Jena University Hospital, Institute of Human Genetics, Jena, Germany.
J Histochem Cytochem. 2011 Sep;59(9):842-8. doi: 10.1369/0022155411412780. Epub 2011 Jun 14.
Small supernumerary maker chromosomes (sSMC) and uniparental disomy (UPD) are rare, and a combination of both is rarely encountered. Accordingly, only 46 sSMC cases UPD have been reported. Despite of its rareness, UPD has to be considered, especially in prenatal cases with sSMC. Here, the authors reviewed all sSMC cases with UPD (sSMC(U+)) and compared them to sSMC without UPD (sSMC(U-)), which resulted in the following correlations: 1) every sSMC, irrespective of its chromosomal origin, may be principally connected with UPD; 2) mixed hetero- and iso-UPD (hUPD/iUPD) can be observed most often in sSMC(U+) cases followed by complete iUPD, complete hUPD, and segmental iUPD; 3) UPD of chromosomes 6, 7, 14, 15, 16, and 20 is most often reported in sSMC(U+); 4) maternal UPD was approximately nine times more frequent than paternal UPD; 5) if mosaic with a normal cell line, acrocentric-derived sSMC had a three times higher chance of occurrence than the corresponding nonmosaic sSMC cases; 6) UPD in connection with a parentally inherited sSMC is, if existent at all, a rare event; and 7) the gender type and shape of sSMC had no effect on UPD formation. Overall, sSMC(U+) cases may have a story to tell about chromosome number control mechanisms in early embryogenesis.
小型额外标记染色体 (sSMC) 和单亲二倍体 (UPD) 较为罕见,两者同时存在的情况更为罕见。因此,仅有 46 例 sSMC 伴 UPD 的病例被报道。尽管其发生率较低,但仍需考虑 UPD 的可能性,尤其是在伴有 sSMC 的产前病例中。在此,作者回顾了所有 sSMC 伴 UPD(sSMC(U+))的病例,并将其与不伴 UPD 的 sSMC(sSMC(U-))进行比较,得出以下相关性:1) 每一条 sSMC,无论其染色体来源如何,都可能主要与 UPD 相关;2) 在 sSMC(U+)病例中最常观察到混合性异源和同源性 UPD(hUPD/iUPD),其次是完全性 iUPD、完全性 hUPD 和节段性 iUPD;3) sSMC(U+)中最常报道 UPD 的染色体为 6、7、14、15、16 和 20;4) 母源 UPD 比父源 UPD 更为常见,约为 9 倍;5) 如果存在正常细胞系嵌合体,则与 acrocentric 衍生的 sSMC 相关的 UPD 发生的可能性比相应的非嵌合体 sSMC 病例高 3 倍;6) 如果存在与亲本遗传的 sSMC 相关的 UPD,则为罕见事件;7) sSMC 的性别类型和形态对 UPD 的形成没有影响。总体而言,sSMC(U+)病例可能有一个关于早期胚胎发生中染色体数量控制机制的故事。
