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(Reference retrieved automatically from Web of Science through information on FAPESP grant and its corresponding number as mentioned in the publication by the authors.)

Expression of connexins 36, 43, and 45 during postnatal development of the mouse retina

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Author(s):
Kihara, Alexandre Hiroaki ; de Castro, Leandro Mantovani ; Belmonte, Monica Aparecida ; Yan, Chao Yun Irene ; Moriscot, Anselmo Sigari ; Hamassaki, Dania Emi
Total Authors: 6
Document type: Journal article
Source: JOURNAL OF NEUROBIOLOGY; v. 66, n. 13, p. 1397-1410, NOV 2006.
Web of Science Citations: 29
Abstract

Gap junction channels formed by connexins (Cx) may play essential roles in some processes that occur during retinal development, such as apoptosis and calcium wave spread. The present study was undertaken to determine the distribution pattern of Cx36, Cx43, and Cx45 by immunofluorescence, as well as their gene expression levels by quantitative PCR during postnatal development of the mouse retina. Our results showed an increased expression of neuronal Cx36 from P1 until P10, when this Cx reached adult levels, and it was mainly distributed in the outer and inner plexiform layers. In turn, Cx43 was almost absent in retinal progenitor cells at PI, it became more prominent in glial cell processes about P10, and did not change until adulthood. Double-labeling studies in situ and in vitro with antivimentin, a Muller cell marker, confirmed that Cx43 was expressed by these cells. In addition, quantitative PCR showed that Cx43 and vimentin shared very similar temporal expression patterns. Finally, in contrast to Cx36 and Cx43, Cx45 mRNA was strongly down-regulated during development. In early postnatal days, Cx45 was seen ubiquitously distributed throughout the retina in cells undergoing proliferation and differentiation, as well in differentiated neurons. In adult retina, this protein had a more restricted distribution both in neurons and glial cells, as confirmed in situ and in vitro. In conclusion, we observed a distinct temporal expression pattern for Cx36, Cx43, and Cx45, which is probably related to particular roles in retinal function and maintenance of homeostasis during development of the mouse retina. (c) 2006 Wiley Periodicals, Inc. (AU)

FAPESP's process: 01/09047-2 - Cellular and molecular aspects of vertebrate retina development and degeneration
Grantee:Dania Emi Hamassaki
Support Opportunities: Research Projects - Thematic Grants