RAT INTERLEUKIN-1-BETA BINDING-SITES IN RAT HYPOTHALAMUS AND PITUITARY-GLAND

被引:37
作者
MARQUETTE, C
VANDAM, AM
BAN, E
LANIECE, P
CRUMEYROLLEARIAS, M
FILLION, G
BERKENBOSCH, F
HAOUR, F
机构
[1] INST PASTEUR,RABIES UNIT,F-75015 PARIS,FRANCE
[2] FREE UNIV AMSTERDAM,FAC MED,NEUROSCI RES INST,DEPT PHARMACOL,AMSTERDAM,NETHERLANDS
[3] UNIV PARIS 11,INST NUCL PHYS,ORSAY,FRANCE
关键词
INTERLEUKINS; INTERLEUKIN RECEPTOR DISTRIBUTION; NEUROIMMUNE INTERACTIONS;
D O I
10.1159/000127026
中图分类号
R5 [内科学];
学科分类号
1002 ; 100201 ;
摘要
In this study, radiolabeled recombinant rat interleukin-1 beta (r(125)I-IL-1 beta) was used to localize and characterize IL-1 beta binding in rat hypothalamus and pituitary gland by quantitative autoradiography. The ability of this ligand to bind to type I IL-1 receptor was first tested on murine lymphoma cells (EL-4). In the rat-tissue sections, high densities of specific r(125)I-IL-1 beta binding sites were localized in the anterior as well as the posterior pituitary and in the choroid plexus. A fine labeling was observed in meninges and third ventricle walls while no binding was detected in the hypothalamic nuclei. Saturation experiments, in the anterior and posterior pituitary, revealed one specific binding site with an affinity constant (K-d) of 0.5 nM. Competition experiments were achieved using either rat IL-1 beta (rIL-1 beta) or human IL-1s (hIL-1 alpha, hIL-1 beta and IL-1 receptor antagonist: hIL-1a). Affinity constants (K-i) were drastically different according to the ligand used, while K-i values were found similar in anterior and posterior pituitary. Competition with rIL-1 beta revealed one binding affinity (K-i of 0.1 nM range). In contrast, competition with hIL-1 beta revealed two binding affinities: a high (K-i: 0.1 pM range) and a low one (K-i: 1 nM range). Competition with hIL-1ra was obtained for high concentrations only (K-i: 10-100 nM range), whereas human IL-1 alpha (hIL-1 alpha) was unable to compete at 1-100 nM. Therefore, two types of IL-1 binding affinities have been identified in rat pituitary tissues: a very high affinity binding, detected with hIL-1 beta only and a lower affinity binding. Human IL-1 beta can therefore be a better ligand for rat receptors than the rat ligand itself while hIL-1 alpha is not. This is suggestive for the existence of several IL-1 receptor subtypes and is in accordance with the biological activity of hIL-1 beta in the rat, Moreover, the high density of binding sites observed in both anterior and posterior pituitary indicates that pituitary tissues are direct targets for IL-1 stimulation. It is worth noting that IL-1 binding sites cannot be detected in the rat hypothalamus, This raises the question of the mechanism of the hypothalamic IL-1-mediated effects and suggests a role of the third ventricular walls in this mediation.
引用
收藏
页码:362 / 369
页数:8
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