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Long-term effects of maternal choline supplementation on CA1 pyramidal neuron gene expression in the Ts65Dn mouse model of Down syndrome and Alzheimer's disease

Alldred, Melissa J; Chao, Helen M; Lee, Sang Han; Beilin, Judah; Powers, Brian E; Petkova, Eva; Strupp, Barbara J; Ginsberg, Stephen D
Choline is critical for normative function of 3 major pathways in the brain, including acetylcholine biosynthesis, being a key mediator of epigenetic regulation, and serving as the primary substrate for the phosphatidylethanolamine N-methyltransferase pathway. Sufficient intake of dietary choline is critical for proper brain function and neurodevelopment. This is especially important for brain development during the perinatal period. Current dietary recommendations for choline intake were undertaken without critical evaluation of maternal choline levels. As such, recommended levels may be insufficient for both mother and fetus. Herein, we examined the impact of perinatal maternal choline supplementation (MCS) in a mouse model of Down syndrome and Alzheimer's disease, the Ts65Dn mouse relative to normal disomic littermates, to examine the effects on gene expression within adult offspring at ∼6 and 11 mo of age. We found MCS produces significant changes in offspring gene expression levels that supersede age-related and genotypic gene expression changes. Alterations due to MCS impact every gene ontology category queried, including GABAergic neurotransmission, the endosomal-lysosomal pathway and autophagy, and neurotrophins, highlighting the importance of proper choline intake during the perinatal period, especially when the fetus is known to have a neurodevelopmental disorder such as trisomy.-Alldred, M. J., Chao, H. M., Lee, S. H., Beilin, J., Powers, B. E., Petkova, E., Strupp, B. J., Ginsberg, S. D. Long-term effects of maternal choline supplementation on CA1 pyramidal neuron gene expression in the Ts65Dn mouse model of Down syndrome and Alzheimer's disease.
PMID: 31180719
ISSN: 1530-6860
CID: 3929822

NREM sleep in the rodent neocortex and hippocampus reflects excitable dynamics

Levenstein, Daniel; Buzsáki, György; Rinzel, John
During non-rapid eye movement (NREM) sleep, neuronal populations in the mammalian forebrain alternate between periods of spiking and inactivity. Termed the slow oscillation in the neocortex and sharp wave-ripples in the hippocampus, these alternations are often considered separately but are both crucial for NREM functions. By directly comparing experimental observations of naturally-sleeping rats with a mean field model of an adapting, recurrent neuronal population, we find that the neocortical alternations reflect a dynamical regime in which a stable active state is interrupted by transient inactive states (slow waves) while the hippocampal alternations reflect a stable inactive state interrupted by transient active states (sharp waves). We propose that during NREM sleep in the rodent, hippocampal and neocortical populations are excitable: each in a stable state from which internal fluctuations or external perturbation can evoke the stereotyped population events that mediate NREM functions.
PMID: 31171779
ISSN: 2041-1723
CID: 3918242

Interneurons: Learning on the Job

Batista-Brito, Renata; Fishell, Gord
In this issue, Wester et al. (2019) examine the obligate relationship between cortical interneurons and pyramidal neurons. By genetically converting superficial IT pyramidal cells into PT-like deep-layer pyramidal cells, they alter the position, connectivity, and gene expression within CGE-derived interneurons.
PMID: 31170396
ISSN: 1097-4199
CID: 4123992

A distinct inferential mechanism for delusions in schizophrenia

Baker, Seth C; Konova, Anna B; Daw, Nathaniel D; Horga, Guillermo
Delusions, a core symptom of psychosis, are false beliefs that are rigidly held with strong conviction despite contradictory evidence. Alterations in inferential processes have long been proposed to underlie delusional pathology, but previous attempts to show this have failed to yield compelling evidence for a specific relationship between inferential abnormalities and delusional severity in schizophrenia. Using a novel, incentivized information-sampling task (a modified version of the beads task), alongside well-characterized decision-making tasks, we sought a mechanistic understanding of delusions in a sample of medicated and unmedicated patients with schizophrenia who exhibited a wide range of delusion severity. In this novel task, participants chose whether to draw beads from one of two hidden jars or to guess the identity of the hidden jar, in order to minimize financial loss from a monetary endowment, and concurrently reported their probability estimates for the hidden jar. We found that patients with higher delusion severity exhibited increased information seeking (i.e. increased draws-to-decision behaviour). This increase was highly specific to delusion severity as compared to the severity of other psychotic symptoms, working-memory capacity, and other clinical and socio-demographic characteristics. Delusion-related increases in information seeking were present in unmedicated patients, indicating that they were unlikely due to antipsychotic medication. In addition, after adjusting for delusion severity, patients as a whole exhibited decreased information seeking relative to healthy individuals, a decrease that correlated with lower socioeconomic status. Computational analyses of reported probability estimates further showed that more delusional patients exhibited abnormal belief updating characterized by stronger reliance on prior beliefs formed early in the inferential process, a feature that correlated with increased information seeking in patients. Other decision-making parameters that could have theoretically explained the delusion effects, such as those related to subjective valuation, were uncorrelated with both delusional severity and information seeking among the patients. In turn, we found some preliminary evidence that subjective valuation (rather than belief updating) may explain group differences in information seeking unrelated to delusions. Together, these results suggest that abnormalities in belief updating, characterized by stronger reliance on prior beliefs formed by incorporating information presented earlier in the inferential process, may be a core computational mechanism of delusional ideation in psychosis. Our results thus provide direct empirical support for an inferential mechanism that naturally captures the characteristic rigidity associated with delusional beliefs.
PMID: 30895299
ISSN: 1460-2156
CID: 3749262

