Your search keyword '"Machulda, Mary M"' showing total 21 results

1. Non-right handed primary progressive apraxia of speech

Author

Botha, Hugo, Duffy, Joseph R., Whitwell, Jennifer L., Strand, Edythe A., Machulda, Mary M., Spychalla, Anthony J., Tosakulwong, Nirubol, Senjem, Matthew L., Knopman, David S., Petersen, Ronald C., Jack, Clifford R., Jr, Lowe, Val J., and Josephs, Keith A.

Published

2018

2. Excessive daytime sleepiness and fatigue may indicate accelerated brain aging in cognitively normal late middle-aged and older adults

Author

Carvalho, Diego Z., St. Louis, Erik K., Boeve, Bradley F., Mielke, Michelle M., Przybelski, Scott A., Knopman, David S., Machulda, Mary M., Roberts, Rosebud O., Geda, Yonas E., Petersen, Ronald C., Jack, Clifford R., Jr., and Vemuri, Prashanthi

Published

2017

3. Antiphospholipid syndrome mimicking posterior cortical atrophy and the “railroad track” sign on brain fluorodeoxyglucose-positron emission tomography

Author

Carlos, Arenn F., Graff-Radford, Jonathan, Crum, Brian A., Machulda, Mary M., Pham, Nha Trang Thu, Lowe, Val J., Whitwell, Jennifer L., and Josephs, Keith A.

Published

2023

4. Brain Regional Glucose Metabolism, Neuropsychiatric Symptoms, and the Risk of Incident Mild Cognitive Impairment: The Mayo Clinic Study of Aging.

Author

Krell-Roesch, Janina, Syrjanen, Jeremy A., Vassilaki, Maria, Lowe, Val J., Vemuri, Prashanthi, Mielke, Michelle M., Machulda, Mary M., Stokin, Gorazd B., Christianson, Teresa J., Kremers, Walter K., Jack, Clifford R., Knopman, David S., Petersen, Ronald C., Geda, Yonas E., and Jack, Clifford R Jr

Abstract

Objective: The authors conducted a prospective cohort study to examine the risk of incident mild cognitive impairment (MCI) as predicted by baseline neuropsychiatric symptoms (NPS) and brain regional glucose metabolic dysfunction.Methods: About 1,363 cognitively unimpaired individuals (52.8% males) aged ≥50 years were followed for a median of 4.8 years to the outcome of incident MCI. NPS were assessed using Beck Depression and Anxiety Inventories and Neuropsychiatric Inventory Questionnaire. Glucose hypometabolism was measured by fluorodeoxyglucose positron emission tomography and defined as standardized uptake value ratio ≤ 1.47 in regions typically affected in Alzheimer disease. Cox proportional hazards models were adjusted for age, sex, education, and APOE ε4 status.Results: Participants with regional glucose hypometabolism and depression (Beck Depression Inventory-II ≥13) had a more than threefold increased risk of incident MCI (hazard ratio [95% confidence interval], 3.66 [1.75, 7.65], p <0.001, χ2 = 11.83, degree of freedom [df] = 1) as compared to the reference group (normal regional glucose metabolism and no depression), and the risk was also significantly elevated (7.21 [3.54, 14.7], p <0.001, χ2 = 29.68, df = 1) for participants with glucose hypometabolism and anxiety (Beck Anxiety Inventory ≥10). Having glucose hypometabolism and ≥1 NPS (3.74 [2.40, 5.82], p <0.001, χ2 = 34.13, df = 1) or ≥2 NPS (3.89 [2.20, 6.86], p <0.001, χ2 = 21.92, df = 1) increased the risk of incident MCI by more than three times, and having ≥3 NPS increased the risk by more than four times (4.12 [2.03, 8.37], p <0.001, χ2 = 15.39, df = 1).Conclusion: Combined presence of NPS with regional glucose hypometabolism is associated with an increased risk of incident MCI, with fluorodeoxyglucose positron emission tomography appearing to be a stronger driving force of cognitive decline than NPS. [ABSTRACT FROM AUTHOR]

Published

2021

5. Aphasia with left occipitotemporal hypometabolism: A novel presentation of posterior cortical atrophy?

Author

Wicklund, Meredith R., Duffy, Joseph R., Strand, Edythe A., Whitwell, Jennifer L., Machulda, Mary M., and Josephs, Keith A.

Abstract

Abstract: Alzheimer’s disease is a common neurodegenerative disease often characterized by initial episodic memory loss. Atypical focal cortical presentations have been described, including the logopenic variant of primary progressive aphasia (lvPPA) which presents with language impairment, and posterior cortical atrophy (PCA) which presents with prominent visuospatial deficits. Both lvPPA and PCA are characterized by specific patterns of hypometabolism: left temporoparietal in lvPPA and bilateral parietoccipital in PCA. However, not every patient fits neatly into these categories. We retrospectively identified two patients with progressive aphasia and visuospatial deficits from a speech and language based disorders study. The patients were further characterized by MRI, fluorodeoxyglucose F18 and Pittsburgh Compound B (PiB) positron emission tomography. Two women, aged 62 and 69, presented with a history of a few years of progressive aphasia characterized by fluent output with normal grammar and syntax, anomia without loss of word meaning, and relatively spared repetition. They demonstrated striking deficits in visuospatial function for which they were lacking insight. Prominent hypometabolism was noted in the left occipitotemporal region and diffuse retention of PiB was noted. Posterior cortical atrophy may present focally with left occipitotemporal metabolism characterized clinically with a progressive fluent aphasia and prominent ventral visuospatial deficits with loss of insight. [Copyright &y& Elsevier]

Published

2013

6. Regional white matter hyperintensities in posterior cortical atrophy and logopenic progressive aphasia.

Author

Pham, Nha Trang Thu, Graff-Radford, Jonathan, Machulda, Mary M., Spychalla, Anthony J., Schwarz, Christopher G, Senjem, Matthew L., Lowe, Val J., Vemuri, Prashanthi, Kantarci, Kejal, Knopman, David S., Petersen, Ronald C., Jack, Clifford R., Josephs, Keith A., and Whitwell, Jennifer L.

