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203. P2-140: Convergent Evidence of Pupillary Response as an Early Indicator of Locus Coeruleus Dysfunction and Risk for MCI

Author

Elman, Jeremy A., primary, Panizzon, Matthew, additional, Hagler, Donald J., additional, Fennema-Notestine, Christine, additional, Franz, Carol, additional, Eyler, Lisa T., additional, Granholm, Eric, additional, Jak, Amy J., additional, Lyons, Michael, additional, Dale, Anders M., additional, and Kremen, William S., additional

Published
2016
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206. Use of an Alzheimer’s disease polygenic risk score to identify mild cognitive impairment in adults in their 50s

Author

Logue, Mark, Panizzon, Matthew, Elman, Jeremy, Gillespie, Nathan, Hatton, Sean, Gustavson, Daniel, Andreassen, Ole, Dale, Anders, Franz, Carol, Lyons, Michael, Neale, Michael, Reynolds, Chandra, Tu, Xin, and Kremen, William

Abstract

Early identification of younger, non-demented adults at elevated risk for Alzheimer’s disease (AD) is crucial because the pathological process begins decades before dementia onset. Toward that end, we showed that an AD polygenic risk score (PRS) could identify mild cognitive impairment (MCI) in adults who were only in their 50s. Participants were 1176 white, non-Hispanic community-dwelling men of European ancestry in the Vietnam Era Twin Study of Aging (VETSA): 7% with amnestic MCI (aMCI); 4% with non-amnestic MCI (naMCI). Mean age was 56 years, with 89% <60 years old. Diagnosis was based on the Jak-Bondi actuarial/neuropsychological approach. We tested six P-value thresholds (0.05–0.50) for single nucleotide polymorphisms included in the ADPRS. After controlling for non-independence of twins and non-MCI factors that can affect cognition, higher PRSs were associated with significantly greater odds of having aMCI than being cognitively normal (odds ratios (ORs) = 1.36–1.43 for thresholds P< 0.20–0.50). The highest OR for the upper vs. lower quartile of the ADPRS distribution was 3.22. ORs remained significant after accounting for APOE-related SNPs from the ADPRS or directly genotyped APOE. Diabetes was associated with significantly increased odds of having naMCI (ORs = 3.10–3.41 for thresholds P< 0.05–0.50), consistent with naMCI having more vascular/inflammation components than aMCI. Analysis of sensitivity, specificity, and negative and positive predictive values supported some potential of ADPRSs for selecting participants in clinical trials aimed at early intervention. With participants 15+ years younger than most MCI samples, these findings are promising with regard to efforts to more effectively treat or slow AD progression.

Published
2019
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207. Atypical brain aging and its association with working memory performance in major depressive disorder

Author

Ho, Natalie C.W., Bethlehem, Richard AI., Seidlitz, Jakob, Nogovitsyn, Nikita, Metzak, Paul, Ballester, Pedro L., Hassel, Stefanie, Rotzinger, Susan, Poppenk, Jordan, Lam, Raymond W., Taylor, Valerie H., Milev, Roumen, Adamson, Chris, Adler, Sophie, Alexander-Bloch, Aaron F., Anagnostou, Evdokia, Anderson, Kevin M., Areces-Gonzalez, Ariosky, Astle, Duncan E., Auyeung, Bonnie, Ayub, Muhammad, Bae, Jong Bin, Ball, Gareth, Baron-Cohen, Simon, Beare, Richard, Bedford, Saashi A., Benegal, Vivek, Bethlehem, Richard A.I., Beyer, Frauke, Blangero, John, Blesa Cábez, Manuel, Boardman, James P., Borzage, Matthew, Bosch-Bayard, Jorge F., Bourke, Niall, Bullmore, Edward T., Calhoun, Vince D., Chakravarty, Mallar M., Chen, Christina, Chertavian, Casey, Chetelat, Gaël, Chong, Yap S., Corvin, Aiden, Costantino, Manuela, Courchesne, Eric, Crivello, Fabrice, Cropley, Vanessa L., Crosbie, Jennifer, Crossley, Nicolas, Delarue, Marion, Delorme, Richard, Desrivieres, Sylvane, Devenyi, Gabriel, Di Biase, Maria A., Dolan, Ray, Donald, Kirsten A., Donohoe, Gary, Dorfschmidt, Lena, Dunlop, Katharine, Edwards, Anthony D., Elison, Jed T., Ellis, Cameron T., Elman, Jeremy A., Eyler, Lisa, Fair, Damien A., Fletcher, Paul C., Fonagy, Peter, Franz, Carol E., Galan-Garcia, Lidice, Gholipour, Ali, Giedd, Jay, Gilmore, John H., Glahn, David C., Goodyer, Ian M., Grant, P.E., Groenewold, Nynke A., Gudapati, Shreya, Gunning, Faith M., Gur, Raquel E., Gur, Ruben C., Hammill, Christopher F., Hansson, Oskar, Hedden, Trey, Heinz, Andreas, Henson, Richard N., Heuer, Katja, Hoare, Jacqueline, Holla, Bharath, Holmes, Avram J., Huang, Hao, Ipser, Jonathan, Jack, Clifford R., Jackowski, Andrea P., Jia, Tianye, Jones, David T., Jones, Peter B., Kahn, Rene S., Karlsson, Hasse, Karlsson, Linnea, Kawashima, Ryuta, Kelley, Elizabeth A., Kern, Silke, Kim, Ki-Woong, Kitzbichler, Manfred G., Kremen, William S., Lalonde, François, Landeau, Brigitte, Lerch, Jason, Lewis, John D., Li, Jiao, Liao, Wei, Liston, Conor, Lombardo, Michael V., Lv, Jinglei, Mallard, Travis T., Marcelis, Machteld, Mathias, Samuel R., Mazoyer, Bernard, McGuire, Philip, Meaney, Michael J., Mechelli, Andrea, Misic, Bratislav, Morgan, Sarah E., Mothersill, David, Ortinau, Cynthia, Ossenkoppele, Rik, Ouyang, Minhui, Palaniyappan, Lena, Paly, Leo, Pan, Pedro M., Pantelis, Christos, Park, Min Tae M., Paus, Tomas, Pausova, Zdenka, Paz-Linares, Deirel, Pichet Binette, Alexa, Pierce, Karen, Qian, Xing, Qiu, Anqi, Raznahan, Armin, Rittman, Timothy, Rodrigue, Amanda, Rollins, Caitlin K., Romero-Garcia, Rafael, Ronan, Lisa, Rosenberg, Monica D., Rowitch, David H., Salum, Giovanni A., Satterthwaite, Theodore D., Schaare, H. Lina, Schabdach, Jenna, Schachar, Russell J., Schöll, Michael, Schultz, Aaron P., Seidlitz, Jakob, Sharp, David, Shinohara, Russell T., Skoog, Ingmar, Smyser, Christopher D., Sperling, Reisa A., Stein, Dan J., Stolicyn, Aleks, Suckling, John, Sullivan, Gemma, Thyreau, Benjamin, Toro, Roberto, Traut, Nicolas, Tsvetanov, Kamen A., Turk-Browne, Nicholas B., Tuulari, Jetro J., Tzourio, Christophe, Vachon-Presseau, Étienne, Valdes-Sosa, Mitchell J., Valdes-Sosa, Pedro A., Valk, Sofie L., van Amelsvoort, Therese, Vandekar, Simon N., Vasung, Lana, Vértes, Petra E., Victoria, Lindsay W., Villeneuve, Sylvia, Villringer, Arno, Vogel, Jacob W., Wagstyl, Konrad, Wang, Yin-Shan S., Warfield, Simon K., Warrier, Varun, Westman, Eric, Westwater, Margaret L., Whalley, Heather C., White, Simon R., Witte, A. Veronica, Yang, Ning, Yeo, B.T. Thomas, Yun, Hyuk Jin, Zalesky, Andrew, Zar, Heather J., Zettergren, Anna, Zhou, Juan H., Ziauddeen, Hisham, Zimmerman, Dabriel, Zugman, Andre, Zuo, Xi-Nian N., Bullmore, Edward T., Alexander-Bloch, Aaron F., Frey, Benicio N., Harkness, Kate L., Addington, Jean, Kennedy, Sidney H., and Dunlop, Katharine

Abstract

Patients with major depressive disorder (MDD) can present with altered brain structure and deficits in cognitive function similar to aging. Yet, the interaction between age-related brain changes and brain development in MDD remains understudied. In a cohort of adolescents and adults with and without MDD, we assessed brain aging differences and associations through a newly developed tool quantifying normative neurodevelopmental trajectories.

