The role of the cyclooxygenase-2 pathway in tissue ischemia and revascularization following skeletal muscle injury induced by bothropic snake venom

IF 2.9 4区医学 Q2 PERIPHERAL VASCULAR DISEASE

Microvascular research Pub Date : 2024-11-05 DOI:10.1016/j.mvr.2024.104760

Melissa Rodrigues Correia , Sang Won Han , Teresa Escalante , Vanessa Moreira

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引用次数: 0

Abstract

Bothrops asper venom (Bav) contains metalloproteinases that disrupt the microvascular system, impairing muscle tissue regeneration after injury. This study investigated the impact of the cyclooxygenase-2 (COX-2) pathway on vascular injury and revascularization in muscle injuries induced by Bav. Mice were injected with Bav into the gastrocnemius muscle and treated with lumiracoxib, a selective COX-2 inhibitor, 30 min, 2 days, and 6 days post-Bav injection. Muscle tissue was analyzed at 24 h, 7 days, and 21 days post-injection. A decrease in COX-2 expression at 24 h post-Bav injection indicated significant necrosis and tissue loss. Both Bav injection and lumiracoxib treatment influenced the decrease of prostaglandin (PG)D₂ and PGE₂ production. Seven and 21 days post-Bav injections, COX-2 expression increased, along with PGDs levels unaffected by lumiracoxib, indicating that the other isoform COX-1 pathway could contribute to the release of PGs. Bav/lumiracoxib treated animals presented exacerbated limb ischemia, implying that COX-2-derived prostaglandins preserve vessel integrity. CD31, an angiogenesis marker, initially (24 h) decreased post-Bav injection but increased at 7 and 21 days in Bav/lumiracoxib mice, suggesting a down-modulatory role for COX-2-derived prostaglandins in early angiogenesis and tissue regeneration. Vascular endothelial growth factor (VEGF) production rose 7 days post-Bav injection, supporting its role in angiogenesis. Previous treatment with lumiracoxib promoted release of VEGF levels 21 days post-Bav injury showing that the inhibition of COX-2 pathway in the early stage of revascularization stimulates the neovascularization regulated by elevated release of VEGF. Similarly, metalloproteinases (MMPs), such as MMP-9, MMP-10, and MMP-13, crucial for vascular remodeling, were elevated 21 days after Bav/lumiracoxib treatment. In conclusion, the COX-2 pathway is essential to decrease the high grade of ischemia caused by acute injury induced by Bav. However, the decrease of activity in the COX-2 pathway in the first stages of revascularization contributes to the elevated production of key pro-angiogenic mediators that up-regulate the restoration of microvasculature and blood flow in muscle tissue injured by botropic venoms.

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环氧化酶-2通路在两种蛇毒引起的骨骼肌损伤后组织缺血和血管再通中的作用。

两栖类毒液（Bav）含有金属蛋白酶，会破坏微血管系统，从而影响肌肉组织在损伤后的再生。本研究调查了环氧化酶-2（COX-2）通路对 Bav 诱发的肌肉损伤中血管损伤和血管再通的影响。向小鼠的腓肠肌注射 Bav，并在注射后 30 分钟、2 天和 6 天使用鲁米拉考昔布（一种选择性 COX-2 抑制剂）治疗。在注射后 24 小时、7 天和 21 天对肌肉组织进行分析。注射 Bav 后 24 小时，COX-2 表达下降，表明肌肉组织严重坏死和损失。Bav 注射和鲁米拉考昔布治疗都会影响前列腺素（PG）D2 和 PGE2 的产生。注射 Bav 后 7 天和 21 天，COX-2 表达增加，而 PGDs 水平不受鲁米拉考昔布的影响，这表明另一种同工酶 COX-1 途径可能有助于 PGs 的释放。经 Bav/lumiracoxib 处理的动物肢体缺血加剧，这意味着 COX-2 衍生的前列腺素可保护血管完整性。血管生成标志物 CD31 在注射 Bav 后最初（24 小时）有所下降，但在注射 Bav/lumiracoxib 后 7 天和 21 天又有所上升，这表明 COX-2 衍生的前列腺素在早期血管生成和组织再生中起到了下调作用。注射 Bav 后 7 天，血管内皮生长因子（VEGF）的生成量上升，支持其在血管生成中的作用。之前使用鲁米拉考昔布（lumiracoxib）治疗可促进巴甫损伤后 21 天血管内皮生长因子水平的释放，这表明在血管再通的早期阶段抑制 COX-2 通路可刺激血管内皮生长因子的释放，从而调节血管新生。同样，对血管重塑至关重要的金属蛋白酶（MMPs），如 MMP-9、MMP-10 和 MMP-13，也在 Bav/lumiracoxib 治疗 21 天后升高。总之，COX-2 通路对于减轻 Bav 引起的急性损伤导致的高度缺血至关重要。然而，在血管再通的最初阶段，COX-2 通路活性的降低有助于促进血管生成的关键介质的生成，从而上调受肉毒中毒损伤的肌肉组织微血管和血流的恢复。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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来源期刊

Microvascular research 医学-外周血管病

CiteScore

6.00

自引率

3.20%

发文量

158

审稿时长

43 days

期刊介绍： Microvascular Research is dedicated to the dissemination of fundamental information related to the microvascular field. Full-length articles presenting the results of original research and brief communications are featured. Research Areas include: • Angiogenesis • Biochemistry • Bioengineering • Biomathematics • Biophysics • Cancer • Circulatory homeostasis • Comparative physiology • Drug delivery • Neuropharmacology • Microvascular pathology • Rheology • Tissue Engineering.