柯萨奇B_4病毒对小鼠胰岛的影响及干扰素的保护作用

采用我国流行的柯萨奇B4病毒 (CB4V)感染swiss小鼠 ,建立I型糖尿病的动物模型 ,并观察干扰素对CB4V引起的I型糖尿病的保护作用。结果表明 ,80 %的小鼠在感染后 72h出现低血糖 ,血糖在 (90 .87±8.2 6 )mg/L范围之内 ,6～ 8周全部发展为高血糖。糖刺激的胰岛素释放量在感染后 72h增加 ,但至 3～ 8周明显低于正常对照组。在用CB4V感染小鼠的同时给予干扰素 ,目的在于观察干扰素对CB4V攻击胰岛 β细胞的保护作用 ,结果经干扰素治疗后的感染小鼠 ,当给干扰素到 6周 ,80 %小鼠血糖在 (118.6 6± 5 .73)mg/L范围之内 ,而低糖与高糖刺激下的胰岛素释放量分别在 (18.34± 3.5 0 )uIU/mL ,(31.5 1± 4 .71)uIU/mL范围之内 ,均与正常对照组无差异 (p >0 .0 5 )。

柯萨奇B3m病毒性心肌炎小鼠细胞免疫状态

作者借助BALB/C小鼠柯萨奇B3m(CoxB3m)病毒性心肌炎模型,用单克隆抗体间接免疫荧光法测定病毒感染后不同天数小鼠脾脏的T细胞亚群;用LDH释放法测定NK细胞活性。结果显示:脾脏的Thy-1(Pan T)、L3T4(TH/I)及Ly-2(TS)细胞在感染后第3天起开始下降,直至第14天,各点所测得的值显著低于正常对照(P<0.05～0.001);T4/T8(L3T4/Ly-2)比值从感染后第3天的2.08±0.97上升到14天时的2.68±0.58;NK细胞活性在感染后呈进行性下降,各点所测得的值均显著低于正常对照(P<0.05～0.001)。这些实验结果提示:细胞免疫异常在本病发病中起一定作用。

柯萨奇B_(3m)病毒致低硒鼠心肌病变检出率与病毒中和抗体效价的关系

5周龄BALB/C雄性鼠经低硒、常硒合成饲料喂养5周后,腹腔注射CoxsackieB_(3m)病毒(CVB_(3m))1000TCD_(50)0.1ml,对照组注射1640营养液0.1ml,7天后处死,取心脏常规切片,HE染色光镜下检查心肌病变。取血清测定CVB_(3m)病毒中和抗体效价。结果表明:低硒鼠感染CVB_(3m)病毒组(Ⅰ组)及常硒鼠感染CVB_(3m)病毒组(Ⅱ组)对照组(Ⅲ组),心肌病变检出率分别为75％、35％、,Ⅲ组末见病变。x^2检验(Ⅰ组)病变检出率显著高于Ⅱ组(P<0.05)。血清中CVB_(3m)病毒中和抗体效价Ⅰ组为1:256,Ⅱ组为1:1024,Ⅰ组中和抗价显著低于Ⅱ组。提示Ⅰ组心脏病变检出率显著高于Ⅱ组,且病变重。除其他因素外,低硒鼠感染病毒后体内产生病毒中和抗体效价降低,导致Ⅰ组鼠体内清除病毒能力下降,有一定的关系。

EFFECT OF VERAPAMIL ONCa^（2＋） INFLUX ANDCVB3－RNA REPLICATION IN CULTURED NEONATALRAT HEART CELLS INFECTED WITH CVB3

The effect of verapamil on Ca2+ influx across the myocardial plasma membrane and coxsackie virus B3 ( CVB3)-RNA replication in cultured neonatal rat heart cells infected with CVB3 was investigated. It was found that the Ca2+ influx could be inhibited significantly (P<O. 01) by verapamil (1 μmol/L) after infection of heart cells for 48h. However, when the cultured heart cells infected with CVB3 and treated with verapamil (Iμmol/L and 10 nmo/L) at the same time for 48h, the amounts of CVB3-RNA in myocytes were significantly higher than that in infected control group (P<O. 05). These phenomena suggest that the increase of Ca2+ influx of cultured heart cells infected with CVB3 could be inhibited by some calcium antagonists, e. g. verapamil at the early stage. On the other hand, verapamil might accelerate viral replication in myocardium. Thus, although verapamil could be beneficial for decreasing the secondary Ca2+ damages and improve the myocardial electric activity, it isn’t a sensible choice for therapy in early stage of virus infection with cardiac symptoms.

北京某幼儿园一起集中发热疫情的病原学分析

目的 对北京市某幼儿园集中发热疫情中的病例进行病因研究,分析其病原学特征.方法 采集该幼儿园13位发热患者的咽拭子标本,利用RT-PCR扩增肠道病毒VP1区基因序列,测序分析病原分子特征.结果 8名病例为肠道病毒核酸通用阳性,测序分析发现其中3名病例为CoxA4病原体阳性.其他5名病例为肠道病毒核酸通用引物扩增阴性.结论 引起此次集中发热疫情的病原体主要为肠道病毒CoxA4,分析VP1区序列它们为同一基因型病原,分别与中国北京2012年序列KJ818321、中国深圳2009年序列HQ728260,还有中国上海2010年序列KJ541164高度一致.

柯萨奇病毒B组4型VP1蛋白原核表达及间接ELISA检测方法的建立

目的 以柯萨奇病毒B组4型(Coxsackievirus B4,CV-B4)VP1基因的原核表达蛋白作为包被抗原,建立并优化间接ELISA方法,用于CV-B4的抗体检测.方法 采用RT-PCR技术扩增CV-B4病毒VP1基因,构建重组表达载体pET-32VP1,并转化至表达菌株大肠埃希菌Rosetta(DE3),进行IPTG诱导表达,经SDS-PAGE和蛋白质谱鉴定目的蛋白成功表达.以纯化的重组蛋白为包被抗原,进行间接ELISA方法反应体系的建立和条件优化.结果 CV-B4的VP1基因可在大肠埃希菌中以包涵体形式稳定表达,确定抗体间接ELISA检测方法的抗原最佳包被浓度为7.5μg/孔,血清最佳稀释浓度为1:100,临界值为OD450值≥0.376,重组蛋白可与CV-B4阳性血清特异识别,与CV-B3阳性血清存在一定交叉反应,但与柯萨奇A组病毒以及CV-B1和CV-B5均无反应,表明蛋白具有良好的免疫原性.结论 大肠埃希菌表达的VP1重组蛋白为抗原建立的间接ELISA方法具有较好的敏感性、特异性和重复性,可用于CV-B4血清抗体的检测.

Design, synthesis, and antiviral properties of 2-aryl-1H- benzimidazole-4-carboxamide derivatives

A series of new benzimidazole derivatives were designed and synthesized.Their chemical structures were testified by 1 H NMR,infrared spectroscopy(IR),mass spectrography(MS),and elemental analysis.Their potent antiviral properties indicated the prospect of new drugs.Compound 13,16,18,19,21,22,and 23 were identified as novel antivirus with much better selective activity and inhibitory activity than the comparable ribavirin against Coxsackie virus B_(3) in VERO cells.