Published
2024
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208. Early Cortical Microstructural Changes in Aging Are Linked to Vulnerability to Alzheimer’s Disease Pathology

Author

Tang, Rongxiang, Franz, Carol E., Hauger, Richard L., Dale, Anders M., Dorros, Stephen M., Eyler, Lisa T., Fennema-Notestine, Christine, Hagler, Donald J., Lyons, Michael J., Panizzon, Matthew S., Puckett, Olivia K., Williams, McKenna E., Elman, Jeremy A., and Kremen, William S.

Abstract

Early identification of Alzheimer’s disease (AD) risk is critical for improving treatment success. Cortical thickness is a macrostructural measure used to assess neurodegeneration in AD. However, cortical microstructural changes appear to precede macrostructural atrophy and may improve early risk identification. Currently, whether cortical microstructural changes in aging are linked to vulnerability to AD pathophysiology remains unclear in nonclinical populations, who are precisely the target for early risk identification.

Published
2024
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209. Probable chronic pain, brain structure, and Alzheimer’s plasma biomarkers in older men

Author

Bell, Tyler R., Franz, Carol E., Eyler, Lisa T., Fennema-Notestine, Christine, Puckett, Olivia K., Dorros, Stephen M., Panizzon, Matthew S., Pearce, Rahul C., Hagler, Donald J., Lyons, Michael J., Beck, Asad, Elman, Jeremy A., and Kremen, William S.

Abstract

Chronic pain leads to tau accumulation and hippocampal atrophy in mice. In this study, we provide one of the first assessments in humans, examining the associations of probable chronic pain with hippocampal volume, integrity of the locus coeruleus (LC)—an upstream site of tau deposition—and Alzheimer’s Disease-related plasma biomarkers. Participants were mostly cognitively unimpaired men. Probable chronic pain was defined as moderate-to-severe pain in 2+ study waves at average ages 56, 62, and 68. At age 68, 424 participants underwent structural magnestic resonance imaging (MRI) of hippocampal volume and LC-sensitive MRI providing an index of LC integrity (LC contrast-to-noise ratio). Analyses adjusted for confounders including major health conditions, depressive symptoms, and opioid use. Models showed that men with probable chronic pain had smaller hippocampal volume and lower rostral-middle—but not caudal—LC contrast-to-noise ratio compared to men without probable chronic pain. Men with probable chronic pain also had higher levels of plasma total tau, beta-amyloid-42, and beta-amyloid-40 compared to men without probable chronic pain. These findings suggest that probable chronic pain is associated with tau accumulation and reduced structural brain integrity in regions affected early in the development of Alzheimer’s Disease.

Published
2024
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217. Hotel's Trademark Extends Beyond Its Geographic Region

Author

Elman, Jeremy

Subjects
TRYP by Wyndham -- Intellectual property -- Cases -- Subsidiaries, divisions and units, Trademark infringement -- Cases, Hotels and motels -- Intellectual property -- Cases -- Subsidiaries, divisions and units -- Spain -- United States, Company legal issue, Business, international
Abstract

Dorpan, S.L. v. Hotel Meli-, Inc. Addressing the issue of whether a senior trademark user of a mark related to travel was entitled to trademark protection outside of its geographic [...]

Published
2013

218. Expert Testimony About New Testing Methodologies Inadmissible When Not Disclosed In Expert Report

Author

Elman, Jeremy

Subjects
Johnson & Johnson Vision Care Inc. -- Cases -- Testing, Evidence, Expert -- Reports, Eyewear industry -- Cases -- Testing, Patent infringement -- Cases, Company legal issue, Business, international
Abstract

Rembrandt Vision Technologies, L.P. v. Johnson & Johnson Vision Care, Inc. Addressing the issue of whether a technical expert's failure to disclose specific testing methodology was merely a 'typo' or [...]

Published
2013

219. Federal Circuit Not The Only Forum That Can Resolve Patent-Related Contract Disputes

Author

Elman, Jeremy

Subjects
Rad Source Technologies Inc. -- Cases, Medical test kit industry -- Cases, Medical equipment and supplies industry -- Cases, Patent infringement -- Cases, Company legal issue, Business, international
Abstract

MDS (Canada) Inc. v. Rad Source Technologies, Inc. In a case of first impression for a regional court of appeals regarding the issue of whether the U.S. Court of Appeals [...]

Published
2013

220. Associations Between Depression and Cardiometabolic Health: A 27-Year Longitudinal Study – Corrigendum.

Author

Ditmars, Hillary L., Logue, Mark W., Toomey, Rosemary, McKenzie, Ruth E., Franz, Carol E., Panizzon, Matthew S., Reynolds, Chandra A., Cuthbert, Kristy N., Vandiver, Richard, Gustavson, Daniel E., Eglit, Graham M. L., Elman, Jeremy A., Sanderson-Cimino, Mark, Williams, McKenna E., Andreassen, Ole A., Dale, Anders M., Eyler, Lisa T., Fennema-Notestine, Christine, Gillespie, Nathan A., and Hauger, Richard L.

Subjects
CARDIOVASCULAR diseases risk factors, ADULT respiratory distress syndrome, MENTAL depression
Abstract

A correction is presented to the article "Associations between depression and cardiometabolic health: A 27-year longitudinal study."

Published
2022
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221. Personal Jurisdiction Found Where Website Harms

Author

Elman, Jeremy

Subjects
United States. Court of Appeals for the 7th Circuit -- Laws, regulations and rules, Copyright infringement -- Laws, regulations and rules, Web sites -- Laws, regulations and rules, Internet -- Laws, regulations and rules, Government regulation, Company Web site/Web page, Internet, Business, international
Abstract

Addressing issues of personal jurisdiction regarding copyright infringement on the internet, the U.S. Court of Appeals for the Eleventh Circuit reversed a lower court's ruling and found that a Tennessee [...]

Published
2008

222. Calling All Patentees: Disclose Potential Alternatives For Claimed Steps In A Method Claim

Author

Elman, Jeremy

Subjects
United States. Court of Appeals for the Federal Circuit -- Laws, regulations and rules -- Cases, Telecommunications services industry -- Cases -- Intellectual property -- Laws, regulations and rules -- Methods, Patent infringement -- Methods -- Cases -- Laws, regulations and rules, Communications industry -- Cases -- Intellectual property -- Laws, regulations and rules -- Methods, Company legal issue, Government regulation, Telecommunications services industry, Business, international
Abstract

Addressing issues of infringement of a method claim patent, the U.S. Court of Appeals for the Federal Circuit reversed a finding of infringement of a method for routing '1-800' telephone [...]

Published
2008

223. It's Not The Design-Just The Idea

Author

Elman, Jeremy

Subjects
Real estate developers -- Cases, Copyright infringement -- Cases, Company legal issue, Business, international
Abstract

Addressing a copyright dispute between an individual designer and developers for Donald Trump, the U.S. Court of Appeals for the Eleventh Circuit affirmed summary judgment for the developers. Oravec v. [...]

Published
2008

224. Associations Between Ambient Air Pollution and Cognitive Abilities from Midlife to Early Old Age: Modification by APOE Genotype.

Author

Franz, Carol E., Gustavson, Daniel E., Elman, Jeremy A., Fennema-Notestine, Christine, Hagler Jr., Donald J., Baraff, Aaron, Tu, Xin M., Wu, Tsung-Chin, De Anda, Jaden, Beck, Asad, Kaufman, Joel D., Whitsel, Nathan, Finch, Caleb E., Chen, Jiu-Chiuan, Lyons, Michael J., and Kremen, William S.

