HEMICHOLINIUM-3 (HC3) BLOCKS THE EFFECTS OF ETHYLCHOLINE MUSTARD AZIRIDINIUM (AF64A) IN THE DEVELOPING RAT

被引：7

作者：

BRAKE, WG ^{[1
]}

PAPPAS, BA ^{[1
]}

机构：

[1] CARLETON UNIV,LIFE SCI RES CTR,OTTAWA,ON K1S 5B6,CANADA

来源：

DEVELOPMENTAL BRAIN RESEARCH | 1994年 / 83卷 / 02期

基金：

加拿大自然科学与工程研究理事会;

关键词：

ACETYLCHOLINE; BRAIN DEVELOPMENT; AF64A; HEMICHOLINIUM-3; CHOLINOTOXIN; SPATIAL LEARNING MEMORY;

D O I：

10.1016/0165-3806(94)00165-0

中图分类号：

Q [生物科学];

学科分类号：

07 ; 0710 ; 09 ;

摘要：

Two- to 3-day-old rat pups received bilateral intracerebroventricular (i.c.v.) injections of 2.0 nmol/mu l AF64A or vehicle. Half of the pups had been preinjected i.c.v. with hemicholinium-3 (HC3) and the other half with saline. The administration of AF64A impaired spatial learning/memory and caused brain damage characterized by marked loss of forebrain cortical/subcortical tissue and ventricular hypertrophy when these were assessed in adulthood. Neither the behavioral nor the histopathoiogical effects of AF64A were observed in rats that had been pretreated with HC3. Since HC3 is a potent and relatively selective inhibitor of high affinity choline uptake (HACU), the results indicate that the toxic effects of AF64A in the neonatal rat are dependent upon its uptake via the HACU site. If as other research suggests, this site is primarily on Ach neurons in the neonatal rat, then the consequences of neonatal damage to cholinergic neurons are severe for forebrain development.

引用

页码：289 / 293

页数：5

共 28 条

[1] THE HISTOPATHOLOGICAL, BEHAVIORAL AND NEUROCHEMICAL EFFECTS OF INTRAVENTRICULAR-INJECTION OF ETHYLCHOLINE MUSTARD AZIRIDINIUM (AF64A) IN THE NEONATAL RAT [J].

ARMSTRONG, JN ;

PAPPAS, BA .

DEVELOPMENTAL BRAIN RESEARCH, 1991, 61 (02) :249-257

[2]

ASANTE JW, 1983, BRIT J PHARMACOL, V80, pP573

[3] HEMICHOLINIUM-3 PREVENTS THE WORKING MEMORY IMPAIRMENTS AND THE CHOLINERGIC HYPOFUNCTION INDUCED BY ETHYLCHOLINE AZIRIDINIUM ION (AF64A) [J].

CHROBAK, JJ ;

SPATES, MJ ;

STACKMAN, RW ;

WALSH, TJ .

BRAIN RESEARCH, 1989, 504 (02) :269-275

[4] THE NEUROBIOLOGICAL CONSEQUENCES OF DOWN-SYNDROME [J].

COYLE, JT ;

OSTERGRANITE, ML ;

GEARHART, JD .

BRAIN RESEARCH BULLETIN, 1986, 16 (06) :773-787

[5] CHOLINE ANALOGS AS POTENTIAL TOOLS IN DEVELOPING SELECTIVE ANIMAL-MODELS OF CENTRAL CHOLINERGIC HYPOFUNCTION [J].

FISHER, A ;

HANIN, I .

LIFE SCIENCES, 1980, 27 (18) :1615-1634

[6]

FISHER A, 1982, J PHARMACOL EXP THER, V222, P140

[7] RAPID RADIOCHEMICAL METHOD FOR DETERMINATION OF CHOLINE-ACETYLTRANSFERASE [J].

FONNUM, F .

JOURNAL OF NEUROCHEMISTRY, 1975, 24 (02) :407-409

[8] BEHAVIORAL AND BIOCHEMICAL EFFECTS OF EARLY POSTNATAL CHOLINERGIC LESION IN THE HIPPOCAMPUS [J].

GASPAR, E ;

HEERINGA, M ;

MARKEL, E ;

LUITEN, PGM ;

NYAKAS, C .

BRAIN RESEARCH BULLETIN, 1992, 28 (01) :65-71

[9] DEVELOPMENT OF HIGH-AFFINITY CHOLINE TRANSPORT SITES IN RAT FOREBRAIN - A QUANTITATIVE AUTORADIOGRAPHY STUDY WITH [H-3] HEMICHOLINIUM-3 [J].

HAPPE, HK ;

MURRIN, LC .

JOURNAL OF COMPARATIVE NEUROLOGY, 1992, 321 (04) :591-611

[10] NEONATAL LESIONS OF THE BASAL FOREBRAIN CHOLINERGIC NEURONS RESULT IN ABNORMAL CORTICAL DEVELOPMENT [J].

HOHMANN, CF ;

BROOKS, AR ;

COYLE, JT .

DEVELOPMENTAL BRAIN RESEARCH, 1988, 42 (02) :253-264

← 1 2 3 →