Your search keyword '"John D. Fryer"' showing total 57 results

1. Urine levels of the polyglutamine ataxin-3 protein are elevated in patients with spinocerebellar ataxia type 3

Author

Rina Hashimoto, Jay A. van Gerpen, Yari Carlomagno, Mark S. LeDoux, Ronald F. Pfeiffer, Joseph H. Friedman, Yuka Koike, Samuel S. Giles, Ashley B. Pena, Leonard Petrucelli, Karen Jansen-West, Jaimin S. Shah, Josephine F. Huang, Philip W. Tipton, Jacek Zaremba, Venka Veerappan, Zbigniew K. Wszolek, John D. Fryer, Ikuko Aiba, Klaas J. Wierenga, Judith A. Dunmore, Jan O. Aasly, Ryan J. Uitti, Yuping Song, Rana Hanna Al-Shaikh, and Mercedes Prudencio

Subjects

Adult, Male, congenital, hereditary, and neonatal diseases and abnormalities, medicine.medical_specialty, Ataxia, Urine, Article, Cerebrospinal fluid, Internal medicine, medicine, Humans, Ataxin-3 (ATXN3), Ataxin-3, medicine.diagnostic_test, business.industry, Spinocerebellar ataxia type 3 (SCA3)/machado-josephs disease (MJD), Machado-Joseph Disease, Biomarker, medicine.disease, Urine levels, Repressor Proteins, Endocrinology, Neurology, Case-Control Studies, Polyglutamine (PolyQ), Ataxin, Immunoassay, Spinocerebellar ataxia, Biomarker (medicine), Female, Neurology (clinical), Geriatrics and Gerontology, medicine.symptom, Peptides, business

Abstract

Introduction Accumulation of polyglutamine (polyQ) ataxin-3 (ATXN3) contributes to the pathobiology of spinocerebellar ataxia type 3 (SCA3). Recently, we showed that polyQ ATXN3 is elevated in the plasma and cerebrospinal fluid (CSF) of SCA3 patients, and has the potential to serve as a biological marker for this disease [1]. Based on these findings, we investigated whether polyQ ATXN3 can also be detected in urine samples from SCA3 patients. Methods We analyzed urine samples from 30 SCA3 subjects (including one pre-symptomatic subject), 35 subjects with other forms of ataxia, and 37 healthy controls. To quantify polyQ ATXN3 protein levels, we used our previously developed immunoassay. Results PolyQ ATXN3 can be detected in the urine of SCA3 patients, but not in urine samples from healthy controls or other forms of ataxia. There was a significant statistical association between polyQ ATXN3 levels in urine samples and those in plasma. Further, the levels of polyQ ATXN3 urine associated with an earlier age of SCA3 disease onset. Conclusion As clinical trials for SCA3 advance, urine polyQ ATXN3 protein has potential to be a useful, non-invasive and inexpensive biomarker for SCA3.

Published

2021

2. Long-read targeted sequencing uncovers clinicopathological associations for C9orf72-linked diseases

Author

Leonard Petrucelli, Keith A. Josephs, Tania F. Gendron, Bjorn Oskarsson, Ronald C. Petersen, John D. Fryer, Neill R. Graff-Radford, David S. Knopman, Mark T. W. Ebbert, Eric D. Wieben, Ian J. McLaughlin, Ross A. Aleff, Jazmyne L. Jackson, Rosa Rademakers, Bradley F. Boeve, Marka van Blitterswijk, Nicole A. Finch, Dennis W. Dickson, Mariely DeJesus-Hernandez, Matt Baker, John Harting, and Melissa E. Murray

Subjects

Male, 0301 basic medicine, amyotrophic lateral sclerosis, Biology, 03 medical and health sciences, 0302 clinical medicine, C9orf72, Cerebellum, Report, medicine, Humans, Survival advantage, Amyotrophic lateral sclerosis, Aged, Southern blot, Genetics, DNA Repeat Expansion, C9orf72 Protein, AcademicSubjects/SCI01870, Intron, Neurodegenerative Diseases, Sequence Analysis, DNA, Frontotemporal lobar degeneration, Middle Aged, medicine.disease, Cross-Sectional Studies, 030104 developmental biology, frontotemporal lobar degeneration, long-read sequencing, motor neuron disease, Female, AcademicSubjects/MED00310, Neurology (clinical), Trinucleotide repeat expansion, 030217 neurology & neurosurgery, GC-content

Abstract

To examine the length of a hexanucleotide expansion in C9orf72, which represents the most frequent genetic cause of frontotemporal lobar degeneration and motor neuron disease, we employed a targeted amplification-free long-read sequencing technology: No-Amp sequencing. In our cross-sectional study, we assessed cerebellar tissue from 28 well-characterized C9orf72 expansion carriers. We obtained 3507 on-target circular consensus sequencing reads, of which 814 bridged the C9orf72 repeat expansion (23%). Importantly, we observed a significant correlation between expansion sizes obtained using No-Amp sequencing and Southern blotting (P = 5.0 × 10−4). Interestingly, we also detected a significant survival advantage for individuals with smaller expansions (P = 0.004). Additionally, we uncovered that smaller expansions were significantly associated with higher levels of C9orf72 transcripts containing intron 1b (P = 0.003), poly(GP) proteins (P = 1.3 × 10− 5), and poly(GA) proteins (P = 0.005). Thorough examination of the composition of the expansion revealed that its GC content was extremely high (median: 100%) and that it was mainly composed of GGGGCC repeats (median: 96%), suggesting that expanded C9orf72 repeats are quite pure. Taken together, our findings demonstrate that No-Amp sequencing is a powerful tool that enables the discovery of relevant clinicopathological associations, highlighting the important role played by the cerebellar size of the expanded repeat in C9orf72-linked diseases., DeJesus-Hernandez et al. employ an innovative long-read sequencing method to examine the length of the expanded C9orf72 repeat that represents the most common genetic cause of frontotemporal dementia and amyotrophic lateral sclerosis. Smaller expansion size confers a survival benefit for patients.

Published

2021

3. TREM2-H157Y Increases Soluble TREM2 Production and Reduces Amyloid Pathology

Author

Wenhui Qiao, Kurti I. Aishe, Na Zhao, Francis Shue, Chia Chen Liu, Yuka A. Martens, John D. Fryer, Yixing Chen, Fuyao Li, Maxwell V. Dacquel, Kai Chen, Joshua Knight, and Guojun Bu

Subjects

Mutation, Chemistry, TREM2, Synaptic plasticity, Neurodegeneration, Mutant, medicine, Wild type, Tauopathy, Microgliosis, medicine.disease_cause, medicine.disease, Cell biology

Abstract

Background: The p.H157Y variant of TREM2 (Triggering Receptor Expressed on Myeloid Cells 2) has been reported to increase Alzheimer’s disease (AD) risk. This mutation in the extracellular domain of TREM2 localizes at the cleavage site and was shown to enhance shedding and impair phagocytosis in vitro by ectopic expression of TREM2-H157Y in HEK293 cells. However, the physiological and AD-related outcomes of TREM2 H157Y mutation in vivo remain unknown.Methods: We generated a novel Trem2 H157Y knock-in mouse model through CRISPR-Cas9 technology and investigated how Trem2 H157Y mutation impacts TREM2 proteolytic processing, synaptic function, and AD-related amyloid pathology by conducting biochemical assays, immunofluorescent staining, hippocampal electrophysiology, and in vivo micro-dialysis in awake, free-moving animals.Results: Consistent with previous in vitro findings, TREM2-H157Y increases the amount of soluble TREM2 (sTREM2) in the cortex and serum of mutant mice compared to the wild type controls. Interestingly, the Trem2 H157Y variant enhances synaptic plasticity without affecting microglial density and morphology. In the presence of amyloid pathology, TREM2-H157Y surprisingly accelerates Aβ clearance and reduces amyloid burden and microgliosis. Conclusion: Taken together, our findings support a beneficial effect of the Trem2 H157Y mutation in synaptic function and in mitigating amyloid pathology. Considering the genetic association of TREM2 p.H157Y with AD, we speculate TREM2-H157Y might increase AD risk through an amyloid-independent pathway, as such its effects on tauopathy and neurodegeneration merit further investigation.

Published

2021

4. APOE3 -Jacksonville (V236E) variant reduces self-aggregation and risk of dementia

Author

Hu Wang, Bradley F. Boeve, Michael G. Heckman, Yingxue Ren, Yan W. Asmann, Ana-Caroline Raulin, Yuan Fu, Thomas R. Caulfield, Tadafumi C. Ikezu, Tanis J. Ferman, Cynthia Linares, Lin Jia, Dennis W. Dickson, Carl Frieden, Jing Zhao, Owen A. Ross, Steven G. Younkin, Zbigniew K. Wszolek, Val J. Lowe, Cassandra L. Rosenberg, David S. Knopman, Xia Li, Yonghe Li, John D. Fryer, Xue Wang, Sydney V. Doss, Melissa E. Murray, Wenyan Lu, Clifford R. Jack, Melissa C. Wren, Xianlin Han, Joshua Knight, Zachary A. Trottier, Na Wang, Yuka A. Martens, Joseph E. Parisi, Yixing Chen, Guojun Bu, Aishe Kurti, Neill R. Graff-Radford, Kejal Kantarci, Chia Chen Liu, Glenn E. Smith, Ronald C. Petersen, Prashanthi Vemuri, Na Zhao, and Francis Shue

Subjects

Apolipoprotein E, business.industry, Self aggregation, Extramural, Genetic variants, General Medicine, Disease, medicine.disease, Bioinformatics, Apolipoproteins E, Text mining, Medicine, Dementia, business

Abstract

A rare APOE variant APOE3 -Jac reduces self-aggregation and promotes healthy brain aging.

Published

2021

5. Enhanced phosphorylation of T153 in soluble tau is a defining biochemical feature of the A152T tau risk variant

Author

Lillian M. Daughrity, John D. Fryer, Monica Castanedes-Casey, Nicole M. Avendano, Virginia Phillips, Casey Cook, Aishe Kurti, Rosa Rademakers, Leonard Petrucelli, Dah Eun Chloe Chung, Jimei Tong, Karen Jansen-West, Dennis W. Dickson, Michael DeTure, Kelly M. Hinkle, Yari Carlomagno, and Mei Yue

Subjects

0301 basic medicine, Male, Somatic cell, A152T, Mice, Transgenic, tau Proteins, Neuropathology, Biology, lcsh:RC346-429, Pathology and Forensic Medicine, Progressive supranuclear palsy, 03 medical and health sciences, Cellular and Molecular Neuroscience, 0302 clinical medicine, In vivo, mental disorders, medicine, Corticobasal degeneration, Animals, Humans, Genetic Predisposition to Disease, Gliosis, Phosphorylation, lcsh:Neurology. Diseases of the nervous system, Aged, Aged, 80 and over, Neurons, Dementia with Lewy bodies, Research, Brain, Neurodegenerative Diseases, Middle Aged, medicine.disease, 3. Good health, Cell biology, Disease Models, Animal, Tauopathy, 030104 developmental biology, Solubility, Female, Neurology (clinical), Human medicine, Risk factor, 030217 neurology & neurosurgery

Abstract

Pathogenic mutations in the tau gene (microtubule associated protein tau, MAPT) are linked to the onset of tauopathy, but the A152T variant is unique in acting as a risk factor for a range of disorders including Alzheimer’s disease (AD), progressive supranuclear palsy (PSP), corticobasal degeneration (CBD), and dementia with Lewy bodies (DLB). In order to provide insight into the mechanism by which A152T modulates disease risk, we developed a novel mouse model utilizing somatic brain transgenesis with adeno-associated virus (AAV) to drive tau expression in vivo, and validated the model by confirming the distinct biochemical features of A152T tau in postmortem brain tissue from human carriers. Specifically, TauA152T-AAV mice exhibited increased tau phosphorylation that unlike animals expressing the pathogenic P301L mutation remained localized to the soluble fraction. To investigate the possibility that the A152T variant might alter the phosphorylation state of tau on T152 or the neighboring T153 residue, we generated a novel antibody that revealed significant accumulation of soluble tau species that were hyperphosphorylated on T153 (pT153) in TauA152T-AAV mice, which were absent the soluble fraction of TauP301L-AAV mice. Providing new insight into the role of A152T in modifying risk of tauopathy, as well as validating the TauA152T-AAV model, we demonstrate that the presence of soluble pT153-positive tau species in human postmortem brain tissue differentiates A152T carriers from noncarriers, independent of disease classification. These results implicate both phosphorylation of T153 and an altered solubility profile in the mechanism by which A152T modulates disease risk. Electronic supplementary material The online version of this article (10.1186/s40478-019-0661-2) contains supplementary material, which is available to authorized users.

Published

2019

6. Toward allele-specific targeting therapy and pharmacodynamic marker for spinocerebellar ataxia type 3

Author

Yari Carlomagno, Paola Giunti, Yuping Song, Bjorn Oskarsson, Jan O. Aasly, Rana Hanna Al-Shaikh, Robin Labrum, Zbigniew K. Wszolek, James M. Polke, João Lemos, Henry L. Paulson, Guojun Bu, Eric R. Eggenberger, Karen Jansen-West, William D. Freeman, Hector Garcia-Moreno, Mercedes Prudencio, Marka van Blitterswijk, Osamu Onodera, Joseph H. Friedman, Ryan J. Uitti, Inês Gomes, Hayley S. McLoughlin, Mark S. LeDoux, Takuya Konno, Venka Veerappan, Nathan P. Staff, Leonard Petrucelli, John N. Caviness, Cristina Januário, Tania F. Gendron, Lillian M. Daughrity, Mari Tada, Iris Vanessa Marin Collazo, Andreas Puschmann, Takeshi Ikeuchi, Katharine Nicholson, Josephine F. Huang, Klaas J. Wierenga, Sorina Gorcenco, Christin Karremo, Matthew R. Spiegel, Akiyoshi Kakita, Jay A. van Gerpen, Judith A. Dunmore, Ronald F. Pfeiffer, Philip W. Tipton, John D. Fryer, Mark R. Pittelkow, Vikram G. Shakkottai, Natalie Byron, and Michael G. Heckman

Subjects

Neurons, congenital, hereditary, and neonatal diseases and abnormalities, medicine.medical_specialty, Neurology, business.industry, Mutant, Machado-Joseph Disease, General Medicine, medicine.disease, Bioinformatics, Article, Repressor Proteins, Clinical trial, Polymorphism (computer science), Spinocerebellar ataxia, medicine, Humans, Allele, Ataxin-3, business, Trinucleotide repeat expansion, Gene, Alleles

Abstract

Spinocerebellar ataxia type 3 (SCA3), caused by a CAG repeat expansion in the ataxin-3 gene (ATXN3), is characterized by neuronal polyglutamine (polyQ) ATXN3 protein aggregates. Although there is no cure for SCA3, gene-silencing approaches to reduce toxic polyQ ATXN3 showed promise in preclinical models. However, a major limitation in translating putative treatments for this rare disease to the clinic is the lack of pharmacodynamic markers for use in clinical trials. Here, we developed an immunoassay that readily detects polyQ ATXN3 proteins in human biological fluids and discriminates patients with SCA3 from healthy controls and individuals with other ataxias. We show that polyQ ATXN3 serves as a marker of target engagement in human fibroblasts, which may bode well for its use in clinical trials. Last, we identified a single-nucleotide polymorphism that strongly associates with the expanded allele, thus providing an exciting drug target to abrogate detrimental events initiated by mutant ATXN3. Gene-silencing strategies for several repeat diseases are well under way, and our results are expected to improve clinical trial preparedness for SCA3 therapies.

