结核与肺部疾病杂志 ›› 2025, Vol. 6 ›› Issue (3): 297-303.doi: 10.19983/j.issn.2096-8493.20250040

• 论著 • 上一篇    下一篇

Ⅲ型前胶原氨基端肽、同型半胱氨酸及超敏C反应蛋白与前白蛋白比值在慢性心力衰竭合并胸腔积液患者中的临床意义

林红(), 于金凤, 张守霞, 刘晔, 陈延闽   

  1. 黑龙江省哈尔滨市胸科医院心内科,哈尔滨 150056
  • 收稿日期:2025-03-03 出版日期:2025-06-20 发布日期:2025-06-12
  • 通信作者: 林红,Emai:linhong19982003@163.com

Clinical significance of serum PⅢNP, homocysteine, and hs-CRP/prealbumin ratio in patients with chronic heart failure complicated by pleural effusion

Lin Hong(), Yu Jinfeng, Zhang Shouxia, Liu Ye, Chen Yanmin   

  1. Department of Cardiology, Harbin Chest Hospital, Heilongjiang Province, Harbin 150056,China
  • Received:2025-03-03 Online:2025-06-20 Published:2025-06-12
  • Contact: Lin Hong,Emai:linhong19982003@163.com

摘要:

目的:探究慢性心力衰竭(CHF)合并胸腔积液患者中Ⅲ型前胶原氨基端肽(PⅢNP)、同型半胱氨酸(Hcy)、超敏C反应蛋白/前白蛋白(hs-CRP/PAB)比值的临床意义。方法:采用前瞻性研究方法,选取2024年1—12月于哈尔滨市胸科医院心内科住院的CHF患者140例,根据是否合并胸腔积液分为无胸腔积液组(80例)和胸腔积液组(60例)。比较胸腔积液组和无胸腔积液组血PⅢNP、Hcy水平及hs-CRP/PAB比值。根据胸腔积液量将患者分为少量组、中量组、大量组,比较3组血PⅢNP、Hcy水平及hs-CRP/PAB比值。经受试者工作特征曲线(ROC)分析血PⅢNP、Hcy、hs-CRP/PAB比值单独及联合诊断CHF合并胸腔积液的效能。根据预后情况将患者分为不良组(25例)、良好组(35例),比较两组一般资料及血PⅢNP、Hcy水平及hs-CRP/PAB比值。结果:胸腔积液组PⅢNP、Hcy水平及hs-CRP/PAB比值分别为(133.19±33.56)ng/ml、(24.07±6.19)μmol/L和0.06±0.02,高于无胸腔积液组[分别为(94.16±12.37)ng/ml、(16.54±4.32)μmol/L和0.02±0.01],差异均有统计学意义(t值分别为9.580、8.475和13.874,P值均<0.05)。中量组血PⅢNP、Hcy水平及hs-CRP/PAB比值[分别为(129.97±30.05)ng/ml、(23.31±4.45)μmol/L和0.05±0.01]和大量组血PⅢNP、Hcy水平及hs-CRP/PAB比值[分别为(156.32±35.48)ng/ml、(29.19±6.68)μmol/L和0.07±0.02]均明显高于少量组血PⅢNP、Hcy水平及hs-CRP/PAB比值[分别为(106.79±15.37)ng/ml、(18.41±3.97)μmol/L和0.03±0.01],差异均有统计学意义(F值分别为9.650、15.670和33.930,P值均<0.001)。ROC曲线显示,血PⅢNP、Hcy、hs-CRP/PAB联合诊断CHF合并胸腔积液的AUC为0.848,明显高于 PⅢNP、Hcy、hs-CRP/PAB比值单独诊断(AUC分别为0.763、0.773和0.746)。不良组血PⅢNP、Hcy水平及hs-CRP/PAB比值[分别为(152.15±36.19)ng/ml、(28.28±5.16)μmol/L和0.07±0.01]高于良好组PⅢNP、Hcy水平及hs-CRP/PAB比值[分别为(119.65±29.46)ng/ml、(21.06±3.45)μmol/L和0.04±0.01],差异均有统计学意义(t值分别为3.829、6.500和10.220,P值均<0.001)。结论:CHF合并胸腔积液患者PⅢNP、Hcy水平及hs-CRP/PAB比值与胸腔积液的发生及积液量密切相关,且随着胸腔积液量增加,血PⅢNP、Hcy水平及hs-CRP/PAB比值逐渐升高。血PⅢNP、Hcy水平及hs-CRP/PAB比值联合检测,对CHF合并胸腔积液患者的诊断具有较好的诊断价值,且联合检测的敏感度优于单独检测。同时,CHF合并胸腔积液患者血PⅢNP、Hcy及hs-CRP/PAB比值水平越高,预后越差。

