Your search keyword '"Represa, J."' showing total 12 results

1. Reduction of glial fibrillary acidic protein-immunoreactive astrocytes in some brain areas of old hairless rhino-j mice (hr-rh-j)

Author

San José, Isabel, Cabo, R., Represa, J., San José, Isabel, Cabo, R., and Represa, J.

Abstract

Mutations in the hairless (hr) gene of mice result in hair follicle and other epithelial defects. The hr gene is expressed at high levels in the brain where it probably participates in the survival and maintenance of some neuronal populations, but whether it also supports glial populations of the central nervous system has been not investigated. To clarify this, quantitative immunohistochemistry for astrocytes (glial fibrillary acidic protein (GFAP)) and microglial cells (CD11b macrophage antigen) was used in the brain of a mutant mouse strain, the hairless (hr-rh-j) type, which carries the homozygous hr gene rhino mutation. The glial cell density was assessed in the cerebral cortex, hippocampus, striatum, hypothalamus and cerebellum of young (3 months) and old (9 months) hr-rh-j mice. No significant differences were found between young wild-type and hr-rh-j mice. The density of GFAP immunoreactive astrocytes normally increased as a function of age, but in older hr-rh-j mice there was a severe reduction (P < 0.01) in the striatum, hypothalamus, and hippocampus. Conversely, the microglial cells were insensible to aging or to hr-rh-j mutation. These results suggest that the hr gene is involved in the maintenance of the GFAP immunoreactive cells in some cerebral areas. Nevertheless, because these animals do not show any neurological signs, the functional significance of the present findings remains to be established. © 2001 Elsevier Science Ireland Ltd. All rights reserved.

Published

2001

2. Trks and p75 genes are differentially expressed in the inner ear of human embryos. What may Trks and p75 null mutant mice suggest on human development?

Author

Vega, José Antonio, San José, Isabel, Cabo, R., Rodríguez de Córdoba, Santiago, Represa, J., Vega, José Antonio, San José, Isabel, Cabo, R., Rodríguez de Córdoba, Santiago, and Represa, J.

Abstract

Recent work has shown the expression of Neurotrophins low (p75) and high affinity (Trk's A, B, and C) receptors in the developing inner ear sensory neurons of chick and mouse. Likewise the biological significance of such receptor expression was demonstrated by using both Trks and Neurotrophins null mutant mice. The present study was conducted to determine the expression of Trks and p75 proteins in the human inner ear throughout development. Hence to assess the potential role of Neurotrophins in the development of auditory and vestibular specific innervation in man. In other words, we intend to address the issue whether or not what null mutant mice for Trks and p75 have revealed on inner ear development may be relevant for human embryos. Fifty-two inner ears and their cochleovestibular ganglions (CVG) from human embryos and fetuses, ranging from 5 to 24 weeks of pregnancy were analyzed. Both Western blot and immunocytochemistry on frozen sections were used as complementary procedures. Quantitative Western blot studies revealed that Trk-B and C immunoreactivity (IR) appeared by embryonic week 5 in CVG neurons, increased at high levels between embryonic weeks 7 and 12, and later on, in 15 week-old specimens and older began to decrease to minimal levels. Trk-A IR was detected at just moderate levels during 5 and 7 weeks reflecting the presence of NGF high affinity receptors only at these earlier developmental ages. The p75 IR was detected at high degrees in the early stage of the 5th week and at abundant levels in all studied inner ears from the 7th to the 24th pregnancy week. These Western blot observations were corroborated by immunocytochemistry on frozen sections, which also revealed a major distribution of both p75 and Trks on neuronal bodies while p75 appears localized on supporting cells. Our findings reveal a tight correlation between p75 and Trks expression throughout human development and specific inner ear developmental events, such as target-dependent neuron

Published

1999

3. Organoculture of otic vesicle and ganglion.

Author

Garrido JJ, Schimmang T, Represa J, and Giraldez F

Subjects

Animals, Chick Embryo, Ear, Inner cytology, Ganglia, Parasympathetic cytology, Organ Culture Techniques methods, Ear, Inner embryology, Ganglia, Parasympathetic embryology

