Humoral and Cellular Immune Response to a Third Dose of SARSCoV- 2 Vaccine in Kidney Transplant Recipients on Belatacept

Mitchell, J.; Alejo, J.; Chiang, T. P.; Blankson, J. N.; Karaba, A. H.; Woldemeskel, B.; Garliss, C.; Chang, A.; Abedon, A.; Avery, R. K.; Tobian, A.; Massie, A. B.; Garonzik-Wang, J.; Segev, D. L.; Werbel, W.

Mitchell, J.; Alejo, J.; Chiang, T. P.; Blankson, J. N.; Karaba, A. H.; Woldemeskel, B.; Garliss, C.; Chang, A.; Abedon, A.; Avery, R. K.; Tobian, A.; Massie, A. B.; Garonzik-Wang, J.; Segev, D. L.; Werbel, W..

American Journal of Transplantation ; 22(Supplement 3):763, 2022.

Article in English | EMBASE | ID: covidwho-2063481

ABSTRACT

ABSTRACT

Purpose:

Kidney transplant recipients taking belatacept (KTR-B) have poor immune response to two-dose SARS-CoV-2 vaccination. We sought to characterize the impact of an additional vaccine dose on plasma neutralizing capacity and cellular responses as compared to that of KTRs controls (KTR-C) not taking belatacept. Method(s) Within an observational cohort, we tested 26 KTR-Bs and 27 KTR-Cs for anti-spike antibody responses before and after a third SARS-CoV-2 vaccine dose (D3) using two clinical assays (Roche Elecsys anti-S Ig and EUROIMMUN anti-S1 IgG). For a subset of 5 KTR-Bs and for all KTR-Cs we used a research assay (Meso Scale Diagnostics V-Plex [MSD]) to further assess anti-spike and RBD IgG, as well as surrogate plasma neutralizing activity (% ACE2 inhibition) versus the ancestral and delta variants. For 3 KTR-Bs, post D3 T cell response was assessed via IFN-y ELISpot and deemed positive if spot forming units > 20 per million PBMC and stimulation index > 3. Result(s) KTR-Bs had significant lower clinical anti-spike seroconversion than KTR-Cs (31% vs 74%, p=0.001) after D3 despite similar demographics, clinical factors, and vaccines administered (Table 1). No KTR-B (0/5) was seropositive by MSD anti-spike or anti-RBD IgG (Figure 1). % ACE2 inhibition versus the ancestral variant was significantly lower in KTR-Bs than in KTR-Cs (Median [IQR] 5.2 [2.8, 6.5] vs 12.5 [7.7, 23.9], p<0.01);all KTR-Bs were below a level consistent with detectable neutralizing antibody. All tested KTR-Bs (3/3) had a negative ELISpot, consistent with negligible cellular response. Conclusion(s) These results suggest minimal humoral or cellular immunogenicity of additional vaccine doses for KTR-Bs and indicates the need for alternative strategies to improve vaccine response such as immunosuppression alteration or use of passive immunoprophylaxis with monoclonal anti-spike antibody to improve protection versus SARS-CoV-2.

Keywords

adult; antibody response; cellular immunity; clinical article; cohort analysis; conference abstract; controlled study; demographics; drug therapy; enzyme linked immunospot assay; female; human; human tissue; humoral immunity; immunoassay analyzer; immunogenicity; immunoprophylaxis; immunosuppressive treatment; kidney graft; male; nonhuman; peripheral blood mononuclear cell; seroconversion; Severe acute respiratory syndrome coronavirus 2; spike; T lymphocyte; belatacept; endogenous compound; immunoglobulin G; monoclonal antibody; neutralizing antibody; SARS-CoV-2 vaccine

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Full text: Available Collection: Databases of international organizations Database: EMBASE Topics: Vaccines Language: English Journal: American Journal of Transplantation Year: 2022 Document Type: Article

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