Your search keyword '"memory cells"' showing total 319 results

1. Antigen-specific T helper cells and cytokine profiles predict intensity and longevity of cellular and humoral responses to SARSCoV-2 booster vaccination.

Author

Page, Lukas, Dennehy, Kevin, Mueller, Katharina, Girl, Philipp, Loell, Eva, Buijze, Hellen, Classen, Johanna-Maria, Messmann, Helmut, Roemmele, Christoph, Hoffmann, Reinhard, Wurster, Sebastian, and Fuchs, Andre

Subjects

MEDICAL personnel, BOOSTER vaccines, T helper cells, ANTIGEN presentation, SUPPORT vector machines

Abstract

Introduction: Pre-existent pools of coronavirus-specific or cross-reactive T cells were shown to shape the development of cellular and humoral immune responses after primary mRNA vaccination against SARS-CoV-2. However, the cellular determinants of responses to booster vaccination remain incompletely understood. Therefore, we phenotypically and functionally characterized spike antigen-specific T helper (Th) cells in healthy, immunocompetent individuals and correlated the results with cellular and humoral immune responses to BNT162b2 booster vaccination over a six-month period. Methods: Blood of 30 healthy healthcare workers was collected before, 1, 3, and 6 months after their 3rd BNT162b2 vaccination. Whole blood was stimulated with spike peptides and analyzed using flow cytometry, a 13-plex cytokine assay, and n Counter-based transcriptomics. Results: Spike-specific IgG levels at 1 month after booster vaccination correlated with pre-existing CD154+CD69+IFN-γ+CD4+ effector memory cells as well as spike-induced IL-2 and IL-17A secretion. Early post-booster (1-month) spike IgG levels (r=0.49), spike-induced IL‑2 (r=0.58), and spike-induced IFN‑γ release (r=0.43) correlated moderately with their respective long-term (6-month) responses. Sustained robust IgG responses were significantly associated with S-specific (CD69+±CD154+±IFN-γ+) Th-cell frequencies before booster vaccination (p=0.038), especially double/triple-positive type-1 Th cells. Furthermore, spike IgG levels, spike-induced IL‑2 release, and spike-induced IFN‑γ release after 6 months were significantly associated with increased IL‑2 & IL‑4, IP‑10 & MCP1, and IFN‑γ & IP‑10 levels at 1 month post-booster, respectively. On the transcriptional level, induction of pathways associated with both T-cell proliferation and antigen presentation was indicative of sustained spike-induced cytokine release and spike-specific IgG production 6 months post-booster. Using support vector machine models, pre-booster spike-specific T-cell frequencies and early post-booster cytokine responses predicted sustained (6-month) responses with F1 scores of 0.80-1.00.Discussion: In summary, spike-specific Th cells and T-cellular cytokine signatures present before BNT162b2 booster vaccination shape sustained adaptive cellular and humoral responses post-booster. Functional T-cell assays might facilitate early identification of potential non-responders. [ABSTRACT FROM AUTHOR]

Published

2024

2. Characteristics of Early Antibody Mediated Rejection in Antibody Incompatible Living Donor Kidney Transplantation.

Author

Punjala, Sai Rithin, Ibrahim, Maria, Phillips, Benedict Lyle, Stojanovic, Jelena, Kessaris, Nicos, Shaw, Olivia, Dorling, Anthony, and Mamode, Nizam

Subjects

*KIDNEY transplantation, *GRAFT survival, *IMMUNOGLOBULINS, *MULTIVARIATE analysis, *T cells

Abstract

Antibody incompatible transplantation (AIT) may be an only option for highly sensitized patients. Severe form of early antibody mediated rejection (AMR) adversely affects graft survival after AIT. The aim of this study was to identify individuals at risk of AMR. We analyzed 213 living donor AITs performed at our center. Among 120 ABOi, 58 HLAi and 35 DSA + FCXM-negative cases, the rates of early AMR were 6%, 31%, and 9%, respectively (p < 0.001). On multivariate analysis for graft loss, early AMR had a HR of 3.28 (p < 0.001). The HLAi group had worse death-censored graft survival (p = 0.003). In the HLAi group, Patients with aggressive variant AMR (AAMR) had greater percentage of C3d complement fixing DSA, higher baseline class I and total DSA MFI levels and B-cell FCXM RMF. C1q and C3d complement fixing DSA and strong positivity of baseline B- or T-cell FXCM as predictors of AAMR had 100% sensitivity. Early AMR is of significant clinical concern in AIT as it results in poor graft survival and is not well described in literature. An aggressive variant is characterized by massive rise in DSA levels at rejection. Baseline DSA, C1q, and C3d and baseline FCXM values can be used to risk-stratify candidates for AIT. [ABSTRACT FROM AUTHOR]

Published

2024

3. Deep Flow Cytometry Unveils Distinct Immune Cell Subsets in Inducible T Cell Co-Stimulator Ligand (ICOSL)- and ICOS-Knockout Mice during Experimental Autoimmune Encephalomyelitis.

Author

Raineri, Davide, Abreu, Hugo, Vilardo, Beatrice, Kustrimovic, Natasa, Venegoni, Chiara, Cappellano, Giuseppe, and Chiocchetti, Annalisa

Subjects

*T cells, *REGULATORY T cells, *FLOW cytometry, *ENCEPHALOMYELITIS, *ANTIGEN presenting cells, *T cell receptors

Abstract

The inducible T cell co-stimulator ligand (ICOSL), expressed by antigen presenting cells, binds to the inducible T cell co-stimulator (ICOS) on activated T cells. Improper function of the ICOS/ICOSL pathway has been implicated in several autoimmune diseases, including multiple sclerosis (MS). Previous studies showed that ICOS-knockout (KO) mice exhibit severe experimental autoimmune encephalomyelitis (EAE), the animal model of MS, but data on ICOSL deficiency are not available. In our study, we explored the impact of both ICOS and ICOSL deficiencies on MOG35-55 -induced EAE and its associated immune cell dynamics by employing ICOSL-KO and ICOS-KO mice with a C57BL/6J background. During EAE resolution, MOG-driven cytokine levels and the immunophenotype of splenocytes were evaluated by ELISA and multiparametric flow cytometry, respectively. We found that both KO mice exhibited an overlapping and more severe EAE compared to C57BL/6J mice, corroborated by a reduction in memory/regulatory T cell subsets and interleukin (IL-)17 levels. It is noteworthy that an unsupervised analysis showed that ICOSL deficiency modifies the immune response in an original way, by affecting T central and effector memory (TCM, TEM), long-lived CD4+ TEM cells, and macrophages, compared to ICOS-KO and C57BL/6J mice, suggesting a role for other binding partners to ICOSL in EAE development, which deserves further study. [ABSTRACT FROM AUTHOR]

Published

2024

4. Antigen-specific T helper cells and cytokine profiles predict intensity and longevity of cellular and humoral responses to SARS-CoV-2 booster vaccination

Author

Lukas Page, Kevin Dennehy, Katharina Mueller, Philipp Girl, Eva Loell, Hellen Buijze, Johanna-Maria Classen, Helmut Messmann, Christoph Roemmele, Reinhard Hoffmann, Sebastian Wurster, and Andre Fuchs

Subjects

COVID-19, immunity, memory cells, immune monitoring, antibodies, cytokines, Immunologic diseases. Allergy, RC581-607

Abstract

IntroductionPre-existent pools of coronavirus-specific or cross-reactive T cells were shown to shape the development of cellular and humoral immune responses after primary mRNA vaccination against SARS-CoV-2. However, the cellular determinants of responses to booster vaccination remain incompletely understood. Therefore, we phenotypically and functionally characterized spike antigen-specific T helper (Th) cells in healthy, immunocompetent individuals and correlated the results with cellular and humoral immune responses to BNT162b2 booster vaccination over a six-month period. MethodsBlood of 30 healthy healthcare workers was collected before, 1, 3, and 6 months after their 3rd BNT162b2 vaccination. Whole blood was stimulated with spike peptides and analyzed using flow cytometry, a 13-plex cytokine assay, and nCounter-based transcriptomics. ResultsSpike-specific IgG levels at 1 month after booster vaccination correlated with pre-existing CD154+CD69+IFN-γ+CD4+ effector memory cells as well as spike-induced IL-2 and IL-17A secretion. Early post-booster (1-month) spike IgG levels (r=0.49), spike-induced IL‑2 (r=0.58), and spike-induced IFN‑γ release (r=0.43) correlated moderately with their respective long-term (6-month) responses. Sustained robust IgG responses were significantly associated with S-specific (CD69+±CD154+±IFN-γ+) Th-cell frequencies before booster vaccination (p=0.038), especially double/triple-positive type-1 Th cells. Furthermore, spike IgG levels, spike-induced IL‑2 release, and spike-induced IFN‑γ release after 6 months were significantly associated with increased IL‑2 & IL‑4, IP‑10 & MCP1, and IFN‑γ & IP‑10 levels at 1 month post-booster, respectively. On the transcriptional level, induction of pathways associated with both T-cell proliferation and antigen presentation was indicative of sustained spike-induced cytokine release and spike-specific IgG production 6 months post-booster. Using support vector machine models, pre-booster spike-specific T-cell frequencies and early post-booster cytokine responses predicted sustained (6-month) responses with F1 scores of 0.80-1.00.DiscussionIn summary, spike-specific Th cells and T-cellular cytokine signatures present before BNT162b2 booster vaccination shape sustained adaptive cellular and humoral responses post-booster. Functional T-cell assays might facilitate early identification of potential non-responders.

