Iacono Diego, Volkman Inga, Nennesmo Inger, Pedersen Nancy L, Fratiglioni Laura, Johansson Boo, Karlsson David, Winblad Bengt, Gatz Margaret
The Brain Bank at Karolinska Institutet, KI Alzheimer Disease Research Center, Department of Neurobiology, Care Sciences and Society (NVS), Karolinska Institutet, Stockholm, Sweden; Neuropathology Research, Biomedical Research Institute of New Jersey, BRInj, Cedar Knolls, NJ.
Brain Pathol. 2014 Jul;24(4):317-33. doi: 10.1111/bpa.12127. Epub 2014 Mar 7.
Twin studies are an incomparable source of investigation to shed light on genetic and non-genetic components of neurodegenerative diseases, as Alzheimer's disease (AD). Detailed clinicopathologic correlations using twin longitudinal data and post-mortem examinations are mostly missing. We describe clinical and pathologic findings of seven monozygotic (MZ) and dizygotic (DZ) twin pairs. Our findings show good agreement between clinical and pathologic diagnoses in the majority of the twin pairs, with greater neuropathologic concordance in MZ than DZ twins. Greater neuropathologic concordance was found for β-amyloid than tau pathology within the pairs. ApoE4 was associated with higher β-amyloid and earlier dementia onset, and importantly, higher frequency of other co-occurring brain pathologies, regardless of the zygosity. Dementia onset, dementia duration, difference between twins in age at dementia onset and at death, did not correlate with AD pathology. These clinicopathologic correlations of older identical and fraternal twins support the relevance of genetic factors in AD, but not their sufficiency to determine the pathology, and consequently the disease, even in monozygotic twins. It is the interaction among genetic and non-genetic risks which plays a major role in influencing, or probably determining, the degeneration of those brain circuits associated with pathology and cognitive deficits in AD.
双胞胎研究是揭示神经退行性疾病(如阿尔茨海默病,AD)的遗传和非遗传成分的无与伦比的研究来源。使用双胞胎纵向数据和尸检进行详细的临床病理相关性分析大多缺失。我们描述了7对同卵(MZ)和异卵(DZ)双胞胎的临床和病理发现。我们的研究结果表明,大多数双胞胎对的临床和病理诊断之间具有良好的一致性,MZ双胞胎的神经病理一致性高于DZ双胞胎。在双胞胎对中,β淀粉样蛋白的神经病理一致性高于tau病理。载脂蛋白E4与更高的β淀粉样蛋白水平和更早的痴呆症发病相关,重要的是,无论合子性如何,其他同时出现的脑部病变的频率更高。痴呆症发病、痴呆症持续时间、双胞胎在痴呆症发病和死亡时的年龄差异与AD病理无关。这些老年同卵和异卵双胞胎的临床病理相关性支持了遗传因素在AD中的相关性,但不支持其足以决定病理,进而决定疾病,即使在同卵双胞胎中也是如此。遗传和非遗传风险之间的相互作用在影响或可能决定与AD病理和认知缺陷相关的脑回路退化方面起着主要作用。