Your search keyword '"Emilie L. Castranio"' showing total 15 results

1. ABCA1 haplodeficiency affects the brain transcriptome following traumatic brain injury in mice expressing human APOE isoforms

Author

Emilie L. Castranio, Cody M. Wolfe, Kyong Nyon Nam, Florent Letronne, Nicholas F. Fitz, Iliya Lefterov, and Radosveta Koldamova

Subjects

Traumatic brain injury, Apolipoprotein E, ABCA1, Transcriptome, WGCNA, Microglia sensome, Neurology. Diseases of the nervous system, RC346-429

Abstract

Abstract Expression of human Apolipoprotein E (APOE) modulates the inflammatory response in an isoform specific manner, with APOE4 isoform eliciting a stronger pro-inflammatory response, suggesting a possible mechanism for worse outcome following traumatic brain injury (TBI). APOE lipidation and stability is modulated by ATP-binding cassette transporter A1 (ABCA1), a transmembrane protein that transports lipids and cholesterol onto APOE. We examined the impact of Abca1 deficiency and APOE isoform expression on the response to TBI using 3-months-old, human APOE3 +/+ (E3/Abca1 +/+) and APOE4 +/+ (E4/Abca1 +/+ ) targeted replacement mice, and APOE3 +/+ and APOE4 +/+ mice with only one functional copy of the Abca1 gene (E3/Abca1 +/− ; E4/Abca1 +/−). TBI-treated mice received a craniotomy followed by a controlled cortical impact (CCI) brain injury in the left hemisphere; sham-treated mice received the same surgical procedure without the impact. We performed RNA-seq using samples from cortices and hippocampi followed by genome-wide differential gene expression analysis. We found that TBI significantly impacted unique transcripts within each group, however, the proportion of unique transcripts was highest in E4/Abca1 +/− mice. Additionally, we found that Abca1 haplodeficiency increased the expression of microglia sensome genes among only APOE4 injured mice, a response not seen in injured APOE3 mice, nor in either group of sham-treated mice. To identify gene networks, or modules, correlated to TBI, APOE isoform and Abca1 haplodeficiency, we used weighted gene co-expression network analysis (WGCNA). The module that positively correlated to TBI groups was associated with immune response and featured hub genes that were microglia-specific, including Trem2, Tyrobp, Cd68 and Hexb. The modules positively correlated with APOE4 isoform and negatively to Abca1 haplodeficient mice represented “protein translation” and “oxidation-reduction process”, respectively. Our results reveal E4/Abca1 +/− TBI mice have a distinct response to injury, and unique gene networks are associated with APOE isoform, Abca1 insufficiency and injury.

Published

2018

2. Gene co-expression networks identify Trem2 and Tyrobp as major hubs in human APOE expressing mice following traumatic brain injury

Author

Emilie L. Castranio, Anais Mounier, Cody M. Wolfe, Kyong Nyon Nam, Nicholas F. Fitz, Florent Letronne, Jonathan Schug, Radosveta Koldamova, and Iliya Lefterov

Subjects

Apolipoprotein E, Traumatic brain injury, Trem2, Tyrobp, Myelination, Immune response, Neurosciences. Biological psychiatry. Neuropsychiatry, RC321-571

Abstract

Traumatic brain injury (TBI) is strongly linked to an increased risk of developing dementia, including chronic traumatic encephalopathy and possibly Alzheimer's disease (AD). APOEε4 allele of human Apolipoprotein E (APOE) gene is the major genetic risk factor for late onset AD and has been associated with chronic traumatic encephalopathy and unfavorable outcome following TBI. To determine if there is an APOE isoform-specific response to TBI we performed controlled cortical impact on 3-month-old mice expressing human APOE3 or APOE4 isoforms. Following injury, we used several behavior paradigms to test for anxiety and learning and found that APOE3 and APOE4 targeted replacement mice demonstrate cognitive impairments following moderate TBI. Transcriptional profiling 14 days following injury revealed a significant effect of TBI, which was similar in both genotypes. Significantly upregulated by injury in both genotypes were mRNA expression and protein level of ABCA1 transporter and APOJ, but not APOE.To identify gene-networks correlated to injury and APOE isoform, we performed Weighted Gene Co-expression Network Analysis. We determined that the network mostly correlated to TBI in animals expressing both isoforms is immune response with major hub genes including Trem2, Tyrobp, Clec7a and Cd68. We also found a significant increase of TREM2, IBA-1 and GFAP protein levels in the brains of injured mice. We identified a network representing myelination that correlated significantly with APOE isoform in both injury groups. This network was significantly enriched in oligodendrocyte signature genes, such as Mbp and Plp1. Our results demonstrate unique and distinct gene networks at this acute time point for injury and APOE isoform, as well as a network driven by APOE isoform across TBI groups.

