Therapy for acute pancreatitis with platelet-activating factor receptor antagonists

Acute pancreatitis (AP) causes release of platelet- activating factor (PAF), which induces systemic effects that contribute to circulatory disturbances and multiple organ failure. PAF is a cell surface secretion of bioactive lipid, which could produce physiological and pathological effects by binding to its cell surface receptor called platelet-activating factor receptor (PAF-R). Studies showed that PAF participates in the occurrence and development of AP and administration of platelet-activating factor receptor antagonists (PAF-RAs) could significantly reduce local and systemic events after AP. PAF has also been implicated as a key mediator in the progression of severe AP, which can lead to complications and unacceptably high mortality rates. Several classes of PAF-RA show PAF- RAs significant local and systemic effects on reducing inflammatory changes. As a preventive treatment, PAF-RA could block a series of PAF-mediated inflammatory injury and thus improve the prognosis of AP. This review introduces the important role of PAF-RA in the treatment of AP.

Predictors and optimal management of tumor necrosis factor antagonist nonresponse in inflammatory bowel disease:A literature review

Tumor necrosis factor-α(TNF-α)antagonists,the first biologics approved for treating patients with inflammatory bowel disease(IBD),are effective for the induction and maintenance of remission and significantly improving prognosis.However,up to one-third of treated patients show primary nonresponse(PNR)to anti-TNF-αtherapies,and 23%-50%of IBD patients experience loss of response(LOR)to these biologics during subsequent treatment.There is still no recognized predictor for evaluating the efficacy of anti-TNF drugs.This review summarizes the existing predictors of PNR and LOR to anti-TNF in IBD patients.Most predictors remain controversial,and only previous surgical history,disease manifestations,drug concentrations,antidrug antibodies,serum albumin,some biologic markers,and some genetic markers may be potentially predictive.In addition,we also discuss the next steps of treatment for patients with PNR or LOR to TNF antagonists.Therapeutic drug monitoring plays an important role in treatment selection.Dose escalation,combination therapy,switching to a different anti-TNF drug,or switching to a biologic with a different mechanism of action can be selected based on the concentration of the drug and/or antidrug antibodies.

Hypoxia inducible factor 1α promotes interleukin-1 receptor antagonist expression during hepatic ischemia-reperfusion injury

BACKGROUND Ischemia-reperfusion injury(IRI) is a major risk associated with liver surgery and transplantation,and its pathological mechanism is complex.Interleukin-1 receptor antagonist(IL-1ra) can protect the liver from IRI.However,the regulatory mechanism of IL-1ra expression is still unclear.AIM To identify the mechanism that could protect the liver in the early stage of IRI.METHODS To screen the key genes in hepatic IRI,we performed RNA sequencing and gene enrichment analysis on liver tissue from mice with hepatic IRI.Subsequently,we verified the expression and effect of IL-1ra in hepatic IRI.We also used promoter mutagenesis and chromatin immunoprecipitation assay to search for the transcriptional regulatory sites of hypoxia-inducible factor(HIF)-1α.Finally,to explore the protective mechanism of ischemic preconditioning(IP),we examined the expression of HIF-1α and IL-1ra after IP.RESULTS We identified IL-1ra as a key regulator in hepatic IRI.The expression of IL-1ra was significantly upregulated after hepatic IRI both in vivo and in vitro.Furthermore,we found that HIF-1αregulated Il-1ra transcription in response to hypoxia.Increased HIF-1α accumulation promoted IL-1ra expression,whereas inhibition of HIF-1α exhibited the opposite effect.We also confirmed a predominant role for hypoxia response element in the regulation of Il1ra transcription by HIF-1αactivation.Of note,we demonstrated that IP protects against hepatic IRI by inducing IL-1ra expression,which is mediated through HIF-1α.CONCLUSION We demonstrated that ischemia or hypoxia leads to increased expression of IL-1ra through HIF-1α.Importantly,IP protects the liver from IRI via the HIF-1α–IL-1ra pathway.

