TY - JOUR
T1 - Systematic mutation screening of the pro-opiomelanocortin gene: Identification of several genetic variants including three different insertions, one nonsense and two missense point mutations in probands of different weight extremes
AU - Hinney, A.
AU - Becker, I.
AU - Heibült, O.
AU - Nottebom, K.
AU - Schmidt, A.
AU - Ziegler, A.
AU - Mayer, H.
AU - Siegfried, W.
AU - Blum, W. F.
AU - Remschmidt, H.
AU - Hebebrand, J.
PY - 1998
Y1 - 1998
N2 - Pro-opiomelanocortin (POMC) is the precursor of melanocortins (adrenocorticotropin: ACTH, β-endorphin, β-lipotropin: β-LPH, corticotropin like intermediate peptide, α-, β- and γ-melanocyte- stimulating hormone: α-, β- and γ-MSH) some of which act in the brain to reduce food intake and are potential mediators of leptin action. Recently, three different mutations in the POMC gene (POMC) were identified in two unrelated children that lead to early-onset extreme obesity, adrenal insufficiency, and red hair pigmentation (1). In the present study we systematically screened the coding region of POMC in 96 extremely obese children and adolescents, 60 healthy underweight individuals and 46 patients with anorexia nervosa (AN) and identified several variants. a) A 9 and an 18 base pair insertion (9bp and 18bp: AGC AGC GGC and AGC AGC GGC AGC AGC GGC, respectively, between codon 73 and 74; 1,2). These in-frame variants lead to the insertion of three or six amino acids (Ser-Ser-Gly; Ser-Ser-Gly-Ser-Ser- Gly) carboxy-terminal to γ-MSH. Frequencies of the 9bp insertion allele varied between 3 and 5% among the different study groups (Pearson's χ2 P>0.5). b) Both an out-of-frame 6 bp insertion (within codon 176: GGG CCC) leading to the insertion of two amino acids (Arg-Ala) and a premature stop- codon (G-7316-T: Glu-180-Stop) within the γ-LPH sequence were maternally inherited in an obese female proband. This proband inherited another missense mutation from her father (Glu-188-Gly). c) A missense mutation (G-7016-A; Asp-80-Asn) was observed in a single patient with AN who also harboured the 9bp insertion on a paternally derived haplotype. d) The allelic co-occurrence of two silent mutations (C-6982-T and C-7285-T) was detected in two obese subjects. e) Two further silent mutations (C-3832-T; C-711 l-G) were detected in an underweight and an obese subject, respectively. We conclude that the POMC gene harbors several different polymorphisms and mutations, none of which can readily be associated with the phenotypes under study.
AB - Pro-opiomelanocortin (POMC) is the precursor of melanocortins (adrenocorticotropin: ACTH, β-endorphin, β-lipotropin: β-LPH, corticotropin like intermediate peptide, α-, β- and γ-melanocyte- stimulating hormone: α-, β- and γ-MSH) some of which act in the brain to reduce food intake and are potential mediators of leptin action. Recently, three different mutations in the POMC gene (POMC) were identified in two unrelated children that lead to early-onset extreme obesity, adrenal insufficiency, and red hair pigmentation (1). In the present study we systematically screened the coding region of POMC in 96 extremely obese children and adolescents, 60 healthy underweight individuals and 46 patients with anorexia nervosa (AN) and identified several variants. a) A 9 and an 18 base pair insertion (9bp and 18bp: AGC AGC GGC and AGC AGC GGC AGC AGC GGC, respectively, between codon 73 and 74; 1,2). These in-frame variants lead to the insertion of three or six amino acids (Ser-Ser-Gly; Ser-Ser-Gly-Ser-Ser- Gly) carboxy-terminal to γ-MSH. Frequencies of the 9bp insertion allele varied between 3 and 5% among the different study groups (Pearson's χ2 P>0.5). b) Both an out-of-frame 6 bp insertion (within codon 176: GGG CCC) leading to the insertion of two amino acids (Arg-Ala) and a premature stop- codon (G-7316-T: Glu-180-Stop) within the γ-LPH sequence were maternally inherited in an obese female proband. This proband inherited another missense mutation from her father (Glu-188-Gly). c) A missense mutation (G-7016-A; Asp-80-Asn) was observed in a single patient with AN who also harboured the 9bp insertion on a paternally derived haplotype. d) The allelic co-occurrence of two silent mutations (C-6982-T and C-7285-T) was detected in two obese subjects. e) Two further silent mutations (C-3832-T; C-711 l-G) were detected in an underweight and an obese subject, respectively. We conclude that the POMC gene harbors several different polymorphisms and mutations, none of which can readily be associated with the phenotypes under study.
UR - http://www.scopus.com/inward/record.url?scp=15644369364&partnerID=8YFLogxK
U2 - 10.1210/jcem.83.10.5298
DO - 10.1210/jcem.83.10.5298
M3 - Journal articles
C2 - 9768693
AN - SCOPUS:15644369364
SN - 0021-972X
VL - 83
SP - 3737
EP - 3741
JO - Journal of Clinical Endocrinology and Metabolism
JF - Journal of Clinical Endocrinology and Metabolism
IS - 10
ER -