Published

2017

3. Effect of high fat diet on phenotype, brain transcriptome and lipidome in Alzheimer’s model mice

Author

Kyong Nyon Nam, Anais Mounier, Cody M. Wolfe, Nicholas F. Fitz, Alexis Y. Carter, Emilie L. Castranio, Hafsa I. Kamboh, Valerie L. Reeves, Jianing Wang, Xianlin Han, Jonathan Schug, Iliya Lefterov, and Radosveta Koldamova

Subjects

Medicine, Science

Abstract

Abstract We examined the effect of chronic high fat diet (HFD) on amyloid deposition and cognition of 12-months old APP23 mice, and correlated the phenotype to brain transcriptome and lipidome. HFD significantly increased amyloid plaques and worsened cognitive performance compared to mice on normal diet (ND). RNA-seq results revealed that in HFD mice there was an increased expression of genes related to immune response, such as Trem2 and Tyrobp. We found a significant increase of TREM2 immunoreactivity in the cortex in response to HFD, most pronounced in female mice that correlated to the amyloid pathology. Down-regulated by HFD were genes related to neuron projections and synaptic transmission in agreement to the significantly deteriorated neurite morphology and cognition in these mice. To examine the effect of the diet on the brain lipidome, we performed Shotgun Lipidomics. While there was no difference in the total amounts of phospholipids of each class, we revealed that the levels of 24 lipid sub-species in the brain were significantly modulated by HFD. Network visualization of correlated lipids demonstrated overall imbalance with most prominent effect on cardiolipin molecular sub-species. This integrative approach demonstrates that HFD elicits a complex response at molecular, cellular and system levels in the CNS.

Published

2017

4. Genome-wide approaches reveal EGR1-controlled regulatory networks associated with neurodegeneration

Author

Radosveta Koldamova, Jonathan Schug, Martina Lefterova, Andrea A. Cronican, Nicholas F. Fitz, Faith A. Davenport, Alexis Carter, Emilie L. Castranio, and Iliya Lefterov

Subjects

Alzheimer's disease, Animal model, ChIP-seq, Brain, Egr1, Histone modifications, Neurosciences. Biological psychiatry. Neuropsychiatry, RC321-571

Abstract

Early growth response gene 1 (Egr1) is a member of the immediate early gene (IEG) family of transcription factors and plays a role in memory formation. To identify EGR1 target genes in brain of Alzheimer's disease (AD) model mice — APP23, we applied chromatin immunoprecipitation (ChIP) followed by high-throughput DNA sequencing (ChIP-seq). Functional annotation of genes associated with EGR1 binding revealed a set of related networks including synaptic vesicle transport, clathrin-mediated endocytosis (CME), intracellular membrane fusion and transmission of signals elicited by Ca2+ influx. EGR1 binding is associated with significant enrichment of activating chromatin marks and appears enriched near genes that are up-regulated in the brains of APP23 mice. Among the putative EGR1 targets identified and validated in this study are genes related to synaptic plasticity and transport of proteins, such as Arc, Grin1, Syn2, Vamp2 and Stx6, and genes implicated in AD such as Picalm, Psen2 and App. We also demonstrate a potential regulatory link between EGR1 and its newly identified targets in vivo, since conditions that up-regulate Egr1 levels in brain, such as a spatial memory test, also lead to increased expression of the targets. On the other hand, protein levels of EGR1 and ARC, SYN2, STX6 and PICALM are significantly lower in the brain of adult APP mice than in age-matched wild type animals. The results of this study suggest that EGR1 regulates the expression of genes involved in CME, vesicular transport and synaptic transmission that may be critical for AD pathogenesis.

