Publikation: A role for mixed lineage kinases in granule cell apoptosis induced by cytoskeletal disruption
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2006
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Müller, Georg Johannes
Geist, Marie Aavang
Veng, Lone Merete
Willesen, Mette Georgi
Johansen, Flemming Fryd
Vaudano, Elisabetta
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Journal of Neurochemistry. 2006, 96(5), pp. 1242-1252. ISSN 0022-3042. eISSN 1471-4159
Zusammenfassung
Microtubule disruption by colchicine induces apoptosis in selected neuronal populations. However, little is known about the upstream death signalling events mediating the neurotoxicity. We investigated first whether colchicine-induced granule cell apoptosis activates the c-Jun N-terminal kinase (JNK) pathway. Cultured murine cerebellar granule cells were exposed to 1 lM colchicine for 24 h. Activation of the JNK pathway was detected by western blotting as well as immunocytochemistry using antibodies against phosphoc- Jun (p-c-Jun). Next, adult male rats were injected intracerebroventricularly with colchicine (10 lg), and JNK pathway activation in dentate granule cells (DGCs) was detected by antibodies against p-c-Jun. The second part of the study tested the involvement of mixed lineage kinases (MLK) as upstream activators of the JNK pathway in colchicine toxicity, using CEP-1347, a potent MLK inhibitor. In vitro, significant inhibition of the JNK pathway, activated by colchicine, was achieved by 100 300 nM CEP-1347, which blocked both activation of cell death proteases and apoptosis. Moreover, CEP-1347 markedly delayed neurite fragmentation and cell degeneration. In vivo, CEP-1347 (1 mg/kg) significantly prevented p-c-jun increase following injection of colchicine, and enhanced survival of DGCs. We conclude that colchicineinduced neuronal apoptosis involves the JNK/MLK pathway, and that protection of granule cells can be achieved by MLK inhibition.
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570 Biowissenschaften, Biologie
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MÜLLER, Georg Johannes, Marie Aavang GEIST, Lone Merete VENG, Mette Georgi WILLESEN, Flemming Fryd JOHANSEN, Marcel LEIST, Elisabetta VAUDANO, 2006. A role for mixed lineage kinases in granule cell apoptosis induced by cytoskeletal disruption. In: Journal of Neurochemistry. 2006, 96(5), pp. 1242-1252. ISSN 0022-3042. eISSN 1471-4159BibTex
@article{Muller2006mixed-7149,
year={2006},
title={A role for mixed lineage kinases in granule cell apoptosis induced by cytoskeletal disruption},
number={5},
volume={96},
issn={0022-3042},
journal={Journal of Neurochemistry},
pages={1242--1252},
author={Müller, Georg Johannes and Geist, Marie Aavang and Veng, Lone Merete and Willesen, Mette Georgi and Johansen, Flemming Fryd and Leist, Marcel and Vaudano, Elisabetta}
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<dcterms:abstract xml:lang="eng">Microtubule disruption by colchicine induces apoptosis in selected neuronal populations. However, little is known about the upstream death signalling events mediating the neurotoxicity. We investigated first whether colchicine-induced granule cell apoptosis activates the c-Jun N-terminal kinase (JNK) pathway. Cultured murine cerebellar granule cells were exposed to 1 lM colchicine for 24 h. Activation of the JNK pathway was detected by western blotting as well as immunocytochemistry using antibodies against phosphoc- Jun (p-c-Jun). Next, adult male rats were injected intracerebroventricularly with colchicine (10 lg), and JNK pathway activation in dentate granule cells (DGCs) was detected by antibodies against p-c-Jun. The second part of the study tested the involvement of mixed lineage kinases (MLK) as upstream activators of the JNK pathway in colchicine toxicity, using CEP-1347, a potent MLK inhibitor. In vitro, significant inhibition of the JNK pathway, activated by colchicine, was achieved by 100 300 nM CEP-1347, which blocked both activation of cell death proteases and apoptosis. Moreover, CEP-1347 markedly delayed neurite fragmentation and cell degeneration. In vivo, CEP-1347 (1 mg/kg) significantly prevented p-c-jun increase following injection of colchicine, and enhanced survival of DGCs. We conclude that colchicineinduced neuronal apoptosis involves the JNK/MLK pathway, and that protection of granule cells can be achieved by MLK inhibition.</dcterms:abstract>
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