Müller Sebastian, Keil Thomas, Grüber Christoph, Zitnik Simona Eva, Lau Susanne, Wahn Ulrich, Witt Heiko, Nickel Renate
Department of Pediatric Pneumology and Immunology, Charité-Universitäts medizin, Berlin, Germany.
Pediatr Allergy Immunol. 2007 Dec;18(8):665-70. doi: 10.1111/j.1399-3038.2007.00573.x. Epub 2007 Jul 25.
Mannose-binding lectin (MBL) is considered an important component of innate immunity. Four functional MBL2 alterations in codons 52, 54, 57 and in the promoter at position c.1-290 are correlated with significantly lowered MBL serum levels. These variants have been associated with susceptibility to a variety of infectious agents as well as with various immunologic disorders including asthma. To reassess these observations, we analysed the four above mentioned MBL2 variants in 749 children, who were recruited by the German Multicenter Allergy Study and were prospectively evaluated for common respiratory childhood infections and atopy-related phenotypes from birth up to the age of 11 yr. We performed genotyping by melting curve analysis using fluorescence resonance energy transfer probes and the LightCycler. In contrast to previous studies, we found an association of MBL2 variants neither with the frequency of common respiratory childhood infections at any age nor with asthma or other atopy-related phenotypes. Our data suggest that MBL deficiency does not represent a pre-disposing factor for respiratory infections or atopic disorders in infants and children.
甘露糖结合凝集素(MBL)被认为是固有免疫的重要组成部分。密码子52、54、57以及启动子位置c.1 - 290处的四种功能性MBL2改变与MBL血清水平显著降低相关。这些变体与多种感染因子的易感性以及包括哮喘在内的各种免疫紊乱有关。为了重新评估这些观察结果,我们分析了德国多中心过敏研究招募的749名儿童中的上述四种MBL2变体,这些儿童从出生到11岁期间接受了常见儿童呼吸道感染和特应性相关表型的前瞻性评估。我们使用荧光共振能量转移探针和LightCycler通过熔解曲线分析进行基因分型。与先前的研究相反,我们发现MBL2变体既与任何年龄的常见儿童呼吸道感染频率无关,也与哮喘或其他特应性相关表型无关。我们的数据表明,MBL缺乏并不代表婴幼儿呼吸道感染或特应性疾病的易感因素。