Your search keyword '"Mielke, Michelle."' showing total 524 results

1. Relationships between PET and blood plasma biomarkers in corticobasal syndrome.

Author

Singh, Neha Atulkumar, Alnobani, Alla, Graff‐Radford, Jonathan, Machulda, Mary M., Mielke, Michelle M., Schwarz, Christopher G., Senjem, Matthew L., Jack, Clifford R., Lowe, Val J., Kanekiyo, Takahisa, Josephs, Keith A., and Whitwell, Jennifer L.

Abstract

INTRODUCTION: Corticobasal syndrome (CBS) can result from underlying Alzheimer's disease (AD) pathologies. Little is known about the utility of blood plasma metrics to predict positron emission tomography (PET) biomarker‐confirmed AD in CBS. METHODS: A cohort of eighteen CBS patients (8 amyloid beta [Aβ]+; 10 Aβ−) and 8 cognitively unimpaired (CU) individuals underwent PET imaging and plasma analysis. Plasma concentrations were compared using a Kruskal–Wallis test. Spearman correlations assessed relationships between plasma concentrations and PET uptake. RESULTS: CBS Aβ+ group showed a reduced Aβ42/40 ratio, with elevated phosphorylated tau (p‐tau)181, glial fibrillary acidic protein (GFAP), and neurofilament light (NfL) concentrations, while CBS Aβ− group only showed elevated NfL concentration compared to CU. Both p‐tau181 and GFAP were able to differentiate CBS Aβ− from CBS Aβ+ and showed positive associations with Aβ and tau PET uptake. DISCUSSION: This study supports use of plasma p‐tau181 and GFAP to detect AD in CBS. NfL shows potential as a non‐specific disease biomarker of CBS regardless of underlying pathology. Highlights: Plasma phosphorylated tau (p‐tau)181 and glial fibrillary acidic protein (GFAP) concentrations differentiate corticobasal syndrome (CBS) amyloid beta (Aβ)− from CBS Aβ+.Plasma neurofilament light concentrations are elevated in CBS Aβ− and Aβ+ compared to controls.Plasma p‐tau181 and GFAP concentrations were associated with Aβ and tau positron emission tomography (PET) uptake.Aβ42/40 ratio showed a negative correlation with Aβ PET uptake. [ABSTRACT FROM AUTHOR]

Published

2024

2. Longitudinal associations of reproductive factors and exogeneous estrogens with neuroimaging biomarkers of Alzheimer's disease and cerebrovascular disease.

Author

Lee, Jillian K., Raghavan, Sheelakumari, Christenson, Luke R., Frank, Ryan D., Kantarci, Kejal, Rocca, Walter A., Vemuri, Prashanthi, and Mielke, Michelle M.

Abstract

INTRODUCTION: Female‐specific reproductive factors and exogeneous estrogen use are associated with cognition in later life. However, the underlying mechanisms are not understood. The present study aimed to investigate the effect of reproductive factors on neuroimaging biomarkers of Alzheimer's disease (AD) and cerebrovascular pathologies. METHODS: We evaluated 389 females (median age of 71.7 years) enrolled in the Mayo Clinic Study of Aging with reproductive history data and longitudinal magnetic resonance imaging (MRI) scans. We used linear mixed effect models to examine the associations between reproductive factors and changes in neuroimaging measures. RESULTS: Ever hormonal contraception (HC) use was longitudinally associated with higher fractional anisotropy across the corpus callosum, lower white matter hyperintensity (WMH) volume, and greater cortical thickness in an AD meta‐region of interest (ROI). The initiation of menopausal hormone therapy (MHT) > 5 years post menopause was associated with higher WMH volume. DISCUSSION: HC use and initiation of MHT >5 years post menopause were generally associated with neuroimaging biomarkers of cerebrovascular pathologies. Highlights: Hormonal contraception use was associated with better brain white matter (WM) integrity.Initiation of menopausal hormone therapy >5 years post menopause was associated with worsening brain WM integrity.Hormonal contraception use was associated with greater cortical thickness.Ages at menarche and menopause and number of pregnancies were not associated with imaging measures.There were few associations between reproductive factors or exogenous estrogens and amyloid or tau PET. [ABSTRACT FROM AUTHOR]

Published

2024

3. Premenopausal bilateral oophorectomy and brain white matter brain integrity in later‐life.

Author

Mielke, Michelle M., Frank, Ryan D., Christenson, Luke R., Reid, Robert I., Fields, Julie A., Knyazhanskaya, Zhenya E., Kara, Firat, Vemuri, Prashanthi, Rocca, Walter A., and Kantarci, Kejal

Abstract

INTRODUCTION: Premenopausal bilateral oophorectomy (PBO) is associated with later‐life cognition, but the underlying brain changes remain unclear. We assessed the impact of PBO and PBO age on white matter integrity. METHODS: Female participants with regional diffusion tensor imaging (DTI) metrics of fractional anisotropy (FA) and mean diffusivity (MD) were included (22 with PBO < 40 years; 43 with PBO 40‐45 years; 39 with PBO 46‐49 years; 907 referents without PBO < 50 years). Linear regression models adjusted for age and apolipoprotein E (APOE) genotype. RESULTS: Females with PBO < 40 years, compared to referents, had lower FA and higher MD in the anterior corona radiata, genu of the corpus collosum, inferior fronto‐occipital fasciculus, superior occipital, and superior temporal white matter. Females who underwent PBO between 45 and 49 also had some changes in white matter integrity. DISCUSSION: Females who underwent PBO < 40 years had reduced white matter integrity across multiple regions in later‐life. These results are important for females considering PBO for noncancerous conditions. Highlights: Females with premenopausal bilateral oophorectomy (PBO) < 40 years had lower FA versus referents.Females with PBO < 40 years had higher MD in many regions versus referents.Adjusting for estrogen replacement therapy use did not attenuate results.Females with PBO 45‐49 years also had some white matter changes versus referents. [ABSTRACT FROM AUTHOR]

Published

2024

4. Associations among plasma, MRI, and amyloid PET biomarkers of Alzheimer's disease and related dementias and the impact of health‐related comorbidities in a community‐dwelling cohort.

Author

Rudolph, Marc D., Sutphen, Courtney L., Register, Thomas C., Whitlow, Christopher T., Solingapuram Sai, Kiran K., Hughes, Timothy M., Bateman, James R., Dage, Jeffrey L., Russ, Kristen A., Mielke, Michelle M., Craft, Suzanne, and Lockhart, Samuel N.

Abstract

INTRODUCTION: We evaluated associations between plasma and neuroimaging‐derived biomarkers of Alzheimer's disease and related dementias and the impact of health‐related comorbidities. METHODS: We examined plasma biomarkers (neurofilament light chain, glial fibrillary acidic protein, amyloid beta [Aβ] 42/40, phosphorylated tau 181) and neuroimaging measures of amyloid deposition (Aβ‐positron emission tomography [PET]), total brain volume, white matter hyperintensity volume, diffusion‐weighted fractional anisotropy, and neurite orientation dispersion and density imaging free water. Participants were adjudicated as cognitively unimpaired (CU; N = 299), mild cognitive impairment (MCI; N = 192), or dementia (DEM; N = 65). Biomarkers were compared across groups stratified by diagnosis, sex, race, and APOE ε4 carrier status. General linear models examined plasma‐imaging associations before and after adjusting for demographics (age, sex, race, education), APOE ε4 status, medications, diagnosis, and other factors (estimated glomerular filtration rate [eGFR], body mass index [BMI]). RESULTS: Plasma biomarkers differed across diagnostic groups (DEM > MCI > CU), were altered in Aβ‐PET‐positive individuals, and were associated with poorer brain health and kidney function. DISCUSSION: eGFR and BMI did not substantially impact associations between plasma and neuroimaging biomarkers. Highlights: Plasma biomarkers differ across diagnostic groups (DEM > MCI > CU) and are altered in Aβ‐PET‐positive individuals.Altered plasma biomarker levels are associated with poorer brain health and kidney function.Plasma and neuroimaging biomarker associations are largely independent of comorbidities. [ABSTRACT FROM AUTHOR]

Published

2024

5. Racial discrimination during middle age predicts higher serum phosphorylated tau and neurofilament light chain levels a decade later: A study of aging black Americans.

Author

Simons, Ronald L., Ong, Mei Ling, Lei, Man‐Kit, Beach, Steven R. H., Zhang, Yue, Philibert, Robert, and Mielke, Michelle M.

Abstract

INTRODUCTION: Recent evidence suggests that exposure to the stress of racism may increase the risk of dementia for Black Americans. METHODS: The present study used 17 years of data from a sample of 255 Black Americans to investigate the extent to which exposure to racial discrimination predicts subsequent changes in serum Alzheimer's Disease Research Center (ADRC) biomarkers: serum phosphorylated tau181(p‐tau181), neurofilament light (NfL), and glial fibrillary acidic protein (GFAP). We hypothesized that racial discrimination assessed during middle age would predict increases in these serum biomarkers as the participants aged into their 60s. RESULTS: Our findings indicate that exposure to various forms of racial discrimination during a person's 40s and early 50s predicts an 11‐year increase in both serum p‐tau181 and NfL. Racial discrimination was not associated with subsequent levels of GFAP. DISCUSSION: These findings suggest that racial discrimination in midlife may contribute to increased AD pathology and neurodegeneration later in life. Highlights: A 17‐year longitudinal study of Black Americans.Assessments of change in serum p‐tau181, neurofilament light, and glial fibrillary acidic protein.Exposure to racial discrimination during middle age predicted increases in p‐tau181 and neurofilament light.Education was positively related to both p‐tau181 and exposure to racial discrimination. [ABSTRACT FROM AUTHOR]

Published

2024

6. Plasma glial fibrillary acidic protein in the visual and language variants of Alzheimer's disease.

Author

Sintini, Irene, Singh, Neha Atulkumar, Li, Danni, Mielke, Michelle M., Machulda, Mary M., Schwarz, Christopher G., Senjem, Matthew L., Jack, Clifford R., Lowe, Val J., Graff‐Radford, Jonathan, Josephs, Keith A., and Whitwell, Jennifer L.

Abstract

INTRODUCTION: Glial fibrillary acidic protein (GFAP) in plasma is a proxy for astrocytic activity and is elevated in amyloid‐β (Aβ)‐positive individuals, making GFAP a potential blood‐based biomarker for Alzheimer's disease (AD). METHODS: We assessed plasma GFAP in 72 Aβ‐positive participants diagnosed with the visual or language variant of AD who underwent Aβ‐ and tau‐PET. Fifty‐nine participants had follow‐up imaging. Linear regression was applied on GFAP and imaging quantities. RESULTS: GFAP did not correlate with Aβ‐ or tau‐PET cross‐sectionally. There was a limited positive correlation between GFAP and rates of tau accumulation, particularly in the language variant of AD, although associations were weaker after removing one outlier patient with the highest GFAP level. DISCUSSION: Among Aβ‐positive AD participants with atypical presentations, plasma GFAP did not correlate with levels of AD pathology on PET, suggesting that the associations between GFAP and AD pathology might plateau during the advanced phase of the disease. [ABSTRACT FROM AUTHOR]

Published

2024

7. Comparison of plasma biomarkers and amyloid PET for predicting memory decline in cognitively unimpaired individuals.

Author

Jack, Clifford R., Wiste, Heather J., Algeciras‐Schimnich, Alicia, Weigand, Stephen D., Figdore, Dan J., Lowe, Val J., Vemuri, Prashanthi, Graff‐Radford, Jonathan, Ramanan, Vijay K., Knopman, David S., Mielke, Michelle M., Machulda, Mary M., Fields, Julie, Schwarz, Christopher G., Cogswell, Petrice M., Senjem, Matthew L., Therneau, Terry M., and Petersen, Ronald C.

