Evaluation of Metabolic and Synaptic Dysfunction Hypotheses of Alzheimer's Disease (AD): A Meta-Analysis of CSF Markers

Manyevitch, Roni; Protas, Matthew; Scarpiello, Sean; Deliso, Marisa; Bass, Brittany; Nanajian, Anthony; Chang, Matthew; Thompson, Stefani; Khoury, Neil; Gonnella, Rachel A.; Trotz, Margit; Moore, D. Blaine; Harms, Emily; Perry, George; Clunes, Lucy A.; Ortiz, Angélica; Friedrich, Jan O.; Murray, Ian V.J.

doi:10.2174/1567205014666170921122458

Cited by 51 publications

(30 citation statements)

References 139 publications

(143 reference statements)

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“…The dual targeting of VEGFA and Ang2 was shown previously to increase M2 to M1-like skewing, which is indicative of a proinflammatory macrophage activation (22,24,25). In other studies, durable antitumor responses observed upon combining CD40 agonism with anti-CSF1R antibodies (36) or small-molecule CSF1R inhibitors (37,48) were attributed to the reduction of immunosuppressive M2-like TAMs and the simultaneous induction of polyfunctional inflammatory M1-like TAMs producing TNFα, IL-6, and IL-12. In our study, we observed a more pronounced effect on TAM depletion after anti-CD40 therapy in MC38 tumors compared to others (36).…”

Section: Discussionmentioning

confidence: 82%

Optimized antiangiogenic reprogramming of the tumor microenvironment potentiates CD40 immunotherapy

Kashyap

Schmittnaegel

Rigamonti

et al. 2019

Proc. Natl. Acad. Sci. U.S.A.

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Cancer immunotherapies are increasingly combined with targeted therapies to improve therapeutic outcomes. We show that combination of agonistic anti-CD40 with antiangiogenic antibodies targeting 2 proangiogenic factors, vascular endothelial growth factor A (VEGFA) and angiopoietin 2 (Ang2/ANGPT2), induces pleiotropic immune mechanisms that facilitate tumor rejection in several tumor models. On the one hand, VEGFA/Ang2 blockade induced regression of the tumor microvasculature while decreasing the proportion of nonperfused vessels and reducing leakiness of the remaining vessels. On the other hand, both anti-VEGFA/Ang2 and anti-CD40 independently promoted proinflammatory macrophage skewing and increased dendritic cell activation in the tumor microenvironment, which were further amplified upon combination of the 2 treatments. Finally, combined therapy provoked brisk infiltration and intratumoral redistribution of cytotoxic CD8+T cells in the tumors, which was mainly driven by Ang2 blockade. Overall, these nonredundant synergistic mechanisms endowed T cells with improved effector functions that were conducive to more efficient tumor control, underscoring the therapeutic potential of antiangiogenic immunotherapy in cancer.

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Section: Discussionmentioning

confidence: 82%

Optimized antiangiogenic reprogramming of the tumor microenvironment potentiates CD40 immunotherapy

Kashyap

Schmittnaegel

Rigamonti

et al. 2019

Proc. Natl. Acad. Sci. U.S.A.

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“…al [63] found that increasing CLPTM1 levels decreased miniature inhibitory postsynaptic potentials, while reciprocally, decreasing CLPTM1 levels elevated GABA currents in the post-synaptic neuron, strongly suggesting that CLPTM1 negatively regulates GABAergic signaling. A recent literature meta-analysis looking at neurotransmitter synaptic dysregulation in AD, found decreased levels GABA in AD patients, supporting the potential dysregulation of GABAergic signaling in AD [65] Far less is known about CEACAM19, and any biological connection to AD. What work has been done is predominantly focused upon oncology.…”

Section: Apoc1 -Ceacam19 -Clptm1 Chr19mentioning

confidence: 97%

Multi-Tissue Neocortical Transcriptome-Wide Association Study Implicates 8 Genes Across 6 Genomic Loci in Alzheimer’s Disease