Subjects

*CEREBRAL atrophy, *WHITE matter (Nerve tissue), *CEREBRAL small vessel diseases, *ALZHEIMER'S disease, *PARIETAL lobe, *APHASIA

Abstract

• Regional WMH frequencies differ between LPA, PCA, and typical AD • Total WMH increased with older age but was not related to beta-amyloid burden • WMH burden was associated with visuoperceptual performance in both atypical AD cohorts White matter hyperintensities (WMH) are markers of cerebral small vessel disease and are associated with higher risk of typical amnestic Alzheimer's disease (tAD). Little is known about the frequency and distribution of WMH in atypical variants of AD, including logopenic progressive aphasia (LPA) and posterior cortical atrophy (PCA). We investigated WMHs in 75 LPA, 39 PCA, and 50 tAD patients and associations with age, beta-amyloid PET burden, and cognition. PCA had greater subcortical WMHs in right occipital, parietal, and temporal lobes compared to LPA, and greater parieto-occipital subcortical and occipital periventricular WMHs than tAD. LPA had greater subcortical WMHs in left parietal lobe and deep white matter WMHs than PCA, and greater fronto-occipital subcortical and occipital periventricular WMHs than tAD. Total WMH increased with increasing age but was not related to beta-amyloid burden. Greater WMH was associated with visuoperceptual performance in LPA and PCA after correcting for atrophy. WMH topography differs across AD variants. Further work is needed to determine whether they reflect cerebrovascular disease or regionally specific neurodegenerative changes. [ABSTRACT FROM AUTHOR]

Published

2022

7. The association between peripheral total IGF-1, IGFBP-3, and IGF-1/IGFBP-3 and functional and cognitive outcomes in the Mayo Clinic Study of Aging.

Author

Wennberg, Alexandra M.V., Hagen, Clinton E., Machulda, Mary M., Hollman, John H., Roberts, Rosebud O., Knopman, David S., Petersen, Ronald C., and Mielke, Michelle M.

Subjects

*SOMATOMEDIN C, *INSULIN-like growth factor-binding proteins, *AGING, *REGRESSION analysis, *COGNITION

Abstract

Levels of insulin-like growth factor (IGF)-1, IGF-binding protein (IGFBP)-3, and their ratio in the blood may be useful for monitoring those at risk of cognitive and functional decline. However, the association between IGF measures and functional and cognitive outcomes has been mixed, and the associations may vary by sex. The present study investigated the cross-sectional, sex-specific associations between serum measures total IGF-1, IGFBP-3, and the IGF-1/IGFBP-3 ratio, gait speed, and cognition in 1320 cognitively unimpaired participants aged 50–95 years enrolled in the Mayo Clinic Study of Aging. We used multivariable linear regression models to determine the association between IGF measures and gait speed or cognitive test performance by sex. IGF measures were not associated with cognitive or functional performance among men. Among women, higher levels of log total IGF-1 and IGFBP-3 were associated with better performance in attention, visuospatial, and global cognitive domains, independent of the gait speed. These findings suggest that among women, IGF measures are associated with cognition, and these associations are independent of function. [ABSTRACT FROM AUTHOR]

Published

2018

8. Functional connectivity to the premotor cortex maps onto longitudinal brain neurodegeneration in progressive apraxia of speech.

Author

Sintini, Irene, Duffy, Joseph R., Clark, Heather M., Utianski, Rene L., Botha, Hugo, Machulda, Mary M., Senjem, Matthew L., Strand, Edythe A., Schwarz, Christopher G., Lowe, Val J., Jack, Clifford R., Josephs, Keith A., and Whitwell, Jennifer L.

Subjects

*SPEECH apraxia, *PREMOTOR cortex, *FUNCTIONAL connectivity, *AGRAMMATISM, *NEURODEGENERATION

Abstract

Primary progressive apraxia of speech (PPAOS) is a neurodegenerative motor speech disorder affecting the ability to produce speech. If agrammatic aphasia is present, it can be referred to as the non-fluent/agrammatic variant of primary progressive aphasia (nfvPPA). We investigated whether resting-state functional MRI (rs-fMRI) connectivity from disease "epicenters" correlated with longitudinal gray matter atrophy and hypometabolism in nfvPPA and PPAOS. Eighteen nfvPPA and 23 PPAOS patients underwent clinical assessment, structural MRI, rs-fMRI, and [18F] fluorodeoxyglucose (FDG)-PET at baseline and ∼2 years follow-up. Rates of neurodegeneration in nfvPPA and PPAOS correlated with functional connectivity to the premotor, motor, and frontal cortex. Connectivity to the caudate and thalamus was more strongly associated with rates of hypometabolism than atrophy. Connectivity to the left Broca's area was more strongly associated with rates of atrophy and hypometabolism in nfvPPA. Finally, functional connectivity to a network of regions, and not to a single epicenter, correlated with rates of neurodegeneration in PPAOS and nfvPPA, suggesting similar biological mechanisms driving disease progression, with regional differences related to language. [ABSTRACT FROM AUTHOR]

Published

2022

9. 1H MR spectroscopy biomarkers of neuronal and synaptic function are associated with tau deposition in cognitively unimpaired older adults.

