Your search keyword '"Janina Mielke"' showing total 7 results

1. Generation and deposition of Aβ43 by the virtually inactive presenilin‐1 L435F mutant contradicts the presenilin loss‐of‐function hypothesis of Alzheimer's disease

Author

Benedikt Kretner, Johannes Trambauer, Akio Fukumori, Janina Mielke, Peer‐Hendrik Kuhn, Elisabeth Kremmer, Armin Giese, Stefan F Lichtenthaler, Christian Haass, Thomas Arzberger, and Harald Steiner

Subjects

Alzheimer's disease, amyloid‐β peptide 43, γ‐secretase, neurodegeneration, presenilin, Medicine (General), R5-920, Genetics, QH426-470

Abstract

Abstract As stated by the prevailing amyloid cascade hypothesis, Alzheimer's disease (AD) is caused by the aggregation and cerebral deposition of long amyloid‐β peptide (Aβ) species, which are released from a C‐terminal amyloid precursor protein fragment by γ‐secretase. Mutations in its catalytic subunit presenilin‐1 (PS1) increase the Aβ42 to Aβ40 ratio and are the major cause of familial AD (FAD). An opposing hypothesis states that loss of essential presenilin functions underlies the disease. A major argument for this hypothesis is the observation that the nearly inactive PS1 L435F mutant, paradoxically, causes FAD. We now show that the very little Aβ generated by PS1 L435F consists primarily of Aβ43, a highly amyloidogenic species which was overlooked in previous studies of this mutant. We further demonstrate that the generation of Aβ43 is not due to a trans‐dominant effect of this mutant on WT presenilin. Furthermore, we found Aβ43‐containing plaques in brains of patients with this mutation. The aberrant generation of Aβ43 by this particular mutant provides a direct objection against the presenilin hypothesis.

Published

2016

2. Substitutions of PrP N-terminal histidine residues modulate scrapie disease pathogenesis and incubation time in transgenic mice.

Author

Sabina Eigenbrod, Petra Frick, Uwe Bertsch, Gerda Mitteregger-Kretzschmar, Janina Mielke, Marko Maringer, Niklas Piening, Alexander Hepp, Nathalie Daude, Otto Windl, Johannes Levin, Armin Giese, Vignesh Sakthivelu, Jörg Tatzelt, Hans Kretzschmar, and David Westaway

Subjects

Medicine, Science

Abstract

Prion diseases have been linked to impaired copper homeostasis and copper induced-oxidative damage to the brain. Divalent metal ions, such as Cu2+ and Zn2+, bind to cellular prion protein (PrPC) at octapeptide repeat (OR) and non-OR sites within the N-terminal half of the protein but information on the impact of such binding on conversion to the misfolded isoform often derives from studies using either OR and non-OR peptides or bacterially-expressed recombinant PrP. Here we created new transgenic mouse lines expressing PrP with disrupted copper binding sites within all four histidine-containing OR's (sites 1-4, H60G, H68G, H76G, H84G, "TetraH>G" allele) or at site 5 (composed of residues His-95 and His-110; "H95G" allele) and monitored the formation of misfolded PrP in vivo. Novel transgenic mice expressing PrP(TetraH>G) at levels comparable to wild-type (wt) controls were susceptible to mouse-adapted scrapie strain RML but showed significantly prolonged incubation times. In contrast, amino acid replacement at residue 95 accelerated disease progression in corresponding PrP(H95G) mice. Neuropathological lesions in terminally ill transgenic mice were similar to scrapie-infected wt controls, but less severe. The pattern of PrPSc deposition, however, was not synaptic as seen in wt animals, but instead dense globular plaque-like accumulations of PrPSc in TgPrP(TetraH>G) mice and diffuse PrPSc deposition in (TgPrP(H95G) mice), were observed throughout all brain sections. We conclude that OR and site 5 histidine substitutions have divergent phenotypic impacts and that cis interactions between the OR region and the site 5 region modulate pathogenic outcomes by affecting the PrP globular domain.

