A comparison of demographic, epidemiological and clinical characteristics of hospital influenza-related viral pneumonia patients

Background Through the comparison of the demographic, epidemiological, and clinical characteristics of hospital human influenza (influenza A (H1N1) pdm09, H3N2, and B)-related and hospitalized avian-origin influenza A (H7N9)-related viral pneumonia patients, find the different between them. Methods A retrospective study was conducted in hospitalized influenza-related viral pneumonia patients. Results Human influenza A-related patients in the 35–49-year-old group were more than those with B pneumonia patients (p = 0.027), and relatively less in the ≥ 65-year-old group than B pneumonia patients (p = 0.079). The proportion of comorbid condition to human influenza A pneumonia was 58%, lower than B pneumonia and H7N9 pneumonia patients (78% vs. 77.8%; p = 0.013). The proportion of invasive mechanical ventilation (IMV), lymphocytopenia, elevated lactate dehydrogenase to hospitalized human influenza A-related viral pneumonia patients was higher than B pneumonia patients (p < 0.05), but lower than H7N9 pneumonia patients (p < 0.05). In the multivariate analysis, pulmonary consolidation (odds ratio (OR): 13.67; 95% confidence interval (CI) 1.54–121.12; p = 0.019) and positive bacterial culture (sputum) (OR: 7.71; 95% CI 2.48–24.03; p < 0.001) were independently associated with IMV, while shock (OR: 13.16; 95% CI 2.06–84.07; p = 0.006), white blood cell count > 10,000/mm3 (OR: 7.22; 95% CI 1.47–35.58; p = 0.015) and positive bacterial culture(blood or sputum) (OR: 6.27; 95% CI 1.36–28.85; p = 0.018) were independently associated with death in the three types hospitalized influenza-related viral pneumonia patients. Conclusions Hospital influenza B-related viral pneumonia mainly affects the elderly and people with underlying diseases, while human influenza A pneumonia mainly affects the young adults; however, the mortality was similar. The hospitalized human influenza A-related viral pneumonia patients was severer than B pneumonia patients, but milder than H7N9 pneumonia patients. Pulmonary consolidation and positive bacterial culture (sputum) were independently associated with IMV, while shock, white blood cell count > 10,000/mm3, and positive bacterial culture (blood or sputum) were independently associated with death to three types hospitalized influenza-related viral pneumonia patients. Supplementary Information The online version contains supplementary material available at 10.1186/s12879-021-06485-x.


Background
Influenza causes considerable morbidity during each annual influenza season. In April 2009, the influenza A (H1N1) pdm09 (pH1N1) virus emerged in Mexico and the USA and spread globally [1]. Since the first report of pneumonia that was caused by the pH1N1 virus in Mexico [2], severe cases have been documented worldwide. Influenza B virus has been classically considered less pathogenic than influenza A virus in adults and mostly responsible for mild respiratory infections, while severe illness and poor prognosis have been associated with bacterial coinfection [3,4]. On March 30, 2013, three individuals with severe pneumonia were found to be infected with a novel avian-origin influenza A (H7N9) virus that had not been detected in humans and animals previously. As of May 9, 2013, 131 laboratory-confirmed cases were reported, including 32 deaths [5], and the majority of these patients were reported in China.
The comparison of the demographic, epidemiological, and clinical characteristics of hospital human influenza (influenza A (H1N1) pdm09, H3N2, and B)-related and hospitalized avian-origin influenza A (H7N9)-related viral pneumonia patients has not been reported. 2017-2018 influenza season was dominated by pH1N1 and B viruses along with co-circulation of H3N2 virus, this season provided a unique opportunity to directly compare the demographic, epidemiological, and clinical characteristics of hospitalized human influenza A (pH1N1 and H3N2)-related viral pneumonia patients to the hospital influenza B-related viral pneumonia patients. Also, we compared the demographic, epidemiological, and clinical characteristics of these hospitalized human influenza (pH1N1, H3N2, and B)-related viral pneumonia patients to the hospital H7N9-related viral pneumonia patients in 2017, and aimed to discover the factors independently associated with invasive mechanical ventilation (IMV) or death among these three types hospitalized influenzarelated viral pneumonia patients.

Study design and study population
A retrospective study was conducted from November 1, 2017 to March 31, 2018 at the First Affiliated Hospital, College of Medicine, Zhejiang University, China. All patients, > 14 years of age and with hospital stay > 24 h with confirmed human influenza A or B-related viral pneumonia were included in this study. In addition to above factors, those with confirmed H7N9-related viral pneumonia from January 1, 2017 to May 3, 2017 were also included. This study was approved by the Ethical Board of the hospital.
This retrospective study evaluated the reverse transcriptase-polymerase chain reaction (RT-PCR) tests and computed tomography results daily in hospitalized patients with confirmed human influenza A-or B-related viral pneumonia or H7N9-related viral pneumonia. These cases were assessed by an Infectious Disease doctor and nasopharyngeal swabs (NPS) or sputum specimens were collected within the first 24 h of hospitalization and processed immediately. Influenza-related viral pneumonia was defined as confirmed human influenza A or B or H7N9 virus infection and the presence of a new infiltrate on computed tomography plus fever or respiratory symptoms. All radiological evaluations were performed by two radiologists who were blinded to the clinical information.