Published

2024

5. Characteristics of Early Antibody Mediated Rejection in Antibody Incompatible Living Donor Kidney Transplantation

Author

Sai Rithin Punjala, Maria Ibrahim, Benedict Lyle Phillips, Jelena Stojanovic, Nicos Kessaris, Olivia Shaw, Anthony Dorling, and Nizam Mamode

Subjects

ABOi, HLAi, kidney transplantation, AMR, memory cells, Specialties of internal medicine, RC581-951

Abstract

Antibody incompatible transplantation (AIT) may be an only option for highly sensitized patients. Severe form of early antibody mediated rejection (AMR) adversely affects graft survival after AIT. The aim of this study was to identify individuals at risk of AMR. We analyzed 213 living donor AITs performed at our center. Among 120 ABOi, 58 HLAi and 35 DSA + FCXM-negative cases, the rates of early AMR were 6%, 31%, and 9%, respectively (p < 0.001). On multivariate analysis for graft loss, early AMR had a HR of 3.28 (p < 0.001). The HLAi group had worse death-censored graft survival (p = 0.003). In the HLAi group, Patients with aggressive variant AMR (AAMR) had greater percentage of C3d complement fixing DSA, higher baseline class I and total DSA MFI levels and B-cell FCXM RMF. C1q and C3d complement fixing DSA and strong positivity of baseline B- or T-cell FXCM as predictors of AAMR had 100% sensitivity. Early AMR is of significant clinical concern in AIT as it results in poor graft survival and is not well described in literature. An aggressive variant is characterized by massive rise in DSA levels at rejection. Baseline DSA, C1q, and C3d and baseline FCXM values can be used to risk-stratify candidates for AIT.

Published

2024

6. Adaptive Immunity and Antigen Receptor Diversity

Author

Carlberg, Carsten, Velleuer, Eunike, Molnár, Ferdinand, Carlberg, Carsten, Velleuer, Eunike, and Molnár, Ferdinand

Published

2023

7. Implications of CD45RA and CD45RO T cell subsets in patients of chronic rhinosinusitis with nasal polyposis infected with Aspergillus flavus.

Author

Rai, Gargi, Das, Shukla, Ansari, Mohammad Ahmad, Singh, Praveen Kumar, Dar, Sajad Ahmad, Gupta, Neelima, Sharma, Sonal, Ramachandran, Vishnampettai Ganapathysubramanian, and Jain, Charu

Subjects

*ASPERGILLUS flavus, *T cells, *MONONUCLEAR leukocytes, *NASAL polyps, *FUNGAL proteins, *SINUSITIS

Abstract

T cell subsets (CD4 and CD8) play a prominent role in the development of chronic rhinosinusitis with nasal polyposis (CRSwNP). Colonization with Aspergillus flavus is recognized as a trigger for the growth of nasal polyps. The fungal proteins initiate the recruitment of T cells into the nasal mucosa, which contributes to the progression of nasal polyps. The study included 50 cases of CRSwNP and 50 healthy controls. Biopsies were subjected to KOH and culture for mycological investigation. We examined the changes in T helper (CD4+) and T cytotoxic (CD8+) in total T cells (CD3+) and expression of naive (CD45RA) and memory (CD45RO) cell markers in T cell subsets in peripheral blood mononuclear cells (PBMCs) challenged by A. flavus antigens in cases before and after treatment and in healthy controls by flow cytometry. Predominantly, A. flavus (86%) identified in nasal polyp biopsies of patients. An increased percentage of CD3+CD4+ T cells observed after A. flavus stimulation in patients when compared with healthy controls. The expression of CD4+CD45RA+ cells was significantly (P <.05) reduced in patients and increased CD4+CD45RO+ was observed upon stimulation with A. flavus in patients when compared with healthy control. Continuous exposure to inhaled fungal spores may induce aberrant immune responses to A. flavus spores, causing an allergic immunological reaction with high CD4+T cell responses, resulting in an unfavourable outcome. Elevated CD4+CD45RO+ T cells may transform the pathogenic response and highlight the chances of A. flavus reactive T cells involvement in prompting inflammation in CRSwNP. [ABSTRACT FROM AUTHOR]

Published

2023

8. Use of Eutectic Effects in the Possible Creation of Phase-Change Memory Cells Based on Ag–Cu Nanoclusters.

Author

Ryzhkova, D. A., Gafner, S. L., and Gafner, Yu. Ya.

Subjects

PHASE change memory, BINARY metallic systems, MOLECULAR dynamics, EUTECTICS, CRYSTAL structure

Abstract

An attractive trend in the further progress of nanoelectronics is the development of a new generation of non-volatile memory devices, namely electric phase memory or PC-RAM (Phase Change Random Access Memory). However, there are a number of related unsolved problems, such as the stability of the amorphous phase, high power consumption, long information storage time, etc. In order to solve these problems, a new approach has been proposed, which consists in using Ag–Cu binary alloy nanoparticles as PC-RAM cells. To this end, the molecular dynamics method was used to study the processes of structuring these alloy nanoparticles (NPs) with a size of D = 2–10 nm of different compositions when the heat energy removal rate was varied. The stability criteria of the amorphous and crystalline structure were evaluated and conclusions were drawn about the target composition and size of NPs, suitable for the fabrication of phase change memory cells. It has been shown that using binary Ag–Cu alloy NPs, it is possible to reduce the size of a single cell to 6–8 nm and the information recording time to 2.5 ns and, for the first time, based on the eutectic approach, to achieve the stability of the amorphous and crystalline structure at different rates of heat energy removal. [ABSTRACT FROM AUTHOR]

Published

2023

9. Analyses of human immune responses to Francisella tularensis identify correlates of protection.

Author

Lindgren, Helena, Eneslätt, Kjell, Golovliov, Igor, Gelhaus, Carl, and Sjöstedt, Anders

Subjects

FRANCISELLA tularensis, MONONUCLEAR leukocytes, IMMUNE response, TRANSVERSE electromagnetic cells, IMMUNOLOGIC memory

Abstract

Francisella tularensis is the etiological agent of the potentially severe infection tularemia. An existing F: tularensis vaccine, the live vaccine strain (LVS), has been used to protect at-risk personnel, but it is not licensed in any country and it has limited efficacy. Therefore, there is a need of a new, efficacious vaccine. The aim of the study was to perform a detailed analysis of the characteristics of the human immune response to F. tularensis, since this will generate crucial knowledge required to develop new vaccine candidates. Nine individuals were administered the LVS vaccine and peripheral blood mononuclear cells (PBMC) were collected before and at four time points up to one year after vaccination. The properties of the PBMC were characterized by flow cytometry analysis of surface markers and intracellular cytokine staining. In addition, the cytokine content of supernatants from F. tularensis-infected PBMC cultures was determined and the protective properties of the supernatants investigated by adding them to cultures with infected monocyte-derived macrophages (MDM). Unlike before vaccination, PBMC collected at all four time points after vaccination demonstrated F. tularensis-specific cell proliferation, cytokine secretion and cytokine-expressing memory cells. A majority of 17 cytokines were secreted at higher levels by PBMC collected at all time points after vaccination than before vaccination. A discriminative analysis based on IFN-γ and IL-13 secretion correctly classified samples obtained before and after vaccination. Increased expression of IFN-γ, IL-2, and MIP-1β were observed at all time points after vaccination vs. before vaccination and the most significant changes occurred among the CD4 transient memory, CD8 effector memory, and CD8 transient memory T-cell populations. Growth restriction of the highly virulent F. tularensis strain SCHU S4 in MDM was conferred by supernatants and protection correlated to levels of IFN-γ, IL-2, TNF, and IL-17. The findings demonstrate that F. tularensis vaccination induces long-term T-cell reactivity, including TEM and TTM cell populations. Individual cytokine levels correlated with the degree of protection conferred by the supernatants. Identification of such memory T cells and effector mechanisms provide an improved understanding of the protective mechanisms against F. tularensis. mechanisms against F. tularensis. [ABSTRACT FROM AUTHOR]

Published

2023

10. Analyses of human immune responses to Francisella tularensis identify correlates of protection

Author

Helena Lindgren, Kjell Eneslätt, Igor Golovliov, Carl Gelhaus, and Anders Sjöstedt

Subjects

F. tularensis, vaccination, immune response, memory cells, human correlates of protection, Immunologic diseases. Allergy, RC581-607

Abstract

Francisella tularensis is the etiological agent of the potentially severe infection tularemia. An existing F: tularensis vaccine, the live vaccine strain (LVS), has been used to protect at-risk personnel, but it is not licensed in any country and it has limited efficacy. Therefore, there is a need of a new, efficacious vaccine. The aim of the study was to perform a detailed analysis of the characteristics of the human immune response to F. tularensis, since this will generate crucial knowledge required to develop new vaccine candidates. Nine individuals were administered the LVS vaccine and peripheral blood mononuclear cells (PBMC) were collected before and at four time points up to one year after vaccination. The properties of the PBMC were characterized by flow cytometry analysis of surface markers and intracellular cytokine staining. In addition, the cytokine content of supernatants from F. tularensis-infected PBMC cultures was determined and the protective properties of the supernatants investigated by adding them to cultures with infected monocyte-derived macrophages (MDM). Unlike before vaccination, PBMC collected at all four time points after vaccination demonstrated F. tularensis-specific cell proliferation, cytokine secretion and cytokine-expressing memory cells. A majority of 17 cytokines were secreted at higher levels by PBMC collected at all time points after vaccination than before vaccination. A discriminative analysis based on IFN-γ and IL-13 secretion correctly classified samples obtained before and after vaccination. Increased expression of IFN-γ, IL-2, and MIP-1β were observed at all time points after vaccination vs. before vaccination and the most significant changes occurred among the CD4 transient memory, CD8 effector memory, and CD8 transient memory T-cell populations. Growth restriction of the highly virulent F. tularensis strain SCHU S4 in MDM was conferred by supernatants and protection correlated to levels of IFN-γ, IL-2, TNF, and IL-17. The findings demonstrate that F. tularensis vaccination induces long-term T-cell reactivity, including TEM and TTM cell populations. Individual cytokine levels correlated with the degree of protection conferred by the supernatants. Identification of such memory T cells and effector mechanisms provide an improved understanding of the protective mechanisms against F. tularensis. mechanisms against F. tularensis.

