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Literature DB >> 7529113

Involvement of enzymatic degradation in the inactivation of tachykinin neurotransmitters in neonatal rat spinal cord.

H Suzuki¹, K Yoshioka, M Yanagisawa, O Urayama, T Kurihara, R Hosoki, K Saito, M Otsuka.

Abstract

1. The possible involvement of enzymatic degradation in the inactivation of tachykinin neurotransmitters was examined in the spinal cord of the neonatal rat. 2. The magnitude of substance P (SP)- or neurokinin A (NKA)-evoked depolarization of a lumbar ventral root in the isolated spinal cord preparation was increased by a mixture of peptidase inhibitors, consisting of actinonin (6 microM), arphamenine B (6 microM), bestatin (10 microM), captopril (10 microM) and thiorphan (0.3 microM). The mixture augmented the response to NKA more markedly than that to SP. 3. In the isolated spinal cord-cutaneous nerve preparation, the saphenous nerve-evoked slow depolarization of the L3 ventral root was augmented by the mixture of peptidase inhibitors in the presence of naloxone (0.5 microM) but not in the presence of both naloxone and a tachykinin receptor antagonist, GR71251 (5 microM). 4. Application of capsaicin (0.5 microM) for 6 min to the spinal cord evoked an increase in the release of SP from the spinal cord. The amount of SP released was significantly augmented by the mixture of peptidase inhibitors. 5. Synaptic membrane fractions were prepared from neonatal rat spinal cords. These fractions showed degrading activities for SP and NKA and the activities were inhibited by the mixture of peptidase inhibitors. The degrading activity for NKA was higher than that for SP and the inhibitory effect of the mixture for NKA was more marked than that for SP. Although some other fractions obtained from homogenates of spinal cords showed higher degrading activities for SP, these activities were insensitive to the mixture of peptidase inhibitors. 6. Effects of individual peptidase inhibitors on the enzymatic degradation of SP and NKA by synaptic membrane fractions were examined. Thiorphan, actinonin and captopril inhibited SP degradation, while thiorphan and actinonin, but not captopril, inhibited NKA degradation. The potency of the inhibition of each peptidase inhibitor was lower than that of the mixture.7. The present results suggest that enzymatic degradation is involved in the inactivation of tachykinin neurotransmitters in the spinal cord of the neonatal rat.

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Year: 1994 PMID： 7529113 PMCID： PMC1510033 DOI： 10.1111/j.1476-5381.1994.tb16210.x

Source DB: PubMed Journal: Br J Pharmacol ISSN： 0007-1188 Impact factor: 8.739

36 in total

1. Enzymatic inactivation of tachykinin neurotransmitters in the isolated spinal cord of the newborn rat.

Authors: M Yanagisawa; K Yoshioka; T Kurihara; K Saito; N Seno; H Suzuki; R Hosoki; M Otsuka
Journal: Neurosci Res Date: 1992-12 Impact factor: 3.304

2. A marine algal Na(+)-activated ATPase possesses an immunologically identical epitope to Na+,K(+)-ATPase.

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3. Protein measurement with the Folin phenol reagent.

Authors: O H LOWRY; N J ROSEBROUGH; A L FARR; R J RANDALL
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Review 4. Neurotransmitter functions of mammalian tachykinins.

Authors: M Otsuka; K Yoshioka
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5. Potentiating effect of peptidase inhibitors on a C fiber-evoked response in the isolated spinal cord preparation of the neonatal rat.

Authors: H Suzuki; N Seno; R Hosoki; M Yanagisawa; K Saito; M Otsuka
Journal: Regul Pept Date: 1993-07-02

6. Electrophysiology of mammalian spinal cord in vitro.

Authors: M Otsuka; S Konishi
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7. The separation of synaptic vesicles from nerve-ending particles ('synaptosomes').

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Authors: B P Roques; F Noble; V Daugé; M C Fournié-Zaluski; A Beaumont
Journal: Pharmacol Rev Date: 1993-03 Impact factor: 25.468

9. Depression of primary afferent-evoked responses by GR71251 in the isolated spinal cord of the neonatal rat.

Authors: J Z Guo; K Yoshioka; M Yanagisawa; R Hosoki; R M Hagan; M Otsuka
Journal: Br J Pharmacol Date: 1993-11 Impact factor: 8.739

10. Cultured human synovial fibroblasts rapidly metabolize kinins and neuropeptides.

Authors: J M Bathon; D Proud; S Mizutani; P E Ward
Journal: J Clin Invest Date: 1992-09 Impact factor: 14.808

7 in total

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Journal: Naunyn Schmiedebergs Arch Pharmacol Date: 1996-02 Impact factor: 3.000

2. Tachykininergic synaptic transmission in the coeliac ganglion of the guinea-pig.

Authors: F Y Zhao; K Saito; K Yoshioka; J Z Guo; T Murakoshi; S Konishi; M Otsuka
Journal: Br J Pharmacol Date: 1996-08 Impact factor: 8.739

3. Involvement of tachykinin receptors in oedema formation and plasma extravasation induced by substance P, neurokinin A, and neurokinin B in mouse ear.

Authors: H Inoue; N Nagata; Y Koshihara
Journal: Inflamm Res Date: 1996-07 Impact factor: 4.575

4. Effect of peptidases on the ability of exogenous and endogenous neurokinins to produce neurokinin 1 receptor internalization in the rat spinal cord.

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Journal: Br J Pharmacol Date: 2003-11-17 Impact factor: 8.739