Published

2020

7. Astrocyte-derived clusterin suppresses amyloid formation in vivo

Author

Aleksandra Wojtas, Karen Jansen-West, John D. Fryer, Dennis W. Dickson, Kelsey E. Baker, Aishe Kurti, Leonard Petrucelli, Silvia S. Kang, Jonathon P. Sens, Taylor J. Berry, Guojun Bu, Lillian M. Daughrity, and Chia Chen Liu

Subjects

0301 basic medicine, Amyloid, Hippocampus, Mice, Transgenic, Plaque, Amyloid, Amyloid plaques, Haploinsufficiency, lcsh:Geriatrics, Biology, Adeno-associated viral vectors, lcsh:RC346-429, 03 medical and health sciences, Cellular and Molecular Neuroscience, 0302 clinical medicine, Downregulation and upregulation, Alzheimer Disease, mental disorders, medicine, Animals, Molecular Biology, lcsh:Neurology. Diseases of the nervous system, Aβ, Amyloid beta-Peptides, Clusterin, Amyloidosis, Neurotoxicity, medicine.disease, lcsh:RC952-954.6, Disease Models, Animal, 030104 developmental biology, medicine.anatomical_structure, Gliosis, Astrocytes, Cancer research, biology.protein, Neurology (clinical), medicine.symptom, Alzheimer’s disease, 030217 neurology & neurosurgery, Astrocyte, Research Article

Abstract

Background Accumulation of amyloid-β (Aβ) peptide in the brain is a pathological hallmark of Alzheimer’s disease (AD). The clusterin (CLU) gene confers a risk for AD and CLU is highly upregulated in AD patients, with the common non-coding, protective CLU variants associated with increased expression. Although there is strong evidence implicating CLU in amyloid metabolism, the exact mechanism underlying the CLU involvement in AD is not fully understood or whether physiologic alterations of CLU levels in the brain would be protective. Results We used a gene delivery approach to overexpress CLU in astrocytes, the major source of CLU expression in the brain. We found that CLU overexpression resulted in a significant reduction of total and fibrillar amyloid in both cortex and hippocampus in the APP/PS1 mouse model of AD amyloidosis. CLU overexpression also ameliorated amyloid-associated neurotoxicity and gliosis. To complement these overexpression studies, we also analyzed the effects of haploinsufficiency of Clu using heterozygous (Clu+/−) mice and control littermates in the APP/PS1 model. CLU reduction led to a substantial increase in the amyloid plaque load in both cortex and hippocampus in APP/PS1; Clu+/− mice compared to wild-type (APP/PS1; Clu+/+) littermate controls, with a concomitant increase in neuritic dystrophy and gliosis. Conclusions Thus, both physiologic ~ 30% overexpression or ~ 50% reduction in CLU have substantial impacts on amyloid load and associated pathologies. Our results demonstrate that CLU plays a major role in Aβ accumulation in the brain and suggest that efforts aimed at CLU upregulation via pharmacological or gene delivery approaches offer a promising therapeutic strategy to regulate amyloid pathology.

Published

2020

8. Loss of Tmem106b exacerbates <scp>FTLD</scp> pathologies and causes motor deficits in progranulin‐deficient mice

Author

Virginia Phillips, Rosa Rademakers, Aamir Zuberi, Matt Baker, John D. Fryer, Mieu Brooks, Dennis W. Dickson, Xiaolai Zhou, Ariston L. Librero, Guojun Bu, Cathleen M. Lutz, Shunsuke Koga, Tammee M. Parsons, Monica Castanedes-Casey, Aishe Kurti, and Peizhou Jiang

Subjects

Nerve Tissue Proteins, Microgliosis, Biochemistry, Mice, 03 medical and health sciences, Progranulins, 0302 clinical medicine, Ubiquitin, mental disorders, Genetics, Paralysis, medicine, Animals, Biology, Molecular Biology, 030304 developmental biology, Mice, Knockout, 0303 health sciences, biology, business.industry, Autophagy, Membrane Proteins, Frontotemporal lobar degeneration, Motor neuron, Spinal cord, medicine.disease, nervous system diseases, Astrogliosis, Chemistry, medicine.anatomical_structure, Frontotemporal Dementia, Mutation, Cancer research, biology.protein, Intercellular Signaling Peptides and Proteins, Human medicine, Frontotemporal Lobar Degeneration, medicine.symptom, business, 030217 neurology & neurosurgery, Reports

Abstract

Progranulin (PGRN) and transmembrane protein 106B (TMEM106B) are important lysosomal proteins implicated in frontotemporal lobar degeneration (FTLD) and other neurodegenerative disorders. Loss‐of‐function mutations in progranulin (GRN) are a common cause of FTLD, while TMEM106B variants have been shown to act as disease modifiers in FTLD. Overexpression of TMEM106B leads to lysosomal dysfunction, while loss of Tmem106b ameliorates lysosomal and FTLD‐related pathologies in young Grn (−/−) mice, suggesting that lowering TMEM106B might be an attractive strategy for therapeutic treatment of FTLD‐GRN. Here, we generate and characterize older Tmem106b (−/−) Grn (−/−) double knockout mice, which unexpectedly show severe motor deficits and spinal cord motor neuron and myelin loss, leading to paralysis and premature death at 11–12 months. Compared to Grn (−/−), Tmem106b (−/−) Grn (−/−) mice have exacerbated FTLD‐related pathologies, including microgliosis, astrogliosis, ubiquitin, and phospho‐Tdp43 inclusions, as well as worsening of lysosomal and autophagic deficits. Our findings confirm a functional interaction between Tmem106b and Pgrn and underscore the need to rethink whether modulating TMEM106B levels is a viable therapeutic strategy.

Published

2020

9. Risk Factors for Persistent Cognitive Impairment After Critical Illness, Nested Case-Control Study

Author

John D. Fryer, Ognjen Gajic, Gregory A. Wilson, Alejandro A. Rabinstein, Amra Sakusic, Ronald C. Petersen, Gregory D. Jenkins, Rahul Kashyap, John C. O’Horo, and Tarun D. Singh

Subjects

medicine.medical_specialty, Critical Illness, MEDLINE, Comorbidity, Critical Care and Intensive Care Medicine, Severity of Illness Index, law.invention, 03 medical and health sciences, 0302 clinical medicine, Risk Factors, law, Severity of illness, Epidemiology, Health care, medicine, Humans, Cognitive Dysfunction, Intensive care medicine, business.industry, Age Factors, 030208 emergency & critical care medicine, Length of Stay, medicine.disease, Intensive care unit, Intensive Care Units, Socioeconomic Factors, Case-Control Studies, Nested case-control study, Observational study, business, 030217 neurology & neurosurgery

Abstract

Persistent cognitive impairment after critical illness is an important healthcare problem forecasted to worsen in the near future. However, the epidemiology is insufficiently explored. We aimed to determine potentially modifiable risk factors during ICU hospitalization that play a significant role in developing persistent cognitive impairment.An observational case-control study.Mayo Clinic ICUs between July 1, 2004, and November 20, 2015.We conducted a study nested in a large cohort of 98,227 adult critically ill patients. Using previously validated computable phenotypes for dementia and cognitive impairment, we determined the onset of cognitive impairment relative to ICU hospitalization and associated risk factors. The primary endpoint of the study was new and persistent cognitive impairment documented between 3 and 24 months after ICU discharge.Unadjusted and adjusted analyses were performed to identify potentially modifiable risk factors during ICU hospitalization.Among 21,923 unique patients identified as cognitively impaired (22% of the entire ICU cohort), 2,428 (2.5%) developed incident new and persistent cognitive dysfunction after the index ICU admission. Compared with age- and sex-matched ICU controls (2,401 pairs), cases had higher chronic illness burden (Charlson Comorbidity Index, 6.2 vs 5.1; p0.01), and were more likely to have multiple ICU stays (22% vs 14%; p0.01). After adjustment for baseline differences, new and persistent cognitive dysfunction was associated with higher frequency of acute brain failure in the ICU, a higher exposure to severe hypotension, hypoxemia, hyperthermia, fluctuations in serum glucose, and treatment with quinolones or vancomycin. Association with sepsis observed in univariate analysis did not persist after adjustment.Cognitive dysfunction is highly prevalent in ICU patients. Incident new and persistent cognitive impairment is less common but important, potentially preventable problem after critical illness. Chronic comorbidities and number of ICU stays increase the risk of post-ICU cognitive dysfunction irrespective of age. Modifiable ICU exposures were identified as potential targets for future prevention trials.

Published

2018

10. Microglial translational profiling reveals a convergent APOE pathway from aging, amyloid, and tau

Author

Leonard Petrucelli, Xuewei Wang, John D. Fryer, Jonathon P. Sens, Kelsey E. Baker, Silvia S. Kang, Jeanne Pierre Kocher, Mark T. W. Ebbert, and Casey Cook

Subjects

0301 basic medicine, Apolipoprotein E, Male, Aging, Amyloid, Immunology, Mice, Transgenic, tau Proteins, Disease, Biology, Transcriptome, 03 medical and health sciences, Mice, Apolipoproteins E, Alzheimer Disease, medicine, Immunology and Allergy, Animals, Chemokine CCL4, Research Articles, Chemokine CCL3, Innate immune system, Microglia, Amyloidosis, Brief Definitive Report, Cell sorting, medicine.disease, Disease Models, Animal, 030104 developmental biology, medicine.anatomical_structure, Female, Tauopathy, Neuroscience, Signal Transduction

Abstract

Microglia are central players in homeostasis and disease. Kang et al. reveal a novel ApoE-driven microglial pathway shared between aging, amyloidosis, and tauopathy that is exacerbated in females, suggesting a convergent mechanism for altering microglial reactivity during Alzheimer’s disease., Alzheimer’s disease (AD) is an age-associated neurodegenerative disease characterized by amyloidosis, tauopathy, and activation of microglia, the brain resident innate immune cells. We show that a RiboTag translational profiling approach can bypass biases due to cellular enrichment/cell sorting. Using this approach in models of amyloidosis, tauopathy, and aging, we revealed a common set of alterations and identified a central APOE-driven network that converged on CCL3 and CCL4 across all conditions. Notably, aged females demonstrated a significant exacerbation of many of these shared transcripts in this APOE network, revealing a potential mechanism for increased AD susceptibility in females. This study has broad implications for microglial transcriptomic approaches and provides new insights into microglial pathways associated with different pathological aspects of aging and AD.

Published

2018

11. Derivation and validation of the automated search algorithms to identify cognitive impairment and dementia in electronic health records

Author

Gregory A. Wilson, Alejandro A. Rabinstein, John C. O’Horo, Ognjen Gajic, John D. Fryer, Rosebud O. Roberts, Rahul Kashyap, Tarun D. Singh, Ronald C. Petersen, and Sakusic Amra

Subjects

Gerontology, medicine.medical_specialty, Critical Illness, Big data, Critical Care and Intensive Care Medicine, law.invention, Automation, 03 medical and health sciences, 0302 clinical medicine, International Classification of Diseases, law, Search algorithm, medicine, Electronic Health Records, Humans, Dementia, Cognitive Dysfunction, Medical physics, 030212 general & internal medicine, Cognitive decline, Cognitive evaluation theory, business.industry, Medical record, medicine.disease, Intensive care unit, Cognitive test, Intensive Care Units, business, Algorithms, 030217 neurology & neurosurgery

Abstract

Purpose Long-term cognitive impairment is a common and important problem in survivors of critical illness. We developed electronic search algorithms to identify cognitive impairment and dementia from the electronic medical records (EMRs) that provide opportunity for big data analysis. Materials and methods Eligible patients met 2 criteria. First, they had a formal cognitive evaluation by The Mayo Clinic Study of Aging. Second, they were hospitalized in intensive care unit at our institution between 2006 and 2014. The “criterion standard” for diagnosis was formal cognitive evaluation supplemented by input from an expert neurologist. Using all available EMR data, we developed and improved our algorithms in the derivation cohort and validated them in the independent validation cohort. Results Of 993 participants who underwent formal cognitive testing and were hospitalized in intensive care unit, we selected 151 participants at random to form the derivation and validation cohorts. The automated electronic search algorithm for cognitive impairment was 94.3% sensitive and 93.0% specific. The search algorithms for dementia achieved respective sensitivity and specificity of 97% and 99%. EMR search algorithms significantly outperformed International Classification of Diseases codes. Conclusions Automated EMR data extractions for cognitive impairment and dementia are reliable and accurate and can serve as acceptable and efficient alternatives to time-consuming manual data review.

Published

2017

12. Hexanucleotide Repeat Expansions in c9FTD/ALS and SCA36 Confer Selective Patterns of Neurodegeneration In Vivo

Author

Tiffany W. Todd, Yuping Song, Wilfried Rossoll, Susana Teijeira Bautista, María Jesús Sobrido, Yong Jie Zhang, Monica Castanedes-Casey, Gary J. Bassell, Alexander R. Burch, Matthew D. Disney, Karen Jansen-West, Beatriz San Millán, Jimei Tong, Manuel Arias, Jeannie Chew, John D. Fryer, Judith Dunmore, Leonard Petrucelli, Mei Yue, Tania F. Gendron, Aishe Kurti, Zachary T. McEachin, and Dennis W. Dickson

Subjects

0301 basic medicine, Biology, General Biochemistry, Genetics and Molecular Biology, Article, 03 medical and health sciences, Mice, 0302 clinical medicine, Stress granule, C9orf72, RAN translation, medicine, Animals, Humans, Amyotrophic lateral sclerosis, poly(GP), lcsh:QH301-705.5, Genetics, Inclusion Bodies, Neurons, DNA Repeat Expansion, C9orf72 Protein, Neurodegeneration, Amyotrophic Lateral Sclerosis, Intron, RNA, Nuclear Proteins, FTD, medicine.disease, 030104 developmental biology, lcsh:Biology (General), SCA36, Frontotemporal Dementia, Spinocerebellar ataxia, ALS, Trinucleotide repeat expansion, 030217 neurology & neurosurgery

Abstract

A G(4)C(2) hexanucleotide repeat expansion in an intron of C9orf72 is the most common cause of frontal temporal dementia and amyotrophic lateral sclerosis (c9FTD/ALS). A remarkably similar intronic TG(3)C(2) repeat expansion is associated with spinocerebellar ataxia 36 (SCA36). Both expansions are widely expressed, form RNA foci, and can undergo repeat-associated non-ATG (RAN) translation to form similar dipeptide repeat proteins (DPRs). Yet, these diseases result in the degeneration of distinct subsets of neurons. We show that the expression of these repeat expansions in mice is sufficient to recapitulate the unique features of each disease, including this selective neuronal vulnerability. Furthermore, only the G(4)C(2) repeat induces the formation of aberrant stress granules and pTDP-43 inclusions. Overall, our results demonstrate that the pathomechanisms responsible for each disease are intrinsic to the individual repeat sequence, highlighting the importance of sequence-specific RNA-mediated toxicity in each disorder.

Published

2019

13. APOE4 exacerbates α-synuclein pathology and related toxicity independent of amyloid

Author

Mary D. Davis, Chia Chen Liu, Joshua Knight, Aishe Kurti, Fuyao Li, Guojun Bu, Cynthia Linares, Wenhui Qiao, John D. Fryer, Olivia N. Attrebi, Yingxue Ren, Marion Delenclos, Jiaying Zheng, Yan W. Asmann, Dennis W. Dickson, Pamela J. McLean, Owen A. Ross, Na Zhao, Francis Shue, Axel D. Meneses, Berkiye Sonustun, Yuka A. Martens, Yixing Chen, and Alexandra J. Van Ingelgom

Subjects

Apolipoprotein E, Lewy Body Disease, Pathology, medicine.medical_specialty, Synucleinopathies, Mice, Knockout, ApoE, Apolipoprotein E4, Disease, Article, Transcriptome, Mice, mental disorders, medicine, Dementia, Animals, Allele, Amyloid beta-Peptides, Lewy body, business.industry, Dementia with Lewy bodies, General Medicine, medicine.disease, Astrogliosis, nervous system diseases, alpha-Synuclein, lipids (amino acids, peptides, and proteins), business, human activities

Abstract

The apolipoprotein E (APOE) ε4 allele is the strongest genetic risk factor for late-onset Alzheimer’s disease mainly by driving amyloid-β pathology. Recently, APOE4 has also been found to be a genetic risk factor for Lewy body dementia (LBD), which includes dementia with Lewy bodies (DLB) and Parkinson’s disease dementia (PDD). How APOE4 drives risk of LBD and whether it has a direct effect on α-synuclein pathology is not clear. Here we generated a mouse model of synucleinopathy using an adeno-associated virus (AAV) gene delivery of α-synuclein in human APOE-targeted replacement mice expressing APOE2, APOE3 or APOEE4. We found that APOE4, but not APOE2 or APOE3, increased α-synuclein pathology, impaired behavioral performances, worsened neuronal and synaptic loss, and increased astrogliosis at nine months of age. Transcriptomic profiling in APOE4-expressing α-synuclein mice highlighted altered lipid and energy metabolism, and synapse-related pathways. We also observed an effect of APOE4 on α-synuclein pathology in human postmortem brains with LBD and minimal amyloid pathology. Our data demonstrates a pathogenic role of APOE4 in exacerbating α-synuclein pathology independent of amyloid, providing mechanistic insights into how APOE4 increases the risk of LBD.