Published

2014

5. Microglial INPP5D limits plaque formation and glial reactivity in the PSAPP mouse model of Alzheimer's disease

Author

Emilie L. Castranio, Philip Hasel, Jean‐Vianney Haure‐Mirande, Angie V. Ramirez Jimenez, B. Wade Hamilton, Rachel D. Kim, Charles G. Glabe, Minghui Wang, Bin Zhang, Sam Gandy, Shane A. Liddelow, and Michelle E. Ehrlich

Subjects

Psychiatry and Mental health, Cellular and Molecular Neuroscience, Developmental Neuroscience, Epidemiology, Health Policy, Neurology (clinical), Geriatrics and Gerontology

Abstract

The inositol polyphosphate-5-phosphatase D (INPP5D) gene encodes a dual-specificity phosphatase that can dephosphorylate both phospholipids and phosphoproteins. Single nucleotide polymorphisms in INPP5D impact risk for developing late onset sporadic Alzheimer's disease (LOAD).To assess the consequences of inducible Inpp5d knockdown in microglia of APPAt age 6 months, we found that the percent area of 6E10These results demonstrate that conditional Inpp5d downregulation in the PSAPP mouse increases plaque burden and recruitment of microglia to plaques. Spatial transcriptomics highlighted an extended gene expression signature associated with plaques and identified CST7 (cystatin F) as a novel marker of plaques.Inpp5d knockdown increases plaque burden and plaque-associated microglia number. Spatial transcriptomics identifies an expanded plaque-specific gene expression profile. Plaque-induced gene expression is altered by Inpp5d knockdown in microglia. Our plaque-associated gene signature overlaps with human Alzheimer's disease gene networks.

Published

2022

6. Molecular subtyping of Alzheimer's disease using RNA sequencing data reveals novel mechanisms and targets

Author

Emrin Horgusluoglu-Moloch, Vahram Haroutunian, Lei Guo, Emilie L. Castranio, Valentina Fossati, Erming Wang, Sam Gandy, Chen Ming, Sezen Vatansever, Julia Tcw, Kristen J. Brennand, Won-Min Song, Qian Wang, Minghui Wang, Aiqun Li, Michelle E. Ehrlich, Bin Zhang, Dongming Cai, Scott Noggle, Alison Goate, Ryan Neff, Lap Ho, Eric E. Schadt, and Pavel Katsel

Subjects

Mitochondrion organization, Diseases and Disorders, tau Proteins, Computational biology, Disease, Biology, 03 medical and health sciences, Mice, 0302 clinical medicine, Alzheimer Disease, medicine, Dementia, Animals, Humans, Molecular Biology, Research Articles, Neuroinflammation, 030304 developmental biology, 0303 health sciences, Multidisciplinary, Amyloid beta-Peptides, Sequence Analysis, RNA, Neurodegeneration, SciAdv r-articles, Brain, medicine.disease, Precision medicine, Subtyping, RNA, Synaptic signaling, 030217 neurology & neurosurgery, Research Article, Neuroscience

Abstract

Three major molecular subtypes of Alzheimer’s disease are identified, cross-validated, and characterized across 1543 individuals., Alzheimer’s disease (AD), the most common form of dementia, is recognized as a heterogeneous disease with diverse pathophysiologic mechanisms. In this study, we interrogate the molecular heterogeneity of AD by analyzing 1543 transcriptomes across five brain regions in two AD cohorts using an integrative network approach. We identify three major molecular subtypes of AD corresponding to different combinations of multiple dysregulated pathways, such as susceptibility to tau-mediated neurodegeneration, amyloid-β neuroinflammation, synaptic signaling, immune activity, mitochondria organization, and myelination. Multiscale network analysis reveals subtype-specific drivers such as GABRB2, LRP10, MSN, PLP1, and ATP6V1A. We further demonstrate that variations between existing AD mouse models recapitulate a certain degree of subtype heterogeneity, which may partially explain why a vast majority of drugs that succeeded in specific mouse models do not align with generalized human trials across all AD subtypes. Therefore, subtyping patients with AD is a critical step toward precision medicine for this devastating disease.