The interleukin-1 receptor antagonist (IL-1-Ra) and soluble tumor necrosis factor receptor I (sTNF RI) in periodontal disease

The course and severity of periodontitis can be significantly affected by bacterial virulence as well as host immunity dysfunction. Periodontal tissue destruction has been proved to result from cascade of cytokines synthesized by reactive cells upon stimulation by pathogenic bacteria and lipopolysaccharides within their cell membranes. The clinical use of genetically programmed cells, producing substances blocking IL-1, based on recombinant IL-1 antagonist, as well as cytokines activating fibroblasts and osteoblasts to regenerate the destroyed periodontal tissue could prove alternative to the conventional treatment. Another cytokine of interest in respect to periodontitis ethiopathogenesis is soluble tumor necrosis factor receptor I (sTNF RI). Observation of soluble TNF receptors as physiologic inhibitors of TNF led to its administration in therapeutic process as well as in therapy selected cases of aggressive periodontitis.

Autoimmune hepatitis and anti-tumor necrosis factor alpha therapy:A single center report of 8 cases

This article describes cases of anti-tumor necrosis factor(TNF)-α-induced autoimmune hepatitis and evaluates the outcome of these patients in relation to their immunosuppressive strategy. A retrospective analysis of medical records was performed in our center, in order to detect cases of autoimmune hepatitis(AIH) associated with anti-TNF biologic agents. We describe and analyze eight cases of AIH following anti-TNF therapy, 7 with infliximab and 1 with adalimumab. A distinction should be made between induction of autoimmunity and clinically evident autoimmune disease. Liver biopsy is useful in detecting the role of the TNF-α antagonist in the development of AIH. The lack of relapse after discontinuing immunosuppressive therapy favors, as in this case series, an immune-mediated drug reaction as most patients with AIH have a relapse after treatment is suspended. Although AIH related to anti-TNF therapy is rare, a baseline immunological panel along with liver function tests should be performed in all patients with autoimmune disease before starting biologics.

Transcription factors specificity protein and nuclear receptor 4A1 in pancreatic cancer

Specificity protein(Sp)transcription factors(TFs)Sp1,Sp3 and Sp4,and the orphan nuclear receptor 4A1(NR4A1)are highly expressed in pancreatic tumors and Sp1 is a negative prognostic factor for pancreatic cancer patient survival.Results of knockdown and overexpression of Sp1,Sp3 and Sp4 in pancreatic and other cancer lines show that these TFs are individually pro-oncogenic factors and loss of one Sp TF is not compensated by other members.NR4A1 is also a prooncogenic factor and both NR4A1 and Sp TFs exhibit similar functions in pancreatic cancer cells and regulate cell growth,survival,migration and invasion.There is also evidence that Sp TFs and NR4A1 regulate some of the same genes including survivin,epidermal growth factor receptor,PAX3-FOXO1,α5-andα6-integrins,β1-,β3-andβ4-integrins;this is due to NR4A1 acting as a cofactor and mediating NR4A1/Sp1/4-regulated gene expression through GC-rich gene promoter sites.Several studies show that drugs targeting Sp downregulation or NR4A1 antagonists are highly effective inhibitors of Sp/NR4A1-regulated pathways and genes in pancreatic and other cancer cells,and the triterpenoid celastrol is a novel dual-acting agent that targets both Sp TFs and NR4A1.

