重症监护病房COVID-19患者气胸和皮下肺气肿的评价

Mehtap Pehlivanlar Küçük, Burcu Öksüz Güngör, A. Küçük, O. Ayçiçek, Atila Türkyılmaz, Funda Öztuna, Y. Bülbül, T. Özlü
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摘要

电子邮件:mehtap_phlvnlr@hotmail.com电话:+90 505 242 44 90 ORCID ID: orcid.org/0000-0003-2247-4074摘要目的:气胸(PNX)和皮下肺气肿(SCE)作为一种常见的并发症,其重要性日益增加。本研究旨在揭示在我院三级重症监护病房(ICU)随访PNX和SCE患者的冠状病毒病-2019 (COVID-19)诊断的频率、时间和可能的危险因素。材料与方法:纳入2020年8月8日至2021年2月20日期间在我科16张床位三级ICU随访治疗的所有确诊COVID-19患者,并在住院期间发生PNX和SCE。结果:我院ICU随访的165例新冠肺炎患者中有16例(9.6%)发生PNX和SCE。16例患者中,3例(18.8%)存活。患者的中位年龄为66.5岁(四分位数范围:58.5-75.5)。糖尿病是PNX和SCE患者最常见的合并症。此外,12例(75%)患者有吸烟史。在15例(93.8%)发生PNX的患者中,4例(25%)为双侧,9例(56.3%)为SCE。PNX和SCE患者有创机械通气12例(75%),自主呼吸3例(18.8%),无创机械通气1例(6.2%)。到PNX和SCE发生时,全组氧支持天数为9(6.25 ~ 17)天,生存组中位时间为6天,非生存组中位时间为9天。结论:在新冠肺炎大流行中,PNX和SCE等并发症的发生率(9.5%)高于普通重症监护人群和重症监护入院后期(中位9天)。在这些患者中,吸烟被定义为一个危险因素;然而,PNX率的增加被认为与COVID-19肺炎和细胞因子风暴引起的实质损伤有关。
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Pneumothorax and Subcutaneous Emphysema Evaluation in Patients with COVID-19 in the Intensive Care Unit
E-mail : mehtap_phlvnlr@hotmail.com Phone : +90 505 242 44 90 ORCID ID : orcid.org/0000-0003-2247-4074 ABSTRACT Objective: Pneumothorax (PNX) and subcutaneous emphysema (SCE) have increased in importance as a frequently occurring complication. This study aimed to reveal the frequency, timing, and possible risk factors in patients with PNX and SCE who are followed up with coronavirus disease-2019 (COVID-19) diagnosis in our tertiary intensive care unit (ICU). Materials and Methods: All patients with confirmed COVID-19 who were followed up and treated in our unit between August 8, 2020, and February 20, 2021, in a 16-bed tertiary ICU and who developed PNX and SCE during their hospitalization were included. Results: PNX and SCE developed in 16 (9.6%) of 165 patients who were followed up in our ICU due to COVID-19. Of these 16 patients, 3 (18.8%) survived. The median age of patients was 66.5 years (interquartile range: 58.5-75.5). Diabetes mellitus was the most common comorbidity in patients with PNX and SCE. Additionally, 12 (75%) patients had a smoking history. Of 15 (93.8%) patients who developed PNX, 4 (25%) were bilateral, and SCE developed in 9 (56.3%) patients. Twelve (75%) patients with PNX and SCE were under invasive mechanical ventilation, 3 (18.8%) under spontaneous breathing, and 1 (6.2%) under non-invasive mechanical ventilation treatment. The number of oxygen support days until the time PNX and SCE developed was 9 (6.25-17) days in the whole group, the median time was 6 days in the survival group and 9 days in the non-survival group. Conclusion: In the COVID-19 pandemic, complications, such as PNX and SCE, are more frequently observed (9.5%) than in the general intensive care population and the later period of intensive care admission (median 9 days). Smoking is defined as a risk factor in most of these patients; however, increased PNX rates are thought to be related to both COVID-19 pneumonia and parenchymal damage due to cytokine storms.
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