Wen Xiang, Zhou Juan, Fang Heping, Li Juan, Wang Run, Zeng Dan, Xie Xiaohong, Deng Yu, Ren Luo, Liu Enmei
Department of Respiratory Medicine, Children's Hospital of Chongqing Medical University, National Clinical Research Center for Child Health and Disorders, Ministry of Education Key Laboratory of Child Development and Disorders, Chongqing, China.
Chongqing Key Laboratory of Child Rare Diseases in Infection and Immunity, Chongqing, China.
Respirology. 2025 Feb;30(2):113-123. doi: 10.1111/resp.14846. Epub 2024 Oct 30.
A disintegrin and metalloprotease 33 (ADAM33) is associated with asthma susceptibility, and its genetic variations impact susceptibility and disease severity. However, the mechanisms remain unclear. This study aimed to investigate ADAM33 single nucleotide polymorphisms (SNPs) in childhood asthma susceptibility and explore their regulatory mechanisms.
Eleven selected SNPs in ADAM33 were genotyped and identified the association with asthma susceptibility. In the validation cohort, we measured plasma sADAM33 levels and compared them with disease severity among children with different SNP genotypes. Computational predictions identified miRNAs targeting the SNP, and the impact of the SNP on miRNA regulation was confirmed using a dual luciferase reporter system. Finally, we validated the regulatory role of miRNAs on ADAM33 expression using an in vitro model with upregulated ADAM33 expression.
Only rs3918400 was associated with asthma susceptibility. In the validation cohort, children with allergic asthma exhibited higher plasma sADAM33 levels. Among asthmatic children, those with the rs3918400 CT/TT genotype had higher sADAM33 levels, poorer asthma control, more severe airway hyper-responsiveness, lower FEV% and higher dust mite-specific IgE activity compared to those with the CC genotype. miR-3928-5p bound strongly to the rs3918400 C allele and effectively reduced ADAM33 protein expression in CC genotype cells. However, the binding affinity of miR-3928-5p to the T allele was weaker, resulting in diminished negative regulation of protein expression.
The rs3918400 SNP affects the negative regulation of ADAM33 by miR-3928-5p, potentially participating in a complex interplay of processes related to childhood asthma susceptibility.
解整合素金属蛋白酶33(ADAM33)与哮喘易感性相关,其基因变异影响易感性和疾病严重程度。然而,其机制尚不清楚。本研究旨在调查ADAM33单核苷酸多态性(SNP)在儿童哮喘易感性中的作用,并探索其调控机制。
对ADAM33中选定的11个SNP进行基因分型,并确定其与哮喘易感性的关联。在验证队列中,我们测量了血浆可溶性ADAM33(sADAM33)水平,并比较了不同SNP基因型儿童的疾病严重程度。通过计算预测确定靶向该SNP的微小RNA(miRNA),并使用双荧光素酶报告系统证实该SNP对miRNA调控的影响。最后,我们使用上调ADAM33表达的体外模型验证了miRNA对ADAM33表达的调控作用。
只有rs3918400与哮喘易感性相关。在验证队列中,过敏性哮喘儿童的血浆sADAM33水平较高。在哮喘儿童中,与CC基因型儿童相比,rs3918400 CT/TT基因型儿童的sADAM33水平更高、哮喘控制更差、气道高反应性更严重、第一秒用力呼气容积(FEV%)更低且尘螨特异性IgE活性更高。miR-3928-5p与rs3918400 C等位基因强烈结合,并有效降低CC基因型细胞中ADAM33蛋白的表达。然而,miR-3928-5p与T等位基因的结合亲和力较弱,导致蛋白表达的负调控减弱。
rs3918400 SNP影响miR-3928-5p对ADAM33的负调控,可能参与了与儿童哮喘易感性相关的复杂相互作用过程。
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