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      Role of Zinc in the Development/Progression of Alcoholic Liver Disease

      , ,
      Current Treatment Options in Gastroenterology
      Springer Nature

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          Mammalian zinc transporters: nutritional and physiologic regulation.

          Research advances defining how zinc is transported into and out of cells and organelles have increased exponentially within the past five years. Research has progressed through application of molecular techniques including genomic analysis, cell transfection, RNA interference, kinetic analysis of ion transport, and application of cell and animal models including knockout mice. The knowledge base has increased for most of 10 members of the ZnT family and 14 members of the Zrt-, Irt-like protein (ZIP) family. Relative to the handling of dietary zinc is the involvement of ZnT1, ZIP4, and ZIP5 in intestinal zinc transport, involvement of ZIP10 and ZnT1 in renal zinc reabsorption, and the roles of ZIP5, ZnT2, and ZnT1 in pancreatic release of endogenous zinc. These events are major factors in regulation of zinc homeostasis. Other salient findings are the involvement of ZnT2 in lactation, ZIP14 in the hypozincemia of inflammation, ZIP6, ZIP7, and ZIP10 in metastatic breast cancer, and ZnT8 in insulin processing and as an autoantigen in diabetes.
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            Zinc homeostasis and signaling in health and diseases

            The essential trace element zinc (Zn) is widely required in cellular functions, and abnormal Zn homeostasis causes a variety of health problems that include growth retardation, immunodeficiency, hypogonadism, and neuronal and sensory dysfunctions. Zn homeostasis is regulated through Zn transporters, permeable channels, and metallothioneins. Recent studies highlight Zn’s dynamic activity and its role as a signaling mediator. Zn acts as an intracellular signaling molecule, capable of communicating between cells, converting extracellular stimuli to intracellular signals, and controlling intracellular events. We have proposed that intracellular Zn signaling falls into two classes, early and late Zn signaling. This review addresses recent findings regarding Zn signaling and its role in physiological processes and pathogenesis.
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              Testosterone therapy increases muscle mass in men with cirrhosis and low testosterone: A randomised controlled trial.

              Low testosterone and sarcopenia are common in men with cirrhosis and both are associated with increased mortality. Whether testosterone therapy in cirrhosis improves muscle mass and other outcomes is unknown.
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                Author and article information

                Journal
                Current Treatment Options in Gastroenterology
                Curr Treat Options Gastro
                Springer Nature
                1092-8472
                1534-309X
                June 2017
                April 26 2017
                June 2017
                : 15
                : 2
                : 285-295
                Article
                10.1007/s11938-017-0132-4
                6206836
                28447197
                49984b19-9a9b-4969-a53e-6639e8aa8eed
                © 2017

                http://www.springer.com/tdm

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