Hydrogen inhalation therapy alone may not alleviate intestinal mucosal damage in NOMI without total-layer necrosis: An experimental swine model study

单纯氢气吸入疗法可能无法缓解非闭塞性肠系膜缺血(NOMI)患者(无全层坏死)的肠黏膜损伤:一项猪模型实验研究

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Abstract

AIM: Hydrogen inhalation therapy, a novel therapy for reducing oxidative stress in post-cardiac arrest syndrome, was beneficial for superior mesenteric artery (SMA) occlusion. We assessed the efficacy and feasibility of hydrogen inhalation therapy in swine models of critically ill conditions leading to non-occlusive mesenteric ischemia (NOMI) without acute surgical intervention. METHODS: NOMI was induced in eight 3- to 4-month-old female swine under general anesthesia. We defined the initiation of epinephrine administration via the SMA as T = 0 and the initiation of phlebotomy as T = -30 relative to this point. Hemorrhagic shock was induced by combining phlebotomy (T = -30 to -10), continuous systemic norepinephrine administration (T = -30 to 240), and continuous epinephrine injection through the SMA (T = 0-240). The extent of mesenteric ischemia was assessed through gross observation of the intestinal serosa, biomarkers, intestinal pathology, and computed tomography angiography. RESULTS: Control (n = 4) and hydrogen (n = 4) groups with similar baseline characteristics were included. All animals survived until euthanasia (T = 240). The serosa became dark during local epinephrine administration. At T = 240, lactate levels in the control and hydrogen groups were 7.4 (4.7-11.3) and 5.6 (5.0-6.4) mmol/L, respectively, while median 8-hydroxy-2'-deoxyguanosinelevels were 0.15 (0.14-0.18) and 0.15 (0.13-0.16) ng/mL. The pH, base excess, and potassium levels were similar. No significant differences existed in the ischemic grade of the intestinal tract at any time or site. CONCLUSION: Although critically ill conditions can trigger NOMI, the model used in this study did not involve transmural necrosis. Under such conditions, hydrogen inhalation therapy did not reduce histological ischemic damage.

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