D A Khabibullina, A A Kolodkina, T V Vizerov, N A Zubkova, O B Bezlepkina
{"title":"[促性腺激素依赖性性早熟:遗传与临床特征]。","authors":"D A Khabibullina, A A Kolodkina, T V Vizerov, N A Zubkova, O B Bezlepkina","doi":"10.14341/probl13215","DOIUrl":null,"url":null,"abstract":"<p><strong>Background: </strong>In 90% cases of girls and 25-60% cases of boys the cause of gonadotropin-dependent precocious puberty (PP) is unclear. Up to 25-27.5% of gonadotropin-dependent PP cases are monogenic and suggest autosomal-dominant inheritance with incomplete sex-dependent penetrance. To date, mutations in genes KISS1, KISS1R, MKRN3, DLK1 have been described as causal variants leading to precocious hypothalamic-pituitary axis activation in childhood. Genetic testing in patients with hereditary forms of PP can expand our knowledge of underlying molecular mechanisms of the disease and it is also necessary for genetic counselling.</p><p><strong>Aim: </strong>To study clinical features and genetic characteristics of patients with idiopathic gonadotropin-dependent precocious puberty.</p><p><strong>Materials and methods: </strong>A group of patients with idiopathic gonadotropin-dependent precocious puberty and positive family history (early or precocious puberty) was examined. Laboratory and instrumental diagnostic tests, full-exome sequencing (NGS, next-generation sequencing) were provided for all patients.</p><p><strong>Results: </strong>The study included 30 patients (29 girls, 1 boy) with idiopathic gonadotropin-dependent precocious puberty. The median of patients age at the time of the examination was 7,2 years [6,5; 7,7]. Positive family history presented in all cases: in 40% of patients on father's side, in 37% - on mother's side, in 23% of patients PP was diagnosed in siblings. The fullexome sequencing was conducted to 21 patients: in 61,9% of cases (95% CI [40;79]) nucleotide variants were identified in genes, associated with gonadotropin-dependent precocious puberty. MKRN3 gene defect was detected in most cases (77% cases (95% CI [49; 92]), which consistent with international data on its highest prevalence in the monogenic forms of PP. In 23% of cases (95% CI [7; 50]) nucleotide variants were identified in other candidate genes associated with neuroontogenesis and neuroendocrine regulation mechanisms of hypothalamic-pituitary axis.</p><p><strong>Conclusion: </strong>Our study confirms that detailed family history data in children with PP provides a rational approach to molecular-genetic testing. Data of inheritance pattern and clinical manifestations will simplify the diagnosis of hereditary forms of disease and enhance genetic counselling of families, followed by timely examination and administration of pathogenetic therapy.</p>","PeriodicalId":20433,"journal":{"name":"Problemy endokrinologii","volume":null,"pages":null},"PeriodicalIF":0.0000,"publicationDate":"2023-05-11","publicationTypes":"Journal Article","fieldsOfStudy":null,"isOpenAccess":false,"openAccessPdf":"https://www.ncbi.nlm.nih.gov/pmc/articles/PMC10204783/pdf/","citationCount":"0","resultStr":"{\"title\":\"[Gonadotropin-dependent precocious puberty: genetic and clinical characteristics].\",\"authors\":\"D A Khabibullina, A A Kolodkina, T V Vizerov, N A Zubkova, O B Bezlepkina\",\"doi\":\"10.14341/probl13215\",\"DOIUrl\":null,\"url\":null,\"abstract\":\"<p><strong>Background: </strong>In 90% cases of girls and 25-60% cases of boys the cause of gonadotropin-dependent precocious puberty (PP) is unclear. Up to 25-27.5% of gonadotropin-dependent PP cases are monogenic and suggest autosomal-dominant inheritance with incomplete sex-dependent penetrance. To date, mutations in genes KISS1, KISS1R, MKRN3, DLK1 have been described as causal variants leading to precocious hypothalamic-pituitary axis activation in childhood. Genetic testing in patients with hereditary forms of PP can expand our knowledge of underlying molecular mechanisms of the disease and it is also necessary for genetic counselling.</p><p><strong>Aim: </strong>To study clinical features and genetic characteristics of patients with idiopathic gonadotropin-dependent precocious puberty.</p><p><strong>Materials and methods: </strong>A group of patients with idiopathic gonadotropin-dependent precocious puberty and positive family history (early or precocious puberty) was examined. Laboratory and instrumental diagnostic tests, full-exome sequencing (NGS, next-generation sequencing) were provided for all patients.