Subjects
*EPISODIC memory, *AIR pollution, *COGNITIVE ability, *APOLIPOPROTEIN E, *COGNITIVE processing speed, *MIDDLE age
Abstract

Background: Fine particulate matter (PM2.5) and nitrogen dioxide (NO2) measures of ambient air pollution are associated with accelerated age-related cognitive impairment, and Alzheimer's disease and related dementias (ADRD). Objective: We examined associations between air pollution, four cognitive factors, and the moderating role of apolipoprotein E (APOE) genotype in the understudied period of midlife. Methods: Participants were ∼1,100 men in the Vietnam Era Twin Study of Aging. Baseline cognitive assessments were from 2003 to 2007. Measures included past (1993–1999) and recent (3 years prior to baseline assessment) PM2.5 and NO2 exposure, in-person assessment of episodic memory, executive function, verbal fluency, and processing speed, and APOE genotype. Average baseline age was 56 years with a 12-year follow-up. Analyses adjusted for health and lifestyle covariates. Results: Performance in all cognitive domains declined from age 56 to 68. Higher PM2.5 exposures were associated with worse general verbal fluency. We found significant exposure-by-APOE genotype interactions for specific cognitive domains: PM2.5 with executive function and NO2 with episodic memory. Higher PM2.5 exposure was related to worse executive function in APOE ɛ4 carriers, but not in non-carriers. There were no associations with processing speed. Conclusion: These results indicate negative effects of ambient air pollution exposure on fluency alongside intriguing differential modifications of cognitive performance by APOE genotype. APOE ɛ4 carriers appeared more sensitive to environmental differences. The process by which air pollution and its interaction with genetic risk for ADRD affects risk for later life cognitive decline or progression to dementia may begin in midlife. [ABSTRACT FROM AUTHOR]

Published
2023
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225. Elevated C-Reactive Protein in Older Men With Chronic Pain: Association With Plasma Amyloid Levels and Hippocampal Volume.

Author

Bell, Tyler R, Franz, Carol E, Thomas, Kelsey R, Williams, McKenna E, Eyler, Lisa T, Lerman, Imanuel, Fennema-Notestine, Christine, Puckett, Olivia K, Dorros, Stephen M, Panizzon, Matthew S, Pearce, Rahul C, Hagler, Donald J, Lyons, Michael J, Elman, Jeremy A, and Kremen, William S

Subjects
*TAU proteins, *CHRONIC pain, *OLDER men, *ALZHEIMER'S disease, *C-reactive protein
Abstract

Background Chronic pain leads to tau accumulation and hippocampal atrophy, which may be moderated through inflammation. In older men, we examined associations of chronic pain with Alzheimer's disease (AD)-related plasma biomarkers and hippocampal volume as moderated by systemic inflammation. Methods Participants were men without dementia. Chronic pain was defined as moderate-to-severe pain in 2+ study waves at average ages 56, 62, and 68. At age 68, we measured plasma amyloid-beta (Aβ42, n  = 871), Aβ40 (n  = 887), total tau (t-tau, n  = 841), and neurofilament light chain (NfL, n  = 915), and serum high-sensitivity C-reactive protein (hs-CRP, n  = 968), a marker of systemic inflammation. A subgroup underwent structural MRI to measure hippocampal volume (n  = 385). Analyses adjusted for medical morbidities, depressive symptoms, and opioid use. Results Chronic pain was related to higher Aβ40 (β = 0.25, p  = .009), but hs-CRP was unrelated to AD-related biomarkers (p s > .05). There was a significant interaction such that older men with both chronic pain and higher levels of hs-CRP had higher levels of Aβ42 (β = 0.36, p  = .001) and Aβ40 (β = 0.29, p  = .003). Chronic pain and hs-CRP did not interact to predict levels of Aβ42/Aβ40, t-tau, or NfL. Furthermore, there were significant interactions such that Aβ42 and Aβ40 were associated with lower hippocampal volume, particularly when levels of hs-CRP were elevated (hs-CRP × Aβ42: β = −0.19, p  = .002; hs-CRP × Aβ40: β = −0.21, p  = .001), regardless of chronic pain status. Conclusions Chronic pain was associated with higher plasma Aβ, especially when hs-CRP was also elevated. Higher hs-CRP and Aβ levels were both related to smaller hippocampal volumes. Chronic pain, when accompanied by systemic inflammation, may elevate the risk of neurodegeneration in AD-vulnerable regions. [ABSTRACT FROM AUTHOR]

Published
2024
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226. Association of neurofilament light chain with renal function: mechanisms and clinical implications.

Author

Tang, Rongxiang, Panizzon, Matthew S., Elman, Jeremy A., Gillespie, Nathan A., Hauger, Richard L., Rissman, Robert A., Lyons, Michael J., Neale, Michael C., Reynolds, Chandra A., Franz, Carol E., and Kremen, William S.

Subjects
*KIDNEY physiology, *CYTOPLASMIC filaments, *TWINS, *CEREBROSPINAL fluid, *OLDER people
Abstract

Background: Blood-based neurofilament light chain (NfL) is a promising biomarker of neurodegeneration across multiple neurodegenerative diseases. However, blood-based NfL is highly associated with renal function in older adults, which leads to the concern that blood-based NfL levels may be influenced by renal function, rather than neurodegeneration alone. Despite growing interest in using blood-based NfL as a biomarker of neurodegeneration in research and clinical practices, whether renal function should always be accounted for in these settings remains unclear. Moreover, the mechanisms underlying this association between blood-based measures of NfL and renal function remain elusive. In this study, we first evaluated the effect of renal function on the associations of plasma NfL with other measures of neurodegeneration. We then examined the extent of genetic and environmental contributions to the association between plasma NfL and renal function. Methods: In a sample of 393 adults (mean age=75.22 years, range=54–90), we examined the associations of plasma NfL with cerebrospinal fluid (CSF) NfL and brain volumetric measures before and after adjusting for levels of serum creatinine (an index of renal function). In an independent sample of 969 men (mean age=67.57 years, range=61–73) that include monozygotic and dizygotic twin pairs, we replicated the same analyses and leveraged biometrical twin modeling to examine the genetic and environmental influences on the plasma NfL and creatinine association. Results: Plasma NfL's associations with cerebrospinal fluid NfL and brain volumetric measures did not meaningfully change after adjusting for creatinine levels. Both plasma NfL and creatinine were significantly heritable (h2=0.54 and 0.60, respectively). Their phenotypic correlation (r=0.38) was moderately explained by shared genetic influences (genetic correlation=0.46) and unique environmental influences (unique environmental correlation=0.27). Conclusions: Adjusting for renal function is unnecessary when assessing associations between plasma NfL and other measures of neurodegeneration but is necessary if plasma NfL is compared to a cutoff for classifying neurodegeneration-positive versus neurodegeneration-negative individuals. Blood-based measures of NfL and renal function are heritable and share common genetic influences. [ABSTRACT FROM AUTHOR]

Published
2022
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227. Lifestyle and the aging brain: interactive effects of modifiable lifestyle behaviors and cognitive ability in men from midlife to old age.

Author

Franz, Carol E., Hatton, Sean N., Elman, Jeremy A., Warren, Teresa, Gillespie, Nathan A., Whitsel, Nathan A., Puckett, Olivia K., Dale, Anders M., Eyler, Lisa T., Fennema-Notestine, Christine, Hagler, Donald J., Hauger, Richard L., McKenzie, Ruth, Neale, Michael C., Panizzon, Matthew S., Pearce, Rahul C., Reynolds, Chandra A., Sanderson-Cimino, Mark, Toomey, Rosemary, and Tu, Xin M.