Published

2020

7. ABCA1 Deficiency Affects Basal Cognitive Deficits and Dendritic Density in Mice

Author

Victor Tapias, Nicholas F. Fitz, Radosveta Koldamova, Iliya Lefterov, Emilie L. Castranio, Alexis Y. Carter, and Ravindra Kodali

Subjects

Male, 0301 basic medicine, Morris water navigation task, Hippocampal formation, Hippocampus, Amyloid beta-Protein Precursor, Basal (phylogenetics), 0302 clinical medicine, Hippocampus (mythology), Spatial Memory, biology, Chemistry, General Neuroscience, General Medicine, ATP-binding cassette transporter A1 (Abca1), amyloid-β oligomers, Psychiatry and Mental health, Clinical Psychology, neurite morphology, Female, Alzheimer’s disease, Research Article, ATP Binding Cassette Transporter 1, Genetically modified mouse, medicine.medical_specialty, Neurite, Amyloid, Mice, Transgenic, APP mice, 03 medical and health sciences, Internal medicine, Presenilin-1, medicine, Animals, Humans, Maze Learning, Cell Size, Amyloid beta-Peptides, behavior, Recognition, Psychology, Dendrites, hippocampal infusion, Mice, Inbred C57BL, 030104 developmental biology, Endocrinology, radial arm water maze, ABCA1, biology.protein, Geriatrics and Gerontology, Cognition Disorders, 030217 neurology & neurosurgery

Abstract

ATP-binding cassette transporter A1 (ABCA1) mediates cholesterol efflux to lipid-free apolipoproteins and regulates the generation of high density lipoproteins. Previously, we have shown that lack of Abca1 significantly increases amyloid deposition and cognitive deficits in Alzheimer's disease model mice expressing human amyloid-β protein precursor (APP). The goal of this study was to determine if ABCA1 plays a role in memory deficits caused by amyloid-β (Aβ) oligomers and examine neurite architecture of pyramidal hippocampal neurons. Our results confirm previous findings that Abca1 deficiency significantly impairs spatial memory acquisition and retention in the Morris water maze and long-term memory in novel object recognition of APP transgenic mice at a stage of early amyloid pathology. Neither test demonstrated a significant difference between Abca1ko and wild-type (WT) mice. We also examined the effect of intra-hippocampal infused Aβ oligomers on cognitive performance of Abca1ko mice, compared to control infusion of scrambled Aβ peptide. Age-matched WT mice undergoing the same infusions were also used as controls. In this model system, we found a statistically significant difference between WT and Abca1ko mice infused with scrambled Aβ, suggesting that Abca1ko mice are vulnerable to the effect of mild stresses. Moreover, examination of neurite architecture in the hippocampi revealed a significant decrease in neurite length, number of neurite segments, and branches in Abca1ko mice when compared to WT mice. We conclude that mice lacking ABCA1 have basal cognitive deficits that prevent them from coping with additional stressors, which is in part due to impairment of neurite morphology in the hippocampus.

Published

2017

8. ABCA1 haplodeficiency affects the brain transcriptome following traumatic brain injury in mice expressing human APOE isoforms

Author

Radosveta Koldamova, Nicholas F. Fitz, Emilie L. Castranio, Florent Letronne, Kyong Nyon Nam, Iliya Lefterov, and Cody M. Wolfe

Subjects

0301 basic medicine, Gene isoform, Apolipoprotein E, medicine.medical_specialty, Traumatic brain injury, ABCA1, Mice, Transgenic, lcsh:RC346-429, Pathology and Forensic Medicine, Transcriptome, Mice, 03 medical and health sciences, Cellular and Molecular Neuroscience, Apolipoproteins E, Microglia sensome, 0302 clinical medicine, Internal medicine, Brain Injuries, Traumatic, Gene expression, medicine, Animals, Humans, Protein Isoforms, Gene Regulatory Networks, RNA, Messenger, lcsh:Neurology. Diseases of the nervous system, biology, WGCNA, TREM2, Research, Brain, medicine.disease, HEXB, Mice, Inbred C57BL, Disease Models, Animal, 030104 developmental biology, Endocrinology, Gene Expression Regulation, biology.protein, lipids (amino acids, peptides, and proteins), Microglia, Neurology (clinical), 030217 neurology & neurosurgery, ATP Binding Cassette Transporter 1

