ABSTRACT
The first record of captive-bred red foxes (Vulpes vulpes) dates to 1896 when a breeding enterprise emerged in the provinces of Atlantic Canada. Because its domestication happened during recent history, the red fox offers a unique opportunity to examine the genetic diversity of an emerging domesticated species in the context of documented historical and economic influences. In particular, the historical record suggests that North American and Eurasian farm-bred populations likely experienced different demographic trajectories. Here, we focus on the likely impacts of founder effects and genetic drift given historical trends in fox farming on North American and Eurasian farms. A total of 15 mitochondrial haplotypes were identified in 369 foxes from 10 farm populations that we genotyped (nâ =â 161) or that were previously published. All haplotypes are endemic to North America. Although most haplotypes were consistent with eastern Canadian ancestry, a small number of foxes carried haplotypes typically found in Alaska and other regions of western North America. The presence of these haplotypes supports historical reports of wild foxes outside of Atlantic Canada being introduced into the breeding stock. These putative Alaskan and Western haplotypes were more frequently identified in Eurasian farms compared to North American farms, consistent with historical documentation suggesting that Eurasian economic and breeding practices were likely to maintain low-frequency haplotypes more effectively than in North America. Contextualizing inter- vs. intra-farm genetic diversity alongside the historical record is critical to understanding the origins of this emerging domesticate and the relationships between wild and farm-bred fox populations.
Subject(s)
Foxes , Genetic Variation , Haplotypes , Foxes/genetics , Animals , DNA, Mitochondrial/genetics , Canada , Genetics, Population , Animals, Domestic/genetics , Domestication , Breeding , Founder Effect , Genetic Drift , FarmsABSTRACT
Since 1959, the Russian Farm-Fox study has bred foxes to be either tame or, more recently, aggressive, and scientists have used them to gain insight into the brain structures associated with these behavioral features. In mice, hippocampal area CA2 has emerged as one of the essential regulators of social aggression, and so to eventually determine whether we could identify differences in CA2 between tame and aggressive foxes, we first sought to identify CA2 in foxes (Vulpes vulpes). As no clearly defined area of CA2 has been described in species such as cats, dogs, or pigs, it was not at all clear whether CA2 could be identified in foxes. In this study, we cut sections of temporal lobes from male and female red foxes, perpendicular to the long axis of the hippocampus, and stained them with markers of CA2 pyramidal cells commonly used in tissue from rats and mice. We observed that antibodies against Purkinje cell protein 4 best stained the pyramidal cells in the area spanning the end of the mossy fibers and the beginning of the pyramidal cells lacking mossy fibers, resembling the pattern seen in rats and mice. Our findings indicate that foxes do have a "molecularly defined" CA2, and further, they suggest that other carnivores like dogs and cats might as well. With this being the case, these foxes could be useful in future studies looking at CA2 as it relates to aggression.
Subject(s)
Cat Diseases , Dog Diseases , Animals , Female , Male , Dogs , Cats , Mice , Rats , Swine , Foxes , Brain , HippocampusABSTRACT
The process of dog domestication likely involved at least two functional stages. The initial stage occurred when subpopulations of wolves became synanthropes, benefiting from life nearby or in human environments. The second phase was characterized by the evolution of novel forms of interspecific cooperation and social relationships between humans and dogs. Here, we discuss possible roles of the oxytocin system across these functional stages of domestication. We hypothesize that in early domestication, oxytocin played important roles in attenuating fear and stress associated with human contact. In later domestication, we hypothesize that oxytocin's most critical functions were those associated with affiliative social behavior, social engagement, and cooperation with humans. We outline possible neurobiological changes associated with these processes and present a Siberian fox model of canid domestication in which these predictions can be tested. Lastly, we identify limitations of current studies on the neuroendocrinology of domestication and discuss challenges and opportunities for future research.
ABSTRACT
The publisher regret that they failed to include the Table 1 before the publication of the original version of this article. The table is presented in this article.