Author

Kara, Firat, Joers, James M., Deelchand, Dinesh K., Park, Young Woo, Przybelski, Scott A., Lesnick, Timothy G., Senjem, Matthew L., Zeydan, Burcu, Knopman, David S., Lowe, Val J., Vemuri, Prashanthi, Mielke, Michelle M., Machulda, Mary M., Jack, Clifford R., Petersen, Ronald C., Öz, Gülin, and Kantarci, Kejal

Subjects

*OLDER people, *PROTON magnetic resonance spectroscopy, *TAU proteins, *CINGULATE cortex

Abstract

• Flortaucipir-PET is associated with MRS biomarkers in cognitively unimpaired adults. • Higher tau deposition is associated with lower glutamate/total creatine. • Higher tau deposition is associated with lower N-acetylaspartate/total creatine. • A sex by tau interaction was observed in association with glutamate/total creatine. • Association of tau with glutamate/total creatine is stronger in women than in men. Proton magnetic resonance spectroscopy (1H MRS) may provide information on pathophysiological changes associated with tau deposition in cognitively unimpaired older adults. In this study, the associations of posterior cingulate gyrus tau and amyloid beta (Aβ) deposition on PET with 1H MRS metabolite ratios acquired from bilateral posterior cingulate gyri were investigated in cognitively unimpaired older adults. Participants (n = 40) from the Mayo Clinic Study of Aging underwent single-voxel sLASER 1H MRS from the posterior cingulate gyrus at 3 Tesla, 18F-flortaucipir, and 11C- Pittsburgh Compound B (PiB) PET. An increase in posterior cingulate gyrus tau deposition, but not elevated Aβ, was associated with lower N-acetylaspartate/total creatine (tCr) and glutamate (Glu)/tCr ratios, and sex by tau interaction was observed in association with Glu/tCr. Higher tau levels in cognitively unimpaired older adults are associated with biomarkers of neural and synaptic injury even in the absence of cognitive impairment and these relationships appear to be stronger in women than in men. [ABSTRACT FROM AUTHOR]

Published

2022

10. Relationship of APOE, age at onset, amyloid and clinical phenotype in Alzheimer disease.

Author

Whitwell, Jennifer L., Tosakulwong, Nirubol, Weigand, Stephen D., Graff-Radford, Jonathan, Ertekin-Taner, Nilufer, Machulda, Mary M., Duffy, Joseph R., Schwarz, Christopher G., Senjem, Matthew L., Jack, Clifford R., Lowe, Val J., and Josephs, Keith A.

Subjects

*APOLIPOPROTEIN E, *DISEASE risk factors, *AGE of onset, *PHENOTYPES, *ALZHEIMER'S disease, *AMYLOID

Abstract

The apolipoprotein E (APOE) ε4 allele is the most well-established risk factor for Alzheimer's disease (AD), although its relationship to age at onset and clinical phenotype is unclear. We aimed to assess relationships between APOE genotype and age at onset, amyloid-beta (Aβ) deposition and typical versus atypical clinical presentations in AD. Frequency of APOE ε4 carriers by age at onset was assessed in 447 AD patients, 138 atypical AD patients recruited by the Neurodegenerative Research Group at Mayo Clinic, and 309 with typical AD from ADNI. APOE ε4 frequency increased with age at onset in atypical AD but showed a bell-shaped curve in typical AD where highest frequencies were observed between 65 and 70 years. Typical AD showed higher APOE ε4 frequencies than atypical AD only between the ages of 57 and 69 years. Global Aβ standard uptake value ratios did not differ according to APOE e4 status in either group. APOE genotype varies by both age at onset and clinical phenotype in AD, highlighting the heterogeneous nature of AD. [ABSTRACT FROM AUTHOR]

Published

2021

11. Comparing classic-onset corticobasal syndrome to speech/language-onset corticobasal syndrome.

Author

Garcia-Guaqueta, Danna P., Stephens, Yehkyoung C., Ali, Farwa, Utianski, Rene L., Duffy, Joseph R., Clark, Heather M., Thu Pham, Nha Trang, Machulda, Mary M., Lowe, Val J., Dickson, Dennis W., Whitwell, Jennifer L., and Josephs, Keith A.

Subjects

*PROGRESSIVE supranuclear palsy, *MOTOR cortex, *DEGENERATION (Pathology), *SYNDROMES, *WHITE matter (Nerve tissue), *DISEASE progression

Abstract

Patients with classic-onset corticobasal syndrome (CBS) present with asymmetric limb apraxia and parkinsonism. We have, however, observed patients who initially present with speech and/or language (SL) problems and several years later develop CBS (i.e., SL-onset CBS). We aimed to compare clinical, neuroimaging and pathological characteristics of classic-onset CBS with SL-onset CBS. We conducted a retrospective cohort study of 62 patients who met criteria for CBS (17 presented with classic-onset CBS and 45 had SL-onset CBS). We compared demographics, clinical characteristics, and grey and white matter volume loss with SPM12 between groups and assessed pathology and corticobasal degeneration (CBD) pathological lesion counts in patients who had died and undergone autopsy. Median age at CBS diagnosis was 66.4 years in classic-onset CBS and 73.6 years in SL-onset CBS. Classic-onset CBS had higher frequencies of dystonia, myoclonus, and alien limb phenomenon, while SL-onset CBS had a higher frequency of vertical supranuclear gaze palsy. Both groups showed smaller frontoparietal volumes than controls, with SL-onset CBS having greater volume loss in the left supplementary motor area than classic-onset CBS. All three classic-onset CBS cases with autopsy (100 %) had CBD pathology while 8/21 of SL-onset CBS cases (38 %) had CBD. Pathological lesion burden (including astrocytic plaques) did not differ between classic-onset and SL-onset CBS. Classic-onset and SL-onset CBS appear to be different syndromes, with the former being a more profuse motor syndrome. The more widespread volume loss in SL-onset CBS likely reflects longer disease course. • Speech/language-onset CBS syndrome differs from classic-onset CBS in anatomy and pathology. • Limb apraxia and dystonia were the most common features in the total cohort. • Myoclonus and alien limb phenomenon were uncommon, especially in speech/language-onset CBS. • Speech/language-onset CBS patients display more atrophy in the left SMA than classic-onset cases. [ABSTRACT FROM AUTHOR]

