在健康个体和不同疾病中偏X染色体失活。

Karen Helene Ørstavik
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引用次数: 0

摘要

未标记:在雌性哺乳动物细胞中,两条X染色体中的一条在胚胎早期失活。雌性是两个细胞群体的嵌合体,一个是母亲的,另一个是父亲的X作为活跃染色体。偏X染色体失活是任意定义的,通常是80%或更多的细胞表现出一条X染色体优先失活的模式。失活被认为是一个细胞所有后代的永久性失活;然而,在大约55岁之后,外周血细胞中歪斜X失活的频率增加,可能是通过选择。在几种X连锁疾病的受影响女性携带者中发现了不利的X失活歪斜,其中携带突变等位基因的X染色体主要是活跃的X;然而,对于许多X连锁疾病,很难证明X失活模式与临床表型之间的一致关系。其中一个原因可能是外周血细胞在许多疾病中不是具有代表性或相关的组织。在一些严重的X连锁疾病中,失活后选择发生在携带突变等位基因的X染色体上,导致X失活模式完全扭曲。在患有乳腺癌的年轻女性中也有偏X失活的报道,这可能表明X连锁基因对这种疾病的发展有影响。结论:X的失活过程和由此产生的偏曲程度对遗传病的表达明显重要。然而,同样重要的是要考虑到,在正常情况下,外周血细胞中X偏失活的频率随着年龄的增长而增加。对X染色体上大部分基因表达的分析表明,X染色体失活的异质性比以前认为的要大。
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Skewed X inactivation in healthy individuals and in different diseases.

Unlabelled: In female mammalian cells, one of the two X chromosomes is inactivated in early embryonic life. Females are mosaics for two cell populations, one with the maternal and one with the paternal X as the active chromosome. Skewed X inactivation is arbitrarily defined, often as a pattern where 80% or more of the cells show a preferential inactivation of one X chromosome. Inactivation is presumed to be permanent for all descendants of a cell; however, after about 55 years of age, the frequency of skewed X inactivation in peripheral blood cells increases, probably through selection. Unfavourable skewing of X inactivation, where the X chromosome carrying a mutant allele is the predominantly active X, has been found in affected female carriers of several X-linked disorders; however, for many X-linked disorders, a consistent relationship between the pattern of X inactivation and clinical phenotype has been difficult to demonstrate. One reason for this may be that peripheral blood cells are not a representative or relevant tissue in many disorders. In some severe X-linked disorders, post-inactivation selection takes place against the X chromosome carrying the mutant allele, leading to a completely skewed X-inactivation pattern. Skewed X inactivation has also been reported in young females with breast cancer, and may indicate an effect of X-linked genes on the development of this condition.

Conclusion: The process of X inactivation and the resultant degree of skewing is clearly important for the expression of genetic diseases. It is also important to consider, however, that under normal conditions the frequency of skewed X inactivation increases with age in peripheral blood cells. Analysis of the expression of a large proportion of the genes on the X chromosome has revealed that X-chromosome inactivation is more heterogeneous than previously thought.

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