Black radish root extract alleviates sodium valproate-induced liver damage via inhibiting mitochondrial membrane potential collapse and oxidative stress in mice

Objective:To explore the effect of black radish(Raphanus sativus L.var niger)root extract on liver enzymes,oxidative stress,and histopathological alterations in mice with sodium valproate-induced hepatotoxicity.Methods:Thirty-two mice were divided into four groups:the control group received drinking water by gavage,the second group was administered with 100 mg/kg of sodium valproate,the third group received 300 mg/kg of black radish root extract,and the fourth group was given both sodium valproate(100 mg/kg)and black radish root extract(300 mg/kg).After 28 days,the mice were euthanized,and serum levels of aspartate aminotransferase(AST),alanine aminotransferase(ALT),and alkaline phosphatase(ALP),along with liver malondialdehyde(MDA),reactive oxygen species(ROS),mitochondrial parameters,tumor necrosis factor-alpha(TNF-α)gene expression,and histopathological changes were assessed.Results:Sodium valproate caused hepatic damage in mice,characterized by elevated serum levels of liver enzymes,increased MDA and ROS levels and TNF-αgene expression,as well as histopathological alterations.The black radish root extract significantly alleviated sodium valproate-caused hepatic injury by decreasing the serum levels of ALT and AST,MDA,ROS,TNF-αgene expression,as well as mitochondrial impairment,but did not have a significant effect on sodium valproate-induced histopathological changes.Conclusions:The black radish root extract demonstrates protective effects against sodium valproate-induced liver injury,possibly through mitigating oxidative stress,mitochondrial impairment,and inflammatory mediator expression.

Sodium valproate suppresses abnormal neurogenesis induced by convulsive status epilepticus

Status epilepticus has been shown to activate the proliferation of neural stem cells in the hippocampus of the brain, while also causing a large amount of neuronal death, especially in the subgranular zone of the dentate gyrus and the subventricular zone. Simultaneously, proliferating stem cells tend to migrate to areas with obvious damage. Our previous studies have clearly confirmed the effect of sodium valproate on cognitive function in rats with convulsive status epilepticus. However, whether neurogenesis can play a role in the antiepileptic effect of sodium valproate remains unknown. A model of convulsive status epilepticus was established in Wistar rats by intraperitoneal injection of 3 mEq/kg lithium chloride, and intraperitoneal injection of pilocarpine 40 mg/kg after 18–20 hours. Sodium valproate(100, 200, 300, 400, 500, or 600 mg/kg) was intragastrically administered six times every day(4-hour intervals) for 5 days. To determine the best dosage, sodium valproate concentration was measured from the plasma. The effective concentration of sodium valproate in the plasma of the rats that received the 300-mg/kg intervention was 82.26 ± 11.23 μg/mL. Thus, 300 mg/kg was subsequently used as the intervention concentration of sodium valproate. The following changes were seen: Recording excitatory postsynaptic potentials in the CA1 region revealed high-frequency stimulation-induced long-term potentiation. Immunohistochemical staining for BrdU-positive cells in the brain revealed that sodium valproate intervention markedly increased the success rate and the duration of induced long-term potentiation in rats with convulsive status epilepticus. The intervention also reduced the number of newborn neurons in the subgranular area of the hippocampus and subventricular zone and inhibited the migration of newborn neurons to the dentate gyrus. These results indicate that sodium valproate can effectively inhibit the abnormal proliferation and migration of neural stem cells and newborn neurons after convulsive status epilepticus, and improve learning and memory ability.

Acute liver failure with thrombotic microangiopathy due to sodium valproate toxicity:A case report

BACKGROUND Sodium valproate is widely used in the treatment of epilepsy in clinical practice.Most adverse reactions to sodium valproate are mild and reversible,while serious idiosyncratic side effects are becoming apparent,particularly hepatotoxicity.Herein,we report a case of fatal acute liver failure(ALF)with thrombotic microangiopathy(TMA)caused by treatment with sodium valproate in a patient following surgery for meningioma.CASE SUMMARY A 42-year-old man who received antiepileptic treatment with sodium valproate after surgery for meningioma exhibited extreme fatigue,severe jaundice accompanied by oliguria,soy sauce-colored urine,and ecchymosis.His postoperative laboratory values indicated a rapid decreased platelet count and hemoglobin level,severe liver and kidney dysfunction,and disturbance of the coagulation system.He was diagnosed with drug-induced liver failure combined with TMA.After plasma exchange combined with hemoperfusion,pulse therapy with high-dose methylprednisolone,and blood transfusion,his liver function deteriorated,and finally,he died.CONCLUSION ALF with TMA is a rare and fatal adverse reaction of sodium valproate which needs to be highly valued.

