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Patients with hematologic malignancies (HMs) may have intensified immune dysregulation resulting from both therapeutic agents and malignancy burden. As a result, these patients are at increased risk for COVID-19 infection complications and mortality.
Much work has been done to explore the effect of COVID-19 on HMs since the beginning of the pandemic, including assessment of patient outcomes and stratification of subgroups by mortality risk. One example is the EPICOVIDEHA platform, which is a collaborative project including all hematology department members of the European Hematology Association who recorded the incidence and outcomes of patients with HMs infected with COVID-19. At the European Hematology Association (EHA)2021 Virtual Congress, Livio Pagano of Università Cattolica del Sacro Cuore presented key results from this platform, summarized below.1
The EPICOVIDEHA survey is a multicenter, retrospective project which began in February 2020 and is ongoing. The first phase, summarized here, focused on assessing outcomes in patients with HMs infected with COVID-19. The second stage will analyze further sub-groups identified by steering committee members who are experts in HMs.2
The main information assessed in the EPICOVIDEHA survey is described in Table 1.
Table 1. Information assessed in EPICOVIDEHA survey*
Category |
Subcategory |
---|---|
Identification |
Institution, city, country, inclusion in other registries, already published |
Demographics |
Sex, age, date of birth, ethnic origin, date of COVID-19 diagnosis, strain of SARS-CoV-2, previous vaccination, and site of state during the COVID-19 |
Underlying diseases |
Chronic cardiopathy (atrial fibrillation, hypertension, obstructive arteriopathy, etc.), chronic pulmonary disease (asthma, COPD, cystic fibrosis, fibrosis, etc.), diabetes (treated with insulin or antidiabetic oral drugs), liver disease, obesity (BMI >30) or underweight (BMI <18.5), renal impairment (creatinine >2 mg/dl), smoking history, other risk factors, no risk factor identified, absolute leukocyte, neutrophil, and lymphocyte number |
Hematologic malignancy |
Type of malignancy, details on the diagnosis, state of the malignancy at COVID-19 diagnosis day, time span between malignancy and COVID-19 diagnosis, type of treatment (chemotherapy, radiotherapy, allo-HSCT, auto-HSCT, CAR-T, others, no treatment) |
COVID-19 |
Identification method, reason for COVID-19 test, ICU stay during COVID-19 (invasive/non-invasive mechanical ventilation) |
Outcome |
Survival status at last contact, last day of follow up, date of death, overall and per ward hospital stay, reason for death |
Allo-HSCT, allogeneic HSCT; auto-HSCT, autologous HSCT; BMI, body mass index; CAR-T, chimeric antigen receptor T; COPD, chronic pulmonary obstructive disease; COVID-19, coronavirus disease 2019; HSCT, hematopoietic stem-cell transplantation; ICU, intensive care unit; SARS-CoV-2, severe acute respiratory syndrome coronavirus 2. |
Currently, over 120 institutions from 29 countries have registered >3,500 cases in EPICOVIDEHA.
Inclusion criteria:
Exclusion criteria:
The primary objective was to assess the epidemiology and outcomes of patients with HMs infected with COVID-19.
The secondary objectives were to:
Overall, 4,117 patients were enrolled and 3,801 valid cases were included for analysis.
Patient characteristics are summarized in Table 2.
Table 2. Patient characteristics*
Characteristic, % (unless otherwise stated) |
N = 3,801 |
---|---|
Median age (range), years |
65 (18–95) |
<25 |
2.6 |
26–50 |
17.5 |
51–69 |
41.1 |
≥70 |
38.8 |
Female |
41.5 |
Ethnicity, white |
86.3 |
Comorbidities |
60.7 |
Type of comorbidity (n = 2,307) |
|
Chronic cardiopathy |
30.1 |
Chronic pulmonary disease |
16.2 |
Diabetes |
16.3 |
Liver disease |
4.4 |
Obesity |
9.1 |
Renal impairment |
8.7 |
Smokers or ex-smokers |
12.5 |
*Adapted from Pagano1 |
In total, 49% of patients had pulmonary symptoms (cough, dyspnea, imaging signs etc.) while 33% had extra-pulmonary symptoms, including anosmia, fever, abdominal disturbances, and skin signs. Overall, >80% of patients were not neutropenic and >70% of patients were not lymphopenic, suggesting that these symptoms associated with HMs and their treatments had no effect on the onset of COVID-19 infection. The proportion of severe COVID cases increased as the number of pre-existing comorbidities increased (Table 3).
Table 3. Number of comorbidities and infection severity*
Number of comorbidities |
Infection severity |
||
---|---|---|---|
Asymptomatic |
Mild |
Severe |
|
0, n |
349 |
327 |
800 (54.2%) |
1, n |
209 |
200 |
696 (63%) |
2, n |
102 |
130 |
448 (65.9) |
≥3, n |
67 |
85 |
341 (69.2%) |
*Adapted from Pagano1 |
In total, >70% of patients received chemotherapy in the 3 months prior to COVID-19 infection (Table 4). There was an even distribution of patients who were in a disease state (stable disease, relapsed/refractory, or onset) compared with those who were in remission (partial or complete remission), 49% vs 47%, respectively (Table 4).