Published

1998

4. Survival of inner ear sensory neurons in trk mutant mice.

Author

Schimmang T, Alvarez-Bolado G, Minichiello L, Vazquez E, Giraldez F, Klein R, and Represa J

Subjects

Animals, Base Sequence, Cell Survival, Cochlea growth & development, Cochlea innervation, DNA Primers genetics, Ear, Inner growth & development, In Situ Hybridization, Mice, Mice, Knockout, Phenotype, Proto-Oncogene Proteins metabolism, Receptor, Ciliary Neurotrophic Factor, Receptor, trkA, Receptor, trkC, Receptors, Nerve Growth Factor genetics, Receptors, Nerve Growth Factor metabolism, Vestibule, Labyrinth growth & development, Vestibule, Labyrinth innervation, Ear, Inner innervation, Neurons, Afferent cytology, Neurons, Afferent enzymology, Receptor Protein-Tyrosine Kinases genetics, Receptor Protein-Tyrosine Kinases metabolism

Abstract

Analysis of trkB-/-; trkC-/- double mutant mice revealed that peripheral and central inner ear sensory neurons are affected in these mice. However, a substantial amount of cochlear and vestibular neurons survive, possibly due to maintenance or upregulation of TrkA expression. To clarify the function of the TrkA receptor during development of the cochlear and vestibular ganglion we analysed trkA-/- mice and the expression of this receptor in inner ear sensory neurons of trkB-/-; trkC-/- animals. TrkA homozygous mutant mice showed normal numbers of neurons and no TrkA expression was detected in neurons of trkB-/-; trkC-/- double mutant mice. We conclude that TrkA is not essential for inner ear development and that in the absence of any of the known catalytic Trk receptors peripheral inner ear sensory neurons are prone to undergo cell death or must use a different signaling mechanism to survive.

Published

1997

5. Developmental regulation of Fos-protein during proliferative growth of the otic vesicle and its relation to differentiation induced by retinoic acid.

Author

León Y, Sanchez JA, Miner C, Ariza-McNaughton L, Represa JJ, and Giraldez F

Subjects

Animals, Base Sequence, Cell Differentiation drug effects, Cell Division, Chick Embryo, Ear, Inner metabolism, Growth Substances pharmacology, Molecular Sequence Data, Ear, Inner embryology, Proto-Oncogene Proteins c-fos biosynthesis, Tretinoin pharmacology

Abstract

This work studies Fos protein expression in the otic vesicle and the developing cochleovestibular ganglion (CVG), focusing on the possible role of Fos in the regulation of cell proliferation and differentiation during otic development. Fos was detected as a product of 56-62 kDa in otic vesicles and CVG lysates. Expression was transient and stage-dependent. Maximal levels occurred at stage 20 in the otic vesicle and at Day 4 in the CVG. Another wave of Fos expression occurred after Day 7 of development, out of the early proliferative period. Fos immunoreactivity was localized in cell nuclei of otic epithelium and CVG. Fos was readily induced by mitogens like serum and bombesin and this induction was inhibited by 25 nM retinoic acid, an inhibitor of cell proliferation in the otic vesicle.c-fos antisense oligonucleotides inhibited growth in the otic vesicle in parallel with a reduction in Fos expression. High levels of Fos protein were not sufficient, however, to sustain growth of isolated otic vesicles in the absence of mitogens. Incubation with retinoic acid (24 hr) induced differentiation of sensory hair-cells in parallel with inhibition of cell proliferation. Contrary to retinoic acid, Fos inhibition by antisense did not induce differentiation. The results suggest that Fos is part of the signaling mechanisms regulating normal development of the inner ear. Regulation of Fos may be required for controlling of the transition between cell proliferation and differentiation.

