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首页> 美国卫生研究院文献>Journal of Neurotrauma >Glibenclamide Produces Region-Dependent Effects on Cerebral Edema in a Combined Injury Model of Traumatic Brain Injury and Hemorrhagic Shock in Mice
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Glibenclamide Produces Region-Dependent Effects on Cerebral Edema in a Combined Injury Model of Traumatic Brain Injury and Hemorrhagic Shock in Mice

机译:格列本脲在小鼠颅脑外伤和失血性休克联合损伤模型中对脑水肿产生区域依赖性作用

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Cerebral edema is critical to morbidity/mortality in traumatic brain injury (TBI) and is worsened by hypotension. Glibenclamide may reduce cerebral edema by inhibiting sulfonylurea receptor-1 (Sur1); its effect on diffuse cerebral edema exacerbated by hypotension/resuscitation is unknown. We aimed to determine if glibenclamide improves pericontusional and/or diffuse edema in controlled cortical impact (CCI) (5m/sec, 1 mm depth) plus hemorrhagic shock (HS) (35 min), and compare its effects in CCI alone. C57BL/6 mice were divided into five groups (n = 10/group): naïve, CCI+vehicle, CCI+glibenclamide, CCI+HS+vehicle, and CCI+HS+glibenclamide. Intravenous glibenclamide (10 min post-injury) was followed by a subcutaneous infusion for 24 h. Brain edema in injured and contralateral hemispheres was subsequently quantified (wet-dry weight). This protocol brain water (BW) = 80.4% vehicle vs. 78.3% naïve, p < 0.01) but was not reduced by glibenclamide (I%BW = 80.4%). Ipsilateral edema also developed in CCI alone (I%BW = 80.2% vehicle vs. 78.3% naïve, p < 0.01); again unaffected by glibenclamide (I%BW = 80.5%). Contralateral (C) %BW in CCI+HS was increased in vehicle (78.6%) versus naive (78.3%, p = 0.02) but unchanged in CCI (78.3%). At 24 h, glibenclamide treatment in CCI+HS eliminated contralateral cerebral edema (C%BW = 78.3%) with no difference versus naïve. By 72 h, contralateral cerebral edema had resolved (C%BW = 78.5 ± 0.09% vehicle vs. 78.3 ± 0.05% naïve). Glibenclamide decreased 24 h contralateral cerebral edema in CCI+HS. This beneficial effect merits additional exploration in the important setting of TBI with polytrauma, shock, and resuscitation. Contralateral edema did not develop in CCI alone. Surprisingly, 24 h of glibenclamide treatment failed to decrease ipsilateral edema in either model. Interspecies dosing differences versus prior studies may play an important role in these findings. Mechanisms underlying brain edema may differ regionally, with pericontusional/osmolar swelling refractory to glibenclamide but diffuse edema (via Sur1) from combined injury and/or resuscitation responsive to this therapy. TBI phenotype may mandate precision medicine approaches to treat brain edema.
机译:脑水肿对于颅脑外伤(TBI)的发病率/死亡率至关重要,而低血压会加重病情。格列本脲可通过抑制磺酰脲受体1(Sur1)减轻脑水肿。其对低血压/复苏加重的弥漫性脑水肿的作用尚不清楚。我们的目的是确定格列本脲是否可改善皮质可控冲击(CCI)(5m / sec,深度为1 depthmm)加上出血性休克(HS)(35 min)的子宫内膜和/或弥漫性水肿,并比较仅在CCI中的效果。 C57BL / 6小鼠分为五组(n = 10)/组:纯种,CCI +载体,CCI +格列本脲,CCI + HS +载体和CCI + HS +格列本脲。静脉注射格列本脲(受伤后10分钟),然后皮下输注24小时。随后对受伤和对侧半球的脑水肿进行定量(干重)。该方案的脑水(BW)= 0.480.4%载体,相比之下,纯水为78.3%,p <0.01),但未被格列本脲降低(I%BW = 80.4%)。仅在CCI中也出现同侧水肿(I%BW = 80.2%媒介物,而单纯时为78.3%,p <0.01);再次不受格列本脲的影响(I%BW = 80.5%)。媒介物(CCI + HS)的对侧(C)%体重增加(78.6%),而天真(78.3%,p = 0.02)增加,但CCI(78.3%)没有变化。 24小时时,在CCI + HS中使用格列本脲治疗可消除对侧脑水肿(C%BW = 78.3%),与单纯治疗无差异。到72 h时,对侧脑水肿已缓解(C%BW = 78.5±0.09%媒介物,相比之下,天真的78.3±0.05%)。格列本脲可降低CCI + HS中24 h对侧脑水肿。这种有益的作用值得在TBI的重要环境中进行多创伤,休克和复苏的其他探索。仅在CCI中未发生对侧水肿。出乎意料的是,两种模型中24小时的格列本脲治疗均未能减轻同侧水肿。种间剂量差异与先前研究可能在这些发现中起重要作用。脑水肿的潜在机制可能因地区而异,对格列本脲难治的围壁/渗透压肿胀,但对这种疗法的综合伤害和/或复苏导致弥漫性水肿(通过Sur1)。 TBI表型可能要求使用精密的医学方法来治疗脑水肿。

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