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首页> 外文期刊>BMC Pulmonary Medicine >Etiology-associated heterogeneity in acute respiratory distress syndrome: a retrospective cohort study
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Etiology-associated heterogeneity in acute respiratory distress syndrome: a retrospective cohort study

机译:急性呼吸窘迫综合征中的病因相关的异质性:回顾性队列研究

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Heterogeneity in acute respiratory distress syndrome (ARDS) has led to many statistically negative clinical trials. Etiology is considered an important source of pathogenesis heterogeneity in ARDS but previous studies have usually adopted a dichotomous classification, such as pulmonary versus extrapulmonary ARDS, to evaluate it. Etiology-associated heterogeneity in ARDS remains poorly described. In this retrospective cohort study, we described etiology-associated heterogeneity in gas exchange abnormality (PaO2/FiO2 [P/F] and ventilatory ratios), hemodynamic instability, non-pulmonary organ dysfunction as measured by the Sequential Organ Failure Assessment (SOFA) score, biomarkers of inflammation and coagulation, and 30-day mortality. Linear regression was used to model the trajectory of P/F ratios over time. Wilcoxon rank-sum tests, Kruskal–Wallis rank tests and Chi-squared tests were used to compare between-etiology differences. From 1725 mechanically ventilated patients in the ICU, we identified 258 (15%) with ARDS. Pneumonia (48.4%) and non-pulmonary sepsis (11.6%) were the two leading causes of ARDS. Compared with pneumonia associated ARDS, extra-pulmonary sepsis associated ARDS had a greater P/F ratio recovery rate (difference?=?13?mmHg/day, p?=?0.01), more shock (48% versus 73%, p?=?0.01), higher non-pulmonary SOFA scores (6 versus 9 points, p??0.001), higher d-dimer levels (4.2 versus 9.7?mg/L, p?=?0.02) and higher mortality (43% versus 67%, p?=?0.02). In pneumonia associated ARDS, there was significant difference in proportion of shock (p?=?0.005) between bacterial and non-bacterial pneumonia. This study showed that there was remarkable etiology-associated heterogeneity in ARDS. Heterogeneity was also observed within pneumonia associated ARDS when bacterial pneumonia was compared with other non-bacterial pneumonia. Future studies on ARDS should consider reporting etiology-specific data and exploring possible effect modification associated with etiology.
机译:急性呼吸窘迫综合征(ARDS)中的异质性导致了许多统计阴性临床试验。病因被认为是ARDS中发病机制异质性的重要来源,但之前的研究通常采用二均相分类,例如肺与胶原体ARDS,以评估它。 ARDS中的病因相关的异质性仍然仍然清楚。在该回顾性队列研究中,我们描述了气体交换异常的病因相关的异质性(Pao2 / FiO2 [p / f]和呼道比),血液动力学不稳定性,通过顺序器官衰竭评估(沙发)评分测量的非肺器官功能障碍,炎症和凝血的生物标志物,30天死亡率。线性回归用于模拟P / F比率的轨迹随时间。 Wilcoxon Rank-Sum测试,Kruskal-Wallis等级测试和Chi方向测试用于比较 - 病因差异之间。从ICU的1725名机械通风患者从ICU,我们鉴定了258(15%)的ARDS。肺炎(48.4%)和非肺脓毒症(11.6%)是ARDS的两个主要原因。与肺炎相关的ARD相比,肺脓毒症相关的ARDS具有更大的p / f比率回收率(差异?=?13?mmhg / day,p?= 0.01),更休克(48%与73%,p? = 0.01),较高的非肺沙发分数(6与9点,p≤≤0.001),较高的D-二聚体水平(4.2与9.7×mg / L,p?= 0.02)和更高的死亡率(43 %与67%,p?= 0.02)。在肺炎相关的ARDS中,细菌和非细菌肺炎之间的休克比例(p?= 0.005)显着差异。该研究表明,ARDS中存在显着的病因相关的异质性。当与其他非细菌肺炎进行比较细菌肺炎时,还观察到肺炎相关ARDS的异质性。关于ARD的未来研究应考虑报告的病因特异性数据,并探索与病因相关的可能效果修改。

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