AI Article Synopsis
- RNA polymerase III (Pol-III) is crucial for making tRNAs and small RNAs, and its deregulation is linked to cancer, but its in vivo role wasn't well understood.
- Researchers manipulated the Brf1 transcription factor that helps Pol-III work, finding that knocking out Brf1 caused embryos to die, while mice with one functional copy were healthy.
- Conditional deletion of Brf1 in certain organs led to cell death and disrupted tissue balance, but Brf1's variation did not influence cancer development, indicating Brf1 is vital for tissue health but doesn’t directly drive cancer in the pancreas or gut.
Article Abstract
RNA polymerase III (Pol-III) transcribes tRNAs and other small RNAs essential for protein synthesis and cell growth. Pol-III is deregulated during carcinogenesis; however, its role in vivo has not been studied. To address this issue, we manipulated levels of Brf1, a Pol-III transcription factor that is essential for recruitment of Pol-III holoenzyme at tRNA genes in vivo. Knockout of Brf1 led to embryonic lethality at blastocyst stage. In contrast, heterozygous Brf1 mice were viable, fertile and of a normal size. Conditional deletion of Brf1 in gastrointestinal epithelial tissues, intestine, liver and pancreas, was incompatible with organ homeostasis. Deletion of Brf1 in adult intestine and liver induced apoptosis. However, Brf1 heterozygosity neither had gross effects in these epithelia nor did it modify tumorigenesis in the intestine or pancreas. Overexpression of BRF1 rescued the phenotypes of Brf1 deletion in intestine and liver but was unable to initiate tumorigenesis. Thus, Brf1 and Pol-III activity are absolutely essential for normal homeostasis during development and in adult epithelia. However, Brf1 overexpression or heterozygosity are unable to modify tumorigenesis, suggesting a permissive, but not driving role for Brf1 in the development of epithelial cancers of the pancreas and gut.
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| http://www.ncbi.nlm.nih.gov/pmc/articles/PMC6861133 | PMC |
| http://dx.doi.org/10.1038/s41418-019-0316-7 | DOI Listing |
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