Hippocampal bone morphogenetic protein signaling mediates behavioral effects of antidepressant treatment

Brooker, Sarah M.; Kt, Gobeske; Chen, J; Cy, Peng; Ja, Kessler

doi:10.1038/mp.2016.160

Cited by 49 publications

(36 citation statements)

References 65 publications

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“…Notably, the direction of effect in these gene sets changed between P14 and adulthood – at P14, gene sets related to proliferation and differentiation were enriched with elevated expression in bLRs, whereas by adulthood elevated expression was seen in bHRs. This pattern fits the changing role of Bmp4 across development: Bmp4 is important for neural induction during early development (102, 103), but later suppresses neurogenesis (100, 104–106) and promotes other cell fates (102, 107). For example, Bmp4 can a promote endothelial proliferation (84), which matches the elevated endothelial-specific gene expression that we observed in the bLR hippocampus at P14.…”

Section: Discussionsupporting

confidence: 69%

“…These results are consistent with the association between Bmp4 and anxiety and depressive-like behaviors in the literature. Blocking Bmp4 expression in mice reduces anxiety and depressive-like behavior and increases the effectiveness of certain anti-depressant treatments (100). Similarly, transgenic mice that are deficient for Bmp receptors have extremely low levels of anxiety and diminished fear conditioning (101).…”

Section: Discussionmentioning

confidence: 99%

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Genetic liability for internalizing versus externalizing behavior manifests in the developing and adult hippocampus: Insight from a meta-analysis of transcriptional profiling studies in a selectively-bred rat model

Birt

Hagenauer

Clinton

et al. 2019

Preprint

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2For over 16 years, we have selectively-bred rats to react differently to a novel, anxiety-3 inducing environment, exhibiting either high or low exploratory activity. These "bred High 4 Responder" (bHR) and "bred Low Responder" (bLR) rats serve as a general model for extreme 5 manifestations of behavioral inhibition and temperament, showing large differences in a variety 6 of internalizing and externalizing behaviors relevant to both mood and substance abuse 7 disorders. The current study elucidated persistent differences in gene expression related to 8 bHR/bLR phenotype across development (P7, P14, P21) and adulthood within the 9 hippocampus, a brain structure critical for emotional regulation. To do this, we meta-analyzed 10 eight transcriptional profiling datasets (microarray and RNA-Seq) spanning 43 generations of 11 selective breeding (n=2-6 rats per group per dataset; total n per meta-analysis: adult: n=46, P7: 12 n=22, P14: n=49, P21: n=21). By cross-referencing these results with a concurrent exome 13 sequencing study performed on our colony, we pinpointed several genes that are strongly 14 implicated in bHR/bLR behavioral phenotype, including two genes previously associated with 15 energy metabolism and mood: Thyrotropin releasing hormone receptor (Trhr) and the 16 mitochondrial protein Uncoupling protein 2 (Ucp2). Our meta-analysis also highlighted robust 17 bHR/bLR functional differences in the hippocampus, including a network essential for 18 neurodevelopmental programming, cell proliferation, and differentiation, which centered on the 19 hub genes Bone morphogenetic protein 4 (Bmp4) and the canonical Marker of proliferation 20 (Mki67). Another functional theme was microglial activation and phagocytosis, including 21 differential expression of pro-inflammatory Complement C1q A chain (C1qa) and the anti- 22inflammatory Milk fat globule-EGF factor 8 (Mfge8), situated within a chromosomal loci 23 implicated by our concurrent genetic study. Given the newly-discovered role of microglia in 24 synaptic pruning in relationship to neuronal activity during both development and adulthood, we 25 propose that these functional pathways have the capability to not only direct bHR and bLR rats 26 along a different developmental trajectory, but to set the stage for a widely-different reactivity to 27 the environment. 28 29 30 35 36 Both mood disorders and substance abuse disorders affect approximately 8-10% of 37 adults in the United States each year (1, 2). Due to high comorbidity, these disorders are often 38 classified as either internalizing and externalizing. Internalizing disorders are associated with 39 neuroticism, anxiety, and depression, whereas externalizing disorders are associated with 40 greater risk-taking and novelty-seeking, as seen in mania, substance abuse, and impulse-41 control disorders (3). This pattern of comorbidity is thought to represent a spectrum of latent 42 liability, which arises from a complex interplay of genetic risk and environmental factors, such as 43 stress and childhood adversity...

