A nomogram for predicting the severity of COVID-19 infections among patients in Chengdu, China

Luo, Fan; Zhang, Na; Zheng, Haiyan; Shi, Nannan; Gao, Yueqin; Xie, Liqiu; Li, Chenxi

doi:10.15212/RADSCI-2023-0006

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A nomogram for predicting the severity of COVID-19 infections among patients in Chengdu, China

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Author(s): Fan Luo ^a , Na Zhang ^a , Haiyan Zheng ^a , Nannan Shi ^b , Yueqin Gao ^a , Liqiu Xie ^a , Chenxi Li ^a ^, ^* ^,

Publication date (Electronic): 09 August 2023

Journal: Radiology Science

Publisher: Compuscript

Keywords: COVID-19, CT score, nomogram, clinical characteristics

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Abstract

Introduction:

Although most COVID-19 infections are currently mild, poor prognoses and fatalities continue to occur, which remain a threat to the safety of people in China. The goal of this study was to create an efficient model that combines the clinical characteristics with computed tomography (CT) scores at the time of admission to predict the severity of COVID-19.

Methodology:

A total of 346 COVID-19 patients in the current study, of whom 46 had severe infections and 300 had non-severe infections according to the clinal outcomes. Clinical, laboratory, CT findings, and CT scores at admission were collected. To identify the independent risk factors, univariable and multivariable logistic regression analyses were performed. A nomogram model was built with the extracted risk factors. The calibration curve and decision curve (DCA) operated to validate model performance.

Results:

The receiver operating characteristic curve indicated that the severity CT score had an area under the curve of 0.933 (95% CI, 0.901-0.965) and a cut-off value of 6.5 (sensitivity, 95.70%; specificity, 78%). The CT score, age, lactic dehydrogenase and hydroxybutyrate dehydrogenase levels, and hypertension were exacted for the nomogram. The nomogram had good calibration (P = 0.539) and excellent clinical value based on the DCA.

Conclusions:

The nomogram presented herein could be a valuable model to predict severe COVID-19 among patients in Chengdu, China.

Main article text

1. INTRODUCTION

It has been 3 years since coronavirus disease 2019 (COVID-19) was first reported. The impact of the emerging disease remains to be determined. China recently implemented a new policy for managing COVID-19. Indeed, termination of the quarantine policy brought new challenges to this developing country with a huge population. Currently, most COVID-19 infections are mild, but there are still patients with a poor prognosis. According to a survey by the Chinese Center for Disease Control and Prevention, up to 15.8% of confirmed cases are severe or critical [1]. The fatality rate of critical cases is up to 49.0% [2], which is of great medical concern. According to previous studies [3–5], older age combined with clinical and laboratory characteristics, such as dyspnea, fever, and elevated creatine kinase, are correlated with severe and critical illnesses. Thus, it is necessary to develop an easy-to-use prediction tool for COVID-19 to improve the prognosis.

A nomogram is a line chart that displays scales for the variables included in a formula so that the appropriate values for each variable lie in a line that intersects all the scales. Nomograms have been used as a prediction tool for the prognosis of multiple diseases [6–8]. The nomogram is a better and easier risk-prediction tool in clinical practice compared to other prediction tools that require computer software [9].

Computed tomography (CT) is an essential technique for the diagnosis and management of COVID-19 [10]. Ground-glass opacities (GGOs) and consolidation distributed predominantly in the bilateral subpleural segments are considered the most common CT characteristics of COVID-19 infections [11]; however, the CT characteristics are not quantifiable, which limits prediction of disease progression. The chest CT score is a quantitative method to demonstrate the extent and nature of pulmonary lesions, and has been used in studies of severe acute respiratory syndrome [SARS] [12] and pulmonary fibrosis [13]. Some studies have also applied CT scores to evaluate COVID-19 severity, which showed that the CT score is correlated with clinical parameters indicating deterioration [14, 15]. Thus, the CT score could be an excellent method for the management of patients > 65 years of age with COVID-19 infections [16].

Several nomograms have been developed for predicting severe and critical COVID-19 cases, the majority have relied on clinical or laboratory characteristics [17, 18]. A few models with excellent performance based on CT radiomics have recently been built [19, 20]. Because CT radiomics is not available in the majority of hospitals in China, we developed a feasible and efficient nomogram using clinical and CT scores to predict COVID-19 severity and optimize the prognosis in a timely fashion.

2. METHODOLOGY

2.1. Patients

A total of 346 patients with confirmed COVID-19 infections were enrolled from the Public Health Clinical Center of Chengdu between August 2021 and December 2022. The patients were divided into non-severe (moderate and common) and severe groups based on clinical outcomes [21]. The severe group was required to fulfill at least 1 of the following criteria: (1) shortness of breath (respiratory rate ≥ 30 breaths/min); (2) arterial oxygen saturation at rest ≤93%; (3) the ratio of partial pressure of oxygen-to-fraction of inspired oxygen (PaO₂:FiO₂) ≤300 mmHg; (4) respiratory distress; (5) onset of shock; (6) requirement for mechanical ventilation due to respiratory failure; and/or (7) organ failure necessitating intensive care unit (ICU) admission.

