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TaubCONNECT Research Perspective:
December 2024
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Regulation of Synapse Density by Pumilio RNA-Binding Proteins
CD33 and SHP-1/PTPN6 Interaction in Alzheimer's Disease
Cellular Communities Reveal Trajectories of Brain Ageing and Alzheimer's Disease
Epigenetic and Genetic Risk of Alzheimer Disease from Autopsied Brains in two Ethnic Groups
Multi-Omic Analysis of Huntington's Disease Reveals a Compensatory Astrocyte State
Design and Methods of the Early Age-Related Hearing Loss Investigation Randomized Controlled Trial
Updated Safety Results From Phase 3 Lecanemab Study in Early Alzheimer's Disease
The Broken Alzheimer's Disease Genome
Rare Genetic Variation in Fibronectin 1 (FN1) Protects Against APOEε4 in Alzheimer's Disease
Cell Subtype-Specific Effects of Genetic Variation in the Alzheimer's Disease Brain
Diet, Pace of Biological Aging, and Risk of Dementia in the Framingham Heart Study
A Comparative Study of Structural Variant Calling in WGS from Alzheimer's Disease Families
Glucocorticoid Stress Hormones Stimulate Vesicle-Free Tau Secretion and Spreading in the Braint
The Effects of Insufficient Sleep and Adequate Sleep on Cognitive Function in Healthy Adults
ZCCHC17 Modulates Neuronal RNA Splicing and Supports Cognitive Resilience in Alzheimer's Disease
Effects of Lithium on Serum Brain-Derived Neurotrophic Factor in Alzheimer's Patients with Agitation
2023 Taub Institute Grants for Emerging Research (TIGER) Awardees!
Rie1 and Sgn1 Form an RNA-Binding Complex that Enforces the Meiotic Entry Cell Fate Decision
Memory and Language Cognitive Data Harmonization Across the United States and Mexico
Education as a Moderator of Help Seeking Behavior in Subjective Cognitive Decline
Multicellular Communities are Perturbed in the Aging Human Brain and Alzheimer's Disease
The Neuropathological Landscape of Hispanic and non-Hispanic White Decedents with Alzheimer Disease
The Early-Onset Alzheimer's Disease Whole-Genome Sequencing Project: Study Design and Methodology
Polygenic Risk Score Penetrance & Recurrence Risk in Familial Alzheimer Disease
High School Quality is Associated with Cognition 58 Years Later
Glucocorticoid-Driven Mitochondrial Damage Stimulates Tau Pathology
A Global View of the Genetic Basis of Alzheimer Disease
ARIA in Patients Treated with Lecanemab (BAN2401) in a Phase 2 Study in Early Alzheimer's Disease
Microglia Reactivity Entails Microtubule Remodeling from Acentrosomal to Centrosomal Arrays
Genuine Selective Caspase-2 Inhibition with new Irreversible Small Peptidomimetics
Cell Type-Specific Changes Identified by Single-Cell Transcriptomics in Alzheimer's Disease
Brain Aging Among Racially and Ethnically Diverse Middle-Aged and Older Adults
First Place: Neuroproteasome Localization and Dysfunction Modulate Pathology in Alzheimer's Disease
Clearance of an Amyloid-Like Translational Repressor is Governed by 14-3-3 Proteins
Diet Moderates the Effect of Resting State Functional Connectivity on Cognitive Function
Retromer Deficiency in Tauopathy Models Enhances the Truncation and Toxicity of Tau
Progranulin Mutations in Clinical and Neuropathological Alzheimer's Disease
Wolframin is a Novel Regulator of Tau Pathology and Neurodegeneration
Homotypic Fibrillization of TMEM106B Across Diverse Neurodegenerative Diseases
Correlation of Plasma and Neuroimaging Biomarkers in Alzheimer's Disease
Tubulin Tyrosination Regulates Synaptic Function and is Disrupted in Alzheimer's Disease
The Penalty of Stress - Epichaperomes Negatively Reshaping the Brain in Neurodegenerative Disorders
The Neuronal Retromer can Regulate Both Neuronal and Microglial Phenotypes of Alzheimer's Disease
Deep Learning Improves Utility of Tau PET in the Study of Alzheimer's Disease
Age of Onset of Huntington's Disease in Carriers of Reduced Penetrance Alleles
Caspase-9: A Multimodal Therapeutic Target With Diverse Cellular Expression in Human Disease
Midlife Vascular Factors and Prevalence of Mild Cognitive Impairment in Late-Life in Mexico
The Association Between Sex and Risk of Alzheimer's Disease in Adults with Down Syndrome
