POLE (DNA polymerase epsilon, catalytic subunit)

2018-05-01 Enric Domingo Affiliation

\\\/ e-Mail Department of Oncology, University of Oxford, Oxford, United Kingdom \\\/ enric.domingo@oncology.ox.ac.uk

Identity

HGNC

POLE

LOCATION

12q24.33

LOCUSID

5426

ALIAS

CRCS12,FILS,IMAGEI,POLE1

DNA/RNA

Description

POLE gene is 63.6 kb long and composed of 49 coding exons, where the first and last one also have a UTR region.

Transcription

The length of the transcript is 7840 bp and results in a protein of 2286 residues.

Proteins

Description

The POLE gene encodes for one of the four subunits that form Polε (DNA polymerase epsilon) together with POLE2, POLE3 and POLE4 genes. This protein is one of the main DNA replicases in eukaryotes and is responsible of the replication of the leading strand. POLE contains both the catalytic active site and the proofreading exonuclease domain (residues 223-517). Accordingly, the POLE gene confers to Polε both replicative and 3 to 5 repair capabilities for the new strand.

Expression

Broadly expressed.

Localisation

Nuclear.

Function

Polε is responsible of the polymerization of the leading strand during DNA replication in yeast and humans. It also possesses 3 to 5 exonuclease capability to repair missincorporated nucleotides during DNA replication. Polε is also involved in DNA repair pathways such as mismatch repair (MMR), base excision repair (BER), nucleotide excision repair (NER) or double-strand break repair.

Mutations

Germinal

A few missense germline mutations in the proofreading domain of POLE have been shown to be pathogenic such as W347C, N363K, D368V, L424V, P436S or Y458F. These are quite rare in the population although for unclear reasons they are more common than similar germline mutations in the polymerase gene POLD1. These mutations affect the exonuclease repair of Polε hence resulting in a mutation rate increase of about 100-fold. Accordingly, these tumours are usually called ultramutated.

Somatic

Pathogenic somatic mutations in the proofreading domain of POLE have been found in some tumour types at moderate or rare frequencies. Some mutations in the polymerase domain have been suggested to be drivers but further research is required to validate these results.

Implicated in

Entity name

Different human sporadic cancers

Note

Somatic pathogenic mutations in the proofreading domain of POLE have been found in 8% of endometrial tumours and at lower frequencies in other tumour types such as colorectal, glioblastoma, ovary, prostate, breast or gastric cancer. These mutations seem to confer similar phenotypes regardless of the tumour tissue type. These are missense, heterozygous mutations where no second hit by either mutation or LOH seem to be required, and they are very early events, possibly initiating. Some mutations are hotspots such as P286R, S297F, V411L or S459F but other rarer mutations have also been identified (eg P286H/L, S297Y, F367S, L424V/I, P436R, M444K, A456P). These mutations affect the proofreading of the protein resulting in ultramutation with an overrepresentation of C>A. More specifically, POLE tumours have mutational signature 10 as reported by Alexandrov et al, with extremely prominent TCG>TTG and TCT>TAT substitutions and transcriptional strand bias. As a result, there is an overrepresentation of some specific missense mutations and nonsense mutations. In addition, it may explain why some cancer driver genes in POLE tumours tend to show mutations otherwise relatively uncommon such as R213X in TP53 or R88Q in PIK3CA. POLE tumours are hardly ever concomitant with microsatellite instability, although a few tumours with both phenotypes have been described, and do not seem to show chromosomal instability as their karyotype is nearly diploid.

Disease

Patients with somatic POLE driver mutations are younger on average, although they have a broad range of ages. For colorectal cancer, most mutations are right-sided so they are relatively rare in rectal cancer.

Prognosis

POLE tumours in endometrial cancer, colorectal cancer and glioblastoma show excellent prognosis in early disease. Similar patterns are expected in any other tumour type although it is not formally proven due to the low frequency of these mutations. Such good prognosis is because of very high immunogenicity with upregulation of immune checkpoint and other immunosuppressive genes. Accordingly, POLE proofreading pathogenic mutation is also a promising candidate biomarker for checkpoint blockade immunotherapy. They may also be sensitive to treatment with nucleoside analogs as they increase the mutation burden to a level where tumour cells are not viable.

Entity name

Proofreading-associated polyposis (PPAP)

Disease

Autosomal dominant disease with high risk for endometrial and/or colorectal adenoma or carcinoma due to germline mutations in POLE or POLD1 genes.

Prognosis

Probably good prognosis in early disease as found with POLE somatic mutations, although not formally proven. Similarly, these patients are likely to respond to checkpoint blockade immunotherapy.

