Phenotypic and Genetic Heterogeneity in Congenital Generalized Lipodystrophy

Agarwal, Anil K.; Simha, Vinaya; Oral, Elif A.; Moran, Stephanie Ann; Görden, Phillip; O’Rahilly, Stephen; Zaidi, Zohra; Gürakan, Figen; Arslanian, Silva; Klar, Aharon; Ricker, Alyne; White, Neil H.; Bindl, Lutz; Herbst, Karen L.; Kennel, Kurt A.; Patel, Shailendra B.; Al‐Gazali, Lihadh; Garg, Abhimanyu

doi:10.1210/jc.2003-030855

Cited by 220 publications

(207 citation statements)

References 21 publications

(33 reference statements)

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“…Affected subjects have extreme paucity of adipose tissue from birth leading to a muscular appearance, with prominent veins and an acromegaloid appearance. Subtle differences in pattern of fat loss have been recognized among the different subtypes of CGL [7], but common features include severe acanthosis nigricans, hepatosplenomegaly and early onset of diabetes, hypertriglyceridemia and steatohepatitis [8]. Marked hypoleptinemia is a universal feature of this disease [9].…”

mentioning

confidence: 99%

Metreleptin for metabolic disorders associated with generalized or partial lipodystrophy

Simha

2014

Expert Review of Endocrinology & Metabolism

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Lipodystrophy is a group of acquired and inherited disorders characterized by selective loss of adipose tissue. Despite wide genotypic and phenotypic variety, many patients with lipodystrophy have similar metabolic complications including insulin resistance, diabetes mellitus, hypertriglyceridemia and hepatic steatosis. Often, these metabolic abnormalities are severe and difficult to treat with conventional glucose and lipid-lowering therapies. Lack of adipose tissue also results in marked hypoleptinemia, and there has recently been much interest in using leptin-replacement therapy to treat the metabolic complications of lipodystrophy. Administration of metreleptin, the human recombinant leptin analogue, has been shown in prospective, open-label studies to improve glucose control, dyslipidemia and steatohepatitis. This article summarizes the current evidence for the safety and efficacy of leptin-replacement therapy in patients with lipodystrophy.

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mentioning

confidence: 99%

Metreleptin for metabolic disorders associated with generalized or partial lipodystrophy

Simha

2014

Expert Review of Endocrinology & Metabolism

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“…As shown in Figure 1a, various AGPAT2 mutations, including null, splice-site, frame-shift, insertion and deletion, have been found in several affected subjects. [5][6][7][8] The IVS4-2A4G mutation was found to recur in pedigrees of African origin and the chromosomes carrying it had the same haplotype for seven SNPs within and around AGPAT2, indicating that this mutation is of ancestral origin. 5 AGPAT2, a 278 amino-acid protein, catalyses an essential acylation reaction in the biosynthesis of all glycerophospholipids and TG in eukaryotes (Figure 1b).…”

Section: Cgl1 Locusmentioning

confidence: 97%

Genetic basis of congenital generalized lipodystrophy

2003

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Congenital generalized lipodystrophy (CGL) is an autosomal recessive disorder characterized by extreme lack of body fat and severe insulin resistance since birth. Recently, mutations have been reported in 1-acylglycerol-3-phosphate-O-acyltransferase 2 (AGPAT2) and Berardinelli-Seip congenital lipodystrophy 2 (BSCL2 or Seipin) genes in affected subjects from pedigrees linked to chromosomes 9q34 and 11q13, respectively. The AGPAT2 catalyses the acylation of the lysophosphatidic acid at the sn-2 position to form phosphatidic acid, a key intermediate in the biosynthesis of triacylglycerol and glycerophospholipids. High expression of AGPAT2 mRNA in adipose tissue compared to other isoforms suggests that the mutations might affect the adipose tissue the most. The function of BSCL2 remains unknown. Several CGL pedigrees reveal no mutation in either of the above genes and are not linked to these loci, suggesting additional genetic loci for CGL. Thus, several distinct mechanisms can lead to extreme lack of adipose tissue in humans and cause CGL.

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“…2 The following molecular defects have been reported: nonsense, missense, splice-site variants, deletions and insertions. 3 Most of them result in frameshift and/or truncated proteins, which are likely to lead to the complete loss of AGPAT2 function. This can be demonstrated in vitro by measurement of AGPAT2 enzymatic activity.…”

Section: Mutational Spectrummentioning

confidence: 99%

“…The following molecular defects have been reported: nonsense, missense, splice-site variants, deletions and insertions. 3,5 Most of them result in frameshift and/or truncated proteins, which are likely to lead to complete loss of BSCL2 function (for more details, see http://databases.lovd.nl/shared/variants/ BSCL2/unique). Notably, disease-causing variants in this gene have also been identified in patients with distal hereditary motor neuropathies or neurodegenerative syndromes.…”

Section: Mutational Spectrummentioning

confidence: 99%