Medin co-aggregates with vascular amyloid-β in Alzheimer’s disease

Wagner, Jessica; Degenhardt, Karoline; Veit, Marleen; Louros, Nikolaos; Konstantoulea, Katerina; Skodras, Angelos; Wild, Katharina; Liu, Ping; Obermüller, Ulrike; Bansal, V.; Dalmia, Anupriya; Häsler, Lisa M.; Lambert, Marius; Vleeschouwer, Matthias De; Davies, Hannah A.; Madine, Jillian; Kronenberg‐Versteeg, Deborah; Feederle, Regina; Turco, Domenico Del; Nilsson, K. Peter R.; Lashley, Tammaryn; Deller, Thomas; Gearing, Marla; Walker, Lary C.; Heutink, Peter; Rousseau, Frédéric; Schymkowitz, Joost; Jucker, Mathias; Neher, Jonas J.

doi:10.1038/s41586-022-05440-3

Cited by 42 publications

(36 citation statements)

References 76 publications

(116 reference statements)

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“…We performed spatial ATAC–RNA-seq on adult (31-year-old male) human brain hippocampal formation, which is a complex brain region involved in cognitive functions and diseases such as major depression disease 40 and Alzheimer’s disease 41 . We identified seven and eight major clusters for ATAC and RNA, respectively, and the spatial pattern agreed with major anatomical landmarks (Fig.…”

Section: Spatial Comapping Of Human Brainmentioning

confidence: 99%

Spatial epigenome–transcriptome co-profiling of mammalian tissues

Zhang

Deng

Kukanja

et al. 2023

Nature

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Emerging spatial technologies, including spatial transcriptomics and spatial epigenomics, are becoming powerful tools for profiling of cellular states in the tissue context1–5. However, current methods capture only one layer of omics information at a time, precluding the possibility of examining the mechanistic relationship across the central dogma of molecular biology. Here, we present two technologies for spatially resolved, genome-wide, joint profiling of the epigenome and transcriptome by cosequencing chromatin accessibility and gene expression, or histone modifications (H3K27me3, H3K27ac or H3K4me3) and gene expression on the same tissue section at near-single-cell resolution. These were applied to embryonic and juvenile mouse brain, as well as adult human brain, to map how epigenetic mechanisms control transcriptional phenotype and cell dynamics in tissue. Although highly concordant tissue features were identified by either spatial epigenome or spatial transcriptome we also observed distinct patterns, suggesting their differential roles in defining cell states. Linking epigenome to transcriptome pixel by pixel allows the uncovering of new insights in spatial epigenetic priming, differentiation and gene regulation within the tissue architecture. These technologies are of great interest in life science and biomedical research.

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Section: Spatial Comapping Of Human Brainmentioning

confidence: 99%

Spatial epigenome–transcriptome co-profiling of mammalian tissues

Zhang

Deng

Kukanja

et al. 2023

Nature

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“…Cerebral amyloid angiopathy (CAA) is a prevalent pathology in amyloidosis. Eight amyloid proteins, Aβ, ATTR, ADan, ABri, ACys, APrP, AGel, AMed [ 159 , 160 ] ( Table 1 ), are known to form amyloid in CAA and can cause vascular dementia. These vascular deposits are associated with accumulation of ApoE, Serum amyloid p component (SAP) and glycosaminoglycans (GAGs) which are amyloid associated proteins and glycans [ 161 ] which together severely impairs the vasculature increasing the risk for haemorrhagic stroke.…”

Section: Covid-19 Sequelae With Similarities and Possible Connections...mentioning

confidence: 99%

Viruses and amyloids - a vicious liaison

Hammarström

Nyström

2023

Prion

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The crosstalk between viral infections, amyloid formation and neurodegeneration has been discussed with varying intensity since the last century. Several viral proteins are known to be amyloidogenic. Post-acute sequalae (PAS) of viral infections is known for several viruses. SARS-CoV-2 and COVID-19 implicate connections between amyloid formation and severe outcomes in the acute infection, PAS and neurodegenerative diseases. Is the amyloid connection causation or just correlation? In this review we highlight several aspects where amyloids and viruses meet. The evolutionary driving forces that dictate protein amyloid formation propensity are different for viruses compared to prokaryotes and eukaryotes, while posttranslational endoproteolysis appears to be a common mechanism leading up to amyloid formation for both viral and human proteins. Not only do human and viral proteins form amyloid irrespective of each other but there are also several examples of co-operativity between amyloids, viruses and the inter-, and intra-host spread of the respective entity. Abnormal blood clotting in severe and long COVID and as a side effect in some vaccine recipients has been connected to amyloid formation of both the human fibrin and the viral Spike-protein. We conclude that there are many intersects between viruses and amyloids and, consequently, amyloid and virus research need to join forces here. We emphasize the need to accelerate development and implementation in clinical practice of antiviral drugs to preclude PAS and downstream neurological damage. There is also an ample need for retake on suitable antigen targets for the further development of next generation of vaccines against the current and coming pandemics.

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“…On the contrary, medin, a known protein, promotes the formation of amyloid aggregates and deposits by coaggregation with Aβ. Researchers hope that medin inhibitors could block the formation of amyloid deposits and may behave as anti-amyloid agents [ 133 ]. It has been published very recently that 14-3-3 proteins also bind amyloids, and thus, they can also be targeted as an anti-aggregation approach [ 134 ].…”

Section: Conventional and Novel Targets For Slowing And/or Preventing...mentioning

confidence: 99%

New Pathways Identify Novel Drug Targets for the Prevention and Treatment of Alzheimer’s Disease

Penke

Szücs

Bogár³

2023

IJMS

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Alzheimer’s disease (AD) is an incurable, progressive neurodegenerative disorder. AD is a complex and multifactorial disease that is responsible for 60–80% of dementia cases. Aging, genetic factors, and epigenetic changes are the main risk factors for AD. Two aggregation-prone proteins play a decisive role in AD pathogenesis: β-amyloid (Aβ) and hyperphosphorylated tau (pTau). Both of them form deposits and diffusible toxic aggregates in the brain. These proteins are the biomarkers of AD. Different hypotheses have tried to explain AD pathogenesis and served as platforms for AD drug research. Experiments demonstrated that both Aβ and pTau might start neurodegenerative processes and are necessary for cognitive decline. The two pathologies act in synergy. Inhibition of the formation of toxic Aβ and pTau aggregates has been an old drug target. Recently, successful Aβ clearance by monoclonal antibodies has raised new hopes for AD treatments if the disease is detected at early stages. More recently, novel targets, e.g., improvements in amyloid clearance from the brain, application of small heat shock proteins (Hsps), modulation of chronic neuroinflammation by different receptor ligands, modulation of microglial phagocytosis, and increase in myelination have been revealed in AD research.

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Medin co-aggregates with vascular amyloid-β in Alzheimer’s disease

Cited by 42 publications

References 76 publications

Spatial epigenome–transcriptome co-profiling of mammalian tissues

Spatial epigenome–transcriptome co-profiling of mammalian tissues

Viruses and amyloids - a vicious liaison

New Pathways Identify Novel Drug Targets for the Prevention and Treatment of Alzheimer’s Disease

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