白细胞介素-8基因启动子-251A/T和白细胞介素-18基因启动子-137G/C多态性与头颈癌风险的关联：一项综合荟萃分析。

Association of IL-8 gene promoter -251 A/T and IL-18 gene promoter -137 G/C polymorphisms with head and neck cancer risk: a comprehensive meta-analysis.

作者信息

Wang Zheng, Gao Zi-Ming, Huang Hai-Bo, Sun Li-Sha, Sun An-Qi, Li Kai

机构信息

Department of Otorhinolaryngology, the First Affiliated Hospital of China Medical University, Shenyang 110001, China.

Department of Surgical Oncology, the First Affiliated Hospital of China Medical University, Shenyang 110001, China,

出版信息

Cancer Manag Res. 2018 Aug 10;10:2589-2604. doi: 10.2147/CMAR.S165631. eCollection 2018.

DOI:10.2147/CMAR.S165631

PMID:30127645

原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC6089118/

Abstract

PURPOSE

No consensus exists on the impact of polymorphisms in cytokines (such as interleukin IL-8 and IL-18) on cancer risk; moreover, there is very little evidence regarding head and neck cancer (HNC).

METHODS

Thus, a meta-analysis including 22 studies with 4731 cases and 8736 controls was conducted to evaluate this association. The summary odds ratio (OR) and corresponding 95% confidence intervals (CIs) for C-X-C motif chemokine ligand 8 (CXCL8, which encodes IL-8) and IL-18 polymorphisms and HNC risk were estimated.

RESULTS

The results showed a significantly increased risk of HNC susceptibility for IL18 -137 G/C in five genetic models, but, interestingly, no significant association was found for the CXCL8 -251 A/T polymorphism. When stratified by cancer type, an increased risk of nasopharyngeal cancer was found for both -137 G/C and -251A/T. When the studies were stratified by ethnicity and genotyping method, there were significant associations between Asian populations and polymerase chain reaction-restriction fragment length polymorphism (PCR-RFLP) studies for -137 G/C, and African populations for -251 A/T in some genetic models. A positive association was also found between the population-based groups in some models for -137 G/C; conversely, significantly decreased risk was found among the -251 A/T hospital-based group. Meta-regression was also conducted. The publication year, control source, and cancer type contributed to CXCL8 -251 A/T heterogeneity; however, no factors were found that contributed to IL-18 -137 G/C heterogeneity. Marginal significance was found in the recessive model for IL-18 -137 G/C by Egger's test, whereas no publication bias was detected for CXCL8 -251 A/T.

CONCLUSIONS

The results indicate that the IL-18 -137 G/C polymorphism is associated with HNC risk, especially nasopharyngeal cancer, in Asian populations and, when using PCR-RFLP, CXCL8 -251 A/T polymorphisms play a complex role in HNC development.

摘要

目的

细胞因子（如白细胞介素IL-8和IL-18）基因多态性对癌症风险的影响尚无定论；此外，关于头颈癌（HNC）的证据非常少。

方法

因此，进行了一项荟萃分析，纳入22项研究，共4731例病例和8736例对照，以评估这种关联。估计了C-X-C基序趋化因子配体8（CXCL8，编码IL-8）和IL-18基因多态性与HNC风险的汇总比值比（OR）及相应的95%置信区间（CI）。

结果

结果显示，在五种遗传模型中，IL18 -137 G/C使HNC易感性风险显著增加，但有趣的是，未发现CXCL8 -251 A/T多态性与HNC有显著关联。按癌症类型分层时，-137 G/C和-251A/T均使鼻咽癌风险增加。当研究按种族和基因分型方法分层时，在某些遗传模型中，亚洲人群与-137 G/C的聚合酶链反应-限制性片段长度多态性（PCR-RFLP）研究之间存在显著关联，非洲人群与-251 A/T存在显著关联。在某些-137 G/C模型中，基于人群的组之间也发现了正相关；相反，在基于医院的-251 A/T组中发现风险显著降低。还进行了meta回归。发表年份、对照来源和癌症类型导致了CXCL8 -251 A/T的异质性；然而，未发现导致IL-18 -137 G/C异质性的因素。通过Egger检验在IL-18 -137 G/C的隐性模型中发现了边缘显著性，而未检测到CXCL8 -251 A/T的发表偏倚。

结论

结果表明，IL-18 -137 G/C多态性与HNC风险相关，尤其是在亚洲人群中与鼻咽癌风险相关，并且在使用PCR-RFLP时，CXCL8 -251 A/T多态性在HNC发生中起复杂作用。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/aede/6089118/923b2384c52d/cmar-10-2589Fig1.jpg

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白细胞介素-8基因启动子-251A/T和白细胞介素-18基因启动子-137G/C多态性与头颈癌风险的关联：一项综合荟萃分析。

Association of IL-8 gene promoter -251 A/T and IL-18 gene promoter -137 G/C polymorphisms with head and neck cancer risk: a comprehensive meta-analysis.

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