Effects of neonatal ethanol on cerebral cortex development through adolescence

Smiley, John F; Bleiwas, Cynthia; Masiello, Kurt; Petkova, Eva; Betz, Judith; Hui, Maria; Wilson, Donald A; Saito, Mariko
Neonatal brain lesions cause deficits in structure and function of the cerebral cortex that sometimes are not fully expressed until adolescence. To better understand the onset and persistence of changes caused by postnatal day 7 (P7) ethanol treatment, we examined neocortical cell numbers, volume, surface area and thickness from neonatal to post-adolescent ages. In control mice, total neuron number decreased from P8 to reach approximately stable levels at about P30, as expected from normal programmed cell death. Cortical thickness reached adult levels by P14, but cortical volume and surface area continued to increase from juvenile (P20-30) to post-adolescent (P54-93) ages. P7 ethanol caused a reduction of total neurons by P14, but this deficit was transient, with later ages having only small and non-significant reductions. Previous studies also reported transient neuron loss after neonatal lesions that might be partially explained by an acute acceleration of normally occurring programmed cell death. GABAergic neurons expressing parvalbumin, calretinin, or somatostatin were reduced by P14, but unlike total neurons the reductions persisted or increased in later ages. Cortical volume, surface area and thickness were also reduced by P7 ethanol. Cortical volume showed evidence of a transient reduction at P14, and then was reduced again in post-adolescent ages. The results show a developmental sequence of neonatal ethanol effects. By juvenile ages the cortex overcomes the P14 deficit of total neurons, whereas P14 GABA cell deficits persist. Cortical volume reductions were present at P14, and again in post-adolescent ages.
PMID: 31049690
ISSN: 1863-2661
CID: 3854952

Elevated Brain Iron in Cocaine Use Disorder as Indexed by Magnetic Field Correlation Imaging

Adisetiyo, Vitria; McGill, Corinne E; DeVries, William H; Jensen, Jens H; Hanlon, Colleen A; Helpern, Joseph A
BACKGROUND:Iron homeostasis is a critical biological process that may be disrupted in cocaine use disorder (CUD). In the brain, iron is required for neural processes involved in addiction and can be lethal to cells if unbound, especially in excess. Moreover, recent studies have implicated elevated brain iron in conditions of prolonged psychostimulant exposure. Thus, the purpose of this study was to examine iron in basal ganglia reward regions of individuals with CUD using an advanced imaging method called magnetic field correlation (MFC) imaging. METHODS:MFC imaging was acquired in 19 non-treatment-seeking individuals with CUD and 19 healthy control individuals (both male and female). Region-of-interest analyses for MFC group differences and within-group correlations with age and years of cocaine use were conducted in the globus pallidus internal segment (GPi), globus pallidus external segment, putamen, caudate nucleus, thalamus, and red nucleus. RESULTS:Individuals with CUD had significantly elevated MFC compared with control individuals within the GPi. In control individuals, MFC significantly increased with age in the GPi, globus pallidus external segment, putamen, and caudate nucleus. Conversely, there were no significant MFC within-group correlations in the CUD group. CONCLUSIONS:Individuals with CUD have excess iron in the GPi, as indexed by MFC, and lack the age-related gradual iron deposition seen in normal aging. Because the globus pallidus is critical for the transition of goal-directed behavior to compulsive behavior, significantly elevated iron in the GPi may contribute to the persistence of CUD. These findings implicate dysregulation of brain iron homeostasis in CUD and support pursuing this new line of research.
PMID: 30581153
ISSN: 2451-9030
CID: 3680272

Neurobiology of maternal regulation of infant fear: the role of mesolimbic dopamine and its disruption by maltreatment

