Miyado Mami, Muroya Koji, Katsumi Momori, Saito Kazuki, Kon Masafumi, Fukami Maki
Cytogenet Genome Res. 2018;154(3):122-125. doi: 10.1159/000488162. Epub 2018 Apr 7.
Isodicentric Y chromosome [idic(Y)] represents a relatively common subtype of Y chromosomal rearrangements in the germline; however, limited evidence supports the postzygotic occurrence of idic(Y). Here, we report a boy with hypospadias and somatically acquired idic(Y). The 3.5-year-old boy has been identified in our previous study for patients with hypospadias. In the present study, cytogenetic analysis including FISH revealed a 45,X[5]/46,X,idic(Y)[7]/46,XY[8] karyotype. MLPA showed a mosaic deletion involving PPP1R12BP1 and RBMY2DP. The idic(Y) was likely to have been formed through aberrant recombination between P1 palindromes and subsequently underwent mosaic loss. The patient's phenotype was attributable to deletion of some Y chromosomal genes and/or mosaic loss of chromosome Y (mLOY). The results suggest that idic(Y) can originate in postzygotic cells via palindrome-mediated crossovers. Moreover, our data indicate that somatically acquired idic(Y) can trigger mLOY, which usually appears as an aging-related phenomenon in elderly men.
等臂双着丝粒Y染色体[idic(Y)]是种系中Y染色体重排相对常见的亚型;然而,支持idic(Y)在合子后发生的证据有限。在此,我们报告一名患有尿道下裂且体细胞获得idic(Y)的男孩。这个3.5岁的男孩在我们之前对尿道下裂患者的研究中已被识别。在本研究中,包括荧光原位杂交(FISH)在内的细胞遗传学分析显示核型为45,X[5]/46,X,idic(Y)[7]/46,XY[8]。多重连接探针扩增(MLPA)显示存在涉及PPP1R12BP1和RBMY2DP的嵌合缺失。idic(Y)可能是通过P1回文序列之间的异常重组形成的,随后发生了嵌合丢失。患者的表型归因于一些Y染色体基因的缺失和/或Y染色体的嵌合丢失(mLOY)。结果表明idic(Y)可通过回文介导的交换在合子后细胞中起源。此外,我们的数据表明体细胞获得的idic(Y)可引发mLOY,而mLOY通常在老年男性中表现为与衰老相关的现象。
