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4. Direct and indirect effects of Puumala hantavirus on platelet function

Author

Waltraud, Schrottmaier, Schmuckenschlager, Anna, Thunberg, Therese, Wigren, Julia, Fors Connolly, Anne-Marie, Assinger, Alice, Ahlm, Clas, Forsell, Mattias N. E., Waltraud, Schrottmaier, Schmuckenschlager, Anna, Thunberg, Therese, Wigren, Julia, Fors Connolly, Anne-Marie, Assinger, Alice, Ahlm, Clas, and Forsell, Mattias N. E.

Abstract

Thrombocytopenia is a cardinal symptom of hantavirus-induced diseases including Puumala virus (PUUV)-induced hemorrhagic fever with renal syndrome (HFRS), which is associated with impaired platelet function, bleeding manifestations and augmented thrombotic risk. However, the underlying mechanisms causing thrombocytopenia and platelet hypo-responsiveness are unknown. Thus, we investigated the direct and indirect impact of PUUV on platelet production, function and degradation. Analysis of PUUV-HFRS patient blood revealed that platelet hypo-responsiveness in PUUV infection was cell-intrinsic and accompanied by reduced platelet-leukocyte aggregates (PLAs) and upregulation of monocyte tissue factor (TF), whereas platelet vasodilator-stimulated phosphoprotein (VASP) phosphorylation was comparable to healthy controls. Plasma CXCL4 levels followed platelet count dynamics throughout disease course. PUUV activated both neutrophils and monocytes in vitro, but platelet desialylation, degranulation and GPIIb/IIIa activation as well as PLA formation and endothelial adhesion under flow remained unaltered in the presence of PUUV. Further, MEG-01 megakaryocytes infected with PUUV displayed unaltered polyploidization, expression of surface receptors and platelet production. However, infection of endothelial cells with PUUV significantly increased platelet sequestration. Our data thus demonstrate that although platelet production, activation or degradation are not directly modulated, PUUV indirectly fosters thrombocytopenia by sequestration of platelets to infected endothelium. Upregulation of immunothrombotic processes in PUUV-HFRS may further contribute to platelet dysfunction and consumption. Given the pathophysiologic similarities of hantavirus infections, our findings thus provide important insights into the mechanisms underlying thrombocytopenia and highlight immune-mediated coagulopathy as potential therapeutic target.

Published
2024
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5. Modulation of innate immune response to mRNA vaccination after SARS-CoV-2 infection or sequential vaccination in humans

Author

Hellgren, Fredrika, Rosdahl, Anja, Cerveira, Rodrigo Arcoverde, Lenart, Klara, Ols, Sebastian, Yongdae, Gwon, Kurt, Seta, Delis, Anna Maria, Joas, Gustav, Evander, Magnus, Normark, Johan, Ahlm, Clas, Forsell, Mattias N. E., Cajander, Sara, Loré, Karin, Hellgren, Fredrika, Rosdahl, Anja, Cerveira, Rodrigo Arcoverde, Lenart, Klara, Ols, Sebastian, Yongdae, Gwon, Kurt, Seta, Delis, Anna Maria, Joas, Gustav, Evander, Magnus, Normark, Johan, Ahlm, Clas, Forsell, Mattias N. E., Cajander, Sara, and Loré, Karin

Abstract

mRNA vaccines are likely to become widely used for the prevention of infectious diseases in the future. Nevertheless, a notable gap exists in mechanistic data, particularly concerning the potential effects of sequential mRNA immunization or preexisting immunity on the early innate immune response triggered by vaccination. In this study, healthy adults, with or without documented prior SARS-CoV-2 infection, were vaccinated with the BNT162b2/Comirnaty mRNA vaccine. Prior infection conferred significantly stronger induction of proinflammatory and type I IFN-related gene signatures, serum cytokines, and monocyte expansion after the prime vaccination. The response to the second vaccination further increased the magnitude of the early innate response in both study groups. The third vaccination did not further increase vaccine-induced inflammation. In vitro stimulation of PBMCs with TLR ligands showed no difference in cytokine responses between groups, or before or after prime vaccination, indicating absence of a trained immunity effect. We observed that levels of preexisting antigen-specific CD4 T cells, antibody, and memory B cells correlated with elements of the early innate response to the first vaccination. Our data thereby indicate that preexisting memory formed by infection may augment the innate immune activation induced by mRNA vaccines.