Published

2019

14. Identification of plexin A4 as a novel clusterin receptor links two Alzheimer’s disease risk genes

Author

Aleksandra Wojtas, Guojun Bu, John D. Fryer, Carlos Cruchaga, Chia Chen Liu, Aishe Kurti, Yuetiva Deming, Takahisa Kanekiyo, Steven Estus, Kelsey E. Baker, and Silvia S. Kang

Subjects

0301 basic medicine, Elevated plus maze, medicine.medical_specialty, Genotype, Receptors, Cell Surface, Biology, Polymorphism, Single Nucleotide, Pathogenesis, Mice, 03 medical and health sciences, Cognition, 0302 clinical medicine, Alzheimer Disease, Memory, Risk Factors, Internal medicine, Genetics, medicine, Animals, Humans, Genetic Predisposition to Disease, Protein Interaction Maps, Receptor, Molecular Biology, Genetics (clinical), Mice, Knockout, Regulation of gene expression, Clusterin, Plexin, Articles, General Medicine, medicine.disease, Phenotype, 030104 developmental biology, Endocrinology, Gene Expression Regulation, biology.protein, Alzheimer's disease, 030217 neurology & neurosurgery

Abstract

Although abundant genetic and biochemical evidence strongly links Clusterin (CLU) to Alzheimer disease (AD) pathogenesis, the receptor for CLU within the adult brain is currently unknown. Using unbiased approaches, we identified Plexin A4 (PLXNA4) as a novel, high-affinity receptor for CLU in the adult brain. PLXNA4 protein expression was high in brain with much lower levels in peripheral organs. CLU protein levels were significantly elevated in the cerebrospinal fluid (CSF) of Plxna4-/- mice and, in humans, CSF levels of CLU were also associated with PLXNA4 genotype. Human AD brains had significantly increased the levels of CLU protein but decreased levels of PLXNA4 by ∼50%. To determine whether PLXNA4 levels influenced cognition, we analyzed the behaviour of Plxna4+/+, Plxna4+/-, and Plxna4-/- mice. In comparison to WT controls, both Plxna4+/- and Plxna4-/- mice were hyperactive in the open field assay while Plxna4-/- mice displayed a hyper-exploratory (low-anxiety phenotype) in the elevated plus maze. Importantly, both Plxna4+/- and Plxna4-/- mice displayed prominent deficits in learning and memory in the contextual fear-conditioning paradigm. Thus, even a 50% reduction in the level of PLXNA4 is sufficient to cause memory impairments, raising the possibility that memory problems seen in AD patients could be due to reductions in the level of PLXNA4. Both CLU and PLXNA4 have been genetically associated with AD risk and our data thus provide a direct relationship between two AD risk genes. Our data suggest that increasing the levels of PLXNA4 or targeting CLU-PLXNA4 interactions may have therapeutic value in AD.

Published

2016

15. APOE2eases cognitive decline during Aging: Clinical and preclinical evaluations

Author

Duane Linthicum, Xianlin Han, Jessica L. Frisch-Daiello, Yuan Fu, Laura Price, Guojun Bu, John D. Fryer, Mitsuru Shinohara, Takahisa Kanekiyo, Motoko Shinohara, and Longyu Yang

Subjects

0301 basic medicine, Apolipoprotein E, medicine.medical_specialty, Amyloid, business.industry, Hippocampus, Water maze, medicine.disease, 03 medical and health sciences, 030104 developmental biology, 0302 clinical medicine, Endocrinology, Neurology, Internal medicine, medicine, lipids (amino acids, peptides, and proteins), Neurology (clinical), Animal studies, Cognitive decline, Alzheimer's disease, business, 030217 neurology & neurosurgery, Neuroinflammation

Abstract

Objective Apolipoprotein E (apoE), a major cholesterol carrier in the brain, is associated with a strong risk for Alzheimer disease. Compared to the risky APOE4 gene allele, the effects of the protective APOE2 gene allele are vastly understudied, and thus need to be further clarified. Methods We reviewed National Alzheimer's Coordinating Center clinical records and performed preclinical experiments using human apoE-targeted replacement (apoE-TR) mice, which do not show amyloid pathology. Results Clinically, the APOE2 allele was associated with less cognitive decline during aging. This effect was also seen in subjects with little amyloid pathology, or after adjusting for Alzheimer disease-related pathologies. In animal studies, aged apoE2-TR mice also exhibited preserved memory function in water maze tests. Regardless, apoE2-TR mice showed similar or greater age-related changes in synaptic loss, neuroinflammation, and oxidative stress compared to apoE3-TR or apoE4-TR mice. Interestingly, apoE concentrations in the cortex, hippocampus, plasma, and cerebrospinal fluid (CSF) were positively correlated with memory performance across apoE isoforms, where apoE2-TR mice had higher apoE levels. Moreover, apoE2-TR mice exhibited the lowest levels of cholesterol in the cortex, despite higher levels in CSF and plasma. These cholesterol levels were associated with apoE levels and memory performance across apoE isoforms. Interpretation APOE2 is associated with less cognitive decline during aging. This can occur independently of age-related synaptic/neuroinflammatory changes and amyloid accumulation. Higher levels of apoE and associated cholesterol metabolism in APOE2 carriers might contribute to this protective effect. Ann Neurol 2016;79:758–774

Published

2016

16. C9ORF72 poly(GA) aggregates sequester and impair HR23 and nucleocytoplasmic transport proteins

Author

Ya Fei Xu, Jeannie Chew, Jonathan C. Grima, Kevin B. Boylan, Amanda M. Liesinger, Wen Lang Lin, Chad A. Dickey, Guojun Bu, Christopher D. Link, Jennifer Gass, Yong Jie Zhang, Zizhao S. Wang, Aliesha Garrett, Emilie A. Perkerson, Jeremy D. Baker, Hiroki Sasaguri, Jeannette N. Stankowski, Mei Yue, Clotilde Lagier-Tourenne, Rebecca B. Katzman, Leonard Petrucelli, Jie Jiang, John D. Fryer, Tania F. Gendron, Karen Jansen-West, Monica Castanedes-Casey, Lillian M. Daughrity, Jimei Tong, Aishe Kurti, Dieter Edbauer, Dennis W. Dickson, Mitsuru Shinohara, Melissa E. Murray, Jeffrey D. Rothstein, Don W. Cleveland, and Rosa Rademakers

Subjects

0301 basic medicine, metabolism [Inclusion Bodies], Gene Expression, Neurodegenerative, Inclusion bodies, Mice, genetics [Gene Expression], 0302 clinical medicine, pathology [Brain], C9orf72, Gene expression, Psychology, pathology [Neurons], Guanine Nucleotide Exchange Factors, ultrastructure [Inclusion Bodies], Neurons, Inclusion Bodies, C9orf72 protein, mouse, pathology [Atrophy], Behavior, Animal, General Neuroscience, Nucleocytoplasmic Transport Proteins, Neurodegeneration, Brain, pathology [Nerve Degeneration], metabolism [Proteins], Ubiquitinated Proteins, DNA-Binding Proteins, poly(glycyl-alanyl), Xpc protein, mouse, metabolism [Neurons], Frontotemporal Dementia, metabolism [Frontotemporal Dementia], Cognitive Sciences, Rad23a protein, mouse, metabolism [DNA-Binding Proteins], metabolism [Ubiquitinated Proteins], metabolism [Guanine Nucleotide Exchange Factors], Primary Cell Culture, Biology, Rad23b protein, mouse, DNA-binding protein, Article, 03 medical and health sciences, TDP-43 protein, mouse, ddc:570, Acquired Cognitive Impairment, medicine, Animals, Humans, pathology [Amyotrophic Lateral Sclerosis], Behavior, Neurology & Neurosurgery, C9orf72 Protein, toxicity [Proteins], Animal, metabolism [Amyotrophic Lateral Sclerosis], Amyotrophic Lateral Sclerosis, Neurosciences, Proteins, medicine.disease, genetics [Proteins], Brain Disorders, 030104 developmental biology, metabolism [Brain], Nucleocytoplasmic Transport, Nerve Degeneration, pathology [Frontotemporal Dementia], Mutation, ultrastructure [Brain], Dementia, Human medicine, Atrophy, Carrier Proteins, Neuroscience, 030217 neurology & neurosurgery, metabolism [Carrier Proteins]

Abstract

Neuronal inclusions of poly(GA), a protein unconventionally translated from G(4)C(2) repeat expansions in C9ORF72, are abundant in patients with frontotemporal dementia (FTD) and amyotrophic lateral sclerosis (ALS) caused by this mutation. To investigate poly(GA) toxicity, we generated mice that exhibit poly(GA) pathology, neurodegeneration and behavioral abnormalities reminiscent of FTD and ALS. These phenotypes occurred in the absence of TDP-43 pathology and required poly(GA) aggregation. HR23 proteins involved in proteasomal degradation and proteins involved in nucleocytoplasmic transport were sequestered by poly(GA) in these mice. HR23A and HR23B similarly colocalized to poly(GA) inclusions in C9ORF72 expansion carriers. Sequestration was accompanied by an accumulation of ubiquitinated proteins and decreased xeroderma pigmentosum C (XPC) levels in mice, indicative of HR23A and HR23B dysfunction. Restoring HR23B levels attenuated poly(GA) aggregation and rescued poly(GA)-induced toxicity in neuronal cultures. These data demonstrate that sequestration and impairment of nuclear HR23 and nucleocytoplasmic transport proteins is an outcome of, and a contributor to, poly(GA) pathology.

Published

2016

17. Aberrant deposition of stress granule-resident proteins linked to C9orf72-associated TDP-43 proteinopathy

Author

Jeannette N. Stankowski, Tania F. Gendron, Giulia del Rosso, Jeannie Chew, Leonard Petrucelli, Yong Jie Zhang, Matthew D. Disney, Aishe Kurti, Karen Jansen-West, Jeffrey D. Rothstein, Lillian M. Daughrity, Monica Castanedes-Casey, John D. Fryer, Dennis W. Dickson, and Casey Cook

Subjects

0301 basic medicine, TDP-43, Biology, lcsh:Geriatrics, lcsh:RC346-429, 03 medical and health sciences, Cellular and Molecular Neuroscience, Mice, 0302 clinical medicine, Stress granule, C9orf72, Sense (molecular biology), medicine, Animals, Neurodegeneration, Molecular Biology, lcsh:Neurology. Diseases of the nervous system, Heat-Shock Proteins, C9orf72 Protein, Amyotrophic Lateral Sclerosis, RNA, medicine.disease, Cell biology, Antisense RNA, lcsh:RC952-954.6, 030104 developmental biology, Gliosis, Stress granules, Frontotemporal Dementia, TDP-43 Proteinopathies, Nerve Degeneration, Neurology (clinical), medicine.symptom, Trinucleotide repeat expansion, Trinucleotide Repeat Expansion, 030217 neurology & neurosurgery, Research Article

Abstract

Background A G4C2 hexanucleotide repeat expansion in the noncoding region of C9orf72 is the major genetic cause of frontotemporal dementia and amyotrophic lateral sclerosis (c9FTD/ALS). Putative disease mechanisms underlying c9FTD/ALS include toxicity from sense G4C2 and antisense G2C4 repeat-containing RNA, and from dipeptide repeat (DPR) proteins unconventionally translated from these RNA products. Methods Intracerebroventricular injections with adeno-associated virus (AAV) encoding 2 or 149 G4C2 repeats were performed on postnatal day 0, followed by assessment of behavioral and neuropathological phenotypes. Results Relative to control mice, gliosis and neurodegeneration accompanied by cognitive and motor deficits were observed in (G4C2)149 mice by 6 months of age. Recapitulating key pathological hallmarks, we also demonstrate that sense and antisense RNA foci, inclusions of poly(GA), poly(GP), poly(GR), poly(PR), and poly(PA) DPR proteins, and inclusions of endogenous phosphorylated TDP-43 (pTDP-43) developed in (G4C2)149 mice but not control (G4C2)2 mice. Notably, proteins that play a role in the regulation of stress granules – RNA-protein assemblies that form in response to translational inhibition and that have been implicated in c9FTD/ALS pathogenesis – were mislocalized in (G4C2)149 mice as early as 3 months of age. Specifically, we observed the abnormal deposition of stress granule components within inclusions immunopositive for poly(GR) and pTDP-43, as well as evidence of nucleocytoplasmic transport defects. Conclusions Our in vivo model of c9FTD/ALS is the first to robustly recapitulate hallmark features derived from both sense and antisense C9orf72 repeat-associated transcripts complete with neurodegeneration and behavioral impairments. More importantly, the early appearance of persistent pathological stress granules prior to significant pTDP-43 deposition implicates an aberrant stress granule response as a key disease mechanism driving TDP-43 proteinopathy in c9FTD/ALS. Electronic supplementary material The online version of this article (10.1186/s13024-019-0310-z) contains supplementary material, which is available to authorized users.

Published

2018

18. APOE ε2 is associated with increased tau pathology in primary tauopathy

Author

Neill R. Graff-Radford, Na Zhao, Owen A. Ross, Zbigniew K. Wszolek, Richard J. Caselli, Joshua Knight, Guojun Bu, Nancy N. Diehl, Cynthia Linares, Olivia N. Attrebi, Melissa E. Murray, Mitsuru Shinohara, Chia Chen Liu, Dennis W. Dickson, John D. Fryer, Rosa Rademakers, Yuka A. Martens, Monica Sanchez-Contreras, Michael G. Heckman, Alexandra J. Van Ingelgom, Leonard Petrucelli, Shunsuke Koga, and Aishe Kurti

Subjects

0301 basic medicine, Genetically modified mouse, Apolipoprotein E, Apolipoprotein E2, Science, Apolipoprotein E4, General Physics and Astronomy, General Biochemistry, Genetics and Molecular Biology, Article, Progressive supranuclear palsy, 03 medical and health sciences, Mice, 0302 clinical medicine, Alzheimer Disease, mental disorders, medicine, Corticobasal degeneration, Animals, Humans, Allele, lcsh:Science, Neuroinflammation, Alleles, Multidisciplinary, business.industry, Neurodegeneration, General Chemistry, medicine.disease, 3. Good health, 030104 developmental biology, Tauopathies, Immunology, Disease Progression, lcsh:Q, lipids (amino acids, peptides, and proteins), Tauopathy, Supranuclear Palsy, Progressive, business, Engineering sciences. Technology, 030217 neurology & neurosurgery

Abstract

Apolipoprotein E (APOE) ε4 allele is the strongest genetic risk factor for late-onset Alzheimer’s disease mainly by modulating amyloid-β pathology. APOE ε4 is also shown to exacerbate neurodegeneration and neuroinflammation in a tau transgenic mouse model. To further evaluate the association of APOE genotype with the presence and severity of tau pathology, we express human tau via an adeno-associated virus gene delivery approach in human APOE targeted replacement mice. We find increased hyperphosphorylated tau species, tau aggregates, and behavioral abnormalities in mice expressing APOE ε2/ε2. We also show that in humans, the APOE ε2 allele is associated with increased tau pathology in the brains of progressive supranuclear palsy (PSP) cases. Finally, we identify an association between the APOE ε2/ε2 genotype and risk of tauopathies using two series of pathologically-confirmed cases of PSP and corticobasal degeneration. Our data together suggest APOE ε2 status may influence the risk and progression of tauopathy., The APOE ε4 allele is a strong genetic risk factor for Alzheimer’s disease, whereas the APOE ε2 allele is protective. Here the authors show that mice expressing the human APOE ε2/ε2 genotype have increased tau pathology and related behavioral deficits; they also find that the APOE ε2 allele is associated with an increased burden of tau pathology in postmortem human brains with progressive supranuclear palsy.

