Targeting CD13/aminopeptidase N as a novel therapeutic approach for scleroderma fibrosis.

IF 11.4 1区 医学 Q1 RHEUMATOLOGY
Sei Muraoka, William D Brodie, Megan N Mattichak, Mikel Gurrea-Rubio, Yuzo Ikari, Caroline Foster, M Asif Amin, Neha Khanna, Hafsa Amin, Phillip L Campbell, Sirapa Vichaikul, Ellen N Model, Morgan M Omara, Steven Petrovski, Karly Kozicki, Camilia Amarista, Anna Webber, Mustafa Ali, Pamela J Palisoc, Jonatan Hervoso, Jeffrey H Ruth, Lam C Tsoi, John Varga, Johann E Gudjonsson, Dinesh Khanna, David A Fox, Pei-Suen Tsou
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引用次数: 0

Abstract

Objective: Systemic sclerosis (SSc) is an autoimmune multisystem disease with poorly understood pathogenesis and ineffective treatment options. Soluble CD13 (sCD13), generated by cleavage of cell surface CD13 via matrix metalloproteinase 14 (MMP14), signals through the bradykinin receptor B1 (B1R) to elicit pro-inflammatory, pro-arthritic, and pro-angiogenic responses. In this study we explored the anti-fibrotic potential of targeting the sCD13-B1R axis in SSc.

Methods: The expression of CD13, B1R and MMP14 was examined in SSc skin and explanted dermal fibroblasts. The efficacy of B1R antagonists in the inhibition on fibrosis was determined in vitro and in vivo.

Results: Expression of the genes for CD13, B1R and MMP14 was elevated in skin biopsies from patients with diffuse cutaneous (dc)SSc. Notably, single cell analysis of SSc skin biopsies revealed the highest BDKRB1 expression in COL8A1-positive myofibroblasts, a population exclusively seen in SSc. TGF-β induced the expression of BDKRB1 and production of sCD13 by dcSSc skin fibroblasts. Treatment of dcSSc fibroblasts with sCD13 promoted fibrotic gene expression, signaling, cell proliferation, migration, and gel contraction. The profibrotic sCD13 or TGFβ responses were prevented by a B1R antagonist. Mice lacking Cd13 or Bdkrb1 were resistant to bleomycin-induced skin fibrosis and inflammation. Pharmacological B1R inhibition had a comparable antifibrotic effect.

Conclusion: These results are the first to demonstrate a key role for sCD13 in SSc skin fibrosis, and suggest that targeting the sCD13-B1R signaling axis is a promising novel therapeutic approach for SSc.

Abstract Image

将 CD13/氨基肽酶 N 作为治疗硬皮病纤维化的新方法。
目的:系统性硬化症(SSc)是一种自身免疫性多系统疾病,其发病机制尚不清楚,治疗效果也不理想。细胞表面 CD13 通过基质金属蛋白酶 14(MMP14)裂解产生可溶性 CD13(sCD13),它通过缓激肽受体 B1(B1R)发出信号,引起促炎症、促关节炎和促血管生成反应。在这项研究中,我们探讨了靶向 sCD13-B1R 轴在 SSc 中的抗纤维化潜力:方法:研究人员检测了 SSc 皮肤和真皮成纤维细胞中 CD13、B1R 和 MMP14 的表达。结果:CD13、B1R 和 MMP14 基因的表达在 SSc 皮肤和外植真皮纤维细胞中进行了检测,并测定了 B1R 拮抗剂在体外和体内抑制纤维化的效果:结果:CD13、B1R 和 MMP14 基因的表达在弥漫性皮肤 (dc) SSc 患者的皮肤活检组织中升高。值得注意的是,SSc 皮肤活检组织的单细胞分析显示,COL8A1 阳性的肌成纤维细胞中 BDKRB1 的表达量最高,而这种细胞群仅见于 SSc。TGF-β 可诱导 dcSSc 皮肤成纤维细胞表达 BDKRB1 和产生 sCD13。用 sCD13 处理 dcSSc 成纤维细胞可促进纤维化基因的表达、信号传导、细胞增殖、迁移和凝胶收缩。B1R拮抗剂可阻止sCD13或TGFβ的促纤维化反应。缺乏 Cd13 或 Bdkrb1 的小鼠对博莱霉素诱导的皮肤纤维化和炎症具有抵抗力。药理 B1R 抑制剂具有类似的抗纤维化作用:这些结果首次证明了sCD13在SSc皮肤纤维化中的关键作用,并表明靶向sCD13-B1R信号轴是治疗SSc的一种很有前景的新方法。
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来源期刊
Arthritis & Rheumatology
Arthritis & Rheumatology RHEUMATOLOGY-
CiteScore
20.90
自引率
3.00%
发文量
371
期刊介绍: Arthritis & Rheumatology is the official journal of the American College of Rheumatology and focuses on the natural history, pathophysiology, treatment, and outcome of rheumatic diseases. It is a peer-reviewed publication that aims to provide the highest quality basic and clinical research in this field. The journal covers a wide range of investigative areas and also includes review articles, editorials, and educational material for researchers and clinicians. Being recognized as a leading research journal in rheumatology, Arthritis & Rheumatology serves the global community of rheumatology investigators and clinicians.
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