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High frequency of mutations seems to determine a higher occurrence of neoepitope formation and, thus, tumor immunogenicity. A somatic hypermutated status could thus act as a predictive biomarker of responsiveness to immunotherapy with recent immune checkpoint inhibitors. Among several factors involved in determining the hypermutated status, such as inactivating mutations in the DNA polymerases as well as exposure to external (cigarette smoke, UV radiation, chemicals) and endogenous (reactive oxygen species) mutagens, a defective DNA mismatch repair system may give rise to genetic instability and, particularly, to microsatellite instability (MSI). The occurrence of MSI has been associated with increased load of mutations and expression of abundant peptides that serve as neoantigens to elicit an immune response within a context of a favorable tumor microenvironment. Here we describe methodological strategies to investigate for the presence of the MSI phenotype in cancer samples, through a combination of molecular approaches performed on paraffin-embedded tissues.

Genetic Instability Markers in Cancer / Palmieri, G.; Casula, M.; Manca, A.; Palomba, G.; Sini, M. C.; Doneddu, V.; Cossu, A.; Colombino, M.. - 2055:(2020), pp. 133-154. [10.1007/978-1-4939-9773-2_6]

Genetic Instability Markers in Cancer

Palmieri G.;Doneddu V.;Cossu A.;
2020-01-01

Abstract

High frequency of mutations seems to determine a higher occurrence of neoepitope formation and, thus, tumor immunogenicity. A somatic hypermutated status could thus act as a predictive biomarker of responsiveness to immunotherapy with recent immune checkpoint inhibitors. Among several factors involved in determining the hypermutated status, such as inactivating mutations in the DNA polymerases as well as exposure to external (cigarette smoke, UV radiation, chemicals) and endogenous (reactive oxygen species) mutagens, a defective DNA mismatch repair system may give rise to genetic instability and, particularly, to microsatellite instability (MSI). The occurrence of MSI has been associated with increased load of mutations and expression of abundant peptides that serve as neoantigens to elicit an immune response within a context of a favorable tumor microenvironment. Here we describe methodological strategies to investigate for the presence of the MSI phenotype in cancer samples, through a combination of molecular approaches performed on paraffin-embedded tissues.
2020
Inglese
Thurin M., Cesano A., Marincola F.
2055
Methods in Molecular Biology
133
154
22
978-1-4939-9772-5
978-1-4939-9773-2
Humana Press Inc.
Defective mismatch repair; Microsatellite instability; Response to immunotherapy; Animals; Antigens, Neoplasm; Biomarkers, Tumor; Humans; Immunohistochemistry; Mutation; Neoplasms; Paraffin Embedding; Polymerase Chain Reaction; Tumor Microenvironment; Microsatellite Instability
2-s2.0-85071991645
MEDLINE:31502150
No
info:eu-repo/semantics/bookPart
Palmieri, G.; Casula, M.; Manca, A.; Palomba, G.; Sini, M. C.; Doneddu, V.; Cossu, A.; Colombino, M.
2 Contributo in Volume::2.1 Contributo in volume (Capitolo o Saggio)
8
268
Genetic Instability Markers in Cancer / Palmieri, G.; Casula, M.; Manca, A.; Palomba, G.; Sini, M. C.; Doneddu, V.; Cossu, A.; Colombino, M.. - 2055:(2020), pp. 133-154. [10.1007/978-1-4939-9773-2_6]
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Utilizza questo identificativo per citare o creare un link a questo documento: https://hdl.handle.net/11388/241185
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