首例 HIF2A 相关红细胞增多症-副神经节瘤综合征临床谱中的双侧嗜铬细胞瘤报告。
First report of bilateral pheochromocytoma in the clinical spectrum of HIF2A-related polycythemia-paraganglioma syndrome.
机构信息
Department of Nuclear Medicine, La Timone University Hospital, Centre Européen de Recherche en Imagerie Médicale, Aix-Marseille University, 13005 Marseille, France.
出版信息
J Clin Endocrinol Metab. 2013 May;98(5):E908-13. doi: 10.1210/jc.2013-1217. Epub 2013 Mar 28.
CONTEXT
Molecular genetic research has so far resulted in the identification of 10 well-characterized susceptibility genes for hereditary pheochromocytoma (PHEO) or paraganglioma (PGL). Recently, a new syndrome characterized by multiple PGLs and somatostatinomas associated with congenital polycythemia due to somatic mutations in HIF2A has been reported.
OBJECTIVE
The aim of the study was to define the genetic defect in a new case of bilateral PHEO and multiple PGLs associated with congenital polycythemia.
PATIENT
A female patient presented with neonatal polycythemia (treated by phlebotomies, 1 session approximately every 4 mo), mildly enlarged cerebral ventricles, and bilateral PHEO and multiple PGLs. There was no family history of any neuroendocrine tumor or polycythemia. Surgical removal of the tumors only temporarily normalized plasma erythropoietin (Epo) levels and discontinued phlebotomies. No germline mutations were initially detected in the SDHB, SDHC, SDHD, VHL, and PHD2 genes, known to be associated with polycythemia. The PHEOs presented with a typical noradrenergic biochemical phenotype.
RESULTS
A heterozygous missense mutation (c.1589C>T) was identified in exon 12 of HIF2A, resulting in an alanine 530 substitution in the HIF-2α protein with valine (A530V). This somatic mutation was detected in the tissue from 1 PHEO and 1 PGL, with no HIF2A germline mutation found. This mutation led to stabilization of HIF-2α and hence a gain-of-function phenotype, as in previously published studies.
CONCLUSION
This case represents the first association of a somatic HIF2A gain-of-function mutation with PHEO and congenital polycythemia, and it alerts physicians to perform proper genetic screening in patients presenting with multiple norepinephrine-producing PHEOs and polycythemia. This report also extends the previous findings of a new syndrome of only multiple PGLs, somatostatinomas, and polycythemia to multiple PHEOs.
背景
分子遗传学研究已经确定了 10 个明确的遗传性嗜铬细胞瘤(PHEO)或副神经节瘤(PGL)易感基因。最近,据报道了一种新的综合征,其特征为多发性 PGL 和生长抑素瘤,与由于 HIF2A 的体细胞突变导致的先天性红细胞增多症有关。
目的
本研究旨在确定一例新的双侧 PHEO 和多发性 PGL 伴先天性红细胞增多症患者的遗传缺陷。
患者
一名女性患者出生时患有新生儿红细胞增多症(通过放血治疗,大约每 4 个月进行 1 次治疗)、轻度扩大的脑室和双侧 PHEO 和多发性 PGL。家族中没有任何神经内分泌肿瘤或红细胞增多症的病史。肿瘤的手术切除仅暂时使血浆促红细胞生成素(Epo)水平正常化,并停止了放血治疗。最初在 SDHB、SDHC、SDHD、VHL 和 PHD2 基因中未检测到与红细胞增多症相关的种系突变。PHEOs 表现出典型的去甲肾上腺素生化表型。
结果
在 HIF2A 的外显子 12 中发现了杂合错义突变(c.1589C>T),导致 HIF-2α 蛋白中的丙氨酸 530 被缬氨酸取代(A530V)。该体细胞突变在 1 个 PHEO 和 1 个 PGL 组织中被检测到,未发现 HIF2A 种系突变。该突变导致 HIF-2α 的稳定,从而产生了之前发表的研究中观察到的功能获得表型。
结论
该病例代表了首例与 PHEO 和先天性红细胞增多症相关的 HIF2A 获得性功能突变,它提醒医生在患有多个产生去甲肾上腺素的 PHEO 和红细胞增多症的患者中进行适当的遗传筛查。该报告还将之前仅发现的多发性 PGL、生长抑素瘤和红细胞增多症的新综合征扩展到了多发性 PHEO。
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