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Section: Discussionsupporting

confidence: 69%

Section: Discussionmentioning

confidence: 99%

Genetic liability for internalizing versus externalizing behavior manifests in the developing and adult hippocampus: Insight from a meta-analysis of transcriptional profiling studies in a selectively-bred rat model

Birt

Hagenauer

Clinton

et al. 2019

Preprint

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“…These NSCs undergo cell division, and some daughter cells differentiate into functional neurons that participate in learning and memory and general cognition through integration into pre‐existing neural networks (de Miranda, Zhang, Katsumoto, & Teixeira, ). Further evidence suggest that it is the dorsal hippocampus that is involved in spatial learning and memory, while the ventral hippocampus is more associated with limbic functions (Brooker, Gobeske, Chen, Peng, & Kessler, ; Hyer, Hunter, Katakam, Wolz, & Glasper, ; Kheirbek & Hen, ; Loxton & Canales, ; McHugh, Fillenz, Lowry, Rawlins, & Bannerman, ; Schoenfeld, McCausland, Sonti, & Cameron, ). Abnormalities in hippocampal function are associated with various neurological and psychiatric disorders in adults such as anxiety, schizophrenia and depression (Ampuero, Jury, Hartel, Marzolo, & Zundert, ; Brooker et al, ; Caruncho et al, ; Danzer, Kotloski, Walter, Hughes, & McNamara, ; Liu et al, ; Perez‐Domper et al, ; Yun et al, ).…”

Section: Locations Of Adult Neural Stem Cells In the Mammalian Brainmentioning

confidence: 99%

“…Studies have demonstrated that decreased neurogenesis may be one cause of depression (Tamura et al, ). Indeed, many antidepressants have been shown to stimulate adult hippocampal neurogenesis (Brooker et al, ). It has been proposed that different sub‐regions of the hippocampus may regulate the distinct functions associated with the hippocampus (Bettio et al, ).…”

Section: Functional Aspects Of New Dgcs In the Adult Hippocampusmentioning

confidence: 99%

“…For example, the dorsal hippocampus appears to be involved in spatial learning and memory, while the ventral hippocampus is associated with stress, emotion and affect (Brooker et al, ; Hyer et al, ; Kheirbek & Hen, ; Loxton & Canales, ; McHugh et al, ; Schoenfeld et al, ). The hippocampus appears to have important functions in neurological and psychiatric disorders including anxiety, schizophrenia and depression (Ampuero et al, ; Brooker et al, ; Caruncho et al, ; Danzer et al, ; Liu et al, ; Perez‐Domper et al, ; Yun et al, ). Lesions in the ventral hippocampus and specifically ventral dentate gyrus lesions in rodents produce decreased anxiety‐like behaviour (Cameron & Glover, ).…”

Section: Functional Aspects Of New Dgcs In the Adult Hippocampusmentioning

confidence: 99%

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Adult neurogenesis in the mammalian dentate gyrus

Abbott

Nigussie

2019

Anat Histol Embryol

128

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Earlier observations in neuroscience suggested that no new neurons form in the mature central nervous system. Evidence now indicates that new neurons do form in the adult mammalian brain. Two regions of the mature mammalian brain generate new neurons: (a) the border of the lateral ventricles of the brain (subventricular zone) and (b) the subgranular zone (SGZ) of the dentate gyrus of the hippocampus. This review focuses only on new neuron formation in the dentate gyrus of the hippocampus. During normal prenatal and early postnatal development, neural stem cells (NSCs) give rise to differentiated neurons. NSCs persist in the dentate gyrus SGZ, undergoing cell division, with some daughter cells differentiating into functional neurons that participate in learning and memory and general cognition through integration into pre‐existing neural networks. Axons, which emanate from neurons in the entorhinal cortex, synapse with dendrites of the granule cells (small neurons) of the dentate gyrus. Axons from granule cells synapse with pyramidal cells in the hippocampal CA3 region, which send axons to synapse with CA1 hippocampal pyramidal cells that send their axons out of the hippocampus proper. Adult neurogenesis includes proliferation, differentiation, migration, the death of some newly formed cells and final integration of surviving cells into neural networks. We summarise these processes in adult mammalian hippocampal neurogenesis and discuss the roles of major signalling molecules that influence neurogenesis, including neurotransmitters and some hormones. The recent controversy raised concerning whether or not adult neurogenesis occurs in humans also is discussed.

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