Your search keyword '"Vaishnavi, Sanjeev"' showing total 5 results

1. Multimodal in vivo and postmortem assessments of tau in Lewy body disorders

Author

Coughlin, David G, Phillips, Jeffrey S, Roll, Emily, Peterson, Claire, Lobrovich, Rebecca, Rascovsky, Katya, Ungrady, Molly, Wolk, David A, Das, Sandhitsu, Weintraub, Daniel, Lee, Edward B, Trojanowski, John Q, Shaw, Leslie M, Vaishnavi, Sanjeev, Siderowf, Andrew, Nasrallah, Ilya M, Irwin, David J, McMillan, Corey T, and Initiative, Alzheimer’s Disease Neuroimaging

Subjects

Biomedical and Clinical Sciences, Clinical Sciences, Acquired Cognitive Impairment, Clinical Research, Neurodegenerative, Brain Disorders, Alzheimer's Disease including Alzheimer's Disease Related Dementias (AD/ADRD), Aging, Alzheimer's Disease Related Dementias (ADRD), Neurosciences, Lewy Body Dementia, Biomedical Imaging, Dementia, Alzheimer's Disease, 2.1 Biological and endogenous factors, 4.2 Evaluation of markers and technologies, Neurological, Alzheimer Disease, Autopsy, Biomarkers, Carbolines, Cognition, Female, Humans, Lewy Body Disease, Male, Positron-Emission Tomography, Severity of Illness Index, tau Proteins, Lewy body diseases, PET imaging, Tau, CSF, Neuropathology, Alzheimer’s Disease Neuroimaging Initiative, Neurology & Neurosurgery, Biological psychology

Abstract

We compared regional retention of 18F-flortaucipir between 20 patients with Lewy body disorders (LBD), 12 Alzheimer's disease patients with positive amyloid positron emission tomography (PET) scans (AD+Aβ) and 15 healthy controls with negative amyloid PET scans (HC-Aβ). In LBD subjects, we compared the relationship between 18F-flortaucipir retention and cerebrospinal fluid (CSF) tau, cognitive performance, and neuropathological tau at autopsy. The LBD cohort was stratified using an Aβ42 cut-off of 192 pg/mL to enrich for groups likely harboring tau pathology (LBD+Aβ = 11, LBD-Aβ = 9). 18F-flortaucipir retention was higher in LBD+AB than HC-Aβ in five, largely temporal-parietal regions with sparing of medial temporal regions. Higher retention was associated with higher CSF total-tau levels (p = 0.04), poorer domain-specific cognitive performance (p = 0.02-0.04), and greater severity of neuropathological tau in corresponding regions. While 18F-flortaucipir retention in LBD is intermediate between healthy controls and AD, retention relates to cognitive impairment, CSF total-tau, and neuropathological tau. Future work in larger autopsy-validated cohorts is needed to define LBD-specific tau biomarker profiles.

Published

2020

2. Tau immunotherapy is associated with glial responses in FTLD-tau

Author

Kim, Boram, Mikytuck, Bailey, Suh, Eunran, Gibbons, Garrett S., Van Deerlin, Vivianna M., Vaishnavi, Sanjeev N., Spindler, Meredith A., Massimo, Lauren, Grossman, Murray, Trojanowski, John Q., Irwin, David J., and Lee, Edward B.

Published

2021

3. Biological effects of sodium phenylbutyrate and taurursodiol in Alzheimer's disease.

Author

Arnold, Steven E., Hendrix, Suzanne, Nicodemus‐Johnson, Jessie, Knowlton, Newman, Williams, Victoria J., Burns, Jeffrey M., Crane, Monica, McManus, Alison J., Vaishnavi, Sanjeev N., Arvanitakis, Zoe, Neugroschl, Judith, Bell, Karen, Trombetta, Bianca A., Carlyle, Becky C., Kivisäkk, Pia, Dodge, Hiroko H., Tanzi, Rudolph E., Yeramian, Patrick D., and Leslie, Kent

Subjects

TAU proteins, ALZHEIMER'S disease, MAGNETIC resonance imaging, MILD cognitive impairment, TREATMENT effectiveness, MITOCHONDRIAL pathology