Published

2023

11. Unique features of the TCR repertoire of reactivated memory T cells in the experimental mouse tumor model

Author

Anastasiia Kalinina, Nadezda Persiyantseva, Olga Britanova, Ksenia Lupyr, Irina Shagina, Ludmila Khromykh, and Dmitry Kazansky

Subjects

T cell receptor, TCR repertoire, TCR physicochemical features, Memory cells, Antigen-specific clonotypes, NGS sequencing, Biotechnology, TP248.13-248.65

Abstract

T cell engineering with T cell receptors (TCR) specific to tumor antigens has become a breakthrough towards personalized cancer adoptive cell immunotherapy. However, the search for therapeutic TCRs is often challenging, and effective strategies are strongly required for the identification and enrichment of tumor-specific T cells that express TCRs with superior functional characteristics. Using an experimental mouse tumor model, we studied sequential changes in TCR repertoire features of T cells involved in the primary and secondary immune responses to allogeneic tumor antigens. In-depth bioinformatics analysis of TCR repertoires showed differences in reactivated memory T cells compared to primarily activated effectors. After cognate antigen re-encounter, memory cells were enriched with clonotypes that express α-chain TCR with high potential cross-reactivity and enhanced strength of interaction with both MHC and docked peptides. Our findings suggest that functionally true memory T cells could be a better source of therapeutic TCRs for adoptive cell therapy. No marked changes were observed in the physicochemical characteristics of TCRβ in reactivated memory clonotypes, indicative of the dominant role of TCRα in the secondary allogeneic immune response. The results of this study could further contribute to the development of TCR-modified T cell products based on the phenomenon of TCR chain centricity.

Published

2023

12. Adaptive Immunity and Antigen Receptor Diversity

Author

Carlberg, Carsten, Velleuer, Eunike, Carlberg, Carsten, and Velleuer, Eunike

Published

2022

13. Schematic Solutions of Digital CMOS Microcircuits

Author

Belous, Anatoly, Saladukha, Vitali, Belous, Anatoly, and Saladukha, Vitali

Published

2022

14. Standard Characteristics of Digital Microcircuits

Author

Belous, Anatoly, Saladukha, Vitali, Belous, Anatoly, and Saladukha, Vitali

Published

2022

15. Circuit Engineering of Bi-CMOS IC

Author

Belous, Anatoly, Saladukha, Vitali, Belous, Anatoly, and Saladukha, Vitali

Published

2022

16. Deep Flow Cytometry Unveils Distinct Immune Cell Subsets in Inducible T Cell Co-Stimulator Ligand (ICOSL)- and ICOS-Knockout Mice during Experimental Autoimmune Encephalomyelitis

Author

Davide Raineri, Hugo Abreu, Beatrice Vilardo, Natasa Kustrimovic, Chiara Venegoni, Giuseppe Cappellano, and Annalisa Chiocchetti

Subjects

ICOSL, experimental autoimmune encephalomyelitis, memory cells, regulatory T cells, multiple sclerosis, Biology (General), QH301-705.5, Chemistry, QD1-999

Abstract

The inducible T cell co-stimulator ligand (ICOSL), expressed by antigen presenting cells, binds to the inducible T cell co-stimulator (ICOS) on activated T cells. Improper function of the ICOS/ICOSL pathway has been implicated in several autoimmune diseases, including multiple sclerosis (MS). Previous studies showed that ICOS-knockout (KO) mice exhibit severe experimental autoimmune encephalomyelitis (EAE), the animal model of MS, but data on ICOSL deficiency are not available. In our study, we explored the impact of both ICOS and ICOSL deficiencies on MOG35-55 -induced EAE and its associated immune cell dynamics by employing ICOSL-KO and ICOS-KO mice with a C57BL/6J background. During EAE resolution, MOG-driven cytokine levels and the immunophenotype of splenocytes were evaluated by ELISA and multiparametric flow cytometry, respectively. We found that both KO mice exhibited an overlapping and more severe EAE compared to C57BL/6J mice, corroborated by a reduction in memory/regulatory T cell subsets and interleukin (IL-)17 levels. It is noteworthy that an unsupervised analysis showed that ICOSL deficiency modifies the immune response in an original way, by affecting T central and effector memory (TCM, TEM), long-lived CD4+ TEM cells, and macrophages, compared to ICOS-KO and C57BL/6J mice, suggesting a role for other binding partners to ICOSL in EAE development, which deserves further study.

Published

2024

17. Vaccination provides superior in vivo recall capacity of SARS-CoV-2-specific memory CD8 T cells

Author

Inga Kavazović, Christoforos Dimitropoulos, Dora Gašparini, Mari Rončević Filipović, Igor Barković, Jan Koster, Niels A. Lemmermann, Marina Babić, Đurđica Cekinović Grbeša, and Felix M. Wensveen

Subjects

CD8 T cells, SARS-CoV-2, COVID-19, memory cells, infection, vaccination, Biology (General), QH301-705.5

Abstract

Summary: Memory CD8 T cells play an important role in the protection against breakthrough infections with severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2). Whether the route of antigen exposure impacts these cells at a functional level is incompletely characterized. Here, we compare the memory CD8 T cell response against a common SARS-CoV-2 epitope after vaccination, infection, or both. CD8 T cells demonstrate comparable functional capacity when restimulated directly ex vivo, independent of the antigenic history. However, analysis of T cell receptor usage shows that vaccination results in a narrower scope than infection alone or in combination with vaccination. Importantly, in an in vivo recall model, memory CD8 T cells from infected individuals show equal proliferation but secrete less tumor necrosis factor (TNF) compared with those from vaccinated people. This difference is negated when infected individuals have also been vaccinated. Our findings shed more light on the differences in susceptibility to re-infection after different routes of SARS-CoV-2 antigen exposure.

Published

2023

18. Different Types of Chronic Inflammation Engender Distinctive Immunosenescent Profiles in Affected Patients.

Author

Moysidou, Eleni, Lioulios, Georgios, Xochelli, Aliki, Nikolaidou, Vasiliki, Christodoulou, Michalis, Mitsoglou, Zoi, Stai, Stamatia, Fylaktou, Asimina, Papagianni, Aikaterini, and Stangou, Maria

Subjects

*B cells, *IMMUNOSENESCENCE, *CHRONIC kidney failure, *T cells, *PHENOTYPIC plasticity, *HEMODIALYSIS patients

Abstract

Immunosenescence encompasses a spectrum of lymphocyte phenotypic alterations. The aim of the study was to evaluate immunosenescent effect of two different forms of chronic inflammation, Systemic Lupus Erythematosous (SLE), a systemic autoimmune disease, and End-Stage Kidney Disease (ESKD), a chronic inflammatory disorder. Certain lymphocyte surface molecules, including CD31, CD45RA, CCR7, CD28, CD57, for T, and IgD, CD27 for B lymphocytes, were analyzed by flow cytometry in 30 SLE and 53 ESKD patients on hemodialysis (HD), and results were compared to 31 healthy controls (HC) of similar age, gender, and nationality. Significant Lymphopenia was evident in both SLE and ESKD-HD patients, compared to HC, affecting B cells 75.4 (14.4–520.8), 97 (32–341), and 214 (84–576) cells/μL, respectively, p < 0.0001, and CD4 cells 651.2 (71.1–1478.2), 713 (234–1509), and 986 (344–1591) cells/μL, respectively, p < 0.0001. The allocation of B cell subpopulations was remarkably different between SLE and ESKD-HD patients. SLE showed a clear shift to senescence (CD19IgD-CD27−) cells, compared to ESKD-HD and HC, 11.75 (10)% vs. 8 (6) vs. 8.1 (10), respectively. Regarding T lymphocytes, Central Memory CD8 cells predominated in both SLE and ESKD-HD patients compared to HC, 53 (50)%, 52 (63), and 24 (64)%, respectively, while ESKD-HD but not SLE patients also had increased expression of CD4CD28− and CD8CD28− cells. In conclusion, both diseases are followed by significant lymphopenia; however, the senescent phenomenon affects the B lymphocyte compartment in SLE patients and T lymphocytes in ESKD-HD patients. [ABSTRACT FROM AUTHOR]

Published

2022

19. Heterologous Booster Dose with CORBEVAX following Primary Vaccination with COVISHIELD Enhances Protection against SARS-CoV-2.

Author

Jaggaiahgari, Shashidhar, Munigela, Apoorva, Mitnala, Sasikala, Gujjarlapudi, Deepika, Simhadri, Venu, and D, Nageshwar Reddy

Subjects

BOOSTER vaccines, COVID-19 vaccines, VACCINATION, SARS-CoV-2, B cells, AUTOBIOGRAPHICAL memory

Abstract

Despite effective vaccination programs, waning immunity in the vaccinated populations and the emergence of variants of concern posed a risk of breakthrough infections. A booster dose was demonstrated to provide substantially increased protection against symptomatic disease and hospitalization. We aimed to evaluate immune memory and the efficacy of reducing the rate of SARS-CoV-2 infection post heterologous booster with CORBEVAX after primary vaccination with two doses of COVISHIELD. SARS-CoV-2 S1/S2 spike IgG and RBD-specific antibody responses were elicited with both booster vaccines, with a greater response in individuals receiving heterologous booster. T and B memory responses were increased with booster dose, whereas B memory needed a longer duration to develop in individuals who received a homologous booster (90 days) in comparison to a heterologous booster (30 days). RBD-specific B memory and antibody-secreting (non-memory) B lymphocytes were enhanced with both boosters; however, the duration of response was longer with the heterologous booster compared to the homologous, indicating greater protection with the heterologous booster. The rate of infection 14 days after administration of the heterologous booster was comparatively lower than that of the homologous booster, with the symptoms being much less or asymptomatic. [ABSTRACT FROM AUTHOR]

Published

2022

20. Imbalanced immunobiological reactivity, infection and mutagenesis factors in the hepatobiliary system affected by a natural focal habitat factor — a trematode invasion by Opisthorchis felineus

Author

A. G. Rybka

Subjects

opisthorchis felineus, opisthorchis, invasion, chronic opisthorchiasis, immunobiological reactivity, immunological memory, memory cells, antigens, antibodies, immune complexes, genotype, genotypic properties, cholangiocytes, proliferation, microflora/ microbiota, primary/secondary bile acids, endogenous mutagens (carcinogens), somatic mutations, carcinogenesis, cholangiocarcinoma, cholangiocarcinogenesis, Infectious and parasitic diseases, RC109-216

