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人类染色体端粒原位检测及比较大小的改进方法

Improved detection and comparative sizing of human chromosomal telomeres in situ.

作者信息

Krejcí K, Koch J

机构信息

Department of Cytogenetics, Danish Cancer Society, Tage Hansens Gade 2, DK-8000 Aarhus C, Denmark.

出版信息

Chromosoma. 1998 Jun;107(3):198-203. doi: 10.1007/s004120050297.

Abstract

Telomeric length dynamics are thought to play an important role both in the processes of cellular aging and cancer progression. We have revised the primed in situ (PRINS) labeling technique to allow an estimation of the relative length of individual telomeres. We illustrate the applicability of the approach by demonstrating different telomeric sizes not only between blood lymphocytes from a young and an old donor, but also among bone marrow cells from hematological cancer patients. In the latter case we found general variations in telomeric sizes as well as individual telomeric variations that would have escaped detection by other methods. An interesting finding was the selective expansion of a single telomere within a specific subset of cells.

摘要

端粒长度动态变化被认为在细胞衰老和癌症进展过程中都起着重要作用。我们改进了引物原位(PRINS)标记技术,以估计单个端粒的相对长度。我们通过展示不仅在年轻和年老供体的血液淋巴细胞之间,而且在血液系统癌症患者的骨髓细胞之间存在不同的端粒大小,来说明该方法的适用性。在后一种情况下,我们发现端粒大小存在普遍变化以及个体端粒变化,而这些变化用其他方法可能无法检测到。一个有趣的发现是在特定细胞亚群中单个端粒的选择性扩增。

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