Subjects
*OLD age, *COGNITIVE ability, *MIDDLE age, *UNHEALTHY lifestyles, *AGE differences, *ALCOHOL drinking, AGE factors in Alzheimer's disease
Abstract

• A lifestyle composite of smoking, alcohol consumption, diet, physical activity, and social engagement at age 40 was associated with accelerated brain aging in old age. • Brain aging and AD-brain signature in old age were worse among participants with lower age 20 cognitive ability. • Lower cognitive ability predicted better brain outcomes if lifestyle was favorable, but high cognitive ability predicted better brain outcomes regardless of lifestyle. • Favorable early midlife lifestyle may be protective against neurodegeneration and dementia risk especially among adults with lower cognitive ability. • Efforts at prevention could be prioritized earlier in midlife. We examined the influence of lifestyle on brain aging after nearly 30 years, and tested the hypothesis that young adult general cognitive ability (GCA) would moderate these effects. In the community-dwelling Vietnam Era Twin Study of Aging (VETSA), 431 largely non-Hispanic white men completed a test of GCA at mean age 20. We created a modifiable lifestyle behavior composite from data collected at mean age 40. During VETSA, MRI-based measures at mean age 68 included predicted brain age difference (PBAD), Alzheimer's disease (AD) brain signature, and abnormal white matter scores. There were significant main effects of young adult GCA and lifestyle on PBAD and the AD signature (p s ≤ 0.012), and a GCA-by-lifestyle interaction on both (p s ≤ 0.006). Regardless of GCA level, having more favorable lifestyle behaviors predicted less advanced brain age and less AD-like brain aging. Unfavorable lifestyles predicted advanced brain aging in those with lower age 20 GCA, but did not affect brain aging in those with higher age 20 GCA. Targeting early lifestyle modification may promote dementia risk reduction, especially among lower reserve individuals. [ABSTRACT FROM AUTHOR]

Published
2021
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228. The genetic organization of longitudinal subcortical volumetric change is stable throughout the lifespan

Author

Fjell, Anders Martin, Grydeland, Hakon, Wang, Yunpeng, Amlien, Inge K, Bartres-Faz, David, Brandmaier, Andreas M, Düzel, Sandra, Elman, Jeremy, Franz, Carol E, Håberg, Asta K, Kietzmann, Tim C, Kievit, Rogier Andrew, Kremen, William S, Krogsrud, Stine K, Kühn, Simone, Lindenberger, Ulman, Macía, Didac, Mowinckel, Athanasia Monika, Nyberg, Lars, Panizzon, Matthew S, Solé-Padullés, Cristina, Sørensen, Øystein, Westerhausen, Rene, and Walhovd, Kristine Beate

Subjects
Adult, Aged, 80 and over, Cerebral Cortex, Male, Adolescent, brain, Longevity, Middle Aged, Magnetic Resonance Imaging, 3. Good health, neuroscience, Young Adult, Child, Preschool, Humans, genetics, Female, human, Child, lifespan, Aged
Abstract

Development and aging of the cerebral cortex show similar topographic organization and are governed by the same genes. It is unclear whether the same is true for subcortical regions, which follow fundamentally different ontogenetic and phylogenetic principles. We tested the hypothesis that genetically governed neurodevelopmental processes can be traced throughout life by assessing to which degree brain regions that develop together continue to change together through life. Analyzing over 6000 longitudinal MRIs of the brain, we used graph theory to identify five clusters of coordinated development, indexed as patterns of correlated volumetric change in brain structures. The clusters tended to follow placement along the cranial axis in embryonic brain development, suggesting continuity from prenatal stages, and correlated with cognition. Across independent longitudinal datasets, we demonstrated that developmental clusters were conserved through life. Twin-based genetic correlations revealed distinct sets of genes governing change in each cluster. Single-nucleotide polymorphisms-based analyses of 38,127 cross-sectional MRIs showed a similar pattern of genetic volume-volume correlations. In conclusion, coordination of subcortical change adheres to fundamental principles of lifespan continuity and genetic organization.

229. The genetic organization of longitudinal subcortical volumetric change is stable throughout the lifespan

Author

Fjell, Anders Martin, Grydeland, Hakon, Wang, Yunpeng, Amlien, Inge K, Bartres-Faz, David, Brandmaier, Andreas M, Düzel, Sandra, Elman, Jeremy, Franz, Carol E, Håberg, Asta K, Kietzmann, Tim C, Kievit, Rogier Andrew, Kremen, William S, Krogsrud, Stine K, Kühn, Simone, Lindenberger, Ulman, Macía, Didac, Mowinckel, Athanasia Monika, Nyberg, Lars, Panizzon, Matthew S, Solé-Padullés, Cristina, Sørensen, Øystein, Westerhausen, Rene, and Walhovd, Kristine Beate

Subjects
brain, genetics, lifespan, 3. Good health, Research Article, Neuroscience, Human
Abstract

Funder: Knut and Alice Wallenberg Foundation; FundRef: http://dx.doi.org/10.13039/501100004063, Funder: Norwegian Research Council; FundRef: http://dx.doi.org/10.13039/501100005416, Funder: Biotechnology and Biological Sciences Research Council; FundRef: http://dx.doi.org/10.13039/501100000268, Funder: Medical Research Council; FundRef: http://dx.doi.org/10.13039/501100000265, Development and aging of the cerebral cortex show similar topographic organization and are governed by the same genes. It is unclear whether the same is true for subcortical regions, which follow fundamentally different ontogenetic and phylogenetic principles. We tested the hypothesis that genetically governed neurodevelopmental processes can be traced throughout life by assessing to which degree brain regions that develop together continue to change together through life. Analyzing over 6000 longitudinal MRIs of the brain, we used graph theory to identify five clusters of coordinated development, indexed as patterns of correlated volumetric change in brain structures. The clusters tended to follow placement along the cranial axis in embryonic brain development, suggesting continuity from prenatal stages, and correlated with cognition. Across independent longitudinal datasets, we demonstrated that developmental clusters were conserved through life. Twin-based genetic correlations revealed distinct sets of genes governing change in each cluster. Single-nucleotide polymorphisms-based analyses of 38,127 cross-sectional MRIs showed a similar pattern of genetic volume–volume correlations. In conclusion, coordination of subcortical change adheres to fundamental principles of lifespan continuity and genetic organization.

230. Copyright Litigation.

Author

Elman, Jeremy

Subjects
*COPYRIGHT lawsuits, *COPYRIGHT infringement, *COPYRIGHT
Published
2018

231. How Well Does Subjective Cognitive Decline Correspond to Objectively Measured Cognitive Decline? Assessment of 10-12 Year Change.

Author

Gustavson, Daniel E., Jak, Amy J., Elman, Jeremy A., Panizzon, Matthew S., Franz, Carol E., Gifford, Katherine A., Reynolds, Chandra A., Toomey, Rosemary, Lyons, Michael J., and Kremen, William S.

Subjects
*EPISODIC memory, *DISEASE risk factors, *EXECUTIVE function, *MENTAL depression, *COGNITIVE ability, *MILD cognitive impairment, *ANXIETY, *MEMORY, *SELF-evaluation, *NEUROPSYCHOLOGICAL tests, *QUESTIONNAIRES, *STATISTICAL models, *LONGITUDINAL method
Abstract

Background: Although not strongly correlated with current objective cognitive ability, subjective cognitive decline (SCD) is a risk factor for Alzheimer's disease. Most studies focus on SCD in relation to future decline rather than objective prior decline that it purportedly measures.Objective: We evaluated whether self-report of cognitive decline-as a continuous measure-corresponds to objectively-assessed episodic memory and executive function decline across the same period.Methods: 1,170 men completed the Everyday Cognition Questionnaire (ECog) at mean age 68 assessing subjective changes in cognitive ability relative to 10 years prior. A subset had mild cognitive impairment (MCI), but MCI was diagnosed without regard to subjective decline. Participants completed up to 3 objective assessments of memory and executive function (M = 56, 62, and 68 years). Informant-reported ECogs were completed for 1,045 individuals. Analyses controlled for depression and anxiety symptoms assessed at mean age 68.Results: Participant-reported ECog scores were modestly associated with objective decline for memory (β= -0.23, 95%CI [-0.37, -0.10]) and executive function (β= -0.19, 95%CI [-0.33, -0.05]) over the same time period. However, these associations were nonsignificant after excluding MCI cases. Results were similar for informant ratings. Participant-rated ECog scores were more strongly associated with concurrent depression and anxiety symptoms, (β= 0.44, 95%CI [0.36, 0.53]).Conclusion: Continuous SCD scores are correlated with prior objective cognitive changes in non-demented individuals, though this association appears driven by individuals with current MCI. However, participants' current depression and anxiety ratings tend to be strongly associated with their SCD ratings. Thus, what primarily drives SCD ratings remains unclear. [ABSTRACT FROM AUTHOR]

Published
2021
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232. The Association between Exposure to Fine Particulate Matter and MRI-Assessed Locus Coeruleus Integrity in the Vietnam Era Twin Study of Aging (VETSA).

Author

Puckett, Olivia K., Fennema-Notestine, Christine, Hagler Jr., Donald J., Braskie, Meredith N., Jiu-Chiuan Chen, Finch, Caleb E., Kaufman, Joel D., Petkus, Andrew J., Reynolds, Chandra A., Salminen, Lauren E., Thompson, Paul M., Xinhui Wang, Kremen, William S., Franz, Carol E., and Elman, Jeremy A.

