Age exacerbates microglial activation, oxidative stress, inflammatory and NOX2 gene expression, and delays functional recovery in a middle-aged rodent model of spinal cord injury.

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The microglial activation profile and associated factors after experimental spinal cord injury in rats

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Age exacerbates microglial activation, oxidative stress, inflammatory and NOX2 gene expression, and delays functional recovery in a middle-aged rodent model of spinal cord injury.

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2017 nî lūn-bûn

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2017年の論文

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2017年论文

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Age exacerbates microglial act ...... t model of spinal cord injury.

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Age exacerbates microglial act ...... t model of spinal cord injury.

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Age exacerbates microglial act ...... t model of spinal cord injury.

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Age exacerbates microglial act ...... nt model of spinal cord injury

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Guzal Khayrullina

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Kasey E Moritz

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Kimberly R Byrnes

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P2860

Microglial priming and enhanced reactivity to secondary insult in aging, and traumatic CNS injury, and neurodegenerative disease

Temporal changes in cell marker expression and cellular infiltration in a controlled cortical impact model in adult male C57BL/6 mice

Improving bioscience research reporting: the ARRIVE guidelines for reporting animal research

A sensitive and reliable locomotor rating scale for open field testing in rats

Age decreases macrophage IL-10 expression: Implications for functional recovery and tissue repair in spinal cord injury

Gait analysis in normal and spinal contused mice using the TreadScan system.

Amyloid precursor protein secretases as therapeutic targets for traumatic brain injury.

IL-4 signaling drives a unique arginase+/IL-1β+ microglia phenotype and recruits macrophages to the inflammatory CNS: consequences of age-related deficits in IL-4Rα after traumatic spinal cord injury.

Free radical theory of aging.

Role of microglia in neurotrauma.

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s12974-017-0933-3

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scholarly article

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10.1186/S12974-017-0933-3

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Ramona E von Leden

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2017-08-18T00:00:00Z

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microglia

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5563003

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Age exacerbates microglial activation, oxidative stress, inflammatory and NOX2 gene expression, and delays functional recovery in a middle-aged rodent model of spinal cord injury.

about

P2860

P2860

Age exacerbates microglial activation, oxidative stress, inflammatory and NOX2 gene expression, and delays functional recovery in a middle-aged rodent model of spinal cord injury.

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