Published

1995

6. Octreotide infusion versus injection sclerotherapy.

Author

Mayol Martinez J and Fernández-Represa JA

Subjects

Humans, Infusions, Intravenous, Injections, Research Design, Esophageal and Gastric Varices therapy, Gastrointestinal Hemorrhage therapy, Octreotide therapeutic use, Sclerotherapy

Published

1993

7. Brain-derived neurotrophic factor and neurotrophin-3 induce cell proliferation in the cochleovestibular ganglion through a glycosyl-phosphatidylinositol signaling system.

Author

Represa J, Avila MA, Romero G, Mato JM, Giraldez F, and Varela-Nieto I

Subjects

Animals, Antibodies immunology, Brain-Derived Neurotrophic Factor, Cell Division, Chick Embryo, Cochlear Nerve cytology, Culture Techniques, Ganglia cytology, Ganglia metabolism, Glycosylphosphatidylinositols immunology, Inositol Phosphates immunology, Kinetics, Neurotrophin 3, Polysaccharides immunology, Vestibular Nerve cytology, Cochlear Nerve metabolism, Glycosylphosphatidylinositols metabolism, Nerve Growth Factors physiology, Nerve Tissue Proteins physiology, Signal Transduction, Vestibular Nerve metabolism

Abstract

We have investigated the role of brain-derived neurotrophic factor (BDNF) and neurotrophin-3 (NT-3) in the regulation of cell proliferation in the early developing cochleovestibular ganglion (CVG). Ganglia were isolated from 72-hr chick embryos and cultured for 24 hr. Both BDNF and NT-3 had a powerful mitogenic effect, at doses of 1-5 ng/ml, consistent with an involvement of the high-affinity receptor. Evidence for the participation of the glycosyl-phosphatidylinositol (GPI)/inositol phosphoglycan (IPG) signaling system in the mediation of proliferative effects of BDNF and NT-3 is presented. Both of these neurotrophins elicited a fast and transient hydrolysis of labeled GPI, approximately 60% in 30 sec. The dose-response profile of GPI hydrolysis overlaps the neurotrophin-induced cell proliferation response profile. Anti-IPG antibodies were able to block the growth-promoting effects of BDNF and NT-3. Anti-IPG antibodies immunoprecipitated a CVG-endogenous IPG, induced upon BDNF treatment, which exhibited proliferative stimulating properties. Both BDNF and NT-3 are proposed as potential candidates for regulation of growth during CVG development, with this mitogenic effect being mediated by the GPI/IPG signaling system.

Published

1993

8. Brain-derived neurotrophic factor and neurotrophin-3 support the survival and neuritogenesis response of developing cochleovestibular ganglion neurons.

Author

Avila MA, Varela-Nieto I, Romero G, Mato JM, Giraldez F, Van De Water TR, and Represa J

Subjects

Animals, Antibodies immunology, Brain-Derived Neurotrophic Factor, Cell Differentiation, Cell Survival, Chick Embryo, Cochlear Nerve growth & development, Culture Techniques, Ear, Inner growth & development, Ear, Inner innervation, Ganglia cytology, Glycosylphosphatidylinositols metabolism, Inositol Phosphates immunology, Inositol Phosphates metabolism, Neurons cytology, Neurotrophin 3, Polysaccharides immunology, Polysaccharides metabolism, Signal Transduction, Vestibular Nerve growth & development, Cochlear Nerve cytology, Nerve Growth Factors physiology, Nerve Tissue Proteins physiology, Neurites, Vestibular Nerve cytology