香蕉抗枯萎病株系内生菌的分离鉴定及抑菌促生效果

【目的】筛选和鉴定从威廉斯香蕉抗枯萎病株系根、球茎及假茎分离得到的可抑制香蕉枯萎病菌(Fusarium oxysporum f.sp.cubense,Foc)内生菌,研究其抑菌促生效果。【方法】通过16S rRNA基因序列测定和生理生化试验,对香蕉抗枯萎病株系内生菌进行种类鉴定和系统发育分析;通过平板对峙试验检测各菌株的抑菌能力,探究拮抗菌分泌抑菌相关活性物质的种类;采用盆栽试验对香蕉抗枯萎病株系内生菌进行生防功能和促生功能的分析,筛选出生防性能优良且兼具促生效果的内生菌,并在大田试验中验证。【结果】分离获得13株代表菌株,其中8株对枯萎病1号生理小种(Foc 1)具有抑菌活性,7株对枯萎病4号生理小种(Foc 4)具有抑菌活性;综合盆栽试验和大田试验中代表菌株的防治效果及促生能力,筛选出贝莱斯芽孢杆菌XG1028、变栖克雷伯氏菌XQJ0301和暹罗芽孢杆菌XG0103共3株具备高抑菌活性以及促生能力的生防菌株。【结论】本研究筛选出的3株菌株丰富了抗香蕉枯萎病微生物种质资源,为防治香蕉枯萎病寻找安全、环保的新型生物防治剂提供参考。

选择性钙通道拮抗剂辅助治疗对溃疡性结肠炎患者血清炎性因子及肠道菌群的影响研究

目的:探索选择性钙通道拮抗剂(SCCBs)辅助治疗对溃疡性结肠炎(UC)患者血清炎性因子及肠道菌群的影响。方法:选取2018年2月—2020年3月河南大学第一附属医院收治的86例UC患者作为研究对象,采用区组随机化法分为参照组与试验组,每组各43例。参照组予以常规治疗,试验组在参照组基础上予以相应的SCCBs辅助治疗,比较两组患者治疗前后的血清炎性因子[白细胞介素-6(IL-6)、白细胞介素-8(IL-8)、C反应蛋白(CRP)、肿瘤坏死因子-α(TNF-α)]水平、肠道菌群水平及超氧化物歧化酶(SOD)、丙二醛(MDA)水平。结果:治疗后,两组患者IL-6、IL-8、CRP及TNF-α水平均有所降低,且试验组患者IL-6、IL-8、CRP及TNF-α水平均显著低于参照组,差异有统计学意义(t=6.735、8.374、7.518、6.840,P<0.05)。治疗后,两组患者乳酸菌、肠球菌及双歧杆菌水平均有所提升,且试验组患者乳酸菌、肠球菌及双歧杆菌水平均显著高于参照组,差异有统计学意义(t=9.612、9.381、6.187,P<0.05)。治疗后,试验组患者SOD水平显著高于参照组,差异有统计学意义(t=7.549,P<0.05),试验组患者MDA水平显著低于参照组,差异有统计学意义(t=9.835,P<0.05)。结论:SCCBs辅助治疗应用于UC患者中,能够有效缓解患者的机体炎性反应,调节其肠道菌群,促进其结肠正常生理功能的恢复。

