Felix C A, D'Amico D, Mitsudomi T, Nau M M, Li F P, Fraumeni J F, Cole D E, McCalla J, Reaman G H, Whang-Peng J
Pediatric Branch, National Cancer Institute, National Institutes of Health, Bethesda, Maryland 20892.
J Clin Invest. 1992 Aug;90(2):653-8. doi: 10.1172/JCI115907.
Germline p53 mutations have been identified in the Li-Fraumeni syndrome but the role of such mutations in familial leukemia is not established. The p53 gene was examined by single-strand conformation polymorphism analysis of exons 4-8 in 10 families with multiple members affected with leukemia. The diagnoses included acute and chronic leukemias and Hodgkin's disease. Identified in two families were p53 mutations that were nonhereditary. These included a 2-bp deletion in exon 6 found in the lymphoblast DNA of one child whose sibling, cousin, and several adult relatives had acute leukemia. The other nonhereditary p53 mutation was a transition at codon 248 (CGG to CAG, arginine to glutamine) found in the lymphoblasts of a patient with a preleukemic syndrome and acute lymphoblastic leukemia (ALL) whose brother is a long-term survivor of ALL. Thus, p53 mutations were found to occur in two families but both were nonhereditary. Moreover, in the remaining eight families no p53 mutation was identified in the regions of p53 where most mutations have been found in other cancers. Although p53 mutations sometimes may be present, they do not appear to be a primary event responsible for hereditary susceptibility to familial leukemia. This study suggests involvement of other genes or mechanisms.
在李-佛美尼综合征中已发现种系p53突变,但此类突变在家族性白血病中的作用尚未明确。通过对10个有多名成员患白血病的家族的第4至8外显子进行单链构象多态性分析,对p53基因进行了检测。诊断包括急性和慢性白血病以及霍奇金病。在两个家族中发现的p53突变是非遗传性的。其中包括在一名儿童的淋巴母细胞DNA中发现的第6外显子2碱基缺失,该儿童的兄弟姐妹、堂兄弟姐妹和几名成年亲属患有急性白血病。另一个非遗传性p53突变是在一名患有白血病前期综合征和急性淋巴细胞白血病(ALL)的患者的淋巴母细胞中发现的密码子248处的转换(CGG到CAG,精氨酸到谷氨酰胺),其兄弟是ALL的长期幸存者。因此,在两个家族中发现了p53突变,但均为非遗传性。此外,在其余8个家族中,在p53的其他癌症中发现大多数突变的区域未发现p53突变。虽然有时可能存在p53突变,但它们似乎不是家族性白血病遗传易感性的主要原因。这项研究提示其他基因或机制的参与。
