Issue title: Disease Markers of the Nervous System
Article type: Research Article
Authors: Fonteh, Alfred N. | Harrington, Robert J. | Huhmer, Andreas F. | Biringer, Roger G. | Riggins, James N. | Harrington, Michael G.
Affiliations: Molecular Neurology Program, Huntington Medical
Research Institutes, Pasadena, CA 91101, USA | Thermo, San Jose, CA 95134, USA
Note: [] Corresponding author. Tel.: +1 626 795 4343; E-mail:
[email protected]
Abstract: Lipids comprise the bulk of the dry mass of the brain. In addition
to providing structural integrity to membranes, insulation to cells and acting
as a source of energy, lipids can be rapidly converted to mediators of
inflammation or to signaling molecules that control molecular and cellular
events in the brain. The advent of soft ionization procedures such as
electrospray ionization (ESI) and atmospheric pressure chemical ionization
(APCI) have made it possible for compositional studies of the diverse lipid
structures that are present in brain. These include phospholipids, ceramides,
sphingomyelin, cerebrosides, cholesterol and their oxidized derivatives. Lipid
analyses have delineated metabolic defects in disease conditions including
mental retardation, Parkinson's Disease (PD), schizophrenia, Alzheimer's
Disease (AD), depression, brain development, and ischemic stroke. In this
review, we examine the structure of the major lipid classes in the brain,
describe methods used for their characterization, and evaluate their role in
neurological diseases. The potential utility of characterizing lipid markers in
the brain, with specific emphasis on disease mechanisms, will be discussed.
Additionally, we describe several proteomic strategies for characterizing
lipid-metabolizing proteins in human cerebrospinal fluid (CSF). These proteins
may be potential therapeutic targets since they transport lipids required for
neuronal growth or convert lipids into molecules that control brain physiology.
Combining lipidomics and proteomics will enhance existing knowledge of disease
pathology and increase the likelihood of discovering specific markers and
biochemical mechanisms of brain diseases.
Keywords: Lipidomics, phospholipidomics, sphingolipidomics, cholesterol, proteomics, mass spectrometry, electrospray ionization, phospholipases, enzymes, lipoproteins, cytochrome P450, acetylhydrolases, fatty acids, eicosanoids, secretion, ion channels, receptors, inflammation, oxidation, cerebrospinal fluid, brain, neurological diseases
Journal: Disease Markers, vol. 22, no. 1-2, pp. 39-64, 2006
Received 11 November 2005
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Accepted 11 November 2005
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Published: 2006
