Effects of anti-CD4 antibody treatment on calcium ions influx in peanut-sensitized C3H/HeJ mice

The precise mechanism underlying the effects of anti-CD4 antibody and calcium ions(Ca^(2+)) in peanut allergy remains unknown.C3 H/HeJ mice sensitized with peanut protein extract(PPE)were injected with anti-CD4 antibodies for 4 weeks.Stimulation with PPE increased the specific immunoglobulin E(IgE),cytokine,histamine,and mMcp-1 levels,upregulated decorin(Dcn)expression,induced Ca^(2+) inflow in the spleen,and augmented the expression of the transcription factors GATA-3 and Foxp3,which resulted in Th2 and Treg cell activation.Notably,the Ca^(2+) levels were positively correlated with the histamine,interleukin(IL)-4,IL-5,and IL-13 levels,and negatively correlated with IL-10 levels.However,administration of anti-CD4 antibodies markedly alleviated allergic symptoms,activated T cells,and reduced Ca^(2+) inflow,cytokine,histamine,mMcp-1,and the IgHG3,CXCLI2,MMP2 and FABP4 gene.Our results indicated that anti-CD4 antibodies can ameliorate PPE-induced allergy,which is probably related to the suppression of Ca^(2+) inflow,and inhibiting histamine,cytokine and IgHG3,CXCL12,MMP2,and FABP4,thus exerting a protective effect against PPEsensitized food allergy.

精神压力对C3H/HeJ小鼠斑秃发病率的影响

目的 研究精神压力对C3H/HeJ小鼠斑秃发病率的影响.方法 选取C3H/HeJ小鼠80只,随机分为4组,即精神压力组、药物诱导组、精神压力与药物诱导组和对照组,每组20只,干预后观察4个月,统计斑秃发病率,并比较各组差异.结果 精神压力组斑秃发病率为10%,对照组没有发生;精神压力与药物诱导组发病率为90%,药物诱导组发病率为60%,差异有统计学意义（P〈0.05）.结论 精神压力在药物诱导下显著提高C3H/HeJ小鼠斑秃发病率.

TLR4在基因突变小鼠C3H/HeJ坐骨神经损伤修复中的作用

目的探究TLR4突变对小鼠坐骨神经损伤修复产生的影响。方法选择TLR4基因突变型C3H/HeJ小鼠和野生型C3H/HeN小鼠作为实验动物,实验设C3H/HeJ夹伤组(HeJ)、C3H/HeN夹伤组(HeN)及C3H/HeN假手术组(control)。在无菌操作条件下,构建小鼠坐骨神经夹伤模型。分别于术后6、12、24和48 h,qPCR检测损伤神经IL-1β、IL-6、TNF-α因子的表达。术后12 h和24 h,Western blot检测损伤神经p75NTR蛋白的表达。术后1周、2周、4周和8周取小鼠坐骨神经,HE染色观察神经恢复情况,免疫组化检测GAP-43、p75NTR蛋白表达情况。坐骨神经功能指数(sciatic functional index,SFI)评价小鼠运动功能恢复情况。结果在6、12和24 h时,与control组相比,HeN组IL-1β和TNF-α的表达量显著升高(P<0.01),而HeJ组的变化不明显。HeN组与HeJ组之间TNF-α的表达差异显著(P<0.001)。与control组相比,在6 h时HeN组IL-6的表达显著上升(P<0.001)。Western blot结果显示,与HeN组相比,坐骨神经损伤后12 h或24 h时HeJ组小鼠p75NTR蛋白表达显著升高(P<0.001)。HE染色表明,与HeN组相比,HeJ组小鼠淋巴细胞表达较少,炎性反应较弱。免疫组化结果发现,与HeN组相比,HeJ组小鼠GAP43和p75NTR的表达显著升高(P<0.01)。SFI结果显示,与HeN组相比,HeJ组小鼠的SFI评分在术后同期相对较高,神经恢复更好。结论成功构建突变小鼠坐骨神经损伤模型,揭示出TLR4突变可减少炎性因子的释放而加快坐骨神经修复。为临床上治疗周围神经损伤提供了实验理论依据。