非酒精性脂肪性肝病患者血清IL-1RA、CTRP13和CK-18水平变化及其临床意义探讨

目的探讨非酒精性脂肪性肝病(NAFLD)患者血清白细胞介素-1受体拮抗剂(IL-1RA)、补体C1q肿瘤坏死因子相关蛋白13(CTRP13)和细胞角蛋白18(CK-18)水平变化及其临床意义。方法2021年1月~2023年1月我院收治的67例NAFLD患者和55例健康体检者,经肝活检诊断肝脏脂肪变性分级,采用ELISA法检测血清IL-1RA、CTRP13和CK-18水平。应用多元Logistic回归分析危险因素。结果NAFLD组血清IL-1RA和CTRP13水平分别为(328.6±54.3)pg/ml和(2634.2±397.5)pg/ml,显著低于健康人组【分别为(673.1±125.4)pg/ml和(3425.7±423.8)pg/ml,P<0.05】,而血清CK-18水平为(15.2±3.1)ng/ml,显著高于健康人组【(3.9±0.7)ng/ml,P<0.05】;17例F3级肝脂肪变性患者血清IL-1RA和CTRP13水平分别为(256.3±47.6)pg/ml和(2056.3±308.4)pg/ml,显著低于29例F1级患者【分别为(388.3±59.4)pg/ml和(3071.5±409.3)pg/ml,P<0.05】或21例F2级患者【分别为(304.7±50.1)pg/ml和(2498.1±374.2)pg/ml,P<0.05】,而血清CK-18水平为(23.4±4.7)ng/ml,显著高于F1级患者【(8.1±1.3)ng/ml,P<0.05】或F2级患者【(18.5±2.9)ng/ml,P<0.05】;F3级肝脂肪变性患者肥胖、合并糖尿病、合并高脂血症、有代谢综合征家族史、血清IL-1RA≥256.5pg/ml、CTRP13≥2056.5pg/ml和CK-18≥21.6 ng/ml占比分别为70.6%、76.5%、88.2%、70.6%、35.3%、35.3%和70.6%,与50例F1/F2级的38.0%、42.0%、40.0%、30.0%、92.0%、80.0%和10.0%比,差异显著(P<0.05);多因素Logistic回归分析表明,肥胖【OR(95%)为2.0(1.1~3.6)】、合并糖尿病【OR(95%)为2.1(1.1~4.1)】、合并高脂血症【OR(95%)为1.6(1.0~2.6)】、IL-1RA【OR(95%)为0.5(0.3~0.9)】、CTRP13【OR(95%)为0.5(0.3~0.9)】和CK-18【OR(95%)为1.7(1.2~2.5)】为影响NAFLD患者肝脏脂肪变性程度的危险因素(P<0.05)。结论NAFLD患者血清IL-1RA、CTRP13和CK-18水平异常变化可能为评估肝脏脂肪变性程度提供一定的依据。

不孕症患者采用促性腺激素释放激素拮抗剂方案联合囊胚移植获得临床妊娠的影响因素分析

目的分析不孕症患者采用促性腺激素释放激素拮抗剂(GnRH-ant)方案联合囊胚移植获得临床妊娠的影响因素。方法回顾性分析2020年1月至2022年1月赣州市妇幼保健院收治的150例使用拮抗剂方案且新鲜移植的不孕症患者的临床资料,按照妊娠结局分为临床妊娠组(n=71)和未妊娠组(n=79),比较两组患者的促排卵情况[(促性腺激素(Gn)总用量、Gn天数、扳机日雌二醇(E2)、扳机日黄体生成素(LH)、扳机日孕酮(P)、内膜厚度、优质胚胎数)],并采用多因素logistic回归分析患者获得临床妊娠的相关因素。结果临床妊娠组患者的Gn总用量、扳机日P、内膜厚度均高于未妊娠组,差异有统计学意义(P<0.05);临床妊娠组患者的扳机日E2、扳机日LH均低于未妊娠组,差异有统计学意义(P<0.05);两组患者的Gn天数、优质胚胎数比较,差异均无统计学意义(P>0.05);多因素logistic回归分析显示,Gn总用量、扳机日E2、扳机日LH、扳机日P均是拮抗剂方案联合囊胚移植的不孕症患者获得临床妊娠的独立影响因素(P<0.05)。结论Gn总用量、扳机日E2、扳机日LH、扳机日P均是使用拮抗剂方案联合囊胚移植的不孕症患者临床妊娠成功的独立影响因素,适量增加上述指标水平有助于提高临床妊娠率。

