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  1. AU="Carsten C. Scholz" AU="Carsten C. Scholz"
  2. AU=Taabazuing Cornelius Y.
  3. AU="Korenchenko, A. S."
  4. AU=Qi Maosong
  5. AU="Tian, Mengting"
  6. AU="Ghosh, Debdatta"
  7. AU="Madheswaran, Suresh"
  8. AU=Rogerio Alexandre de Paula
  9. AU=Warshaw A L
  10. AU="Waqar Ahmed"
  11. AU="Harper, William A."
  12. AU="Fargo, Keith"
  13. AU=Reed Matthew J
  14. AU="Harris, Hannah L"
  15. AU="Asahi, Hiroko"
  16. AU="Mohamed El Mohadab"
  17. AU="Jamjoom, Maan"
  18. AU="Benjamin K. Harley"
  19. AU="Redpath, Stephanie"
  20. AU="Costa Oliveira, Diogo"
  21. AU="Ibarra-Meneses, Ana Victoria"
  22. AU=Ozgenel Guzin Yesim
  23. AU="Shu-Ying Li"
  24. AU="Umemura, Yutaka"
  25. AU=Eiring A M
  26. AU="Eunhee Ha"
  27. AU="Espíndola, Otávio M"
  28. AU=Shahbazian Heshmatollah
  29. AU="Esmaeel Panahi kokhdan"
  30. AU=Peekhaus N
  31. AU="Ferrari-Toniolo, Simone"
  32. AU="Oleg M. Mikhailenok"

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  1. Artikel ; Online: The Deubiquitinase OTUB1 Is a Key Regulator of Energy Metabolism

    Amalia Ruiz-Serrano / Christina N. Boyle / Josep M. Monné Rodríguez / Julia Günter / Agnieszka E. Jucht / Svende Pfundstein / Andreas M. Bapst / Thomas A. Lutz / Roland H. Wenger / Carsten C. Scholz

    International Journal of Molecular Sciences, Vol 23, Iss 1536, p

    2022  Band 1536

    Abstract: Dysregulated energy metabolism is a major contributor to a multitude of pathologies, including obesity and diabetes. Understanding the regulation of metabolic homeostasis is of utmost importance for the identification of therapeutic targets for the ... ...

    Abstract Dysregulated energy metabolism is a major contributor to a multitude of pathologies, including obesity and diabetes. Understanding the regulation of metabolic homeostasis is of utmost importance for the identification of therapeutic targets for the treatment of metabolically driven diseases. We previously identified the deubiquitinase OTUB1 as substrate for the cellular oxygen sensor factor-inhibiting HIF (FIH) with regulatory effects on cellular energy metabolism, but the physiological relevance of OTUB1 is unclear. Here, we report that the induced global deletion of OTUB1 in adult mice ( Otub1 iKO) elevated energy expenditure, reduced age-dependent body weight gain, facilitated blood glucose clearance and lowered basal plasma insulin levels. The respiratory exchange ratio was maintained, indicating an unaltered nutrient oxidation. In addition, Otub1 deletion in cells enhanced AKT activity, leading to a larger cell size, higher ATP levels and reduced AMPK phosphorylation. AKT is an integral part of insulin-mediated signaling and Otub1 iKO mice presented with increased AKT phosphorylation following acute insulin administration combined with insulin hypersensitivity. We conclude that OTUB1 is an important regulator of metabolic homeostasis.
    Schlagwörter deubiquitinating enzyme ; energy expenditure ; insulin ; liver ; ubiquitin system ; FIH ; Biology (General) ; QH301-705.5 ; Chemistry ; QD1-999
    Thema/Rubrik (Code) 571
    Sprache Englisch
    Erscheinungsdatum 2022-01-01T00:00:00Z
    Verlag MDPI AG
    Dokumenttyp Artikel ; Online
    Datenquelle BASE - Bielefeld Academic Search Engine (Lebenswissenschaftliche Auswahl)

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  2. Artikel ; Online: Oxygen-dependent bond formation with FIH regulates the activity of the client protein OTUB1

    Christina Pickel / Julia Günter / Amalia Ruiz-Serrano / Patrick Spielmann / Jacqueline-Alba Fabrizio / Witold Wolski / Daniel J. Peet / Roland H. Wenger / Carsten C. Scholz

    Redox Biology, Vol 26, Iss , Pp - (2019)

    2019  

    Abstract: Protein:protein interactions are the basis of molecular communication and are usually of transient non-covalent nature, while covalent interactions other than ubiquitination are rare. For cellular adaptations, the cellular oxygen and peroxide sensor ... ...

