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Anaesthesiology Intensive Therapy
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5/2023
vol. 55
 
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Original article

Reporting SOFA in research: we should always present each of the SOFA subscores

Zbigniew Putowski
1
,
Marcelina Czok
1
,
Kamil Polok
2
,
Bertrand Guidet
3
,
Christian Jung
4
,
Raphael Romano Bruno
4
,
Dylan de Lange
5
,
Susannah Leaver
6
,
Rui Moreno
7, 8
,
Bernhard Wernly
9, 10
,
Hans Flaatten
11
,
Wojciech Szczeklik
1

1.
Centre for Intensive Care and Perioperative Medicine, Jagiellonian University Medical College, Kraków, Poland
2.
Department of Pulmonology, Jagiellonian University Medical College, Kraków, Poland
3.
Sorbonne Universités, UPMC Univ Paris 06, INSERM, UMR_S 1136, Institut Pierre Louis d’Epidémiologie et de Santé Publique, Equipe: Epidémiologie Hospitalière Qualité et Organisation des Soins, F-75012, Paris, France
4.
Department of Cardiology, Pulmonology and Vascular Medicine, Medical Faculty, Heinrich-Heine-University Duesseldorf, Duesseldorf, Germany
5.
Department of Intensive Care Medicine, University Medical Centre, University Utrecht, Utrecht, The Netherlands
6.
Department of Critical Care, St George’s Hospital, London, United Kingdom
7.
Hospital de São José, Centro Hospitalar Universitário de Lisboa Central, Faculdade de Ciências Médicas de Lisboa (Nova Médical School), Lisbon, Portugal
8.
Faculdade de Ciências da Saúde, Universidade da Beira Interior. Covilhã, Portugal
9.
Department of Internal Medicine, General Hospital Oberndorf, Teaching Hospital of the Paracelsus Medical University, Salzburg, Austria
10.
Institute of General Practice, Family Medicine and Preventive Medicine, Paracelsus Medical University of Salzburg, Salzburg, Austria
11.
Department of Anaesthesia and Intensive Care, Haukeland University Hospital, Bergen, Norway
Anaesthesiol Intensive Ther 2023; 55, 4: 326–329
Online publish date: 2024/12/30
Article file
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The Sequential Organ Failure Assessment (SOFA) score has been utilised as a primary tool to describe organ dysfunction in critically ill patients for over 25 years. The SOFA score is a sum of 6 components, each representing one organ system whose dysfunction is classified on a 4-point scale. Since its inception, the score has been validated across diffe-rent critically ill populations and has often served as a prognosticator of mortality. Both total SOFA score as well as changes in total SOFA score have been widely used as an endpoint in clinical trials [13]. However, each case of multiorgan failure differs in terms of the degree of each organ’s involvement; therefore, 2 seemingly similar total SOFA scores may reflect completely different clinical scenarios and prognoses. Hence, to promote comprehensive reporting of SOFA in clinical trials, we compared 2 critically ill, elderly cohorts in terms of differences in the distribution of each SOFA subscore.

METHODS

We conducted a retrospective analysis by comparing 2 different, multicentre, prospectively enrolled cohorts: 1) VIP-2 (ID: NCT03370692), which was a cohort focused on the critically ill elderly (≥ 80 years old) and 2) COVIP (ID: NCT04321265), which was a population of critically ill, older COVID-19 patients [4, 5]. National coordinators were responsible for the recruitment of intensive care units (ICUs), coordinated the national and local ethical permission, and supervised patient recruitment at the national level. Ethical approval was mandatory for study participation in each country. Due to the diversity of ethical consent procedures, some countries could recruit patients without informed consent while the rest had to obtain it.

Because both cohorts were designed to analyse frailty in the context of critical illness, the cohorts were analogous in design and in data handling. To maximise the similarity between the groups, only respiratory admissions (n = 910) from the VIP-2 study (non-COVID-19 cohort) and only patients ≥ 80 years old (n = 551) from the COVIP study (COVID-19 cohort) were taken into account. Hence, both cohorts included only elderly patients (≥ 80 years old) with a primary respiratory cause of admission.

The baseline characteristics encompassed key details such as the patients’ age, gender, frailty (by using the Clinical Frailty Scale), and the treatment details in the ICU. Within the initial 24 hours of ICU admission, we employed the SOFA score to evaluate the extent of organ dysfunction. The SOFA score encompasses 6 organ systems, namely cardiovascular, respiratory, renal, neurological, hepatic, and coagulation systems. Each system was assigned a score ranging from 0 to 4 points, with higher scores indicating more severe organ failure. The maximum score recorded within the first 24 hours was documented.

Rank-sum tests were used to analyse the diffe-rences in SOFA subscore distributions. Continuous variables are presented as median (IQR) and compared using rank-sum tests. Categorical variables were compared using the χ2 test. The SOFA score was approached from 2 perspectives: first as a categorical variable with assigned points (1, 2, 3, or 4) in each organ system, and secondly as a dichotomous indicator of organ failure (specifically, a SOFA score of 3 points or higher in each domain).