Protective effect of sodium valproate on motor neurons in the spinal cord following sciatic nerve injury in rats

BACKGROUND: Sodium valproate (VPA) is used to be an effective anti-epileptic drug. VPA possesses the characteristics of penetrating rapidly through the blood-brain barrier (BBB) and increasing levels of Bcl-2 and growth cone-associated protein (GAP) 43 in spinal cord. OBJECTIVE: To observe the effect of VPA on Bcl-2 expression and motor neuronal apoptosis in spinal cord of rats following sciatic nerve transection. DESIGN: Randomized controlled experiment. SETTING: Department of Hand Surgery and Microsurgery, Wuhan Puai Hospital. MATERIALS: A total of 30 male healthy SD rats of clean grade and with the body mass of 180-220 g were provided by Experimental Animal Center of Medical College of Wuhan University. Sodium Valproate Tablets were purchases from Hengrui Pharmaceutical Factory, Jiangsu. METHODS: The experiment was performed in the Central Laboratory of Wuhan Puai Hospital and Medical College of Wuhan University from February to May 2006. Totally 30 rats were randomly divided into two groups: treatment group (n =15) and model group (n =15). Longitudinal incision along backside of right hind limbs of rats was made to expose sciatic nerves, which were sharply transected 1 cm distal to the inferior margin of piriform muscle after nerve liberation under operation microscope to establish sciatic nerve injury rat models. Sodium Valproate Tablets were pulverized and diluted into 50 g/L suspension with saline. On the day of operation, the rats in the treatment group received 6 mL/kg VPA suspension by gastric perfusion, once a day, whereas model group received 10 mL/kg saline by gastric perfusion, once a day. L4-6 spinal cords were obtained at days 1, 4, 7, 14 and 28 after operation, respectively. Terminal deoxyribonucleotidyl transferase (TdT)-mediated dUTP-biotin nick end labeling (TUNEL) technique and immunohistochemical method (SP method) were used to detect absorbance (A) of neurons with positive Bcl-2 expression. Apoptotic rate of cells (number of apoptotic cells/total number of cells×100%) was calculated. MAIN OUTCOME MEASURES: A value of neurons with positive Bcl-2 expression and apoptotic rate in spinal cord of rats in the two groups. RESULTS: A total of 30 SD rats were involved in the result analysis. ①expression of positive Bcl-2 neurons: A value of positive Bcl-2 neurons were 0.71±0.02, 0.86±0.04, 1.02±0.06 at days 4, 7 and 14, respectively after operation in the treatment group, which were obviously higher than those in the model group (0.62±0.03, 0.71±0.05, 0.89±0.04, t = 3.10-4.50, P < 0.05). ②apoptotic result of motor neurons: Apoptotic rate of motor neurons in spinal cord was (6.91±0.89)% and (15.12±2.34)% at days 7 and 14 in the treatment group, which was significantly lower than those in the model group [(9.45±1.61)%, (19.35±0.92)%, t = 2.39, 3.03. P < 0.05]. CONCLUSION: VPA can increase expression of Bcl-2 in spinal cord and reduce neuronal apoptosis in rats following sciatic nerve injury, and has protective effect on motor neuron in spinal cord of rats.

Effects of lamotrigine + sodium valproate therapy on the nerve cell nutrition and apoptosis status as well as inflammatory response in patients with intractable epilepsy

Objective: To investigate the effects of lamotrigine + sodium valproate therapy on the nerve cell nutrition and apoptosis as well as inflammatory response in patients with intractable epilepsy. Methods: A total of 70 patients with intractable epilepsy who were treated in our hospital between August 2013 and October 2016 were divided into routine group (n=35) and study group (n=35) by random number table method, routine group received sodium valproate therapy and study group received lamotrigine combined with sodium valproate therapy. The differences in serum levels of neurotrophy indexes, nerve apoptosis indexes and inflammatory factors were compared between the two groups before and after treatment. Results: Before treatment, there was no statistically significant difference in serum levels of neurotrophy indexes, nerve apoptosis indexes and inflammatory factors between the two groups. After treatment, serum BDNF and NGF levels of study group were higher than those of routine group;serum Bcl-2, Fas and FasL levels of study group were lower than those of routine group whereas Bax level was higher than that of routine group;serum IL-1β, IL-6 and PGE2 levels of study group were lower than those of routine group. Conclusion: Lamotrigine combined with sodium valproate therapy can effectively increase the neurotrophy, inhibit the nerve apoptosis and reduce the systemic inflammatory response in patients with intractable epilepsy.

