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In vivo characterization of doxycycline-mediated protection of aortic function and structure in a mouse model of Marfan syndrome-associated aortic aneurysm

机译:在马凡氏综合征相关主动脉瘤小鼠模型中强力霉素介导的主动脉功能和结构保护的体内表征

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摘要

Aortic aneurysm is the most life-threatening complication in Marfan syndrome (MFS) patients. Doxycycline, a nonselective matrix metalloproteinases inhibitor, was reported to improve the contractile function and elastic fiber structure and organization in a Marfan mouse aorta using ex vivo small chamber myography. In this study, we assessed the hypothesis that a long-term treatment with doxycycline would reduce aortic root growth, improve aortic wall elasticity as measured by pulse wave velocity, and improve the ultrastructure of elastic fiber in the mouse model of MFS. In our study, longitudinal measurements of aortic root diameters using high-resolution ultrasound imaging display significantly decreased aortic root diameters and lower pulse wave velocity in doxycycline-treated Marfan mice starting at 6 months as compared to their non-treated MFS counterparts. In addition, at the ultrastructural level, our data show that long-term doxycycline treatment corrects the irregularities of elastic fibers within the aortic wall of Marfan mice to the levels similar to those observed in control subjects. Our findings underscore the key role of matrix metalloproteinases during the progression of aortic aneurysm, and provide new insights into the potential therapeutic value of doxycycline in blocking MFS-associated aortic aneurysm.
机译:在马凡综合征(MFS)患者中,主动脉瘤是最致命的并发症。据报道,强力霉素是一种非选择性基质金属蛋白酶抑制剂,使用离体小腔室肌成像可以改善Marfan小鼠主动脉的收缩功能,弹性纤维结构和组织。在这项研究中,我们评估了以下假设:在MFS小鼠模型中,长期用多西环素治疗会降低主动脉根生长,改善主动脉壁弹性(通过脉搏波速度测量)并改善弹性纤维的超微结构。在我们的研究中,与未治疗的MFS相比,使用强力霉素治疗的Marfan小鼠从6个月开始使用高分辨率的超声成像纵向测量主动脉根直径可显着降低主动脉根直径并降低脉搏波速度。此外,在超微结构水平上,我们的数据表明,长期使用强力霉素可将Marfan小鼠主动脉壁内弹性纤维的不规则性校正为与对照组相似的水平。我们的发现强调了基质金属蛋白酶在主动脉瘤进展过程中的关键作用,并为强力霉素在阻断MFS相关的主动脉瘤方面的潜在治疗价值提供了新的见解。

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