    Abstract Protein:protein interactions are the basis of molecular communication and are usually of transient non-covalent nature, while covalent interactions other than ubiquitination are rare. For cellular adaptations, the cellular oxygen and peroxide sensor factor inhibiting HIF (FIH) confers oxygen and oxidant stress sensitivity to the hypoxia inducible factor (HIF) by asparagine hydroxylation. We investigated whether FIH contributes to hypoxia adaptation also through other mechanisms and identified a hypoxia sensitive, likely covalent, bond formation by FIH with several client proteins, including the deubiquitinase ovarian tumor domain containing ubiquitin aldehyde binding protein 1 (OTUB1). Biochemical analyses were consistent with a co-translational amide bond formation between FIH and OTUB1, occurring within mammalian and bacterial cells but not between separately purified proteins. Bond formation is catalysed by FIH and highly dependent on oxygen availability in the cellular microenvironment. Within cells, a heterotrimeric complex is formed, consisting of two FIH and one covalently linked OTUB1. Complexation of OTUB1 by FIH regulates OTUB1 deubiquitinase activity. Our findings reveal an alternative mechanism for hypoxia adaptation with remarkably high oxygen sensitivity, mediated through covalent protein-protein interactions catalysed by an asparagine modifying dioxygenase. Keywords: Hydroxylase, HIF, Hypoxia, Oxygen sensor, Deubiquitinase, Ubiquitin system
    Schlagwörter Medicine (General) ; R5-920 ; Biology (General) ; QH301-705.5
    Thema/Rubrik (Code) 610
    Sprache Englisch
    Erscheinungsdatum 2019-09-01T00:00:00Z
    Verlag Elsevier
    Dokumenttyp Artikel ; Online
    Datenquelle BASE - Bielefeld Academic Search Engine (Lebenswissenschaftliche Auswahl)

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  3. Artikel ; Online: FIH Regulates Cellular Metabolism through Hydroxylation of the Deubiquitinase OTUB1.

    Carsten C Scholz / Javier Rodriguez / Christina Pickel / Stephen Burr / Jacqueline-Alba Fabrizio / Karen A Nolan / Patrick Spielmann / Miguel A S Cavadas / Bianca Crifo / Doug N Halligan / James A Nathan / Daniel J Peet / Roland H Wenger / Alex Von Kriegsheim / Eoin P Cummins / Cormac T Taylor

    PLoS Biology, Vol 14, Iss 1, p e

    2016  Band 1002347

    Abstract: The asparagine hydroxylase, factor inhibiting HIF (FIH), confers oxygen-dependence upon the hypoxia-inducible factor (HIF), a master regulator of the cellular adaptive response to hypoxia. Studies investigating whether asparagine hydroxylation is a ... ...

    Abstract The asparagine hydroxylase, factor inhibiting HIF (FIH), confers oxygen-dependence upon the hypoxia-inducible factor (HIF), a master regulator of the cellular adaptive response to hypoxia. Studies investigating whether asparagine hydroxylation is a general regulatory oxygen-dependent modification have identified multiple non-HIF targets for FIH. However, the functional consequences of this outside of the HIF pathway remain unclear. Here, we demonstrate that the deubiquitinase ovarian tumor domain containing ubiquitin aldehyde binding protein 1 (OTUB1) is a substrate for hydroxylation by FIH on N22. Mutation of N22 leads to a profound change in the interaction of OTUB1 with proteins important in cellular metabolism. Furthermore, in cultured cells, overexpression of N22A mutant OTUB1 impairs cellular metabolic processes when compared to wild type. Based on these data, we hypothesize that OTUB1 is a target for functional hydroxylation by FIH. Additionally, we propose that our results provide new insight into the regulation of cellular energy metabolism during hypoxic stress and the potential for targeting hydroxylases for therapeutic benefit.
    Schlagwörter Biology (General) ; QH301-705.5
    Thema/Rubrik (Code) 610 ; 500
    Sprache Englisch
    Erscheinungsdatum 2016-01-01T00:00:00Z
    Verlag Public Library of Science (PLoS)
    Dokumenttyp Artikel ; Online
    Datenquelle BASE - Bielefeld Academic Search Engine (Lebenswissenschaftliche Auswahl)

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