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  1. Publikacije
  2. Transcriptome analysis of newly established carboplatin-resistant ovarian cancer cell model reveals genes shared by drug resistance and drug- induced EMT
izvor podataka: crosbi

Transcriptome analysis of newly established carboplatin-resistant ovarian cancer cell model reveals genes shared by drug resistance and drug- induced EMT (CROSBI ID 321520)

Prilog u časopisu | izvorni znanstveni rad | međunarodna recenzija

Kralj, Juran ; Pernar Kovač, Margareta ; Dabelić, Sanja ; Stupin Polančec, Darija ; Wachtmeister, Thorsten ; Köhrer, Karl ; Brozovic, Anamaria Transcriptome analysis of newly established carboplatin-resistant ovarian cancer cell model reveals genes shared by drug resistance and drug- induced EMT // British journal of cancer, 128 (2023), 1344-1359. doi: 10.1038/s41416-023-02140-1

Podaci o odgovornosti

Kralj, Juran ; Pernar Kovač, Margareta ; Dabelić, Sanja ; Stupin Polančec, Darija ; Wachtmeister, Thorsten ; Köhrer, Karl ; Brozovic, Anamaria

engleski

Transcriptome analysis of newly established carboplatin-resistant ovarian cancer cell model reveals genes shared by drug resistance and drug- induced EMT

Background: In ovarian cancer (OC) therapy, even initially responsive patients develop drug resistance. Methods: Here, we present an OC cell model composed of variants with differing degrees of acquired resistance to carboplatin (CBP), cross-resistance to paclitaxel, and CBP-induced metastatic properties (migration and invasion). Transcriptome data were analysed by two approaches identifying differentially expressed genes and CBP sensitivity-correlating genes. The impact of selected genes and signalling pathways on drug resistance and metastatic potential, along with their clinical relevance, was examined by in vitro and in silico approaches. Results: TMEM200A and PRKAR1B were recognised as potentially involved in both phenomena, also having high predictive and prognostic values for OC patients. CBP-resistant MES-OV CBP8 cells were more sensitive to PI3K/Akt/mTOR pathway inhibitors Rapamycin, Wortmannin, SB216763, and transcription inhibitor Triptolide compared with parental MES-OV cells. When combined with CBP, Rapamycin decreased the sensitivity of parental cells while Triptolide sensitised drug-resistant cells to CBP. Four PI3K/Akt/mTOR inhibitors reduced migration in both cell lines. Conclusions: A newly established research model and two distinct transcriptome analysis approaches identified novel candidate genes enrolled in CBP resistance development and/or CBP-induced EMT and implied that one-gene targeting could be a better approach than signalling pathway inhibition for influencing both phenomena.

ovarian cancer ; carboplatin resistance ; gene expression ; drug-induced EMT

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Podaci o izdanju

128

2023.

1344-1359

objavljeno

0007-0920

1532-1827

10.1038/s41416-023-02140-1

Povezanost rada

Povezane osobe
Juran Kralj (autor/i)
Margareta Pernar Kovač (autor/i)
Sanja Dabelić (autor/i)
Darija Stupin Polančec (autor/i)
Anamaria Brozovic (autor/i)
Povezane ustanove
Institut Ruđer Bošković (098) (autorova ustanova)
Povezani projekti
Određivanje ključnih molekula epitelno-mezenhimalne tranzicije kao mogućih ciljeva za terapiju raka jajnika (rezultat rada na projektu)

Biologija, Temeljne medicinske znanosti

Poveznice
doi.org
nature.com
static-content.springer.com
Indeksiranost
Scopus
Current Contents Connect (CCC)
Medline
Web of Science Core Collection, Science Citation Index Expanded (WoSCC-SCI-Exp)
Web of Science Core Collection, SCI-Exp, SSCI & A&HCI (WoSCC-SCI-Exp, SSCI, A&HCI)
Krugovi, vizual Srca