The Role of lncRNAs TAPIR-1 and -2 as Diagnostic Markers and Potential Therapeutic Targets in Prostate Cancer

Author:

Friedrich MaikORCID,Wiedemann Karolin,Reiche Kristin,Puppel Sven-HolgerORCID,Pfeifer Gabriele,Zipfel Ivonne,Binder Stefanie,Köhl Ulrike,Müller Gerd A.ORCID,Engeland KurtORCID,Aigner Achim,Füssel Susanne,Fröhner Michael,Peitzsch ClaudiaORCID,Dubrovska AnnaORCID,Rade Michael,Christ Sabina,Schreiber Stephan,Hackermüller JörgORCID,Lehmann Jörg,Toma Marieta I.,Muders Michael H.,Sommer Ulrich,Baretton Gustavo B.,Wirth Manfred,Horn Friedemann

Abstract

In search of new biomarkers suitable for the diagnosis and treatment of prostate cancer, genome-wide transcriptome sequencing was carried out with tissue specimens from 40 prostate cancer (PCa) and 8 benign prostate hyperplasia patients. We identified two intergenic long non-coding transcripts, located in close genomic proximity, which are highly expressed in PCa. Microarray studies on a larger cohort comprising 155 patients showed a profound diagnostic potential of these transcripts (AUC~0.94), which we designated as tumor associated prostate cancer increased lncRNA (TAPIR-1 and -2). To test their therapeutic potential, knockdown experiments with siRNA were carried out. The knockdown caused an increase in the p53/TP53 tumor suppressor protein level followed by downregulation of a large number of cell cycle- and DNA-damage repair key regulators. Furthermore, in radiation therapy resistant tumor cells, the knockdown leads to a renewed sensitization of these cells to radiation treatment. Accordingly, in a preclinical PCa xenograft model in mice, the systemic application of nanoparticles loaded with siRNA targeting TAPIR-1 significantly reduced tumor growth. These findings point to a crucial role of TAPIR-1 and -2 in PCa.

Publisher

MDPI AG

Subject

Cancer Research,Oncology

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