Published
2024
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6. Intravenous immunoglobulin therapy for COVID-19 in immunocompromised patients : A retrospective cohort study

Author

Gröning, Remigius, Walde, Jonatan, Ahlm, Clas, Forsell, Mattias N. E., Normark, Johan, Rasmuson, Johan, Gröning, Remigius, Walde, Jonatan, Ahlm, Clas, Forsell, Mattias N. E., Normark, Johan, and Rasmuson, Johan

Abstract

Objectives: To investigate the effectiveness of intravenous immunoglobulin (IVIG) as treatment for COVID-19 in immunocompromised patients. Methods: This retrospective study investigated outcomes for immunocompromised, vaccine non-responsive, patients that between September 2022 and April 2023 received IVIG as treatment for COVID-19 in the region of Västerbotten, Sweden. We analyzed clinical data, viral load, and anti-SARS-CoV-2 IgG binding and neutralization levels of patient serum samples and IVIG production batches. Primary and secondary outcomes were clinical cure and viral clearance, respectively. Results: Sixteen patients were analyzed. After a median COVID-19 duration of 4 weeks, a median 60 g IVIG infusion increased SARS-CoV-2 binding and neutralizing antibody levels, with broad in vitro activity against tested variants. The treatment resulted in abrogation of viremia in all patients and general improvement in 15 survivors that all met the primary endpoint. Thirteen patients met the secondary endpoint at follow-up after a median of four months. Two subjects with persistent SARS-CoV-2 carriage relapsed but were successfully retreated with IVIG. Conclusions: Antibodies in IVIG efficiently neutralized several SARS-CoV-2 variants. Treatment with IVIG was associated with clinical cure and viral clearance in immunocompromised patients. Our data suggests that IVIG could be a novel treatment alternative for COVID-19 for this patient category.

Published
2024
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7. Olfactory dysfunction as an early predictor for post-COVID condition at 1-year follow-up

Author

Granvik, Christoffer, Andersson, Sara, Andersson, Linus, Brorsson, Camilla, Forsell, Mattias N. E., Ahlm, Clas, Normark, Johan, Edin, Alicia, Granvik, Christoffer, Andersson, Sara, Andersson, Linus, Brorsson, Camilla, Forsell, Mattias N. E., Ahlm, Clas, Normark, Johan, and Edin, Alicia

Abstract

Background: Olfactory dysfunction together with neurological and cognitive symptoms are common after COVID-19. We aimed to study whether performance on olfactory and neuropsychological tests following infection predict post-COVID condition (PCC), persisting symptoms, and reduced health-related quality of life. Methods: Both hospitalized (N = 10) and non-hospitalized individuals (N = 56) were enrolled in this prospective cohort study. Participants were evaluated 1–3 months after infection with an olfactory threshold test and neuropsychological tests, which was used as predictors of PCC. A questionnaire outlining persisting symptoms and the validated instrument EuroQol five-dimension five-level for health-related quality of life assessment were used as outcome data 1 year after infection (N = 59). Principal component analysis was used to identify relevant predictors for PCC at 1 year. Results: Objectively assessed olfactory dysfunction at 1–3 months post infection, but not subjective olfactory symptoms, predicted post-COVID condition with reduced health-related quality of life (PCC+) at 1 year. The PCC+ group scored more often below the cut off for mild cognitive impairment on the Montreal Cognitive Assessment (61.5% vs. 21.7%) and higher on the Multidimensional Fatigue Inventory-20, compared to the group without PCC+. Conclusion: Our results indicate that objectively assessed, olfactory dysfunction is a predictor for PCC+. These findings underscore the importance of objective olfactory testing. We propose that olfactory screening in the early post-acute phase of COVID-19 infection might identify individuals that are at higher risk of developing long-term health sequalae.