Subjects
*ALZHEIMER'S disease risk factors, *RISK assessment, *AIR pollution, *RESEARCH funding, *BRAIN, *MULTIPLE regression analysis, *MAGNETIC resonance imaging, *IN vivo studies, *DESCRIPTIVE statistics, *AGING, *ENVIRONMENTAL exposure, *PARTICULATE matter, *CONFIDENCE intervals
Abstract

BACKGROUND: Increased exposure to ambient air pollution, especially fine particulate matter ≤2.5 μm (PM2.5) is associated with poorer brain health and increased risk for Alzheimer’s disease (AD) and related dementias. The locus coeruleus (LC), located in the brainstem, is one of the earliest regions affected by tau pathology seen in AD. Its diffuse projections throughout the brain include afferents to olfactory areas that are hypothesized conduits of cerebral particle deposition. Additionally, extensive contact of the LC with the cerebrovascular system may present an additional route of exposure to environmental toxicants. OBJECTIVE: Our aim was to investigate if exposure to PM2.5 was associated with LC integrity in a nationwide sample of men in early old age, potentially representing one pathway through which air pollution can contribute to increased risk for AD dementia. METHODS: We examined the relationship between PM2.5 and in vivo magnetic resonance imaging (MRI) estimates of LC structural integrity indexed by contrast to noise ratio (LCCNR) in 381 men [mean age = 67.3; standard deviation (SD)= 2.6] from the Vietnam Era Twin Study of Aging (VETSA). Exposure to PM2.5 was taken as a 3-year average over the most recent period for which data were available (average of 5.6 years prior to the MRI scan). We focused on LCCNR in the rostral-middle portion of LC due to its stronger associations with aging and AD than the caudal LC. Associations between PM2.5 exposures and LC integrity were tested using linear mixed effects models adjusted for age, scanner, education, household income, and interval between exposure and MRI. A co-twin control analysis was also performed to investigate whether associations remained after controlling for genetic confounding and rearing environment. RESULTS: Multiple linear regressions revealed a significant association between PM2.5 and rostral-middle LCCNR (β= -0.16; 푝= 0.02), whereby higher exposure to PM2.5 was associated with lower LCCNR. A co-twin control analysis found that, within monozygotic pairs, individuals with higher PM2.5 exposure showed lower LCCNR (β= -0.11; 푝= 0.02), indicating associations were not driven by genetic or shared environmental confounds. There were no associations between PM2.5 and caudal LCCNR or hippocampal volume, suggesting a degree of specificity to the rostralmiddle portion of the LC. DISCUSSION: Given previous findings that loss of LC integrity is associated with increased accumulation of AD-related amyloid and tau pathology, impacts on LC integrity may represent a potential pathway through which exposure to air pollution increases AD risk. [ABSTRACT FROM AUTHOR]

Published
2024
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233. Associations of plasma neurofilament light chain with cognition and neuroimaging measures in community-dwelling early old age men.

Author

Tang, Rongxiang, Buchholz, Erik, Dale, Anders M., Rissman, Robert A., Fennema-Notestine, Christine, Gillespie, Nathan A., Hagler Jr, Donald J, Lyons, Michael J., Neale, Michael C., Panizzon, Matthew S., Puckett, Olivia K., Reynolds, Chandra A., Franz, Carol E., Kremen, William S., and Elman, Jeremy A.

Subjects
*COGNITIVE processing speed, *OLDER men, *OLD age, *COGNITION, *CYTOPLASMIC filaments
Abstract

Background: Plasma neurofilament light chain (NfL) is a promising biomarker of neurodegeneration with potential clinical utility in monitoring the progression of neurodegenerative diseases. However, the cross-sectional associations of plasma NfL with measures of cognition and brain have been inconsistent in community-dwelling populations. Methods: We examined these associations in a large community-dwelling sample of early old age men (N = 969, mean age = 67.57 years, range = 61–73 years), who are either cognitively unimpaired (CU) or with mild cognitive impairment (MCI). Specifically, we investigated five cognitive domains (executive function, episodic memory, verbal fluency, processing speed, visual-spatial ability), as well as neuroimaging measures of gray and white matter. Results: After adjusting for age, health status, and young adult general cognitive ability, plasma NfL level was only significantly associated with processing speed and white matter hyperintensity (WMH) volume, but not with other cognitive or neuroimaging measures. The association with processing speed was driven by individuals with MCI, as it was not detected in CU individuals. Conclusions: These results suggest that in early old age men without dementia, plasma NfL does not appear to be sensitive to cross-sectional individual differences in most domains of cognition or neuroimaging measures of gray and white matter. The revealed plasma NfL associations were limited to WMH for all participants and processing speed only within the MCI cohort. Importantly, considering cognitive status in community-based samples will better inform the interpretation of the relationships of plasma NfL with cognition and brain and may help resolve mixed findings in the literature. [ABSTRACT FROM AUTHOR]

Published
2024
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234. Pupillary dilation responses as a midlife indicator of risk for Alzheimer's disease: association with Alzheimer's disease polygenic risk.

Author

Kremen, William S., Panizzon, Matthew S., Elman, Jeremy A., Granholm, Eric L., Andreassen, Ole A., Dale, Anders M., Gillespie, Nathan A., Gustavson, Daniel E., Logue, Mark W., Lyons, Michael J., Neale, Michael C., Reynolds, Chandra A., Whitsel, Nathan, and Franz, Carol E.

Subjects
*ALZHEIMER'S disease, *LOCUS coeruleus, *MILD cognitive impairment, *MIDDLE-aged persons, *PUPILLARY reflex
Abstract

Locus coeruleus (LC) tau accumulation begins early. Targeting LC (dys)function might improve early identification for Alzheimer's disease (AD) risk. Pupillary responses during cognitive tasks are driven by the LC and index cognitive effort. Despite equivalent task performance, adults with mild cognitive impairment have greater pupil dilation/effort during digit span than cognitively normal (CN) individuals. We hypothesized that AD polygenic risk scores (AD-PRSs) would be associated with pupillary responses in middle-aged CN adults. Pupillary responses during digit span tasks were heritable (h2 = 0.30–0.36) in 1119 men aged 56–66 years. In a CN subset—all with comparable span capacities (n = 539)—higher AD-PRSs were associated with greater pupil dilation/effort in a high (9-digit) cognitive load condition (Cohen's d = 0.36 for upper vs. lower quartile of AD-PRS distribution). Results held up after controlling for APOE genotype. Results support pupillary response—and by inference, LC dysfunction—as a genetically mediated biomarker of early mild cognitive impairment/AD risk. In combination with other biomarkers, task-evoked pupillary responses may provide additional information for early screening of genetically at-risk individuals even before cognitive declines. • Locus coeruleus function may point to early Alzheimer's disease risk. • Pupil dilation response during cognitive tasks is thought to reflect locus coeruleus function. • Pupil response in cognitively normal adults is associated with Alzheimer's disease polygenic risk. • Pupil response may improve early screening before cognitive performance declines. [ABSTRACT FROM AUTHOR]

Published
2019
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235. On the winning side.

Author

Elman, Jeremy T.

Subjects
ALICE Corp. Pty. Ltd. v. CLS Bank International, STRYKER Corp. v. Zimmer Inc. (Supreme Court case), PATENT suits
Published
2017

236. Alcohol use and cognitive aging in middle-aged men: The Vietnam Era Twin Study of Aging.

Author

Garduno, Alexis C., Laughlin, Gail A., Bergstrom, Jaclyn, Tu, Xin M., Cummins, Kevin M., Franz, Carol E., Elman, Jeremy A., Lyons, Michael J., Reynolds, Chandra A., Neale, Michael C., Gillespie, Nathan A., Xian, Hong, McKenzie, Ruth E., Toomey, Rosemary, Kremen, William S., Panizzon, Matthew S., and McEvoy, Linda K.

