From Neuroprogression to Neuroprotection: Implications for Clinical Care

Overview

Journal Med J Aust

Specialty General Medicine

Date 2010 Aug 18

PMID 20712560

Citations 27

Authors

Michael Berk

Philippe Conus

Flavio Kapczinski

Ana C Andreazza

Murat Yucel

Stephen J Wood

Christos Pantelis

Gin S Malhi

Seetal Dodd

Andreas Bechdolf

G Paul Amminger

Ian B Hickie

Patrick D McGorry

Affiliations

Soon will be listed here.

Abstract

Bipolar disorder follows a staged trajectory in which persistence of illness is associated with a number of clinical features such as progressive shortening of the inter-episode interval and decreased probability of treatment response. This neuroprogressive clinical process is reflected by both progressive neuroanatomical changes and evidence of cognitive decline. The biochemical foundation of this process appears to incorporate changes in inflammatory cytokines, cortisone, neurotrophins and oxidative stress. There is a growing body of evidence to suggest that these markers may differ between the early and late stages of the disorder. The presence of a series of tangible targets raises the spectre of development of rational neuroprotective strategies, involving judicious use of current therapies and novel agents. Most of the currently used mood stabilisers share effects on oxidative stress and neurotrophins, while novel potentially neuroprotective agents are being developed. These developments need to be combined with service initiatives to maximise the opportunities for early diagnosis and intervention.

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