Published
2024
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8. SARS-CoV-2 infection induces hyaluronan production in vitro and hyaluronan levels in COVID-19 patients relate to morbidity and long-term lung impairment : a prospective cohort study

Author

Hellman, Urban, Rosendal, Ebba, Lehrstrand, Joakim, Henriksson, Johan, Björsell, Tove, Wennemo, Alfred, Hahn, Max, Österberg, Björn, Dorofte, Luiza, Nilsson, Emma, Forsell, Mattias N. E., Smed-Sörensen, Anna, Lange, Anna, Karlsson, Mats, Ahlm, Clas, Blomberg, Anders, Cajander, Sara, Ahlgren, Ulf, Lind, Alicia, Normark, Johan, Överby, Anna K., Lenman, Annasara, Hellman, Urban, Rosendal, Ebba, Lehrstrand, Joakim, Henriksson, Johan, Björsell, Tove, Wennemo, Alfred, Hahn, Max, Österberg, Björn, Dorofte, Luiza, Nilsson, Emma, Forsell, Mattias N. E., Smed-Sörensen, Anna, Lange, Anna, Karlsson, Mats, Ahlm, Clas, Blomberg, Anders, Cajander, Sara, Ahlgren, Ulf, Lind, Alicia, Normark, Johan, Överby, Anna K., and Lenman, Annasara

Abstract

We previously demonstrated that the lungs of deceased COVID-19 patients were filled with a clear hydrogel consisting of hyaluronan (HA). In this translational study, we investigated the role of HA at all stages of COVID-19 disease to map the consequences of elevated HA on morbidity and identify the mechanism of severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2)-induced HA production. A reduced alveolar surface area was observed in the lungs of deceased COVID-19 patients compared to healthy controls, as visualized by a 3D rendering of lung morphology using light-sheet fluorescence microscopy. We confirmed the presence of HA in lung biopsies and found large quantities of proinflammatory fragmented HA. The association of systemic HA in blood plasma and disease severity was assessed in patients with mild (WHO Clinical Progression Scale, WHO-CPS, 1-5) and severe COVID-19 (WHO-CPS, 6-9) during the acute and convalescent phases and related to lung function. We found that systemic levels of HA were high during acute COVID-19 disease, remained elevated during convalescence, and were associated with a reduced diffusion capacity. In vitro 3D-lung models, differentiated from primary human bronchial epithelial cells, were used to study the effects of SARS-CoV-2 infection on HA metabolism, and transcriptomic analyses revealed a dysregulation of HA synthases and hyaluronidases, both contributing to increased HA in apical secretions. Furthermore, corticosteroid treatment reduced the inflammation and downregulated HA synthases. Our findings demonstrate that HA plays a role in COVID-19 morbidity and that sustained elevated HA concentrations may contribute to long-term respiratory impairment.IMPORTANCEThis study provides insights into the role of hyaluronan (HA) in the severity and long-term impact of COVID-19 on lung function. Through extensive morphological examination of lung tissues and a multicenter study, we identified that HA levels are significantly elevated in COVID, This study was supported by the Swedish Heart-Lung Foundation (20200385 to A.K.Ö. and A. Lenman, 20200325 and 20210078 to C.A., and 20200366 and 20210049 to A.B.), SciLife Lab COVID-19 research program funded by the Knut and Alice Wallenberg Foundation (2020.0182 and C19R:028 to A.K.Ö. and A. Lenman, and VC-2020-0015 to C.A.), Kempestiftelserna (grant no. JCK-1827 to A.K.Ö.), Umeå University and County Council of Västerbotten (#RV-938855 to C.A. and #RV-970074 to A.K.Ö.), Carl Bennet AB (A. Lenman), the Fundraising Foundation for Medical Research, Umeå University (978018 to A. Lenman and 964781 to U.H.), Nyckelfonden Örebro (OLL-938628 and OLL-961416 to S.C.) Regional Research Council Mid Sweden (RFR-968856 and RFR-940474 to S.C.), the Swedish Research Council (2020-06235 to M.N.E.F., 2016-06514 to J.N., and 2021-06602 to J.H.), Åke Wiberg’s foundation (M22-0106 to A. Lenman), Emil and Wera Cornell’s foundation (A. Lenman), and Magnus Bergvall's foundation (2022-186 to A. Lenman).

