Mitochondrial DNA polymorphisms specifically modify cerebral β-amyloid proteostasis

Scheffler, Katja; Krohn, Markus; Dunkelmann, Tina; Stenzel, Jan; Miroux, Bruno; Ibrahim, Saleh M.; Halbach, Oliver von Bohlen und; Heinze, Hans‐Jochen; Walker, Lary C.; Gsponer, Jörg; Pahnke, Jens

doi:10.1007/s00401-012-0980-x

Cited by 54 publications

(47 citation statements)

References 39 publications

(49 reference statements)

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“…These findings add to evidence suggesting that impaired clearance of Aβ might be a crucial factor in sporadic Alzheimer disease-a view seconded at the meeting by data presented by Jens Pahnke (U. Magdeburg and DZNEMagdeburg, Germany), who showed that loss of ABC transporters B1 and C1, which extrude Aβ from the CNS parenchyma, can lead to a substantial increase in Aβ-load [24]. These transporters not only are regulated by mitochondria [25], but also have a substantial impact on cerebral regeneration [26]. Thus, future investigations into toxic protein aggregation will have to consider production, as well as clearance, and hence the homeostatic contributions of the immune system and tissue barriers, such as the neurovascular unit or the choroid plexus.…”

Section: Translation Meets Systems Medicinesupporting

confidence: 73%

Between new genetic discoveries and large randomized trials—neurological research in the era of systems medicine

2013

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The 2012 Eibsee meeting on ‘Cellular Mechanisms of Neurodegeneration’ addressed the need to integrate research on classical neurodegenerative mechanisms with investigations that relate to the immunological, glial and vascular sequels that accompany and often propagate neuronal injury. We report on the central topics that were addressed and discuss future directions towards establishing ‘systems neurology’ as a new integrated research field.

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Section: Translation Meets Systems Medicinesupporting

confidence: 73%

Between new genetic discoveries and large randomized trials—neurological research in the era of systems medicine

2013

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“…This functional activation is limited by a still unknown mechanism and leads to a 'hibernating' microglia species enclosed the growing amyloid deposits. The phagocytosis function is not only modulated by amyloid-beta but also by specific mitochondrial activity changes [34] that show a direct relation of cerebral ATP levels and microglia activity. A current report demonstrated that CCR2 deficiency in the transgenic mouse model of Alzheimer's disease provokes a rapid cognitive impairment closely correlated with brain amyloid pathology [35].…”

Section: Multiple Sclerosis Eae and Alzheimer's Diseasementioning

confidence: 99%

Monocytes in health and disease — Minireview

Karlmark

Tacke²,

Dunay³

2012

European Journal of Microbiology and Immunology

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“…Paraffi n-embedded, 4-μm-thick sections were deparaffi nized and conventionally stained with hematoxylin-eosin (H&E) stain. Immunohistochemical analysis was performed according to our previous publications [52][53][54][55][56][57][58] using a BOND-MAX (Leica Microsystems GmbH/Menarini, Germany) with antibodies against ionized calcium-binding adapter molecule 1 (IBA1, 1:2,000, Wako 019-19741, Germany) to label microglia, glialfi brillary acid protein (GFAP, 1:1,000, DAKO Z033401, Germany) to label astrocytes, myelinbasic protein (MBP, 1:1,600, DAKO A062301, Germany) to label myelin sheets, neurofi lament (NF200; 1:160, Sigma-Aldrich N4142-.5ML, Germany) to label axons, NeuN (1:1,000, Millipore MAB377, Germany) to label neurons, and anti-Toxo (1:200, Dianova DLN-16734, Germany) to label T. gondii. Slides were developed using the Bond™ Polymer Refi ne Detection kit (Menarini/Leica, Germany).…”

Section: Histopathologymentioning

confidence: 99%

Spinal cord pathology in chronic experimentalToxoplasma gondiiinfection

Möhle¹,

Parlog²,

Pahnke³

et al. 2014

European Journal of Microbiology and Immunology

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Infection with the protozoan Toxoplasma (T.) gondii causes chronic infection of the central nervous system and can lead to lifethreatening encephalomyelitis in immunocompromised patients. While infection with T. gondii has long time been considered asymptomatic in immunocompetent hosts, this view is challenged by recent reports describing links between seropositivity and behavioral alterations.However, past and current researches are mainly focused on the brain during Toxoplasma encephalitis, neglecting the spinal cord as a key structure conveying brain signals into motion. Therefore, our study aimed to fill the gap and describes the spinal cord pathology in an experimental murine model of toxoplasmosis.In the spinal cord, we found distinct histopathological changes, inflammatory foci and T. gondii cysts similar to the brain. Furthermore, the recruitment of immune cells from the periphery was detected. Moreover, resident microglia as well as recruited monocytes displayed an increased MHC classes I and II expression. Additionally, the expression of pro-and anti-inflammatory cytokines was enhanced in the brain as well as in the spinal cord. In summary, the pathology observed in the spinal cord was similar to the previously described changes in the brain during the infection.This study provides the first detailed description of histopathological and immunological alterations due to experimental T. gondii induced myelitis in mice. Thus, our comparison raises awareness of the importance of the spinal cord in chronic T. gondii infection.

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Mitochondrial DNA polymorphisms specifically modify cerebral β-amyloid proteostasis

Cited by 54 publications

References 39 publications

Between new genetic discoveries and large randomized trials—neurological research in the era of systems medicine

Between new genetic discoveries and large randomized trials—neurological research in the era of systems medicine

Monocytes in health and disease — Minireview

Spinal cord pathology in chronic experimentalToxoplasma gondiiinfection

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