Aggregates of RNA Binding Proteins and ER Chaperones Linked to Exosomes in Granulovacuolar Degeneration of the Alzheimer’s Disease Brain

Yamoah, Alfred; Tripathi, Priyanka; Sechi, Antonio; Köhler, Christoph; Guo, Haihong; Chandrasekar, Akila; Nolte, Kay; Wruck, Christoph Jan; Katona, István; Anink, Jasper J.; Troost, Dirk; Aronica, Eleonora; Steinbusch, Harry W.M.; Weis, Joachim; Goswami, Anand

doi:10.3233/jad-190722

Cited by 23 publications

(37 citation statements)

References 90 publications

(125 reference statements)

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“…Furthermore, a higher GVB load is found in bigenic TAPP mice that express both human tau P301L and human mutant amyloid precursor protein (APP) K670M/N671L (APP Sw ) compared to JNPL3 mice carrying only the human tau P301L transgene [54,78] (Table 2). This higher GVB frequency is likely related to the exacerbated tau pathology in TAPP mice rather than the comorbid Aβ pathology, as GVBs are absent in mouse models of pure Aβ amyloidosis by overexpression of APP Sw (Tg2576), APP Sw,Ind (J20), APP Sw/L /PS1 M146L or APP Sw /PS1 dE9 [54,67,90] although the recent detection of granular structures with an immunogenicity profile that partially overlaps with GVBs in APP Sw /PS1 dE9 mice requires further investigation [148]. Taken together, the data indicate that neither in human nor in Tg mouse brain, GVBs and extracellular Aβ pathology are associated.…”

Section: Table 2 Putative Gvb Observations In Experimental Models Andmentioning

confidence: 99%

“…A few studies have reported GVBs in tau transgenic (Tg) mouse models. GVBs are found in the brains of aged tau Tg mice expressing human mutant tau – more specifically, in mice from the strains JNPL3 [ 54 , 78 ] and pR5 [ 64 , 66 , 67 , 90 , 148 ] expressing human tau P301L (Table 2 ). In contrast, GVBs are not or only rarely found in age-matched non-Tg littermates [ 54 , 64 , 66 , 67 , 90 ].…”

Section: Gvbs As Pathological Companion Of Tau Pathologymentioning

confidence: 99%

“…The Thal GVD neuropathological staging system [132] is based on immunopositivity for CK1δ and CK1ε and in addition pTDP-43 [59]. pTDP-43 localizes to structures that morphologically resemble GVBs in the human [59,79,132] and mouse brain [148], but has so far not been tested in the in vitro GVB model. pTDP-43 staining in tissue overlaps with CK1δ-and CK1ε-immunolabeled GVBs [132,148], although the co-localization was not quantified.…”

mentioning

confidence: 99%

“…pTDP-43 localizes to structures that morphologically resemble GVBs in the human [59,79,132] and mouse brain [148], but has so far not been tested in the in vitro GVB model. pTDP-43 staining in tissue overlaps with CK1δ-and CK1ε-immunolabeled GVBs [132,148], although the co-localization was not quantified. However, in the human brain the distribution pattern of GVBs is similar when determining the Thal GVD stage using CK1δ, CK1ε or pTDP-43 [132].…”

mentioning

confidence: 99%

“…1 a-d) and CK1ε [ 33 , 67 , 143 ], CHMP2B [ 90 , 143 , 147 ], pPERK (Fig. 1 c-f), peIF2α and pIRE1α [ 43 , 67 , 143 ] and pTDP-43 [ 47 , 59 , 79 , 148 ]. In Supplementary Table 1 , an overview of primary antibodies used to detect these common GVB markers in tissue and culture is provided.…”

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confidence: 99%

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Untangling the origin and function of granulovacuolar degeneration bodies in neurodegenerative proteinopathies

Wiersma

Hoozemans

Scheper

2020

acta neuropathol commun

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In the brains of tauopathy patients, tau pathology coincides with the presence of granulovacuolar degeneration bodies (GVBs) both at the regional and cellular level. Recently, it was shown that intracellular tau pathology causes GVB formation in experimental models thus explaining the strong correlation between these neuropathological hallmarks in the human brain. These novel models of GVB formation provide opportunities for future research into GVB biology, but also urge reevaluation of previous post-mortem observations. Here, we review neuropathological data on GVBs in tauopathies and other neurodegenerative proteinopathies. We discuss the possibility that intracellular aggregates composed of proteins other than tau are also able to induce GVB formation. Furthermore, the potential mechanisms of GVB formation and the downstream functional implications hereof are outlined in view of the current available data. In addition, we provide guidelines for the identification of GVBs in tissue and cell models that will help to facilitate and streamline research towards the elucidation of the role of these enigmatic and understudied structures in neurodegeneration.

