AI Article Synopsis
- The cyclobutane thymine dimer, caused by sunlight exposure, is a major DNA damage type linked to skin cancer, the most common cancer in the Northern Hemisphere.
- Nucleotide excision repair is the only known cellular mechanism in humans that can remove this dimer, but the specifics of how this repair process works remain unclear.
- Research shows that several proteins work together to recognize and remove the dimer efficiently, using a cooperative approach to ensure effective repair despite each factor's low specificity on its own.
Article Abstract
The cyclobutane thymine dimer is the major DNA lesion induced in human skin by sunlight and is a primary cause of skin cancer, the most prevalent form of cancer in the Northern Hemisphere. In humans, the only known cellular repair mechanism for eliminating the dimer from DNA is nucleotide excision repair. Yet the mechanism by which the dimer is recognized and removed by this repair system is not known. Here we demonstrate that the six-factor human excision nuclease recognizes and removes the dimer at a rate consistent with the in vivo rate of removal of this lesion, even though none of the six factors alone is capable of efficiently discriminating the dimer from undamaged DNA. We propose a recognition mechanism by which the low-specificity recognition factors, RPA, XPA, and XPC, act in a cooperative manner to locate the lesion and, aided by the kinetic proofreading provided by TFIIH, form a high-specificity complex at the damage site that initiates removal of thymine dimers at a physiologically relevant rate and specificity.
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Source |
|---|---|
| http://www.ncbi.nlm.nih.gov/pmc/articles/PMC218148 | PMC |
| http://dx.doi.org/10.1101/gad.1131003 | DOI Listing |
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