Cancers (Apr 2022)

Microsatellite Status Detection in Gastrointestinal Cancers: PCR/NGS Is Mandatory in Negative/Patchy MMR Immunohistochemistry

  • Federica Zito Marino,
  • Martina Amato,
  • Andrea Ronchi,
  • Iacopo Panarese,
  • Franca Ferraraccio,
  • Ferdinando De Vita,
  • Giuseppe Tirino,
  • Erika Martinelli,
  • Teresa Troiani,
  • Gaetano Facchini,
  • Felice Pirozzi,
  • Michele Perrotta,
  • Pasquale Incoronato,
  • Raffaele Addeo,
  • Francesco Selvaggi,
  • Francesco Saverio Lucido,
  • Michele Caraglia,
  • Giovanni Savarese,
  • Roberto Sirica,
  • Marika Casillo,
  • Eva Lieto,
  • Annamaria Auricchio,
  • Francesca Cardella,
  • Ludovico Docimo,
  • Gennaro Galizia,
  • Renato Franco

DOI
https://doi.org/10.3390/cancers14092204
Journal volume & issue
Vol. 14, no. 9
p. 2204

Abstract

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Background: Microsatellite instability (MSI) is a predictive biomarker for immune checkpoint inhibitors. The main goal was to investigate the discordance between IHC and PCR/NGS for MSI testing in gastrointestinal cancers. Methods: Two series were analyzed through IHC for mismatch-repair-system proteins (MMRP) and PCR, with one series of 444 colorectal cancers (CRC) and the other of 176 gastric cancers (GC). All cases with discordant results between IHC and PCR were analyzed by NGS. IHC staining was evaluated as follows: proficient MMR (pMMR), with all MMR positive; deficient MMR (dMMR), with the loss of one heterodimer; and cases with the loss/patchy expression of one MMR (lo-paMMR). Cases with instability in at least two markers by PCR were MSI-high (MSI-H) and with instability in one marker, MSI-low (MSI-L). Cases without instability were evaluated as microsatellite-stable (MSS). Results: In the CRC cohort, 15 out of 444 cases were dMMR and 46 lo-paMMR. Among the 15 dMMR, 13 were MSI-H and 2 MSS. Among the 46 lo-paMMR, 13 were MSI-H and 33 were MSS. In the GC cohort, 13 out of 176 cases were dMMR and 6 cases lo-paMMR. Among the 13 dMMR, 12 were MSI-H and only 1 was MSS. All six lo-paMMR cases were MSS. All NGS results were in agreement with PCR. Conclusions: In clinical practice, MMR–IHC could be used as a screening test and additional molecular analysis is mandatory exclusively in cases carrying loss/patchy MMR-IHC.

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