TY - JOUR
T1 - Cancer- and endotoxin-induced cachexia require intact glucocorticoid signaling in skeletal muscle
AU - Braun, Theodore P.
AU - Grossberg, Aaron J.
AU - Krasnow, Stephanie M.
AU - Levasseur, Peter R.
AU - Szumowski, Marek
AU - Zhu, Xin Xia
AU - Maxson, Julia E.
AU - Knoll, J. Gabriel
AU - Barnes, Anthony P.
AU - Marks, Daniel L.
PY - 2013/9
Y1 - 2013/9
N2 - Cachexia is a wasting condition defined by skeletal muscle atrophy in the setting of systemic inflammation. To explore the site at which inflammatory mediators act to produce atrophy in vivo, we utilized mice with a conditional deletion of the inflammatory adaptor protein myeloid differentiation factor 88 (MyD88). Although whole-body MyD88-knockout (wbMyD88KO) mice resist skeletal muscle atrophy in response to LPS, muscle-specific deletion of MyD88 is not protective. Furthermore, selective reexpression of MyD88 in the muscle of wbMyD88KO mice via electroporation fails to restore atrophy gene induction by LPS. To evaluate the role of glucocorticoids as the inflammation- induced mediator of atrophy in vivo, we generated mice with targeted deletion of the glucocorticoid receptor in muscle (mGRKO mice). Muscle-specific deletion of the glucocorticoid receptor affords a 71% protection against LPS-induced atrophy compared to control animals. Furthermore, mGRKO mice exhibit 77% less skeletal muscle atrophy than control animals in response to tumor growth. These data demonstrate that glucocorticoids are a major determinant of inflammation-induced atrophy in vivo and play a critical role in the pathogenesis of endotoxemic and cancer cachexia.-Braun, T. P., Grossberg, A. J., Krasnow, S. M., Levasseur, P. R., Szumowski, M., Zhu, X. X., Maxson, J. E., Knoll, J. G., Barnes, A. P., and Marks, D. L. Cancer- and endotoxin-induced cachexia require intact glucocorticoid signaling in skeletal muscle.
AB - Cachexia is a wasting condition defined by skeletal muscle atrophy in the setting of systemic inflammation. To explore the site at which inflammatory mediators act to produce atrophy in vivo, we utilized mice with a conditional deletion of the inflammatory adaptor protein myeloid differentiation factor 88 (MyD88). Although whole-body MyD88-knockout (wbMyD88KO) mice resist skeletal muscle atrophy in response to LPS, muscle-specific deletion of MyD88 is not protective. Furthermore, selective reexpression of MyD88 in the muscle of wbMyD88KO mice via electroporation fails to restore atrophy gene induction by LPS. To evaluate the role of glucocorticoids as the inflammation- induced mediator of atrophy in vivo, we generated mice with targeted deletion of the glucocorticoid receptor in muscle (mGRKO mice). Muscle-specific deletion of the glucocorticoid receptor affords a 71% protection against LPS-induced atrophy compared to control animals. Furthermore, mGRKO mice exhibit 77% less skeletal muscle atrophy than control animals in response to tumor growth. These data demonstrate that glucocorticoids are a major determinant of inflammation-induced atrophy in vivo and play a critical role in the pathogenesis of endotoxemic and cancer cachexia.-Braun, T. P., Grossberg, A. J., Krasnow, S. M., Levasseur, P. R., Szumowski, M., Zhu, X. X., Maxson, J. E., Knoll, J. G., Barnes, A. P., and Marks, D. L. Cancer- and endotoxin-induced cachexia require intact glucocorticoid signaling in skeletal muscle.
KW - Adenocarcinoma
KW - Atrophy
KW - Corticosterone
KW - Inflammation
KW - Lipopolysaccharide
KW - MyD88
KW - Sickness behavior
UR - http://www.scopus.com/inward/record.url?scp=84883437100&partnerID=8YFLogxK
UR - http://www.scopus.com/inward/citedby.url?scp=84883437100&partnerID=8YFLogxK
U2 - 10.1096/fj.13-230375
DO - 10.1096/fj.13-230375
M3 - Article
C2 - 23733748
AN - SCOPUS:84883437100
SN - 0892-6638
VL - 27
SP - 3572
EP - 3582
JO - FASEB Journal
JF - FASEB Journal
IS - 9
ER -