Abstract
Centrally administered insulin-like growth factor (IGF)-I has anti-depressant activity in several rodent models, including lipopolysaccharide (LPS)-induced depression. In this study we tested the ability of IGF-I and GPE (the N-terminal tri-peptide derived from IGF-I) to alter depression-like behavior induced by intraperitoneal (i.p.) administration of LPS in a preventive and curative manner. In the first case, IGF-I (1 μg) or GPE (5 μg) was administered i.c.v. to CD-1 mice followed 30 min later by 330 μg/kg body weight i.p. LPS. In the second case, 830 μg/kg body weight LPS was given 24 h prior to either IGF-I or GPE. When administered i.p., LPS induced full-blown sickness assessed as a loss of body weight, decrease in food intake and sickness behavior. None of these indices were affected by IGF-I or GPE. LPS also induced depression-like behavior; assessed as an increased duration of immobility in the tail suspension and forced swim tests. When administered before or after LPS, IGF-I and GPE abrogated the LPS response; attenuating induction of depression-like behaviors and blocking preexistent depression-like behaviors. Similar to previous work with IGF-I, GPE decreased brain expression of cytokines in response to LPS although unlike IGF-I, GPE did not induce the expression of brain-derived neurotrophic factor (BDNF). LPS induced expression of tryptophan dioxygenases, IDO1, IDO2 and TDO2, but expression of these enzymes was not altered by GPE. Thus, both IGF-I and GPE elicit specific improvement in depression-like behavior independent of sickness, an action that could be due to their anti-inflammatory properties.
Highlights
There is accumulating evidence that depression may develop in response to activation of the innate immune system [1,2,3]
Post-hoc analysis revealed that duration of immobility did not differ between controls and mice treated with insulin-like growth factor (IGF)-I, time spent immobile by mice treated with IGF-I + LPS was still above that of controls or IGF-I, p < 0.05; IGF-I did not completely block LPS-induced depression-like behavior
Three new findings are evident from the current studies, 1) they both share an inflammatory component, sickness and depression-like behavior are independently modulated by the IGF system, 2) when added exogenously, two naturally occurring products found in the naïve brain, mature IGF-I and GPE, act centrally to temper LPS-induced changes in depression-like behavior, and 3) GPE can temper the central innate immune response to LPS providing a possible mechanism by which to regulate depression-like behavior
Summary
There is accumulating evidence that depression may develop in response to activation of the innate immune system [1,2,3]. LPS induces transient sickness with the changes in preference for a sweetened solution or immobility in the FST and TST still being evident after the disappearance of sickness; i.e. after locomotor activity, social exploration of a novel juvenile, body weight or food intake have normalized. These depression-like behaviors are reversed by anti-depressants and importantly by minocycline which attenuates LPS-induced expression of brain cytokines [9,11,12,13,14]. These types of studies support the human data that inflammation is causative in the development or maintenance of depressive disorders
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