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肥大细胞组织蛋白酶抗菌肽可预防皮肤A组链球菌侵袭性感染。

Mast cell cathelicidin antimicrobial peptide prevents invasive group A Streptococcus infection of the skin.

作者信息

Di Nardo Anna, Yamasaki Kenshi, Dorschner Robert A, Lai Yuping, Gallo Richard L

机构信息

Department of Medicine, Division of Dermatology, University of California, San Diego and Veteran's Affairs Medical Center San Diego, CA 92161, USA.

出版信息

J Immunol. 2008 Jun 1;180(11):7565-73. doi: 10.4049/jimmunol.180.11.7565.

Abstract

Mast cells (MC) express cathelicidin antimicrobial peptides that act as broad-spectrum antibiotics and influence the immune defense of multiple epithelial surfaces. We hypothesized that MC help protect against skin infection through the expression of cathelicidin. The susceptibility of MC-deficient mice (Kit Wsh(-/-)) to invasive group A streptococcus (GAS) was compared with control mice. Following s.c. injection of GAS, MC-deficient mice had 30% larger skin lesions, 80% more lesional bacteria, and 30% more spleens positive for bacteria. In contrast to results obtained when GAS was injected into skin, no significant differences were noted between MC-deficient mice and control mice after GAS was applied topically, indicating that MC activity is most important after barrier penetration. To determine whether these differences were due to MC expression of cathelicidin, MC-deficient mice were reconstituted with MC derived from either wild-type or cathelicidin-deficient (Camp(-/-)) mice and challenged with GAS. Forty-eight hours after bacterial injection, mice that did not receive MC had an average lesion size of 200 mm(2), mice reconstituted with wild-type MC showed lesions comparable to control mice (25 mm(2)), while mice reconstituted with Camp(-/-) MC showed an average lesion size of 120 mm(2). Surface-enhanced laser desorption/ionization time-of-flight mass spectrometry (SELDI-TOF-MS) analysis of cathelicidin peptide purified from mast cells defined this as a unique 28-aa peptide. Combined, these results show that MC confer defense against Gram-positive bacterial infection in the skin, a function mediated in part by the expression of a unique cathelicidin peptide.

摘要

肥大细胞(MC)表达的cathelicidin抗菌肽可作为广谱抗生素,并影响多个上皮表面的免疫防御。我们推测MC通过表达cathelicidin来帮助抵御皮肤感染。将MC缺陷小鼠(Kit Wsh(-/-))对侵袭性A组链球菌(GAS)的易感性与对照小鼠进行比较。皮下注射GAS后,MC缺陷小鼠的皮肤损伤面积大30%,损伤部位的细菌多80%,脾脏细菌阳性率高30%。与将GAS注入皮肤时获得的结果相反,局部应用GAS后,MC缺陷小鼠与对照小鼠之间未观察到显著差异,这表明MC活性在屏障穿透后最为重要。为了确定这些差异是否归因于MC对cathelicidin的表达,用来自野生型或cathelicidin缺陷(Camp(-/-))小鼠的MC重建MC缺陷小鼠,并对其进行GAS攻击。细菌注射48小时后,未接受MC的小鼠平均损伤面积为200 mm(2),用野生型MC重建的小鼠显示出与对照小鼠相当的损伤(25 mm(2)),而用Camp(-/-) MC重建的小鼠平均损伤面积为120 mm(2)。对从肥大细胞中纯化的cathelicidin肽进行表面增强激光解吸/电离飞行时间质谱(SELDI-TOF-MS)分析,确定其为一种独特的28个氨基酸的肽。综合这些结果表明,MC赋予皮肤对革兰氏阳性细菌感染的防御能力,这一功能部分由一种独特的cathelicidin肽的表达介导。

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