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在健康献血者中,后天获得性莱昂化偏斜在较长时间内保持稳定。

Acquired skewing of Lyonization remains stable for a prolonged period in healthy blood donors.

作者信息

van Dijk J P, Heuver L, Stevens-Linders E, Jansen J H, Mensink E J B M, Raymakers R A P, de Witte T

机构信息

Central Hematology Laboratory, University Medical Center Nijmegen, Nijmegen, The Netherlands.

出版信息

Leukemia. 2002 Mar;16(3):362-7. doi: 10.1038/sj.leu.2402379.

Abstract

The pattern of X-chromosome inactivation (XCIP), or Lyonization, can be used to distinguish monoclonal from polyclonal cell populations in females. However, a skewed XCIP exists in hematopoietic cells in approximately 40% of healthy elderly females, interfering with interpretation of clonality assays. In hematopoiesis, an active stem cell pool is assumed to be present within a larger population of inactive stem cells, with a continuous exchange of cells between the two compartments. The assumption that the active stem cell pool size decreases with age may explain the phenomenon of acquired skewing occurring by chance and predicts the XCIP of this population to fluctuate. This fluctuation should be reflected in the XCIP of peripheral granulocytes. We examined the XCIP for fluctuations in time in peripheral granulocytes, monocytes and T cells of young, middle-aged and elderly healthy females. We used an optimized HUMARA PCR assay that eliminates unbalanced DNA amplification. We found no fluctuations in XCIP in any age group in up to 18 months follow-up. We conclude that acquired skewing arises gradually in life without fluctuations in XCIP and that analysis at multiple time points cannot distinguish monoclonal hematopoiesis from normal, skewed hematopoiesis.

摘要

X染色体失活模式(XCIP),即莱昂化现象,可用于区分女性体内的单克隆细胞群和多克隆细胞群。然而,约40%的健康老年女性造血细胞中存在X染色体失活偏斜,这干扰了克隆性检测结果的解读。在造血过程中,假定活跃干细胞池存在于大量不活跃干细胞群体中,两个区室之间存在细胞的持续交换。活跃干细胞池大小随年龄增长而减小这一假设,或许可以解释偶然发生的获得性偏斜现象,并预测该群体的X染色体失活模式会发生波动。这种波动应在外周血粒细胞的X染色体失活模式中得到体现。我们检测了年轻、中年和老年健康女性外周血粒细胞、单核细胞和T细胞的X染色体失活模式随时间的波动情况。我们采用了优化的HUMARA PCR检测方法,该方法可消除不平衡的DNA扩增。在长达18个月的随访中,我们发现任何年龄组的X染色体失活模式均无波动。我们得出结论,获得性偏斜在生命过程中逐渐出现,X染色体失活模式并无波动,且在多个时间点进行分析无法区分单克隆造血与正常的偏斜造血。

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