Endocrinology and Diabetes Research Group, Molecular Genetics Laboratory, Hospital de Cruces, 48903 Barakaldo, Bizkaia, Spain.
Eur J Endocrinol. 2010 Dec;163(6):953-62. doi: 10.1530/EJE-10-0435. Epub 2010 Sep 13.
Type I pseudohypoparathyroidism (PHP-I) can be subclassified into Ia and Ib, depending on the presence or absence of Albright's hereditary osteodystrophy's phenotype, diminished α-subunit of the stimulatory G protein (G(s)α) activity and multihormonal resistance. Whereas PHP-Ia is mainly associated with heterozygous inactivating mutations in G(s)α-coding exons of GNAS, PHP-Ib is caused by imprinting defects of GNAS. To date, just one patient with PHP and complete paternal uniparental disomy (UPD) has been described. We sought to identify the underlining molecular defect in twenty patients with parathyroid hormone resistance, hypocalcemia and hyperphosphatemia, and abnormal methylation pattern at GNAS locus.
Microsatellite typing and comparative genome hybridization were performed for proband and parents.
We describe four patients with partial paternal UPD of chromosome 20 involving pat20qUPD in one case, from 20q13.13-qter in two cases, and pat20p heterodisomy plus interstitial 20q isodisomy in one patient.
These observations demonstrate that mitotic recombination of chromosome 20 can also give rise to UPD and PHP, a situation similar to other imprinting disorders, such as Beckwith-Wiedemann syndrome or neonatal diabetes.
I 型假性甲状旁腺功能减退症(PHP-I)可根据是否存在阿尔布莱特遗传性骨营养不良的表型、刺激性 G 蛋白(G(s)α)α亚单位活性降低和多种激素抵抗,分为 Ia 和 Ib 亚型。PHP-Ia 主要与 GNAS 编码外显子的 G(s)α 异源失活突变相关,而 PHP-Ib 则由 GNAS 的印迹缺陷引起。迄今为止,仅描述了一例 PHP 和完全父源单亲二体性(UPD)的患者。我们试图在 20 名甲状旁腺激素抵抗、低钙血症和高磷血症以及 GNAS 基因座异常甲基化模式的患者中确定潜在的分子缺陷。
对先证者及其父母进行微卫星分型和比较基因组杂交。
我们描述了 4 名患者存在部分父源 UPD 20 号染色体,其中 1 例涉及 pat20qUPD,2 例涉及 20q13.13-qter,1 例涉及 pat20p 杂合性和 20q 染色体间异源二体性。
这些观察结果表明,20 号染色体的有丝分裂重组也可导致 UPD 和 PHP,这种情况类似于其他印迹疾病,如贝克威思-威德曼综合征或新生儿糖尿病。
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