Published
2024
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9. Hybrid capture-based next-generation sequencing of new and old world Orthohantavirus strains and wild-type Puumala isolates from humans and bank voles

Author

Rosenbaum, William, Bovinder Ylitalo, Erik, Castel, Guillaume, Sjödin, Andreas, Larsson, Pär, Wigren Byström, Julia, Forsell, Mattias N. E., Ahlm, Clas, Pettersson, Lisa, Tuiskunen-Bäck, Anne, Rosenbaum, William, Bovinder Ylitalo, Erik, Castel, Guillaume, Sjödin, Andreas, Larsson, Pär, Wigren Byström, Julia, Forsell, Mattias N. E., Ahlm, Clas, Pettersson, Lisa, and Tuiskunen-Bäck, Anne

Abstract

Orthohantaviruses, transmitted primarily by rodents, cause hemorrhagic fever with renal syndrome (HFRS) in Eurasia and hantavirus pulmonary syndrome in the Americas. These viruses, with documented human-to-human transmission, exhibit a wide case-fatality rate, 0.5–40 %, depending on the virus species, and no vaccine or effective treatment for severe Orthohantavirus infections exists. In Europe, the Puumala virus (PUUV), carried by the bank vole Myodes glareolus, causes a milder form of HFRS. Despite the reliance on serology and PCR for diagnosis, the three genomic segments of Swedish wild-type PUUV have yet to be completely sequenced. We have developed a targeted hybrid-capture method aimed at comprehensive genomic sequencing of wild-type PUUV isolates and the identification of other Orthohantaviruses. Our custom-designed panel includes >11,200 probes covering the entire Orthohantavirus genus. Using this panel, we sequenced complete viral genomes from bank vole lung tissue, human plasma samples, and cell-cultured reference strains. Analysis revealed that Swedish PUUV isolates belong to the Northern Scandinavian lineage, with nucleotide diversity ranging from 2.8 % to 3.7 % among them. Notably, no significant genotypic differences were observed between the viral sequences from reservoirs and human cases except in the nonstructural protein. Despite the high endemicity of PUUV in Northern Sweden, these are the first complete Swedish wild-type PUUV genomes and substantially increase our understanding of PUUV evolution and epidemiology. The panel's sensitivity enables genomic sequencing of human samples with viral RNA levels reflecting the natural progression of infection and underscores our panel's diagnostic value, and could help to uncover novel Orthohantavirus transmission routes.

Published
2024
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10. SARS-CoV-2-related mortality decrease in nursing home residents given multiple COVID-19 boosters

Author

Blom, Kim, primary, Fjällström, Peter, additional, Molnár, Christian, additional, Åberg, Mikael, additional, Vikström, Linnea, additional, Wigren-Byström, Julia, additional, Bennet, Louise, additional, Widerström, Micael, additional, Rasmussen, Gunlög, additional, Klingström, Jonas, additional, Forsell, Mattias N E, additional, and Johansson, Anders F, additional

Published
2023
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11. Progress in vaccine development for infectious diseases—a Keystone Symposia report

Author

Cable, Jennifer, primary, Graham, Barney S., additional, Koup, Richard A., additional, Seder, Robert A., additional, Karikó, Katalin, additional, Pardi, Norbert, additional, Barouch, Dan H., additional, Sharma, Bhawna, additional, Rauch, Susanne, additional, Nachbagauer, Raffael, additional, Forsell, Mattias N. E., additional, Schotsaert, Michael, additional, Ellebedy, Ali H., additional, Loré, Karin, additional, Irvine, Darrell J., additional, Pilkington, Emily, additional, Tahtinen, Siri, additional, Thompson, Elizabeth A., additional, Feraoun, Yanis, additional, King, Neil P., additional, Saunders, Kevin, additional, Alter, Galit, additional, Moin, Syed M., additional, Sliepen, Kwinten, additional, Hedestam, Gunilla B. Karlsson, additional, Wardemann, Hedda, additional, Pulendran, Bali, additional, Doria‐Rose, Nicole A., additional, He, Wan‐Ting, additional, Juno, Jennifer A., additional, Ataca, Sila, additional, Wheatley, Adam K., additional, McLellan, Jason S., additional, Walker, Laura M., additional, Lederhofer, Julia, additional, Lindesmith, Lisa C., additional, Wille, Holger, additional, Hotez, Peter J., additional, and Bekker, Linda‐Gail, additional

