Yang Yuqi, Da Jingjing, Yuan Jing, Zha Yan
Department of Nephrology, Guizhou Provincial People's Hospital, Guiyang, China.
J Cachexia Sarcopenia Muscle. 2023 Oct;14(5):2264-2274. doi: 10.1002/jcsm.13311. Epub 2023 Aug 9.
Our study aimed to evaluate change in sarcopenia, its defining components over 1 year follow-up and investigate associations with subsequent cognitive decline, incident mild cognitive impairment (MCI) and dementia among patients undergoing haemodialysis (HD).
In the multicentre, longitudinal study, 1117 HD patients aged 56.8 ± 14.3 years (654 men; and 463 women) from 17 dialysis centres in Guizhou Province, China, were recruited in 2019 and followed up for 1 year in 2020. Sarcopenia was diagnosed with Asian Working Group for Sarcopenia criteria using appendicular skeletal muscle mass index (ASMI) and handgrip strength (HGS). Body composition was measured using body composition monitor; body water, weight, and height were corrected to calculate ASMI. HGS was measured by mechanical handgrip dynamometer. Cognitive function was measured with Mini Mental State Examination. Multivariate linear, logistic regression models and subgroup analyses were employed to examine the associations of changes in sarcopenia, ASMI, and HGS with Mini Mental State Examination score change, and incident MCI, dementia.
Four hundred fourteen (37.1%) patients had sarcopenia at baseline; during 1 year follow-up, 257 (23.0%) developed MCI and 143 (12.8%) developed dementia. According to changes in sarcopenia, patients were stratified into four groups: non-sarcopenia; non-sarcopenia to sarcopenia; sarcopenia; and sarcopenia to non-sarcopenia. HD patients in sarcopenia and non-sarcopenia to sarcopenia groups had higher risk of MCI (34.8%, 32.0%, vs. 17.4%) and dementia (20.6%, 19.8%, vs. 8.7%), compared non-sarcopenia group (P < 0.001). Multivariate linear regression analyses showed that sarcopenia [regression coefficients (β) -1.098, 95% confidence interval (CI) -1.872, -0.324, P = 0.005] and non-sarcopenia to sarcopenia (β -1.826, -2.441, -1.212, P < 0.001) were associated with faster cognitive decline compared to non-sarcopenia. HGS decline (β 0.046, 0.027-0.064, P < 0.001) and ASMI decline (β 0.236, 0.109-0.362, P < 0.001) were both positively associated with cognitive decline. Multivariate logistic regression analyses demonstrated that patients with sarcopenia and non-sarcopenia to sarcopenia were both at increased risk of developing MCI [odds ratio (OR) 1.788, 95% CI 1.115-2.870, P = 0.016 and OR 1.589, 95% CI 1.087-2.324, P = 0.017, respectively], but only non-sarcopenia to sarcopenia was at increased risk of dementia (OR 1.792, 95% CI 1.108-2.879, P = 0.017). Both greater change of ASMI and HGS had lower risk of MCI with adjusted ORs of 0.857 (0.778-0.945, P = 0.002) and 0.976 (0.963-0.989, P < 0.001). Robust associations were found among female individuals, aged >60 years, and with low educational level.
Longitudinal associations were observed between new-onset, persistent sarcopenia, and cognitive impairment. Early detection and intervention should be implemented to delay the onset of sarcopenia and improve cognitive health among HD patients.
我们的研究旨在评估血液透析(HD)患者在1年随访期间肌肉减少症及其定义成分的变化,并调查其与随后认知功能下降、轻度认知障碍(MCI)和痴呆症的关联。
在这项多中心纵向研究中,2019年招募了来自中国贵州省17个透析中心的1117例HD患者,年龄为56.8±14.3岁(男性654例;女性463例),并于2020年进行了1年的随访。采用亚洲肌肉减少症工作组标准,通过四肢骨骼肌质量指数(ASMI)和握力(HGS)诊断肌肉减少症。使用身体成分监测仪测量身体成分;校正身体水分、体重和身高以计算ASMI。用机械握力计测量HGS。用简易精神状态检查表测量认知功能。采用多变量线性、逻辑回归模型和亚组分析来检验肌肉减少症、ASMI和HGS的变化与简易精神状态检查表评分变化以及新发MCI、痴呆症之间的关联。
414例(37.1%)患者在基线时患有肌肉减少症;在1年随访期间,257例(23.0%)发生MCI,143例(12.8%)发生痴呆症。根据肌肉减少症的变化,将患者分为四组:非肌肉减少症组;非肌肉减少症转变为肌肉减少症组;肌肉减少症组;肌肉减少症转变为非肌肉减少症组。与非肌肉减少症组相比,肌肉减少症组和非肌肉减少症转变为肌肉减少症组的HD患者发生MCI(34.8%、32.0%对17.4%)和痴呆症(20.6%、19.8%对8.7%)的风险更高(P<0.001)。多变量线性回归分析显示,与非肌肉减少症相比,肌肉减少症[回归系数(β)-1.098,95%置信区间(CI)-1.872,-0.324,P=0.005]和非肌肉减少症转变为肌肉减少症(β-1.826,-2.441,-1.212,P<0.001)与认知功能下降更快相关。HGS下降(β0.046,0.027 - 0.064,P<0.001)和ASMI下降(β0.236,0.109 - 0.362,P<0.001)均与认知功能下降呈正相关。多变量逻辑回归分析表明,肌肉减少症患者和非肌肉减少症转变为肌肉减少症患者发生MCI的风险均增加[比值比(OR)分别为1.788,95%CI 1.115 - 2.870,P=0.016和OR 1.589,95%CI 1.087 - 2.324,P=0.017],但只有非肌肉减少症转变为肌肉减少症患者发生痴呆症的风险增加(OR 1.792,95%CI 1.108 - 2.879,P=0.017)。ASMI和HGS变化越大,发生MCI的风险越低,校正后的OR分别为0.857(0.778 - 0.945,P=0.002)和0.976(0.963 - 0.989,P<0.001)。在女性、年龄>60岁和低教育水平人群中发现了显著关联。
观察到新发、持续性肌肉减少症与认知障碍之间存在纵向关联。应尽早进行检测和干预,以延缓肌肉减少症的发生并改善HD患者的认知健康。
