Inhibition of ceramide synthesis ameliorates body wasting in a cancer cachexia model
Pauline Morigny, Honglei Ji, Laura Cussonneau, Sabrina Zorzato, Yun Kwon, Fabien Riols, Doris Kaltenecker, Alisa Maier, Vignesh Karthikaisamy, Samantha Corrà, Tanja Krauss, Claudine Seeliger, Syed Qaaifah Gillani, Joël J. Tissink, Sandra Lacas-Gervais, Tuna Felix Samanci, Adriano Maida, Raul Terron-Exposito, Angela Trinca, Christine von Toerne, Leonardo Nogara, Melina Claussnitzer, Olga Prokopchuk, Jeannine Bachmann, Mauricio Berriel Diaz, Laure B. Bindels, Ondrej Kuda, Hans Hauner, Mark Haid, Stephan Herzig, Carlo Fiore Viscomi, Jerome Gilleron, Anja Zeigerer, Bert Blaauw, Maria Rohm
Pauline Morigny, Honglei Ji, Laura Cussonneau, Sabrina Zorzato, Yun Kwon, Fabien Riols, Doris Kaltenecker, Alisa Maier, Vignesh Karthikaisamy, Samantha Corrà, Tanja Krauss, Claudine Seeliger, Syed Qaaifah Gillani, Joël J. Tissink, Sandra Lacas-Gervais, Tuna Felix Samanci, Adriano Maida, Raul Terron-Exposito, Angela Trinca, Christine von Toerne, Leonardo Nogara, Melina Claussnitzer, Olga Prokopchuk, Jeannine Bachmann, Mauricio Berriel Diaz, Laure B. Bindels, Ondrej Kuda, Hans Hauner, Mark Haid, Stephan Herzig, Carlo Fiore Viscomi, Jerome Gilleron, Anja Zeigerer, Bert Blaauw, Maria Rohm
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Research Article Metabolism Oncology

Inhibition of ceramide synthesis ameliorates body wasting in a cancer cachexia model

Abstract

Cachexia is a metabolic wasting syndrome affecting many patients with cancer, with poor survival outcomes. Disturbed lipid metabolism is a hallmark of cachexia, and our previous work has identified increased levels of circulating ceramides, which are bioactive lipids with adverse effects in metabolic diseases, as biomarkers for cachexia in mouse models and patients. Here, we investigated the role of ceramides on cachexia development using the well-established C26 colon carcinoma model. We demonstrated that elevated ceramides in cachexia arose from increased liver synthesis. We showed that ceramides directly contributed to impaired mitochondrial function and energy homeostasis in cachexia target tissues. Targeting ceramide synthesis using miRNA interference, or myriocin, an approved compound targeting the key synthesis enzyme serine palmitoyltransferase (SPT), improved markers of muscle atrophy in cachectic male mice. Importantly, we demonstrated that key enzymes involved in ceramide production were also elevated in livers, but not in other organs, of patients with cancer cachexia, correlating with disease severity. Our data place ceramides as contributors to metabolic dysfunction in cachexia and highlight the suitability of the ceramide synthesis pathway for therapeutic targeting.

Authors

Pauline Morigny, Honglei Ji, Laura Cussonneau, Sabrina Zorzato, Yun Kwon, Fabien Riols, Doris Kaltenecker, Alisa Maier, Vignesh Karthikaisamy, Samantha Corrà, Tanja Krauss, Claudine Seeliger, Syed Qaaifah Gillani, Joël J. Tissink, Sandra Lacas-Gervais, Tuna Felix Samanci, Adriano Maida, Raul Terron-Exposito, Angela Trinca, Christine von Toerne, Leonardo Nogara, Melina Claussnitzer, Olga Prokopchuk, Jeannine Bachmann, Mauricio Berriel Diaz, Laure B. Bindels, Ondrej Kuda, Hans Hauner, Mark Haid, Stephan Herzig, Carlo Fiore Viscomi, Jerome Gilleron, Anja Zeigerer, Bert Blaauw, Maria Rohm

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Figure 6

Inhibition of CER synthesis improves mitochondrial phenotypes in skeletal muscle of cachectic animals.

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Inhibition of CER synthesis improves mitochondrial phenotypes in skeleta...
(AF) Mice were injected with C26 cells and treated with vehicle (C26-V) or myriocin (C26-M) (advanced cachexia experiment). Dotted lines represent the values from PBS-V–treated mice. (AD) Confocal microscopy of mitochondria in tibialis anterior from 4 animals per group (n = 9 images quantified per group). Quantification of mitochondrial morphology: branch numbers (B), junction numbers (C), and mean branch lengths (D), indicating mitochondrial connectivity. (E and F) Citrate synthase (E) and OXPHOS complex (F) activity in gastrocnemius (n = 6 animals per group). (GJ) Mice were injected with an AAV expressing a control miRNA (miRCTR) or a miRNA against Sptlc2 (miRSPT2) in a hepatocyte-specific manner, and then later with C26 cells (early cachexia experiment). Dotted lines represent the values from PBS-injected mice. Confocal microscopy of mitochondria in tibialis anterior from 4 animals per group (n = 9 images quantified per group). Quantification of mitochondrial morphology: branch numbers (H), junction numbers (I), and mean branch lengths (J), indicating mitochondrial connectivity. Scale bars: 20 μm, original magnification, ×60; insets ×3,5 (A and G). Data indicate the mean ± SEM. *P < 0.05, **P < 0.01, ***P < 0.001, and ****P < 0.0001. Statistical analysis was done using an unpaired, 2-tailed t test (B, C, E, and HJ), a Mann-Whitney U test (D), or unpaired, 2-way ANOVA with Tukey’s post hoc test (F).