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颈动脉内注射腺苷用于调控人体脑血管阻力的可行性。

The feasibility of intracarotid adenosine for the manipulation of human cerebrovascular resistance.

作者信息

Joshi S, Young W L, Pile-Spellman J, Duong D H, Vang M C, Hacein-Bey L, Lee H T, Ostapkovich N

机构信息

Department of Anesthesiology, College of Physicians and Surgeons, Columbia University, New York, New York 10032, USA.

出版信息

Anesth Analg. 1998 Dec;87(6):1291-8. doi: 10.1097/00000539-199812000-00015.

Abstract

UNLABELLED

To assess the feasibility of manipulating human cerebrovascular resistance with adenosine, we measured cerebral blood flow (CBF) by determining the initial slope (IS) of tracer washout 20-80 s after intracarotid 133Xe injection (standard IS) during sequential 3-min intracarotid infusions of (a) saline; (b) adenosine 1.2-mg bolus followed by an infusion of 1 mg/min (bolus + infusion); (c) saline; and (d) nicardipine (0.1 mg/min). During 133Xe washout, adenosine caused a rapidly clearing compartment. Therefore, tracer washout was also analyzed 5-25 s after injection (early IS). Nicardipine (n = 8) increased both standard IS (from 39+/-12 to 53+/-16 mL 100g.min(-1); P < 0.005) and early IS (from 40+/-9 to 55+/-20 arbitrary units; P < 0.02) to a similar degree. Adenosine bolus + infusion increased early IS (from 33+/-6 to 82+/-43 arbitrary units; P < 0.02) but did not increase standard IS (from 41+/-12 to 43 +/-16 mL 100g(-1) min(-1)). Standard and early IS values were then determined before and after adenosine delivered either by infusion alone (2 mg/min for 3 min, n = 5) or bolus alone (2 mg in 1 s, n = 3). Neither standard nor early IS changed after adenosine infusion alone. Early IS increased after adenosine bolus alone. Increase in early IS, but not standard IS, suggests a transient (<30 s) increase in CBF.

IMPLICATIONS

Intracarotid adenosine, in the 1- to 2-mg dose range, may cause a transient, but not a sustained, increase in cerebral blood flow. Intracarotid adenosine in such a dose range does not seem to be an appropriate drug for sustained manipulation of cerebrovascular resistance.

摘要

未标记

为评估用腺苷调控人体脑血管阻力的可行性,我们在依次进行3分钟颈内动脉输注期间,通过测定颈内注射133Xe后20 - 80秒示踪剂清除的初始斜率(IS)(标准IS)来测量脑血流量(CBF),输注顺序为:(a) 生理盐水;(b) 1.2毫克腺苷推注,随后以1毫克/分钟的速度输注(推注 + 输注);(c) 生理盐水;以及(d) 尼卡地平(0.1毫克/分钟)。在133Xe清除期间,腺苷导致一个快速清除的房室。因此,还在注射后5 - 25秒分析示踪剂清除情况(早期IS)。尼卡地平(n = 8)使标准IS(从39±12增加到53±16毫升·100克-1·分钟-1;P < 0.005)和早期IS(从40±9增加到55±20任意单位;P < 0.02)增加到相似程度。腺苷推注 + 输注使早期IS增加(从33±6增加到82±43任意单位;P < 0.02),但未增加标准IS(从41±12增加到43±16毫升·100克-1·分钟-1)。然后在单独输注腺苷(2毫克/分钟,持续3分钟,n = 5)或单独推注腺苷(2毫克,1秒内推注,n = 3)之前和之后测定标准IS和早期IS值。单独输注腺苷后,标准IS和早期IS均未改变。单独推注腺苷后早期IS增加。早期IS增加但标准IS未增加,提示脑血流量有短暂(<30秒)增加。

启示

颈内注射1至2毫克剂量范围的腺苷可能导致脑血流量短暂增加,但非持续增加。在此剂量范围内的颈内注射腺苷似乎不是持续调控脑血管阻力的合适药物。

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