Por favor, use este identificador para citar o enlazar este ítem: http://repositorio.ufc.br/handle/riufc/10169
Tipo: Artigo de Periódico
Título : Intestinal cell kinase is a novel participant in intestinal cell signaling responses to protein malnutrition
Autor : Bolick, David T.
Chen, Tufeng
Alves, Luis Antonio de Oliveira
Tong, Yixin
Wu, Di
Joyner, Linwood T.
Oriá, Reinaldo B.
Guerrant, Richard L.
Fu, Zheng
Palabras clave : Deficiências Nutricionais;Cancro
Fecha de publicación : sep-2014
Editorial : Plos One
Citación : BOLICK, D. T. et al. Intestinal cell kinase is a novel participant in intestinal cell signaling responses to protein malnutrition. Plos One, v. 9, n. 9, p. e106902, set. 2014.
Abstract: Nutritional deficiency and stress can severely impair intestinal architecture, integrity and host immune defense, leading to increased susceptibility to infection and cancer. Although the intestine has an inherent capability to adapt to environmental stress, the molecular mechanisms by which the intestine senses and responds to malnutrition are not completely understood. We hereby report that intestinal cell kinase (ICK), a highly conserved serine/threonine protein kinase, is a novel component of the adaptive cell signaling responses to protein malnutrition in murine small intestine. Using an experimental mouse model, we demonstrated that intestinal ICK protein level was markedly and transiently elevated upon protein deprivation, concomitant with activation of prominent pro-proliferation and pro-survival pathways of Wnt/b-catenin, mammalian target of rapamycin (mTOR), mitogen-activated protein kinase (MAPK), and protein kinase B (PKB/Akt) as well as increased expression of intestinal stem cell markers. Using the human ileocecal epithelial cell line HCT-8 as an in vitro model, we further demonstrated that serum starvation was able to induce up-regulation of ICK protein in intestinal epithelial cells in a reversible manner, and that serum albumin partially contributed to this effect. Knockdown of ICK expression in HCT-8 cells significantly impaired cell proliferation and down-regulated active b-catenin signal. Furthermore, reduced ICK expression in HCT-8 cells induced apoptosis through a caspase-dependent mechanism. Taken together, our findings suggest that increased ICK expression/activity in response to protein deprivation likely provides a novel protective mechanism to limit apoptosis and support compensatory mucosal growth under nutritional stress.
URI : http://www.repositorio.ufc.br/handle/riufc/10169
ISSN : 1932-6203 Online
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