Abstract

BACKGROUND: We compared the ability of several plasma biomarkers versus amyloid positron emission tomography (PET) to predict rates of memory decline among cognitively unimpaired individuals. METHODS: We studied 645 Mayo Clinic Study of Aging participants. Predictor variables were age, sex, education, apolipoprotein E (APOE) ε4 genotype, amyloid PET, and plasma amyloid beta (Aβ)42/40, phosphorylated tau (p‐tau)181, neurofilament light (NfL), glial fibrillary acidic protein (GFAP), and p‐tau217. The outcome was a change in a memory composite measure. RESULTS: All plasma biomarkers, except NfL, were associated with mean memory decline in models with individual biomarkers. However, amyloid PET and plasma p‐tau217, along with age, were key variables independently associated with mean memory decline in models combining all predictors. Confidence intervals were narrow for estimates of population mean prediction, but person‐level prediction intervals were wide. DISCUSSION: Plasma p‐tau217 and amyloid PET provide useful information about predicting rates of future cognitive decline in cognitively unimpaired individuals at the population mean level, but not at the individual person level. [ABSTRACT FROM AUTHOR]

Published

2024

8. Liver integrity and the risk of Alzheimer's disease and related dementias.

Author

Lu, Yifei, Pike, James Russell, Hoogeveen, Ron C., Walker, Keenan A., Raffield, Laura M., Selvin, Elizabeth, Avery, Christy L., Engel, Stephanie M., Mielke, Michelle M., Garcia, Tanya, and Palta, Priya

Abstract

INTRODUCTION: We examined midlife (1990–1992, mean age 57) and late‐life (2011–2013, mean age 75) nonalcoholic fatty liver disease (NAFLD) and aminotransferase with incident dementia risk through 2019 in the Atherosclerosis Risk in Communities (ARIC) Study. METHODS: We characterized NAFLD using the fatty liver index and fibrosis‐4, and we categorized aminotransferase using the optimal equal‐hazard ratio (HR) approach. We estimated HRs for incident dementia ascertained from multiple data sources. RESULTS: Adjusted for demographics, alcohol consumption, and kidney function, individuals with low, intermediate, and high liver fibrosis in midlife (HRs: 1.45, 1.40, and 2.25, respectively), but not at older age, had higher dementia risks than individuals without fatty liver. A U‐shaped association was observed for alanine aminotransferase with dementia risk, which was more pronounced in late‐life assessment. DISCUSSION: Our findings highlight dementia burden in high‐prevalent NAFLD and the important feature of late‐life aminotransaminase as a surrogate biomarker linking liver hypometabolism to dementia. Highlights: Although evidence of liver involvement in dementia development has been documented in animal studies, the evidence in humans is limited.Midlife NAFLD raised dementia risk proportionate to severity.Late‐life NAFLD was not associated with a high risk of dementia.Low alanine aminotransferase was associated with an elevated dementia risk, especially when measured in late life. [ABSTRACT FROM AUTHOR]

Published

2024

9. Modeling the temporal evolution of plasma p‐tau in relation to amyloid beta and tau PET.

Author

Cogswell, Petrice M., Lundt, Emily S., Therneau, Terry M., Wiste, Heather J., Graff‐Radford, Jonathan, Algeciras‐Schimnich, Alicia, Lowe, Val J., Mielke, Michelle M., Schwarz, Christopher G., Senjem, Matthew L., Gunter, Jeffrey L., Knopman, David S., Vemuri, Prashanthi, Petersen, Ronald C., and Jack Jr, Clifford R.

Abstract

INTRODUCTION: The timing of plasma biomarker changes is not well understood. The goal of this study was to evaluate the temporal co‐evolution of plasma and positron emission tomography (PET) Alzheimer's disease (AD) biomarkers. METHODS: We included 1408 Mayo Clinic Study of Aging and Alzheimer's Disease Research Center participants. An accelerated failure time (AFT) model was fit with amyloid beta (Aβ) PET, tau PET, plasma p‐tau217, p‐tau181, and glial fibrillary acidic protein (GFAP) as endpoints. RESULTS: Individual timing of plasma p‐tau progression was strongly associated with Aβ PET and GFAP progression. In the population, GFAP became abnormal first, then Aβ PET, plasma p‐tau, and tau PET temporal meta‐regions of interest when applying cut points based on young, cognitively unimpaired participants. DISCUSSION: Plasma p‐tau is a stronger indicator of a temporally linked response to elevated brain Aβ than of tau pathology. While Aβ deposition and a rise in GFAP are upstream events associated with tau phosphorylation, the temporal link between p‐tau and Aβ PET was the strongest. Highlights: Plasma p‐tau progression was more strongly associated with Aβ than tau PET.Progression on plasma p‐tau was associated with Aβ PET and GFAP progression.P‐tau181 and p‐tau217 become abnormal after Aβ PET and before tau PET.GFAP became abnormal first, before plasma p‐tau and Aβ PET. [ABSTRACT FROM AUTHOR]

Published

2024

10. Associations of reproductive factors and exogenous estrogens with global and domain‐specific cognition in later life.

Author

Lee, Jillian K., Frank, Ryan D., Christenson, Luke R., Fields, Julie A., Rocca, Walter A., and Mielke, Michelle M.

Abstract

INTRODUCTION: Few studies have comprehensively examined the impact of reproductive factors (i.e., reproductive window, parity, hormonal contraception [HC], and menopausal hormone therapy [MHT]) on global and domain‐specific cognition in later life. METHODS: We studied a population‐based sample of 2458 women (median age 74.2 years) residing in Olmsted County, Minnesota; participants underwent a clinical evaluation and comprehensive cognitive testing. RESULTS: The length of a woman's reproductive window was not associated with cognition. Higher parity was associated with greater cognitive decline in all domains. Ever HC use was associated with less decline in all domains. Ever MHT use was associated with greater decline in global cognition and all domain‐specific z‐scores except visuospatial; results were driven by women who initiated MHT 5 or more years after menopause. Additional adjustments for APOE and vascular‐related covariates did not attenuate the results. DISCUSSION: Multiple reproductive risk factors are associated with cognitive decline in later life. Highlights: The length of a woman's reproductive window was not associated with cognition longitudinally.Greater parity was associated with greater cognitive decline longitudinally.Ever HC use was associated with less decline in global cognition and all domain‐specific z‐scores longitudinally (all p < 0.01).Ever MHT use was associated with greater decline in global cognition and all domain‐specific z‐scores except visuospatial longitudinally (all p < 0.01).The greatest cognitive decline was among women who initiated MHT more than 5 years after menopause. [ABSTRACT FROM AUTHOR]

Published

2024

11. Associations among plasma, MRI and amyloid PET biomarkers of dementia and the impact of health‐related comorbidities.

Author

Rudolph, Marc D., Sutphen, Courtney L., Register, Thomas C., Whitlow, Christopher T., Sai, Kiran K. Solingapuram, Hughes, Timothy M., Bateman, James R., Dage, Jeff L., Russ, Kristen A., Mielke, Michelle M., Craft, Suzanne, and Lockhart, Samuel N.

Abstract

Background: Knowledge regarding associations between plasma and neuroimaging biomarkers indexing neurodegeneration and neuropathology observed in dementia is limited. Further, it is uncertain how comorbid health complications (e.g., kidney function) may alter plasma levels and impact associations with neuroimaging biomarkers. Method: We examined associations between plasma and neuroimaging biomarkers in cognitively normal participants (NC; N = 300) and individuals with consensus diagnosis (Dx) of mild cognitive impairment (MCI; N = 192) or dementia (DEM; N = 64) enrolled in the Wake Forest ADRC (Table 1). We examined plasma biomarkers (Quanterix SIMOA HD‐X: Aβ42/40, GFAP, NfL, p‐tau181) and neuroimaging measures of amyloid deposition (global PiB PET SUVr; Aβ‐PET), total brain volume (BVOL), global white matter hyperintensity volume (WMH), diffusion‐weighted fractional anisotropy (FA) and NODDI freewater (FW; white matter). Linear models adjusted for APOE‐ε4 carrier status, demographics (age, sex, race, education), and cardiometabolic factors (estimated glomerular filtration rate (eGFR); BMI). Results: Plasma biomarkers were moderately correlated with each other (absolute r =.22‐.64; all p<.001) and significantly elevated (Aβ42/40 lower) in DEM and MCI (Figure 1) versus NC, and Aβ‐PET‐positive (SUVr >1.21) versus negative individuals (all p<.001). Plasma and neuroimaging markers were significantly associated in both unadjusted models and models including eGFR and BMI (all p<.05; attenuation effect <10% with and without Dx; Figure 2a & 2b). In fully adjusted models (Figure 2b: Dx and all covariates), age, sex, and race differentially impacted associations of Aβ42/40, p‐tau181, and NfL with neuroimaging biomarkers (coefficients p <.05). APOE‐ε4 status exclusively impacted associations with Aβ‐PET SUVr/status. GFAP remained significantly associated with all neuroimaging biomarkers after covariate adjustment; no Aβ42/40 associations survived adjustment. P‐tau181 remained significantly associated with Aβ‐PET and BVOL, while associations with NfL were reduced in models stratified by Dx. Conclusion: Among aging community‐dwelling participants, plasma biomarkers significantly differed between diagnostic groups (DEM>MCI>NC), were elevated in Aβ‐PET positive individuals, and associated with poorer brain health. Except for GFAP, and to an extent p‐tau181, associations between plasma and neuroimaging biomarkers were differentially impacted by inclusion of comorbidities and covariates when stratified by diagnosis. Future work will examine high‐dimensional interactions among comorbidities, demographic information, and plasma and neuroimaging biomarkers in individuals with or at‐risk of dementia. [ABSTRACT FROM AUTHOR]

Published

2023

12. Using neuroimaging biomarkers to define plasma thresholds in a community dwelling cohort.

Author

Rudolph, Marc D., Sutphen, Courtney L., Register, Thomas C., Whitlow, Christopher T., Sai, Kiran K. Solingapuram, Hughes, Timothy M., Bateman, James R., Dage, Jeff L., Russ, Kristen A., Mielke, Michelle M., Craft, Suzanne, and Lockhart, Samuel N.

Abstract

Background: AD Imaging biomarkers (IBM) include measures of amyloid (A) on PET, and neurodegeneration (N) on MRI, with thresholds for classification of imaging A/N positivity commonly used at research centers. Novel AD plasma biomarkers (PBM) can potentially enhance neuropathological characterization; however, knowledge regarding which thresholds to use to characterize PBM abnormalities is limited. Method: We evaluated a range of PBM thresholds based on (1) plasma data alone (gaussian mixture models [GMM]), and (2) when classifying A/N IBM using both existing and data‐driven cutoffs (ROC analyses). Baseline plasma and imaging data were obtained in a community‐dwelling cohort enrolled in the Wake Forest ADRC, including cognitively normal participants (N = 300) and individuals with consensus diagnosis of mild cognitive impairment (N = 192) or dementia (N = 64; Table 1). We examined PBMs (Quanterix SIMOA HD‐X from NCRAD: Aβ42/40, GFAP, NfL, p‐tau181) and IBM measures of A (global PiB PET; A+>1.21 SUVR) and N (FreeSurfer temporal cortical thickness; MAYOTHCK), N+≤2.68mm; FreeSurfer hippocampal volume, N+≤0.454% head size; HPC‐VOL). Results: Optimal/low/high GMM‐derived thresholds based on PBM distributions (Figure 1a) are provided in Figure 1b. ROC analysis using existing IBM cutoffs are in Figure 1c, with details (sensitivity/specificity/AUC) in Figure 1d. GMM‐ and ROC‐derived p‐tau181 thresholds were highly aligned (range 3.698‐4.071 pg/ml). For NfL and GFAP, imaging ROC‐derived thresholds were lower than GMM‐derived thresholds. AUCs were highest when PBM classification was used to predict A‐PET using existing PET‐positivity cutoffs, with PBM performing more poorly for MRI‐based cutoffs. A/N IBM histograms and current/optimal/low/high GMM‐derived thresholds for each IBM are in Figure 2a. Figure 2b represents how different data‐driven IBM cutoffs impact PBM thresholds in ROC analyses, with AUC statistics for these ROC analyses in Figures 2c‐e. Notably, GMM‐optimal IBM cutoffs performed similarly to current cutoffs for defining PBM thresholds, especially when using A‐PET (AUCs for current and GMM‐optimal >0.747). Conclusion: While use of existing and data‐driven IBM cutoffs to define PBM thresholds in a community‐dwelling cohort is feasible, some plasma assays (e.g., p‐tau181) are more consistent than others, and caution is warranted against selecting a single threshold. To facilitate clinical use, future work will focus on establishing confidence intervals for PBM abnormalities. [ABSTRACT FROM AUTHOR]

Published

2023

13. Biomarkers of cellular senescence and risk of death in humans.

Author

St. Sauver, Jennifer L., Weston, Susan A., Atkinson, Elizabeth J., Mc Gree, Michaela E., Mielke, Michelle M., White, Thomas A., Heeren, Amanda A., Olson, Janet E., Rocca, Walter A., Palmer, Allyson K., Cummings, Steven R., Fielding, Roger A., Bielinski, Suzette J., and LeBrasseur, Nathan K.

Subjects

CELLULAR aging, RECEPTOR for advanced glycation end products (RAGE), OLDER people, EXTRACELLULAR matrix proteins, BIOMARKERS, GROWTH factors

Abstract

A robust and heterogenous secretory phenotype is a core feature of most senescent cells. In addition to mediators of age‐related pathology, components of the senescence associated secretory phenotype (SASP) have been studied as biomarkers of senescent cell burden and, in turn, biological age. Therefore, we hypothesized that circulating concentrations of candidate senescence biomarkers, including chemokines, cytokines, matrix remodeling proteins, and growth factors, could predict mortality in older adults. We assessed associations between plasma levels of 28 SASP proteins and risk of mortality over a median follow‐up of 6.3 years in 1923 patients 65 years of age or older with zero or one chronic condition at baseline. Overall, the five senescence biomarkers most strongly associated with an increased risk of death were GDF15, RAGE, VEGFA, PARC, and MMP2, after adjusting for age, sex, race, and the presence of one chronic condition. The combination of biomarkers and clinical and demographic covariates exhibited a significantly higher c‐statistic for risk of death (0.79, 95% confidence interval (CI): 0.76–0.82) than the covariates alone (0.70, CI: 0.67–0.74) (p < 0.001). Collectively, these findings lend further support to biomarkers of cellular senescence as informative predictors of clinically important health outcomes in older adults, including death. [ABSTRACT FROM AUTHOR]

Published

2023

14. Continuous associations between remote self‐administered cognitive measures and amyloid and tau PET biomarkers of Alzheimer's disease.

