| Literature DB >> 35544585 |
Petra Langerbeins1, Michael Hallek1.
Abstract
The coronavirus infectious disease (COVID-19) shows a remarkable symptomatic heterogeneity. Several risk factors including advanced age, previous illnesses, and a compromised immune system contribute to an unfavorable outcome. In patients with hematologic malignancy, the immune response to severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2) is significantly reduced explaining why the mortality rate of hematologic patients hospitalized for a SARS-CoV-2 infection is about 34%. Active immunization is an essential pillar to prevent SARS-CoV-2 infections in patients with hematologic malignancy. However, the immune response to SARS-CoV-2 vaccines may be significantly impaired, as only half of patients with hematologic malignancy develop a measurable antiviral antibody response. The subtype of hematologic malignancy and B cell-depleting treatment predict a poor immune response to vaccination. Recently, antiviral drugs and monoclonal antibodies for pre-exposure or postexposure prophylaxis and for early treatment of COVID-19 have become available. These therapies should be offered to patients at high risk for severe COVID-19 and vaccine nonresponders. Importantly, as the virus evolves, some therapies may lose their clinical efficacy against new variants. Therefore, the ongoing pandemic will remain a major challenge for patients with hematologic malignancy and their caregivers who need to constantly monitor the scientific progress in this area.Entities:
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Year: 2022 PMID: 35544585 PMCID: PMC9098396 DOI: 10.1182/blood.2021012251
Source DB: PubMed Journal: Blood ISSN: 0006-4971 Impact factor: 25.476
COVID-19 in patients with hematologic malignancy: summary of studies of COVID-19 in >50 patients with hematologic malignancy
| Reference | Investigator | Patient population | Study design | Clinical severity (%) | Mortality (%) | Risk factors for severe COVID-19 |
|---|---|---|---|---|---|---|
| NCATS' National COVID Cohort Collaborative | 63 413 cancer patients with COVID-19 | Retrospective cohort | • Age ≥ 65 | |||
| European Haematology Association Survey (EPICOVIDEHA) | 3 801 patients with HM with COVID-19 | Survey | Hospitalization (73.1) | HM patients died (31.2) | • Age | |
| COVID-19 and Cancer Consortium Registry (CCC19) | 4 966 cancer patients with COVID-19 (10.5% patients with HM) | Registry | Hospitalization (57.8) | Cancer patients died (14) | • Older age | |
| Republic of Turkey, Ministry of Health database | 740 patients with HM with COVID-19 | Retrospective cohort | Hospital admission (61.1), ICU admission (18.9), Mechanical ventilation (13.8) | HM patients died (13.7) | ||
| Italian Hematology Alliance on COVID-19 | 536 patients with HM with COVID-19 | Retrospective cohort | HM patients died (36.9%) | • Older age | ||
| Argentine Society of Hematology | 419 patients with HM with COVID-19 | Survey | Hospital admission (64.9), ICU (24.1) | HM patients died (20.7) | • Comorbidities | |
| Republic of Turkey, Ministry of Health database | 497 patients with HM with COVID-19 | Retrospective cohort | Mechanical ventilation (16.7) | HM patients died (12.1) | ||
| European Society for Blood and Marrow Transplantation (EBMT) and the Spanish Group of Hematopoietic Stem Cell Transplantation (GETH) | 382 SCT recipients with COVID-19 | Prospective survey | SCT recipients died (28) | • Older age | ||
| Spanish transplant group and cell therapy (GETH) | 367 patients with HM with COVID-19 | Retrospective cohort | • Hospitalization (56.4) | HM patients died 28.6% (105) | • Age > 70 y | |
| Turkish Society of Hematology, Infectious Complications and Supportive Care Working Party | 340 patients with HM with COVID-19 | Retrospective cohort | Hospitalization (73.8) | HM patients died (26.5) | • Disease status | |
| NHS England | 10 926 COVID-related deaths | Analytic platform OpenSAFELY | HM patients died (3.1) | • Male | ||
