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Biomarker concordance between primary colorectal cancer and ovarian metastases: a Dutch cohort study. | LitMetric

AI Article Synopsis

  • - The study investigates whether the genetic features and mismatch repair (MMR) status of primary colorectal cancer (CRC) are the same as those in corresponding ovarian metastases, which is unclear and significant for treatment response.
  • - Researchers analyzed paired samples from CRC patients with ovarian metastases, using advanced sequencing and other techniques to determine gene mutation and MMR status.
  • - They found a 100% agreement in biomarker status, concluding that testing the primary CRC tissue is sufficient for understanding the MMR status and suggesting that genetic differences are not likely the reason for poorer treatment responses in ovarian metastases.

Article Abstract

Purpose: The genetic characteristics and mismatch repair (MMR) status of the primary tumor and corresponding metastases in colorectal cancer (CRC) are generally considered to be highly concordant. This implies that either the primary or metastatic tumor can be used for testing gene mutation and MMR status. However, whether this is also true for CRC and their ovarian metastases is currently unknown. Ovarian metastases generally show a poorer response to systemic therapy compared to other metastatic sites. Differences in biomarker status between primary CRC and ovarian metastases could possibly explain this difference in therapy response.

Methods: The study cohort was selected from CRC patients treated in two Dutch hospitals. Eligible patients with CRC and ovarian metastasis who were surgically treated between 2011 and 2018 were included. CRC and corresponding ovarian metastatic tissues were paired. Gene mutation status was established using next-generation sequencing, while the MMR status was established using either immunohistochemistry or microsatellite instability analysis.

Results: Matched samples of CRC and ovarian metastasis from 26 patients were available for analysis. A biomarker concordance of 100% was detected.

Conclusion: Complete biomarker concordance was found between MMR proficient CRC and their matching ovarian metastasis. Biomarker testing of MMR proficient CRC tissue appears to be sufficient, and additional testing of metastatic ovarian tissue is not necessary. Differences in therapy response between ovarian metastases and other metastases from CRC are thus unlikely to be caused by differences in the genetic status.

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Source
http://dx.doi.org/10.1007/s00432-022-04502-3DOI Listing

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