Abstract

Expression of human Apolipoprotein E (APOE) modulates the inflammatory response in an isoform specific manner, with APOE4 isoform eliciting a stronger pro-inflammatory response, suggesting a possible mechanism for worse outcome following traumatic brain injury (TBI). APOE lipidation and stability is modulated by ATP-binding cassette transporter A1 (ABCA1), a transmembrane protein that transports lipids and cholesterol onto APOE. We examined the impact of Abca1 deficiency and APOE isoform expression on the response to TBI using 3-months-old, human APOE3 +/+ (E3/Abca1 +/+) and APOE4 +/+ (E4/Abca1 +/+ ) targeted replacement mice, and APOE3 +/+ and APOE4 +/+ mice with only one functional copy of the Abca1 gene (E3/Abca1 +/− ; E4/Abca1 +/−). TBI-treated mice received a craniotomy followed by a controlled cortical impact (CCI) brain injury in the left hemisphere; sham-treated mice received the same surgical procedure without the impact. We performed RNA-seq using samples from cortices and hippocampi followed by genome-wide differential gene expression analysis. We found that TBI significantly impacted unique transcripts within each group, however, the proportion of unique transcripts was highest in E4/Abca1 +/− mice. Additionally, we found that Abca1 haplodeficiency increased the expression of microglia sensome genes among only APOE4 injured mice, a response not seen in injured APOE3 mice, nor in either group of sham-treated mice. To identify gene networks, or modules, correlated to TBI, APOE isoform and Abca1 haplodeficiency, we used weighted gene co-expression network analysis (WGCNA). The module that positively correlated to TBI groups was associated with immune response and featured hub genes that were microglia-specific, including Trem2, Tyrobp, Cd68 and Hexb. The modules positively correlated with APOE4 isoform and negatively to Abca1 haplodeficient mice represented “protein translation” and “oxidation-reduction process”, respectively. Our results reveal E4/Abca1 +/− TBI mice have a distinct response to injury, and unique gene networks are associated with APOE isoform, Abca1 insufficiency and injury.

Published

2018

9. Opposing effects ofApoe/Apoa1double deletion on amyloid-β pathology and cognitive performance in APP mice

Author

Nicholas F. Fitz, Martina I. Lefterova, Emilie L. Castranio, Muzamil Saleem, Radosveta Koldamova, Alexis Y. Carter, Iliya Lefterov, Victor Tapias, and Andrea A. Cronican

Subjects

Apolipoprotein E, medicine.medical_specialty, Very low-density lipoprotein, Amyloid, Apolipoprotein B, Biology, Endocrinology, Internal medicine, ABCA1, mental disorders, Immunology, Knockout mouse, medicine, biology.protein, lipids (amino acids, peptides, and proteins), Neurology (clinical), Gene knockout, Lipoprotein

Abstract

ATP binding cassette transporter A1 (encoded by ABCA1 ) regulates cholesterol efflux from cells to apolipoproteins A-I and E (ApoA-I and APOE; encoded by APOA1 and APOE , respectively) and the generation of high density lipoproteins. In Abca1 knockout mice (Abca1ko), high density lipoproteins and ApoA-I are virtually lacking, and total APOE and APOE-containing lipoproteins in brain substantially decreased. As the e4 allele of APOE is the major genetic risk factor for late-onset Alzheimer’s disease, ABCA1 role as a modifier of APOE lipidation is of significance for this disease. Reportedly, Abca1 deficiency in mice expressing human APP accelerates amyloid deposition and behaviour deficits. We used APP/PS1dE9 mice crossed to Apoe and Apoa1 knockout mice to generate Apoe / Apoa1 double-knockout mice. We hypothesized that Apoe / Apoa1 double-knockout mice would mimic the phenotype of APP/Abca1ko mice in regards to amyloid plaques and cognitive deficits. Amyloid pathology, peripheral lipoprotein metabolism, cognitive deficits and dendritic morphology of Apoe / Apoa1 double-knockout mice were compared to APP/Abca1ko, APP/PS1dE9, and single Apoa1 and Apoe knockouts. Contrary to our prediction, the results demonstrate that double deletion of Apoe and Apoa1 ameliorated the amyloid pathology, including amyloid plaques and soluble amyloid. In double knockout mice we show that 125I-amyloid-β microinjected into the central nervous system cleared at a rate twice faster compared to Abca1 knockout mice. We tested the effect of Apoe , Apoa1 or Abca1 deficiency on spreading of exogenous amyloid-β seeds injected into the brain of young pre-depositing APP mice. The results show that lack of Abca1 augments dissemination of exogenous amyloid significantly more than the lack of Apoe. In the periphery, Apoe / Apoa1 double-knockout mice exhibited substantial atherosclerosis and very high levels of low density lipoproteins compared to APP/PS1dE9 and APP/Abca1ko. Plasma level of amyloid-β42 measured at several time points for each mouse was significantly higher in Apoe / Apoa1 double-knockout then in APP/Abca1ko mice. This result demonstrates that mice with the lowest level of plasma lipoproteins, APP/Abca1ko, have the lowest level of peripheral amyloid-β. Unexpectedly, and independent of amyloid pathology, the deletion of both apolipoproteins worsened behaviour deficits of double knockout mice and their performance was undistinguishable from those of Abca1 knockout mice. Finally we observed that the dendritic complexity in the CA1 region of hippocampus but not in CA2 is significantly impaired by Apoe / Apoa1 double deletion as well as by lack of ABCA1. In conclusion: (i) plasma lipoproteins may affect amyloid-β clearance from the brain by the ‘peripheral sink’ mechanism; and (ii) deficiency of brain APOE-containing lipoproteins is of significance for dendritic complexity and cognition. * Abbreviations : Aβ : Amyloid-β Abca1ko : Abca1 knockout APP : APP/PS1dE9 mouse model ApoA-I : apolipoprotein A-I ApoE : apolipoprotein E APP/DKO : APP mice with double deletion of Apoe and Apoa1 Ako : Apoa1 knockout Eko : Apoe knockout VLDL/LDL : very-low-density lipoprotein/low-density lipoprotein

