Literature DB >> 35851312

T cell responses against SARS-CoV-2 and its Omicron variant in a patient with B cell lymphoma after multiple doses of a COVID-19 mRNA vaccine.

Djordje Atanackovic1,2,3, Robert J Kreitman4, Jeffrey Cohen5, Nancy M Hardy6,2, Destiny Omili6,2, Thierry Iraguha6,2, Peter D Burbelo7, Etse Gebru6,2, Xiaoxuan Fan2, John Baddley2,8, Tim Luetkens2,3, Saurabh Dahiya6,2, Aaron P Rapoport6,2.   

Abstract

Anti-SARS-CoV-2 antibodies are crucial for protection from future COVID-19 infections, limiting disease severity, and control of viral transmission. While patients with the most common type of hematologic malignancy, B cell lymphoma, often develop insufficient antibody responses to messenger RNA (mRNA) vaccines, vaccine-induced T cells would have the potential to 'rescue' protective immunity in patients with B cell lymphoma. Here we report the case of a patient with B cell lymphoma with profound B cell depletion after initial chemoimmunotherapy who received a total of six doses of a COVID-19 mRNA vaccine. The patient developed vaccine-induced anti-SARS-CoV-2 antibodies only after the fifth and sixth doses of the vaccine once his B cells had started to recover. Remarkably, even in the context of severe treatment-induced suppression of the humoral immune system, the patient was able to mount virus-specific CD4+ and CD8+ responses that were much stronger than what would be expected in healthy subjects after two to three doses of a COVID-19 mRNA vaccine and which were even able to target the Omicron 'immune escape' variant of the SARS-CoV-2 virus. These findings not only have important implications for anti-COVID-19 vaccination strategies but also for future antitumor vaccines in patients with cancer with profound treatment-induced immunosuppression. © Author(s) (or their employer(s)) 2022. Re-use permitted under CC BY-NC. No commercial re-use. See rights and permissions. Published by BMJ.

Entities:  

Keywords:  COVID-19; Hematologic Neoplasms; IMMUNOLOGY; T-Lymphocytes; Vaccination

Mesh:

Substances:

Year:  2022        PMID: 35851312      PMCID: PMC9295666          DOI: 10.1136/jitc-2022-004953

Source DB:  PubMed          Journal:  J Immunother Cancer        ISSN: 2051-1426            Impact factor:   12.469


COVID-19 is caused by SARS-CoV-2, which contains the spike (S) and nucleocapsid (N) proteins.1 2 The S protein has S1 and S2 domains and the virus uses the receptor-binding domain (RBD) within S1 to bind to ACE-2 receptor3 and enter normal cells such as the pneumocytes in the lungs.1 4 Unfortunately, patients with hematologic malignancies and COVID-19 show dramatically increased mortality rate,5 6 which correlates with the intensity of prior antilymphoma treatments.5–7 Disease-induced or vaccine-induced anti-SARS-CoV-2 antibodies are crucial for protection from future COVID-19 infections, limiting disease severity, and control of viral transmission.8 9 Unfortunately, patients with the most common type of hematologic malignancy, namely B cell lymphoma, often develop insufficient antibody responses to messenger RNA (mRNA) vaccines due to the immunosuppression caused by their anti-B cell treatments.10 In addition to antibody responses, antiviral T cells have been shown to improve survival in patients with COVID-19,11 including patients with hematologic cancers,12 and vaccine-induced T cells have the potential to ‘rescue’ protective immunity in patients with B cell lymphoma. However, it is not entirely clear whether patients with B cell lymphoma are capable of mounting a vaccine-induced T cell response in the framework of treatment-induced immunosuppression and whether such T cells would be able to recognize and target immune escape variants such as Omicron. In this study we performed a comprehensive monitoring of anti-SARS-CoV-2 antibody and T cell immunity in a patient with B cell lymphoma with profound immunosuppression receiving multiple doses of a COVID-19 mRNA vaccine (For methods used please see online supplemental methods and online supplemental tables 1–3). The patient is a man in his early 70s with diffuse large B cell lymphoma involving the left cervical chain (stage 1) who received four cycles of R-CHOP (rituximab/cyclophosphamide/doxorubicin/vincristine/prednisone) followed by two cycles of rituximab alone. He achieved complete remission which was sustained. While the patient was under treatment with the final two doses of rituximab (figure 1A and online supplemental figure 1), he simultaneously received the first two doses of the BNT162b2 COVID-19 mRNA vaccine (online supplemental figure 1). At that time, he did not have any B cells in his peripheral blood (figure 1A), and accordingly he did not develop antibodies against the S protein of SARS-CoV-2 (figure 1A). Two more doses of the same vaccine did not lead to the development of endogenous antiviral antibodies, and as a consequence he received Regeneron’s antibody cocktail REGN-COV2 off-label as an alternative prophylactic measure (figure 1A). Shortly thereafter, anti-S1 antibodies became detectable, presumably due to the exogenous antibodies persisting in his blood (figure 1A). In October 2021 the patient’s B cell counts finally started to recover from anti-CD20 treatment (figure 1A). Off-label he received a fifth dose of the COVID-19 vaccine, with normal B cells detectable but still low, which led to a stabilization of total anti-S antibody levels (figure 1A) without any additional doses of the REGN-COV2 antibody cocktail, presumably representing early signs of an initial endogenous humoral immune response to the fifth dose of the vaccine. A sixth dose of the same mRNA COVID-19 vaccine given after normalization of B cell numbers led to a substantial increase in anti-S1 antibody levels. We performed a comprehensive analysis of vaccine-induced T cell and B cell responses between administration of the fifth and sixth doses of the vaccine (figure 1A).
Figure 1

