2019
DOI: 10.1016/j.pscychresns.2019.04.005
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Circuit activity underlying a distinct modulator of prepulse inhibition

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Cited by 6 publications
(6 citation statements)
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“…However, these alterations were absent at PND30, which indicated that PPI changes caused by Poly I:C were also age-dependent. The functional basis of PPI is regulated by the brainstem, but it is highly modulated by cerebral (including frontocortical) inputs [ 91 , 92 ] as well as dopamine [ 93 , 94 ] and serotonin transmission [ 95 , 96 ]. Since CX3CL1 signalling participates in the regulation of these neurotransmitters [ 97 , 98 ], the question arises whether and how the increase in CX3CL1 level in the frontal cortex of offspring during the neurodevelopmental period could affect PPI deficits.…”
Section: Discussionmentioning
confidence: 99%
“…However, these alterations were absent at PND30, which indicated that PPI changes caused by Poly I:C were also age-dependent. The functional basis of PPI is regulated by the brainstem, but it is highly modulated by cerebral (including frontocortical) inputs [ 91 , 92 ] as well as dopamine [ 93 , 94 ] and serotonin transmission [ 95 , 96 ]. Since CX3CL1 signalling participates in the regulation of these neurotransmitters [ 97 , 98 ], the question arises whether and how the increase in CX3CL1 level in the frontal cortex of offspring during the neurodevelopmental period could affect PPI deficits.…”
Section: Discussionmentioning
confidence: 99%
“…Sensorimotor gating is a process that allows an animal to allocate attentional resources to more salient stimuli in the environment [ 90 ]. The functional basis of PPI is regulated by the brainstem, but it is highly modulated by cerebral [ 92 ] and hippocampal [ 93 ] inputs as well as dopamine [ 94 ] and serotonin [ 95 , 96 ] transmission. Here, we provide evidence that MIA in Sprague-Dawley offspring did not interfere with sensorimotor gating in adolescence.…”
Section: Discussionmentioning
confidence: 99%
“…Furthermore, the CX3CL1-CX3CR1 dyad contributes to the regulation of synaptic organization [103,104], hippocampal cognitive function, and neurogenesis [105,106] as well as to a reduction in excitotoxicity [107]. Since the functional basis of PPI is regulated by interactions between various structures, including hippocampal and cerebral inputs [108,109], as well as by dopamine [108,110] and serotonin transmission [111,112], and CX3CL1 participates in the regulation of these neurotransmitters, the changes in this signalling observed between the offspring groups (MIA PPI-low and MIA PPI-high ) may be reflected by differences in behavioural schizophrenia-like patterns. However, this hypothesis should be a focus of further studies.…”
Section: Discussionmentioning
confidence: 99%