Hemorrhagic shock due to submucosal esophageal hematoma along with mallory-weiss syndrome:A case report

BACKGROUND Esophageal submucosal hematoma is a rare condition.Although the exact etiology remains uncertain,vessel fragility with external factors is believed to have led to submucosal bleeding and hematoma formation;the vessel was ruptured by a sudden increase in pressure due to nausea,and the hematoma was enlarged by antiplatelet or anticoagulant therapy.Serious conditions are rare,with a better prognosis.We present the first known case of submucosal esophageal hematoma-subsequent hemorrhagic shock due to Mallory-Weiss syndrome.CASE SUMMARY A 73-year-old female underwent endovascular treatment for an unruptured cerebral aneurysm.The patient received aspirin and clopidogrel before surgery and heparin during surgery,and was well during the surgery.Several hours after returning to the ICU,she complained of chest discomfort,vomited 500 m L of fresh blood,and entered hemorrhagic shock.Esophageal submucosal hematoma with Mallory-Weiss syndrome was diagnosed through an endoscopic examination and computed tomography.In addition to a massive fluid and erythrocyte transfusion,we performed a temporary compression for hemostasis with a Sengstaken-Blakemore(S-B)tube.Afterwards,she became hemodynamically stable.On postoperative day 1,we performed an upper gastrointestinal endoscopy and confirmed no expansion of the hematoma nor any recurring bleeding;therefore,we removed the S-B tube and clipped the gastric mucosal laceration at the esophagogastric junction.We started oral intake on postoperative day 10.The patient made steady progress,and was discharged on postoperative day 33.CONCLUSION We present the first known case of submucosal esophageal hematoma subsequent hemorrhagic shock due to Mallory-Weiss syndrome.

Heat shock protein 72 normothermic ischemia,and the impact of congested portal blood reperfusion on rat liver

INTRODUCTIONFrom the technical aspect of liver surgery ,control of bleeding during hepatic parenchymal resection is one of the most important procedures in hepatectomy .Pringle,s maneuver ,a temporary cross-clamping of the hepatoduodnal ligament ,has often been used for this purpose[1],This is the simplest and userul technique to reduce intraoperative blood loss .

Effect of cholecystokinin on cytokines during endotoxic shock in rats

AIM: To study the effect of cholecystokinin-octapeptide (CCK-8) on systemic hypotension and cytokine production in lipopolysaccharide (LPS)-induced endotoxic shock (ES) rats. METHODS: The changes of blood pressure were observed using physiological record instrument in four groups of rats: LPS (8mg.kg(-1),iv) induced ES; CCK-8 (40 microg.kg(-1), iv) pretreatment 10 min before LPS (8mg.kg(-1)); CCK-8 (40 micro.kg(-1), iv) or normal saline (control) groups. Differences in tissue and circulating specificity of the proinflammatory cytokines (TNF-alpha, IL-1beta and IL-6) were assayed with ELISA kits. RESULTS: CCK-8 reversed LPS-induced decrease of mean artery blood pressure (MABP) in rats. Compared with control, LPS elevated the serum level of IL-6 significantly (3567 +/- 687 ng.L(-1) vs 128 +/- 22 ng.L(-1), P【0.01), while contents of TNF-alpha and IL-1beta elevated significantly (277 +/- 86 ng.L(-1) vs not detectable and 43 +/- 9 ng.L(-1) vsnot detectable, P【0.01) but less extent than IL-6. CCK-8 significantly inhibited the LPS-induced increase in serum TNF-alpha IL-1beta and IL-6. LPS elevated spleen and lung content of IL-1beta significantly (5184 +/- 85 ng.L(-1) vs 1047 +/- 21 ng.L(-1) and 4050 +/- 614 ng.L(-1) vs not detectable, P【0.01), while levels of TNF-alpha and IL-6 also rose significantly but in less extent than IL-1beta. CCK-8 inhibited the LPS-induced increase of the cytokines in spleen and lung. In the heart, CCK-8 significantly inhibited LPS-induced increase of TNF-alpha (864 +/- 123 ng.L(-1) in CCK-8+LPS group vs 1599 +/- 227 ng.L(-1) in LPS group, P 【 0.01), and IL-1beta (282 +/- 93 ng.L(-1) in CCK-8+LPS group vs 621 +/- 145ng.L(-1) in LPS group, P 【 0.01). CONCLUSION: CCK-8 reverses ES, which may be related to its inhibitory effect on the overproduction of cytokines.