Time course of immune parameters including anti-SARS-CoV-2 antibodies in a patient with lymphoma receiving multiple COVID-19 vaccinations. (A) Absolute numbers of peripheral blood B cells and levels of antibodies directed against SARS-CoV proteins S1 and N after one dose of Regeneron’s antibody cocktail REGN-COV2 and multiple doses of the BNT162b2 COVID-19 vaccine, respectively. (B) Absolute serum concentrations of IgG, IgA, and IgM immunoglobulins over time. (C) Absolute white blood cell count (WBC), absolute lymphocyte count (ALC), and number of peripheral blood CD4+ T cells over time. The dotted line indicates the timepoint when comprehensive immunomonitoring was performed.

Time course of immune parameters including anti-SARS-CoV-2 antibodies in a patient with lymphoma receiving multiple COVID-19 vaccinations. (A) Absolute numbers of peripheral blood B cells and levels of antibodies directed against SARS-CoV proteins S1 and N after one dose of Regeneron’s antibody cocktail REGN-COV2 and multiple doses of the BNT162b2 COVID-19 vaccine, respectively. (B) Absolute serum concentrations of IgG, IgA, and IgM immunoglobulins over time. (C) Absolute white blood cell count (WBC), absolute lymphocyte count (ALC), and number of peripheral blood CD4+ T cells over time. The dotted line indicates the timepoint when comprehensive immunomonitoring was performed. When we asked whether the lack of a vaccine-induced anti-SARS-CoV-2 antibody response to the first four doses was due to an unspecific and global treatment-induced and/or disease-induced immunosuppression, we found that the patient indeed showed lower levels of total IgG, IgM, and IgA immunoglobulins compared with a group of healthy controls (online supplemental figure 2A). However, there was no decline in immunoglobulins over time (figure 1B), and even more importantly the patient with B cell-depleted lymphoma maintained normal levels of IgG antibodies against recall antigens such as influenza A, tetanus toxoid, and Epstein-Barr virus even after six cycles of anti-B cell lymphoma treatment (online supplemental figure 2B). Taking a closer look at the anti-SARS-CoV-2 immunity our patient had developed after five doses of the vaccine, we detected, in agreement with the routine laboratory assay (figure 1A), IgG antibodies directed against the S1, RBD (online supplemental figure 2C), and S2 proteins, with no detectable anti-N antibodies (online supplemental figure 2E). The antibody titers were lower compared with those of seven healthy controls at 4 weeks after the second dose of a COVID-19 mRNA vaccine (online supplemental figure 2C); however, they still led to an almost 100% antiviral neutralizing activity (online supplemental figure 2D). Consistent with our longitudinal analyses of peripheral B cell numbers in this patient who initially showed therapy-induced B cell depletion (figure 1A), we were able to detect a significant number of CD19+/CD20+ B cells (online supplemental figure 2F), including CD19+ B cells secreting IgG antibodies against the S protein (online supplemental figure 2G), after five doses of the vaccine. Unfortunately, the comparably low antibody titers in our patient were further reduced when binding to the Omicron variant instead of the ancestral S1 and RBD proteins (online supplemental figure 2C). The reduced binding resulted in a dramatically diminished anti-Omicron neutralizing activity of the polyclonal antibodies (online supplemental figure 2D). We next asked whether our patient evidenced anti-SARS-CoV-2 T cells despite an only very slowly developing humoral antiviral immune component, which was still suboptimal after the fifth dose of the vaccine. We found that the patient actually showed vaccine-induced CD4+ and CD8+ T cell responses in their blood targeting the S protein of the SARS-CoV-2 virus that were much stronger than what we had observed in a group of healthy individuals who had received two doses of the mRNA vaccine (figure 2). Unfortunately, we were not able to measure T cell responses in our patient after only two doses of the vaccine; however, after five doses, the number of SARS-CoV-2-specific CD8+ T cells was almost 100 times higher than what we had observed in healthy vaccinated individuals after the two initial doses (figure 2). For both CD4+ and CD8+ T cells targeting the S protein, most of the immunodominant epitopes of the anti-SARS-CoV-2 CD4+ T cells were within the S1 component of the fusion protein (figure 2).
Figure 2