Abstract

An interaction between decreasing host anti-infective defense due to long-term invasion with Opisthorchis felineus in the hepatobiliary system, duct bile colonization by microflora and revealing the endogenous mutagenesis (carcinogenesis) factor in bile — secondary bile acids — is considered in the article. The role of organism genotype in pathogen-related immune response to Opisthorchis felineus trematode and helminth development in the hepatobiliary system has been shown. The role of dysregulated mechanisms of tissue homeostasis in induction of compensatory chronic homeostatic proliferation and somatic cell oncogenesis is discussed. The study results evidence that disturbed functioning of regulatory T cells, inhibition of the NK cell effector function and very high functional activity of memory B cells are of great importance in imbalanced host immunobiological reactivity, caused by chronic opistorchis invasion. Decreased host anti-infective protection causes intrahepatic bile duct infection with different bacterial species. Presence of secondary bile acids in hepatobiliary system was associated with biliary bacterial strains inhabiting intestinal tract: Proteus vulgaris, Proteus mirabilis, Citrobacter freundii, Bacteroides alcaligues faecalis, Clostridium, Streptococcus faecalis, Еscherichia coli — gut microflora agents. Participation of microbiota in bile acid biotransformation immediately in the duct bile has been confirmed in experiments in vitro. Experimental methods on Drosophila melanogaster and Salmonella typhimurium strains: TA100, TA98 allowed to find out that bile from chronic opistorchiasis patients exerts higher mutagenic activity compared to control groups. Mutational events in somatic and bacterial cells depend on the presence of secondary bile acids (deoxycholic, lithocholic) in duct bile, as well as the level of total bile acid concentration. The study data confirm the concept by Professor A.A. Shain about the presence of endogenous risk factor for developing primary cholangiocellular liver cancer such as secondary bile acids in the bile of chronic opistorchiasis patients. A concept of cholangiocarcinogenesis, based on mutational events, is added up with disturbance of generative cycle in tissue cells and their differentiation due to decreased chalone factor activity, as well as sensitivity threshold to it. Level of investigation and understanding of mechanisms underlying cholangiocarcinogenesis during chronic opisthorchis invasion will allow to develop pathogenetic approaches to correct homeostasis regulation and prevention of cholangiocarcinomas.

Published

2021

21. Role of the cellular immunity in the formation of the immune response in coronavirus infections

Author

I. A. Ivanova, N. D. Omelchenko, A. V. Filippenko, A. A. Trufanova, and A. K. Noskov

Subjects

sars-cov, mers-cov, sars-cov-2, cellular immune response, t lymphocytes, memory cells, Immunologic diseases. Allergy, RC581-607

Abstract

The data obtained during previous epidemics caused by coronaviruses, and current pandemic indicate that assessing the role of certain immune interactions between these viruses and the microorganism is the main pre-requisite for development of diagnostic test systems as well as effective medical drugs and preventive measures. The review summarizes the results of studying patho– and immunogenesis of SARSCoV, MERS-CoV, and SARS-CoV-2 infections. These coronaviruses were proven to suppress development of adaptive immune response at the stage of its induction, affecting the number and functional activity of lymphocytes, effectors of cellular immunity, causing impairment of lymphopoiesis, apoptosis and «depletion» of these cells, thus leading to longer duration of the disease and increased viral load. Information about the role of cellular immunity in development of immune response to coronaviruses is presented. It was proven that the causative agents of SARS, MERS and COVID-19 trigger adaptive immune response in the microorganism according to both humoral and cellular types. Moreover, the synthesis of specific immunoglobulins does not yet point to presence of protective immune response. Activation of the cellular link of immunity is also important. A high degree of antigenic epitope homology in SARS-CoV, MERS-CoV and SARS-CoV-2 is described, thus suggesting an opportunity for cross-immunity to coronaviruses. The review addresses issues related to the terms of specific memory immune cells to SARS-CoV, MERS-CoV and SARS-CoV-2, and their role in providing long-term protection against these infections. Given that specific antibodies to SARS and MERS pathogens persisted for a year, were often not detected or briefly registered in patients with mild and asymptomatic infections, we can talk about important role of the cellular immune response in providing immunity to these coronaviruses. It was shown that, in contrast to antibodies, the antigen-specific memory T cells were registered in patients with SARS virus for 4 to 11 years, and Middle East Respiratory Syndrome – up to two years. Further research is needed to determine presence and number of memory T cells in COVID-19. A comparative analysis of data obtained during previous epidemics with respect to formation of adaptive immunity to coronaviruses. Description of proteins and epitopes recognized by human T lymphocytes will be useful in monitoring immune responses in COVID-19 patients, as well as in developing informative tests to study T cell immune response to SARS-CoV-2 and new preventive drugs.

Published

2021

22. Evaluation of calpain T-cell epitopes as vaccine candidates against experimental Leishmania major infection: a pilot study.

Author

Brakat, Reham, Mahmoud, Amal, Abd El Gayed, Eman, Soliman, Shaimaa, and Sharaf-El-Deen, Shaimaa

Subjects

*CALPAIN, *LEISHMANIA major, *EPITOPES, *PEROXIREDOXINS, *CHIMERIC proteins, *MOLECULAR dynamics, *T cells

Published

2022

23. Assessment of the Mitochondrial Condition in CD4+ and CD8+ T-Lymphocytes from Healthy Subjects.

Author

Korolevskaya, L. B., Saidakova, E. V., Shmagel, N. G., and Shmagel, K. V.

Abstract

Despite the active study of T-lymphocyte mitochondria under pathology, data on the organelles' condition in healthy people are not presented in the available literature. The aim of this work was to assess mitochondrial condition in CD4+ and CD8+ T-lymphocytes of healthy subjects. In both cell subsets, the mitochondrial mass and mitochondrial membrane potential, as well as the content of the mitochondrial-activity regulator (PGC-1α), were determined by flow cytometry. Naive and memory cells, as well as resting and cycling lymphocytes were compared. It was shown for the first time that in healthy subjects, mitochondrial condition differs between CD4+ and CD8+ T-lymphocytes. Despite the cell maturation stage or resting/cycling status, the mass and membrane potential of mitochondria in CD4+ T-lymphocytes significantly exceed those in CD8+ T-cells. Both CD4+ and CD8+ T-lymphocytes have higher mitochondrial mass, mitochondrial membrane potential, and PGC-1α content in memory cells and cycling elements. Furthermore in healthy individuals, the relationship between the level of the mitochondrial activity regulator and the indices of mitochondrial condition differ significantly between CD4+ and CD8+ T-lymphocytes: in CD4+ T-cells, the PGC-1α content is directly related to the mass of mitochondria, but in CD8+ T-lymphocytes, it is directly related with the organelles' transmembrane potential. [ABSTRACT FROM AUTHOR]

Published

2022

24. Self-Adjuvanting Adenoviral Nanovaccine for Effective T-Cell-Mediated Immunity and Long-Lasting Memory Cell Activation against Tuberculosis.

Author

Sowndharya CK, Mehnath S, Ponbharathi A, and Jeyaraj M

Subjects

Animals, Mice, Adenoviridae, Immunity, Cellular, Chitosan chemistry, Chitosan administration & dosage, Mycobacterium smegmatis immunology, Female, Dendritic Cells immunology, Adjuvants, Immunologic administration & dosage, Nanoparticles chemistry, Immunologic Memory, T-Lymphocytes immunology, Mice, Inbred C57BL, Mice, Inbred BALB C, Adjuvants, Vaccine administration & dosage, Nanovaccines, Tuberculosis Vaccines immunology, Tuberculosis Vaccines administration & dosage, Tuberculosis prevention & control, Tuberculosis immunology

Abstract

An enhanced vaccine is immediately required to swap the more than 100 year-old bacillus Calmette-Guerin (BCG) vaccine against tuberculosis. Here, trimethyl chitosan-loaded inactivated Mycobacterium smegmatis (MST), along with potent adenovirus hexon protein (AdHP), and toll-like receptor (TLR)-1/2 as a nanovaccine, was developed against tuberculosis (TB). The nanoformulation increased the bioavailability of MST and elicited the targeting ability. Nanovaccines have a size range of 183.5 ± 9.5 nm with a spherical morphology and uniform distribution. The nanovaccine exhibited a higher release of antigen in acidic pH, and this is mainly due to protonation of ionizable groups in polymeric materials. The nanovaccine facilitated the effective cellular uptake of bone-marrow-derived dendritic cells and progressive endosomal escape in a shorter period. In vitro analyses indicated that the nanovaccine activated cytokine and T-cell production and also assisted in humoral immunity by producing antibodies. The nanovaccine was able to induce more cellular and humoral memory cells and a better protective immune response. Nanomaterials effectively delivered the MST, AdHP, and TLR1/2 antigens to the major histocompatibility complex class I and II pathways to generate protective cytotoxic CD8 + and CD4 + T-cells. In vivo experiments, compared with free MST and BCG, showed that mice immunized with the nanovaccine induced more specific CD4 + , CD8 + , and memory T-cell activations. Overall, the fabricated nanovaccine was able to control the release of antigens and adjuvants and enhance memory cell activation and humoral immunity against TB.