Published

2018

19. A matter of balance

Author

Aaron D Gitler and John D Fryer

Subjects

0301 basic medicine, RNA-binding protein, mRNA splicing, Heterogeneous-Nuclear Ribonucleoproteins, 0302 clinical medicine, C9orf72, Biology (General), Amyotrophic lateral sclerosis, DNA Repeat Expansion, General Neuroscience, RNA-Binding Proteins, Brain, General Medicine, DNA-Binding Proteins, Frontotemporal Dementia, RNA splicing, Medicine, RNA binding proteins, Insight, TD-43, Human, Polypyrimidine Tract-Binding Protein, Frontotemporal dementia, amyotrophic lateral aclerosis, QH301-705.5, Science, RNA Splicing, Chemical biology, Biology, General Biochemistry, Genetics and Molecular Biology, 03 medical and health sciences, Biochemistry and Chemical Biology, mental disorders, medicine, Humans, Human Biology and Medicine, Balance (ability), C9orf72 Protein, General Immunology and Microbiology, Amyotrophic Lateral Sclerosis, nutritional and metabolic diseases, medicine.disease, nervous system diseases, Mutagenesis, Insertional, 030104 developmental biology, Research Advance, Neuroscience, 030217 neurology & neurosurgery

Abstract

Amyotrophic lateral sclerosis (ALS) and frontotemporal dementia (FTD) represent two ends of a disease spectrum with shared clinical, genetic and pathological features. These include near ubiquitous pathological inclusions of the RNA-binding protein (RBP) TDP-43, and often the presence of a GGGGCC expansion in the C9ORF72 (C9) gene. Previously, we reported that the sequestration of hnRNP H altered the splicing of target transcripts in C9ALS patients (Conlon et al., 2016). Here, we show that this signature also occurs in half of 50 postmortem sporadic, non-C9 ALS/FTD brains. Furthermore, and equally surprisingly, these ‘like-C9’ brains also contained correspondingly high amounts of insoluble TDP-43, as well as several other disease-related RBPs, and this correlates with widespread global splicing defects. Finally, we show that the like-C9 sporadic patients, like actual C9ALS patients, were much more likely to have developed FTD. We propose that these unexpected links between C9 and sporadic ALS/FTD define a common mechanism in this disease spectrum.

Published

2018

20. TRIO gene segregation in a family with cerebellar ataxia

Author

Ryan J. Uitti, Mavis Matthew, Thomas R. Caulfield, Karen Jansen-West, Audrey Strongosky, Rana Hanna Al Shaikh, Zbigniew K. Wszolek, Leonard Petrucelli, Mercedes Prudencio, and John D. Fryer

Subjects

0301 basic medicine, Ataxia, Adolescent, Cerebellar Ataxia, Gene mutation, 03 medical and health sciences, 0302 clinical medicine, Genotype, medicine, Humans, Child, Genetics, Comparative Genomic Hybridization, Cerebellar ataxia, business.industry, Limb ataxia, medicine.disease, Pedigree, 030104 developmental biology, Phenotype, Child, Preschool, Anticipation (genetics), Mutation, Spinocerebellar ataxia, Surgery, Neurology (clinical), Age of onset, medicine.symptom, business, 030217 neurology & neurosurgery

Abstract

Aim of the study To report a family with a novel TRIO gene mutation associated with phenotype of cerebellar ataxia. Materials and methods Seven family members of Caribbean descent were recruited through our ataxia research protocol; of the family members, the mother and all 3 children were found to be affected with severe young-onset and rapidly progressive truncal and appendicular ataxia leading to early disability. Array comparative genomic hybridization, mitochondrial DNA analysis, and whole-exome sequencing were performed on 3 of the family members (mother and 2 daughters). Results While the maternal grandmother, great uncle and great aunt were unaffected, the mother and 3 children displayed cognitive dysfunction, severe ataxia, spasticity, and speech disturbances. Age of onset ranged between 3 and 17 years, with average current disease duration of 21 years. Whole-exome sequencing showed a variant p.A1214V in exon 22 of the TRIO gene in 3 of the family members. Array comparative genomic hybridization and mitochondrial DNA analysis were normal. The same variant was later discovered in all but one family member. Conclusions and clinical implications The TRIO p.A1214V variant is associated with cerebellar ataxia in the studied family; it was present in all affected and unaffected family members. Phenotype is severe and broad. Anticipation seems to be present (based on 2 affected generations). It is warranted to screen additional familial early-onset and rapidly progressive ataxia cases for this genotype. TRIO gene mutations may well represent a novel spinocerebellar ataxia subtype.

Published

2018

21. Loss of Tmem106b is unable to ameliorate frontotemporal dementia-like phenotypes in an AAV mouse model of C9ORF72-repeat induced toxicity

Author

Linda Rousseau, Tania F. Gendron, Xiaolai Zhou, John D. Fryer, Jeannie Chew, Virginia Phillips, Billie J. Matchett, Tammee M. Parsons, Leonard Petrucelli, Monica Castanedes-Casey, Aishe Kurti, Melissa E. Murray, Karen Jansen-West, Rosa Rademakers, Ni Cole A. Finch, Fenghua Hu, Lillian M. Daughrity, Mieu Brooks, Alexandra M. Nicholson, Dennis W. Dickson, Ralph B. Perkerson, Emilie A. Perkerson, and Mariely DeJesus-Hernandez

Subjects

0301 basic medicine, Genetic Vectors, Biology, lcsh:RC346-429, Pathology and Forensic Medicine, Mice, 03 medical and health sciences, Cellular and Molecular Neuroscience, 0302 clinical medicine, Transduction, Genetic, C9orf72, Conditioning, Psychological, medicine, Animals, Humans, Interpersonal Relations, RNA, Small Interfering, Gene, lcsh:Neurology. Diseases of the nervous system, Neuroinflammation, Cell Line, Transformed, Mice, Knockout, DNA Repeat Expansion, C9orf72 Protein, Research, Tumor Suppressor Proteins, Membrane Proteins, Fear, Frontotemporal lobar degeneration, medicine.disease, Phenotype, Transmembrane protein, 3. Good health, Astrogliosis, Cell biology, Mice, Inbred C57BL, Disease Models, Animal, 030104 developmental biology, Gene Expression Regulation, Glycerophosphates, Exploratory Behavior, Human medicine, Neurology (clinical), Frontotemporal Lobar Degeneration, 030217 neurology & neurosurgery, Frontotemporal dementia

Abstract

Loss-of-function mutations in progranulin (GRN) and a non-coding (GGGGCC)n hexanucleotide repeat expansions in C9ORF72 are the two most common genetic causes of frontotemporal lobar degeneration with aggregates of TAR DNA binding protein 43 (FTLD-TDP). TMEM106B encodes a type II transmembrane protein with unknown function. Genetic variants in TMEM106B associated with reduced TMEM106B levels have been identified as disease modifiers in individuals with GRN mutations and C9ORF72 expansions. Recently, loss of Tmem106b has been reported to protect the FTLD-like phenotypes in Grn−/− mice. Here, we generated Tmem106b−/− mice and examined whether loss of Tmem106b could rescue FTLD-like phenotypes in an AAV mouse model of C9ORF72-repeat induced toxicity. Our results showed that neither partial nor complete loss of Tmem106b was able to rescue behavioral deficits induced by the expression of (GGGGCC)66 repeats (66R). Loss of Tmem106b also failed to ameliorate 66R-induced RNA foci, dipeptide repeat protein formation and pTDP-43 pathological burden. We further found that complete loss of Tmem106b increased astrogliosis, even in the absence of 66R, and failed to rescue 66R-induced neuronal cell loss, whereas partial loss of Tmem106b significantly rescued the neuronal cell loss but not neuroinflammation induced by 66R. Finally, we showed that overexpression of 66R did not alter expression of Tmem106b and other lysosomal genes in vivo, and subsequent analyses in vitro found that transiently knocking down C9ORF72, but not overexpression of 66R, significantly increased TMEM106B and other lysosomal proteins. In summary, reducing Tmem106b levels failed to rescue FTLD-like phenotypes in a mouse model mimicking the toxic gain-of-functions associated with overexpression of 66R. Combined with the observation that loss of C9ORF72 and not 66R overexpression was associated with increased levels of TMEM106B, this work suggests that the protective TMEM106B haplotype may exert its effect in expansion carriers by counteracting lysosomal dysfunction resulting from a loss of C9ORF72. Electronic supplementary material The online version of this article (10.1186/s40478-018-0545-x) contains supplementary material, which is available to authorized users.

Published

2018

22. C9ORF72 repeat expansions in mice cause TDP-43 pathology, neuronal loss, and behavioral deficits

Author

Mercedes Prudencio, Aishe Kurti, Jeannette N. Stankowski, Dennis W. Dickson, Linda Rousseau, Emilie A. Perkerson, Yong Jie Zhang, Tania F. Gendron, Ena C. Whitelaw, Dieter Edbauer, Peter O. Bauer, Karen Overstreet, Lillian M. Daughrity, Leonard Petrucelli, Pamela Desaro, Karen Jansen-West, Kevin F. Bieniek, John D. Fryer, Melissa E. Murray, Amelia Johnston, Rosa Rademakers, Monica Castanedes-Casey, Chris W. Lee, Hiroki Sasaguri, Caroline Stetler, Jeannie Chew, and Kevin B. Boylan

Subjects

Pathology, medicine.medical_specialty, Multidisciplinary, Neurodegeneration, Cerebellar Purkinje cell, Biology, medicine.disease, Astrogliosis, C9orf72 Protein, C9orf72, medicine, Amyotrophic lateral sclerosis, Trinucleotide repeat expansion, Engineering sciences. Technology, Frontotemporal dementia

Abstract

The major genetic cause of frontotemporal dementia and amyotrophic lateral sclerosis is a G(4)C(2) repeat expansion in C9ORF72. Efforts to combat neurodegeneration associated with "c9FTD/ALS" are hindered by a lack of animal models recapitulating disease features. We developed a mouse model to mimic both neuropathological and clinical c9FTD/ALS phenotypes. We expressed (G(4)C(2))(66) throughout the murine central nervous system by means of somatic brain transgenesis mediated by adeno-associated virus. Brains of 6-month-old mice contained nuclear RNA foci, inclusions of poly(Gly-Pro), poly(Gly-Ala), and poly(Gly-Arg) dipeptide repeat proteins, as well as TDP-43 pathology. These mouse brains also exhibited cortical neuron and cerebellar Purkinje cell loss, astrogliosis, and decreased weight. (G(4)C(2))(66) mice also developed behavioral abnormalities similar to clinical symptoms of c9FTD/ALS patients, including hyperactivity, anxiety, antisocial behavior, and motor deficits.

Published

2015

23. Poly(GR) impairs protein translation and stress granule dynamics in C9orf72-associated frontotemporal dementia and amyotrophic lateral sclerosis

Author

Rosa Rademakers, John D. Fryer, Yong Jie Zhang, Karen Jansen-West, Bjorn Oskarsson, Jimei Tong, Monica Castanedes-Casey, Sarah R. Pickles, Tania F. Gendron, Leonard Petrucelli, Casey Cook, Mark T. W. Ebbert, Aliesha D. O’Raw, Xu Zhang, Dennis W. Dickson, Wenqian Hu, Yuping Song, Mei Yue, Mercedes Prudencio, Aishe Kurti, Jeannie Chew, Lillian M. Daughrity, and Aaron D. Gitler

Subjects

0301 basic medicine, Ribosomal Proteins, Cytoplasmic Granules, General Biochemistry, Genetics and Molecular Biology, Article, Pathogenesis, 03 medical and health sciences, Stress granule, Atrophy, C9orf72, Stress, Physiological, medicine, Animals, Cluster Analysis, Humans, Amyotrophic lateral sclerosis, Biology, Behavior, Animal, C9orf72 Protein, Chemistry, Gene Expression Profiling, HEK 293 cells, Neurodegeneration, Amyotrophic Lateral Sclerosis, RNA, General Medicine, Dipeptides, medicine.disease, Cell biology, Mice, Inbred C57BL, 030104 developmental biology, HEK293 Cells, Frontotemporal Dementia, Protein Biosynthesis, Human medicine

Abstract

The major genetic cause of frontotemporal dementia (FTD) and amyotrophic lateral sclerosis (ALS) is a C9orf72 G(4)C(2) repeat expansion(1,2). Proposed mechanisms by which the expansion causes c9FTD/ALS include toxicity from repeat-containing RNA and from dipeptide repeat proteins translated from these transcripts. To investigate the contribution of poly(GR) dipeptide repeat proteins to c9FTD/ALS pathogenesis in a mammalian in vivo model, we generated mice that expressed GFP-(GR)(100) in the brain. GFP-(GR)(100) mice developed age-dependent neurodegeneration, brain atrophy, and motor and memory deficits through the accumulation of diffuse, cytoplasmic poly(GR). Poly(GR) co-localized with ribosomal subunits and the translation initiation factor elF3 eta in GFP-(GR)(100) mice and, of importance, in c9FTD/ALS patients. Combined with the differential expression of ribosome-associated genes in GFP-(GR)(100 )mice, these findings demonstrate poly(GR)-mediated ribosomal distress. Indeed, poly(GR) inhibited canonical and non-canonical protein translation in HEK293T cells, and also induced the formation of stress granules and delayed their disassembly. These data suggest that poly(GR) contributes to c9FTD/ALS by impairing protein translation and stress granule dynamics, consequently causing chronic cellular stress and preventing cells from mounting an effective stress response. Decreasing poly(GR) and/or interrupting interactions between poly(GR) and ribosomal and stress granule-associated proteins may thus represent potential therapeutic strategies to restore homeostasis.

Published

2017

24. Exercise training-induced modification of the gut microbiota persists after microbiota colonization and attenuates the response to chemically-induced colitis in gnotobiotic mice

Author

Jeffrey A. Woods, Vandana Nehra, C. Salmonson, Bryan A. White, Josh Cohrs, Lucy J. Mailing, Vanessa L. Hale, John D. Fryer, Jacob M. Allen, and Purna C. Kashyap

Subjects

0301 basic medicine, Microbiology (medical), Male, Colon, Gut flora, Microbiology, digestive system, 03 medical and health sciences, Mice, 0302 clinical medicine, Sex Factors, Physical Conditioning, Animal, medicine, Animals, Germ-Free Life, Homeostasis, Colonization, Microbiome, Colitis, Cecum, Acute colitis, Gastrointestinal tract, biology, Body Weight, Dextran Sulfate, Gastroenterology, Chemical colitis, Fecal Microbiota Transplantation, medicine.disease, biology.organism_classification, Fatty Acids, Volatile, Mucus, Gastrointestinal Microbiome, Mice, Inbred C57BL, Disease Models, Animal, 030104 developmental biology, Infectious Diseases, Gene Expression Regulation, 030220 oncology & carcinogenesis, Immunology, Research Paper/Report, Cytokines, Female

Abstract

Exercise reduces the risk of inflammatory disease by modulating a variety of tissue and cell types, including those within the gastrointestinal tract. Recent data indicates that exercise can also alter the gut microbiota, but little is known as to whether these changes affect host function. Here, we use a germ-free (GF) animal model to test whether exercise-induced modifications in the gut microbiota can directly affect host responses to microbiota colonization and chemically-induced colitis. Donor mice (n = 19) received access to a running wheel (n = 10) or remained without access (n = 9) for a period of six weeks. After euthanasia, cecal contents were pooled by activity treatment and transplanted into two separate cohorts of GF mice. Two experiments were then conducted. First, mice were euthanized five weeks after the microbiota transplant and tissues were collected for analysis. A second cohort of GF mice were colonized by donor microbiotas for four weeks before dextran-sodium-sulfate was administered to induce acute colitis, after which mice were euthanized for tissue analysis. We observed that microbial transplants from donor (exercised or control) mice led to differences in microbiota β-diversity, metabolite profiles, colon inflammation, and body mass in recipient mice five weeks after colonization. We also demonstrate that colonization of mice with a gut microbiota from exercise-trained mice led to an attenuated response to chemical colitis, evidenced by reduced colon shortening, attenuated mucus depletion and augmented expression of cytokines involved in tissue regeneration. Exercise-induced modifications in the gut microbiota can mediate host-microbial interactions with potentially beneficial outcomes for the host.

