腺苷A2A类似物可减轻钝性脊柱创伤后的长期神经损伤。

Adenosine A2A analogue reduces long-term neurologic injury after blunt spinal trauma.

作者信息

Reece T Brett, Davis Jonathan D, Okonkwo David O, Maxey Thomas S, Ellman Peter I, Li Xinning, Linden Joel, Tribble Curtis G, Kron Irving L, Kern John A

机构信息

Department of Surgery, University of Virginia, Charlottesville, VA 22908, USA.

出版信息

J Surg Res. 2004 Sep;121(1):130-4. doi: 10.1016/j.jss.2004.04.006.

DOI:10.1016/j.jss.2004.04.006

PMID:15313386

Abstract

BACKGROUND

ATL-146e is an adenosine A(2A) agonist that has recently been demonstrated to improve neurological outcome in spinal cord injury in animals. In the current study, we extended the treatment paradigm and tested neurobehavioral functioning out to 1 week after injury to assess if early neurological improvement is sustained long term by an adenosine analogue.

MATERIALS AND METHODS

New Zealand White rabbits (3.0-3.5 kg) sustained mid-thoracic blunt spinal cord injury using a weight-drop model (10 g weight dropped from 6 cm directly onto dura). Animals received either (1) 3 h iv infusion of saline carrier (Trauma, N = 21); (2) 3 h iv infusion of 0.06 microg/kg/min ATL-146e followed by intraperitoneal bolus of 10.8 microg/kg ATL-146e at 3 h postinjury (ATL, N = 14); or (3) 3 h iv infusion of 0.06 microg/kg/min ATL-146e followed by intraperitoneal bolus injection of 10.8 microg/kg ATL-146e at 3, 12, and 24 h postinjury (ATL-PLUS, N = 11). Fourteen animals underwent sham injury. Hemodynamic parameters were monitored and hind limb motor functioning was assessed by Tarlov scores (0 = paralyzed to 5 = normal hop) for 7 days after injury.

RESULTS

ATL-146e significantly improved Tarlov scores of ATL-146e groups compared with saline-treated controls (P < 0.01 12, 24, 36, and 48 h). Control animals, severely neurologically impaired at 48 h (Tarlov 1.61 +/- 0.35), were euthanized early due to ethical concerns, thus not permitting later statistical comparisons. Early neurological improvements in both ATL-146e-treated groups were sustained longer term (7 day mean Tarlov, SHAM 4.9 +/- 0.30, ATL 5.0 +/- 0, ATL-PLUS 4.25 +/- 0.31).

CONCLUSIONS

ATL-146e given immediately after blunt spinal cord trauma significantly improves neurological outcome, which is sustained through 7 days. Early adenosine A2A receptor agonism may be critical since additional IP administration afforded no further neurological improvement. The current data further support the potential clinical utility of adenosine A(2A) agonists in the treatment of spinal cord injury.

摘要

背景

ATL - 146e是一种腺苷A(2A)激动剂，最近已被证明可改善动物脊髓损伤后的神经功能结局。在本研究中，我们扩展了治疗模式，并在损伤后1周测试神经行为功能，以评估腺苷类似物是否能长期维持早期神经功能的改善。

材料与方法

使用重量下降模型（将10 g重物从6 cm高处直接落在硬脑膜上）对体重3.0 - 3.5 kg的新西兰白兔造成中胸段钝性脊髓损伤。动物分为三组：(1)静脉输注生理盐水载体3小时（创伤组，N = 21）；(2)损伤后3小时静脉输注ATL - 146e，速率为0.06 μg/kg/min，随后在损伤后3小时腹腔推注10.8 μg/kg ATL - 146e（ATL组，N = 14）；(3)损伤后3、12和24小时静脉输注ATL - 146e，速率为0.06 μg/kg/min，随后在上述时间点腹腔推注10.8 μg/kg ATL - 146e（ATL - PLUS组，N = 11）。14只动物接受假损伤。监测血流动力学参数，并在损伤后7天通过塔尔洛夫评分（0 = 瘫痪至5 = 正常跳跃）评估后肢运动功能。

结果

与生理盐水处理的对照组相比，ATL - 146e组的塔尔洛夫评分显著改善（在12、24、36和48小时，P < 0.01）。由于伦理问题，对照组动物在48小时时神经功能严重受损（塔尔洛夫评分1.61 ± 0.35），提前实施安乐死，因此无法进行后续的统计学比较。两个ATL - 146e治疗组的早期神经功能改善均能长期维持（7天平均塔尔洛夫评分，假手术组4.9 ± 0.30，ATL组5.0 ± 0，ATL - PLUS组4.25 ± 0.31）。