Published

2024

25. Significant Role of Cellular Activation in Viral Infections

Author

Chidipi, Bojjibabu, Bolleddu, Samuel Ignatious, Sheela, Ganugula Mohana, Matta Reddy, Alavala, and Bramhachari, Pallaval Veera, editor

Published

2020

26. CELLULAR IMMUNITY PARAMETERS IN PATIENTS WITH REMITTING MULTIPLE SCLEROSIS

Author

I. P. Ivanova, D. V. Dyomina, M. N. Davydova, and G. V. Seledtsova

Subjects

cellular immunity, t-cells, cytokines, memory cells, multiple sclerosis, t-cell vaccine, Immunologic diseases. Allergy, RC581-607

Abstract

The aim of this work was to study some parameters of cellular immunity in patients with multiple sclerosis (MS). The study included 10 patients with relapsing-remitting MS aged 32 to 50 years. Diagnosis was clinically established and confirmed by magnetic resonance imaging. Patients did not receive immunosuppressive therapy for at least 6 months prior to study entry. The neurological status of all examined patients was assessed using the Kurtzke functional scale using the Extended Disability Scale (EDSS) and averaged 4.0±0.67 points, the mean number of exacerbations per year was 1.25±0.25. While studying such parameters of the immune status such as the number of T, B, NK-cells, the content of immunoglobulins, the phagocytic activity of monocytes and granulocytes, their production of reactive oxygen species, no significant differences were observed in patients with MS in comparison with the normal donor level. At the same time, we have noted an increase in the proliferative response of mononuclear blood cells to myelin antigen by 2.35 times. The content of CD4+CD45RO+CD62L+ and CD8+CD45RO+CD62L+ central memory T-cells, as well as CD8+CD45RO+CD62L- effector memory T-cells in the blood of MS patients significantly exceeded the control values (p < 0.05). Also, in MS patients, compared with healthy individuals, there was an increased level of naive IFNγ-positive CD4+CD45RO- and CD8+CD45ROT-cells (p < 0.01), and an increase in CD4+CD45RO+ and CD8+CD45RO+ memory T-cells producing IFNγg or IFNγg together with IL-4 in response to the activation (p < 0.01). Consistent with these data, there were significantly increased serum IFNγ and IL-17 levels and no changes in IL-4 levels. The relative level of naive CD4+CD25+FoxP3+, as well as induced CD4+CD25- FoxP3+ regulatory T-cells in MS patients did not significantly change compared to donor values. The results of assessing some parameters of the immune status in MS patients indicate a functional reshaping of the immune system towards the Th1 type of immune response. It is obvious that immunotropic treatment of MS should be aimed at inactivating auto-immune Tand B-lymphocytes, suppressing the production of proinflammatory mediators, and enhancing the activity of natural and induced regulatory T-cells.

Published

2021

27. Tapping the immunological imprints to design chimeric SARS-CoV-2 vaccine for elderly population.

Author

Biswas, Asim, Mandal, Rahul Shubhra, Chakraborty, Suparna, and Maiti, George

Subjects

*INFLUENZA, *OLDER people, *COVID-19 vaccines, *COVID-19, *EXTRACELLULAR matrix proteins, *VIRUS-like particles, *PSYCHONEUROIMMUNOLOGY

Abstract

The impact of SARS-CoV-2 and COVID-19 disease susceptibility varies depending on the age and health status of an individual. Currently, there are more than 140 COVID-19 vaccines under development. However, the challenge will be to induce an effective immune response in the elderly population. Analysis of B cell epitopes indicates the minor role of the stalk domain of spike protein in viral neutralization due to low surface accessibility. Nevertheless, the accumulation of mutations in the receptor-binding domain (RBD) might reduce the vaccine efficacy in all age groups. We also propose the concept of chimeric vaccines based on the co-expression of SARS-CoV-2 spike and influenza hemagglutinin (HA) and matrix protein 1 (M1) proteins to generate chimeric virus-like particles (VLP). This review discusses the possible approaches by which influenza-specific memory repertoire developed during the lifetime of the elderly populations can converge to mount an effective immune response against the SARS-CoV-2 spike protein with the possibilities of designing single vaccines for COVID-19 and influenza. Immunosenescence aggravates COVID-19 symptoms in elderly individuals. Low immunogenicity of SARS-CoV-2 vaccines in elderly population. Tapping the memory T and B cell repertoire in elderly can enhance vaccine efficiency. Chimeric vaccines can mount effective immune response against COVID-19 in elderly. Chimeric vaccines co-express SARS-CoV-2 spike and influenza HA and M1 proteins. [ABSTRACT FROM AUTHOR]

Published

2022

28. Perspective trends of topical therapy of patients with psoriasis

Author

Alexander S. Zhukov, Vladislav R. Khairutdinov, and Alexey V. Samtsov

Subjects

psoriasis, topical therapy, methotrexate, memory cells, serine proteases, Dermatology, RL1-803

Abstract

Topical medications are used to treat not only limited, but also common forms of the disease. Currently prescribed external anti-inflammatory drugs have a low selectivity of action, which does not allow achieving a long-term and pronounced clinical effect without the development of undesirable phenomena. This review presents new options for the use of methotrexate in modern topical forms (AuNPs-3MPS), which make it possible to reduce the incidence of adverse events with a high efficiency of therapy. Shown is an innovative drug that blocks resident memory cells (PAP-1), which will influence the course and relapses of the disease, and possibly even lead to the cure of the patient from psoriasis. A new direction has been described inhibition of serine proteases (ER143, AAN-16) and thus inhibition of IL-36-mediated inflammation, which will allow controlling the inflammatory process in psoriasis in the early stages of its development. In addition, a number of drugs are shown whose action is based on blocking intracellular signaling pathways, which leads to inhibition of the development of the inflammatory response and resolution of psoriatic eruptions: inhibitors of Janus kinases (tofacitinib), transcription factor Stat3 (rS3-PA), secondary messenger of signals (SIS3), phosphodiesterase 7 (ASB16165) and 4 (AN-2728/crisaborol), ROR transcription factor (PF-06763809), phospholipase A2 (AVX001), hydrolases (DZ2002). The results of preclinical and initial stages of clinical trials with an assessment of the safety and tolerability of the studied substances are presented. Based on the review, the advantages and disadvantages of the proposed drugs are characterized. Topical therapy with a selective effect on the key links in the development of psoriasis will increase the effectiveness of treatment and reduce the frequency of unwanted effects.

Published

2021

29. Clinical features and lymphocyte immunophenotyping analysis in primary immunodeficiency patients with non-transplant lymphoproliferative disorders.

Author

Lee, Wen-I, Huang, Jing-Long, Hsieh, Meng-Ying, Chen, Li-Chen, Yeh, Kuo-Wei, Ou, Liang-Shiou, Yao, Tsung-Chieh, Wu, Chao-Yi, Lin, Syh-Jae, Chen, Shih-Hsiang, Jaing, Tang-Her, Liang, Chi-Jou, and Kang, Chen-Chen

Subjects

*IMMUNOPHENOTYPING, *LYMPHOPROLIFERATIVE disorders, *PRIMARY immunodeficiency diseases, *INFLAMMATORY bowel diseases

Abstract

Lymphoproliferative disorders (LPD) comprise a heterogeneous group and are originally classified into the "Disease of immune dysregulation" category. Of 96 Taiwanese patients during 2003–2022, 31 (median 66, range 0.03–675 months) developed LPD, mainly including palpable lymphadenopathy (in 10 patients), intestinal lymphadenopathy associated with refractory inflammatory bowel disease (IBD in 8) and hepatosplenomegaly (in 7) during long-term follow-up (median 144, range 3–252 months). They distributed in the categories of antibody deficiency (2 CVID, 2 TTC37 , PIK3CD , PIK3R1 and AICDA each), phagocyte (4 CYBB , 1 STAT1 and 1 IFNRG1), immune dysregulation (2 FOXP3 , 2 XIAP and 2 HLH), combined immunodeficiencies (2 IL2RG ; CD40L , ZAP70 and unknown each), syndromic features (2 STAT3 -LOF, 1 WAS and 1 ATM) and three with anti-IFN-γ autoantibodies. An increased senescent (CD8 + CD57+) and CD21-low, disturbed transitional B (CD38 + IgM++), plasmablast B (CD38++IgM-), memory B (CD19 + CD27+) and T EMRA (CD27-IgD-) components were often observed in cross-sectional immunophenotyping and trended to develop LPD. • Approximate one third (31/96) Taiwanese patients developed lymphoproliferative disorders (LPD). • Palpable lymphadenopathy, intestinal lymphadenopathy associated with refractory inflammatory bowel disease (IBD) and hepatosplenomegaly were common in the LPD. • An increased senescent and CD21-low components, and disturbed transitional, plasamablast, memory B and T EMRA components were often observed in these patients. [ABSTRACT FROM AUTHOR]

Published

2024

30. Adaptive Immunity: Antigen Recognition by T and B Lymphocytes

Author

Kavathas, Paula B., Krause, Peter J., Ruddle, Nancy H., Krause, Peter J., editor, Kavathas, Paula B., editor, and Ruddle, Nancy H., editor

Published

2019

31. Exhausted NK cells and cytokine storms in COVID-19: Whether NK cell therapy could be a therapeutic choice.

Author

Ghasemzadeh, Mehran, Ghasemzadeh, Alireza, and Hosseini, Ehteramolsadat

Subjects

*KILLER cells, *CYTOKINE release syndrome, *CELLULAR therapy, *COVID-19, *VIRUS diseases, *INFECTION, *THYROID crisis

Abstract

• SARS-CoV-2 subtly disrupts the equations of immune responses in COVID-19 patients. • The virus activates infected macrophages and CD4+ T cells to induce cytokine storm. • Cytokine storm and direct interaction of viruses inhibit NK cell cytolytic effect. • Exhausted NK cell fails to lyse infected cells to avoid their unleashed cytokine release. • Adoptive transfer of cytolytic NK cell may reduce cytokine storm while decreasing viral load. The global outbreak of coronavirus-2019 (COVID-19) still claims more lives daily around the world due to the lack of a definitive treatment and the rapid tendency of virus to mutate, which even jeopardizes vaccination efficacy. At the forefront battle against SARS-CoV-2, an effective innate response to the infection has a pivotal role in the initial control and treatment of disease. However, SARS-CoV-2 subtly interrupts the equations of immune responses, disrupting the cytolytic antiviral effects of NK cells, while seriously activating infected macrophages and other immune cells to induce an unleashed "cytokine storm", a dangerous and uncontrollable inflammatory response causing life-threatening symptoms in patients. Notably, the NK cell exhaustion with ineffective cytolytic function against the sources of exaggerated cytokine release, acts as an Achilles' heel which exacerbates the severity of COVID-19. Given this, approaches that improve NK cell cytotoxicity may benefit treatment protocols. As a suggestion, adoptive transfer of NK or CAR-NK cells with proper cytotolytic potentials and the lowest capacity of cytokine-release (for example CD56dim NK cells brightly express activating receptors), to severe COVID-19 patients may provide an effective cure especially in cases suffering from cytokine storms. More intriguingly, the ongoing evidence for persistent clonal expansion of NK memory cells characterized by an activating phenotype in response to viral infections, can benefit the future studies on vaccine development and adoptive NK cell therapy in COVID-19. Whether vaccinated volunteers or recovered patients can also be considered as suitable candidates for cell donation could be the subject of future research. [ABSTRACT FROM AUTHOR]

Published

2022

32. Evaluación de subpoblaciones linfocitarias en individuos seropositivos a Helicobacter pylori.

Author

Palacios Martínez, M., Nájera Medina, O., González López, M., Ramírez Navarro, K., Solís Chávez, P. C., and Gutiérrez Cárdenas, E. M.

