Introduction

The novel coronavirus, named severe acute respiratory syndrome coronavirus-2 (SARS-CoV-2) that causes the coronavirus disease 2019 (COVID-19) [1], was first detected in Wuhan, the provincial capital of Hubei, China, in December 2019. SARS-CoV-2 has rapidly spread to many other countries worldwide becoming an unprecedented astounding and devastating pandemic in a short period of time.

Following an exponential upward trend, the increasing number of cases and death toll remain to concern the scientific community around the globe. Currently, more than 13.8 million cases are confirmed worldwide, with more than 593,000 deaths [2]. The first case of COVID-19 in Brazil was detected on February 26, 2020. Standing out worldwide for having one of the steepest epidemiological curves, the country has 2.04 million confirmed cases and more than 77,800 deaths so far [3]. As the most populous areas, the states of São Paulo and Rio de Janeiro have predictably concentrated the highest numbers of cases and deaths. Thus far, Brazil has been considered the new epicenter of the global pandemic [4].

In general, the vast majority of COVID-19 patients develop mild symptoms or remain asymptomatic over the course of the disease. An intermediate group of patients have moderate symptoms requiring hospitalization and some noninvasive intervention. Another group of patients have a more severe course of the disease with desaturation, dyspnea, septic shock, and/or multiple organ dysfunction leading to life-threatening consequences or death [5].

Patients with cancer are more likely to have severe complications and even death when affected by COVID-19 [6–8], mainly due to the effects of the immunosuppressive anticancer treatments, frequent use of corticosteroids, advanced age, comorbidities and pulmonary involvement (primary tumors or secondary lung metastases). Particularly in low- and middle-income countries, COVID-19 has brought a heavy burdening to the public health systems and induced new planning and adjustments in the clinical approach to cancer patients [9].

Based on a few series previously published around the world, data evaluating the impact of COVID-19 outbreak in management and survival of patients with cancer are still very scarce, incomplete, with heterogeneous outcomes and descriptions [10–15]. Brazilian data in this specific field are still unknown due to the lack of publications.

The aim of this report was to describe the demographics, clinical characteristics and laboratory abnormalities of cancer inpatients with COVID-19 admitted to the hospital ward of the Brazilian National Cancer Institute (INCA), exploring factors associated with death.

Methods

Results

A total of 181 patients had the diagnosis of COVID-19 confirmed at INCA and were considered eligible for this study. The median follow-up for the general population was 5 days (interquartile range, IQR 2–10.3).

The demographic and clinical characteristics are described in detail in Table 1. The mean age was 55.3 years (standard deviation, SD ±21.1) and 92 (50.8%) patients aged 60 or older. Female gender was more prevalent (110 [60.8%]) and 40 patients (22.1%) were former or current smokers. Comorbidities were found in 110 (60.8%) cases, of which the most common were hypertension (77 [42.5%]) and diabetes (31 [17.1%]), and 21 (11.6%) patients had three or more comorbidities. Long-term use of corticosteroids was seen in 21 (11.6%) cases.

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Table 1. Baseline demographic and clinical characteristics of the patients.

https://doi.org/10.1371/journal.pone.0241261.t001

The most prevalent solid tumors were breast (40 [22.1%]), gastrointestinal (24 [13.3%]), gynecological (22 [12.2%]) and urological (17 [9.4%]). Lung cancer patients made up only 7 (3.9%) cases. Among hematological malignancies, lymphoma (20 [11%]) and leukemia (10 [5.5%]) predominated. A more detailed list of the frequency of cancers by site is detailed in the supporting information section (S1 Table). Patients with metastatic disease accounted for almost half of the cases (90 [49.7%]) and 32 (17.7%) patients had lung metastases. More than a third of the cases (63 [34.8%]) had recently undergone cytotoxic chemotherapy within the last 60 days before the COVID-19 diagnosis, 32 (17.7%) were in best supportive care and 27 (14.9%), in post-treatment clinical surveillance. Only nine patients (5%) were receiving targeted therapy or immunotherapy with checkpoint inhibitors as the current treatment line (Table 1).

