AI Article Synopsis
- Oxidative DNA damage is linked to cancer development and is mainly repaired by a process called base excision repair (BER), which is triggered by DNA glycosylases.
- The study focused on a specific variant of the NTHL1 glycosylase, R33K, which, when expressed in human cells, led to increased cell growth and potential tumor formation.
- Despite similar enzyme functions between the normal and mutated NTHL1, the R33K mutation disrupts important aspects of BER, possibly elevating cancer risk for individuals with this variant.
Article Abstract
Oxidatively-induced DNA damage, widely accepted as a key player in the onset of cancer, is predominantly repaired by base excision repair (BER). BER is initiated by DNA glycosylases, which locate and remove damaged bases from DNA. NTHL1 is a bifunctional DNA glycosylase in mammalian cells that predominantly removes oxidized pyrimidines. In this study, we investigated a germline variant in the N-terminal domain of NTHL1, R33K. Expression of NTHL1 R33K in human MCF10A cells resulted in increased proliferation and anchorage-independent growth compared to NTHL1 WT-expressing cells. However, wt-NTHL1 and R33K-NTHL1 exhibited similar substrate specificity, excision kinetics, and enzyme turnover and . The results of this study indicate an important function of R33 in BER that is disrupted by the R33K mutation. Furthermore, the cellular transformation induced by R33K-NTHL1 expression suggests that humans harboring this germline variant may be at increased risk for cancer incidence.
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Source |
|---|---|
| http://www.ncbi.nlm.nih.gov/pmc/articles/PMC7299534 | PMC |
| http://dx.doi.org/10.18632/oncotarget.27548 | DOI Listing |
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