Subjects
*COGNITIVE aging, *MIDDLE-aged men, *OLDER men, *TWIN studies, *ALCOHOL drinking, *COGNITION, *VERBAL memory
Abstract

Objective: To determine associations of alcohol use with cognitive aging among middle-aged men. Method: 1,608 male twins (mean 57 years at baseline) participated in up to three visits over 12 years, from 2003–2007 to 2016–2019. Participants were classified into six groups based on current and past self-reported alcohol use: lifetime abstainers, former drinkers, very light (1–4 drinks in past 14 days), light (5–14 drinks), moderate (15–28 drinks), and at-risk drinkers (>28 drinks in past 14 days). Linear mixed-effects regressions modeled cognitive trajectories by alcohol group, with time-based models evaluating rate of decline as a function of baseline alcohol use, and age-based models evaluating age-related differences in performance by current alcohol use. Analyses used standardized cognitive domain factor scores and adjusted for sociodemographic and health-related factors. Results: Performance decreased over time in all domains. Relative to very light drinkers, former drinkers showed worse verbal fluency performance, by –0.21 SD (95% CI –0.35, –0.07), and at-risk drinkers showed faster working memory decline, by 0.14 SD (95% CI 0.02, –0.20) per decade. There was no evidence of protective associations of light/moderate drinking on rate of decline. In age-based models, light drinkers displayed better memory performance at advanced ages than very light drinkers (+0.14 SD ; 95% CI 0.02, 0.20 per 10-years older age); likely attributable to residual confounding or reverse association. Conclusions: Alcohol consumption showed minimal associations with cognitive aging among middle-aged men. Stronger associations of alcohol with cognitive aging may become apparent at older ages, when cognitive abilities decline more rapidly. [ABSTRACT FROM AUTHOR]

Published
2023
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237. Alzheimer's Disease Polygenic Scores Predict Changes in Episodic Memory and Executive Function Across 12 Years in Late Middle Age.

Author

Gustavson, Daniel E., Reynolds, Chandra A., Hohman, Timothy J., Jefferson, Angela L., Elman, Jeremy A., Panizzon, Matthew S., Neale, Michael C., Logue, Mark W., Lyons, Michael J., Franz, Carol E., and Kremen, William S.

Subjects
*EXECUTIVE function, *ALZHEIMER'S disease, *EPISODIC memory, *MIDDLE age, *DISEASE risk factors, *GENOME-wide association studies
Abstract

Objective: Alzheimer's disease (AD) is highly heritable, and AD polygenic risk scores (AD-PRSs) have been derived from genome-wide association studies. However, the nature of genetic influences very early in the disease process is still not well known. Here we tested the hypothesis that an AD-PRSs would be associated with changes in episodic memory and executive function across late midlife in men who were cognitively unimpaired at their baseline midlife assessment.. Method: We examined 1168 men in the Vietnam Era Twin Study of Aging (VETSA) who were cognitively normal (CN) at their first of up to three assessments across 12 years (mean ages 56, 62, and 68). Latent growth models of episodic memory and executive function were based on 6–7 tests/subtests. AD-PRSs were based on Kunkle et al. (Nature Genetics, 51, 414–430, 2019), p  < 5×10−8 threshold. Results: AD-PRSs were correlated with linear slopes of change for both cognitive abilities. Men with higher AD-PRSs had steeper declines in both memory (r  = −.19, 95% CI [−.35, −.03]) and executive functioning (r  = −.27, 95% CI [−.49, −.05]). Associations appeared driven by a combination of APOE and non- APOE genetic influences. Conclusions: Memory is most characteristically impaired in AD, but executive functions are one of the first cognitive abilities to decline in midlife in normal aging. This study is among the first to demonstrate that this early decline also relates to AD genetic influences, even in men CN at baseline. [ABSTRACT FROM AUTHOR]

Published
2023
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238. Age‐dependent white matter disruptions after military traumatic brain injury: Multivariate analysis results from ENIGMA brain injury.

Author

Bouchard, Heather C., Sun, Delin, Dennis, Emily L., Newsome, Mary R., Disner, Seth G., Elman, Jeremy, Silva, Annelise, Velez, Carmen, Irimia, Andrei, Davenport, Nicholas D., Sponheim, Scott R., Franz, Carol E., Kremen, William S., Coleman, Michael J., Williams, M. Wright, Geuze, Elbert, Koerte, Inga K., Shenton, Martha E., Adamson, Maheen M., and Coimbra, Raul

Subjects
*BRAIN injuries, *WHITE matter (Nerve tissue), *MULTIVARIATE analysis, *NONNEGATIVE matrices, *MATRIX decomposition, *POST-traumatic stress disorder, *MILITARY nursing
Abstract

Mild Traumatic brain injury (mTBI) is a signature wound in military personnel, and repetitive mTBI has been linked to age‐related neurogenerative disorders that affect white matter (WM) in the brain. However, findings of injury to specific WM tracts have been variable and inconsistent. This may be due to the heterogeneity of mechanisms, etiology, and comorbid disorders related to mTBI. Non‐negative matrix factorization (NMF) is a data‐driven approach that detects covarying patterns (components) within high‐dimensional data. We applied NMF to diffusion imaging data from military Veterans with and without a self‐reported TBI history. NMF identified 12 independent components derived from fractional anisotropy (FA) in a large dataset (n = 1,475) gathered through the ENIGMA (Enhancing Neuroimaging Genetics through Meta‐Analysis) Military Brain Injury working group. Regressions were used to examine TBI‐ and mTBI‐related associations in NMF‐derived components while adjusting for age, sex, post‐traumatic stress disorder, depression, and data acquisition site/scanner. We found significantly stronger age‐dependent effects of lower FA in Veterans with TBI than Veterans without in four components (q < 0.05), which are spatially unconstrained by traditionally defined WM tracts. One component, occupying the most peripheral location, exhibited significantly stronger age‐dependent differences in Veterans with mTBI. We found NMF to be powerful and effective in detecting covarying patterns of FA associated with mTBI by applying standard parametric regression modeling. Our results highlight patterns of WM alteration that are differentially affected by TBI and mTBI in younger compared to older military Veterans. [ABSTRACT FROM AUTHOR]

Published
2022
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239. Long‐term associations of cigarette smoking in early mid‐life with predicted brain aging from mid‐ to late life.

Author

Whitsel, Nathan, Reynolds, Chandra A., Buchholz, Erik J., Pahlen, Shandell, Pearce, Rahul C., Hatton, Sean N., Elman, Jeremy A., Gillespie, Nathan A., Gustavson, Daniel E., Puckett, Olivia K., Dale, Anders M., Eyler, Lisa T., Fennema‐Notestine, Christine, Hagler, Donald J., Hauger, Richard L., McEvoy, Linda K., McKenzie, Ruth, Neale, Michael C., Panizzon, Matthew S., and Sanderson‐Cimino, Mark

Subjects
*BRAIN physiology, *STRUCTURAL equation modeling, *SCIENTIFIC observation, *CONFIDENCE intervals, *TIME, *SELF-evaluation, *AGE distribution, *MAGNETIC resonance imaging, *REGRESSION analysis, *AGING, *ALCOHOL drinking, *HEALTH, *INFORMATION resources, *DESCRIPTIVE statistics, *SMOKING, *DATA analysis software, *LONGITUDINAL method, *ADULTS, *MIDDLE age
Abstract

Background and aims: Smoking is associated with increased risk for brain aging/atrophy and dementia. Few studies have examined early associations with brain aging. This study aimed to measure whether adult men with a history of heavier smoking in early mid‐life would have older than predicted brain age 16–28 years later. Design Prospective cohort observational study, utilizing smoking pack years data from average age 40 (early mid‐life) predicting predicted brain age difference scores (PBAD) at average ages 56, 62 (later mid‐life) and 68 years (early old age). Early mid‐life alcohol use was also evaluated. Setting: Population‐based United States sample. Participants/cases: Participants were male twins of predominantly European ancestry who served in the United States military between 1965 and 1975. Structural magnetic resonance imaging (MRI) began at average age 56. Subsequent study waves included most baseline participants; attrition replacement subjects were added at later waves. Measurements Self‐reported smoking information was used to calculate pack years smoked at ages 40, 56, 62, and 68. MRIs were processed with the Brain‐Age Regression Analysis and Computation Utility software (BARACUS) program to create PBAD scores (chronological age—predicted brain age) acquired at average ages 56 (n = 493; 2002–08), 62 (n = 408; 2009–14) and 68 (n = 499; 2016–19). Findings In structural equation modeling, age 40 pack years predicted more advanced age 56 PBAD [β = −0.144, P = 0.012, 95% confidence interval (CI) = –0.257, −0.032]. Age 40 pack years did not additionally predict PBAD at later ages. Age 40 alcohol consumption, but not a smoking × alcohol interaction, predicted more advanced PBAD at age 56 (β = −0.166, P = 0.001, 95% CI = –0.261, –0.070) with additional influences at age 62 (β = −0.115, P = 0.005, 95% CI = –0.195, –0.036). Age 40 alcohol did not predict age 68 PBAD. Within‐twin‐pair analyses suggested some genetic mechanism partially underlying effects of alcohol, but not smoking, on PBAD. Conclusions: Heavier smoking and alcohol consumption by age 40 appears to predict advanced brain aging by age 56 in men. [ABSTRACT FROM AUTHOR]

Published
2022
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240. The value of slot machine patents.