Information regarding the conditions of hospital admission and clinical evolution of patients are summarized in Table 2. More than half of the patients (98 [54.1%]) were admitted due to clinical worsening related to COVID-19 and 151 (83.4%) were symptomatic at the time of diagnostic confirmation. The most frequent symptoms were dyspnea (94 [51.9%]), cough (87 [48.1%]) and fever (66 [36.5%]). Admission to the ICU occurred in 32 (17.7%) cases, 130 (71.8%) patients required supplemental oxygen, and 35 (19.3%) cases progressed unfavorably with the need for mechanical ventilation. Ten patients (5.5%) were transferred out from INCA during the course of COVID-19. Fig 1 shows, from the day of swab collection, the timeline of events during hospital stay for COVID-19 patients and highlights that some patients had a rapidly deterioration of their clinical course once infected with SARS-CoV-2.

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Fig 1. Timeline individual cancer inpatients with COVID-19 for events during hospital stay.

All cases were represented in the graphic, with some overlaps of timelines.

https://doi.org/10.1371/journal.pone.0241261.g001

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Table 2. Patient characteristics at admission and events throughout the hospital stay.

https://doi.org/10.1371/journal.pone.0241261.t002

The most common complications during hospitalization were respiratory failure (70 [38.7%]), septic shock (40 [22.1%]) and acute kidney injury (33 [18.2%]), with 19 (10.5%) patients requiring hemodialysis support. As for laboratory results, the median absolute lymphocytes count was 988/μL (IQR 588–1488), the mean C-reactive protein levels were 19.4 mg/dL (SD ±15.0) and median D-dimer levels were 2099 ng/mL (IQR 909–5948).

Under the clinical diagnosis of a severe acute respiratory syndrome, where influenza infection was considered one of the causative hypotheses and before the final RT-PCR result was confirmed as SARS-CoV-2 infection, oseltamivir was administered to 41 (22.7%) cases. During the course of COVID-19, more than half of the patients (98 [54.1%]) received corticosteroids, 148 (81.8%) were treated with antibiotics (including those against bacterial coinfections), and therapeutic anticoagulation was prescribed to 39 (21.5%) patients. Eight (4.4%) patients received chloroquine and 36 (19.9%), ivermectin.

At the time of analysis, a total of 60 patients (33.1%) had died due to COVID-19. For solid tumors, the COVID-19-specific mortality rate was 37.7% (52/138) and for hematological malignancies (leukemia, lymphoma and multiple myeloma) was 23.5% (8/34). Four out of seven (57.1%) patients with lung cancer died from COVID-19, as well 52.5% (21/40) of breast cancer patients (Fig 2).

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Fig 2. COVID-19-related mortality rate according to the cancer type.

https://doi.org/10.1371/journal.pone.0241261.g002

As shown in Table 3, mortality related to COVID-19 was significantly associated to older age (P < .001 for patients between 60 to 74 years and P = .002 for patients aged 75 years or older), metastatic cancer (P < .001), two or more sites of metastases (P < .001), the presence of lung (P < .001) or bone metastases (P = .001), non-curative treatment or best supportive care intent (P < .001), higher C-reactive protein levels (P = .002), admission due to COVID-19 (P = .009), and antibiotics use (P = .02). Isolated or combined comorbidities and elevated D-dimer levels did not demonstrate increased risk of dying from COVID-19.

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Table 3. Variables associated to the risk of death from COVID-19^*.

https://doi.org/10.1371/journal.pone.0241261.t003

Different modalities of cancer therapy, including systemic agents (chemotherapy, hormone therapy, targeted therapy, immunotherapy), surgical procedures or radiotherapy within 60 days before COVID-19 were not associated with mortality. Also, specific therapies during the COVID-19 course, such as oseltamivir, therapeutic anticoagulation, corticosteroids, ivermectin and chloroquine did not influence the risk of death (S2 Table).

