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《 unraveling :心脏和肌肉骨骼缺陷及其在常见阿尔茨海默病发病和死亡中的作用》。

The Unraveling: Cardiac and Musculoskeletal Defects and Their Role in Common Alzheimer Disease Morbidity and Mortality.

机构信息

Indiana Center for Musculoskeletal Health, Indiana University School of Medicine, Indianapolis, Indiana.

Department of Medicine, Medical University of South Carolina, Charleston, South Carolina.

出版信息

Am J Pathol. 2020 Aug;190(8):1609-1621. doi: 10.1016/j.ajpath.2020.04.013. Epub 2020 May 11.

DOI:10.1016/j.ajpath.2020.04.013
PMID:32407731
Abstract

Alzheimer disease (AD) is characterized by deterioration of cognitive capabilities with an estimated 44 million individuals worldwide living with it. Beyond memory deficits, the most common AD co-morbidities include swallowing defects (muscle), fractures (bone, muscle), and heart failure. The underlying causes of these co-morbidities and their role in AD pathophysiology are currently unknown. This review is the first to summarize the emerging picture of the cardiac and musculoskeletal deficits in human AD. We present the involvement of the heart, characterized by diastolic heart failure, the presence of amyloid deposits, and electrophysiological changes, compared with age-matched control subjects. The characteristic musculoskeletal defects in AD come from recent clinical studies and include potential underlying mechanisms (bone) in animal models. These studies detail a primary muscle weakness (without a loss of muscle mass) in patients with mild cognitive impairment, with progression of cognitive impairment to AD associating with ongoing muscle weakness and the onset of muscle atrophy. We conclude by reviewing the loss of bone density in patients with AD, paralleling the increase in fracture and fall risk in specific populations. These studies paint AD as a systemic disease in broad strokes, which may help elucidate AD pathophysiology and to allow for new ways of thinking about therapeutic interventions, diagnostic biomarkers, and the pathogenesis of this multidisciplinary disease.

摘要

阿尔茨海默病(AD)的特征是认知能力的恶化,据估计,全球有 4400 万人患有这种疾病。除了记忆缺陷,AD 最常见的合并症包括吞咽缺陷(肌肉)、骨折(骨骼、肌肉)和心力衰竭。这些合并症的根本原因及其在 AD 病理生理学中的作用目前尚不清楚。这是第一篇综述,总结了人类 AD 中心脏和肌肉骨骼缺陷的新发现。我们介绍了心脏的参与情况,其特征是舒张性心力衰竭、淀粉样蛋白沉积和电生理变化,并与年龄匹配的对照组进行了比较。AD 的特征性肌肉骨骼缺陷来自最近的临床研究,包括动物模型中的潜在潜在机制(骨骼)。这些研究详细描述了轻度认知障碍患者的主要肌肉无力(无肌肉质量损失),随着认知障碍进展为 AD,肌肉无力持续存在,肌肉萎缩开始出现。最后,我们回顾了 AD 患者的骨密度丧失,这与特定人群中骨折和跌倒风险的增加是平行的。这些研究将 AD 描绘成一种全身性疾病,这可能有助于阐明 AD 的病理生理学,并为治疗干预、诊断生物标志物和这种多学科疾病的发病机制提供新的思路。

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