Data collection and definitions
Clinical data were acquired from electronic medical records. The following variables were recorded: demographics, comorbid conditions, current smoking status, alcohol abuse, pregnancy, body mass index (BMI), clinical feature, laboratory data, radiographic finding, complication, treatment, and clinical outcome. The definitions of obesity, current smoking status, alcohol abuse, confirmed human influenza A or B, confirmed H7N9, lymphocytopenia, thrombocytopenia, rhabdomyolysis, acute kidney injury, immunosuppression, early antiviral therapy, exposure to live poultry and severe cases were provided in Additional file 1.

Statistical analysis
Categorical variables were compared by the Chi-square or Fisher's exact test. Continuous variables were compared by the t-test or the Mann-Whitney test. The multivariate logistic regression analysis of factors potentially associated with IMV or in-hospital mortality included the variables that were significant in the univariate analysis and clinically important variables. Statistical significance was established at p-value < 0.05. All statistical analyses were performed using SPSS v.18. (SPSS Inc., Chicago, IL, USA).

Demographic and epidemiological characteristics
From November 1, 2017 to March 31, 2018, a total of 4297 cases of laboratory-confirmed human influenza A and B viral infection were reported in our hospital. Of these, 2335 cases were human influenza A (about 85% were pH1N1 and 15% were H3N2), 1880 cases were influenza B, and 82 cases were infected with both viruses. Finally, 138 cases of hospitalized human influenza A-related viral pneumonia and 59 cases of hospitalized influenza B-related viral pneumonia were included in this study. From January 1, 2017 to May 3, 2017, a total of 18 cases of hospitalized H7N9-related viral pneumonia were also included in the current study. The median age of hospitalized human influenza A-related viral pneumonia patients was lower than those with B pneumonia (57 years (interquartile range (IQR), 45.8-66.3) vs. 62 years (IQR, 53-74); p = 0.034). In the 35-49-yearold age group, the proportion of hospitalized human influenza A-related viral pneumonia patients was 23.9%, which was higher than B pneumonia patients (10.2%; p = 0.027). In the ≥ 65-year-old group, the proportion of hospitalized human influenza A-related viral pneumonia patients was 32.6%, which was relatively lower than B pneumonia patients (45.8%; p = 0.079; Table 1). The proportion of comorbid conditions in hospitalized human influenza A-related viral pneumonia patients was 58%, which was lower than the B pneumonia patients and hospitalized H7N9 pneumonia patients (78% vs. 77.8%; p = 0.013). Interestingly, 66.7% of hospitalized H7N9-related viral pneumonia patients were exposed to live poultry.

Complications, treatment, and clinical outcomes
In the current study, the proportion of intensive care unit (ICU) admission in hospitalized human influenza A-related viral pneumonia patients was 19.6%, which higher than 6.8% of B pneumonia patients (p = 0.024). The proportion of IMV in hospitalized human influenza A-related viral pneumonia patients was 16.7%, which also higher than that in B pneumonia patients 3.4% (p = 0.01) ( Table 3). The proportion of IMV in hospitalized H7N9-related viral pneumonia patients was 38.9%, which was higher than that in human influenza A and B pneumonia patients ( In the treatment, the rate of glucocorticoid use in hospitalized H7N9-related viral pneumonia patients was 100%, which was higher than human influenza A and B pneumonia patients (55.8% vs. 40.7%; p < 0.001). All the hospitalized human influenza A-related viral pneumonia patients and hospitalized influenza B-related viral pneumonia patients were treated with oseltamivir or peramivir or both, and all the hospitalized H7N9-related viral pneumonia patients were treated with a combination of oseltamivir with peramivir. However, the time from onset of illness to administration of antiviral therapy in hospitalized H7N9-related viral pneumonia patients was 4 days (IQR, 3-8.3), which was relatively shorter than that of human influenza A and B pneumonia patients (7 days (IQR, 5-10.8) vs. 6 days (range, [3][4][5][6][7][8][9][10][11][12][13][14]; p = 0.089). The time of administration of antiviral therapy to virusnegative time of hospitalized H7N9-related viral pneumonia patients was 5.5 days (IQR, 2.8-10), shorter than human influenza A and B pneumonia patients (10 days (IQR, 6-14.5) vs. 11 days (IQR, 6-17.75); p = 0.007).

