Evaluation of Associations of Growth Differentiation Factor-11, Growth Differentiation Factor-8, and Their Binding Proteins Follistatin and Follistatin-Like Protein-3 With Dementia and Cognition.

IF 4.3 2区 医学 Q1 GERIATRICS & GERONTOLOGY Journals of Gerontology Series A-Biological Sciences and Medical Sciences Pub Date : 2023-10-28 DOI:10.1093/gerona/glad019
Anne B Newman, Sheena Patel, Jorge R Kizer, Se-Jin Lee, Shalinder Bhasin, Peggy Cawthon, Nathan LeBrasseur, Russel P Tracy, Peter Ganz, Steven R Cummings
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Abstract

Background: Studies using heterochronic parabiosis discovered that circulating factors mediate brain aging in animal models.

Methods: We assessed growth differentiation factors (GDF)-11 and GDF-8 using mass spectrometry and inhibitors follistatin and follistatin-like protein-3 (FSTL-3) with ELISA in the Cardiovascular Health Study (CHS; N = 1 506) and the Health, Aging and Body Composition (Health ABC) Study (N = 1 237). CLL-11 and beta-2 microglobulin (β2M) were measured with ELISA in a subset of 400 individuals in Health ABC. Associations were assessed with cognitive function, brain magnetic resonance imaging (MRI) findings (CHS only), and incident dementia using correlations, linear regression, and Cox proportional hazards models.

Results: In CHS, levels of GDF-11, GDF-8, and follistatin were not correlated cross-sectionally with the 3MSE or DSST, brain MRI findings of white matter hyperintensity, atrophy, or small infarcts, nor were they associated with incident dementia. FSTL-3 was modestly correlated with poorer cognitive function, greater white matter hyperintensities, and atrophy on MRI, as well as with incident dementia with an adjusted hazard ratio (HR) of 1.72 (95% CI = 1.13, 2.61) per doubling of FSTL-3. FSTL-3 was not associated with cognition or dementia in Health ABC, but GDF-8 was associated with both. The adjusted HR for incident dementia was 1.50 (95% CI = 1.07, 2.10) per doubling of GDF-8.

Conclusions: Total GDF-11 level was not related to cognition or dementia in older adults. Associations of GDF-8 with cognitive outcomes in Health ABC were not expected, but consistent with animal models. Associations of FSTL-3 with cognition, brain abnormalities, and incident dementia in CHS implicate TGFβ superfamily inhibition in the pathogenesis of dementia.

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生长分化因子-11、生长分化因子-8及其结合蛋白Follistatin和Follistatin-样蛋白-3与痴呆和认知的相关性评估。
背景:利用异时共生研究发现,循环因子在动物模型中介导大脑衰老。方法:我们在心血管健康研究(CHS;N=1 506)和健康、衰老和身体成分研究(Health ABC)(N=1 237)中使用质谱法和抑制剂卵泡抑素和卵泡抑素样蛋白-3(FSTL-3)评估生长分化因子(GDF)-11和GDF-8。CLL-11和β-2微球蛋白(β2M)在健康ABC的400个个体的亚群中用ELISA进行测量。使用相关性、线性回归和Cox比例风险模型评估了认知功能、脑磁共振成像(MRI)结果(仅CHS)和痴呆事件的相关性。结果:在CHS中,GDF-11、GDF-8和卵泡抑素的水平与3MSE或DSST、白质高信号、萎缩或小梗死的脑MRI表现无横断面相关性,也与痴呆事件无关。FSTL-3与较差的认知功能、更大的白质高信号和MRI上的萎缩以及痴呆事件适度相关,FSTL-3每增加一倍,调整后的风险比(HR)为1.72(95%CI=1.132.61)。在健康ABC中,FSTL-3与认知或痴呆无关,但GDF-8与两者均相关。GDF-8每增加一倍,发生痴呆的校正HR为1.50(95%CI=1.07,2.10)。结论:老年人的总GDF-11水平与认知或痴呆无关。在健康ABC中,GDF-8与认知结果的相关性是不可预期的,但与动物模型一致。FSTL-3与CHS认知、大脑异常和偶发性痴呆的相关性表明TGFβ超家族抑制在痴呆的发病机制中。
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来源期刊
CiteScore
10.00
自引率
5.90%
发文量
233
审稿时长
3-8 weeks
期刊介绍: Publishes articles representing the full range of medical sciences pertaining to aging. Appropriate areas include, but are not limited to, basic medical science, clinical epidemiology, clinical research, and health services research for professions such as medicine, dentistry, allied health sciences, and nursing. It publishes articles on research pertinent to human biology and disease.
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