ABSTRACT
Genetically selected short attack latency (SAL) and long attack latency (LAL) male wild house mice behave differently in the defensive burying test. When challenged, SAL males respond actively with more time spent on defensive burying, whereas LAL males are more passive with more time remaining immobile. The first aim of this study was to find out whether the nonpairing part of the Y chromosome (Y(NPAR)) affects the behavioral stress response in this paradigm. Second, to determine if the differential behavioral profile found in males is also present in females, SAL and LAL females were tested. Third, nonattacking and attacking LAL males were compared. Five behavioral elements were recorded: defensive burying, immobility, rearing, grooming, and exploration. Males were first tested for attack latency. The results show that the Y(NPAR) influences defensive burying. However, the size of this effect is overshadowed by the background of the mice. Furthermore, although females differed from males, they tended to demonstrate the same behavioral profile as males. Nongenetic factors may also play a role, as attacking LAL males showed more defensive burying than nonattacking LAL males.
Subject(s)
Aggression/physiology , Behavior, Animal/physiology , Stress, Psychological/psychology , Y Chromosome/physiology , Animals , Exploratory Behavior/physiology , Female , Genotype , Grooming/drug effects , Grooming/physiology , Male , Mice , Sex CharacteristicsABSTRACT
This study takes the first step toward testing a Y chromosomal effect on both aggression and thermoregulatory nest-building behavior in mouse lines either bidirectionally selected for short (SAL) and long (LAL) attack latency or high (HIGH) and low (LOW) nest-building behavior. Using reciprocal crosses between SAL and LAL, and between HIGH and LOW, we found no indications for Y chromosomal effects on thermoregulatory nest-building behavior. As for aggression, we confirmed earlier studies on SAL and LAL, i.e., the origin of the Y chromosome influences attack latency, i.e., aggression. However, we did not find indications for a Y chromosomal effect on aggression in the HIGH and LOW lines. Since aggression and nest-building behavior have been shown to be characteristic parameters of two fundamentally different behavioral strategies, the present data underline the improbability of Y chromosomal genes underlying the genetic architecture of alternative behavioral strategies.
Subject(s)
Aggression/physiology , Body Temperature Regulation/genetics , Nesting Behavior/physiology , Y Chromosome , Animals , Arousal/genetics , Biological Evolution , Crosses, Genetic , Female , Male , Mice , Reaction Time/genetics , Selection, GeneticABSTRACT
This paper reviews our present state of knowledge of genetic variation in (offensive) aggression in wild house mice. The basic tools in this research were lines bidirectionally selected for attack latency (fast attacking SAL and slow attacking LAL males), descended from a feral population. Using congenic lines for the nonpseudoautosomal region of the Y chromosome (YNPAR), reciprocal crosses between (parental) SAL and LAL, and crosses between parentals and congenics, an autosomally dependent Y chromosomal effect on aggression has been found. Both the pseudoautosomal (YPAK) region and the YNPAR play a role. As for environmental sources of variation, prenatal and postnatal maternal effects are of minor importance for the development of aggression differences. One of the physiological factors by which genetic effects may be mediated is testosterone (T). Besides quantitative aspects, the timing of T release seems crucial. Two important time frames are discussed: the perinatal and pubertal time periods. Finally, neurochemical and neuroanatomical correlates are considered. Differences in neostriatal dopaminergic activity, and sizes of the intra- and infrapyramidal mossy fiber terminal fields, as well as Y chromosomal effects on the latter two, are discussed.
Subject(s)
Aggression/physiology , Genetic Variation/genetics , Genotype , Animals , Animals, Wild/genetics , Brain Mapping , Female , Male , Mice , Models, Genetic , Sexual Maturation/genetics , Social Environment , Testosterone/physiology , Y ChromosomeABSTRACT
The effect of the maternal environment on intermale aggression was studied by means of embryo transfer of genetically selected aggressive (SAL) and nonaggressive wild house mice (LAL), and their reciprocal F1's, to standard (NMR1) females. No effect was found on the attack latency scores (ALS), i.e., aggression: all genotypes born and raised under natural conditions showed an ALS similar that of genotypes born and raised by NMR1 females. Since previous studies on wild house mice failed to demonstrate postnatal effects on aggression, and the present results indicate the absence of prenatal maternal environmental effects on aggression, the primacy of genetic over maternal variance in the development of adult intermale aggression in wild house mice is indicated.