2.2. Clinical data

Demographic information (age and gender) and clinical parameters (symptoms, comorbidities, and cigarette smoking history) at the time of admission were derived from medical records. Laboratory parameters included routine blood tests, arterial blood gas values, coagulation testing, cardiac enzyme levels, and hepatic and renal function tests.

2.3. CT image characteristics and CT scores

All CT images were non-contrast. Images of the first CT examination were evaluated separately by two senior radiologists. In circumstances in which there were conflicts, the final judgment was reached by consensus. The Radiology Society of North America consensus statement on reporting chest CT abnormalities related to COVID-19 was used to classify the CT signs [22]. Chest CT signs included GGOs, consolidation, nodules, the halo sign, reticular patterns, crazy-paving patterns, septal thickening, traction bronchiectasis, bronchial wall thickening, air bronchograms, lymphadenopathy, pleural thickening, and pleural effusions.

We adopted the CT scoring system designed by Salaffi et al. [23]. Bilateral lobes were assessed at 3 levels with 6 parts and divided by the carina and the inferior pulmonary vein from top-to-bottom. Each part received two scores that indicated the extent and nature of the lung lesions. The extent of involvement was graded as follows: 0 for no involvement;1 for 1%–24%; 2 for 25%–49%; 3 for 50%–74%; and 4 for ≥75%. The nature of lesions were graded as follows: 1 for normal lung without abnormal changes; 2 for at least 75% GGOs or crazy-paving pattern; 3 for the simultaneous appearance of GGOs/crazy-paving pattern and consolidation, and each contributed <75% of the total; 4 for 75% or more consolidation. The above two scores (the extent and the nature) were multiplied and totaled to achieve a final score for all six parts.

2.4. Statistical analysis

Frequencies and percentages were used to describe categorical variables. Clinical, laboratory results, CT findings, and CT scores were compared between the severe and non-severe types with a χ² test or Fisher’s exact test. A two-sided α < 0.05 was considered a statistically significant difference. The efficiency of the CT score predicting the risk of severity was assessed using receiver operator characteristic (ROC) curve analysis.

To identify the independent risk factors, univariable and multivariable logistic regression analyses were utilized. The initial selection of all data was performed using univariate logistic regression analysis. Variables with P-values < 0.05 were incorporated into the multivariable logistic regression analysis. The final features in the multivariable logistic regression analysis were selected as risk factors with a P < 0.05.

The collected risk factors were used to build a nomogram model in R (version 3.6.3) along with the rms statistical tools. The model performance was then verified using a calibration curve and decision curve (DCA).

3. RESULTS

3.1. Clinical and laboratory findings

A total of 346 patients in all were included in our study. Table 1 displays the demographic and clinical factors. The non-severe and severe cohorts consisted of 300 patients with a median age of 35 years (age range, 4-78 years) and 46 patients with a median age of 58 years (age range, 34-89 years), respectively. Patients with a severe COVID-19 infection had a higher median age. The gender and cigarette smoking histories of the two cohorts were comparable. Patients in the severe cohort were more likely to experience cough, fever, and dyspnea than patients in the non-severe cohort (78.26% vs. 16.33%, 71.74% vs. 21.67, and 13.04% vs. 3.67%, respectively). The severe cohort had a significantly higher incidence of co-morbidities (hypertension [34.78% vs. 6.0%], diabetes [17.39% vs. 3.33%], coronary heart disease [17.39% vs. 0.67%], and surgical history [19.57% vs. 1.0%]) than the non-severe cohort.

Table 1 |

Clinical characteristics of patients with COVID-19.

Characteristic	Non-severe NO. (%)	Severe NO. (%)	P
Age, Y	35 (4~78)	58 (34~89)	<0.01
Gender,			0.212
Female	78 (26.0)	16 (34.78)
Male	222 (74.0)	30 (65.22)
Smoking history			0.811
Yes	67 (22.33)	11 (13.04)
No	233 (77.67)	35 (86.96)
Fever			<0.01
Yes	49 (16.33)	36 (78.26)
No	251 (83.67)	10 (21.74)
Cough			<0.01
Yes	65 (21.67)	33 (71.74)
No	235 (78.33)	13 (28.26)
Dyspnea			0.006
Yes	11 (3.67)	6 (13.04)
No	289 (96.33)	40 (86.96)
Chest pain			0.656
Yes	4 (1.33)	1 (2.17)
No	296 (98.67)	45 (97.83)
Headache			0.947
Yes	7 (2.33)	1 (2.17)
No	293 (97.67)	45 (97.83)
Anorexia			0.165
Yes	8 (2.67)	3 (6.52)
No	292 (97.33)	43 (93.48)
Fatigue			0.395
Yes	15 (5.0)	1 (2.17)
No	285 (95.0)	45 (97.83)
Sore muscles			0.324
Yes	6 (2.0)	2 (4.35)
No	294 (98.0)	44 (95.65)
Hypertension			<0.001
Yes	18 (6.0)	16 (34.78)
No	282 (94)	30 (65.22)
Diabetes			<0.001
Yes	10 (3.33)	8 (17.39)
No	290 (96.67)	38 (82.61)
Cardiovascular disease			<0.001
Yes	2 (0.67)	8 (17.39)
No	298 (99.33)	38 (82.61)
COPD
Yes	3 (1.0)	1 (2.17)	0.488
No	297 (99.0)	45 (97.83)
History of surgery			<0.001
Yes	3 (1.0)	9 (19.57)
No	297 (99.0)	37 (80.43)

