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19 results on '"Henke, Nadine"'

1. Activation-induced cytidine deaminase acts as a mutator in BCR-ABL1–transformed acute lymphoblastic leukemia cells

Author

Feldhahn, Niklas, Henke, Nadine, Melchior, Kai, Duy, Cihangir, Soh, Bonaventure Ndikung, Klein, Florian, von Levetzow, Gregor, Giebel, Bernd, Li, Aihong, Hofmann, Wolf-Karsten, Jumaa, Hassan, and Müschen, Markus

Subjects
Pediatric, Genetics, Childhood Leukemia, Pediatric Research Initiative, Cancer, Hematology, Pediatric Cancer, Rare Diseases, 2.1 Biological and endogenous factors, Aetiology, B-Lymphocytes, Base Sequence, Blotting, Western, Cytidine Deaminase, DNA Mutational Analysis, DNA-Binding Proteins, Flow Cytometry, Fusion Proteins, bcr-abl, Gene Expression Regulation, Neoplastic, Genes, myc, Humans, Immunoglobulin Variable Region, Molecular Sequence Data, Mutation, Oligonucleotide Array Sequence Analysis, Oligonucleotides, Philadelphia Chromosome, Precursor Cell Lymphoblastic Leukemia-Lymphoma, Protein-Tyrosine Kinases, Proto-Oncogene Proteins c-bcl-6, RNA Interference, Reverse Transcriptase Polymerase Chain Reaction, Sequence Alignment, Medical and Health Sciences, Immunology
Abstract

The Philadelphia chromosome (Ph) encoding the oncogenic BCR-ABL1 kinase defines a subset of acute lymphoblastic leukemia (ALL) with a particularly unfavorable prognosis. ALL cells are derived from B cell precursors in most cases and typically carry rearranged immunoglobulin heavy chain (IGH) variable (V) region genes devoid of somatic mutations. Somatic hypermutation is restricted to mature germinal center B cells and depends on activation-induced cytidine deaminase (AID). Studying AID expression in 108 cases of ALL, we detected AID mRNA in 24 of 28 Ph(+) ALLs as compared with 6 of 80 Ph(-) ALLs. Forced expression of BCR-ABL1 in Ph(-) ALL cells and inhibition of the BCR-ABL1 kinase showed that aberrant expression of AID depends on BCR-ABL1 kinase activity. Consistent with aberrant AID expression in Ph(+) ALL, IGH V region genes and BCL6 were mutated in many Ph(+) but unmutated in most Ph(-) cases. In addition, AID introduced DNA single-strand breaks within the tumor suppressor gene CDKN2B in Ph(+) ALL cells, which was sensitive to BCR-ABL1 kinase inhibition and silencing of AID expression by RNA interference. These findings identify AID as a BCR-ABL1-induced mutator in Ph(+) ALL cells, which may be relevant with respect to the particularly unfavorable prognosis of this leukemia subset.

Published
2007

7. Effects of dimethyl fumarate on neuroprotection and immunomodulation

Author

Albrecht Philipp, Bouchachia Imane, Goebels Norbert, Henke Nadine, Hofstetter Harald H, Issberner Andrea, Kovacs Zsuzsa, Lewerenz Jan, Lisak Dmitrij, Maher Pamela, Mausberg Anne-Kathrin, Quasthoff Kim, Zimmermann Corinna, Hartung Hans-Peter, and Methner Axel

Subjects
Dimethyl fumarate, Oxidative stress, Neuroprotection, Neuromodulation, Neurology. Diseases of the nervous system, RC346-429
Abstract