Vaccine-induced SARS-CoV-2-specific T cells in a patient with B cell lymphoma after multiple doses of a COVID-19 mRNA vaccine. After the patient had received five doses of the COVID-19 mRNA vaccine, T cells specific for the S protein of the SARS-CoV-2 were identified ex vivo after short-term stimulation of the total peripheral blood mononuclear cells (PBMC) using libraries of overlapping peptides covering the complete sequence of the protein. Intracellular staining of cytokines followed by flow cytometry served as the read-out assay. SARS-CoV-2-specific CD4+ T cells (upper panel) were defined as tumor necrosis factor (TNF) α/CD40L (CD154) double-positive CD3+CD4+ T cells, and SARS-CoV-2-specific CD8+ T cells (lower panel) were defined as interferon (IFN) γ/TNFα double-positive CD3+CD8+ T cells. The number of vaccine-induced CD4+ and CD8+ T cells specific for the complete sequence of the S fusion protein was compared with the number of T cells from the same individual recognizing the N-terminal S1 protein or the N-terminal portion (amino acids 689–895) of the S2 protein (‘S+’). Background levels were typically <0.01% of all CD4+ or CD8+ T cells. Plots on the right show the patient’s S-specific CD4+ and CD8+ T cells (red dot) in relation to the median number (dotted line) of the same T cells from a group of six healthy control subjects, where the results were available from 4 weeks after the second dose of a COVID-19 mRNA vaccine. mRNA, messenger RNA.

Vaccine-induced SARS-CoV-2-specific T cells in a patient with B cell lymphoma after multiple doses of a COVID-19 mRNA vaccine. After the patient had received five doses of the COVID-19 mRNA vaccine, T cells specific for the S protein of the SARS-CoV-2 were identified ex vivo after short-term stimulation of the total peripheral blood mononuclear cells (PBMC) using libraries of overlapping peptides covering the complete sequence of the protein. Intracellular staining of cytokines followed by flow cytometry served as the read-out assay. SARS-CoV-2-specific CD4+ T cells (upper panel) were defined as tumor necrosis factor (TNF) α/CD40L (CD154) double-positive CD3+CD4+ T cells, and SARS-CoV-2-specific CD8+ T cells (lower panel) were defined as interferon (IFN) γ/TNFα double-positive CD3+CD8+ T cells. The number of vaccine-induced CD4+ and CD8+ T cells specific for the complete sequence of the S fusion protein was compared with the number of T cells from the same individual recognizing the N-terminal S1 protein or the N-terminal portion (amino acids 689–895) of the S2 protein (‘S+’). Background levels were typically <0.01% of all CD4+ or CD8+ T cells. Plots on the right show the patient’s S-specific CD4+ and CD8+ T cells (red dot) in relation to the median number (dotted line) of the same T cells from a group of six healthy control subjects, where the results were available from 4 weeks after the second dose of a COVID-19 mRNA vaccine. mRNA, messenger RNA. It has previously been shown that SARS-CoV-2 vaccination is capable of inducing T cells with the potential to cross-recognize the Omicron variant13 14; however, to the best of our knowledge, the same phenomenon has not been demonstrated in patients with B cell lymphoma. When we examined cross-recognition by our patient’s T cells, we found that, while there was a certain decrease in T cell reactivity when exposed to the Omicron variant of the S protein, most of the patient’s polyclonal vaccine-induced CD4+ and CD8+ T cells also recognized this immune escape variant of the ancestral SARS-CoV-2 virus (online supplemental figure 3). While this certainly cannot serve as evidence of a protective function of the vaccine-induced T cells, it has indeed previously been shown that postinfection and vaccine-induced anti-SARS-CoV-2 T cells can play a protective role,12 15–17 and our patient never developed COVID-19 despite multiple known close exposures to family members with a proven infection. We have shown here that a patient with B cell lymphoma whose B cells were initially depleted following antilymphoma chemoimmunotherapy was not able to mount an antibody response to four doses of a COVID-19 mRNA vaccine. The patient only developed vaccine-induced anti-SARS-CoV-2 antibodies once his B cells had started to recover. Importantly, even in the context of severe treatment-induced suppression of the humoral immune system, the patient was able to mount SARS-CoV-2-specific CD4+ and CD8+ responses that were much stronger than what would be expected in healthy subjects after two to three rounds of a COVID-19 mRNA vaccine and which were even able to target the Omicron ‘immune escape’ variant18 of the virus. These findings not only have important implications for anti-COVID-19 vaccination strategies but also for future antitumor vaccines in patients with cancer with profound treatment-induced immunosuppression.
  18 in total

