Astrocytic-neuronal-astrocytic pathway selection for formation and degradation of glutamate/GABA

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Astrocytic-neuronal-astrocytic pathway selection for formation and degradation of glutamate/GABA / Leif Hertz and Tiago B. Rodrigues.

One research field that early recognized the importance of intercellular interactions was endocrinology, initially in processes involved in lactation, pubertal maturation and regulation of the female ovarian cycle and later in appetite regulation. These interactions included, but were not restricted...

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Tiago B. Rodrigues
TeilnehmendeR:
Rodrigues, Tiago B.,
Hertz, Leif,
Place / Publishing House:Lausanne, Switzerland : : Frontiers Media SA,, 2014.
©2014
Year of Publication:2014
Language:English
Series:Frontiers Research Topics.
Physical Description:1 online resource (168 pages) :; illustrations; digital, PDF file(s).
Notes:
  • Bibliographic Level Mode of Issuance: Monograph
  • Published in Frontiers in Endocrinology.
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Astrocytic-neuronal-astrocytic pathway selection for formation and degradation of glutamate/GABA [electronic resource] / Leif Hertz and Tiago B. Rodrigues.
Frontiers Media SA 2014
Lausanne, Switzerland : Frontiers Media SA, 2014.
©2014
1 online resource (168 pages) : illustrations; digital, PDF file(s).
text txt rdacontent
computer c rdamedia
online resource cr rdacarrier
text file rda
Frontiers Research Topics.
Bibliographic Level Mode of Issuance: Monograph
Published in Frontiers in Endocrinology.
Includes bibliographical references.
Open access Unrestricted online access star
One research field that early recognized the importance of intercellular interactions was endocrinology, initially in processes involved in lactation, pubertal maturation and regulation of the female ovarian cycle and later in appetite regulation. These interactions included, but were not restricted to neuronal-astrocytic interactions. The importance of glutamatergic and GABAergic signaling during all of these events is now realized. At the same time huge advances have been made in i) determination of metabolic rates in the human and rodent brain in vivo, including oxidative metabolism rates in astrocytes which per volume are at par with those in neurons; ii) understanding the unique ability of astrocytes, but not neurons to synthetize tricarboxylic acid intermediates necessary for net synthesis of glutamate and thereby also GABA; iii) determination of the rates at which such synthesis occurs, and iv) the two-fold higher rates at which glutamate and GABA are cycled between astrocytes and neurons in the brain in vivo. This quantitative difference reflects that most transmitter uptake, especially that of glutamate, occurs in astrocytes and that on average two thirds of astrocytically accumulated neuronal transmitters are recycled to neurons, whereas the last one third is oxidatively degraded, mainly or exclusively in astrocytes. The progress in these areas puts emphasis on i) firmly establishing whether or not aralar, a necessary component of the aspartate/glutamate exchanger in the malate-aspartate cycle is expressed in astrocytes, and ii) the detailed processes occurring in astrocytes and in neurons during the formation and subsequent oxidative degradation of transmitter glutamate and GABA. Initial observations by different groups showed no astrocytic aralar expression in mature brain. However, a recent paper by Pardo et al. (J. Cereb Blood Flow & Met.) used improved cytochemical techniques and showed some protein expression in astrocytes in mature brain; Hertz (same journal) calculated that the amount would be sufficient for normal oxidative degradation. However, there are indications that the astrocytic-neuronal-astrocytic interactions in formation, transfer and re-oxidation of transmitter glutamate and GABA may repeatedely require additional MAS function. Equal expression of aralar mRNA has been shown by the Nedergaard group in neurons and astrocytes obtained by fluorescence-activated cell sorting of brain cells from mice co-expressing astrocytic and neuronal markers with different fluorescent signals. This has recently been confirmed and also shown to be the case for aralar protein (J. Neurochem, under revision).
English
Endocrinology.
Neuroscience HILCC
Human Anatomy & Physiology HILCC
Health & Biological Sciences HILCC
Brain glutamine
brain metabolism
Appetite Regulation
Astrocyte-oligdendrocyte interaction
Brain ammonia
GABA
Astrocytic gene expression
pancreatic islets
Brain aspartate
Brain glutamate
Rodrigues, Tiago B., editor.
Hertz, Leif, editor, contributor.
2-88919-243-1
language English
format Electronic
eBook
author Tiago B. Rodrigues
spellingShingle Tiago B. Rodrigues
Astrocytic-neuronal-astrocytic pathway selection for formation and degradation of glutamate/GABA
Frontiers Research Topics.
author_facet Tiago B. Rodrigues
Rodrigues, Tiago B.,
Hertz, Leif,
author_variant t b r tbr
author2 Rodrigues, Tiago B.,
Hertz, Leif,
author2_variant t b r tb tbr
l h lh
author2_role TeilnehmendeR
TeilnehmendeR
author_sort Tiago B. Rodrigues
title Astrocytic-neuronal-astrocytic pathway selection for formation and degradation of glutamate/GABA
title_full Astrocytic-neuronal-astrocytic pathway selection for formation and degradation of glutamate/GABA [electronic resource] / Leif Hertz and Tiago B. Rodrigues.
title_fullStr Astrocytic-neuronal-astrocytic pathway selection for formation and degradation of glutamate/GABA [electronic resource] / Leif Hertz and Tiago B. Rodrigues.
title_full_unstemmed Astrocytic-neuronal-astrocytic pathway selection for formation and degradation of glutamate/GABA [electronic resource] / Leif Hertz and Tiago B. Rodrigues.
title_auth Astrocytic-neuronal-astrocytic pathway selection for formation and degradation of glutamate/GABA
title_new Astrocytic-neuronal-astrocytic pathway selection for formation and degradation of glutamate/GABA
title_sort astrocytic-neuronal-astrocytic pathway selection for formation and degradation of glutamate/gaba
series Frontiers Research Topics.
series2 Frontiers Research Topics.
publisher Frontiers Media SA
Frontiers Media SA,
publishDate 2014
physical 1 online resource (168 pages) : illustrations; digital, PDF file(s).
isbn 2-88919-243-1
callnumber-first Q - Science
callnumber-subject QP - Physiology
callnumber-label QP363
callnumber-sort QP 3363.2
illustrated Illustrated
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