Article Bibliography

Pubmed ID	Last Year	Title	Authors
23945592	2013	Signatures of mutational processes in human cancer.	Alexandrov LB et al
26133394	2016	POLE and POLD1 mutations in 529 kindred with familial colorectal cancer and/or polyposis: review of reported cases and recommendations for genetic testing and surveillance.	Bellido F et al
29056344	2017	Comprehensive Analysis of Hypermutation in Human Cancer.	Campbell BB et al
23528559	2013	DNA polymerase ε and δ exonuclease domain mutations in endometrial cancer.	Church DN et al
25505230	2015	Prognostic significance of POLE proofreading mutations in endometrial cancer.	Church DN et al
28404093	2016	Somatic POLE proofreading domain mutation, immune response, and prognosis in colorectal cancer: a retrospective, pooled biomarker study.	Domingo E et al
28344870	2017	Immunological profiling of molecularly classified high-risk endometrial cancers identifies POLE-mutant and microsatellite unstable carcinomas as candidates for checkpoint inhibition.	Eggink FA et al
25740784	2015	Somatic POLE mutations cause an ultramutated giant cell high-grade glioma subtype with better prognosis.	Erson-Omay EZ et al
24583393	2014	Replicative DNA polymerase mutations in cancer.	Heitzer E et al
27683556	2016	Immunogenomics of Hypermutated Glioblastoma: A Patient with Germline POLE Deficiency Treated with Checkpoint Blockade Immunotherapy.	Johanns TM et al
23263490	2013	Germline mutations affecting the proofreading domains of POLE and POLD1 predispose to colorectal adenomas and carcinomas.	Palles C et al
26822575	2016	A panoply of errors: polymerase proofreading domain mutations in cancer.	Rayner E et al
29604063	2018	Somatic POLE exonuclease domain mutations are early events in sporadic endometrial and colorectal carcinogenesis, determining driver mutational landscape, clonal neoantigen burden and immune response.	Temko D et al
24501277	2014	New insights into POLE and POLD1 germline mutations in familial colorectal cancer and polyposis.	Valle L et al
29559562	2018	Adjuvant Treatment for POLE Proofreading Domain-Mutant Cancers: Sensitivity to Radiotherapy, Chemotherapy, and Nucleoside Analogues.	Van Gool IC et al
27141333	2016	POLE proofreading mutation, immune response and prognosis in endometrial cancer.	van Gool IC et al

Other Information

Locus ID:

NCBI: 5426
MIM: 174762
HGNC: 9177
Ensembl: ENSG00000177084

Variants:

dbSNP: 5426
ClinVar: 5426
TCGA: ENSG00000177084
COSMIC: POLE

RNA/Proteins

Gene ID	Transcript ID	Uniprot
ENSG00000177084	ENST00000320574	Q07864
ENSG00000177084	ENST00000441786	A0A087WX51
ENSG00000177084	ENST00000535270	F5H1D6
ENSG00000177084	ENST00000537064	F5H7E4
ENSG00000177084	ENST00000544870	A0A087WW42

Expression (GTEx)

