真菌病和塞扎里综合征中的血源性播种:现有证据和临床意义。

IF 11 1区 医学 Q1 DERMATOLOGY
Robert Gniadecki, Emmanuella Guenova, Christiane Querfeld, Jan P Nicolay, Julia Scarisbrick, Lubomir Sokol
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引用次数: 0

摘要

皮肤 T 细胞淋巴瘤(CTCLs)是一类异质性疾病,其特征是皮肤中出现异常的肿瘤性 T 细胞生长。放线菌病(MF)是最常见的皮肤 T 细胞淋巴瘤,表现为皮肤红斑和/或斑块、肿瘤或红斑。该病可累及血液、淋巴结,很少累及内脏。塞扎里综合征(SS)是与 MF 相关的一种独特的白血病/淋巴瘤综合征,确诊时表现为血液和皮肤受累。MF/SS 的发病机制尚未完全阐明。远处皮肤病变的出现支持了一种假设,即 MF/SS 病变可能是通过血源性播种形成的。恶性 T 细胞和正常 T 细胞在表型上的相似性使人们认为,疾病的诱发突变发生在特定亚型的成熟 T 细胞中,它们是大多数 CTCL 的罪魁祸首。然而,这种成熟 T 细胞前体模型并不总是与 MF/SS 发病机制的临床观察和研究相一致。在此,我们回顾了支持 MF/SS 发病机制替代模型的证据,该模型将血源性播种作为疾病发生和发展的关键过程。根据这一假说,恶性转化发生在 T 细胞发育的早期阶段(可能在骨髓或胸腺中),产生循环肿瘤性 T 细胞,这些细胞在微环境最有利于增殖和进化的皮肤上定植。这些变异的前体细胞在皮肤上播种,并在那里找到合适的生长环境,发展成临床上可感知的疾病。随后,恶性 T 细胞会再次进入血液,重新播种已有的病灶,并播种新的皮肤区域,导致病灶和肿瘤的转录组发生同步和趋同的变化,并导致临床疾病进展--"连续血源性播种 "捕捉到了这一时间现象。这一模型从根本上改变了目前对 CTCL 发病机制的认识,将其从一种主要是皮肤病、继发于血液的疾病转变为一种全身性疾病,在这种疾病中,恶性细胞通过血液扩散到皮肤并不是疾病晚期的一种现象,而是发病机制的一个重要组成部分。对 MF/SS 的这种认识可能会产生一些临床影响,包括使我们评估血液肿瘤负荷的方法标准化、预后和监测方面的潜在进步以及研究改善患者预后的综合治疗方法。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Haematogenous seeding in mycosis fungoides and Sézary syndrome: Current evidence and clinical implications.

Cutaneous T-cell lymphomas (CTCLs) are a heterogeneous group of diseases characterised by abnormal neoplastic T-cell growth in the skin. Mycosis fungoides (MF), the most common CTCL, manifests as erythematous skin patches and/or plaques, tumours or erythroderma. The disease may involve blood, lymph nodes and rarely viscera. Sézary syndrome (SS) is a unique leukaemia/lymphoma syndrome related to MF, which presents with blood and skin involvement at diagnosis. The pathogenesis of MF/SS is not fully elucidated. The presence of skin lesions at distant sites underpins a hypothesis that MF/SS lesions may develop through haematogenous seeding. Phenotypic similarities between malignant and normal T-cells led to the notion that disease-initiating mutations occur in specific subtypes of mature T-cells, which are responsible for most CTCLs. However, this mature T-cell precursor model is not always consistent with clinical observations and research on MF/SS pathogenesis. Here, we review evidence supporting an alternative model of pathogenesis for MF/SS involving haematogenous seeding as a key process responsible for the initiation and progression of the disease. According to this hypothesis, malignant transformation occurs at an early stage of T-cell development (probably in bone marrow or thymus), yielding circulating neoplastic T-cells which colonise the skin where the microenvironment is most permissive for proliferation and evolution. These mutated precursor cells seed the skin where they find a suitable niche to develop into clinically perceptible disease. Subsequently, malignant T-cells can re-enter the bloodstream, re-seed pre-existing lesions and seed new areas of the skin, causing synchronous and convergent changes in the transcriptomic profile of lesions and tumours, and clinical disease progression - 'consecutive haematogenous seeding' captures this temporal phenomenon. This model radically changes the current understanding of CTCL pathogenesis, transforming it from a primarily cutaneous disease with secondary involvement of blood, to a systemic disease, where the spread of malignant cells through the blood to the skin is not a phenomenon of advanced disease but is an essential component of pathogenesis. This understanding of MF/SS could have several clinical implications, including standardising our approach to assessing blood tumour burden, potential advances in prognosis and monitoring, and investigating combination treatments to improve patient outcomes.

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来源期刊
British Journal of Dermatology
British Journal of Dermatology 医学-皮肤病学
CiteScore
16.30
自引率
3.90%
发文量
1062
审稿时长
2-4 weeks
期刊介绍: The British Journal of Dermatology (BJD) is committed to publishing the highest quality dermatological research. Through its publications, the journal seeks to advance the understanding, management, and treatment of skin diseases, ultimately aiming to improve patient outcomes.
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