Published

2024

12. Reduced fractional anisotropy of the genu of the corpus callosum as a cerebrovascular disease marker and predictor of longitudinal cognition in MCI.

Author

Raghavan, Sheelakumari, Przybelski, Scott A., Reid, Robert I., Graff-Radford, Jonathan, Lesnick, Timothy G., Zuk, Samantha M., Knopman, David S., Machulda, Mary M., Mielke, Michelle M., Petersen, Ronald C., Jack, Clifford R., and Vemuri, Prashanthi

Subjects

*CORPUS callosum, *CEREBROVASCULAR disease, *KNEE, *DIFFUSION tensor imaging, *POSITRON emission tomography, *CEREBRAL amyloid angiopathy, *AGENESIS of corpus callosum

Abstract

Our goal was to evaluate the utility of diffusion tensor imaging (DTI) for predicting future cognitive decline in mild cognitive impairment (MCI) in conjunction with Alzheimer's disease (AD) biomarkers (amyloid positron emission tomography and AD signature neurodegeneration) in 132 MCI individuals ≥60 year old with structural magnetic resonance imaging, DTI, amyloid positron emission tomography, and at least one clinical follow-up. We used mixed-effect models to evaluate the prognostic ability of fractional anisotropy of the genu of the corpus callosum (FA-Genu), as a cerebrovascular disease marker, for predicting cognitive decline along with AD biomarkers. We contrasted the value of white matter hyperintensities, a traditional cerebrovascular disease marker as well as FA in the hippocampal cingulum bundle with the FA-Genu models. FA-Genu significantly predicted cognitive decline even after accounting for AD biomarkers. WMH was not associated with cognitive decline in the model with both WMH and FA-Genu. DTI specifically FA-Genu provides unique complementary information to AD biomarkers and has significant utility for prediction of cognitive decline in MCI. • DTI changes in the genu of the corpus callosum, an indicator of cerebrovascular disease, predicts cognitive decline in MCI. • Poor white matter health provided prognostic information beyond Alzheimer's disease biomarkers. • DTI measure in the genu provided greater prognostic information about cognitive decline in MCI in comparison to white matter hyperintensities which is the traditional cerebrovascular disease marker. [ABSTRACT FROM AUTHOR]

Published

2020

13. The evolution of parkinsonism in primary progressive apraxia of speech: A 6-year longitudinal study.

Author

Seckin, Zeynep Idil, Duffy, Joseph R., Strand, Edythe A., Clark, Heather M., Utianski, Rene L., Machulda, Mary M., Botha, Hugo, Ali, Farwa, Thu Pham, Nha Trang, Lowe, Val J., Whitwell, Jennifer L., and Josephs, Keith A.

Subjects

*PARKINSONIAN disorders, *SPEECH apraxia, *PROGRESSIVE supranuclear palsy, *MOVEMENT disorders, *SPEECH disorders, *DIAGNOSIS, *LONGITUDINAL method

Abstract

Introduction: Primary progressive apraxia of speech (PPAOS) is a neurodegenerative syndrome in which patients present with an isolated motor speech disorder. Some PPAOS patients develop parkinsonism and other features of progressive supranuclear palsy (PSP) and/or corticobasal syndrome (CBS) over time. We aimed to assess the evolution of parkinsonian characteristics in PPAOS patients who had been followed yearly for at least six years.Methods: From a large cohort of 46 PPAOS patients, eight were followed yearly for > 6-years in multiple NIH-funded grants. Parkinsonian and other features, including bradykinesia, tremor, rigidity, postural instability, apraxia, ocular motor function and cognition were assessed at each visit, and research criteria applied for PSP and CBS diagnosis. Neurological, speech-language test scores, and [18F]fluorodeoxyglucose PET (FDG-PET) and MRI midbrain volumes were assessed.Results: A Parkinson's plus syndrome developed in all eight patients (100%). Bradykinesia was the earliest feature, followed by rigidity and postural instability. Tremor was not a significant feature. Parkinsonism, limb apraxia and ocular motor impairment tended to develop four-to-five years after onset with some patients having slight asymmetric parkinsonism. Six patients (75%) met research criteria for probable PSP, although only one for PSP-Richardson's syndrome; three patients met criteria for possible CBS. Slightly asymmetric, left-sided, hypometabolism was observed on FDG-PET, not matching asymmetry of Parkinsonism. Midbrain hypometabolism was absent-minimal. Three patients had progressive midbrain volumes in the PSP-Richardson's syndrome range.Conclusions: A Parkinson's plus syndrome may inevitably develop in PPAOS supporting PPAOS as an early presentation of a Parkinson's plus disorder. [ABSTRACT FROM AUTHOR]

Published

2020

14. Longitudinal association between phosphatidylcholines, neuroimaging measures of Alzheimer's disease pathophysiology, and cognition in the Mayo Clinic Study of Aging.