According to the multivariate analysis patients admitted due to COVID-19 symptoms (OR 2.3, 95% CI—1.1 to 4.9, P = .027) and with two (OR 10.0, 95% CI—3.6 to 28.3, P < .001) or more metastatic sites (OR 14.8, 95% CI—4.1 to 53.2, P < .001) showed a significantly higher risk of COVID-19-specific death.

Discussion

The findings of this cohort highlight, in detail, several significant aspects of the COVID-19 course in patients already diagnosed with cancer. Although the emergency period for case selection was considerably short, due to the large number of cancer patients admitted to INCA with COVID-19, 181 patients were successfully included for analysis. Women had greater representation, more than half of the patients aged 60 years or older and almost a quarter of the patients had also reported smoking. Patients with two or more comorbidities accounted for more than a quarter of the study population as well, in which hypertension and diabetes prevailed.

Almost half of the patients (83 [45.9%]) were hospitalized due to conditions unrelated to the SARS-CoV-2 infection which can be explained by patients asymptomatic for COVID-19 having been admitted to hospital for other cancer-related clinical complications. An intra-hospital transmission may also be considered, raising an important issue about the remarkable risk of infection to patients admitted for elective procedures. As for the symptoms present at diagnosis, similarly to data of other series [7, 8, 10, 12, 14], in the current cohort, dyspnea, cough and fever were all highly frequent.

The odds of some COVID-related complications were quite similar to the findings reported by Kuderer et al.(14) in an international prospective series in which more than 928 patients were analyzed. The rate of ICU admission of 14% (versus 17.7% in the current study) and the mechanical ventilation requirement rate of 12% (versus 19.3% in the current study) were also alike in proportional terms. Zhang et al. [6] also showed paralleled data with respect to other variables such as the demand of supplemental oxygen in 78.6% of cases (versus 71.8% in the current study).

Early data from non-cancer patients suggested that 14–19% of cases progress with severe complications, such as septic shock, respiratory failure, acute kidney injury and multiple organ failure [5, 15, 18]. In the present study, these rates were much higher, ranging from 18.2 to 38.7%, highlighting the increased likelihood of severe complications in cancer patients. Conversely, cerebrovascular and cardiovascular events were less frequent.

In total, 69 (38.1%) of 181 patients died. Herein, COVID-19-related mortality was considered as the endpoint. Consequently, nine patients who clearly have recovered from COVID-19, and died due to other cancer-related reasons, were excluded from this mortality analysis. Therefore, the overall COVID-19-related mortality rate reached almost one third of the cases (60 [33.1%]), which was higher than that reported by other series with cancer patients [7, 8, 10, 12, 14], and far exceeding the mortality reported for non-cancer patients [5]. It is important to point out that some patients had the definition of non-invasive support after or even before the diagnosis of COVID-19 due to the severity of their advanced malignancies, which may have overestimated the mortality rate. In addition to this, a noticeable number of the analyzed patients (103 [56.9%]) were under non-curative treatment or best supportive care at the time, reflecting the advanced stage of their respective diseases.

Unlike in the multicenter studies recently published by Mehta et al. [10] and Dai et al. [15], the mortality rate was higher in patients with solid tumors than in patients with hematological malignancies, possibly due to the small number of hematological patients in this cohort. But likewise, lung cancer, breast cancer and gastrointestinal cancer stood for the highest numbers of cases progressing to death.

In line with the results published by Kuderer et al. [14], the characteristics associated with clinical fragility, such as being elderly, having advanced stage, a greater number of metastases, pulmonary metastases, non-curative treatment or supportive treatment and symptomatic patients at hospital admission were significantly associated with a higher risk of death. In this same context, the type of anti-cancer treatment received by patients within the previous 60 days did not influence survival outcome.

Except for the association of C-reactive protein with mortality (OR 1.04; p = 0.002), none of the laboratory markers were likely to predict a higher risk of mortality. Other laboratory exams, including inflammatory markers such as lactate, ferritin, fibrinogen, and lactate dehydrogenase were not regularly collected in this cohort, preventing related analyses. A prospective study in order to evaluate the immune response markers in our cohort of cancer patients with COVID-19 is being currently conducted.

