87 research outputs found
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Altered Cortical Ensembles in Mouse Models of Schizophrenia
In schizophrenia, brain-wide alterations have been identified at the molecular and cellular levels, yet how these phenomena affect cortical circuit activity remains unclear. We studied two mouse models of schizophrenia-relevant disease processes: chronic ketamine (KET) administration and Df(16)A+/-, modeling 22q11.2 microdeletions, a genetic variant highly penetrant for schizophrenia. Local field potential recordings in visual cortex confirmed gamma-band abnormalities similar to patient studies. Two-photon calcium imaging of local cortical populations revealed in both models a deficit in the reliability of neuronal coactivity patterns (ensembles), which was not a simple consequence of altered single neuron activity. This effect was present in ongoing and sensory-evoked activity and was not replicated by acute ketamine administration or pharmacogenetic parvalbumin-interneuron suppression. These results are consistent with the hypothesis that schizophrenia is an ‘‘attractor’’ disease and demonstrate that degraded neuronal ensembles are a common consequence of diverse genetic, cellular, and synaptic alterations seen in chronic schizophrenia
Derepression of a Neuronal Inhibitor due to miRNA Dysregulation in a Schizophrenia-Related Microdeletion
Summary22q11.2 microdeletions result in specific cognitive deficits and schizophrenia. Analysis of Df(16)A+/− mice, which model this microdeletion, revealed abnormalities in the formation of neuronal dendrites and spines, as well as altered brain microRNAs. Here, we show a drastic reduction of miR-185, which resides within the 22q11.2 locus, to levels more than expected by a hemizygous deletion, and we demonstrate that this reduction alters dendritic and spine development. miR-185 represses, through an evolutionarily conserved target site, a previously unknown inhibitor of these processes that resides in the Golgi apparatus and shows higher prenatal brain expression. Sustained derepression of this inhibitor after birth represents the most robust transcriptional disturbance in the brains of Df(16)A+/− mice and results in structural alterations in the hippocampus. Reduction of miR-185 also has milder age- and region-specific effects on the expression of some Golgi-related genes. Our findings illuminate the contribution of microRNAs in psychiatric disorders and cognitive dysfunction
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Reduced natriuretic response to acute sodium loading in COMT Gene deleted mice
BACKGROUND: The intrarenal natriuretic hormone dopamine (DA) is metabolised by catechol-O-methyltransferase (COMT) and monoamine oxidase (MAO). Inhibition of COMT, as opposed to MAO, results in a potent natriuretic response in the rat. The present study in anaesthetized homozygous and heterozygous COMT gene deleted mice attempted to further elucidate the importance of COMT in renal DA and sodium handling. After acute intravenous isotonic sodium loading, renal function was followed. RESULTS: COMT activity in heterozygous mice was about half of that in wild type mice and was zero in the homozygous mice. MAO activity did not differ between the genotypes. Urinary sodium excretion increased 10-fold after sodium loading in wild type mice. In heterozygous and homozygous mice, the natriuretic effects of sodium loading were only 29 % and 39 %, respectively, of that in wild type mice. Arterial pressure and glomerular filtration rate did not differ between genotypes. Baseline norepinephrine and DA excretions in urine were elevated in the homozygous, but not in heterozygous, COMT gene deleted mice. Urinary DA excretion increased after isotonic sodium loading in the wild type mice but not in the COMT gene deleted mice. CONCLUSIONS: Mice with reduced or absent COMT activity have altered metabolism of catecholamines and are unable to increase renal DA activity and produce normal natriuresis in response to acute sodium loading. The results support the hypothesis that COMT has an important role in the DA-mediated regulation of renal sodium excretion
Scan statistic-based analysis of exome sequencing data identifies FAN1 at 15q13.3 as a susceptibility gene for schizophrenia and autism
We used a family-based cluster detection approach designed to
localize significant rare disease–risk variants clusters within a region
of interest to systematically search for schizophrenia (SCZ)
susceptibility genes within 49 genomic loci previously implicated
by de novo copy number variants. Using two independent wholeexome
sequencing family datasets and a follow-up autism spectrum
disorder (ASD) case/control whole-exome sequencing dataset,
we identified variants in one gene, Fanconi-associated nuclease 1
(FAN1), as being associated with both SCZ and ASD. FAN1 is located
in a region on chromosome 15q13.3 implicated by a recurrent copy
number variant, which predisposes to an array of psychiatric and
neurodevelopmental phenotypes. In both SCZ and ASD datasets,
rare nonsynonymous risk variants cluster significantly in affected
individuals within a 20-kb window that spans several key functional
domains of the gene. Our finding suggests that FAN1 is a
key driver in the 15q13.3 locus for the associated psychiatric and
neurodevelopmental phenotypes. FAN1 encodes a DNA repair enzyme,
thus implicating abnormalities in DNA repair in the susceptibility
to SCZ or ASD.National
Science Foundation Grant DMS-1100279 and National Institutes of Health
Grants R01MH095797 (to I.I.-L.) and R01MH61399 (to M.K.).http://www.pnas.orghj201
Fine mapping on chromosome 13q32-34 and brain expression analysis implicates MYO16 in schizophrenia
We previously reported linkage of schizophrenia and schizoaffective disorder to 13q32–34 in the European descent Afrikaner population
from South Africa. The nature of genetic variation underlying linkage peaks in psychiatric disorders remains largely unknown and both
rare and common variants may be contributing. Here, we examine the contribution of common variants located under the 13q32–34
linkage region. We used densely spaced SNPs to fine map the linkage peak region using both a discovery sample of 415 families and a
meta-analysis incorporating two additional replication family samples. In a second phase of the study, we use one family-based data set
with 237 families and independent case–control data sets for fine mapping of the common variant association signal using HapMap SNPs.
