Androgen receptor CAG repeat polymorphism might be a possible cause of familial constitutional delay of growth and puberty.

IF 5.4 2区 医学 Q1 Medicine Journal of Endocrinological Investigation Pub Date : 2024-11-21 DOI:10.1007/s40618-024-02502-3
Gözde Akın Kağızmanlı, Reyhan Deveci Sevim, Hayrullah Manyas, Ahu Paketçi, Korcan Demir, Ece Böber, Gönül Çatlı, Ahmet Anık, Ayhan Abacı
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Abstract

Background: Induction of puberty in boys with constitutional delay of growth and puberty (CDGP) through a short course of low-dose testosterone therapy indicates the critical interaction between testosterone and the androgen receptor (AR) during the activation and maturation of the hypothalamic-pituitary-gonadal axis at puberty onset. Previous studies have shown an inverse relationship between the CAG repeat length and the transactivation function or expression level of the AR gene.

Objective: We aimed to investigate whether the AR CAG repeat polymorphism has any implications on pubertal delay.

Subjects and methods: Thirty-three male patients with CDGP were enrolled in the study group, while 53 age-matched healthy individuals who had entered puberty on time were included in the control group. The CAG repeat length was determined through direct DNA sequencing analysis.

Results: The median chronological age of boys with CDGP was 14.2 (14.1-14.6) years, compared to 14.2 (13.65-14.8) years for healthy subjects (p = 0.5). In the CDGP group, 22 (66.7%) children had a family history of the condition. There was no significant difference between the groups in terms of AR CAG repeat length (median AR CAG repeat length: 21 (20-24.5) and 20 (20-24), respectively, p = 0.1). However, in boys with CDGP with a similar family history (n = 22), a significantly longer AR CAG repeat length was found compared to the control group (n = 53) (median AR CAG repeat length: 22 (20-25) and 20 (20-24), respectively, p = 0.03). The median AR CAG repeat length in boys without a family history was 21 (20-22) triplets. Although boys with a family history had a slightly longer AR CAG repeat length than those without, the difference was not statistically significant (p = 0.07). Additionally, no significant differences were observed between boys with non-familial CDGP and control subjects (p = 0.8). Furthermore, no significant differences in anthropometric characteristics or hormonal parameters were found when patients with CDGP were categorized by AR CAG repeat length quartiles.

Conclusion: This is the first study to investigate the role of AR CAG polymorphism in the etiopathogenesis of CDGP. Our findings suggest that the AR CAG repeat length may be associated with familial CDGP.

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雄激素受体 CAG 重复多态性可能是导致家族性发育和青春期延迟的原因之一。
背景:通过短期低剂量睾酮治疗诱导发育和青春期延迟(CDGP)男孩进入青春期表明,在青春期开始时,下丘脑-垂体-性腺轴的激活和成熟过程中,睾酮和雄激素受体(AR)之间的相互作用至关重要。以往的研究表明,CAG重复长度与AR基因的反式激活功能或表达水平之间存在反比关系:我们旨在研究AR CAG重复多态性是否对青春期延迟有影响:研究组包括 33 名男性 CDGP 患者,对照组包括 53 名年龄匹配、按时进入青春期的健康人。通过直接DNA测序分析确定CAG重复长度:结果:患有 CDGP 的男孩的中位实际年龄为 14.2(14.1-14.6)岁,而健康人的中位实际年龄为 14.2(13.65-14.8)岁(P = 0.5)。在 CDGP 组中,22 名儿童(66.7%)有家族病史。两组儿童的AR CAG重复长度无明显差异(AR CAG重复长度中位数分别为21(20-24.5)和20(20-24),p = 0.1)。然而,在具有相似家族史的 CDGP 男孩(n = 22)中,发现与对照组(n = 53)相比,AR CAG 重复长度明显更长(AR CAG 重复长度中位数分别为:22(20-25)和 20(20-24),p = 0.03)。无家族史男孩的 AR CAG 重复长度中位数为 21(20-22)三倍。虽然有家族史的男孩的 AR CAG 重复长度略长于无家族史的男孩,但差异无统计学意义(p = 0.07)。此外,非家族性 CDGP 男孩与对照组之间也未发现明显差异(p = 0.8)。此外,按AR CAG重复长度四分位数对CDGP患者进行分类,也未发现其人体测量特征或激素参数存在明显差异:这是首次研究 AR CAG 多态性在 CDGP 发病机制中的作用。我们的研究结果表明,AR CAG重复长度可能与家族性CDGP有关。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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来源期刊
Journal of Endocrinological Investigation
Journal of Endocrinological Investigation ENDOCRINOLOGY & METABOLISM-
CiteScore
8.10
自引率
7.40%
发文量
242
期刊介绍: The Journal of Endocrinological Investigation is a well-established, e-only endocrine journal founded 36 years ago in 1978. It is the official journal of the Italian Society of Endocrinology (SIE), established in 1964. Other Italian societies in the endocrinology and metabolism field are affiliated to the journal: Italian Society of Andrology and Sexual Medicine, Italian Society of Obesity, Italian Society of Pediatric Endocrinology and Diabetology, Clinical Endocrinologists’ Association, Thyroid Association, Endocrine Surgical Units Association, Italian Society of Pharmacology.
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