The microtubule-associated protein tau (MAPT) region has been conceptualized as a model of the interaction between genetics and functional disease outcomes in neurodegenerative disorders, such as Parkinson disease (PD). Indeed, haplotype-specific differences in expression and alternative splicing of MAPT transcripts affect cellular functions at different levels, increasing susceptibility to a range of neurodegenerative processes. In order to evaluate a possible link between MAPT variants, PD risk and PD motor phenotype, we analyzed the genetic architecture of MAPT in a cohort of PD patients. We observed a statistically significant association between the H1 haplotype and PD risk (79.5 vs 69.5%; χ~(2)= 9.9; OR, 1.7; 95% CI, 1.2–2.4; p = 0.002). The effect was more evident in non tremor dominant (TD) PD subjects (NTD-PD) (82 vs 69.5%; χ~(2)= 13.6; OR, 2.03; 95% CI, 1.4–3; p = 0.0003), while no difference emerged between PD subgroup of tremor dominant patients (TD-PD) and control subjects. Examination of specific intra-H1 variations showed that the H1h subhaplotype was overrepresented in NTD-PD patients compared with controls ( p = 0.007; OR, 2.9; 95% CI, 1.3–6.3). Although we cannot exclude that MAPT variation may be associated with ethnicity, our results may support the hypothesis that MAPT H1 clade and a specific H1 subhaplotype influence the risk of PD and modulate the clinical expression of the disease, including motor phenotype.
展开▼
机译:微管相关蛋白tau(MAPT)区域已被概念化为遗传和神经退行性疾病(如帕金森病(PD))中功能性疾病结局之间相互作用的模型。实际上,MAPT转录物的表达和替代剪接的单倍型特异性差异在不同水平上影响细胞功能,增加了对一系列神经变性过程的敏感性。为了评估MAPT变异,PD风险和PD运动表型之间的可能联系,我们分析了一群PD患者中MAPT的遗传结构。我们观察到H1单倍型与PD风险之间存在统计学上的显着相关性(79.5 vs 69.5%;χ〜(2)= 9.9; OR,1.7; 95%CI,1.2–2.4; p = 0.002)。在非震颤显性(TD)PD受试者(NTD-PD)中,这种效应更为明显(82 vs 69.5%;χ〜(2)= 13.6; OR,2.03; 95%CI,1.4–3; p = 0.0003),而震颤显性患者的PD亚组(TD-PD)与对照组之间没有差异。检查特定的H1内变异表明,NTD-PD患者的H1h亚型与对照组相比过高(p = 0.007; OR,2.9; 95%CI,1.3–6.3)。尽管我们不能排除MAPT变异可能与种族有关,但我们的结果可能支持MAPT H1进化枝和特定H1亚型影响PD风险并调节疾病临床表达(包括运动表型)的假设。
展开▼
