AUTHOR=Nawrocka Paulina Maria , Galka-Marciniak Paulina , Urbanek-Trzeciak Martyna Olga , M-Thirusenthilarasan Ilamathi , Szostak Natalia , Philips Anna , Susok Laura , Sand Michael , Kozlowski Piotr 

TITLE=Profile of Basal Cell Carcinoma Mutations and Copy Number Alterations - Focus on Gene-Associated Noncoding Variants

JOURNAL=Frontiers in Oncology

VOLUME=11

YEAR=2021

URL=https://www.frontiersin.org/journals/oncology/articles/10.3389/fonc.2021.752579

DOI=10.3389/fonc.2021.752579

ISSN=2234-943X

ABSTRACT=<p>Basal cell carcinoma (BCC) of the skin is the most common cancer in humans, characterized by the highest mutation rate among cancers, and is mostly driven by mutations in genes involved in the hedgehog pathway. To date, almost all BCC genetic studies have focused exclusively on protein-coding sequences; therefore, the impact of noncoding variants on the BCC genome is unrecognized. In this study, with the use of whole-exome sequencing of 27 tumor/normal pairs of BCC samples, we performed an analysis of somatic mutations in both protein-coding sequences and gene-associated noncoding regions, including 5’UTRs, 3’UTRs, and exon-adjacent intron sequences. Separately, in each region, we performed hotspot identification, mutation enrichment analysis, and cancer driver identification with OncodriveFML. Additionally, we performed a whole-genome copy number alteration analysis with GISTIC2. Of the &gt;80,000 identified mutations, ~50% were localized in noncoding regions. The results of the analysis generally corroborated the previous findings regarding genes mutated in coding sequences, including <italic>PTCH1</italic>, <italic>TP53</italic>, and <italic>MYCN</italic>, but more importantly showed that mutations were also clustered in specific noncoding regions, including hotspots. Some of the genes specifically mutated in noncoding regions were identified as highly potent cancer drivers, of which <italic>BAD</italic> had a mutation hotspot in the 3’UTR, <italic>DHODH</italic> had a mutation hotspot in the Kozak sequence in the 5’UTR, and <italic>CHCHD2</italic> frequently showed mutations in the 5’UTR. All of these genes are functionally implicated in cancer-related processes (e.g., apoptosis, mitochondrial metabolism, and <italic>de novo</italic> pyrimidine synthesis) or the pathogenesis of UV radiation-induced cancers. We also found that the identified <italic>BAD</italic> and <italic>CHCHD2</italic> mutations frequently occur in melanoma but not in other cancers <italic>via</italic> The Cancer Genome Atlas analysis. Finally, we identified a frequent deletion of chr9q, encompassing <italic>PTCH1</italic>, and unreported frequent copy number gain of chr9p, encompassing the genes encoding the immune checkpoint ligands PD-L1 and PD-L2. In conclusion, this study is the first systematic analysis of coding and noncoding mutations in BCC and provides a strong basis for further analyses of the variants in BCC and cancer in general.</p>