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Influence of serotonin transporter gene polymorphisms on cognitive decline and cognitive abilities in a nondemented elderly population

机译:血清素转运蛋白基因多态性对无痴呆老年人群认知能力下降和认知能力的影响

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Dysfunction of the serotonergic pathway disrupts normal cognitive functioning and is believed to be the underlying basis for a variety of psychiatric disorders. Two functional polymorphisms within the serotonin transporter (SLC6A4) gene (promoter 44bp insertion/deletion (HTTLPR) and an intron two 16 or 17bp variable number tandem repeat (VNTR2)) have been extensively studied in psychiatric conditions but not in the cognitive functioning of normal individuals. We have investigated these two polymorphisms for association with both the level of cognitive abilities and their decline with age using a cohort consisting of over 750 elderly nondemented individuals with a follow-up of up to 15 years. We found that volunteers homozygous for the VNTR2 12 allele had a faster rate of decline for all cognitive tests. This reached significance for both tests of fluid intelligence (novel problem solving) (AH1 P=0.002, AH2 P=0.014), the test of semantic memory (P=0.010) and general cognitive ability (P=0.006). No association was observed between the HTTLPR polymorphism and the rate of cognitive decline when analysed either independently or in combination with the VNTR2 polymorphism based on their influence on expression in vitro. No associations were observed between the two polymorphisms and the baseline level of cognitive abilities. This is only the second gene that has been reported to regulate the rate of cognitive decline in nondemented individuals and may be a target for the treatment of cognitive impairment in the elderly.
机译:血清素能通路的功能障碍破坏了正常的认知功能,被认为是各种精神疾病的潜在基础。血清素转运蛋白(SLC6A4)基因中的两个功能多态性(启动子44bp插入/缺失(HTTLPR)和一个内含子两个16或17bp可变数目的串联重复序列(VNTR2))已在精神病学条件下进行了广泛研究,但未在正常人的认知功能中进行研究个人。我们已经研究了这两个多态性与认知能力水平及其随年龄下降的关系,该队列由超过750名老年非痴呆症患者组成,随访时间长达15年。我们发现VNTR2 12等位基因纯合的志愿者在所有认知测验中的下降速度都更快。这对于流体智力测试(新问题解决)(AH1 P = 0.002,AH2 P = 0.014),语义记忆测试(P = 0.010)和一般认知能力测试(P = 0.006)都具有重要意义。根据其对体外表达的影响,单独或与VNTR2多态性结合分析时,在HTTLPR多态性与认知下降率之间未发现关联。在两个多态性和认知能力的基线水平之间未发现关联。这只是据报道调节非痴呆个体认知下降速度的第二个基因,可能是治疗老年人认知障碍的目标。

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