Author

Boots, Elizabeth A., Frank, Ryan D., Fan, Winnie Z., Christianson, Teresa J., Karstens, Aimee J., Kremers, Walter K., Stricker, John L., Machulda, Mary M., Fields, Julie A., Hassenstab, Jason J., Graff‐Radford, Jonathan, Vemuri, Prashanthi, Jack, Clifford R., Knopman, David S., Mielke, Michelle M., Petersen, Ronald C., and Stricker, Nikki H.

Abstract

Background: Easily accessible and self‐administered cognitive assessments that can aide early identification of individuals at risk for Alzheimer's disease (AD) dementia are critical for timely intervention. Mayo Test Drive (MTD) is a remote, self‐administered, multi‐device compatible, web‐based cognitive assessment (Stricker et al., 2022). We investigated continuous associations between MTD and amyloid and tau PET biomarkers and compared the strength of association to PET biomarkers and in‐person cognitive measures. Method: 556 adults from the Mayo Clinic Study of Aging participated (mean age = 70.6; mean education = 16.0 years; 50.7% female; 97.5% white). Participants were predominantly cognitively unimpaired (95.3%; 4.7% had a consensus diagnosis of mild cognitive impairment). Participants completed (1) brain amyloid and tau PET scans, (2) in‐person neuropsychological assessment including Mayo Preclinical Alzheimer's disease Cognitive Composite (Mayo‐PACC) and Global‐z, and (3) remote MTD comprised of the Stricker Learning Span (SLS) and the Symbols test, which are combined into an MTD composite. Multiple regressions adjusted for age, sex, and education queried associations between imaging biomarkers [amyloid meta‐region of interest (ROI), tau meta‐ROI, and tau entorhinal cortex (EC)‐ROI)] and composite and subtest scores from remote and in‐person measures. Davidson‐Mackinnon J‐test compared R‐squared values of models with remote versus in‐person composites. Result: Lower performances on MTD composite and Mayo‐PACC were associated with higher amyloid meta‐ROI (p's<.05; Table 1). MTD composite was also negatively associated with tau meta‐ROI and EC‐ROI (p's<.05). For memory measures, SLS sum of trials was negatively associated with tau meta‐ROI (p =.01) and EC‐ROI (p<.001) with no associations between AVLT sum of trials and PET (p's≥.06; Table 2). Among processing speed/executive function measures, worse Trails B performance was associated with higher amyloid meta‐ROI (p<.001). Symbols and Digit Symbol Coding were not associated with PET (p's≥.29). A multivariable model with MTD explained significantly less variance (p =.04) for amyloid meta‐ROI (adjusted R‐squared = 0.165) than a multivariable model with Mayo‐PACC (adjusted R‐squared = 0.176); remote and in‐person composite measures were comparable for other associations (p's>.05). Conclusion: MTD is associated with continuous measures of amyloid and tau PET biomarkers of AD, demonstrating criterion validity for MTD. Several associations were comparable to relationships between gold‐standard in‐person neuropsychological tests and imaging biomarkers. [ABSTRACT FROM AUTHOR]

Published

2023

15. Comparing associations of Alzheimer's disease plasma biomarkers with remote self‐administered cognitive measures versus in‐person neuropsychological tests.

Author

Boots, Elizabeth A., Frank, Ryan D., Fan, Winnie Z., Christianson, Teresa J., Karstens, Aimee J., Kremers, Walter K., Stricker, John L., Machulda, Mary M., Fields, Julie A., Hassenstab, Jason J., Graff‐Radford, Jonathan, Vemuri, Prashanthi, Jack, Clifford R., Knopman, David S., Mielke, Michelle M., Petersen, Ronald C., and Stricker, Nikki H.

Abstract

Background: Brief self‐administered cognitive assessments deployed remotely and combined with plasma biomarkers of Alzheimer's disease (AD) are well suited to assess clinical symptoms and underlying biology in large‐scale decentralized studies. We investigated whether associations of self‐administered cognitive measures and plasma biomarkers were comparable to associations of in‐person cognitive measures and plasma biomarkers. Method: Participants included 327 adults from the Mayo Clinic Study of Aging (mean age = 70.8; 48% female; mean education = 16.0 years; 96.9% white). Most (94.5%) were cognitively unimpaired; 5.5% had consensus diagnosis of mild cognitive impairment. Participants completed Mayo Test Drive (MTD; Stricker et al., 2022), a remote, self‐administered, multi‐device compatible web‐based cognitive assessment comprised of the Stricker Learning Span (SLS) and Symbols test that are combined into a MTD composite. Participants also completed in‐person neuropsychological assessment (global‐z; Mayo Preclinical Alzheimer's disease Cognitive Composite [Mayo‐PACC]) and fasting venipuncture. Plasma was assayed via HD‐X simoa platform for amyloid‐beta (Aβ)‐42 and Aβ‐40 to create an Aβ42/40 ratio, glial fibrillary acidic protein (GFAP), and neurofilament light chain (NfL) using the N4PE Quanterix kit as well as phosphorylated‐tau protein 181 (p‐tau181). P‐tau181, GFAP, and NfL were log10‐transformed. Multiple regression analyses adjusting for age, sex, and education examined associations between plasma biomarkers and composite and subtest scores from remote and in‐person measures. Davidson‐Mackinnon J‐test compared R‐squared values of models with remote versus in‐person composites. Result: Lower performances on MTD, global‐z, and Mayo‐PACC (Table 1) were associated with higher GFAP (p's≤.02), NfL (p's≤.003), and p‐tau181 (p's =.04). For memory, worse SLS and AVLT sum of trials were associated with higher GFAP (p's≤.01) and NfL (p's≤.03). For processing speed/executive function, worse Symbols and Trails B were associated with higher p‐tau181 (p's≤.02). Worse Trails B and Digit Symbol Coding were associated with higher NfL (p's≤.02), and worse Digit Symbol Coding was associated with lower Aβ42/40 (p = 0.03; Table 2). A multivariable model with MTD explained significantly more variance (p =.04) for NfL (adjusted R‐squared = 0.461) than a multivariable model with Mayo‐PACC (adjusted R‐squared = 0.447); remote and in‐person composite measures were comparable for other associations (p's>.05). Conclusion: Remote and in‐person composite measures showed comparable associations with AD‐related plasma biomarkers, supporting MTD's criterion validity. [ABSTRACT FROM AUTHOR]

Published

2023

16. Plasma ceramides relate to mild cognitive impairment in middle‐aged men: The Maastricht Study.

Author

van Kruining, Daan, Losen, Mario, Crivelli, Simone M., de Jong, Joost J. A., Jansen, Jacobus F. A., Backes, Walter H., Monereo‐Sánchez, Jennifer, van Boxtel, Martin P. J., Köhler, Sebastian, Linden, David E. J., Schram, Miranda T., Mielke, Michelle M., and Martinez‐Martinez, Pilar

Subjects

MILD cognitive impairment, MIDDLE-aged men, CERAMIDES, DISEASE risk factors, MAGNETIC resonance imaging

Abstract

Introduction: There is an urgent need for biomarkers identifying individuals at risk of early‐stage cognitive impairment. Using cross‐sectional data from The Maastricht Study, this study included 197 individuals with mild cognitive impairment (MCI) and 200 cognitively unimpaired individuals aged 40 to 75, matched by age, sex, and educational level. Methods: We assessed the association of plasma sphingolipid and ceramide transfer protein (CERT) levels with MCI and adjusted for potentially confounding risk factors. Furthermore, the relationship of plasma sphingolipids and CERTs with magnetic resonance imaging brain volumes was assessed and age‐ and sex‐stratified analyses were performed. Results: Associations of plasma ceramide species C18:0 and C24:1 and combined plasma ceramide chain lengths (ceramide risk score) with MCI were moderated by sex, but not by age, and higher levels were associated with MCI in men. No associations were found among women. In addition, higher levels of ceramide C20:0, C22:0, and C24:1, but not the ceramide risk score, were associated with larger volume of the hippocampus after controlling for covariates, independent of MCI. Although higher plasma ceramide C18:0 was related to higher plasma CERT levels, no association of CERT levels was found with MCI or brain volumes. Discussion: Our results warrant further analysis of plasma ceramides as potential markers for MCI in middle‐aged men. In contrast to previous studies, no associations of plasma sphingolipids with MCI or brain volumes were found in women, independent of age. These results highlight the importance of accounting for sex‐ and age‐related factors when examining sphingolipid and CERT metabolism related to cognitive function. [ABSTRACT FROM AUTHOR]

Published

2023

17. Mayo‐PACC: A parsimonious preclinical Alzheimer's disease cognitive composite comprised of public‐domain measures to facilitate clinical translation.

Author

Stricker, Nikki H., Twohy, Erin L., Albertson, Sabrina M., Karstens, Aimee J., Kremers, Walter K., Machulda, Mary M., Fields, Julie A., Jack, Clifford R., Knopman, David S., Mielke, Michelle M., and Petersen, Ronald C.

Abstract

Introduction: We aimed to define a Mayo Preclinical Alzheimer's disease Cognitive Composite (Mayo‐PACC) that prioritizes parsimony and use of public domain measures to facilitate clinical translation. Methods: Cognitively unimpaired participants aged 65 to 85 at baseline with amyloid PET imaging were included, yielding 428 amyloid negative (A‐) and 186 amyloid positive (A+) individuals with 7 years mean follow‐up. Sensitivity to amyloid‐related cognitive decline was examined using slope estimates derived from linear mixed models (difference in annualized change across A+ and A‐ groups). We compared differences in rates of change between Mayo‐PACC and other composites (A+ > A‐ indicating more significant decline in A+). Results: All composites showed sensitivity to amyloid‐related longitudinal cognitive decline (A+ > A‐ annualized change p < 0.05). Comparisons revealed that Mayo‐PACC (AVLT sum of trials 1‐5+6+delay, Trails B, animal fluency) showed comparable longitudinal sensitivity to other composites. Discussion: Mayo‐PACC performs similarly to other composites and can be directly translated to the clinic. [ABSTRACT FROM AUTHOR]

Published

2023

18. Dual cognitive and mobility impairments and future dementia ‐ Setting a research agenda.

Author

Tian, Qu, Montero‐Odasso, Manuel, Buchman, Aron S., Mielke, Michelle M., Espinoza, Sara, DeCarli, Charles S., Newman, Anne B., Kritchevsky, Stephen B., Rebok, George W., Resnick, Susan M., Thambisetty, Madhav, Verghese, Joe, and Ferrucci, Luigi

Abstract

Dual cognitive and mobility impairments are associated with an increased risk of dementia. Recent studies examining temporal trajectories of mobility and cognitive function in aging found that dual decline is associated with higher dementia risk than memory decline or gait decline only. Although initial data show that individuals with dual decline or impairment have excessive cardiovascular and metabolic risk factors, the causes of dual decline or what underlies dual decline with a high risk of dementia remain largely unknown. In December 2021, the National Institute on Aging Intramural and Extramural Programs jointly organized a workshop on Biology Underlying Moving and Thinking to explore the hypothesis that older persons with dual decline may develop dementia through a specific pathophysiological pathway. The working group discussed assessment methods for dual decline and possible mechanisms connecting dual decline with dementia risk and pinpointed the most critical questions to be addressed from a translational perspective. [ABSTRACT FROM AUTHOR]

Published

2023

19. Phosphorylated tau sites that are elevated in Alzheimer's disease fluid biomarkers are visualized in early neurofibrillary tangle maturity levels in the post mortem brain.

Author

Moloney, Christina M., Labuzan, Sydney A., Crook, Julia E., Siddiqui, Habeeba, Castanedes‐Casey, Monica, Lachner, Christian, Petersen, Ronald C., Duara, Ranjan, Graff‐Radford, Neill R., Dickson, Dennis W., Mielke, Michelle M., and Murray, Melissa E.

