Your search keyword '"Keil, Allison"' showing total 13 results

1. Baseline characteristics of the North American prodromal Synucleinopathy cohort.

Author

Elliott, Jonathan, Lim, Miranda, Keil, Allison, Postuma, Ronald, Pelletier, Amelie, Gagnon, Jean-François, St Louis, Erik, Forsberg, Leah, Fields, Julie, Huddleston, Daniel, Bliwise, Donald, Avidan, Alon, Howell, Michael, Schenck, Carlos, McLeland, Jennifer, Criswell, Susan, Videnovic, Aleksandar, During, Emmanuel, Miglis, Mitchell, Shprecher, David, Lee-Iannotti, Joyce, Boeve, Bradley, and Ju, Yo-El

Subjects

Female, Humans, Male, Lewy Body Disease, Longitudinal Studies, Multiple System Atrophy, Parkinson Disease, REM Sleep Behavior Disorder, Synucleinopathies

Abstract

OBJECTIVE: Rapid eye movement (REM) sleep behavior disorder (RBD) is widely considered a prodromal synucleinopathy, as most with RBD develop overt synucleinopathy within ~10 years. Accordingly, RBD offers an opportunity to test potential treatments at the earliest stages of synucleinopathy. The North American Prodromal Synucleinopathy (NAPS) Consortium has created a multisite RBD participant, primarily clinic-based cohort to better understand characteristics at diagnosis, and in future work, identify predictors of phenoconversion, develop synucleinopathy biomarkers, and enable early stage clinical trial enrollment. METHODS: Participants ≥18 years of age with overnight polysomnogram-confirmed RBD without Parkinsons disease, dementia, multiple system atrophy, or narcolepsy were enrolled from nine sites across North America (8/2018 to 4/2021). Data collection included family/personal history of RBD and standardized assessments of cognitive, motor, sensory, and autonomic function. RESULTS: Outcomes are primarily reported based on sex (361 total: n = 295 male, n = 66 female), and secondarily based on history of antidepressant use (n = 200 with, n = 154 without; with correction for sex differences) and based on extent of synucleinopathy burden (n = 56 defined as isolated RBD, n = 305 defined as RBD+ [i.e., exhibiting ≥1 abnormality]). Overall, these participants commonly demonstrated abnormalities in global cognition (MoCA; 38%), motor function (alternate tap test; 48%), sensory (BSIT; 57%), autonomic function (orthostatic hypotension, 38.8%), and anxiety/depression (BAI and PHQ-9; 39.3% and 31%, respectively). INTERPRETATION: These RBD participants, assessed with extensive history, demographic, cognitive, motor, sensory, and autonomic function demonstrated a lack of sex differences and high frequency of concomitant neurological abnormalities. These participants will be valuable for future longitudinal study and neuroprotective clinical trials.

Published

2023

2. Sleep disorders and mortality: A prospective study in the Canadian longitudinal study on aging

Author

Zolfaghari, Sheida, Keil, Allison, Pelletier, Amélie, and Postuma, Ronald B.

Published

2024

3. Overexpression of mitochondrial fission or mitochondrial fusion genes enhances resilience and extends longevity.

Author

Traa, Annika, Keil, Allison, AlOkda, Abdelrahman, Jacob‐Tomas, Suleima, Tamez González, Aura A., Zhu, Shusen, Rudich, Zenith, and Van Raamsdonk, Jeremy M.

Subjects

*MITOCHONDRIAL dynamics, *GENE fusion, *GENETICS, *CAENORHABDITIS elegans, *MORPHOLOGY

Abstract

The dynamicity of the mitochondrial network is crucial for meeting the ever‐changing metabolic and energy needs of the cell. Mitochondrial fission promotes the degradation and distribution of mitochondria, while mitochondrial fusion maintains mitochondrial function through the complementation of mitochondrial components. Previously, we have reported that mitochondrial networks are tubular, interconnected, and well‐organized in young, healthy C. elegans, but become fragmented and disorganized with advancing age and in models of age‐associated neurodegenerative disease. In this work, we examine the effects of increasing mitochondrial fission or mitochondrial fusion capacity by ubiquitously overexpressing the mitochondrial fission gene drp‐1 or the mitochondrial fusion genes fzo‐1 and eat‐3, individually or in combination. We then measured mitochondrial function, mitochondrial network morphology, physiologic rates, stress resistance, and lifespan. Surprisingly, we found that overexpression of either mitochondrial fission or fusion machinery both resulted in an increase in mitochondrial fragmentation. Similarly, both mitochondrial fission and mitochondrial fusion overexpression strains have extended lifespans and increased stress resistance, which in the case of the mitochondrial fusion overexpression strains appears to be at least partially due to the upregulation of multiple pathways of cellular resilience in these strains. Overall, our work demonstrates that increasing the expression of mitochondrial fission or fusion genes extends lifespan and improves biological resilience without promoting the maintenance of a youthful mitochondrial network morphology. This work highlights the importance of the mitochondria for both resilience and longevity. [ABSTRACT FROM AUTHOR]

Published

2024

4. Power-Sharing in Europe: Past Practice, Present Cases, and Future Directions

Author

Soeren Keil, Allison McCulloch, Soeren Keil, Allison McCulloch

Published

2020

5. Comorbid neurotrauma increases neurodegenerative-relevant cognitive, motor, and autonomic dysfunction in patients with rapid eye movement sleep behavior disorder: a substudy of the North American Prodromal Synucleinopathy Consortium.