Effect of sodium valproate retard tablet on the oxidative stress system and cognitive function in patients with epilepsy

Objective:To explore the effect of sodium valproate retard tablet on the oxidative stress system, cognitive function, and thyroid hormone level in patients with epilepsy.Methods:A total of 68 patients with epilepsy were included in the study and randomized into the treatment group and the control group with 34 cases in each group. The patients in the treatment group were given sodium valproate retard tablets, while the patients in the control group were given carbamazepine. The patients in the two groups were treated continuously for 6 months. The oxidative stress indicators and thyroid hormone level before and after treatment in the two groups were detected and compared. MMSE was used to evaluate the cognitive function in the two groups.Results: MPO, SOD, CAT, and GSH-Px levels after treatment in the two groups were significantly reduced when compared with before treatment, while MDA level was significantly elevated. The improvement of the above indicators after treatment in the treatment group was significantly superior to that in the control group. FT3 and FT4 levels after treatment in the control group were significantly reduced when compared with before treatment, but were significantly lower than those in the treatment group. MMSE score 3 and 6 months after treatment in the two groups was significantly elevated when compared with before treatment. MMSE score at each timing point after treatment in the treatment group was significantly higher than that in the control group.Conclusions: The sodium valproate has a small effect on the balance of oxidation and anti-oxidation in patients with epilepsy, and can significantly improve the cognitive function.

Effects of sodium valproate combined with levetiracetam in treatment of children epilepsy and its influences on serum S-100βand high mobility group box-1

Objective:To explore the effects of sodium valproate combined with levetiracetam in the treatment of children epilepsy,and its influences on serum S-100βand high mobility group box-1(HMGB-1)in children with epilepsy.Methods:A total of 160 children who were diagnosed as epilepsy in Baogang Hospital of Inner Mongolia from July 2016 to October 2018 were selected as research objects.They were randomly divided into the study group(n=80)and the control group(n=80)by the random number table method,i.e.,they were treated with sodium valproate combined with levetiracetam and sodium valproate alone,respectively.After 16 weeks of treatment,the effective rates of epileptic seizure treatment and the improvement of epileptiform discharge were evaluated,and chi-square test was used for statistical comparison.The related indicators,including serum tumor necrosis factor-(TNF-α),hypersensitive C-reactive protein(hs-CRP),homocysteine(Hcy),haematocrit(HCT),erythrocyte sedimentation rate(ESR),serum S-100βand HMGB-1,were measured before and after treatment.Paired t-test was used for the comparison in the above indicators within a group before and after treatment;group t-test was used for the comparison between two groups.Chi-square test was used for the comparison in the rate of adverse reactions during treatment between two groups.The study was approved by Ethics Committee of Baogang Hospital(Approval No.:BG201606073),and all children’s guardians were required to sign informed consent forms for clinical study.There were no statistically significant differences between two groups in general clinical data(p>0.05),such as sex constituent ratio,age,the course of disease,the frequency of epileptic seizure per year before treatment,the incidence of epileptiform discharge before treatment and the constituent ratio of types of epileptic seizure,etc.Results:1)After treatment,the effective rates of epileptic seizure treatment and the improvement of epileptiform discharge in the study group were 92.5%(74/80)and 85.0%(68/80)respectively,which were both significantly higher than those in the control group[68.8%(55/80)and 58.8%(47/80)],and the differences were statistically significant(Х^(2)=14.444,13.635;p<0.001).2)In the study group,the levels of serum TNF-α,hs-CRP and Hcy,as well as HCT and ESR after treatment were(53.1±14.0)pg/ml,(5.0±2.5)mg/L,(12.5±3.1)μmol/L,(38.1±5.1)%and(3.0±0.5)mm/h respectively,which were all significantly lower than those[(107.9±17.8)pg/ml,(10.1±2.5)mg/L,(42.2±5.8)μmol/L,(45.3±4.5)%and(5.2±0.6)mm/h]before treatment,and all the differences were statistically significant(t=21.644,12.902,40.393,9.468,25.194;p<0.001).In the control group,the levels of serum TNF-α,hs-CRP and Hcy,as well as HCT and ESR after treatment were(60.6±17.8)pg/ml,(8.2±2.2)mg/L,(15.2±3.1)μmol/L,(40.2±3.4)%and(4.5±0.6)mm/h respectively,which were all significantly lower than those[(112.4±14.3)pg/ml,(9.3±3.8)mg/L,(41.1±2.8)μmol/L,(44.6±5.5)%and(5.4±0.8)mm/h]before treatment,and all the differences were statistically significant(t=20.292,2.241,55.456,3.320,8.050;p<0.05).After treatment,the above indicators in the study group were all significantly lower than those in the control group,and all the differences were statistically significant(t=2.962,8.595,5.508,3.064,17.178;p<0.05).3)In the study group,the levels of serum S-100βand HMGB-1 after treatment were(0.65±0.38)μg/L and(5.3±2.4)μg/L respectively,which were significantly lower than those[(0.91±0.32)μg/L and(8.1±2.0)μg/L]before treatment,and the differences were statistically significant(t=4.681,8.020;p<0.001).In the control group,the levels of serum S-100βand HMGB-1 after treatment were(0.78±0.27)μg/L and(6.4±2.2)μg/L respectively,which were significantly lower than those[(0.88±0.25)μg/L and(7.9±1.7)μg/L]before treatment,and the differences were statistically significant(t=2.431,p=.016;t=4.826,p<0.001).After treatment,the levels of serum S-100βand HMGB-1 in the study group were significantly lower than those in the control group,and the differences were statistically significant(t=2.495,p=.014;t=2.840,p=.005).4)There was no significant difference between two groups in the rate of adverse reactions,such as nausea,vomiting,poor appetite,dizziness,drowsiness,hepatic and renal injury during treatment(p>0.05).Conclusions:The efficacy of sodium valproate combined with levetiracetam is obviously better than that of sodium valproate alone in the treatment of children epilepsy.The children patients’serum S-100βand HMGB-1 are more significantly reduced,resulting in a lower rate of adverse reactions,which has a certain clinical value.