Abstract

Introduction: Alzheimer's disease (AD) biomarkers are increasingly more reliable in predicting neuropathology. To facilitate interpretation of phosphorylated tau sites as an early fluid biomarker, we sought to characterize which neurofibrillary tangle maturity levels (pretangle, intermediary 1, mature tangle, intermediary 2, and ghost tangle) are recognized. Methods: We queried the Florida Autopsied Multi‐Ethnic (FLAME) cohort for cases ranging from Braak stages I through VI, excluding non‐AD neuropathologies and tauopathies. Thioflavin‐S staining was compared to immunohistochemical measures of phosphorylated threonine (pT) 181, pT205, pT217, and pT231 in two hippocampal subsectors across n = 24 cases. Results: Each phosphorylated tau site immunohistochemically labeled early neurofibrillary tangle maturity levels compared to advanced levels recognized by thioflavin‐S. Hippocampal burden generally increased with each Braak stage. Discussion: These results provide neurobiologic evidence that these phosphorylated tau fluid biomarker sites are present during early neurofibrillary tangle maturity levels and may explain why these fluid biomarker measures are observed before symptom onset. Highlights: Immunohistochemical evaluation of four phosphorylated tau fluid biomarker sites.Earlier neurofibrillary tangle maturity levels recognized by phosphorylated tau in proline‐rich region.Advanced tangle pathology is elevated in the subiculum compared to the cornu ammonis 1 of the hippocampus.Novel semi‐quantitative frequency to calculate tangle maturity frequency. [ABSTRACT FROM AUTHOR]

Published

2023

20. Association of neighborhood socioeconomic disadvantage and cognitive impairment.

Author

Vassilaki, Maria, Aakre, Jeremiah A., Castillo, Anna, Chamberlain, Alanna M., Wilson, Patrick M., Kremers, Walter K., Mielke, Michelle M., Geda, Yonas E., Machulda, Mary M., Alhurani, Rabe E., Graff‐Radford, Jonathan, Vemuri, Prashanthi, Lowe, Val J., Jack, Clifford R., Knopman, David S., and Petersen, Ronald C.

Abstract

Introduction: We investigated the association of the area deprivation index (ADI) with cognitive decline, mild cognitive impairment (MCI), and dementia in older adults (≥50 years old). ADI is a neighborhood socioeconomic disadvantage measure assessed at the census block group level. Methods: The study included 4699 participants, initially without dementia, with available ADI values for 2015 and at least one study visit in 2008 through 2018. Using logistic regression and Cox proportional hazards models with age as the time scale, we assessed the odds for MCI and the risk for dementia, respectively. Results: In cognitively unimpaired (CU) adults at baseline, the risk for progression to dementia increased for every decile increase in the ADI state ranking (hazard ratio = 1.06, 95% confidence interval (1.01–1.11), P =.01). Higher ADI values were associated with subtly faster cognitive decline. Discussion: In older CU adults, higher baseline neighborhood socioeconomic deprivation levels were associated with progression to dementia and slightly faster cognitive decline. Highlights: The study used area deprivation index, a composite freely available neighborhood deprivation measure.Higher levels of neighborhood deprivation were associated with greater mild cognitive impairment odds.Higher neighborhood deprivation levels were associated with higher dementia risk. [ABSTRACT FROM AUTHOR]

Published

2023

21. Association of raloxifene and tamoxifen therapy with cognitive performance, odds of mild cognitive impairment, and brain MRI markers of neurodegeneration.

Author

Kara, Firat, Lohse, Christine M., Castillo, Anna M., Tosakulwong, Nirubol, Lesnick, Timothy G., Jack, Clifford R., Petersen, Ronald C., Olson, Janet E., Couch, Fergus J., Ruddy, Kathryn J., Kantarci, Kejal, and Mielke, Michelle M.

Subjects

RALOXIFENE, COGNITIVE ability, COGNITIVE therapy, MILD cognitive impairment, TAMOXIFEN, MAGNETIC resonance imaging

Abstract

The aim of this cross‐sectional study was to examine whether a history of selective estrogen receptor modifiers (SERMs), tamoxifen and raloxifene, use was associated with cognitive performance, odds of mild cognitive impairment (MCI), or magnetic resonance imaging (MRI) markers of neurodegeneration associated with Alzheimer's disease. We included women with prior history of breast cancer or no prior history of any cancer at enrollment in the Mayo Clinic Study of Aging (MCSA). This information was abstracted using the Rochester Epidemiology Project medical‐linkage system. Logistic regression was used to examine associations of SERMs with odds of MCI. Linear regression models were used to examine associations of SERMs with cognitive z‐scores (Memory, Executive Function, Language, Visuospatial Skills, Global Cognition), and MRI markers. Among 2840 women aged 50 and older in the MCSA, 151 had a history of breast cancer, and 42 (28%) of these had a history of tamoxifen treatment. A total of 2235 women had no prior history of any cancer, and 76 (3%) of these had a history of raloxifene use. No significant associations between tamoxifen use and cognition, or odds of MCI were observed among women with a history of breast cancer after adjusting for confounders. Similarly, raloxifene use was not significantly associated with cognition, or odds of MCI in women without a history of cancer after adjusting for confounders. We did not find significant associations between the use of either SERM and MRI markers. Use of tamoxifen or raloxifene was not significantly associated with cognition in postmenopausal women. [ABSTRACT FROM AUTHOR]

Published

2023

22. Plasma amyloid beta 40/42, phosphorylated tau 181, and neurofilament light are associated with cognitive impairment and neuropathological changes among World Trade Center responders: A prospective cohort study of exposures and cognitive aging at midlife.

Author

Kritikos, Minos, Diminich, Erica D., Meliker, Jaymie, Mielke, Michelle, Bennett, David A., Finch, Caleb E., Gandy, Sam E., Carr, Melissa A., Yang, Xiaohua, Kotov, Roman, Kuan, Pei‐Fen, Bromet, Evelyn J., Clouston, Sean A. P., and Luft, Benjamin J.

Subjects

COGNITIVE aging, POST-traumatic stress disorder, COGNITION disorders, MILD cognitive impairment, TAU proteins, MIDDLE age, AMYLOID

Abstract

Introduction: World Trade Center (WTC) responders are experiencing a high risk of mild cognitive impairment (MCI) and dementia, though the etiology remains inadequately characterized. This study investigated whether WTC exposures and chronic post‐traumatic stress disorder (PTSD) were correlated with plasma biomarkers characteristic of Alzheimer's disease (AD) neuropathology. Methods: Eligible participants included WTC‐exposed individuals with a baseline cognitive assessment and available plasma sample. We examined levels of the amyloid beta (Aβ)40/42 ratio, phosphorylated tau 181 (p‐tau181), and neurofilament light chain (NfL) and associations with a WTC exposures (duration on site ≥15 weeks, dust cloud), the PTSD Symptom Checklist for Diagnostic and Statistical Manual of Mental Disorders, 4th edition PTSD, and classification of amyloid/tau/neurodegeneration (AT[N]) profiles. Multinomial logistic regressions assessed whether biomarkers predicted increased risk of MCI or dementia. Results: Of 1179 eligible responders, 93.0% were male, mean (standard deviation) age 56.6 years (7.8). Aβ40/42, p‐tau181, and NfL intercorrelated and increased with age. In subgroup analyses of responders with available neuroimaging data (n = 75), Aβ40/42 and p‐tau181 were further associated with decreased hippocampal volume (Spearman's ρ = −0.3). Overall, 58.08% of responders with dementia had ≥1 elevated biomarker, and 3.45% had elevations across all biomarkers. In total, 248 (21.05%) had MCI and 70 (5.94%) had dementia. Increased risk of dementia was associated with plasma AT(N) profile T+ or A+N+. Exposure on site ≥15 weeks was independently associated with T+ (adjusted risk ratio [aRR] = 1.03 [1.01−1.05], P = 0.009), and T+N+ profile (aRR = 2.34 [1.12−4.87]). The presence of PTSD was independently associated with risk of A+ (aRR = 1.77 [1.11−2.82]). Discussion: WTC exposures and chronic PTSD are associated with plasma biomarkers consistent with neurodegenerative disease. [ABSTRACT FROM AUTHOR]

Published

2023

23. Convergent and criterion validity of a computer adaptive self‐administered word list memory test and the Mayo Test Drive composite: correlations with traditional measures and group difference by PET imaging biomarker status in persons without...

Author

Stricker, Nikki H., Twohy, Erin L, Albertson, Sabrina M., Christianson, Teresa J., Stricker, John L, Machulda, Mary M., Karstens, Aimee J, Kremers, Walter K., Hassenstab, Jason J., Jack, Clifford R., Knopman, David S., Mielke, Michelle M., and Petersen, Ronald C.

Abstract

Background: Mayo Test Drive (MTD): Test Development through Rapid Iteration, Validation and Expansion, is a web‐based platform optimized for remote self‐administered assessment that includes a computer adaptive word list memory test (Stricker Learning Span; SLS) and a measure of processing speed (Symbols Test). Study aims were to determine 1) convergent validity of MTD through correlations with in‐person neuropsychological measures and 2) criterion validity of MTD by qualitatively comparing the ability of Mayo Test Drive and in‐person administered neuropsychological measures to differentiate biomarker‐defined groups, independent of clinical diagnosis. Methods: Mayo Clinic Study of Aging participants (N = 282) completed a brief remote cognitive assessment (mean age = 74, SD = 12; 262 CU and 20 MCI per consensus conference diagnosis; see Table 1). A subset of participants had brain amyloid and/or brain tau PET scans available within 3 years; overlapping groups were formed for 1) those on the Alzheimer's disease (AD) continuum (A+, n = 31) or not (A‐, n = 57) and for 2) those with biological AD (A+T+, n = 19) or without any AD biomarkers (A‐T‐, n = 47). Primary outcome variables were SLS sum of trials, AVLT sum of trials, SYM Correct Trials response time, Digit Symbol Coding, MTD composite and Mayo‐PACC (AVLT sum of trials, Trails B, animals). Bivariate correlations were performed across all participants. Linear model ANOVAs were used to investigate biomarker subgroup differences; Hedge's g effect sizes are reported. Results: Convergent validity was supported through significant correlation (p's <.001) of SLS and AVLT (r =.63), SYM and Coding (r = ‐.64), and MTD composite with Mayo‐PACC (r =.67); see Table 2. MTD subtests showed expected relationships with age and education (p's <.05; Table 3). All MTD performances were significantly lower for A+ and A+T+ participants relative to A‐ or A‐T‐ (p's<.001; Table 4). All MTD outcome measures showed a similar or greater group difference effect size relative to traditional in‐person administered neuropsychological measures for separating A+ vs. A‐ and A+T+ vs. A‐T‐ groups. See Figure 1 and Table 4. Conclusions: MTD subtests show evidence of convergent validity through strong correlations with traditional in‐person cognitive measures. Preliminary analyses suggest MTD has promise for differentiating PET biomarker groups. [ABSTRACT FROM AUTHOR]

Published

2022

24. Diagnostic accuracy of the Stricker Learning Span and Mayo Test Drive Composite for amnestic Mild Cognitive Impairment.

Author

Stricker, Nikki H., Twohy, Erin L, Albertson, Sabrina M., Christianson, Teresa J., Stricker, John L, Machulda, Mary M., Karstens, Aimee J, Patel, Jay S, Kremers, Walter K., Hassenstab, Jason J., Jack, Clifford R., Knopman, David S., Mielke, Michelle M., and Petersen, Ronald C.

Abstract

Background: Remote assessment tools offer significant promise for aiding early detection of cognitive impairment. Mayo Test Drive (MTD): Test Development through Rapid Iteration, Validation and Expansion, is a web‐based platform for remote self‐administered assessment that includes a computer adaptive word list memory test (Stricker Learning Span; SLS) and a measure of processing speed (Symbols Test). We examined the diagnostic accuracy of the SLS and a MTD composite (SLS max span, SLS trials 1–5 total correct, SLS delay correct, [Symbols correct item response time*‐1]) for amnestic mild cognitive impairment (aMCI). We also explored diagnostic accuracy for a broader group that included individuals with possible MCI (pMCI; see Figure 1). Methods: Participants were recruited from the Mayo Clinic Study of Aging for this ancillary remote study. 226 were cognitively unimpaired (CU; concordant CU diagnosis by 3 independent raters). Fifty‐six participants had possible MCI (at least 1 of 3 raters indicated MCI) and 16 had a consensus diagnosis of aMCI. Primary outcome variables were SLS sum of trials, AVLT sum of trials, Symbols correct items response time, and MTD composite. Mean difference analyses used linear model ANOVAs (alpha =.05). Receiver operating characteristic (ROC) curves were applied; we derived optimal cutoff scores based on the Youden index method. Results: Both aMCI and possible MCI groups showed significantly lower performance than the CU group on SLS (Hedge's g aMCI = ‐1.72, pMCI = ‐1.04), Symbols (Hedge's g aMCI = 1.38, pMCI = 0.64), and MTD composite (Hedge's g aMCI = ‐1.89, pMCI = ‐1.09); see Tables 1 and 2 (all p's<.01 even when additionally covarying age, education, sex). Total area under the curve was high for differentiating of CU vs. aMCI (MTD Composite = 0.91, SLS = 0.91) and acceptable for CU vs. pMCI (MTD Composite = 0.77, SLS = 0.77); see Table 2. Consistent with our flexible platform, a variety of device types were used to complete remote testing (32% smartphone, 12% tablet, 56% PC). Conclusions: MTD and the SLS show high diagnostic accuracy for aMCI. MTD is a flexible, brief, and easy‐to‐use remote cognitive assessment tool with great potential for scalable use in future studies seeking to maximize inclusion of individuals with aMCI in clinical trials or for cognitive screening in clinical settings. [ABSTRACT FROM AUTHOR]

Published

2022

25. An examination of the usability of the Mayo Test Drive remote cognitive testing platform in older adults with and without cognitive impairment.

