磷酸二酯酶11A是原发性双侧大结节性肾上腺增生的表型调节因子：334例患者系列研究结果

PDE11A Is a Phenotype Modulator of Primary Bilateral Macronodular Adrenal Hyperplasia: Results of a 334-Patient Series.

作者信息

Vaduva Patricia, Bouys Lucas, Jouinot Anne, Espiard Stephanie, Chansavang Albain, Berthon Annabel, Néou Mario, Vaczlavik Anna, Violon Florian, Charchar Helaine, Kroiss Matthias, Raverot Gerald, Lasolle Helene, Guignat Laurence, Libé Rossella, Assié Guillaume, Tabarin Antoine, Kamenicky Peter, Pasmant Eric, Fragoso Maria, Stratakis Constantine, Ragazzon Bruno, Bertherat Jérôme

机构信息

Institut Cochin, INSERM U1016, CNRS UMR8104, Paris Descartes University, Paris 75014, France.

Department of Endocrinology, Reference Center for Rare Adrenal Diseases, Assistance Publique Hôpitaux de Paris, Hôpital Cochin, Paris 75014, France.

出版信息

J Clin Endocrinol Metab. 2025 Aug 7;110(9):e2946-e2955. doi: 10.1210/clinem/dgae918.

DOI:10.1210/clinem/dgae918

PMID:39774659

Abstract

CONTEXT

Primary bilateral macronodular adrenal hyperplasia (PBMAH), the most common cause of Cushing syndrome due to bilateral nodules, is a heterogeneous disease at the clinical, hormonal, and morphological levels. ARMC5-inactivating pathogenic variants are causative of PBMAH, and rare variants of PDE11A have been associated with PBMAH.

OBJECTIVE

The aim of this study, on a large cohort of individuals with PBMAH from Europe and America, was to study the ARMC5 and PDE11A genotype to determine the genotype/phenotype correlation and to investigate the hypothesis that PDE11A could be a modifying gene of the adrenal phenotype.

METHODS

Leukocyte DNA of 354 PBMAH index cases was sequenced for ARMC5 and PDE11A genes by next-generation sequencing. Phenotypic characteristics of 334 of these patients were analyzed to study the genotype/phenotype correlations.

RESULTS

Seven out of 16 PDE11A variants were considered damaging according to in silico predictions: 6 missense variants (p.Tyr727Cys, p.Met623Arg, p.Tyr658Cys, p.Ag867Trp, p.Asn298Ser, p.Glu840Lys) and 1 stop-gain variant (p.Arg307Ter). In the cohort, 11.4% of patients had one of these variants and 19.2% had ARMC5-pathogenic variants. There was no statistically significant difference in the distribution of PDE11A-damaging variants according to ARMC5 status (P = .83; OR = 0.79; 95% CI, 0.26-2.03) nor in the distribution of ARMC5 pathogenic variants according to PDE11A status (P = .83; OR = 0.81; 95% CI, 0.27-2.04). Patients with PDE11A-damaging variants had lower urinary free cortisol (0.7 vs 1.25 upper limit of normal; P = .0002), midnight plasma cortisol (157.81 vs 222.19 nmol/L, P = .016), and number of adrenal nodules (3.46 vs 4.74; P = .048) compared to PDE11A wild-type patients. Patients with ARMC5-pathogenic variants had a more severe phenotype with more frequent comorbidities and were more often treated by adrenalectomy (60%).

CONCLUSION

PDE11A appears to be a modulator of PBMAH phenotype, damaging variants being associated with an attenuated form. This may contribute to the heterogeneity of PBMAH and could affect patient management.

摘要

背景

原发性双侧大结节性肾上腺增生（PBMAH）是双侧结节导致库欣综合征的最常见原因，在临床、激素和形态学水平上是一种异质性疾病。ARMC5失活的致病变异是PBMAH的病因，PDE11A的罕见变异与PBMAH有关。

目的

本研究针对来自欧美地区的一大群PBMAH患者，旨在研究ARMC5和PDE11A基因型，以确定基因型/表型相关性，并探讨PDE11A可能是肾上腺表型修饰基因的假设。

方法

通过下一代测序对354例PBMAH索引病例的白细胞DNA进行ARMC5和PDE11A基因测序。分析其中334例患者的表型特征以研究基因型/表型相关性。

结果

根据计算机预测，16个PDE11A变异中有7个被认为具有损害性：6个错义变异（p.Tyr727Cys、p.Met623Arg、p.Tyr658Cys、p.Ag867Trp、p.Asn298Ser、p.Glu840Lys）和1个无义变异（p.Arg307Ter）。在该队列中，11.4%的患者有这些变异之一，19.2%的患者有ARMC5致病变异。根据ARMC5状态，PDE11A损害性变异的分布无统计学显著差异（P = 0.83；OR = 0.79；95%CI，0.26 - 2.03），根据PDE11A状态，ARMC5致病变异的分布也无统计学显著差异（P = 0.83；OR = 0.81；95%CI，0.27 - 2.