Rhythm generation in organotypic medullary cultures of newborn rats

被引:17
作者
Baker, RE
Ballantyne, D
Bingmann, D
Jones, D
Widman, G
机构
[1] UNIV ESSEN GESAMTHSCH,INST PHYSIOL,D-45122 ESSEN,GERMANY
[2] NETHERLANDS INST BRAIN RES,AMSTERDAM,NETHERLANDS
[3] INST PHYSIOL,BOCHUM,GERMANY
[4] INST EXPTL ORTHOPADIE,MUNSTER,GERMANY
关键词
D O I
10.1016/0736-5748(95)00081-X
中图分类号
Q [生物科学];
学科分类号
07 ; 0710 ; 09 ;
摘要
Organotypic transverse medullary slices (obex level) from six-day-old rats, cultured for two to four weeks in chemically defined medium contained rhythmically discharging neurones which were activated by CO2 and H+. The mechanisms underlying this rhythmicity and the spread of excitation and synaptic transmission within this organotypic tissue were examined by modifying the composition of the external solution. Our findings showed that (1) Exposure to tetrodotoxin (0.2 mu M) or to high magnesium (6 mM) and low calcium (0.2 mM) concentrations abolished periodic activity. (2) Neither the blockade of GABAergic potentials with bicuculline methiodide (200 mu M) and/or hydroxysaclofen (200 mu M) nor the blockade of glycinergic potentials with strychnine hydrochloride (100 mu M) abolished rhythmicity. (3) While atropine sulphate (5 mu M) was ineffective in modulating periodic discharges nicotine (100 mu M) like CO2- shortened the intervals between the periodic events; hexamethonium (50-100 mu M) reduced both periodic and aperiodic activity. (4) Exposure to the NMDA antagonist 2-aminophosphone valeric acid (50 mu M) suppressed period ic events only transiently. In the presence of 2-aminophosphone valeric acid rhythmicity recovered. However, the AMPA-antagonist 6-cyano-7-nitroquinoxaline-2,3-dione (10-50 mu M), abolished periodic activity reversibly within less than 5 min. When 6-cyano-7-nitroquinoxaline-2,3-dione and nicotine were administered simultaneously periodic events persisted for up to 10 min. These findings indicate that synaptic excitatory drive is a prerequisite for the generation of rhythmic discharges of medullary neurones in this preparation. This drive may activate voltage-dependent channels or it may facilitate endogenous cellular mechanisms which initiate oscillations of intracellular calcium concentration. To test the latter possibility (5) calcium antagonists were added to the bath saline. The organic calcium antagonists verapamil and flunarizine (50-100 mu M each) and the inorganic calcium antagonists cobalt (2 mM) and magnesium (6 mM) suppressed periodic activity and abolished or weakened the chemosensitivity towards CO2/acidosis. (6) Dantrolene (10 mu M), an inhibitor of intracellular calcium release decreased the periodicity, while thapsigargin (2 mu M) which blocks endoplasmic Ca2+-ATPase, transiently accelerated the occurrence of periodic events. (7) Oscillations of intracellular free calcium concentrations in Fura-2 AM-loaded cells were weakened or abolished by cobalt (2 mM). The results of (5)-(7) indicate that transmembrane calcium fluxes as well as intracellular Ca2+-release and -clearance mechanisms are a prerequisite for intracellular free calcium oscillations which may be important in the generation of rhythmic discharges in medullary neurones.
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页码:799 / 809
页数:11
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