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Featured researches published by Akio Namimatsu.


European Journal of Pharmacology | 1988

Release of inflammatory mediators by noxious stimuli; effect of neurotropin on the release

Hiroyuki Ohara; Akio Namimatsu; Koki Fukuhara; Hisashi Yago; Ryozo Yoneda; Kihachi Saito; Reizo Inoki

Anesthetized rats were perfused with saline in the subcutaneous space of the hind paw and the release of inflammatory mediators induced by noxious stimuli was studied. Not only immunoreactive bradykinin (BK) but also histamine, serotonin (5-HT) and immunoreactive prostaglandin E2 (PGE2) were found to be released into the perfusate when the paw was pinched. Neurotropin, used clinically as an analgesic and anti-allergic drug in Japan, inhibited the release of BK in dose-dependent manner without altering the release of histamine, 5-HT and PGE2. The maximal inhibition of BK release was observed 60 min after p.o. administration of neurotropin. Indomethacin failed to inhibit the release of BK.


Life Sciences | 1992

Changes in muscarinic acetylcholine receptors in the isolated duodenum from repeatedly cold-stressed rats and the effect of neurotropin.

Akio Namimatsu; Koichiro Go; Hiroyuki Ohara; Ryozo Yoneda

In rats repeatedly cold-stressed by specific alternation of rhythm in environmental temperature (SART-stressed rats), the contractile response to acetylcholine (ACh) of the isolated duodenum was remarkably decreased, whereas the contractile responses to K+, Ba2+ and Ca2+ were comparable to those in non-stressed rats. The amount of [3H]quinuclidinyl benzilate in the duodenum of SART-stressed rats was about 50% of that in non-stressed rats, but the KD value remained unchanged. Long-term administration of hexamethonium prevented the changes in SART-stressed rats. The daily treatment with Neurotropin, an extract isolated from inflamed rabbit dermis inoculated with vaccinia virus, dose-dependently prevented the changes in SART-stressed rats. However, Neurotropin had no effect on the ACh-induced decrease in muscarinic ACh receptor (m-ACh.R) in cultured vas deferens of guinea pig. These results suggest that down-regulation of m-ACh.R in duodenum by SART stress may be associated with enhanced activity in the parasympathetic center. Moreover, Neurotropin is thought to prevent the down-regulation of m-ACh.R throughout the central nervous system.


International Archives of Allergy and Immunology | 1992

Mechanism of nasal secretion mediated via nerve reflex in guinea pigs and evaluation of antiallergic drugs

Akio Namimatsu; Koichiro Go; Hideji Tanimoto; Minoru Okuda

In order to confirm the mechanism of nasal secretion mediated via a nerve reflex in guinea pigs, the secretory response from the contralateral side was studied which was induced by local application of various stimulators. There was no difference in the nasal secretion between the contralateral and the stimulated sides when the secretion was induced by allergen, histamine, and capsaicin at lower doses. Methacholine caused a nasal secretion only on the stimulated side. Pretreatment with local anesthetic and ganglionic blockers blocked the secretory response bilaterally which was induced by allergen, histamine, and capsaicin. Antihistaminics also blocked the secretory response induced by allergen and histamine on both sides, but not the capsaicin-induced nasal secretion. Unilateral pretreatment with local anticholinergics prevented all secretory responses only on the stimulated side. Thus, exogenous and endogenous histamine released by the allergen-antibody reaction may stimulate histamine H1 receptors located in the sensory nerve endings as trigger, resulting in the secretory response mediated via a nerve reflex, while methacholine may act directly on nasal glands. Ketotifen and azelastine, which are chemical mediators releasing inhibitor with antihistaminergic activity, prevented the nasal secretion induced by histamine and allergen. On the other hand, disodium cromoglycate, amlexanox, and tranilast had only a slight effect on the allergen-induced nasal secretion. The secretory response on the contralateral side induced by various stimulators would be useful in the in vivo evaluation of anti-allergic drugs to demonstrate the difference in their modes of action.