Marked Mild Cognitive Deficits in Humanized Mouse Model of Alzheimer's-Type Tau Pathology
Rapid ATF4 Depletion Resets Synaptic Responsiveness after cLTP
Polygenic Risk Score for Alzheimer's Disease in Caribbean Hispanics
Recognition Memory and Divergent Cognitive Profiles in Prodromal Genetic Frontotemporal Dementia
The Microtubule Cytoskeleton at the Synapse & The Synaptic Life of Microtubules
Optimizing Subjective Cognitive Decline to Detect Early Cognitive Dysfunction
The AD Tau Core Spontaneously Self-Assembles and Recruits Full-Length Tau to Filaments
Olfactory Impairment is Related to Tau Pathology and Neuroinflammation in Alzheimer's Disease
Pathogenic Role of Delta 2 Tubulin in Bortezomib-Induced Peripheral Neuropathy
1: Synaptic and Cognitive Impairment Associated with L444P Heterozygous Glucocerebrosidase Mutation
2: Elevated Expression of the Retrotransposon LINE-1 Drives Alzheimer's Disease-Associated Microglial Dysfunction
3: "Rest of the Folks are Tired and Weary": The Impact of Historical Lynchings on Biological and Cognitive Health for Older Adults Racialized as Black
2: Elevated Expression of the Retrotransposon LINE-1 Drives Alzheimer's Disease-Associated Microglial Dysfunction
3: "Rest of the Folks are Tired and Weary": The Impact of Historical Lynchings on Biological and Cognitive Health for Older Adults Racialized as Black
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| Wudu Lado, PhD | Ahrom Ham, PhD | |
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| Hongyu Li, PhD | Guomei Tang, PhD |
Synaptic and Cognitive Impairment Associated with L444P Heterozygous Glucocerebrosidase Mutation
Cognitive impairment is a prevalent yet insufficiently understood non-motor feature of Parkinson's disease (PD), significantly reducing patients' functional abilities and quality of life. The underlying mechanisms of cognitive decline in PD remain unclear, hindering effective prevention and treatment approaches. To address this knowledge gap, our team, including co-first authors Wudu Lado, Ahrom Ham, and Hongyu Li, explored the molecular and cellular processes contributing to cognitive impairment linked to heterozygous mutations in GBA1, the primary genetic risk factor for PD.
Figure 1. Mutations in GBA1 are the strongest genetic risk factor for Parkinson's disease. Lado et al report that GBA1 mutation perturbs hippocampal synaptic structure and function and causes cognitive impairment without motor deficits. When α-synuclein overexpression, this mutation synergizes with αSyn pathology, accelerating cognitive decline and motor symptoms associated with Parkinson's disease
GBA1 encodes glucocerebrosidase (GCase), a lysosomal enzyme responsible for breaking down glucosylceramide into glucose and ceramide. As recently reported in BRAIN, in collaboration with the laboratories of Drs. Serge Przedborski, Arancio Ottavio, and Roy Alcalay, we utilized the Gba1L444P/+ mouse model to demonstrate that the heterozygous L444P Gba1 mutation (L444P/+) induces deficits in hippocampus-dependent spatial and reference memory. These effects occur independently of α-synuclein (αSyn) aggregation, lipid substrate accumulation of GCase, dopaminergic dysfunction, or motor impairments. The mutation impairs hippocampal synaptic plasticity and basal synaptic transmission by reducing the density of CA3-CA1 synapses in the hippocampus, a process that is distinct from αSyn-driven presynaptic neurotransmitter release dysfunction.
In a Thy1-αSyn pre-symptomatic PD mouse model, which overexpresses human αSyn, we observed that the L444P/+ mutation intensifies hippocampal αSyn accumulation, synaptic abnormalities, and cognitive deficits in young double mutant Gba1L444P/+:Thy1-αSyn mice. As the Thy1-αSyn mice age, motor impairments emerge, and double mutant mice experience more severe synaptic and motor impairments compared to Thy1-αSyn mice alone.
Taken together, our findings indicate that the heterozygous L444P GBA1 mutation disrupts hippocampal synaptic structure and function, contributing to a subclinical burden for cognitive impairment. When coupled with αSyn overexpression, this mutation synergizes with αSyn pathology, accelerating cognitive decline and motor symptoms associated with Parkinson's disease.
