Litcius/Paper detail

Acid ceramidase controls apoptosis and increases autophagy in human melanoma cells treated with doxorubicin

Michele Lai, Rachele Amato, Veronica La Rocca, Mesut Bilgin, Giulia Freer, Piergiorgio Spezia, Paola Quaranta, Daniele Piomelli, Mauro Pistello

2021Scientific Reports31 citationsDOIOpen Access PDF

Abstract

Acid ceramidase (AC) is a lysosomal hydrolase encoded by the ASAH1 gene, which cleaves ceramides into sphingosine and fatty acid. AC is expressed at high levels in most human melanoma cell lines and may confer resistance against chemotherapeutic agents. One such agent, doxorubicin, was shown to increase ceramide levels in melanoma cells. Ceramides contribute to the regulation of autophagy and apoptosis. Here we investigated the impact of AC ablation via CRISPR-Cas9 gene editing on the response of A375 melanoma cells to doxorubicin. We found that doxorubicin activates the autophagic response in wild-type A375 cells, which effectively resist apoptotic cell death. In striking contrast, doxorubicin fails to stimulate autophagy in A375 AC-null cells, which rapidly undergo apoptosis when exposed to the drug. The present work highlights changes that affect melanoma cells during incubation with doxorubicin, in A375 melanoma cells lacking AC. We found that the remarkable reduction in recovery rate after doxorubicin treatment is strictly associated with the impairment of autophagy, that forces the AC-inhibited cells into apoptotic path.

Topics & Concepts

CeramideDoxorubicinAutophagyApoptosisMelanomaProgrammed cell deathCancer researchBiologyCell cultureSphingosineCell biologyChemistryBiochemistryChemotherapyReceptorGeneticsAutophagy in Disease and TherapyCalcium signaling and nucleotide metabolismSphingolipid Metabolism and Signaling
Acid ceramidase controls apoptosis and increases autophagy in human melanoma cells treated with doxorubicin | Litcius