Somatic mosaicism is something that is observed in everyday lives of cytogeneticists. Chromosome instability is one of the leading causes of large-scale genome variation analyzable since the correct human chromosome number was established in 1956. Somatic mosaicism is also a well-known fact to be present in cases with small supernumerary marker chromosomes (sSMC), i.e. karyotypes of 47,+mar/46. In this study, the data available in the literature were collected concerning the frequency mosaicism in different subgroups of patients with sSMC. Of 3124 cases with sSMC 1626 (52%) present with somatic mosaicism. Some groups like patients with Emanuel-, cat-eye- or i(18p)- syndrome only tend rarely to develop mosaicism, while in Pallister-Killian syndrome every patient is mosaic. In general, acrocentric and non-acrocentric derived sSMCs are differently susceptible to mosaicism; non-acrocentric derived ones are hereby the less stable ones. Even though, in the overwhelming majority of the cases, somatic mosaicism does not have any detectable clinical effects, there are rare cases with altered clinical outcomes due to mosaicism. This is extremely important for prenatal genetic counseling. Overall, as mosaicism is something to be considered in at least every second sSMC case, array-CGH studies cannot be offered as a screening test to reliably detect this kind of chromosomal aberration, as low level mosaic cases and cryptic mosaics are missed by that.
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机译:体细胞镶嵌症是细胞遗传学家日常生活中观察到的东西。自从1956年建立了正确的人类染色体数目以来,染色体的不稳定性是可分析的大规模基因组变异的主要原因之一。体细胞镶嵌症也是一个众所周知的事实,存在于超小的数字标记染色体(sSMC)的病例中,即47,+ mar / 46的核型。在这项研究中,收集了文献中有关sSMC患者不同亚组的频率镶嵌的数据。在3124例sSMC中有1626例(52%)存在体细胞镶嵌症。一些群体,例如患有伊曼纽尔病,猫眼病或i(18p)综合征的患者很少会发展成马赛克,而在Pallister-Killian综合征中,每个患者都是马赛克。总的来说,以非中心为中心的sSMCs对镶嵌的敏感性不同。因此,非acrocentric派生的是不稳定的。即使在绝大多数情况下,体细胞镶嵌症并没有任何可检测到的临床效果,但也有少数病例因镶嵌症而改变了临床预后。这对于产前遗传咨询极为重要。总体而言,由于至少在每第二个sSMC病例中都要考虑镶嵌现象,因此无法提供阵列CGH研究作为可靠检测这种染色体畸变的筛查测试,因为低水平的镶嵌病例和隐秘镶嵌会被忽略。
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