Published

2017

25. Potentially Modifiable Risk Factors for Long-Term Cognitive Impairment After Critical Illness: A Systematic Review

Author

Amra Sakusic, Ronald C. Petersen, Mikhail A. Dziadzko, John D. Fryer, Rashid Ali, Alejandro A. Rabinstein, Dziadzko Volha, Ann M. Farrell, Ognjen Gajic, Rahul Kashyap, John C. O’Horo, and Tarun D. Singh

Subjects

Adult, Male, medicine.medical_specialty, Traumatic brain injury, medicine.medical_treatment, Critical Illness, Hypoglycemia, law.invention, 03 medical and health sciences, 0302 clinical medicine, law, Risk Factors, Intensive care, medicine, Extracorporeal membrane oxygenation, Humans, Survivors, Risk factor, Intensive care medicine, Aged, Aged, 80 and over, business.industry, 030208 emergency & critical care medicine, Cognition, General Medicine, Middle Aged, medicine.disease, Intensive care unit, 030228 respiratory system, Delirium, Female, medicine.symptom, business, Cognition Disorders

Abstract

Long-term cognitive impairment is common in survivors of critical illness. Little is known about the etiology of this serious complication. We sought to summarize current scientific knowledge about potentially modifiable risk factors during intensive care unit (ICU) treatment that may play a substantial role in the development of long-term cognitive impairment. All searches were run on October 1, 2017. The search strategy included Ovid MEDLINE, Ovid Embase, Ovid CDR, Cochrane Central Register of Controlled Trials and Database of Abstracts of Reviews of Effect, Scopus, and Web of Science, and included MeSH headings and keywords related to intensive care, critical care, and cognitive disorders. Searches were restricted to adult subjects. Inclusion required follow-up cognitive evaluation at least 2 months after ICU discharge. Studies assessing patients with cardiac arrest, traumatic brain injury, and cardiac surgery history were excluded. The search strategy resulted in 3180 studies. Of these, 28 studies (.88%) met our inclusion criteria and were analyzed. Delirium and duration of delirium were associated with long-term cognitive impairment after ICU admission in 6 of 9 studies in which this factor was analyzed. Weaker and more inconsistent associations have been reported with hypoglycemia, hyperglycemia, fluctuations in serum glucose levels, and in-hospital acute stress symptoms. Instead, most of the studies did not find significant associations between long-term cognitive impairment and mechanical ventilation; use of sedatives, vasopressors, or analgesic medications; enteral feeding; hypoxia; extracorporeal membrane oxygenation; systolic blood pressure; pulse rate; or length of ICU stay. Prolonged delirium may be a risk factor for long-term cognitive impairment after critical illness, though this association has not been entirely consistent across studies. Other potentially preventable factors have not been shown to have strong or consistent associations with long-term cognitive dysfunction in survivors of critical illness.

Published

2017

26. [P4–125]: THE MOLECULAR CHAPERONE BRICHOS INHIBITS Aβ AGGREGATION AND OTHER NEUROPATHOLOGICAL PHENOTYPES IN A MOUSE MODEL OF Aβ AMYLOIDOSIS

Author

Krystal C. Belmonte, Chaeyoung Kim, Luis Flores, John D. Fryer, Jenny Presto, Jan Johansson, Jungsu Kim, Aishe Kurti, and Lisa Dolfe

Subjects

Epidemiology, Chemistry, Health Policy, Amyloidosis, medicine.disease, Molecular biology, Phenotype, Cell biology, Psychiatry and Mental health, Cellular and Molecular Neuroscience, Developmental Neuroscience, medicine, Neurology (clinical), Geriatrics and Gerontology

Published

2017

27. Neonatal AAV delivery of alpha-synuclein induces pathology in the adult mouse brain

Author

Pamela J. McLean, Aishe Kurti, Marion Delenclos, Ayman H. Faroqi, Mei Yue, Linda Rousseau, Dennis W. Dickson, Monica Castanedes-Casey, John D. Fryer, and Virginia Phillips

Subjects

0301 basic medicine, Pathology, medicine.medical_specialty, Genetic Vectors, Hippocampus, Motor Activity, Biology, lcsh:RC346-429, Pathology and Forensic Medicine, Alpha-synuclein, Neonatal injection, Aggregation, 03 medical and health sciences, Cellular and Molecular Neuroscience, chemistry.chemical_compound, 0302 clinical medicine, Memory, medicine, Animals, Humans, Learning, Dementia, Gliosis, lcsh:Neurology. Diseases of the nervous system, Synucleinopathies, Lewy body, Research, Brain, Neurodegenerative Diseases, Dependovirus, medicine.disease, 3. Good health, Olfactory bulb, Mice, Inbred C57BL, Disease Models, Animal, HEK293 Cells, 030104 developmental biology, Animals, Newborn, chemistry, Astrocytes, Microglia, Neurology (clinical), Viral vector model, medicine.symptom, Neuroscience, 030217 neurology & neurosurgery, Immunostaining

Abstract

Abnormal accumulation of alpha-synuclein (αsyn) is a pathological hallmark of Lewy body related disorders such as Parkinson’s disease and Dementia with Lewy body disease. During the past two decades, a myriad of animal models have been developed to mimic pathological features of synucleinopathies by over-expressing human αsyn. Although different strategies have been used, most models have little or no reliable and predictive phenotype. Novel animal models are a valuable tool for understanding neuronal pathology and to facilitate development of new therapeutics for these diseases. Here, we report the development and characterization of a novel model in which mice rapidly express wild-type αsyn via somatic brain transgenesis mediated by adeno-associated virus (AAV). At 1, 3, and 6 months of age following intracerebroventricular (ICV) injection, mice were subjected to a battery of behavioral tests followed by pathological analyses of the brains. Remarkably, significant levels of αsyn expression are detected throughout the brain as early as 1 month old, including olfactory bulb, hippocampus, thalamic regions and midbrain. Immunostaining with a phospho-αsyn (pS129) specific antibody reveals abundant pS129 expression in specific regions. Also, pathologic αsyn is detected using the disease specific antibody 5G4. However, this model did not recapitulate behavioral phenotypes characteristic of rodent models of synucleinopathies. In fact no deficits in motor function or cognition were observed at 3 or 6 months of age. Taken together, these findings show that transduction of neonatal mouse with AAV-αsyn can successfully lead to rapid, whole brain transduction of wild-type human αsyn, but increased levels of wildtype αsyn do not induce behavior changes at an early time point (6 months), despite pathological changes in several neurons populations as early as 1 month. Electronic supplementary material The online version of this article (doi:10.1186/s40478-017-0455-3) contains supplementary material, which is available to authorized users.

Published

2017

28. Poly(GP) proteins are a useful pharmacodynamic marker for C9ORF72-associated amyotrophic lateral sclerosis

Author

Timothy M. Miller, Jon B. Toledo, Jennifer Farren, Jeffrey D. Rothstein, John Q. Trojanowski, Luc Pregent, Michael G. Heckman, Alessandro Prelle, Aliesha D. O’Raw, Beth K. Rush, Bryan J. Traynor, Laura Braun, Matthew D. Disney, Yari Carlomagno, Veronique V. Belzil, Antonia Ratti, Lilia J. Tabassian, Monica Castanedes-Casey, Dennis W. Dickson, Michael Tierney, John C. van Swieten, Adam L. Boxer, Jeannie Chew, Lauren Elman, Murray Grossman, Emilie A. Perkerson, Mercedes Prudencio, Ana M. Caputo, Frank Rigo, Lillian M. Daughrity, Casey Cook, Otto Pedraza, James D. Berry, David Lacomis, Christina Fournier, Jennifer Jockel-Balsarotti, Leonard Petrucelli, Giovanna Antognetti, Marka van Blitterswijk, Lindsey R. Hayes, Robert H. Brown, Joanne Wuu, Kevin B. Boylan, Jimei Tong, Edythe Wiggs, Amelia Robertson, Linda Rousseau, Karen Jansen-West, Mary Kay Floeter, Yuping Song, John D. Fryer, Tania D Gendron, Robert Bowser, Barbara Poletti, Jennifer D. McBride, Shafeeq Ladha, Federica Solca, Alexander McCampbell, Leo McCluskey, Bruce L. Miller, Weixing Yang, Rosa Rademakers, Virginia Phillips, Chris W. Lee, Mei Yue, Denitza Raitcheva, Carla Palmucci, Jonathan D. Glass, Nancy N. Diehl, Vincenzo Silani, Jeannette N. Stankowski, Pamela Desaro, Cinzia Tiloca, Claudia Morelli, Abhishek Datta, William T. Hu, Yong Jie Zhang, Michael Benatar, Christine Ambrose, and Neurology

Subjects

0301 basic medicine, Oligonucleotides, Neurodegenerative, medicine.disease_cause, Medical and Health Sciences, Mice, 0302 clinical medicine, C9orf72, Leukocytes, Longitudinal Studies, Amyotrophic lateral sclerosis, Dinucleotide Repeats, Neurons, Mutation, Brain, General Medicine, Middle Aged, Biological Sciences, Prognosis, Editorial, Neurological, Adult, Mononuclear, Induced Pluripotent Stem Cells, Clinical Trials and Supportive Activities, Peripheral blood mononuclear cell, Article, Cell Line, 03 medical and health sciences, Rare Diseases, Clinical Research, medicine, Extracellular, Acquired Cognitive Impairment, Genetics, Animals, Humans, Antisense, Biology, Aged, C9orf72 Protein, Oligonucleotide, business.industry, Amyotrophic Lateral Sclerosis, Neurosciences, RNA, Oligonucleotides, Antisense, medicine.disease, Molecular biology, Brain Disorders, 030104 developmental biology, Cancer research, Leukocytes, Mononuclear, Dementia, Human medicine, ALS, Trinucleotide repeat expansion, business, 030217 neurology & neurosurgery, Biomarkers

Abstract

There is no effective treatment for amyotrophic lateral sclerosis (ALS), a devastating motor neuron disease. However, discovery of a G(4)C(2) repeat expansion in the C9ORF72 gene as the most common genetic cause of ALS has opened up new avenues for therapeutic intervention for this form of ALS. G(4)C(2) repeat expansion RNAs and proteins of repeating dipeptides synthesized from these transcripts are believed to play a key role in C9ORF72-associated ALS (c9ALS). Therapeutics that target G(4)C(2) RNA, such as antisense oligonucleotides (ASOs) and small molecules, are thus being actively investigated. A limitation in moving such treatments from bench to bedside is a lack of pharmacodynamic markers for use in clinical trials. We explored whether poly(GP) proteins translated from G(4)C(2) RNA could serve such a purpose. Poly(GP) proteins were detected in cerebrospinal fluid (CSF) and in peripheral blood mononuclear cells from c9ALS patients and, notably, from asymptomatic C9ORF72 mutation carriers. Moreover, CSF poly(GP) proteins remained relatively constant over time, boding well for their use in gauging biochemical responses to potential treatments. Treating c9ALS patient cells or a mouse model of c9ALS with ASOs that target G(4)C(2) RNA resulted in decreased intracellular and extracellular poly(GP) proteins. This decrease paralleled reductions in G(4)C(2) RNA and downstream G(4)C(2) RNA-mediated events. These findings indicate that tracking poly(GP) proteins in CSF could provide a means to assess target engagement of G(4)C(2) RNA-based therapies in symptomatic C9ORF72 repeat expansion carriers and presymptomatic individuals who are expected to benefit from early therapeutic intervention.

Published

2017

29. Severe amygdala dysfunction in a MAPT transgenic mouse model of frontotemporal dementia

Author

Linda Rousseau, Leonard Petrucelli, Monica Castanedes-Casey, Nawsheen Shukoor, Dennis W. Dickson, John D. Fryer, Kristyn Scheffel, Casey Cook, Michael S. Penuliar, Judy Dunmore, Jimei Tong, Virginia Phillips, Melissa E. Murray, and Aishe Kurti

Subjects

Genetically modified mouse, Aging, Elevated plus maze, Mice, Transgenic, tau Proteins, Severity of Illness Index, Amygdala, Article, Mice, Memory, Conditioning, Psychological, medicine, Animals, Humans, Learning, Fear conditioning, Language, Behavior, Animal, General Neuroscience, Parkinsonism, Neurodegeneration, Fear, medicine.disease, Disease Models, Animal, medicine.anatomical_structure, Frontotemporal Dementia, Mutation, Nerve Degeneration, Exploratory Behavior, Neurology (clinical), Tauopathy, Geriatrics and Gerontology, Psychology, Neuroscience, Developmental Biology, Frontotemporal dementia

Abstract

Frontotemporal dementia with Parkinsonism-linked to chromosome 17 (FTDP-17) is a neurodegenerative tauopathy caused by mutations in the tau gene (MAPT). Individuals with FTDP-17 have deficits in learning, memory and language, in addition to personality and behavioral changes that are often characterized by a lack of social inhibition. Several transgenic mouse models expressing tau mutations have been tested extensively for memory or motor impairments, though reports of amygdala-dependent behaviors are lacking. To this end, we tested the rTg4510 mouse model on a behavioral battery that included amygdala-dependent tasks of exploration. As expected, rTg4510 mice exhibit profound impairments in hippocampal-dependent learning and memory tests, including contextual fear conditioning. However, rTg4510 mice also display an abnormal hyper-exploratory phenotype in the open field assay, elevated plus maze, light-dark exploration, and cued fear conditioning, indicative of amygdala dysfunction. Furthermore, significant tau burden is detected in the amygdala of both rTg4510 mice and human FTDP-17 patients, suggesting that the rTg4510 mouse model recapitulates the behavioral disturbances and neurodegeneration of the amygdala characteristic of FTDP-17.

