Artículo
Organization of nuclear architecture during adipocyte differentiation
Charó, Nancy Lorena
; Rodríguez Ceschan, María I.; Galigniana, Natalia Maricel
; Toneatto, Judith
; Piwien Pilipuk, Graciela
Fecha de publicación:
05/2016
Editorial:
Taylor & Francis
Revista:
Nucleus
ISSN:
1949-1034
Idioma:
Inglés
Tipo de recurso:
Artículo publicado
Clasificación temática:
Resumen
Obesity is a serious health problem worldwide since it is a major risk factor for chronic diseases such as type II diabetes. Obesity is the result of hyperplasia (associated with increased adipogenesis) and hypertrophy (associated with decreased adipogenesis) of the adipose tissue. Therefore, understanding the molecular mechanisms underlying the process of adipocyte differentiation is relevant to delineate new therapeutic strategies for treatment of obesity. As in all differentiation processes, temporal patterns of transcription are exquisitely controlled, allowing the acquisition and maintenance of the adipocyte phenotype. The genome is spatially organized; therefore decoding local features of the chromatin language alone does not suffice to understand how cell type-specific gene expression patterns are generated. Elucidating how nuclear architecture is built during the process of adipogenesis is thus an indispensable step to gain insight in how gene expression is regulated to achieve the adipocyte phenotype. Here we will summarize the recent advances in our understanding of the organization of nuclear architecture as progenitor cells differentiate in adipocytes, and the questions that still remained to be answered.
Palabras clave:
ADIPOGENESIS
,
CHROMOSOME TERRITORY
,
NUCLEAR LAMINA
,
NUCLEOSKELETON
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Colecciones
Articulos(IBYME)
Articulos de INST.DE BIOLOGIA Y MEDICINA EXPERIMENTAL (I)
Articulos de INST.DE BIOLOGIA Y MEDICINA EXPERIMENTAL (I)
Citación
Charó, Nancy Lorena; Rodríguez Ceschan, María I.; Galigniana, Natalia Maricel; Toneatto, Judith; Piwien Pilipuk, Graciela; Organization of nuclear architecture during adipocyte differentiation; Taylor & Francis; Nucleus; 7; 3; 5-2016; 249-269
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