Subject(s)
Aggression/physiology , Genotype , Prenatal Exposure Delayed Effects , Selection, Genetic , Social Environment , Animals , Animals, Wild , Embryo Transfer , Female , Male , Mice , Mice, Inbred Strains , Models, Genetic , Pregnancy , Y ChromosomeABSTRACT
Genetically selected aggressive and nonaggressive male wild house mice were tested in the shock-probe/defensive burying test: Five distinct behaviors (burying, immobility, rearing, grooming, and exploration) were recorded in two environmental situations: fresh and home cage sawdust. Nonaggressive animals, characterized by a Long Attack Latency (LAL), showed more immobility in both test situations than animals having Short Attack Latencies (SAL), whereas SAL males displayed more defensive burying than LAL ones when tested with fresh sawdust. Testing with home cage sawdust, however, resulted in the same duration of defensive burying in SAL and LAL. These results support earlier findings about the existence of two heritable, fundamentally different strategies to cope with aversive situations. Aggressive (SAL) animal react actively to environmental challenges, whereas nonaggressive animals react actively or passively, depending on the characteristics of the stressful environment. These mouse lines, selected for attack latency, i.e., aggression, may, therefore, be important tools to unravel the genetic architecture underlying the physiological and neuronal mechanisms of behavioral strategies towards stressful events.
Subject(s)
Aggression/physiology , Behavior, Animal/physiology , Stress, Psychological/genetics , Stress, Psychological/psychology , Animals , Electroshock , Environment , Exploratory Behavior/physiology , Grooming/physiology , Male , Mice , Motor Activity/physiologyABSTRACT
The behavioral response to apomorphine, a dopamine agonist, was shown to be different between a selection line characterized by Short Attack Latencies (SAL) and a selection line having Long Attack Latencies (LAL) (4). Aggressive SAL mice were more sensitive to apomorphine than nonaggressive LAL males. The aim of this research was to determine whether the stereotyped response to apomorphine is affected by the Y chromosome in the same way as it influences attack latency. For this purpose, F1 reciprocal hybrids as well as congenic lines (SAL.LY and LAL.SY) were used. The major difference between the congenic and parental lines is the nonpairing part of the Y chromosome (non-PAR). Apomorphine was injected subcutaneously at a preselected dose level of 5.0 mg/kg to induce stereotyped behavior manifested in compulsive sniffing, gnawing, and licking. Both the autosomes and the non-PAR Y chromosome affected the response to apomorphine. The effect of the autosomes was in accordance with the aggression data, whereas the effect of the non-PAR Y chromosome was different, and suggests a specific relation between dopamine systems and the non-PAR Y chromosome.
Subject(s)
Apomorphine/pharmacology , Chromosomes/physiology , Dopamine Agonists/pharmacology , Stereotyped Behavior/drug effects , Y Chromosome/physiology , Aggression/drug effects , Animals , Dose-Response Relationship, Drug , Male , Mice , Mice, Inbred Strains , Movement/drug effects , Phenotype , Posture/physiology , Stereotyped Behavior/physiologyABSTRACT
Previous findings have shown a difference in attack latencies, i.e., aggression, between reciprocal F1's of a line selected for short attack latency (SAL) and a line selected for long attack latency (LAL). In the present study, we investigated the influence of postnatal maternal environment on attack latency scores (ALSs). The results show that only the evolution of the ALSs over 3 consecutive days is influenced by crossfostering. Accordingly, we conclude that the postnatal maternal environment affects ALSs only to a small extent.
Subject(s)
Aggression/physiology , Maternal Behavior/physiology , Selection, Genetic , Social Environment , Y Chromosome , Agonistic Behavior/physiology , Animals , Male , Mice , Mice, Inbred Strains , Phenotype , Reaction Time/geneticsABSTRACT
The influence of the non-pseudoautosomal region of the Y chromosome (YNPAR) on the sizes of the hippocampal intra- and infrapyramidal mossy fiber (IIPMF) terminal fields were examined in wild house mice. For this purpose selection lines for short attack latency (SAL), long attack latency (LAL), and their respective congenics for the YNPAR were used. We found an incremental effect of the (non-aggressive) LAL YNPAR, combined with an additive effect of the line background on the sizes of the IIPMF terminal fields. In contrast, only the line background affected attack latency. The implications of this finding for the previously observed correlation between the size of the IIPMF and aggression in male house mice are discussed.