Published

2017

3. Intramedullary pilomyxoid astrocytoma with intracerebral metastasis exhibiting oligodendroglioma-like features

Author

Sabina Eigenbrod, Niklas Thon, Nathalie Jansen, Hendrik Janssen, Janina Mielke, Michael Ruiter, Christian la Fougère, Aurelia Peraud, Rupert Egensperger, and Hans Kretzschmar

Subjects

Intramedullary glioma, pilomyxoid astrocytoma, metastasis, 1p19q, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282

Abstract

Intramedullary glioma are rare and their biological behaviour can differ from their cerebral counterparts. Pilomyxoid astrocytoma (PMA, WHO grade II), predominantly occur in the hypothalamic/chiasmatic region of infants and children. The few reported cases of pediatric intramedullary PMA displayed a particularly aggressive behavior. Here, we report a diagnostically challenging case of a five year old female patient presenting with intramedullary glioma and local tumor recurrence three years later. Twelve years after the initial manifestation, a second tumor was found intracerebrally. We performed a comprehensive histological, molecular pathological and imaging analysis of the tumors from both localizations. The results revealed a metastasizing PMA with unique histological and genetic features. Our study indicates that PMA comprise a heterogeneous group including aggressive subtypes which may not be compatible with the current classification according to WHO grade II. Furthermore, the case emphasizes the increasing relevance of molecular pathological markers complementing classic histological diagnosis.

Published

2012

4. Single-nucleus chromatin accessibility profiling highlights distinct astrocyte signatures in progressive supranuclear palsy and corticobasal degeneration

Author

Nils Briel, Viktoria C. Ruf, Katrin Pratsch, Sigrun Roeber, Jeannine Widmann, Janina Mielke, Mario M. Dorostkar, Otto Windl, Thomas Arzberger, Jochen Herms, and Felix L. Struebing

Subjects

pathology [Tauopathies], snATAC-seq, pathology [Supranuclear Palsy, Progressive], Progressive supranuclear palsy, Corticobasal degeneration, genetics [Tauopathies], tau Proteins, metabolism [tau Proteins], Chromatin, Pathology and Forensic Medicine, Cellular and Molecular Neuroscience, genetics [tau Proteins], Tauopathy, Corticobasal Degeneration, Tauopathies, Astrocytes, Humans, Neurology (clinical), ddc:610, Supranuclear Palsy, Progressive, Neurodegeneration, pathology [Astrocytes]

Abstract

Tauopathies such as progressive supranuclear palsy (PSP) and corticobasal degeneration (CBD) exhibit characteristic neuronal and glial inclusions of hyperphosphorylated Tau (pTau). Although the astrocytic pTau phenotype upon neuropathological examination is the most guiding feature in distinguishing both diseases, regulatory mechanisms controlling their transitions into disease-specific states are poorly understood to date. Here, we provide accessible chromatin data of more than 45,000 single nuclei isolated from the frontal cortex of PSP, CBD, and control individuals. We found a strong association of disease-relevant molecular changes with astrocytes and demonstrate that tauopathy-relevant genetic risk variants are tightly linked to astrocytic chromatin accessibility profiles in the brains of PSP and CBD patients. Unlike the established pathogenesis in the secondary tauopathy Alzheimer disease, microglial alterations were relatively sparse. Transcription factor (TF) motif enrichments in pseudotime as well as modeling of the astrocytic TF interplay suggested a common pTau signature for CBD and PSP that is reminiscent of an inflammatory immediate-early response. Nonetheless, machine learning models also predicted discriminatory features, and we observed marked differences in molecular entities related to protein homeostasis between both diseases. Predicted TF involvement was supported by immunofluorescence analyses in postmortem brain tissue for their highly correlated target genes. Collectively, our data expand the current knowledge on risk gene involvement (e.g., MAPT, MAPK8, and NFE2L2) and molecular pathways leading to the phenotypic changes associated with CBD and PSP.