| SEMI-COVID-19 Registry in Spain | 2 111 immunosuppressed patients with COVID-19 | Retrospective cohort | HM patients died (41.9) | |||
| National Israeli Study | 313 patients with HM with COVID-19 | Retrospective cohort | Hospitalization (56.9) | HM patients died (19.1) | • Severe COVID-19 | |
| Center for International Blood and Marrow Transplant Research (CIBMTR) | 318 SCT recipients with COVID-19 | Retrospective cohort | Mechanical ventilation (14.2) | SCT recipients died (20.8) | Allogeneic cohort: | |
| Tertiary level medical institute in North India | 242 patients with HM with COVID-19 | Retrospective cohort of electronic database system | Mechanical ventilation (21.1) | HM patients died (19.8) | • Severity of COVID-19 | |
| UK Coronavirus Cancer Monitoring Project (UKCCMP) | 1 044 cancer patients with COVID-19 | Prospective cohort | Cancer patients died (30.6) | • Age | ||
| Electronic health record data collected by the IBM Watson Health Explorys from 360 US hospitals | 306 640 patients with HM | Retrospective case-control of electronic records | • Leukemia | |||
| Cancer centers in France | 425 cancer patients with COVID-19 | Observational prospective | Cancer patients died (27.9) | • Male sex | ||
| 11 centers across India | 130 HM with COVID-19 | Retrospective cohort | Oxygen support (51.5), | HM patients died (20) | • Age ≥ 60 | |
| Italian north-eastern Veneto Region | 1 090 cancer patients with COVID-19 | Retrospective population-based study | • Prevalent-active disease | |||
| Guy's Cancer Centre and King's College Hospital in London | 306 cancer patients | Retrospective cohort | HM patients died (31.6) | • Male sex | ||
| 2 hematologic departments located in Lombardy, Italy | 102 HM with COVID-19 | HM patients died (39.2) | • Active hematologic treatment | |||
| single hematology center in the Czech Republic | 96 HM with COVID-19 | HM patients died (15.6) | • Age ≥ 60 | |||
| King's College Hospital | 80 HM with COVID-19 | Retrospective cohort | HM patients died (35) | |||
| Republic of Turkey, Ministry of Health database | 77 HM with COVID-19 | Retrospective cohort | Mechanical ventilation (20.8) | HM patients died (20.8) | ||
| Memorial Sloan-Kettering Cancer Center | 309 cancer patients with COVID-19 | Hospital admission (47.6) | Cancer patients died (10) | • Active hematologic or lung malignancy | ||
| London North West University Healthcare NHS Trust | 69 patients with HM with COVID-19 | Retrospective cohort | HM patients died (31.9) | |||
| Memorial Sloan-Kettering Cancer Center | 77 cellular therapy recipients with COVID-19 | Retrospective cohort | Cellular therapy recipients died (36.4) | |||
| Regional network of 7 hospitals | 66 HM with COVID-19 | Retrospective cohort | HM patients died (51.5) | |||
| Danish hematology departments | 66 HM with COVID-19 | ICU (21.2) | HM patients died (24.2) | • Older patients | ||
| 4 hospitals in Europe: Spain, Northern-Italy and the Netherlands | 59 HM with COVID-19 | Retrospective cohort | HM patients died (33.9) | • | ||
| Institute of Immunity and Transplantation, University College London | 55 HM with COVID-19 | Retrospective cohort | CPAP (34.5), endotracheal intubation (10.9) | HM patients died (34.5) | • CRP | |
| New York Hospital System | 218 cancer patients with COVID-19 | Retrospective cohort | Cancer patients died (28) | • Older age | ||
| NHS Hospitals in England | 179 cancer patients with COVID-19 | Retrospective cohort | Cancer patients died (36.9) | • Age | ||
| Gustave Roussy in France | 51 HM with COVID-19 | • Hypogammaglobulinemia | ||||
AML, acute myeloid leukemia; CPAP, continuous positive airway pressure; CRP, C-reactive protein; ECOG PS, Eastern Cooperative Oncology Group Performance Status; MDS, myelodysplastic syndrome; MV, mechanical ventilation; NCATS, National Center for Advancing Translational Sciences; NHL, non-Hodgkin lymphoma; NHS, National Health Service; SCT, stem cell transplantion; SEMI, Sociedad Espanola de Medicina interna; US, United States.