Author

Patel, Jay S, Christianson, Teresa J., Karstens, Aimee J, Stricker, John L, Kremers, Walter K., Jack, Clifford R., Knopman, David S., Mielke, Michelle M., Petersen, Ronald C., and Stricker, Nikki H.

Abstract

Background: Mayo Test Drive (MTD): Test Development through Rapid Iteration, Validation and Expansion, is a web‐based platform for self‐administered assessment for novel (Stricker Learning Span) and open access (Symbols Test) cognitive measures with previously demonstrated validity and reliability. Our study aim was to examine the usability of MTD, defined as the extent to which MTD was used to achieve the desired study goal of completing a testing session among participants willing to engage in an all‐remote study. Methods: 248 Mayo Clinic Study of Aging and Mayo Alzheimer's Disease Research Center participants were invited to participate in this ancillary, uncompensated remote pilot study via email. To examine 1) willingness to participate in a remote cognitive assessment study and 2) usability of MTD, the initiation and completion rates of MTD were examined by cognitively unimpaired (CU; n = 142) and cognitively impaired (CI; n = 106) groups (see Figure 1). These rates and other factors associated with MTD feasibility were further explored across age in CU (i.e., 50–69, 70–79, and 80+ years) and specific diagnostic groups in CI (i.e., individuals with dementia, mild cognitive impairment (MCI), and possible MCI). Results: Session completion rate (usability) was 98% across all participants who chose to participate, and, surprisingly, completion rates did not vary by age or diagnostic groups (p =.69; see Table 1). As expected, more individuals chose to participate in the CU (77%) versus CI (52%) group (p <.001). In terms of feasibility, individuals over 80 and with CI were more likely to have some contact with the study coordinator. Use of smartphones decreased with age, with most CU individuals over 70 using a personal computer (69‐73%; Table 2). Conclusions: Though the CI group was less likely to choose to participate than the CU group, out of those that did choose to participate the rate of completion was 98%. This demonstrates high usability of MTD. Study coordinator support and a flexible testing platform is critical for facilitating participation in remote testing across the aging population, and more supports and incentives may be needed for individuals with cognitive impairment to improve participation rates. [ABSTRACT FROM AUTHOR]

Published

2022

26. The Alzheimer's Association appropriate use recommendations for blood biomarkers in Alzheimer's disease.

Author

Hansson, Oskar, Edelmayer, Rebecca M., Boxer, Adam L., Carrillo, Maria C., Mielke, Michelle M., Rabinovici, Gil D., Salloway, Stephen, Sperling, Reisa, Zetterberg, Henrik, and Teunissen, Charlotte E.

Abstract

Blood‐based markers (BBMs) have recently shown promise to revolutionize the diagnostic and prognostic work‐up of Alzheimer's disease (AD), as well as to improve the design of interventional trials. Here we discuss in detail further research needed to be performed before widespread use of BBMs. We already now recommend use of BBMs as (pre‐)screeners to identify individuals likely to have AD pathological changes for inclusion in trials evaluating disease‐modifying therapies, provided the AD status is confirmed with positron emission tomography (PET) or cerebrospinal fluid (CSF) testing. We also encourage studying longitudinal BBM changes in ongoing as well as future interventional trials. However, BBMs should not yet be used as primary endpoints in pivotal trials. Further, we recommend to cautiously start using BBMs in specialized memory clinics as part of the diagnostic work‐up of patients with cognitive symptoms and the results should be confirmed whenever possible with CSF or PET. Additional data are needed before use of BBMs as stand‐alone diagnostic AD markers, or before considering use in primary care. [ABSTRACT FROM AUTHOR]

Published

2022

27. Consideration of sex and gender in Alzheimer's disease and related disorders from a global perspective.

Author

Mielke, Michelle M., Aggarwal, Neelum T., Vila‐Castelar, Clara, Agarwal, Puja, Arenaza‐Urquijo, Eider M., Brett, Benjamin, Brugulat‐Serrat, Anna, DuBose, Lyndsey E., Eikelboom, Willem S., Flatt, Jason, Foldi, Nancy S., Franzen, Sanne, Gilsanz, Paola, Li, Wei, McManus, Alison J., van Lent, Debora Melo, Milani, Sadaf Arefi, Shaaban, C. Elizabeth, Stites, Shana D., and Sundermann, Erin

Abstract

Sex or gender differences in the risk of Alzheimer's disease and related dementias (ADRD) differ by world region, suggesting that there are potentially modifiable risk factors for intervention. However, few epidemiological or clinical ADRD studies examine sex differences; even fewer evaluate gender in the context of ADRD risk. The goals of this perspective are to: (1) provide definitions of gender, biologic sex, and sexual orientation. and the limitations of examining these as binary variables; (2) provide an overview of what is known with regard to sex and gender differences in the risk, prevention, and diagnosis of ADRD; and (3) discuss these sex and gender differences from a global, worldwide perspective. Identifying drivers of sex and gender differences in ADRD throughout the world is a first step in developing interventions unique to each geographical and sociocultural area to reduce these inequities and to ultimately reduce global ADRD risk. Highlights: The burden of dementia is unevenly distributed geographically and by sex and gender.Scientific advances in genetics and biomarkers challenge beliefs that sex is binary.Discrimination against women and sex and gender minority (SGM) populations contributes to cognitive decline.Sociocultural factors lead to gender inequities in Alzheimer's disease and related dementias (ADRD) worldwide. [ABSTRACT FROM AUTHOR]

Published

2022

28. Prescription opioids and longitudinal changes in cognitive function in older adults: A population‐based observational study.

Author

Warner, Nafisseh S., Hanson, Andrew C., Schulte, Phillip J., Habermann, Elizabeth B., Warner, David O., and Mielke, Michelle M.

Subjects

COGNITION disorder risk factors, MEMORY, SCIENTIFIC observation, CONFIDENCE intervals, MULTIVARIATE analysis, LANGUAGE & languages, RISK assessment, DRUGS, ATTENTION, VISUAL perception, DESCRIPTIVE statistics, COGNITIVE testing, SECONDARY analysis, SPACE perception, PROPORTIONAL hazards models, OLD age

Abstract

Background: Opioids are frequently prescribed to alleviate pain in older adults, yet the relationships between prescription opioids and long‐term cognitive function are unclear. Methods: In this analysis of the Mayo Clinic Study of Aging, a longitudinal population‐based cohort study of older adults with formal neuropsychological testing and cognitive evaluations performed every 15 months, the associations between prescription opioids, global and domain‐specific cognitive function, and mild cognitive impairment were evaluated through time‐dependent linear mixed effects and Cox proportional hazards models. Results: Four thousand two hundred eighteen participants (51% male) were included with enrollment between 11/1/2004 and 4/1/2019 and median age of 76 (interquartile range 72, 82) years. Two thousand nine hundred seventy‐seven subjects (71%) received at least 1 opioid prescription during a median follow‐up of 7.5 (5.0, 10.7) years. Overall, there was an estimated 0.096 reduction in the global cognitive Z‐score per year, including decreases of 0.050 in memory, 0.080 in language, 0.044 in visual–spatial cognition, and 0.112 in attention. In multivariable analyses, each receipt of an opioid prescription resulted in an additional −0.007 (95% CI −0.009, −0.005) change in global cognitive Z‐score (p < 0.001), with significant effects seen in the domains of memory (−0.005, 95% CI −0.007, −0.003; p < 0.001), language (−0.002, 95% CI −0.003, 0.000; p = 0.024) and attention (−0.004, 95% CI −0.006, −0.002; p < 0.001) but not visual–spatial function (0.000, 95% CI −0.001, 0.001; p = 0.897). Opioid prescriptions were associated with incident mild cognitive impairment (MCI) in adjusted analysis (hazard ratio 1.21, 95% CI 1.04, 1.42; p = 0.014). Conclusion: Prescription opioids are associated with small but statistically significant declines in long‐term cognitive function in older adults, which may represent effects of opioids or other related factors. [ABSTRACT FROM AUTHOR]

Published

2022

29. Association of tamoxifen and raloxifene therapy with cognitive performance, odds of mild cognitive impairment, and neuroimaging markers of neurodegeneration.

Author

Kara, Firat, Lohse, Christine M., Castillo, Anna, Tosakulwong, Nirubol, Lesnick, Timothy G., Jack, Clifford R., Petersen, Ronald C., Olson, Janet E., Couch, Fergus J., Ruddy, Kathryn J., Kantarci, Kejal, and Mielke, Michelle M.

Abstract

Background: Tamoxifen is used as a selective estrogen receptor modifier (SERM) to treat hormone receptor‐positive breast cancer. Raloxifene, another SERM, has been used for the treatment of osteoporosis in post‐menopausal women. The aim of this cross‐sectional study was to examine whether a history of tamoxifen or raloxifene use was associated with cognitive performance, odds of mild cognitive impairment (MCI), or structural neurodegenerative MRI markers. Method: The study included women with and without a personal history of breast cancer enrolled in the Mayo Clinic Study of Aging (MCSA). A history of breast cancer and use of SERMs before the MCSA enrollment visit was abstracted using the Rochester Epidemiology Project medical‐linkage system. Participants had a diagnosis of MCI (prevalent) at the time of enrollment into the MCSA. Logistic regression was used to examine associations of SERMs with odds of MCI. Linear regression models were used to examine associations of SERMs with cognitive measures z‐scores (Memory, Executive Function, Language, Visuospatial Skills, Global Cognition), hippocampal volume, and Alzheimer's disease signature cortical thickness. Result: Among the women aged ≥ 50 at enrollment in the MCSA, 151 had a history of breast cancer, and 2235 had no prior history of any cancer. Of the 151 women with a history of breast cancer, 42 (28%) had taken tamoxifen and 109 (72%) had not at enrollment in the MCSA; 54 had neuroimaging data (tamoxifen = 16; no tamoxifen = 38). Among the women without prior history of cancer at enrollment in the MCSA, 76 (3%) had taken raloxifene and 2159 (97%) had not; 755 had neuroimaging data (raloxifene = 25; no raloxifene = 730). No significant associations between tamoxifen with global or domain‐specific cognition or odds of MCI were observed among women with a history of breast cancer after adjusting for confounders (Table 1). Likewise raloxifene was not significantly associated with global or domain‐specific cognition or odds of MCI in women without a history of cancer after adjusting for confounders (Table 2). We did not find significant associations between SERMs and any neuroimaging outcome (Table 3). Conclusion: Our results suggest use of tamoxifen or raloxifene is not significantly associated with cognition in postmenopausal women. [ABSTRACT FROM AUTHOR]

Published

2023

30. Mayo‐PACC: Optimizing a parsimonious Preclinical Alzheimer's disease cognitive composite comprised of public‐domain measures.

Author

Karstens, Aimee J., Twohy, Erin L, Albertson, Sabrina M., Kremers, Walter K., Machulda, Mary M., Jack, Clifford R., Knopman, David S., Mielke, Michelle M., Petersen, Ronald C., and Stricker, Nikki H.

