Whole-exome sequencing identifies ADRA2A mutation in atypical familial partial lipodystrophy
Abhimanyu Garg, … , Chao Xing, Anil K. Agarwal
Abhimanyu Garg, … , Chao Xing, Anil K. Agarwal
Published June 16, 2016
Citation Information: JCI Insight. 2016;1(9):e86870. https://doi.org/10.1172/jci.insight.86870.
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Research Article Endocrinology

Whole-exome sequencing identifies ADRA2A mutation in atypical familial partial lipodystrophy

Abstract

Despite identification of causal genes for various lipodystrophy syndromes, the molecular basis of some peculiar lipodystrophies remains obscure. In an African-American pedigree with a novel autosomal dominant, atypical familial partial lipodystrophy (FPLD), we performed linkage analysis for candidate regions and whole-exome sequencing to identify the disease-causing mutation. Affected adults reported marked loss of fat from the extremities, with excess fat in the face and neck at age 13–15 years, and developed metabolic complications later. A heterozygous g.112837956C>T mutation on chromosome 10 (c.202C>T, p.Leu68Phe) affecting a highly conserved residue in adrenoceptor α 2A (ADRA2A) was found in all affected subjects but not in unaffected relatives. ADRA2A is the main presynaptic inhibitory feedback G protein–coupled receptor regulating norepinephrine release. Activation of ADRA2A inhibits cAMP production and reduces lipolysis in adipocytes. As compared with overexpression of a wild-type ADRA2A construct in human embryonic kidney–293 cells and differentiated 3T3-L1 adipocytes, the mutant ADRA2A produced more cAMP and glycerol, which were resistant to the effects of the α2-adrenergic receptor agonist clonidine and the α2-adrenergic receptor antagonist yohimbine, suggesting loss of function. We conclude that heterozygous p.Leu68Phe ADRA2A mutation causes a rare atypical FPLD, most likely by inducing excessive lipolysis in some adipose tissue depots.

Authors

Abhimanyu Garg, Shireesha Sankella, Chao Xing, Anil K. Agarwal

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Figure 2

FPLD 122 pedigree and the disease-causing mutation.

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FPLD 122 pedigree and the disease-causing mutation. (A) FPLD 122 pedigre...
(A) FPLD 122 pedigree. Circles denote women, and squares denote men. Subjects with heterozygous c.202C>T ADRA2A mutation are indicated with “C/T,” and those with the wild-type alleles are indicated with “C/C.” Symbols half-filled with black represent adult subjects with confirmed clinical diagnosis of lipodystrophy, whereas symbols half-filled with gray represent children in whom the clinical diagnosis of lipodystrophy could not be confirmed; white symbols indicate unaffected subjects. Vertical arrows indicate subjects for whom DNA was available, and a slanted arrow indicates the proband. Diagonal lines across the symbols indicate deceased subjects. (B) Sequence electropherogram from Sanger sequencing, showing normal sequence of ADRA2A. (C) Sequence electropherogram from FPLD 122.3, showing heterozygous c.202C>T (p.Leu68Phe) mutation.