软骨形成II型(ACG2)是由COL2A1中的显性致病变异引起的致死性骨骼发育不良。在患有ACG2的患者中发现的大多数变体影响Gly-X-Y三肽重复中包括的甘氨酸残基,其表征II型胶原螺旋。在这项研究中,我们报道了一例患有ACG2的胎儿中COL2A1的新型剪接变体。胎儿DNA的NGS分析揭示了位于内含子20/外显子21中的杂合变体c.1267-2_1269del。该变体从头发生,因为在来自父母的血液样品的DNA中未检测到它。我们产生了合适的小基因构建体以研究检测到的变体的作用。小基因表达导致缺乏外显子21的COL2A1信使RNA的合成,从而产生了预测的框内缺失蛋白。通常,COL2A1的框内缺失变体导致表型,如Kniest发育不良,比ACG2温和。因此,我们认为COL2A1中框内缺失的大小和位置可能与确定骨骼发育不良的表型有关.
Achondrogenesis type II (ACG2) is a lethal skeletal dysplasia caused by dominant pathogenic variants in COL2A1. Most of the variants found in patients with ACG2 affect the glycine residue included in the Gly-X-Y tripeptide repeat that characterizes the type II collagen helix. In this study, we reported a case of a novel splicing variant of COL2A1 in a fetus with ACG2. An NGS analysis of fetal DNA revealed a heterozygous variant c.1267-2_1269del located in intron 20/exon 21. The variant occurred de novo since it was not detected in DNA from the blood samples of parents. We generated an appropriate minigene construct to study the effect of the variant detected. The minigene expression resulted in the synthesis of a COL2A1 messenger RNA lacking exon 21, which generated a predicted in-frame deleted protein. Usually, in-frame deletion variants of COL2A1 cause a phenotype such as Kniest dysplasia, which is milder than ACG2. Therefore, we propose that the size and position of an in-frame deletion in COL2A1 may be relevant in determining the phenotype of skeletal dysplasia.
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