The laboratory findings are shown in Table 2 . Seventeen characteristics were evaluated with significant differences between the two cohorts.

Table 2 |

Laboratory findings of patients with COVID-19.

Characteristic	Non-severe	Severe	P
LDH U/L	167.5 (95~374)	266 (145~671)	<0.001
CK	80 (16~614)	100.5 (27~1360)	0.038
CK-MB	10 (3~43)	13 (2~33)	<0.001
HBDH	129 (80~311)	189.5 (75~502)	<0.001
ALT	26 (6~407)	27.5 (4~153)	0.56
AST	21 (10~184)	33 (13~126)	<0.001
GGT	22 (7~213)	24.5 (12~148)	0.031
ALP	66 (15~278)	67 (30~175)	0.429
TBIL	9.65 (1.4~107)	7.75 (2~28.8)	0.182
DBIL	0.47 (0~86)	0.73 (0.06~9.6)	0.024
BUN	3.88 (1.09~7.79)	4.56 (2.05~25.69)	0.006
Creatinine	67 (27~390)	67.75 (32.8~969)	0.395
Glucose	5.19 (2.61~24.79)	7.23 (4.32~1057)	<0.001
WBC 10⁹	6.31 (2.14~17.84)	5.47 (1.84~14.84)	0.125
Neutrophil count 10⁹	3.68 (0.65~323)	3.8 (0.6~12.7)	0.262
Lymphocyte count 10⁹	1.81 (0.44~6.24)	0.74 (0.2~4.21)	<0.001
Monocyte Count	0.46 (0.11~7.7)	0.41 (0.12~325)	0.150
PLT	225 (1.66~502)	148.5 (69.5~380)	<0.001
RBC	4.91 (1.52~2089)	4.6 (2.09~156)	0.003
Hb	147 (12.5~184)	129 (60~210.18)	<0.001
CRP	0.8 (0.5~129.55)	0.5 (174.17)	<0.001
PaO₂	87.85 (30.2~211.5)	83.6 (36.5~178.6)	0.157
PCO₂	44.5 (31.1~71.2)	40.1 (1.1~54.7)	<0.001
D-dimer ug/ml	0.64 (0.28~6.43)	1.07 (0.32~21.11)	<0.001
APTT	28.7 (19.8~50.2)	28.95 (20.6~74.4)	0.231
FDP	1.9 (0~19.5)	3.25 (1.6~42.8)	<0.001
PT	1.3 (13~18.7)	13 (11.6~99.3)	0.134

Abbreviations: LDH: lactate dehydrogenase; CK: creatine kinase; CK-MB: creatine kinase-MB; HBDH: hydroxybutyrate dehydrogenase; ALT: alanine aminotransferase; AST: aspartate aminotransferase; GGT: gamma-glutamyl transpeptidase; ALP: alkaline phosphatase; TBIL: total bilirubin; DBIL: direct bilirubin; BUN: blood urea nitrogen; PLT: platelets; Hb: hemoglobin; CRP: C-reactive protein; APTT: activated partial thromboplastin time; FDP: fibrinogen degradation products; PT: prothrombin time.

3.2. CT findings and CT scores

Table 3 lists the CT findings and CT scores. Patients with a severe COVID-19 infection had a higher incidence of GGOs (P<0.001), consolidation (P<0.001), reticular opacities (P<0.001), a crazy-paving pattern (P=0.012), interlobular septal thickening (P<0.001), bronchial wall thickening (P=0.006), and air bronchograms (P<0.001). Furthermore, patients in the severe cohort had a higher incidence of lymphadenopathy and pleural effusions (P<0.001 for both) than patients in the non-severe cohort.

Table 3 |

CT findings and CT scores of patients with COVID-19.