1.  SARS-CoV-2-specific T cell responses and correlations with COVID-19 patient predisposition.

Authors:  Arne Sattler; Stefan Angermair; Helena Stockmann; Katrin Moira Heim; Dmytro Khadzhynov; Sascha Treskatsch; Fabian Halleck; Martin E Kreis; Katja Kotsch
Journal:  J Clin Invest       Date:  2020-12-01       Impact factor: 14.808

2.  Delayed production of neutralizing antibodies correlates with fatal COVID-19.

Authors:  Carolina Lucas; Jon Klein; Maria E Sundaram; Feimei Liu; Patrick Wong; Julio Silva; Tianyang Mao; Ji Eun Oh; Subhasis Mohanty; Jiefang Huang; Maria Tokuyama; Peiwen Lu; Arvind Venkataraman; Annsea Park; Benjamin Israelow; Chantal B F Vogels; M Catherine Muenker; C-Hong Chang; Arnau Casanovas-Massana; Adam J Moore; Joseph Zell; John B Fournier; Anne L Wyllie; Melissa Campbell; Alfred I Lee; Hyung J Chun; Nathan D Grubaugh; Wade L Schulz; Shelli Farhadian; Charles Dela Cruz; Aaron M Ring; Albert C Shaw; Adam V Wisnewski; Inci Yildirim; Albert I Ko; Saad B Omer; Akiko Iwasaki
Journal:  Nat Med       Date:  2021-05-05       Impact factor: 53.440

3.  CD8+ T cells contribute to survival in patients with COVID-19 and hematologic cancer.

Authors:  Erin M Bange; Nicholas A Han; Paul Wileyto; Justin Y Kim; Sigrid Gouma; James Robinson; Allison R Greenplate; Madeline A Hwee; Florence Porterfield; Olutosin Owoyemi; Karan Naik; Cathy Zheng; Michael Galantino; Ariel R Weisman; Caroline A G Ittner; Emily M Kugler; Amy E Baxter; Olutwatosin Oniyide; Roseline S Agyekum; Thomas G Dunn; Tiffanie K Jones; Heather M Giannini; Madison E Weirick; Christopher M McAllister; N Esther Babady; Anita Kumar; Adam J Widman; Susan DeWolf; Sawsan R Boutemine; Charlotte Roberts; Krista R Budzik; Susan Tollett; Carla Wright; Tara Perloff; Lova Sun; Divij Mathew; Josephine R Giles; Derek A Oldridge; Jennifer E Wu; Cécile Alanio; Sharon Adamski; Alfred L Garfall; Laura A Vella; Samuel J Kerr; Justine V Cohen; Randall A Oyer; Ryan Massa; Ivan P Maillard; Kara N Maxwell; John P Reilly; Peter G Maslak; Robert H Vonderheide; Jedd D Wolchok; Scott E Hensley; E John Wherry; Nuala J Meyer; Angela M DeMichele; Santosha A Vardhana; Ronac Mamtani; Alexander C Huang
Journal:  Nat Med       Date:  2021-05-20       Impact factor: 87.241

4.  Isolation and characterization of a bat SARS-like coronavirus that uses the ACE2 receptor.

Authors:  Xing-Yi Ge; Jia-Lu Li; Xing-Lou Yang; Aleksei A Chmura; Guangjian Zhu; Jonathan H Epstein; Jonna K Mazet; Ben Hu; Wei Zhang; Cheng Peng; Yu-Ji Zhang; Chu-Ming Luo; Bing Tan; Ning Wang; Yan Zhu; Gary Crameri; Shu-Yi Zhang; Lin-Fa Wang; Peter Daszak; Zheng-Li Shi
Journal:  Nature       Date:  2013-10-30       Impact factor: 49.962

