Cytoplasmic Aggregation of RPB1 Predicts Failure of Neoadjuvant Chemotherapy
Author:
Nagy-Mikó Bence, Németh-Szatmári Orsolya, Faragó-Mészáros Réka, Csókási Aliz, Bognár Bence, Ördög NóraORCID, Borsos Barbara N., Majoros Hajnalka, Ujfaludi Zsuzsanna, Oláh-Németh Orsolya, Nikolényi AlizORCID, Dobi Ágnes, Kószó Renáta, Sántha Dóra, Lázár György, Simonka Zsolt, Paszt Attila, Ormándi Katalin, Pankotai TiborORCID, Boros Imre M., Villányi Zoltán, Vörös András
Abstract
AbstractWe aimed to investigate the contribution of co-translational protein aggregation to the chemotherapy resistance of tumor cells. Increased co-translational protein aggregation reflects altered translation regulation that may have the potential to buffer transcription under genotoxic stress. As an indicator for such event, we followed cytoplasmic aggregation of RPB1, the aggregation prone largest subunit of RNA polymerase II, in biopsy samples taken from patients with invasive carcinoma of no special type. RPB1 frequently aggregates co-translationally in the absence of proper HSP90 chaperone function or in ribosome mutant cells as revealed formerly in yeast. We found that cytoplasmic foci of RPB1 occur in larger sizes in tumors that showed no regression after therapy. Based on these results, we propose that monitoring the cytoplasmic aggregation of RPB1 may be suitable for determining – from biopsy samples taken before treatment – the effectiveness of neoadjuvant chemotherapy.
Publisher
Cold Spring Harbor Laboratory
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