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  • west china medical publishers
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    find Author "李海泉" 2 results
    • 慢性阻塞性肺疾病急性加重引起患者疼痛的病因初步探討

      目的初步探討慢性阻塞性肺疾病(簡稱慢阻肺)急性加重引起患者不同部位疼痛發生的病因。方法回顧性分析自 2017 年 6 月至 2019 年 3 月入住徐州醫科大學第二附屬醫院呼吸內科因慢阻肺急性加重引發不同部位疼痛的 50 例患者的臨床資料。入選患者均依據病情需要給予化痰、抗感染、解痙止喘、吸氧改善通氣等綜合治療。評估時間點為入院初治療前、治療后第 3 天、治療后 1 周;評估方法采用簡式麥吉爾疼痛問卷(SF-MPQ)量表對各時間點患者疼痛情況進行評分。同時評估各時間點患者血細胞分析、降鈣素原、超敏 C 反應蛋白、血氣分析;酶聯免疫吸附試驗法測定各時間點患者血清 5-羥色胺及緩激肽水平。結果與治療前比較,經治療后第 3 天、治療后 1 周后,患者 SF-MPQ 疼痛量表評分值明顯降低,血清 5-羥色胺及緩激肽水平降低(均 P<0.05)。患者 SF-MPQ 疼痛量表評分與血細胞分析中白細胞計數、超敏 C 反應蛋白、降鈣素原、動脈血二氧化碳分壓、血清 5-羥色胺及緩激肽水平呈正相關(均 P<0.05),與動脈血氧分壓呈負相關(P<0.05)。結論慢阻肺急性加重引起的疼痛癥狀可能與全身炎癥反應、低氧血癥及體內二氧化碳潴留致高碳酸血癥有一定關系。

      Release date:2021-01-26 05:01 Export PDF Favorites Scan
    • Effects of Ambroxol on JNK Signaling Pathway in Gastric Aspiration Induced Lung Injury in Rats

      ObjectiveTo investigate the effect of ambroxol hydrochloride on c-Jun N-terminal kinase (JNK) signal pathway in gastric aspiration lung injury. MethodsForty healthy male Sprague Dawley rats were randomly divided into a control group, an injury group, a SP600125 (JNK specific inhibitor) group and an ambroxol group. The model of gastric aspiration lung injury was established by aspiration of gastric contents. The rats in the SP600125 group preoperatively received intravenous injection of JNK specific inhibitor SP600125 (3 mg/100 g). The rats in the ambroxol group received intravenous injection of ambroxol hydrochloride (50 mg/kg) 2 hours after the damage occurred. The neutrophil count and malondialdehyde (MDA) activity in bronchoalveolar lavage fluid (BALF), the lung wet weight/dry weight ratio (W/D), and myeloperoxidase (MPO) activity were measured. The protein expressions of JNK and phosphorylated JNK (p-JNK) and inducible nitric oxide synthase (iNOS) in lung tissue were detected by Western blot method. The changes of lung tissue structure were observed under light microscope. ResultsIn the injury group, the neutrophil counts and MDA activity in BALF, W/D, MPO activity, p-JNK and iNOS protein expression increased significantly, lung tissue appeared obvious histopathological injury compared with the control group. In the SP600125 group and the ambroxol group, neutrophil count and MDA activity in BALF, lung W/D, MPO activity, p-JNK and iNOS protein expression were significantly decreased compared with the injury group (P < 0.05), and the damage of the lung tissue pathology was reduced. The expression of JNK protein in lung tissue was not different in all groups (P > 0.05). ConclusionsJNK is involved in inflammatory reaction of gastric aspiration lung injury. The protective effect of ambroxol may be related to the inhibition of JNK signaling pathway and the inhibition of iNOS expression.

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  • 松坂南