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Biomedical Chemistry
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Issue:
Volume 56, issue 2
Title: GENETIC VARIATIONS IN THE REGULATION OF ENERGETIC BALANCE
Authors: Y.A.
Pankov
Address:
Endocrine
Research Center, Moscvorechye str. 1, Moscow, 115478 Russia; tel.: (495)324-93-15;
e-mail:
yurpankov@yandex.ru
Abstract:
Single nucleotide
polymorphism (SNP) near certain genes revealed association of FAT (fat
mass and obesity-associated gene), MC4R (melanocortin 4 receptor gene),
and other genes with obesity. Participation of the FAT expression
products in the regulation of energy balance remains to be clarified. The
function of MC4R encoding melanocortin 4 receptor (MC4R) is somewhat
better understood. a-, b-, and g-MSH encoded by the POMC gene bind to MC4R, reduce food intake,
and slow down fat accumulation. Expression of POMC that codes MSH is
enhanced by leptin binding to the receptor (LepRb) in hypothalamic neurons.
Mutations in human and animal MC4R, POMC, and LEP
genes are known to be associated with obesity. More than 60 mutations in MC4R,
more than 20 mutations in POMC and fewer LEP mutations have
been reported. Nonsense mutations and reading frame shifts block gene
expression and thereby disrupt protein synthesis. Missense mutations frequently
affect protein folding in endoplasmic reticulum; unfolded or misfolded proteins
remain in the cytoplasm and undergo degradation. Certain missence mutations do
not interfere with gene expression and folding of proteins but impair their
functioning at the periphery. P.S127L mutation in MC4R, p.E206X and
p.F144L mutations in POMC as well as other mutations in homozygous and
heterozygous forms account for disturbed energy balance in man. The LEP gene
has been reported to contain G133fsX15, p.R105X, p.R105W, and p.S141C mutations.
As a rule, they are associated with obesity and other pathological conditions
only in homozygous forms.
Key words: gene,
mutation, obesity.
Biomedical Chemistry, 2010 Volume 56, Issue 2, p. 152-167.
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