Published

2015

10. [P1–189]: APOE ISOFORM‐SPECIFIC EFFECTS ON AMYLOID‐β‐INDUCED PATHOLOGY: MICROGLIAL FUNCTION, NEURONAL INTEGRITY AND COGNITIVE DECLINE

Author

Nicholas F. Fitz, Cody M. Wolfe, Emilie L. Castranio, Jonathan Schug, Florent Letronne, Kyong Nyon Nam, Radosveta Koldamova, Iliya Lefterov, and Brittany E. Playso

Subjects

Gene isoform, Apolipoprotein E, Amyloid β, Epidemiology, Health Policy, Psychiatry and Mental health, Cellular and Molecular Neuroscience, Developmental Neuroscience, Neurology (clinical), Geriatrics and Gerontology, Cognitive decline, Psychology, Neuroscience, Function (biology)

Published

2017

11. Gene co-expression networks identify Trem2 and Tyrobp as major hubs in human APOE expressing mice following traumatic brain injury

Author

Nicholas F. Fitz, Radosveta Koldamova, Emilie L. Castranio, Jonathan Schug, Anais Mounier, Iliya Lefterov, Kyong Nyon Nam, Cody M. Wolfe, and Florent Letronne

Subjects

0301 basic medicine, Apolipoprotein E, Anxiety, Myelination, Mice, 0302 clinical medicine, Traumatic brain injury, Brain Injuries, Traumatic, Protein Isoforms, Gene Regulatory Networks, Receptors, Immunologic, Principal Component Analysis, Membrane Glycoproteins, Glial fibrillary acidic protein, biology, CLEC7A, Up-Regulation, Neurology, Tyrobp, lipids (amino acids, peptides, and proteins), Psychology, Gene isoform, Trem2, Mice, Transgenic, Article, lcsh:RC321-571, 03 medical and health sciences, Apolipoproteins E, Glial Fibrillary Acidic Protein, medicine, Dementia, Animals, Humans, RNA, Messenger, Immune response, Maze Learning, lcsh:Neurosciences. Biological psychiatry. Neuropsychiatry, Adaptor Proteins, Signal Transducing, TREM2, medicine.disease, Mice, Inbred C57BL, Chronic traumatic encephalopathy, Disease Models, Animal, 030104 developmental biology, Astrocytes, Immunology, biology.protein, Cognition Disorders, 030217 neurology & neurosurgery

