Whole exome sequencing reveals novel risk genes of pituitary neuroendocrine tumors

Author:

Peculis RaitisORCID,Rovite Vita,Megnis KasparsORCID,Balcere Inga,Breiksa Austra,Nazarovs Jurijs,Stukens Janis,Konrade Ilze,Sokolovska Jelizaveta,Pirags Valdis,Klovins JanisORCID

Abstract

Somatic genetic alterations in pituitary neuroendocrine tumors (PitNET) tissues have been identified in several studies, but detection of overlapping somatic PitNET candidate genes is rare. We sequenced and by employing multiple data analysis methods studied the exomes of 15 PitNET patients to improve discovery of novel factors involved in PitNET development. PitNET patients were recruited to the study before PitNET removal surgery. For each patient, two samples for DNA extraction were acquired: venous blood and PitNET tissue. Exome sequencing was performed using Illumina NexSeq 500 sequencer and data analyzed using two separate workflows and variant calling algorithms: GATK and Strelka2. A combination of two data analysis pipelines discovered 144 PitNET specific somatic variants (mean = 9.6, range 0–19 per PitNET) of which all were SNVs. Also, we detected previously knownGNASPitNET mutation and identified somatic variants in 11 genes, which have contained somatic variants in previous WES and WGS studies of PitNETs. Noteworthy, this is the third study detecting somatic variants in geneRYR1in the exomes of PitNETs. In conclusion, we have identified two novel PitNET candidate genes (AC002519.6andAHNAK) with recurrent somatic variants in our PitNET cohort and found 13 genes overlapping from previous PitNET studies that contain somatic variants. Our study demonstrated that the use of multiple sequencing data analysis pipelines can provide more accurate identification of somatic variants in PitNETs.

Funder

European Regional Development Fund

Publisher

Public Library of Science (PLoS)

Subject

Multidisciplinary

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