5.  A pneumonia outbreak associated with a new coronavirus of probable bat origin.

Authors:  Peng Zhou; Xing-Lou Yang; Xian-Guang Wang; Ben Hu; Lei Zhang; Wei Zhang; Hao-Rui Si; Yan Zhu; Bei Li; Chao-Lin Huang; Hui-Dong Chen; Jing Chen; Yun Luo; Hua Guo; Ren-Di Jiang; Mei-Qin Liu; Ying Chen; Xu-Rui Shen; Xi Wang; Xiao-Shuang Zheng; Kai Zhao; Quan-Jiao Chen; Fei Deng; Lin-Lin Liu; Bing Yan; Fa-Xian Zhan; Yan-Yi Wang; Geng-Fu Xiao; Zheng-Li Shi
Journal:  Nature       Date:  2020-02-03       Impact factor: 69.504

6.  COVID-19 and CAR T cells: a report on current challenges and future directions from the EPICOVIDEHA survey by EHA-IDWP.

Authors:  Alessandro Busca; Jon Salmanton-García; Paolo Corradini; Francesco Marchesi; Alba Cabirta; Roberta Di Blasi; Remy Dulery; Sylvain Lamure; Francesca Farina; Barbora Weinbergerová; Josip Batinić; Anna Nordlander; Alberto López-García; Ľuboš Drgoňa; Ildefonso Espigado-Tocino; Iker Falces-Romero; Ramón García-Sanz; Carolina García-Vidal; Anna Guidetti; Nina Khanna; Austin Kulasekararaj; Johan Maertens; Martin Hoenigl; Nikolai Klimko; Philipp Koehler; Antonio Pagliuca; Francesco Passamonti; Oliver A Cornely; Livio Pagano
Journal:  Blood Adv       Date:  2022-04-12

7.  Characterization of spike glycoprotein of SARS-CoV-2 on virus entry and its immune cross-reactivity with SARS-CoV.

Authors:  Xiuyuan Ou; Yan Liu; Xiaobo Lei; Pei Li; Dan Mi; Lili Ren; Li Guo; Ruixuan Guo; Ting Chen; Jiaxin Hu; Zichun Xiang; Zhixia Mu; Xing Chen; Jieyong Chen; Keping Hu; Qi Jin; Jianwei Wang; Zhaohui Qian
Journal:  Nat Commun       Date:  2020-03-27       Impact factor: 14.919

8.  COVID-19 prevalence and mortality in patients with cancer and the effect of primary tumour subtype and patient demographics: a prospective cohort study.

Authors:  Lennard Y W Lee; Jean-Baptiste Cazier; Thomas Starkey; Sarah E W Briggs; Roland Arnold; Vartika Bisht; Stephen Booth; Naomi A Campton; Vinton W T Cheng; Graham Collins; Helen M Curley; Philip Earwaker; Matthew W Fittall; Spyridon Gennatas; Anshita Goel; Simon Hartley; Daniel J Hughes; David Kerr; Alvin J X Lee; Rebecca J Lee; Siow Ming Lee; Hayley Mckenzie; Chris P Middleton; Nirupa Murugaesu; Tom Newsom-Davis; Anna C Olsson-Brown; Claire Palles; Thomas Powles; Emily A Protheroe; Karin Purshouse; Archana Sharma-Oates; Shivan Sivakumar; Ashley J Smith; Oliver Topping; Chris D Turnbull; Csilla Várnai; Adam D M Briggs; Gary Middleton; Rachel Kerr
Journal:  Lancet Oncol       Date:  2020-08-24       Impact factor: 41.316

9.  Outcomes of patients with hematologic malignancies and COVID-19: a systematic review and meta-analysis of 3377 patients.

Authors:  Abi Vijenthira; Inna Y Gong; Thomas A Fox; Stephen Booth; Gordon Cook; Bruno Fattizzo; Fernando Martín-Moro; Jerome Razanamahery; John C Riches; Jeff Zwicker; Rushad Patell; Marie Christiane Vekemans; Lydia Scarfò; Thomas Chatzikonstantinou; Halil Yildiz; Raphaël Lattenist; Ioannis Mantzaris; William A Wood; Lisa K Hicks
Journal:  Blood       Date:  2020-12-17       Impact factor: 22.113

10.  Vaccines elicit highly conserved cellular immunity to SARS-CoV-2 Omicron.

Authors:  Jinyan Liu; Abishek Chandrashekar; Daniel Sellers; Julia Barrett; Catherine Jacob-Dolan; Michelle Lifton; Katherine McMahan; Michaela Sciacca; Haley VanWyk; Cindy Wu; Jingyou Yu; Ai-Ris Y Collier; Dan H Barouch
Journal:  Nature       Date:  2022-01-31       Impact factor: 49.962
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