RDH10, RALDH2, and CRABP2 are required components of PPARγ-directed ATRA synthesis and signaling in human dendritic cells

Gyöngyösi, Adrienn; Szatmári, István; Pap, Attila; Dezső, Balázs; Pós, Zoltán; Széles, Lajos; Varga, Tamás; Nagy, László

doi:10.1194/jlr.m038984

Cited by 27 publications

(27 citation statements)

References 66 publications

(104 reference statements)

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“…Outside of the gut, examination of peripheral DC subsets have identified DCs expressing aldh1a2 residing in the lung and skin, pointing to a role for RA in steady‐state immune responses at barrier sites . Although the majority of peripheral DCs express negligible or low levels of RALDH, the identification of cytokines and pathogen‐associated molecular patterns that can induce RALDH expression indicates that RA synthesis and signaling may be a widespread occurrence during the course of a peripheral immune response.…”

Section: Retinoic Acid: Mucosal Immunity and Beyondmentioning

confidence: 99%

Seeing through the dark: New insights into the immune regulatory functions of vitamin A

2015

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Summary The importance of vitamin A for host defense is undeniable and the study of its mechanisms is paramount. Of the estimated 250 million preschool children who are vitamin A deficient (VAD), 10% will die from their increased susceptibility to infectious disease. Vitamin A supplementation was established in the 1980s as one of the most successful interventions in the developing world. Understanding how Vitamin A controls immunity will curb the mortality and morbidity associated with VAD and exploit the immune enhancing capacity of vitamin A to heighten host resistance to infectious disease. The discoveries that retinoic acid (RA) imprints the homing of leukocytes to the gut and enhanced the induction of regulatory T-cells highlighted a potential role for RA in mucosal tolerance. However, emerging data tells of a more profound systemic impact of RA on leukocyte function and commitment. In animal models using genetic manipulation of RA signaling, we learn when and how RA controls T-cell fate. Here we review the role for RA as a critical checkpoint regulator in the differentiation of CD4+ T-cells within the immune system.

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Section: Retinoic Acid: Mucosal Immunity and Beyondmentioning

confidence: 99%

Seeing through the dark: New insights into the immune regulatory functions of vitamin A

2015

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“…Thus, DC RA production is thought to contribute to intestinal tolerance to commensal bacteria and dietary antigens. RA is generated from retinol (ROL, Vitamin A) through a two-step reaction, the first step involving oxidation of ROL to retinal by a retinol dehydrogenase, most importantly RDH10, and the second step involving further oxidation of retinal to all- trans RA by tissue-specific isoforms of retinaldehyde dehydrogenase, RALDH1, RALDH2 and RALDH3 ( 9 ). The ability of intestinal DCs to generate RA depends on tissue-specific crosstalk between epithelial cells and DCs.…”

Section: Introductionmentioning

confidence: 99%

Human gastric epithelial cells contribute to gastric immune regulation by providing retinoic acid to dendritic cells

et al. 2015

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Despite the high prevalence of chronic gastritis caused by H. pylori, the gastric mucosa has received little investigative attention as a unique immune environment. Here, we analyzed whether retinoic acid (RA), an important homeostatic factor in the small intestinal mucosa, also contributes to gastric immune regulation. We report that human gastric tissue contains high levels of the RA precursor molecule, retinol, and that gastric epithelial cells express both RA biosynthesis genes and RA response genes, indicative of active RA biosynthesis. Moreover, primary gastric epithelial cells cultured in the presence of retinol synthesized RA in vitro and induced RA biosynthesis in co-cultured monocytes through an RA-dependent mechanism, suggesting that gastric epithelial cells may also confer the ability to generate RA on gastric DCs. Indeed, DCs purified from gastric mucosa had similar levels of aldehyde dehydrogenase activity and RA biosynthesis gene expression as small intestinal DCs, although gastric DCs lacked CD103. In H. pylori-infected gastric mucosa, gastric RA biosynthesis gene expression was severely disrupted, which may lead to reduced RA signaling and thus contribute to disease progression. Collectively, our results support a critical role for RA in human gastric immune regulation.

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“…However, the wide RDH10 tissue distribution (Cammas et al 2007;Picozzi et al 2003;Shou et al 2005) and its activity leading to an increase of retinynaldehyde and retinoic acid concentration (Belyaeva et al 2008) suggest a role for this enzyme also in embryonic development and differentiation (Ashique et al 2012;Rhinn et al 2011;Sandell et al 2007). This role was further confirmed by recent studies linking RDH10 to DHRS3 (Adams et al 2014) or to PPAR␥ activity (Gyongyosi et al 2013). It is thus well established that RDH10 has a dual function in the retinoid metabolism.…”

Section: Knockout Mice For the Functional Investigation Of Retinol Dementioning

confidence: 52%

Retinol dehydrogenases: Membrane-bound enzymes for the visual function

Lhor

Salesse

2014

Biochem. Cell Biol.

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Retinoid metabolism is important for many physiological functions, such as differenciation, growth, and vision. In the visual context, after the absorption of light in rod photoreceptors by the visual pigment rhodopsin, 11-cis retinal is isomerized to all-trans retinal. This retinoid subsequently undergoes a series of modifications during the visual cycle through a cascade of reactions occurring in photoreceptors and in the retinal pigment epithelium. Retinol dehydrogenases (RDHs) are enzymes responsible for crucial steps of this visual cycle. They belong to a large family of proteins designated as short-chain dehydrogenases/reductases. The structure of these RDHs has been predicted using modern bioinformatics tools, which allowed to propose models with similar structures including a common Rossman fold. These enzymes undergo oxidoreduction reactions, whose direction is dictated by the preference and concentration of their individual cofactor (NAD(H)/NADP(H)). This review presents the current state of knowledge on functional and structural features of RDHs involved in the visual cycle as well as knockout models. RDHs are described as integral or peripheral enzymes. A topology model of the membrane binding of these RDHs via their N- and (or) C-terminal domain has been proposed on the basis of their individual properties. Membrane binding is a crucial issue for these enzymes because of the high hydrophobicity of their retinoid substrates.

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RDH10, RALDH2, and CRABP2 are required components of PPARγ-directed ATRA synthesis and signaling in human dendritic cells

Cited by 27 publications

References 66 publications

Seeing through the dark: New insights into the immune regulatory functions of vitamin A

Seeing through the dark: New insights into the immune regulatory functions of vitamin A

Human gastric epithelial cells contribute to gastric immune regulation by providing retinoic acid to dendritic cells

Retinol dehydrogenases: Membrane-bound enzymes for the visual function

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