Uterotonic drugs use for post partum hemorrhage: An audit of the third stage of labor management

Objectives: Worldwide the use of uterotonic drugs has significantly reduced maternal mortality from postpartum hemorrhage. The objective is to audit the use of uterotonics in the active management of the third and fourth stages of labor. Methods: Personal data, diagnostic clinical information, blood loss and uterotonics administered were extracted from a cohort of 634 consecutive parturient. Trend in Shock Index (Pulse Rate/Systolic Blood Pressure) and 48 hours hematocrit changes were computed and analyzed. Results: There were 422 vagina deliveries and 212 caesarean sections. Primiparous mothers were 141 (34.2%), while grand multiparous mothers were 14 (3.4%). The mean visually estimated postpartum blood loss 165.9 ± 80 ml. There was no significant difference in the mean blood loss between the three parity groups of parturient [P = 0.09]. Fourteen parturient (3.44%) had blood loss ≥500 ml. The value of Shock Index (Pulse Rate/Systolic Blood Pressure) in the study ranged between 0.43 and 1.38. Logistic regression analysis of the variables associated with the switch between the three regimens of uterotonic drugs, showed a significant positive correlation between VEBL and uterotonic drugs administered [Pearson correlation = 0.130, P-value = 0.008]. In addition, there was a significant negative correlation between uterotonic drugs administered and Shock Index at 30 minutes and 2 hours postpartum. The correlation coefficient between VEBL and regimens of uterotonic drugs used was positive and significant (P = 0.019). Conclusion: Visually estimated blood loss, with shock are the main Triggers involved in switching between uterotonic drugs regimens used in active management of PPH. Shock index calculation is vital in management decision. We advocate training of all birth attendants on VEBL.

Clinical Study on the Needling and Drug Treatment of Acute Cerebral Hemorrhage

Researches in recent years have shown that cellular immune factor plays an important role in the generation and development of cerebral hemorrhage1-3.

New Developments in Drug Therapy and Research of Cerebral Vasospasm

In this manuscript a comprehensive coverage of recent developments in the drug therapy of vasospasm while providing the background information that neuroscientists need to understand its rationale. The range of new agents available for treatment of cerebral vasospasm is expanding rapidly along with rapid advances in pharmacology and physiology that are uncovering the mechanisms of this disease. Although there are many publications for treatment of cerebral vaso-spasm, most are focusing on different aspects of vasospasm treatment and many have limited value due to insufficient quality. Moreover, the complexity of this, in many cases deleterious condition, is enormous and the information needed to understand drug effects is accordingly often not readily available in a single source. A number of pharmacological and medical therapies are currently in use or being investigated in an attempt to reverse cerebral vasospasm, but only a few have proven to be useful. Current research efforts promise the eventual production of new medical therapies. At last, recommendations for the use of different treatment stages based on currently available clinical data are provided.

Spontaneous diuresis and negative fluid balance predicting recovery and survival in patients with trauma-hemorragic shock

Most patients with trauma-hemorragic shock, prior to ICU admission, have been resuscitated and stabilized in the emergency room (ER) and/or operation room (OR). Many of them suffer from systemic edema. This extra-vascular fluid is caused by massive infusion of fluid and blood for the maintenance of blood pressure. During the recovery stage, the patients exhibit spontaneous diuresis followed by negative fluid balance. Urine volumes of some patients are more than 10000 ml/d. Do we need to maintain a balance between daily input and output of water at this situation? There are many references in the medical literature and textbooks about fluid resuscitation and the principles in maintaining the balance between input and output of water, but rarely about when and how to restrict it, that is, when and how to permit a negative balance. In this retrospective review, we examined the resuscitation records of 205 patients with systemic edema after trauma-hemorragic shock.

