AI Article Synopsis

  • Migraine symptoms can include sensitivity to sound, and researchers studied how a substance called nitroglycerin affects auditory pathways in rats.
  • The study involved measuring brainstem auditory evoked potentials (BAEPs) before and after nitroglycerin injection, using electrodes to collect data from different frequency stimuli.
  • Findings indicated significant delays in certain auditory processing peaks in rats after nitroglycerin injection, suggesting potential changes in brain function related to migraines, which aligns with similar results found in human studies.

Article Abstract

Migraine symptoms often include auditory discomfort. Nitroglycerin (NTG)-triggered central sensitization (CS) provides a rodent model of migraine, but auditory brainstem pathways have not yet been studied in this example. Our objective was to examine brainstem auditory evoked potentials (BAEPs) in rat CS as a measure of possible auditory abnormalities. We used four subdermal electrodes to record horizontal (h) and vertical (v) dipole channel BAEPs before and after injection of NTG or saline. We measured the peak latencies (PLs), interpeak latencies (IPLs), and amplitudes for detectable waveforms evoked by 8, 16, or 32 kHz auditory stimulation. At 8 kHz stimulation, vertical channel positive PLs of waves 4, 5, and 6 (vP4, vP5, and vP6), and related IPLs from earlier negative or positive peaks (vN1-vP4, vN1-vP5, vN1-vP6; vP3-vP4, vP3-vP6) increased significantly 2h after NTG injection compared to the saline group. However, BAEP peak amplitudes at all frequencies, PLs and IPLs from the horizontal channel at all frequencies, and the vertical channel stimulated at 16 and 32 kHz showed no significant/consistent change. For the first time in the rat CS model, we show that BAEP PLs and IPLs ranging from putative bilateral medial superior olivary nuclei (P4) to the more rostral structures such as the medial geniculate body (P6) were prolonged 2h after NTG administration. These BAEP alterations could reflect changes in neurotransmitters and/or hypoperfusion in the midbrain. The similarity of our results with previous human studies further validates the rodent CS model for future migraine research.

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http://www.ncbi.nlm.nih.gov/pmc/articles/PMC4020271PMC
http://dx.doi.org/10.1016/j.brainres.2014.03.033DOI Listing

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