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人体前臂的再灌注损伤很轻微,且不会因短期缺血预处理而减轻。

Reperfusion injury in the human forearm is mild and not attenuated by short-term ischaemic preconditioning.

作者信息

Kilian J G, Nakhla S, Griffith K, Harmer J, Skilton M, Celermajer D S

机构信息

The Royal Prince Alfred Hospital, Camperdown, New South Wales, Australia.

出版信息

Clin Exp Pharmacol Physiol. 2005 Jan-Feb;32(1-2):86-90. doi: 10.1111/j.1440-1681.2005.04163.x.

DOI:10.1111/j.1440-1681.2005.04163.x
PMID:15730440
Abstract
  1. Ischaemia-reperfusion (IR) injury is an important contributor to tissue damage and has been shown to be attenuated by preconditioning (PC) in some animal models. A recent report has suggested that the forearm can be used for the study of this phenomenon in humans. We aimed to reproduce and further characterize this model. 2. Healthy young adult volunteers (mean (+/-SEM) age 32+/-6 years) were studied on two occasions. During one visit, IR alone was induced by 10 min of upper arm cuff occlusion, whereas on another occasion a PC stimulus (three 3 min cuff inflations) preceded IR. Endothelial function in the ischaemic arm was assessed by measuring arterial flow-mediated dilatation (FMD) and by calculation of forearm blood flow at baseline and 15 and 60 min after IR. Systemic venous blood was sampled from the non-ischaemic arm at baseline, after PC and at 2, 15 and 30 min after IR to assess neutrophil/leucocyte (CD11b) and platelet (bound glycoprotein IIb/IIIa and fibrinogen) activation, as well as numbers of platelet-leucocyte complexes, which were determined by flow cytometry. Because of a lack of measurable effects, the IR experiment was repeated with 20 min ischaemia in six subjects. 3. Five females and eight males completed the study. Flow-mediated dilatation was significantly impaired 30 min after IR (4.1 vs 6.2% at baseline; P<0.05);however, this was not significantly attenuated by ischaemic PC (FMD reduction at 30 min compared with baseline was 2.1+/-0.5% with IR alone and 2.6+/-1.4% with IR after PC; NS). No significant effect was seen on the number of platelet-leucocyte aggregates or on white cell or platelet activation after IR alone or after IR with PC (P>0.6 for all comparisons). Similar results were obtained in six subjects studied subjected to 20 min ischaemia. 4. In conclusion, in healthy young adults, brief periods of skeletal muscle ischaemia lead to arterial endothelial dysfunction, but no significant platelet or white cell activation. Preconditioning does not attenuate this effect on the endothelium. Further experiments with longer ischaemia times and varying PC stimuli may be necessary to produce measurable effects; however, this may prove difficult in conscious human subjects.
摘要
  1. 缺血再灌注(IR)损伤是导致组织损伤的重要因素,在一些动物模型中,预处理(PC)已被证明可减轻这种损伤。最近的一份报告表明,前臂可用于人类该现象的研究。我们旨在重现并进一步描述该模型。2. 对健康的年轻成年志愿者(平均(±标准误)年龄32±6岁)进行了两次研究。在一次就诊期间,通过上臂袖带闭塞10分钟诱导单纯缺血再灌注,而在另一次就诊时,在缺血再灌注之前给予预处理刺激(三次3分钟袖带充气)。通过测量动脉血流介导的扩张(FMD)以及计算缺血再灌注前、缺血再灌注后15分钟和60分钟时的前臂血流量,评估缺血手臂的内皮功能。在基线、预处理后以及缺血再灌注后2分钟、15分钟和30分钟,从非缺血手臂采集全身静脉血,以评估中性粒细胞/白细胞(CD11b)和血小板(结合糖蛋白IIb/IIIa和纤维蛋白原)的活化情况,以及血小板 - 白细胞复合物的数量,这些通过流式细胞术测定。由于缺乏可测量的效应,对6名受试者进行了20分钟缺血的缺血再灌注实验。3. 5名女性和8名男性完成了研究。缺血再灌注后30分钟,血流介导的扩张显著受损(基线时为6.2%,缺血再灌注后为4.1%;P<0.05);然而,缺血预处理并未显著减轻这种损伤(与基线相比,单纯缺血再灌注组30分钟时FMD降低2.1±0.5%,缺血预处理后缺血再灌注组为2.6±1.4%;无显著性差异)。单独缺血再灌注或缺血预处理后缺血再灌注对血小板 - 白细胞聚集体数量、白细胞或血小板活化均无显著影响(所有比较P>0.6)。对6名进行20分钟缺血研究的受试者也得到了类似结果。4. 总之,在健康的年轻成年人中,短暂的骨骼肌缺血会导致动脉内皮功能障碍,但不会引起显著的血小板或白细胞活化。预处理不会减弱对内皮的这种影响。可能需要进行更长缺血时间和不同预处理刺激的进一步实验以产生可测量的效应;然而,这在清醒的人类受试者中可能会很困难。

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