食品致敏性评价啮齿类动物模型研究——C3H/HeJ小鼠动物模型

目的研究C3H/HeJ小鼠作为食品致敏性评价动物模型的可行性,探讨不同致敏途径适当的致敏周期以及辅助性T淋巴细胞因子的变化。方法通过经口灌胃及腹腔注射两种途径给予雌性C3H/HeJ小鼠致敏蛋白——卵清蛋白(OVA),共35天。分别在第14、28、35天内眦取血分离血清,测定OVA特异性IgE。于第35天取脾脏,荧光实时定量PCR检测Th2型细胞因子IL-4及Th1型细胞因子IFN-γ的mRNA表达水平。结果与阴性对照组相比,经口灌胃OVA组小鼠第28和35天血清中OVA特异性IgE浓度显著升高(P<0.05);腹腔注射OVA+Al(OH)3组小鼠第14、28和35天血清中OVA特异性IgE浓度显著升高(P<0.05)。与阴性对照组相比,OVA组与OVA+Al(OH)3组小鼠细胞因子IL-4的表达水平均显著升高;细胞因子IFN-γ的mRNA表达水平均显著降低。结论C3H/HeJ小鼠可以作为食品致敏性评价动物模型,经口灌胃途径及腹腔注射途径的最佳致敏周期分别为14天和28天。

应用抗CD137L单克隆抗体阻断CD137/CD137L信号通路抑制小鼠SGVHD的发生

目的:探讨抗CD137L单克隆抗体阻断CD137/CD137L信号通路在小鼠同基因型移植物抗宿主病(SGVHD)诱导中的作用,以阐明SGVHD的发生机制。方法:用致死剂量的X射线照射受体小鼠后,移植同基因骨髓细胞,从移植的当天开始连续21天腹腔注射环孢素A(CsA)诱导SGVHD。于诱导的第10天起给治疗组小鼠腹腔注射抗CD137L单克隆抗体进行干预治疗。观察各组小鼠的临床症状(体重下降,腹泻)、组织病理学和细胞因子改变。结果:抗CD137L单克隆抗体治疗组小鼠SGVHD的发生率明显低于诱导组小鼠SGVHD的发生率(25%vs 67%),两者差异具有统计学意义(P<0.01)。SGVHD小鼠肝脏和结肠组织病理学呈严重炎症细胞浸润,组织中细胞因子IL-12、IFN-γ、TNF-αmRNA水平升高。而抗体治疗组小鼠织病理学呈轻度炎症细胞浸润,组织中细胞因子IL-12、IFNγ-、TNF-αmRNA水平较低或检测不到。结论:单独用抗CD137L单克隆抗体阻断CD137/CD137L信号通路可明显抑制小鼠SGVHD的发生,提示CD137/CD137L信号通路在小鼠SGVHD免疫反应中是较为重要的通路之一。

TLR4对MHV-3诱导的C3H/He小鼠病毒性肝炎转归的影响

目的探讨TLR4对3型鼠肝炎病毒(MHV-3)诱导的C3H/He小鼠肝炎转归的影响。方法观察C3H/HeJ及C3H/HeN小鼠感染MHV-3后的临床症状(皮毛异常、呼吸加快及身体颤抖)并进行评分。记录两亚系小鼠的存活情况并进行比较。所有小鼠观察至感染后40d。结果小鼠品系对临床症状评分不起作用(P=0.718)。临床评分有随时间变化的趋势(P<0.001),且时间因素的作用随小鼠品系而不同(P=0.004)。C3H/HeJ及C3H/HeN小鼠临床症状评分仅在感染后第5、6、13天出现差异:(13.071±1.184)和(10.933±4.608)(P<0.001),(8.321±5.048)和(11.304±3.901)(P<0.001),(13.091±1.578)和(10.846±3.671)(P=0.015)。C3H/HeJ及C3H/HeN小鼠存活率分别为26.7%和23.3%,平均存活时间分别为16.267d和16.433d,无显著差异(P=0.922)。结论 MHV-3诱导的C3H/He小鼠病毒性肝炎转归不依赖于TLR4。

