Differential Bone Loss in Mouse Models of Colon Cancer Cachexia

Bonetto, Andrea; Kays, Joshua K.; Parker, Valorie A.; Matthews, Ryan R.; Barreto, Rafael; Puppa, Melissa; Kang, Keonwook; Carson, James A.; Guise, Theresa A.; Mohammad, Khalid S.; Robling, Alexander G.; Couch, Marion E.; Koniaris, Leonidas G.; Zimmers, Teresa A.

doi:10.3389/fphys.2016.00679

Cited by 45 publications

(54 citation statements)

References 62 publications

(76 reference statements)

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“…Indeed, examining this organ crosstalk within cachexia may provide important clues to teasing out the mechanisms that drive this morose disease. Our group and others have demonstrated that cancer-induced cachexia does not solely affect skeletal muscle, but that heart, fat, and bone are also impaired (23,26,28,50). In particular, recent observations have implicated that abnormal muscle-bone crosstalk may play a significant role in cancer cachexia.…”

Section: Discussionmentioning

confidence: 74%

“…In particular, recent observations have implicated that abnormal muscle-bone crosstalk may play a significant role in cancer cachexia. For example, observations generated in several mouse models of CRC, including C26, HT-29, and Apc min/+ , revealed differential bone loss, despite consistent loss of skeletal muscle mass (28). Interestingly, cancellous bone in the femurs of C26 tumor hosts was generally maintained, whereas in the present study, the use of C26 tumor cells to induce LMs was sufficient to drive both skeletal muscle and bone loss (Figure 9), further indicating an exacerbation in bone phenotype with LMs.…”

Section: Discussionmentioning

confidence: 99%

“…CRC (23,(26)(27)(28). Interestingly, the traditional C26 allograft model does not present with significant bone disruption (28). Therefore, we sought to examine whether the mC26 model drove bone loss in addition to skeletal muscle wasting.…”

Section: Formation Of Colorectal Lms Leads To Loss Of Body Weight Mumentioning

confidence: 99%

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Formation of colorectal liver metastases induces musculoskeletal and metabolic abnormalities consistent with exacerbated cachexia

Huot¹,

Novinger²,

Pin³

et al. 2020

JCI Insight

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Section: Discussionmentioning

confidence: 74%

Section: Discussionmentioning

confidence: 99%

See 1 more Smart Citation

Formation of colorectal liver metastases induces musculoskeletal and metabolic abnormalities consistent with exacerbated cachexia

Huot¹,

Novinger²,

Pin³

et al. 2020

JCI Insight

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“…Although no functional measurements were performed on the bones from ES-2 hosts, our previous evidence suggests that bone content generally correlates with the overall bone strength in cancer cachexia. 67 Although the molecular mechanism(s) responsible for bone depletion in association with the occurrence of OC are not known, high levels of IL-6, as shown in the animals bearing the ES-2 OC, have been previously reported in association not only with the development of paraneoplastic complications, such as cachexia, leucocytosis, and thrombocytosis, but also with the occurrence of hypercalcaemia, a condition responsible for severe loss of bone mass, 68 or juvenile idiopathic arthritis, a systemic inflammatory condition characterized by clinical features that include stunted growth and skeletal abnormalities. 69,70 In this regard, elevated IL-6 seems to play a relevant role by primarily affecting bone turnover, along with increased bone resorption and reduced bone formation.…”

Section: Es-2 Cells Cause Cachexia In Vivomentioning

confidence: 99%

“…69,70 In this regard, elevated IL-6 seems to play a relevant role by primarily affecting bone turnover, along with increased bone resorption and reduced bone formation. 71 Unlike our previous reports describing the occurrence of bone loss following development of colorectal tumours or after prolonged administration of chemotherapy, 48,67 bone tissue is not generally investigated in the experimental models utilized for the study of HGS-OCs. In the clinical setting, OC is not frequently associated with enhanced bone fractures per se or described as a risk factor for the development of osteoporosis, although elevated bone turnover markers were detected in women undergoing risk-reducing salpingooophorectomy to decrease the risk for breast cancer and OC.…”

Section: Es-2 Cells Cause Cachexia In Vivomentioning

confidence: 99%

Growth of ovarian cancer xenografts causes loss of muscle and bone mass: a new model for the study of cancer cachexia