Author

Li, Danni, Hagen, Clinton, Fett, Ashely R., Bui, Hai H., Knopman, David, Vemuri, Prashanthi, Machulda, Mary M., Jack, Clifford R., Petersen, Ronald C., and Mielke, Michelle M.

Subjects

*ALZHEIMER'S disease, *AGE factors in cognition, *PATHOLOGICAL physiology, *COGNITIVE testing, *OLDER people, *GLUCOSE metabolism, AGE factors in cognition disorders

Abstract

Plasma phosphatidylcholines (PCs) have been examined in the context of Alzheimer's disease dementia. However, their association with longitudinal changes in amyloid deposition remains unknown. This study investigated the associations of 8 plasma PC levels (PC aa [14:0_14:0], PC aa [16:0_16:0], PC aa [16:0_18:2], PC aa [16:0_22:6], PC aa [18:0_18:0], PC aa [18:0_18:1], PC aa [18:0_20:4], PC aa [18:1_18:1]) with cross-sectional and longitudinal measures of amyloid deposition, Alzheimer's disease–associated neurodegeneration (glucose metabolism and cortical thickness), and cognition (global- and domain-specific) of 1440 cognitively unimpaired participants (47% female, aged 50.7–95.3 years) in the Mayo Clinic Study of Aging. Longitudinally, higher baseline levels of PC aa [16:0_18:2], PC aa [18:0_18:1], and PC aa [18:1_18:1] were associated with slower decline in performance on tests of global cognition and specific cognitive domains. Furthermore, higher baseline levels of plasma PC aa (14:0_14:0) were associated with slower amyloid deposition and cortical thinning after multiple covariable adjustment (age, sex, education, medical comorbidity, dyslipidemia, statin use, and APOE4 allele presence). Our study findings support an independent association between plasma PC aa (14:0_14:0) with slower amyloid deposition and cortical thinning among cognitively unimpaired older adults. • We examined associations of 8 plasma phosphatidylcholines (PCs) with neuroimaging measures and cognition. • Higher levels of 4 PCs are associated with better performance on cognitive tests. • Higher PC aa (14:0_14:0) is associated with better AD neuroimaging measures over time. [ABSTRACT FROM AUTHOR]

Published

2019

15. The influence of tau, amyloid, alpha-synuclein, TDP-43, and vascular pathology in clinically normal elderly individuals.

Author

Wennberg, Alexandra M., Whitwell, Jennifer L., Tosakulwong, Nirubol, Weigand, Stephen D., Murray, Melissa E., Machulda, Mary M., Petrucelli, Leonard, Mielke, Michelle M., Jack, Clifford R., Knopman, David S., Parisi, Joseph E., Petersen, Ronald C., Dickson, Dennis W., and Josephs, Keith A.

Subjects

*APOLIPOPROTEIN E, *ALPHA-synuclein, *ENTORHINAL cortex, *AMYLOID, *CEREBRAL atrophy, *PATHOLOGY

Abstract

Many individuals live to older ages without clinical impairment. It is unknown whether brain pathologies in these individuals are associated with subtle clinical deficits. We analyzed the brains of 161 clinically normal (Clinical Dementia Rating score = 0) older individuals enrolled in the Mayo Clinic Patient Registry or Study of Aging. We assessed for the presence and burden of beta-amyloid, tau, alpha-synuclein, TDP-43, and vascular pathology. We investigated whether pathologies were associated with antemortem cognitive and motor function, depression, MRI volumetric measures, or the apolipoprotein E (APOE) ε4 allele. Eighty-six percent had at least 1 pathology, and 63% had mixed pathologies. Tau and vascular pathology were associated with poorer memory scores. Tau was also associated with poorer general cognition scores and smaller amygdala, hippocampi, and entorhinal cortex volumes. Beta-amyloid neuritic plaque burden was associated with greater depression scores. The presence of a greater number of pathologies was associated with APOE e4 carrier status and with poorer memory performance. Some dementia-related pathologies are associated with poorer performance in clinical measures and brain atrophy in the unimpaired elderly. • Clinically normal elderly may have dementia-related pathology and subtle deficits. • Tau and vascular pathology are associated with poorer memory scores. • Tau is also associated with smaller medial temporal lobe volumes. • Tau may be necessary but not sufficient to cause dementia. • APOE ε4 appears to be a risk factor for more than 1 pathology. [ABSTRACT FROM AUTHOR]

Published

2019

16. The MAPT p.E342K and p.R406W mutations are associated with progressive supranuclear palsy with atypical features.

Author

Badihian, Negin, Ali, Farwa, Botha, Hugo, Savica, Rodolfo, Machulda, Mary M., Clark, Heather M., Stierwalt, Julie A.G., Pham, Nha Trang Thu, Baker, Matthew C., Rademakers, Rosa, Lowe, Val, Whitwell, Jennifer L., and Josephs, Keith A.

