Parshad R, Sanford K K, Kraemer K H, Jones G M, Tarone R E
Pathology Department, Howard University College of Medicine, Washington, DC 20059.
J Clin Invest. 1990 Jan;85(1):135-8. doi: 10.1172/JCI114403.
We were able to detect clinically normal carriers of xeroderma pigmentosum (XP) genes with coded samples of either peripheral blood lymphocytes or skin fibroblasts, using a cytogenetic assay shown previously to detect individuals with cancer-prone genetic disorders. Metaphase cells of phytohemagglutinin-stimulated T-lymphocytes from eight individuals who are obligate heterozygotes for XP were compared with those from nine normal controls at 1.3, 2.3, and 3.3 h after x-irradiation (58 R) during the G2 phase of the cell cycle. Lymphocytes from the XP heterozygotes had twofold higher frequencies of chromatid breaks or chromatid gaps than normal (P less than 10(-5)) when fixed at 2.3 or 3.3 h after irradiation. Lymphocytes from six XP homozygotes had frequencies of breaks and gaps threefold higher than normal. Skin fibroblasts from an additional obligate XP heterozygote, when fixed approximately 2 h after x-irradiation (68 R), had a twofold higher frequency of chromatid breaks and a fourfold higher frequency of gaps than fibroblasts from a normal control. This frequency of aberrations in cells from the XP heterozygote was approximately half that observed in the XP homozygote. The elevated frequencies of chromatid breaks and gaps after G2 phase x-irradiation may provide the basis of a test for identifying carriers of the XP gene(s) within known XP families.
我们能够使用一种先前已被证明可检测易患癌症遗传疾病个体的细胞遗传学检测方法,通过外周血淋巴细胞或皮肤成纤维细胞的编码样本,来检测临床正常的着色性干皮病(XP)基因携带者。在细胞周期的G2期,对来自8名XP基因必然杂合子个体的植物血凝素刺激的T淋巴细胞中期细胞,与9名正常对照者的细胞在X射线照射(58伦琴)后1.3、2.3和3.3小时进行了比较。当在照射后2.3或3.3小时固定时,XP杂合子的淋巴细胞中染色单体断裂或染色单体间隙的频率比正常情况高出两倍(P小于10^(-5))。来自6名XP纯合子的淋巴细胞中,断裂和间隙的频率比正常情况高出三倍。来自另一名XP基因必然杂合子个体的皮肤成纤维细胞,在X射线照射(68伦琴)后约2小时固定时,其染色单体断裂频率比正常对照的成纤维细胞高出两倍,间隙频率高出四倍。XP杂合子细胞中的这种畸变频率约为XP纯合子中观察到的频率的一半。G2期X射线照射后染色单体断裂和间隙频率的升高,可能为在已知XP家族中识别XP基因携带者的检测提供基础。
