Inhibition of HSP90 reverses STAT3‐mediated muscle wasting in cancer cachexia mice

Cachexia is commonly seen in cancer and is characterized by severe muscle wasting, but little is known about the effect of cancer cachexia on expression of contractile protein isoforms such as myosin. Other causes of muscle atrophy shift expression of myosin isoforms toward increased fast (type II) isoform expression. We injected mice with murine C-26 adenocarcinoma cells, a tumor cell line that has been shown to cause muscle wasting. Mice were killed 21 days after tumor injection, and hindlimb muscles were removed. Myosin heavy chain (MHC) and myosin light chain (MLC) content was determined in muscle homogenates by SDS-PAGE. Body weight was significantly lower in tumor-bearing (T) mice. There was a significant decrease in muscle mass in all three muscles tested compared with control, with the largest decrease occurring in the soleus. Although no type IIb MHC was detected in the soleus samples from control mice, type IIb comprised 19% of the total MHC in T soleus. Type I MHC was significantly decreased in T vs. control soleus muscle. MHC isoform content was not significantly different from control in plantaris and gastrocnemius muscles. These data are the first to show a change in myosin isoform expression accompanying muscle atrophy during cancer cachexia.

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Mathematical Model of Muscle Wasting in Cancer Cachexia

10.1101/2020.03.30.016709 ◽

2020 ◽

Author(s):

Suzan Farhang-Sardroodi ◽

Kathleen P. Wilkie

Keyword(s):

Mathematical Model ◽

Satellite Cell ◽

Muscle Tissue ◽

Cancer Cachexia ◽

Muscle Wasting ◽

Tissue Growth ◽

Colon 26 ◽

Treatment Conditions ◽

Risk Of Mortality ◽

Pharmacological Blockade

Cancer cachexia is a debilitating condition characterized by an extreme loss of skeletal muscle mass which negatively impacts patient’s quality of life, reduces their ability to sustain anticancer therapies, and increases the risk of mortality. Recent discoveries have identified the myostatin/activin-ActRIIB pathway as critical to muscle wasting by inducing satellite cell quiescence and increasing muscle-specific ubiquitin ligases responsible for atrophy. Remarkably, pharmacological blockade of the ActRIIB pathway has shown to reverse muscle wasting and prolong the survival time of tumor-bearing animals. To explore the implications of this signaling pathway and potential therapeutic targets in cachexia, we construct a novel mathematical model of muscle tissue subjected to tumor-derived cachexic factors. The model formulation tracks the intercellular interactions between cancer, satellite cell, and muscle cell populations. The model is parameterized by fitting to colon-26 mouse model data, and analysis provides insight into tissue growth in healthy, cancerous, and post-treatment conditions. Model predictions suggest that cachexia fundamentally alters muscle tissue health, as measured by the stem cell ratio, and this is only partially recovered by anti-cachexia treatment. Our mathematical findings suggest that the activation and proliferation of satellite cells, after blocking the myostatin/activin B pathway, is required to partially recover cancer-induced muscle loss.

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Complete reversal of muscle wasting in experimental cancer cachexia: Additive effects of activin type II receptor inhibition and β-2 agonist

International Journal of Cancer ◽

10.1002/ijc.29930 ◽

2015 ◽

Vol 138 (8) ◽

pp. 2021-2029 ◽

Cited By ~ 35

Author(s):

Míriam Toledo ◽

Sílvia Busquets ◽

Fabio Penna ◽

Xiaolan Zhou ◽

Enrica Marmonti ◽

...

Keyword(s):

Cancer Cachexia ◽

Muscle Wasting ◽

Type Ii ◽

Additive Effects ◽

Experimental Cancer ◽

Receptor Inhibition ◽

Complete Reversal

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Mathematical Model of Muscle Wasting in Cancer Cachexia

Journal of Clinical Medicine ◽

10.3390/jcm9072029 ◽

2020 ◽

Vol 9 (7) ◽

pp. 2029 ◽

Cited By ~ 1

Author(s):

Suzan Farhang-Sardroodi ◽

Kathleen P. Wilkie

Keyword(s):

Mathematical Model ◽

Satellite Cell ◽

Muscle Tissue ◽

Cancer Cachexia ◽

Muscle Wasting ◽

Functional Differentiation ◽

Activin A ◽

Tissue Growth ◽

Partial Recovery ◽

Colon 26

Cancer cachexia is a debilitating condition characterized by an extreme loss of skeletal muscle mass, which negatively impacts patients’ quality of life, reduces their ability to sustain anti-cancer therapies, and increases the risk of mortality. Recent discoveries have identified the myostatin/activin A/ActRIIB pathway as critical to muscle wasting by inducing satellite cell quiescence and increasing muscle-specific ubiquitin ligases responsible for atrophy. Remarkably, pharmacological blockade of the ActRIIB pathway has been shown to reverse muscle wasting and prolong the survival time of tumor-bearing animals. To explore the implications of this signaling pathway and potential therapeutic targets in cachexia, we construct a novel mathematical model of muscle tissue subjected to tumor-derived cachectic factors. The model formulation tracks the intercellular interactions between cancer cell, satellite cell, and muscle cell populations. The model is parameterized by fitting to colon-26 mouse model data, and the analysis provides insight into tissue growth in healthy, cancerous, and post-cachexia treatment conditions. Model predictions suggest that cachexia fundamentally alters muscle tissue health, as measured by the stem cell ratio, and this is only partially recovered by anti-cachexia treatment. Our mathematical findings suggest that after blocking the myostatin/activin A pathway, partial recovery of cancer-induced muscle loss requires the activation and proliferation of the satellite cell compartment with a functional differentiation program.

