martes, 22 de octubre de 2019

Validation of computational determination of microsatellite status using whole exome sequencing data from colorectal cancer patients | BMC Cancer | Full Text

Validation of computational determination of microsatellite status using whole exome sequencing data from colorectal cancer patients | BMC Cancer | Full Text

BMC Cancer

Validation of computational determination of microsatellite status using whole exome sequencing data from colorectal cancer patients

Abstract

Background

Microsatellite instability (MSI), resulting from a defective mismatch repair system, occurs in approximately 15% of sporadic colorectal cancers (CRC). Since MSI is associated with a poor response to 5-fluorouracile based chemotherapy and is a positive predictive marker of immunotherapy, it is routine practice to evaluate the MSI status of resected tumors in CRC patients. MSIsensor is a novel computational tool for determining MSI status using Next Generation Sequencing. However, it is not widely used in the clinic and has not been independently validated in exome data from CRC. To facilitate clinical implementation of computational determination of MSI status, we compared MSIsensor to current gold standard methods for MSI testing.

Methods

MSI status was determined for 130 CRC patients (UICC stage I-IV) using immunohistochemistry, PCR based microsatellite stability testing and by applying MSIsensor to exome sequenced tumors and paired germline DNA. Furthermore, we investigated correlation between MSI status, mutational load and mutational signatures.

Results

Eighteen out of 130 (13.8%) patients were microsatellite instable. We found a 100% agreement between MSIsensor and gold standard methods for MSI testing. All MSI tumors were hypermutated. In addition, two microsatellite stable (MSS) tumors were hypermutated, which was explained by a dominant POLE signature and pathogenic POLE mutations (p.Pro286Arg and p.Ser459Phe).

Conclusion

MSIsensor is a robust tool, which can be used to determine MSI status of tumor samples from exome sequenced CRC patients.

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