Avigad S, Barel D, Blau O, Malka A, Zoldan M, Mor C, Fogel M, Cohen I J, Stark B, Goshen Y, Stein J, Zaizov R
Cancer Molecular Genetics, Pediatric Hematology Oncology, Schneider Children's Medical Center of Israel, Petah Tiqva.
Oncogene. 1997 Apr 3;14(13):1541-5. doi: 10.1038/sj.onc.1200990.
Screening for p53 mutations in exons 5 to 8 in 124 pediatric malignancies identified 18 abnormal shifts using single strand conformation polymorphism: 12 were missense mutations and in 6, no mutation was detected in the exon or in the splice donor acceptor sequences. Sequencing was then performed in the adjacent introns, revealing a G to A base substitution at 39 base pairs upstream to exon 7. This mutation was identified in the germ line of five of the patients, and also in the father of one, whose parents were available. For comparison, of the 184 normal controls similarly screened, only one had this mutation (P=0.036). Positive staining of p53 protein was observed in three of the paraffin embedded tissues that were available: brain tumor, rhabdomyosarcoma, and lymphocytes from a normal lymph node from the rhabdomyosarcoma patient. All tumors with the identified intron mutation were Li-Fraumeni syndrome tumors. Sequencing of all exons including splice sites was performed and revealed no mutation. We suggest that this mutation in intron 6 of the p53 gene stabilizes the wild type p53 protein, resulting in its abnormal accumulation. Mutations in the noncoding region of p53 should be further studied.
对124例儿童恶性肿瘤的5至8号外显子进行p53突变筛查,采用单链构象多态性鉴定出18个异常迁移:12个为错义突变,6个在外显子或剪接供体/受体序列中未检测到突变。随后对相邻内含子进行测序,发现在外显子7上游39个碱基对处有一个G到A的碱基替换。在5名患者的生殖系中发现了这种突变,在其中一名患者的父亲(其父母可供检测)中也发现了该突变。作为对照,在同样筛查的184名正常对照中,只有1人有这种突变(P=0.036)。在可获得的3个石蜡包埋组织中观察到p53蛋白阳性染色:脑肿瘤、横纹肌肉瘤以及横纹肌肉瘤患者正常淋巴结中的淋巴细胞。所有鉴定出内含子突变的肿瘤均为李-弗劳梅尼综合征肿瘤。对包括剪接位点在内的所有外显子进行测序,未发现突变。我们认为p53基因内含子6中的这种突变使野生型p53蛋白稳定,导致其异常积累。p53非编码区的突变应进一步研究。