Published

2014

30. ABCA7 Deficiency Accelerates Amyloid-β Generation and Alzheimer's Neuronal Pathology

Author

Xianlin Han, Masaya Tachibana, Miao Wang, Fanggeng Zou, Yu Yamazaki, Yasumasa Ohyagi, Nobutaka Sakae, Romain Fol, Aishe Kurti, Minerva M. Carrasquillo, Jessica L. Frisch-Daiello, Daniel Sevlever, Linda H. Younkin, Ming Gan, Gina Bisceglio, Steven G. Younkin, Guojun Bu, Chia Chen Liu, John D. Fryer, Li Ma, Takahisa Kanekiyo, Michael L. Fitzgerald, Mitsuru Shinohara, and Patrick Knight

Subjects

0301 basic medicine, Male, Amyloid, Eukaryotic Initiation Factor-2, Mice, Transgenic, Presenilin, ABCA7, 03 medical and health sciences, Amyloid beta-Protein Precursor, Mice, 0302 clinical medicine, Alzheimer Disease, mental disorders, medicine, Amyloid precursor protein, Presenilin-1, Animals, Humans, Protein kinase A, Memory Disorders, Amyloid beta-Peptides, biology, General Neuroscience, P3 peptide, Brain, Articles, medicine.disease, Lipid Metabolism, Cell biology, Disease Models, Animal, 030104 developmental biology, Gene Expression Regulation, ABCA1, Immunology, Mutation, biology.protein, ATP-Binding Cassette Transporters, Female, Alzheimer's disease, 030217 neurology & neurosurgery, Signal Transduction

Abstract

In Alzheimer's disease (AD), the accumulation and deposition of amyloid-β (Aβ) peptides in the brain is a central event. Aβ is cleaved from amyloid precursor protein (APP) by β-secretase and γ-secretase mainly in neurons. Although mutations inAPP,PS1, orPS2cause early-onset familial AD,ABCA7encoding ATP-binding cassette transporter A7 is one of the susceptibility genes for late-onset AD (LOAD), in which itsloss-of-functionvariants increase the disease risk. ABCA7 is homologous to a major lipid transporter ABCA1 and is highly expressed in neurons and microglia in the brain. Here, we show that ABCA7 deficiency altered brain lipid profile and impaired memory in ABCA7 knock-out (Abca7−/−) mice. When bred to amyloid model APP/PS1 mice, plaque burden was exacerbated by ABCA7 deficit.In vivomicrodialysis studies indicated that the clearance rate of Aβ was unaltered. Interestingly, ABCA7 deletion facilitated the processing of APP to Aβ by increasing the levels of β-site APP cleaving enzyme 1 (BACE1) and sterol regulatory element-binding protein 2 (SREBP2) in primary neurons and mouse brains. Knock-down of ABCA7 expression in neurons caused endoplasmic reticulum stress highlighted by increased level of protein kinase R-like endoplasmic reticulum kinase (PERK) and increased phosphorylation of eukaryotic initiation factor 2α (eIF2α). In the brains of APP/PS1;Abca7−/−mice, the level of phosphorylated extracellular regulated kinase (ERK) was also significantly elevated. Together, our results reveal novel pathways underlying the association of ABCA7 dysfunction and LOAD pathogenesis.SIGNIFICANCE STATEMENTGene variants inABCA7encoding ATP-binding cassette transporter A7 are associated with the increased risk for late-onset Alzheimer's disease (AD). Importantly, we found the altered brain lipid profile and impaired memory in ABCA7 knock-out mice. The accumulation of amyloid-β (Aβ) peptides cleaved from amyloid precursor protein (APP) in the brain is a key event in AD pathogenesis and we also found that ABCA7 deficit exacerbated brain Aβ deposition in amyloid AD model APP/PS1 mice. Mechanistically, we found that ABCA7 deletion facilitated the processing of APP and Aβ production by increasing the levels of β-secretase 1 (BACE1) in primary neurons and mouse brains without affecting the Aβ clearance rate in APP/PS1 mice. Our study demonstrates a novel mechanism underlying how dysfunctions of ABCA7 contribute to the risk for AD.

Published

2016

31. Impact of sex and APOE4 on cerebral amyloid angiopathy in Alzheimer's disease

Author

Julia E. Crook, Yu Yamazaki, Motoko Shinohara, Melissa E. Murray, Takahisa Kanekiyo, Ryan D. Frank, Meghan M. Painter, Mitsuru Shinohara, Chia Chen Liu, Dennis W. Dickson, John D. Fryer, Guojun Bu, Mary D. Davis, Na Zhao, Yuka Atagi, Ronald C. Petersen, Masaya Tachibana, and Michael DeTure

Subjects

0301 basic medicine, Apolipoprotein E, Male, Pathology, medicine.medical_specialty, Amyloid, Genotype, Apolipoprotein E4, Plaque, Amyloid, Article, Pathology and Forensic Medicine, 03 medical and health sciences, Cellular and Molecular Neuroscience, 0302 clinical medicine, Alzheimer Disease, mental disorders, medicine, Humans, cardiovascular diseases, Pathological, Aged, Temporal cortex, Aged, 80 and over, Sex Characteristics, Amyloid beta-Peptides, business.industry, nutritional and metabolic diseases, Brain, Neurofibrillary tangle, Neurofibrillary Tangles, medicine.disease, Cerebral Amyloid Angiopathy, 030104 developmental biology, lipids (amino acids, peptides, and proteins), Female, Neurology (clinical), Cerebral amyloid angiopathy, Alzheimer's disease, business, 030217 neurology & neurosurgery, Sex characteristics

Abstract

Cerebral amyloid angiopathy (CAA) often coexists with Alzheimer's disease (AD). APOE4 is a strong genetic risk factor for both AD and CAA. Sex-dependent differences have been shown in AD as well as in cerebrovascular diseases. Therefore, we examined the effects of APOE4, sex, and pathological components on CAA in AD subjects. A total of 428 autopsied brain samples from pathologically confirmed AD cases were analyzed. CAA severity was histologically scored in inferior parietal, middle frontal, motor, superior temporal and visual cortexes. In addition, subgroups with severe CAA (n = 60) or without CAA (n = 39) were subjected to biochemical analysis of amyloid-β (Aβ) and apolipoprotein E (apoE) by ELISA in the temporal cortex. After adjusting for age, Braak neurofibrillary tangle stage and Thal amyloid phase, we found that overall CAA scores were higher in males than females. Furthermore, carrying one or more APOE4 alleles was associated with higher overall CAA scores. Biochemical analysis revealed that the levels of detergent-soluble and detergent-insoluble Aβ40, and insoluble apoE were significantly elevated in individuals with severe CAA or APOE4. The ratio of Aβ40/Aβ42 in insoluble fractions was also increased in the presence of CAA or APOE4, although it was negatively associated with male sex. Levels of insoluble Aβ40 were positively associated with those of insoluble apoE, which were strongly influenced by CAA status. Pertaining to insoluble Aβ42, the levels of apoE correlated regardless of CAA status. Our results indicate that sex and APOE genotypes differentially influence the presence and severity of CAA in AD, likely by affecting interaction and aggregation of Aβ40 and apoE.

Published

2016

32. Exercise and Genetic Rescue of SCA1 via the Transcriptional Repressor Capicua

Author

Yan Gao, Angela N. Carter, Hyojin Kang, Chad A. Shaw, Juan Crespo-Barreto, Harry T. Orr, Peng Yu, Caleigh Mandel-Brehm, Huda Y. Zoghbi, Adriano Flora, and John D. Fryer

Subjects

Spinocerebellar Ataxia Type 1, Offspring, Repressor, Ataxin 1, Nerve Tissue Proteins, Disease, Bioinformatics, Mice, Epidermal growth factor, Cerebellum, medicine, Animals, Spinocerebellar Ataxias, Gene Knock-In Techniques, Nuclear protein, Ataxin-1, Genetics, Multidisciplinary, biology, Nuclear Proteins, medicine.disease, Mice, Mutant Strains, Exercise Therapy, Mice, Inbred C57BL, Repressor Proteins, Disease Models, Animal, Ataxins, Spinocerebellar ataxia, biology.protein

Abstract

Spinocerebellar ataxia type 1 (SCA1) is a fatal neurodegenerative disease caused by expansion of a translated CAG repeat in Ataxin-1 (ATXN1). To determine the long-term effects of exercise, we implemented a mild exercise regimen in a mouse model of SCA1 and found a considerable improvement in survival accompanied by up-regulation of epidermal growth factor and consequential down-regulation of Capicua, which is an ATXN1 interactor. Offspring of Capicua mutant mice bred to SCA1 mice showed significant improvement of all disease phenotypes. Although polyglutamine-expanded Atxn1 caused some loss of Capicua function, further reduction of Capicua levels--either genetically or by exercise--mitigated the disease phenotypes by dampening the toxic gain of function. Thus, exercise might have long-term beneficial effects in other ataxias and neurodegenerative diseases.

Published

2011

33. A partial loss of function allele of Methyl-CpG-binding protein 2 predicts a human neurodevelopmental syndrome

Author

Yaling Sun, Jun Ren, Jeffrey L. Neul, John J. Greer, Hsiao-Tuan Chao, John D. Fryer, Huda Y. Zoghbi, Rodney C. Samaco, and Sharyl L. Fyffe

Subjects

Male, Reflex, Startle, congenital, hereditary, and neonatal diseases and abnormalities, Methyl-CpG-Binding Protein 2, MECP2 duplication syndrome, Fluorescent Antibody Technique, Pain, Rett syndrome, Anxiety, Biology, Hippocampus, Nesting Behavior, MECP2, Mice, Neurodevelopmental disorder, mental disorders, Rett Syndrome, Genetics, medicine, Animals, Humans, Learning, Protein Isoforms, Allele, Social Behavior, Molecular Biology, Crosses, Genetic, Genetics (clinical), Loss function, Body Weight, Brain, Articles, General Medicine, Amygdala, medicine.disease, Startle reaction, nervous system diseases, Rotarod Performance Test, Autism, Female, Psychomotor Performance

Abstract

Rett Syndrome, an X-linked dominant neurodevelopmental disorder characterized by regression of language and hand use, is primarily caused by mutations in methyl-CpG-binding protein 2 (MECP2). Loss of function mutations in MECP2 are also found in other neurodevelopmental disorders such as autism, Angelman-like syndrome and non-specific mental retardation. Furthermore, duplication of the MECP2 genomic region results in mental retardation with speech and social problems. The common features of human neurodevelopmental disorders caused by the loss or increase of MeCP2 function suggest that even modest alterations of MeCP2 protein levels result in neurodevelopmental problems. To determine whether a small reduction in MeCP2 level has phenotypic consequences, we characterized a conditional mouse allele of Mecp2 that expresses 50% of the wild-type level of MeCP2. Upon careful behavioral analysis, mice that harbor this allele display a spectrum of abnormalities such as learning and motor deficits, decreased anxiety, altered social behavior and nest building, decreased pain recognition and disrupted breathing patterns. These results indicate that precise control of MeCP2 is critical for normal behavior and predict that human neurodevelopmental disorders will result from a subtle reduction in MeCP2 expression.

Published

2008

34. Tau deposition drives neuropathological, inflammatory and behavioral abnormalities independently of neuronal loss in a novel mouse model

Author

Casey Cook, Mitsuru Shinohara, Leonard Petrucelli, Wen Lang Lin, Guojun Bu, Mei Yue, Dennis W. Dickson, Yari Carlomagno, Silvia S. Kang, Linda Rousseau, Emilie A. Perkerson, Monica Castanedes-Casey, Virginia Phillips, Karen Jansen-West, Aishe Kurti, and John D. Fryer

Subjects

Transgene, Tau protein, Mice, Transgenic, tau Proteins, Biology, Silver stain, Mice, Genetics, medicine, Animals, Humans, Molecular Biology, Genetics (clinical), Neuroinflammation, Ultrasonography, Neurons, Behavior, Animal, Cell Death, Brain, Neurofibrillary tangle, Neurofibrillary Tangles, General Medicine, Articles, medicine.disease, Phenotype, Disease Models, Animal, Gliosis, Tauopathies, biology.protein, Tauopathy, medicine.symptom, Neuroscience

Abstract

Aberrant tau protein accumulation drives neurofibrillary tangle (NFT) formation in several neurodegenerative diseases. Currently, efforts to elucidate pathogenic mechanisms and assess the efficacy of therapeutic targets are limited by constraints of existing models of tauopathy. In order to generate a more versatile mouse model of tauopathy, somatic brain transgenesis was utilized to deliver adeno-associated virus serotype 1 (AAV1) encoding human mutant P301L-tau compared with GFP control. At 6 months of age, we observed widespread human tau expression with concomitant accumulation of hyperphosphorylated and abnormally folded proteinase K resistant tau. However, no overt neuronal loss was observed, though significant abnormalities were noted in the postsynaptic scaffolding protein PSD95. Neurofibrillary pathology was also detected with Gallyas silver stain and Thioflavin-S, and electron microscopy revealed the deposition of closely packed filaments. In addition to classic markers of tauopathy, significant neuroinflammation and extensive gliosis were detected in AAV1-Tau(P301L) mice. This model also recapitulates the behavioral phenotype characteristic of mouse models of tauopathy, including abnormalities in exploration, anxiety, and learning and memory. These findings indicate that biochemical and neuropathological hallmarks of tauopathies are accurately conserved and are independent of cell death in this novel AAV-based model of tauopathy, which offers exceptional versatility and speed in comparison with existing transgenic models. Therefore, we anticipate this approach will facilitate the identification and validation of genetic modifiers of disease, as well as accelerate preclinical assessment of potential therapeutic targets.

Published

2015

35. Alzheimer Research Forum Live Discussion: Making a BioMark on Alzheimer Disease

Author

Anne M. Fagan, Mony J. de Leon, Clary B. Clish, Patrick Lynn, Nancy B. Emerson Lombardo, June Kinoshita, John D. Fryer, Tom Fagan, Hasan K. Siddiqi, John Q. Trojanowski, Les Shaw, and John R. Ciallella

Subjects

Gerontology, Psychiatry and Mental health, Clinical Psychology, business.industry, General Neuroscience, Medicine, General Medicine, Geriatrics and Gerontology, Alzheimer's disease, business, medicine.disease

Published

2006

36. Human Apolipoprotein E4 Alters the Amyloid-β 40:42 Ratio and Promotes the Formation of Cerebral Amyloid Angiopathy in an Amyloid Precursor Protein Transgenic Model

Author

Steven M. Paul, Patrick Sullivan, Kelly R. Bales, Maia Parsadanian, David M. Holtzman, John D. Fryer, and Kelly Simmons

Subjects

Apolipoprotein E, Genetically modified mouse, Pathology, medicine.medical_specialty, Apolipoprotein E4, BACE1-AS, Apolipoprotein E3, Enzyme-Linked Immunosorbent Assay, Mice, Transgenic, Plaque, Amyloid, Alkenes, Benzoates, Amyloid beta-Protein Precursor, Mice, Apolipoproteins E, Alzheimer Disease, Neurobiology of Disease, mental disorders, Amyloid precursor protein, medicine, Extracellular, Animals, Humans, cardiovascular diseases, Senile plaques, Amyloid beta-Peptides, biology, Chemistry, General Neuroscience, P3 peptide, nutritional and metabolic diseases, medicine.disease, Peptide Fragments, Mice, Inbred C57BL, Cerebral Amyloid Angiopathy, Disease Models, Animal, Gene Expression Regulation, biology.protein, Blood Vessels, lipids (amino acids, peptides, and proteins), Cerebral amyloid angiopathy

Abstract

Alzheimer's disease (AD) is characterized by the aggregation and deposition of the normally soluble amyloid-β (Aβ) peptide in the extracellular spaces of the brain as parenchymal plaques and in the walls of cerebral vessels as cerebral amyloid angiopathy (CAA). CAA is a common cause of brain hemorrhage and is found in most patients with AD. As in AD, the ϵ4 allele of the apolipoprotein E (apoE) gene (APOE) is a risk factor for CAA. To determine the effect of human apoE on CAAin vivo, we bred humanAPOE3andAPOE4“knock-in” mice to a transgenic mouse model (Tg2576) that develops amyloid plaques as well as CAA. The expression of both human apoE isoforms resulted in a delay in Aβ deposition of several months relative to murine apoE. Tg2576 mice expressing the more fibrillogenic murine apoE develop parenchymal amyloid plaques and CAA by 9 months of age. At 15 months of age, the expression of human apoE4 led to substantial CAA with very few parenchymal plaques, whereas the expression of human apoE3 resulted in almost no CAA or parenchymal plaques. Additionally, young apoE4-expressing mice had an elevated ratio of Aβ 40:42 in brain extracellular pools and a lower 40:42 ratio in CSF, suggesting that apoE4 results in altered clearance and transport of Aβ species within different brain compartments. These findings demonstrate that, once Aβ fibrillogenesis occurs, apoE4 favors the formation of CAA over parenchymal plaques and suggest that molecules or treatments that increase the ratio of Aβ 40:42 may favor the formation of CAA versus parenchymal plaques.

