Whole-genome sequencing of follicular thyroid carcinomas reveal recurrent mutations in microRNA processing subunit DGCR8

SND-ID: 2021-108-1. Version: 1. DOI: https://doi.org/10.5878/6fcv-1795

Associated documentation

Citation

Creator/Principal investigator(s)

Christofer Juhlin - Karolinska Institutet, Department of Oncology-Pathology orcid

Johan Paulsson - Karolinska Institutet, Department of Oncology-Pathology

Research principal

Karolinska Institutet - Department of Oncology-Pathology rorId

Description

Data availability
This dataset can only be shared within Sweden due to legal restrictions.

Background
The genomic and transcriptomic landscape of widely invasive follicular thyroid carcinomas (wiFTCs) is poorly characterized, and a large subset of these tumours lack information on credible genetic driver events. The aim of this study was to bridge this gap.
Methods
We performed whole-genome and RNA sequencing and subsequent bioinformatic analyses of 13 wiFTCs with a particularly poor prognosis, and matched normal tissue.
Results
Ten out of thirteen (77%) tumours exhibited one or several mutations in established genes ranked as the top 20 mutated in thyroid cancer, including TERT (n=4), NRAS (n=3), HRAS, KRAS, AKT, PTEN, PIK3CA, MUTYH and MEN1 (n=1 each). Recurrent somatic mutations in three genes were annotated as significant according to MutSig2CV: FAM72D (n=3), TP53 (n=3) and EIF1AX (n=3), with DGCR8 (n=2) as borderline significant. Of interest, both DGCR8 mutations were recurrent p.E518K missense alterations, a mutation known to cause familial multinodular goiter (MNG) via disruption of m

... Show more..
Data availability
This dataset can only be shared within Sweden due to legal restrictions.

Background
The genomic and transcriptomic landscape of widely invasive follicular thyroid carcinomas (wiFTCs) is poorly characterized, and a large subset of these tumours lack information on credible genetic driver events. The aim of this study was to bridge this gap.
Methods
We performed whole-genome and RNA sequencing and subsequent bioinformatic analyses of 13 wiFTCs with a particularly poor prognosis, and matched normal tissue.
Results
Ten out of thirteen (77%) tumours exhibited one or several mutations in established genes ranked as the top 20 mutated in thyroid cancer, including TERT (n=4), NRAS (n=3), HRAS, KRAS, AKT, PTEN, PIK3CA, MUTYH and MEN1 (n=1 each). Recurrent somatic mutations in three genes were annotated as significant according to MutSig2CV: FAM72D (n=3), TP53 (n=3) and EIF1AX (n=3), with DGCR8 (n=2) as borderline significant. Of interest, both DGCR8 mutations were recurrent p.E518K missense alterations, a mutation known to cause familial multinodular goiter (MNG) via disruption of microRNA (miRNA) processing. Expression analyses pinpointed a trend towards reduced DGCR8 mRNA expression in FTCs in general. Copy number analyses revealed recurrent gains of loci on chromosomes 4, 6 and 10, and fusion gene analyses revealed 27 high-quality events. Based on the transcriptome data FTCs clustered in two principal clusters, displaying significant differences in expression of genes associated with metabolic pathways.
Conclusion
In summary, we describe the genomic and transcriptomic landscape in wiFTCs and identify novel recurrent mutations and copy number alterations with possible driver properties and lay the foundation for future studies.

The dataset consists of tables and lists containing underlying data, and supplementary figures for a manuscript submitted to "Journal of Clinical Endocrinology & Metabolism". It includes 8 tables and 3 figures:

File name: T1_Detailed-characteristics-of-the-study-cohort.csv
Contains "Table 1: Detailed characteristics of the study cohort." 

File name: T2_List-of-Somatic-SNVs.csv
Contains "Table 2: List of Somatic SNV's (Small nucleotide variants)." 

File name: T3_MutSig2CV-input-genes.csv
Contains "Table 3: MutSig2CV input genes." 

File name: T4_MutSig2CV-genes-ranked-by-p-value.csv
Contains "Table 4: MutSig2CV genes ranked by p-value."