Adipose - Subcutaneous

Adipose - Visceral

Adrenal Gland

Artery - Aorta

Artery - Tibial

Bladder

Brain - Amygdala

Brain - Anterior cingulate cortex

Brain - Caudate

Brain - Cerebellar Hemisphere

Brain - Cerebellum

Brain - Cortex

Brain - Frontal Cortex

Brain - Hippocampus

Brain - Hypothalamus

Brain - Nucleus accumbens

Brain - Putamen

Brain - Spinal cord

Brain - Substantia nigra

Breast - Mammary Tissue

Cells - Cultured fibroblasts

Cells - EBV - transformed lymphocytes

Cervix - Ectocervix

Cervix - Endocervix

Colon - Sigmoid

Colon - Transverse

Esophagus - Gastroesophageal Junction

Esophagus - Mucosa

Esophagus - Muscularis

Fallopian Tube

Heart - Atrial Appendage

Heart - Left Ventricle

Kidney - Cortex

Kidney - Medulla

Liver

Lung

Minor Salivary Gland

Muscle - Skeletal

Nerve - Tibial

Ovary

Pancreas

Pituitary

Prostate

Skin - Not Sun Exposed

Skin - Sun Exposed

Small Intestine - Terminal Ileum

Spleen

Stomach

Testis

Thyroid

Uterus

Vagina

Whole Blood

Pathways

Pathway	Source	External ID
Purine metabolism	KEGG	ko00230
Pyrimidine metabolism	KEGG	ko00240
DNA replication	KEGG	ko03030
Base excision repair	KEGG	ko03410
Nucleotide excision repair	KEGG	ko03420
Purine metabolism	KEGG	hsa00230
Pyrimidine metabolism	KEGG	hsa00240
DNA replication	KEGG	hsa03030
Base excision repair	KEGG	hsa03410
Nucleotide excision repair	KEGG	hsa03420
Metabolic pathways	KEGG	hsa01100
HTLV-I infection	KEGG	ko05166
HTLV-I infection	KEGG	hsa05166
DNA polymerase epsilon complex	KEGG	hsa_M00263
DNA polymerase epsilon complex	KEGG	M00263
Cell Cycle	REACTOME	R-HSA-1640170
Cell Cycle, Mitotic	REACTOME	R-HSA-69278
Mitotic G1-G1/S phases	REACTOME	R-HSA-453279
G1/S Transition	REACTOME	R-HSA-69206
Activation of the pre-replicative complex	REACTOME	R-HSA-68962
S Phase	REACTOME	R-HSA-69242
Synthesis of DNA	REACTOME	R-HSA-69239
DNA replication initiation	REACTOME	R-HSA-68952
M/G1 Transition	REACTOME	R-HSA-68874
DNA Replication Pre-Initiation	REACTOME	R-HSA-69002
Chromosome Maintenance	REACTOME	R-HSA-73886
Telomere Maintenance	REACTOME	R-HSA-157579
Extension of Telomeres	REACTOME	R-HSA-180786
Telomere C-strand (Lagging Strand) Synthesis	REACTOME	R-HSA-174417
Telomere C-strand synthesis initiation	REACTOME	R-HSA-174430
DNA Replication	REACTOME	R-HSA-69306
DNA Repair	REACTOME	R-HSA-73894
Base Excision Repair	REACTOME	R-HSA-73884
Resolution of Abasic Sites (AP sites)	REACTOME	R-HSA-73933
Resolution of AP sites via the multiple-nucleotide patch replacement pathway	REACTOME	R-HSA-110373
PCNA-Dependent Long Patch Base Excision Repair	REACTOME	R-HSA-5651801
DNA Damage Bypass	REACTOME	R-HSA-73893
Recognition of DNA damage by PCNA-containing replication complex	REACTOME	R-HSA-110314
Translesion synthesis by Y family DNA polymerases bypasses lesions on DNA template	REACTOME	R-HSA-110313
Termination of translesion DNA synthesis	REACTOME	R-HSA-5656169
DNA Double-Strand Break Repair	REACTOME	R-HSA-5693532
Homology Directed Repair	REACTOME	R-HSA-5693538
HDR through Homologous Recombination (HR) or Single Strand Annealing (SSA)	REACTOME	R-HSA-5693567
HDR through Homologous Recombination (HRR)	REACTOME	R-HSA-5685942
Nucleotide Excision Repair	REACTOME	R-HSA-5696398
Global Genome Nucleotide Excision Repair (GG-NER)	REACTOME	R-HSA-5696399
Dual Incision in GG-NER	REACTOME	R-HSA-5696400
Gap-filling DNA repair synthesis and ligation in GG-NER	REACTOME	R-HSA-5696397
Transcription-Coupled Nucleotide Excision Repair (TC-NER)	REACTOME	R-HSA-6781827
Dual incision in TC-NER	REACTOME	R-HSA-6782135
Gap-filling DNA repair synthesis and ligation in TC-NER	REACTOME	R-HSA-6782210

References

Pubmed ID	Year	Title	Citations
37891003	2024	Exploring the basis of heterogeneity of cancer aggressiveness among the mutated POLE variants.	2
38148087	2024	Cervical Cytology Preserves Histologically Detected Surface Epithelial Slackening, Unique to the POLE Mutation-subtype in Endometrial Cancer.	0
38219146	2024	DNA polymerase ε and δ variants drive mutagenesis in polypurine tracts in human tumors.	1
38231514	2024	Race, Prevalence of POLE and POLD1 Alterations, and Survival Among Patients With Endometrial Cancer.	0
38238314	2024	The P286R mutation of DNA polymerase ε activates cancer-cell-intrinsic immunity and suppresses endometrial tumorigenesis via the cGAS-STING pathway.	2
38282550	2024	Exploring Co-occurring POLE Exonuclease and Non-exonuclease Domain Mutations and Their Impact on Tumor Mutagenicity.	1
37891003	2024	Exploring the basis of heterogeneity of cancer aggressiveness among the mutated POLE variants.	2
38148087	2024	Cervical Cytology Preserves Histologically Detected Surface Epithelial Slackening, Unique to the POLE Mutation-subtype in Endometrial Cancer.	0
38219146	2024	DNA polymerase ε and δ variants drive mutagenesis in polypurine tracts in human tumors.	1
38231514	2024	Race, Prevalence of POLE and POLD1 Alterations, and Survival Among Patients With Endometrial Cancer.	0
38238314	2024	The P286R mutation of DNA polymerase ε activates cancer-cell-intrinsic immunity and suppresses endometrial tumorigenesis via the cGAS-STING pathway.	2
38282550	2024	Exploring Co-occurring POLE Exonuclease and Non-exonuclease Domain Mutations and Their Impact on Tumor Mutagenicity.	1
36727290	2023	Cytopathological features associated with POLE mutation in endometrial cancer.	2
37990341	2023	Rare germline variants in POLE and POLD1 encoding the catalytic subunits of DNA polymerases ε and δ in glioma families.	0
36727290	2023	Cytopathological features associated with POLE mutation in endometrial cancer.	2

Citation

Enric Domingo

POLE (DNA polymerase epsilon, catalytic subunit)

Atlas Genet Cytogenet Oncol Haematol. 2018-05-01

Online version: http://atlasgeneticsoncology.org/gene/41773/favicon/js/lib/gene-fusions-explorer/