Subject(s)
Aggression/physiology , Hippocampus/physiology , Nerve Fibers/physiology , Y Chromosome/physiology , Animals , Cell Size , DNA, Mitochondrial/metabolism , Genetics, Behavioral , Hippocampus/cytology , Hippocampus/ultrastructure , Male , Mice , Nerve Fibers/ultrastructure , Y Chromosome/ultrastructureABSTRACT
House mouse lines bidirectionally selected for either nest-building behavior or attack latency were tested for both attack latency and nest-building behavior under identical conditions. Male mice selected for high nest-building behavior had shorter attack latencies, i.e., were more aggressive, than those selected for low nest-building behavior and their randomly bred control lines. Conversely, male wild house mice selected for short attack latency showed more nest-building behavior than those selected for long attack latency when tested at 110 days of age. These findings imply a common genetic basis for control of aggression and nesting and support earlier proposals as to how animals may exhibit fundamentally different responses to environmental challenges, either reacting actively to aversive situations (aggressive and high-nesting animals: active copers) or adopting a passive strategy (nonaggressive and low-nesting animals: passive copers).
Subject(s)
Agonistic Behavior , Mice/genetics , Nesting Behavior , Reaction Time/genetics , Selection, Genetic , Aggression , Animals , Male , Social Environment , Species SpecificityABSTRACT
The sizes of the hippocampal intra- and infrapyramidal mossy fiber terminal fields (IIPMF) of mice from two lines bidirectionally selected for attack latency were measured. Aggressive males possess smaller IIPMF than do non-aggressive ones. We hypothesize that both differences in aggression and sizes of the IIPMF may be mediated by perinatal testosterone.
Subject(s)
Aggression/physiology , Hippocampus/ultrastructure , Animals , Animals, Wild , Male , Mice , Nerve Endings/ultrastructure , Nerve Fibers/ultrastructure , Reaction TimeABSTRACT
Congenic lines were made for the Y chromosome between aggressive and nonaggressive lines of house mice, which were previously established by artificial selection in wild mice for short attack latencies (SAL line) and long attack latencies (LAL line). The aggressiveness of the males in successive backcross generations of the congenic lines is reported. Results fit the hypothesis that the Y-chromosomal effect that is often found for aggression in house mice may be located on the pseudo-autosomal region of this chromosome.
Subject(s)
Aggression , Animals, Wild/genetics , Arousal/genetics , Mice/genetics , Reaction Time/genetics , Selection, Genetic , Y Chromosome , Aggression/psychology , Agonistic Behavior , Animals , Female , Genotype , MaleABSTRACT
Male mice, genetically selected for aggression, characterized by short attack latency (SAL) or long attack latency (LAL), differ on several testosterone (T)-related parameters during ontogeny and adult age. The variation in aggressive behavior at adult age may be due to differences in degree of androgenization prenatally. When exposed to T at prenatal, neonatal, and/or adult age, nonlactating females also display intraspecific fighting behavior. In the present study, we investigated in females of the SAL and LAL selection lines, whether the differentiation of aggression involves processes similar to ones seen in males. Therefore, we injected females with testosterone propionate (TP) or vehicle on the day of birth, treated them after ovariectomy at adult age with T, estradiol (E), or vehicle, and tested their aggressive response. We found that neonatally vehicle-treated SAL females show a higher aggressive response to chronic T treatment at adult age than LAL females receiving the same treatment. Females of both selection lines treated with vehicle or E as adults were not aggressive. Neonatal TP treatment did not influence the adult T sensitivity and difference between selection lines in response to T at adult age. However, neonatally TP-treated SAL females showed aggressive behavior when treated with E at adult age, whereas LAL females failed to do so. These results suggest a genetic difference in susceptibility to T and E, which plays a major role prenatally, in organizing the development of sex steroid-dependent neural systems.