International Archives of Allergy and Immunology | 1991

Nasal Mucosal Hypersensitivity in Guinea Pigs Intermittingly Exposed to Cold

Akio Namimatsu; Koichiro Go; Taeko Hata

To develop an animal model for experimental nasal hypersensitivity and hyperreactivity, guinea pigs were subjected to intermittent exposure to cold temperature (intermittent cold stress, SART stress) for 5 consecutive days. In SART-stressed guinea pigs, nasal mucosal hypersensitivity to histamine evoking sneeze response and nasal hypersecretion in response to methacholine were observed. The hypersensitivity remained for further 7 days after being released from SART stress. On the other hand, such nasal mucosal hypersensitivity was not caused by a continuous cold stress alone, suggesting that intermittent exposure to cold may be of importance for the appearance of nasal mucosal hypersensitivity. In passively sensitized SART-stressed guinea pigs, the quantity of nasal secretion induced by an allergen was significantly increased compared with that of a group of normal animals. The expression of muscarinic acetylcholine receptor (m-ACh.R) became higher in SART-stressed guinea pigs. Thus, hypersensitivity and hyperreactivity in this system were found to be associated with an increase in density of m-ACh.R. SART-stressed guinea pigs will serve as an animal model for hypersensitivity in nasal mucosa, which would be useful for the study of nasal allergy.


International Archives of Allergy and Immunology | 1991

A New Method of the Measurement of Nasal Secretion in Guinea Pigs

Akio Namimatsu; Satomi Yamaura; Koichiro Go; Hideji Tanimoto; Minoru Okuda

A simple quantitative method to measure nasal secretion in guinea pigs is described. Nasal secretion was measured with a piece of cotton thread dyed with fluorescein at one end which was inserted into an anterior naris and kept there for 60 s. The stretch of color of a thread dyed with fluorescein was proportional to fluid volume and to increase in weight of a thread due to absorbed nasal secretion induced by nasal provocation. In addition, the stretch of color due to nasal secretion was associated with the score of rhinorrhea. Thus, it is considered that the amount of nasal secretion can be reflected to the length of the stretch of color. Each secretion on the ipsilateral and the contralateral sides induced by nasal provocation could be separately measured by this method. The amount of nasal secretion induced by allergen in passively sensitized guinea pigs could be reduced by pretreatment with ketotifen or flutropium. These results suggest that our method may serve as a quantitative test for nasal secretion in guinea pigs, which would be useful in the study of hypersecretory response in the allergic model or in evaluating the effect of antiallergic drugs on nasal allergy.


Japanese Journal of Pharmacology | 1991

Mechanism of Hyperalgesia in SART Stressed (Repeated Cold Stress) Mice: Antinociceptive Effect of Neurotropin

Hiroyuki Ohara; Minoru Kawamura; Akio Namimatsu; Tomoshi Miura; Ryozo Yoneda; Taeko Hata


Folia Pharmacologica Japonica | 1982

SART stress負荷ラットにおける血圧・血流の異常とそれに及ぼすNeurotropinその他の薬物作用

Taeko Hata; Tomitaro Kita; Akio Namimatsu; Eiji Itoh; Yasuo Oda


Folia Pharmacologica Japonica | 1982

Changes of the function of the heart of SART stressed (repeated cold stressed) mice and the action of neurotropin on these changes

Taeko Hata; Tomitaro Kita; Eiji Itoh; Akio Namimatsu


Japanese journal of psychosomatic medicine | 1983

Testing Methods for Vegetative Syndrome in the Rat and Effects of Neurotropin and Other Drugs

Tomitaro Kita; Taeko Hata; Eiji Itoh; Akio Namimatsu


Japanese Journal of Pharmacology | 1992

Regulatory effect of neurotropin on nasal mucosal hypersensitivity in guinea pigs caused by SART (intermittent exposure to cold) stress.

Akio Namimatsu; Koichiro Go; Taeko Hata

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