Author

ELMAN, JEREMY T.

Subjects
SLOT machines, PATENTS, GAMING equipment
Abstract

The article focuses on the importance of slot machine patents. Topics include introduction of patent to the slot machine entitled "Electronic Gaming Device Utilizing a Random Number Generator for Selecting the Reel Stop Positions" by Norwegian mathematician Inge Telnaes, claim of slot machines manufacturer Bally Technologies Inc. and IGT (International Game Technology) regarding invention of wheel bonusing and constant demand for new and varied games as of March 2014.

Published
2014

243. The genetic and environmental etiology of novel frequency-driven regional parcellations of abnormal white matter.

Author

Lin SJ, Gillespie NA, Notestine R, Gamst AC, Chen AM, McEvoy LK, Panizzon MS, Elman JA, Glatt SJ, Hagler DJ Jr, Neale MC, Franz CE, Kremen WS, and Fennema-Notestine C

Subjects
Humans, Aged, Male, Female, Middle Aged, Brain pathology, Brain diagnostic imaging, White Matter diagnostic imaging, White Matter pathology, Magnetic Resonance Imaging, Gene-Environment Interaction
Abstract

The prevalence of white matter disease increases with age and is associated with cerebrovascular disease, cognitive decline, and risk for dementia. MRI measures of abnormal signal in the white matter (AWM) provide estimates of damage, however, regional patterns of AWM may be differentially influenced by genetic or environmental factors. With our data-driven regional parcellation approach, we created a probability distribution atlas using Vietnam Era Twin Study of Aging (VETSA) data (n = 475, mean age 67.6 years) and applied a watershed algorithm to define separate regional parcellations. We report biometrical twin modeling for five anatomically distinct regions: (1) Posterior, (2) Superior frontal and parietal, (3) Anterior and inferior frontal with deep areas, (4) Occipital, and (5) Anterior periventricular. We tested competing multivariate hypotheses to identify unique influences and to explain sources of covariance among the parcellations. Family aggregation could be entirely explained by additive genetic influences, with additive genetic variance (heritability) ranging from 0.69 to 0.79. Most genetic correlations between parcellations ranged from moderate to high (r g  = 0.57-0.85), although two were small (r g  = 0.35-0.39), consistent with varying degrees of unique genetic influences. This proof-of-principle investigation demonstrated the value of our novel, data-driven parcellations, with identifiable genetic and environmental differences, for future exploration., (© 2024 Wiley Periodicals LLC.)

Published
2025
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244. Cortical Surface Area Profile Mediates Effects of Childhood Disadvantage on Later-Life General Cognitive Ability.

Author

Tang R, Elman JA, Reynolds CA, Puckett OK, Panizzon MS, Lyons MJ, Hagler DJ Jr, Fennema-Notestine C, Eyler LT, Dorros SM, Dale AM, Kremen WS, and Franz CE

Subjects
Humans, Male, Aged, Middle Aged, Cognition physiology, Adverse Childhood Experiences statistics & numerical data, Magnetic Resonance Imaging, Cerebral Cortex diagnostic imaging
Abstract

Objectives: Childhood disadvantage is associated with lower general cognitive ability (GCA) and brain structural differences in midlife and older adulthood. However, the neuroanatomical mechanisms underlying childhood disadvantage effects on later-life GCA remain poorly understood. Although total surface area (SA) has been linked to lifespan GCA differences, total SA does not capture the nonuniform nature of childhood disadvantage effects on neuroanatomy, which varies across unimodal and transmodal cortices. Here, we examined whether cortical SA profile-the extent to which the spatial patterning of SA deviates from the normative unimodal-transmodal cortical organization-is a mediator of childhood disadvantage effects on later-life GCA., Methods: In 477 community-dwelling men aged 56-72 years old, childhood disadvantage index was derived from four indicators of disadvantages and GCA was assessed using a standardized test. Cortical SA was obtained from structural magnetic resonance imaging. For cortical SA profile, we calculated the spatial similarity between maps of individual cortical SA and MRI-derived principal gradient (i.e., unimodal-transmodal organization). Mediation analyses were conducted to examine the indirect effects of childhood disadvantage index through cortical SA profile on GCA., Results: Around 1.31% of childhood disadvantage index effects on later-life GCA were mediated by cortical SA profile, whereas total SA did not. Higher childhood disadvantage index was associated with more deviation of the cortical SA spatial patterning from the principal gradient, which in turn related to lower later-life GCA., Discussion: Childhood disadvantage may contribute to later-life GCA differences partly by influencing the spatial patterning of cortical SA in a way that deviates from the normative cortical organizational principle., (© The Author(s) 2024. Published by Oxford University Press on behalf of The Gerontological Society of America. All rights reserved. For commercial re-use, please contact reprints@oup.com for reprints and translation rights for reprints. All other permissions can be obtained through our RightsLink service via the Permissions link on the article page on our site—for further information please contact journals.permissions@oup.com.)

Published
2024
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245. Detecting Boolean Asymmetric Relationships with a Loop Counting Technique and its Implications for Analyzing Heterogeneity within Gene Expression Datasets.

Author

Zhou H, Lin W, Labra SR, Lipton SA, Elman JA, Schork NJ, and Rangan AV

Abstract

Many traditional methods for analyzing gene-gene relationships focus on positive and negative correlations, both of which are a kind of 'symmetric' relationship. Biclustering is one such technique that typically searches for subsets of genes exhibiting correlated expression among a subset of samples. However, genes can also exhibit 'asymmetric' relationships, such as 'if-then' relationships used in boolean circuits. In this paper we develop a very general method that can be used to detect biclusters within gene-expression data that involve subsets of genes which are enriched for these 'boolean-asymmetric' relationships (BARs). These BAR-biclusters can correspond to heterogeneity that is driven by asymmetric gene-gene interactions, e.g., reflecting regulatory effects of one gene on another, rather than more standard symmetric interactions. Unlike typical approaches that search for BARs across the entire population, BAR-biclusters can detect asymmetric interactions that only occur among a subset of samples. We apply our method to a single-cell RNA-sequencing data-set, demonstrating that the statistically-significant BARbiclusters indeed contain additional information not present within the more traditional 'boolean-symmetric'-biclusters. For example, the BAR-biclusters involve different subsets of cells, and highlight different gene-pathways within the data-set. Moreover, by combining the boolean-asymmetric- and boolean-symmetricsignals, one can build linear classifiers which outperform those built using only traditional boolean-symmetric signals.

Published
2024
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246. Heterogeneity analysis provides evidence for a genetically homogeneous subtype of bipolar-disorder.

Author

McGrouther CC, Rangan AV, Di Florio A, Elman JA, Schork NJ, and Kelsoe J

Abstract

Background: Bipolar Disorder (BD) is a complex disease. It is heterogeneous, both at the phenotypic and genetic level, although the extent and impact of this heterogeneity is not fully understood. One way to assess this heterogeneity is to look for patterns in the subphenotype data. Because of the variability in how phenotypic data was collected by the various BD studies over the years, homogenizing this subphenotypic data is a challenging task, and so is replication. An alternative methodology, taken here, is to set aside the intricacies of subphenotype and allow the genetic data itself to determine which subjects define a homogeneous genetic subgroup (termed 'bicluster' below)., Results: In this paper, we leverage recent advances in heterogeneity analysis to look for genetically-driven subgroups (i.e., biclusters) within the broad phenotype of Bipolar Disorder. We first apply this covariate-corrected biclustering algorithm to a cohort of 2524 BD cases and 4106 controls from the Bipolar Disease Research Network (BDRN) within the Psychiatric Genomics Consortium (PGC). We find evidence of genetic heterogeneity delineating a statistically significant bicluster comprising a subset of BD cases which exhibits a disease-specific pattern of differential-expression across a subset of SNPs. This disease-specific genetic pattern (i.e., 'genetic subgroup') replicates across the remaining data-sets collected by the PGC containing 5781/8289, 3581/7591, and 6825/9752 cases/controls, respectively. This genetic subgroup (discovered without using any BD subtype information) was more prevalent in Bipolar type-I than in Bipolar type-II., Conclusions: Our methodology has successfully identified a replicable homogeneous genetic subgroup of bipolar disorder. This subgroup may represent a collection of correlated genetic risk-factors for BDI. By investigating the subgroup's bicluster-informed polygenic-risk-scoring (PRS), we find that the disease-specific pattern highlighted by the bicluster can be leveraged to eliminate noise from our GWAS analyses and improve risk prediction. This improvement is particularly notable when using only a relatively small subset of the available SNPs, implying improved SNP replication. Though our primary focus is only the analysis of disease-related signal, we also identify replicable control-related heterogeneity., Competing Interests: Competing interests The authors declare that they have no competing interests.