A Primary Study of the Subgroups of T Lymphocytes in MHV-3 Induced Chronic Viral Hepatitis

To study the contribution of T cell subsets in the pathogenesis of Murine hepatitis virus Type 3(MHV-3) induced chronic viral hepatitis in C3H/Hej mice,ninety C3H/Hej mice were chosen to individually receive 10 plaque forming units(PFU)of MHV-3 intraperitoneally.The changes of virus titer and pathology in liver tissue were examined by standard plaque assay and by the hematoxylin/eosin(HE) staining method from 2 days post MHV-3 infection.The ratios of T cell subsets including CD3+CD4+CD8-,CD3+CD4-CD8+,CD3+CD4-CD8-,CD3+CD4+CD25+,CD3+CD4+CD25-and CD3+ CD4-CD25+ T lymphocyte of total T lymphocytes in blood,spleen and liver were examined at 0,2,4,6,8,10,12,15,20,25,30,40 days post MHV-3 infection by flow cytosorting.We observed that the virus titer raised and showed persistent virus duplications and inflammatory changes in the livers of C3H/Hej mice from 2 days post MHV-3 infection.The double negative T cell(DN Treg cell) and CD4+CD25+ T cell ratios increased significantly from 2 days post MHV-3 infection in C3H/Hej mice,and CD3+CD4+CD8-,CD3+CD4-CD8+,CD3+CD4+CD25-and CD3+CD4-CD25+ T cell ratios decreased accordingly.In conclusion,the changes of virus titer and pathology in the livers of C3H/Hej mice post MHV-3 suggest their contribution to viral persistence.Further characterizations of DN Treg cells are that infection indicates that MHV-3 could induce the chronic inflammation in livers of C3H/Hej mice.The increase of the DN Treg cell and CD4+CD25+ T cell ratios in C3H/Hej mice post MHV-3 infection suggests that DN Treg cells and CD4+CD25+ T cells may both have important suppressive immunomodulation functions in the development of chronic viral hepatitis and have important roles in the virus persistent infection.Further characterizations of DNT cell and CD4+CD25+ T cell are under investigation.

Aberrant Light-Induced Depression is Associated with Impaired Sensorimotor Gating in Mice

Mice subjected to an irregular light-dark cycle are known to lose their capacity to synchronize their behavioral rhythm to environmental light, and to show endophenotypes related to depressive disorders. Here we observed that a susceptible strain of mice (C3H/HeJ) subjected to an irregular 3.5 hr:3.5 hr light-dark cycle showed an enhanced acoustic startle reflex and deficits in prepulse inhibition. As impaired sensorimotor gating is associated with the onset of a variety of mental disorders such as schizophrenia and major depressive disorder, irregular environmental light without circadian photo-entrainment may cause stress that has the potential to be involved in humans’ susceptibility to neuropsychiatric abnormalities.

TLR-4和CD14在急性前葡萄膜炎小鼠虹膜中的表达

目的观察内毒素诱导的小鼠急性前葡萄膜炎模型中虹膜Toll样受体-4(Toll-like receptor-4,TLR-4)和CD14的表达。方法C3H/HeN(野生型)和C3H/HeJ(TLR-4基因缺陷型)小鼠足底注射霍乱弧菌内毒素,建立急性前葡萄膜炎动物模型,注射后每隔2h用裂隙灯进行眼前节观察,并做组织病理学检查。用Western blotting及免疫组织化学法检测小鼠虹膜中TLR-4及CD14蛋白的表达。结果C3H/HeN小鼠在内毒素注射后4～6h,小鼠结膜囊内出现大量白色分泌物,12～18h瞳孔区偶见白色渗出,22～24h可见虹膜后粘连及渗出物,36～48h前房内未见炎症消退;C3H/HeJ小鼠未见眼前节炎症反应。通过Western boltting发现正常C3H/HeN小鼠虹膜内有TLR-4蛋白的表达,注射内毒素24h后TLR-4的表达量显著增高,与12h相比差异有显著统计学意义(P=0.009)。免疫组织化学显示在内毒素诱导后24h,TLR-4与CD14在急性前葡萄膜炎模型虹膜组织中大量表达,而在C3H/HeJ小鼠中未见TLR-4蛋白的表达。结论TLR-4在内毒素诱导的C3H/HeJ(TLR-4基因缺陷)小鼠中未见表达,而在C3H/HeN(野生型)急性前葡萄膜炎动物模型虹膜组织中大量表达,TLR-4可能在急性前葡萄膜炎发病环节中发挥着重要作用。

