Biotechnologia Acta (Apr 2022)
THE ACQUISITION OF RESISTANCE IN HUMAN NON-SMALL LUNG ADENOCARCINOMA MOR CELLS IS ASSOCIATED WITH UP-REGULATION OF ADAPTOR PROTEIN RUK/CIN85 AND EPITHELIAL-TO-MESENCHYMAL TRANSITION (EMT)
Abstract
The aim of this study was to elucidate the regulatory role of Ruk/CIN85 in chemoresistance and EMT using human NSCLC MOR cells as a model. Methods. MOR (ECACC 84112312) cell line and drug-resistant cell line MOR/0.2R (ECACC 96042335) were cultured under standard conditions in DMEM medium. Knockdown of Ruk/CIN85 in MOR/0.2R cells was performed using shRNA lentiviral technology. Expression levels of Ruk/CIN85, vimentin and E-cadherin were estimated by RT-PCR. Results and Discussion. According to the results of qPCR, MOR/0.R cells showed an extremely higher level of Ruk/CIN85 mRNA expression, more than 10 times higher than the parental MOR cells. Preliminary data revealed that knockdown of Ruk/CIN85 in the MOR/0.2R cells led to significant decrease of their resistance to doxorubicin and development of epithelial phenotype. High content of RukCIN85 in doxorubicin-resistant (MOR/R) cells strongly correlate with their mesenchymal phenotype (high expression level of vimentin and low – E-cadherin), while its down-regulation is followed by restoration of expression values characteristic of parental MOR cells. Conclusions. In summary, high expression level of Ruk/CIN85 in doxorubicin-resistant MOR cells and the reversion of EMT-related transcriptome parameters and sensitivity to drug due to knockdown of adaptor protein in this subline suggests its involvement in regulation of EMT as well as cancer cells chemoresistance. Thus, the adaptor protein Ruk/CIN85 can be considered as a tissue-specific marker of carcinogenesis and perspective target for drug development.
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