The multiple cascades of signal transduction pathways that lead from receptors on the cell membrane to the nucleus, thus translating extracellular signals into changes in gene expression, may represent important targets for neurotoxic compounds. Among the biochemical steps and pathways that have been investigated are the metabolism of cyclic nucleotides, the formation of nitric oxide, the metabolism of membrane phospholipids, the activation of a multitude of protein kinases and the induction of transcription factors. This brief review will focus on the interactions of three known neurotoxicants, lead, ethanol and polychlorinated biphenyls, with signal transduction pathways, particularly the family of protein kinase C isozymes, and discusses how such effects may be involved in their neurotoxicity. © 2001 Elsevier Science Ireland Ltd.
Intracellular signal transduction pathways as targets for neurotoxicants / Costa, Lucio Guido; M., Guizzetti; H., Lu; F., Bordi; Vitalone, Annabella; Tita, Beatrice; Palmery, Maura; Valeri, Pacifico; Silvestrini, Bruno. - In: TOXICOLOGY. - ISSN 0300-483X. - STAMPA. - 160:1-3(2001), pp. 19-26. [10.1016/s0300-483x(00)00435-2]
Intracellular signal transduction pathways as targets for neurotoxicants
COSTA, Lucio Guido;VITALONE, Annabella;TITA, Beatrice;PALMERY, Maura;VALERI, Pacifico;SILVESTRINI, Bruno
2001
Abstract
The multiple cascades of signal transduction pathways that lead from receptors on the cell membrane to the nucleus, thus translating extracellular signals into changes in gene expression, may represent important targets for neurotoxic compounds. Among the biochemical steps and pathways that have been investigated are the metabolism of cyclic nucleotides, the formation of nitric oxide, the metabolism of membrane phospholipids, the activation of a multitude of protein kinases and the induction of transcription factors. This brief review will focus on the interactions of three known neurotoxicants, lead, ethanol and polychlorinated biphenyls, with signal transduction pathways, particularly the family of protein kinase C isozymes, and discusses how such effects may be involved in their neurotoxicity. © 2001 Elsevier Science Ireland Ltd.I documenti in IRIS sono protetti da copyright e tutti i diritti sono riservati, salvo diversa indicazione.
