KATP通道功能获得性Cantú综合征小鼠模型的淋巴收缩功能障碍。

IF 5.1 Q2 CELL BIOLOGY
Michael J Davis, Jorge A Castorena-Gonzalez, Hae Jin Kim, Min Li, Maria Remedi, Colin G Nichols
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引用次数: 2

摘要

Cantú综合征(CS)是一种常染色体显性遗传病,由KATP通道Kir6.1和SUR2亚基的功能获得(GoF)突变引起。KATP过度活动导致动脉张力的慢性降低和低血压,导致其他系统性心血管并发症。然而,50%以上的CS患者出现淋巴水肿的潜在机制尚不清楚。我们研究了表达CS基因Kir6.1 (Kir6.1[V65M])或SUR2 (SUR2[A478V], SUR2[R1154Q])突变的小鼠是否会发生淋巴收缩功能障碍。在生理压力范围内腘窝淋巴管收缩功能的压力肌图测试显示,与对照组相比,杂合子Kir6.1[V65M]血管在所有压力下的收缩强度明显受损,自发收缩频率降低。在近红外荧光显微镜下证实了完整腘窝淋巴在体内的收缩功能障碍。纯合子SUR2[A478V]血管在体外表现出严重的收缩功能障碍,而杂合子SUR2[A478V]血管在体外表现出基本正常的收缩功能。然而,对所有三种GoF小鼠品系血管的进一步研究显示,收缩波携带明显中断,传导速度和距离减少,起搏器位点多,波方向逆转。对2阀淋巴管在逆压梯度下被迫泵送的试验显示,所有cs相关基因型在施加的流出负荷下基本上不能泵送。我们的研究结果表明,不同程度的淋巴收缩功能障碍与Kir6.1或SUR2中分子GoF的程度成正比。这是由平滑肌离子通道突变引起的淋巴收缩功能障碍的第一个例子,可能解释了CS患者对淋巴水肿的易感性。
本文章由计算机程序翻译,如有差异,请以英文原文为准。

Lymphatic contractile dysfunction in mouse models of Cantú Syndrome with K<sub>ATP</sub> channel gain-of-function.

Lymphatic contractile dysfunction in mouse models of Cantú Syndrome with K<sub>ATP</sub> channel gain-of-function.

Lymphatic contractile dysfunction in mouse models of Cantú Syndrome with K<sub>ATP</sub> channel gain-of-function.

Lymphatic contractile dysfunction in mouse models of Cantú Syndrome with KATP channel gain-of-function.

Cantú Syndrome (CS) is an autosomal dominant disorder caused by gain-of-function (GoF) mutations in the Kir6.1 and SUR2 subunits of KATP channels. KATP overactivity results in a chronic reduction in arterial tone and hypotension, leading to other systemic cardiovascular complications. However, the underlying mechanism of lymphedema, developed by >50% of CS patients, is unknown. We investigated whether lymphatic contractile dysfunction occurs in mice expressing CS mutations in Kir6.1 (Kir6.1[V65M]) or SUR2 (SUR2[A478V], SUR2[R1154Q]). Pressure myograph tests of contractile function of popliteal lymphatic vessels over the physiological pressure range revealed significantly impaired contractile strength and reduced frequency of spontaneous contractions at all pressures in heterozygous Kir6.1[V65M] vessels, compared to control littermates. Contractile dysfunction of intact popliteal lymphatics in vivo was confirmed using near-infrared fluorescence microscopy. Homozygous SUR2[A478V] vessels exhibited profound contractile dysfunction ex vivo, but heterozygous SUR2[A478V] vessels showed essentially normal contractile function. However, further investigation of vessels from all three GoF mouse strains revealed significant disruption in contraction wave entrainment, decreased conduction speed and distance, multiple pacemaker sites, and reversing wave direction. Tests of 2-valve lymphatic vessels forced to pump against an adverse pressure gradient revealed that all CS-associated genotypes were essentially incapable of pumping under an imposed outflow load. Our results show that varying degrees of lymphatic contractile dysfunction occur in proportion to the degree of molecular GoF in Kir6.1 or SUR2. This is the first example of lymphatic contractile dysfunction caused by a smooth muscle ion channel mutation and potentially explains the susceptibility of CS patients to lymphedema.

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来源期刊
CiteScore
5.70
自引率
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