Changes in blood-brain barrier permeability and expression of related factors in a rat model of intracerebral hemorrhage following minocycline treatment

Inflammatory factor aggregation and blood-brain barrier（BBB）damage occur around hematoma foci following intracerebral hemorrhage.Minocycline is lipophilic,can pass through the BBB,and shows anti-inflammatory effects in models of central nervous system disease.We found that minocycline application at 6 hours after intracerebral hemorrhage reduced BBB permeability,decreased vascular endothelial growth factor expression,and increased nerve growth factor and heat shock protein 70 expression,primarily in neurons and microglia.Early intraperitoneal injection of minocycline attenuated BBB damage possibly by reducing vascular endothelial growth factor expression and enhancing nerve growth factor and heat shock protein 70 expression.

失血性休克后肾脏保护的研究进展

失血性抗休克是一种由于创伤等原因引起的临床常见的急危重症。尤其是肾脏在缺血缺氧后引起的局部组织灌注不足和细胞缺氧,极易导致急性肾损伤。临床上在不断探寻患者失血性休克后更安全、实用和有效的复苏方法,如从晶胶液体到高渗液体、从常压复苏到低压复苏、从纠正血压到恢复组织细胞的氧供、从维持血流动力学稳定到抑制细胞凋亡、从血管活性药到中药再到酶抑制剂的应用等等,以达到更好地保护肾脏的目的。本文就近年来关于失血性休克患者肾脏的保护研究进展进行综述。

1例药物超敏反应综合征合并多脏器衰竭行连续性肾脏替代治疗的护理

本文总结1例以中毒性表皮坏死松解症为表现特征的药物超敏反应综合征样皮炎合并多脏器衰竭患者行连续性肾脏替代治疗(CRRT)的护理经验。患者病情复杂,入院后积极完善评估和检查,采取CRRT治疗,同时加强脏器衰竭护理、CRRT护理、管路护理、皮肤护理,做好饮食指导和健康宣教,积极预防并发症,患者的皮损明显减轻,生命体征相对恢复稳定。

川芎嗪对肠粘膜屏障功能的保护作用

目的 :探讨川芎嗪对失血性休克再灌注后肠粘膜屏障功能的保护作用。方法 :30只日本大耳白兔随机分为 3组 :假手术组 (A组 ) ,单纯休克组 (B组 ) ,川芎嗪治疗组 (C组 )。以硫代巴比妥酸比色法、放射免疫法及硝酸还原酶法测定末端回肠粘膜丙二醛 (MDA)、肿瘤坏死因子 (TNFα)、白细胞介素 - 1β(IL - 1β)及一氧化氮代谢产物(NO-2 /NO-3 )含量 ,并取体循环血做细菌培养 ,取肠粘膜行光镜和电镜观察。结果 :B组肠粘膜MDA、TNFα、IL - 1β含量明显高于A组 ,NO-2 /NO-3 浓度显著低于A组 ,而C组变化无显著 ;B组细菌移位率明显高于A组 ,而C组与A组比较无显著差异 ;B组肠粘膜损伤明显重于A组 ,C组明显轻于B组 ,而C组与A组差异无显著。结论 :川芎嗪能保护失血性休克再灌注后肠粘膜屏障功能 ,这可能与其清除体内氧自由基。

