褪黑素对谷氨酸钠致痫大鼠海马5-羟色胺水平的影响

目的观察褪黑素(Melatonin,MT)对谷氨酸钠(Glutamate,Glu)致痫大鼠海马5-羟色胺(5-hydroxytryptamine,5-HT)水平的影响,研究其抑制癫痫的作用机制。方法40只健康雄性SD大鼠随机分为4组(每组10只),分别为生理盐水对照组(NS组);谷氨酸钠致痫组(Glu组);褪黑素 谷氨酸钠组(MT Glu组);Luzidole 褪黑素 谷氨酸钠组(Luz MT Glu组)。观察并记录大鼠行为学及脑电图改变,用免疫组织化学方法检测大鼠海马内5-HT含量变化。结果行为学观察和EEG显示,NS组无痫样发作和痫样放电,Glu组和Luz MT Glu组痫样发作重(Ⅲ-Ⅴ级),脑电图显示频发高幅的痫样波,TM Glu组无或仅有轻微发作(0-Ⅱ级),脑电图上无或偶见散在单个微小痫样波;免疫组织化学分析结果显示,Glu组和Luz MT Glu组大鼠海马内5-HT含量与对照组比较均减少,差异性明显(P<0.05),MT Glu组较Glu组和Luz MT Glu组5-HT含量升高,差异性明显(P<0.05)。结论MT对谷氨酸钠致痫大鼠痫样发作程度、痫样放电有抑制作用,其机制之一是经由其特异性的膜受体,通过某种机制增强5-HT作用,进而发挥抑痫效应。     

褪黑素对谷氨酸致痫大鼠海马内谷氨酸、GABA及其受体水平的影响

目的探讨褪黑素(melatonin,MT)对谷氨酸(glutamate,Glu)致痫大鼠海马内Glu及GluR2、γ-氨基丁酸(γ-aminobutyric-acid,GABA)及其受体GABRA1水平的影响,进而研究褪黑素的抑痫作用机制。方法随机将健康SD雄性大鼠40只分为A、B、C、D组,每组10只。A组:生理盐水组;B组:MT Glu组;C组:Glu致痫组;D组:Luzidole MT Glu组。观察并记录行为学变化,采用免疫组化法进行Glu、GluR2、GABA和GABRA1免疫组化染色和图像分析。结果行为学观察结果显示,C组和D组大鼠均有不同程度的癫痫发作,B组大鼠癫痫发作不明显,A组无发作;免疫组化结果显示,C组和D组海马内CA1-CA3区和齿状回Glu阳性反应较A组增强(P<0.05),GluR2、GABA和GABRA1均较A组减弱(P<0.05),B组Glu较C组和D组阳性反应有显著性减弱(P<0.05),GluR2、GABA和GABRA1阳性反应均较C组和D组有显著性增强(P<0.05),而B组与A组无明显差异性。结论MT通过增加GABA及其受体GABRA1和GluR2的作用和抑制Glu作用对Glu致痫大鼠癫痫发作发挥抑制作用。     

褪黑素对谷氨酸钠致痫大鼠脑内一氧化氮含量的影响

目的观察褪黑素(Melatonin,MT)对谷氨酸钠致痫大鼠脑内一氧化氮(nitric oxide,NO)含量的影响,研究其抑制癫痫的作用机制。方法40只健康雄性SD大鼠随机分为4组(每组10只):生理盐水对照组(NS组);谷氨酸钠致痫组(Glu组);褪黑素+谷氨酸钠组(MT+Glu组);Luzidole+褪黑素+谷氨酸组(Luz+MT+Glu组)。观察大鼠行为变化,记录脑电图,用NADPH组织化学反应检测大鼠海马内NO含量变化。结果行为学观察和EEG显示,NS组无痫样发作和痫样放电,Glu组和Luz+MT+Glu组痫样发作重(Ⅲ-Ⅴ级),脑电图显示频发高幅的痫样波,MT+Glu组有轻微发作(0-Ⅱ级),脑电图上偶见散在单个微小痫样波;NADPH组织化学反应结果显示,Glu组和Luz+MT+Glu组大鼠大脑皮质及海马内NOS阳性细胞与对照组比较增多,差异性明显(P<0.05),MT+Glu组较Glu组和Luz+MT+Glu组内NOS阳性细胞减少,差异性明显(P<0.05)。结论MT对谷氨酸钠致痫大鼠痫样发作程度、痫样放电有抑制作用,其机制之一是经其特异性受体,减弱NO作用,进而发挥抑痫效应。     

