OCP2 immunoreactivity in the human fetal cochlea at weeks 11, 17, 20, and 28, and the human adult cochlea

The two most abundant proteins of the organ of Corti, OCP1 and OCP2, are acidic, cytosolic, low molecular weight proteins diffusely distributed within the cytoplasm of supporting cells. A recent study by Henzl et al. (2001) found first, that these two proteins co-localize with connexin 26 along the...

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Veröffentlicht in:Hearing research 2002-05, Vol.167 (1), p.102-109
Hauptverfasser: Kammen-Jolly, Keren, Scholtz, Arne W, Kreczy, Alfons, Glückert, Rudolf, Thalmann, Isolde, Thalmann, Rudiger, Schrott-Fischer, Anneliese
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container_end_page 109
container_issue 1
container_start_page 102
container_title Hearing research
container_volume 167
creator Kammen-Jolly, Keren
Scholtz, Arne W
Kreczy, Alfons
Glückert, Rudolf
Thalmann, Isolde
Thalmann, Rudiger
Schrott-Fischer, Anneliese
description The two most abundant proteins of the organ of Corti, OCP1 and OCP2, are acidic, cytosolic, low molecular weight proteins diffusely distributed within the cytoplasm of supporting cells. A recent study by Henzl et al. (2001) found first, that these two proteins co-localize with connexin 26 along the epithelial gap junction system and second, that OCP2 could participate with OCP1 in an organ of Corti-specific SCF complex (Skp1, cul1in, and Fbp), a ubiquitin ligase complex. Previous study has also implicated OCP2 in the recycling and regulation of intracellular K + efflux as well as pH homeostatic mechanisms. In the present study, we document the emergence and distribution features of OCP2 through various stages (weeks 11–28) of gestation in human fetal cochleae. Four fetal cochleae, the cochleae of a normal hearing human adult and a mature rat for positive control were fixed in 4% formalin within 2 h post mortem. Immunohistochemical studies were performed using a rabbit polyclonal antibody raised against a synthetic peptide corresponding to amino acids 3–16. Specimens were mounted in paraffin sections. Results show that OCP2 immunoreactivity is evident at a prenatal age of 11 weeks, peaks in expression at the onset of cochlear function at 20 weeks and achieves adult-like patterns of distribution just prior to histological maturation at 28 weeks. Though this protein could be associated with the development, maturation, and electrochemical maintenance of the cochlear gap junction system, the nature of this protein’s function in the developing and mature human cochlea remains unclear.
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Results show that OCP2 immunoreactivity is evident at a prenatal age of 11 weeks, peaks in expression at the onset of cochlear function at 20 weeks and achieves adult-like patterns of distribution just prior to histological maturation at 28 weeks. Though this protein could be associated with the development, maturation, and electrochemical maintenance of the cochlear gap junction system, the nature of this protein’s function in the developing and mature human cochlea remains unclear.</abstract><cop>Amsterdam</cop><pub>Elsevier B.V</pub><pmid>12117534</pmid><doi>10.1016/S0378-5955(02)00354-4</doi><tpages>8</tpages></addata></record>
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source Elsevier ScienceDirect Journals Complete - AutoHoldings; MEDLINE
subjects Adult
Animals
Biological and medical sciences
Cochlea - embryology
Cochlea - growth & development
Cochlea - metabolism
Ear and associated structures. Auditory pathways and centers. Hearing. Vocal organ. Phonation. Sound production. Echolocation
Epithelial gap junction system
Fetal cochlea
Fetus - metabolism
Fundamental and applied biological sciences. Psychology
Gestational Age
Human
Humans
Immunohistochemistry
OCP1
OCP2
Organ of Corti - embryology
Organ of Corti - growth & development
Organ of Corti - metabolism
Rats
S-Phase Kinase-Associated Proteins
Transcription Factors - metabolism
Vertebrates: nervous system and sense organs
title OCP2 immunoreactivity in the human fetal cochlea at weeks 11, 17, 20, and 28, and the human adult cochlea
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