Published
2024

247. Brain reserve in midlife is associated with executive function changes across 12 years.

Author

Gustavson DE, Elman JA, Reynolds CA, Eyler LT, Fennema-Notestine C, Puckett OK, Panizzon MS, Gillespie NA, Neale MC, Lyons MJ, Franz CE, and Kremen WS

Subjects
Humans, Male, Cognition physiology, Genotype, Longitudinal Studies, Neuroimaging, Aging physiology, Aging genetics, Aging psychology, Apolipoproteins E genetics, Brain diagnostic imaging, Brain physiology, Cognitive Reserve physiology, Executive Function physiology
Abstract

We examined how brain reserve in midlife, measured by brain-predicted age difference scores (Brain-PADs), predicted executive function concurrently and longitudinally into early old age, and whether these associations were moderated by young adult cognitive reserve or APOE genotype. 508 men in the Vietnam Era Twin Study of Aging (VETSA) completed neuroimaging assessments at mean age 56 and six executive function tasks at mean ages 56, 62, and 68 years. Results indicated that greater brain reserve at age 56 was associated with better concurrent executive function (r=.10, p=.040) and less decline in executive function over 12 years (r=.34, p=.001). These associations were not moderated by cognitive reserve or APOE genotype. Twin analysis suggested associations with executive function slopes were driven by genetic influences. Our findings suggest that greater brain reserve allowed for better cognitive maintenance from middle- to old age, driven by a genetic association. The results are consistent with differential preservation of executive function based on brain reserve that is independent of young adult cognitive reserve or APOE genotype., Competing Interests: Declaration of Competing Interest The authors declare that they have no known competing financial interests or personal relationships that could have appeared to influence the work reported in this paper., (Copyright © 2024 Elsevier Inc. All rights reserved.)

Published
2024
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248. Testing the causal impact of amyloidosis on total Tau using a genetically informative sample of adult male twins.

Author

Gillespie NA, Neale MC, Panizzon MS, McKenzie RE, Tu XM, Xian H, Reynolds CA, Lyons MJ, Rissman RA, Elman JA, Franz C, and Kremen WS

Abstract

Introduction: The amyloid cascade hypothesis predicts that amyloid-beta (Aβ) aggregation drives tau tangle accumulation. We tested competing causal and non-causal hypotheses regarding the direction of causation between Aβ40 and Aβ42 and total Tau (t-Tau) plasma biomarkers., Methods: Plasma Aβ40, Aβ42, t-Tau, and neurofilament light chain (NFL) were measured in 1,035 men (mean = 67.0 years) using Simoa immunoassays. Genetically informative twin modeling tested the direction of causation between Aβs and t-Tau., Results: No clear evidence that Aβ40 or Aβ42 directly causes changes in t-Tau was observed; the alternative causal hypotheses also fit the data well. In contrast, exploratory analyses suggested a causal impact of the Aβ biomarkers on NFL. Separately, reciprocal causation was observed between t-Tau and NFL., Discussion: Plasma Aβ40 or Aβ42 do not appear to have a direct causal impact on t-Tau. In contrast, Aβ aggregation may causally impact NFL in cognitively unimpaired men in their late 60s., Competing Interests: Conflicts No authors reported a conflict of interest.

Published
2024
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249. Association Between Traumatic Brain Injury and Cognitive Decline Among Middle-to-Older Aged Men in the Vietnam Era Twin Study of Aging.

Author

Posis AIB, Alcaraz JE, Parada H Jr, Shadyab AH, Elman JA, Panizzon MS, Reynolds CA, Franz CE, Kremen WS, and McEvoy LK

Abstract

Traumatic brain injury (TBI) is associated with increased risk of dementia. However, whether TBI is associated with greater cognitive decline over time in specific cognitive domains among older adults is not well understood. This prospective cohort study used data from 1476 male Vietnam Era Twin Study of Aging participants (average age at study entry = 57.9 years, range = 51-71 years; 97.6% non-Hispanic; 92.5% White) collected from 2003 to 2019, who had complete information on prior TBI. Participants completed a comprehensive neuropsychological assessment at up to three visits over up to a 12-year follow-up period during which they also self-reported their history of TBI. Multivariable, linear mixed-effects models were used to assess associations between TBI and cognitive performance trajectories. Effect measure modification by apolipoprotein E ( APOE ) epsilon 4 ( ε4 ) genotype status was assessed in a subset of participants. Thirty-one percent of participants reported a history of TBI; 29.4% were APOE ε4 carrier status, TBI was associated with a larger magnitude of decline in executive function for APOE ε4 carrier status, TBI was associated with a larger magnitude of decline in executive function for APOE ε4 carriers and among those who reported TBI in early life. These findings support the importance of a life course perspective when considering factors that may influence cognitive health in aging.P Interaction = 0.03). In sensitivity analyses, TBI earlier in life (before military induction, average age = 20 years) was associated with faster declines in executive function compared to no TBI, irrespective of APOE ε4 status. In this sample of middle-to-older aged men, TBI was associated with faster declines in executive function among APOE ε4 carriers and among those who reported TBI in early life. These findings support the importance of a life course perspective when considering factors that may influence cognitive health in aging., (© Alexander Ivan B. Posis et al., 2024; Published by Mary Ann Liebert, Inc.)

Published
2024
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250. Exploring the genetic heterogeneity of Alzheimer's disease: Evidence for genetic subtypes.

Author

Elman JA, Schork NJ, and Rangan AV

Abstract

Background: Alzheimer's disease (AD) exhibits considerable phenotypic heterogeneity, suggesting the potential existence of subtypes. AD is under substantial genetic influence, thus identifying systematic variation in genetic risk may provide insights into disease origins., Objective: We investigated genetic heterogeneity in AD risk through a multi-step analysis., Methods: We performed principal component analysis (PCA) on AD-associated variants in the UK Biobank (AD cases=2,739, controls=5,478) to assess structured genetic heterogeneity. Subsequently, a biclustering algorithm searched for distinct disease-specific genetic signatures among subsets of cases. Replication tests were conducted using the Alzheimer's Disease Neuroimaging Initiative (ADNI) dataset (AD cases=500, controls=470). We categorized a separate set of ADNI individuals with mild cognitive impairment (MCI; n=399) into genetic subtypes and examined cognitive, amyloid, and tau trajectories., Results: PCA revealed three distinct clusters ("constellations") driven primarily by different correlation patterns in a region of strong LD surrounding the MAPT locus. Constellations contained a mixture of cases and controls, reflecting disease-relevant but not disease-specific structure. We found two disease-specific biclusters among AD cases. Pathway analysis linked bicluster-associated variants to neuron morphogenesis and outgrowth. Disease-relevant and disease-specific structure replicated in ADNI, and bicluster 2 exhibited increased CSF p-tau and cognitive decline over time., Conclusions: This study unveils a hierarchical structure of AD genetic risk. Disease-relevant constellations may represent haplotype structure that does not increase risk directly but may alter the relative importance of other genetic risk factors. Biclusters may represent distinct AD genetic subtypes. This structure is replicable and relates to differential pathological accumulation and cognitive decline over time., Competing Interests: Conflict of interest Jeremy Elman is an Editorial Board Member of this journal but was not involved in the peer-review process of this article nor had access to any information regarding its peer-review. All other authors have no conflict of interest to report.

Published
2024
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