Abstract Background Neuronal degeneration in multiple sclerosis has been linked to oxidative stress. Dimethyl fumarate is a promising novel oral therapeutic option shown to reduce disease activity and progression in patients with relapsing-remitting multiple sclerosis. These effects are presumed to originate from a combination of immunomodulatory and neuroprotective mechanisms. We aimed to clarify whether neuroprotective concentrations of dimethyl fumarate have immunomodulatory effects. Findings We determined time- and concentration-dependent effects of dimethyl fumarate and its metabolite monomethyl fumarate on viability in a model of endogenous neuronal oxidative stress and clarified the mechanism of action by quantitating cellular glutathione content and recycling, nuclear translocation of transcription factors, and the expression of antioxidant genes. We compared this with changes in the cytokine profiles released by stimulated splenocytes measured by ELISPOT technology and analyzed the interactions between neuronal and immune cells and neuronal function and viability in cell death assays and multi-electrode arrays. Our observations show that dimethyl fumarate causes short-lived oxidative stress, which leads to increased levels and nuclear localization of the transcription factor nuclear factor erythroid 2-related factor 2 and a subsequent increase in glutathione synthesis and recycling in neuronal cells. Concentrations that were cytoprotective in neuronal cells had no negative effects on viability of splenocytes but suppressed the production of proinflammatory cytokines in cultures from C57BL/6 and SJL mice and had no effects on neuronal activity in multi-electrode arrays. Conclusions These results suggest that immunomodulatory concentrations of dimethyl fumarate can reduce oxidative stress without altering neuronal network activity.

Published
2012
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10. Mechanisms of clonal evolution in childhood acute lymphoblastic leukemia

Author

Swaminathan, Srividya, primary, Klemm, Lars, additional, Park, Eugene, additional, Papaemmanuil, Elli, additional, Ford, Anthony, additional, Kweon, Soo-Mi, additional, Trageser, Daniel, additional, Hasselfeld, Brian, additional, Henke, Nadine, additional, Mooster, Jana, additional, Geng, Huimin, additional, Schwarz, Klaus, additional, Kogan, Scott C, additional, Casellas, Rafael, additional, Schatz, David G, additional, Lieber, Michael R, additional, Greaves, Mel F, additional, and Müschen, Markus, additional

Published
2015
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11. Mechanisms of Clonal Evolution of Pre-Leukemic Clones in Childhood Pre-B Acute Lymphoblastic Leukemia

Author

Swaminathan, Srividya, primary, Klemm, Lars, additional, Park, Eugene, additional, Ford, Anthony M, additional, Kweon, Soo-mi, additional, Trageser, Daniel, additional, Hasselfeld, Brian, additional, Henke, Nadine, additional, Geng, Huimin, additional, Schwarz, Klaus, additional, Casellas, Rafael, additional, Schatz, David G., additional, Lieber, Michael R, additional, Papaemmanuil, Elli, additional, Greaves, Mel, additional, and Muschen, Markus, additional

Published
2014
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12. Interaction of Bcl-2 with the Autophagy-related GABAA Receptor-associated Protein (GABARAP)

Author

Ma, Peixiang, primary, Schwarten, Melanie, additional, Schneider, Lars, additional, Boeske, Alexandra, additional, Henke, Nadine, additional, Lisak, Dmitrij, additional, Weber, Stephan, additional, Mohrlüder, Jeannine, additional, Stoldt, Matthias, additional, Strodel, Birgit, additional, Methner, Axel, additional, Hoffmann, Silke, additional, Weiergräber, Oliver H., additional, and Willbold, Dieter, additional

Published
2013
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14. The C Terminus of Bax Inhibitor-1 Forms a Ca2+-permeable Channel Pore

Author

Bultynck, Geert, primary, Kiviluoto, Santeri, additional, Henke, Nadine, additional, Ivanova, Hristina, additional, Schneider, Lars, additional, Rybalchenko, Volodymyr, additional, Luyten, Tomas, additional, Nuyts, Koen, additional, De Borggraeve, Wim, additional, Bezprozvanny, Ilya, additional, Parys, Jan B., additional, De Smedt, Humbert, additional, Missiaen, Ludwig, additional, and Methner, Axel, additional

Published
2012
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15. Charcot–Marie–Tooth disease CMT4A: GDAP1 increases cellular glutathione and the mitochondrial membrane potential

Author

Noack, Rebecca, primary, Frede, Svenja, additional, Albrecht, Philipp, additional, Henke, Nadine, additional, Pfeiffer, Annika, additional, Knoll, Katrin, additional, Dehmel, Thomas, additional, Meyer zu Hörste, Gerd, additional, Stettner, Mark, additional, Kieseier, Bernd C., additional, Summer, Holger, additional, Golz, Stefan, additional, Kochanski, Andrzej, additional, Wiedau-Pazos, Martina, additional, Arnold, Susanne, additional, Lewerenz, Jan, additional, and Methner, Axel, additional

Published
2011
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18. The C Terminus of Bax Inhibitor-1 Forms a Ca2+-permeable Channel Pore.

