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SV-129和C57黑/6小鼠对短暂性前脑缺血易感性的品系相关差异。

Strain-related differences in susceptibility to transient forebrain ischemia in SV-129 and C57black/6 mice.

作者信息

Fujii M, Hara H, Meng W, Vonsattel J P, Huang Z, Moskowitz M A

机构信息

Department of Neurosurgery and Neurology, Massachusetts General Hospital, Harvard Medical School, Boston, USA.

出版信息

Stroke. 1997 Sep;28(9):1805-10; discussion 1811. doi: 10.1161/01.str.28.9.1805.

Abstract

BACKGROUND AND PURPOSE

We explored susceptibility to injury after global ischemia in SV-129 and C57Black/6 mice, two commonly used-background strains in genetically engineered mice.

METHODS

Mice (n = 84) were subjected to 15, 30, or 75 minutes of bilateral common carotid artery (BCCA) occlusion followed by reperfusion for 72 hours. BCCA occlusion was performed under halothane or chloral hydrate anesthesia, in one experiment, mean arterial blood pressure and regional cerebral blood flow (laser Doppler flowmetry) were matched by controlled exsanguination. Baseline absolute blood flow measurements were obtained in both strains using a tracer, N-isopropyl-[methyl 1,3-14C]-p-iodoamphetamine, indicator fractionation technique (n = 5 per group). Vascular anatomy of the circle of Willis was visualized by intravascular perfusion of carbon black ink (n = 10 per group). Cerebrovascular reactivity was assessed by measuring the diameter of pial vessels (intravital microscopy) to acetylcholine (ACh) superfusion (0.1 to 10 mmol/L) in a closed cranial window preparation (n = 29).

RESULTS

Resting blood flow values did not differ between groups in striatum, cerebellum, and brain-stem regions. SV-129 mice were less susceptible than C57Black/6 mice to ischemic injury (0.0 +/- 0.0 versus 1.3 +/- 0.3 damage in hippocampal CA1 region after 30 minutes of ischemia in SV-129 and C57Black/6, respectively; P < .01). Cellular damage (grade 1 to 3 injury) comparable to 30-minute BCCA occlusion was achieved only after 75 minutes of ischemia in SV-129 mice (1.1 +/- 0.3). Ischemic damage was also significantly less in SV-129 mice after blood pressure and flow were matched during ischemia in halothane-anesthetized SV-129 mice (0.5 +/- 0.3 versus 1.4 +/- 0.2, P < .05), or after chloral hydrate anesthesia (0.4 +/- 0.2 versus 1.5 +/- 0.4, P < .05). Hypoplastic posterior communicating arteries were found in all 10 C57Black/6 mice and may explain the greater susceptibility of these mice to injury after BCCA occlusion. More robust vasodilation to ACh in C57Black/6 mice could also indicate genetic differences in responses to vasoactive substances.

CONCLUSIONS

C57Black/6 mice exhibit enhanced susceptibility to global cerebral ischemic injury, an incompletely formed circle of Willis, and augmented pial vessel dilation to ACh compared with SV-129 mice. Our findings suggest that strain differences may confound results when genetically engineered mice generated from more than a single background strain are used.

摘要

背景与目的

我们探究了基因工程小鼠中常用的两种背景品系——SV - 129和C57Black/6小鼠在全脑缺血后对损伤的易感性。

方法

84只小鼠接受15、30或75分钟的双侧颈总动脉(BCCA)闭塞,随后再灌注72小时。BCCA闭塞在氟烷或水合氯醛麻醉下进行,在一项实验中,通过控制性放血使平均动脉血压和局部脑血流(激光多普勒血流仪)相匹配。使用示踪剂N - 异丙基 - [甲基1,3 - 14C] - 对碘安非他明和指示剂分离技术在两种品系中获取基线绝对血流测量值(每组n = 5)。通过向血管内灌注炭黑墨水观察Willis环的血管解剖结构(每组n = 10)。在封闭颅窗制备中,通过测量软脑膜血管对乙酰胆碱(ACh)超灌注(0.1至10 mmol/L)的直径来评估脑血管反应性(n = 29)。

结果

纹状体、小脑和脑干区域各组间静息血流值无差异。SV - 129小鼠比C57Black/6小鼠对缺血损伤更不易感(SV - 129和C57Black/6小鼠分别在缺血30分钟后海马CA1区损伤为0.0±0.0和1.3±0.3;P <.01)。仅在SV - 129小鼠缺血75分钟后才出现与30分钟BCCA闭塞相当的细胞损伤(1.1±0.3)。在氟烷麻醉的SV - 129小鼠缺血期间使血压和血流相匹配后,或在水合氯醛麻醉后,SV - 129小鼠的缺血损伤也显著减轻(分别为0.5±0.3对1.4±0.2,P <.05;0.4±0.2对1.5±0.4,P <.05)。在所有10只C57Black/6小鼠中均发现后交通动脉发育不全,这可能解释了这些小鼠在BCCA闭塞后对损伤更易感的原因。C57Black/ /6小鼠对ACh的血管舒张反应更强也可能表明对血管活性物质反应的基因差异。

结论

与SV - 129小鼠相比,C57Black/6小鼠对全脑缺血损伤的易感性增强,Willis环发育不完全,软脑膜血管对ACh的舒张增强。我们的研究结果表明,当使用来自多个背景品系的基因工程小鼠时,品系差异可能会混淆实验结果。

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