COVID-19 vaccines in patients with hematologic malignancy: summary of studies evaluating the efficacy of COVID-19 vaccines in >10 patients with hematologic malignancy
| Reference | Patient population | Vaccine type/ vaccine regimen | Endpoint | Results |
|---|---|---|---|---|
| 200 cancer patients | FDA-approved COVID-19 vaccines | Seroconversion | ||
| Overall | 94% | |||
| Type of vaccine | ||||
| BNT162b2 | 95% | |||
| mRNA-1273 | 94% | |||
| Ad26.COV2.S | 85% | |||
| Type of cancer therapy | ||||
| Anti-CD20 | 70% | |||
| Stem cell transplant | 73% | |||
| CAR-T cell | 0 | |||
| Hormonal | 100% | |||
| Immune checkpoint inhibitor | 97% | |||
| 80 HM patients | Double-dose BNT162b2 | Seroconversion | ||
| Type of treatment | ||||
| CAR-T cell | 36% | |||
| Allogeneic stem cell transplant | 75% | |||
| ELISpot positivity | ||||
| Type of treatment | ||||
| CAR-T cell | 50% | |||
| Allogeneic stem cell transplant | 19% | |||
| 32 HM patients | Double-dose BNT162b2 and Ad26-COV2.S boost | Seroconversion | ||
| Overall | 31% | |||
| Type of HM | ||||
| CLL or lymphoma | 16.7% | |||
| 270 HM patients | Double-dose mRNA-1273 | Seroconversion | ||
| Overall | 76.3% | |||
| Treatment status | ||||
| Off-therapy >6 mo | 91.7% | |||
| On-therapy/off-therapy <6 mo | 63.7% | |||
| Treatment-naïve | 96.7% | |||
| Type of treatment | ||||
| BTK | 86.2% | |||
| IMIDs | 100% | |||
| Anti-CD20 alone | 18.5% | |||
| CHI ±anti-CD20 | 27.8% | |||
| Cellular response | ||||
| Overall | 79% | |||
| Treatment status | ||||
| Off-therapy >6 mo | 85.7% | |||
| On-therapy/off-therapy < 6 mo | 78% | |||
| Treatment-naïve | 86.7% | |||
| Type of treatment | ||||
| BTK | 81.5% | |||
| IMIDs | 92.3% | |||
| Anti-CD20 alone | 80% | |||
| CHI ±anti-CD20 | 50% | |||
| 49 HM patients | Booster BNT162b2 or mRNA-1273 | Seroconversion | ||
| Overall | 65% | |||
| Treatment status | ||||
| Off-treatment >24 mo | 92.9% | |||
| Completed anti-CD20 | 42.9% | |||
| Prior anti-CD20 <7 mo | 71.4% | |||
| BTK | 61.1% | |||
| 100 HM patients | Double-dose BNT162b2 or mRNA-1273 | Seroconversion | ||
| Overall | 49% | |||
| Treatment status | ||||
| Anti-CD20 <12 mo prior | 26% | |||
| After booster dose | 41.7% | |||
| 160 HM patients | FDA-approved COVID-19 vaccines | Seroconversion Overall | 39.4% | |
| Treatment status | ||||
| B-cell/plasma cell-depleting mAb | 29% | |||
| Active disease | 27% | |||
| In remission | 49% | |||
| Watch & wait | 67% | |||
| CHI >12 mo prior | 69% | |||
| CHI < 12 mo prior | 24% | |||
| 239 HM patients | Double-dose BNT162b2 | Seroconversion | ||
| Overall | 47% | |||
| Cellular response | Cellular response | |||
| Overall | 53% | |||