控制性与非控制性失血性休克早期液体复苏的对比研究

目的比较在失血已控制及失血未控制两种状态下常规液体复苏治疗失血性休克的效果,探索早期液体复苏对策。方法健康雄性SD大鼠28只,随机分为对照组(n=8)、失血已控制休克组(CHS组,n=10)及失血未控制休克组(UHS组,n=10)。CHS组及UHS组大鼠股动脉放血,使血压在15min内降至30mmHg,然后截断3组大鼠尾根部,对照组及CHS组立即结扎止血,UHS组不予处理使其自然流血。模拟战创伤实际情况,将动物分为院前期(30～90min)、医院救治期(90～150min)及康复期(150min～72h)3个阶段。院前期通过输液将大鼠血压维持在60mmHg;医院救治期结扎出血灶,输血、输液维持大鼠血压至90mmHg;康复期观察至72h。监测平均动脉压(MAP)、中心静脉压(CVP)、心功能、血气分析及血细胞比容(Hct)、血乳酸水平等,观察记录出血量、补液量及动物存活时间。结果根据实验设计,通过液体复苏使CHS组及UHS组大鼠院前期及医院救治期MAP分别维持在60mmHg及90mmHg。CHS组及UHS组同一时相MAP及CVP均无显著差异。院前期UHS组大鼠Hct明显低于CHS组。自院前期开始,UHS组大鼠血乳酸水平即持续性升高,而医院救治期以后CHS组血乳酸水平升高不明显。从医院救治期开始UHS组心率及最大心室内压上升速度明显低于CHS组。液体复苏后CHS组动物酸中毒及低氧血症得到明显纠正,但UHS组仍持续处于低氧血症及酸中毒状态。CHS组院前期补液量(44.5±10.1ml/kg)明显低于UHS组(74.5±11.4ml/kg,P<0.01)。CHS组及UHS组72h死亡率分别为30%及80%。结论较失血已控制的休克而言,对失血未控制的休克进行快速复苏可导致出血量增加、血液稀释、心功能损害及死亡率增加。

不同严重程度急性缺血性卒中患者静脉溶栓预后的影响因素分析

目的：观察不同严重程度急性缺血性卒中（AIS）患者静脉溶栓远期预后和出血转化的影响因素。方法：回顾性分析2009年6月至2013年12月在浙江大学医学院附属第二医院神经内科因AIS接受静脉溶栓治疗患者的资料，根据美国国立卫生研究院卒中量表（NIHSS）将患者分为轻度（≤8分）、中度（9～15分）、重度（≥16分）三组，分别观察影响患者溶栓后的预后（3月时改良Rankin评分≤2分定义为预后良好）及发生出血转化的因素。结果：共365例患者纳入分析：轻度134例、中度121例、重度110例。轻度AIS患者中，年龄[ OR＝0．937，95％可信区间（CI）：0．898～0．978；P＝0．003]、基线NIHSS（OR＝0．732，95％CI：0．564～0．950；P＝0．019）、发病至治疗时间在270 min内（ OR＝4．109，95％CI：1．441～11．719；P＝0．008）是预后良好的独立影响因素；而基线血糖（ OR＝1．326，95％CI：1．009～1．743；P＝0．043）是发生脑实质出血型出血转化的独立影响因素。中度AIS患者中，年龄（ OR＝0．954，95％CI：0．924～0．984；P＝0．003）、基线NIHSS （ OR＝0．760，95％CI：0．619～0．933；P＝0．009）是预后良好的独立影响因素；而心房颤动（ OR＝3．307，95％CI：1．140～9．596；P＝0．028）、收缩压（ OR＝0．967， 95％CI：0．943～0．991；P＝0．008）是发生出血性梗死型出血转化的独立影响因素，心房颤动（ OR＝36．972，95％CI：1．770～772．462；P＝0．02）是发生脑实质出血型出血转化的独立影响因素。重度AIS患者中，基线NIHSS （ OR＝0．808，95％CI：0．677～0．963；P＝0．018）是预后良好的独立影响因素，未发现发生溶栓后出血转化的独立影响因素。结论：对于不同严重程度的AIS患者，影响静脉溶栓后远期预后及发生出血转化的影响因素不尽相同；发病至治疗时间在270 min内是轻度AIS患者静脉溶栓后3个月预后良好的独立影响因素；心房颤动是中度AIS患者静脉溶栓后发生出血转化的独立影响因素。