Factors associated with IMV due to three types hospitalized influenza-related viral pneumonia patients
In the univariate analysis, the three types hospitalized influenza-related viral pneumonia patients with IMV had significantly higher neutrophil percentage, C-reactive protein, AST, DD, blood urea nitrogen, pro-B-type natriuretic peptides, and partial pressure arterial oxygen/ fraction of inspired oxygen (PaO 2 :FiO 2 ) levels than the three types hospitalized influenza-related viral pneumonia patients without IMV. Furthermore, the proportion of patients with shortness of breaths, lymphocytopenia, elevated procalcitonin, AST, CK, DD, and LDH, positive bacterial culture (sputum) on presentation or during hospitalization, positive bacterial culture (blood or sputum) on presentation or during hospitalization, CURB-65 score ≥ 2, bilateral pneumonia, and pulmonary consolidation in the three types of hospitalized influenza-related viral pneumonia patients with IMV was significantly higher than those without IMV, while the lymphocyte count in the three types of pneumonia patients with IMV was lower than those without IMV (Additional file 2: Table S1). In the multivariate analysis, pulmonary consolidation (odds ratio (OR): 13.67; 95% confidence interval (CI) 1.54-121.12; p = 0.019) and positive bacterial culture (sputum) at the time of presentation or during hospitalization (OR: 7.71; 95% CI 2.48-24.03; p < 0.001) were independently associated with IMV in the three types hospitalized influenza-related viral pneumonia patients (Additional file 4: Table S3).

Factors associated with death due to the three types hospitalized influenza-related viral pneumonia patients
In the univariate analysis, the three types of hospitalized influenza-related viral pneumonia patients who die in the hospital had significantly higher neutrophil percentage, hemoglobin, blood platelet counts, C-reactive protein, DD, blood urea nitrogen, pro-B-type natriuretic peptides, and PaO 2 :FiO 2 levels than the survivors. Also, the proportion of elevated white blood cell count and procalcitonin, positive bacterial culture (sputum) on presentation or during hospitalization, CURB-65 score ≥ 2, IMV, shock to the three types hospitalized influenzarelated viral pneumonia patients who die in the hospital was significantly higher than that of the survivors (Additional file 3: Table S2). In the multivariate analysis, shock (OR: 13.16; 95% CI 2.06-84.07; p = 0.006), white blood cell count > 10,000/mm 3 (OR: 7.22; 95% CI 1.47-35.58; p = 0.015) and positive bacterial culture (blood or sputum) on presentation or during hospitalization (OR: 6.27; 95% CI 1.36-28.85; p = 0.018) were independently associated with death in the three types hospitalized influenzarelated viral pneumonia patients (Table 4).