Characteristic	Non-severe NO. (%)	Severe NO. (%)	P
Ground-glass opacity (GGO)			<0.001
Yes	168 (56.00)	45 (97.83)
No	132 (44.00)	1 (2.17)
Consolidation			<0.001
Yes	15 (5.00)	17 (36.96)
No	285 (95.00)	29 (63.04)
Reticular pattern			<0.001
Yes	102 (34.00)	40 (86.96)
No	198 (66.00)	6 (13.04)
Nodules			0.397
Yes	76 (25.33)	9 (19.57)
No	224 (74.67)	37 (80.43)
Crazy-paving pattern			0.012
Yes	6 (2.00)	4 (8.70)
No	294 (98.00)	42 (91.30)
Septal thickening			0.001
Yes	16 (5.33)	9 (19.57)
No	284 (94.67)	37 (80.43)
Halo sign			0.938
Yes	6 (2.00)	1 (2.17)
No	294 (98.00)	45 (97.83)
Bronchial wall thickening			0.006
Yes	1 (0.33)	2 (4.35)
No	299 (99.67)	44 (95.65)
Traction bronchiectasis			0.695
Yes	1 (0.33)	0 (0)
No	299 (99.67)	46 (100)
Air bronchogram			<0.001
Yes	3 (1.00)	10 (21.74)
No	297 (99.00)	36 (78.26)
Pleural thickening			<0.001
Yes	24 (8.00)	13 (28.26)
No	276 (92.00)	33 (71.74)
Pleural effusion			<0.001
Yes	6 (2.00)	13 (28.26)
No	294 (98.00)	33 (71.74)
Lymphadenopathy			0.695
Yes	1 (0.33)	0 (0)
No	299 (99.67)	46 (100)
CT score, median (range)	2 (0~34)	20 (2~51)	<0.001

The median CT score was 21.67±11.58 in the severe cohort and 4.27±6.02 in the non-severe cohort (P<0.001). Analysis of the ROC curve yielded an area under the ROC curve (AUC) for the CT score of 0.933%. (95% CI, 0.901–0.965; P<0.001), and a Youden index of 0.737, with 6.5 serving as the ideal cut-off value for identifying a severe COVID-19 infection (sensitivity, 95.70%; specificity, 78%; Figure 1 ).

Figure 1 |

The ROC curves of CT scores used in predicting severe COVID-19.

The AUC was 0.933. The cut-off value was 6.5 provided a sensitivity and specificity of 95.70% and 78%, respectively. AUC, area under the curve.

3.3. Nomogram construction and validation

The clinical and laboratory characteristics combined with CT scores were included in the univariable analysis, and a total of 26 features were included in the multivariable logistic regression analysis. Five features, including CT score, age, lactic dehydrogenase (LDH) and hydroxybutyrate dehydrogenase (HBDH) levels, and hypertension were extracted as risk factors for severe COVID-19 infections. Based on these 5 risk factors, a nomogram for predicting the severity of a COVID-19 infection was created ( Figure 2 ).

Figure 2 |

The nomogram for predicting severe COVID-19.

Each of the variables can be located on the corresponding variable axis. The point of each variable was determined by vertically referring to the top point line. By summing up the total points of each corresponding variable, the total point was calculated, and the risk of severe COVID-19 was determined by reading against the risk axis.

We verified the model performance using a calibration curve and DCA. As shown in Figure 3 , the nomogram demonstrated excellent performance.

Figure 3 |

The calibration curves and DCA of the nomogram in predicting severe COVID-19.

The calibration curves of the nomogram (a), the model predicted severe COVID-19 was plotted on the x-axis, and the actual disease progression probability was plotted on the y-axis. DCA of the nomogram (b), compares the net benefits of three models in predicting severe COVID-19: The y-axis represents the net benefit. The x-axis denotes the threshold probability. The red line represents the model based on the CT score alone, the blue line represents the model based on the clinical characteristics alone, and the green line represents the model based on clinical characteristics and CT score. DCA, decision curves analysis.

4. DISCUSSION

COVID-19 is continuing to have an impact on a worldwide scale. Severe and critical cases have created a huge medical burden to society, especially in countries with large populations or limited medical resources. An easy and feasible clinical model predicting the severity of COVID-19 infections in a timely fashion is vital for optimal management of potentially severe cases and to achieve better clinical outcomes. Our study developed a nomogram derived from the baseline clinical and laboratory findings, CT characteristics, and CT score. Five variables were identified as risk factors for severe COVID-19 infections, including the CT score, age, LDH and HBDH levels, and hypertension. These factors can be assessed easily and in a timely fashion. In addition, the correlation between the CT score and patients with severe COVID-19 infections was investigated. The nomogram described herein, which was based on a combination of clinical characteristics and the CT score, demonstrated good performance in the calibration curve and DCA. Indeed, the model showed better prognostic ability compared to the clinical characteristics or CT score model alone.