褪黑素对谷氨酸钠致痫大鼠海马5-色胺水平的影响

目的观察褪黑素（Melatonin,MT）对谷氨酸钠（Glutamate,Glu）致痫大鼠海马5-羟色胺（5-hydroxytryptamine,5-HT）水平的影响,研究其抑制癫痫的作用机制。方法40只健康雄性SD大鼠随机分为4组（每组10只）,分别为生理盐水对照组（NS组）;谷氨酸钠致痫组（Glu组）;褪黑素＋谷氨酸钠组（MT＋Glu组）;Luzidole＋褪黑素＋谷氨酸钠组（Luz＋MT＋Glu组）。观察并记录大鼠行为学及脑电图改变,用免疫组织化学方法检测大鼠海马内5-HT含量变化。结果行为学观察和EEG显示,NS组无痫样发作和痫样放电,Glu组和Luz＋MT＋Glu组痫样发作重（Ⅲ—Ⅴ级）,脑电图显示频发高幅的痫样波,TM＋Glu组无或仅有轻微发作（0-Ⅱ级）,脑电图上无或偶见散在单个微小痫样波;免疫组织化学分析结果显示,Glu组和Luz＋MT＋Glu组大鼠海马内5-HT含量与对照组比较均减少,差异性明显（P〈0．05）,MT＋Glu组较Glu组和Luz＋MT＋Glu组5-HT含量升高,差异性明显（P〈0．05）。结论MT对谷氨酸钠致痫大鼠痫样发作程度、痫样放电有抑制作用,其机制之一是经由其特异性的膜受体,通过某种机制增强5-HT作用,进而发挥抑痫效应。     

褪黑素对马桑内酯致痫大鼠海马内SP水平的影响

目的探讨褪黑素（melatonin,MT）对马桑内酯致痫大鼠海马内P物质水平的影响,以探讨褪黑素的抑痫作用机制。方法随机将健康成年雄性SD大鼠40只分为A、B、C、D 4组,每组10只。A组：生理盐水组;B组：马桑内酯组;C组：褪黑素＋马桑内酯组;D组：Luzindole＋褪黑素＋马桑内酯组。观察并记录行为学变化,然后分别采用免疫组织化学方法进行SP免疫组织化学染色,实时荧光定量PCR方法检测海马内SP mRNA含量变化。结果B组和D组大鼠均有不同程度的癫痫发作,而C组大鼠癫痫发作不明显,A组几乎均无发作;免疫组化结果显示,四组大鼠海马各区均有SP免疫反应阳性神经元,B组、D组与A组、C组比海马内SP免疫阳性反应明显增强（P〈0.05）,而A组与C组比无明显差异（P〉0.05）;RT-PCR结果提示,B组、D组与A组、C组相比,大鼠海马内SP mRNA明显升高（P〈0.05）,而A组与C组比无明显差异（P〉0.05）。结论MT能通过下调海马内SP水平抑制癫痫发作。     

氯喹对戊四氮致痫大鼠皮质和海马谷氨酸和NMDAR1表达的影响

目的观察氯喹对戊四氮致痫大鼠皮质和海马谷氨酸(glutamate,Glu)和N-甲基-D-天冬氨酸受体1(NMDAR1,NR1)表达的影响,探讨氯喹在癫痫发生发展过程中对神经递质传导的作用。方法48只健康雄性SD大鼠随机分为对照组(12只)、戊四氮致痫组(60mg/kg,i.p.,18只)和氯喹干预组(0.61mg/kg,i.c.v.,18只)。每组分6个时间点:1h、2h、4h、8h、12h和24h。观察大鼠行为表现和脑电图改变,用免疫组化检测大鼠皮质和海马Glu和NR1的变化。结果对照组无痫样发作,戊四氮致痫组有重型的痫样发作(Ⅲ-Ⅴ级),氯喹干预组有轻型的痫样发作(Ⅰ-Ⅲ级)(P<0.05);戊四氮致痫组脑电记录呈频发高幅的痫样波,氯喹干预组痫样波幅低且缓;Glu和NR1在戊四氮致痫组表达强,以海马为著,与对照组比较有显著性差异(P<0.05),氯喹干预组与对照组比较无显著性差异(P>0.05)。结论氯喹通过对戊四氮致痫大鼠皮质和海马神经递质Glu和NR1信号传导通路的抑制作用,影响致痫大鼠痫样发作的发生和发展。     

