Appropriate inhibition of orexigenic hypothalamic arcuate nucleus neurons independently of leptin receptor/STAT3 signaling

H Münzberg, EE Jobst, SH Bates, J Jones… - Journal of …, 2007 - Soc Neuroscience
H Münzberg, EE Jobst, SH Bates, J Jones, E Villanueva, R Leshan, M Björnholm, J Elmquist…
Journal of Neuroscience, 2007Soc Neuroscience
Leptin directly suppresses the activity of orexigenic neurons in the hypothalamic arcuate
nucleus (ARC). We examined c-Fos-like immunoreactivity (CFLIR) as a marker of ARC
neuronal activity in db/db mice devoid of the signaling form of the leptin receptor (LRb) and
s/s mice that express LRbS1138 [which is defective for STAT3 (signal transducer and
activator of transcription) signaling]. Both db/db and s/s animals are hyperphagic and obese.
This analysis revealed that CFLIR in agouti related peptide-expressing orexigenic ARC …
Leptin directly suppresses the activity of orexigenic neurons in the hypothalamic arcuate nucleus (ARC). We examined c-Fos-like immunoreactivity (CFLIR) as a marker of ARC neuronal activity in db/db mice devoid of the signaling form of the leptin receptor (LRb) and s/s mice that express LRbS1138 [which is defective for STAT3 (signal transducer and activator of transcription) signaling]. Both db/db and s/s animals are hyperphagic and obese. This analysis revealed that CFLIR in agouti related peptide-expressing orexigenic ARC neurons is basally elevated in db/db but not s/s mice. Consistent with these observations, electrophysiologic evaluation of a small number of neurons in s/s animals suggested that leptin appropriately suppresses the frequency of IPSCs on ARC proopiomelanocortin (POMC) neurons that are mediated by the release of GABA from orexigenic ARC neurons. CFLIR in POMC neurons of s/s mice was also increased compared with db/db animals. Thus, these data suggest that, although LRb→STAT3 signaling is crucial for the regulation of feeding, it is not required for the acute or chronic regulation of orexigenic ARC neurons, and the activation of STAT3-mediated transcription by leptin is not required for the appropriate development of leptin responsiveness in these neurons.
Soc Neuroscience