Autotaxin inhibition attenuates endothelial permeability after ischemia-reperfusion injury

被引:2
作者
Strumwasser, Aaron [1 ,2 ]
Cohan, Caitlin M. [2 ]
Beattie, Genna [2 ]
Chong, Vincent [2 ]
Victorino, Gregory P. [2 ]
机构
[1] Univ Southern Calif, Keck Sch Med, Los Angeles, CA 90007 USA
[2] Univ Calif San Francisco East Bay, Dept Surg, Oakland, CA USA
来源
CLINICAL HEMORHEOLOGY AND MICROCIRCULATION | 2020年 / 75卷 / 04期
关键词
Autotaxin; anoxia-reoxygenation; ischemia-reperfusion; hydraulic permeability; LYSOPHOSPHATIDIC ACID; LYSOPHOSPHOLIPASE-D; INFLAMMATION; CELLS; ALBUMIN; PLASMA; LIPOPOLYSACCHARIDE; IDENTIFICATION; INCREASES; ADHERENCE;
D O I
10.3233/CH-190732
中图分类号
R5 [内科学];
学科分类号
1002 ; 100201 ;
摘要
BACKGROUND: Autotaxin (ATX-secretory lysophospholipase D) is the primary lysophosphatidic acid (LPA) producing enzyme. LPA promotes endothelial hyper-permeability and microvascular dysfunction following cellular stress. OBJECTIVE: We sought to assess whether ATX inhibition would attenuate endothelial monolayer permeability after anoxiareoxygenation (A-R) in vitro and attenuate the increase in hydraulic permeability observed after ischemia-reperfusion injury (IRI) in vivo. METHODS: A permeability assay assessed bovine endothelial monolayer permeability during anoxia-reoxygenation with/without administration of pipedimic acid, a specific inhibitor of ATX, administered either pre-anoxia or post-anoxia. Hydraulic permeability (L-p) of rat mesenteric post-capillary venules was evaluated after IRI, with and without ATX inhibition. Lastly, L-p was evaluated after the administration of ATX alone. RESULTS: Anoxia-reoxygenation increased monolayer permeability 4-fold (p < 0.01). Monolayer permeability was reduced to baseline similarly in both the pre-anoxia and post-anoxia ATX inhibition groups (each p < 0.01, respectively). L-p was attenuated by 24% with ATX inhibition (p < 0.01). ATX increased L-p from baseline in a dose dependent manner (p < 0.05). CONCLUSIONS: Autotaxin inhibition attenuated increases in endothelial monolayer permeability during A-R in vitro and hydraulic permeability during IRI in vivo. Targeting ATX may be especially beneficial by limiting its downstream mediators that contribute to mechanisms associated with endothelial permeability. ATX inhibitors may therefore have potential for pharmacotherapy during IRI.
引用
收藏
页码:399 / 407
页数:9
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