Abstract

Background: Preclinical Alzheimer's cognitive composites (PACC) are designed to detect subtle cognitive changes in clinical trials. PACCs often include measures of memory, attention, and semantic fluency, with variations based on available measures. We created a Mayo Clinic PACC (Mayo‐PACC) to address limitations of existing PACCs by prioritizing parsimony, non‐proprietary measures, clinical applicability, and psychometric properties. We developed a Mayo‐PACC and examined sensitivity to detecting longitudinal cognitive change in amyloid positive (A+) older adults relative to the Preclinical Alzheimer's Cognitive Composite‐Revised (PACC‐R). Exploratory analyses included comparison to other composites. Method: Participants included 614 individuals in the Mayo Clinic Study of Aging (428 A‐ and 186 A+) age 65‐85 who were cognitively unimpaired at baseline with 7 years mean follow‐up. A+ was defined as PiB‐PET meta‐ROI SUVR ≥ 1.48 (centiloid 22). The Mayo‐PACC included the AVLT sum of trials (trials 1‐5, short delay, long delay), Trails B and Animal fluency. Measures included in the PACC‐R and other comparison composites are listed in Table 1. We calculated study‐specific z‐scores and examined psychometric properties of component measures including test‐retest reliability, practice effects, and distributional properties (ceiling/floor effects, skew, kurtosis). We examined sensitivity to preclinical cognitive change using slope estimates (difference in annualized change across A+ and A‐ groups) from linear mixed models (LMMs) for each composite. A jackknife procedure was used to calculate the standard error and subsequent confidence intervals of differences in rates of change (A+>A‐ indicating more significant decline in A+). Significance was determined based on whether the 95% Confidence Interval (CI) contained 0 (alpha =.05). Result: All composites showed sensitivity to amyloid‐related longitudinal cognitive decline (A+>A‐ annualized change p<.05; see Table 2). Jack‐knife comparisons revealed comparable utility of Mayo‐PACC and PACC‐R (CI contained 0, see Table 3). Exploratory analyses revealed Mayo‐PACC performed similarly to an adaptation of the ADCS‐PACC, Global‐z, Memory‐z and Attention‐z. The Mayo‐PACC performed better than a 2‐measure Mayo‐PACC‐remote and a single memory measure. Conclusion: The Mayo‐PACC provides a parsimonious composite score that has comparable utility for detecting A+>A‐ cognitive decline compared to the PACC‐R and other composites and can be widely used in both research and clinical settings. [ABSTRACT FROM AUTHOR]

Published

2023

31. Improving community health‐care systems' early detection of cognitive decline and dementia.

Author

Au, Rhoda, Ferrell, Phyllis Barkman, Beeri, Michal, Boden‐Albala, Bernadette, Frank, Lori, Jimenez‐Maggiora, Gustavo, Khachaturian, Ara, Kirkendall, Eric, Kivipelto, Miia, Larson, Eric, Mattke, Soren, Mielke, Michelle, Paschalidis, Ioannis, Readhead, Benjamin, Schnitzler, Peter, Schultze, Joachim, Tang, Yi, Teipel, Stefan, Williamson, Jeff, and Zabar, Yuval

Abstract

Preliminary estimates suggest that current global health‐care systems lack the resource capacity to provide persons with dementia timely access to diagnosis, treatment, and care. There is an increasing need to improve timely identification of individuals who will likely progress to Alzheimer's disease (AD) dementia particularly among under‐represented, underserved, and vulnerable populations. The rapidly evolving area of bioinformatics of health system data and the emergence of fluid‐based biomarkers for pre‐symptomatic AD may provide an innovative strategic option for health system planners. A think‐tank style meeting entitled "The Campaign to Prevent Alzheimer's Disease Work Group on Community‐Based Detection and Assessment of Cognitive Decline" developed recommendations to guide future sustainability activities, public policy campaigns, and implementation pilots. The group identified and explored different pathways of community‐based detection using electronic health records, from different international health‐care systems, to detect and surveil individuals with early possible cognitive impairment. [ABSTRACT FROM AUTHOR]

Published

2022

32. Alzheimer's disease cerebrospinal fluid biomarkers differentiate patients with Creutzfeldt–Jakob disease and autoimmune encephalitis.

Author

Chang, Bryce K., Day, Gregory S., Graff‐Radford, Jonathan, McKeon, Andrew, Flanagan, Eoin P., Algeciras‐Schimnich, Alicia, Mielke, Michelle M., Nguyen, Aivi, Jones, David T., Toledano, Michel, Kremers, Walter K., Knopman, David S., Petersen, Ronald C., and Li, Wentao

Subjects

ALZHEIMER'S disease, CREUTZFELDT-Jakob disease, CEREBROSPINAL fluid, CELL adhesion molecules, ENCEPHALITIS, AUTOANTIBODY analysis, BRAIN tumors

Abstract

Background and purpose: Autoimmune encephalitis (AE) is a potentially treatable cause of rapidly progressive dementia that may mimic Creutzfeldt–Jakob disease (CJD). Alzheimer disease (AD) cerebrospinal fluid (CSF) biomarkers may discriminate CJD from AD, but utility in discriminating CJD and AE is unclear. This study compared AD CSF biomarkers in CJD and AE. Methods: Patients with probable or definite CJD and probable or definite AE who underwent Roche Elecsys AD CSF biomarker testing at Mayo Clinic from March 2020 through April 2021 were included. Total‐tau, phosphorylated181 tau and amyloid‐β42 levels were compared. Results: Of 11 CJD cases, four were autopsy proven; the rest had positive real‐time quaking‐induced conversion testing. Disease‐associated autoantibodies were detected in 8/15 cases of AE: leucine‐rich glioma‐inactivated 1 and neuronal intermediate filaments (two cases each), and N‐methyl‐d‐aspartate receptor, contactin‐associated protein‐like 2, dipeptidyl‐peptidase‐like protein 6 and immunoglobulin‐like cell adhesion molecule IgLON family member 5. Total‐tau provided excellent discrimination between CJD and AE in a univariate model (odds ratio 1.46 per 100 pg/ml, 95% confidence interval 1.17–2.11, p < 0.05, c = 0.93). Total‐tau was elevated in 91% of CJD cases (median > 1300, range 236–>1300 pg/ml), of which 55% were above the limit of assay measurement (>1300 pg/ml). Total‐tau was elevated in 20% of AE cases (median 158, range 80–>1300 pg/ml). Conclusion: Total‐tau was greater in CJD than AE. Given that amyloid‐β42 and phosphorylated181 tau were comparable, the ratio differences were probably driven by elevated total‐tau in CJD. This study supports the role for AD biomarker testing in patients with rapidly progressive dementia. [ABSTRACT FROM AUTHOR]

Published

2022

33. Biomarkers of Alzheimer syndrome and related dementias: A&D author's guide.

Author

Lutz, Michael W., Khachaturian, Ara S., Zetterberg, Henrik, Blennow, Kaj, Willette, Auriel A., Mielke, Michelle M., Hayden, Kathleen M., Dodge, Hiroko H., Tang, Yi, Greenberg, Barry D., Kukull, Walter A, and Khachaturian, Zaven S

Published

2022

34. Slowing gait speed precedes cognitive decline by several years.

Author

Skillbäck, Tobias, Blennow, Kaj, Zetterberg, Henrik, Skoog, Johan, Rydén, Lina, Wetterberg, Hanna, Guo, Xinxin, Sacuiu, Simona, Mielke, Michelle M., Zettergren, Anna, Skoog, Ingmar, and Kern, Silke

Abstract

Introduction: In this longitudinal study, we aimed to examine if slowing gait speed preceded cognitive decline and correlated with brain amyloidosis. Methods: The sample (n = 287) was derived from the Gothenburg H70 Birth Cohort Studies, with follow‐ups between 2000 and 2015. Gait speed was measured by indoor walk, and cognition using the Clinical Dementia Rating (CDR) score. All participants had CDR = 0 at baseline. Some participants had data on cerebrospinal fluid (CSF) amyloid beta (Aβ)1‐42 concentrations at the 2009 examination. Results: Gait speed for participants who worsened in CDR score during follow‐up was slower at most examinations. Baseline gait speed could significantly predict CDR change from baseline to follow‐up. Subjects with pathological CSF Aβ1‐42 concentrations at the 2009 visit had lost more gait speed compared to previous examinations. Discussion: Our results indicate that gait speed decline precedes cognitive decline, is linked to Alzheimer's pathology, and might be used for early detection of increased risk for dementia development. [ABSTRACT FROM AUTHOR]

Published

2022

35. NIA-AA Alzheimer's Disease Framework: Clinical Characterization of Stages.

Author

Petersen, Ronald C., Wiste, Heather J., Weigand, Stephen D., Fields, Julie A., Geda, Yonas E., Graff‐Radford, Jonathan, Knopman, David S., Kremers, Walter K., Lowe, Val, Machulda, Mary M., Mielke, Michelle M., Stricker, Nikki H., Therneau, Terry M., Vemuri, Prashanthi, Jack, Clifford R., Graff-Radford, Jonathan, Machulda, Mary, Mielke, Michelle, Jack, Clifford R Jr, and Mielke, Michelle M PhD

Subjects

ALZHEIMER'S disease, COGNITION disorders, COGNITIVE aging, DEMENTIA, CEREBRAL amyloid angiopathy, DISEASE progression, RESEARCH, CROSS-sectional method, RESEARCH methodology, MEDICAL cooperation, EVALUATION research, COMPARATIVE studies, AGE factors in Alzheimer's disease, RESEARCH funding, LONGITUDINAL method

Abstract

Background: To operationalize the National Institute on Aging - Alzheimer's Association (NIA-AA) Research Framework for Alzheimer's Disease 6-stage continuum of clinical progression for persons with abnormal amyloid.Methods: The Mayo Clinic Study of Aging is a population-based longitudinal study of aging and cognitive impairment in Olmsted County, Minnesota. We evaluated persons without dementia having 3 consecutive clinical visits. Measures for cross-sectional categories included objective cognitive impairment (OBJ) and function (FXN). Measures for change included subjective cognitive impairment (SCD), objective cognitive change (ΔOBJ), and new onset of neurobehavioral symptoms (ΔNBS). We calculated frequencies of the stages using different cutoff points and assessed stability of the stages over 15 months.Results: Among 243 abnormal amyloid participants, the frequencies of the stages varied with age: 66 to 90% were classified as stage 1 at age 50 but at age 80, 24 to 36% were stage 1, 32 to 47% were stage 2, 18 to 27% were stage 3, 1 to 3% were stage 4 to 6, and 3 to 9% were indeterminate. Most stage 2 participants were classified as stage 2 because of abnormal ΔOBJ only (44-59%), whereas 11 to 21% had SCD only, and 9 to 13% had ΔNBS only. Short-term stability varied by stage and OBJ cutoff points but the most notable changes were seen in stage 2 with 38 to 63% remaining stable, 4 to 13% worsening, and 24 to 41% improving (moving to stage 1).Interpretation: The frequency of the stages varied by age and the precise membership fluctuated by the parameters used to define the stages. The staging framework may require revisions before it can be adopted for clinical trials. ANN NEUROL 2021;89:1145-1156. [ABSTRACT FROM AUTHOR]

Published

2021

36. Associations of amyloid and neurodegeneration plasma biomarkers with comorbidities.

Author

Syrjanen, Jeremy A., Campbell, Michelle R., Algeciras‐Schimnich, Alicia, Vemuri, Prashanthi, Graff‐Radford, Jonathan, Machulda, Mary M., Bu, Guojun, Knopman, David S., Jack, Clifford R., Petersen, Ronald C., and Mielke, Michelle M.

Abstract

Introduction: Blood‐based biomarkers of amyloid pathology and neurodegeneration are entering clinical use. It is critical to understand what factors affect the levels of these markers. Methods: Plasma markers (Aβ42, Aβ40, NfL, T‐tau, Aβ42/40 ratio) were measured on the Quanterix Simoa HD‐1 analyzer for 996 Mayo Clinic Study of Aging (MCSA) participants, aged 51 to 95 years. All other data were collected during in‐person MCSA visits or abstracted from the medical record. Results: Among cognitively unimpaired (CU) participants, all plasma markers correlated with age. Linear regression models revealed multiple relationships. For example, higher Charlson Comorbidity Index and chronic kidney disease were associated with higher levels of all biomarkers. Some relationships differed between mild cognitive impairment and dementia participants. Discussion: Multiple variables affect plasma biomarkers of amyloid pathology and neurodegeneration among CU in the general population. Incorporating this information is critical for accurate interpretation of the biomarker levels and for the development of reference ranges. [ABSTRACT FROM AUTHOR]

Published

2022

37. Incidence and prevalence of immune‐mediated necrotizing myopathy in adults in Olmsted County, Minnesota.

Author

Shelly, Shahar, Mielke, Michelle M., Paul, Pritikanta, Milone, Margherita, Tracy, Jennifer A., Mills, John R., Klein, Christopher J., Ernste, Floranne C., Mandrekar, Jay, and Liewluck, Teerin

Abstract

Introduction/Aims: Immune‐mediated necrotizing myopathy (IMNM) is considered a rare subtype of the immune‐mediated myopathies, but its incidence and prevalence are unknown. In this study we aimed to determine the incidence and prevalence of IMNM among adults in Olmsted County, Minnesota. Methods: We identified adult patients with IMNM, as defined by the 2016 European Neuromuscular Centre diagnostic criteria, among residents of Olmsted County, Minnesota over a 20‐year period. Results: Seven patients fulfilled the inclusion criteria. Six patients were tested for IMNM antibodies: four were anti–3‐hydroxy‐3‐methylglutaryl‐coenzyme A reductase (HMGCR) positive, one was anti–signal recognition particle positive, and one was seronegative. The incidence of IMNM during 2010‐2019 was 8.3 per million person‐years. The prevalence of IMNM in 2010 was 1.85 per 100 000 people at least 50 years of age. Median age at symptom onset was 64 (range, 52‐86) years and median time from symptom onset to diagnosis was 3 (range, <1 to 156) months. Statin use among anti‐HMGCR IMNM patients, but not the entire IMNM cohort, was higher than in controls (P =.024). Two IMNM patients developed cancers. The incidence of malignancy in IMNM was not higher than that of the general population. Treatment outcome was favorable in all patients except for one patient with delayed treatment and another with insufficient therapy. Among three deceased patients, one died of cancer and another died of IMNM‐related cardiorespiratory complications. Discussion: IMNM is a rare disease. Its prevalence is one tenth that of inclusion‐body myositis in Olmsted County, Minnesota. IMNM patients in our cohort were not at higher risk for developing cancer. [ABSTRACT FROM AUTHOR]

Published

2022

38. Comparison of CSF phosphorylated tau 181 and 217 for cognitive decline.

Author

Mielke, Michelle M., Aakre, Jeremiah A., Algeciras‐Schimnich, Alicia, Proctor, Nicholas K., Machulda, Mary M., Eichenlaub, Udo, Knopman, David S., Vemuri, Prashanthi, Graff‐Radford, Jonathan, Jack, Clifford R., Petersen, Ronald C., and Dage, Jeffrey L.

