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干燥综合征唾液腺的细胞和分子多样性:迈向对疾病亚组的更好定义。

Cellular and molecular diversity in Sjogren's syndrome salivary glands: Towards a better definition of disease subsets.

作者信息

Pontarini Elena, Coleby Rachel, Bombardieri Michele

机构信息

Centre for Experimental Medicine and Rheumatology, William Harvey Research Institute, Queen Mary University of London, London, United Kingdom.

Centre for Experimental Medicine and Rheumatology, William Harvey Research Institute, Queen Mary University of London, London, United Kingdom.

出版信息

Semin Immunol. 2021 Dec;58:101547. doi: 10.1016/j.smim.2021.101547. Epub 2021 Dec 4.

DOI:10.1016/j.smim.2021.101547
PMID:34876330
Abstract

Primary Sjögren's syndrome (pSS) is a highly heterogeneous disease in terms of clinical presentation ranging from a mild disease localised to the salivary and lacrimal glands, to multiorgan complications of various degrees of severity, finishing with the evolution, in around 5% of pSS patients, to B cell lymphomas most commonly arising in the inflamed salivary glands. Currently, there are poor positive or negative predictors of disease evolution able to guide patient management and treatment at early stages of the diseases. Recent understanding of the pathogenic mechanisms driving immunopathology in pSS, particularly through histological and transcriptomic analysis of minor and parotid salivary gland (SG) biopsies, has highlighted a high degree of cellular and molecular heterogeneity of the inflammatory lesions but also allowed the identification of clusters of patients with similar underlying SG immunopathology. In particular, patients presenting with high degrees of B/T cell infiltration and the formation of ectopic lymphoid structures (ELS) in the SG have been associated, albeit with conflicting results, with higher degree of disease severity and enhanced risk of lymphoma evolution, suggesting that a dysregulated adaptive immune response plays a key role in driving disease manifestations in pSS. Recent data from randomised clinical trials with novel biological therapies in pSS have also highlighted the potential role of SG immunopathology and molecular pathology in stratifying patients for trial inclusion as well as assessing proof of mechanisms in longitudinal SG biopsies before and after treatment. Although significant progress has been made in the understanding of disease pathogenesis and heterogeneity through cellular and molecular SG pathology, further work is needed to validate their clinical utility in routine clinical settings and in randomised clinical trials.

摘要

原发性干燥综合征(pSS)在临床表现上是一种高度异质性疾病,范围从局限于唾液腺和泪腺的轻度疾病,到不同严重程度的多器官并发症,约5%的pSS患者最终会发展为最常见于炎症性唾液腺的B细胞淋巴瘤。目前,在疾病早期能够指导患者管理和治疗的疾病进展的阳性或阴性预测指标都很匮乏。最近对pSS免疫病理学致病机制的认识,特别是通过对小唾液腺和腮腺活检进行组织学和转录组分析,突出了炎症病变在细胞和分子水平上的高度异质性,但也使得能够识别具有相似潜在唾液腺免疫病理学特征的患者群体。特别是,在唾液腺中出现高度B/T细胞浸润和异位淋巴结构(ELS)形成的患者,尽管结果存在矛盾,但已被认为与更高程度的疾病严重程度和淋巴瘤进展风险增加有关,这表明适应性免疫反应失调在驱动pSS疾病表现中起关键作用。pSS新型生物疗法的随机临床试验的最新数据也突出了唾液腺免疫病理学和分子病理学在对患者进行分层以纳入试验以及评估治疗前后纵向唾液腺活检中的机制证据方面的潜在作用。尽管通过细胞和分子唾液腺病理学在理解疾病发病机制和异质性方面取得了重大进展,但仍需要进一步开展工作,以验证其在常规临床环境和随机临床试验中的临床实用性。

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