Subjects

*PROGRESSIVE supranuclear palsy, *DENTATE nucleus, *ALZHEIMER'S disease, *FRONTAL lobe, *TEMPORAL lobe, *ENTORHINAL cortex

Abstract

Progressive supranuclear palsy (PSP) is an atypical parkinsonism caused by the intracerebral aggregation of the microtubule-associated protein tau (MAPT) which is encoded by MAPT gene. Although PSP is a sporadic disease, MAPT mutations have been reported in rare cases. Among 190 patients with PSP who were recruited by the Neurodegenerative Research Group at Mayo Clinic during 2009–2023, we identified two patients who fulfilled diagnostic criteria for PSP-Richardson's syndrome (PSP-RS) and harbor novel MAPT mutations. To better investigate the potential effects of these mutations, we compared the clinical, and neuroimaging characteristics of these two patients to 20 randomly selected patients with PSP-RS without a MAPT mutation. MAPT c.1024G > A, p. Glu342Lys, and MAPT c.1217 G > A, p. Arg406Gln mutations were found in 2 men who developed PSP-RS with atypical features at the ages of 60 and 62 years, respectively. Glu342Lys mutation was associated with features resembling alpha-synucleinopathies (autonomic dysfunction, dream enactment behavior), while both mutations were associated with features suggestive of Alzheimer's disease with poorer performance on tests of episodic memory. Comparison of 18F-flortaucipir uptake between the two MAPT mutation cases with 20 patients without a mutation revealed increased signal on flortaucipir-PET in bilateral medial temporal lobe regions (amygdala, entorhinal cortices, hippocampus, parahippocampus) but not in PSP-related regions (globus pallidum, midbrain, superior frontal cortex and dentate nucleus of the cerebellum). Glu342Lys and Arg406Gln mutations appear to modify the PSP-RS phenotype by targeting the medial temporal lobe regions resulting in more memory loss and greater flortaucipir uptake. • MAPT mutations have been reported in rare cases of progressive supranuclear palsy. • We found novel MAPT mutations: c.1024G > A, p. Glu342Lys, and c.1217 G > A, p. Arg406Gln. • Both mutations were associated with greater memory loss and flortaucipir uptake. • Patients showed medial temporal lobe neurodegeneration. • These mutations modify PSP-RS phenotype by targeting medial temporal lobe regions. [ABSTRACT FROM AUTHOR]

Published

2024

17. Joint associations of β-amyloidosis and cortical thickness with cognition.

Author

Knopman, David S., Lundt, Emily S., Therneau, Terry M., Vemuri, Prashanthi, Lowe, Val J., Kantarci, Kejal, Gunter, Jeffrey L., Senjem, Matthew L., Mielke, Michelle M., Machulda, Mary M., Roberts, Rosebud O., Boeve, Bradley F., Jones, David T., Petersen, Ronald C., and Jr.Jack, Clifford R.

Subjects

*COGNITION, *AMYLOIDOSIS, *ALZHEIMER'S disease, *MACHINE learning, *AMYLOID

Abstract

In 1164 cognitively unimpaired persons, aged 50–95 years, from the population-based Mayo Clinic Study of Aging, we examined the relationships of baseline cognition and cognitive changes across the full range of cortical thickness of an Alzheimer signature region of interest and global β-amyloid levels measured by Pittsburgh compound B positron emission tomography (PIB PET) standardized uptake value ratio (SUVR). In machine-learning models accounting for both biomarkers simultaneously, worsening biomarker values were additive and associated with lower baseline global cognition and greater subsequent decline in global cognition. Associations between Alzheimer's disease signature cortical thickness or PIB PET β-amyloid SUVR and baseline cognition were mainly linear. Lower Alzheimer's disease signature cortical thickness values across the entire range of thickness predicted future decline in global cognitive scores, demonstrating its close relationship to cognitive functioning. PIB PET β-amyloid SUVR also predicted cognitive decline across its full range, even when cortical thickness was accounted for. PIB PET β-amyloid's relationship to cognitive decline was nonlinear, more prominent at lower β-amyloid levels and less prominent at higher β-amyloid levels. [ABSTRACT FROM AUTHOR]

Published

2018

18. Age-specific and sex-specific prevalence of cerebral β-amyloidosis, tauopathy, and neurodegeneration in cognitively unimpaired individuals aged 50-95 years: a cross-sectional study.

Author

JrJack, Clifford R, Wiste, Heather J, Weigand, Stephen D, Therneau, Terry M, Knopman, David S, Lowe, Val, Vemuri, Prashanthi, Mielke, Michelle M, Roberts, Rosebud O, Machulda, Mary M, Senjem, Matthew L, Gunter, Jeffrey L, Rocca, Walter A, Petersen, Ronald C, and Jack, Clifford R Jr

Subjects

*CEREBRAL amyloid angiopathy, *AMYLOIDOSIS, *CEREBRAL arterial diseases, *NEURODEGENERATION, *MILD cognitive impairment, *AGE distribution, *MAGNETIC resonance imaging, *PEPTIDES, *SEX distribution, *POSITRON emission tomography, *DISEASE prevalence, *CROSS-sectional method