冠心病患者PCI术后β受体阻滞剂用药依从性下降的危险因素分析

目的:研究冠心病(CHD)患者经皮冠状动脉介入(PCI)术后β受体阻滞剂用药依从性下降的危险因素。方法:选择2020年1月至2021年7月期间本院收治的160例行PCI治疗的CHD患者。术后根据Morisky用药依从性量表(MMAS-8)评分,≥6分者纳入高依从性组(100例),<6分者纳入低依从性组(60例)。采用单因素和多因素Logistic回归分析CHD患者PCI术后β受体阻滞剂用药依从性降低的影响因素。结果:160例患者的平均MMAS-8评分为(5.81±0.12)分。与高依从性组比较,低依从性组年龄<60岁(74.00%比36.67%)、高中及以上(68.00%比40.00%)、支架植入<2年(54.00%比28.33%)比例、家庭关怀指数调查问卷(APGAR)评分[(5.12±1.60)分比(4.52±2.10)分]、APGAR评分≥7分比例(68.00%比33.33%)显著降低,家庭收入<3000元(34.00%比61.67%)、自费(36.00%比60.00%)、糖尿病(47.00%比66.67%)和高血压(42.00%比65.00%)比例显著升高,P<0.05或<0.01。多因素Logistic回归分析显示初中文化程度、年龄≥60岁、家庭收入<3000元、自费、支架植入时间≥2年、高血压、糖尿病是CHD患者PCI术后β受体阻滞剂用药依从性下降的独立危险因素(OR=8.445~97725.056,P<0.05或<0.01),而APGAR评分≥7分为其独立保护因素(OR=0.005,P=0.001)。结论:CHD患者PCI术后的β受体阻滞剂用药依从性降低的影响因素包括年龄、支架植入时间、文化程度等,应该重点监督存在危险因素患者的用药情况并给予干预,有助于提升用药依从性。

夜间高血压患者临床治疗特征及相关影响因素分析

目的探讨夜间高血压(nocturnal hypertension,NH)患者临床治疗特征及相关影响因素。方法采用横断面研究方法,收集2021年1月至2022年12月于湖南医药学院第一附属医院体检并经动态血压监测诊断为夜间高血压的患者829例,同时收集患者的一般人口学资料、生化检验指标、24h动态血压监测数据及基础疾病等临床资料。根据患者不同用药治疗情况,将夜间高血压患者分为单药组(n=294)、双药联合组(n=400)和多药联合组(n=135),单药组应用血管紧张素转换酶抑制剂(ACEI)/血管紧张素Ⅱ受体拮抗剂(ARB)或钙拮抗剂,双药联合组应用ACEI/ARB联合钙拮抗剂,多药联合组应用ACEI/ARB、钙拮抗剂、β受体阻滞剂和利尿剂中的任意三种或四种联合。对三组患者的临床资料进行比较并分析其影响因素。结果NH患者经不同组合降压药物治疗后,三组患者的夜间收缩压(NSBP)、夜间舒张压(NDBP)较治疗前显著下降,差异有统计学意义(P<0.001)。治疗后的NSBP和NDBP下降幅度双药联合组(21.75%,20.06%)显著大于单药组(17.60%,15.26%)及多药联合组(18.23%,16.51%),差异有统计学意义(P<0.05)。多因素Logistic回归分析显示,吸烟(OR=2.142,P=0.016)、肥胖(OR=1.563,P=0.029)、睡眠差(OR=1.412,P=0.040)、脑卒中(OR=1.806,P=0.021)及冠心病(OR=3.017,P=0.000)均为影响夜间高血压的危险因素。结论经治疗后三组患者均有效降低夜间血压,但ACEI/ARB联合钙拮抗剂降低夜间血压效果更优。戒烟、减肥、控制心脑血管疾病及改善睡眠质量是降低夜间血压的重要手段。

大麻素受体1在阻塞性睡眠呼吸暂停低通气综合征炎症反应中的神经免疫调节作用研究进展

阻塞性睡眠呼吸暂停低通气综合征(OSA)是一种全身性炎症性疾病,OSA病人睡眠结构的紊乱与下丘脑-垂体-肾上腺(HPA)轴的失调相互作用,持续激活HPA轴可诱导免疫细胞的糖皮质激素抵抗,使免疫系统反应转向促炎,导致并发症的加重,其特征性的慢性间歇低氧(CIH)也可通过多种途径激活糖皮质激素抑制核因子-κB(NF-κB)和相关炎症因子的表达,导致氧化应激、炎症、内皮功能障碍。内源性大麻素系统(ECS)在HPA轴活动以及对应激的神经内分泌反应中发挥主要调节作用,为机体提供重要的免疫防御。CIH可引起大麻素受体1(CB1R)表达增加,而CB1R拮抗剂可发挥抗炎作用,减轻CIH引起的器官损伤。CB1R拮抗剂已被证明可作为免疫抑制剂和抗炎剂,通过下调NF-κB信号发挥有益作用。现就CB1R拮抗剂调节OSA炎症反应潜在机制的研究进展进行综述。

