Increases of M2a macrophages and fibrosis in aging muscle are influenced by bone marrow aging and negatively regulated by muscle-derived nitric oxide. - Wikidata - awgldk - TriplyDB

Increases of M2a macrophages and fibrosis in aging muscle are influenced by bone marrow aging and negatively regulated by muscle-derived nitric oxide.

Increases of M2a macrophages and fibrosis in aging muscle are influenced by bone marrow aging and negatively regulated by muscle-derived nitric oxide.

http://www.wikidata.org/entity/Q35935193

about

Aging, inflammation, stem cells, and bone healing The effect of calorie restriction on mouse skeletal muscle is sex, strain and time-dependent.Alternatively Activated (M2) Macrophage Phenotype Is Inducible by Endothelin-1 in Cultured Human Macrophages.Dynamic macrophage polarization-specific miRNA patterns reveal increased soluble VEGF receptor 1 by miR-125a-5p inhibition Cell Therapy Strategies to Combat Immunosenescence.Klotho gene silencing promotes pathology in the mdx mouse model of Duchenne muscular dystrophy.Aging Affects Bone Marrow Macrophage Polarization: Relevance to Bone Healing.Doxorubicin inhibits muscle inflammation after eccentric exercise.Biomimetic scaffolds for regeneration of volumetric muscle loss in skeletal muscle injuries.Regulation of muscle growth and regeneration by the immune system Effects of age-related shifts in cellular function and local microenvironment upon the innate immune response to implants.Immunological aspects of age-related diseases Controlled delivery of SDF-1α and IGF-1: CXCR4(+) cell recruitment and functional skeletal muscle recovery.Macrophage density in pharyngeal and laryngeal muscles greatly exceeds that in other striated muscles: an immunohistochemical study using elderly human cadavers.Macrophages escape Klotho gene silencing in the mdx mouse model of Duchenne muscular dystrophy and promote muscle growth and increase satellite cell numbers through a Klotho-mediated pathway.Inflammation, ageing, and bone regeneration.β2-Adrenoceptor is involved in connective tissue remodeling in regenerating muscles by decreasing the activity of MMP-9.Aging alters the immunological response to ischemic stroke.Age-related changes in skeletal muscle: changes to life-style as a therapy Macrophage Depletion in Elderly Mice Improves Response to Tumor Immunotherapy, Increases Anti-tumor T Cell Activity and Reduces Treatment-Induced Cachexia

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Increases of M2a macrophages and fibrosis in aging muscle are influenced by bone marrow aging and negatively regulated by muscle-derived nitric oxide.

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2015 nî lūn-bûn

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Giuseppina Samengo

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James G Tidball

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Michelle Wehling-Henricks

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Ying Wang

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P2860

Release of hepatocyte growth factor from mechanically stretched skeletal muscle satellite cells and role of pH and nitric oxide.

Increased Wnt signaling during aging alters muscle stem cell fate and increases fibrosis

Arginine metabolism by macrophages promotes cardiac and muscle fibrosis in mdx muscular dystrophy.

Connective tissue changes and physical properties of developing and ageing skeletal muscle.

Intrinsic stiffness of extracellular matrix increases with age in skeletal muscles of mice.

Relationship of interleukin-6 and tumor necrosis factor-alpha with muscle mass and muscle strength in elderly men and women: the Health ABC Study.

A special population of regulatory T cells potentiates muscle repair.

Interleukin-10 reduces the pathology of mdx muscular dystrophy by deactivating M1 macrophages and modulating macrophage phenotype.

Inducible depletion of satellite cells in adult, sedentary mice impairs muscle regenerative capacity without affecting sarcopenia.

Inflammatory mediators in the elderly.

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678-688

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10.1111/ACEL.12350

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