Myokines and Biomarkers of Frailty in Older Inpatients with Undernutrition: A Prospective Study.

IF 3.3 Q2 GERIATRICS & GERONTOLOGY

Journal of Frailty & Aging Pub Date : 2024-01-01 DOI:10.14283/jfa.2024.9

H Liu, W Li, M Zhu, X Wen, J Jin, H Wang, D Lv, S Zhao, X Wu, J Jiao

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Abstract

Background: Population aging might increase the prevalence of undernutrition in older people, which increases the risk of frailty. Numerous studies have indicated that myokines are released by skeletal myocytes in response to muscular contractions and might be associated with frailty. This study aimed to evaluate whether myokines are biomarkers of frailty in older inpatients with undernutrition.

Methods: The frailty biomarkers were extracted from the Gene Expression Omnibus and Genecards datasets. Relevant myokines and health-related variables were assessed in 55 inpatients aged ≥ 65 years from the Peking Union Medical College Hospital prospective longitudinal frailty study. Serum was prepared for enzyme-linked immunosorbent assay using the appropriate kits. Correlations between biomarkers and frailty status were calculated by Spearman's correlation analysis. Multiple linear regression was performed to investigate the association between factors and frailty scores.

Results: The prevalence of frailty was 13.21%. The bioinformatics analysis indicated that leptin, adenosine 5'-monophosphate-activated protein kinase (AMPK), irisin, decorin, and myostatin were potential biomarkers of frailty. The frailty group had significantly higher concentrations of leptin, AMPK, and MSTN than the robust group (p < 0.05). AMPK was significantly positively correlated with frailty (p < 0.05). The pre-frailty and frailty groups had significantly lower concentrations of irisin than the robust group (p < 0.05), whereas the DCN concentration did not differ among the groups. Multiple linear regression suggested that the 15 factors influencing the coefficients of association, the top 50% were the ADL score, MNA-SF score, serum albumin concentration, urination function, hearing function, leptin concentration, GDS-15 score, and MSTN concentration.

Conclusions: Proinflammatory myokines, particularly leptin, myostatin, and AMPK, negatively affect muscle mass and strength in older adults. ADL and nutritional status play major roles in the development of frailty. Our results confirm that identification of frailty relies upon clinical variables, myokine concentrations, and functional parameters, which might enable the identification and monitoring of frailty.

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老年营养不良住院病人的肌动蛋白和虚弱生物标志物：一项前瞻性研究

背景：人口老龄化可能会增加老年人营养不良的发生率，从而增加虚弱的风险。大量研究表明，骨骼肌细胞在肌肉收缩时会释放肌动蛋白，而肌动蛋白可能与虚弱有关。本研究旨在评估肌动蛋白是否是老年营养不良住院患者虚弱的生物标志物：方法：从基因表达总库（Gene Expression Omnibus）和基因卡（Genecards）数据集中提取虚弱生物标志物。对北京协和医院前瞻性纵向虚弱研究中 55 名年龄≥ 65 岁的住院患者进行了相关肌酸激酶和健康相关变量的评估。使用适当的试剂盒制备血清进行酶联免疫吸附测定。通过斯皮尔曼相关分析计算生物标志物与虚弱状态之间的相关性。采用多元线性回归法研究各因素与虚弱评分之间的关系：结果：虚弱患病率为 13.21%。生物信息学分析表明，瘦素、5'-单磷酸腺苷激活的蛋白激酶（AMPK）、鸢尾素、decorin 和肌生长激素是潜在的虚弱生物标志物。虚弱组的瘦素、AMPK 和 MSTN 浓度明显高于健壮组（P < 0.05）。AMPK 与虚弱程度呈显著正相关（p < 0.05）。虚弱前组和虚弱组的鸢尾素浓度明显低于健壮组（p < 0.05），而 DCN 浓度在各组之间没有差异。多元线性回归表明，在影响相关系数的15个因素中，排在前50%的是ADL评分、MNA-SF评分、血清白蛋白浓度、排尿功能、听力功能、瘦素浓度、GDS-15评分和MSTN浓度：结论：促炎肌激蛋白，尤其是瘦素、肌促蛋白和 AMPK 会对老年人的肌肉质量和力量产生负面影响。ADL和营养状况在体弱的发展过程中起着重要作用。我们的研究结果证实，虚弱的识别依赖于临床变量、肌动素浓度和功能参数，这可能有助于识别和监测虚弱。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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来源期刊

Journal of Frailty & Aging GERIATRICS & GERONTOLOGY-

CiteScore

5.90

自引率

7.70%

发文量

期刊介绍： The Journal of Frailty & Aging is a peer-reviewed international journal aimed at presenting articles that are related to research in the area of aging and age-related (sub)clinical conditions. In particular, the journal publishes high-quality papers describing and discussing social, biological, and clinical features underlying the onset and development of frailty in older persons. The Journal of Frailty & Aging is composed by five different sections: - Biology of frailty and aging In this section, the journal presents reports from preclinical studies and experiences focused at identifying, describing, and understanding the subclinical pathophysiological mechanisms at the basis of frailty and aging. - Physical frailty and age-related body composition modifications Studies exploring the physical and functional components of frailty are contained in this section. Moreover, since body composition plays a major role in determining physical frailty and, at the same time, represents the most evident feature of the aging process, special attention is given to studies focused on sarcopenia and obesity at older age. - Neurosciences of frailty and aging The section presents results from studies exploring the cognitive and neurological aspects of frailty and age-related conditions. In particular, papers on neurodegenerative conditions of advanced age are welcomed. - Frailty and aging in clinical practice and public health This journal’s section is devoted at presenting studies on clinical issues of frailty and age-related conditions. This multidisciplinary section particularly welcomes reports from clinicians coming from different backgrounds and specialties dealing with the heterogeneous clinical manifestations of advanced age. Moreover, this part of the journal also contains reports on frailty- and age-related social and public health issues. - Clinical trials and therapeutics This final section contains all the manuscripts presenting data on (pharmacological and non-pharmacological) interventions aimed at preventing, delaying, or treating frailty and age-related conditions.The Journal of Frailty & Aging is a quarterly publication of original papers, review articles, case reports, controversies, letters to the Editor, and book reviews. Manuscripts will be evaluated by the editorial staff and, if suitable, by expert reviewers assigned by the editors. The journal particularly welcomes papers by researchers from different backgrounds and specialities who may want to share their views and experiences on the common themes of frailty and aging.The abstracting and indexing of the Journal of Frailty & Aging is covered by MEDLINE (approval by the National Library of Medicine in February 2016).

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