人类淋巴水肿引起的Connexin47 R260C点突变的CRISPR小鼠模型中的异常淋巴表型

IF 0.7 4区 医学 Q4 IMMUNOLOGY Lymphology Pub Date : 2021-01-01
D J Mustacich, R I Kylat, M J Bernas, R J Myles, J A Jones, J D Kanady, A M Simon, T G Georgieva, M H Witte, R P Erickson, P W Pires
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引用次数: 0

摘要

连接蛋白形成缝隙连接,控制细胞间离子和小分子的交换,在淋巴管内的淋巴运动中起重要作用。Connexin47 (CX47)在淋巴内皮细胞中高表达,CX47错义突变,即R260C,与人类原发性淋巴水肿共分离。然而,利用CX47基因敲除小鼠的研究未能证明任何淋巴异常。为了揭示表达突变的CX47蛋白的淋巴后果,我们使用CRISPR技术创建了一只携带CX47错义突变(Cx47R259C)的小鼠,该突变相当于与人类原发性淋巴水肿相关的人类CX47R260C错义突变。皮内Evans Blue染料注射发现纯合子Cx47R259C小鼠的区域淋巴结比野生型增加了2倍,特别是在颈静脉区域(分别为4.8±0.4和2.0±0.0),p
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Abnormal lymphatic phenotype in a CRISPR mouse model of the human lymphedema-causing Connexin47 R260C point mutation.

Connexin proteins form gap junctions controlling exchange of ions and small molecules between cells and play an important role in movement of lymph within lymphatic vessels. Connexin47 (CX47) is highly expressed in lymphatic endothelial cells and CX47 missense mutations, i.e., R260C, cosegregate with primary lymphedema in humans. However, studies utilizing CX47 knockout mice have failed to demonstrate any lymphatic anomalies. To unravel the lymphatic consequences of expressing a mutant CX47 protein, we used CRISPR technology to create a mouse carrying a Cx47 missense mutation (Cx47R259C) equivalent to the human CX47R260C missense mutation associated with human primary lymphedema. Intradermal Evans Blue dye injection identified a 2-fold increase in regional lymph nodes in homozygous Cx47R259C mice compared to wildtype, particularly in the jugular region (4.8 ± 0.4 and 2.0 ± 0.0, respectively, p<0.01). Associated lymphatic channels were increased in Cx47R259C mice and mesenteric lymph reflux occurred in homozygous Cx47R259C mice but not in wildtype. Contractility of superficial cervical lymphatics, assessed by pressure myography, was reduced in homozygous Cx47R259C mice compared to wildtype. In conclusion, our data are the first to demonstrate a role for the Cx47 protein in lymphatic anatomy and function. This phenotype is similar to that found with other valve deficient mouse mutants, e.g., in Foxc2. Of significance, this study is the first to use CRISPR technology to develop a pre-clinical model of primary lymphedema and demonstrates the importance of distinguishing between lack of and presence of mutant protein when developing clinically relevant animal models for translation of pre-clinical findings.

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来源期刊
Lymphology
Lymphology 医学-免疫学
CiteScore
5.20
自引率
8.00%
发文量
29
审稿时长
3 months
期刊介绍: The Journal contains original articles, special features (see below), and information regarding the International Society of Lymphology. It seeks original papers dealing with clinical and basic studies of the lymphatic system and its disorders including related fields. Articles are accepted for external review and publication on the condition that they are contributed to Lymphology only and that no substantial part has been or will be published elsewhere.
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