Chronic postnatal chemogenetic activation of forebrain excitatory neurons evokes persistent changes in mood behavior

Pati, Sthitapranjya; Saba, Kamal; Salvi, Sonali S.; Tiwari, Praachi; Chaudhari, Pratik R.; Verma, Vijaya; Mukhopadhyay, Sourish; Kapri, Darshana; Suryavanshi, Shital; Clement, James P.; Patel, Anant B.; Vaidya, Vidita A.

doi:10.7554/elife.56171

Cited by 13 publications

(20 citation statements)

References 151 publications

(345 reference statements)

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“…In several previous studies, DREADD-induced selective and consecutive stimulation was used as an intervention for damaged optic nerves (Li et al, 2016;Lim et al, 2016), damaged peripheral nerves (Gao et al, 2021;Wu et al, 2020), stressrelated behavior (Chen et al, 2020;Pati et al, 2020), alcohol abuse (Pozhidayeva et al, 2020), pain control (Xu et al, 2021), epilepsy (Desloovere et al, 2019;Goossens et al, 2021), intracerebral hemorrhage (Ling et al, 2020), microglial inflammation (Binning et al, 2020), and b-amyloid deposition (Rodriguez et al, 2020;Yuan and Grutzendler, 2016). In a study stimulating dorsal root ganglia neurons after crush injury (Wu et al, 2020), 4 weeks of repetitive stimulations did not alter the functional scores or axon regeneration, which was significant after 12 weeks.…”

Section: Discussionmentioning

confidence: 99%

Long-term selective stimulation of transplanted neural stem/progenitor cells for spinal cord injury improves locomotor function

et al. 2021

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Section: Discussionmentioning

confidence: 99%

Long-term selective stimulation of transplanted neural stem/progenitor cells for spinal cord injury improves locomotor function

et al. 2021

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“…DREADD‐based chemogenetic approaches using both transgenic and viral strategies allow for spatiotemporal regulation of select G protein‐coupled signaling cascades in discrete neuronal populations [138]. It is only relatively recently that DREADD‐mediated chemogenetic strategies have been exploited to address the contribution of Gq‐ and Gi‐mediated signaling pathways in mediating the effects of early stress in programming persistent changes in anxio‐depressive behavioral states [48,139,140].…”

Section: Dreadd‐based Approaches To Address the Role Of Gpcrs In The Effects Of Early Stressmentioning

confidence: 99%

“…In contrast, the Gq-coupled hM3Dq-based DREADD activation of PFC neurons with a pan-neuronal hSyn promoter in pups subjected to the MS paradigm can prevent the emergence of MS-evoked short-term memory impairments and enhanced despair-like behavior [139]. Work from our laboratory has recently demonstrated that chronic chemogenetic activation of Gq signaling in CaMKIIa-positive forebrain excitatory neurons during the early postnatal window (P2-14) is sufficient to program a persistent increase in anxiety and despair-like behavior, accompanied by sensorimotor gating deficits [140]. Adult animals with a history of hM3Dq-based DREADD activation of excitatory forebrain neurons display an altered excitatory/inhibitory balance in cortical circuits as revealed through metabolomic and electrophysiological signatures, phenocopying some of the functional changes associated with preclinical models of psychiatric disorders [140].…”

Section: Dreadd-based Approaches To Address the Role Of Gpcrs In The Effects Of Early Stressmentioning

confidence: 99%

“…Work from our laboratory has recently demonstrated that chronic chemogenetic activation of Gq signaling in CaMKIIa-positive forebrain excitatory neurons during the early postnatal window (P2-14) is sufficient to program a persistent increase in anxiety and despair-like behavior, accompanied by sensorimotor gating deficits [140]. Adult animals with a history of hM3Dq-based DREADD activation of excitatory forebrain neurons display an altered excitatory/inhibitory balance in cortical circuits as revealed through metabolomic and electrophysiological signatures, phenocopying some of the functional changes associated with preclinical models of psychiatric disorders [140]. The differences noted across the studies described above could arise as a consequence of the specific population of neurons targeted and the neurocircuit that is being regulated (Fig.…”