Gockley

Montgomery

Poehlman

et al. 2020

Preprint

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AbstractBackgroundAlzheimer’s disease (AD), an incurable neurodegenerative disease, currently affecting 1.75% of the United States population, with projected growth to 3.46% by 2050. Identifying common genetic variants driving differences in transcript expression that confer AD-risk is necessary to elucidate AD mechanism and develop therapeutic interventions. We modify the FUSION Transcriptome Wide Association Study (TWAS) pipeline to ingest expression from multiple neocortical regions, provide a set of 6780 gene weights which are abstracatable across the neocortex, and leverage these to find 8 genes from six loci with associated AD risk validated through summary mendelian randomization (SMR) utilizing IGAP summary statistics.MethodA combined dataset of 2003 genotypes clustered to Central European (CEU) ancestry was used to construct a training set of 790 genotypes paired to 888 RNASeq profiles across 6 Neo-cortical tissues (TCX=248, FP=50, IFG=41, STG=34, PHG=34, DLPFC=461). Following within-tissue normalization and covariate adjustment, predictive weights to impute expression components based on a gene’s surrounding cis-variants were trained. The FUSION pipeline was modified to support input of pre-scaled expression values and provide support for cross validation with a repeated measure design arising from the presence of multiple transcriptome samples from the same individual across different tissues.ResultsCis-variant architecture alone was informative to train weights and impute expression for 6780 (49.67%) autosomal genes, the majority of which significantly correlated with gene expression; FDR < 5%: N=6775 (99.92%), Bonferroni: N=6716 (99.06%). Validation of weights in 515 matched genotype to RNASeq profiles from the CommonMind Consortium (CMC) was (72.14%) in DLPFC profiles. Association of imputed expression components from all 2003 genotype profiles yielded 8 genes significantly associated with AD (FDR < 0.05); APOC1, EED, CD2AP, CEACAM19, CLPTM1, MTCH2, TREM2, KNOP1.ConclusionWe provide evidence of cis-genetic variation conferring AD risk through 8 genes across six distinct genomic loci. Moreover, we provide expression weights for 6780 genes as a valuable resource to the community, which can be abstracted across the neocortex and a wide range of neuronal phenotypes.

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“…Some authors reported higher CSF glutamate values in AD patients than in controls [42,43], whereas others reported decreased values [44,45] or no changes at all [46][47][48]. A recent study using C13-glutamine performed in APP/PS1 mice suggests that reduced glutamine uptake and impaired oxidative glutamine metabolism could be very early markers of AD pathogenesis, as they precede the amyloid plaque formation in this model [49]. This hypothesis may be plausible in the rTg4510 mouse of the AD model at an early pathological stage.…”

Section: Discussionmentioning

confidence: 87%

Altered Brain Metabolome Is Associated with Memory Impairment in the rTg4510 Mouse Model of Tauopathy

et al. 2020

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Alzheimer’s disease (AD) is characterized, amongst other features, by the pathologic accumulation of abnormally phosphorylated tau filaments in neurons that lead to neurofibrillary tangles. However, the molecular mechanisms by which the abnormal processing of tau leads to neurodegeneration and cognitive impairment remain unknown. Metabolomic techniques can comprehensively assess disturbances in metabolic pathways that reflect changes downstream from genomic, transcriptomic and proteomic systems. In the present study, we undertook a targeted metabolomic approach to determine a total of 187 prenominated metabolites in brain cortex tissue from wild type and rTg4510 animals (a mice model of tauopathy), in order to establish the association of metabolic pathways with cognitive impairment. This targeted metabolomic approach revealed significant differences in metabolite concentrations of transgenic mice. Brain glutamine, serotonin and sphingomyelin C18:0 were found to be predictors of memory impairment. These findings provide informative data for future research on AD, since some of them agree with pathological alterations observed in diseased humans.

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Evaluation of Metabolic and Synaptic Dysfunction Hypotheses of Alzheimer's Disease (AD): A Meta-Analysis of CSF Markers

Cited by 51 publications

References 139 publications

Optimized antiangiogenic reprogramming of the tumor microenvironment potentiates CD40 immunotherapy

Optimized antiangiogenic reprogramming of the tumor microenvironment potentiates CD40 immunotherapy

Multi-Tissue Neocortical Transcriptome-Wide Association Study Implicates 8 Genes Across 6 Genomic Loci in Alzheimer’s Disease

Altered Brain Metabolome Is Associated with Memory Impairment in the rTg4510 Mouse Model of Tauopathy

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