Bierkarre H, Harder J, Cuthbert R, Emery P, Leuschner I, Mrowietz U, Hedderich J, McGonagle D, Gläser R
a Department of Dermatology , University Hospital of Schleswig-Holstein , Kiel , Germany.
b Leeds Institute of Rheumatic and Musculoskeletal Medicine , University of Leeds , Leeds , United Kingdom.
Scand J Rheumatol. 2016;45(3):188-96. doi: 10.3109/03009742.2015.1091497. Epub 2015 Nov 24.
This study tested the hypothesis that a differential innate immune antimicrobial peptide (AMP) profile was evident between the skin and joints in psoriasis and psoriatic arthritis (PsA) and that PsA synovitis may have a distinct AMP pattern compared to other arthropathies.
Twenty-two cases had knee biopsies [10 PsA, eight rheumatoid arthritis (RA), and four osteoarthritis (OA)]. Lesional and non-lesional skin biopsies in psoriasis and control tissue were also obtained (n = 4 each). Immunohistochemistry with semi-quantitative scoring of both synovium and skin was performed using the following panel of AMPs: S100 A8, S100 A9, human neutrophil peptides 1-3 (HNP1-3), human β-defensins 2 and 3 (hBD-2 and hBD-3), cathelicidin LL-37, psoriasin (S100 A7), and ribonuclease 7 (RNase 7).
Similar expression of S100 A8, S100 A9, and HNP1-3 was detectable in PsA and RA synovium but only in the synovium sublining layer (SSL). No expression of psoriasin, RNase 7, hBD-2, and hBD-3 could be detected in the synovial tissue of PsA, RA, or OA. All psoriasis skin samples exhibited broad expression of all investigated AMPs, with strong keratinocyte expression.
Given that some AMPs, especially hBD-2, are genetically linked to psoriasis and are only expressed in the skin, these findings show how differential AMP expression in innate immune responses may contribute to disease heterogeneity between PsA and psoriasis and provides a genetic basis for the non-progression of psoriasis subgroups to PsA.
本研究检验了以下假设:在银屑病和银屑病关节炎(PsA)中,皮肤和关节之间存在明显不同的先天性免疫抗菌肽(AMP)谱,并且与其他关节病相比,PsA滑膜炎可能具有独特的AMP模式。
对22例患者进行膝关节活检[10例PsA、8例类风湿性关节炎(RA)和4例骨关节炎(OA)]。还获取了银屑病患者的病变和非病变皮肤活检样本以及对照组织(各n = 4)。使用以下一组AMP对滑膜和皮肤进行免疫组织化学及半定量评分:S100 A8、S100 A9、人中性粒细胞肽1 - 3(HNP1 - 3)、人β - 防御素2和3(hBD - 2和hBD - 3)、杀菌肽LL - 37、银屑素(S100 A7)和核糖核酸酶7(RNase 7)。
在PsA和RA滑膜中可检测到S100 A8、S100 A9和HNP1 - 3的相似表达,但仅在滑膜衬里下层(SSL)。在PsA、RA或OA的滑膜组织中未检测到银屑素、RNase 7、hBD - 2和hBD - 3的表达。所有银屑病皮肤样本均表现出所有研究的AMP的广泛表达,角质形成细胞表达强烈。
鉴于一些AMP,尤其是hBD - 2,与银屑病存在遗传关联且仅在皮肤中表达,这些发现表明先天性免疫反应中AMP表达的差异可能如何导致PsA和银屑病之间的疾病异质性,并为银屑病亚组不发展为PsA提供了遗传基础。
