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Clinical Impact of Somatic Mosaicism in Cases with Small Supernumerary Marker Chromosomes

机译:体细胞镶嵌术在小数量标记物染色体病例中的临床影响

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摘要

Somatic mosaicism is present in slightly more than 50% of small supernumerary marker chromosome (sSMC) carriers. Interestingly, non-acrocentric derived sSMC show mosaicism much more frequently than acrocentric ones. sSMC can be present in different mosaic rates, which may go below 5% of the studied cells. Also cryptic mosaicism can be present and mosaics may be differently expressed in different tissues of the body. Even though in the overwhelming majority of the cases somatic sSMC mosaicism has no direct clinical effect, there are also cases with altered clinical outcomes due to mosaicism. Also clinically important is the fact that a de novo sSMC, even present in mosaic, may be a hint of uniparental disomy (UPD). As it is under discussion to possibly replace standard karyotyping by methods like array-CGH, the impracticality of the latter to detect low-level sSMC mosaics and/or UPD has to be considered as well. Overall, sSMC mosaicism has to be studied carefully in each individual case, as it can be extremely informative and of importance, especially for prenatal genetic counseling.
机译:体细胞镶嵌存在于略多于50%的小型超数字标记染色体(sSMC)携带者中。有趣的是,非杂技派生的sSMC显示镶嵌的频率比杂技派生的更频繁。 sSMC可以不同的镶嵌率存在,可能低于所研究细胞的5%。也可能存在隐秘的马赛克现象,并且马赛克可能在人体的不同组织中表达不同。即使在绝大多数情况下,体细胞sSMC镶嵌症没有直接的临床效果,也有一些病例由于镶嵌症而改变了临床预后。临床上也很重要的一个事实是,即使存在于马赛克中的新生sSMC也可能暗示了单亲二体性(UPD)。由于正在讨论通过阵列CGH之类的方法替换标准核型分析的方法,因此还必须考虑后者检测低级sSMC镶嵌图和/或UPD的不切实际性。总体而言,必须对每个病例​​的sSMC镶嵌进行认真研究,因为它可能非常有用,而且非常重要,特别是对于产前遗传咨询。

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