不同剂量丙戊酸钠对双相情感障碍患者血清促甲状腺激素、泌乳素及多巴胺水平的影响

目的探讨不同剂量丙戊酸钠对双相情感障碍(BPD)患者血清促甲状腺激素(TSH)、泌乳素(PRL)及多巴胺(DA)水平的影响。方法选择2020年5月至2022年5月接受治疗的90例BPD患者为研究对象,随机数字表法分为A、B、C三组,均为30例,A、B、C三组每天分别口服10、15、20 mg/kg丙戊酸钠。比较3组临床疗效、治疗前后各项精神疾病评分、血药浓度相关指标、治疗前后血清水平、肝功能相关指标以及不良反应发生率。结果3组治疗后总有效率差异无统计学意义(P>0.05);治疗后3组各项评分相较于治疗前显著性改善(P<0.05);3组达稳态血药浓度谷值时间比较差异有统计学意义(P<0.05);治疗后3组TSH、PRL及DA水平相较于治疗前差异无统计学意义(P>0.05);治疗后3组ALT、AST水平相较于治疗前均有所上升(P<0.05),治疗后3组ALT、AST水平比较差异有统计学意义(P<0.05);3组不良反应发生率比较差异有统计学意义(P<0.05)。结论丙戊酸钠可有效治疗BPD患者,缓解狂躁或抑郁程度,对TSH、PRL及DA水平无明显影响,其中小剂量丙戊酸钠在保证治疗效果的同时对肝功能的影响较小,且不良反应更少,安全性高,值得临床推广。

