Phosphodiesterase 4 is overexpressed in human keloids and its inhibition reduces fibroblast activation and skin fibrosis

IF 4.7 2区 医学 Q1 BIOCHEMISTRY & MOLECULAR BIOLOGY
Javier Milara , Pilar Ribera , Severiano Marín , Paula Montero , Inés Roger , Herman Tenor , Julio Cortijo
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引用次数: 0

Abstract

There is a pressing medical need for improved treatments in skin fibrosis including keloids and hypertrophic scars (HTS). This study aimed to characterize the role of phosphodiesterase 4 (PDE4), specifically PDE4B in fibrotic skin remodeling in vitro and in vivo.

In vitro, effects of PDE4A-D (Roflumilast) or PDE4B (siRNA) inhibition on TGFβ1-induced myofibroblast differentiation and dedifferentiation were studied in normal (NHDF) and keloid (KF) human dermal fibroblasts. In vivo, the role of PDE4 on HOCl-induced skin fibrosis in mice was addressed in preventive and therapeutic protocols.

PDE4B (mRNA, protein) was increased in Keloid > HTS compared to healthy skin and in TGFβ-stimulated NHDF and KF. In Keloid > HTS, collagen Iα1, αSMA, TGFβ1 and NOX4 mRNA were all elevated compared to healthy skin confirming skin fibrosis.

In vitro, inhibition of PDE4A-D and PDE4B similarly prevented TGFβ1-induced Smad3 and ERK1/2 phosphorylation and myofibroblast differentiation, elevated NOX4 protein and proliferation in NHDF. PDE4A-D inhibition enabled myofibroblast dedifferentiation and curbed TGFβ1-induced reactive oxygen species and fibroblast senescence. In KF PDE4A-D inhibition restrained TGFβ1-induced Smad3 and ERK1/2 phosphorylation, myofibroblast differentiation and senescence. Mechanistically, PDE4A-D inhibition rescued from TGFβ1-induced loss in PPM1A, a Smad3 phosphatase. In vivo, PDE4 inhibition mitigated HOCl-induced skin fibrosis in mice in preventive and therapeutic protocols.

The current study provides novel evidence evolving rationale for PDE4 inhibitors in skin fibrosis (including keloids and HTS) and delivered evidence for a functional role of PDE4B in this fibrotic condition.

Abstract Image

磷酸二酯酶 4 在人类瘢痕疙瘩中过度表达,抑制该酶可减少成纤维细胞活化和皮肤纤维化。
目前,医学界迫切需要改进治疗皮肤纤维化(包括瘢痕疙瘩和增生性疤痕)的方法。本研究旨在阐明磷酸二酯酶4(PDE4),特别是PDE4B在体外和体内皮肤纤维化重塑中的作用。在体外,研究了在正常(NHDF)和瘢痕疙瘩(KF)人真皮成纤维细胞中抑制 PDE4A-D (Roflumilast) 或 PDE4B (siRNA) 对 TGFβ1 诱导的肌成纤维细胞分化和去分化的影响。在预防和治疗方案中,研究了 PDE4 对 HOCl 诱导的小鼠皮肤纤维化的作用。与健康皮肤相比,在 Keloid > HTS 中,以及在 TGFβ 刺激的 NHDF 和 KF 中,PDE4B(mRNA、蛋白质)均有所增加。与健康皮肤相比,在瘢痕疙瘩 > HTS 中,胶原 Iα1、αSMA、TGFβ1 和 NOX4 mRNA 均升高,证实了皮肤纤维化。在体外,抑制 PDE4A-D 和 PDE4B 同样能阻止 TGFβ1 诱导的 Smad3 和 ERK1/2 磷酸化、肌成纤维细胞分化、NOX4 蛋白质升高以及 NHDF 的增殖。抑制 PDE4A-D 可使肌成纤维细胞去分化,并抑制 TGFβ1 诱导的活性氧和成纤维细胞衰老。在KF中,PDE4A-D抑制剂抑制了TGFβ1诱导的Smad3和ERK1/2磷酸化、肌成纤维细胞分化和衰老。从机理上讲,PDE4A-D抑制剂可挽救TGFβ1诱导的Smad3磷酸化酶PPM1A的损失。在体内,在预防和治疗方案中,抑制 PDE4 可减轻 HOCl 诱导的小鼠皮肤纤维化。目前的研究提供了新的证据,进一步证明了 PDE4 抑制剂在皮肤纤维化(包括瘢痕疙瘩和 HTS)中的合理性,并提供了 PDE4B 在这种纤维化状况中发挥功能性作用的证据。
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来源期刊
CiteScore
7.70
自引率
3.90%
发文量
410
审稿时长
36 days
期刊介绍: Chemico-Biological Interactions publishes research reports and review articles that examine the molecular, cellular, and/or biochemical basis of toxicologically relevant outcomes. Special emphasis is placed on toxicological mechanisms associated with interactions between chemicals and biological systems. Outcomes may include all traditional endpoints caused by synthetic or naturally occurring chemicals, both in vivo and in vitro. Endpoints of interest include, but are not limited to carcinogenesis, mutagenesis, respiratory toxicology, neurotoxicology, reproductive and developmental toxicology, and immunotoxicology.
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