Author

Elliott, Jonathan E, Ligman, Brittany R, Bryant-Ekstrand, Mohini D, Keil, Allison T, Powers, Katherine, Olivo, Cosette, Neilson, Lee E, Postuma, Ronald B, Pelletier, Amélie, Gagnon, Jean-François, Gan-Or, Ziv, Yu, Eric, Liu, Lang, Louis, Erik K St., Forsberg, Leah K, Fields, Julie A, Ross, Owen A, Huddleston, Daniel E, Bliwise, Donald L, and Avidan, Alon Y

Published

2024

6. DNA Methylation Age Acceleration as a Potential Biomarker for Early Onset of Rapid Eye Movement Sleep Behavior Disorder

Author

Senkevich, Konstantin, primary, Pelletier, Amélie, additional, Sato, Christine, additional, Liu, Lang, additional, Keil, Allison, additional, Gan‐Or, Ziv, additional, Lang, Anthony E., additional, Postuma, Ronald B., additional, and Rogaeva, Ekaterina, additional

Published

2023

7. DNA Methylation Age Acceleration as a Potential Biomarker for Early Onset of Rapid Eye Movement Sleep Behavior Disorder.

Author

Senkevich, Konstantin, Pelletier, Amélie, Sato, Christine, Liu, Lang, Keil, Allison, Gan‐Or, Ziv, Lang, Anthony E., Postuma, Ronald B., and Rogaeva, Ekaterina

Subjects

RAPID eye movement sleep, DNA methylation, SLEEP disorders, DISEASE risk factors, MONOGENIC & polygenic inheritance (Genetics)

Abstract

Rapid eye movement sleep behavior disorder (RBD) is the strongest prodromal marker for α‐synucleinopathies. The Horvath DNA methylation age (DNAm‐age) is an epigenetic clock reflecting biological aging. We found an association of DNAm‐age acceleration with RBD age at onset at baseline (N = 162, B = −0.68, standard error [SE] = 0.12, p = 2.59e‐08) and follow‐up (n = 45, B = −1.07, SE = 0.21, p = 9.73e‐06). The result remained similar after accounting for genetic risk factors (eg, RBD polygenic risk score). On average, RBD patients with faster versus slow/normal epigenetic aging had a 5.2‐year earlier phenoconversion, and the Cox regression analysis revealed a trend toward significance (n = 53, hazard ratio = 1.05, 95% confidence interval = 0.99–1.11, p = 0.06). Our findings suggest that DNAm‐age acceleration is a potential biomarker for earlier RBD onset. ANN NEUROL 2024;95:190–194 [ABSTRACT FROM AUTHOR]

Published

2024

8. 0640 North American Prodromal Synucleinopathy Consortium: Baseline characteristics in 251 patients with REM Sleep Behavior Disorder

Author

Elliott, Jonathan, primary, Lim, Miranda, additional, Keil, Allison, additional, Avidan, Alon, additional, Bliwise, Don, additional, Gagnon, Jean-François, additional, Howell, Michael, additional, Huddleston, Daniel, additional, McLeland, Jennifer, additional, Postuma, Ronald, additional, Louis, Erik St, additional, Videnovic, Aleksandar, additional, Boeve, Bradley, additional, and Ju, Yo-El, additional

Published

2022

9. Dietary Supplementation With Branched Chain Amino Acids to Improve Sleep in Veterans With Traumatic Brain Injury: A Randomized Double-Blind Placebo-Controlled Pilot and Feasibility Trial

Author

Elliott, Jonathan E., primary, Keil, Allison T., additional, Mithani, Sara, additional, Gill, Jessica M., additional, O’Neil, Maya E., additional, Cohen, Akiva S., additional, and Lim, Miranda M., additional

Published

2022

10. 524 NAPS

Author

Elliott, Jonathan, primary, Lim, Miranda, additional, Keil, Allison, additional, Avidan, Alon, additional, Bliwise, Donald, additional, Gagnon, Jean-Francois, additional, Howell, Michael, additional, Huddleston, Daniel, additional, McCleland, Jennifer, additional, St. Louis, Erik, additional, Postuma, Ronald, additional, Videnovic, Aleksandar, additional, Boeve, Bradley, additional, and Ju, Yo-El, additional

Published

2021

11. Morning bright light therapy for sleep to augment cognitive rehabilitation in Veterans with comorbid traumatic brain injury and post‐traumatic stress disorder: A pilot study

Author

Keil, Allison, primary, Elliott, Jonathan, additional, McBride, Alisha, additional, Callahan, Megan, additional, and Lim, Miranda, additional

Published

2021

12. Feasibility and acceptability for LION, a fully remote, randomized clinical trial within the VA for light therapy to improve sleep in Veterans with and without TBI: An MTBI 2 sponsored protocol.