丙戊酸钠辅助治疗小儿癫痫临床疗效及血清NSE、Hcy与T细胞17水平变化分析

目的 分析丙戊酸钠辅助治疗小儿癫痫临床疗效及对血清神经元特异性烯醇化酶(NSE)、同型半胱氨酸(Hcy)及T细胞17水平(Th17)变化的影响。方法 选取2020年1月至2023年3月邯郸市第二医院收治的小儿癫痫患儿152例,根据治疗方案不同分为对照组73例(托吡酯)和观察组79例(丙戊酸钠+托吡酯)。比较两组总疗效率、炎性因子[肿瘤坏死因子-α(TNF-α)、白介素-2(IL-2)、Hcy]、脑源性神经营养因子(BDNF)、NSE、Th17水平及不良反应。结果 观察组总疗效率为91.81%,对照组总疗效率为75.29%,观察组总疗效率高于对照组,差异有统计学意义(P<0.05)。两组治疗后TNF-α、IL-2、NSE、Hcy、Th17水平均下降,且观察组TNF-α、IL-2、NSE、Hcy、Th17水平低于对照组,差异有统计学意义(P<0.05)。两组治疗后BDNF水平均上升,且观察组BDNF水平高于对照组,差异有统计学意义(P<0.05)。对照组及观察组不良反应总发生率分别为9.59%、5.04%,两组不良反应总发生率比较差异无统计学意义(P>0.05)。结论 丙戊酸钠辅助托吡酯治疗小儿癫痫临床疗效较为理想,可有效减轻炎症反应,显著降低NSE、Th17水平。

复方氨基丁酸维E联合丙戊酸钠对癫痫患儿认知功能及血清α-Syn、HSP70水平的影响

目的研究复方氨基丁酸维E联合丙戊酸钠对癫痫患儿认知功能及血清α-突触核蛋白(α-Syn)、热休克蛋白70(HSP70)水平的影响。方法选取周口市中心医院收治的116例癫痫患儿,根据治疗方案分为联合组和对照组,各58例。对照组接受丙戊酸钠治疗,联合组接受复方氨基丁酸维E联合丙戊酸钠治疗。比较两组临床疗效、治疗前、治疗3、6个月后癫痫持续发作时间及发作频率、韦氏儿童智力量表第四版(WISC-Ⅳ)及简易精神状态检测量表(MMSE)评分、血清相关因子[α-Syn、神经元特异性烯醇化酶(NSE)、HSP70、脑源性神经营养因子(BDNF)]水平、不良反应发生率。结果联合组临床总有效率高于对照组(P<0.05)。治疗3、6个月后,联合组癫痫发作频率少于对照组,持续发作时间短于对照组(P<0.05);WISC-Ⅳ、MMSE评分高于对照组(P<0.05);血清HSP70、α-Syn、NSE水平低于对照组,BDNF水平高于对照组(P<0.05)。两组间不良反应总发生率差异无统计学意义(P>0.05)。结论采用复方氨基丁酸维E与丙戊酸钠联合治疗可有效改善癫痫患儿认知功能及神经功能,降低癫痫持续发作时间及发作频率,增强疗效,安全性良好。

癫痫患者CYP2C19基因多态性与丙戊酸钠血药浓度、疗效的相关性研究

目的研究癫痫患者CYP2C19基因多态性与丙戊酸钠血药浓度、疗效的相关性。方法选取2022年8月至2023年7月乌鲁木齐市第四人民医院收治的115例癫痫患者作为研究对象,采用实时荧光聚合酶链反应(PCR)技术检测所有患者的CYP2C19基因型,同时给予丙戊酸钠治疗,将患者按CYP2C19基因型别分为强代谢型(*1/*1)47例、中间代谢型(*1/*2,*1/*3)50例和弱代谢型(*2/*2,*3/*3,*2/*3)18例,比较CYP2C19代谢型对血药浓度的影响;并根据丙戊酸钠治疗效果分为疗效良好组(n=85)和疗效不佳组(n=30),比较两组患者的一般资料,采用Logistic多因素回归分析影响丙戊酸钠治疗效果的因素。结果癫痫患者CYP2C19基因分型分布频率符合Hardy-Weinberg平衡定律检验;CYP2C19弱代谢型的丙戊酸钠血药浓度为(3.80±1.02)μg/mL,明显高于强代谢的(2.67±0.34)μg/mL和中间代谢型的(2.73±0.36)μg/mL,差异均有统计学意义(P<0.05),而强代谢型和中间代谢型的丙戊酸钠血药浓度比较差异无统计学意义(P>0.05);经单因素分析结果显示,月发病频率≥4次、继发性病因为热性惊厥、丙戊酸钠血药浓度<50μg/mL、服药依从性差、CYP2C19基因型为弱代谢型与丙戊酸钠治疗效果有关(P<0.05);经Logistic多因素回归分析结果显示,月发病频率≥4次、继发性病因为热性惊厥、丙戊酸钠血药浓度<50μg/mL、服药依从性差、CYP2C19基因型为弱代谢型均为影响丙戊酸钠治疗效果的独立危险因素(P<0.05)。结论癫痫患者的CYP2C19基因具有多态性,且与丙戊酸钠血药浓度及疗效具有相关性。因此,在采用丙戊酸钠治疗癫痫患者时,可检测CYP2C19基因分型,以指导癫痫患者的临床个体化治疗。

