Weak linkage at 4p16 to predisposition for human neuroblastoma

被引:0
作者
Patrizia Perri
Luca Longo
Roberto Cusano
Carmel M McConville
Sally A Rees
Marcella Devoto
Massimo Conte
Giovanni Battista Ferrara
Marco Seri
Giovanni Romeo
Gian Paolo Tonini
机构
[1] Laboratory of Neuroblastoma Research,Department of Paediatrics and Child Health
[2] Advanced Biotechnology Center,Department of Oncology
[3] Laboratory of Population Genetics,Department of Research
[4] National Institute for Cancer Research (IST),Department of Hematology and Oncology
[5] Laboratory of Molecular Genetics,Department of Internal Medicine
[6] Gaslini Children's Hospital,undefined
[7] University of Birmingham,undefined
[8] Biology and Genetics,undefined
[9] University of Genoa,undefined
[10] AI duPont Hospital for Children,undefined
[11] Gaslini Children's Hospital,undefined
[12] Laboratory of Immunogenetics,undefined
[13] National Institute for Cancer Research (IST),undefined
[14] Cardioangiology and Hepatology,undefined
[15] University of Bologna,undefined
来源
Oncogene | 2002年 / 21卷
关键词
neuroblastoma; chromosome 4p; LOH; linkage analysis; tumor suppressor genes;
D O I
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中图分类号
学科分类号
摘要
The most frequent genetic alterations described in neuroblastoma (NB) are amplification of MYCN oncogene and deletion of chromosome 1p, although somatic deletions have been demonstrated at other chromosomal intervals. Since loss of heterozygosity (LOH) at distal 4p has been observed in about 20–29% of neuroblastomas, we have evaluated deletions in 41 Italian NB samples by LOH analysis at loci mapping to 4p as follows: pter-D4S2936-D4S412-D4S2957-D4S432-D4S3023-D4S431-cen. Our analysis showed allele losses in eight out of 41 samples (19.5%) and allowed the identification of a smallest region of overlapping deletion (SRO) of 3.0 cM, delimited by D4S412 and D4S3023. Two of these tumors with 4p LOH are from patients belonging to a family with recurrent NB. Interestingly the genotyping of this family revealed an identical haplotype that includes the nonrecombinant loci D4S412, D4S2957 and D4S432 shared by all affected children and demonstrated that this haplotype is retained in the two tumors carrying somatic deletions from patients of this family. Furthermore linkage analysis was performed in two NB families and yielded an overall lod-score of 3.0 in the interval including the haplotype. This provides a confirmatory indication that the region delimited by D4S2936 and D4S3023, which also includes the new defined SRO, may harbor NB predisposing gene/s.
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收藏
页码:8356 / 8360
页数:4
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