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肝硬化住院患者的复合性肌少症随年龄增长会使预后恶化。

Compound Sarcopenia in Hospitalized Patients with Cirrhosis Worsens Outcomes with Increasing Age.

作者信息

Welch Nicole, Attaway Amy, Bellar Annette, Alkhafaji Hayder, Vural Adil, Dasarathy Srinivasan

机构信息

Department of Gastroenterology and Hepatology, Cleveland Clinic, Cleveland, OH 44195, USA.

Department of Inflammation and Immunity, Cleveland Clinic, Cleveland, OH 44195, USA.

出版信息

Nutrients. 2021 Feb 18;13(2):659. doi: 10.3390/nu13020659.

Abstract

BACKGROUND

There are limited data on outcomes of older patients with chronic diseases. Skeletal muscle loss of aging (primary sarcopenia) has been extensively studied but the impact of secondary sarcopenia of chronic disease is not as well evaluated. Older patients with chronic diseases have both primary and secondary sarcopenia that we term compound sarcopenia. We evaluated the clinical impact of compound sarcopenia in hospitalized patients with cirrhosis given the increasing number of patients and high prevalence of sarcopenia in these patients.

DESIGN

The Nationwide Inpatients Sample (NIS) database (years 2010-2014) was analyzed to study older patients with cirrhosis. Since there is no universal hospital diagnosis code for "muscle loss", we used a comprehensive array of codes for "muscle loss phenotype" in the international classification of diseases-9 (ICD-9). A randomly selected 2% sample of hospitalized general medical population (GMP) and inpatients with cirrhosis were stratified into 3 age groups based on age-related changes in muscle mass. In-hospital mortality, length of stay (LoS), cost of hospitalization (CoH), comorbidities and discharge disposition were analyzed.

RESULTS

Of 517,605 hospitalizations for GMP and 106,835 hospitalizations for treatment of cirrhosis or a cirrhosis-related complication, 207,266 (40.4%) GMP and 29,018 (27.7%) patients with cirrhosis were >65 years old, respectively. Muscle loss phenotype in both GMP and inpatients with cirrhosis 51-65 years old and >65 years old was significantly ( < 0.001 for all) associated with higher mortality, LoS, and CoH compared to those ≤50 years old. Patients >65 years old with cirrhosis and muscle loss phenotype had higher mortality (adjusted OR: 1.06, 95% CI [1.04, 1.08] and CoH (adjusted odds ratio (OR): 1.10, 95% confidence interval (CI) [1.04, 1.08])) when compared to >65 years old GMP with muscle loss phenotype. Muscle loss in younger patients with cirrhosis (≤50 years old) was associated with worse outcomes compared to GMP >65 years old. Non-home discharges (nursing, skilled, long-term care) were more frequent with increasing age to a greater extent in patients with cirrhosis with muscle loss phenotype for each age stratum.

CONCLUSION

Muscle loss is more frequent in older patients with cirrhosis than younger patients with cirrhosis and older GMP. Younger patients with cirrhosis had clinical outcomes similar to those of older GMP, suggesting an accelerated senescence in cirrhosis. Compound sarcopenia in older patients with cirrhosis is associated with higher inpatient mortality, increased LoS, and CoH compared to GMP with sarcopenia.

摘要

背景

关于老年慢性病患者预后的数据有限。衰老引起的骨骼肌丢失(原发性肌肉减少症)已得到广泛研究,但慢性病继发性肌肉减少症的影响尚未得到充分评估。患有慢性病的老年患者同时存在原发性和继发性肌肉减少症,我们将其称为复合性肌肉减少症。鉴于肝硬化住院患者数量不断增加且肌肉减少症患病率较高,我们评估了复合性肌肉减少症对肝硬化住院患者的临床影响。

设计

分析全国住院患者样本(NIS)数据库(2010 - 2014年)以研究老年肝硬化患者。由于没有通用的“肌肉丢失”医院诊断代码,我们在国际疾病分类 - 9(ICD - 9)中使用了一系列综合代码来表示“肌肉丢失表型”。根据肌肉质量与年龄相关的变化,将随机抽取的2%的住院普通内科患者样本(GMP)和肝硬化住院患者分为3个年龄组。分析了住院死亡率、住院时间(LoS)、住院费用(CoH)、合并症和出院处置情况。

结果

在517,605例GMP住院患者和106,835例因肝硬化或肝硬化相关并发症住院治疗的患者中,分别有分别有207,266例(40.4%)GMP患者和29,018例(27.7%)肝硬化患者年龄>65岁。与年龄≤50岁的患者相比,51 - 65岁和>65岁的GMP患者及肝硬化住院患者的肌肉丢失表型均与较高的死亡率、LoS和CoH显著相关(所有P<0.001)。与年龄>65岁且有肌肉丢失表型的GMP患者相比,年龄>65岁且有肝硬化和肌肉丢失表型的患者死亡率更高(调整后的OR:1.06,95%CI[1.04, 1.08]),CoH更高(调整后的优势比(OR):1.10,95%置信区间(CI)[1.04, 1.08])。与年龄>65岁的GMP患者相比,年龄较小的肝硬化患者(≤50岁)的肌肉丢失与更差的预后相关。在每个年龄层中,有肌肉丢失表型的肝硬化患者非家庭出院(护理、专业护理、长期护理)随年龄增长更为频繁。

结论

老年肝硬化患者的肌肉丢失比年轻肝硬化患者和老年GMP患者更常见。年轻肝硬化患者的临床预后与老年GMP患者相似,提示肝硬化患者存在加速衰老。与有肌肉减少症的GMP患者相比,老年肝硬化患者的复合性肌肉减少症与更高的住院死亡率、更长的LoS和更高的CoH相关。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/4317/7923160/cb428b896563/nutrients-13-00659-g001.jpg

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