        ISSN: 0027-8424            Impact factor:   11.205


  28 in total

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3.  Report and abstracts of the First International Workshop on Human Chromosome 1 Mapping 1994. Bethesda, Maryland, March 25-27, 1994.

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4.  Recurrent 1;17 translocations in human neuroblastoma reveal nonhomologous mitotic recombination during the S/G2 phase as a novel mechanism for loss of heterozygosity.

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5.  Translocation involving 1p and 17q is a recurrent genetic alteration of human neuroblastoma cells.

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6.  Identification of human DAN gene, mapping to the putative neuroblastoma tumor suppressor locus.

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7.  Alterations in the PITSLRE protein kinase gene complex on chromosome 1p36 in childhood neuroblastoma.

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9.  Two distinct deleted regions on the short arm of chromosome 1 in neuroblastoma.

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10.  1;17 translocations and other chromosome 17 rearrangements in human primary neuroblastoma tumors and cell lines.

Authors:  N Van Roy; G Laureys; N C Cheng; P Willem; G Opdenakker; R Versteeg; F Speleman
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6.  Evidence for a rare prostate cancer-susceptibility locus at chromosome 1p36.

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10.  An 85-kb tandem triplication in the slow Wallerian degeneration (Wlds) mouse.

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