Published

2022

5. Substitutions of PrP N-terminal histidine residues modulate scrapie disease pathogenesis and incubation time in transgenic mice

Author

Hans A. Kretzschmar, Marko Maringer, Nathalie Daude, Alexander Hepp, David Westaway, Gerda Mitteregger-Kretzschmar, Janina Mielke, Sabina Eigenbrod, Armin Giese, Petra Frick, Vignesh Sakthivelu, Jörg Tatzelt, Uwe Bertsch, Otto Windl, Niklas Piening, and Johannes Levin

Subjects

0301 basic medicine, Central Nervous System, animal diseases, lcsh:Medicine, Scrapie, Biochemistry, Nervous System, chemistry [Prion Proteins], law.invention, Animal Diseases, Prion Diseases, Mice, law, chemistry [Histidine], Zoonoses, Medicine and Health Sciences, Amino Acids, lcsh:Science, Brain Diseases, Multidisciplinary, Chemistry, Organic Compounds, Animal Models, Proteases, Phenotype, Enzymes, Animal Prion Diseases, Infectious Diseases, Experimental Organism Systems, Neurology, Physical Sciences, Recombinant DNA, Basic Amino Acids, Anatomy, Research Article, pathology [Scrapie], Gene isoform, Genetically modified mouse, Transgene, Mice, Transgenic, Mouse Models, Research and Analysis Methods, Prion Proteins, 03 medical and health sciences, Model Organisms, In vivo, Animals, Histidine, ddc:610, lcsh:R, Organic Chemistry, Chemical Compounds, Biology and Life Sciences, Proteins, Molecular biology, nervous system diseases, 030104 developmental biology, Enzymology, lcsh:Q, Zoology

Abstract

Prion diseases have been linked to impaired copper homeostasis and copper induced-oxidative damage to the brain. Divalent metal ions, such as Cu2+ and Zn2+, bind to cellular prion protein (PrPC) at octapeptide repeat (OR) and non-OR sites within the N-terminal half of the protein but information on the impact of such binding on conversion to the misfolded isoform often derives from studies using either OR and non-OR peptides or bacterially-expressed recombinant PrP. Here we created new transgenic mouse lines expressing PrP with disrupted copper binding sites within all four histidine-containing OR's (sites 1-4, H60G, H68G, H76G, H84G, 'TetraH>G' allele) or at site 5 (composed of residues His-95 and His-110; 'H95G' allele) and monitored the formation of misfolded PrP in vivo. Novel transgenic mice expressing PrP(TetraH>G) at levels comparable to wild-type (wt) controls were susceptible to mouse-adapted scrapie strain RML but showed significantly prolonged incubation times. In contrast, amino acid replacement at residue 95 accelerated disease progression in corresponding PrP(H95G) mice. Neuropathological lesions in terminally ill transgenic mice were similar to scrapie-infected wt controls, but less severe. The pattern of PrPSc deposition, however, was not synaptic as seen in wt animals, but instead dense globular plaque-like accumulations of PrPSc in TgPrP(TetraH>G) mice and diffuse PrPSc deposition in (TgPrP(H95G) mice), were observed throughout all brain sections. We conclude that OR and site 5 histidine substitutions have divergent phenotypic impacts and that cis interactions between the OR region and the site 5 region modulate pathogenic outcomes by affecting the PrP globular domain.

Published

2017

6. Generation and deposition of Aβ43 by the virtually inactive presenilin-1 L435F mutant contradicts the presenilin loss-of-function hypothesis of Alzheimer's disease

Author

Harald Steiner, Armin Giese, Thomas Arzberger, Christian Haass, Benedikt Kretner, Janina Mielke, Akio Fukumori, Elisabeth Kremmer, Peer-Hendrik Kuhn, Stefan F. Lichtenthaler, and Johannes Trambauer

