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Publication : Apolipoprotein E as a novel therapeutic neuroprotection target after traumatic spinal cord injury.

First Author  Cheng X Year  2018
Journal  Exp Neurol Volume  299
Issue  Pt A Pages  97-108
PubMed ID  29056364 Mgi Jnum  J:261143
Mgi Id  MGI:6153036 Doi  10.1016/j.expneurol.2017.10.014
Citation  Cheng X, et al. (2018) Apolipoprotein E as a novel therapeutic neuroprotection target after traumatic spinal cord injury. Exp Neurol 299(Pt A):97-108
abstractText  Apolipoprotein E (apoE), a plasma lipoprotein well known for its important role in lipid and cholesterol metabolism, has also been implicated in many neurological diseases. In this study, we examined the effect of apoE on the pathophysiology of traumatic spinal cord injury (SCI). ApoE-deficient mutant (apoE(-/-)) and wild-type mice received a T9 moderate contusion SCI and were evaluated using histological and behavioral analyses after injury. At 3days after injury, the permeability of spinal cord-blood-barrier, measured by extravasation of Evans blue dye, was significantly increased in apoE(-/-) mice compared to wild type. The inflammation and spared white matter was also significantly increased and decreased, respectively, in apoE(-/-) mice compared to the wild type ones. The apoptosis of both neurons and oligodendrocytes was also significantly increased in apoE(-/-) mice. At 42days after injury, the inflammation was still robust in the injured spinal cord in apoE(-/-) but not wild type mice. CD45+ leukocytes from peripheral blood persisted in the injured spinal cord of apoE(-/-) mice. The spared white matter was significantly decreased in apoE(-/-) mice compared to wild type ones. Locomotor function was significantly decreased in apoE(-/-) mice compared to wild type ones from week 1 to week 8 after contusion. Treatment of exogenous apoE mimetic peptides partially restored the permeability of spinal cord-blood-barrier in apoE(-/-) mice after SCI. Importantly, the exogenous apoE peptides decreased inflammation, increased spared white matter and promoted locomotor recovery in apoE(-/-) mice after SCI. Our results indicate that endogenous apoE plays important roles in maintaining the spinal cord-blood-barrier and decreasing inflammation and spinal cord tissue loss after SCI, suggesting its important neuroprotective function after SCI. Our results further suggest that exogenous apoE mimetic peptides could be a novel and promising neuroprotective reagent for SCI.
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