Acetaminophen affects the duration but not the occurrence of BOLD signal decline in the dorsal hippocampus after induction of neuronal afterdischarges.

Imaging neuroscience (Cambridge, Mass.) Pub Date : 2025-09-22 eCollection Date: 2025-01-01 DOI:10.1162/IMAG.a.161
Alberto Arboit, Karla Krautwald, Frank Angenstein
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Abstract

Combined in vivo electrophysiological and functional magnetic resonance imaging (fMRI) measurements were used to monitor neuronal and hemodynamic responses in the right dorsal hippocampus during and after electrical stimulation of the right perforant pathway with a short period of 20 Hz pulses. These measurements were performed under two conditions: 1.5% isoflurane (which has a long-term vasodilator effect) or 100 µg/kg medetomidine (which has a long-term vasoconstrictor effect). The stimulation elicited a short period of neuronal afterdischarges (nAD) followed by a sustained decline in fMRI BOLD signals, as previously described (Arboit et al., 2024). While the duration of nAD was similar in presence of isoflurane and medetomidine, the subsequent decline of BOLD signal was significantly longer with isoflurane than with medetomidine. However, when the same experiments were performed in the presence of acetaminophen, the duration of the sustained decline of BOLD signals became similar: acetaminophen significantly prolonged the decline in the presence of medetomidine, whereas it only slightly shortened it in the presence of isoflurane. As acetaminophen did not affect the generation and intensity of nAD, the results indicate that nAD activates at least two different neurovascular coupling (NVC) mechanisms that mediate the sustained BOLD signal decline, of which acetaminophen affects the maintenance.

对乙酰氨基酚影响神经元后放电后海马背侧BOLD信号下降的持续时间,但不影响其发生。
使用体内电生理和功能磁共振成像(fMRI)相结合的测量方法来监测右海马背侧在短周期20hz脉冲电刺激右穿孔通路期间和之后的神经元和血流动力学反应。这些测量在两种条件下进行:1.5%异氟醚(具有长期血管舒张作用)或100µg/kg美托咪定(具有长期血管收缩作用)。刺激引发了短时间的神经元放电后(nAD),随后fMRI BOLD信号持续下降,如前所述(Arboit et al., 2024)。虽然异氟醚和美托咪定存在时nAD的持续时间相似,但异氟醚的BOLD信号随后的下降时间明显长于美托咪定。然而,当在对乙酰氨基酚存在的情况下进行相同的实验时,BOLD信号持续下降的持续时间变得相似:对乙酰氨基酚显著延长了美托咪定存在时的下降时间,而在异氟醚存在时仅略微缩短了下降时间。由于对乙酰氨基酚不影响nAD的产生和强度,结果表明nAD激活至少两种不同的神经血管偶联(NVC)机制,介导持续的BOLD信号下降,其中对乙酰氨基酚影响维持。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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