Pretto Dalyir I, Eid John S, Yrigollen Carolyn M, Tang Hiu-Tung, Loomis Erick W, Raske Chris, Durbin-Johnson Blythe, Hagerman Paul J, Tassone Flora
Department of Biochemistry and Molecular Medicine, University of California, School of Medicine, Davis, California, USA.
Pacific Biosciences, Menlo Park, California, USA.
J Med Genet. 2015 Jan;52(1):42-52. doi: 10.1136/jmedgenet-2014-102593. Epub 2014 Oct 30.
Over 40% of male and ∼16% of female carriers of a premutation FMR1 allele (55-200 CGG repeats) will develop fragile X-associated tremor/ataxia syndrome, an adult onset neurodegenerative disorder, while about 20% of female carriers will develop fragile X-associated primary ovarian insufficiency. Marked elevation in FMR1 mRNA transcript levels has been observed with premutation alleles, and RNA toxicity due to increased mRNA levels is the leading molecular mechanism proposed for these disorders. However, although the FMR1 gene undergoes alternative splicing, it is unknown whether all or only some of the isoforms are overexpressed in premutation carriers and which isoforms may contribute to the premutation pathology.
To address this question, we have applied a long-read sequencing approach using single-molecule real-time (SMRT) sequencing and qRT-PCR.
Our SMRT sequencing analysis performed on peripheral blood mononuclear cells, fibroblasts and brain tissue samples derived from premutation carriers and controls revealed the existence of 16 isoforms of 24 predicted variants. Although the relative abundance of all mRNA isoforms was significantly increased in the premutation group, as expected based on the bulk increase in mRNA levels, there was a disproportionate (fourfold to sixfold) increase, relative to the overall increase in mRNA, in the abundance of isoforms spliced at both exons 12 and 14, specifically Iso10 and Iso10b, containing the complete exon 15 and differing only in splicing in exon 17.
These findings suggest that RNA toxicity may arise from a relative increase of all FMR1 mRNA isoforms. Interestingly, the Iso10 and Iso10b mRNA isoforms, lacking the C-terminal functional sites for fragile X mental retardation protein function, are the most increased in premutation carriers relative to normal, suggesting a functional relevance in the pathology of FMR1-associated disorders.
携带前突变FMR1等位基因(55 - 200个CGG重复序列)的男性中超过40%以及女性中约16%会患上脆性X相关震颤/共济失调综合征,这是一种成人起病的神经退行性疾病,而约20%的女性携带者会患上脆性X相关原发性卵巢功能不全。在前突变等位基因中观察到FMR1 mRNA转录水平显著升高,并且由于mRNA水平升高导致的RNA毒性是针对这些疾病提出的主要分子机制。然而,尽管FMR1基因经历可变剪接,但尚不清楚所有异构体还是只有一些异构体在前突变携带者中过度表达,以及哪些异构体可能导致前突变病理。
为了解决这个问题,我们应用了使用单分子实时(SMRT)测序和qRT - PCR的长读长测序方法。
我们对来自前突变携带者和对照的外周血单核细胞、成纤维细胞和脑组织样本进行的SMRT测序分析揭示了24个预测变体中的16种异构体的存在。尽管基于mRNA水平的总体增加,所有mRNA异构体的相对丰度在前突变组中显著增加,但相对于mRNA的总体增加,在第12和14外显子均进行剪接的异构体丰度有不成比例的(四倍至六倍)增加,特别是Iso10和Iso10b,它们包含完整的第15外显子,仅在第17外显子的剪接上有所不同。
这些发现表明RNA毒性可能源于所有FMR1 mRNA异构体的相对增加。有趣的是,缺乏脆性X智力低下蛋白功能的C末端功能位点的Iso10和Iso10b mRNA异构体在前突变携带者中相对于正常情况增加最多,表明其在FMR1相关疾病的病理中具有功能相关性。
