Department of Anatomy and Anthropology, Sackler School of Medicine, Tel-Aviv University, Tel-Aviv, 69978, Israel.
Drug Design & Development Section, Translational Gerontology Branch, Intramural Research Program, National Institute on Aging, National Institutes of Health, Baltimore, MD, 21224, USA.
Sci Rep. 2017 Jun 16;7(1):3735. doi: 10.1038/s41598-017-03792-9.
Mild blast traumatic brain injury (B-TBI) induced lasting cognitive impairments in novel object recognition and less severe deficits in Y-maze behaviors. B-TBI significantly reduced the levels of synaptophysin (SYP) protein staining in cortical (CTX) and hippocampal (HIPP) tissues. Treatment with exendin-4 (Ex-4) delivered by subcutaneous micro-osmotic pumps 48 hours prior to or 2 hours immediately after B-TBI prevented the induction of both cognitive deficits and B-TBI induced changes in SYP staining. The effects of a series of biaxial stretch injuries (BSI) on a neuronal derived cell line, HT22 cells, were assessed in an in vitro model of TBI. Biaxial stretch damage induced shrunken neurites and cell death. Treatment of HT22 cultures with Ex-4 (25 to 100 nM), prior to injury, attenuated the cytotoxic effects of BSI and preserved neurite length similar to sham treated cells. These data imply that treatment with Ex-4 may represent a viable option for the management of secondary events triggered by blast-induced, mild traumatic brain injury that is commonly observed in militarized zones.
轻度爆炸创伤性脑损伤(B-TBI)导致新物体识别的持续认知障碍,以及 Y 迷宫行为的较轻缺陷。B-TBI 显著降低了皮质(CTX)和海马(HIPP)组织中突触素(SYP)蛋白染色的水平。在 B-TBI 之前 48 小时或之后 2 小时通过皮下微渗透泵给予 exendin-4(Ex-4)治疗,可预防认知缺陷的诱导和 B-TBI 诱导的 SYP 染色变化。在 TBI 的体外模型中,评估了一系列双轴拉伸损伤(BSI)对神经元衍生细胞系 HT22 细胞的影响。双轴拉伸损伤导致神经元突起收缩和细胞死亡。在损伤前用 Ex-4(25 至 100 nM)处理 HT22 培养物可减轻 BSI 的细胞毒性作用,并保持类似于假处理细胞的神经元突起长度。这些数据表明,在用爆炸物引起的轻度创伤性脑损伤治疗中,用 Ex-4 治疗可能是一种可行的选择,这种损伤在军事化地区很常见。