Barreto

Kitase

et al. 2018

J cachexia sarcopenia muscle

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124

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BackgroundCachexia frequently occurs in women with advanced ovarian cancer (OC), along with enhanced inflammation. Despite being responsible for one third of all cancer deaths, cachexia is generally under‐studied in OC due to a limited number of pre‐clinical animal models. We aimed to address this gap by characterizing the cachectic phenotype in a mouse model of OC.MethodsNod SCID gamma mice (n = 6–10) were injected intraperitoneally with 1 × 107 ES‐2 human OC cells to mimic disseminated abdominal disease. Muscle size and strength, as well as bone morphometry, were assessed. Tumour‐derived effects on muscle fibres were investigated in C2C12 myotube cultures. IL‐6 levels were detected in serum and ascites from tumour hosts, as well as in tumour sections.ResultsIn about 2 weeks, ES‐2 cells developed abdominal tumours infiltrating omentum, mesentery, and adjacent organs. The ES‐2 tumours caused severe cachexia with marked loss of body weight (–12%, P < 0.01) and ascites accumulation in the peritoneal cavity (4.7 ± 1.5 mL). Skeletal muscles appeared markedly smaller in the tumour‐bearing mice (approximately –35%, P < 0.001). Muscle loss was accompanied by fibre atrophy, consistent with reduced muscle cross‐sectional area (–34%, P < 0.01) and muscle weakness (–50%, P < 0.001). Body composition assessment by dual‐energy X‐ray absorptiometry revealed decreased bone mineral density (–8%, P < 0.01) and bone mineral content (–19%, P < 0.01), also consistent with reduced trabecular bone in both femurs and vertebrae, as suggested by micro‐CT imaging of bone morphometry. In the ES‐2 mouse model, cachexia was also associated with high tumour‐derived IL‐6 levels in plasma and ascites (26.3 and 279.6 pg/mL, respectively) and with elevated phospho‐STAT3 (+274%, P < 0.001), reduced phospho‐AKT (–44%, P < 0.001) and decreased mitochondrial proteins, as well as with increased protein ubiquitination (+42%, P < 0.001) and expression of ubiquitin ligases in the skeletal muscle of tumour hosts. Similarly, ES‐2 conditioned medium directly induced fibre atrophy in C2C12 mouse myotubes (–16%, P < 0.001), consistent with elevated phospho‐STAT3 (+1.4‐fold, P < 0.001) and altered mitochondrial homoeostasis and metabolism, while inhibition of the IL‐6/STAT3 signalling by means of INCB018424 was sufficient to restore the myotubes size.ConclusionsOur results suggest that the development of ES‐2 OC promotes muscle atrophy in both in vivo and in vitro conditions, accompanied by loss of bone mass, enhanced muscle protein catabolism, abnormal mitochondrial homoeostasis, and elevated IL‐6 levels. Therefore, this represents an appropriate model for the study of OC cachexia. Our model will aid in identifying molecular mediators that could be effectively targeted in order to improve muscle wasting associated with OC.

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Osteopenia is associated with wasting in pancreatic adenocarcinoma and predicts survival after surgery

et al. 2021

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Pancreatic ductal adenocarcinoma (PDAC) is among the deadliest of all common malignancies. Treatment is difficult and often complicated by the presence of cachexia. The clinical portrait of cachexia contributes to the poor prognosis experienced by PDAC patients and worsens therapeutic outcomes. We propose that low bone mineral density is a component of cachexia, which we explore herein through a retrospective review of all patients at our facility that underwent surgery for PDAC between 2011 and 2018 and compared to sex-, age-and comorbidity-matched control individuals. Data were abstracted from the medical record and pre-operative computed tomography scans. Muscle mass and quality were measured at the L3 level and bone mineral density was measured as the radiation attenuation of the lumbar vertebral bodies. Patients with PDAC displayed typical signs of cachexia such as weight loss and radiologically appreciable deterioration of skeletal muscle. Critically, PDAC patients had significantly lower bone mineral density than controls, with 61.2% of PDAC patients categorized as osteopenic compared to 36.8% of controls. PDAC patients classified as osteopenic had significantly reduced survival (1.01 years) compared to patients without osteopenia (2.77 years). The presence of osteopenia was the strongest clinical predictor of 1-and 2-year disease-specific mortality, increasing the risk of death by 107% and 80%, respectively. Osteopenia serves as a test of 2-year mortality with sensitivity of 76% and specificity of 58%. These data therefore identify impaired bone mineral density as a key component of cachexia and predictor of postoperative survival in patients with PDAC. The mechanisms that lead to bone wasting in tumor-bearing hosts deserve further study.

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Differential Bone Loss in Mouse Models of Colon Cancer Cachexia

Cited by 45 publications

References 62 publications

Formation of colorectal liver metastases induces musculoskeletal and metabolic abnormalities consistent with exacerbated cachexia

Formation of colorectal liver metastases induces musculoskeletal and metabolic abnormalities consistent with exacerbated cachexia

Growth of ovarian cancer xenografts causes loss of muscle and bone mass: a new model for the study of cancer cachexia

Osteopenia is associated with wasting in pancreatic adenocarcinoma and predicts survival after surgery

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