Chapman R M, Corcoran M M, Gardiner A, Hawthorn L A, Cowell J K, Oscier D G
Department of Haematology, Royal Bournemouth Hospital, Bournemouth, London.
Oncogene. 1994 Apr;9(4):1289-93.
Cytogenetic studies of B-cell chronic lymphocytic leukaemia show structural abnormalities involving the 13q14 chromosome region as the only karyotypic change in a significant proportion of tumours. This observation suggests the location of a gene important in leukaemogenesis. A series of 68 BCLL tumours have been analysed for allele loss using a series of probes from 13q14. Using intragenic polymorphic markers from the retinoblastoma predisposition gene LOH was observed in 25% of tumours including 3/6 showing cytogenetically obvious deletions of the 13q14 region and 3/6 showing translocations involving 13q14. However, three deletions with proximal breakpoints in 13q14 did not show allele loss, demonstrating that the breakpoint lay distal to RB1. Using the D13S25 locus, which lies 1.6 cM distal to RB1, allele loss was seen in 90% of tumours with structural rearrangements of 13q14 and 75% of tumours with an apparently normal karyotype. 50% of these tumours showed homozygous loss of D13S25, suggesting that a 'tumour suppressor gene' lies in this region. The more distal D13S31 locus, 1 cM distal to D13S25, was infrequently involved in allele loss demonstrating that the minimum region of overlap for homozygous deletions is approximately 1 Mbp around the D13S25 locus.
B 细胞慢性淋巴细胞白血病的细胞遗传学研究表明,在相当比例的肿瘤中,涉及 13q14 染色体区域的结构异常是唯一的核型变化。这一观察结果提示了一个在白血病发生过程中起重要作用的基因的位置。使用来自 13q14 的一系列探针,对 68 例 B 细胞慢性淋巴细胞白血病肿瘤进行了等位基因缺失分析。利用视网膜母细胞瘤易感基因的基因内多态性标记,在 25%的肿瘤中观察到杂合性缺失,其中包括 3/6 例细胞遗传学上显示 13q14 区域明显缺失的肿瘤和 3/6 例显示涉及 13q14 易位的肿瘤。然而,在 13q14 近端有断点的三个缺失并未显示等位基因缺失,这表明断点位于 RB1 基因的远端。使用位于 RB1 基因远端 1.6 cM 的 D13S25 位点,在 90%的 13q14 结构重排的肿瘤和 75%核型明显正常的肿瘤中观察到等位基因缺失。其中 50%的肿瘤显示 D13S25 纯合缺失,提示该区域存在一个“肿瘤抑制基因”。更远端的 D13S31 位点,位于 D13S25 远端 1 cM,很少发生等位基因缺失,这表明纯合缺失的最小重叠区域约为 D13S25 位点周围 1 Mbp。
