Effects of hypertonic sodium chloride hydroxyethyl starch 40 on cerebral perfusion of pigs with traumatic brain injury and hemorrhagic shock

doi:10.3969/j.issn.1674-8115.2010.12.003

›› 2010, Vol. 30 ›› Issue (12): 1460-.doi: 10.3969/j.issn.1674-8115.2010.12.003

• Monographic report (Traumatic medicine) • Previous Articles Next Articles

Effects of hypertonic sodium chloride hydroxyethyl starch 40 on cerebral perfusion of pigs with traumatic brain injury and hemorrhagic shock

LUO Wei¹, LI Xue-yuan², SHEN Bo-xiong¹, FENG Dong-fu²

1.Department of Anesthesiology, The Third People's Hospital, Institute of Traumatic Medicine, 2.Department of |Neurosurgery, The Third People's Hospital, Institute of Traumatic Medicine, Shanghai Jiaotong University School of Medicine, Shanghai 201900, China

Online:2010-12-25 Published:2010-12-31
Supported by:
Shanghai Science and Technology Committee Foundation, 064119639；Foundation of The Third People's Hospital, Shanghai Jiaotong University School of Medicine, syz09-12

Abstract

Abstract:

Objective To investigate the effects of hypertonic sodium chloride hydroxyethyl starch 40 (HSH40) on cerebral perfusion of pigs with traumatic brain injury (TBI) and hemorrhagic shock. Methods Models of TBI, acute intracranial hypertension and hemorrhagic shock were established in 12 miniature pigs under anesthesia and mechanical ventilation by controlled cortical impact, epidural balloon method and blood withdrawal via femoral artery. One hour after model establishment, animals were divided into three groups (n=4), and were intravenously infused with hydroxyethyl starch 200/0.5 (HES group, equivalent volume of removed blood), hypertonic saline 7.5% (HS group, 20% volume of removed blood) and HSH40 (HSH group, 35% volume of removed blood), respectively. Physiological data, including mean arterial pressure(MAP), intracranial pressure(ICP) and cerebral perfusion pressure (CPP) were observed before model establishment(T01), 60 min after model establishment (before resuscitation)(T0) and 15 min(T15), 30 min(T30), 60 min(T60), 120 min(T120) and 180 min(T180) after resuscitation. Besides, changes of serum sodium, plasma osmotic pressure(OSM), arteriovenous oxygen difference (Da-jvO2) and cerebral oxygen enhancement ratios (OER) of T01, T0, T15, T60 and T120 were observed. Results After resuscitation treatment, MAP in each group significantly increased (P<0.05), and the increase in HSH group was the fastest. After reaching the peak, MAP in HSH group and HES group slowly decreased, while MAP in HS group decreased fast. After resuscitation treatment, ICP in HSH group and HS group of each time point decreased significantly (P<0.05), whereas an elevated ICP occurred in HES group (P<0.05 except for T15). After resuscitation treatment, CPP in each group increased fast, and decreased after reaching the peak, with CCP of each time point significantly higher than those of T0 (P<0.05). CPP in HSH group and HS group increased faster than that in HES group, with HSH group higher than HES group at each time point after resuscitation treatment (P<0.05) and higher than HS group after reaching the peak (P<0.05). Da-jvO2 and OER of T0 in each group were significantly higher than those of T01 (P<0.05), and Da-jvO2 and OER of time points after resuscitation treatment were significantly lower than those of T0 (P<0.05). OER in HS group and HSH group of T60 decreased to those of T01 (P>0.05), while OER of T120 was significantly higher than that of T01 in HS group (P<0.05). Serum sodium and OSM of each time point after resuscitation treatment were significantly higher than those of T0 in HSH group and HS group (P<0.05), and the peak values reached at T15. Conclusion HSH40 (6.6 mL/kg) can effectively resuscitate MAP, reduce ICP, increase CCP and cerebral blood flow, and improve the balance of supply and demand of cerebral oxygen of pigs with TBI and hemorrhagic shock.

