Comprehensive Analysis of Juvenile Nasopharyngeal Angiofibromas via Whole Exome Sequencing

Author:

Kumari Kiran,Afroj Shariya,Madhry Deeksha,Verma Yash,Kairo Arvind K.,Thakar Alok,Sikka Kapil,Verma Hitesh,Verma BhupendraORCID

Abstract

ABSTRACTObjectivesThe molecular basis and mechanisms of Juvenile Nasopharyngeal Angiofibromas (JNA) pathogenesis are still unknown. Despite being a rare and benign neoplasm, JNA is a locally aggressive and potentially destructive neoplasm among head and neck tumors, typically diagnosed in young males. The advancement of genome technologies and analytical tools has provided an unparalleled opportunity to explore the intricacy of JNA. The present study provides the first evidence of the involvement of chromosome Y genes in JNA.MethodsThirteen JNA patients at an advanced disease stage and 5 age-matched male controls were registered for this study. Whole-exome sequencing (WES) analysis was conducted followed by functional analysis to understand the molecular mechanism of the JNA.ResultsWES analysis revealed a high prevalence of mutations in 14 genes within the protein-coding, Male-Specific Region of the Y-chromosome of young males (mean age: 13.8 ± 2.4) with JNA. These mutations, occurring at 28 distinct positions, were characterized as moderate to high impact and were prevalent in 9 JNA patients but not in the control group. The most frequently mutated genes were USP9Y and UTY, followed by KDM5D, DDX3Y and TSPY4. The expression of USP9Y, UTY and DDX3Y was found to be co-modulated, implying their coordinated regulation as a complex. Furthermore, somatic mutations were detected in genes previously linked to JNA.ConclusionThe wide array of genetic and somatic mutations identified in JNA provides novel insight into JNA pathophysiology.

Publisher

Cold Spring Harbor Laboratory

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