全身性免疫炎症指数与肌少症的全因和死因特异性死亡率:来自 1999-2018 年全国健康和营养调查的研究。
Systemic immune-inflammation index and all-cause and cause-specific mortality in sarcopenia: a study from National Health and Nutrition Examination Survey 1999-2018.
机构信息
General Practice Ward/International Medical Center Ward, General Practice Medical Center, National Clinical Research Center for Geriatrics, West China Hospital, Sichuan University, Chengdu, Sichuan, China.
Department of Critical Care Medicine, West China Hospital, Sichuan University/West China School of Nursing, Sichuan University, Chengdu, China.
出版信息
Front Immunol. 2024 Apr 4;15:1376544. doi: 10.3389/fimmu.2024.1376544. eCollection 2024.
BACKGROUND
Sarcopenia, common in the elderly, often linked to chronic diseases, correlates with inflammation.The association between SII and mortality in sarcopenia patients is underexplored, this study investigates this relationship in a U.S. adult cohort.
METHODS
We analyzed 1999-2018 NHANES data, focusing on 2,974 adults with sarcopenia. Mortality outcomes were determined by linking to National Death Index (NDI) records up to December 31, 2019. Using a weighted sampling design, participants were grouped into three groups by the Systemic Immune-Inflammation Index (SII). We used Cox regression models, adjusting for demographic and clinical variables, to explore SII's association with all-cause and cause-specific mortality in sarcopenia, performing sensitivity analyses for robustness.
RESULTS
Over a median follow-up of 9.2 years, 829 deaths occurred. Kaplan-Meier analysis showed significant survival differences across SII groups. The highest SII group showed higher hazard ratios (HRs) for all-cause and cause-specific mortality in both crude and adjusted models. The highest SII group had a higher HR for all-cause(1.57, 1.25-1.98), cardiovascular(1.61, 1.00-2.58), cancer(2.13, 1.32-3.44), and respiratory disease mortality(3.21, 1.66-6.19) in fully adjusted models. Subgroup analyses revealed SII's association with all-cause mortality across various demographics, including age, gender, and presence of diabetes or cardiovascular disease. Sensitivity analyses, excluding participants with cardiovascular diseases, those who died within two years of follow-up, or those under 45 years of age, largely reflected these results, with the highest SII group consistently demonstrating higher HRs for all types of mortality in both unadjusted and adjusted models.
CONCLUSION
Our study is the first to demonstrate a significant relationship between SII and increased mortality risks in a sarcopenia population.
背景
肌少症常见于老年人,常与慢性病相关,与炎症相关。SII 与肌少症患者死亡率之间的关系尚未得到充分研究,本研究在美国成年队列中对此进行了调查。
方法
我们分析了 1999-2018 年 NHANES 数据,重点关注了 2974 名肌少症患者。通过与截至 2019 年 12 月 31 日的国家死亡指数(NDI)记录相链接,确定了死亡率结局。使用加权抽样设计,根据系统性免疫炎症指数(SII)将参与者分为三组。我们使用 Cox 回归模型,调整人口统计学和临床变量,探讨 SII 与肌少症患者全因和特定原因死亡率之间的关系,并进行稳健性敏感性分析。
结果
在中位数为 9.2 年的随访期间,发生了 829 例死亡。Kaplan-Meier 分析显示,SII 组之间的生存差异具有统计学意义。在粗模型和调整模型中,SII 最高组的全因和特定原因死亡率的风险比(HR)更高。SII 最高组的全因死亡率(1.57,1.25-1.98)、心血管疾病(1.61,1.00-2.58)、癌症(2.13,1.32-3.44)和呼吸疾病死亡率(3.21,1.66-6.19)的 HR 更高。亚组分析显示,SII 与各种人口统计学特征(包括年龄、性别以及是否患有糖尿病或心血管疾病)的全因死亡率相关。敏感性分析排除了患有心血管疾病的参与者、随访两年内死亡的参与者以及年龄小于 45 岁的参与者,这些分析结果与上述结果基本一致,在未调整和调整模型中,SII 最高组的全因死亡率的 HR 均更高。
结论
本研究首次证明 SII 与肌少症人群的死亡率升高之间存在显著关系。
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