Subject(s)
Aggression/drug effects , Selection, Genetic , Testosterone/pharmacology , Agonistic Behavior/drug effects , Animals , Estradiol/pharmacology , Female , Male , Mice , Reaction Time/drug effects , Reaction Time/genetics , Sex Differentiation/drug effects , Sex Differentiation/genetics , Social Environment , Species SpecificityABSTRACT
Testosterone secretory capacity of testicular Leydig cells was determined in fetal males of an aggressive and a nonaggressive genetic selection line of wild house mice. They were studied at Days 15-18 of gestation and on the first day after birth. A previously described morphometric method was used to quantify 3 beta-hydroxy steroid dehydrogenase (3 beta-HSD)-stained Leydig cells in testicular sections to determine testosterone secretory capacity, which may be considered to reflect circulating plasma testosterone in the fetus. The results of this study show that the testosterone secretory capacity of Leydig cells in the testis changes differentially during intrauterine development in males of the aggressive and nonaggressive selection lines. The peak secretory capacity is reached at Day 17 of gestation for the males of the aggressive selection line, while the peak for the nonaggressive males is reached on the first neonatal day. The larger anogenital distance observed in aggressive males suggests a higher prenatal testosterone level in these males. The importance of the difference in timing of the perinatal 3 beta-HSD peak top individual variation in adult aggressive behavior is discussed.
Subject(s)
Aggression/physiology , Cell Differentiation/physiology , Leydig Cells/cytology , Sexual Behavior, Animal/physiology , Sexual Maturation/physiology , Testosterone/metabolism , 3-Hydroxysteroid Dehydrogenases/physiology , Animals , Cell Count , Female , Gestational Age , Male , Mice , Pregnancy , Reaction Time/physiology , Sex Differentiation/physiology , Species SpecificityABSTRACT
Selection lines of mice, artificially selected for aggression based upon the attack latency score (ALS), were used. In order to determine the relative contribution of neonatal testosterone (T) in the development of aggression, we vary the plasma-T level in males of both selection lines on the day of birth. At 14 weeks the ALS was measured. Neonatal T treatment results in a reduction of aggression in the long attack latency (LAL) line, whereas aggressive behaviour of the short attack latency (SAL) line is not affected. Both selection lines show reduction in testicular weight, although the total amount of T-producing Leydig cells was not affected. Neonatal T may cause a permanent reduction in aggressive behaviour in in the LAL line only, probably due to differential appearance of critical periods. It is suggested that the difference in aggressive behaviour between SAL and LAL selection lines is due to a prenatally determined difference in neonatal T sensitivity of the brain.
Subject(s)
Aggression/physiology , Prenatal Exposure Delayed Effects , Selection, Genetic , Sex Differentiation/genetics , Sex Differentiation/physiology , Testosterone/physiology , Animals , Brain/physiology , Female , Male , Mice , Pregnancy , Receptors, Androgen/genetics , Receptors, Androgen/physiology , Sexual Maturation/genetics , Sexual Maturation/physiologyABSTRACT
Evidence is presented in rodents, that individual differences in aggression reflect heritable, fundamentally different, but equally valuable alternative strategies to cope with environmental demands. Generally, aggressive individuals show an active response to aversive situations. In a social setting, they react with flight or escape when defeated; in non-social situations, they react with active avoidance of controllable shocks and with sustained activity during an uncontrollable task. In contrast, non-aggressive individuals generally adopt a passive strategy. In social and non-social aversive situations, they react with immobility and withdrawal. A main aspect of these two alternative strategies is that individuals with an active strategy easily develop routines (intrinsically determined behaviour), and consequently do not react (properly) to 'minor' changes in their environment, whereas in passively reacting animals it is just the other way around (extrinsically determined behaviour). It has become clear that active and passive behavioural strategies represent two different, but equivalent, coping styles. The coping style of the aggressive males is aimed at the removal of themselves from the source of stress or at removal of the stress source itself (i.e. active manipulation). Non-aggressive individuals seem to aim at the reduction of the emotional impact of the stress (i.e. passive confrontation). The success of both coping styles depends upon the variability or stability of the environment. The fact that aggressive males develop routines may contribute to a fast execution of their anticipatory responses, which is necessary for an effective manipulation of events. However, this is only of advantage in predictable (stable) situations, but is maladaptive (e.g. expressed by the development of stress pathologies) when the animal is confronted with the unexpected (variable situations). The flexible behaviour of non-aggressive individuals, depending strongly upon external stimuli, will be of advantage under changing conditions. Studies on wild house mice living under natural conditions show how active and passive coping functions in nature, and how the two types have been brought about by natural selection.