依达拉奉联合丙戊酸钠治疗卒中后癫痫的有效性及安全性的系统评价和Meta分析

目的评估依达拉奉联合丙戊酸钠治疗卒中后癫痫的有效性及安全性。方法计算机检索the Cochrane Library、PubMed、Embase、Web of Science、CNKI、万方数据库、VIP数据库,检索时限均为自建库起至2023年5月。收集依达拉奉联合丙戊酸钠对比丙戊酸钠单药治疗癫痫的随机对照试验,使用RoB 2工具评估所纳入文献的偏倚风险,使用RevMan 5.4软件进行Meta分析。结果纳入13篇文献,总计1092例患者。Meta分析结果显示,联合治疗组的有效率显著高于丙戊酸钠组[RR=0.18,95%CI(0.13,0.22),P<0.01]。且不良反应发生率更低[RR=0.73,95%CI(0.48,1.13),P=0.16]。联合治疗组患者发作频次[MD=-0.30,95%CI(-0.43,-0.11),P<0.01]、发作持续时间[MD=-0.81,95%CI(-0.89,-0.72),P<0.01]均显著低于丙戊酸钠组;炎症因子肿瘤坏死因子-α[MD=-8.00,95%CI(-9.15,-6.84),P<0.01]。白细胞介素-2[MD=-10.19,95%CI(-14.61,-5.78),P<0.01]、白细胞介素-8[MD=-5.6,95%CI(-6.48,-4.73),P<0.01]均显著低于丙戊酸钠组;联合治疗组癫痫患者神经元特异性烯醇化酶(NSE)水平治疗后1个月[MD=-4.73,95%CI(-4.99,-4.46),P<0.01]、3个月[MD=-2.10,95%CI(-3.26,-0.95),P<0.01]、6个月[MD=-1.31,95%CI(-2.35,-0.27),P<0.01]显著优于丙戊酸钠组。12个月后NSE水平[MD=0.06,95%CI(-0.07,0.19),P=0.34]无明显差别。结论依达拉奉联合丙戊酸钠治疗卒中后癫痫,可提高患者癫痫控制率,缩短发作频率及发作持续时间,可降低患者体内炎症因子水平,促进NSE水平降低,提高其生活质量,具有一定的安全性。

某院2022年丙戊酸钠血药浓度监测结果分析

目的分析某院丙戊酸钠(VPA)血药浓度监测结果及其影响因素,为临床合理用药提供参考。方法回顾性收集2022年1月~12月在常熟市第二人民医院行VPA血药浓度监测的241例患者资料,采用卡方检验或Fisher精确检验分析年龄、药物剂型及联合用药对VPA血药浓度的影响。结果241例患者共行438例次VPA治疗药物监测,血药浓度达标率为58.7%。监测多次的患者中,调整剂量后的监测结果达标率较调整前均有提高。单因素分析显示,剂型和联合用药是影响VPA血药浓度的相关因素(P<0.05)。结论临床使用丙戊酸钠时应注重血药浓度监测,并及时根据监测结果及临床症状调整给药剂量,以提高抗癫痫治疗效果,降低不良反应发生率。

丙戊酸钠在蛛网膜下腔出血早期脑损伤大鼠中的实验研究

目的 探讨丙戊酸钠在蛛网膜下腔出血早期脑损伤大鼠中的实验研究。方法 将120只健康成年雄性SD大鼠根据随机数字表法分为三组,假手术组、模型组及丙戊酸钠组,各40只。颈内动脉穿刺法建立蛛网膜下腔出血模型,丙戊酸钠组大鼠每隔12 h给予丙戊酸钠(300 mg/kg)腹腔注射。原位末端转移酶标记技术检测蛛网膜下腔出血后皮质的细胞和神经元凋亡情况。结果 假手术组大鼠脑底动脉清晰可见,模型组大鼠脑底面有明显的蛛网膜下腔出血。组内比较:与第1天比较,模型组、丙戊酸钠组第3、4天大鼠改良Garcia评分升高,差异有统计学意义(P<0.05);组间比较:前3天,模型组大鼠改良Garcia评分均低于假手术组,差异有统计学意义(P<0.05);第4天,丙戊酸钠组大鼠改良Garcia评分高于模型组,差异有统计学意义(P<0.05)。模型组大鼠脑皮质阳性细胞占比高于假手术组,差异有高度统计学意义(P<0.01);丙戊酸钠组大鼠脑皮质阳性细胞占比低于模型组,差异有统计学意义(P<0.05)。结论 丙戊酸钠减少蛛网膜下腔出血后细胞和神经元的凋亡,改善神经损伤和功能障碍。

