Hinney A, Becker I, Heibült O, Nottebom K, Schmidt A, Ziegler A, Mayer H, Siegfried W, Blum W F, Remschmidt H, Hebebrand J
Department of Child and Adolescent Psychiatry, University of Marburg, FRG.
J Clin Endocrinol Metab. 1998 Oct;83(10):3737-41. doi: 10.1210/jcem.83.10.5298.
Pro-opiomelanocortin (POMC) is the precursor of melanocortins (adrenocorticotropin: ACTH, beta-endorphin, beta-lipotropin: beta-LPH, corticotropin like intermediate peptide, alpha-, beta- and gamma-melanocyte-stimulating hormone: alpha-, beta- and gamma-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. 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 gamma-MSH. Frequencies of the 9bp insertion allele varied between 3 and 5% among the different study groups (Pearson's chi2 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 gamma-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-occurence 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-7111-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.
阿黑皮素原(POMC)是促黑素细胞激素(促肾上腺皮质激素:ACTH、β-内啡肽、β-促脂素:β-LPH、促肾上腺皮质激素样中间肽、α-、β-和γ-促黑素细胞激素:α-、β-和γ-MSH)的前体,其中一些在大脑中发挥作用以减少食物摄入,并且是瘦素作用的潜在介质。最近,在两名无血缘关系的儿童中发现了POMC基因(POMC)的三种不同突变,这些突变导致早发性极度肥胖、肾上腺功能不全和红发色素沉着。在本研究中,我们系统地筛查了96名极度肥胖儿童和青少年、60名健康体重过轻个体以及46名神经性厌食症(AN)患者的POMC编码区,并鉴定出了几种变体。a)一个9个碱基对和一个18个碱基对的插入(9bp和18bp:分别为AGC AGC GGC和AGC AGC GGC AGC AGC GGC,位于密码子73和74之间;1,2)。这些框内变体导致在γ-MSH的羧基末端插入三个或六个氨基酸(Ser-Ser-Gly;Ser-Ser-Gly-Ser-Ser-Gly)。9bp插入等位基因的频率在不同研究组之间在3%至5%之间变化(Pearson卡方检验P>0.5)。b)在一名肥胖女性先证者中,一个导致插入两个氨基酸(Arg-Ala)的框外6bp插入(在密码子176内:GGG CCC)和γ-LPH序列内的一个提前终止密码子(G-7316-T:Glu-180-Stop)均为母系遗传。该先证者从其父亲那里继承了另一个错义突变(Glu-188-Gly)。c)在一名AN患者中观察到一个错义突变(G-7016-A;Asp-80-Asn),该患者在父系单倍型上也携带9bp插入。d)在两名肥胖受试者中检测到两个沉默突变(C-6982-T和C-7285-T)的等位基因共出现。e)分别在一名体重过轻和一名肥胖受试者中检测到另外两个沉默突变(C-3832-T;C-7111-G)。我们得出结论,POMC基因存在几种不同的多态性和突变,其中没有一种能轻易与所研究的表型相关联。
