http://stroke.ahajournals.org/content/47/1/214.abstract?etoc
- Xu Cui, MD, PhD;
- Michael Chopp, PhD;
- Alex Zacharek, MS;
- Chengcheng Cui, MD;
- Tao Yan, MD, PhD;
- Ruizhuo Ning, MD;
- Jieli Chen, MD
+ Author Affiliations
- Correspondence to Jieli Chen, MD, Neurology Research, E&R Bldg, Room No 3091, Henry Ford Hospital, 2799 W Grand Blvd, Detroit, MI 48202. E-mail jieli@neuro.hfh.edu
Abstract
Background and Purpose—Stroke-induced
neuroinflammation and white matter damage are associated with
neurological deficits. Whether D-4F, an apolipoprotein
A-I mimetic peptide, treatment of stroke
decreases neuroinflammation and white matter damage and improves
functional outcome
has not been investigated.
Methods—Adult male
C57BL/6 mice were subjected to permanent middle cerebral artery
occlusion (MCAo) and were orally administered saline
as a vehicle control and different doses of
D-4F (2, 4, 8, 16, or 32 mg/kg) starting at 2 h after MCAo and daily
until euthanized
at 7 days after MCAo. D-4F treatment did not
alter the blood levels of high-density lipoprotein, total cholesterol,
triglyceride,
blood–brain barrier leakage, and infarction
volume compared with control group.
Results—D-4F (16
mg/kg) treatment of stroke significantly improved functional outcome,
increased the white matter density and the
number of oligodendrocyte progenitor cells in
the ischemic boundary zone of the ipsilateral striatum, and increased
myelin
basic protein, insulin-like growth factor-1
(IGF1), but decreased inflammatory factor Toll-like receptor-4 and tumor
necrosis
factor-α expression in the ischemic brain 7
days after MCAo (P<0.05, n=11/group). The neurite/axonal
outgrowth in primary cultured neurons was significantly increased when
treated with
D-4F (100 ng/mL) and IGF1 (100 ng/mL)
compared with the nontreatment control. Inhibition of IGF1 significantly
attenuated
D-4F or IGF1 treatment–induced axonal
outgrowth. D-4F-treatment did not increase oligodendrocyte–progenitor
cell proliferation
but decreased oligodendrocyte–progenitor cell
death.
Conclusions—D-4F
treatment initiated 2 h after MCAo decreases neuroinflammation and white
matter damage and improves functional outcome
after stroke. D-4F-induced increase in IGF1
may contribute to D-4F–induced neurite/axonal outgrowth after stroke.
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