As in the study performed by Kuderer et al. [14], none of the specific therapies prescribed such as antiviral oseltamivir (used for the initial suspicion of influenza infection), therapeutic anticoagulation, ivermectin or chloroquine influenced the risk of death in the current cohort. The strong association between the use of antibiotics and the outcome of death can be explained by the fact that these patients showed a more serious condition than COVID-19, including coinfections.

Lastly, finishing on a positive note, some strengths of the current study can also be recognized. The Brazilian National Cancer Institute is the most important national reference center for the treatment of cancer patients through the Brazilian Public Health System (SUS), with a high admission charge, enabling a quick inclusion of patients for this study.

This was one of the largest series ever undertaken to explore the impacts of SARS-CoV-2 infection specifically in cancer patients. Throughout the analysis, many variables were presented, allowing us to explore the possibility of their association with risk of death. Ultimately, this is the first set of Brazilian data in this field, ever.

Some important limitations are also worth mentioning in this study. As a single-center cohort in a country of continental proportions, such as Brazil, a selection bias may well exist, hindering an external validity. The missing data rate for some variables was considerably high due to the retrospective design of the study. There was no paired sample with non-cancer patients with COVID-19 or cancer patients without COVID-19 to provide a better comparison between the outcomes of morbidity and mortality. Due to the in-hospital follow-up only, there was no report of long-term morbidity. Finally, the general population of the study was very heterogeneous with several types of neoplasia and anti-cancer treatment, making it difficult to design a more reliable portrait by tumor site.

Conclusions

Like other comorbidities, cancer is suggested to be an important prognostic factor for patients with COVID-19, probably due to the greater clinical fragility and the negative impact of immunosuppressive treatments. Despite having formulated early institutional emergency measures, since the onset of the pandemic in Brazil, to reduce the exposure of this group of patients to SARS-CoV-2, INCA had a considerable burden of infected patients in need of hospitalization. The rates of complications and COVID-19-specific death were significantly high.

Supporting information

Acknowledgments

The authors thank all INCA health workers for taking care of cancer patients with COVID-19, especially the members of INCA COVID-19 Task Force: Luiza M. Abdo^, Maria Theresa Accioly, Lucas R. Almendra, Rodrigo O.C. Araujo, Elisa Bouret C. Barroso, Marcelo A. Bello, Anke Bergmann, Ricardo S. Bigni, Franz S. Campos, Pedro S. Carvalho, Samuel Z.B. Cordeiro, Susanne Crocamo, Carolina S. Dantas, Roberto R.M. de Araujo Lima, Erico L. Ferreira, Renata de Freitas, Fernando L. Dias, Jorge L.A. Dias, Michelle M.Q. dos Santos, André F. Duarte, Sima E. Ferman, Vanessa C. Fernandes, Priscila S. Ferreira, Kelly M. Fireman, Livia R. Goes, Renan G. Gomes Junior, Bruno A.A. Gonçalves, Juliana G. Gonçalves, Gustavo H.C. Guimarães, Nelson J. Jabour Fiod, Ana Cristina M. Leão, Décio Lerner, Valdirene S. Lima, Eduardo Linhares, Monique S.A. Lopes, Ianick S. Martins, Amanda S. Medeiros, Brunna L. Misael Alves, Paulo A. Mora, Daniela P. Oliveira, Alexandre M. Palladino, Diego J.G. Paula, Bárbara C. Peixoto, Patrícia A. Possik, Matheus A. Rajão, Fernando L.B. Rocha Gutierrez, Maria D.M. Rocha, Giovani B. Santos, Antonio A.D. Souto, Marcelo R. Schirmer, Karina L. Silva, Lilian S. Silva, Juliana D. Siqueira, Leandro S. Thiago, Fabiana Tonellotto, Gisele M. Vasconcelos, Dolival L. Veras Filho. All membership of INCA COVID-19 Task Force is affiliated to Brazilian National Cancer Institute, Rio de Janeiro, Rio de Janeiro, Brazil. ^ Lead member of the INCA COVID-19 Task Force.