Cross-Sectional Exploration of Plasma Biomarkers of Alzheimer’s Disease in Down Syndrome: Early Data from the Longitudinal Investigation for Enhancing Down Syndrome Research (LIFE-DSR) Study

Hendrix, James A.; Airey, David; Britton, Angela; Burke, Anna; Capone, George T.; Chávez, R Cortés; Chen, Jacqueline; Chicoine, Brian; Costa, Alberto C. S.; Dage, Jeffrey L.; Doran, Eric; Esbensen, Anna J.; Evans, Casey L.; Faber, Kelley; Foroud, Tatiana; Hart, Sarah J.; Haugen, Kelsey; Head, Elizabeth; Hendrix, Suzanne; Hillerstrom, Hampus; Kishnani, Priya S.; Krell, Kavita; Ledesma, Duvia Lara; Lai, Florence; Lott, Ira T.; Ochoa-Lubinoff, Cesar; Mason, Jennifer; Nicodemus‐Johnson, Jessie; Proctor, Nicholas K.; Pulsifer, Margaret B.; Revta, Carolyn; Rosas, H. Diana; Rosser, Tracie C.; Santoro, Stephanie L.; Schafer, Kimberly; Scheidemantel, Thomas; Schmitt, Frederick A.; Skotko, Brian G.; Stasko, Melissa R.; Talboy, Amy; Torres, Amy; Wilmes, Kristi; Woodward, Julie; Zimmer, Jennifer A.; Feldman, Howard; Mobley, William C.

doi:10.3390/jcm10091907

Cited by 20 publications

(22 citation statements)

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“…Activation of astrocytes and microglia, the secretion of inflammatory cytokines (e.g., IL-1, IL-6, and TNFα), and acute phase proteins are observed in both the brains and blood of people with DS, indicating an “inflammatory endophenotype” (Petersen and O’Bryant, 2019 ). In a cross-sectional analysis of people with DS, plasma glial fibrillary acidic protein (GFAP), a marker of astrogliosis, was found to increase starting in their mid-40s (Hendrix et al, 2021 ).…”

Section: Introductionmentioning

confidence: 99%

“…Higher plasma levels of GFAP are correlated with lower measures of episodic memory and microstructural integrity in AD, MCI, and also in healthy aged donors (Bettcher et al, 2021 ). As discussed, people with DS also have increasing levels of plasma GFAP starting in their mid-40s (Hendrix et al, 2021 ). Thus, although initially thought to be a secondary effect of aberrant protein accumulation, changes in the innate immune system and neuroinflammation are now thought to be a core, early feature of both DS and AD that interface with, and may contribute to, clinical manifestations of cognitive disorders and decline (Lucin and Wyss-Coray, 2009 ; Heneka et al, 2015 ).…”

Section: Introductionmentioning

confidence: 99%

“…Biomarkers of neuroinflammation, amyloid and tau pathology, and neurodegeneration increase over the lifetimes of the vast majority of individuals with DS. Neuroinflammatory biomarkers such as GFAP may begin increasing as early as the late teenage years and progressively increase throughout life (Hendrix et al, 2021 ). Changes in amyloid biomarkers are detectable after 20 years of age, with APOE genotype significantly contributing to risk (Rubinsztein et al, 1999 ; Deb et al, 2000 ), likely due to apoE-catalyzed amyloid-β (Aβ) polymerization during the early seeding stages of amyloid formation (Potter and Wisniewski, 2012 ).…”

Section: Introductionmentioning

confidence: 99%

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Innate Immune System Activation and Neuroinflammation in Down Syndrome and Neurodegeneration: Therapeutic Targets or Partners?

Ahmed

Johnson

Boyd

et al. 2021

Front. Aging Neurosci.

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Innate immune system activation and inflammation are associated with and may contribute to clinical outcomes in people with Down syndrome (DS), neurodegenerative diseases such as Alzheimer’s disease (AD), and normal aging. In addition to serving as potential diagnostic biomarkers, innate immune system activation and inflammation may play a contributing or causal role in these conditions, leading to the hypothesis that effective therapies should seek to dampen their effects. However, recent intervention studies with the innate immune system activator granulocyte-macrophage colony-stimulating factor (GM-CSF) in animal models of DS, AD, and normal aging, and in an AD clinical trial suggest that activating the innate immune system and inflammation may instead be therapeutic. We consider evidence that DS, AD, and normal aging are accompanied by innate immune system activation and inflammation and discuss whether and when during the disease process it may be therapeutically beneficial to suppress or promote such activation.

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Section: Introductionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

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Innate Immune System Activation and Neuroinflammation in Down Syndrome and Neurodegeneration: Therapeutic Targets or Partners?

Ahmed

Johnson

Boyd

et al. 2021

Front. Aging Neurosci.

