Publication:
Molecular Characterization of Muellerian Tumors of the Urinary Tract

dc.bibliographiccitation.firstpage880
dc.bibliographiccitation.issue6
dc.bibliographiccitation.journalGenes
dc.bibliographiccitation.volume12
dc.contributor.authorOrtiz-Brüchle, Nadina
dc.contributor.authorWucherpfennig, Sophie
dc.contributor.authorRose, Michael
dc.contributor.authorGarczyk, Stefan
dc.contributor.authorBertz, Simone
dc.contributor.authorHartmann, Arndt
dc.contributor.authorReis, Henning
dc.contributor.authorSzarvas, Tibor
dc.contributor.authorKiss, András
dc.contributor.authorGaisa, Nadine T.
dc.contributor.authorBremmer, Felix
dc.contributor.authorGolz, Reinhard
dc.contributor.authorKnüchel, Ruth
dc.date.accessioned2021-08-12T07:45:57Z
dc.date.available2021-08-12T07:45:57Z
dc.date.issued2021
dc.description.abstractIn the 2016 WHO classification of genitourinary tumors Muellerian tumors of the urinary tract (MTUT) comprise clear cell adenocarcinomas and endometrioid carcinomas. Since these rare tumors remained understudied, we aimed to characterize their molecular background by performing DNA- and RNA-based targeted panel sequencing. All tumors (n = 11) presented single nucleotide alterations (SNVs), with ARID1A mutations being the most prevalent (5/11, 45%). Besides frequent ARID1A mutations, loss of ARID1A protein is not a suitable marker since protein expression is (partly) preserved also in mutated cases. Copy number alterations (CNVs) were found in 64% of cases (7/11), exclusively gene amplifications. Interestingly, a functionally relevant RSPO2 gene fusion/microdeletion was discovered in the endometrioid adenocarcinoma case. Comparing our findings with mutational profiles of other tumor entities, absence of TERT promoter mutations argues for a non-urothelial origin. No similarities were also found between MTUT and kidney cancers while parallels were observed for specific SNVs with endometrial carcinomas. In conclusion, immunohistochemical PAX8-positivity and lack of TERT promoter mutations could serve as key diagnostic features in difficult cases. Thus, understanding the molecular background of these tumors helps to refine treatment options and offers the possibility of targeted therapies in cases where needed.
dc.description.abstractIn the 2016 WHO classification of genitourinary tumors Muellerian tumors of the urinary tract (MTUT) comprise clear cell adenocarcinomas and endometrioid carcinomas. Since these rare tumors remained understudied, we aimed to characterize their molecular background by performing DNA- and RNA-based targeted panel sequencing. All tumors (n = 11) presented single nucleotide alterations (SNVs), with ARID1A mutations being the most prevalent (5/11, 45%). Besides frequent ARID1A mutations, loss of ARID1A protein is not a suitable marker since protein expression is (partly) preserved also in mutated cases. Copy number alterations (CNVs) were found in 64% of cases (7/11), exclusively gene amplifications. Interestingly, a functionally relevant RSPO2 gene fusion/microdeletion was discovered in the endometrioid adenocarcinoma case. Comparing our findings with mutational profiles of other tumor entities, absence of TERT promoter mutations argues for a non-urothelial origin. No similarities were also found between MTUT and kidney cancers while parallels were observed for specific SNVs with endometrial carcinomas. In conclusion, immunohistochemical PAX8-positivity and lack of TERT promoter mutations could serve as key diagnostic features in difficult cases. Thus, understanding the molecular background of these tumors helps to refine treatment options and offers the possibility of targeted therapies in cases where needed.
dc.identifier.doi10.3390/genes12060880
dc.identifier.piigenes12060880
dc.identifier.urihttps://resolver.sub.uni-goettingen.de/purl?gro-2/88581
dc.item.fulltextWith Fulltext
dc.language.isoen
dc.notes.internDOI Import GROB-448
dc.publisherMDPI
dc.relation.eissn2073-4425
dc.rightshttps://creativecommons.org/licenses/by/4.0/
dc.titleMolecular Characterization of Muellerian Tumors of the Urinary Tract
dc.typejournal_article
dc.type.internalPublicationyes
dspace.entity.typePublication

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