Molecular analysis and intestinal expression of SAR1 genes and proteins in Anderson's disease (Chylomicron retention disease)

Georges, Amandine; Bonneau, Jessica; Bonnefont‐Rousselot, Dominique; Champigneulle, J.; Rabès, Jean-Pierre; Abifadel, Marianne; Aparicio, Thomas; Guenedet, Jean C; Bruckert, Éric; Boileau, Cathérine; Morali, A.; Varret, Mathilde; Aggerbeck, Lawrence P.; Samson-Bouma, Marie Elisabeth

doi:10.1186/1750-1172-6-1

Cited by 104 publications

(122 citation statements)

References 73 publications

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“…The phenotypes of the three female patients were consistent with those of RTT but the five males not. To our knowledge, only about 28 familial cases with MECP2 mutations have been reported (Augenstein et al, 2009; Couvert et al, 2001; Dayer et al, 2007; Evans et al, 2006; Kankirawatanaet al, 2006; Khajuria et al, 2012; Klauck et al, 2002; Lambert et al, 2016; Meloni et al, 2000; Moog et al, 2006; Orrico et al, 2000; Ravn et al, 2011; Villard, 2007; Yntema et al, 2002), with genotypic mutations including missense, frameshift, and nonsense mutations, intragenic deletions and copy number variations (CNV). The phenotypes of those mutation carriers manifested from classical RTT congenital encephalopathy, nonspecific XLMR, and to clinically asymptomatic.…”

Section: Discussionmentioning

confidence: 99%

“…To our knowledge, anecdotal reports over the past decades accumulated only approximately 28 reports in literature (Augenstein, Lane, Horton, Schanen, & Percy, 2009; Couvert et al, 2001; Dayer et al, 2007; Evans, Archer, Whatley, & Clarke, 2006; Kankirawatana et al, 2006; Khajuria et al, 2012; Klauck et al, 2002; Lambert et al, 2016; Meloni et al, 2000; Moog et al, 2006; Orrico et al, 2000; Ravn et al, 2011; Villard, 2007; Yntema et al, 2002). In this paper, we report Chinese familial cases of eight children and their six mothers with MECP2 mutations, and address their clinical and molecular characteristics and its possibly underlying genetic mechanisms.…”

Section: Introductionmentioning

confidence: 99%

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Familial cases and male cases with MECP2 mutations

Zhang

Zhao

Bao

et al. 2017

American J of Med Genetics Pt B

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This is the first report of Chinese familial cases with Rett syndrome (RTT) or X‐linked mental retardation (XLMR). RTT is a neurodevelopmental disorder that almost exclusively affects females. Most RTT cases are sporadic. We have studied eight cases with MECP2 mutations in six Chinese families, including three females and five males with RTT or XLMR. All shared identical MECP2 mutations with their mothers. The three females fulfilled the diagnostic criteria for RTT, while the five males were XLMR. A random X‐chromosome inactive (XCI) pattern was seen in all the three female patients and two mothers while a skewed XCI in the rest four mothers. The clinical manifestations and pathogenic gene spectrum between male and female patients were different. The different MECP2 mutations and different XCI pattern may be the determinants of the phenotypic heterogeneity between the family members.

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Section: Discussionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

Familial cases and male cases with MECP2 mutations

Zhang

Zhao

Bao

et al. 2017

American J of Med Genetics Pt B

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“…2 ). The obligatory role of Sar1b GTPase is evidenced by the presence of its paralog Sar1a GTPase (216)(217)(218) that is 90% identical, differing by only 20 amino acid residues, but does not compensate for the lack of the Sar1b protein in CRD ( 219 ). Of note, if Sar1a could not compensate for loss of Sar1b in the gut, only limited data are, however, available regarding its contributions in the liver despite the fact that VLDL secretion was not substantially affected in CRD ( 220 ).…”

Section: Sar1b Propertiesmentioning

confidence: 99%

Insights from human congenital disorders of intestinal lipid metabolism

Lévy

2015

Journal of Lipid Research

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“…His summary includes a detailed overview of the features and underlying mechanisms contributing to phenotypes in familial hypobetalipoproteinemia and abetalipoproteinemia ( 6 ) as well as a review of chylomicron retention disease (CRD) ( 7 ). Each of these disorders is linked to distinct genes that represent critical points in chylomicron assembly and secretion.…”

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confidence: 99%

Overview and Introduction: Thematic Review Series on Intestinal Lipid Metabolism

Davidson

2015

Journal of Lipid Research

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The last decade has seen extraordinary advances in our understanding of intestinal lipid metabolism, driven at least in part through attempts to mitigate the ongoing epidemic of obesity and metabolic disease ( 1 ). For example, weight loss strategies including gastric bypass surgery have brought to light unanticipated adaptations in metabolic homeostasis, including altered bile acid signaling and shifts in host-microbial ecology ( 2 ). As a result, our understanding of the role of the intestine in lipid metabolism now includes an expanded role in a range of homeostatic processes, including glucose metabolism, energy utilization, and growth and infl ammation to name but a few. Our Thematic Review Series will selectively cover several of these areas. In particular, we have solicited reviews that summarize a detailed elucidation of the pathways regulating the fl ux of complex lipids across the small intestinal enterocyte, including an emerging role in energy utilization and the role of circadian cues. We have also solicited reviews to provide a thorough understanding of the molecular, genetic, and regulatory pathways involved in modulating intestinal bile acid transport and signaling and new insights into the role of nuclear hormone receptors in the intestine in maintenance of systemic lipid metabolism.In the fi rst article in our series, Eric Yen and his colleagues will review the role and regulation of enterocyte triglyceride synthesis, including the abundantly expressed genes acyl CoA:monoacylglycerol acyltransferase 2 (MGAT2) and acyl CoA:diacylglycerol acyltransferase 1 (ACAT1), whose functions have been examined in numerous model systems and have been shown to play crucial roles in the regulation of fat metabolism and energy utilization. There is heightened interest also in the possibility that these pathways represent druggable targets for obesity and metabolic disorders ( 3 ).In the second article, Mahmood Hussain and Xiaoyue Pan have summarized some of the recent developments in our understanding of the relevance of circadian rhythm to intestinal lipid metabolism. They summarize the role of innate intestinal Clock genes and outline the integration of central signals (via the suprachiasmatic nucleus) with

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Molecular analysis and intestinal expression of SAR1 genes and proteins in Anderson's disease (Chylomicron retention disease)

Cited by 104 publications

References 73 publications

Familial cases and male cases with MECP2 mutations

Familial cases and male cases with MECP2 mutations

Insights from human congenital disorders of intestinal lipid metabolism

Overview and Introduction: Thematic Review Series on Intestinal Lipid Metabolism

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