Research Center for Molecular Medicine of the Austrian Academy of Sciences (CeMM), Vienna, Austria.
J Pediatr. 2012 Apr;160(4):679-683.e2. doi: 10.1016/j.jpeds.2011.09.019. Epub 2011 Nov 1.
To delineate the phenotypic and molecular spectrum of patients with a syndromic variant of severe congenital neutropenia (SCN) due to mutations in the gene encoding glucose-6-phosphatase catalytic subunit 3 (G6PC3).
Patients with syndromic SCN were characterized for associated malformations and referred to us for G6PC3 mutational analysis.
In a cohort of 31 patients with syndromic SCN, we identified 16 patients with G6PC3 deficiency including 11 patients with novel biallelic mutations. We show that nonhematologic features of G6PC3 deficiency are good predictive indicators for mutations in G6PC3. Additionally, we demonstrate genetic variability in this disease and define novel features such as growth hormone deficiency, genital malformations, disrupted bone remodeling, and abnormalities of the integument. G6PC3 mutations may be associated with hydronephrosis or facial dysmorphism. The risk of transition to myelodysplastic syndrome/acute myeloid leukemia may be lower than in other genetically defined SCN subgroups.
The phenotypic and molecular spectrum in G6PC3 deficiency is wider than previously appreciated. The risk of transition to myelodysplastic syndrome or acute myeloid leukemia may be lower in G6PC3 deficiency compared with other subgroups of SCN.
描述由于编码葡萄糖-6-磷酸酶催化亚基 3(G6PC3)的基因突变导致的综合征变异严重先天性中性粒细胞减少症(SCN)患者的表型和分子谱。
对伴有相关畸形的综合征性 SCN 患者进行特征描述,并将其转介至我们处进行 G6PC3 突变分析。
在一组 31 例综合征性 SCN 患者中,我们鉴定出 16 例 G6PC3 缺乏症患者,包括 11 例新的双等位基因突变患者。我们表明,G6PC3 缺乏症的非血液学特征是 G6PC3 突变的良好预测指标。此外,我们证明了这种疾病的遗传变异性,并定义了新的特征,如生长激素缺乏、生殖器畸形、骨重塑中断和皮肤异常。G6PC3 突变可能与肾积水或面部畸形有关。向骨髓增生异常综合征/急性髓系白血病转化的风险可能低于其他遗传定义的 SCN 亚组。
G6PC3 缺乏症的表型和分子谱比以前认识的更广泛。与其他 SCN 亚组相比,G6PC3 缺乏症向骨髓增生异常综合征或急性髓系白血病转化的风险可能更低。