Abstract

Introduction: The prognostic utility of cerebrospinal fluid (CSF) phosphorylated tau 217 (p‐tau217) and p‐tau181 is not understood. Methods: Analyses included 753 Mayo Clinic Study on Aging participants (median age = 71.6; 57% male). CSF amyloid beta (Aβ)42 and p‐tau181 were measured with Elecsys immunoassays. CSF p‐tau181 and p‐tau217 were also measured with Meso Scale Discovery (MSD). We used Cox proportional hazards models for risk of mild cognitive impairment (MCI) and linear mixed models for risk of global and domain‐specific cognitive decline and cortical thickness. Analyses were stratified by elevated brain amyloid based on CSF Aβ42 or amyloid positron emission tomography for those with imaging. Results: CSF p‐tau217 was superior to p‐tau181 for the diagnosis of Alzheimer's disease (AD) pathology. CSF MSD p‐tau181 and p‐tau217 were associated with risk of MCI among amyloid‐positive individuals. Differences between CSF p‐tau measures predicting cortical thickness were subtle. Discussion: There are subtle differences for CSF p‐tau217 and p‐tau181 as prognostic AD markers. [ABSTRACT FROM AUTHOR]

Published

2022

39. Detection of Alzheimer's disease amyloid beta 1‐42, p‐tau, and t‐tau assays.

Author

van Harten, Argonde C., Wiste, Heather J., Weigand, Stephen D., Mielke, Michelle M., Kremers, Walter K., Eichenlaub, Udo, Dyer, Roy B., Algeciras‐Schimnich, Alicia, Knopman, David S., Jack, Clifford R., and Petersen, Ronald C.

Abstract

Introduction: We aimed to provide cut points for the automated Elecsys Alzheimer's disease (AD) cerebrospinal fluid (CSF) biomarkers. Methods: Cut points for Elecsys amyloid beta 42 (Aβ42), total tau (t‐tau), hyperphosphorylated tau (p‐tau), and t‐tau/Aβ42 and p‐tau/Aβ42 ratios were evaluated in Mayo Clinic Study of Aging (n = 804) and Mayo Clinic Alzheimer's Disease Research Center (n = 70) participants. Results: The t‐tau/Aβ42 and p‐tau/Aβ42 ratios had a higher percent agreement with normal/abnormal amyloid positron emission tomography (PET) than the individual CSF markers. Reciever Operating Characteristic (ROC)‐based cut points were 0.26 (0.24–0.27) for t‐tau/Aβ42 and 0.023 (0.020–0.025) for p‐tau/Aβ42. Ratio cut points derived from other cohorts performed as well in our cohort as our own did. Individual biomarkers had worse diagnostic properties and more variable results in terms of positive and negative percent agreement (PPA and NPA). Conclusion: CSF t‐tau/Aβ42 and p‐tau/Aβ42 ratios are very robust indicators of AD. For individual biomarkers, the intended use should determine which cut point is chosen. [ABSTRACT FROM AUTHOR]

Published

2022

40. Medical and nursing home costs: From cognitively unimpaired through dementia.

Author

Long, Kirsten Hall, Smith, Carin, Petersen, Ronald, Emerson, Jane, Ransom, Jeanine, Mielke, Michelle M., Hass, Steven, and Leibson, Cynthia

Abstract

Introduction: Efforts to model the cost‐effectiveness of managing/modifying cognitive impairment lack reliable, objective, baseline medical, and nursing‐home (NH) costs. Methods: A stratified‐random sample of Olmsted County, MN, residents ages 70–89 years (N = 3545), well‐characterized as cognitively unimpaired, mild cognitive impairment (MCI), or dementia, were followed forward ≤1 year in provider‐linked billing data and the Centers for Medicare & Medicaid Services NH assessments. Direct medical/nursing home/medical + NH costs were estimated. Costs were stratified by vital status and NH‐use intensity (NH days/follow‐up days [0%, 1% to 24%, 25% to 99%, and 100%]). Between‐category mean‐annual cost differences were adjusted for patient characteristics and follow‐up days. Results: Costs/follow‐up day distributions differed significantly across cognitive categories. Mean costs/follow‐up days were 2.5 to 18 times higher for decedents versus survivors. Among all persons with MCI, <9% with any NH use accounted for 18% of all total annual medical + NH costs. Adjusted‐between‐category comparisons revealed significantly higher medical and medical + NH costs for MCI versus cognitively unimpaired. Discussion: Cost‐effectiveness for managing/modifying both MCI and dementia should consider end‐of‐life costs and NH‐use intensity. Results can help inform cost‐effectiveness models, predict future‐care needs, and aid decision‐making by individuals/providers/payers/policymakers. [ABSTRACT FROM AUTHOR]

Published

2022

41. Comparing cerebrovascular disease diffusion MRI markers using post‐mortem and longitudinal imaging data.

Author

Raghavan, Sheelakumari, Przybelski, Scott A., Kamykowski, Michael G., Reid, Robert I., Lesnick, Timothy G., Murray, Melissa E., Reichard, Ross R., Graff‐Radford, Jonathan, Nguyen, Aivi T., Knopman, David S., Mielke, Michelle M., Jack, Clifford R., Petersen, Ronald C., and Vemuri, Prashanthi

Abstract

Background: Diffusion MRI (dMRI) based quantification of microstructural changes in white matter (WM) are increasingly proposed to measure cerebrovascular disease (CVD) related changes. Our objective was to compare the proposed dMRI markers using postmortem neuropathologic CVD data and then evaluate the predictors of longitudinal dMRI markers using serial scans. Method: We identified n=51 participants (mean age: 83.8 years, 63% males) with ante‐mortem dMRI and postmortem CVD evaluation and n=718 participants (mean age: 71.1 years, 56% males) with at least two dMRI scans from the population‐based sample of Mayo Clinic Study of Aging. We computed dMRI measures proposed for measuring CVD: Free Water (FW), Fractional Anisotropy (FA) adjusted for FW (FAadj), Peak width Skeletonized Mean Diffusivity (PSMD), and FA of the genu of corpus callosum (Genu‐FA). We used the FW and PSMD (PSMD release 1.8.1) kits from the MarkVCID consortium. Using weighted linear regression models with adjustments for MRI scan time to death, we evaluated associations between the baseline dMRI and two pathology CVD scores: Strozyk (represents the presence and number of macroscopic lesions) and Kalaria (represents the summary score of vessel wall modifications) scales. We ran linear mixed effect models with all available serial dMRI measures as outcomes and vascular risk (measured by the number of cardiovascular and metabolic conditions‐CMC), baseline imaging measures (amyloid and white matter hyperintensities (WMH)) and their interaction with time as key predictors. Result: Most dMRI markers were predictors of postmortem CVD pathology (Table 1). In longitudinal dMRI models, terms associated with amyloid explained little variability in dMRI (<1%) (Table 2). WMH was a significant predictor of baseline and decline in dMRI measures with WMH explaining a considerable percentage of variability in FW (34%) and PSMD (28%). Vascular risk measures were significant predictors of three out of the four dMRI measures. Conclusion: The diffusion measures proposed as surrogate markers of CVD map reasonably well to CVD pathological scales and do not change substantially as a function of baseline amyloidosis. Our findings shed light on variability in the proposed diffusion markers using postmortem data and longitudinal imaging data. Further work is needed to evaluate their clinical utility. [ABSTRACT FROM AUTHOR]

Published

2022

42. White matter health in the context of Alzheimer's disease pathophysiology.

Author

Raghavan, Sheelakumari, Przybelski, Scott A., Reid, Robert I., Lesnick, Timothy G., Ramanan, Vijay K, Botha, Hugo, Matchett, Billie J, Murray, Melissa E., Reichard, Ross R., Knopman, David S., Radford, Jonathan Graff, Jones, David T., Lowe, Val J., Mielke, Michelle M., Machulda, Mary M., Petersen, Ronald C., Kantarci, Kejal, Whitwell, Jennifer L, Josephs, Keith A, and Jack, Clifford R.

Abstract

Background: Multi‐compartment modelling of white matter (WM) microstructure using Neurite Orientation Dispersion and Density Imaging (NODDI) can provide information on WM health through the neurite (axons and dendrites) density index and free water measures. We hypothesized that cerebrovascular disease (CVD), Alzheimer's disease (AD), and an FDG pattern suggestive of TDP‐43 proteinopathy would be associated with distinct NODDI readouts of WM damage which would be informative for identifying the substrate for cognitive impairment. Method: We identified two independent cohorts with multi‐shell diffusion MRI, amyloid and tau PET, and cognitive assessments. One, were participants from the Mayo Clinic Study of Aging, a population‐based cohort of 347 elderly randomly sampled from the Olmsted county, Minnesota. The second were 61 amyloid positive AD participants from the Mayo AD Research Center. Result: We observed an increase in free water and decrease in neurite density in the genu of the corpus callosum associated with vascular risk factors, which we refer to as vascular WM component (Figure 1). Tau PET signal reflective of 3R/4R tau deposition was associated with worsening neurite density index in the temporal WM where we measured parahippocampal cingulum and inferior temporal WM bundles. Worsening temporal neurite density was associated with (antemortem confirmed) FDG TDP‐43 signature. Post‐mortem neuropathologic data on a small subset (n=9) of this sample lend support to our findings. In the population‐based cohort where vascular disease was more prevalent, the vascular WM component explained variability in global cognition (partial R2 of free water and neurite density = 8.3%) and MMSE performance (8.2%) which was comparable to amyloid PET (7.4% for global cognition and 6.6% for memory) (Table 1). In the AD dementia clinic‐based cohort, tau deposition was the greatest contributor to cognitive performance (9.6%), but there was also a non‐trivial contribution of the temporal WM component (8.5%) to cognitive performance. The differences observed between the two cohorts were reflective of their distinct clinical composition. Conclusion: White matter microstructural damage assessed using advanced diffusion models may add significant value for distinguishing the underlying substrate (whether CVD versus neurodegenerative disease caused by tau deposition or TDP‐43 pathology) for cognitive impairment in older individuals. [ABSTRACT FROM AUTHOR]

Published

2022

43. A blood screening tool for detecting mild cognitive impairment and Alzheimer’s disease among community-dwelling Mexican Americans and non-Hispanic Whites: A method for increasing representation of diverse populations in clinical research.

Author

O’Bryant, Sid E., Fan Zhang, Petersen, Melissa, Hall, James R., Johnson, Leigh A., Yaffe, Kristine, Mason, David, Braskie, Meredith, Barber, Robert A., Rissman, Robert A., Mapstone, Mark, Mielke, Michelle M., and Toga, Arthur W.

Abstract

ntroduction: Representation of Mexican Americans in Alzheimer’s disease (AD) clinical research has been extremely poor. Methods: Data were examined from the ongoing community-based, multi-ethnic Health & Aging Brain among Latino Elders (HABLE) study. Participants underwent functional exams, clinical labs, neuropsychological testing, and 3T magnetic resonance imaging of the brain. Fasting proteomic markers were examined for predicting mild cognitive impairment (MCI) and AD using support vector machine models. Results: Data were examined from n = 1649 participants (Mexican American n = 866; non-Hispanic White n = 783). Proteomic profiles were highly accurate in detecting MCI (area under the curve [AUC] = 0.91) and dementia (AUC = 0.95). The proteomic profiles varied significantly between ethnic groups and disease state. Negative predictive value was excellent for ruling out MCI and dementia across ethnic groups.Discussion: A blood-based screening tool can serve as a method for increasing access to state-of-the-art AD clinical research by bridging between community-based and clinic-based settings. [ABSTRACT FROM AUTHOR]

Published

2022

44. Mayo normative studies: A conditional normative model for longitudinal change on the Auditory Verbal Learning Test and preliminary validation in preclinical Alzheimer's disease.

Author

Alden, Eva C., Lundt, Emily S., Twohy, Erin L., Christianson, Teresa J., Kremers, Walter K., Machulda, Mary M., Jack, Clifford R., Knopman, David S., Mielke, Michelle M., Petersen, Ronald C., and Stricker, Nikki H.