参芨阻克方对失血性休克大鼠肠粘膜上皮细胞线粒体细胞色素和能荷的影响

目的 研究参芨阻克方 (简称参芨 )对失血性休克大鼠小肠粘膜上皮细胞线粒体功能的影响。方法 采用Wigger’s法建立失血性休克动物模型 ,分离小肠粘膜上皮细胞线粒体 ,检测细胞色素aa3、b、c、c1 和能荷的水平。结果 失血性休克后小肠粘膜上皮细胞线粒体细胞色素aa3、b、c、c1 和能荷均显著降低 ;而参芨治疗组小肠粘膜上皮细胞线粒体细胞色素aa3、b、c、c1 和能荷均显著提高 (P <0 .0 5vs休克组 )。结论 失血性休克大鼠小肠粘膜上皮细胞线粒体呼吸链电子传递活性受到损伤 ,能量合成障碍 ,而参芨能显著改善线粒体的呼吸功能。

合并颅内微出血对急性缺血性卒中患者静脉溶栓治疗后临床结局的影响

目的：明确合并颅内微出血对急性缺血性卒中患者静脉重组组织型纤溶酶原激活剂（rt-PA）溶栓后的出血转化以及3个月后神经功能结局的影响.方法：连续收集225例2009年6月至2013年5月期间在浙江大学医学院附属第二医院神经内科接受静脉rt-PA溶栓治疗并行磁敏感序列检查的急性缺血性卒中患者的临床及实验室检查资料,评估患者溶栓后出血转化情况及3个月改良Rankin量表,在磁敏感序列上评估微出血严重程度.采用多元logistic回归分析出血转化,以无出血转化为参照,分析不同出血转化类型的影响因素;采用二元logistic回归分析症状性出血与神经功能结局的影响因素.结果：225例患者平均年龄（66 29±13 01）岁,女性73例（32 4%）,发病至溶栓时间为（238 40±89 16）min,溶栓前美国国立卫生研究院卒中量表（NIHSS）评分为（11 40±5 89）分;共91例（36 1%）合并颅内微出血,微出血数目总计522个;共64例（28 4%）发生溶栓后出血转化,其中43例（19 1%）为出血性脑梗死型,21例（9 3%）为脑实质血肿型.多元logistic回归分析结果提示,多发（≥3个）颅内微出血增加溶栓治疗后脑实质血肿型出血转化（OR=4 957,95%CI 1 306~18 811,P=0 019）.二元logistic回归分析结果提示,多发（≥3个）颅内微出血是溶栓治疗后神经功能不良的独立危险因素（OR=3 496,95%CI 1 381~8 849,P=0 008）.结论：多发（≥3个）颅内微出血增加急性缺血性卒中患者静脉rt-PA溶栓后的脑实质血肿型出血转化风险,并与溶栓治疗后3个月不良神经功能结局有关.