Abstract

The effects of brain-derived neurotrophic factor (BDNF) and neurotrophin-3 (NT-3) on the differentiation of avian cochleovestibular ganglion and their possible association with the hydrolysis of glycosyl-phosphatidylinositol (GPI) were studied. BDNF and NT-3 (2 ng/ml) promoted neurite outgrowth in explants of both cochlear and vestibular ganglia. This effect on neuritogenesis was stage-dependent, reaching a maximum at E7 for NT-3 and at E9 for BDNF. The magnitude of the response of the vestibular ganglion to BDNF was always smaller than that of the cochlear ganglion of an equivalent stage. BDNF and NT-3 stimulation of neuronal survival and neurite extension was also demonstrated in dissociated neuronal cell cultures. The effect was concentration-dependent with saturation of the response occurring at 4 ng/ml for BDNF and at 2 ng/ml for NT-3, the half-maximal effect occurring at 2 and 1 ng/ml, respectively, for the most sensitive stages of the chick cochlear ganglion. Inositol phosphoglycan (IPG) did not mimic the effects of BDNF or NT-3 on neuronal survival and neurite outgrowth, nor was it able to potentiate their responses. Antibodies raised against IPG did not block the effects of these neurotrophins. The results suggest that BDNF and NT-3 may act in cooperation to establish the innervation pattern of the inner ear. Unlike their early proliferative effects, neurotrophic effects are uncoupled from the GPI/IPG signal transduction system.

Published

1993

9. Myb p75 oncoprotein is expressed in developing otic and epibranchial placodes.

Author

León Y, Miner C, Represa J, and Giraldez F

Subjects

Animals, Chick Embryo, Gene Expression, Immunohistochemistry, Oncogene Proteins v-myb, Time Factors, Ear embryology, Ectoderm metabolism, Retroviridae Proteins, Oncogenic analysis

Abstract

The c-myb proto-oncogene encodes a transcriptional regulatory protein which is highly conserved throughout evolution. Myb has been considered to be normally restricted to hematopoietic tissues, but there are indications that this might not always be the case. The present work shows the expression of a p75 Myb oncoprotein in the otic vesicle and epibranchial placodes of the early chick embryo. Expression was sequential and followed the same time course as the formation of placode-derived cranial ganglia. The results suggest a potential role for c-myb in regulation of placode development and neurogenesis.

Published

1992

10. Inositol phospho-oligosaccharide stimulates cell proliferation in the early developing inner ear.

Author

Varela-Nieto I, Represa J, Avila MA, Miner C, Mato JM, and Giraldez F

Subjects

Animals, Cell Division drug effects, Chick Embryo, Culture Techniques, Ear, Inner cytology, Insulin pharmacology, Nerve Growth Factors pharmacology, Ear, Inner embryology, Inositol Phosphates pharmacology, Oligosaccharides pharmacology

Abstract

The ability of an inositol phospho-oligosaccharide (POS) to mimic the mitogenic effects of nerve growth factor (NGF) and insulin on the early development of the inner ear was investigated. POS (10 microM) stimulated the incorporation of [3H]thymidine into the cochleovestibular ganglion by 3.9-fold. NGF (50 ng/ml) stimulation was 4.7-fold. POS and NGF showed no additivity. Cells induced to proliferate by POS overlapped with those expressing NGF receptors. POS, like insulin, potentiated the mitogenic effect of bombesin on the otic vesicle epithelium. DNA synthesis in the presence of bombesin (100 nM) plus POS (10 microM) was increased by 6.4-fold. POS stimulation was not additive with insulin. The results suggest that POS may play a role in growth factor regulation of cell proliferation during embryonic development.

Published

1991

11. Nerve growth factor and serum differentially regulate development of the embryonic otic vesicle and cochleovestibular ganglion in vitro.

Author

Represa J and Bernd P

Subjects

Amiloride pharmacology, Animals, Cell Differentiation, Cell Division, Cell Survival, Culture Techniques, DNA biosynthesis, Dose-Response Relationship, Drug, Ear, Inner metabolism, Nerve Growth Factors administration & dosage, Protein Biosynthesis, Spiral Ganglion metabolism, Blood, Cochlea embryology, Coturnix embryology, Ear, Inner embryology, Nerve Growth Factors pharmacology, Quail embryology, Spiral Ganglion embryology