Published

2005

37. A Synthetic Peptide Blocking the Apolipoprotein E/β-Amyloid Binding Mitigates β-Amyloid Toxicity and Fibril Formation in Vitro and Reduces β-Amyloid Plaques in Transgenic Mice

Author

Henrieta Scholtzova, Paul M. Mathews, Yong-Sheng Li, Stephen D. Schmidt, Marcin Sadowski, Thomas Wisniewski, James A. Ripellino, Joanna Pankiewicz, John D. Fryer, Einar M. Sigurdsson, and David M. Holtzman

Subjects

Male, Genetically modified mouse, Apolipoprotein E, Apolipoprotein B, Transgene, Mice, Transgenic, Peptide, Biology, Presenilin, Pathology and Forensic Medicine, Mice, Neuroblastoma, Apolipoproteins E, Alzheimer Disease, Presenilin-1, Tumor Cells, Cultured, medicine, Animals, Humans, Binding site, Mice, Knockout, chemistry.chemical_classification, Amyloid beta-Peptides, Binding Sites, Brain, Membrane Proteins, medicine.disease, Molecular biology, Competitive Bidding, Peptide Fragments, Mice, Inbred C57BL, chemistry, Blood-Brain Barrier, Astrocytes, Mutation, biology.protein, Female, Alzheimer's disease, Half-Life, Protein Binding, Regular Articles

Abstract

Alzheimer's disease (AD) is associated with accumulation of beta-amyloid (Abeta). A major genetic risk factor for sporadic AD is inheritance of the apolipoprotein (apo) E4 allele. ApoE can act as a pathological chaperone of Abeta, promoting its conformational transformation from soluble Abeta into toxic aggregates. We determined if blocking the apoE/Abeta interaction reduces Abeta load in transgenic (Tg) AD mice. The binding site of apoE on Abeta corresponds to residues 12 to 28. To block binding, we synthesized a peptide containing these residues, but substituted valine at position 18 to proline (Abeta12-28P). This changed the peptide's properties, making it non-fibrillogenic and non-toxic. Abeta12-28P competitively blocks binding of full-length Abeta to apoE (IC50 = 36.7 nmol). Furthermore, Abeta12-28P reduces Abeta fibrillogenesis in the presence of apoE, and Abeta/apoE toxicity in cell culture. Abeta12-28P is blood-brain barrier-permeable and in AD Tg mice inhibits Abeta deposition. Tg mice treated with Abeta12-28P for 1 month had a 63.3% reduction in Abeta load in the cortex (P = 0.0043) and a 59.5% (P = 0.0087) reduction in the hippocampus comparing to age-matched control Tg mice. Antibodies against Abeta were not detected in sera of treated mice; therefore the observed therapeutic effect of Abeta12-28P cannot be attributed to an antibody clearance response. Our experiments demonstrate that compounds blocking the interaction between Abeta and its pathological chaperones may be beneficial for treatment of beta-amyloid deposition in AD.

Published

2004

38. Abstract # 1852 Exercise-induced changes in gut microbiota alters response to colitis in mice: Clinical scores and body weight differences

Author

John D. Fryer, Purna C. Kashyap, C. Salmonson, J.A. Woods, Vandana Nehra, Bryan A. White, and Jacob M. Allen

Subjects

medicine.medical_specialty, biology, Endocrine and Autonomic Systems, Immunology, Free access, Inflammation, Gut flora, biology.organism_classification, Body weight, medicine.disease, digestive system, Gut microbiome, Behavioral Neuroscience, Endocrinology, Weight loss, Internal medicine, medicine, medicine.symptom, Colitis, Dextran sodium sulfate

Abstract

We have previously shown that voluntary exercise alters the gut microbiome and prevents inflammation in a mouse model of colitis. Here, we investigated whether exercise-induced changes in the gut microbiota plays a role. Donor C57Bl6/J mice ( n = 20) were given free access to a wheel ( n = 10) or remained sedentary ( n = 10) for six weeks. Mice were then euthanized, cecal contents were collected, pooled by treatment and gavage-fed to 65 germ-free C57Bl6/J mice housed in a gnotobiotic facility ( n = 32–33 in sedentary and exercise groups, respectively). After 4 weeks, half of the mice were administered 2% dextran sodium sulfate (DSS) in their water or remained as controls (water only). After 5 days, DSS-treated mice were switched to water for 3 days until euthanasia at day 8 (peak of symptoms). DSS caused significant weight loss over the 8-day period ( p p p

Published

2016

39. TIA1 Mutations in Amyotrophic Lateral Sclerosis and Frontotemporal Dementia Promote Phase Separation and Alter Stress Granule Dynamics

Author

Lorne Zinman, Carol F. Lippa, Ralph B. Perkerson, David Lacomis, Aishe Kurti, Billie J. Matchett, Cyril Pottier, J. Paul Taylor, Hong Joo Kim, Eileen H. Bigio, Heather Stewart, Zbigniew K. Wszolek, Leonard Petrucelli, M.-Marsel Mesulam, Elizabeth Finger, Kavya Annu, Ronald C. Petersen, Jamshid Temirov, Tanja Mittag, Charles Krieger, Rosa Rademakers, James Messing, Veronica Hirsch-Reinshagen, Ian R. A. Mackenzie, Sasha Zivkovic, Stephan Züchner, Alexandra M. Nicholson, Julia Keith, Ekaterina Rogaeva, Dennis W. Dickson, Neill R. Graff-Radford, Richard J. Caselli, Matt Baker, Melissa E. Murray, Kevin B. Boylan, Sandra Weintraub, Ging-Yuek Robin Hsiung, Masato Kato, Raymond P. Roos, John D. Fryer, Maria D. Purice, and Mohona Sarkar

Subjects

Adult, Male, 0301 basic medicine, Pathology, medicine.medical_specialty, Time Factors, TIA1, Heterogeneous Nuclear Ribonucleoprotein A1, Green Fluorescent Proteins, Neuropathology, Biology, Transfection, medicine.disease_cause, Poly(A)-Binding Proteins, Article, Pathogenesis, 03 medical and health sciences, Stress granule, Stress, Physiological, Heterogeneous-Nuclear Ribonucleoprotein Group A-B, mental disorders, medicine, Humans, Amyotrophic lateral sclerosis, Aged, Family Health, Genetics, Mutation, Microscopy, Confocal, General Neuroscience, Amyotrophic Lateral Sclerosis, nutritional and metabolic diseases, Frontotemporal lobar degeneration, Middle Aged, medicine.disease, T-Cell Intracellular Antigen-1, nervous system diseases, 3. Good health, DNA-Binding Proteins, 030104 developmental biology, Frontotemporal Dementia, RNA-Binding Protein FUS, Female, Human medicine, HeLa Cells, Frontotemporal dementia

Abstract

Summary Amyotrophic lateral sclerosis (ALS) and frontotemporal dementia (FTD) are age-related neurodegenerative disorders with shared genetic etiologies and overlapping clinical and pathological features. Here we studied a novel ALS/FTD family and identified the P362L mutation in the low-complexity domain (LCD) of T cell-restricted intracellular antigen-1 (TIA1). Subsequent genetic association analyses showed an increased burden of TIA1 LCD mutations in ALS patients compared to controls (p = 8.7 × 10 −6 ). Postmortem neuropathology of five TIA1 mutations carriers showed a consistent pathological signature with numerous round, hyaline, TAR DNA-binding protein 43 (TDP-43)-positive inclusions. TIA1 mutations significantly increased the propensity of TIA1 protein to undergo phase transition. In live cells, TIA1 mutations delayed stress granule (SG) disassembly and promoted the accumulation of non-dynamic SGs that harbored TDP-43. Moreover, TDP-43 in SGs became less mobile and insoluble. The identification of TIA1 mutations in ALS/FTD reinforces the importance of RNA metabolism and SG dynamics in ALS/FTD pathogenesis.

Published

2017

40. Voluntary and forced exercise differentially alters the gut microbiome in C57BL/6J mice

Author

Jeffrey A. Woods, Vandana Nehra, Bryan A. White, H. Rex Gaskins, Keith Whitlock, John D. Fryer, Brandt D. Pence, Jacob M. Allen, and Margret E. Berg Miller

Subjects

Male, Physiology, Colon, Microbial Consortia, Biology, Bioinformatics, Andrology, Cecum, Feces, Random Allocation, Physiology (medical), Physical Conditioning, Animal, medicine, Animals, Microbiome, Treadmill, Colitis, computer.programming_language, sed, Gastrointestinal Microbiome, Body Weight, medicine.disease, Mice, Inbred C57BL, Disease Models, Animal, medicine.anatomical_structure, Turnover, Sedentary Behavior, computer, Stress, Psychological

Abstract

We have previously shown that voluntary wheel running (VWR) attenuates, whereas forced treadmill running (FTR) exacerbates, intestinal inflammation and clinical outcomes in a mouse model of colitis. As the gut microbiome is implicated in colitis, we hypothesized that VWR and FTR would differentially affect the gut microbiome. Mice (9-10/treatment) were randomly assigned to VWR, FTR, or sedentary home cage control (SED) for 6 wk. VWR were given running wheel access, whereas FTR ran on a treadmill for 40 min/day at 8–12 m/min, 5% grade. Forty-eight hours after the last exercise session, DNA was isolated from the fecal pellets and cecal contents, and the conserved bacterial 16S rRNA gene was amplified and sequenced using the Illumina Miseq platform. Permutational multivariate analysis of variance based on weighted UniFrac distance matrix revealed different bacterial clusters between feces and cecal contents in all groups ( P < 0.01). Interestingly, the community structures of the three treatment groups clustered separately from each other in both gut regions ( P < 0.05). Contrary to our hypothesis, the α-diversity metric, Chao1, indicated that VWR led to reduced bacterial richness compared with FTR or SED ( P < 0.05). Taxonomic evaluation revealed that both VWR and FTR altered many individual bacterial taxa. Of particular interest, Turicibacter spp., which has been strongly associated with immune function and bowel disease, was significantly lower in VWR vs. SED/FTR. These data indicate that VWR and FTR differentially alter the intestinal microbiome of mice. These effects were observed in both the feces and cecum despite vastly different community structures between each intestinal region.

Published

2014

41. Dietary intervention rescues maternal obesity induced behavior deficits and neuroinflammation in offspring

Author

Aishe Kurti, John D. Fryer, Damien A. Fair, and Silvia S. Kang

Subjects

Male, medicine.medical_specialty, Offspring, Immunology, Enzyme-Linked Immunosorbent Assay, Biology, Diet, High-Fat, Real-Time Polymerase Chain Reaction, ASD, Cellular and Molecular Neuroscience, Mice, Neuroinflammation, Maternal obesity, Pregnancy, Lactation, Internal medicine, medicine, Attention deficit hyperactivity disorder, ADHD, Animals, Obesity, Inflammation, Behavior, Behavior, Animal, General Neuroscience, Research, Brain, medicine.disease, Immunohistochemistry, 3. Good health, Mice, Inbred C57BL, Dietary intervention, Endocrinology, medicine.anatomical_structure, Neurology, Autism spectrum disorder, Prenatal Exposure Delayed Effects, Gestation, Anxiety, Female, medicine.symptom

Abstract

Obesity induces a low-grade inflammatory state and has been associated with behavioral and cognitive alterations. Importantly, maternal environmental insults can adversely impact subsequent offspring behavior and have been linked with neurodevelopmental disorders such as autism spectrum disorder (ASD) and attention deficit hyperactivity disorder (AHDH). It is unknown if maternal obesity significantly alters offspring sociability, a key ASD feature, and if altering maternal diet will provide an efficacious intervention paradigm for behavioral deficits. Here we investigated the impact of maternal high fat diet (HFD) and maternal dietary intervention during lactation on offspring behavior and brain inflammation in mice. We found that maternal HFD increased anxiety and decreased sociability in female offspring. Additionally, female offspring from HFD-fed dams also exhibited increased brain IL-1β and TNFα and microglial activation. Importantly, maternal dietary intervention during lactation was sufficient to alleviate social deficits and brain inflammation. Maternal obesity during gestation alone was sufficient to increase hyperactivity in male offspring, a phenotype that was not ameliorated by dietary intervention. These data suggest that maternal HFD acts as a prenatal/perinatal insult that significantly impacts offspring behavior and inflammation and that dietary intervention during lactation may be an easily translatable, efficacious intervention to offset some of these manifestations. Electronic supplementary material The online version of this article (doi:10.1186/s12974-014-0156-9) contains supplementary material, which is available to authorized users.

Published

2014

42. Deficiency of Capicua disrupts bile acid homeostasis

Author

Yoontae Lee, Hoe Yune Jung, Daehee Hwang, Nahyun Choi, John D. Fryer, Jieon Lee, Jeehyun Yoe, Eunjeong Kim, Sungjun Park, Soeun Kim, Kyong-Tai Kim, Huda Y. Zoghbi, and Hyojin Kang

Subjects

medicine.medical_specialty, Genotype, medicine.drug_class, Biology, Article, Proinflammatory cytokine, Bile Acids and Salts, Mice, Cholestasis, Internal medicine, medicine, Animals, Homeostasis, Mice, Knockout, Pregnane X receptor, Multidisciplinary, Retinoid X receptor alpha, Bile acid, Gene Expression Profiling, medicine.disease, Repressor Proteins, Endocrinology, Phenotype, Gene Expression Regulation, Liver, Cytokines, Tumor necrosis factor alpha, Female, FOXA2, Inflammation Mediators, Blood Chemical Analysis, Transcription Factors

Abstract

Capicua (CIC) has been implicated in pathogenesis of spinocerebellar ataxia type 1 and cancer in mammals; however, the in vivo physiological functions of CIC remain largely unknown. Here we show that Cic hypomorphic (Cic-L-/-) mice have impaired bile acid (BA) homeostasis associated with induction of proinflammatory cytokines. We discovered that several drug metabolism and BA transporter genes were down-regulated in Cic-L-/- liver, and that BA was increased in the liver and serum whereas bile was decreased within the gallbladder of Cic-L-/- mice. We also found that levels of proinflammatory cytokine genes were up-regulated in Cic-L-/- liver. Consistent with this finding, levels of hepatic transcriptional regulators, such as hepatic nuclear factor 1 alpha (HNF1 alpha), CCAAT/enhancer-binding protein beta (C/EBP beta), forkhead box protein A2 (FOXA2), and retinoid X receptor alpha (RXR alpha), were markedly decreased in Cic-L-/- mice. Moreover, induction of tumor necrosis factor alpha (Tnf alpha) expression and decrease in the levels of FOXA2, C/EBP beta, and RXRa were found in Cic-L-/- liver before BA was accumulated, suggesting that inflammation might be the cause for the cholestasis in Cic-L-/- mice. Our findings indicate that CIC is a critical regulator of BA homeostasis, and that its dysfunction might be associated with chronic liver disease and metabolic disorders.

Published

2014

43. Clusterin contributes to caspase-3–independent brain injury following neonatal hypoxia-ischemia

Author

Robert P. Brendza, Laura L. Dugan, Malca Kierson, David M. Holtzman, Ronald Demattos, Byung Hee Han, Bruce J. Aronow, Judith A.K. Harmony, Jeong Sook Kim-Han, Kevin L. Quick, John D. Fryer, and John R. Cirrito

Subjects

Pathology, medicine.medical_specialty, Programmed cell death, Blotting, Western, Ischemia, Fluorescent Antibody Technique, Caspase 3, General Biochemistry, Genetics and Molecular Biology, Mice, In vivo, medicine, Animals, Microscopy, Immunoelectron, Glycoproteins, Mice, Knockout, Cell Death, Clusterin, biology, Brain, Colocalization, General Medicine, medicine.disease, eye diseases, Mice, Inbred C57BL, Blot, Animals, Newborn, Apoptosis, Caspases, Hypoxia-Ischemia, Brain, biology.protein, Cancer research, sense organs, Molecular Chaperones

Abstract

Clusterin, also known as apolipoprotein J, is a ubiquitously expressed molecule thought to influence a variety of processes including cell death. In the brain, it accumulates in dying neurons following seizures and hypoxic-ischemic (H-I) injury. Despite this, in vivo evidence that clusterin directly influences cell death is lacking. Following neonatal H-I brain injury in mice (a model of cerebral palsy), there was evidence of apoptotic changes (neuronal caspase-3 activation), as well as accumulation of clusterin in dying neurons. Clusterin-deficient mice had 50% less brain injury following neonatal H-I. Surprisingly, the absence of clusterin had no effect on caspase-3 activation, and clusterin accumulation and caspase-3 activation did not colocalize to the same cells. Studies with cultured cortical neurons demonstrated that exogenous purified astrocyte-secreted clusterin exacerbated oxygen/glucose-deprivation-induced necrotic death. These results indicate that clusterin may be a new therapeutic target to modulate non-caspase-dependent neuronal death following acute brain injury.