关键词: 心力衰竭, 胸腔积液, 半胱氨酸, C反应蛋白质, 前白蛋白, 预后

Abstract:

Objective: This study aimed to investigate the clinical significance of the N-terminal propeptide of type Ⅲ procollagen (PⅢNP), homocysteine (Hcy), and the high-sensitivity C-reactive protein to prealbumin ratio (hs-CRP/PAB) among patients diagnosed with CHF complicated by pleural effusion. Methods: This prospective study enrolled 140 patients with chronic heart failure (CHF) who were hospitalized in the Department of Cardiology at Harbin Chest Hospital between January and December 2024. Based on the presence or absence of pleural effusion, patients were categorized into a pleural effusion group (n=60) and a non-effusion group (n=80). Serum levels of PⅢNP, Hcy, and hs-CRP/PAB were statistically compared between the two groups. Patients with pleural effusion were further stratified into small-, moderate-, and large-volume subgroups according to effusion volume, and biomarker levels were compared among these three subgroups. The diagnostic performance of PⅢNP, Hcy, and hs-CRP/PAB—alone and in combination—for identifying CHF complicated by pleural effusion was evaluated using receiver operating characteristic (ROC) curve analysis.Patients were also divided into a favorable prognosis group (n=35) and a poor prognosis group (n=25) based on clinical outcomes. Clinical characteristics and biomarker levels were compared between the two prognosis groups. Results: Serum levels of PⅢNP, Hcy, and the hs-CRP/PAB ratio were significantly elevated in patients with pleural effusion compared to those without ((133.19±33.56) ng/ml vs. (94.16±12.37) ng/ml; (24.07±6.19) μmol/L vs. (16.54±4.32) μmol/L; 0.06±0.02 vs. 0.02±0.01; t=9.580, 8.475 and 13.874, respectively, all P<0.001). Stratification by pleural effusion volume revealed progressive increases in all three biomarkers. Patients with moderate effusion (129.97±30.05 ng/ml PⅢNP, 23.31±4.45 μmol/L Hcy, 0.05±0.01 hs-CRP/PAB) and large effusion (156.32±35.48 ng/ml, 29.19±6.68 μmol/L, and 0.07±0.02, respectively) had significantly higher levels than those with small effusion ((106.79±15.37) ng/ml, (18.41±3.97) μmol/L and 0.03±0.01; all P<0.001; F=9.650, 15.670 and 33.930, respectively). Receiver operating characteristic (ROC) analysis demonstrated that the combination of PⅢNP, Hcy, and hs-CRP/PAB yielded an area under the curve (AUC) of 0.848, outperforming any single biomarker (AUCs of 0.763, 0.773 and 0.746 for PⅢNP, Hcy, and hs-CRP/PAB, respectively). Additionally, patients in the poor prognosis group showed markedly elevated levels of PⅢNP ((152.15±36.19) ng/ml vs. (119.65±29.46) ng/ml, Hcy (28.28±5.16) μmol/L vs. (21.06±3.45) μmol/L), and hs-CRP/PAB (0.07±0.01 vs. 0.04±0.01), compared with those in the favorable prognosis group (all P<0.001; t=3.829, 6.500 and 10.220, respectively). Conclusion: Serum levels of PⅢNP, Hcy, and the hs-CRP/PAB ratio were significantly associated with both the presence and volume of pleural effusion in patients with CHF. These biomarkers exhibited a stepwise increase corresponding to effusion severity. Combined detection of PⅢNP, Hcy, and hs-CRP/PAB ratio demonstrated superior diagnostic performance compared to individual markers, particularly in identifying CHF complicated by pleural effusion. Moreover, elevated levels of these biomarkers were significantly correlated with poor clinical prognosis, suggesting their potential utility in both diagnostic evaluation and prognostic risk stratification.

Key words: Heart failure, Pleural effusion, Cysteine, C-reactive protein, Prealbumin, Prognosis

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