Flexible lab-tailored cut-offs for suitability of formalin-fixed tumor samples for diagnostic mutational analyses.
The selection of proper tissues from formalin-fixed and paraffin-embedded tumors before diagnostic molecular testing is responsibility of the pathologist and represents a crucial step to produce reliable test results. The international guidelines suggest two cut-offs, one for the percentage and one...
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doaj-d88a50c3fd0142b5bfa94eeffd51c0d52020-11-25T02:04:38ZengPublic Library of Science (PLoS)PLoS ONE1932-62032015-01-01104e012181510.1371/journal.pone.0121815Flexible lab-tailored cut-offs for suitability of formalin-fixed tumor samples for diagnostic mutational analyses.Sara MarianiCristiana Di BelloLisa BonelloFabrizio TondatDonatella PacchioniLuca MolinaroAntonella BarrecaLuigia MacrìLuigi ChiusaPaola Francia di CellePaola CassoniAnna SapinoThe selection of proper tissues from formalin-fixed and paraffin-embedded tumors before diagnostic molecular testing is responsibility of the pathologist and represents a crucial step to produce reliable test results. The international guidelines suggest two cut-offs, one for the percentage and one for the number of tumor cells, in order to enrich the tumor content before DNA extraction. The aim of the present work was two-fold: to evaluate to what extent a low percentage or absolute number of tumor cells can be qualified for somatic mutation testing; and to determine how assay sensitivities can guide pathologists towards a better definition of morphology-based adequacy cut-offs. We tested 1797 tumor specimens from melanomas, colorectal and lung adenocarcinomas. Respectively, their BRAF, K-RAS and EGFR genes were analyzed at specific exons by mutation-enriched PCR, pyrosequencing, direct sequencing and real-time PCR methods. We demonstrate that poorly cellular specimens do not modify the frequency distribution of either mutated or wild-type DNA samples nor that of specific mutations. This observation suggests that currently recommended cut-offs for adequacy of specimens to be processed for molecular assays seem to be too much stringent in a laboratory context that performs highly sensitive routine analytical methods. In conclusion, new cut-offs are needed based on test sensitivities and documented tumor heterogeneity.http://europepmc.org/articles/PMC4386759?pdf=render |
collection |
DOAJ |
language |
English |
format |
Article |
sources |
DOAJ |
author |
Sara Mariani Cristiana Di Bello Lisa Bonello Fabrizio Tondat Donatella Pacchioni Luca Molinaro Antonella Barreca Luigia Macrì Luigi Chiusa Paola Francia di Celle Paola Cassoni Anna Sapino |
spellingShingle |
Sara Mariani Cristiana Di Bello Lisa Bonello Fabrizio Tondat Donatella Pacchioni Luca Molinaro Antonella Barreca Luigia Macrì Luigi Chiusa Paola Francia di Celle Paola Cassoni Anna Sapino Flexible lab-tailored cut-offs for suitability of formalin-fixed tumor samples for diagnostic mutational analyses. PLoS ONE |
author_facet |
Sara Mariani Cristiana Di Bello Lisa Bonello Fabrizio Tondat Donatella Pacchioni Luca Molinaro Antonella Barreca Luigia Macrì Luigi Chiusa Paola Francia di Celle Paola Cassoni Anna Sapino |
author_sort |
Sara Mariani |
title |
Flexible lab-tailored cut-offs for suitability of formalin-fixed tumor samples for diagnostic mutational analyses. |
title_short |
Flexible lab-tailored cut-offs for suitability of formalin-fixed tumor samples for diagnostic mutational analyses. |
title_full |
Flexible lab-tailored cut-offs for suitability of formalin-fixed tumor samples for diagnostic mutational analyses. |
title_fullStr |
Flexible lab-tailored cut-offs for suitability of formalin-fixed tumor samples for diagnostic mutational analyses. |
title_full_unstemmed |
Flexible lab-tailored cut-offs for suitability of formalin-fixed tumor samples for diagnostic mutational analyses. |
title_sort |
flexible lab-tailored cut-offs for suitability of formalin-fixed tumor samples for diagnostic mutational analyses. |
publisher |
Public Library of Science (PLoS) |
series |
PLoS ONE |
issn |
1932-6203 |
publishDate |
2015-01-01 |
description |
The selection of proper tissues from formalin-fixed and paraffin-embedded tumors before diagnostic molecular testing is responsibility of the pathologist and represents a crucial step to produce reliable test results. The international guidelines suggest two cut-offs, one for the percentage and one for the number of tumor cells, in order to enrich the tumor content before DNA extraction. The aim of the present work was two-fold: to evaluate to what extent a low percentage or absolute number of tumor cells can be qualified for somatic mutation testing; and to determine how assay sensitivities can guide pathologists towards a better definition of morphology-based adequacy cut-offs. We tested 1797 tumor specimens from melanomas, colorectal and lung adenocarcinomas. Respectively, their BRAF, K-RAS and EGFR genes were analyzed at specific exons by mutation-enriched PCR, pyrosequencing, direct sequencing and real-time PCR methods. We demonstrate that poorly cellular specimens do not modify the frequency distribution of either mutated or wild-type DNA samples nor that of specific mutations. This observation suggests that currently recommended cut-offs for adequacy of specimens to be processed for molecular assays seem to be too much stringent in a laboratory context that performs highly sensitive routine analytical methods. In conclusion, new cut-offs are needed based on test sensitivities and documented tumor heterogeneity. |
url |
http://europepmc.org/articles/PMC4386759?pdf=render |
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