Author

Bultynck, Geert, Kiviluoto, Santeri, Henke, Nadine, Ivanova, Hristina, Schneider, Lars, Rybalchenko, Volodymyr, Luyten, Tomas, Nuyts, Koen, Borggraeve, Wim De, Bezprozvanny, Ilya, Parys, Jan B., Smedt, Humbert De, Missiaen, Ludwig, and Methner, Axel

Subjects
*ENDOPLASMIC reticulum, *APOPTOSIS, *HOMEOSTASIS, *CALCIUM, *AMINO acids
Abstract

Bax inhibitor-1 (BI-1) is a multitransmembrane domainspanning endoplasmic reticulum (ER)-located protein that is evolutionarily conserved and protects against apoptosis and ER stress. Furthermore, BI-1 is proposed to modulate ER Ca2+ homeostasis by acting as a Ca2+-leak channel. Based on experimental determination of the BI-1 topology, we propose that itsC terminus forms a Ca2+ pore responsible for its Ca2+-leak properties. We utilized a set of C-terminal peptides to screen for Ca2+ leak activity in unidirectional 45Ca2+-flux experiments and identified an α-helical 20-amino acid peptide causing Ca2+ leak from the ER. The Ca2+leak was independent of endogenous ER Ca2+-release channels or other Ca2+-leak mechanisms, namely translocons and presenilins. The Ca2+-permeating property of the peptide was confirmed in lipid-bilayer experiments. Using mutant peptides, we identified critical residues responsible for the Ca2+-leak properties of this BI-1 peptide, including a series of critical negatively charged aspartate residues. Using peptides corresponding to the equivalent BI-1 domain from various organisms, we found that the Ca2+-leak properties were conserved among animal, but not plant and yeast orthologs. By mutating one of the critical aspartate residues in the proposed Ca2+-channel pore in full-length BI-1, we found that Asp-213 was essential for BI-1-dependent ER Ca2+ leak. Thus, we elucidated residues critically important for BI-1- mediated Ca2+ leak and its potential channel pore. Remarkably, one of these residues was not conserved among plant and yeast BI-1 orthologs, indicating that the ER Ca2+-leak properties of BI-1 are an added function during evolution. [ABSTRACT FROM AUTHOR]

Published
2012
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19. Interaction of Bcl-2 with the Autophagy-related GABAA Receptor-associated Protein (GABARAP) BIOPHYSICAL CHARACTERIZATION AND FUNCTIONAL IMPLICATIONS.

Author

Ma, Peixiang, Schwarten, Melanie, Schneider, Lars, Boeske, Alexandra, Henke, Nadine, Lisak, Dmitrij, Weber, Stephan, Mohrlüder, Jeannine, Stoldt, Matthias, Strodel, Birgit, Methner, Axel, Hoffmann, Silke, Weiergräber, Oliver H., and Willbold, Dieter

Subjects
*GABA, *APOPTOSIS, *CELL death, *DEATH (Biology), *AMINO acid neurotransmitters
Abstract

Apoptosis and autophagy are fundamental homeostatic processes in eukaryotic organisms fulfilling essential roles in development and adaptation. Recently, the anti-apoptotic factor Bcl-2 has been reported to also inhibit autophagy, thus establishing a potential link between these pathways, but the mechanistic details are only beginning to emerge. Here we show that Bcl-2 directly binds to the phagophore-associated protein GABARAP. NMR experiments revealed that the interaction critically depends on a three-residue segment (EWD) of Bcl-2 adjacent to the BH4 region, which is anchored to one of the two hydrophobic pockets on the GABARAP molecule. This is at variance with the majority of GABARAP interaction partners identified previously, which occupy both hydrophobic pockets simultaneously. Bcl-2 affinity could also be detected for GEC1, but not for other mammalian Atg8 homologs. Finally, we provide evidence that overexpression of Bcl-2 inhibits lipidation of GABARAP,a key step in autophagosome formation, possibly via competition with the lipid conjugation machinery. These results support the regulatory role of Bcl-2 in autophagy and define GABARAP as a novel interaction partner involved in this intricate connection. [ABSTRACT FROM AUTHOR]

Published
2013
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