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Cpt1c Downregulation Causes Plasma Membrane Remodelling and Anthracycline Resistance in Breast Cancer

Authors :
0000-0003-0979-4815
0000-0002-2882-7427
0000-0002-3293-2342
0000-0002-6719-4300
Muley, Helena
Valencia, Karmele
Casas, Josefina
Moreno, Bea
Botella, Luis
Lecanda, Fernando
Fadó, Rut
Casals, Núria
0000-0003-0979-4815
0000-0002-2882-7427
0000-0002-3293-2342
0000-0002-6719-4300
Muley, Helena
Valencia, Karmele
Casas, Josefina
Moreno, Bea
Botella, Luis
Lecanda, Fernando
Fadó, Rut
Casals, Núria
Publication Year :
2023

Abstract

Breast cancer (BC) is the most common malignancy in women worldwide. While the main systemic treatment option is anthracycline-containing chemotherapy, chemoresistance continues to be an obstacle to patient survival. Carnitine palmitoyltransferase 1C (CPT1C) has been described as a poor-prognosis marker for several tumour types, as it favours tumour growth and hinders cells from entering senescence. At the molecular level, CPT1C has been associated with lipid metabolism regulation and important lipidome changes. Since plasma membrane (PM) rigidity has been associated with reduced drug uptake, we explored whether CPT1C expression could be involved in PM remodelling and drug chemoresistance. Liquid chromatography-high resolution mass spectrometry (LC-HRMS) lipid analysis of PM-enriched fractions of MDA-MB-231 BC cells showed that CPT1C silencing increased PM phospholipid saturation, suggesting a rise in PM rigidity. Moreover, CPT1C silencing increased cell survival against doxorubicin (DOX) treatment in different BC cells due to reduced drug uptake. These findings, further complemented by ROC plotter analysis correlating lower CPT1C expression with a lower pathological complete response to anthracyclines in patients with more aggressive types of BC, suggest CPT1C as a novel predictive biomarker for BC chemotherapy.

Details

Database :
OAIster
Notes :
English
Publication Type :
Electronic Resource
Accession number :
edsoai.on1373150871
Document Type :
Electronic Resource