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体细胞重编程揭示了构成环染色体结构和(不)稳定性的复杂生物学。

Complex biology of constitutional ring chromosomes structure and (in)stability revealed by somatic cell reprogramming.

机构信息

Research Institute of Medical Genetics, Tomsk National Research Medical Center, Ushaika Street 10, Tomsk, 634050, Russia.

Department of Molecular Mechanisms of Development, Institute of Cytology and Genetics SB RAS, Novosibirsk, 630090, Russia.

出版信息

Sci Rep. 2021 Feb 22;11(1):4325. doi: 10.1038/s41598-021-83399-3.

Abstract

Human ring chromosomes are often unstable during mitosis, and daughter cells can be partially or completely aneuploid. We studied the mitotic stability of four ring chromosomes, 8, 13, 18, and 22, in long-term cultures of skin fibroblasts and induced pluripotent stem cells (iPSCs) by GTG karyotyping and aCGH. Ring chromosome loss and secondary aberrations were observed in all fibroblast cultures except for r(18). We found monosomy, fragmentation, and translocation of indexed chromosomes. In iPSCs, aCGH revealed striking differences in mitotic stability both between iPSC lines with different rings and, in some cases, between cell lines with the same ring chromosome. We registered the spontaneous rescue of karyotype 46,XY,r(8) to 46,XY in all six iPSC lines through ring chromosome loss and intact homologue duplication with isoUPD(8)pat occurrence, as proven by SNP genotype distribution analysis. In iPSCs with other ring chromosomes, karyotype correction was not observed. Our results suggest that spontaneous correction of the karyotype with ring chromosomes in iPSCs is not universal and that pluripotency is compatible with a wide range of derivative karyotypes. We conclude that marked variability in the frequency of secondary rearrangements exists in both fibroblast and iPSC cultures, expanding the clinical significance of the constitutional ring chromosome.

摘要

人类环状染色体在有丝分裂过程中通常不稳定,子细胞可能部分或完全非整倍体。我们通过 GTG 核型分析和 aCGH 研究了皮肤成纤维细胞和诱导多能干细胞 (iPSC) 中长期培养中的四条环状染色体 8、13、18 和 22 的有丝分裂稳定性。除 r(18) 外,所有成纤维细胞培养物中都观察到环状染色体丢失和次级畸变。我们发现了单体、碎片化和索引染色体易位。在 iPSC 中,aCGH 揭示了不同环状 iPSC 系之间以及某些情况下具有相同环状染色体的细胞系之间有丝分裂稳定性的显著差异。我们通过 SNP 基因型分布分析证实,在所有六个 iPSC 系中,自发挽救了核型 46,XY,r(8) 至 46,XY,通过环状染色体丢失和完整同源物复制以及 isoUPD(8)pat 的发生来实现。在具有其他环状染色体的 iPSC 中,未观察到核型校正。我们的结果表明,iPSC 中环状染色体的自发核型校正并非普遍现象,并且多能性与广泛的衍生核型兼容。我们得出结论,在成纤维细胞和 iPSC 培养物中,次级重排的频率存在明显的可变性,扩展了环状染色体的临床意义。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/71b7/7900208/b30916180974/41598_2021_83399_Fig1_HTML.jpg

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