CHARACTERIZATION OF THE IRREVERSIBLE INHIBITION OF HIGH-AFFINITY CHOLINE TRANSPORT PRODUCED BY HEMICHOLINIUM MUSTARD

被引：6

作者：

GYLYS, KH ^{[1
]}

MELLIN, C ^{[1
]}

AMSTUTZ, R ^{[1
]}

JENDEN, DJ ^{[1
]}

机构：

[1] UNIV CALIF LOS ANGELES,SCH MED,BRAIN RES INST,LOS ANGELES,CA 90024

来源：

JOURNAL OF NEUROCHEMISTRY | 1992年 / 59卷 / 04期

关键词：

ALKYLATION; CHOLINERGIC; CHOLINE TRANSPORT; HEMICHOLINIUM-3; SYNAPTOSOMES;

D O I：

10.1111/j.1471-4159.1992.tb08441.x

中图分类号：

Q5 [生物化学]; Q7 [分子生物学];

学科分类号：

071010 ; 081704 ;

摘要：

The inhibition of high-affinity choline transport by hemicholinium mustard (HCM), an alkylating analogue of hemicholinium-3, was examined in rat brain synaptosomes and guinea pig myenteric plexus. In synaptosomes, 50% high-affinity choline transport inhibition occurs with an HCM concentration of 104 nM (4-min incubation). A 10-min preincubation with 10-mu-M HCM results in essentially complete (>95%) inactivation that persists after washing. Low-affinity choline transport in synaptosomes is unaffected by HCM inhibition at all concentrations examined (1-50-mu-M). Time course experiments indicate that the maximum irreversible inhibition (58%) seen after a 1-min preincubation with 500 nM HCM decreases to 46% inhibition after a 15-min preincubation; however, analysis of variance reveals that this difference is not significant. HCM inhibition of acetylcholine release from myenteric plexus-longitudinal muscle preparations persists for at least 2 h after removal of drug from the incubation bath; this inactivation can be prevented by coincubation with a high choline concentration during treatment with the mustard. In contrast, inhibition produced by the parent compound hemicholinium-3 is largely reversed by washing in both preparations examined. The observed potency and selectivity of HCM suggest its usefulness as a covalent probe for high-affinity choline transport.

引用

页码：1302 / 1308

页数：7

共 50 条

[31] REGULATION OF HIGH-AFFINITY CHOLINE UPTAKE
BREER, H
KNIPPER, M
JOURNAL OF NEUROBIOLOGY, 1990, 21 (02): : 269 - 275
[32] MODULATION OF THE HIGH-AFFINITY CHOLINE TRANSPORTER
VOGELSBERG, V
COPELAND, BJ
NEFF, NH
HADJICONSTANTINOU, M
JOURNAL OF NEUROCHEMISTRY, 1994, 62 : S101 - S101
[33] REVERSIBLE AND IRREVERSIBLE INHIBITION, BY STILBENEDISULPHONATES, OF LACTATE TRANSPORT INTO RAT ERYTHROCYTES - IDENTIFICATION OF SOME NEW HIGH-AFFINITY INHIBITORS
POOLE, RC
HALESTRAP, AP
BIOCHEMICAL JOURNAL, 1991, 275 : 307 - 312
[34] Identification and Characterization of a High-Affinity Choline Uptake System of Brucella abortus
Herrmann, Claudia K.
Bukata, Lucas
Melli, Luciano
Marchesini, M. Ines
Caramelo, Julio J.
Comerci, Diego J.
JOURNAL OF BACTERIOLOGY, 2013, 195 (03) : 493 - 501
[35] STEREOSPECIFICITY OF HIGH-AFFINITY AND LOW-AFFINITY TRANSPORT OF CHOLINE ANALOGS INTO RAT CORTICAL SYNAPTOSOMES
FERGUSON, SSG
DIKSIC, M
COLLIER, B
JOURNAL OF NEUROCHEMISTRY, 1991, 57 (03) : 915 - 921
[36] INHIBITION BY HEMICHOLINIUM-3 OF [C-14] ACETYLCHOLINE SYNTHESIS AND [H-3] CHOLINE HIGH-AFFINITY UPTAKE IN RAT STRIATAL SYNAPTOSOMES
GUYENET, P
LEFRESNE, P
ROSSIER, J
BEAUJOUAN, JC
GLOWINSKI, J
MOLECULAR PHARMACOLOGY, 1973, 9 (05) : 630 - 639
[37] DECREASED [H-3] HEMICHOLINIUM BINDING TO HIGH-AFFINITY CHOLINE UPTAKE SITES IN AGED RAT-BRAIN
FORLONI, G
ANGERETTI, N
BRAIN RESEARCH, 1992, 570 (1-2) : 354 - 357
[38] INHIBITION OF HIGH-AFFINITY CHOLINE UPTAKE BY N-ALLYL-3-QUINUCLIDINOL
ASERMELY, KE
ONEILL, JJ
FEDERATION PROCEEDINGS, 1986, 45 (03) : 662 - 662
[39] INHIBITION OF HIGH-AFFINITY CHOLINE UPTAKE IN THE HIPPOCAMPUS - STUDIES ON THE SITE OF PENTOBARBITAL ACTION
RICHTER, JA
GORMLEY, JM
JOURNAL OF PHARMACOLOGY AND EXPERIMENTAL THERAPEUTICS, 1982, 222 (03): : 778 - 785
[40] MONOCLONAL-ANTIBODIES AGAINST THE HIGH-AFFINITY CHOLINE TRANSPORT-SYSTEM
KNIPPER, M
STROTMANN, J
MADLER, U
KAHLE, C
BREER, H
NEUROCHEMISTRY INTERNATIONAL, 1989, 14 (02) : 217 - 222

← 1 2 3 4 5 →