Abstract

INTRODUCTION: Sodium phenylbutyrate and taurursodiol (PB and TURSO) is hypothesized to mitigate endoplasmic reticulum stress and mitochondrial dysfunction, two of many mechanisms implicated in Alzheimer's disease (AD) pathophysiology. METHODS: The first‐in‐indication phase 2a PEGASUS trial was designed to gain insight into PB and TURSO effects on mechanistic targets of engagement and disease biology in AD. The primary clinical efficacy outcome was a global statistical test combining three endpoints relevant to disease trajectory (cognition [Mild/Moderate Alzheimer's Disease Composite Score], function [Functional Activities Questionnaire], and total hippocampal volume on magnetic resonance imaging). Secondary clinical outcomes included various cognitive, functional, and neuropsychiatric assessments. Cerebrospinal fluid (CSF) biomarkers spanning multiple pathophysiological pathways in AD were evaluated in participants with both baseline and Week 24 samples (exploratory outcome). RESULTS: PEGASUS enrolled 95 participants (intent‐to‐treat [ITT] cohort); cognitive assessments indicated significantly greater baseline cognitive impairment in the PB and TURSO (n = 51) versus placebo (n = 44) group. Clinical efficacy outcomes did not significantly differ between treatment groups in the ITT cohort. CSF interleukin‐15 increased from baseline to Week 24 within the placebo group (n = 34). In the PB and TURSO group (n = 33), reductions were observed in core AD biomarkers phosphorylated tau‐181 (p‐tau181) and total tau; synaptic and neuronal degeneration biomarkers neurogranin and fatty acid binding protein‐3 (FABP3); and gliosis biomarker chitinase 3‐like protein 1 (YKL‐40), while the oxidative stress marker 8‐hydroxy‐2‐deoxyguanosine (8‐OHdG) increased. Between‐group differences were observed for the Aβ42/40 ratio, p‐tau181, total tau, neurogranin, FABP3, YKL‐40, interleukin‐15, and 8‐OHdG. Additional neurodegeneration, inflammation, and metabolic biomarkers showed no differences between groups. DISCUSSION: While between‐group differences in clinical outcomes were not observed, most likely due to the small sample size and relatively short treatment duration, exploratory biomarker analyses suggested that PB and TURSO engages multiple pathophysiologic pathways in AD. Highlights: Proteostasis and mitochondrial stress play key roles in Alzheimer's disease (AD).Sodium phenylbutyrate and taurursodiol (PB and TURSO) targets these mechanisms.The PEGASUS trial was designed to assess PB and TURSO effects on biologic AD targets.PB and TURSO reduced exploratory biomarkers of AD and neurodegeneration.Supports further clinical development of PB and TURSO in neurodegenerative diseases. [ABSTRACT FROM AUTHOR]

Published

2024

4. Multimodal in vivo and postmortem assessments of tau in Lewy body disorders.

Author

Coughlin, David G., Phillips, Jeffrey S., Roll, Emily, Peterson, Claire, Lobrovich, Rebecca, Rascovsky, Katya, Ungrady, Molly, Wolk, David A., Das, Sandhitsu, Weintraub, Daniel, Lee, Edward B., Trojanowski, John Q., Shaw, Leslie M., Vaishnavi, Sanjeev, Siderowf, Andrew, Nasrallah, Ilya M., Irwin, David J., and McMillan, Corey T.

Subjects

*POSITRON emission tomography, *ALZHEIMER'S patients, *AUTOPSY, *COGNITION disorders, *AMYLOID