斑秃动物模型研究的现状与进展

斑秃是一种临床常见的非瘢痕性秃发,以突然出现的圆形或类圆形脱发斑为特征,严重时可累及整个头皮和全身的毛发。斑秃的发病机制及治疗相关研究是皮肤科研究的热点之一,其中斑秃动物模型是重要的研究工具,通过斑秃动物模型发现了斑秃的发病与免疫赦免的关联以及新的靶向药疗法等。目前主要的斑秃模型以C3H/HeJ小鼠、SCID小鼠和DEBR大鼠为主。该文综述了斑秃动物模型研究的现状与研究进展。

慢性病毒性肝炎小鼠动物模型的建立及其特征分析

慢性病毒型肝炎是一种严重危害人类健康的常见病,多发病,目前尚缺乏理想的实验动物模型来阐明其具体的发病机制,从而使得对其防治的研究受到限制。本研究采用纯化的3型鼠肝炎病毒(MHV-3)经腹腔注入近交系C3H/HeJ小鼠体内,小鼠感染MHV-3后,约63%存活,存活的小鼠一般情况较正常对照组差,肝脏组织呈现持续炎性改变,血清ALT、AST升高而TP、ALB有所下降,与人类慢性病毒性肝炎的发生发展极为相似,可作为研究慢性病毒性肝炎的比较理想动物模型。

TLR4基因突变对小鼠坐骨神经损伤修复的影响

目的探讨Toll样受体4(TLR4)基因突变达对小鼠坐骨神经损伤修复的影响。方法取10只C3H/HeJ小鼠(TLR4基因突变作为突变组,20只C3H/HeN小鼠(TLR4基因正常)随机分为假手术组(n=10)和模型组(n=10)。突变组和模型组在暴露的坐骨神经中部用止血钳夹持60 s以建立小鼠坐骨神经损伤模型,假手术组仅暴露坐骨神经而不进行夹伤。造模后4周,采用坐骨神经功能指数(SFI)评分评定坐骨神经功能,然后每组取3只小鼠行HE染色观察坐骨神经病理改变,每组取3只小鼠采用RT-PCR检测坐骨神经组织白细胞介素-1β(IL-1β)、肿瘤坏死因子-α(TNF-α)、白细胞介素-6(IL-6)mRNA表达水平,每组取4只小鼠采用免疫印迹法检测坐骨神经组织生长相关蛋白43(GAP43)、p75神经营养素受体(p75NTR)蛋白表达水平。结果与假手术组相比,模型组SFI评分显著降低(P<0.05),HE染色显示细胞形态异常并出现大量嗜中性粒细胞和巨噬细胞,坐骨神经组织IL-1β、IL-6、TNF-αmRNA表达水平以及GAP43、p75NTR蛋白表达水平均显著增高(P<0.05)。与模型组相比,突变组SFI评分明显增高(P<0.05),组织结构病理改变明显改善,IL-1β、IL-6、TNF-αmRNA表达水平以及GAP43、p75NTR蛋白表达水平显著降低(P<0.05)。结论TLR4基因突变可促进小鼠坐骨神经损伤后修复,可能与降低IL-1β、IL-6、TNF-α等炎症因子水平有关。