| 123 HM patients | BNT162b2 | Seroconversion | ||
| 1 dose | 43.4% | |||
| Double-dose | 71.4% | |||
| 58 HM patients | Single dose BNT162b2 or AZD1222 | Neutralizing antibodies | ||
| ≥30% | 14% | |||
| ≥50% | 5% | |||
| 102 HM patients | Single dose BNT162b2 or mRNA-1273 | Seroconversion | ||
| Overall | 61.8% | |||
| Treatment | ||||
| Anti-CD20 <12 mo | 5.9% | |||
| Anti-CD20 >12 mo | 63.6% | |||
| 857 HM patients | Single-dose and double-dose BNT162b2 | Median anti-S IgG level (AU/mL) | ||
| Overall | 6 961 | |||
| Age | ||||
| >60 y | 1 140 | |||
| Treatment | ||||
| Treatment-naïve | 5 761 | |||
| Ruxolitinib | 10 | |||
| BTKi | 0 | |||
| Anti-CD20 | 17 | |||
| Hydroxycarbamide | 1 825 | |||
| IMID | 679 | |||
| TKIs | 10 537 | |||
| Anagrelide/interferon | 6 927 | |||
| Auto SCT | 6 203 | |||
| Allogeneic SCT | 6 304 | |||
| 315 HM patients | Double-dose BNT162b2 | Seroconversion | ||
| Overall | 75% | |||
| HM subtype | ||||
| Aggressive NHL | 71% | |||
| Indolent NHL | 60% | |||
| Hodgkin lymphoma | 94% | |||
| Multiple myeloma | 76% | |||
| CLL | 47% | |||
| Acute leukemia | 80% | |||
| MDS | 94% | |||
| MPN | 84% | |||
| CML | 91% | |||
| 1 445 HM patients | Double-dose BNT162b2 or mRNA-1273 | Seroconversion | ||
| Overall | 75% | |||
| HM subtype | ||||
| ALL | 88.2% | |||
| AML | 91.2% | |||
| Burkitt lymphoma | 100% | |||
| CLL | 64.2% | |||
| CML | 97.1% | |||
| Diffuse large B cell lymphoma | 78.8% | |||
| Follicular lymphoma | 77.6% | |||
| Hairy cell leukemia | 100% | |||
| Hodgkin lymphoma | 98.5% | |||
| Mantle cell lymphoma | 44.4% | |||
| Marginal zone lymphoma | 61.8% | |||
| MDS/MPN | 97.1% | |||
| Multiple myeloma | 95.1% | |||
| Primary CNS lymphoma | 50% | |||
| Primary mediastinal large B-NHL | 100% | |||
| Smoldering myeloma | 100% | |||
| T cell lymphoma | 84.6% | |||
| Waldenstrom macroglobulinemia | 74.2% | |||
| 585 cancer patients | Double-dose BNT162b2 or AZD1222 | Seroconversion | ||
| Overall | 78% | |||
| Cancer subtype | ||||
| HM | 59% | |||
| Solid cancer | 85% | |||
| 132 HM patients | BNT162b2 | Neutralizing SARS-CoV-2 antibodies inhibition titer | ||
| Median | 32.5% | |||
| ≥30% | 50.8% | |||
| ≥50% | 43.9% | |||
AML, acute myeloid leukemia; CAR-T, chimeric antigen receptor; CHI, chemoimmunotherapy; CLL, chronic lymphocytic leukemia; CML, chronic myeloid leukemia; ELISpot, enzyme-linked immunospot; IMIDs, immunomodulatory imide drugs; MDS, myelodysplastic syndrome; MPN, myeloproliferative disease; NHL, non-Hodgkin lymphoma; SCT, stem cell transplantion; TKI, tyrosine kinase inhibitor.
Figure 1Management of a patient with hematologic malignancy during the pandemic.