Discussion
This was the first study that compared the demographic, epidemiological, and clinical characteristics of hospitalized human influenza-related viral pneumonia patients with H7N9 pneumonia patients. The study revealed that the hospitalized human influenza A-related viral pneumonia patients were younger than those with B pneumonia, and the infection was primarily detected in young adults. On the other hand, the influenza B-related viral pneumonia was common in the elderly, usually with comorbid conditions. Hospitalized human influenza A-related viral pneumonia patients was severer than B pneumonia patients, but milder than H7N9 pneumonia patients.
The proportion of patients who have at least one comorbid condition in those with human influenza A-related viral pneumonia was lower than those with B pneumonia and H7N9 pneumonia patients. Moreover, the average age of hospitalized human influenza A-related viral pneumonia patients was lower than that of B pneumonia patients, and the proportion of the hospitalized human influenza A-related viral pneumonia patients in the 35-49 age group was more than that of the B pneumonia patients, and the proportion in the ≥ 65 years age group was relatively less than that of the B pneumonia patients. Some studies have reported that influenza B mainly affects the elderly and people with underlying diseases [6,7]; however, pH1N1 mainly affects young adults, similar to our research. Early-life exposure to an antigenically related virus, i.e., the A (H1N1) strain that circulated after the 1918 pandemic and prior to the 1957 A (H2N2) pandemic might mitigate the severity for the pH1N1 strain in older individuals; this phenomenon explained the survival of elderly in the pandemic. In China, the old people retire at 60 years of age and have more opportunities to shop in live-animal markets, therefore more likely to be exposed to the livepoultry, it can partially explain why the H7N9 patients have more comorbid conditions.
In the aspect of clinical characteristics and diagnostic findings, CK was designated as a biomarker of severity in pH1N1 infection; the elevation of CK was associated with complications, increased length of ICU stay, and healthcare resources [8]. Another study included 155 hospitalized adult patients with pH1N1; LDH was an independent risk factor of hospital death as assessed by multivariate logistic regression analysis [9]. The elevation of DD may be caused by the embolism of the small  pulmonary vessels, then the pulmonary ventilation and blood flow ratio became abnormal, and the blood oxygen saturation declined. Finally, the rate of mortality was elevated; however, this hypothesis needs further substantiation. A lymphocyte count of < 300 lymphocytes/μL was observed in a subgroup of patients with poor outcome in a study encompassing 239 inpatients with confirmed influenza virus infection [10]. Thus, we can conclude that the proportion of elevated CK, LDH, DD, and lymphocytopenia was positively relative to the severity of influenza. In this study, the elevated LDH and lymphocytopenia in hospitalized human influenza A-related viral pneumonia patients was higher than that in B pneumonia patients, and the elevated CK, LDH, DD, and lymphocytopenia in hospitalized H7N9related viral pneumonia patients was higher than that in human influenza A and B pneumonia patients. The proportion of ICU admission and invasive mechanical ventilation in hospitalized human influenza A-related viral pneumonia patients was higher than that in B pneumonia patients. The proportion of IMV and the median value of hospitalization expense in hospitalized H7N9related viral pneumonia patients were higher than that in human influenza A and B pneumonia patients. Taken together, it can be concluded that the hospitalized human influenza A-related viral pneumonia patients was severer than B pneumonia patients, but milder than H7N9 pneumonia patients. A study consisting of 57 cases of H7N9 patients and 14 cases of pH1N1 patients demonstrated that the proportion of acute respiratory distress syndrome to H7N9 was much higher than that of pH1N1 [11], which was also observed in the current study. Furthermore, the proportion of ICU admission and IMV to pH1N1 was twofold higher than that of B, and no difference was detected in the mortality as reported by a study including 2791 cases of adult patients [12]. Another study reported that the mortality of adults influenza B patients was similar to that of pH1N1 patients [13]. Although all the influenza viruses infect the respiratory epithelium from the nasal passages to bronchioles, pH1N1 tends to infect pneumocytes and interalveolar macrophages, causing extensive areas of inflammation in the alveoli, which could partially explain the increased severity of pH1N1 [14][15][16][17]. Hospitalized influenza B-related viral pneumonia mainly affects the elderly and those with underlying diseases, rendering them as severe cases, such that the mortality of B pneumonia patients was elevated and similar to human influenza A pneumonia patients. Hypercytokinemia is characterized by the over-production of various proinflammatory cytokines and plays an significant role in disease severity and mortality in H5N1 patients [18]. Compared with pH1N1 infection, H7N9 virus infection tends to induce higher cytokine expression, resembling the cytokine storm observed in H5N1 infection [19], which could partially explain why the H7N9 infection was severer than pH1N1. The World Health Organization Guidelines recommended that prompt empirical antiviral treatment should be initiated when influenza is suspected, even before laboratory results are known [20]. Improved clinical outcomes have been described among adults treated with antiviral drugs after hospitalization or up to 5 days from illness onset [21][22][23]. Early antiviral therapy within 2 days of illness accelerated viral shedding and reduced the mortality in patients with H7N9 viral infection [24]. Moreover, compared to early antiviral therapy, H7N9 patients with delayed antiviral therapy became severe cases [25]. Interestingly, in a study comprising of 82 cases of H7N9 virus infection, the time of onset of illness to administration of antiviral therapy was 6 days (IQR: 4-8), longer than that in the current study 4 days (IQR:3-8.3), and the administration of antiviral therapy to virus-negative time of the study was 7 days (IQR: 5-9), also longer than 5.5 days (IQR: 2.8-10) in the current study; the mortality was 34.1% [26]. Gao et al. [27] reported that the rate of glucocorticoid use of the H7N9 cases was 62.2%, lower than our study 100% and the mortality was 27%. The mortality of hospitalized H7N9-related viral pneumonia patients was much higher than that of human influenza A and B pneumonia. However, in the current study, the mortality of hospitalized H7N9-related viral pneumonia patients was lower than before and similar to human influenza A and B pneumonia. This phenomenon might be explicated by the initial antiviral time relatively early than before and the rate of glucocorticoid use for H7N9 was high. All our patients received oseltamivir with peramivir that also may reduce the mortality, although these findings need to be substantiated further. In the current study, the proportion of early antiviral therapy in the three types of hospitalized influenza-related viral pneumonia patients was similar.
Nevertheless, the present study has several limitations. First, influenza testing was ordered at the physicians' discretion, and therefore, not all individuals with influenza were tested, or testing could be biased towards severe cases. However, this bias would not affect our main findings because influenza testing was ordered independently of the knowledge of the virus type or subtype. Second, we only included the hospitalized influenza-related viral pneumonia patients and excluded the outpatient cases and hospitalized patients without influenza-related viral pneumonia, such that it cannot reflect the whole disease spectrum. Finally, because the RT-PCR was not accurate absolutely, the real influenza-positive patients may be diagnosed as negative.