ABSTRACT
Animal domestication was an important stage in the human history, which coincided with or probably even promoted the advent of a turning point at which part of the humankind switched from hunting and gathering to husbandry. The leading factor in evolutionary changes at the dawn of domestication was probably selection for behavior towards humans: first natural (as the animals were habituating to a new ecological niche close to humans), then nonconscious, artificial. Selection was supposed to work on the systems that regulate behavior by reducing stress response and aggression and by inducing an emotionally positive response to humans. A possible role of the neuropeptides adrenocorticotropic hormone (ACTH), oxytocin (ÐТ), arginine vasopressin (AVP), and their receptors is in the reduction in stress response and in the shaping of domestic behavior. Effects of oxytocin on the behavior of domestic animals have been actively explored in the last 10 years, with special focus on the dog. The results obtained so far suggest that this neuropeptide is substantially important for human-canine interactions, together with sex, amount of aggression experienced, and other factors. The study of AVP demonstrated its importance in aggression in domestic animals. This work lends support to the hypothesis that a substantial factor in the shaping of domestic behavior and in the reduction in stress-response might be selection for an enhanced activity of the central OT system and a reduced activity of the central AVP system, which have effects on ACTH and social behavior.
Subject(s)
Domestication , Neuropeptides/metabolism , Aggression , Animals , Arginine Vasopressin/metabolism , Humans , Polymorphism, Genetic , Receptors, Oxytocin/geneticsABSTRACT
Work on laboratory and wild rodents suggests that domestication may impact on the extent of adult hippocampal neurogenesis and its responsiveness to regulatory factors. There is, however, no model of laboratory rodents and their nondomesticated conspecifics that would allow a controlled comparison of the effect of domestication. Here, we present a controlled within-species comparison of adult hippocampal neurogenesis in farm-bred foxes (Vulpes vulpes) that differ in their genetically determined degree of tameness. Quantitative comparisons of cell proliferation (Ki67) and differentiating cells of neuronal lineage (doublecortin, DCX) in the hippocampus of foxes were performed as a proxy for neurogenesis. Higher neurogenesis was observed in tameness-selected foxes, notably in an extended subgranular zone of the middle and temporal compartments of the hippocampus. Increased neurogenesis is negatively associated with aggressive behavior. Across all animals, strong septotemporal gradients were found, with higher numbers of proliferating cells and young neurons relative to resident granule cells in the temporal than in the septal hippocampus. The opposite gradient was found for the ratio of DCX/Ki67- positive cells. When tameness-selected and unselected foxes are compared with rodents and primates, proliferation is similar, while the number of young neurons is higher. The difference may be mediated by an extended period of differentiation or higher rate of survival. On the background of this species-specific neurogenic pattern, selection of foxes for a single behavioral trait key to domestication, i.e., genetic tameness, is accompanied by global and region-specific increases in neurogenesis.
Subject(s)
Animals, Domestic/physiology , Entorhinal Cortex/cytology , Hippocampus/cytology , Neurogenesis/physiology , Neurons/physiology , Aggression/physiology , Analysis of Variance , Animals , Cell Count , Cell Differentiation , Cell Proliferation/physiology , Doublecortin Domain Proteins , Doublecortin Protein , Foxes/anatomy & histology , Ki-67 Antigen/metabolism , Male , Microtubule-Associated Proteins/metabolism , Neuropeptides/metabolismABSTRACT
It is well known that the early life experiences affect stress responses and other physiological and behavioral traits in adulthood. Both rat and human studies have shown that early postnatal effects are associated with methylation of the hippocampal glucocorticoid receptor gene exon 1(7) (rat) and 1-F (human) promoters. Methylation of these sites is also seen following methionine administration in adult rats. However, it remains unclear whether similar alterations in DNA methylation profiles can result from prenatal influences. To address this question, we fed pregnant rats a methyl-supplemented diet that resulted in alteration of the stress response. However, methylation analysis revealed no effect of methyl supplements on methylation patterns of the glucocorticoid receptor gene exon 1(7) promoter in offspring. These results suggest that the pre- and postnatal effects of methyl supplementation have different mechanisms.