File name: T5_Genes-in-copy-number-altered-minimal-region-of-amplification.csv
Contains "Table 5: List of genes in copy number altered minimal region of amplification." 

File name: T6_Aberrant-cell-fraction-and-ploidy-as-determined-by-ASCAT.csv
Contains "Table 6: Aberrant cell fraction and ploidy as determined by ASCAT." 

File name: T7_High-confidence-structural-variations-in-the-tumor-cohort.csv
Contains "Table 7: List of high-confidence structural variations in the tumor cohort." 

File name: T8_Significant-differentially-expressed-genes-in-tumor-vs-normal-thyroid.csv
Contains "Table 8: List of significant differentially expressed genes in tumor versus normal thyroid."

File name: List_of_variables.pdf
Contains List of variables: Metadata and abbreviation explanations for Table 1-8.

File name: Whole-genome-sequencing-follicular-thyroid-carcinomas_Figures.pdf
Contains Supplementary Figure S1-S3:
- Supplementary Figure S1: Somatic mutational overview in the WGS cohort. 
- Supplementary Figure S2: Normalized DGCR8 mRNA expression in tumours with or without loss of heterozygosity (LOH) of the DGCR8 locus. 
- Supplementary Figure S3: a Gene set enrichment analysis (GSEA). Show less..

Data contains personal data

Yes

Sensitive personal data

Yes

Code key exists

Yes

Language

Method and outcome

Population

The study included 13 patients with follicular thyroid carcinoma. All diagnosed at the Karolinska University Hospital, Stockholm.

Study design

Experimental study

Description of study design

Whole-genome and RNA sequencing of 13 tumor and normal tissue pairs.

Biobank is connected to the study

This study has used existing samples from a scientific collection or biobank

Scientific collection or biobank name: KI Biobank

Type(s) of sample: tumor tissue

Number of individuals/objects

13

Data format / data structure

Data collection
  • Mode of collection: Measurements and tests
  • Source of the data: Biological samples
Geographic coverage

Geographic spread

Geographic location: Sweden

Administrative information

Responsible department/unit

Department of Oncology-Pathology

Contributor(s)

Sebastian DiLorenzo - Uppsala University, Department of Medical Biochemistry and Microbiology / Department of Cell and Molecular Biology

Jan Zedenius - Karolinska Institutet, Department of Molecular Medicine and Surgery orcid

Felix Haglund - Karolinska Institutet, Department of Oncology-Pathology

Yi Chen - Karolinska Institutet, Department of Oncology-Pathology

Nima Rafati - Uppsala University, Department of Medical Biochemistry and Microbiology / Department of Cell and Molecular Biology

Ethics Review

Stockholm - Ref. Dnr 2015/959-31

Topic and keywords

Research area

Genetics (Standard för svensk indelning av forskningsämnen 2011)

Medical genetics (Standard för svensk indelning av forskningsämnen 2011)

Cell and molecular biology (Standard för svensk indelning av forskningsämnen 2011)

Cancer and oncology (Standard för svensk indelning av forskningsämnen 2011)

Endocrinology and diabetes (Standard för svensk indelning av forskningsämnen 2011)

Surgery (Standard för svensk indelning av forskningsämnen 2011)

Publications

Paulsson, J. O., Rafati, N., DiLorenzo, S., Chen, Y., Haglund, F., Zedenius, J., & Juhlin, C. C. (n.d.). Whole-genome Sequencing of Follicular Thyroid Carcinomas Reveal Recurrent Mutations in MicroRNA Processing Subunit DGCR8. In Journal of Clinical Endocrinology and Metabolism (Vol. 106, Issue 11, pp. 3265–3282). https://doi.org/10.1210/clinem/dgab471
DOI: https://doi.org/10.1210/clinem/dgab471
SwePub: oai:DiVA.org:uu-459861

If you have published anything based on these data, please notify us with a reference to your publication(s). If you are responsible for the catalogue entry, you can update the metadata/data description in DORIS.

Versions

Version 1. 2021-06-24

Version 1: 2021-06-24

DOI: https://doi.org/10.5878/6fcv-1795

Contact for questions about the data

Johan Paulsson

johan.paulsson@ki.se

This resource has the following relations

Published: 2021-06-24
Last updated: 2024-07-04