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Human germ cell formation in xenotransplants of induced pluripotent stem cells carrying X chromosome aneuploidies

机译:带有X染色体非整倍性的诱导多能干细胞异种移植中的人类生殖细胞形成

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Turner syndrome is caused by complete or partial loss of the second sex chromosome and is characterized by spontaneous fetal loss in >90% of conceptions. Survivors possess an array of somatic and germline clinical characteristics. Induced pluripotent stem cells (iPSCs) offer an opportunity for insight into genetic requirements of the X chromosome linked to Turner syndrome. We derived iPSCs from Turner syndrome and control individuals and examined germ cell development as a function of X chromosome composition. We demonstrate that two X chromosomes are not necessary for reprogramming or maintenance of pluripotency and that there are minimal differences in gene expression, at the single cell level, linked to X chromosome aneuploidies. Formation of germ cells, as assessed in vivo through a murine xenotransplantation model, indicated that undifferentiated iPSCs, independent of X chromosome composition, are capable of forming germ-cell-like cells (GCLCs) in vivo. In combination with clinical data regarding infertility in women with X chromosome aneuploidies, results suggest that two intact X chromosomes are not required for human germ cell formation, qualitatively or quantitatively, but rather are likely to be required for maintenance of human germ cells to adulthood.
机译:特纳综合症是由第二性染色体的全部或部分丧失引起的,其特征是在> 90%的受孕中自然流产。幸存者具有一系列的体细胞和种系临床特征。诱导多能干细胞(iPSC)为深入了解与特纳综合征相关的X染色体的遗传需求提供了机会。我们从特纳综合征和对照个​​体中获得了iPSC,并检查了生殖细胞发育与X染色体组成的关系。我们证明了两个X染色体对于重新编程或维持多能性不是必需的,并且在单细胞水平上与X染色体非整倍性相关的基因表达的差异很小。如通过鼠异种移植模型在体内评估的,生殖细胞的形成表明未分化的iPSC,独立于X染色体组成,能够在体内形成生殖细胞样细胞(GCLC)。结合有关X染色体非整倍性女性不育症的临床数据,结果表明,定性或定量地确定人类生殖细胞不需要两个完整的X染色体,而维持人类生殖细胞至成年则可能需要两个完整的X染色体。

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