Subjects

0301 basic medicine, Mutant, pathology [Frontal Lobe], Bioinformatics, medicine.disease_cause, pathology [Alzheimer Disease], 0302 clinical medicine, Amyloid precursor protein, presenilin, metabolism [Peptide Fragments], Mutation, Microscopy, biology, Chemistry, metabolism [Presenilin-1], Neurodegeneration, neurodegeneration, genetics [Presenilin-1], Alzheimer's disease, Immunohistochemistry, Frontal Lobe, Cell biology, amyloid‐β peptide 43, genetics [Mutant Proteins], Molecular Medicine, Amyloid, metabolism [Amyloid beta-Peptides], amyloid beta-protein (1-43), Presenilin, 03 medical and health sciences, PSEN1 protein, human, Alzheimer Disease, Report, mental disorders, medicine, Presenilin-1, Humans, ddc:610, metabolism [Mutant Proteins], Loss function, γ‐secretase, Amyloid beta-Peptides, medicine.disease, Peptide Fragments, nervous system diseases, 030104 developmental biology, biology.protein, Mutant Proteins, 030217 neurology & neurosurgery, Reports, Neuroscience

Abstract

As stated by the prevailing amyloid cascade hypothesis, Alzheimer's disease (AD) is caused by the aggregation and cerebral deposition of long amyloid‐β peptide (Aβ) species, which are released from a C‐terminal amyloid precursor protein fragment by γ‐secretase. Mutations in its catalytic subunit presenilin‐1 (PS1) increase the Aβ42 to Aβ40 ratio and are the major cause of familial AD (FAD). An opposing hypothesis states that loss of essential presenilin functions underlies the disease. A major argument for this hypothesis is the observation that the nearly inactive PS1 L435F mutant, paradoxically, causes FAD. We now show that the very little Aβ generated by PS1 L435F consists primarily of Aβ43, a highly amyloidogenic species which was overlooked in previous studies of this mutant. We further demonstrate that the generation of Aβ43 is not due to a trans‐dominant effect of this mutant on WT presenilin. Furthermore, we found Aβ43‐containing plaques in brains of patients with this mutation. The aberrant generation of Aβ43 by this particular mutant provides a direct objection against the presenilin hypothesis.

Published

2016

7. Intramedullary pilomyxoid astrocytoma with intracerebral metastasis exhibiting oligodendroglioma-like features

Author

Hendrik Janssen, Sabina Eigenbrod, Hans A. Kretzschmar, Christian la Fougère, Rupert Egensperger, Aurelia Peraud, Nathalie Jansen, Michael Ruiter, Janina Mielke, and Niklas Thon

Subjects

Pilomyxoid astrocytoma, Pathology, medicine.medical_specialty, Histology, Intramedullary glioma, Case Report, lcsh:RC254-282, law.invention, Metastasis, Intramedullary rod, law, Glioma, Female patient, medicine, metastasis, 1p19q, Pathological, Heterogeneous group, business.industry, medicine.disease, lcsh:Neoplasms. Tumors. Oncology. Including cancer and carcinogens, Tumor recurrence, Oncology, pilomyxoid astrocytoma, business

Abstract

Intramedullary glioma are rare and their biological behaviour can differ from their cerebral counterparts. Pilomyxoid astrocytoma (PMA, WHO grade II), predominantly occur in the hypothalamic/chiasmatic region of infants and children. The few reported cases of pediatric intramedullary PMA displayed a particularly aggressive behavior. Here, we report a diagnostically challenging case of a five year old female patient presenting with intramedullary glioma and local tumor recurrence three years later. Twelve years after the initial manifestation, a second tumor was found intracerebrally. We performed a comprehensive histological, molecular pathological and imaging analysis of the tumors from both localizations. The results revealed a metastasizing PMA with unique histological and genetic features. Our study indicates that PMA comprise a heterogeneous group including aggressive subtypes which may not be compatible with the current classification according to WHO grade II. Furthermore, the case emphasizes the increasing relevance of molecular pathological markers complementing classic histo-logical diagnosis.

Published

2012