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The Metabolic Map into the Pathomechanism and Treatment of PGM1-CDG

机译:代谢地图进入PGM1-CDG的土地机制和治疗

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摘要

Phosphoglucomutase 1 (PGM1) encodes the metabolic enzyme that interconverts glucose-6-P and glucose-1-P. Mutations in PGM1 cause impairment in glycogen metabolism and glycosylation, the latter manifesting as a congenital disorder of glycosylation (CDG). This unique metabolic defect leads to abnormal N-glycan synthesis in the endoplasmic reticulum (ER) and the Golgi apparatus (GA). On the basis of the decreased galactosylation in glycan chains, galactose was administered to individuals with PGM1-CDG and was shown to markedly reverse most disease-related laboratory abnormalities. The disease and treatment mechanisms, however, have remained largely elusive. Here, we confirm the clinical benefit of galactose supplementation in PGM1-CDG-affected individuals and obtain significant insights into the functional and biochemical regulation of glycosylation. We report here that, by using tracer-based metabolomics, we found that galactose treatment of PGM1-CDG fibroblasts metabolically re-wires their sugar metabolism, and as such replenishes the depleted levels of galactose-1-P, as well as the levels of UDP-glucose and UDP-galactose, the nucleotide sugars that are required for ER- and GA-linked glycosylation, respectively. To this end, we further show that the galactose in UDP-galactose is incorporated into mature, de novo glycans. Our results also allude to the potential of monosaccharide therapy for several other CDG.
机译:磷酰型酶1(PGM1)编码代谢酶,其互连葡萄糖-6-P和葡萄糖-1-p。 PGM1中的突变导致糖原代谢和糖基化的损伤,后者表现为先天性糖基化(CDG)。这种独特的代谢缺陷导致内质网(ER)和GOLGI装置(GA)中的N-聚糖合成异常。基于甘草链中的半乳糖基化下降,将半乳糖施用于具有PGM1-CDG的个体,并显示出明显逆转最多的疾病相关的实验室异常。然而,疾病和治疗机制仍然很大程度上难以捉摸。在这里,我们确认了半乳糖补充剂在PGM1-CDG受影响的个体中的临床效益,并对糖基化的功能性和生化调节获得了显着的见解。我们在这里报告,通过使用基于特拉克的代谢组学,我们发现将PGM1-CDG成纤维细胞的半乳糖处理代谢地重新连接它们的糖代谢,并因此补充了半乳糖-1-P的耗尽水平,以及水平UDP-葡萄糖和UDP-半乳糖,分别是ER-和GA与糖基化所需的核苷酸糖。为此,我们进一步表明UDP-半乳糖中的半乳糖掺入成熟,De Novo聚糖中。我们的结果还暗示了几种其他CDG的单糖治疗的潜力。

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    VIB Ctr Canc Biol Metabol Expertise Ctr Ctr Canc Biol B-3000 Leuven Belgium;

    VIB Ctr Canc Biol Metabol Expertise Ctr Ctr Canc Biol B-3000 Leuven Belgium;

    Radboud Univ Nijmegen Med Ctr Donders Inst Brain Cognit &

    Behav Dept Anat NL-6535 HR Nijmegen;

    Tulane Univ Sch Med Hayward Genet Ctr New Orleans LA 70112 USA;

    Katholieke Univ Leuven Dept Chron Dis Metab &

    Aging Lab Hepatol B-3000 Leuven Belgium;

    Univ Missouri Biochem Dept Columbia MO 65211 USA;

    Tulane Univ Sch Med Hayward Genet Ctr New Orleans LA 70112 USA;

    Heidelberg Univ Dept 1 Ctr Child &

    Adolescent Med D-69120 Heidelberg Germany;

    Heidelberg Univ Ctr Organismal Studies D-69120 Heidelberg Germany;

    Katholieke Univ Leuven Dept Chron Dis Metab &

    Aging Lab Hepatol B-3000 Leuven Belgium;

    Mayo Clin Dept Clin Genom Ctr Individualized Med Rochester MN 55905 USA;

    Univ Hosp Leuven Metab Ctr B-3000 Leuven Belgium;

    Univ Hosp Leuven Metab Ctr B-3000 Leuven Belgium;

    Charles Univ Prague Fac Med 1 Dept Pediat &

    Adolescent Med Prague 12108 Czech Republic;

    Ankara Univ Sch Med Dept Pediat Metab &

    Nutr TR-06560 Ankara Turkey;

    Phoenix Childrens Hosp Phoenix Childrens Med Grp Genet &

    Metab Phoenix AZ 85016 USA;

    Childrens Hosp Philadelphia Dept Pediat Div Human Genet Philadelphia PA 19104 USA;

    United Arab Emirates Univ Dept Pediat Al Ain U Arab Emirates;

    Radboud Univ Nijmegen Med Ctr Donders Inst Brain Cognit &

    Behav Dept Anat NL-6535 HR Nijmegen;

    Heidelberg Univ Dept 1 Ctr Child &

    Adolescent Med D-69120 Heidelberg Germany;

    Univ Hosp Leuven Clin Dept Lab Med B-3000 Leuven Belgium;

    Katholieke Univ Leuven Dept Chron Dis Metab &

    Aging Lab Hepatol B-3000 Leuven Belgium;

    Univ Missouri Biochem Dept Columbia MO 65211 USA;

    Mayo Clin Dept Clin Genom Ctr Individualized Med Rochester MN 55905 USA;

    VIB Ctr Canc Biol Metabol Expertise Ctr Ctr Canc Biol B-3000 Leuven Belgium;

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  • 正文语种 eng
  • 中图分类 医学遗传学;
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