We report a significant association with a genetic variant (rs9583277) within the gene encoding for the myosin heavy-chain Myr 8
(MYO16), which has been implicated in neuronal phosphoinositide 3-kinase signaling. Follow-up analysis of HapMap variation within
MYO16 in a second set of Afrikaner families and additional case–control data sets of European descent highlighted a region across introns
2–6 as the most likely region to harbor common MYO16 risk variants. Expression analysis revealed a significant increase in the level of
MYO16 expression in the brains of schizophrenia patients. Our results suggest that common variation within MYO16 may contribute to
the genetic liability to schizophrenia.National Institute of Mental Health (NIMH) Grant MH061399, the Lieber Center for Schizophrenia Research at Columbia University, Gray Matters Fellowship and NARSAD Young Investigator Award.http://www.nature.com/npphb201
From Shortage to Surge : A Developmental Switch in Hippocampal-Prefrontal Coupling in a Gene-Environment Model of Neuropsychiatric Disorders
Cognitive deficits represent a major burden of neuropsychiatric disorders and result in part from abnormal communication within hippocampal-prefrontal circuits. While it has been hypothesized that this network dysfunction arises during development, long before the first clinical symptoms, experimental evidence is still missing. Here, we show that pre-juvenile mice mimicking genetic and environmental risk factors of disease (dual-hit GE mice) have poorer recognition memory that correlates with augmented coupling by synchrony and stronger directed interactions between prefrontal cortex and hippocampus. The network dysfunction emerges already during neonatal development, yet it initially consists in a diminished hippocampal theta drive and consequently, a weaker and disorganized entrainment of local prefrontal circuits in discontinuous oscillatory activity in dual-hit GE mice when compared with controls. Thus, impaired maturation of functional communication within hippocampal-prefrontal networks switching from hypo- to hyper-coupling may represent a mechanism underlying the pathophysiology of cognitive deficits in neuropsychiatric disorders.Peer reviewe
Management of intra-abdominal infections : recommendations by the WSES 2016 consensus conference
This paper reports on the consensus conference on the management of intra-abdominal infections (IAIs) which was held on July 23, 2016, in Dublin, Ireland, as a part of the annual World Society of Emergency Surgery (WSES) meeting. This document covers all aspects of the management of IAIs. The Grading of Recommendations Assessment, Development and Evaluation recommendation is used, and this document represents the executive summary of the consensus conference findings.Peer reviewe
Synaptic plasticity, neural circuits and the emerging role of altered short-term information processing in schizophrenia
Synaptic plasticity alters the strength of information flow between presynaptic and postsynaptic neurons and thus modifies the likelihood that action potentials in a presynaptic neuron will lead to an action potential in a postsynaptic neuron. As such, synaptic plasticity and pathological changes in synaptic plasticity impact the synaptic computation which controls the information flow through the neural microcircuits responsible for the complex information processing necessary to drive adaptive behaviors. As current theories of neuropsychiatric disease suggest that distinct dysfunctions in neural circuit performance may critically underlie the unique symptoms of these diseases, pathological alterations in synaptic plasticity mechanisms may be fundamental to the disease process. Here we consider mechanisms of both short-term and long-term plasticity of synaptic transmission and their possible roles in information processing by neural microcircuits in both health and disease. As paradigms of neuropsychiatric diseases with strongly implicated risk genes, we discuss the findings in schizophrenia and autism and consider the alterations in synaptic plasticity and network function observed in both human studies and genetic mouse models of these diseases. Together these studies have begun to point towards a likely dominant role of short-term synaptic plasticity alterations in schizophrenia while dysfunction in autism spectrum disorders may be due to a combination of both short-term and long-term synaptic plasticity alterations
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