Subjects

LYMPHOCYTE subsets, RURAL population, HELICOBACTER pylori, RURAL geography, CD8 antigen

Abstract

Copyright of Acta Universitaria is the property of Universidad de Guanajuato/Acta Universitaria and its content may not be copied or emailed to multiple sites or posted to a listserv without the copyright holder's express written permission. However, users may print, download, or email articles for individual use. This abstract may be abridged. No warranty is given about the accuracy of the copy. Users should refer to the original published version of the material for the full abstract. (Copyright applies to all Abstracts.)

Published

2022

33. Antigen-specific T helper cells and cytokine profiles predict intensity and longevity of cellular and humoral responses to SARS-CoV-2 booster vaccination.

Author

Page L, Dennehy K, Mueller K, Girl P, Loell E, Buijze H, Classen JM, Messmann H, Roemmele C, Hoffmann R, Wurster S, and Fuchs A

Subjects

Humans, Male, Adult, Female, Middle Aged, COVID-19 Vaccines immunology, Immunity, Cellular, Immunoglobulin G blood, Immunoglobulin G immunology, Vaccination, Cytokines metabolism, BNT162 Vaccine immunology, BNT162 Vaccine administration & dosage, Immunization, Secondary, COVID-19 immunology, COVID-19 prevention & control, SARS-CoV-2 immunology, Spike Glycoprotein, Coronavirus immunology, Immunity, Humoral, Antibodies, Viral blood, Antibodies, Viral immunology, T-Lymphocytes, Helper-Inducer immunology

Abstract

Introduction: Pre-existent pools of coronavirus-specific or cross-reactive T cells were shown to shape the development of cellular and humoral immune responses after primary mRNA vaccination against SARS-CoV-2. However, the cellular determinants of responses to booster vaccination remain incompletely understood. Therefore, we phenotypically and functionally characterized spike antigen-specific T helper (Th) cells in healthy, immunocompetent individuals and correlated the results with cellular and humoral immune responses to BNT162b2 booster vaccination over a six-month period., Methods: Blood of 30 healthy healthcare workers was collected before, 1, 3, and 6 months after their 3rd BNT162b2 vaccination. Whole blood was stimulated with spike peptides and analyzed using flow cytometry, a 13-plex cytokine assay, and nCounter-based transcriptomics., Results: Spike-specific IgG levels at 1 month after booster vaccination correlated with pre-existing CD154+CD69+IFN-γ+CD4+ effector memory cells as well as spike-induced IL-2 and IL-17A secretion. Early post-booster (1-month) spike IgG levels (r=0.49), spike-induced IL‑2 (r=0.58), and spike-induced IFN‑γ release (r=0.43) correlated moderately with their respective long-term (6-month) responses. Sustained robust IgG responses were significantly associated with S-specific (CD69+±CD154+±IFN-γ+) Th-cell frequencies before booster vaccination (p=0.038), especially double/triple-positive type-1 Th cells. Furthermore, spike IgG levels, spike-induced IL‑2 release, and spike-induced IFN‑γ release after 6 months were significantly associated with increased IL‑2 & IL‑4, IP‑10 & MCP1, and IFN‑γ & IP‑10 levels at 1 month post-booster, respectively. On the transcriptional level, induction of pathways associated with both T-cell proliferation and antigen presentation was indicative of sustained spike-induced cytokine release and spike-specific IgG production 6 months post-booster. Using support vector machine models, pre-booster spike-specific T-cell frequencies and early post-booster cytokine responses predicted sustained (6-month) responses with F1 scores of 0.80-1.00., Discussion: In summary, spike-specific Th cells and T-cellular cytokine signatures present before BNT162b2 booster vaccination shape sustained adaptive cellular and humoral responses post-booster. Functional T-cell assays might facilitate early identification of potential non-responders., Competing Interests: The authors declare that the research was conducted in the absence of any commercial or financial relationships that could be construed as a potential conflict of interest., (Copyright © 2024 Page, Dennehy, Mueller, Girl, Loell, Buijze, Classen, Messmann, Roemmele, Hoffmann, Wurster and Fuchs.)

Published

2024

34. Memory Cells

Author

Vonk, Jennifer, editor and Shackelford, Todd K., editor

Published

2022

35. SARS-CoV-2 Vaccine Induced Atypical Immune Responses in Antibody Defects: Everybody Does their Best.

Author

Salinas, Ane Fernandez, Mortari, Eva Piano, Terreri, Sara, Quintarelli, Concetta, Pulvirenti, Federica, Di Cecca, Stefano, Guercio, Marika, Milito, Cinzia, Bonanni, Livia, Auria, Stefania, Romaggioli, Laura, Cusano, Giuseppina, Albano, Christian, Zaffina, Salvatore, Perno, Carlo Federico, Spadaro, Giuseppe, Locatelli, Franco, Carsetti, Rita, and Quinti, Isabella

Subjects

*COMMON variable immunodeficiency, *PRIMARY immunodeficiency diseases, *SARS-CoV-2, *ANTIBODY formation, *IMMUNE response

Abstract

Background: Data on immune responses to SARS-CoV-2 in patients with Primary Antibody Deficiencies (PAD) are limited to infected patients and to heterogeneous cohorts after immunization. Methods: Forty-one patients with Common Variable Immune Deficiencies (CVID), six patients with X-linked Agammaglobulinemia (XLA), and 28 healthy age-matched controls (HD) were analyzed for anti-Spike and anti-receptor binding domain (RBD) antibody production, generation of Spike-specific memory B-cells, and Spike-specific T-cells before vaccination and one week after the second dose of BNT162b2 vaccine. Results: The vaccine induced Spike-specific IgG and IgA antibody responses in all HD and in 20% of SARS-CoV-2 naive CVID patients. Anti-Spike IgG were detectable before vaccination in 4 out 7 CVID previously infected with SARS-CoV-2 and were boosted in six out of seven patients by the subsequent immunization raising higher levels than patients naïve to infection. While HD generated Spike-specific memory B-cells, and RBD-specific B-cells, CVID generated Spike-specific atypical B-cells, while RBD-specific B-cells were undetectable in all patients, indicating the incapability to generate this new specificity. Specific T-cell responses were evident in all HD and defective in 30% of CVID. All but one patient with XLA responded by specific T-cell only. Conclusion: In PAD patients, early atypical immune responses after BNT162b2 immunization occurred, possibly by extra-follicular or incomplete germinal center reactions. If these responses to vaccination might result in a partial protection from infection or reinfection is now unknown. Our data suggests that SARS-CoV-2 infection more effectively primes the immune response than the immunization alone, possibly suggesting the need for a third vaccine dose for patients not previously infected. [ABSTRACT FROM AUTHOR]

Published

2021

36. Different Types of Chronic Inflammation Engender Distinctive Immunosenescent Profiles in Affected Patients

Author

Eleni Moysidou, Georgios Lioulios, Aliki Xochelli, Vasiliki Nikolaidou, Michalis Christodoulou, Zoi Mitsoglou, Stamatia Stai, Asimina Fylaktou, Aikaterini Papagianni, and Maria Stangou

Subjects

end-stage kidney disease, systemic lupus erythematosus, lymphocytes, naïve cells, memory cells, senescence, Biology (General), QH301-705.5, Chemistry, QD1-999

Abstract

Immunosenescence encompasses a spectrum of lymphocyte phenotypic alterations. The aim of the study was to evaluate immunosenescent effect of two different forms of chronic inflammation, Systemic Lupus Erythematosous (SLE), a systemic autoimmune disease, and End-Stage Kidney Disease (ESKD), a chronic inflammatory disorder. Certain lymphocyte surface molecules, including CD31, CD45RA, CCR7, CD28, CD57, for T, and IgD, CD27 for B lymphocytes, were analyzed by flow cytometry in 30 SLE and 53 ESKD patients on hemodialysis (HD), and results were compared to 31 healthy controls (HC) of similar age, gender, and nationality. Significant Lymphopenia was evident in both SLE and ESKD-HD patients, compared to HC, affecting B cells 75.4 (14.4–520.8), 97 (32–341), and 214 (84–576) cells/μL, respectively, p < 0.0001, and CD4 cells 651.2 (71.1–1478.2), 713 (234–1509), and 986 (344–1591) cells/μL, respectively, p < 0.0001. The allocation of B cell subpopulations was remarkably different between SLE and ESKD-HD patients. SLE showed a clear shift to senescence (CD19IgD-CD27−) cells, compared to ESKD-HD and HC, 11.75 (10)% vs. 8 (6) vs. 8.1 (10), respectively. Regarding T lymphocytes, Central Memory CD8 cells predominated in both SLE and ESKD-HD patients compared to HC, 53 (50)%, 52 (63), and 24 (64)%, respectively, while ESKD-HD but not SLE patients also had increased expression of CD4CD28− and CD8CD28− cells. In conclusion, both diseases are followed by significant lymphopenia; however, the senescent phenomenon affects the B lymphocyte compartment in SLE patients and T lymphocytes in ESKD-HD patients.

Published

2022

37. Effects of Teriflunomide on B Cell Subsets in MuSK-Induced Experimental Autoimmune Myasthenia Gravis and Multiple Sclerosis.