Abstract

We compared regional retention of 18F-flortaucipir between 20 patients with Lewy body disorders (LBD), 12 Alzheimer's disease patients with positive amyloid positron emission tomography (PET) scans (AD+Aβ) and 15 healthy controls with negative amyloid PET scans (HC−Aβ). In LBD subjects, we compared the relationship between 18F-flortaucipir retention and cerebrospinal fluid (CSF) tau, cognitive performance, and neuropathological tau at autopsy. The LBD cohort was stratified using an Aβ42 cut-off of 192 pg/mL to enrich for groups likely harboring tau pathology (LBD+Aβ = 11, LBD−Aβ = 9). 18F-flortaucipir retention was higher in LBD+AB than HC−Aβ in five, largely temporal-parietal regions with sparing of medial temporal regions. Higher retention was associated with higher CSF total-tau levels (p = 0.04), poorer domain-specific cognitive performance (p = 0.02–0.04), and greater severity of neuropathological tau in corresponding regions. While 18F-flortaucipir retention in LBD is intermediate between healthy controls and AD, retention relates to cognitive impairment, CSF total-tau, and neuropathological tau. Future work in larger autopsy-validated cohorts is needed to define LBD-specific tau biomarker profiles. • LBD has moderate intensity 18F-Flortaucipir retention in temporo-parietal regions. • LBD with low CSF Aβ42 has more regions of elevated 18F-Flortaucipir retention. • In LBD, 18F-Flortaucipir retention relates to CSF total-tau. • In LBD, regional 18F-Flortaucipir retention relates to cognitive dysfunction. • In LBD, neuropathologic tau is higher in regions with greater retention. [ABSTRACT FROM AUTHOR]

Published

2020

5. Neocortical origin and progression of gray matter atrophy in nonamnestic Alzheimer's disease.

Author

Phillips, Jeffrey S., Da Re, Fulvio, Dratch, Laynie, Xie, Sharon X., Irwin, David J., McMillan, Corey T., Vaishnavi, Sanjeev N., Ferrarese, Carlo, Lee, Edward B., Shaw, Leslie M., Trojanowski, John Q., Wolk, David A., and Grossman, Murray

Subjects

*ALZHEIMER'S disease, *CEREBRAL atrophy, *GRAY matter (Nerve tissue), *NEOCORTEX, *AMYLOID beta-protein, *PHENOTYPES, *TAU proteins, *PHYSIOLOGY

Abstract

Amnestic Alzheimer's disease (AD) is characterized by early atrophy of the hippocampus and medial temporal lobes before spreading to the neocortex. In contrast, nonamnestic Alzheimer's patients have relative sparing of the hippocampus, but the pattern in which the disease spreads is unclear. We examined spreading disease in nonamnestic AD using a novel magnetic resonance imaging–based analysis adapted from pathologic staging studies, applied here to cross-sectional imaging data. We selected 240 T1-weighted scans from 129 patients with pathology confirmed by autopsy or cerebrospinal fluid, and atrophy maps were computed relative to 238 scans from 115 elderly controls. For each phenotype, the frequency of atrophy in 116 brain regions was used to infer the anatomical origin of disease and its progression across 4 phases of atrophy. Results from the amnestic cohort were used to determine appropriate parameter settings for the phase assignment algorithm, based on correspondence to Braak pathology staging. Phase 1 regions, which represent the origin of disease, included the hippocampus for the amnestic group (comprising 33 scans); left lateral temporal lobe for logopenic-variant primary progressive aphasia (88 scans); occipitoparietal cortex for posterior cortical atrophy (51 scans); temporoparietal cortex for corticobasal syndrome (31 scans); and frontotemporal cortex for behavioral/dysexecutive variant AD (37 scans). In nonamnestic patients, atrophy spread to other neocortical areas in later phases, but the hippocampus exhibited only late-phase atrophy in posterior cortical atrophy and corticobasal syndrome. Region-specific phase values were also associated with regional measures of tau, beta amyloid, neuronal loss, and gliosis for the subset of patients (n = 17) with neuropathology findings; this comparison represented a first validation of the phase assignment algorithm. We subsequently assigned a phase to each patient scan based on the similarity of regional atrophy patterns with atrophy predicted for the corresponding phenotype at each phase. Scan-specific phases were correlated with disease duration as well as global and domain-specific cognition, supporting these phase values as global estimates of patients' disease progression. Logistic regression models based on spatial overlap with model-predicted atrophy patterns reliably discriminated nonamnestic phenotypes from each other and from amnestic AD. The frequency-based phase assignment algorithm used in the present study thus represents a promising approach for studying the neocortical origin and spread of disease in nonamnestic AD. [ABSTRACT FROM AUTHOR]

Published

2018