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Gilabert-Juan, JavierAuthor

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March 22, 2021
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Astrocytes of the murine model for Down Syndrome Ts65Dn display reduced intracellular ionic zinc

Publicated to: NEUROCHEMISTRY INTERNATIONAL. 75 48-53 - 2014-09-01 75(), DOI: 10.1016/j.neuint.2014.05.013

Authors:

Ballestin, Raul; Miguel Blasco-Ibanez, Jose; Crespo, Carlos; Nacher, Juan; Lopez-Hidalgo, Rosa; Gilabert-Juan, Javier; Molto, Dolores; Varea, Emilio
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Affiliations

Univ Valencia, Dept Cell Biol, Neurobiol Unit, E-46100 Burjassot, Spain - Author
Univ Valencia, Dept Cell Biol, Program Basic & Appl Neurosci, E-46100 Burjassot, Spain - Author
Univ Valencia, INCLIVA, CIBERSAM, Dept Genet, E-46100 Burjassot, Spain - Author
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Abstract

Zinc is an essential trace element that is critical for a large number of structural proteins, enzymatic processes and transcription factors. In the brain, zinc ions are involved in synaptic transmission. The homeostasis of zinc is crucial for cell survival and function, and cells have developed a wide variety of systems to control zinc concentration. Alterations in free zinc concentration have been related with brain dysfunction. Down Syndrome individuals present alterations in free zinc concentration and in some of the proteins related with zinc homeostasis. We have analyzed the amount of free zinc and the zinc chelating protein metallothionein 3 in the astrocytes using primary cultures of the murine model Ts65Dn. We have observed a higher number of zinc positive spots in the cytoplasm of trisomic astrocytes but a decrease in the total concentration of total intracellular free zinc concentration (including the spots) respect to control astrocytes. Using FM1-43 staining, we found that the endocytic function remains unaltered. Therefore, a possible explanation for this lower concentration of free zinc could be the higher concentration of metallothionein 3 present in the cytoplasm of trisomic astrocytes. The blockade of metallothionein 3 expression using an specific siRNA induced an increase in the concentration of free zinc in basal conditions but failed to increase the uptake of zinc after incubation with zinc ions. (C) 2014 Elsevier Ltd. All rights reserved.
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Keywords

astrocytedown syndromemetallothionein 3ts65dntsqAbnormalitiesApoptosisAstrocyteBrainCalcium homeostasisDown syndromeHistochemically reactive zincMetallothioneinMetallothionein 3Mouse modelProliferationReleaseTransportersTs65dnTsqZinc

Quality index

Bibliometric impact. Analysis of the contribution and dissemination channel

The work has been published in the journal NEUROCHEMISTRY INTERNATIONAL due to its progression and the good impact it has achieved in recent years, according to the agency WoS (JCR), it has become a reference in its field. In the year of publication of the work, 2014, it was in position 112/252, thus managing to position itself as a Q2 (Segundo Cuartil), in the category Neurosciences. Notably, the journal is positioned en el Cuartil Q2 para la agencia Scopus (SJR) en la categoría Cell Biology.

Independientemente del impacto esperado determinado por el canal de difusión, es importante destacar el impacto real observado de la propia aportación.

Según las diferentes agencias de indexación, el número de citas acumuladas por esta publicación hasta la fecha 2026-04-05:

  • WoS: 10
  • Scopus: 9
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Impact and social visibility

From the perspective of influence or social adoption, and based on metrics associated with mentions and interactions provided by agencies specializing in calculating the so-called "Alternative or Social Metrics," we can highlight as of 2026-04-05:

  • The use of this contribution in bookmarks, code forks, additions to favorite lists for recurrent reading, as well as general views, indicates that someone is using the publication as a basis for their current work. This may be a notable indicator of future more formal and academic citations. This claim is supported by the result of the "Capture" indicator, which yields a total of: 23 (PlumX).
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