Your search keyword '"Rodríguez-León J"' showing total 2 results

1. Senescence-associated β-galactosidase activity in the developing avian retina.

Author

de Mera-Rodríguez JA, Álvarez-Hernán G, Gañán Y, Martín-Partido G, Rodríguez-León J, and Francisco-Morcillo J

Subjects

Animals, Biomarkers analysis, Birds, Cell Differentiation, Embryo, Nonmammalian, Neurons cytology, Retina cytology, Retina growth & development, Cellular Senescence, Retina embryology, beta-Galactosidase metabolism

Abstract

Background: Senescence-associated β-galactosidase (SA-β-GAL) histochemistry is the most commonly used biomarker of cellular senescence. These SA-β-GAL-positive cells are senescent embryonic cells that are usually removed by apoptosis from the embryo, followed by macrophage-mediated clearance., Results: Some authors have proposed that SA-β-GAL activity in differentiated neurons from young and adult mammals cannot be uniquely attributed to cell senescence, whether in vivo or in vitro. Using the developing visual system of the chicken as a model, the present study found that SA-β-GAL detected in the developing retina corresponded to lysosomal β-galactosidase activity, and that SA-β-GAL activity did not correlate with the chronotopographical distribution of apoptotic cells. However, SA-β-GAL staining in the undifferentiated retina coincided with the appearance of early differentiating neurons. In the laminated retina, SA-β-GAL staining was concentrated in the ganglion, amacrine, and horizontal cell layers. The photoreceptors and pigment epithelial cells also exhibited SA-β-GAL activity throughout retinal development. We have also found that SA-β-GAL staining strongly correlated p21 immunoreactivity., Conclusion: In conclusion, the results clearly show that SA-β-GAL activity cannot be regarded as a specific marker of senescence during retinal development, and that it is mainly expressed in subpopulations of postmitotic neurons, which are nonproliferative cells, even at early stages of cell differentiation., (© 2019 Wiley Periodicals, Inc.)

Published

2019

2. Ontogenetic cell death and phagocytosis in the visual system of vertebrates.

Author

Francisco-Morcillo J, Bejarano-Escobar R, Rodríguez-León J, Navascués J, and Martín-Partido G

Subjects

Animals, Cell Death genetics, Eye cytology, Humans, Morphogenesis genetics, Neurons physiology, Ocular Physiological Phenomena genetics, Phagocytosis genetics, Visual Pathways cytology, Visual Pathways embryology, Visual Pathways metabolism, Apoptosis genetics, Eye embryology, Phagocytosis physiology, Vertebrates embryology, Vertebrates genetics

Abstract

Programmed cell death (PCD), together with cell proliferation, cell migration, and cell differentiation, is an essential process during development of the vertebrate nervous system. The visual system has been an excellent model on which to investigate the mechanisms involved in ontogenetic cell death. Several phases of PCD have been reported to occur during visual system ontogeny. During these phases, comparative analyses demonstrate that dying cells show similar but not identical spatiotemporally restricted patterns in different vertebrates. Additionally, the chronotopographical coincidence of PCD with the entry of specialized phagocytes in some regions of the developing vertebrate visual system suggests that factors released from degenerating cells are involved in the cell migration of macrophages and microglial cells. Contradicting this hypothesis however, in many cases the cell corpses generated during degeneration are rapidly phagocytosed by neighboring cells, such as neuroepithelial cells or Müller cells. In this review, we describe the occurrence and the sites of PCD during the morphogenesis and differentiation of the retina and optic pathways of different vertebrates, and discuss the possible relationship between PCD and phagocytes during ontogeny., (Copyright © 2014 Wiley Periodicals, Inc.)

Published

2014