基于发病年龄、淋巴异常和遗传的原发性淋巴水肿最新分类。

Lymphology Pub Date : 2023-01-01
N F Liu, M Z Gao, P E Maltese, M Bertelli
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引用次数: 0

摘要

原发性淋巴水肿(PLE)是一种由淋巴发育不良引起的慢性疾病,会发展为不可逆转的组织水肿和肥大。迄今为止,人们对原发性淋巴水肿的了解还很有限。本研究的目的是为下肢淋巴结肿大性水肿设计一个最新的分类系统,共纳入 1013 名下肢淋巴结肿大性水肿患者。研究记录了患者的性别、发病年龄、部位、家族史和发病率。评估了磁共振淋巴造影(MRL)、吲哚菁绿淋巴造影(ICGL)和淋巴霉素造影(LSG)的淋巴成像结果、皮肤组织免疫组织化学染色、全外显子组测序以及基因型与表型的相关性。患者被分为先天发病和晚期发病两类。晚期发病类别根据发育年龄进一步划分。先天性发病与晚发性PLE的比例为1:4,青少年时期发病率最高。先天性发病组和晚期发病组的性别比例分别为1.04:1和1.5:1。研究发现了三种主要的淋巴异常,其中以淋巴管延迟或部分显示为特征的节段性淋巴功能障碍最为常见,与FLT4、GJC2、CELSR1和PTPN14突变有关。其次是淋巴管增生,这与 FOXC2 和 GATA2 变体有关,然后是初始淋巴管增生或功能障碍,这在先天性 PLE 患者中更为常见,与 FLT4 突变有关。本文提出了淋巴异常的功能和结构综合分类法,包括节段性淋巴功能障碍、淋巴增生和初始淋巴增生或功能障碍。
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An Updated Classification of Primary Lymphedema Based on Age of Onset, Lymphatic Anomalies, and Genetics.

Primary lymphedema (PLE) is a chronic disease caused by lymphatic dysplasia and progresses to irreversible tissue edema and hypertrophy. Understanding of PLE has been hitherto limited. The aim of this study is to devise an updated classification system for PLE of 1013 patients with PLE of lower limb were enrolled. Sex, age of onset, location, family history and morbidity were documented. The lymphatic imaging findings of magnetic reso-nance lymphography (MRL), indocyanine green lymphography (ICGL) and lymphoscin-tigraphy (LSG), skin tissue immunohisto-chemical staining, whole exome sequencing and the correlation of genotype-phenotype were evaluated. Patients were divided into a congenital onset category and a late onset category. The late onset category was further divided according to developmental age. The ratio of congenital-onset to late-onset PLE was 1:4 and that the highest incidence was in adolescence. The sex ratio was 1.04:1 and 1.5:1 in congenital-onset and late-onset groups, respectively. Three major lymphatic anomalies were identified, in which segmental lymphatic dysfunction, characterized by delayed or partial demonstration of lymph vessels, is the most common and associated with FLT4, GJC2, CELSR1, and PTPN14 mutations. The next most common type is lymphatic hyperplasia, which is associated with FOXC2 and GATA2 variants, followed by initial lymphatic aplasia or dysfunction, which is more common in pa-tients with congenital PLE and associated with FLT4 mutation. A functional and structural combined classification of lymphatic anomalies is proposed, which includes segmental lymphatic dysfunction, lymphatic hyperplasia and initial lymphatic aplasia or dysfunction.

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