In the current study age was a significant risk factor for severe COVID-19. Previous studies [24–26] concluded that elderly patients were at increased risk to deteriorate during the course of a COVID-19 infection. A model created by age and laboratory findings showed that patients > 65 years of age had a substantially increased probability of developing a severe COVID-19 infection than patients < 65 years of age [27]. Earlier nomograms with clinical characteristics also demonstrated that age was a significant variable in severe cases [1, 17]. It was shown that age and COVID-19 mortality were associated [28, 29], and a research involving COVID-19 patients from various nations reported the average age of the majority of COVID-19 fatalities was > 60 years. [30]. Angiotensin-converting enzyme 2 (ACE2) receptor is the gateway to human cells for SARS-CoV-2, and in patients with a severe COVID-19 infection, ACE2 expression has been shown to increase with age [31]. This finding might explain why the elderly are at highest risk for a severe COVID-19 infection.

In the present study the CT score served as an independent risk indicator for severe COVID-19 infections. Analysis of the ROC curve revealed an AUC for the CT score of 0.933% (95% CI, 0.901–0.965; P=0.000) with a 6.5 cut-off value (sensitivity, 95.70%; specificity, 78%). The CT score was the most significant variable based on multivariable logistic regression analysis (P=0.009). The relationship between the CT score and a severe COVID-19 infection has been supported by numerous investigators. Francone et al. [32] used a semi-quantitative method based on CT scores (only assessing the extent of lung lesions) in a study involving 1274 patients, which indicated that the CT score was related to age, inflammatory features, and severity. Likewise, Yang et al. [33] and Hajiahmadi et al. [34] adopted a similar scoring system and reported AUCs of 0.892 (95% CI, 0.814-0.944) and 0.764 (95% CI, 0.682-0.847), respectively. The current study used a quantitative CT scoring system that assessed the extent and nature of the lung lesions. The AUC reached 0.933 (95% CI, 0.901–0.965), demonstrating a superior power of predicting severity. Additional studies [35–37] reported nomograms that combined CT and clinical characteristics. The models outperformed the model based on clinical factors or CT features alone; however, most focused on CT radiomics and deep learning techniques. Artificial intelligence is not a widely used technique among the hospitals in China, while the CT scoring method can be easily adopted clinically.

Co-morbidities have been reported to be correlated with severe COVID-19 infections [2, 38]. Our study identified hypertension as a risk factor for poor prognosis. Previous studies [18, 39] extracted hypertension as an important variable in the development of clinical models, which is consistent with our study.

Laboratory parameters, including the LDH and HBDH levels, were shown to be independent risk factors for severe COVID-19 infections based on multivariate logistic regression analysis. The LDH level has an important role in predicting severe COVID-19 infections [4, 40, 41]. Our study also showed the HBDH level to be a risk factor. Most severe and critical patients had multiple organ dysfunction syndromes, which may be attributed to the widespread distribution of ACE2 in multiple organs, including the heart [42]. This finding explains why there are COVID-19 patients developing myocarditis in Chengdu city.

Our research has a few shortcomings and restrictions. First, there was a limited number of people in the sample. Second, this research only focused on a single site and used retrospective data. Finally, the study period was short. A larger sample and multi-centered study should be conducted to confirm our model in the future.

5. CONCLUSION

CT score, age, hypertension, and LDH and HBDH levels were shown to be risk factors to predict severe COVID-19 infections. We constructed a straightforward nomogram that has excellent predictive power to forecast poor prognosis in patients with severe COVID-19 infections, which could give early advice in medical management and increase the likelihood of a positive outcome for patients in Chengdu, China.

CONFLICT OF INTEREST

None

DATA AVAILABILITY STATEMENT

The raw/processed data required to reproduce the above findings are available from the corresponding author on reasonable request.

ETHICS STATEMENT

This retrospective study was approved by the Ethics Committee of Chengdu Public Health Clinical Center and was carried out in adherence with the Declaration of Helsinki. Due to the retrospective nature of the study, obtaining informed consent from all patients was waived.

