Gilad S, Khosravi R, Shkedy D, Uziel T, Ziv Y, Savitsky K, Rotman G, Smith S, Chessa L, Jorgensen T J, Harnik R, Frydman M, Sanal O, Portnoi S, Goldwicz Z, Jaspers N G, Gatti R A, Lenoir G, Lavin M F, Tatsumi K, Wegner R D, Shiloh Y, Bar-Shira A
Department of Human Genetics, Sackler School of Medicine, Tel Aviv University, Ramat Aviv, Israel.
Hum Mol Genet. 1996 Apr;5(4):433-9. doi: 10.1093/hmg/5.4.433.
Ataxia-telangiectasia (A-T) is an autosomal recessive disorder involving cerebellar degeneration, immunodeficiency, chromosomal instability, radiosensitivity and cancer predisposition. The responsible gene, ATM, was recently identified by positional cloning and found to encode a putative 350 kDa protein with a Pl 3-kinase-like domain, presumably involved in mediating cell cycle arrest in response to radiation-induced DNA damage. The nature and location of A-T mutations should provide insight into the function of the ATM protein and the molecular basis of this pleiotropic disease. Of 44 A-T mutations identified by us to date, 39 (89%) are expected to inactivate the ATM protein by truncating it, by abolishing correct initiation or termination of translation, or by deleting large segments. Additional mutations are four smaller in-frame deletions and insertions, and one substitution of a highly conserved amino acid at the Pl 3-kinase domain. The emerging profile of mutations causing A-T is thus dominated by those expected to completely inactivate the ATM protein. ATM mutations with milder effects may result in phenotypes related, but not identical, to A-T.
共济失调毛细血管扩张症(A-T)是一种常染色体隐性疾病,涉及小脑变性、免疫缺陷、染色体不稳定、辐射敏感性和癌症易感性。其致病基因ATM最近通过定位克隆得以确定,发现它编码一种推定的350 kDa蛋白,该蛋白具有磷脂酰肌醇3激酶样结构域,可能参与介导因辐射诱导的DNA损伤而导致的细胞周期停滞。A-T突变的性质和位置应能为了解ATM蛋白的功能以及这种多效性疾病的分子基础提供线索。在我们迄今确定的44个A-T突变中,39个(89%)预计会通过截断ATM蛋白、废除翻译的正确起始或终止或删除大片段来使其失活。另外的突变是四个较小的框内缺失和插入,以及一个在磷脂酰肌醇3激酶结构域处高度保守氨基酸的替换。因此,导致A-T的突变的新情况主要由那些预计会使ATM蛋白完全失活的突变所主导。具有较轻影响的ATM突变可能会导致与A-T相关但不相同的表型。