Table 4. Chemotherapy and disease status prior to COVID-19 infection*
Chemotherapy and disease status, % |
N = 3,801 |
---|---|
Chemotherapy ended >3 months before COVID-19 infection |
29 |
Chemotherapy received in the 3 months prior to COVID-19 infection |
15 |
Chemotherapy received in the month prior to COVID-19 infection |
56 |
Disease status |
|
Stable disease |
14 |
Unknown |
4 |
Relapsed/refractory |
12 |
Onset |
23 |
Partial remission |
16 |
Complete remission |
31 |
*Data from Pagano1 |
Immunochemotherapy was the most common treatment type received by participants.
Regarding transplants, 261 patients had a history of allo-HSCT, though only 173 underwent this procedure as the last therapy prior to COVID-19 infection. A total of 293 patients received auto-HSCT, though only 74 patients underwent the procedure as their last therapy prior to COVID-19 infection. When compared with the total number of patients who were transplanted in 2020, analysis showed a 2% incidence of COVID-19 infection in auto-HSCT recipients and a 6.4% incidence in auto-HSCT recipients, compared with a 4.6% incidence among patients receiving CAR T-cell infusion. The incidence of COVID-19 infection was 6.7% in haploidentical transplants, which was similar to matched sibling (7.6%) and matched unrelated donor (5.2%) transplants.
Of the patients who required hospitalization, 25% required admission to ICU following COVID-19 infection, and 65% required ventilation. The median duration of hospital stay was 15 days; however, it was highlighted that there was evaluation bias resulting from the inclusion of patients who died early.
The all-cause mortality rate was 31%, with 26% attributed to COVID-19 infection. When stratified by age, mortality rate was higher in patients >70 years old. When stratified by hematologic malignancy, patients with acute myeloid leukemia (AML) and MDS had higher mortality rates (near 40%) and patients with high-risk MDS had an even higher rate of 46%, indicating an at-risk population. The severity of COVID-19 infection was also unsurprisingly associated with mortality.
Demethylating agents were associated with the highest mortality rates from COVID-19 infection (58.8%), while palliative care (53.7%) and CAR T-cell infusion (47.6%) were also associated with significant mortality rates. The impact of all treatments on mortality are summarized in Table 5.
Table 5. The mortality rate of patients with COVID-19 infections classified by therapy regimen*
Therapy |
Total number of patients |
Mortality rate, % |
---|---|---|
Anagrelide/HU |
145 |
26.8 |
Conventional Chemotherapy |
572 |
29.8 |
Demethylating agents |
141 |
58.8 |
Immunotherapy only |
125 |
28.8 |
Immunochemotherapy |
857 |
30.6 |
IMiDs |
218 |
36.2 |
Targeted therapies |
607 |
25.3 |
Palliative |
151 |
53.7 |
Maintenance |
25 |
12.0 |
Allo-HSCT |
173 |
24.8 |
Auto-HSCT |
74 |
27.0 |
CAR-T |
21 |
47.6 |
No treatment |
538 |
29.0 |
Unknown |
41 |
31.7 |
Supportive |
75 |
26.6 |
Other |
38 |
31.5 |
Allo-HSCT; allogeneic hematopoietic stem cell transplant; Auto-HSCT; autologous hematopoietic stem cell transplant; CAR-T, chimeric antigen receptor T; HU, hydroxyurea; IMiDs, immunomodulatory drugs. |
The mortality rates in patients receiving auto-HSCT and allo-HSCT were 24.8% and 27% respectively, nearly half the rate seen in patients receiving CAR T-cell therapy. There was no difference in mortality rate in patients receiving chemotherapy or auto-HSCT. Mortality in the first wave of COVID-19 was near 40.7%, while in the second wave, despite an increase in number of cases, it was significantly lower (24%), perhaps owing to more knowledge on how to manage HMs. When looking at influences on mortality rates, using Hodgkin lymphoma as a control, factors with higher risk of mortality included AML, MDS, active disease, older age, cardiovascular disease comorbidities, and smoking.
The EPICOVIDEHA survey has provided extensive insight into the incidence and impact of COVID-19 infection on patients with HMs. AML and MDS, active disease, older age, demethylating agents, and smoking were identified as factors influencing greater risk of COVID-19 infection-related complications. The investigators also demonstrated an association of the number of baseline comorbidities with severity of infection.
Limitations of this study included that survey was created in April/May of 2020, therefore other risk factors that have been subsequently identified as important to the symptomology of COVID-19, such as the role of platelets and increased thrombotic risk, were not included in the survey. Also, data was not requested regarding treatment of COVID-19, and common denominators were unknown for HM treatment types (with the exception of HSCT procedures).
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