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Simpson S, Kay F, Abbara S, Bhalla S, Chung J, et al.. Radiological Society of North America expert consensus statement on reporting chest CT findings related to COVID-19. Endorsed by the Society of Thoracic Radiology, the American College of Radiology, and RSNA – secondary publication. J Thorac Imaging. 2020. Vol. 35:219–27. 32324653 10.1097/RTI.0000000000000524
Salaffi F, Carotti M, Tardella M, Borgheresi A, Agostini A, et al.. The role of a chest computed tomography severity score in coronavirus disease 2019 pneumonia. Medicine. 2020. Vol. 99:e22433. 33080676 10.1097/MD.0000000000022433
Chen S, Sun H, Heng M, Tong X, Geldsetzer P, et al.. Factors predicting progression to severe COVID-19: a competing risk survival analysis of 1753 patients in community isolation in Wuhan, China. Engineering (Beijing, China). 2022. Vol. 13:99–106. 34721935 10.1016/j.eng.2021.07.021
Kaeuffer C, Le Hyaric C, Fabacher T, Mootien J, Dervieux B, et al.. Clinical characteristics and risk factors associated with severe COVID-19: prospective analysis of 1,045 hospitalised cases in North-Eastern France, March 2020. Euro Surveill. 2020. Vol. 25:2000895. 33272355 10.2807/1560-7917.ES.2020.25.48.2000895
Nasir N, Habib K, Iffat Khanum, Khan N, Muhammad Z, et al.. Clinical characteristics and outcomes of COVID-19: experience at a major tertiary care center in Pakistan. J Infect Dev Ctries. 2021. Vol. 15:480–9. 33956647 10.3855/jidc.14345
Jiang J, Zhong W, Huang W, Gao Y, He Y, et al.. Development and validation of a predictive nomogram with age and laboratory findings for severe COVID-19 in Hunan Province, China. Ther Clin Risk Manag. 2022. Vol. 18:579–91. 35607424 10.2147/TCRM.S361936
Moon H, Kim K, Kang E, Yang H, Lee E. Prediction of COVID-19-related mortality and 30-day and 60-day survival probabilities using a Nomogram. J Korean Med Sci. 2021. Vol. 36:e248. 34490756 10.3346/jkms.2021
Li L, Fang X, Cheng L, Wang P, Li S, et al.. Development and validation of a prognostic nomogram for predicting in-hospital mortality of COVID-19: a multicenter retrospective cohort study of 4086 cases in China. Aging. 2021. Vol. 13:3176–89. 33561834 10.18632/aging.202605
Shakor J, Isa R, Babakir-Mina M, Ali S, Hama-Soor T, et al.. Health related factors contributing to COVID-19 fatality rates in various communities across the world. J Infect Dev Ctries. 2021. Vol. 15:1263–72. 34669594 10.3855/jidc.13876
Baker S, Kwok S, Berry G, Montine T. Angiotensin-converting enzyme 2 (ACE2) expression increases with age in patients requiring mechanical ventilation. PLoS One. 2021. Vol. 16:e0247060. 33592054 10.1371/journal.pone.0247060
Francone M, Iafrate F, Masci G, Coco S, Cilia F, et al.. Chest CT score in COVID-19 patients: correlation with disease severity and short-term prognosis. Eur Radiol. 2020. Vol. 30:6808–17. 32623505 10.1007/s00330-020-07033-y
Yang R, Li X, Liu H, Zhen Y, Zhang X, et al.. Chest CT severity score: an imaging tool for assessing severe COVID-19. Radiol Cardiothorac Imaging. 2020. Vol. 2:e200047. 33778560 10.1148/ryct.2020200047
Hajiahmadi S, Shayganfar A, Janghorbani M, Esfahani M, Mahnam M, et al.. Chest Computed tomography severity score to predict adverse outcomes of patients with COVID-19. Infect Chemother. 2021. Vol. 53:308–18. 34216124 10.3947/ic.2021.0024
Li L, Wang L, Zeng F, Peng G, Ke Z, et al.. Development and multicenter validation of a CT-based radiomics signature for predicting severe COVID-19 pneumonia. Eur Radiol. 2021. Vol. 31:7901–12. 33786655 10.1007/s00330-021-07727-x
Chen Z, Li X, Li J, Zhang S, Zhou P, et al.. A COVID-19 risk score combining chest CT radiomics and clinical characteristics to differentiate COVID-19 pneumonia from other viral pneumonias. Aging. 2021. Vol. 13:9186–224. 33713401 10.18632/aging.202735
Xiong Y, Ma Y, Ruan L, Li D, Lu C, et al.. Comparing different machine learning techniques for predicting COVID-19 severity. Infect Dis Poverty. 2022. Vol. 11:19 35177120 10.1186/s40249-022-00946-4
Liu S, Luo H, Wang Y, Cuevas L, Wang D, et al.. Clinical characteristics and risk factors of patients with severe COVID-19 in Jiangsu province, China: a retrospective multicentre cohort study. BMC Infect Dis. 2020. Vol. 20:584 32762665 10.1186/s12879-020-05314-x
Zhou Y, He Y, Yang H, Yu H, Wang T, et al.. Development and validation a nomogram for predicting the risk of severe COVID-19: a multi-center study in Sichuan, China. PLoS One. 2020. Vol. 15:e0233328. 32421703 10.1371/journal.pone.0233328
Liang W, Yao J, Chen A, Lv Q, Zanin M, et al.. Early triage of critically ill COVID-19 patients using deep learning. Nat Commun. 2020. Vol. 11:3543 32669540 10.1038/s41467-020-17280-8
Ramosaço E, Kolovani E, Çomo N, Gjermeni N, Shpata V, et al.. Risk factors for poor outcome of patients with Coronavirus disease 2019 (COVID-19) in Albania. J Infect Dev Ctries. 2021. Vol. 15:1236–43. 34669590 10.3855/jidc.14592
Hamming I, Timens W, Bulthuis M, Lely A, Navis G, et al.. Tissue distribution of ACE2 protein, the functional receptor for SARS coronavirus. A first step in understanding SARS pathogenesis. J Pathol. 2004. Vol. 203:631–7. 15141377 10.1002/path.1570

