Bhattacharyya Swati, Varga John
Division of Rheumatology, Northwestern University Feinberg School of Medicine, 240 E. Huron St., Chicago, IL, 60611, USA,
Curr Rheumatol Rep. 2015 Jan;17(1):474. doi: 10.1007/s11926-014-0474-z.
Pathological fibrosis is a distinguishing hallmark of systemic sclerosis (SSc) as well as a number of more common conditions. Fibrosis is a complex and dynamic process associated with immune dysregulation, vasculopathy, and uncontrolled extracellular matrix production leading to intractable scar formation in the skin and internal organs. Persistent or recurrent chemical, infectious, mechanical, or autoimmune injury in genetically predisposed individuals causes sustained fibroblasts activation. Innate immune signaling via toll-like receptors (TLRs) is increasingly recognized as a key player driving the persistent fibrotic response in SSc. In particular, expression of TLR4 as well as its endogenous ligands are elevated in lesional tissue from patients with SSc. Ligand-induced TLR4 activation elicits potent stimulatory effects on fibrotic gene expression and myofibroblast differentiation. Furthermore, TLR4 appears to sensitize fibroblasts to the profibrotic stimulatory effect of transforming growth factor-β. This review highlights recent advances and emerging paradigms for understanding the regulation, complex functional roles, and therapeutic potential of TLRs in SSc pathogenesis.
病理性纤维化是系统性硬化症(SSc)以及一些更常见病症的显著标志。纤维化是一个复杂且动态的过程,与免疫失调、血管病变以及不受控制的细胞外基质产生相关,导致皮肤和内脏器官形成难治性瘢痕。在具有遗传易感性的个体中,持续或反复的化学、感染、机械或自身免疫损伤会导致成纤维细胞持续活化。通过Toll样受体(TLR)的固有免疫信号传导日益被认为是驱动SSc中持续性纤维化反应的关键因素。特别是,TLR4及其内源性配体在SSc患者的病变组织中表达升高。配体诱导的TLR4激活对纤维化基因表达和肌成纤维细胞分化产生强大的刺激作用。此外,TLR4似乎使成纤维细胞对转化生长因子-β的促纤维化刺激作用敏感。本综述重点介绍了在理解TLR在SSc发病机制中的调节、复杂功能作用和治疗潜力方面的最新进展和新兴范例。