Author

Elliott JE, Brewer JS, Keil AT, Ligman BR, Bryant-Ekstrand MD, McBride AA, Powers K, Sicard SJ, Twamley EW, O'Neil ME, Hildebrand AD, Nguyen T, Morasco BJ, Gill JM, Dengler BA, and Lim MM

Abstract

Sleep-wake disturbances frequently present in Veterans with mild traumatic brain injury (mTBI). These TBI-related sleep impairments confer significant burden and commonly exacerbate other functional impairments. Therapies to improve sleep following mTBI are limited and studies in Veterans are even more scarce. In our previous pilot work, morning bright light therapy (MBLT) was found to be a feasible behavioral sleep intervention in Veterans with a history of mTBI; however, this was single-arm, open-label, and non-randomized, and therefore was not intended to establish efficacy. The present study, LION (light vs ion therapy) extends this preliminary work as a fully powered, sham-controlled, participant-masked randomized controlled trial (NCT03968874), implemented as fully remote within the VA (target n=120 complete). Randomization at 2:1 allocation ratio to: 1) active: MBLT (n=80), and 2) sham: deactivated negative ion generator (n=40); each with identical engagement parameters (60-min duration; within 2-hrs of waking; daily over 28-day duration). Participant masking via deception balanced expectancy assumptions across arms. Outcome measures were assessed following a 14-day baseline (pre-intervention), following 28-days of device engagement (post-intervention), and 28-days after the post-intervention assessment (follow-up). Primary outcomes were sleep measures, including continuous wrist-based actigraphy, self-report, and daily sleep dairy entries. Secondary/exploratory outcomes included cognition, mood, quality of life, circadian rhythm via dim light melatonin onset, and biofluid-based biomarkers. Participant drop out occurred in <10% of those enrolled, incomplete/missing data was present in <15% of key outcome variables, and overall fidelity adherence to the intervention was >85%, collectively establishing feasibility and acceptability for MBLT in Veterans with mTBI.

Published

2024

13. Frequency of Orthostatic Hypotension in Isolated REM Sleep Behavior Disorder.

Author

Elliott JE, Bryant-Ekstrand MD, Keil AT, Ligman BR, Lim MM, Zitser J, During EH, Gagnon JF, St Louis EK, Fields JA, Huddleston DE, Bliwise DL, Avidan AY, Schenck CH, McLeland J, Criswell SR, Davis AA, Videnovic A, Lee-Iannotti JK, Postuma R, Boeve BF, Ju YS, and Miglis MG

Subjects

Humans, Male, Female, REM Sleep Behavior Disorder diagnosis, Hypotension, Orthostatic diagnosis, Hypotension, Orthostatic epidemiology, Synucleinopathies, Parkinson Disease complications, Parkinson Disease epidemiology, Autonomic Nervous System Diseases diagnosis, Autonomic Nervous System Diseases epidemiology

Abstract

Background and Objectives: Although orthostatic hypotension (OH) can be an early feature of autonomic dysfunction in isolated REM sleep behavior disorder (iRBD), no large-scale studies have examined the frequency of OH in iRBD. In this study, we prospectively evaluated the frequency of OH in a large multicenter iRBD cohort., Methods: Participants 18 years or older with video polysomnogram-confirmed iRBD were enrolled through the North American Prodromal Synucleinopathy consortium. All participants underwent 3-minute orthostatic stand testing to assess the frequency of OH, and a Δ heart rate/Δ systolic blood pressure (ΔHR/ΔSBP) ratio <0.5 was used to define reduced HR augmentation, suggestive of neurogenic OH. All participants completed a battery of assessments, including the Scales for Outcomes in Parkinson Disease-Autonomic Dysfunction (SCOPA-AUT) and others assessing cognitive, motor, psychiatric, and sensory domains., Results: Of 340 iRBD participants (65 ± 10 years, 82% male), 93 (27%) met criteria for OH (ΔHR/ΔSBP 0.37 ± 0.28; range 0.0-1.57), and of these, 72 (77%) met criteria for OH with reduced HR augmentation (ΔHR/ΔSBP 0.28 ± 0.21; range 0.0-0.5). Supine hypertension (sHTN) was present in 72% of those with OH. Compared with iRBD participants without OH, those with OH were older, reported older age of RBD symptom onset, and had worse olfaction. There was no difference in autonomic symptom scores as measured by SCOPA-AUT., Discussion: OH and sHTN are common in iRBD. However, as patients may have reduced autonomic symptom awareness, orthostatic stand testing should be considered in clinical evaluations. Longitudinal studies are needed to clarify the relationship between OH and phenoconversion risk in iRBD., Trial Registration Information: ClinicalTrials.gov: NCT03623672; North American Prodromal Synucleinopathy Consortium.

Published

2023