Your search keyword '"Blanco, Enrique J."' showing total 2 results

1. The expression of AIB1 correlates with cellular proliferation in human prolactinomas.

Author

Carretero, José, Blanco, Enrique J., Carretero, Manuel, Carretero-Hernández, Marta, García-Barrado, Mª José, Iglesias-Osma, Mª Carmen, Burks, Deborah Jane, and Font de Mora, Jaime

Subjects

CELL proliferation, GENE expression, PROLACTINOMA, ESTROGEN, GROWTH factors, MOLECULAR biology, STEROID receptor coactivators

Abstract

Summary: Estrogens as well as certain growth factors strongly influence the development and growth of prolactinomas. However, the molecular mechanisms by which extracellular factors trigger prolactinomas are not well known. Amplified in breast cancer 1 (AIB1), also known as steroid receptor co-activator 3 (SRC-3), belongs to the p160/SRC family of nuclear receptor co-activators and is a major co-activator of the estrogen receptor. Here, we report that the estrogen receptor coactivator AIB1 is overexpressed in human prolactinomas and correlates with the detection of aromatase and estrogen receptor α (ERα). Of the 87 pituitary tumors evaluated in women, 56%, corresponding to hyperoprolactinemic women, contained an enriched population of prolactin-positive cells and hence were further classified as prolactinomas. All prolactinomas stained positive for both ERα and AIB1. Moreover, AIB1 sub-cellular distribution was indicative of the cell-cycle status of tumors; the nuclear expression of AIB1 was correlated with proliferative markers whereas the cytoplasmic localization of AIB1 coincided with active caspase-3. Thus, our results demonstrate for the first time that AIB1 is expressed in prolactinomas and suggest its participation in the regulation of proliferation and apoptosis of tumoral cells. Because aromatase expression is also enhanced in these prolactinomas and it is involved in the local production of estradiol, both mechanisms, ER-AIB1 and aromatase could be related. [Copyright &y& Elsevier]

Published

2013

2. The lack of Irs2 induces changes in the immunocytochemical expression of aromatase in the mouse retina.

Author

Iglesias-Osma, Maria Carmen, Blanco, Enrique J., Carretero-Hernández, Marta, Catalano-Iniesta, Leonardo, García-Barrado, Maria Jose, Sánchez-Robledo, Virginia, Blázquez, Juan Luis, and Carretero, Jose

Subjects

AROMATASE, RETINA, PHOTORECEPTORS, GLUTAMINE synthetase, INSULIN receptors, TYROSINE hydroxylase

Abstract

• We studied retinal neuromodulators expression in normoglycemic Irs2-deficient mice. • Expression of P450 Aromatase in the retinal layers was significantly increased. • Müller cells showed decreased immunocytochemical expression for GS. • A reduced immunopositive reaction for TH was observed in the amacrine cells. • Aromatase could promote local neuroprotective mediators for repairing retina damage. Insulin receptor substrate (Irs) belongs to a family of proteins that mediate the intracellular signaling of insulin and IGF-1. Insulin receptor substrate 2 (Irs2) is necessary for retinal function, since its failure in Irs2-deficient mice in hyperglycemic situation promotes photoreceptor degeneration and visual dysfunction, like in diabetic retinopathy. The expression of P450 aromatase, which catalyzes androgen aromatization to form 17ß-estradiol, increases in some neurodegenerative diseases thus promoting the local synthesis of neuroestrogens that exert relevant neuroprotective functions. Aromatase is also expressed in neurons and glial cells of the central nervous system (CNS), including the retina. To further understand the role of Irs2 at the retinal level, we performed an immunocytochemical study in adult normoglycemic Irs2-deficient mice. For this aim, the retinal immunoexpression of neuromodulators, such as aromatase, glutamine synthetase (GS), and tyrosine hydroxylase (TH) was analyzed, joint to a morphometric and planimetric study of the retinal layers. Comparing with wild-type (WT) control mice, the Irs2-knockout (Irs2-KO) animals showed a significant increase in the immunopositivity to aromatase in almost all of the retinal layers. Besides, Irs2-KO mice exhibited a decreased immunopositive reaction for GS and TH, in Müller and amacrine cells, respectively; morphological variations were also found in these retinal cell types. Furthermore, the retina of Irs2-KO mice displayed alterations in the structural organization, and a generalized decrease in the retinal thickness was observed in each of the layers, except for the inner nuclear layer. Our findings suggest that the absence of Irs2 induces retinal neurodegenerative changes in Müller and amacrine cells that are unrelated to hyperglycemia. Accordingly, in the Irs2-KO mice, the increased retinal immunocytochemical reactivity of aromatase could be associated with an attempt to repair such neural retina injuries by promoting local neuroprotective mediators. [ABSTRACT FROM AUTHOR]

Published

2022