Instituto de Investigaciones Biomédicas, Consejo Superior de Investigaciones Científicas, Universidad Autónoma de Madrid, Madrid, Spain.
Hum Mutat. 2012 Oct;33(10):1444-9. doi: 10.1002/humu.22133. Epub 2012 Jul 5.
PLOD2 and FKBP10 are genes mutated in Bruck syndrome (BS), a condition resembling osteogenesis imperfecta (OI), but that is also typically associated with congenital joint contractures. Herein, we sought mutations in six consanguineous BS families and detected changes in either PLOD2 or FKBP10 in all cases. Two probands were found with a homozygous frameshift mutation in the alternative exon 13a of PLOD2, indicating that specific inactivation of the longer protein isoform encoded by this gene is sufficient to cause BS. In addition, by homozygosity mapping, followed by a candidate gene approach, we identified a homozygous donor splice site mutation in PLOD2 in a patient with autosomal-recessive OI (AR-OI). Screening of additional samples also revealed compound heterozygous mutations in PLOD2 in two brothers, one affected with mild AR-OI and the other with mild BS. Thus, PLOD2 in addition to causing BS is also associated with AR-OI phenotypes of variable severity.
PLOD2 和 FKBP10 是 Bruck 综合征(BS)的突变基因,该病类似于成骨不全症(OI),但通常还与先天性关节挛缩有关。在此,我们在六个近亲 BS 家族中寻找突变,并在所有病例中均发现 PLOD2 或 FKBP10 发生变化。两名先证者被发现 PLOD2 的选择性外显子 13a 中存在纯合移码突变,表明该基因编码的较长蛋白异构体的特异性失活足以导致 BS。此外,通过纯合子作图,然后通过候选基因方法,我们在一名常染色体隐性 OI(AR-OI)患者中发现 PLOD2 的纯合供体剪接位点突变。对其他样本的筛查还显示,两名兄弟均存在 PLOD2 的复合杂合突变,其中一人患有轻度 AR-OI,另一人患有轻度 BS。因此,PLOD2 除了引起 BS 之外,还与不同严重程度的 AR-OI 表型有关。