Published

2001

44. Differences in the A?40/A?42 ratio associated with cerebrospinal fluid lipoproteins as a function of apolipoprotein E genotype

Author

Linda H. Younkin, Anne M. Fagan, Steven G. Younkin, John D. Fryer, Thomas G. Cole, John C. Morris, and David M. Holtzman

Subjects

Apolipoprotein E, medicine.medical_specialty, Cholesterol, Lipid metabolism, Biology, medicine.disease, Central nervous system disease, chemistry.chemical_compound, Cerebrospinal fluid, Endocrinology, Neurology, chemistry, Internal medicine, mental disorders, Genotype, medicine, lipids (amino acids, peptides, and proteins), Neurology (clinical), Alzheimer's disease, Lipoprotein

Abstract

The epsilon4 allele of apolipoprotein E (ApoE) is a risk factor for Alzheimer's disease (AD). ApoE, which is important for lipid metabolism, is also a major constituent of cerebrospinal fluid (CSF) lipoproteins (LPs). Although ApoE in the CSF is derived from the central nervous system, the relation between LP metabolism in plasma and CSF is not clear. Soluble amyloid-beta (Abeta) protein may normally be associated with CSF LPs. It is converted in AD to a fibrillar form in brain parenchyma. ApoE and CSF LPs may regulate this process. The purpose of this study was to characterize CSF LPs from healthy, cognitively normal, fasted, elderly individuals at different risk for AD based on ApoE genotype. Lipid composition of CSF LPs did not differ with ApoE genotype. Interestingly, plasma and CSF high-density lipoprotein (HDL) cholesterol and apolipoprotein AI (ApoAI) levels were correlated. Importantly, as assessed by size-exclusion chromatography, Abeta in CSF coeluted in fractions containing LPs and was influenced by ApoE genotype: E4-positive subjects displayed significant elevations in Abeta40/Abeta42 ratios. These results suggest that plasma ApoAI/HDL levels can influence CSF ApoAI/HDL levels and that interactions between Abeta and central nervous system LPs may reflect changes in brain Abeta metabolism before the onset of clinical disease.

Published

2000

45. Autophagy in astrocytes: a novel culprit in lysosomal storage disorders

Author

Andrea Ballabio, John D. Fryer, Chiara Di Malta, Carmine Settembre, Di Malta, C, Fryer, Jd, Settembre, Carmine, and Ballabio, Andrea

Subjects

Cell type, Autophagosome maturation, Biology, Mice, Purkinje Cells, Multiple sulfatase deficiency, Lysosome, Phagosomes, medicine, Autophagy, Animals, Molecular Biology, Phagosome, Inflammation, Neurodegeneration, Cell Biology, medicine.disease, Autophagic Punctum, Cell biology, Lysosomal Storage Diseases, medicine.anatomical_structure, Astrocytes, Sulfatases, Lysosomes, Astrocyte

Abstract

Neurodegeneration is a prominent feature of lysosomal storage disorders (LSDs). Emerging data identify autophagy dysfunction in neurons as a major component of the phenotype. However, the autophagy pathway in the CNS has been studied predominantly in neurons, whereas in other cell types it has been largely unexplored. We studied the lysosome-autophagic pathway in astrocytes from a murine model of multiple sulfatase deficiency (MSD), a severe form of LSD. Similar to what was observed in neurons, we found that lysosomal storage in astrocytes impairs autophagosome maturation and this, in turn, has an impact upon the survival of cortical neurons and accounts for some of the neurological features found in MSD. Thus, our data indicate that lysosomal/autophagic dysfunction in astrocytes is an important component of neurodegeneration in LSDs.

Published

2012

46. Astrocyte dysfunction triggers neurodegeneration in a lysosomal storage disorder

Author

Andrea Ballabio, Carmine Settembre, John D. Fryer, Chiara Di Malta, Di Malta, C, Fryer, Jd, Settembre, Carmine, and Ballabio, Andrea

Subjects

Lysosomal Storage Diseases, Nervous System, Cell Survival, Multiple Sulfatase Deficiency Disease, Endocrinology, Diabetes and Metabolism, Cell Communication, Biology, Biochemistry, Mice, Purkinje Cells, Endocrinology, In vivo, Multiple sulfatase deficiency, Lysosome, Cerebellum, Genetics, medicine, Animals, Oxidoreductases Acting on Sulfur Group Donors, Molecular Biology, Neuroinflammation, Cells, Cultured, Cerebral Cortex, Neurons, Multidisciplinary, business.industry, Neurodegeneration, Autophagy, medicine.disease, Mice, Mutant Strains, Mice, Inbred C57BL, Microscopy, Electron, medicine.anatomical_structure, PNAS Plus, Astrocytes, Nerve Degeneration, Sulfatases, business, Lysosomes, Neuroscience, Ex vivo, Astrocyte

Abstract

The role of astrocytes in neurodegenerative processes is increasingly appreciated. Here we investigated the contribution of astrocytes to neurodegeneration in multiple sulfatase deficiency (MSD), a severe lysosomal storage disorder caused by mutations in the sulfatase modifying factor 1 ( SUMF1 ) gene. Using Cre/Lox mouse models, we found that astrocyte-specific deletion of Sumf1 in vivo induced severe lysosomal storage and autophagy dysfunction with consequential cytoplasmic accumulation of autophagic substrates. Lysosomal storage in astrocytes was sufficient to induce degeneration of cortical neurons in vivo. Furthermore, in an ex vivo coculture assay, we observed that Sumf1 −/− astrocytes failed to support the survival and function of wild-type cortical neurons, suggesting a non-cell autonomous mechanism for neurodegeneration. Compared with the astrocyte-specific deletion of Sumf1 , the concomitant removal of Sumf1 in both neurons and glia in vivo induced a widespread neuronal loss and robust neuroinflammation. Finally, behavioral analysis of mice with astrocyte-specific deletion of Sumf1 compared with mice with Sumf1 deletion in both astrocytes and neurons allowed us to link a subset of neurological manifestations of MSD to astrocyte dysfunction. This study indicates that astrocytes are integral components of the neuropathology in MSD and that modulation of astrocyte function may impact disease course.

Published

2012

47. Partial loss of ataxin-1 function contributes to transcriptional dysregulation in spinocerebellar ataxia type 1 pathogenesis

Author

Juan Crespo-Barreto, John D. Fryer, Chad A. Shaw, Harry T. Orr, and Huda Y. Zoghbi

Subjects

Cancer Research, Spinocerebellar Ataxia Type 1, Transcription, Genetic, lcsh:QH426-470, Ataxin 1, Nerve Tissue Proteins, Biology, Pathogenesis, Mice, 03 medical and health sciences, 0302 clinical medicine, Cerebellum, Genetics, medicine, Animals, Spinocerebellar Ataxias, RNA, Messenger, Molecular Biology, Cell Biology/Gene Expression, Neurological Disorders/Movement Disorders, Ataxin-1, Genetics (clinical), Ecology, Evolution, Behavior and Systematics, Loss function, Oligonucleotide Array Sequence Analysis, 030304 developmental biology, Mice, Knockout, Regulation of gene expression, 0303 health sciences, Neuroscience/Behavioral Neuroscience, Gene Expression Profiling, Nuclear Proteins, Polyglutamine tract, medicine.disease, 3. Good health, Genetics and Genomics/Gene Function, lcsh:Genetics, Genetics and Genomics/Disease Models, Neurological Disorders/Neurogenetics, Ataxins, Gene Expression Regulation, Ataxin, Spinocerebellar ataxia, biology.protein, 030217 neurology & neurosurgery, Research Article

Abstract

Spinocerebellar ataxia type 1 (SCA1) is a dominantly inherited neurodegenerative disease caused by expansion of a CAG repeat that encodes a polyglutamine tract in ATAXIN1 (ATXN1). Molecular and genetic data indicate that SCA1 is mainly caused by a gain-of-function mechanism. However, deletion of wild-type ATXN1 enhances SCA1 pathogenesis, whereas increased levels of an evolutionarily conserved paralog of ATXN1, Ataxin 1-Like, ameliorate it. These data suggest that a partial loss of ATXN1 function contributes to SCA1. To address this possibility, we set out to determine if the SCA1 disease model (Atxn1154Q/+ mice) and the loss of Atxn1 function model (Atxn1−/− mice) share molecular changes that could potentially contribute to SCA1 pathogenesis. To identify transcriptional changes that might result from loss of function of ATXN1 in SCA1, we performed gene expression microarray studies on cerebellar RNA from Atxn1−/− and Atxn1154Q/+ cerebella and uncovered shared gene expression changes. We further show that mild overexpression of Ataxin-1-Like rescues several of the molecular and behavioral defects in Atxn1 −/− mice. These results support a model in which Ataxin 1-Like overexpression represses SCA1 pathogenesis by compensating for a partial loss of function of Atxn1. Altogether, these data provide evidence that partial loss of Atxn1 function contributes to SCA1 pathogenesis and raise the possibility that loss-of-function mechanisms contribute to other dominantly inherited neurodegenerative diseases., Author Summary Spinocerebellar Ataxia type 1 (SCA1) is one of nine neurodegenerative diseases caused by an increase in the number of the amino acid glutamine in their respective proteins. Genetic studies have pointed to the fact that the glutamine expansion in Ataxin-1 causes SCA1 by causing Ataxin-1 to gain some function(s). Here, we demonstrate that in addition to the toxic gain-of-function mechanism, partial loss of the normal functions of Ataxin-1 contributes to SCA1. Ataxin-1 forms protein complexes with Capicua, a protein that silences expression of other genes, and we found that in SCA1 mouse models the levels of these complexes are reduced, resulting in increased expression of some genes. We also demonstrate that increased levels of Ataxin-1-Like, a protein that is similar to Ataxin-1 and protects against mutant Ataxin-1 in mice, rescues molecular and behavioral defects in mice deficient in Ataxin-1. These results show that Ataxin-1-Like compensates for loss of Ataxin-1 and that Ataxin-1 and Ataxin-1-Like share some normal functions. Together, these findings suggest that rescue of SCA1 symptoms by Ataxin-1-Like could be partly due to restoration of lost normal functions of Ataxin-1 in mice that express the mutant polyglutamine-expanded Ataxin-1.

Published

2010

48. Duplication of Atxn1l suppresses SCA1 neuropathology by decreasing incorporation of polyglutamine-expanded ataxin-1 into native complexes

Author

Yung C. Lam, Harry T. Orr, Juliette J. Kahle, Paymaan Jafar-Nejad, Huda Y. Zoghbi, Hung Kai Chen, Ronald Richman, Aaron B. Bowman, Rodney C. Samaco, and John D. Fryer

Subjects

Spinocerebellar Ataxia Type 1, Mutant, Molecular Sequence Data, Ataxin 1, Mice, Transgenic, Nerve Tissue Proteins, Neuropathology, Biology, Models, Biological, Mice, Purkinje Cells, Cerebellum, Gene duplication, Genetics, medicine, Animals, Spinocerebellar Ataxias, Gene, Ataxin-1, Cells, Cultured, Embryonic Stem Cells, Mice, Knockout, DNA Repeat Expansion, Models, Genetic, Neurodegeneration, Nuclear Proteins, medicine.disease, Cell biology, Glutamine, Mice, Inbred C57BL, Repressor Proteins, Ataxins, biology.protein, Peptides

Abstract

Spinocerebellar ataxia type 1 (SCA1) is a dominantly inherited neurodegenerative disease caused by expansion of a glutamine tract in ataxin-1 (ATXN1). SCA1 pathogenesis studies support a model in which the expanded glutamine tract causes toxicity by modulating the normal activities of ATXN1. To explore native interactions that modify the toxicity of ATXN1, we generated a targeted duplication of the mouse ataxin-1-like (Atxn1l, also known as Boat) locus, a highly conserved paralog of SCA1, and tested the role of this protein in SCA1 pathology. Using a knock-in mouse model of SCA1 that recapitulates the selective neurodegeneration seen in affected individuals, we found that elevated Atxn1l levels suppress neuropathology by displacing mutant Atxn1 from its native complex with Capicua (CIC). Our results provide genetic evidence that the selective neuropathology of SCA1 arises from modulation of a core functional activity of ATXN1, and they underscore the importance of studying the paralogs of genes mutated in neurodegenerative diseases to gain insight into mechanisms of pathogenesis.

Published

2006

49. The bad seed in Alzheimer's disease

Author

David M. Holtzman and John D. Fryer

Subjects

Pathology, medicine.medical_specialty, Amyloid, Neuroscience(all), Transgene, Mice, Transgenic, Plaque, Amyloid, Disease, Mice, In vivo, Alzheimer Disease, mental disorders, Amyloid precursor protein, Medicine, Animals, Humans, Amyloid beta-Peptides, biology, business.industry, General Neuroscience, medicine.disease, Peptide Fragments, Cerebral Amyloid Angiopathy, Disease Models, Animal, medicine.anatomical_structure, Amyloid deposition, biology.protein, Neuron, Cerebral amyloid angiopathy, business, Neuroscience

Abstract

In this issue of Neuron, McGowan et al. report on a new mouse model of amyloid deposition as occurs in Alzheimer's disease. Unlike previous models in which overexpression of the amyloid precursor protein results in amyloid plaque formation, McGowan et al. have produced mice that overexpress only Abeta40 or Abeta42 and prove that Abeta42 is critical for the formation of amyloid deposits in vivo.

Published

2005

50. The low density lipoprotein receptor regulates the level of central nervous system human and murine apolipoprotein E but does not modify amyloid plaque pathology in PDAPP mice

Author

Guojun Bu, David M. Holtzman, Kelly R. Bales, Michael L. Spinner, Patrick Sullivan, Ronald B. DeMattos, John D. Fryer, Mark Odell, Steven M. Paul, Maia Parsadanian, and Lynn M. McCormick

Subjects

Apolipoprotein E, medicine.medical_specialty, Central nervous system, Biology, Endocytosis, Biochemistry, Amyloid beta-Protein Precursor, Mice, Cerebrospinal fluid, Apolipoproteins E, Alzheimer Disease, Internal medicine, medicine, Extracellular, Animals, Humans, Receptor, Molecular Biology, Mice, Knockout, Brain, Cell Biology, medicine.disease, Mice, Inbred C57BL, Disease Models, Animal, Endocrinology, medicine.anatomical_structure, Receptors, LDL, LDL receptor, lipids (amino acids, peptides, and proteins), Alzheimer's disease

Abstract

Apolipoprotein E (apoE), a chaperone for the amyloid beta (Abeta) peptide, regulates the deposition and structure of Abeta that deposits in the brain in Alzheimer disease (AD). The primary apoE receptor that regulates levels of apoE in the brain is unknown. We report that the low density lipoprotein receptor (LDLR) regulates the cellular uptake and central nervous system levels of astrocyte-derived apoE. Cells lacking LDLR were unable to appreciably endocytose astrocyte-secreted apoE-containing lipoprotein particles. Moreover, cells overexpressing LDLR showed a dramatic increase in apoE endocytosis and degradation. We also found that LDLR knock-out (Ldlr-/-) mice had a significant, approximately 50% increase in the level of apoE in the cerebrospinal fluid and extracellular pools of the brain. However, when the PDAPP mouse model of AD was bred onto an Ldlr-/- background, we did not observe a significant change in brain Abeta levels either before or after the onset of Abeta deposition. Interestingly, human APOE3 or APOE4 (but not APOE2) knock-in mice bred on an Ldlr-/- background had a 210% and 380% increase, respectively, in the level of apoE in cerebrospinal fluid. These results demonstrate that central nervous system levels of both human and murine apoE are directly regulated by LDLR. Although the increase in murine apoE caused by LDLR deficiency was not sufficient to affect Abeta levels or deposition by 10 months of age in PDAPP mice, it remains a possibility that the increase in human apoE3 and apoE4 levels caused by LDLR deficiency will affect this process and could hold promise for therapeutic targets in AD.

Published

2005