Guomei Tang, PhD
Assistant Professor of Neurological Sciences (in Neurology)
gt2107@cumc.columbia.edu
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| Nainika Roy, PhD | Jason C. Ngo | Falak Sher, PhD |
Transposable elements, once dismissed as "junk DNA," are now recognized as critical regulators of cellular function and dysfunction. Among these, long interspersed nuclear element-1 (LINE-1) is the most abundant retrotransposon in the human genome, comprising approximately 17% of our DNA. LINE-1 activity is typically suppressed in healthy cells, but aging and pathological states, such as Alzheimer’s disease (AD), can lead to its aberrant activation. This dysregulation raises fascinating questions about the role of LINE-1 in brain aging and neurodegeneration, making it a promising target for research into mechanisms underlying AD.
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Figure. (A) Representative images showing LINE-1 ORF1p (red) protein expression in neurons (NeuN), microglia (IBA1), oligodendrocytes (CNPase), and astrocytes (GFAP) in dorsolateral prefrontal cortex (DLPFC) of an aged human brain. (B) Representative images of microglia and LINE-1 (ORF1p) staining in postmortem brain tissues from cognitively healthy controls (C) and LOAD patients, highlighting microglial morphology and LINE-1 activity. Scale bars: 10 µm.
In a study spearheaded by recent PhD graduate Dr. Nainika Roy, my laboratory explored the role of elevated LINE-1 activity in microglial dysfunction associated with late-onset Alzheimer’s disease (LOAD). Published in Acta Neuropathologica, our research utilized human postmortem brain tissue and a next-generation CRISPR-activation system in iPSC-derived microglia to uncover a significant link between heightened LINE-1 expression and disease-relevant microglial changes. These changes include impaired phagocytosis of amyloid-beta, altered cytokine secretion, and disrupted lipid metabolism—key processes essential for preserving brain health. Our findings highlight aberrant LINE-1 activity as a potential driver of microglial dysfunction and a contributing factor to Alzheimer’s disease pathogenesis.
This study highlights the underappreciated role of LINE-1 in neurodegenerative processes and opens new avenues for therapeutic interventions. By targeting LINE-1 activity, we may uncover novel strategies to mitigate neuroinflammation and restore microglial function in Alzheimer’s disease. This work reflects the innovative approaches pursued at TAUB Institute to advance the understanding of complex brain disorders and translate these insights into actionable treatments.
Falak Sher, PhD
Assistant Professor of Neurological Sciences (in Neurology and in the Taub Institute)
fs2644@cumc.columbia.edu
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Paris Adkins-Jackson, PhD, MPH | Jennifer J. Manly, PhD |
Our recent publication in Social Science and Medicine estimates the association between a common experience of modern older adults, historical lynchings, and markers for Alzheimer’s disease risk like poor cognitive performance and elevated systemic inflammation (via C-reactive protein). This study began as an exploration of common historical experiences that modern older adults lived through. For many marginalized groups, lynchings are not a distant historical event. A lynching is the murder of individual by another individual or group based on racial prejudice. This act was most often committed by people racialized as White towards people racialized as Black following the Emancipation Proclamation through to the present.
Figure 1. Conceptual model of hypothesized pathway of proportion of historic lynchings on C-reactive protein and cognitive test performance.
Previous literature on lynchings suggests most occurred between 1882-1968, which means modern older adults racialized as Black might have experienced this phenomenon or grew up hearing about it. With this premise, and our earlier studies that suggest both before birth and early life exposures play a role in cognitive decline, we explored the association of historical lynchings between 1882-1968 with cognitive performance and systemic inflammation in mid-late life.
Our findings suggest adults racialized as Black experience greater systemic inflammation and lower cognitive performance in mid-late life when they live in states where a greater proportion of people racialized as Black were lynched between 1882-1968, compared to participants living in states with lower proportions of lynchings. This relationship demonstrates the link between historical experiences and mid-late life health consequences for modern older adults.
Paris Adkins-Jackson, PhD, MPH
Assistant Professor of Epidemiology and Sociomedical Sciences
pa2629@cumc.columbia.edu
Jennifer J. Manly, PhD
Professor of Neuropsychology (in Neurology, the Sergievsky Center, and the Taub Institute)
jjm71@cumc.columbia.edu
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