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冠状动脉闭塞和再灌注期间心肌铊-201动力学:再灌注方法及铊-201给药时间的影响

Myocardial thallium-201 kinetics during coronary occlusion and reperfusion: influence of method of reflow and timing of thallium-201 administration.

作者信息

Granato J E, Watson D D, Flanagan T L, Gascho J A, Beller G A

出版信息

Circulation. 1986 Jan;73(1):150-60. doi: 10.1161/01.cir.73.1.150.

Abstract

Thallium-201 (201Tl) uptake and redistribution kinetics were examined in an open-chest canine preparation of occlusion and reperfusion. Seven dogs (group I) underwent 3 hr of sustained occlusion and received 1.5 mCi of 201Tl after 40 min of occlusion of the left anterior descending coronary artery (LAD). Group II (n = 18) underwent 60 min of LAD occlusion followed by sudden and total release of the ligature. Group IIa (n = 8) received intravenous 201Tl during occlusion of the LAD, whereas group IIb (n = 10) received intravenous 201Tl at the time of peak reflow. Group III dogs (n = 26) also underwent 60 min of LAD occlusion that was followed by gradual reflow through a residual critical stenosis. Animals in this group also received 201Tl either before (IIIa; n = 16) or after reflow was established (IIIb; n = 10). In group I, the relative 201Tl gradient (nonischemic minus ischemic activity) decreased from 88 +/- 8% (mean +/- SEM) to 59 +/- 6% during 3 hr of coronary occlusion (p = .034). After rapid and total reperfusion (group IIa), this gradient decreased from 71 +/- 6% during occlusion to 26 +/- 5% after reflow (p less than .001). After slow reperfusion through a residual stenosis (group IIIa), the gradient decreased from 81 +/- 5% to 31 +/- 5% (p less than .001) (p = .56 compared with group IIa). In rapidly reperfused dogs receiving intravenous thallium during peak reflow (IIb), initial 201Tl activity in the ischemic zone was 155 +/- 20% of initial normal activity and fell to 93 +/- 13% of normal after 2 hr of reperfusion. Similarly, in dogs reperfused slowly through a critical stenosis (IIIb), which received 201Tl during reflow, 201Tl activity soon after reflow was 94 +/- 4% of initial normal and decreased to 80 +/- 6% at 2 hr of reperfusion (p = .10). Histochemical evidence of necrosis was present in the biopsy region in 80% of the 20 dogs subjected to triphenyl tetrazolium chloride (TTC) staining. Microsphere-determined transmural blood flow was similar in all groups during LAD occlusion and final flows after 2 hr were comparable in all subgroups undergoing reflow. Ischemic zone flow (% normal) was significantly higher at the time of 201Tl administration in groups IIb (192 +/- 25%) and IIIb (110 +/- 5%), which received 201Tl during reflow, than in groups IIa (31 +/- 9%) and IIIa (22 +/- 5%), which received 201Tl during occlusion.(ABSTRACT TRUNCATED AT 400 WORDS)

摘要

在开胸犬的冠状动脉闭塞和再灌注实验中,研究了铊 - 201(²⁰¹Tl)的摄取和再分布动力学。7只犬(第一组)经历3小时的持续闭塞,在左前降支冠状动脉(LAD)闭塞40分钟后给予1.5毫居里的²⁰¹Tl。第二组(n = 18)经历60分钟的LAD闭塞,然后突然完全松开结扎线。第二组a(n = 8)在LAD闭塞期间静脉注射²⁰¹Tl,而第二组b(n = 10)在再灌注峰值时静脉注射²⁰¹Tl。第三组犬(n = 26)也经历60分钟的LAD闭塞,随后通过残余严重狭窄实现逐渐再灌注。该组动物在再灌注建立之前(第三组a;n = 16)或之后(第三组b;n = 10)接受²⁰¹Tl。在第一组中,相对²⁰¹Tl梯度(非缺血区减去缺血区活性)在冠状动脉闭塞3小时期间从88±8%(平均值±标准误)降至59±6%(p = 0.034)。快速完全再灌注后(第二组a),该梯度从闭塞期间的71±6%降至再灌注后的26±5%(p<0.001)。通过残余狭窄缓慢再灌注后(第三组a),梯度从81±5%降至31±5%(p<0.001)(与第二组a相比p = 0.56)。在再灌注峰值时接受静脉注射铊的快速再灌注犬(第二组b)中,缺血区的初始²⁰¹Tl活性为初始正常活性的155±20%,再灌注2小时后降至正常活性的93±13%。同样,在通过严重狭窄缓慢再灌注的犬(第三组b)中,在再灌注期间接受²⁰¹Tl,再灌注后不久²⁰¹Tl活性为初始正常活性的94±4%,再灌注2小时时降至80±6%(p = 0.10)。在接受氯化三苯基四氮唑(TTC)染色的20只犬中,80%的活检区域存在坏死的组织化学证据。在LAD闭塞期间,所有组的微球测定的透壁血流量相似,在所有进行再灌注的亚组中,2小时后的最终血流量相当。在再灌注期间接受²⁰¹Tl的第二组b(192±25%)和第三组b(110±5%)中,²⁰¹Tl给药时缺血区血流量(正常的百分比)显著高于在闭塞期间接受²⁰¹Tl的第二组a(31±9%)和第三组a(22±5%)。(摘要截于400字)

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