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      Slc25a17 Gene Trapped Mice: PMP34 Plays a Role in the Peroxisomal Degradation of Phytanic and Pristanic Acid

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          Abstract

          Mice lacking PMP34, a peroxisomal membrane transporter encoded by Slc25a17, did not manifest any obvious phenotype on a Swiss Webster genetic background, even with various treatments designed to unmask impaired peroxisomal functioning. Peroxisomal α- and β-oxidation rates in PMP34 deficient fibroblasts or liver slices were not or only modestly affected and in bile, no abnormal bile acid intermediates were detected. Peroxisomal content of cofactors like CoA, ATP, NAD +, thiamine-pyrophosphate and pyridoxal-phosphate, based on direct or indirect data, appeared normal as were tissue plasmalogen and very long chain fatty acid levels. However, upon dietary phytol administration, the knockout mice displayed hepatomegaly, liver inflammation, and an induction of peroxisomal enzymes. This phenotype was partially mediated by PPARα. Hepatic triacylglycerols and cholesterylesters were elevated and both phytanic acid and pristanic acid accumulated in the liver lipids, in females to higher extent than in males. In addition, pristanic acid degradation products were detected, as wells as the CoA-esters of all these branched fatty acids. Hence, PMP34 is important for the degradation of phytanic/pristanic acid and/or export of their metabolites. Whether this is caused by a shortage of peroxisomal CoA affecting the intraperoxisomal formation of pristanoyl-CoA (and perhaps of phytanoyl-CoA), or the SCPx-catalyzed thiolytic cleavage during pristanic acid β-oxidation, could not be proven in this model, but the phytol-derived acyl-CoA profile is compatible with the latter possibility. On the other hand, the normal functioning of other peroxisomal pathways, and especially bile acid formation, seems to exclude severe transport problems or a shortage of CoA, and other cofactors like FAD, NAD(P) +, TPP. Based on our findings, PMP34 deficiency in humans is unlikely to be a life threatening condition but could cause elevated phytanic/pristanic acid levels in older adults.

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          Isolation of intracellular membranes by means of sodium carbonate treatment: application to endoplasmic reticulum

          S Fowler, Y Fujiki, P. Lazarow (1982)
          A rapid and simple method for the isolation of membranes from subcellular organelles is described. The procedure consists of diluting the organelles in ice-cold 100 mM Na2CO3 followed by centrifugation to pellet the membranes. Closed vesicles are converted to open membrane sheets, and content proteins and peripheral membrane proteins are released in soluble form. Here we document the method by applying it to various subfractions of a rat liver microsomal fraction, prepared by continuous density gradient centrifugation according to Beaufay et al. (1974, J. Cell Biol. 61:213-231). The results confirm and extend those of previous investigators on the distribution of enzymes and proteins among the membranes of the smooth and rough endoplasmic reticulum. In the accompanying paper (1982, J. Cell Biol. 93:103-110) the procedure is applied to peroxisomes and mitochondria.
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            Inorganic and organic phosphate measurements in the nanomolar range.

            P Van Veldhoven, G P Mannaerts (1987)
            A procedure, based on the complex formation of malachite green with phosphomolybdate under acidic conditions, to measure inorganic orthophosphate in the nanomolar range is described. The addition of polyvinyl alcohol is required to stabilize the dye-phosphomolybdate complex. The advantages of the assay are simplicity, stability of the reagents, and high sensitivity. Due to the high permissible acidity in the assay (0.9 N H2SO4), the method can be adapted easily to measure nanomolar amounts of phosphate, liberated from organic compounds like phosphoproteins and phospholipids after wet digestion.
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              The human peroxisomal ABC half transporter ALDP functions as a homodimer and accepts acyl-CoA esters.

