TLR4基因rs4986790和rs4986791多态性与哮喘易感性的关系:荟萃分析和试验序列分析。

Annals of Saudi medicine Pub Date : 2024-05-01 Epub Date: 2024-06-06 DOI:10.5144/0256-4947.2024.183
Nan Guo, Haokun Tian, Tiangang Song, Yu Peng
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引用次数: 0

摘要

背景:目前对 TLR4 基因(toll 样受体 4)rs4986790 和 rs4986791 多态性与哮喘易感性之间相关性的理解尚无定论,研究和人群得出的结果相互矛盾:利用荟萃分析和试验序列分析(TSA)评估这种关系:按照预定义的纳入和排除标准,系统查询数据库中从数据库建立到 2023 年 6 月 19 日的相关文章。两位作者独立进行筛选、数据提取和质量评估。元分析和TSA使用RevMan 5.4、StataMP 17.0和TSA 0.9.5.10 Beta进行,α=0.05。根据种族人口统计学进行了分组分析。采用逐一排除法进行了敏感性分析。采用 Begg 和 Egger 检验对发表偏倚进行了评估:哮喘易感性与 TLR4 基因 rs4986790 和 rs4986791 多态性的关系。样本量:23 篇文章,包括 22 项关于 TLR4 基因 rs4986790 多态性的研究和 11 项关于 TLR4 基因 rs4986791 多态性的研究:在筛选出的 692 项研究中,有 23 项符合纳入标准。虽然总体荟萃分析表明 TLR4 rs4986790 多态性与哮喘易感性之间没有显著关联,但亚组分析显示在白种人群中存在显著关联。在荟萃分析中发现,rs4986791 多态性与哮喘易感性有明显关联,尤其是在亚洲人群中。敏感性分析表明,荟萃分析结果相对稳定。发表偏倚分析显示,发表偏倚的影响微乎其微。然而,TSA强调需要更多的原创性研究来进一步验证特定结果:我们的研究强调了种族特异性对 TLR4 多态性与哮喘易感性之间关系的影响。虽然 rs4986790 的总体结果并不显著,但与白种人群的关联值得进一步研究。此外,rs4986791 与哮喘易感性有显著相关性,特别是在亚洲人群中:我们的研究主要考察了 rs4986790 和 rs4986791 多态性,忽略了 TLR4 中其他遗传变异的潜在影响。
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Association of TLR4 gene rs4986790 and rs4986791 polymorphisms with asthma susceptibility: meta-analysis and trial sequential analysis.

Background: The current understanding of the correlation between TLR4 gene (toll-like receptor 4) rs4986790 and rs4986791 polymorphisms and asthma susceptibility is inconclusive, with studies and populations yielding conflicting results.

Objectives: Evaluate this relationship using meta-analysis and trial sequential analysis (TSA).

Patients and methods: Databases were systematically queried for relevant articles from the establishment of the database to 19 June 2023 adhering to predefined inclusion and exclusion criteria. Two authors independently conducted screening, data extraction, and quality evaluation. Meta-analysis and TSA were carried out using RevMan 5.4, StataMP 17.0, and TSA 0.9.5.10 Beta, with α=0.05. Subgroup analyses were conducted based on racial demographics. A sensitivity analysis was conducted employing a one-by-one exclusion method. Publication bias was assessed using the Begg and Egger tests.

Main outcome measures: Association of asthma susceptibility with TLR4 gene rs4986790 and rs4986791 polymorphisms.

Sample size: 23 articles included 22 studies on the rs4986790 polymorphism and 11 studies on the rs4986791 polymorphism on the TLR4 gene.

Results: Out of 692 studies screened, 23 met the inclusion criteria. While the overall meta-analysis showed no significant association between the TLR4 rs4986790 polymorphism and asthma susceptibility, subgroup analysis revealed a significant link in the Caucasian population. A significant association was noted in the meta-analysis, particularly among Asian populations, on the rs4986791 polymorphism. The sensitivity analysis indicated that the meta-analysis results were relatively stable. Publication bias analysis revealed minimal influence from publication bias. However, TSA was underscored by the necessity for additional original studies to further validate specific outcomes.

Conclusions: Our study underscores the ethnicity-specific impact on the relationship between TLR4 polymorphisms and asthma susceptibility. While the overall findings for rs4986790 were not significant, the association with the Caucasian population merits further investigation. Furthermore, rs4986791 demonstrated a significant correlation with asthma susceptibility, specifically among Asian populations.

Limitations: Our study predominantly examined the rs4986790 and rs4986791 polymorphisms, overlooking the potential influence of other genetic variants within TLR4.

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