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肿瘤细胞中的染色质异常。

Abnormalities of chromatin in tumor cells.

作者信息

Drobic Bojan, Dunn Katherine L, Espino Paula S, Davie James R

机构信息

Manitoba Institute of Cell Biology, University of Manitoba, Winnipeg, Manitoba, R3E OV9 Canada.

出版信息

EXS. 2006(96):25-47. doi: 10.1007/3-7643-7378-4_2.

Abstract

Nuclear morphometric descriptors such as nuclear size, shape, DNA content and chromatin organization are used by pathologists as diagnostic markers for cancer. Tumorigenesis involves a series of poorly understood morphological changes that lead to the development of hyperplasia, dysplasia, in situ carcinoma, invasive carcinoma, and in many instances finally metastatic carcinoma. Nuclei from different stages of disease progression exhibit changes in shape and the reorganization of chromatin, which appears to correlate with malignancy. Multistep tumorigenesis is a process that results from alterations in the function of DNA. These alterations result from stable genetic changes, including those of tumor suppressor genes, oncogenes and DNA stability genes, and potentially reversible epigenetic changes, which are modifications in gene function without a change in the DNA sequence. DNA methylation and histone modifications are two epigenetic mechanisms that are altered in cancer cells. The impact of genetic (e.g., mutations in Rb and ras family) and epigenetic alterations with a focus on histone modifications on chromatin structure and function in cancer cells are reviewed here.

摘要

核形态学描述符,如核大小、形状、DNA含量和染色质组织,被病理学家用作癌症的诊断标志物。肿瘤发生涉及一系列理解不足的形态学变化,这些变化导致增生、发育异常、原位癌、浸润癌的发展,并且在许多情况下最终发展为转移性癌。疾病进展不同阶段的细胞核呈现出形状变化和染色质重组,这似乎与恶性肿瘤相关。多步骤肿瘤发生是一个由DNA功能改变导致的过程。这些改变源于稳定的基因变化,包括肿瘤抑制基因、癌基因和DNA稳定性基因的变化,以及潜在可逆的表观遗传变化,即基因功能的修饰而DNA序列不变。DNA甲基化和组蛋白修饰是癌细胞中发生改变的两种表观遗传机制。本文综述了遗传改变(如Rb和ras家族的突变)和以组蛋白修饰为重点的表观遗传改变对癌细胞染色质结构和功能的影响。

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