Abstract

The preceding paper (P. Bernd and J. Represa, 1989, Dev. Biol. 134) describes the characterization and localization of nerve growth factor (NGF) receptors in inner ear primordia, the otic vesicle (OV) and cochleovestibular ganglion (CVG), obtained from 72-hr (stage 19-20) quail embryos. The studies described in this paper investigated whether NGF serves as a mitogen, a survival factor, and/or a differentiation factor in this system. Explants of isolated OV and CVG were maintained for 24 hr in serum-free medium alone (M-199), M-199 containing serum, M-199 containing NGF, or M-199 containing both serum and NGF. [3H]Thymidine was also present for the entire culture period. Both OV and CVG incorporated greater amounts of [3H]thymidine in the presence of serum or NGF, and their combined effect was additive. NGF's effects were dose dependent, saturable, and specific (blocked by anti-NGF). NGF caused little or no morphological differentiation of OV and no increase in protein levels, in contrast to OV grown in the presence of serum. CVG had both cochlear and vestibular portions present in all cases, but the apparent size and protein content of CVG was increased in the presence of either serum or NGF. Effects of serum and NGF were completely, but reversibly, blocked by amiloride, suggesting that the Na+-H+ exchange system had been activated. In order to determine whether increases in [3H]thymidine incorporation were due to increased cell survival or perhaps to an increase in proliferation, explants were initially grown for a 24-hr period in serum-free medium, followed by reactivation for an additional 24 hr in medium containing serum and/or NGF. It is likely that cells requiring either serum or NGF for survival would die during a 24-hr period in their absence. Our results revealed that the level of [3H]thymidine incorporation in OV was the same after reactivation. In the case of CVG, only NGF treatment yielded similar results; [3H]thymidine incorporation was lower in CVG reactivated with serum. It appears, therefore, that serum has probable proliferative effects upon OV and CVG, as well as survival effects for CVG. NGF, however, does not appear to affect survival in either OV or CVG, so that increases in [3H]thymidine incorporation in response to NGF are most likely due to proliferative effects upon OV or CVG, at least at this embryonic stage.

Published

1989

12. Characterization and localization of nerve growth factor receptors in the embryonic otic vesicle and cochleovestibular ganglion.

Author

Bernd P and Represa J

Subjects

Animals, Autoradiography, Ear, Inner analysis, Iodine Radioisotopes, Male, Mice, Nerve Growth Factors metabolism, Receptors, Cell Surface metabolism, Receptors, Nerve Growth Factor, Spiral Ganglion analysis, Tissue Distribution, Cochlea embryology, Coturnix embryology, Ear, Inner embryology, Quail embryology, Receptors, Cell Surface analysis, Spiral Ganglion embryology

Abstract

We have investigated the possibility that nerve growth factor (NGF) may play a role in the development of the inner ear. Primordia of the inner ear, the otic vesicle (OV) and cochleovestibular ganglion (CVG), were isolated from 72-hr (stage 19-20) quail embryos and examined for the presence of NGF receptors. Quantitative binding studies revealed that both OV and CVG exhibited specific 125I-NGF binding; levels of nonspecific binding were 6 to 26% of total binding. Scatchard analysis yielded a linear plot, indicating the presence of a single class of NGF receptor. The average binding constant (Kd) was 8.0 nM for OV and 8.6 nM for CVG, corresponding to the low affinity (site II) NGF receptor. Examination of light microscopic radioautographs indicated that most of the specific 125I-NGF binding was located in the ventromedial wall of the OV, with little or no binding in the lateral wall and endolymphatic primordia. These studies were corroborated by microdissection of OV, in which 70% of the radioactivity was found to be localized in the medial half of the OV. In CVG, specific 125I-NGF binding was more concentrated in the cochlear portion of the ganglion, with silver grains primarily over areas containing support cells and immature neurons. Quantitative binding studies with isolated cochlear and vestibular ganglia obtained from 144-hr (stage 29-30) quail embryos revealed that the cochlear ganglion exhibited three times more specific 125I-NGF binding than the vestibular ganglion. The presence of NGF receptors on OV and CVG suggests that these structures are responsive to and/or dependent upon NGF. The following paper (J. Represa and P. Bernd, 1989, Dev. Biol. 134) examines the question of whether NGF serves either as a mitogen, a survival factor, or a differentiation factor in this system.

Published

1989