RESULTS

There were 910 patients in the non-COVID-19 cohort and 551 patients in the COVID-19 cohort. Patient characteristics are shown in Table 1. Changes in the distribution of SOFA subscores are presented in Figure 1. Both groups had a similar median total SOFA score (5 vs. 5 points; P = 0.5); however, they differed significantly in respiratory, neurological, cardiovascular, and coagulation SOFA subscores (Table 1, Figure 1). As for the differences in organ failures (SOFA subscore ≥ 3 points), the non-COVID-19 cohort had significantly more patients with neurological failure, while the COVID-19 cohort had a higher fraction of respiratory and cardiovascular failures (Table 2).

TABLE 1

Characteristics of COVID-19 and non-COVID-19 cohorts

VariableNon-COVID-19 cohort (VIP-2 study)COVID-19 cohort (COVIP study)P-value
Number of patients (n)910551
Age (years)84 (81–86)83 (81–85)< 0.0001
Male sex (yes/no)458 (50.3)367 (66.6)< 0.0001
SOFA: total (points)5 (3–8)5 (3–8)0.5
Clinical Frailty Scale (points)4 (3–6)3 (3–5)< 0.0001
Vasopressors (yes/no)394 (43.3)336 (60.9)< 0.0001
Invasive mechanical ventilation (yes/no)401 (44.1)315 (57.2)< 0.0001
Renal replacement therapy (yes/no)73 (8.3)67 (12.2)0.019

[i] SOFA – Sequential Organ Failure Assessment

[ii] Continuous variables are presented as median (IQR); categorical variables are presented as n (%).

FIGURE 1

Distribution of SOFA subscores across the non-COVID-19 and COVID-19 cohorts

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TABLE 2

Differences in organ failures (SOFA subscore ≥ 3 points) between the non-COVID-19 and COVID-19 cohorts

VariableNon-COVID-19 cohort (VIP-2 study)COVID-19 cohort (COVIP study)P-value
SOFA: respiratory failure ≥ 3 points (yes/no)400 (44.1)275 (49.9)0.0339
SOFA: neurological failure ≥ 3 points (yes/no)157 (17.3)46 (8.3)< 0.0001
SOFA: cardiovascular failure ≥ 3 points (yes/no)227 (25.0)175 (31.8)0.0061
SOFA: liver failure ≥ 3 points (yes/no)4 (0.4)2 (0.4)1
SOFA: coagulation failure ≥ 3 points (yes/no)10 (1.1)3 (0.5)0.4
SOFA: kidney failure ≥ 3 points (yes/no)72 (7.9)32 (5.8)0.16

[i] SOFA – Sequential Organ Failure Assessment

[ii] Variables are presented as n (%).

DISCUSSION

In this study, we compared 2 cohorts of critically ill elderly patients with respiratory cause of admission to investigate differences in SOFA subscores. Considering the variability in multi-organ failure, we aimed to emphasise the importance of reporting individual SOFA subscores in addition to the total score. Despite the seemingly similar total SOFA score (5 vs. 5 points, P = 0.5), both cohorts exhibited different degrees of organ failure.

The total SOFA score and its derivatives (such as delta SOFA, mean SOFA, maximum SOFA, etc.) are frequently employed as endpoints in clinical trials. De Grooth et al. [6] concluded that while fixed-day SOFA was the most frequently reported SOFA-based outcome, only delta SOFA showed any consistent association with mortality. Meanwhile, Pölkki et al. [7] showed that each point of each of the SOFA subscores carries different, not necessarily proportional, information regarding the severity of organ failure and its relationship to mortality. Consequently, solely reporting the total SOFA values poses a risk of reduced statistical sensitivity and fails to provide readers with a comprehensive understanding of the patients’ condition. Our analysis confirmed that if one were to adjust 2 different critically ill populations for organ failure, doing so by using total SOFA score would not suffice because these population differ in details.

CONCLUSIONS

Our findings underscore the need to report individual SOFA subscores in clinical trials to provide a comprehensive understanding of organ dysfunction.

ACKNOWLEDGEMENTS

Assistance with the article

none.

Financial support and sponsorship

none.

Conflicts of interest

none.

Presentation

none.

References

1 

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2 

Brunkhorst FM, Oppert M, Marx G, et al. Effect of empirical treatment with moxifloxacin and meropenem vs meropenem on sepsis-related organ dysfunction in patients with severe sepsis: a randomized trial. JAMA 2012; 307: 2390-2399. doi: 10.1001/jama.2012.5833.

3 

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4 

Guidet B, de Lange DW, Boumendil A, et al. The contribution of frailty, cognition, activity of daily life and comorbidities on outcome in acutely admitted patients over 80 years in European ICUs: the VIP2 study. Intensive Care Med 2020; 46: 57-69. doi: 10.1007/s00134-019-05853-1.

5 

Jung C, Flaatten H, Fjølner J, et al. The impact of frailty on survival in elderly intensive care patients with COVID-19: the COVIP study. Crit Care 2021; 25. doi: 10.1186/s13054-021-03551-3.

6 

de Grooth HJ, Geenen IL, Girbes AR, Vincent JL, Parienti JJ, Oudemans-van Straaten HM. SOFA and mortality endpoints in randomized controlled trials: A systematic review and meta-regression analysis. Crit Care 2017; 21. doi: 10.1186/s13054-017-1609-1.

7 

Pölkki A, Pekkarinen PT, Takala J, Selander T, Reinikainen M. Association of Sequential Organ Failure Assessment (SOFA) components with mortality. Acta Anaesthesiol Scand 2022; 66: 731-741. doi: 10.1111/aas.14067.

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