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肿瘤坏死因子 α-308 G/A 和白细胞介素 1β-511 C/T 基因多态性与瘢痕性痤疮患者的相关性研究。

Tumor necrosis factor α-308 G/A and interleukin 1 β-511 C/T gene polymorphisms in patients with scarring acne.

机构信息

Dermatovenereology, Ataturk Training and Research Hospital, Ankara, Turkey.

Pediatric Immunology, Hacettepe University School of Medicine, Ankara, Turkey.

出版信息

J Cosmet Dermatol. 2019 Feb;18(1):395-400. doi: 10.1111/jocd.12558. Epub 2018 Apr 19.

Abstract

BACKGROUND

Acne is a chronic inflammatory skin disorder which may heal with scarring. Tumor necrosis factor alpha (TNF α) and interleukin 1 β (IL-1β) are considered as the main responsible proinflammatory mediators of acne pathogenesis. Oversecretion of these cytokines was found to be associated with TNF α-308 G>A and IL-1β-511 C<T polymorphisms.

AIM

To evaluate the association of TNF α-308 and IL-1β-511 gene polymorphisms with acne and postacne scarring susceptibility and acne severity.

METHODS

Study subjects included 90 patients with acne vulgaris (31 males, 59 females; mean age: 19.6 ± 3.7 years) and 30 healthy controls (11 males, 19 females; mean age: 19.2 ± 5.1 years). Patients were sub-grouped on the basis of acne severity into mild, moderate, and severe acne groups and on the presence postacne scarring into scarring acne and nonscarring acne groups. Peripheral venous blood samples were obtained for performing real-time PCR analysis for detecting TNF α-308 and IL-1β-511 genotypic variants.

RESULTS

Among patients, 21.7% (n = 26) had mild, 22.5% (n = 27) had moderate, 30.8% (n = 37) had severe, and 30% (n = 36) had scarring acne. Genotypic variants of TNF α-308 and IL-1β-511 did not statistically differ between acne patients and controls (P values: .245 and .466). When compared in terms of acne severity and the presence of postacne scarring, no statistical significance was observed regarding frequencies of genotypic variants related to the both TNF α-308 and IL-1β polymorphisms (P > .05).

CONCLUSION

TNF α-308 and IL-1β polymorphic variants are not associated with acne and postacne scarring susceptibility and acne severity.

摘要

背景

痤疮是一种慢性炎症性皮肤病,可能会留下疤痕。肿瘤坏死因子-α(TNF-α)和白细胞介素 1β(IL-1β)被认为是痤疮发病机制中的主要致炎细胞因子。这些细胞因子的过度分泌与 TNF-α-308 G>A 和 IL-1β-511 C>T 多态性有关。

目的

评估 TNF-α-308 和 IL-1β-511 基因多态性与痤疮和痤疮后瘢痕易感性及痤疮严重程度的关系。

方法

研究对象包括 90 例寻常性痤疮患者(男 31 例,女 59 例;平均年龄:19.6±3.7 岁)和 30 名健康对照者(男 11 例,女 19 例;平均年龄:19.2±5.1 岁)。根据痤疮严重程度将患者分为轻度、中度和重度痤疮组,并根据是否有痤疮后瘢痕分为有瘢痕痤疮组和无瘢痕痤疮组。采集外周静脉血样,进行实时 PCR 分析,以检测 TNF-α-308 和 IL-1β-511 基因型变异。

结果

患者中,21.7%(n=26)为轻度、22.5%(n=27)为中度、30.8%(n=37)为重度和 30%(n=36)为有瘢痕痤疮。TNF-α-308 和 IL-1β-511 的基因型变异在痤疮患者和对照组之间无统计学差异(P 值:.245 和.466)。在比较痤疮严重程度和痤疮后瘢痕存在情况时,TNF-α-308 和 IL-1β 多态性相关基因型的频率无统计学意义(P>.05)。

结论

TNF-α-308 和 IL-1β 多态性变异与痤疮和痤疮后瘢痕易感性及痤疮严重程度无关。

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