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Impaired T-cell and antibody immunity after COVID-19 infection in chronically immunosuppressed transplant recipients

Ashokkumar, C.; Rohan, V.; Kroemer, A. H.; Rao, S.; Mazariegos, G.; Higgs, B. W.; Nadig, S.; Almeda, J.; Dhani, H.; Khan, K.; Yazigi, N.; Ekong, U.; Kaufman, S.; Betancourt-Garcia, M. M.; Mukund, K.; Sethi, P.; Mehrotra, S.; Soltys, K.; Singh, M. S.; Bond, G.; Khanna, A.; Ningappa, M.; Spishock, B.; Sindhi, E.; Atale, N.; Saunders, M.; Baliga, P.; Fishbein, T.; Subramaniam, S.; Sindhi, R.

2021-05-04 immunology
10.1101/2021.05.03.442371 bioRxiv
Show abstract

Assessment of T-cell immunity to the COVID-19 coronavirus requires reliable assays and is of great interest, given the uncertain longevity of the antibody response. Some recent reports have used immunodominant spike (S) antigenic peptides and anti-CD28 co-stimulation in varying combinations to assess T-cell immunity to SARS-CoV-2. These assays may cause T-cell hyperstimulation and could overestimate antiviral immunity in chronically immunosuppressed transplant recipients, who are predisposed to infections and vaccination failures. Here, we evaluate CD154-expressing T-cells induced by unselected S antigenic peptides in 204 subjects-103 COVID-19 patients and 101 healthy unexposed subjects. Subjects included 72 transplanted and 130 non-transplanted subjects. S-reactive CD154+T-cells co-express and can thus substitute for IFN{gamma} (n=3). Assay reproducibility in a variety of conditions was acceptable with coefficient of variation of 2-10.6%. S-reactive CD154+T-cell frequencies were a) higher in 42 healthy unexposed transplant recipients who were sampled pre-pandemic, compared with 59 healthy non-transplanted subjects (p=0.02), b) lower in Tr COVID-19 patients compared with healthy transplant patients (p<0.0001), c) lower in Tr patients with severe COVID-19 (p<0.0001), or COVID-19 requiring hospitalization (p<0.05), compared with healthy Tr recipients. S-reactive T-cells were not significantly different between the various COVID-19 disease categories in NT recipients. Among transplant recipients with COVID-19, cytomegalovirus co-infection occurred in 34%; further, CMV-specific T-cells (p<0.001) and incidence of anti-receptor-binding-domain IgG (p=0.011) were lower compared with non-transplanted COVID-19 patients. Healthy unexposed transplant recipients exhibit pre-existing T-cell immunity to SARS-CoV-2. COVID-19 infection leads to impaired T-cell and antibody responses to SARS-CoV-2 and increased risk of CMV co-infection in transplant recipients.

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