莫沙比利对40%血容量丢失大鼠口服补液时胃排空率和血浆胃动素水平的影响

目的研究莫沙比利(MOS)对40%血容量丢失大鼠早期口服葡萄糖-电解质液(GES)时胃排空的影响。方法雄性SD大鼠随机分为GES组(假手术后口服GES)、H+GES组(失血后口服GES液)和H+GES/MOS组(失血后口服GES和莫沙比利)。用氯胺酮-速眠新Ⅱ肌肉注射复合麻醉后,行右侧颈动脉插管,按全身血容量的40%分两次间隔15min放血制作失血性休克模型。于失血后0.5、1.0h分两次给予2倍失血量的GES灌胃。莫沙比利(0.5mg.kg-1.w-1)溶于GES,于首次灌胃时给予。失血后4.0h腹主动脉取血处死动物,检测血浆胃动素(MTL)和一氧化氮(NO)水平,酚红法测定胃排空率。结果失血后4.0hGES组、H+GES组和H+GES/MOS组胃排空率分别为(92±13)%、(62±11)%和(80±11)%,3组间差别有统计学意义(P<0.05)。H+GES/MOS组胃动素水平显著高于H+GES组〔(104±11)pg/L和(73±14)pg/L〕,但低于GES组〔(132±24)pg/L,P<0.05〕。H+GES/MOS组NO水平显著低于H+GES组〔(83±13)μmol/L和(106±13)μmol/L〕,但高于GES组〔(54±7)μmol/L,P<0.05〕。结论莫沙比利能显著增加大鼠失血性休克时血浆胃动素水平,降低NO水平,促进胃对口服液体的排空,提高口服补液复苏的效果。

急性缺血性卒中患者静脉溶栓后不同部位出血转化的危险因素及预后分析

目的：比较急性缺血性卒中患者静脉溶栓后发生不同部位出血转化的危险因素及溶栓后患者神经功能结局的差异,分析深部出血转化与非深部出血转化的独立预测因素,并了解不同梗死部位出血转化对急性缺血性卒中患者静脉溶栓后神经功能结局的影响.方法：回顾性分析2009年6月至2013年5月浙江大学医学院附属第二医院接受静脉溶栓治疗的急性缺血性卒中患者的临床及影像学资料.按照无出血转化、深部出血转化和非深部出血转化分成三组进行基线特征及神经功能结局的比较.三组间连续变量的比较用单因素方差分析,分类变量的比较用多组卡方检验,并用logistic 回归分析各部位出血转化的影响因素及其对预后的影响.结果：292例患者纳入分析,82例（28 1%）发生出血转化,其中深部出血47例（57 3%）、脑实质血肿型19例（6 5%）、出血性脑梗死型63例（21 6%）;症状性出血 8例（2 7%）.三组患者的年龄、基线NIHSS评分、收缩压以及心房颤动发生率差异有统计学意义（均P〈0 05）.校正后发现基线NIHSS评分（OR=1 126,95%CI：1 063~1 193,P〈0 001）和收缩压（OR=0 982,95%CI：0 967~0 998,P=0 025）是深部出血转化的独立影响因素.未发现非深部出血转化的独立危险因素.多因素分析显示,深部出血转化是影响溶栓后3个月神经功能结局的独立危险因素（OR=0 291,95%CI：0 133~0 640,P=0 002）.结论：基线神经功能缺损程度及收缩压是预测急性缺血性卒中患者溶栓后发生深部出血转化的独立危险因素,且深部出血转化提示患者静脉溶栓治疗后神经功能结局不良.

SOD与NaHCO_3对重症失血性休克低血管反应性的影响

目的 探讨超氧化物岐化酶(SOD)和NaHCO3治疗重症失血性休克低血管反应性的效果。方法 将28只重症失血性休克SD大鼠随机均分为SOD组、NaHCO3组、SOD+NaHCO33个治疗组以及1个对照组，分别观察用药后各组大鼠的血管反应性、血压、微动脉血流量和24h存活率。结果 休克2h后，各组动物微血管对去甲肾上腺素(NE)的反应性显著减低，NE阈值比失血前提高24-27倍。复苏治疗2h后，3个治疗组血管反应性都有回升，其中以SOD+NaHCO3组效果最显著，NE阈值下降至失血前的4．7倍。此外，给SOD+NaHCO3后再给多巴胺的升压效应最为显著，是对照组的1．9倍，且在回输血液后动物血压稳定在13.33kPa以上；治疗2h后，微动脉血流量是对照组的2．54倍，动物存活时间比对照组延长2．9倍。结论 SOD和NaHCO3对重症失血性休克大鼠的血管低反应性有恢复作用；先给SOD+NaHCO3再给升压药物(多巴胺)可明显稳定提升动物血压，并提高动物存活率，提示SOD+碱可能是治疗重症失血性休克低血管反应性的一种新的治疗方法。

