Immunoglobulins (Ig), particularly IgE, are believed to be crucially involved in the pathogenesis of asthma and, equally, in allergic models of the disease. To validate this paradigm we examined homozygous mutant C57BL/6 mice, which are B cell deficient, lacking all Ig. Mice were immunized intraperitoneally with 10 μg ovalbumin (OVA) plus alum, followed by daily (day 14–20) 30 min exposures to OVA aerosol (OVA/OVA group). Three control groups were run: OVA intraperitoneally plus saline (SAL) aerosol (OVA/SAL group); saline intraperitoneally plus saline aerosol; saline intraperitoneally plus OVA aerosol ( n = 6–7). Lung and large airway tissues obtained 24 h after the last OVA or SAL exposure were examined by light microscopy and transmission electron microscopy (TEM). The Ig-deficient mice receiving OVA/ OVA treatment had swollen and discolored lungs and exhibited marked eosinophilia both in large airway subepithelial tissue (49.2 ± 12.0 cells/mm basement membrane [BM] versus OVA/ SAL control 1.2 ± 0.3 cells/mm BM; P 0.001), and perivascularly and peribronchially in the lung (49.3 ± 9.0 cells/unit area versus OVA/SAL control 2.6 ± 0.6 cells/unit area; P 0.001). The eosinophilia extended to the regional lymph nodes. TEM confirmed the subepithelial and perivascular localization of eosinophils. Mucus cells in large airway epithelium increased from 1.5 ± 0.8 (OVA/SAL mice) to 39.5 ± 5.7 cells/mm BM in OVA/OVA treated mice ( P 0.001). OVA/SAL mice never differed from the other control groups. Corresponding experiments in wild-type mice ( n = 6–7 in each group) showed qualitatively similar but less pronounced eosinophil and mucus cell changes. Macrophages and CD4+ T cells increased in lungs of all OVA/OVA-treated mice. Mast cell number did not differ but degranulation was detected only in OVA/OVA-treated wild-type mice. Immunization to OVA followed by OVA challenges thus cause eosinophil-rich inflammation in airways and lungs of mice without involvement of B cells and Ig.
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机译:免疫球蛋白(Ig),尤其是IgE被认为与哮喘的发病机理以及该疾病的过敏模型均至关重要。为了验证这种范例,我们检查了纯合突变体C57BL / 6小鼠,这些小鼠是B细胞缺陷型,缺乏所有Ig。用10μg卵清蛋白(OVA)和明矾腹膜内免疫小鼠,然后每天(第14–20天)暴露于OVA气雾剂(OVA / OVA组)30分钟。运行三个对照组:腹膜内OVA加生理盐水(SAL)气雾剂(OVA / SAL组);腹腔注射生理盐水加生理盐水喷雾;腹膜内加生理盐水加OVA气雾剂(n = 6–7)。在最后一次OVA或SAL暴露24小时后,通过光学显微镜和透射电子显微镜(TEM)检查肺和大气道组织。接受OVA / OVA处理的Ig缺陷型小鼠的肺部肿胀和变色,在大的气道上皮下组织中均表现出明显的嗜酸性粒细胞增多(49.2±12.0细胞/ mm基底膜[BM],而OVA / SAL对照为1.2±0.3细胞/ mm BM; P <0.001),以及肺部血管周围和支气管周围(49.3±9.0个细胞/单位面积,而OVA / SAL对照为2.6±0.6个细胞/单位面积; P <0.001)。嗜酸性粒细胞扩大到区域淋巴结。透射电镜证实了嗜酸性粒细胞在上皮下和血管周围的定位。 OVA / OVA处理的小鼠中,大气道上皮中的粘液细胞从1.5±0.8(OVA / SAL小鼠)增至39.5±5.7细胞/ mm BM(P <0.001)。 OVA / SAL小鼠从未与其他对照组不同。在野生型小鼠(每组n = 6–7)中进行的相应实验显示,在质量上相似,但嗜酸性粒细胞和黏液细胞变化不明显。在所有OVA / OVA处理的小鼠的肺中,巨噬细胞和CD4 + T细胞均增加。肥大细胞数目没有变化,但是仅在OVA / OVA处理的野生型小鼠中检测到脱颗粒。接种OVA疫苗后再进行OVA攻击会在小鼠的气道和肺中引起富含嗜酸性粒细胞的炎症,而不会涉及B细胞和Ig。
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