褪黑素对马桑内酯致痫大鼠海马及皮质内TNF—α水平的影响

目的观察褪黑素（melatonin,MT）对马桑内酯（coriaria lactone,CL）致痫大鼠海马及皮质内TNF-α水平的影响,探讨其抑制癫痫的作用机制。方法60]5健康雄性SD大鼠随机分为4组（每组15只）,分别为A组：生理盐水对照组（NS组）;B组：马桑内酯致痫组（CL组）;C组：褪黑素＋马桑内酯组（MT＋CL组）;D组：Luzidole＋褪黑素＋马桑内酯组（Luz＋MT＋CL组）。观察并记录火鼠行为学改变,用免疫组织化学方法检测大鼠海马及皮质内TNF-α含量的变化。用实时荧光定量PCR的方法检测大鼠海马内TNF—dmRNA含量的变化。结果行为学观察,NS组无痫样发作,CL组和Luz＋MT＋CL组痫样发作重（Ⅲ—Ⅴ级）,MT＋CL组无或仅有轻微发作（0-Ⅱ级）;免疫组织化学观察,与正常对照组比较,CL组和Luz＋MT＋CL组大鼠海马及皮质内TNF-α含量均明显增高（P〈0．05）;与CL组和Luz＋MT＋CL组比较,MT＋CL组TNF-α含量明显降低（P〈0．05）。实时荧光定量PCR结果显示,与正常对照组比较,CL组和Luz＋MT＋CL组大鼠海马TNF-αmRNA含量均明显增高（P〈0．05）;与CL组和Luz＋MT＋CL组比较,MT＋CL组大鼠海马TNFQmRNA含量明显降低（P〈0．05）;结论褪黑素能明显地抑制马桑内酯引起的致痫作用,其机制可能与影响海马及皮质内TNF-α水平有关。     

功率谱熵在痫性发作大鼠脑电检测中的应用研究

目的:研究功率谱熵在痫性发作大鼠脑电检测中的应用。方法:采用青霉素在大鼠海马微注射制备急性痫性发作模型,以深部电极记录大鼠原始脑电信号,将24只SD大鼠随机分成四组,即正常组(A),对照组(B),单电极组(C),多电极组(D)。C、D组大鼠经致痫后观察未发作期、发作前期、发作期和发作后期四期脑电信号的变化,运用谱熵对四期脑电信号进行分析,并与A、B组进行对比。结果:C组和D组脑电功率谱熵显示两组发作期与未发作期、发作前期、发作后期比较有显著差异(P0.05),发作期明显低于其它各期;未发作期和发作前期相比有明显差异(P0.05),发作前期较未发作期降低;将D组大鼠海马致痫灶(a)及其同侧附近(b)、对侧(c)三点发作各期脑电功率谱熵进行对比分析,发作前期和发作期a、b、c三点比较有明显差异(P0.05),a点最低,c点的功率谱熵值最高。结论:功率谱熵可以预报痫性发作并可对癫痫病灶的定位提供一定的帮助。     

IL-1β对L-谷氨酸致痫大鼠大脑皮质、海马PLCβ1表达的影响

目的探讨白细胞介素-1β(Interleukin-1 beta,IL-1β)对L-谷氨酸致痫大鼠大脑PLCβ1表达的影响,为阐明IL-1β在致痫中的作用机制提供资料.方法随机将健康成年SD大鼠分为5组,每组8只,即对照组、Glu组、IL-1β Glu组、IL-1ra IL-1β Glu组和MPEP IL-1β Glu组,采用行为学及Western blot和免疫组织化学方法进行研究.结果行为观察显示,对照组、IL-1ra IL-1β Glu组和MPEP组无痫性发作;Western blot结果显示PLCβ1含量在Glu组和IL-1β Glu组大鼠鼠脑皮质及海马内均较对照组、IL-1ra IL-1β Glu组和MPEP IL-1β Glu组明显增多(P<0.05),而对照组、IL-1ra IL-1β Glu组和MPEP IL-1β Glu组组间无明显差别(P>0.05);免疫组织化学染色显示,PLCβ1免疫反应增强主要表现在海马CA3区和大脑皮质,各组间的变化规律与Western blot检测结果一致.结论 IL-1β对L-谷氨酸致痫有促进作用,mGluR5介导的PLCβ1激活参与了IL-1的促痫机制.     

