Prete Marcella, Dammacco Rosanna, Fatone Maria Celeste, Racanelli Vito
Internal Medicine Unit, Department of Biomedical Sciences and Human Oncology (DIMO), University of Bari Medical School, Piazza G. Cesare 11, 70124, Bari, Italy.
Department of Otorhinolaryngology and Ophthalmology, University of Bari Medical School, Bari, Italy.
Clin Exp Med. 2016 May;16(2):125-36. doi: 10.1007/s10238-015-0345-6. Epub 2015 Mar 28.
Autoimmune uveitis (AU), an inflammatory non-infectious process of the vascular layer of the eye, can lead to visual impairment and, in the absence of a timely diagnosis and suitable therapy, can even result in total blindness. The majority of AU cases are idiopathic, whereas fewer than 20 % are associated with systemic diseases. The clinical severity of AU depends on whether the anterior, intermediate, or posterior part of the uvea is involved and may range from almost asymptomatic to rapidly sight-threatening forms. Race, genetic background, and environmental factors can also influence the clinical picture. The pathogenetic mechanism of AU is still poorly defined, given its remarkable heterogeneity and the many discrepancies between experimental and human uveitis. Even so, the onset of AU is thought to be related to an aberrant T cell-mediated immune response, triggered by inflammation and directed against retinal or cross-reactive antigens. B cells may also play a role in uveal antigen presentation and in the subsequent activation of T cells. The management of AU remains a challenge for clinicians, especially because of the paucity of randomized clinical trials that have systematically evaluated the effectiveness of different drugs. In addition to topical treatment, several different therapeutic options are available, although a standardized regimen is thus far lacking. Current guidelines recommend corticosteroids as the first-line therapy for patients with active AU. Immunosuppressive drugs may be subsequently required to treat steroid-resistant AU and for steroid-sparing purposes. The recent introduction of biological agents, such as those targeting tumor necrosis factor-α, is expected to remarkably increase the percentages of responders and to prevent irreversible sight impairment. This paper reviews the clinical features of AU and its crucial pathogenetic targets in relation to the current therapeutic perspectives. Also, the largest clinical trials conducted in the last 12 years for the treatment of AU are summarized and critically discussed.
自身免疫性葡萄膜炎(AU)是一种眼部血管层的炎症性非感染性疾病,可导致视力损害,若未及时诊断和进行适当治疗,甚至会导致完全失明。大多数AU病例为特发性,而与全身性疾病相关的病例不到20%。AU的临床严重程度取决于葡萄膜的前部、中间部或后部是否受累,其范围可从几乎无症状到迅速威胁视力的形式。种族、遗传背景和环境因素也会影响临床表现。由于AU具有显著的异质性以及实验性葡萄膜炎与人类葡萄膜炎之间存在许多差异,其发病机制仍不清楚。即便如此,AU的发病被认为与异常的T细胞介导的免疫反应有关,这种反应由炎症触发并针对视网膜或交叉反应性抗原。B细胞也可能在葡萄膜抗原呈递及随后的T细胞激活中发挥作用。AU的治疗对临床医生来说仍然是一项挑战,尤其是因为缺乏系统评估不同药物疗效的随机临床试验。除局部治疗外,有几种不同的治疗选择,尽管目前还缺乏标准化方案。目前的指南推荐将皮质类固醇作为活动性AU患者的一线治疗药物。随后可能需要使用免疫抑制药物来治疗对类固醇耐药的AU以及为了减少类固醇的使用。最近引入的生物制剂,如那些靶向肿瘤坏死因子-α的药物,预计将显著提高缓解率并预防不可逆的视力损害。本文回顾了AU的临床特征及其与当前治疗观点相关的关键发病靶点。此外,还总结并批判性地讨论了过去12年中为治疗AU而进行的最大规模临床试验。
