The neural basis for a persistent internal state in Drosophila females.

ABSTRACT

Sustained changes in mood or action require persistent changes in neural activity, but it has been difficult to identify the neural circuit mechanisms that underlie persistent activity and contribute to long-lasting changes in behavior. Here, we show that a subset of Doublesex+ pC1 neurons in the Drosophila female brain, called pC1d/e, can drive minutes-long changes in female behavior in the presence of males. Using automated reconstruction of a volume electron microscopic (EM) image of the female brain, we map all inputs and outputs to both pC1d and pC1e. This reveals strong recurrent connectivity between, in particular, pC1d/e neurons and a specific subset of Fruitless+ neurons called aIPg. We additionally find that pC1d/e activation drives long-lasting persistent neural activity in brain areas and cells overlapping with the pC1d/e neural network, including both Doublesex+ and Fruitless+ neurons. Our work thus links minutes-long persistent changes in behavior with persistent neural activity and recurrent circuit architecture in the female brain.

Long-term mental states such as arousal and mood variations rely on persistent changes in the activity of certain neural circuits which have been difficult to identify. For instance, in male fruit flies, the activation of a particular circuit containing 'P1 neurons' can escalate aggressive and mating behaviors. However, less is known about the neural networks that underlie arousal in female flies. A group of female-specific, 'pC1 neurons' similar to P1 neurons could play this role, but it was unclear whether it could drive lasting changes in female fly behavior. To investigate this question, Deutsch et al. stimulated or shut down pC1 circuits in female flies, and then recorded the insects' interactions with male flies. Stimulation was accomplished using optogenetics, a technique which allows researchers to precisely control the activity of specially modified light-sensitive neurons. Silencing pC1 neurons in female flies diminished their interest in male partners and their suitor's courtship songs. Activating these neural circuits made the females more receptive to males; it also triggered long-lasting aggressive behaviors not typically observed in virgin females, such as shoving and chasing. Deutsch et al. then identified the brain cells that pC1 neurons connect to, discovering that these neurons are part of an interconnected circuit also formed of aIPg neurons ­ a population of fly brain cells that shows sex differences and is linked to female aggression. The brains of females were then imaged as pC1 neurons were switched on, revealing a persistent activity which outlasted the activation in circuits containing both pC1 and aIPg neurons. Thus, these results link neural circuit architecture to long lasting changes in neural activity, and ultimately, in behavior. Future experiments can build on these results to determine how this circuit is activated during natural social interactions.