High mutational burden in colorectal carcinomas with monoallelic POLE mutations: absence of allelic loss and gene promoter methylation

Maja Hühns; Sylvia Nürnberg; Krishna Kumar Kandashwamy; Claudia Maletzki; Peter Bauer; Friedrich Prall

doi:10.1038/s41379-019-0430-6

High mutational burden in colorectal carcinomas with monoallelic POLE mutations: absence of allelic loss and gene promoter methylation

Mod Pathol. 2020 Jun;33(6):1220-1231. doi: 10.1038/s41379-019-0430-6. Epub 2019 Dec 19.

Authors

Maja Hühns¹, Sylvia Nürnberg², Krishna Kumar Kandashwamy², Claudia Maletzki³, Peter Bauer², Friedrich Prall⁴

Affiliations

¹ Institute of Pathology, University Medicine of Rostock, Strempelstraße 14, 18057, Rostock, Germany.
² Centogene AG, Am Strande 7, 18055, Rostock, Germany.
³ Clinic for Hematology, Oncology and Palliative Care, University Medical Center Rostock, University of Rostock, Ernst-Heydemann-Strasse 6, 18057, Rostock, Germany.
⁴ Institute of Pathology, University Medicine of Rostock, Strempelstraße 14, 18057, Rostock, Germany. friedrich.prall@med.uni-rostock.de.

PMID: 31857678
DOI: 10.1038/s41379-019-0430-6

Abstract

Hypermutator-type colorectal carcinomas are microsatellite-stable and have point mutations of the exonuclease domain of the DNA polymerase ε or δ genes (POLE and POLD1, respectively), and an ultrahigh tumor mutational burden (TMB). These tumors may be associated with enhanced antitumor immunity and preferentially afflict younger patients, but this notion awaits validation by accrual of further cases for detailed correlative phenotypic and molecular study. We performed POLE and POLD1 exonuclease domain Sanger sequencing of 271 unselected colorectal carcinomas. We identified two microsatellite-stable tumors with somatic POLE p.P286R variants, both with ultrahigh TMBs as demonstrated by whole exome sequencing. A POLE p.V411L was found in another two microsatellite-stable tumors with ultrahigh TMBs. Two of these four tumors were from young patients (<50 years old, nonsyndromic), and there was seen a prominent T-cell infiltration in three of them. Furthermore, a somatic POLE p.A465T was found in a Lynch-associated tumor, which, hypothetically, might have enhanced TMB (which was the highest of all). In two tumors, a somatic POLE p.V411L and a POLD1 p.E279K, respectively, were found only focally, and TMBs were low. It is commonly assumed that compromise of one allele is sufficient, but this has not been specifically addressed. Therefore, resequencing of the POLE or POLD1 mutations was done with DNA from tumor cells isolated by laser-capture microdissection. This demonstrated that the mutations were monoallelic, and there was no evidence of a "second hit", neither by allelic loss (allelotyping with polymorphic microsatellite markers), nor by promoter methylation (Pyromark CpG assays). Taken together, including at least the more common DNA polymerase mutations in NGS panels allows for straightforward identification of hypermutator-type colorectal carcinomas which often may be "immunoreactive". This is important at least in young patients or when a metastasizing stage of disease has been reached and immune-checkpoint therapy enters deliberation.

MeSH terms

Adult
Aged
Aged, 80 and over
Alleles
Colorectal Neoplasms / genetics*
Colorectal Neoplasms / pathology
DNA Methylation
DNA Mutational Analysis
DNA Polymerase II / genetics*
DNA Polymerase III / genetics*
Female
Humans
Loss of Heterozygosity*
Male
Middle Aged
Mutation*
Poly-ADP-Ribose Binding Proteins / genetics*
Promoter Regions, Genetic*
Young Adult

Substances

Poly-ADP-Ribose Binding Proteins
POLD1 protein, human
DNA Polymerase II
DNA Polymerase III
POLE protein, human