氯喹对戊四氮致痫大鼠皮质和海马白细胞介素1β及肿瘤坏死因子α表达的影响

目的观察氯喹对戊四氮致痫大鼠皮质和海马白细胞介素1β(IL-1β)及肿瘤坏死因子α(TNF-α)表达的影响,探讨其在癫痫发生发展过程中的作用.方法 48只健康雄性SD大鼠随机分为对照组(12只)、戊四氮(PTZ)致痫组(18只,60mg/kg,i.p.)和氯喹干预组(18只,氯喹0.61mg/kg,i.c.v.,2h后注射PTZ).每组确定6个时间点:1h、2h、4h、8h、12h和24h.观察大鼠行为表现,记录脑电改变,用免疫组化检测皮质和海马IL-1β和TNF-α表达的变化.结果对照组无痫样发作和痫样放电,戊四氮致痫组痫样发作重(Ⅲ-Ⅴ级),氯喹干预组轻(Ⅰ-Ⅲ级)(P<0.05);脑电记录显示戊四氮致痫组呈频发高幅的痫样波,氯喹干预组痫样波幅低且缓;LI-1β和TNF-α在戊四氮致痫组皮质和海马表达强,与对照组比较差异有显著性(P<0.05),氯喹干预组与对照组比较差异无显著性(P>0.05).结论氯喹可能通过对IL-1β和TNF-α表达的抑制减轻戊四氮致痫大鼠的痫样放电和痫样发作程度.这些结果提示,氯喹在防治癫痫方面可能是理想的抗痫剂.     

The relation between reduced serum melatonin levels and zinc in rats with induced hypothyroidism

The objective of the study was to explore the changes in melatonin and zinc levels in rats with induced hypothyroidism. Thirty adult male rats used in the study were allocated to three groups with equal numbers. Group 1: General control group which was not subjected to any procedure. Group 2: Sham-hypothyroidism group to which was administered 10 mg kg(-1) intraperitoneal (i.p.) physiologic saline (0.09% NaCl) for 4 weeks. Group 3: Hypothyroidism group which was supplemented with intraperitoneal 10 mg kg(-1) propylthiouracil (PTU) for 4 weeks. Blood samples collected from all animals at the end of the study by decapitation were analysed for serum Total T4 (TT4), Total T3 (TT3), Free T4 (FT4), Free T3 (FT3) (ELISA) as well as for melatonin (RIA) hormones and zinc levels (atomic emission). Comparison of the study groups in terms of thyroid hormones, melatonin and zinc levels showed that TT4, TT3, FT4, FT3, melatonin and zinc levels in group 3 were lower than those in groups 1 and 2 (p < 0.01). These parameters were not different in groups 1 and 2. The results of the study demonstrate that PTU supplementation for 4 weeks results in a significant inhibition in both melatonin and zinc levels. Inhibited melatonin levels may result from the decrease in zinc levels.     

脑内5-羟色胺减少对致痫大鼠癫痫发作及学习记忆的影响

目的:于中脑正中中缝核局部微量注射5,7-二羟色胺(5,7-DHT),探讨5-羟色胺(5-HT)与癫痫的关系及匹罗卡品(PILO)致痫大鼠学习记忆改变的可能机制。方法:成年SD大鼠随机分为PILO组、PILO+5,7-DHT组、空白对照组三组,然后根据是否出现癫痫持续状态(SE)再将PILO组分成:PILO+SE组和PILO-SE组两亚组;利用视频脑电图观察大鼠癫痫发作及皮层脑电变化;运用Morris水迷宫测评大鼠空间学习记忆水平;最后运用免疫组化法观察大鼠中缝核5-HT能神经元。结果:大鼠予以5,7-DHT(PILO+5,7-DHT组)处理后造模成功率、死亡率及慢性期自发性发作频率均增高;与空白组比较PILO+SE组中缝核5-HT能神经元数目有所下降(P<0.05),而PILO+5,7-DHT组下降更明显(P<0.01);与空白组比较PILO+SE组平均逃避潜伏期延长、穿越平台次数减少、原平台象限停留时间缩短(P<0.05),而与PILO+SE组比较PILO+5,7-DHT组变化不明显。结论:脑内5-HT水平的降低容易诱发癫痫发作,尚不能认为癫痫大鼠合并认知功能障碍与脑内5-HT水平下降有关。     