Opendak, Maya; Robinson-Drummer, Patrese; Blomkvist, Anna; Zanca, Roseanna M; Wood, Kira; Jacobs, Lily; Chan, Stephanie; Tan, Stephen; Woo, Joyce; Venkataraman, Gayatri; Kirschner, Emma; Lundström, Johan N; Wilson, Donald A; Serrano, Peter A; Sullivan, Regina M
Child development research highlights caregiver regulation of infant physiology and behavior as a key feature of early life attachment, although mechanisms for maternal control of infant neural circuits remain elusive. Here we explored the neurobiology of maternal regulation of infant fear using neural network and molecular levels of analysis in a rodent model. Previous research has shown maternal suppression of amygdala-dependent fear learning during a sensitive period. Here we characterize changes in neural networks engaged during maternal regulation and the transition to infant self-regulation. Metabolic mapping of 2-deoxyglucose uptake during odor-shock conditioning in postnatal day (PN)14 rat pups showed that maternal presence blocked fear learning, disengaged mesolimbic circuitry, basolateral amygdala (BLA), and plasticity-related AMPA receptor subunit trafficking. At PN18, when maternal presence only socially buffers threat learning (similar to social modulation in adults), maternal presence failed to disengage the mesolimbic dopaminergic system, and failed to disengage both the BLA and plasticity-related AMPA receptor subunit trafficking. Further, maternal presence failed to block threat learning at PN14 pups following abuse, and mesolimbic dopamine engagement and AMPA were not significantly altered by maternal presence-analogous to compromised maternal regulation of children in abusive relationships. Our results highlight three key features of maternal regulation: (1) maternal presence blocks fear learning and amygdala plasticity through age-dependent suppression of amygdala AMPA receptor subunit trafficking, (2) maternal presence suppresses engagement of brain regions within the mesolimbic dopamine circuit, and (3) early-life abuse compromises network and molecular biomarkers of maternal regulation, suggesting reduced social scaffolding of the brain.
PMID: 30758321
ISSN: 1740-634x
CID: 3656282

Value of MRI in medicine: More than just another test? [Editorial]

van Beek, Edwin J R; Kuhl, Christiane; Anzai, Yoshimi; Desmond, Patricia; Ehman, Richard L; Gong, Qiyong; Gold, Garry; Gulani, Vikas; Hall-Craggs, Margaret; Leiner, Tim; Lim, C C Tschoyoson; Pipe, James G; Reeder, Scott; Reinhold, Caroline; Smits, Marion; Sodickson, Daniel K; Tempany, Clare; Vargas, H Alberto; Wang, Meiyun
There is increasing scrutiny from healthcare organizations towards the utility and associated costs of imaging. MRI has traditionally been used as a high-end modality, and although shown extremely important for many types of clinical scenarios, it has been suggested as too expensive by some. This editorial will try and explain how value should be addressed and gives some insights and practical examples of how value of MRI can be increased. It requires a global effort to increase accessibility, value for money, and impact on patient management. We hope this editorial sheds some light and gives some indications of where the field may wish to address some of its research to proactively demonstrate the value of MRI. Level of Evidence: 5 Technical Efficacy: Stage 5 J. Magn. Reson. Imaging 2019;49:e14-e25.
PMID: 30145852
ISSN: 1522-2586
CID: 3990552

Effect of multislit collimator motion on sparsect image quality for low-dose CT examinations [Meeting Abstract]

Chen, B; Kobler, E; Allmendinger, T; Sodickson, A; Sodickson, D; Otazo, R
Purpose: SparseCT is a practical compressed sensing approach for CT dose reduction, which undersamples each view along the row dimension with a multislit collimator (MSC). The MSC is mounted between tube and patient and moves along the row direction to change the undersampling pattern along the row dimension for each view. This study aims to investigate the impact of MSC motion on SparseCT image quality.
Method(s): A SparseCT prototype was built with the MSC installed on a state-of-art clinical CT scanner. The MSC is a tungsten plate with periodic slits parallel to detector row direction. The slit separation is 3 times wider than the slit width, such that the dose reduction factor is 3. A liver phantom was scanned repeatedly at various MSC locations, each sampling different rows. The MSC was static during each scan, but 'dynamic MSC' scans were retrospectively simulated by stitching together projections from different scans. Six MSC motions were tested, including 3 patterns (linear, back-and-forth, and random) and 2 speeds (1 and 5 row(s)/projection). The dynamic MSC scans were reconstructed iteratively using a compressed sensing reconstruction algorithm that enforces 3D sparsity using total variation regularization. Image quality for different motions were compared in terms of PSNR and SSIM.
Result(s): Increasing MSC motion speed significantly improved PSNR and SSIM while the effect of motion pattern was negligible. Higher motion speeds also markedly reduced undersampling artifacts observed around high attenuation, high frequency objects such as the spine. The best PSNR and SSIM were achieved using a combination of linear motion and a speed of 5 rows/projection.
Conclusion(s): The motion of the MSC has a significant impact on the performance of SparseCT. Higher motion speed yields more incoherent undersampling artifacts and thus improves reconstruction quality
EMBASE:628827271
ISSN: 0094-2405
CID: 4044152

Resonate: Reflections and recommendations on implicit biases within the ISMRM [Editorial]

Warnert, Esther A H; Nayak, Krishna; Menon, Ravi; Rice, Curt; Port, John; Morris, Elizabeth A; Sodickson, Daniel K; Sundgren, Pia; Miller, Karla L; Anazodo, Udunna C
PMID: 30666751
ISSN: 1522-2586
CID: 3610502