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微管相关蛋白Tau具有心血管功能的证据。

Evidence of a Cardiovascular Function for Microtubule-Associated Protein Tau.

作者信息

Betrie Ashenafi H, Ayton Scott, Bush Ashley I, Angus James A, Lei Peng, Wright Christine E

机构信息

Department of Pharmacology and Therapeutics, Cardiovascular Therapeutics Unit, The University of Melbourne, VIC, Australia.

The Florey Institute for Neuroscience and Mental Health, The University of Melbourne, Parkville, VIC, Australia.

出版信息

J Alzheimers Dis. 2017;56(2):849-860. doi: 10.3233/JAD-161093.

Abstract

Aggregation of tau protein into intracellular deposits is a pathognomonic feature of tauopathies such as Alzheimer's disease (AD) and lowering tau is a prominent therapeutic strategy under development. However, the physiological function of tau protein is not well known, particularly in the periphery. Lowering tau protein risks disrupting its physiological role leading to unwanted effects. In this study, the presence of tau protein in cardiac tissue is confirmed and the functional role in the cardiovascular system and the consequences of its loss were explored. Isolated right and left atria and small mesenteric arteries from wild type and tau deficient (KO) mice of two age groups (13 and 23 months old) were used to assess cardiovascular phenotypes. Tau KO mice showed an increased systolic blood pressure and cardiac hypertrophy at 13 months, which was accompanied by a significantly lower right atrial rate and a subtle decrease in the maximum contractility to calcium, isoprenaline, and electrical sympathetic nerve stimulation. Aging tau KO mice to 23 months resulted in cardiac hypertrophy with significantly attenuated left atrial contractility, increased blood pressure, and sensitivity of isolated mesenteric arteries to angiotensin II contraction and isoprenaline relaxation compared to their younger counterparts. This study supports a functional role of tau in the heart and loss of this protein leads to a deterioration in cardiovascular performance which worsens with age. Taken together, these results provide insight into the peripheral function of tau protein, and give caution to the therapeutic strategy of lowering tau protein.

摘要

tau蛋白聚集成细胞内沉积物是诸如阿尔茨海默病(AD)等tau蛋白病的一个特征性表现,降低tau蛋白水平是正在研发的一项重要治疗策略。然而,tau蛋白的生理功能尚不清楚,尤其是在外周组织中。降低tau蛋白水平可能会破坏其生理作用,从而导致不良影响。在本研究中,证实了心脏组织中存在tau蛋白,并探讨了其在心血管系统中的功能作用及其缺失的后果。使用来自两个年龄组(13个月和23个月大)的野生型和tau蛋白缺陷(KO)小鼠的分离右心房和左心房以及小肠系膜小动脉来评估心血管表型。13个月大的tau KO小鼠收缩压升高且出现心脏肥大,同时右心房率显著降低,对钙、异丙肾上腺素和交感神经电刺激的最大收缩力略有下降。将tau KO小鼠饲养至23个月,与年轻小鼠相比,出现心脏肥大,左心房收缩力显著减弱,血压升高,分离的小肠系膜动脉对血管紧张素II收缩和异丙肾上腺素舒张的敏感性增加。本研究支持tau蛋白在心脏中的功能作用,该蛋白的缺失会导致心血管功能恶化,且随着年龄增长而加剧。综上所述,这些结果为tau蛋白的外周功能提供了见解,并对降低tau蛋白的治疗策略提出了警示。

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