NF-κB–mediated Pax7 dysregulation in the muscle microenvironment promotes cancer cachexia
Wei A. He, … , Federica Montanaro, Denis C. Guttridge
Wei A. He, … , Federica Montanaro, Denis C. Guttridge
Published October 1, 2013
Citation Information: J Clin Invest. 2013;123(11):4821-4835. https://doi.org/10.1172/JCI68523.
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Research Article Oncology

NF-κB–mediated Pax7 dysregulation in the muscle microenvironment promotes cancer cachexia

Abstract

Cachexia is a debilitating condition characterized by extreme skeletal muscle wasting that contributes significantly to morbidity and mortality. Efforts to elucidate the underlying mechanisms of muscle loss have predominantly focused on events intrinsic to the myofiber. In contrast, less regard has been given to potential contributory factors outside the fiber within the muscle microenvironment. In tumor-bearing mice and patients with pancreatic cancer, we found that cachexia was associated with a type of muscle damage resulting in activation of both satellite and nonsatellite muscle progenitor cells. These muscle progenitors committed to a myogenic program, but were inhibited from completing differentiation by an event linked with persistent expression of the self-renewing factor Pax7. Overexpression of Pax7 was sufficient to induce atrophy in normal muscle, while under tumor conditions, the reduction of Pax7 or exogenous addition of its downstream target, MyoD, reversed wasting by restoring cell differentiation and fusion with injured fibers. Furthermore, Pax7 was induced by serum factors from cachectic mice and patients, in an NF-κB–dependent manner, both in vitro and in vivo. Together, these results suggest that Pax7 responds to NF-κB by impairing the regenerative capacity of myogenic cells in the muscle microenvironment to drive muscle wasting in cancer.

Authors

Wei A. He, Emanuele Berardi, Veronica M. Cardillo, Swarnali Acharyya, Paola Aulino, Jennifer Thomas-Ahner, Jingxin Wang, Mark Bloomston, Peter Muscarella, Peter Nau, Nilay Shah, Matthew E.R. Butchbach, Katherine Ladner, Sergio Adamo, Michael A. Rudnicki, Charles Keller, Dario Coletti, Federica Montanaro, Denis C. Guttridge

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Figure 8

Circulating cachectic factors deregulate Pax7 through NF-κB activation.

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Circulating cachectic factors deregulate Pax7 through NF-κB activation. ...
(A) Pax7 Western blot from C2C12 control cells and IκBα-SR cells (SR) that were treated with 5% serum from control or LLC tumor–bearing mice. Quantitation of Pax7 normalized to α-tubulin is also shown. (B) Similar to A, except serum was collected from NC and PC patients with weight loss as indicated (expressed as a percentage of the premorbid state). n.d., not determined. Asterisks denote samples from Figure 2D. Quantitation of Pax7 normalized to α-tubulin is also shown. (C) Cachectic serum was heat inactivated (HI), delipidated (DL), or size fractionated <10 kDa (SF) and used to treat C2C12 cells. Pax7 was examined by Western blot. (D) Fibers from control and LLC tumor–bearing mice were immunostained for Pax7 and GFP. (E) Quantitation of Pax7+GFP+ cells in D. Scale bars: 20 μm (D). *P < 0.05.