Abstract

Traumatic brain injury (TBI) is strongly linked to an increased risk of developing dementia, including chronic traumatic encephalopathy and possibly Alzheimer's disease (AD). APOEe4 allele of human Apolipoprotein E (APOE) gene is the major genetic risk factor for late onset AD and has been associated with chronic traumatic encephalopathy and unfavorable outcome following TBI. To determine if there is an APOE isoform-specific response to TBI we performed controlled cortical impact on 3-month-old mice expressing human APOE3 or APOE4 isoforms. Following injury, we used several behavior paradigms to test for anxiety and learning and found that APOE3 and APOE4 targeted replacement mice demonstrate cognitive impairments following moderate TBI. Transcriptional profiling 14days following injury revealed a significant effect of TBI, which was similar in both genotypes. Significantly upregulated by injury in both genotypes were mRNA expression and protein level of ABCA1 transporter and APOJ, but not APOE. To identify gene-networks correlated to injury and APOE isoform, we performed Weighted Gene Co-expression Network Analysis. We determined that the network mostly correlated to TBI in animals expressing both isoforms is immune response with major hub genes including Trem2, Tyrobp, Clec7a and Cd68. We also found a significant increase of TREM2, IBA-1 and GFAP protein levels in the brains of injured mice. We identified a network representing myelination that correlated significantly with APOE isoform in both injury groups. This network was significantly enriched in oligodendrocyte signature genes, such as Mbp and Plp1. Our results demonstrate unique and distinct gene networks at this acute time point for injury and APOE isoform, as well as a network driven by APOE isoform across TBI groups.

Published

2017

12. Improvement of Memory Deficits and Amyloid-β Clearance in Aged APP23 Mice Treated with a Combination of Anti-Amyloid-β Antibody and LXR Agonist

Author

Nicholas F. Fitz, Alexis Y. Carter, Ravindra Kodali, Iliya Lefterov, Emilie L. Castranio, and Radosveta Koldamova

Subjects

Male, Apolipoprotein E, Genetically modified mouse, Agonist, medicine.medical_specialty, Hydrocarbons, Fluorinated, Side effect, Amyloid, medicine.drug_class, Amyloidogenic Proteins, Mice, Transgenic, Pharmacology, Article, Amyloid beta-Protein Precursor, Random Allocation, Apolipoproteins E, Alzheimer Disease, Internal medicine, Conditioning, Psychological, medicine, Animals, Maze Learning, Liver X receptor, Nootropic Agents, Memory Disorders, Sulfonamides, Amyloid beta-Peptides, biology, General Neuroscience, Immunization, Passive, Antibodies, Monoclonal, Brain, Fear, General Medicine, medicine.disease, Combined Modality Therapy, Mice, Inbred C57BL, Disease Models, Animal, Psychiatry and Mental health, Clinical Psychology, Endocrinology, ABCA1, biology.protein, Female, lipids (amino acids, peptides, and proteins), Geriatrics and Gerontology, Alzheimer's disease, ATP Binding Cassette Transporter 1

Abstract

Passive amyloid-β (Aβ) vaccination has shown significant effects on amyloid pathology in pre-depositing amyloid-β protein precursor (AβPP) mice but the results in older mice are inconsistent. A therapeutic effect of LXR and RXR agonists consisting of improved memory deficits and Aβ pathology has been demonstrated in different Alzheimer's disease (AD) mouse models. Here, we report the effect of a combination of N-terminal Aβ antibody and synthetic LXR agonist T0901317 (T0) on AD-like phenotype of APP23 mice. To examine the therapeutic potential of this combination, the treatment of mice started at 11 months of age, when amyloid phenotype in this model is fully developed, and continued for 50 days. We show that Aβ immunization with or without LXR agonist restored the performance of APP23 transgenic mice in two behavior paradigms without affecting the existing amyloid plaques. Importantly, we did not observe an increase of brain microhemorrhage which is considered a significant side effect of Aβ vaccination. Target engagement was confirmed by increased Abca1 and ApoE protein level as well as increased ApoE lipidation in soluble brain extract. In interstitial fluid obtained by microdialysis, we demonstrate that immunization and T0 significantly reduced Aβ levels, indicating an increased Aβ clearance. We found no interaction between the immunotherapy and T0, suggesting no synergism, at least with these doses. The results of our study demonstrate that anti-Aβ treatments can ameliorate cognitive deficits in AβPP mice with advanced AD-like phenotype in conjunction with a decrease of Aβ in brain interstitium and increase of ApoE lipidation without affecting the existing amyloid plaques.

