Your search keyword '"Mihail S. Iordanov"' showing total 3 results

1. Proximal Giant Neurofilamentous Axonopathy in Mice Genetically Engineered to Resist Calpain and Caspase Cleavage of α-II Spectrin

Author

G. Nicolas, Desire Tshala-Katumbay, Victor Monterroso, A. L. Ramos, E. Couchi, Jill S. Wentzell, Doris Kretzschmar, Roman M. Kassa, M. C. Lecomte, and Mihail S. Iordanov

Subjects

Nervous system, biology, Mutant, Neurodegeneration, Calpain, General Medicine, medicine.disease, Molecular biology, Pathogenesis, Cellular and Molecular Neuroscience, medicine.anatomical_structure, biology.protein, medicine, Spectrin, Caspase, Giant axonal neuropathy

Abstract

We use 1,2-diacetylbenzene (1,2-DAB) to probe molecular mechanisms of proximal giant neurofilamentous axonopathy (PGNA), a pathological hallmark of amyotrophic lateral sclerosis. The spinal cord proteome of rodents displaying 1,2-DAB PGNA suggests a reduction in the abundance of α-II spectrin (Spna2), a key protein in the maintenance of axonal integrity. Protein immunoblotting indicates that this reduction is due to Spna2 degradation. We investigated the importance of such degradation in 1,2-DAB PGNA. Spna2 mutant mice lacking a calpain- and/or caspase-sensitive domain (CSD), thus hypothetically resistant to 1,2-DAB, and wild-type littermates, were treated with 1,2-DAB, 35 mg/kg/day, or saline control, for 3 weeks. 1,2-DAB induced motor weakness and PGNA, irrespective of the genotype. Spna2-calpain breakdown products were not detected in mutant mice, which displayed a normal structure of the nervous system under saline treatment. Intriguingly, treatment with 1,2-DAB reduced the abundance of the caspase-specific 120-kDa Spna2 breakdown products. Our findings indicate that degradation of Spna2 by calpain- and/or caspase is not central to the pathogenesis of 1,2-DAB axonopathy. In addition, the Spna2-CSD seems to be not required for the maintenance of the cytoskeleton integrity. Our conceptual framework offers opportunities to study the role of calpain-caspase cross talk, including that of the protease degradomics, in models of axonal degeneration.

Published

2012

2. Two mechanisms of caspase 9 processing in double-stranded RNA- and virus-triggered apoptosis

Author

Olga P. Ryabinina, Bruce E. Magun, Pascal Schneider, and Mihail S. Iordanov

Subjects

Cancer Research, viruses, Clinical Biochemistry, Caspase 2, Pharmaceutical Science, Apoptosis, Breast Neoplasms, Caspase 3, Caspase 8, Breast Neoplasms/pathology, Caspase 9, Caspases/metabolism, Cell Line, Tumor, Encephalomyocarditis virus/genetics, Encephalomyocarditis virus/physiology, Enzyme Activation, Female, Hela Cells, Humans, RNA, Double-Stranded/metabolism, Encephalomyocarditis virus, Caspase, RNA, Double-Stranded, Pharmacology, biology, NLRP1, Cytochrome c, Biochemistry (medical), Cell Biology, Molecular biology, Cell biology, XIAP, Caspases, biology.protein, Caspase 10, HeLa Cells

Abstract

Viral double-stranded RNA (dsRNA) is a ubiquitous intracellular "alert signal" used by cells to detect viral infection and to mount anti-viral responses. DsRNA triggers a rapid (complete within 2-4 h) apoptosis in the highly-susceptible HeLa cell line. Here, we demonstrate that the apical event in this apoptotic cascade is the activation of procaspase 8. Downstream of caspase 8, the apoptotic signaling cascade bifurcates into a mitochondria-independent caspase 8/caspase 3 arm and a mitochondria-dependent, caspase 8/Bid/Bax/Bak/cytochrome c arm. Both arms impinge upon, and activate, procaspase 9 via two different cleavage sites within the procaspase 9 molecule (D330 and D315, respectively). This is the first in vivo demonstration that the "effector" caspase 3 plays an "initiator" role in the regulation of caspase 9. The dsRNA-induced apoptosis is potentiated by the inhibition of protein synthesis, whose role is to accelerate the execution of all apoptosis steps downstream of, and including, the activation of caspase 8. Thus, efficient apoptosis in response to viral dsRNA results from the co-operation of the two major apical caspases (8 and 9) and the dsRNA-activated protein kinase R (PKR)/ribonuclease L (RNase L) system that is essential for the inhibition of protein synthesis in response to viral infection.

Published

2005

3. D-MEKK1, the Drosophila orthologue of mammalian MEKK4/MTK1, and Hemipterous/D-MKK7 mediate the activation of D-JNK by cadmium and arsenite in Schneider cells

Author

Mihail S. Iordanov, Olga P. Ryabinina, and Ezhilkani Subbian

Subjects

Sodium arsenite, Arsenites, MAP Kinase Kinase Kinase 1, MAP Kinase Kinase Kinase 4, p38 Mitogen-Activated Protein Kinases, Cell Line, Hemiptera, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, RNA interference, Animals, Drosophila Proteins, lcsh:QH573-671, 030304 developmental biology, Arsenite, Mammals, 0303 health sciences, biology, lcsh:Cytology, Kinase, Schneider 2 cells, JNK Mitogen-Activated Protein Kinases, Cell Biology, biology.organism_classification, Cell biology, Enzyme Activation, Kinetics, Drosophila melanogaster, chemistry, Biochemistry, Signal transduction, 030217 neurology & neurosurgery, Drosophila Protein, Research Article, Cadmium

Abstract

BackgroundThe family of c-Jun NH2-terminal kinases (JNK) plays important roles in embryonic development and in cellular responses to stress. Toxic metals and their compounds are potent activators of JNK in mammalian cells. The mechanism of mammalian JNK activation by cadmium and sodium arsenite involves toxicant-induced oxidative stress. The study of mammalian signaling pathways to JNK is complicated by the significant degree of redundancy among upstream JNK regulators, especially at the level of JNK kinase kinases (JNKKK).ResultsUsingDrosophila melanogasterS2 cells, we demonstrate here that cadmium and arsenite activateDrosophilaJNK (D-JNK) via oxidative stress as well, thus providing a simpler model system to study JNK signaling. To elucidate the signaling pathways that lead to activation of D-JNK in response to cadmium or arsenite, we employed RNA interference (RNAi) to knock down thirteen upstream regulators of D-JNK, either singly or in combinations of up to seven at a time.ConclusionD-MEKK1, the fly orthologue of mammalian MEKK4/MTK1, andHemipterous/D-MKK7 mediates the activation of D-JNK by cadmium and arsenite.

Published

2006