TY - JOUR
T1 - Inflammatory monocytes promote progression of Duchenne muscular dystrophy and can be therapeutically targeted via CCR2
AU - Mojumdar, Kamalika
AU - Liang, Feng
AU - Giordano, Christian
AU - Lemaire, Christian
AU - Danialou, Gawiyou
AU - Okazaki, Tatsuma
AU - Bourdon, Johanne
AU - Rafei, Moutih
AU - Galipeau, Jacques
AU - Divangahi, Maziar
AU - Petrof, Basil J.
N1 - Publisher Copyright:
© 2014 EMBO611 November 2014 10.15252/emmm.201403967 Research Article Research Articles © 2014 The Authors. Published under the terms of the CC BY 4.0 license.
PY - 2014/11/1
Y1 - 2014/11/1
N2 - Myofiber necrosis and fibrosis are hallmarks of Duchenne muscular dystrophy (DMD), leading to lethal weakness of the diaphragm. Macrophages (MPs) are required for successful muscle regeneration, but the role of inflammatory monocyte (MO)-derived MPs in either promoting or mitigating DMD is unclear. We show that DMD (mdx) mouse diaphragms exhibit greatly increased expression of CCR2 and its chemokine ligands, along with inflammatory (Ly6Chigh) MO recruitment and accumulation of CD11bhigh MO-derived MPs. Loss-of-function of CCR2 preferentially reduced this CD11bhigh MP population by impeding the release of Ly6Chigh MOs from the bone marrow but not the splenic reservoir. CCR2 deficiency also helped restore the MP polarization balance by preventing excessive skewing of MPs toward a proinflammatory phenotype. These effects were linked to amelioration of histopathological features and increased muscle strength in the diaphragm. Chronic inhibition of CCR2 signaling by mutated CCL2 secreted from implanted mesenchymal stem cells resulted in similar improvements. These data uncover a previously unrecognized role of inflammatory MOs in DMD pathogenesis and indicate that CCR2 inhibition could offer a novel strategy for DMD management. Synopsis: Inflammatory macrophages are shown here to play a central role in the mdx-mouse pathology, a model for Duchenne muscular dystrophy. Genetic ablation or pharmacologic inhibition of CCR2 confers therapeutic benefits in animals, improving muscle structure and function. CD11b(high) macrophages (MP) derived from Ly6C(high) inflammatory monocytes are key pathogenesis mediators in the mdx mouse model of Duchenne muscular dystrophy. Loss of CCR2 preferentially reduces CD11b(high) MP accumulation in the mdx diaphragm and mitigates proinflammatory polarization of intramuscular MP. Genetic as well as pharmacological blockade of CCR2 in mdx mice ameliorates dystrophic histopathologic features and improves mdx diaphragm muscle force production. CCR2 blockade may serve as a useful therapeutic modulator of the immune response in muscular dystrophy. Inflammatory macrophages are shown here to play a central role in the mdx-mouse pathology, a model for Duchenne muscular dystrophy. Genetic ablation or pharmacologic inhibition of CCR2 confers therapeutic benefits in animals, improving muscle structure and function.
AB - Myofiber necrosis and fibrosis are hallmarks of Duchenne muscular dystrophy (DMD), leading to lethal weakness of the diaphragm. Macrophages (MPs) are required for successful muscle regeneration, but the role of inflammatory monocyte (MO)-derived MPs in either promoting or mitigating DMD is unclear. We show that DMD (mdx) mouse diaphragms exhibit greatly increased expression of CCR2 and its chemokine ligands, along with inflammatory (Ly6Chigh) MO recruitment and accumulation of CD11bhigh MO-derived MPs. Loss-of-function of CCR2 preferentially reduced this CD11bhigh MP population by impeding the release of Ly6Chigh MOs from the bone marrow but not the splenic reservoir. CCR2 deficiency also helped restore the MP polarization balance by preventing excessive skewing of MPs toward a proinflammatory phenotype. These effects were linked to amelioration of histopathological features and increased muscle strength in the diaphragm. Chronic inhibition of CCR2 signaling by mutated CCL2 secreted from implanted mesenchymal stem cells resulted in similar improvements. These data uncover a previously unrecognized role of inflammatory MOs in DMD pathogenesis and indicate that CCR2 inhibition could offer a novel strategy for DMD management. Synopsis: Inflammatory macrophages are shown here to play a central role in the mdx-mouse pathology, a model for Duchenne muscular dystrophy. Genetic ablation or pharmacologic inhibition of CCR2 confers therapeutic benefits in animals, improving muscle structure and function. CD11b(high) macrophages (MP) derived from Ly6C(high) inflammatory monocytes are key pathogenesis mediators in the mdx mouse model of Duchenne muscular dystrophy. Loss of CCR2 preferentially reduces CD11b(high) MP accumulation in the mdx diaphragm and mitigates proinflammatory polarization of intramuscular MP. Genetic as well as pharmacological blockade of CCR2 in mdx mice ameliorates dystrophic histopathologic features and improves mdx diaphragm muscle force production. CCR2 blockade may serve as a useful therapeutic modulator of the immune response in muscular dystrophy. Inflammatory macrophages are shown here to play a central role in the mdx-mouse pathology, a model for Duchenne muscular dystrophy. Genetic ablation or pharmacologic inhibition of CCR2 confers therapeutic benefits in animals, improving muscle structure and function.
KW - CCR2
KW - Chemokines
KW - Inflammatory monocytes
KW - Macrophage polarization
KW - Muscular dystrophy
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U2 - 10.15252/emmm.201403967
DO - 10.15252/emmm.201403967
M3 - Article
C2 - 25312642
AN - SCOPUS:84910645572
SN - 1757-4676
VL - 6
SP - 1476
EP - 1492
JO - EMBO Molecular Medicine
JF - EMBO Molecular Medicine
IS - 11
ER -