Effects of melatonin on oxidative-antioxidative status of tissues in streptozotocin-induced diabetic rats

In view of the antioxidant properties of melatonin, the effects of melatonin on the oxidative-antioxidative status of tissues affected by diabetes, e.g. liver, heart and kidneys, were investigated in streptozotocin (STZ)-induced diabetic rats in the present study. Concentrations of malondialdehyde (MDA) and reduced glutathione (GSH), and activities of superoxide dismutase (SOD) and glutathione peroxidase (GSH-Px) in the tissues were compared in three groups of 10 rats each (control non-diabetic rats (group I), untreated diabetic rats (group II) and diabetic rats treated with melatonin (group III)). In the study groups, diabetes developed 3 days after intraperitoneal (i.p.) administration of a single 60 mg kg(-1) dose of STZ. Thereafter, while the rats in group II received no treatment, the rats in group III began to receive a 10 mg kg(-1) i.p. dose of melatonin per day. After 6 weeks, the rats in groups II and III had significantly lower body weights and higher blood glucose levels than the rats in group I (p < 0.001 and p < 0.001, respectively). MDA levels in the liver, kidney and heart of group II rats were higher than that of the control group (p < 0.01, p < 0.05, p < 0.01, respectively) and diabetic rats treated with melatonin (p < 0.05). The GSH, GSH-Px and SOD levels increased in diabetic rats. Treatment with melatonin changed them to near control values. Our results confirm that diabetes increases oxidative stress in many organs such as liver, kidney and heart and indicate the role of melatonin in combating the oxidative stress via its free radical-scavenging and antioxidant properties.     

Sensory nerves in central and peripheral control of pancreatic integrity by leptin and melatonin.

Central nervous system affects pancreatic secretion of enzymes however, the neural modulation of acute pancreatitis has not been investigated. Leptin and melatonin have been recently reported to affect the inflammatory response of various tissues. The identification of specific receptors for both peptides in the pancreas suggests that leptin and melatonin could contribute to the pancreatic protection against inflammation. The aim of this study was: 1/ to compare the effect of intracerebroventricular (i.c.v.) or intraperitoneal (i.p.) administration of leptin or melatonin on the course of caerulein-induced pancreatitis (CIP) in the rat, 2/ to examine the involvement of sensory nerves (SN) and calcitonin gene-related peptide (CGRP) in pancreatic protection afforded by leptin or melatonin, 3/ to assess the effect of tested peptides on lipid peroxidation products (MDA + 4-HNE) in the pancreas of CIP rats, 4/ to investigate the influence of leptin or melatonin on nitric oxide (NO) release from isolated pancreatic acini and 5/ to determine the effects of caerulein and leptin on leptin receptor gene expression in these acini by RT-PCR. CIP was induced by subcutaneous (s.c.) infusion of caerulein (25 microg/kg) to the conscious rats, confirmed by the significant increases of pancreatic weight and plasma amylase and by histological examination. This was accompanied in marked reduction of pancreatic blood flow and significant rise of MDA + 4-HNE in the pancreas. Leptin or melatonin were administered i.p. or i.c.v. 30 min prior to the start of CIP. Deactivation of SN was produced by s.c. capsaicin (100 mg/kg). An antagonist of CGRP, CGRP 8-37 (100 microg/kg i.p.), was given together with leptin or melatonin to the CIP rats. MDA + 4-HNE was measured using LPO commercial kit. NO was determined using the Griess reaction. Pretreatment of CIP rats with i.p. leptin (2 or 10 microg/kg) or melatonin (10 or 50 mg/kg) significantly attenuated the severity of CIP. Similar protective effects were observed following i.c.v. application of leptin (0.4 or 2 microg/rat) but not melatonin (10 or 40 microg/rat) to the CIP rats. Capsaicin deactivation of SN oradministration of CGRP 8-37 abolished above beneficial effects of leptin on CIP, whereas melatonin-induced protection of pancreas was unaffected. Pretreatment with i.p. melatonin (10 or 50 mg/kg), but not leptin, significantly reduced MDA + 4-HNE in the pancreas of CIP rats. Leptin (10(-10) - 10(-6) M) but not melatonin (10(-8) - 10(-5) M) significantly stimulated NO release from isolated pancreatic acini. Leptin receptor gene expression in these acini was significantly increased by caerulein and leptin. We conclude that 1/ central or peripheral pretreatment with leptin protects the pancreas against its damage induced by CIP, whereas melatonin exerts its protective effect only when given i.p., but not following its i.c.v. adminstration, 2/ activation of leptin receptor in the pancreatic acini appears to be involved in the beneficial effects of leptin on acute pancreatitis, 3/ the protective effects of leptin involve sensory nerves, CGRP and increased generation of NO whereas melatonin-induced protection of the pancreas depends mainly on the antioxidant local effect of this indole, and scavenging of the radical oxygen species in the pancreatic tissue.     

