4.6 Article

Heterogeneous responses of nucleus incertus neurons to corticotrophin-releasing factor and coherent activity with hippocampal theta rhythm in the rat

Journal

JOURNAL OF PHYSIOLOGY-LONDON
Volume 591, Issue 16, Pages 3981-4001

Publisher

WILEY
DOI: 10.1113/jphysiol.2013.254300

Keywords

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Funding

  1. National Health and Medical Research Council (NHMRC) of Australia [520299, 277609, 509246, 1005988, 350207]
  2. Polish Ministry of Science and Higher Education [N N303 569939]
  3. Commonwealth of Australia Endeavour Research Fellowship
  4. Florey Neuroscience Institutes Foundation
  5. National Heart Foundation of Australia
  6. Austin Hospital Foundation
  7. The Ministry of Health, Spain [ISCIII-FIS PI061816]
  8. Johnson & Johnson Pharmaceutical Research & Development, LLC, San Diego, USA
  9. Besen Family Foundation
  10. Pratt Foundation
  11. Victorian Government Operational Infrastructure Support Program
  12. NHMRC (Australia) Biomedical Postdoctoral Fellowship

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The nucleus incertus (NI) of the rat hindbrain is a putative node in the ascending control of the septohippocampal system and hippocampal theta rhythm and is stress and arousal responsive. NI contains GABA neurons that express multiple neuropeptides, including relaxin-3 (RLN3) and neuropeptide receptors, including corticotrophin-releasing factor receptor-1 (CRF-R1), but the precise anatomical and physiological characteristics of NI neurons are unclear. Therefore, we examined the firing properties of NI neurons and their responses to CRF, the correlation of these responses with occurrence of relaxin-3, and NI neuron morphology in the rat. Most NI neurons excited by intracerebroventricular CRF infusion were RLN3-positive (9 of 10), whereas all inhibited cells were RLN3-negative (8 of 8). The spontaneous firing of RLN3 (n = 6) but not non-RLN3 neurons (n = 6) was strongly modulated and phase-locked with the initial ascending phase of hippocampal theta oscillations. In brain slices, the majority of recorded NI neurons (15 of 19) displayed excitatory responses to CRF, which uniformly increased action potential frequency and membrane potential depolarization in the presence of tetrodotoxin, indicating a direct, postsynaptic action of CRF on NI neurons. This excitation was associated with reduction in the slow component of afterhyperpolarization and a strong depolarization. Quantitative analysis in naive rats of validated CRF-R1, RLN3 and neuronal nuclear antigen (NeuN) immunoreactivity revealed 52% of NI neurons as CRF-R1 positive, of which 53% were RLN3 positive, while 48% of NI neurons lacked CRF-R1 and RLN3. All RLN3 neurons expressed CRF-R1. CRF neurons that projected to the NI were identified in lateral preoptic hypothalamus, but not in paraventricular hypothalamus, bed nucleus of stria terminalis or central amygdala. Our findings suggest NI is an important site for CRF modulation of hippocampal theta rhythm via effects on GABA/RLN3 transmission.

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