Author

Yilmaz, Vuslat, Ulusoy, Canan, Hajtovic, Sabastian, Turkoglu, Recai, Kurtuncu, Murat, Tzartos, John, Lazaridis, Konstantinos, and Tuzun, Erdem

Subjects

*MYASTHENIA gravis, *B cells, *MULTIPLE sclerosis, *PLASMA cells, *PROTEIN-tyrosine kinases, *MYONEURAL junction, *ANTIGENS

Abstract

Antigen-specific immune responses are crucially involved in both multiple sclerosis (MS) and myasthenia gravis (MG). Teriflunomide is an immunomodulatory agent approved for treatment of MS through inhibition of lymphocyte proliferation. MG associated with muscle-specific tyrosine kinase (MuSK) antibodies often manifests with a severe disease course, prompting development of effective treatment methods. To evaluate whether teriflunomide treatment may ameliorate MuSK-autoimmunity, experimental autoimmune MG (EAMG) was induced by immunizing C57BL/6 (B6) mice three times with MuSK in complete Freund's adjuvant (CFA) (n = 17). MuSK-immunized mice were treated daily with teriflunomide (n = 8) or PBS (n = 9) starting from the third immunization (week 8) to termination (week 14). Clinical severity of EAMG was monitored. Immunological alterations were evaluated by measurement of anti-MuSK IgG, neuromuscular junction deposits, and flow cytometric analysis of lymph node cells. In MS patients under teriflunomide treatment, the peripheral blood B cell subset profile was analyzed. B6 mice treated with teriflunomide displayed relatively preserved body weight, lower EAMG prevalence, reduced average clinical grades, higher inverted screen scores, diminished anti-MuSK antibody and NMJ deposit levels. Amelioration of EAMG findings was associated with reduced memory B cell ratios in the lymph nodes. Similarly, MS patients under teriflunomide treatment showed reduced memory B cell, plasma cell, and plasmablast ratios. Teriflunomide treatment has effectively ameliorated MuSK-autoimmunity and thus may putatively be used in long-term management of MuSK-MG as an auxiliary treatment method. Teriflunomide appears to exert beneficial effects through inhibition of effector B cells. [ABSTRACT FROM AUTHOR]

Published

2021

38. Coronavirus infection: An immunologists' perspective.

Author

De Sanctis, Juan Bautista, García, Alexis Hipólito, Moreno, Dolores, and Hajduch, Marián

Subjects

*COVID-19, *SARS disease, *IMMUNOLOGISTS, *VIRUS diseases

Abstract

Coronavirus infections are frequent viral infections in several species. As soon as the severe acute respiratory syndrome (SARS) appeared in the early 2000s, most of the research focused on pulmonary disease. However, disorders in immune response and organ dysfunctions have been documented. Elderly individuals with comorbidities exhibit worse outcomes in all the coronavirus that cause SARS. Disease severity in SARS‐CoV‐2 infection is related to severe inflammation and tissue injury, and effective immune response against the virus is still under analysis. ACE2 receptor expression and polymorphism, age, gender and immune genetics are factors that also play an essential role in patients' clinical features and immune responses and have been partially discussed. The present report aims to review the physiopathology of SARS‐CoV‐2 infection and propose new research topics to understand the complex mechanisms of viral infection and viral clearance. [ABSTRACT FROM AUTHOR]

Published

2021

39. A prognostic model for SARS-CoV-2 breakthrough infection: Analyzing a prospective cellular immunity cohort.

Author

Yang, Mei, Meng, Yuan, Hao, Wudi, Zhang, Jin, Liu, Jianhua, Wu, Lina, Lin, Baoxu, Liu, Yong, Zhang, Yue, Yu, Xiaojun, Wang, Xiaoqian, gong, Yu, Ge, Lili, Fan, Yan, Xie, Conghong, Xu, Yiyun, Chang, Qing, Zhang, Yixiao, and Qin, Xiaosong

Subjects

*BREAKTHROUGH infections, *CELLULAR immunity, *B cells, *T cells, *MACHINE learning, *PROGNOSTIC models, *SARS-CoV-2, *IMMUNOLOGIC memory

Abstract

• Breakthrough infection of SARS-CoV-2 induces perturbations in cellular immunity. • After breakthrough infection with SARS-CoV-2, there was a decrease in effector T cells and an increase in naïve T cells. • The assessment of cellular immunity prior to breakthrough infection can serve as a prognostic tool for SARS-CoV-2 infection. • TNF-α, CD27-CD19+cells, and T EMRA subsets were identified as high predictors in prognostic models of SARS-CoV-2 infection. Following the COVID-19 pandemic, studies have identified several prevalent characteristics, especially related to lymphocyte subsets. However, limited research is available on the focus of this study, namely, the specific memory cell subsets among individuals who received COVID-19 vaccine boosters and subsequently experienced a SARS-CoV-2 breakthrough infection. Flow cytometry (FCM) was employed to investigate the early and longitudinal pattern changes of cellular immunity in patients with SARS-CoV-2 breakthrough infections following COVID-19 vaccine boosters. XGBoost (a machine learning algorithm) was employed to analyze cellular immunity prior to SARS-CoV-2 breakthrough, aiming to establish a prognostic model for SARS-CoV-2 breakthrough infections. Following SARS-CoV-2 breakthrough infection, naïve T cells and T EMRA subsets increased while the percentage of T CM and T EM cells decreased. Naïve and non-switched memory B cells increased while switched and double-negative memory B cells decreased. The XGBoost model achieved an area under the curve (AUC) of 0.78, with an accuracy rate of 81.8 %, a sensitivity of 75 %, and specificity of 85.7 %. TNF-α, CD27-CD19+cells, and T EMRA subsets were identified as high predictors. An increase in TNF-α, cTfh, double-negative memory B cells, IL-6, IL-10, and IFN-γ prior to SARS-CoV-2 infection was associated with enduring clinical symptoms; conversely, an increase in CD3+ T cells, CD4+ T cells, and IL-2 was associated with clinical with non-enduring clinical symptoms. SARS-CoV-2 breakthrough infection leads to disturbances in cellular immunity. Assessing cellular immunity prior to breakthrough infection serves as a valuable prognostic tool for SARS-CoV-2 infection, which facilitates clinical decision-making. [ABSTRACT FROM AUTHOR]

Published

2024

40. Viral rebound occurrence immediately after drug discontinuation involving neither drug resistance nor latent reservoir.

Author

Hayashi, Rena, Hara, Akane, and Iwasa, Yoh

Subjects

*CYTOTOXIC T cells, *DRUG resistance, *ANTIVIRAL agents, *IMMUNOLOGIC memory, *VIRAL load, *DRUG administration

Abstract

Some viruses exhibit "rebound" when the administration of antiviral drugs is discontinued. Viral rebound caused by resistance mutations or latent reservoirs has been studied mathematically. In this study, we investigated the viral rebound due to other causes. Since immunity is weaker during antiviral treatment than without the treatment, drug discontinuation may lead to an increase in the viral load. We analyzed the dynamics of the number of virus-infected cells, cytotoxic T lymphocytes, and memory cells and identified the conditions under which the viral load increased upon drug discontinuation. If drug is administered for an extended period, a viral rebound occurs when the ratio of viral growth rate in the absence to that in the presence of the antiviral drug exceeds the "rebound threshold." We analyzed how the rebound threshold depended on the patient's conditions and the type of treatment. Mathematical and numerical analyses revealed that rebound after discontinuation was more likely to occur when the drug effectively reduced viral proliferation, drug discontinuation was delayed, and the processes activating immune responses directly were stronger than those occurring indirectly through immune memory formation. We discussed additional reasons for drugs to cause viral rebound more likely. [ABSTRACT FROM AUTHOR]

Published

2024

41. Assessment of the Mitochondrial Condition in CD4+ and CD8+ T-Lymphocytes from Healthy Subjects

Author

Korolevskaya, L. B., Saidakova, E. V., Shmagel, N. G., and Shmagel, K. V.

Published

2022

42. Detecting specific memory t and b cells in volunteers annually revaccinated with live anthrax vaccine

Author

V. V. Firstova, A. S. Kartseva, M. V. Silkina, M. A. Marin, Ia. O. Muntian, A. K. Ryabko, and I. G. Shemyakin

Subjects

memory cells, anthrax, flow cytometry, vaccine, antibodies, lethal toxin, protective antigen, Infectious and parasitic diseases, RC109-216

Abstract

Currently, live anthrax vaccine has been used for vaccine prophylaxis in Russia and neighbor countries for seve ral decades, but precise mechanism of post-vaccination protection mechanism remains unclear. Here, we provide data on examining serum antibody level against protective antigen (PA) and lethal factor (LF) in repeatedly vaccinated volun teers at early stage (5–8 days) and 1 month after the performing pre-scheduled annual revaccination. Amount of peripheral blood antigen-specific memory T cells after previous vaccinations was analyzed. It was showed that frequency of CD3+CD45RO+CD62L– memory effector T cells was increased in the majority of volunteers on day 5-8 day after performing pre-scheduled annual revaccination that peaked at day 7 by elevating it by 2-fold compared with the control group. Percentage of anthrax-specific central memory T cells did not increase at early stage after vaccination, whereas amount of activated CD3+CD45RO+CD62L+HLA-DR+ subset within this memory T cell population was increased. Likewise, percentage of activated CD3+CD45RO+CD62L–HLA-DR+ effector memory T cell subset was also increased. Moreover, serum anti-PA IgG were detected on day 5–8 day after pre-scheduled annual revaccination in half of volunteers, whereas anti-LF IgG were found only in a single volunteer. Rapidly elevated amount of serum anthrax-specific IgG antibodies evidences about sustained memory B cell response in peripheral blood samples in volunteers after pre-scheduled annual revaccination. However, percentage of CD19+CD27+ memory B cells was not significantly elevated at early stage after revaccination that tended to increase. Both helper and cytotoxic T cell subsets were activated on day 5–8 after revaccination revealed by upregulated expression of CD69 and/or CD25 markers, with the latter predominantly found on helper T cells, thereby accounting for their high proliferative activity, whereas the former — on cytotoxic T cell subsets. Detection of anti-PA IgG antibodies correlates with protection against anthrax, which was confirmed in animal models. Unfortunately, the level of serum anti-PA IgG antibodies rapidly declines after vaccination. Ability of memory B cells to rapidly trigger production of anthrax-specific antibodies in response to revaccination suggests that anti-anthrax immunity may be evaluated by measuring frequency of peripheral blood anthrax-specific memory B and T cells.