Published

2014

13. P4‐065: Impact of Apoe Polymorphisms on Amyloid‐Beta Oligomerization and Associated Cognitive Decline

Author

Nicholas F. Fitz, Emilie L. Castranio, Alexis Y. Carter, Kyong Nyon Nam, Radosveta Koldamova, Anais Mounier, Iliya Lefterov, and Cody M. Wolfe

Subjects

Apolipoprotein E, medicine.medical_specialty, biology, Epidemiology, Amyloid beta, business.industry, Health Policy, Psychiatry and Mental health, Cellular and Molecular Neuroscience, Endocrinology, Developmental Neuroscience, Internal medicine, medicine, biology.protein, Neurology (clinical), Geriatrics and Gerontology, Cognitive decline, business

Published

2016

14. Bexarotene-Activated Retinoid X Receptors Regulate Neuronal Differentiation and Dendritic Complexity

Author

Jonathan Schug, Radosveta Koldamova, Andrea A. Cronican, Nicholas F. Fitz, Kyong Nyon Nam, Danko Georgiev, Emilie L. Castranio, Anais Mounier, Iliya Lefterov, and Cody M. Wolfe

Subjects

Male, medicine.medical_specialty, Neurite, Tetrahydronaphthalenes, Cellular differentiation, Neurogenesis, Mice, Transgenic, Biology, Retinoid X receptor, Rats, Sprague-Dawley, Mice, Pregnancy, Internal medicine, medicine, Animals, Humans, Cells, Cultured, Bexarotene, General Neuroscience, Dentate gyrus, Neuron projection, Cell Differentiation, Articles, Dendrites, Cell biology, Rats, Mice, Inbred C57BL, Endocrinology, Retinoid X Receptors, Cistrome, lipids (amino acids, peptides, and proteins), Female, medicine.drug

Abstract

Bexarotene-activated retinoid X receptors (RXRs) ameliorate memory deficits in Alzheimer9s disease mouse models, including mice expressing human apolipoprotein E (APOE) isoforms. The goal of this study was to gain further insight into molecular mechanisms whereby ligand-activated RXR can affect or restore cognitive functions. We used an unbiased approach to discover genome-wide changes in RXR cistrome (ChIP-Seq) and gene expression profile (RNA-Seq) in response to bexarotene in the cortex of APOE4 mice. Functional categories enriched in both datasets revealed that bexarotene-liganded RXR affected signaling pathways associated with neurogenesis and neuron projection development. To further validate the significance of RXR for these functions, we used mouse embryonic stem (ES) cells, primary neurons, and APOE3 and APOE4 mice treated with bexarotene. In vitro data from ES cells confirmed that bexarotene-activated RXR affected neuronal development at different levels, including proliferation of neural progenitors and neuronal differentiation, and stimulated neurite outgrowth. This effect was validated in vivo by demonstrating an increased number of neuronal progenitors after bexarotene treatment in the dentate gyrus of APOE3 and APOE4 mice. In primary neurons, bexarotene enhanced the dendritic complexity characterized by increased branching, intersections, and bifurcations. This effect was confirmed by in vivo studies demonstrating that bexarotene significantly improved the compromised dendritic structure in the hippocampus of APOE4 mice. We conclude that bexarotene-activated RXRs promote genetic programs involved in the neurogenesis and development of neuronal projections and these results have significance for the improvement of cognitive deficits. SIGNIFICANCE STATEMENT Bexarotene-activated retinoid X receptors (RXRs) ameliorate memory deficits in Alzheimer9s disease mouse models, including mice expressing human apolipoprotein E (APOE) isoforms. The goal of this study was to gain further insight into molecular mechanisms whereby ligand-activated RXR can affect or restore cognitive functions. We used an unbiased approach to discover genome-wide changes in RXR cistrome (ChIP-Seq) and gene expression profile (RNA-Seq) in response to bexarotene in the cortex of APOE4 mice. Functional categories enriched in both datasets revealed that liganded RXR affected signaling pathways associated with neurogenesis and neuron projection development. The significance of RXR for these functions was validated in mouse embryonic stem cells, primary neurons, and APOE3 and APOE4 mice treated with bexarotene.

Published

2015

15. P1‐074: EFFECTS OF APOLIPOPROTEIN E ON COGNITIVE PERFORMANCE AND AMYLOID OLIGOMERIZATION IN A MOUSE MODEL

Author

Emilie L. Castranio, Nicholas F. Fitz, Alexis Y. Carter, Radosveta Koldamova, and Iliya Lefterov

Subjects

Apolipoprotein E, Psychiatry and Mental health, Cellular and Molecular Neuroscience, Developmental Neuroscience, Amyloid, Epidemiology, Chemistry, Health Policy, Neurology (clinical), Effects of sleep deprivation on cognitive performance, Geriatrics and Gerontology, Neuroscience

Published

2014