ABSTRACT
A comprehensive understanding of neuronal diversity and connectivity is essential for understanding the anatomical and cellular mechanisms that underlie functional contributions. With the advent of single-cell analysis, growing information regarding molecular profiles leads to the identification of more heterogeneous cell types. Therefore, the need for additional orthogonal recombinase systems is increasingly apparent, as heterogeneous tissues can be further partitioned into increasing numbers of specific cell types defined by multiple features. Critically, new recombinase systems should work together with pre-existing systems without cross-reactivity in vivo. Here, we introduce novel site-specific recombinase systems based on ΦC31 bacteriophage recombinase for labeling multiple cell types simultaneously and a novel viral strategy for versatile and robust intersectional expression of any transgene. Together, our system will help researchers specifically target different cell types with multiple features in the same animal.
Subject(s)
Integrases , Recombinases , Animals , Recombinases/genetics , Integrases/genetics , Genetic Vectors , Neurons/metabolism , TransgenesABSTRACT
Optogenetic stimulation of Adora2a receptor-expressing spiny projection neurons (A2A-SPNs) in the striatum drives locomotor suppression and transient punishment, results attributed to activation of the indirect pathway. The sole long-range projection target of A2A-SPNs is the external globus pallidus (GPe). Unexpectedly, we found that inhibition of the GPe drove transient punishment but not suppression of movement. Within the striatum, A2A-SPNs inhibit other SPNs through a short-range inhibitory collateral network, and we found that optogenetic stimuli that drove motor suppression shared a common mechanism of recruiting this inhibitory collateral network. Our results suggest that the indirect pathway plays a more prominent role in transient punishment than in motor control and challenges the assumption that activity of A2A-SPNs is synonymous with indirect pathway activity.
Subject(s)
Basal Ganglia , Punishment , Corpus Striatum , Globus Pallidus/physiology , Movement/physiologyABSTRACT
Pharmacological agents that treat anxiety disorders are often validated in animal models prior to clinical trials. Yet results suggest little consistency in rodent anxiety-like behavior across tests. The current study examined the relationship between anxiety-like behaviors of male rats in the open field test and free exploratory paradigm. Results indicate most anxiety-like behaviors between tests were not correlated and few correlations existed within tests, despite similarity in testing apparatus, procedures, and quantified behaviors. These results suggest even very similar tests may provide insight into different facets of anxiety and urge caution when translating animal results to the human condition.