              Maxim Boek, Antonie Visser, Wim Kulik (2008)
              Peroxisomes play a major role in human cellular lipid metabolism, including the beta-oxidation of fatty acids. The most frequent peroxisomal disorder is X-linked adrenoleukodystrophy (X-ALD), which is caused by mutations in the ABCD1 gene. The protein involved, called ABCD1, or alternatively ALDP, is a member of the ATP-binding-cassette (ABC) transporter family and is located in the peroxisomal membrane. The biochemical hallmark of X-ALD is the accumulation of very long-chain fatty acids (VLCFAs), due to an impaired peroxisomal beta-oxidation. Although this suggests a role of ALDP in VLCFA import, no experimental evidence is available to substantiate this. In the yeast Saccharomyces cerevisiae, peroxisomes are the exclusive site of fatty acid beta-oxidation. Earlier work has shown that uptake of fatty acids into peroxisomes may occur via two routes, either as free fatty acids thus requiring intraperoxisomal activation into acyl-CoA esters or as long-chain acyl-CoA esters. The latter route involves the two peroxisomal half ABC transporters Pxa1p and Pxa2p that form a heterodimeric complex in the peroxisomal membrane. Using different strategies, including the analysis of intracellular acyl-CoA esters by tandem-MS, we show that the Pxa1p/Pxa2p heterodimer is involved in the transport of a spectrum of acyl-CoA esters. Interestingly, we found that the mutant phenotype of the pxa1/pxa2Delta mutant can be rescued, at least partially, by the sole expression of the human ABCD1 cDNA coding for ALDP, the protein that is defective in the human disease X-linked adrenoleukodystrophy. Our data indicate that ALDP can function as a homodimer and is involved in the transport of acyl-CoA esters across the peroxisomal membrane.
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                Author and article information

                Contributors
                Journal
                Journal ID (nlm-ta): Front Cell Dev Biol
                Journal ID (iso-abbrev): Front Cell Dev Biol
                Journal ID (publisher-id): Front. Cell Dev. Biol.
                Title: Frontiers in Cell and Developmental Biology
                Publisher: Frontiers Media S.A.
                ISSN (Electronic): 2296-634X
                Publication date (Electronic): 24 March 2020
                Publication date Collection: 2020
                Volume: 8
                Electronic Location Identifier: 144
                Affiliations
                [1] 1LIPIT, Department of Cellular and Molecular Medicine, KU Leuven , Leuven, Belgium
                [2] 2Departments of Medicine and Human Genetics, David Geffen School of Medicine, University of California, Los Angeles , Los Angeles, CA, United States
                [3] 3Laboratory of Developmental Signaling, Department Human Genetics, VIB-KU Leuven , Leuven, Belgium
                [4] 4Department of Anatomy, Embryology, Histology and Medical Physics, Ghent University , Ghent, Belgium
                [5] 5Laboratory of Cell Metabolism, Faculty of Pharmaceutical Sciences, KU Leuven , Leuven, Belgium
                Author notes

                Edited by: Peter Kijun Kim, Hospital for Sick Children, Canada

                Reviewed by: Johannes Berger, Medical University of Vienna, Austria; J. Kalervo Hiltunen, University of Oulu, Finland; Ronald Wanders, University of Amsterdam, Netherlands

                *Correspondence: Paul P. Van Veldhoven, paul.vanveldhoven@ 123456med.kuleuven.be

                This article was submitted to Membrane Traffic, a section of the journal Frontiers in Cell and Developmental Biology

                Article
                DOI: 10.3389/fcell.2020.00144
                PMC ID: 7106852
                PubMed ID: 32266253
                SO-VID: 2060c336-94a9-4cb9-8fd2-953b772c9b1a
                Copyright © Copyright © 2020 Van Veldhoven, de Schryver, Young, Zwijsen, Fransen, Espeel, Baes and Van Ael.
                License:

                This is an open-access article distributed under the terms of the Creative Commons Attribution License (CC BY). The use, distribution or reproduction in other forums is permitted, provided the original author(s) and the copyright owner(s) are credited and that the original publication in this journal is cited, in accordance with accepted academic practice. No use, distribution or reproduction is permitted which does not comply with these terms.

                History
                Date received : 20 December 2019
                Date accepted : 20 February 2020
                Page count
                Figures: 10, Tables: 1, Equations: 0, References: 123, Pages: 24, Words: 0
                Categories
                Subject: Cell and Developmental Biology
                Subject: Original Research

                Keywords: atp,beta-oxidation,bile acids,coenzyme a,membrane transport,mitochondrial solute transporter,phytol,refsum
                Data availability:
                Keywords: atp, beta-oxidation, bile acids, coenzyme a, membrane transport, mitochondrial solute transporter, phytol, refsum

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