AI Article Synopsis
- Recent molecular tests for KRAS mutations in colorectal cancer highlight the importance of proper tissue sample preparation, particularly regarding cold ischemia and formalin fixation times.
- A study on 401 specimens found that biopsy specimens yielded better DNA quality than resection specimens, especially with a cold ischemia time of one hour or less.
- While formalin fixation time showed less impact within routine ranges, prolonged fixation beyond three months significantly degraded DNA quality.
Article Abstract
Background: With the recent development of molecular tests for various biomarkers, it has become even more important to prepare adequate tissue samples. However, little is known about how the effect of cold ischemia time or formalin fixation time can affect KRAS mutation detection in colorectal cancer.
Methods: This study included the results of KRAS mutation tests for colorectal cancer in 401 specimens. We investigated clinicopathologic factors that may affect DNA quality of formalin-fixed, paraffin-embedded (FFPE) tissue including specimen type, cold ischemia time, and formalin fixation time and assessed the detection rate of the KRAS mutation in samples with varying DNA quality.
Results: Sample DNA quality for KRAS mutation test was better in biopsy specimens, which showed markedly shorter cold ischemia time and shorter formalin fixation time compared to resection specimens. A cold ischemia time of one hour or less was associated with better sample DNA quality. But the formalin fixation time was not a significant factor when it fell within the range performed in routine pathology diagnosis. When prolonged formalin fixation was tested, we confirmed that the specimen DNA quality gradually got worse from one month to three months.
Conclusions: The biopsy specimens showed better sample DNA quality for KRAS mutation test compared to resection specimens. In a routine diagnostic pathology setting, the cold ischemia time was an important factor affecting DNA quality and the formalin fixation had a wide time range for optimal DNA quality.
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| http://dx.doi.org/10.1016/j.prp.2019.02.018 | DOI Listing |
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