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Original Article

Korean J Physiol Pharmacol 2010; 14(3): 157-161

Published online June 30, 2010 https://doi.org/10.4196/kjpp.2010.14.3.157

Copyright © Korean J Physiol Pharmacol.

Loss of hsp70.1 Decreases Functional Motor Recovery after Spinal Cord Injury in Mice

Hyun Jeong Kim1, Ji-In Jung2, Youngkyung Kim2, Jae-Seon Lee4, Young Wook Yoon2, and June sun Kim3

1Department of Dental Anesthesiology and Dental Research Institute, Seoul National University School of Dentistry, Seoul 110-744, 2Department of Physiology, Korea University College of Medicine, Seoul 136-705, 3Department of Physical Therapy, Korea University College of Health Science, Seoul 136-703, 4Divisions of Radiation Cancer Research and Korea Institute of Radiological and Medical Sciences, Seoul 139-706, Korea

Abstract

Heat shock proteins (HSPs) are specifically induced by various forms of stress. Hsp70.1, a member of the hsp70 family is known to play an important role in cytoprotection from stressful insults. However, the functional role of Hsp70 in motor function after spinal cord injury (SCI) is still unclear. To study the role of hsp70.1 in motor recovery following SCI, we assessed locomotor function in hsp70.1 knockout (KO) mice and their wild-type (WT) mice via the Basso, Beattie and Bresnahan (BBB) locomotor rating scale, before and after spinal hemisection at T13 level. We also examined lesion size in the spinal cord using Luxol fast blue/cresyl violet staining. One day after injury, KO and WT mice showed no significant difference in the motor function due to complete paralysis following spinal hemisection. However, when it compared to WT mice, KO mice had significantly delayed and decreased functional outcomes from 4 days up to 21 days after SCI. KO mice also showed significantly greater lesion size in the spinal cord than WT mice showed at 21 days after spinal hemisection. These results suggest that Hsp70 has a protective effect against traumatic SCI and the manipulation of the hsp70.1 gene may help improve the recovery of motor function, thereby enhancing neuroprotection after SCI.

Keywords: Spinal cord injury, Neuroprotection, Heat shock protein, Mice