Publications by authors named "Alysabeth Phillips"

Article Synopsis
  • A population of neurons in the ventral tegmental area (VTA) co-transmit two neurotransmitters, glutamate and GABA, but their inputs and functions are not fully understood.
  • Using advanced tracing techniques in mice, researchers discovered that these neurons receive diverse inputs from various brain regions, with significant inputs from the superior colliculus and lateral hypothalamus.
  • Optical activation of these inputs revealed that lateral hypothalamus involvement leads to active behavior, while superior colliculus stimulation results in brief activation and freezing behavior, indicating the complex integration of signals by VTA neurons related to motivation and behavior.
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Ventral tegmental area (VTA) glutamatergic neurons participate in reward, aversion, drug-seeking, and stress. Subsets of VTA VGluT2+ neurons are capable of co-transmitting glutamate and GABA (VGluT2+VGaT+ neurons), transmitting glutamate without GABA (VGluT2+VGaT- neurons), or co-transmitting glutamate and dopamine (VGluT2+TH+ neurons), but whether these molecularly distinct subpopulations show behavior-related differences is not wholly understood. We identified that neuronal activity of each VGluT2+ subpopulation is sensitive to reward value but signaled this in different ways.

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A unique population of ventral tegmental area (VTA) neurons co-transmits glutamate and GABA as well as functionally signals rewarding and aversive outcomes. However, the circuit inputs to VTA VGluT2+VGaT+ neurons are unknown, limiting our understanding of the functional capabilities of these neurons. To identify the inputs to VTA VGluT2+VGaT+ neurons, we coupled monosynaptic rabies tracing with intersectional genetic targeting of VTA VGluT2+VGaT+ neurons in mice.

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A significant portion of prescription opioid users self-administer orally rather than intravenously. Animal models of opioid addiction have demonstrated that intravenous cues are sufficient to cause drug seeking. However, intravenous models may not characterize oral users, and the preference to self-administer orally appears to be partially influenced by the user's sex.

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