Graphical abstract

Key points

The nomogram based on CT score and clinical factors showed good calibration (P = 0.539) in the calibration curve and was of significant clinical value in DCA. Thus, the nomogram could be a valuable tool for the management of COVID-19.
CT score, age, hypertension, and LDH and HBDH levels were the risk factors shown to predict severe COVID-19.
ROC analysis yielded an AUC for the CT score of 0.933% with 6.5 serving as the ideal cut-off value to predict severe COVID-19.

Author and article information

Journal

Journal ID (publisher-id): radsci

Title: Radiology Science

Publisher: Compuscript (Ireland )

ISSN (Electronic): 2811-5635

Publication date (Electronic): 09 August 2023

Volume: 2

Issue: 1

Pages: 46-55

Affiliations

[a ]Department of Radiology, Public Health Clinical Center of Chengdu, Chengdu city, China

[b ]Department of Radiology, Public Health Clinical Center of Shanghai, Shanghai city, China

Author notes

*Correspondence: 349501104@ 123456qq.com (C. Li), Tel.: +86 18080126886

Article

DOI: 10.15212/RADSCI-2023-0006

SO-VID: 464b44c6-7f85-4282-821f-f76580db9ba3

License:

This work is licensed under the Attribution-NonCommercial-NoDerivatives 4.0 International.

History

Date received : 09 June 2023

Date revision received : 08 July 2023

Date accepted : 26 July 2023

Page count

Figures: 3, Tables: 3, References: 42, Pages: 10

Funding

Funded by: The Sichuan Medical Association Youth Innovation Project

Award ID: Q21088

This study was supported by a grant from The Sichuan Medical Association Youth Innovation Project (Q21088). We are grateful to the professional advice from Yujie Yuan in this study.

Comments

Comment on this article

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[20] Shi H, Xu Z, Cheng G, Ji H, He L, et al.. CT-based radiomic nomogram for predicting the severity of patients with COVID-19. Eur J Med Res. 2022. Vol. 27:13 35078525 10.1186/s40001-022-00634-x

[21] Yin X, Min X, Nan Y, Feng Z, Li B, et al.. Assessment of the severity of Coronavirus disease: quantitative computed tomography parameters versus semiquantitative visual score. Korean J Radiol. 2020. Vol. 21:998–1006. 32677384 10.3348/kjr.2020.0423

[22] Simpson S, Kay F, Abbara S, Bhalla S, Chung J, et al.. Radiological Society of North America expert consensus statement on reporting chest CT findings related to COVID-19. Endorsed by the Society of Thoracic Radiology, the American College of Radiology, and RSNA – secondary publication. J Thorac Imaging. 2020. Vol. 35:219–27. 32324653 10.1097/RTI.0000000000000524

[23] Salaffi F, Carotti M, Tardella M, Borgheresi A, Agostini A, et al.. The role of a chest computed tomography severity score in coronavirus disease 2019 pneumonia. Medicine. 2020. Vol. 99:e22433. 33080676 10.1097/MD.0000000000022433

[24] Chen S, Sun H, Heng M, Tong X, Geldsetzer P, et al.. Factors predicting progression to severe COVID-19: a competing risk survival analysis of 1753 patients in community isolation in Wuhan, China. Engineering (Beijing, China). 2022. Vol. 13:99–106. 34721935 10.1016/j.eng.2021.07.021

[25] Kaeuffer C, Le Hyaric C, Fabacher T, Mootien J, Dervieux B, et al.. Clinical characteristics and risk factors associated with severe COVID-19: prospective analysis of 1,045 hospitalised cases in North-Eastern France, March 2020. Euro Surveill. 2020. Vol. 25:2000895. 33272355 10.2807/1560-7917.ES.2020.25.48.2000895

[26] Nasir N, Habib K, Iffat Khanum, Khan N, Muhammad Z, et al.. Clinical characteristics and outcomes of COVID-19: experience at a major tertiary care center in Pakistan. J Infect Dev Ctries. 2021. Vol. 15:480–9. 33956647 10.3855/jidc.14345

[27] Jiang J, Zhong W, Huang W, Gao Y, He Y, et al.. Development and validation of a predictive nomogram with age and laboratory findings for severe COVID-19 in Hunan Province, China. Ther Clin Risk Manag. 2022. Vol. 18:579–91. 35607424 10.2147/TCRM.S361936

