Pituitary Acrogigantism: From the Past to the Future.

Adrian F Daly, Patrick Pétrossians, Albert Beckers
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Abstract

Pituitary acrogigantism is a very rare disease that is caused by chronic growth hormone (GH) axis excess that begins during childhood and adolescence. As such, it represents one of the most severe manifestations of acromegaly. In most cases, acrogigantism is caused by a pituitary adenoma, but hyperplasia can also accompany the adenoma or rarely occur alone. Individual cases of pituitary acrogigantism due to peripheral neuroendocrine tumor-derived GH-secreting hormone excess that stimulates pituitary GH hypersecretion have been reported. About half of patients with pituitary acrogigantism carry an identifiable germline genetic alteration (pathogenic variants, copy number variations, alterations of topologically associated domains (TADs), mosaicism), making it one of the most genetically-determined endocrine tumors. Among the genetic causes, pathogenic variants in the AIP gene (30%), the TADopathy X-linked acrogigantism (10%), and McCune-Albright syndrome (5%) are the most frequent causes. Molecular alterations induced by these genetic and genomic changes lead to large aggressive somatotropinomas that occur at an early age, secrete abundant amounts of GH, and produce treatment-resistant increases in insulin-like growth factor 1. X-linked acrogigantism occurs in the first year of life and is usually present by the age of 36 months, whereas, McCune-Albright syndrome-related GH excess usually presents before 5 years of age. AIP-related pituitary acrogigantism has a median age at diagnosis of about 16 years of age. Patients with pituitary acrogigantism have a heavy burden of disease and a complex treatment journey; the need to control final height makes it imperative to provide a diagnosis and effective hormonal control as rapidly as possible. Multimodal therapy is often required, and this can be complicated by the need for medical therapies that are not labeled for use in the pediatric population.

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垂体促性腺激素:从过去到未来。
垂体促性腺激素亢进症是一种非常罕见的疾病,它是由于生长激素(GH)轴长期过剩而引起的,起病于儿童和青少年时期。因此,它是肢端肥大症最严重的表现之一。在大多数情况下,促肾上腺皮质激素增多症是由垂体腺瘤引起的,但增生也可能伴随腺瘤或很少单独发生。由于外周神经内分泌肿瘤分泌的促肾上腺皮质激素过多,刺激垂体促肾上腺皮质激素分泌过多,导致垂体促性腺激素亢进症的个别病例也有报道。约有一半的垂体促性腺激素增多症患者携带可识别的种系基因改变(致病变体、拷贝数变异、拓扑相关域(TAD)改变、嵌合),使其成为基因决定性最强的内分泌肿瘤之一。在遗传原因中,AIP 基因的致病变异(30%)、TAD 病变 X 连锁渐冻人症(10%)和 McCune-Albright 综合征(5%)是最常见的原因。这些遗传和基因组变化引起的分子改变会导致大型侵袭性体细胞瘤,这种瘤发生于幼年,能分泌大量 GH,并能使胰岛素样生长因子 1 产生抗药性。X-连锁性促甲状腺机能亢进症发生在出生后的第一年,通常在 36 个月大时出现,而与麦库恩-阿尔布莱特综合征相关的 GH 过多症通常在 5 岁前出现。与 AIP 相关的垂体促性腺激素过剩症的中位诊断年龄约为 16 岁。垂体促性腺激素增多症患者的疾病负担沉重,治疗过程复杂;由于需要控制最终身高,因此必须尽快确诊并进行有效的激素控制。通常需要进行多模式治疗,而这可能会因为需要使用未标注用于儿童的药物疗法而变得复杂。
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