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Exercise as an anti-inflammatory therapy for cancer cachexia: a focus on interleukin-6 regulation

AJP Regulatory Integrative and Comparative Physiology ◽

10.1152/ajpregu.00147.2019 ◽

2020 ◽

Vol 318 (2) ◽

pp. R296-R310 ◽

Cited By ~ 7

Author(s):

Hélène N. Daou

Keyword(s):

Skeletal Muscle ◽

Systemic Inflammation ◽

Cancer Cachexia ◽

Muscle Wasting ◽

Skeletal Muscle Atrophy ◽

Ampk Signaling ◽

Skeletal Muscle Wasting ◽

Skeletal Muscle Loss ◽

Anti Inflammatory ◽

Tumor Growth And Metastasis

Cancer cachexia is a complicated disorder of extreme, progressive skeletal muscle wasting. It is directed by metabolic alterations and systemic inflammation dysregulation. Numerous studies have demonstrated that increased systemic inflammation promotes this type of cachexia and have suggested that cytokines are implicated in the skeletal muscle loss. Exercise is firmly established as an anti-inflammatory therapy that can attenuate or even reverse the process of muscle wasting in cancer cachexia. The interleukin IL-6 is generally considered to be a key player in the development of the microenvironment of malignancy; it promotes tumor growth and metastasis by acting as a bridge between chronic inflammation and cancerous tissue and it also induces skeletal muscle atrophy and protein breakdown. Paradoxically, a beneficial role for IL-6 has also been identified recently, and that is its status as a “founding member” of the myokine class of proteins. Skeletal muscle is an important source of circulating IL-6 in people who participate in exercise training. IL-6 acts as an anti-inflammatory myokine by inhibiting TNFα and improving glucose uptake through the stimulation of AMPK signaling. This review discusses the action of IL-6 in skeletal muscle tissue dysfunction and the role of IL-6 as an “exercise factor” that modulates the immune system. This review also sheds light on the main considerations related to the treatment of muscle wasting in cancer cachexia.

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MicroRNA-mRNA Co-sequencing Identifies Transcriptional and Post-transcriptional Regulatory Networks Underlying Muscle Wasting in Cancer Cachexia

Frontiers in Genetics ◽

10.3389/fgene.2020.00541 ◽

2020 ◽

Vol 11 ◽

Cited By ~ 2

Author(s):

Geysson Javier Fernandez ◽

Juarez Henrique Ferreira ◽

Ivan José Vechetti ◽

Leonardo Nazario de Moraes ◽

Sarah Santiloni Cury ◽

...

Keyword(s):

Regulatory Networks ◽

Cancer Cachexia ◽

Muscle Wasting ◽

Transcriptional Regulatory Networks ◽

Transcriptional Regulatory

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Muscle alterations in the development and progression of cancer-induced muscle atrophy: a review

Journal of Applied Physiology ◽

10.1152/japplphysiol.00622.2019 ◽

2020 ◽

Vol 128 (1) ◽

pp. 25-41 ◽

Cited By ~ 5

Author(s):

Megan E. Rosa-Caldwell ◽

Dennis K. Fix ◽

Tyrone A. Washington ◽

Nicholas P. Greene

Keyword(s):

Cancer Patients ◽

Protein Turnover ◽

Cancer Cachexia ◽

Muscle Wasting ◽

Cell Function ◽

Developmental Stages ◽

Muscle Loss ◽

Inflammatory Signaling ◽

Mortality And Morbidity ◽

Cancer Types

Cancer cachexia—cancer-associated body weight and muscle loss—is a significant predictor of mortality and morbidity in cancer patients across a variety of cancer types. However, despite the negative prognosis associated with cachexia onset, there are no clinical therapies approved to treat or prevent cachexia. This lack of treatment may be partially due to the relative dearth of literature on mechanisms occurring within the muscle before the onset of muscle wasting. Therefore, the purpose of this review is to compile the current scientific literature on mechanisms contributing to the development and progression of cancer cachexia, including protein turnover, inflammatory signaling, and mitochondrial dysfunction. We define “development” as changes in cell function occurring before the onset of cachexia and “progression” as alterations to cell function that coincide with the exacerbation of muscle wasting. Overall, the current literature suggests that multiple aspects of cellular function, such as protein turnover, inflammatory signaling, and mitochondrial quality, are altered before the onset of muscle loss during cancer cachexia and clearly highlights the need to study more thoroughly the developmental stages of cachexia. The studying of these early aberrations will allow for the development of effective therapeutics to prevent the onset of cachexia and improve health outcomes in cancer patients.

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