[28] Moon H, Kim K, Kang E, Yang H, Lee E. Prediction of COVID-19-related mortality and 30-day and 60-day survival probabilities using a Nomogram. J Korean Med Sci. 2021. Vol. 36:e248. 34490756 10.3346/jkms.2021

[29] Li L, Fang X, Cheng L, Wang P, Li S, et al.. Development and validation of a prognostic nomogram for predicting in-hospital mortality of COVID-19: a multicenter retrospective cohort study of 4086 cases in China. Aging. 2021. Vol. 13:3176–89. 33561834 10.18632/aging.202605

[30] Shakor J, Isa R, Babakir-Mina M, Ali S, Hama-Soor T, et al.. Health related factors contributing to COVID-19 fatality rates in various communities across the world. J Infect Dev Ctries. 2021. Vol. 15:1263–72. 34669594 10.3855/jidc.13876

[31] Baker S, Kwok S, Berry G, Montine T. Angiotensin-converting enzyme 2 (ACE2) expression increases with age in patients requiring mechanical ventilation. PLoS One. 2021. Vol. 16:e0247060. 33592054 10.1371/journal.pone.0247060

[32] Francone M, Iafrate F, Masci G, Coco S, Cilia F, et al.. Chest CT score in COVID-19 patients: correlation with disease severity and short-term prognosis. Eur Radiol. 2020. Vol. 30:6808–17. 32623505 10.1007/s00330-020-07033-y

[33] Yang R, Li X, Liu H, Zhen Y, Zhang X, et al.. Chest CT severity score: an imaging tool for assessing severe COVID-19. Radiol Cardiothorac Imaging. 2020. Vol. 2:e200047. 33778560 10.1148/ryct.2020200047

[34] Hajiahmadi S, Shayganfar A, Janghorbani M, Esfahani M, Mahnam M, et al.. Chest Computed tomography severity score to predict adverse outcomes of patients with COVID-19. Infect Chemother. 2021. Vol. 53:308–18. 34216124 10.3947/ic.2021.0024

[35] Li L, Wang L, Zeng F, Peng G, Ke Z, et al.. Development and multicenter validation of a CT-based radiomics signature for predicting severe COVID-19 pneumonia. Eur Radiol. 2021. Vol. 31:7901–12. 33786655 10.1007/s00330-021-07727-x

[36] Chen Z, Li X, Li J, Zhang S, Zhou P, et al.. A COVID-19 risk score combining chest CT radiomics and clinical characteristics to differentiate COVID-19 pneumonia from other viral pneumonias. Aging. 2021. Vol. 13:9186–224. 33713401 10.18632/aging.202735

[37] Xiong Y, Ma Y, Ruan L, Li D, Lu C, et al.. Comparing different machine learning techniques for predicting COVID-19 severity. Infect Dis Poverty. 2022. Vol. 11:19 35177120 10.1186/s40249-022-00946-4

[38] Liu S, Luo H, Wang Y, Cuevas L, Wang D, et al.. Clinical characteristics and risk factors of patients with severe COVID-19 in Jiangsu province, China: a retrospective multicentre cohort study. BMC Infect Dis. 2020. Vol. 20:584 32762665 10.1186/s12879-020-05314-x

[39] Zhou Y, He Y, Yang H, Yu H, Wang T, et al.. Development and validation a nomogram for predicting the risk of severe COVID-19: a multi-center study in Sichuan, China. PLoS One. 2020. Vol. 15:e0233328. 32421703 10.1371/journal.pone.0233328

[40] Liang W, Yao J, Chen A, Lv Q, Zanin M, et al.. Early triage of critically ill COVID-19 patients using deep learning. Nat Commun. 2020. Vol. 11:3543 32669540 10.1038/s41467-020-17280-8

[41] Ramosaço E, Kolovani E, Çomo N, Gjermeni N, Shpata V, et al.. Risk factors for poor outcome of patients with Coronavirus disease 2019 (COVID-19) in Albania. J Infect Dev Ctries. 2021. Vol. 15:1236–43. 34669590 10.3855/jidc.14592

[42] Hamming I, Timens W, Bulthuis M, Lely A, Navis G, et al.. Tissue distribution of ACE2 protein, the functional receptor for SARS coronavirus. A first step in understanding SARS pathogenesis. J Pathol. 2004. Vol. 203:631–7. 15141377 10.1002/path.1570

Radiology Science

A nomogram for predicting the severity of COVID-19 infections among patients in Chengdu, China

Introduction:

Methodology:

Results:

Conclusions:

1. INTRODUCTION

2. METHODOLOGY

2.1. Patients

2.2. Clinical data

2.3. CT image characteristics and CT scores

2.4. Statistical analysis

3. RESULTS

3.1. Clinical and laboratory findings

3.2. CT findings and CT scores

3.3. Nomogram construction and validation

4. DISCUSSION

5. CONCLUSION

Key points

Journal

Affiliations

Author notes

Article

History

Page count

Funding

Categories

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