Both zinc deficiency and supplementation affect plasma melatonin levels in rats

At physiological levels, zinc and various hormones affect each other reciprocally. Reduction in zinc levels in pinealectomized rats suggests the relation between zinc and melatonin. The effect of both zinc deficiency and supplementation on plasma melatonin levels in rats were investigated in this study. The study was done in Sel?uk University, Experimental Medicine Research and Application Center. Twenty-four adult male Sprague Dawley rats were divided into 3 groups. Eight rats were fed with zinc-deficient diet. Zinc supplementation was administered intaperitoneally to 8 rats. The remaining 8 rats were used as controls. All rats sacrificed 3 weeks later. Plasma melatonin and zinc levels were determined. The plasma zinc levels of the zinc-supplemented group were higher than those of the other groups as expected (P<0.01). Similarly, the melatonin levels in the zinc-supplemented group were higher than those in the other groups. A significant decrease was observed in melatonin levels of the zinc-deficient group compared to the control and zinc-supplemented group (P<0.01). The results of this study suggest that zinc deficiency decreases the melatonin levels and zinc supplementation may increase the plasma melatonin levels in rats.     

多巴胺联合NE对感染性休克致急性肝损伤大鼠肝功能、炎性因子及NF-κB p65蛋白的影响

目的:本研究通过研究多巴胺(Dopamine,DA)和去甲肾上腺素(Noradrenaline,NE)对感染性休克致急性肝损伤大鼠肝功能、炎性因子及NF-NF-κB p65蛋白的影响,以期为临床治疗提供一定的试验依据。方法:以48只SPF级健康雄性SD大鼠为研究对象,根据随机数字表法分为四组,每组12只,分别为对照组,脂多糖(lipopolysaccharide,LPS)组,NE组,DA+NE组。LPS、NE和DA+NE建立感染性休克模型,NE组静脉输注去甲肾上腺素,DA+NE组在NE组的基础上静脉输注DA。对各组大鼠肝功能、炎性因子和NF-κB p65蛋白水平进行检测。结果:与对照组相比,LPS、NE和DA+NE组血清天冬氨酸转氨酶(aspartate transaminase,AST)和丙氨酸转氨酶(alanine Transaminase,ALT)水平均显著升高(P<0.05),与LPS组相比,NE和DA+NE组大鼠血清AST和ALT均有不同程度的降低(P<0.05),与NE组相比,DA+NE组大鼠血清AST和ALT水平降低更显著(P<0.05)。与对照组相比,LPS、NE和DA+NE组血清白细胞介素6(interleukin-6,IL-6)和肿瘤坏死因子(tumornecrosis factor,TNF-α)水平均显著升高(P<0.05),与LPS组相比,NE和DA+NE组大鼠血清IL-6和TNF-α均有不同程度的降低(P<0.05),与NE组相比,DA+NE组大鼠血清IL-6和TNF-α水平降低更显著(P<0.05)。与对照组相比,LPS、NE和DA+NE组NF-κB p65蛋白表达水平均显著升高(P<0.05),与LPS组相比,NE和DA+NE组大鼠NF-κB p65蛋白表达均有不同程度的降低(P<0.05),与NE组相比,DA+NE组大鼠NF-κB p65蛋白表达水平降低更显著(P<0.05)。结论:多巴胺联合NE对对大鼠感染性休克所导致的急性肝损伤具有良好的保护作用。