Abstract 148P
Background
The resistance of patients with ovarian cancer (OC) to chemotherapy drugs is a major problem of modern oncology. In the first treatment the ovarian tumor is responsive to DNA-damaging drugs such as carboplatin and cisplatin. However, patients with relapses become resistant to subsequent treatment with platinum drugs. The mechanisms of resistance occurrence are associated with a change of response to DNA damage caused by chemotherapy drugs. The search for genes affecting the sensitivity of OC cells to chemotherapeutic agents is important for understanding the mechanisms of resistance and identification of new predictive markers of response to chemotherapy treatment. In this regard, this research aimed to identify new potential predictive markers of OC.
Methods
The relative mRNA level of 6 target genes previously identified as potential predictive markers of head and neck cancers was evaluated by qPCR analysis in ovarian cancer tumor samples. The sensitivity index (SI) for each of the 8 drugs (carboplatin, cisplatin, paclitaxel, etoposide, doxorubicin, gemcitabine, oxaliplatin, topotecan) was calculated for primary cell lines obtained from ovarian cancer samples using the formula SI=600-∑TGI200-6.2TDC, where TGI is % of cell growth inhibition, and TDC are standard test concentrations. The obtained data were statistically analyzed.
Results
Increased CSNK2B gene expression is associated with sensitivity to carboplatin (R 0.539, p 0.038) while low CSNK2B gene expression is associated with sensitivity to gemcitabine (R -0.847, p 0.016). Low expression of the UBE2V2 (R -0.669, p 0.024) and WDHD1 (R -0.827, p 0.003) genes is associated with sensitivity to doxorubicin and the low expression of POLR2I gene to topotecan (R -0.757, p 0.049).
Conclusions
Our results supported by the Kazan Federal University Strategic Academic Leadership Program (PRIORITY-2030) found that the mRNA levels of CSNK2B, UBE2V2, WDHD1, and POLR2I genes are proposed as potential predictive markers of OC chemotherapy treatment response.
Editorial acknowledgement
Clinical trial identification
Legal entity responsible for the study
Research Laboratory \"Biomarker\", Institute of Fundamental Medicine and Biology, Kazan Federal University.
Funding
This work has been supported by the Kazan Federal University Strategic Academic Leadership Program (PRIORITY-2030).
Disclosure
All authors have declared no conflicts of interest.
Resources from the same session
169P - A real-world molecular pre-screening program in advanced breast cancer (ABC) at Institut Català d'Oncologia l'Hospitalet: Clinical practice study to assess treatment-decision choice based on molecular results
Presenter: David Lluís Garulo
Session: Cocktail & Poster Display session
Resources:
Abstract
170P - KRAS status in patients with pancreatic ductal adenocarcinoma: A single-center study from 2020 to 2023
Presenter: Manukyan Mariam
Session: Cocktail & Poster Display session
Resources:
Abstract
171P - Benefit of next-generation sequencing for lung cancer patients in a limited-resource area
Presenter: Kijjakom Thanasombunsukh
Session: Cocktail & Poster Display session
Resources:
Abstract
172P - Survival prediction using CT based radiomic features in patients of pancreatic cancer treated by chemotherapy followed by SBRT: A pilot study
Presenter: Divya Khosla
Session: Cocktail & Poster Display session
Resources:
Abstract
173P - Overcoming monocyte imbalance and T cell exhaustion in obesity-associated colorectal cancer liver metastasis
Presenter: Alyssa Cristea
Session: Cocktail & Poster Display session
Resources:
Abstract
174TiP - A pivotal clinical trial of a functional ex vivo organ culture assay for cancer precision medicine
Presenter: Sandra Hanks
Session: Cocktail & Poster Display session
Resources:
Abstract
177TiP - Myeloid-derived suppressor cells in the peripheral blood of patients with colorectal cancer: A trial in progress
Presenter: Hans Raskov
Session: Cocktail & Poster Display session
Resources:
Abstract