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局部莫匹罗星治疗通过靶向葡萄球菌属减少皮肤红斑狼疮病变中的干扰素和髓系特征。

Topical Mupirocin Treatment Reduces Interferon and Myeloid Signatures in Cutaneous Lupus Erythematous Lesions Through Targeting of Staphylococcus Species.

作者信息

Abernathy-Close Lisa, Mears Joseph, Billi Allison C, Sirobhushanam Sirisha, Berthier Celine, Lu Annie, Zhang Zeran, Hurst Amy, Gudjonsson Johann E, Kahlenberg J Michelle

机构信息

University of Michigan, Ann Arbor.

出版信息

Arthritis Rheumatol. 2025 Jun;77(6):705-715. doi: 10.1002/art.43079. Epub 2025 Jan 23.

Abstract

OBJECTIVE

Cutaneous lupus erythematosus (CLE) is an inflammatory skin manifestation of systemic lupus erythematosus. Type I interferons (IFNs) promote inflammatory responses and are elevated in CLE lesions. We recently reported that CLE lesions are frequently colonized with Staphylococcus aureus. Here, we follow up via a proof-of-concept study to investigate whether type I IFN and inflammatory gene signatures in CLE lesions can be modulated with mupirocin, a topical antibiotic treatment against S aureus-mediated skin infections.

METHODS

Participants with active CLE lesions (n = 12) were recruited and randomized into a week of topical treatment with either 2% mupirocin or petroleum jelly vehicle. Paired samples were collected before and after seven days of treatment to assess microbial lesional skin responses. Microbial samples from nares and lesional skin were used to determine baseline and posttreatment Staphylococcus abundance and microbial community profiles by 16S ribosomal RNA gene sequencing. Inflammatory responses were evaluated by bulk RNA sequencing of lesional skin biopsies.

RESULTS

We identified 173 differentially expressed genes in CLE lesions after topical mupirocin treatment. Decreased lesional Staphylococcus burden correlated with decreased IFN pathway signaling and inflammatory gene expression and barrier dysfunction. Interestingly, mupirocin treatment lowered skin monocyte levels, and this mupirocin-associated depletion of monocytes correlated with decreased inflammatory gene expression.

CONCLUSION

Mupirocin treatment decreased lesional Staphylococcus, and this correlated with decreased IFN signaling and inflammatory gene expression. This study suggests a topical antibiotic could be employed to decrease lupus skin inflammation and type I IFN responses by reducing Staphylococcus colonization.

摘要

目的

皮肤红斑狼疮(CLE)是系统性红斑狼疮的一种炎症性皮肤表现。I型干扰素(IFN)可促进炎症反应,且在CLE皮损中水平升高。我们最近报道CLE皮损中常定植有金黄色葡萄球菌。在此,我们通过一项概念验证研究进行跟进,以调查CLE皮损中的I型干扰素和炎症基因特征是否可通过莫匹罗星(一种针对金黄色葡萄球菌介导的皮肤感染的外用抗生素治疗药物)进行调节。

方法

招募有活动性CLE皮损的参与者(n = 12),并随机分为两组,一组接受为期一周的2%莫匹罗星外用治疗,另一组接受凡士林载体治疗。在治疗七天前后收集配对样本,以评估皮损皮肤的微生物反应。利用来自鼻孔和皮损皮肤的微生物样本,通过16S核糖体RNA基因测序确定基线和治疗后金黄色葡萄球菌丰度及微生物群落概况。通过皮损皮肤活检的大量RNA测序评估炎症反应。

结果

我们在外用莫匹罗星治疗后的CLE皮损中鉴定出173个差异表达基因。皮损中金黄色葡萄球菌负担的降低与IFN信号通路及炎症基因表达和屏障功能障碍的降低相关。有趣的是,莫匹罗星治疗降低了皮肤单核细胞水平,且这种与莫匹罗星相关的单核细胞减少与炎症基因表达降低相关。

结论

莫匹罗星治疗降低了皮损中的金黄色葡萄球菌,这与IFN信号和炎症基因表达的降低相关。本研究表明,一种外用抗生素可通过减少金黄色葡萄球菌定植来减轻狼疮皮肤炎症和I型干扰素反应。

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