Published

2019

43. Evaluation of applicability of small silver nanoparticles as the cells of PCM memory

Author

Yu.Ya. Gafner, D.A. Bashkova, S.L. Gafner, and L.V. Redel

Subjects

phase transition, memory cells, silver, nanoclusters, Physical and theoretical chemistry, QD450-801

Abstract

In this paper, one of the aspects of using metallic nanoclusters was considered, namely the use of silver nanoparticles as separate bits of information in memory devices based on the phase-change memory (PCM) method. The basic principle of this approach is that to locally change the phase state of a memory cell from crystalline to amorphous, keep this phase as long as you like and, if necessary, and return the material to its original crystalline state. Based on the results of simulation of silver nanostructures, it was concluded that their use as a memory element based on phase transitions is allowed, but with a particle size limitation exceeding 8.0 nm.

Published

2018

44. Using nanoparticles of Ag-Cu alloy as separate bits of PCM memory

Author

Yu.Ya. Gafner, D.A. Bashkova, and S.L. Gafner

Subjects

phase transition, memory cells, silver, copper, nanoclusters, Physical and theoretical chemistry, QD450-801

Abstract

One of the promising areas of application of metallic nanoparticles is the creation of devices on their basis with a high information recording density that generates interest in the study of their magnetic, optical and structural-phase properties. In this paper, one of the aspects of using metallic nanoclusters. Namely we mean the use of silver-copper nanoparticles as separate bits of information in memory devices based on the phase-change memory.

Published

2018

45. Nanostructures as a material for phase-inverse memory

Author

Yu.Ya. Gafner, S.L. Gafner, and L.V. Redel

Subjects

phase transition, memory cells, nanostructures, Physical and theoretical chemistry, QD450-801

Abstract

Despite on long researches, chalcogenide alloys are still generally used in the contemporary PCM layouts as the operating layer material undergoing structural transformations. However, the evolution of the technique aimed at the creation of new non-volatile arrays of information requires different technical solutions. First of all, it deals with the reduction of one bit storage area to several nanometers and reduction of the access time, in particular the possible application in the PCM memory of small metallic nanoclusters.

Published

2018

46. Göttingen Minipigs as a Model to Evaluate Longevity, Functionality, and Memory of Immune Response Induced by Pertussis Vaccines

Author

Céline Vaure, Véronique Grégoire-Barou, Virginie Courtois, Emilie Chautard, Cyril Dégletagne, and Yuanqing Liu

Subjects

Göttingen minipigs, longitudinal study, pertussis vaccines, antibody response, T helper polarization, memory cells, Immunologic diseases. Allergy, RC581-607

Abstract

Evaluation of the short-term and long-term immunological responses in a preclinical model that simulates the targeted age population with a relevant vaccination schedule is essential for human vaccine development. A Göttingen minipig model was assessed, using pertussis vaccines, to demonstrate that vaccine antigen-specific humoral and cellular responses, including IgG titers, functional antibodies, Th polarization and memory B cells can be assessed in a longitudinal study. A vaccination schedule of priming with a whole cell (DTwP) or an acellular (DTaP) pertussis vaccine was applied in neonatal and infant minipigs followed by boosting with a Tdap acellular vaccine. Single cell RNAsequencing was used to explore the long-term maintenance of immune memory cells and their functionality for the first time in this animal model. DTaP but not DTwP vaccination induced pertussis toxin (PT) neutralizing antibodies. The cellular immune response was also characterized by a distinct Th polarization, with a Th-2-biased response for DTaP and a Th-1/Th-17-biased response for DTwP. No difference in the maintenance of pertussis-specific memory B cells was observed in DTaP- or DTwP-primed animals 6 months post Tdap boost. However, an increase in pertussis-specific T cells was still observed in DTaP primed minipigs, together with up-regulation of genes involved in antigen presentation and interferon pathways. Overall, the minipig model reproduced the humoral and cellular immune responses induced in humans by DTwP vs. DTaP priming, followed by Tdap boosting. Our data suggest that the Göttingen minipig is an attractive preclinical model to predict the long-term immunogenicity of human vaccines against Bordetella pertussis and potentially also vaccines against other pathogens.

Published

2021

47. Basic Immunobiology

Author

Parker, George A., Papenfuss, Tracey L., DeWitt, Jamie, Series editor, and Parker, George A., editor

Published

2017

48. Göttingen Minipigs as a Model to Evaluate Longevity, Functionality, and Memory of Immune Response Induced by Pertussis Vaccines.

Author

Vaure, Céline, Grégoire-Barou, Véronique, Courtois, Virginie, Chautard, Emilie, Dégletagne, Cyril, and Liu, Yuanqing

Subjects

IMMUNOLOGIC memory, WHOOPING cough vaccines, IMMUNE response, DPT vaccines, HUMORAL immunity

Abstract

Evaluation of the short-term and long-term immunological responses in a preclinical model that simulates the targeted age population with a relevant vaccination schedule is essential for human vaccine development. A Göttingen minipig model was assessed, using pertussis vaccines, to demonstrate that vaccine antigen-specific humoral and cellular responses, including IgG titers, functional antibodies, Th polarization and memory B cells can be assessed in a longitudinal study. A vaccination schedule of priming with a whole cell (DTwP) or an acellular (DTaP) pertussis vaccine was applied in neonatal and infant minipigs followed by boosting with a Tdap acellular vaccine. Single cell RNAsequencing was used to explore the long-term maintenance of immune memory cells and their functionality for the first time in this animal model. DTaP but not DTwP vaccination induced pertussis toxin (PT) neutralizing antibodies. The cellular immune response was also characterized by a distinct Th polarization, with a Th-2-biased response for DTaP and a Th-1/Th-17-biased response for DTwP. No difference in the maintenance of pertussis-specific memory B cells was observed in DTaP- or DTwP-primed animals 6 months post Tdap boost. However, an increase in pertussis-specific T cells was still observed in DTaP primed minipigs, together with up-regulation of genes involved in antigen presentation and interferon pathways. Overall, the minipig model reproduced the humoral and cellular immune responses induced in humans by DTwP vs. DTaP priming, followed by Tdap boosting. Our data suggest that the Göttingen minipig is an attractive preclinical model to predict the long-term immunogenicity of human vaccines against Bordetella pertussis and potentially also vaccines against other pathogens. [ABSTRACT FROM AUTHOR]

Published

2021

49. Cell‐mediated and humoral adaptive immune responses to SARS‐CoV‐2 are lower in asymptomatic than symptomatic COVID‐19 patients.

Author

Mazzoni, Alessio, Maggi, Laura, Capone, Manuela, Spinicci, Michele, Salvati, Lorenzo, Colao, Maria Grazia, Vanni, Anna, Kiros, Seble Tekle, Mencarini, Jessica, Zammarchi, Lorenzo, Mantengoli, Elisabetta, Menicacci, Lorenzo, Caldini, Eleonora, Romagnani, Sergio, Liotta, Francesco, Morettini, Alessandro, Rossolini, Gian Maria, Bartoloni, Alessandro, Cosmi, Lorenzo, and Annunziato, Francesco

Subjects

HUMORAL immunity, COVID-19, SARS-CoV-2, IMMUNOLOGIC memory, IMMUNOGLOBULIN A

Abstract

The characterization of cell‐mediated and humoral adaptive immune responses to SARS‐CoV‐2 is fundamental to understand COVID‐19 progression and the development of immunological memory to the virus. In this study, we detected T‐cells reactive to SARS‐CoV‐2 proteins M, S, and N, as well as serum virus‐specific IgM, IgA, IgG, in nearly all SARS‐CoV‐2 infected individuals, but not in healthy donors. Virus‐reactive T cells exhibited signs of in vivo activation, as suggested by the surface expression of immune‐checkpoint molecules PD1 and TIGIT. Of note, we detected antigen‐specific adaptive immune response both in asymptomatic and symptomatic SARS‐CoV‐2 infected subjects. More importantly, symptomatic patients displayed a significantly higher magnitude of both cell‐mediated and humoral adaptive immune response to the virus, as compared to asymptomatic individuals. These findings suggest that an uncontrolled adaptive immune response contribute to the development of the life‐threatening inflammatory phase of the disease. Finally, this study might open the way to develop effective vaccination strategies. [ABSTRACT FROM AUTHOR]

Published

2020

50. CD8 T-Cell Induction against Vascular Endothelial Growth Factor Receptor 2 by Salmonella for Vaccination Purposes against a Murine Melanoma

Author

Jellbauer, Stefan, Panthel, Klaus, Hetrodt, Justin H., and Russmann, Holger

Subjects

iii secretion system, stem-like cells, antigen delivery, tumor-growth, selective expression, bacterial-infection, memory cells, host-cells, angiogenesis, immunotherapy

Abstract

The Salmonella type III secretion system (T3SS) efficiently translocates heterologous proteins into the cytosol of eukaryotic cells. This leads to an antigen-specific CD8 T-cell induction in mice orally immunized with recombinant Salmonella. Recently, we have used Salmonella's T3SS as a prophylactic and therapeutic intervention against a murine fibrosarcoma. In this study, we constructed a recombinant Salmonella strain translocating the immunogenic H-2Db-specific CD8 T-cell epitope VILTNPISM (KDR2) from the murine vascular endothelial growth factor receptor 2 (VEGFR2). VEGFR2 is a member of the tyrosine protein kinase family and is upregulated on proliferating endothelial cells of the tumor vasculature. After single orogastric vaccination, we detected significant numbers of KDR2-tetramer-positive CD8 T cells in the spleens of immunized mice. The efficacy of these cytotoxic T cells was evaluated in a prophylactic setting to protect mice from challenges with B16F10 melanoma cells in a flank tumor model, and to reduce dissemination of spontaneous pulmonary melanoma metastases. Vaccinated mice revealed a reduction of angiogenesis by 62% in the solid tumor and consequently a significant decrease of tumor growth as compared to non-immunized mice. Moreover, in the lung metastasis model, immunization with recombinant Salmonella resulted in a reduction of the metastatic melanoma burden by approximately 60%.

Published

2012