Your search keyword '"Meine Ramakers"' showing total 3 results

1. Heterotypic Amyloid beta interactions facilitate amyloid assembly and modify amyloid structure

Author

Emiel Michiels, Patricia Guerreiro, Yulia Lampi, Frederic Rousseau, Bert Houben, Joris de Wit, Meine Ramakers, Katerina Konstantoulea, Luís Ribeiro, Liam D. Aubrey, Nikolaos N. Louros, Joost Schymkowitz, Wei-Feng Xue, and Matthias De Vleeschouwer

Subjects

Biochemistry & Molecular Biology, Proteome, Amyloid, Amyloid β, ALPHA-SYNUCLEIN, Amyloid beta, PROPAGATION, Proteomics, General Biochemistry, Genetics and Molecular Biology, FORCE, Homologous chromosome, Humans, Protein Interaction Maps, Molecular Biology, SPECIFICITY, A-BETA, Amyloid beta-Peptides, Science & Technology, General Immunology and Microbiology, biology, General Neuroscience, toxicity, Articles, Cell Biology, Alzheimer's disease, SEQUENCE DETERMINANTS, In vitro, Cell biology, amyloid beta, ALZHEIMERS-DISEASE, PATHOLOGY, HEK293 Cells, heterotypic aggregation, Cell culture, biology.protein, Aβ amyloid, Protein Multimerization, QP517, TAU, PROTEIN AGGREGATION, Life Sciences & Biomedicine, Protein Binding

Abstract

It is still unclear why pathological amyloid deposition initiates in specific brain regions or why some cells or tissues are more susceptible than others. Amyloid deposition is determined by the self-assembly of short protein segments called aggregation-prone regions (APRs) that favour cross-β structure. Here, we investigated whether Aβ amyloid assembly can be modified by heterotypic interactions between Aβ APRs and short homologous segments in otherwise unrelated human proteins. Mining existing proteomics data of Aβ plaques from AD patients revealed an enrichment in proteins that harbour such homologous sequences to the Aβ APRs, suggesting heterotypic amyloid interactions may occur in patients. We identified homologous APRs from such proteins and show that they can modify Aβ assembly kinetics, fibril morphology and deposition pattern in vitro. Moreover, we found three of these proteins upon transient expression in an Aβ reporter cell line promote Aβ amyloid aggregation. Strikingly, we did not find a bias towards heterotypic interactions in plaques from AD mouse models where Aβ self-aggregation is observed. Based on these data, we propose that heterotypic APR interactions may play a hitherto unrealized role in amyloid-deposition diseases. ispartof: EMBO JOURNAL vol:41 issue:2 ispartof: location:England status: published

Published

2022

2. Protein aggregation as an antibiotic design strategy

Author

Isabel Vogel, Rodrigo Gallardo, Johan Van Eldere, An Staes, Natalia G. Bednarska, Marc Goethals, Pieter Baatsen, Kris Gevaert, Meine Ramakers, Frederic Rousseau, Joost Schymkowitz, Ashok Ganesan, Per Hammarström, and K. Peter R. Nilsson

Subjects

0301 basic medicine, biology, Antimicrobial peptides, Bacterial genome size, Protein aggregation, Staphylococcal infections, medicine.disease, Antimicrobial, biology.organism_classification, Microbiology, 3. Good health, 03 medical and health sciences, 030104 developmental biology, Biochemistry, Chaperone (protein), medicine, biology.protein, Molecular Biology, Bacterial morphological plasticity, Bacteria

Abstract

Taking advantage of the xenobiotic nature of bacterial infections, we tested whether the cytotoxicity of protein aggregation can be targeted to bacterial pathogens without affecting their mammalian hosts. In particular, we examined if peptides encoding aggregation-prone sequence segments of bacterial proteins can display antimicrobial activity by initiating toxic protein aggregation in bacteria, but not in mammalian cells. Unbiased in vitro screening of aggregating peptide sequences from bacterial genomes lead to the identification of several peptides that are strongly bactericidal against methicillin-resistant Staphylococcus aureus. Upon parenteral administration in vivo, the peptides cured mice from bacterial sepsis without apparent toxic side effects as judged from histological and hematological evaluation. We found that the peptides enter and accumulate in the bacterial cytosol where they cause aggregation of bacterial polypeptides. Although the precise chain of events that leads to cell death remains to be elucidated, the ability to tap into aggregation-prone sequences of bacterial proteomes to elicit antimicrobial activity represents a rich and unexplored chemical space to be mined in search of novel therapeutic strategies to fight infectious diseases.

Published

2015

3. Inflammation-Induced Downregulation of Butyrate Uptake and Oxidation Is Not Caused by a Reduced Gene Expression

Author

Vicky De Preter, Ingrid Arijs, Frans Schuit, Wiebe Vanhove, Kristin Verbeke, Meine Ramakers, Paul Rutgeerts, Leen Boesmans, and Karen Windey

Subjects

Physiology, Chemistry, Clinical Biochemistry, Inflammation, Cell Biology, Butyrate, medicine.disease, Molecular biology, Biochemistry, Downregulation and upregulation, Gene expression, medicine, Tumor necrosis factor alpha, Interleukin 8, medicine.symptom, Incubation, Cell damage

Abstract

In ulcerative colitis (UC) the butyrate metabolism is impaired, leading to energy-deficiency in the colonic cells. The effect of inflammation on the butyrate metabolism was investigated. HT-29 cells were incubated with pro-inflammatory cytokines (TNF-α and/or IFN-γ) for 1 and 24 h. Cells were additionally stimulated with butyrate to investigate its anti-inflammatory potential. Butyrate uptake and oxidation were measured using 14C-labeled butyrate. Gene expression of the butyrate metabolism enzymes, interleukin 8 (IL-8; inflammatory marker) and villin-1 (VIL-1; epithelial cell damage marker) was measured via quantitative RT-PCR. Significantly increased IL-8 expression and decreased VIL-1 expression after 24 h incubation with TNF-α and/or IFN-γ confirmed the presence of inflammation. These conditions induced a decrease of both butyrate uptake and oxidation, whereas the gene expression was not reduced. Simultaneous incubation with butyrate counteracted the reduced butyrate oxidation. In contrast, 1 h incubation with TNF-α induced a significant increased IL-8 expression and decreased butyrate uptake. Incubation with TNF-α and/or IFN-γ for 1 h did not induce cell damage nor influence butyrate oxidation. The inflammation-induced downregulation of the butyrate metabolism was not caused by a reduced gene expression, but appeared consequential to a decreased butyrate uptake. Increasing the luminal butyrate levels might have therapeutic potential in UC. J. Cell. Physiol. 230: 418–426, 2015. © 2014 Wiley Periodicals, Inc.

Published

2014