银杏苦内酯对急性胰腺炎大鼠的治疗作用及机制

观察血小板活化因子受体特异性拮抗刘银杏苦内酯（ＢＮ５２０２１）对牛磺胆酸钠诱导的急性胰腺炎（ＡＰ）大鼠的治疗作用及其对胰腺组织丙二醛（ＭＤＡ）．ＳＯＤ和Ｃａ２＋的影响。结果表明：ＢＮ５２０２１显著降低ＡＰ大鼠死亡率，延长平均存活时间、降低血清淀粉酶活性、减轻胰组织病理损伤；显著降低胰组织Ｃａ２＋含量和ＭＤＡ含量、提高ＳＯＤ活性。提示ＢＮ５２０２１对ＡＰ大鼠有一定治疗作用，此与其抑制钙超载、清除自由基有关。

银杏苦内酯对过敏性豚鼠气道内低密度嗜酸性粒细胞增多的调制作用

用卵蛋白吸入诱导豚鼠哮喘动物模型（哮喘组），然后，进行支气管肺泡灌洗，分析支气管肺泡灌洗细胞学改变。哮喘组支气管肺泡灌洗液中的细胞总数、嗜酸性粒细胞绝对计数及低密度嗜酸性粒细胞比例均显著高于正常对照组（Ｐ＜０．０５、Ｐ＜０．０１）。哮喘动物模型在吸入抗原激发之前，用血小板活化因子特异性拮抗剂银杏苦内酯（ＢＮ５２０２１）预处理后，支气管肺泡灌洗液中细胞总数、分类和嗜酸性粒细胞数量均与哮喘组差异无显著性。但低密度嗜酸性粒细胞比例却显著降低（Ｐ＜０．０５）。用地塞米松预处理动物模型（激素组）后，支气管肺泡灌洗液中的细胞总数、嗜酸性粒细胞数、细胞分类及低密度嗜酸性粒细胞比例均降至正常对照组水平。结果表明：银杏苦内酯能显著减少哮喘动物气道内“活化”状态的低密度嗜酸性粒细胞，可能是一种有用的哮喘抗炎药物。

血浆血小板激活因子与急性肺损伤相关性及“神农33”注射液对其影响的观察

目的：探讨内毒素（ＬＰＳ）诱导急性肺损伤（ＡＬＩ）时血小板激活因子（ＰＡＦ）含量变化情况及“神农３３”注射液对ＰＡＦ及ＡＬＩ的影响。方法：给Ｗｉｓｔａｒ大鼠静脉注射ＬＰＳ，制成ＡＬＩ模型；采用反相高效液相色谱法检测ＬＰＳ攻击后１小时大鼠血浆ＰＡＦ含量，观察ＬＰＳ攻击后３小时大鼠肺湿、干重，光镜观察大鼠肺病理形态学变化。结果：ＡＬＩ组动物的肺湿重、湿干重比、肺含水量均明显高于正常对照组（Ｐ均＜０．０５），肺病理组织学改变明显且严重。ＡＬＩ组大鼠血浆ＰＡＦ含量明显高于正常对照组（Ｐ＜０．０１），单独给予“神农３３”注射液无明显降低ＰＡＦ的作用（Ｐ＞０．０５），而以“神农３３”注射液保护的大鼠ＰＡＦ含量明显低于ＡＬＩ组，同时肺损伤也较轻。结论：ＰＡＦ在ＬＰＳ诱导的ＡＬＩ中起重要作用，“神农３３”

