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Martijn O. Hoeke

University Medical Center Groningen

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Featured researches published by Martijn O. Hoeke.

PLOS ONE | 2014

Human FXR Regulates SHP Expression through Direct Binding to an LRH-1 Binding Site, Independent of an IR-1 and LRH-1

Martijn O. Hoeke; Janette Heegsma; Mark Hoekstra; Han Moshage; Klaas Nico Faber

Background Farnesoid X receptor/retinoid X receptor-alpha (FXR/RXRα) is the master transcriptional regulator of bile salt synthesis and transport in liver and intestine. FXR is activated by bile acids, RXRα by the vitamin A–derivative 9-cis retinoic acid (9cRA). Remarkably, 9cRA inhibits binding of FXR/RXRα to its response element, an inverted repeat-1 (IR-1). Still, most FXR/RXRα target genes are maximally expressed in the presence of both ligands, including the small heterodimer partner (SHP). Here, we revisited the FXR/RXRα-mediated regulation of human SHP. Methods A 579-bp hSHP promoter element was analyzed to locate FXR/chenodeoxycholic acid (CDCA)- and RXRα/9cRA-responsive elements. hSHP promoter constructs were analyzed in FXR/RXRα-transfected DLD-1, HEK293 and HepG2 cells exposed to CDCA, GW4064 (synthetic FXR ligand) and/or 9cRA. FXR-DNA interactions were analyzed by in vitro pull down assays. Results hSHP promoter elements lacking the previously identified IR-1 (−291/−279) largely maintained their activation by FXR/CDCA, but were unresponsive to 9cRA. FXR-mediated activation of the hSHP promoter was primarily dependent on the −122/−69 region. Pull down assays revealed a direct binding of FXR to the −122/−69 sequence, which was abrogated by site-specific mutations in a binding site for the liver receptor homolog-1 (LRH-1) at −78/−70. These mutations strongly impaired the FXR/CDCA-mediated activation, even in the context of a hSHP promoter containing the IR-1. LRH-1 did not increase FXR/RXRα-mediated activation of hSHP promoter activity. Conclusion FXR/CDCA-activated expression of SHP is primarily mediated through direct binding to an LRH-1 binding site, which is not modulated by LRH-1 and unresponsive to 9cRA. 9cRA-induced expression of SHP requires the IR-1 that overlaps with a direct repeat-2 (DR-2) and DR-4. This establishes for the first time a co-stimulatory, but independent, action of FXR and RXRα agonists.

Biochimica et Biophysica Acta | 2017

The interrelationship between bile acid and vitamin A homeostasis

Ali Saeed; Mark Hoekstra; Martijn O. Hoeke; Janette Heegsma; Klaas Nico Faber

Hepatology | 2004

Low retinol levels potentiate bile acid-induced expression of the bile salt export pump in vitro and in vivo

[No Value] Plass; Martijn O. Hoeke; Mariska Geuken; Janette Heegsma; D van Rijsbergen; Julius F. W. Baller; Folkert Kuipers; Plm Jansen; Klaas Nico Faber

Hepatology | 2011

IDENTIFICATION OF A NOVEL FXR RESPONSE ELEMENT; HUMAN FXR INDUCES SHP EXPRESSION THROUGH DIRECT BINDING TO AN LRH-1 BINDING SITE, INDEPENDENT OF THE PRESENCE OF AN IR-1 AND LRH-1

Martijn O. Hoeke; Mark Hoekstra; Janette Heegsma; Han Moshage; Klaas Nico Faber

Hepatology | 2011

Vitamin A deficiency results in an uncontrolled immune response and aggravates liver damage during obstructive cholestasis

Mark Hoekstra; Martijn O. Hoeke; Janette Heegsma; Vincent W. Bloks; Albert Moshage; Klaas Nico Faber

Cellular Oncology | 2009

Low retinol levels differentially modulate bile salt-induced expression of human and mouse hepatic bile salt transporters

Martijn O. Hoeke; Jacqueline R. M. Plass; Janette Heegsma; Mariska Geuken; Duncan van Rijsbergen; Julius F. W. Baller; Folkert Kuipers; Han Moshage; Peter L. M. Jansen; Klaas Nico Faber

Hepatology | 2008