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腺苷及 A1 选择性激动剂对离体大鼠心肌细胞缺血性损伤的保护作用微乎其微。

Adenosine and A1 selective agonists offer minimal protection against ischaemic injury to isolated rat cardiomyocytes.

作者信息

Ganote C E, Armstrong S, Downey J M

机构信息

Department of Veterans Affairs Medical Center, Johnson City, TN.

出版信息

Cardiovasc Res. 1993 Sep;27(9):1670-6. doi: 10.1093/cvr/27.9.1670.

DOI:10.1093/cvr/27.9.1670
PMID:8287447
Abstract

OBJECTIVE

The aim was to determine if isolated rat cardiomyocytes could be protected from ischaemic cell death by preincubation with adenosine or adenosine agonists.

METHODS

Cardiomyocytes isolated from rat hearts were preincubated in the presence of adenosine, CCPA (2-chloro-N6-cyclopentyladenosine), or carbachol prior to concentration into an ischaemic slurry. Effects of glycolysis and of isoprenaline were determined by addition of iodoacetic acid or isoprenaline to the ischaemic incubates and by exclusion of glucose from all media. Rates of ischaemic contracture were determined and survival of the myocytes versus paired control preparations was determined after various times of ischaemia, following resuspension of the cells in isotonic or hypotonic media.

RESULTS

Adenosine and CCPA produced only a small reduction of the rates of contracture and death of isolated myocytes. Carbachol gave no significant protection. Neither the degree of injury of control cells nor the amount of protection by CCPA was altered in the presence of added isoprenaline. Protection was abolished by the A1 receptor blocker sulphophenyl theophylline, iodoacetic acid, and exclusion of glucose.

CONCLUSIONS

Adenosine and adenosine agonists afford a minimal degree of protection to ischaemic isolated myocytes by a glucose dependent mechanism. This protection does not appear to account for the larger degree of protection seen in intact hearts, following similar preconditioning protocols. The failure of adenosine to protect may be related to the quiescent state of isolated cardiomyocytes, or be species specific in that adenosine may not be the trigger for preconditioning in rats.

摘要

目的

旨在确定分离的大鼠心肌细胞预先用腺苷或腺苷激动剂孵育是否能免受缺血性细胞死亡。

方法

从大鼠心脏分离的心肌细胞在腺苷、CCPA(2-氯-N6-环戊基腺苷)或卡巴胆碱存在的情况下预先孵育,然后浓缩成缺血悬液。通过向缺血孵育液中添加碘乙酸或异丙肾上腺素以及从所有培养基中排除葡萄糖来确定糖酵解和异丙肾上腺素的作用。在将细胞重悬于等渗或低渗培养基中后,在不同缺血时间后测定缺血挛缩率以及心肌细胞与配对对照制剂的存活率。

结果

腺苷和CCPA仅使分离的心肌细胞的挛缩率和死亡率略有降低。卡巴胆碱未提供显著保护。在添加异丙肾上腺素的情况下,对照细胞的损伤程度和CCPA的保护量均未改变。A1受体阻滞剂磺苯基茶碱、碘乙酸和排除葡萄糖可消除保护作用。

结论

腺苷和腺苷激动剂通过葡萄糖依赖性机制为缺血分离的心肌细胞提供最小程度的保护。这种保护似乎不能解释在完整心脏中遵循类似预处理方案时所观察到的更大程度的保护。腺苷未能提供保护可能与分离的心肌细胞的静止状态有关,或者具有物种特异性,因为腺苷可能不是大鼠预处理的触发因素。

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