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Section: Table 2 Putative Gvb Observations In Experimental Models Andmentioning

confidence: 99%

Section: Gvbs As Pathological Companion Of Tau Pathologymentioning

confidence: 99%

mentioning

confidence: 99%

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confidence: 99%

mentioning

confidence: 99%

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Untangling the origin and function of granulovacuolar degeneration bodies in neurodegenerative proteinopathies

Wiersma

Hoozemans

Scheper

2020

acta neuropathol commun

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PolyGA targets the ER stress-adaptive response by impairing GRP75 function at the MAM in C9ORF72-ALS/FTD

et al. 2022

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ER stress signaling is linked to the pathophysiological and clinical disease manifestations in amyotrophic lateral sclerosis (ALS). Here, we have investigated ER stress-induced adaptive mechanisms in C9ORF72-ALS/FTD, focusing on uncovering early endogenous neuroprotective mechanisms and the crosstalk between pathological and adaptive responses in disease onset and progression. We provide evidence for the early onset of ER stress-mediated adaptive response in C9ORF72 patient-derived motoneurons (MNs), reflected by the elevated increase in GRP75 expression. These transiently increased GRP75 levels enhance ER–mitochondrial association, boosting mitochondrial function and sustaining cellular bioenergetics during the initial stage of disease, thereby counteracting early mitochondrial deficits. In C9orf72 rodent neurons, an abrupt reduction in GRP75 expression coincided with the onset of UPR, mitochondrial dysfunction and the emergence of PolyGA aggregates, which co-localize with GRP75. Similarly, the overexpression of PolyGA in WT cortical neurons or C9ORF72 patient-derived MNs led to the sequestration of GRP75 within PolyGA inclusions, resulting in mitochondrial calcium (Ca2+) uptake impairments. Corroborating these findings, we found that PolyGA aggregate-bearing human post-mortem C9ORF72 hippocampal dentate gyrus neurons not only display reduced expression of GRP75 but also exhibit GRP75 sequestration within inclusions. Sustaining high GRP75 expression in spinal C9orf72 rodent MNs specifically prevented ER stress, normalized mitochondrial function, abrogated PolyGA accumulation in spinal MNs, and ameliorated ALS-associated behavioral phenotype. Taken together, our results are in line with the notion that neurons in C9ORF72-ALS/FTD are particularly susceptible to ER–mitochondrial dysfunction and that GRP75 serves as a critical endogenous neuroprotective factor. This neuroprotective pathway, is eventually targeted by PolyGA, leading to GRP75 sequestration, and its subsequent loss of function at the MAM, compromising mitochondrial function and promoting disease onset.

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Loss of PML nuclear bodies in familial amyotrophic lateral sclerosis-frontotemporal dementia

Antoniani,

Cimino,

Mediani

et al. 2023

Cell Death Discov.

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Amyotrophic Lateral Sclerosis (ALS) and Frontotemporal Dementia (FTD) are two neurodegenerative disorders that share genetic causes and pathogenic mechanisms. The critical genetic players of ALS and FTD are the TARDBP, FUS and C9orf72 genes, whose protein products, TDP-43, FUS and the C9orf72-dipeptide repeat proteins, accumulate in form of cytoplasmic inclusions. The majority of the studies focus on the understanding of how cells control TDP-43 and FUS aggregation in the cytoplasm, overlooking how dysfunctions occurring at the nuclear level may influence the maintenance of protein solubility outside of the nucleus. However, protein quality control (PQC) systems that maintain protein homeostasis comprise a cytoplasmic and a nuclear arm that are interconnected and share key players. It is thus conceivable that impairment of the nuclear arm of the PQC may have a negative impact on the cytoplasmic arm of the PQC, contributing to the formation of the cytoplasmic pathological inclusions. Here we focused on two stress-inducible condensates that act as transient deposition sites for misfolding-prone proteins: Promyelocytic leukemia protein (PML) nuclear bodies (PML-NBs) and cytoplasmic stress granules (SGs). Upon stress, PML-NBs compartmentalize misfolded proteins, including defective ribosomal products (DRiPs), and recruit chaperones and proteasomes to promote their nuclear clearance. SGs transiently sequester aggregation-prone RNA-binding proteins linked to ALS-FTD and mRNAs to attenuate their translation. We report that PML assembly is impaired in the human brain and spinal cord of familial C9orf72 and FUS ALS-FTD cases. We also show that defective PML-NB assembly impairs the compartmentalization of DRiPs in the nucleus, leading to their accumulation inside cytoplasmic SGs, negatively influencing SG dynamics. Although it is currently unclear what causes the decrease of PML-NBs in ALS-FTD, our data highlight the existence of a cross-talk between the cytoplasmic and nuclear PQC systems, whose alteration can contribute to SG accumulation and cytoplasmic protein aggregation in ALS-FTD.

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Aggregates of RNA Binding Proteins and ER Chaperones Linked to Exosomes in Granulovacuolar Degeneration of the Alzheimer’s Disease Brain

Cited by 23 publications

References 90 publications

Untangling the origin and function of granulovacuolar degeneration bodies in neurodegenerative proteinopathies

Untangling the origin and function of granulovacuolar degeneration bodies in neurodegenerative proteinopathies

PolyGA targets the ER stress-adaptive response by impairing GRP75 function at the MAM in C9ORF72-ALS/FTD

Loss of PML nuclear bodies in familial amyotrophic lateral sclerosis-frontotemporal dementia

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