大豆胞囊线虫病的生防因子研究进展

综述了大豆胞囊线虫的各类生防因子,如食线虫真菌、食线虫细菌、杀线虫植物、捕食性线虫和捕食性土壤动物等,其中研究较深入的是食线虫真菌和细菌,食线虫真菌可归纳为5种类型,即捕食性真菌、专性内寄生菌物、机会真菌、产毒真菌和菌根菌;另外,还对其他生防因子的最新研究结果进行了归类综述,并对大豆胞囊线虫的生物防治进行了展望。

红花总黄色素体外抑制血小板激活因子受体结合作用的研究

目的 观察硅胶吸附法制得的红花总黄色素体外对氚标记血小板激活因子 (3HPAF)血小板受体结合的影响 ,试图证明该药为一新型血小板激活因子 (PAF)受体拮抗剂。方法 以洗涤的家兔血小板 (WRP) ,血小板膜 (PM)及血小板膜蛋白 (PMP)为受体制剂 ,配体为3HPAF进行受体结合实验 ,观察红花总黄色素对3HPAF受体结合的抑制作用。结果 3种浓度3HPAF作为配体进行WRP受体结合实验 ,不同浓度的红花总黄色素抑制3HPAF与受体的特异性结合均可见明显的量效关系 ;3种浓度3HPAF作为配体进行PM受体结合实验 ,不同浓度的红花总黄色素抑制3HPAF与受体的特异性结合均可见明显的量效关系 ;两种浓度3HPAF作为配体进行PMP受体结合实验 ,不同浓度的红花总黄色素抑制3HPAF与受体的特异性结合均可见明显的量效关系。

血小板激活因子在肝脏缺血-再灌注损伤中的变化及山莨菪碱的保护作用

目的 :探讨血小板激活因子 (PAF)在肝脏缺血再灌注损伤中的意义及山莨菪碱的保护作用。方法 :测定大鼠肝脏局部缺血再灌注损伤和应用山莨菪碱时肝组织 PAF含量、丙二醛 (MDA)含量及肝脏病理变化。结果 :肝脏缺血再灌注损伤时肝组织 PAF含量增高 ,由 (2 2 7.72± 31.13) pg/ g升至 (4 6 7.16± 5 3.48) pg/ g,且随再灌注时间的延长而增高 ;山莨菪碱明显减少肝脏缺血再灌注损伤时肝组织 PAF的释放 ,减轻肝脏脂质过氧化程度 ,改善肝功能 ,减轻肝脏病变程度。结论 :山莨菪碱部分是通过抑制 PAF的产生而对肝脏缺血再灌注损伤起保护作用。

银杏苦内酯拮抗血小板活化因子部分体外作用的实验研究

血小板活化因子（ＰＡＦ）加入血小板孵化液后能引起离体气管条的强烈收缩，５０％抑制浓度（ＩＣ５０）达到６．１４×１０－７ｍｏｌ／Ｌ，而单纯ＰＡＦ的气管收缩作用则较微弱（ＩＣ５０仅为６．３２×１０－４ｍｏｌ／Ｌ），两组差异显著（Ｐ＜０．０５）；预先在血小板孵化液中加银杏苦内酯，则ＰＡＦ和血小板混合液的缩气管作用明显减弱（Ｐ＜０．０１）。ＰＡＦ能减少肺组织β－肾上腺素受体的数量，使β－受体激动剂的舒张气管作用减弱，５０％有效浓度（ＥＣ５０）由１．４４×１０－６ｍｏｌ／Ｌ增至１．０６×１０－５ｍｏｌ／Ｌ（Ｐ＜０．０５），ＰＡＦ的这一作用同样能用银杏苦内酯拮抗（Ｐ＜０．０５）。提示银杏苦内酯是一种有希望的ＰＡＦ受体拮抗剂，能用于治疗哮喘。