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大鼠体感皮层激活过程中内在光学信号、脑血流量与诱发电位的相关性

Correlation of intrinsic optical signal, cerebral blood flow, and evoked potentials during activation of rat somatosensory cortex.

作者信息

Haglund Michael M, Meno Joseph R, Hochman Daryl W, Ngai Al C, Winn H Richard

机构信息

Department of Neurological Surgery, Duke University, Durham, North Carolina, USA.

出版信息

J Neurosurg. 2008 Oct;109(4):654-63. doi: 10.3171/JNS/2008/109/10/0654.

Abstract

OBJECT

This study was undertaken to test the hypothesis that cerebral blood flow (CBF) and the intrinsic optical signal could be dissociated by altering adenosine receptor activity and to uncover the origin of the optic signal using a cranial window in the anesthetized rat.

METHODS

In anesthetized, ventilated, and temperature-controlled rats with closed cranial windows, the authors evaluated simultaneously the alterations in pial arteriolar diameter, intrinsic optical signals (690 nm), and somatosensory evoked potentials during cortical activation evoked by contralateral sciatic nerve stimulation (SNS). To dissociate the vascular and intrinsic signal, they topically applied the adenosine receptors antagonists theophylline (5 microM), which affects A1 and A2A receptors, and 8-cyclopentyl-1,3-dipropylxanthine (CPX, 1 microM), which blocks the A(1) receptor. The former interacts primarily with the vasculature whereas the latter influences the parenchyma exclusively.

RESULTS

During 20 seconds of contralateral SNS, pial arterioles in the hindlimb somatosensory cortex dilated in a characteristic peak and shoulder pattern. As compared with mock cerebrospinal fluid alone, theophylline significantly (p<0.05) attenuated SNS-induced vasodilation (mean+/-standard deviation 8.1+/-2.5% vs 21.7+/-1.9%; 4 rats in each group). In contrast, CPX potentiated vasodilation significantly (p<0.05) during SNS (54.7+/-15.8% for the CPX group vs 20.1+/-1.9% for the controls; 5 rats in each group). The change in optical signal persisted after cessation of SNS in all the animals. Thus, the pattern of change of the optical signal was distinctly different from the pattern of changes in arteriolar diameter (which returned rapidly to baseline). Moreover, the optical signal during SNS was increased by 50% by theophylline and by almost 5-fold by CPX (p<0.05). The area of change of the intrinsic signal was also increased by the topical application of theophylline and CPX. The somatosensory evoked potential recordings revealed no significant changes after theophylline application, but CPX caused a small diminution of the N1 wave (p<0.01).

CONCLUSIONS

The noncongruent temporal profiles of the changes in pial arteriolar diameter and optical signal, imaged at 690 nm, indicate that the optical signal at 690 nm is not related to CBF. Alteration of adenosine receptor activity independently changed cortical activity, as measured by the optical signal, and CBF, as determined by pial arteriolar diameter. Manipulation of the adenosine receptor activity during increased cortical activity confirmed the temporal dissociation of optical signal and CBF and provided further evidence for the role of adenosine in regulating CBF.

摘要

目的

本研究旨在验证以下假设,即通过改变腺苷受体活性可使脑血流量(CBF)与内在光学信号分离,并利用麻醉大鼠的颅骨视窗揭示光学信号的来源。

方法

在麻醉、通气并控制体温的大鼠身上制作闭合颅骨视窗,作者在对侧坐骨神经刺激(SNS)诱发皮层激活期间,同时评估软脑膜小动脉直径、内在光学信号(690nm)和体感诱发电位的变化。为分离血管信号和内在信号,他们局部应用腺苷受体拮抗剂茶碱(5μM),其作用于A1和A2A受体,以及8-环戊基-1,3-二丙基黄嘌呤(CPX,1μM),其阻断A1受体。前者主要与血管系统相互作用,而后者仅影响实质组织。

结果

在对侧SNS的20秒内,后肢体感皮层的软脑膜小动脉以特征性的峰谷模式扩张。与单独使用模拟脑脊液相比,茶碱显著(p<0.05)减弱了SNS诱导的血管舒张(均值±标准差8.1±2.5%对21.7±1.9%;每组4只大鼠)。相反,CPX在SNS期间显著(p<0.05)增强了血管舒张(CPX组为54.7±15.8%,对照组为20.1±1.9%;每组5只大鼠)。所有动物在SNS停止后光学信号的变化持续存在。因此,光学信号的变化模式与小动脉直径的变化模式明显不同(小动脉直径迅速恢复至基线)。此外,SNS期间的光学信号在使用茶碱后增加了50%,在使用CPX后增加了近5倍(p<0.05)。局部应用茶碱和CPX也增加了内在信号的变化面积。体感诱发电位记录显示使用茶碱后无显著变化,但CPX使N1波略有减小(p<0.01)。

结论

在690nm处成像的软脑膜小动脉直径变化和光学信号的时间变化曲线不一致,表明690nm处的光学信号与CBF无关。腺苷受体活性的改变独立地改变了皮层活动(通过光学信号测量)和CBF(通过软脑膜小动脉直径确定)。在皮层活动增加期间对腺苷受体活性的操纵证实了光学信号和CBF的时间分离,并为腺苷在调节CBF中的作用提供了进一步证据。

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