丙戊酸钠联合鲁拉西酮治疗双相障碍抑郁发作的疗效及对血清催乳素的影响

目的:研究丙戊酸钠联合鲁拉西酮治疗双相障碍抑郁发作的疗效及对血清催乳素(PRL)的影响。方法:按随机数表法将100例双相障碍抑郁发作患者分为观察组和对照组,各50例。两组分别采用鲁拉西酮、丙戊酸钠联合鲁拉西酮治疗。比较两组临床疗效、促甲状腺激素(TSH)、PRL、雌二醇(E2)水平、自知力与治疗态度问题(ITAQ)评分、正负性情绪量表(PANAS)评分、不良反应发生率。结果:两组有效率分别为95.65%、81.40%,两组有效率比较差异有统计学意义(P<0.05)。治疗后观察组正性情绪评分高于对照组、负性情绪评分低于对照组,并且观察组治疗前后PANAS评分差值较高(P<0.05)。治疗后两组PRL、E2有所升高且观察组高于对照组,此外观察组治疗前后TSH、PRL、E2水平差值较高(P<0.05)。治疗后两组ITAQ评分增高,观察组ITAQ评分高于对照组,此外观察组治疗前后ITAQ评分差值较高(P<0.05)。结论:丙戊酸钠联合鲁拉西酮用于双相障碍抑郁发作疗效好,能改善患者的情绪状态,增加血清PRL水平,提高患者认知能力,且安全性较高。

丙戊酸钠联合左乙拉西坦治疗对癫痫患儿智力认知水平及脑电图的影响

目的 探讨癫痫患儿采用丙戊酸钠与左乙拉西坦联合治疗对其智力、认知水平及脑电图的影响。方法 选取郑州大学第三附属医院于2022-01-2023-01收治的100例癫痫患儿为研究对象,分为对照组和试验组各50例,对照组采用丙戊酸钠治疗,试验组采用丙戊酸钠联合左乙拉西坦治疗,比较2组患儿疗效、智力、认知水平及脑电图情况。结果 试验组患儿总有效率(92.00%)高于对照组(76.00%,P<0.05)。2组患儿治疗4个月后中国韦氏儿童智力量表(C-WISC)及蒙特利尔认知评估量表(MoCA)评分均较治疗前上升,试验组操作智商(PIQ)、言语智商(VIQ)、总智商(FIQ)、言语理解因子智商、知觉组织因子智商及不分心/记忆因子智商分数及MoCA评分均高于对照组(P<0.05)。2组治疗4个月后θ、α、δ脑电频率均较治疗前稳定,试验组θ、α、δ脑电频率优于对照组(P<0.05)。结论 对癫痫患儿采用丙戊酸钠与左乙拉西坦联合治疗可显著提升疗效、智力及认知水平,控制痫性放电。

丙戊酸钠促进神经根回植术后神经元存活的机制研究

目的探讨丙戊酸钠对大鼠臂丛神经根回植术后脊髓神经元保护的作用机制。方法将成年大鼠随机分为空白组、手术组和丙戊酸钠组。手术组和丙戊酸钠组对大鼠行臂丛根性撕脱伤后神经根回植术,其中丙戊酸钠组通过饮水喂食丙戊酸钠。术后第1、2、3、7、14天收集相应节段脊髓,应用TUNEL法检测神经元凋亡情况,应用Western blot法及实时荧光定量PCR检测Bcl-2的表达情况。结果TUNEL法检测在术后第1、2天未发现凋亡细胞,术后第3~14天发现凋亡神经元,术后第3、7天丙戊酸钠组凋亡神经元个数少于手术组(P<0.05);应用Western blot法检测发现,术后第2、3、7天丙戊酸钠组Bcl-2的蛋白表达明显高于手术组(P<0.05);应用实时荧光定量PCR检测Bcl-2的mRNA表达发现,术后第2、3、7天丙戊酸钠组Bcl-2的mRNA表达明显高于手术组(P<0.05)。结论臂丛根性撕脱伤行神经根回植术后早期应用丙戊酸钠可以抑制神经元的凋亡,其机制可能是通过促进脊髓内部Bcl-2表达、抑制凋亡信号传导路径而实现的。

