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5-氮杂脱氧胞苷可区分活性和非活性X染色体的浓缩。

5-Azadeoxycytidine distinguishes between active and inactive X chromosome condensation.

作者信息

Haaf T, Werner P, Schmid M

机构信息

Department of Genetics, Yale University School of Medicine, New Haven, Connecticut 06510-8005.

出版信息

Cytogenet Cell Genet. 1993;63(3):160-8. doi: 10.1159/000133526.

Abstract

Treatment with 5-azadeoxycytidine (5-aza-dC) causes dramatic inhibition of mitotic condensation in the inactive X chromosome, without affecting the active X chromosome and autosomes. The undercondensed chromatin structure is most prominent in the late-replicating regions of the inactive X chromosome, whereas specific earlier-replicating segments on the inactive X probably associated with large blocks of genes that escape inactivation remain normally condensed. This segmentation of inactive X chromosomes has been evolutionarily conserved and is unique to mammals. It suggests temporal or mechanistic separation in condensation of inactive X chromatin. Condensation of chromatin structure is a novel and general feature of inactive X chromosomes that may be involved, directly or indirectly, in the maintenance and stabilization of X inactivation.

摘要

用5-氮杂脱氧胞苷(5-aza-dC)处理会显著抑制失活X染色体中的有丝分裂凝聚,而不影响活性X染色体和常染色体。凝聚不足的染色质结构在失活X染色体的晚复制区域最为明显,而失活X染色体上特定的早复制片段可能与逃避失活的大片段基因相关,这些片段仍保持正常凝聚。失活X染色体的这种分段在进化上是保守的,且是哺乳动物所特有的。这表明失活X染色质凝聚存在时间或机制上的分离。染色质结构的凝聚是失活X染色体的一个新的普遍特征,可能直接或间接地参与X染色体失活的维持和稳定。

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