Sedlacek Z, Kodet R, Kriz V, Seemanova E, Vodvarka P, Wilgenbus P, Mares J, Poustka A, Goetz P
Institute of Biology and Medical Genetics, Second Medical School, Charles University, Prague, Czech Republic.
Br J Cancer. 1998 Apr;77(7):1034-9. doi: 10.1038/bjc.1998.172.
We describe two Li-Fraumeni syndrome families. Family A was remarkable for two early childhood cases of adrenocortical tumours, family B for a high incidence of many characteristic cancers, including a childhood case of choroid plexus tumour. Using direct sequencing, we analysed exons 5-9 of the p53 gene in constitutional DNA of individuals from both families and found two novel germline mutations in exon 5. In family A, we detected a point substitution in codon 138 (GCC to CCC), which resulted in the replacement of the alanine by a proline residue. Family B harboured a single-base pair deletion in codon 178 (CAC to -AC), resulting in a frameshift and premature chain termination. Three out of six tumours examined from both families, a renal cell carcinoma, a rhabdomyosarcoma and a breast cancer, showed loss of heterozygosity and contained only the mutant p53 allele. The remaining three neoplasms, both adrenocortical tumours and the choroid plexus tumour retained heterozygosity. Immunohistochemistry with anti-p53 antibody confirmed accumulation of p53 protein in tumours with loss of heterozygosity, while the remaining tumours were p53 negative. These results support the view that complete loss of activity of the wild-type p53 need not be the initial event in the formation of all tumours in Li-Fraumeni individuals.
我们描述了两个李-弗劳梅尼综合征家族。家族A以两例儿童期肾上腺皮质肿瘤为显著特征,家族B则以多种特征性癌症的高发病率为特点,包括一例儿童期脉络丛肿瘤。我们采用直接测序法,分析了两个家族个体的生殖细胞DNA中p53基因的第5至9外显子,在第5外显子中发现了两个新的种系突变。在家族A中,我们检测到密码子138处的一个点突变(GCC突变为CCC),导致丙氨酸被脯氨酸残基取代。家族B在密码子178处存在一个单碱基对缺失(CAC突变为-AC),导致移码和提前链终止。从两个家族检测的6个肿瘤中,一个肾细胞癌、一个横纹肌肉瘤和一个乳腺癌显示杂合性缺失,且仅含有突变型p53等位基因。其余三个肿瘤,即肾上腺皮质肿瘤和脉络丛肿瘤保留了杂合性。用抗p53抗体进行免疫组织化学证实,杂合性缺失的肿瘤中p53蛋白积聚,而其余肿瘤p53呈阴性。这些结果支持这样一种观点,即野生型p53活性的完全丧失不一定是李-弗劳梅尼个体所有肿瘤形成的初始事件。
