Plastic, Reconstructive and Hand Surgery, Erasmus MC, Rotterdam, The Netherlands
Plastic, Reconstructive and Hand Surgery, Erasmus MC, Rotterdam, The Netherlands.
J Med Genet. 2021 Jun;58(6):362-368. doi: 10.1136/jmedgenet-2020-106948. Epub 2020 Jun 26.
Pathogenic DNA variants in the GLI-Kruppel family member 3 ( gene are known to cause multiple syndromes: for example, Greig syndrome, preaxial polydactyly-type 4 (PPD4) and Pallister-Hall syndrome. Out of these, Pallister-Hall is a different entity, but the distinction between Greig syndrome and PPD4 is less evident. Using latent class analysis (LCA), our study aimed to investigate the correlation between reported limb anomalies and the reported variants in these GLI3-mediated polydactyly syndromes. We identified two subclasses of limb anomalies that relate to the underlying variant.
Both local and published cases were included for analysis. The presence of individual limb phenotypes was dichotomised and an exploratory LCA was performed. Distribution of phenotypes and genotypes over the classes were explored and subsequently the key predictors of latent class membership were correlated to the different clustered genotypes.
297 cases were identified with 127 different variants in the gene. A two-class model was fitted revealing two subgroups of patients with anterior versus posterior anomalies. Posterior anomalies were observed in cases with truncating variants in the activator domain (postaxial polydactyly; hand, OR: 12.7; foot, OR: 33.9). Multivariate analysis supports these results (Beta: 1.467, p=0.013 and Beta: 2.548, p<0.001, respectively). Corpus callosum agenesis was significantly correlated to these variants (OR: 8.8, p<0.001).
There are two distinct phenotypes within the GLI3-mediated polydactyly population: anteriorly and posteriorly orientated. Variants that likely produce haploinsufficiency are associated with anterior phenotypes. Posterior phenotypes are associated with truncating variants in the activator domain. Patients with these truncating variants have a greater risk for corpus callosum anomalies.
已知 GLI-Kruppel 家族成员 3(基因中的致病 DNA 变体可导致多种综合征:例如,Greig 综合征、前轴多指畸形 4(PPD4)和 Pallister-Hall 综合征。在这些综合征中,Pallister-Hall 是一种不同的实体,但 Greig 综合征和 PPD4 之间的区别不太明显。使用潜在类别分析(LCA),我们的研究旨在调查报告的肢体异常与这些 GLI3 介导的多指畸形综合征中报告的变体之间的相关性。我们确定了与潜在变体相关的两种肢体异常亚类。
本研究纳入了局部和已发表的病例进行分析。将个体肢体表型的存在进行二分,并进行探索性 LCA。研究了表型和基因型在各分类中的分布,并随后将潜在类别成员的关键预测因子与不同聚类的基因型相关联。
共确定了 297 例病例,其中基因存在 127 种不同的变体。拟合了一个两类别模型,揭示了具有前侧和后侧异常的两个亚组患者。在后激活域截断变体中观察到后侧异常(多指畸形;手,OR:12.7;脚,OR:33.9)。多变量分析支持这些结果(Beta:1.467,p=0.013 和 Beta:2.548,p<0.001)。胼胝体发育不全与这些变体显著相关(OR:8.8,p<0.001)。
在 GLI3 介导的多指畸形人群中存在两种不同的表型:前向和后向定向。可能产生杂合不足的变体与前表型相关。后表型与激活域的截断变体相关。这些截断变体的患者胼胝体异常的风险更大。
