Evaluation of early gastric mucosal permeability induced by central thyrotropin-releasing hormone administration

doi:10.1152/ajpgi.00100.2004

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Am J Physiol Gastrointest Liver Physiol 288: G230-G234, 2005. First published October 21, 2004; doi:10.1152/ajpgi.00100.2004
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MUCOSAL BIOLOGY

Evaluation of early gastric mucosal permeability induced by central thyrotropin-releasing hormone administration

Takashi Joh,¹ Tadayuki Oshima,¹ Nobuo Takahashi,¹ Hiroshi Kaneko,² Makoto Sasaki,¹ Hiromi Kataoka,¹ Katsushi Watanabe,¹ Masashi Sobue,¹ Hideo Suzuki,¹ Tomoyuki Nomura,¹ Hirotaka Ohara,¹ and Makoto Itoh¹

¹Department of Internal Medicine and Bioregulation, Nagoya City University Graduate School of Medical Sciences, Nagoya; and ²Department of Internal Medicine, Division of General Medicine, Aichi Medical University School of Medicine, Aichi, Japan

Submitted 8 March 2004 ; accepted in final form 8 October 2004

Accumulating evidence suggests that central thyrotropin-releasinghormone (TRH) administration induces gastric erosion 4 h afteradministration through the vagal nerves. However, early changesin the gastric mucosa during these 4 h have not been described.To assess early changes in the gastric mucosa after intracisternalinjection of a stable TRH analog, pGlu-His-(3,3'-dimethyl)-ProNH₂(RX-77368), we measured the blood-to-lumen ⁵¹Cr-labeled EDTAclearance and examined the effects of vagotomy, atropine, omeprazole,and hydrochloric acid (HCl) on RX-77368-induced mucosal permeability.A cytoprotective dose of RX-77368 (1.5 ng) did not increasemucosal permeability. However, higher doses significantly increasedmucosal permeability. Permeability peaked within 20 min andgradually returned to control levels in response to a 15-ngdose (submaximal dose). Increased mucosal permeability was notrecovered after a 150-ng dose (ulcerogenic dose). This increasein permeability was inhibited by vagotomy or atropine. Intragastricperfusion with HCl did not change the RX-77368 (15 ng)-inducedincrease in permeability, but completely inhibited the recoveryof permeability after the peak. Pretreatment with omeprazoledid not change the RX-77368 (15 ng)-induced increase in permeability,but quickened the recovery of permeability after the peak. Thesedata indicate that the RX-77368-induced increase in permeabilityis mediated via the vagal-cholinergic pathway and is not a secondarychange in RX-77368-induced acid secretion. Inhibited recoveryof permeability on exposure to an ulcerogenic RX-77368 doseor on exposure to HCl plus a submaximal dose of RX-77368 maybe crucial for the induction of gastric mucosal lesions by centralRX-77368 administration.

intracisternal injection; ⁵¹Cr-labeled EDTA clearance

Address for reprint requests and other correspondence: T. Joh, Dept. of Internal Medicine and Bioregulation, Nagoya City Univ. Graduate School of Medical Sciences, 1 Kawasumi, Mizuho, Nagoya, 467-8601, Japan (E-mail: tjoh{at}med.nagoya-cu.ac.jp)