Section: Dreadd-based Approaches To Address the Role Of Gpcrs In The Effects Of Early Stressmentioning

confidence: 99%

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GPCR signaling: role in mediating the effects of early adversity in psychiatric disorders

et al. 2021

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Early adversity is a key risk factor for the development of several psychiatric disorders, including anxiety and depression. During early life, neurocircuits that regulate emotionality undergo substantial structural remodeling and functional maturation, and are thus particularly susceptible to modification by environmental experience. Preclinical evidence indicates that early stress enhances adult anxio-depressive behaviors. A commonality noted across diverse early stress models is life-long alterations in neuroendocrine stress responses and monoaminergic neurotransmission in key limbic circuits. Dysregulation of G protein-coupled receptor (GPCR) signaling is noted across multiple early stress models and is hypothesized to be an important player in the programming of aberrant emotionality. This raises the possibility that disruption of GPCR signaling in key limbic regions during critical temporal windows could establish a substrate for enhanced risk of adult psychopathology. Here, we review literature, predominantly from preclinical models, which supports the building hypothesis that a disruption of GPCR signaling could play a central role in programming persistent molecular, cellular, functional, and behavioral changes as a consequence of early adversity.

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“…Loss of function of the G q -coupled 5-HT 2A receptor, in particular in the forebrain, is associated with reduced anxiety-like behavior ( Weisstaub, 2006 ), whereas loss of function of the G i -coupled 5-HT 1A receptor during postnatal life, in both forebrain and raphe neurocircuits, has been linked to increased anxiety-like behavior ( Gross et al, 2002 ; Vinkers et al, 2010 ; Richardson-Jones et al, 2010 , 2011 ; Mineur et al, 2015 ). Furthermore, pharmacological blockade of the G i -coupled 5-HT 1A receptor during postnatal life is associated with the emergence of increased anxiety in adulthood ( Vinkers et al, 2010 ; Garcia-Garcia et al, 2014 ; Sarkar et al, 2014 ), whereas pharmacological stimulation of the G q -coupled 5-HT 2A receptors ( Sarkar et al, 2014 ) or enhanced G q signaling driven via chemogenetic activation of excitatory forebrain neurons during postnatal window programs increased anxiety- and despair-like behavior in adulthood ( Pati et al, 2020 ).…”

Section: Introductionmentioning

confidence: 99%

Chronic hM4Di-DREADD-Mediated Chemogenetic Inhibition of Forebrain Excitatory Neurons in Postnatal or Juvenile Life Does Not Alter Adult Mood-Related Behavior

Tiwari

Kapri

Pradhan

et al. 2022

eNeuro

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G-protein-coupled receptors (GPCRs) coupled to G i signaling, in particular downstream of monoaminergic neurotransmission, are posited to play a key role during developmental epochs (postnatal and juvenile) in shaping the emergence of adult anxiodepressive behaviors and sensorimotor gating. To address the role of G i signaling in these developmental windows, we used a CaMKIIα-tTA::TRE hM4Di bigenic mouse line to express the hM4Di-DREADD (designer receptor exclusively activated by designer drugs) in forebrain excitatory neurons and enhanced G i signaling via chronic administration of the DREADD agonist, clozapine- N -oxide (CNO) in the postnatal window (postnatal days 2–14) or the juvenile window (postnatal days 28–40). We confirmed that the expression of the HA-tagged hM4Di-DREADD was restricted to CaMKIIα-positive neurons in the forebrain, and that the administration of CNO in postnatal or juvenile windows evoked inhibition in forebrain circuits of the hippocampus and cortex, as indicated by a decline in expression of the neuronal activity marker c-Fos. hM4Di-DREADD-mediated inhibition of CaMKIIα-positive forebrain excitatory neurons in postnatal or juvenile life did not impact the weight profile of mouse pups, and also did not influence the normal ontogeny of sensory reflexes. Further, postnatal or juvenile hM4Di-DREADD-mediated inhibition of CaMKIIα-positive forebrain excitatory neurons did not alter anxiety- or despair-like behaviors in adulthood and did not impact sensorimotor gating. Collectively, these results indicate that chemogenetic induction of G i signaling in CaMKIIα-positive forebrain excitatory neurons in postnatal and juvenile temporal windows does not appear to impinge on the programming of anxiodepressive behaviors in adulthood.

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Chronic postnatal chemogenetic activation of forebrain excitatory neurons evokes persistent changes in mood behavior

Cited by 13 publications

References 151 publications

Long-term selective stimulation of transplanted neural stem/progenitor cells for spinal cord injury improves locomotor function

Long-term selective stimulation of transplanted neural stem/progenitor cells for spinal cord injury improves locomotor function

GPCR signaling: role in mediating the effects of early adversity in psychiatric disorders

Chronic hM4Di-DREADD-Mediated Chemogenetic Inhibition of Forebrain Excitatory Neurons in Postnatal or Juvenile Life Does Not Alter Adult Mood-Related Behavior

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