VPA和As2O3对Molt-4细胞的协同作用及可能机制

本研究探讨丙戊酸钠(sodium valproate,VPA)单药或与亚砷酸(arsenie trioxide,As2O3)联用对人急性T细胞白血病细胞株Molt-4增殖活力的抑制、去甲基化作用及其可能机制。用MTT法检测药物对细胞增殖的抑制作用,利用金氏公式观察两药联用体外抗癌的协同作用。采用半巢式甲基化特异PCR(hnMS-PCR)检测p15INK4B基因甲基化,RT-PCR方法检测p15基因、DNA甲基转移酶DNMT-1、DNMT3A、DNMT3B的表达。结果表明:VPA和As2O3均可明显抑制细胞增殖,二者联用在体外有相加作用(Q值均大于0.85),在5mmol/L VPA与10μmol/L As2O3联用时抑制率达(70.31±2.54)%。Molt-4细胞p15基因因高甲基化而失表达,经VPA和As2O3联合作用后p15基因甲基化程度明显下降,p15基因表达增强,两药联用时DNMT-1、DNMT-3A、DNMT3BmRNA的表达都有下降。结论:VPA可能通过抑制DNA甲基转移酶DNMT-1和(或)DNMT3B使p15INK4B基因去甲基化,使p15基因表达上调,恢复其活性。VPA和As2O3均可明显抑制Mol-4细胞增殖,两药合用有协同相加作用,可减少砷剂的副作用。

左乙拉西坦联合奥卡西平、丙戊酸钠对良性癫痫伴中央颞区棘波合并睡眠中癫痫性电持续状态患儿临床症状、认知功能的影响

目的:探究左乙拉西坦联合奥卡西平、丙戊酸钠对良性癫痫伴中央颞区棘波(BECT)合并睡眠中癫痫性电持续状态(ESES)患儿临床症状、认知功能的影响。方法:选取2020年4月~2022年4月在某院接受治疗的100例BECT合并ESES患儿作为研究对象,采用随机数字表法分为对照组和观察组,每组50例。对照组给予奥卡西平和丙戊酸钠,而观察组在对照组治疗基础上加用左乙拉西坦,比较两组临床疗效、治疗前后脑电图改善情况及脑电活动情况,并对患儿治疗前后的认知情况进行评价,记录患儿在治疗期间的不良反应发生情况。结果:治疗后,观察组患儿的治疗有效率(92.00%)高于对照组(76.00%,P<0.05)。观察组患儿脑电图改善总有效率(74.00%)高于对照组(46.00%,P<0.05)。两种治疗方案均可影响患儿的脑电波活动,特别是在α、β、θ、δ波段,且与对照组相比,观察组患者在这些波段的变化更为显著(P<0.05)。治疗前,两组在操作智商、全量表智商、言语智商方面的得分无统计学差异(P>0.05);治疗后,观察组各评分均升高,且优于对照组(P<0.05)。两组患儿不良反应发生率比较无统计学差异(P>0.05)。结论:与奥卡西平联合丙戊酸钠的治疗方案比较,左乙拉西坦联合奥卡西平和丙戊酸钠治疗儿童BECT合并ESES的疗效更优,能够有效提高患儿的治疗有效率和脑电图改善总有效率,提高患儿的认知功能。

丙戊酸钠治疗成人癫痫合并非酒精性脂肪性肝病的临床研究进展

癫痫患者易发生肥胖和代谢综合征,其风险高于一般人群,非酒精性脂肪性肝病(NAFLD)是代谢综合征的一种表现,以肝脂肪变性为主要特征,在一定程度上可加重癫痫患者病情。丙戊酸钠作为临床常用抗癫痫药物,可导致肝细胞内三酰甘油蓄积,诱发NAFLD风险。对于成人癫痫合并NAFLD患者,使用丙戊酸钠治疗,会使已经受脂肪变性影响的肝脏更易引起损伤,影响丙戊酸钠代谢。丙戊酸钠和NAFLD均可诱导肝脏脂肪变性,在癫痫治疗过程中可加重彼此诱导的肝脂肪变性,具有协同作用。该文就丙戊酸钠应用于成人癫痫合并NAFLD患者的临床研究进展进行综述,以期为相关研究提供参考。