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Perinatal Tumor Necrosis Factor-α Production Influenced by Maternal Pregnancy Weight Gain Predicts Childhood Asthma

机译:围产期肿瘤坏死因子-α的产生受孕期孕妇体重增加的影响可预测儿童哮喘

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摘要

Rationale: Innate immune responses marked by increases in tumor necrosis factor (TNF)-α have been associated with asthma but whether such alterations are evident before symptoms is not yet clear.Objectives: To determine if prevalence of childhood asthma or asthma-related traits is predicted by perinatal innate immune status and if maternal factors related to pregnancy influence asthma prevalence and innate immune status.Methods: In the Tucson Infant Immune Study (a nonselected birth cohort), presence of eczema and wheezing in the child's first year and physician-diagnosed asthma through age 9 and asthma in the parents was obtained from parent-completed questionnaires. TNF-α, IL-6, IL-10, and IL-12 were measured in supernatants of LPS-stimulated peripheral blood mononuclear cells at birth and 3 months as was TNF-α in plasma. TNF-α single nucleotide polymorphisms were genotyped by Sequenom. Percent predicted FEV1/FVC was measured at age 9. Maternal weight gain during pregnancy and prepregnancy weight were ascertained from medical records.Measurements and Main Results: Infants with persistently elevated LPS-induced TNF-α at birth and 3 months were at increased risk for childhood asthma (odds ratio [OR], 4.1; confidence interval [CI], 1.9–8.8; n = 233; P = 0.0003) and had decreased FEV1/FVC ratios at age 9. Children with mothers in the top tertile for pregnancy weight gain had increased risk for asthma (OR, 3.4; CI, 1.7–6.9; n = 225; P = 0.001) and persistently elevated TNF-α in early life (OR, 2.9; CI, 1.4–8.2; n = 195; P = 0.013). These relations were independent of maternal asthma and rhinitis.Conclusions: Persistently elevated LPS-induced TNF-α production early in life acts as a predictive biomarker for childhood asthma, and excess pregnancy weight gain in the mother seems to contribute to both.
机译:理由:以肿瘤坏死因子(TNF)-α为特征的先天免疫应答与哮喘有关,但这种改变在症状尚未明确之前是否明显。目的:确定儿童哮喘的患病率或与哮喘相关的特征是否通过围产期先天免疫状态进行预测,以及是否与妊娠相关的母亲因素影响哮喘的患病率和先天免疫状态。方法:在图森婴儿免疫研究(一项非选定的出生队列)中,儿童第一年出现湿疹和喘息并经医生诊断从父母填写的问卷中可以获得9岁以下的哮喘和父母的哮喘。在出生时和3个月时,在LPS刺激的外周血单个核细胞上清液中测定TNF-α,IL-6,IL-10和IL-12,血浆中TNF-α也是如此。 Sequenom对TNF-α单核苷酸多态性进行基因分型。在9岁时测量了预测的FEV1 / FVC百分比。从医疗记录中确定了孕妇在怀孕期间的体重增加和怀孕前的体重。测量和主要结果:出生时和出生后3个月LPS诱导的TNF-α持续升高的婴儿患高脂血症的风险增加。儿童哮喘(比值[OR]为4.1;置信区间[CI]为1.9–8.8; n = 233; P = 0.0003),并且在9岁时FEV1 / FVC比率降低。体重增加会增加患哮喘的风险(OR,3.4; CI,1.7–6.9; n = 225; P = 0.001)并在生命早期持续升高TNF-α(OR,2.9; CI,1.4–8.2; n = 195; P = 0.013)。这些关系与母亲哮喘和鼻炎无关。结论:生命早期一直持续升高的LPS诱导的TNF-α产生可作为儿童哮喘的预测生物标志物,而母亲过多的妊娠体重增加似乎对这两者都有影响。

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