Department of Pediatrics, Vanderbilt University Medical Center, Nashville, TN, USA.
Clin Genet. 2010 Mar;77(3):280-6. doi: 10.1111/j.1399-0004.2009.01311.x. Epub 2010 Jan 20.
Bone morphogenetic protein receptor type 2 (BMPR2) gene mutations are a major risk factor for heritable pulmonary arterial hypertension (HPAH), an autosomal dominant fatal disease. We have previously shown that BMPR2 transcripts that contain premature termination codon (PTC) mutations are rapidly and nearly completely degraded through nonsense mediated decay (NMD). Here we report a unique PTC mutation (W13X) that did not behave in the predicted manner. We found that patient-derived cultured lymphocytes (CLs) contained readily detectable levels of the PTC-containing transcript. Further analysis suggested that this transcript escaped NMD by translational re-initiation at a downstream Kozak sequence, resulting in the omission of 173 amino acids. Treatment of CLs containing the PTC with an aminoglycoside decreased the truncated protein levels, with a reciprocal increase in full-length BMPR2 protein and, importantly, BMPR-II signaling. This is the first demonstration of aminoglycoside-mediated 'repair' of a BMPR2 mutation at the protein level in patient-derived cells and has obvious implications for treatment of HPAH where no disease-specific treatment options are available. Our data also suggest the need for a more thorough characterization of mutations prior to labeling them as haploinsufficient or dominant negative based simply on sequencing data.
骨形成蛋白受体 2 型(BMPR2)基因突变是遗传性肺动脉高压(HPAH)的一个主要危险因素,HPAH 是一种常染色体显性致命疾病。我们之前已经表明,含有提前终止密码子(PTC)突变的 BMPR2 转录本通过无意义介导的衰变(NMD)迅速且几乎完全降解。在这里,我们报告了一个独特的 PTC 突变(W13X),其行为不符合预期。我们发现,源自患者的培养淋巴细胞(CL)中含有可检测到的 PTC 转录本。进一步的分析表明,该转录本通过在下游 Kozak 序列处进行翻译重新起始而逃脱了 NMD,从而导致 173 个氨基酸缺失。用氨基糖苷类药物处理含有 PTC 的 CLs 会降低截短蛋白的水平,同时全长 BMPR2 蛋白的水平会相应增加,重要的是,BMPR-II 信号也会增加。这是首次在患者来源的细胞中在蛋白质水平上证明氨基糖苷类药物介导的 BMPR2 突变“修复”,这对 HPAH 的治疗具有明显意义,因为目前尚无针对这种疾病的特定治疗方法。我们的数据还表明,在简单地根据测序数据将突变标记为杂合不足或显性负性之前,需要更彻底地对突变进行特征描述。