环磷酰胺与糖皮质激素双重冲击疗法治疗重症紫癜性肾炎患儿的临床研究

目的观察环磷酰胺(CTX)与甲基泼尼松龙双重冲击疗法与单纯甲基泼尼松龙冲击疗法治疗重症紫癜性肾炎(HSPN)的临床疗效与安全性。方法回顾性分析2011年6月—2014年8月河南省新乡医学院第三附属医院肾病风湿科收治的61例重症HSPN患儿的临床资料,根据治疗方案不同分为联合组(32例)和对照组(29例),2组均常规治疗,在此基础上对照组加用甲基强地松龙冲击疗法,联合组加用CTX与甲基泼尼松龙双重冲击疗法,CTX最多冲击6个疗程,疗程均为6个月,治疗后定量评价肾脏功能,判定临床疗效。结果治疗期间,联合组与对照组分别有1例、3例改血液透析治疗。治疗后联合组完全缓解率(46.8%)、总有效率(90.6%)均高于对照组(27.6%、72.4%),但差异比较无统计学意义(x^2=2.410,P=0.121;x^2=3.413,P=0.065)。与治疗前比较,治疗6个月后2组尿微量蛋白(mAlb)、血尿素氮(BUN)、血肌酐(SCr)、24 h尿蛋白定量均显著改善(P<0.01),且治疗后联合组24 h尿蛋白定量(0.9±0.3)g/d、mAlb(62.5±17.1)mg/L、BUN(4.2±0.9)mmol/L、SCr(42.5±8.2)μmol/L均显著低于对照组(1.1±0.4)g/d、(80.7±22.5)mg/L、(5.9±1.0)mmol/L、(49.7±10.4)μmol/L(P<0.05)。联合组胃肠道反应(18.8%)、上呼吸道感染(15.6%)、脱发(9.4%)、白细胞减少(3.1%)发生率高于对照组(6.9%、10.3%、0、0),而转氨酶升高(3.1%)、库欣貌发生率(3.1%)则低于对照组(3.4%、13.8%),但差异均无统计学意义(P>0.05)。结论 CTX与甲基泼尼松龙双重冲击疗法治疗重症HSPN较单纯甲基强地松龙冲击疗法能进一步改善肾功能,提高临床疗效,累计CTX冲击量小于150 mg/kg不良反应可控。

多模式MRI指导缺血性脑卒中静脉溶栓降低出血转化的研究

目的:对比CT与多模式MRI指导下缺血性脑卒中静脉溶栓治疗后出血转化的差异,明确多模式MRI指导溶栓的安全性。方法:回顾分析2009年6月-2011年10月期间接受静脉重组组织型纤溶酶原激活剂(rtPA)溶栓治疗的缺血性脑卒中患者资料,包括性别、年龄、既往史、溶栓时间、基线NIHSS、血压、血糖、电解质、凝血谱和心电图,以及溶栓后CT与MRI检查等,按照中国缺血性卒中亚型(CISS)标准予以病因分组。结果:共113例患者接受静脉rtPA治疗,平均年龄:(66±12)岁,男性74例,占65.5%,溶栓前美国国立卫生院卒中量表(National Institute of Health StrokeScale,NIHSS)评分12.4±6.5,发病至溶栓时间:(259.7±131.7)min;溶栓后24 h复查发现,34例(30.1%)出现溶栓后出血转化,其中9例(8%)为症状性出血。Logistic回归分析发现,多模式MRI指导下溶栓后的出血转化风险明显减少(OR=0.599,95%CI:0.373～0.962;P=0.034)。结论:多模式MRI指导溶栓相对于CT筛查,在静脉rtPA溶栓治疗后显示更低的出血转化率。