Subjects

VERBAL learning, ALZHEIMER'S disease, AUDITORY learning, POSITRON emission, COGNITION disorders

Abstract

Introduction: The aim of this study was to develop a conditional normative model for Rey's Auditory Verbal Learning Test (AVLT) that accounts for practice effects. Methods: In our normative sample, robust conditional norms were derived from 1001 cognitively unimpaired (CU) adults ages 50 to 89 who completed the AVLT up to eight times. Linear mixed‐effects models adjusted for baseline performance, prior test exposures, time, demographics, and interaction terms. In our preliminary validation, mean performance on conditional and typical normative scores across two to four completed follow‐up tests in preclinical Alzheimer's disease participants at baseline with positive amyloid and tau positron emission (n = 27 CU amyloid [A]+tau[T]+) was compared to biomarker negative individuals (n = 269 CU A–T–). Results: AVLT performance using typical norms did not differ across A+T+ and A–T– groups. Conditional norms z‐scores were lower in the A+T+ relative to the A–T– group for 30‐minute recall (P =.033) and sum of trials (P =.030). Discussion: Conditional normative methods that account for practice effects show promise for identifying longitudinal cognitive decline. [ABSTRACT FROM AUTHOR]

Published

2022

45. A novel computer adaptive word list memory test optimized for remote assessment: Psychometric properties and associations with neurodegenerative biomarkers in older women without dementia.

Author

Stricker, Nikki H., Stricker, John L., Karstens, Aimee J., Geske, Jennifer R., Fields, Julie A., Hassenstab, Jason, Schwarz, Christopher G., Tosakulwong, Nirubol, Wiste, Heather J., Jack, Clifford R., Kantarci, Kejal, and Mielke, Michelle M.

Subjects

PSYCHOMETRICS, MEMORY testing, OLDER women, ALZHEIMER'S disease, VALUATION of real property

Abstract

Introduction: This study established the psychometric properties and preliminary validity of the Stricker Learning Span (SLS), a novel computer adaptive word list memory test designed for remote assessment and optimized for smartphone use. Methods: Women enrolled in the Mayo Clinic Specialized Center of Research Excellence (SCORE) were recruited via e‐mail or phone to complete two remote cognitive testing sessions. Convergent validity was assessed through correlation with previously administered in‐person neuropsychological tests (n = 96, ages 55–79) and criterion validity through associations with magnetic resonance imaging measures of neurodegeneration sensitive to Alzheimer's disease (n = 47). Results: SLS performance significantly correlated with the Auditory Verbal Learning Test and measures of neurodegeneration (temporal meta‐regions of interest and entorhinal cortical thickness, adjusting for age and education). Test–retest reliabilities across two sessions were 0.71–0.76 (two‐way mixed intraclass correlation coefficients). Discussion: The SLS is a valid and reliable self‐administered memory test that shows promise for remote assessment of aging and neurodegenerative disorders. [ABSTRACT FROM AUTHOR]

Published

2022

46. Association of plasma glial fibrillary acidic protein (GFAP) with neuroimaging of Alzheimer's disease and vascular pathology.

Author

Shir, Dror, Graff‐Radford, Jonathan, Hofrenning, Ekaterina I., Lesnick, Timothy G., Przybelski, Scott A., Lowe, Val J., Knopman, David S., Petersen, Ronald C., Jack, Clifford R., Vemuri, Prashanthi, Algeciras‐Schimnich, Alicia, Campbell, Michelle R., Stricker, Nikki H., and Mielke, Michelle M.

Subjects

GLIAL fibrillary acidic protein, ALZHEIMER'S disease, PATHOLOGY, POSITRON emission tomography, VASCULAR diseases

Abstract

Introduction: Plasma glial fibrillary acidic protein (GFAP) may be associated with amyloid burden, neurodegeneration, and stroke but its specificity for Alzheimer's disease (AD) in the general population is unclear. We examined associations of plasma GFAP with amyloid and tau positron emission tomography (PET), cortical thickness, white matter hyperintensities (WMH), and cerebral microbleeds (CMBs). Methods: The study included 200 individuals from the Mayo Clinic Study of Aging who underwent amyloid and tau PET and magnetic resonance imaging and had plasma GFAP concurrently assayed; multiple linear regression and hurdle model analyses were used to investigate associations controlling for age and sex. Results: GFAP was associated with amyloid and tau PET in multivariable models. After adjusting for amyloid, the association with tau PET was no longer significant. GFAP was associated with cortical thickness, WMH, and lobar CMBs only among those who were amyloid‐positive. Discussion: This cross‐sectional analysis demonstrates the utility of GFAP as a plasma biomarker for AD‐related pathologies. [ABSTRACT FROM AUTHOR]

Published

2022

47. Baseline CSF phosphorylated tau as an indicator of subsequent tau accumulation on tau PET.

Author

Cogswell, Petrice M, Wiste, Heather J., Mielke, Michelle M., Schwarz, Christopher G., Weigand, Stephen D, Lowe, Val J, Therneau, Terry M., Knopman, David S., Graff‐Radford, Jonathan, Vemuri, Prashanthi, Senjem, Matthew L., Gunter, Jeffrey L., Petersen, Ronald C., and Jack, Clifford R.

Abstract

Background: Alzheimer’s disease biomarkers of tau pathology may be assessed by both CSF and PET. Cross‐sectional associations between CSF phosphorylated tau (p‐tau) and tau PET have been studied and regional tau PET SUVR has been shown to have similar diagnostic performance as CSF p‐tau. The association between CSF p‐tau and longitudinal tau PET has not been studied. CSF measures may be thought of as a result of the imbalance of influx vs efflux of soluble tau, whereas, tau PET reflects total tau accumulation into insoluble aggregates to date. We therefore hypothesize that baseline CSF p‐tau may be a leading indicator of future tau PET accumulation. Method: We identified Mayo Clinic Study of Aging (MCSA) and Mayo Alzheimer’s Disease Research Center (ADRC) participants with diagnoses of cognitively unimpaired, mild cognitive impairment, and amnestic dementia who had CSF p‐tau (Elecsys p‐tau [181P]) and subsequent serial tau PET (flortaucipir) exams. The first tau PET scan was within 3 years of the CSF p‐tau collection. A longitudinal pipeline with two‐compartment partial volume correction was used to measure change in tau PET in a temporal‐lobe meta‐ROI (amygdala, fusiform, middle/inferior temporal, entorhinal, and parahippocampal regions) with a composite reference region (eroded supratentorial white matter, pons, and whole cerebellum). Spearman correlation was used to assess the association between CSF p‐tau and annual percent change in tau PET. A linear mixed effects model was fit to assess the association adjusting for age and sex. Result: The study included 143 participants (76% cognitively unimpaired) (). CSF p‐tau was significantly associated with annual percent change in tau PET overall (Spearman R=0.19, p=0.023) () and after adjusting for age and sex (p<0.001) (). There was nonlinearity in the CSF p‐tau effect, with higher values (>20 pg/mL) having a greater association with annual change in tau PET than lower values. Conclusion: In a group of cognitively unimpaired and impaired participants, CSF p‐tau predicted subsequent tau PET accumulation rate. A threshold effect is suggested with subsequent tau PET accumulation primarily in participants with elevated CSF p‐tau levels near the Mayo threshold of 22 pg/mL. [ABSTRACT FROM AUTHOR]

Published

2021

48. Effects of protocol and scanner changes on segmentation volume estimates in a dedicated crossover data set.

Author

Gunter, Jeffrey L., Wiste, Heather J., Kantarci, Kejal, Weigand, Stephen D, Vemuri, Prashanthi, Schwarz, Christopher G., Mielke, Michelle M., Graff‐Radford, Jonathan, Knopman, David S., Petersen, Ronald C., and Jack, Clifford R.

Abstract

Background: The Mayo Clinic Study of Aging and Alzheimer's Disease Research Center used GE scanners exclusively for MRI from 2005‐2017, employing consistent imaging parameters throughout. In 2017 the MRI protocol was updated and migrated to Siemens Prisma scanners; 113 participants were scanned with each configuration. The GE protocol included a 2D FLAIR. The Siemens protocol includes 3D FLAIR and T2‐weighted images. Both vendor protocols included a 3D T1. Experience with multi‐center trials suggests such changes may introduce systematic variations. Methods: GE scanning was carried out on 3T scanners with 12 channel phased array head coils. Siemens Prisma scanning was carried out with 64 channel head/neck coils. Imaging sequences and parameters are given in Table 1. We used the MCALT template and priors to perform standard six‐class segmentation on T1‐weighted (T1w) images. SPM12 unified segmentation supports the simultaneous use of multiple input contrasts; segmentation of multi‐contrast inputs was done using eight tissue classes including deep grey and white matter hyperintensity (WMH) priors. For a given MRI study (either GE or Siemens) all images were registered and resampled to the study's T1w image. Two‐channel (T1+FLAIR) segmentation was performed on GE scans. Two and three‐channel segmentations were performed on Siemens scans. Comparisons included total intracranial volume, total tissue volume and total grey matter volumes, as well as hippocampal volumes and grey matter volume in a temporal lobe meta‐ROI. Results: Four participants were excluded for poor image quality: one poor GE T1w quality, one poor Siemens T1, T2 and FLAIR quality, and two poor Siemens T2 quality. Comparisons were made among 109 participants aged 34–97 (Table 2). By visual assessment, adding T2‐weighted images always improved intracranial volume correctness. Using the combination of single‐channel GE and three‐channel Siemens generally improved cross‐vendor agreement on grey matter volumes with the exceptions of hippocampal and intracranial volume estimates. Conclusion: Requiring multiple input channels increases the likelihood that the result of a study being excluded. Combining T1w, FLAIR and T2w images allows the delineation of WMH and deep grey matter probability outputs but may introduce differences in GM volumes. [ABSTRACT FROM AUTHOR]

Published

2021

49. Knowledge gaps in Alzheimer's disease immune biomarker research.

Author

Morgan, David G. and Mielke, Michelle M.

Abstract

Considerable evidence has accumulated implicating a role for immune mechanisms in moderating the pathology in Alzheimer's disease dementia. However, the appropriate therapeutic target, the appropriate direction of manipulation, and the stage of disease at which to begin treatment remain unanswered questions. Part of the challenge derives from the absence of any selective pressure to develop a coordinated beneficial immune response to severe neural injury in adults. Thus, immune responses to the prevailing stimuli are likely to contain both beneficial and detrimental components. Knowledge gaps include: (1) how a biomarker change relates to the underlying biology, (2) the degree to which pathological stage group differences reflect a response to pathology versus trait differences among individuals regulating risk of developing pathology, (3) the degree to which biomarker levels are predictive of subsequent changes in pathology and/or cognition, and (4) experimental manipulations in model systems to determine whether differences in immune biomarkers are causally related to pathology. [ABSTRACT FROM AUTHOR]

Published

2021

50. Bridging the Gap: The Global CEOi Collaborative Workgroup for Adoption of Alzheimer's disease Blood‐Based Biomarkers in Clinical Practice.

Author

Udeh‐Momoh, Chi T., Mielke, Michelle M., Schindler, Suzanne E., Hansson, Oskar, Khachaturian, Ara S, and Weiss, Joan

Abstract

Background: The United States healthcare system is not prepared for disease modifying therapies (DMTs) of Alzheimer's disease (AD). Eligibility for DMTs will be contingent on confirmation of AD pathology using biomarkers. Major difficulties are expected in providing PET and CSF testing in the population. Blood‐based biomarkers (BBMs) could greatly reduce the burden of biomarker testing by triaging patients for subsequent confirmation of AD brain pathology in specialty and primary care. The Global CEO Initiative on Alzheimer's Disease (CEOi) has convened a Workgroup (WG) to develop guidelines and recommendations for the widespread adoption of BBMs in clinical practice to support feasible, timely, and accurate AD dementia diagnosis among symptomatic patients. Method: Over 80 stakeholders spanning academia, healthcare, advocacy, industry, non‐profit, and venture capital have joined the Workgroup, ensuring a wide range of expertise. The Workgroup consists of three active workstreams. Workstream A has defined use cases for symptomatic patients and minimum viable test specifications; Workstream B will provide recommendations on implementing BBMs in clinical practice; and Workstream C serves to educate practicing clinicians on outputs garnered from Workstreams A and B. Jointly led by 2 CEOi‐nominated experts, each Workstream has a core team, consisting of 6‐8 experts, and meet on a weekly basis to drive the WG objectives. General Workstream meetings are held periodically for the core team to present plans and outputs for full group input and feedback. Result: Workgroup members have conceptualized the clinical care pathway for operationalizing BBM across specialty and primary care settings; and will present a feasible framework for real‐world implementation of BBMs. We have defined appropriate‐use criteria for BBMs in clinical settings, including test specifications, and will provide actionable recommendations to accelerate adoption in clinical care, while critically considering implementation challenges such as test result interpretation, and value to existing diagnostic pathway. Strategies to facilitate optimal implementation including novel educational tools will be disseminated. Conclusion: The Workgroup seeks rapid, efficient and effective utility of BBMs in clinical practice that is scientifically valid, and patient focused. Successful adoption will facilitate effectual triaging of patients for comprehensive diagnostic evaluations, streamlining patient access to appropriate and integrated care. [ABSTRACT FROM AUTHOR]

Published

2023