Key words: hypertonic sodium chloride hydroxyethyl starch 40, traumatic brain injury, intracranial hypertension, hemorrhagic shock, O₂ suturation of jugular venous blood, fluid resuscitation

LUO Wei, LI Xue-yuan, SHEN Bo-xiong, et al. Effects of hypertonic sodium chloride hydroxyethyl starch 40 on cerebral perfusion of pigs with traumatic brain injury and hemorrhagic shock[J]. , 2010, 30(12): 1460-.

[1]	WANG Ju, CHEN Jin, XU Xin-Lu, YU Qi, SONG Ming-ke. Effect of intranasal administration of glibenclamide on the treatment of traumatic brain injury in mice [J]. , 2020, 40(2): 157-.
[2]	SONG He-bao, GAO Guo-yi, FENG Jun-feng, LI Yong-tao, Lü Shou-hua, MAO Qing, JIANG Ji-yao. Value of monitoring N20 somatosensory evoked potentials for predicting the prognosis of coma patients with traumatic brain injury [J]. , 2016, 36(08): 1196-.
[3]	WANG Kai, JING Yao, XU Chen, et al. Effects of deferoxamine on neuroblobin expression and lesions in rats with traumatic brain injury in acute stage [J]. , 2016, 36(03): 349-.
[4]	LIU Tao, BAO Ying-hui, WANG Yong, et al. Signal transduction mechanisms of necroptosis and relevant advances in neurosurgical diseases research [J]. , 2016, 36(01): 115-.
[5]	HE Duo-qi, ZHANG Xi-qiang, YUN Hui-bin, et al. Effects of nasojejunal nutrition enhanced by glutamine on intestinal mucosal barrier and immune function of old patients with severe traumatic brain injury [J]. , 2015, 35(5): 785-.
[6]	SHU Guo-wei, FEI Zhi-min, CAI Pei-hao, et al. Application of intracranial pressure monitoring in treatment of acute severe traumatic brain injury [J]. , 2013, 33(9): 1276-.
[7]	YIN Yu-hua, LI Ming, JIA Feng, et al. Effect of hypothermia on expression CIB1 in hippocampus after traumatic brain injury in rats [J]. , 2013, 33(4): 392-.
[8]	YUAN Lu-tao, WEI Xiao-er, XU Chen, et al. Value of 3.0T magnetic resonance imaging in diagnosis of severe traumatic brain injury and outcome prediction [J]. , 2013, 33(4): 454-.
[9]	YUAN Fang, DING Jun, GUO Yan, et al. Early prediction of intracranial progressive hemorrhagic injury after traumatic brain injury [J]. , 2012, 32(4): 478-.
[10]	DING Jun, GUO Yan, CHEN Shi-wen, et al. Clinical study of routine repeat CT after traumatic brain injury [J]. , 2011, 31(6): 793-.
[11]	YUAN Fang, DING Jun, GUO Yan, et al. Development and validation of prognostic models for patients with traumatic brain injury [J]. , 2011, 31(11): 1592-.
[12]	LUO Wei, LI Xue-yuan, LI Jia, et al. Miniature pig model of combined traumatic brain injury and acute intracranial hypertension with hemorrhagic shock [J]. , 2010, 30(9): 1106-.
[13]	LIANG Yu-min, WU Hai-bo, BAO Ying-hui, et al. One case report of traumatic progressive bilateral epidural hematomas of posterior cranial fossa [J]. , 2010, 30(9): 1181-.
[14]	ZHOU Zheng-wen, WANG Yong, FAN Yi-ling, et al. Effects of hyperbaric oxygen on mitochondrial function of brain tissues and cognitive function after fluid-percussion injury in rats [J]. , 2010, 30(7): 802-.
[15]	DING Jun, CHEN Shi-wen, GUO Yan, et al. Analysis of risk factors of intracranial progressive hemorrhage after traumatic brain injury [J]. , 2010, 30(7): 829-.

Effects of hypertonic sodium chloride hydroxyethyl starch 40 on cerebral perfusion of pigs with traumatic brain injury and hemorrhagic shock

PDF (PC)

Knowledge

Abstract

Cite this article

share this article

TrendMD

References

Related Articles 15

Recommended Articles

Metrics

Comments