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After determining the enriched regions for each modification in normal and tumor samples (Table 1 and Additional file 1), they were annotated to human genes using the UCSC knownGenes databases [ 19] (Table 1) (Methods).
A much better understanding of the role of DNA methylation in cancer, either as a marker of disease or as an active driver of tumorigenesis, will likely be gained from genome-wide studies of this modification in normal and malignant cells.
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The establishment of cell cell junctions and polarity are both implicated in the regulation of epithelial modifications in normal and cancer situations.
In addition to the accumulation of mutations that occurs with age, there is also an increase in epigenetic modifications in normal tissues that can then also predispose to malignant transformation, for example, by the inactivation of tumour suppressor genes.
One of the goals of ENCODE was to characterize histone modifications in normal human cell lines, e.g., GM06990 (lymphoblastoid) and HFL1 (lung fibroblast), and also in cancer cell lines, e.g., K562 (leukemia), HeLa (cervical carcinoma).
To answer that, we systematically investigated the pattern of DNA methylation and histone modifications, which are known to be differentially set during embryonic development of the germ line, in CIS cells and derived cancers and compared them to the epigenetic patterns of the same modifications in normal human germ cells in the adult testis and in foetal gonocytes.
This observation is based on the limited clinical utility of epidrugs in treating defined hematopoietic neoplasms, our better understanding of epigenetic modifications in normal and cancer cells, the development of promising second-generation epigenetic inhibitor, and data from preclinical and clinical studies.
Likewise, the analysis of proteins, their post-translational modifications in normal and pathological conditions, coupled with the development of highly specific antibodies targeted to recognize different forms and states of proteins, including antibodies that work inside living cells (Attreed et al., 2012), will play pivotal roles in deciphering the molecular mechanisms of lens development.
By comparing histone modification patterns in normal mucosa and tumors, we found that alterations predicted to have major functional consequences were quite rare.
Extension of studies will also need to consider whether changes in global levels of histone modifications occur in normal or malignant lung tissue exposed to Ni in vivo.
The wide variation in the level of histone modifications seen in normal cells, the use of FRDA cell lines with very different repeat numbers and mRNA levels and differences in the experimental design and data analysis have added to the difficulty in reaching a consensus.
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Since I tried Ludwig back in 2017, I have been constantly using it in both editing and translation. Ever since, I suggest it to my translators at ProSciEditing.

Justyna Jupowicz-Kozak
CEO of Professional Science Editing for Scientists @ prosciediting.com