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揭开染色体制备之谜以及有丝分裂期间染色体凝聚概念的影响。

Demystifying chromosome preparation and the implications for the concept of chromosome condensation during mitosis.

作者信息

Claussen U, Michel S, Mühlig P, Westermann M, Grummt U-W, Kromeyer-Hauschild K, Liehr T

机构信息

Institute of Human Genetics and Anthropology, Friedrich Schiller University, Jena, Germany.

出版信息

Cytogenet Genome Res. 2002;98(2-3):136-46. doi: 10.1159/000069817.

Abstract

The processes taking place during routine chromosome preparation are not well understood. In this study, the morphological changes in amniotic fluid cells, blood lymphocytes, and bone marrow cells in the metaphase stage were examined under an inverted microscope during chromosome preparation. The putative processes that occur during chromosome preparation were simulated in suspension, and the cells were treated with different mixtures of hypotonic solution, fixative, methanol, acetic acid, and water. Evaporation of the fixative was performed under normal atmospheric conditions and under vacuum at different levels of humidity. Freeze fracture electron microscopy was used to analyze the effects of fixative on the cell membrane. Confocal microscopic analysis was used to investigate three-dimensionally the effects of hypotonic treatment on the positions of chromosomes in fixed mitotic lymphocytes. Chromosome preparation-induced changes in the lengths of single chromosomes were also investigated. The results show that chromosome spreading involves significant water-induced swelling of mitotic cells during evaporation of the fixative from the slide, which is a prerequisite for chromosomal elongation, the production of metaphase spreads for chromosome analysis, and the appearance of Giemsa banding patterns. Hypotonic treatment is essential for well-spread metaphase chromosomes because it moves the chromosomes from a central to a more peripheral position in the cell, where they can be stretched more effectively during mitotic swelling. Like mitotic cells, isolated single chromosomes also have their own potential to swell and lengthen during chromosome preparation. We hypothesize that chromosome preparation leads to a genome-wide chromosomal region-specific opening of chromatin structures as GTG-light bands and sub-bands. Living cells may possess a similar mechanism, which is used only to open single chromatin structures to facilitate transcription. We propose the concept of chromosomal region-specific protein swelling.

摘要

常规染色体制备过程中发生的具体机制尚未完全明确。在本研究中,在染色体制备过程中,利用倒置显微镜观察了处于中期阶段的羊水细胞、血液淋巴细胞和骨髓细胞的形态变化。在悬浮状态下模拟了染色体制备过程中可能发生的过程,并用不同的低渗溶液、固定剂、甲醇、乙酸和水的混合物处理细胞。在正常大气条件和不同湿度水平的真空条件下进行固定剂的蒸发。采用冷冻断裂电子显微镜分析固定剂对细胞膜的影响。利用共聚焦显微镜三维研究低渗处理对固定有丝分裂淋巴细胞中染色体位置的影响。还研究了染色体制备引起的单条染色体长度变化。结果表明,染色体铺展涉及在固定剂从载玻片上蒸发过程中,有丝分裂细胞因水诱导而显著肿胀,这是染色体伸长、产生用于染色体分析的中期铺片以及吉姆萨带型出现的前提条件。低渗处理对于中期染色体的良好铺展至关重要,因为它能将染色体从细胞中央移至更外围的位置,在有丝分裂肿胀过程中染色体在此处能更有效地伸展。与有丝分裂细胞一样,分离的单条染色体在染色体制备过程中也有自身肿胀和延长的潜力。我们推测,染色体制备会导致全基因组范围内染色质结构在GTG浅带和亚带区域特异性开放。活细胞可能具有类似机制,仅用于打开单个染色质结构以促进转录。我们提出了染色体区域特异性蛋白质肿胀的概念。

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