Subject(s)
Adaptation, Psychological/physiology , Aggression/physiology , Genetic Variation , Animals , Humans , Male , Mice , Rats , Y ChromosomeABSTRACT
The present study reports a first attempt to unravel the neurochemical background that underlies the difference in behavioural profiles between aggressive and non-aggressive male mice. For this purpose two bidirectionally selected lines for attack latency (SAL and LAL) were used. In pursuit of Cools'9 approach, the susceptibility of individuals of both selection lines to the dopamine agonist apomorphine was measured. The apomorphine was injected subcutaneously at dose levels of 2.5 and 5.0 mg/kg. Apomorphine is considered to stimulate the dopamine receptors in the telencephalon and induces stereotyped behaviour. The responsivity to apomorphine can be rated as a total stereotypy-score. SAL (aggressive) mice showed a significantly greater enhancement of stereotyped behaviour in response to apomorphine than LAL (non-aggressive) mice. In addition, it was demonstrated that this difference is of a quantitative rather than qualitative character. Pharmacokinetic variation between the two lines could be ruled out as cause of the difference. Hence, it was concluded that SAL mice are more sensitive to apomorphine than LAL males, which provides evidence for a difference in the dopaminergic system between the two selection lines. It was suggested that this difference underlies the difference in flexibility in behaviour between aggressive and non-aggressive male mice.
Subject(s)
Aggression/drug effects , Agonistic Behavior/drug effects , Apomorphine/pharmacology , Behavior, Animal/drug effects , Selection, Genetic , Animals , Brain/drug effects , Male , Mice , Reaction Time/drug effects , Reaction Time/genetics , Receptors, Dopamine/genetics , Species Specificity , Stereotyped Behavior/drug effectsABSTRACT
The effect of exposure to inescapable long-duration shocks of moderate intensity on intershock activity and on subsequent escape or avoidance performance was studied in aggressive and non-aggressive male mice. The activity of the non-aggressive mice was severely suppressed during the inescapable shock session, while that of the aggressive males was hardly influenced. The decremental effect of prior shock exposure on subsequent response latency and activity in an active two-way escape or avoidance task was greater in the non-aggressive than in the aggressive mice. There was no evidence that learned inactivity or learned helplessness (an associative deficit) could explain the results. Instead, individual differences in behavioural strategy in response to threatening situations appeared to account for the effects of inescapable shock. Aggressive male mice predominantly adopted an active behavioural strategy in challenging situations, which resulted in persistent attempts to exercise control over the external situation and hence in a sustained tendency to initiate responses. Non-aggressive mice primarily assumed a passive strategy; their tendency to exercise control was low, which readily resulted in a reduced tendency to initiate responses.
ABSTRACT
The hypothesis, partly based on findings in social interactions, that aggressive mice generally adopt an active behavioural strategy (cf. fight-flight) in threatening situations, while non-aggressive ones generally assume a passive strategy (cf. conservation-withdrawal) was tested using a two-way active shock avoidance paradigm. Overall, aggressive mice were found to be better active shock avoiders than non-aggressive animals; a finding that is consistent with our hypothesis. However, within the non-aggressive mice a clear dichotomy in high and low avoidance individuals was found. The high intertrial activity in the superior avoidance groups and the low activity in the poor avoidance group was interpreted as another indication of an active versus passive strategy respectively. Accordingly, it was concluded that not all non-aggressive mice assume a passive strategy, but that some mice adopt an active strategy, like all aggressive males.
ABSTRACT
In wild house mice, the hypothesis that in the organization of behavior the relative contribution of intrinsic factors is more important in aggressive males, while that of extrinsic factors is more important in nonaggressive individuals was confirmed using the circadian rhythmicity of activity. The faster rate of reentrainment and the suppression of activity during a subjective night and during adaptation to the new LD cycle in the nonaggressive males indicate that their circadian rhythmicity of activity is to a large extent determined by the Zeitgeber, an extrinsic factor. The slower reentrainment rate, the lack of response to a subjective night and the normal activity level seen during reentrainment in the aggressive mice suggest strong control by the pacemaker, an intrinsic factor. Tau differences between the aggressive and nonaggressive mice provide some evidence that the pacemaker of nonaggressive males is fairly labile and is easily influenced by external factors, whereas the pacemaker of aggressive animals is rather stable.