</p><p><strong>Results: </strong>The study included 30 patients (29 girls, 1 boy) with idiopathic gonadotropin-dependent precocious puberty. The median of patients age at the time of the examination was 7,2 years [6,5; 7,7]. Positive family history presented in all cases: in 40% of patients on father's side, in 37% - on mother's side, in 23% of patients PP was diagnosed in siblings. The fullexome sequencing was conducted to 21 patients: in 61,9% of cases (95% CI [40;79]) nucleotide variants were identified in genes, associated with gonadotropin-dependent precocious puberty. MKRN3 gene defect was detected in most cases (77% cases (95% CI [49; 92]), which consistent with international data on its highest prevalence in the monogenic forms of PP. In 23% of cases (95% CI [7; 50]) nucleotide variants were identified in other candidate genes associated with neuroontogenesis and neuroendocrine regulation mechanisms of hypothalamic-pituitary axis.</p><p><strong>Conclusion: </strong>Our study confirms that detailed family history data in children with PP provides a rational approach to molecular-genetic testing. 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引用次数: 0
摘要
背景:在90%的女孩和25-60%的男孩中,促性腺激素依赖性性性早熟(PP)的病因尚不清楚。高达25-27.5%的促性腺激素依赖性PP病例是单基因的,表明常染色体显性遗传具有不完全的性别依赖外显率。迄今为止,基因KISS1、KISS1R、MKRN3、DLK1的突变已被描述为导致儿童期下丘脑-垂体轴过早激活的因果变异。遗传形式PP患者的基因检测可以扩大我们对该疾病潜在分子机制的认识,对遗传咨询也是必要的。目的:探讨特发性促性腺激素依赖性性性早熟的临床特点和遗传特征。材料和方法:对一组特发性促性腺激素依赖性性性早熟且家族史阳性(性早熟或性早熟)的患者进行调查。为所有患者提供实验室和仪器诊断测试,全外显子组测序(NGS,下一代测序)。结果:本研究纳入特发性促性腺激素依赖性性性早熟患者30例(女孩29例,男孩1例)。检查时患者年龄的中位数为7,2岁[6,5;7、7]。所有病例均有阳性家族史:父亲侧40%的患者,母亲侧37%的患者,兄弟姐妹中23%的患者被诊断为PP。对21例患者进行了全基因组测序:61.9%的病例(95% CI[40;79])在基因中鉴定出与促性腺激素依赖性性早熟相关的核苷酸变异。大多数病例检测到MKRN3基因缺陷(77%)(95% CI [49;92]),这与国际上关于单基因型PP患病率最高的数据一致。23%的病例(95% CI [7;[50])在与下丘脑-垂体轴神经肿瘤发生和神经内分泌调节机制相关的其他候选基因中发现了核苷酸变异。结论:我们的研究证实了详细的PP患儿家族史数据为分子基因检测提供了合理的方法。遗传模式和临床表现的数据将简化遗传病的诊断,加强对家庭的遗传咨询,随后及时检查和实施病理治疗。
[Gonadotropin-dependent precocious puberty: genetic and clinical characteristics].
Background: In 90% cases of girls and 25-60% cases of boys the cause of gonadotropin-dependent precocious puberty (PP) is unclear. Up to 25-27.5% of gonadotropin-dependent PP cases are monogenic and suggest autosomal-dominant inheritance with incomplete sex-dependent penetrance. To date, mutations in genes KISS1, KISS1R, MKRN3, DLK1 have been described as causal variants leading to precocious hypothalamic-pituitary axis activation in childhood. Genetic testing in patients with hereditary forms of PP can expand our knowledge of underlying molecular mechanisms of the disease and it is also necessary for genetic counselling.
Aim: To study clinical features and genetic characteristics of patients with idiopathic gonadotropin-dependent precocious puberty.
Materials and methods: A group of patients with idiopathic gonadotropin-dependent precocious puberty and positive family history (early or precocious puberty) was examined. Laboratory and instrumental diagnostic tests, full-exome sequencing (NGS, next-generation sequencing) were provided for all patients.
Results: The study included 30 patients (29 girls, 1 boy) with idiopathic gonadotropin-dependent precocious puberty. The median of patients age at the time of the examination was 7,2 years [6,5; 7,7]. Positive family history presented in all cases: in 40% of patients on father's side, in 37% - on mother's side, in 23% of patients PP was diagnosed in siblings. The fullexome sequencing was conducted to 21 patients: in 61,9% of cases (95% CI [40;79]) nucleotide variants were identified in genes, associated with gonadotropin-dependent precocious puberty. MKRN3 gene defect was detected in most cases (77% cases (95% CI [49; 92]), which consistent with international data on its highest prevalence in the monogenic forms of PP. In 23% of cases (95% CI [7; 50]) nucleotide variants were identified in other candidate genes associated with neuroontogenesis and neuroendocrine regulation mechanisms of hypothalamic-pituitary axis.
Conclusion: Our study confirms that detailed family history data in children with PP provides a rational approach to molecular-genetic testing. Data of inheritance pattern and clinical manifestations will simplify the diagnosis of hereditary forms of disease and enhance genetic counselling of families, followed by timely examination and administration of pathogenetic therapy.
期刊介绍:
Since 1955 the “Problems of Endocrinology” (or “Problemy Endocrinologii”) Journal publishes timely articles, balancing both clinical and experimental research, case reports, reviews and lectures on pressing problems of endocrinology. The Journal is aimed to the most topical issues of endocrinology: to chemical structure, biosynthesis and metabolism of hormones, the mechanism of their action at cellular and molecular level; pathogenesis and to clinic of the endocrine diseases, new methods of their diagnostics and treatment. The Journal: features original national and foreign research articles, reflecting world endocrinology development; issues thematic editions on specific areas; publishes chronicle of major international congress sessions and workshops on endocrinology, as well as state-of-the-art guidelines; is intended for scientists, endocrinologists diabetologists and specialists of allied trade, general practitioners, family physicians and pediatrics.