Abstract

Background: A new classification for biomarkers in Alzheimer's disease and cognitive ageing research is based on grouping the markers into three categories: amyloid deposition (A), tauopathy (T), and neurodegeneration or neuronal injury (N). Dichotomising these biomarkers as normal or abnormal results in eight possible profiles. We determined the clinical characteristics and prevalence of each ATN profile in cognitively unimpaired individuals aged 50 years and older.Methods: All participants were in the Mayo Clinic Study of Aging, a population-based study that uses a medical records linkage system to enumerate all individuals aged 50-89 years in Olmsted County, MN, USA. Potential participants are randomly selected, stratified by age and sex, and invited to participate in cognitive assessments; individuals without medical contraindications are invited to participate in brain imaging studies. Participants who were judged clinically as having no cognitive impairment and underwent multimodality imaging between Oct 11, 2006, and Oct 5, 2016, were included in the current study. Participants were classified as having normal (A-) or abnormal (A+) amyloid using amyloid PET, normal (T-) or abnormal (T+) tau using tau PET, and normal (N-) or abnormal (N+) neurodegeneration or neuronal injury using cortical thickness assessed by MRI. We used the cutoff points of standard uptake value ratio (SUVR) 1·42 (centiloid 19) for amyloid PET, 1·23 SUVR for tau PET, and 2·67 mm for MRI cortical thickness. Age-specific and sex-specific prevalences of the eight groups were determined using multinomial models combining data from 435 individuals with amyloid PET, tau PET, and MRI assessments, and 1113 individuals who underwent amyloid PET and MRI, but not tau PET imaging.Findings: The numbers of participants in each profile group were 165 A-T-N-, 35 A-T+N-, 63 A-T-N+, 19 A-T+N+, 44 A+T-N-, 25 A+T+N-, 35 A+T-N+, and 49 A+T+N+. Age differed by ATN group (p<0·0001), ranging from a median 58 years (IQR 55-64) in A-T-N- and 57 years (54-64) in A-T+N- to a median 80 years (75-84) in A+T-N+ and 79 years (73-87) in A+T+N+. The number of APOE ε4 carriers differed by ATN group (p=0·04), with carriers roughly twice as frequent in each A+ group versus the corresponding A- group. White matter hyperintensity volume (p<0·0001) and cognitive performance (p<0·0001) also differed by ATN group. Tau PET and neurodegeneration biomarkers were discordant in most individuals who would be categorised as stage 2 or 3 preclinical Alzheimer's disease (A+T+N-, A+T-N+, and A+T+N+; 86% at age 65 years and 51% at age 80 years) or with suspected non-Alzheimer's pathophysiology (A-T+N-, A-T-N+, and A-T+N+; 92% at age 65 years and 78% at age 80 years). From age 50 years, A-T-N- prevalence declined and A+T+N+ and A-T+N+ prevalence increased. In both men and women, A-T-N- was the most prevalent until age late 70s. After about age 80 years, A+T+N+ was most prevalent. By age 85 years, more than 90% of men and women had one or more biomarker abnormalities.Interpretation: Biomarkers of fibrillar tau deposition can be included with those of β-amyloidosis and neurodegeneration or neuronal injury to more fully characterise the heterogeneous pathological profiles in the population. Both amyloid- dependent and amyloid-independent pathological profiles can be identified in the cognitively unimpaired population. The prevalence of each ATN group changed substantially with age, with progression towards more biomarker abnormalities among individuals who remained cognitively unimpaired.Funding: National Institute on Aging (part of the US National Institutes of Health), the Alexander Family Professorship of Alzheimer's Disease Research, the Mayo Clinic, and the GHR Foundation. [ABSTRACT FROM AUTHOR]

Published

2017

19. Evolution of neurodegeneration-imaging biomarkers from clinically normal to dementia in the Alzheimer disease spectrum.

Author

Knopman, David S., Jr.Jack, Clifford R., Lundt, Emily S., Weigand, Stephen D., Vemuri, Prashanthi, Lowe, Val J., Kantarci, Kejal, Gunter, Jeffrey L., Senjem, Matthew L., Mielke, Michelle M., Machulda, Mary M., Roberts, Rosebud O., Boeve, Bradley F., Jones, David T., and Petersen, Ronald C.

Subjects

*NEURODEGENERATION, *BIOMARKERS, *DEMENTIA, *ALZHEIMER'S disease, *POSITRON emission tomography, *DIAGNOSIS

Abstract

The availability of antemortem biomarkers for Alzheimer's disease (AD) enables monitoring the evolution of neurodegenerative processes in real time. Pittsburgh compound B (PIB) positron emission tomography (PET) was used to select participants in the Mayo Clinic Study of Aging and the Mayo Alzheimer's Disease Research Center with elevated β-amyloid, designated as “A+,” and hippocampal volume and 18 fluorodeoxyglucose (FDG) positron emission tomography were used to characterize participants as having evidence of neurodegeneration (“N+”) at the baseline evaluation. There were 145 clinically normal (CN) A+ individuals, 62 persons with mild cognitive impairment (MCI) who were A+ and 20 with A+ AD dementia. Over a period of 1–6 years, MCI A+N+ individuals showed declines in medial temporal, lateral temporal, lateral parietal, and to a lesser extent, medial parietal regions for both FDG standardized uptake value ratio and gray matter volume that exceeded declines seen in the CN A+N+ group. The AD dementia group showed declines in the same regions on FDG standardized uptake value ratio and gray matter volume with rates that exceeded that in MCI A+N+. Expansion of regional involvement and faster rate of neurodegeneration characterizes progression in the AD pathway. [ABSTRACT FROM AUTHOR]

Published

2016

20. Longitudinal clinical decline and baseline predictors in progressive supranuclear palsy.

Author

Pavone, Costanza, Weigand, Stephen W., Ali, Farwa, Clark, Heather M., Botha, Hugo, Machulda, Mary M., Savica, Rodolfo, Pham, Nha Trang Thu, Grijalva, Rosalie M., Schwarz, Christopher G., Senjem, Matthew L., Agosta, Federica, Filippi, Massimo, Jack, Clifford R., Lowe, Val J., Josephs, Keith A., and Whitwell, Jennifer L.

