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母体对过敏性气道疾病发展的抗性传递。

Maternal transmission of resistance to development of allergic airway disease.

作者信息

Matson Adam P, Zhu Li, Lingenheld Elizabeth G, Schramm Craig M, Clark Robert B, Selander Dawn M, Thrall Roger S, Breen Elena, Puddington Lynn

机构信息

Department of Immunology, University of Connecticut Health Center, Farmington, CT 06030, USA.

出版信息

J Immunol. 2007 Jul 15;179(2):1282-91. doi: 10.4049/jimmunol.179.2.1282.

Abstract

Parental phenotype is known to influence the inheritance of atopic diseases, such as allergic asthma, with a maternal history being a more significant risk factor for progeny than paternal history. We hypothesized that recall Th1- or Th2-type immune responses during pregnancy would result in transfer of maternal factors that would differentially impact development of immune responsiveness in offspring. Following weaning, susceptibility and severity of allergic airway disease (a murine model of human asthma) was evaluated in progeny, disease being elicited by immunization with OVA-Al(OH)(3) and challenge with aerosolized OVA. We found that progeny of mothers with Th1-biased immunity to OVA subjected to recall aerosol challenge during pregnancy had reduced levels of Ag-specific IgE and airway eosinophilia compared with progeny of mothers with Th2-biased immunity to OVA or naive mothers. Interestingly, progeny of mothers with Th1-type immunity to a heterologous albumin, BSA, were not protected from developing OVA-induced allergic airway disease. These findings demonstrated that maternal transfer of protection from development of allergic airway disease to offspring in this model of maternal Th1-type immunity was Ag specific.

摘要

已知父母的表型会影响过敏性疾病(如过敏性哮喘)的遗传,母亲的病史对后代来说是比父亲的病史更重要的风险因素。我们推测,孕期的回忆性Th1或Th2型免疫反应会导致母体因素的传递,这些因素会对后代免疫反应性的发展产生不同影响。断奶后,对后代评估过敏性气道疾病(人类哮喘的小鼠模型)的易感性和严重程度,该疾病通过用OVA - Al(OH)₃免疫并雾化OVA激发。我们发现,与对OVA具有Th2偏向性免疫的母亲或未接触过抗原的母亲的后代相比,孕期接受回忆性雾化激发且对OVA具有Th1偏向性免疫的母亲的后代,其抗原特异性IgE水平和气道嗜酸性粒细胞增多程度降低。有趣的是,对异源白蛋白BSA具有Th1型免疫的母亲的后代,并未免受OVA诱导的过敏性气道疾病的影响。这些发现表明,在这种母体Th1型免疫模型中,母体向后代传递的预防过敏性气道疾病发生的保护作用是抗原特异性的。

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