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“…Recent improvements in medical care have contributed to the increased longevity of individuals with DS, and advancements in diagnostic biomarkers have facilitated studies of key questions regarding the interconnected clinical and neuropathological features that develop with age in DS (Neale et al, 2018 ; Handen et al, 2020 ; Head and Ances, 2020 ; Petersen et al, 2020 , 2021 ; Rafii et al, 2020 ; Hendrix et al, 2021 ). Positron emission tomography (PET) studies using Pittsburgh Compound-B ( 11 C-PiB) and related amyloid-binding radiopharmaceuticals provide insight into regional distributions and temporal changes in Aβ pathology in living people with AD (Klunk et al, 2004 ; Rowe et al, 2007 ; Cohen et al, 2012 ; Mathis et al, 2017 ; Villemagne et al, 2021 ) and this technology is being applied increasingly to studies of individuals with DS (Landt et al, 2011 ; Handen et al, 2012 ; Hartley et al, 2014 , 2017 , 2020 ; Annus et al, 2016 , 2017 ; Lao et al, 2016 , 2017 , 2018 ; Cole et al, 2017 ; Cohen et al, 2018 ; Neale et al, 2018 ; Mak et al, 2019a , b ; Mihaila et al, 2019 ; Tudorascu et al, 2019 , 2020 ; Wilson et al, 2019 ; Cody et al, 2020 ; Zammit et al, 2020 , 2021 ).…”

Section: Introductionmentioning

confidence: 99%

Postmortem Neocortical 3H-PiB Binding and Levels of Unmodified and Pyroglutamate Aβ in Down Syndrome and Sporadic Alzheimer’s Disease

Pivtoraiko

Racic

Abrahamson

et al. 2021

Front. Aging Neurosci.

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Individuals with Down syndrome (DS) have a genetic predisposition for amyloid-β (Aβ) overproduction and earlier onset of Aβ deposits compared to patients with sporadic late-onset Alzheimer’s disease (AD). Positron emission tomography (PET) with Pittsburgh Compound-B (PiB) detects fibrillar Aβ pathology in living people with DS and AD, but its relationship with heterogeneous Aβ forms aggregated within amyloid deposits is not well understood. We performed quantitative in vitro3H-PiB binding assays and enzyme-linked immunosorbent assays of fibrillar (insoluble) unmodified Aβ40 and Aβ42 forms and N-terminus truncated and pyroglutamate-modified AβNpE3-40 and AβNpE3-42 forms in postmortem frontal cortex and precuneus samples from 18 DS cases aged 43–63 years and 17 late-onset AD cases aged 62–99 years. Both diagnostic groups had frequent neocortical neuritic plaques, while the DS group had more severe vascular amyloid pathology (cerebral amyloid angiopathy, CAA). Compared to the AD group, the DS group had higher levels of Aβ40 and AβNpE3-40, while the two groups did not differ by Aβ42 and AβNpE3-42 levels. This resulted in lower ratios of Aβ42/Aβ40 and AβNpE3-42/AβNpE3-40 in the DS group compared to the AD group. Correlations of Aβ42/Aβ40 and AβNpE3-42/AβNpE3-40 ratios with CAA severity were strong in DS cases and weak in AD cases. Pyroglutamate-modified Aβ levels were lower than unmodified Aβ levels in both diagnostic groups, but within group proportions of both pyroglutamate-modified Aβ forms relative to both unmodified Aβ forms were lower in the DS group but not in the AD group. The two diagnostic groups did not differ by 3H-PiB binding levels. These results demonstrate that compared to late-onset AD cases, adult DS individuals with similar severity of neocortical neuritic plaques and greater CAA pathology have a preponderance of both pyroglutamate-modified AβNpE3-40 and unmodified Aβ40 forms. Despite the distinct molecular profile of Aβ forms and greater vascular amyloidosis in DS cases, cortical 3H-PiB binding does not distinguish between diagnostic groups that are at an advanced level of amyloid plaque pathology. This underscores the need for the development of CAA-selective PET radiopharmaceuticals to detect and track the progression of cerebral vascular amyloid deposits in relation to Aβ plaques in individuals with DS.

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“…Several clinical cohorts in the US and Europe are working together to determine the best panels of blood biomarkers for adults with DS related to dementia. In Hendrix et al’s (2021) [ 4 ] paper, the Longitudinal Investigation for Enhancing Down Syndrome Research (LIFE-DSR) Study reported early findings from a natural history study of adults with DS in the USA. The LIFE-DSR study consists of 11 sites, who are collectively recruiting 270 individuals with DS over the age of 25.…”

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confidence: 99%

Aging in Down Syndrome: Latest Clinical Advances and Prospects

Martini

Alldred

Granholm

2021

JCM

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Cross-Sectional Exploration of Plasma Biomarkers of Alzheimer’s Disease in Down Syndrome: Early Data from the Longitudinal Investigation for Enhancing Down Syndrome Research (LIFE-DSR) Study

Cited by 20 publications

References 44 publications

Innate Immune System Activation and Neuroinflammation in Down Syndrome and Neurodegeneration: Therapeutic Targets or Partners?

Innate Immune System Activation and Neuroinflammation in Down Syndrome and Neurodegeneration: Therapeutic Targets or Partners?

Postmortem Neocortical 3H-PiB Binding and Levels of Unmodified and Pyroglutamate Aβ in Down Syndrome and Sporadic Alzheimer’s Disease

Aging in Down Syndrome: Latest Clinical Advances and Prospects

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