Subjects

*PROGRESSIVE supranuclear palsy, *MONTREAL Cognitive Assessment, *MOTOR cortex, *PROGNOSIS, *DISEASE progression, *COGNITION disorders

Abstract

Progressive supranuclear palsy (PSP) is associated with several clinical variants defined based on ocular motor dysfunction, postural instability, akinesia, and cognitive dysfunction, although little is known about how these features progress over time. We aimed to assess the evolution of these core clinical features across variants and assess baseline clinical and neuroimaging predictors of progression. Ninety-three PSP patients were recruited by the Neurodegenerative Research Group, Mayo Clinic, and underwent two visits 1-year apart, with baseline MRI and [18F]flortaucipir PET. We compared baseline and annualized rates of clinical change on the PSP Rating Scale (total, ocular motor, gait/midline scores) and Montreal Cognitive Assessment, across PSP-Richardson's, PSP-Cortical and PSP-Subcortical variants and assessed relationships between rates of change and baseline regional imaging. Ocular motor scores differed across groups at baseline and follow-up, with lowest scores observed in PSP-subcortical, but no differences were observed in rate of change across groups. PSP Rating Scale total and gait/midline scores differed across groups at follow-up and in rates of change, with PSP-subcortical showing the least impairment and slowest progression. Greatest cognitive impairment was observed in PSP-Cortical. Sample size estimates for treatment trials differed across PSP variants. Greater baseline flortaucipir uptake, but not volume, of midbrain and motor cortex correlated with faster rates of clinical decline. The PSP Rating Scale and its subscores might be useful markers for the prognostic stratification of PSP variants. Flortaucipir imaging at baseline may help predict rate of decline. • Subcortical variants of PSP show the slowest rates of clinical progression. • Cortical variants of PSP show fastest decline in motor symptoms. • Sample size estimates for treatment trials differ across PSP variants. • Tau-PET uptake in midbrain and motor cortex predict rates of clinical decline. [ABSTRACT FROM AUTHOR]

Published

2023

21. Transition rates between amyloid and neurodegeneration biomarker states and to dementia: a population-based, longitudinal cohort study.

Author

JrJack, Clifford R, Therneau, Terry M, Wiste, Heather J, Weigand, Stephen D, Knopman, David S, Lowe, Val J, Mielke, Michelle M, Vemuri, Prashanthi, Roberts, Rosebud O, Machulda, Mary M, Senjem, Matthew L, Gunter, Jeffrey L, Rocca, Walter A, Petersen, Ronald C, and Jack, Clifford R Jr

Subjects

*AMYLOID, *NEURODEGENERATION, *BIOMARKERS, *TREATMENT of dementia, *LONGITUDINAL method, *COGNITION disorders diagnosis, *DIAGNOSIS of dementia, *DEMENTIA, *COGNITION disorders, *PUBLIC health surveillance, *RESEARCH funding, *CROSS-sectional method, *DISEASE progression, *PSYCHOLOGICAL factors, *PSYCHOLOGY, *DIAGNOSIS

Abstract

Background: In a 2014 cross-sectional analysis, we showed that amyloid and neurodegeneration biomarker states in participants with no clinical impairment varied greatly with age, suggesting dynamic within-person processes. In this longitudinal study, we aimed to estimate rates of transition from a less to a more abnormal biomarker state by age in individuals without dementia, as well as to assess rates of transition to dementia from an abnormal state.Methods: Participants from the Mayo Clinic Study of Aging (Olmsted County, MN, USA) without dementia at baseline were included in this study, a subset of whom agreed to multimodality imaging. Amyloid PET (with (11)C-Pittsburgh compound B) was used to classify individuals as amyloid positive (A(+)) or negative (A(-)). (18)F-fluorodeoxyglucose ((18)F-FDG)-PET and MRI were used to classify individuals as neurodegeneration positive (N(+)) or negative (N(-)). We used all observations, including those from participants who did not have imaging results, to construct a multistate Markov model to estimate four different age-specific biomarker state transition rates: A(-)N(-) to A(+)N(-); A(-)N(-) to A(-)N(+) (suspected non-Alzheimer's pathology); A(+)N(-) to A(+)N(+); and A(-)N(+) to A(+)N(+). We also estimated two age-specific rates to dementia: A(+)N(+) to dementia and A(-)N(+) to dementia. Using these state-to-state transition rates, we estimated biomarker state frequencies by age.Findings: At baseline (between Nov 29, 2004, to March 7, 2015), 4049 participants did not have dementia (3512 [87%] were clinically normal and 537 [13%] had mild cognitive impairment). 1541 individuals underwent imaging between March 28, 2006, to April 30, 2015. Transition rates were low at age 50 years and, with one exception, exponentially increased with age. At age 85 years compared with age 65 years, the rate was nearly 11-times higher (17.2 vs 1.6 per 100 person-years) for the transition from A(-)N(-) to A(-)N(+), three-times higher (20.8 vs 6.1) for A(+)N(-) to A(+)N(+), and five-times higher (13.2 vs 2.6) for A(-)N(+) to A(+)N(+). The rate of transition was also increased at age 85 years compared with age 65 years for A(+)N(+) to dementia (7.0 vs 0.8) and for A(-)N(+) to dementia (1.7 vs 0.6). The one exception to an exponential increase with age was the transition rate from A(-)N(-) to A(+)N(-), which increased from 4.0 transitions per 100 person-years at age 65 years to 6.9 transitions per 100 person-years at age 75 and then plateaued beyond that age. Estimated biomarker frequencies by age from the multistate model were similar to cross-sectional biomarker frequencies.Interpretation: Our transition rates suggest that brain ageing is a nearly inevitable acceleration toward worse biomarker and clinical states. The one exception is the transition to amyloidosis without neurodegeneration, which is most dynamic from age 60 years to 70 years and then plateaus beyond that age. We found that simple transition rates can explain complex, highly interdependent biomarker state frequencies in our population.Funding: National Institute on Aging, Alexander Family Professorship of Alzheimer's Disease Research, the GHR Foundation. [ABSTRACT FROM AUTHOR]

Published

2016