Published
2023
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12. SARS-CoV-2-related mortality decrease in nursing home residents given multiple COVID-19 boosters

Author

Blom, Kim, Fjällström, Peter, Molnár, Christian, Åberg, Mikael, Vikström, Linnea, Wigren-Byström, Julia, Bennet, Louise, Widerström, Micael, Rasmussen, Gunlög, Klingström, Jonas, Forsell, Mattias N. E., Johansson, Anders F., Blom, Kim, Fjällström, Peter, Molnár, Christian, Åberg, Mikael, Vikström, Linnea, Wigren-Byström, Julia, Bennet, Louise, Widerström, Micael, Rasmussen, Gunlög, Klingström, Jonas, Forsell, Mattias N. E., and Johansson, Anders F.

Published
2023
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13. High prevalence of persistent symptoms and reduced health-related quality of life 6 months after COVID-19

Author

Ahmad, Irma, Edin, Alicia, Granvik, Christoffer, Persson, Lowa Kumm, Tevell, Staffan, Månsson, Emeli, Magnuson, Anders, Marklund, Ingela, Persson, Ida-Lisa, Kauppi, Anna, Ahlm, Clas, Forsell, Mattias N. E., Sundh, Josefin, Lange, Anna, Cajander, Sara, Normark, Johan, Ahmad, Irma, Edin, Alicia, Granvik, Christoffer, Persson, Lowa Kumm, Tevell, Staffan, Månsson, Emeli, Magnuson, Anders, Marklund, Ingela, Persson, Ida-Lisa, Kauppi, Anna, Ahlm, Clas, Forsell, Mattias N. E., Sundh, Josefin, Lange, Anna, Cajander, Sara, and Normark, Johan

Abstract

BackgroundThe long-term sequelae after COVID-19 constitute a challenge to public health and increased knowledge is needed. We investigated the prevalence of self-reported persistent symptoms and reduced health-related quality of life (HRQoL) in relation to functional exercise capacity, 6 months after infection, and explored risk factors for COVID-19 sequalae. MethodsThis was a prospective, multicenter, cohort study including 434 patients. At 6 months, physical exercise capacity was assessed by a 1-minute sit-to-stand test (1MSTST) and persistent symptoms were reported and HRQoL was evaluated through the EuroQol 5-level 5-dimension (EQ-5D-5L) questionnaire. Patients with both persistent symptoms and reduced HRQoL were classified into a new definition of post-acute COVID syndrome, PACS+. Risk factors for developing persistent symptoms, reduced HRQoL and PACS+ were identified by multivariable Poisson regression. ResultsPersistent symptoms were experienced by 79% of hospitalized, and 59% of non-hospitalized patients at 6 months. Hospitalized patients had a higher prevalence of self-assessed reduced overall health (28 vs. 12%) and PACS+ (31 vs. 11%). PACS+ was associated with reduced exercise capacity but not with abnormal pulse/desaturation during 1MSTST. Hospitalization was the most important independent risk factor for developing persistent symptoms, reduced overall health and PACS+. ConclusionPersistent symptoms and reduced HRQoL are common among COVID-19 survivors, but abnormal pulse and peripheral saturation during exercise could not distinguish patients with PACS+. Patients with severe infection requiring hospitalization were more likely to develop PACS+, hence these patients should be prioritized for clinical follow-up after COVID-19.

Published
2023
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14. Extracellular galectin 4 drives immune evasion and promotes T-cell apoptosis in pancreatic cancer

Author

Lidström, Tommy, Cumming, Joshua, Gaur, Rahul, Frängsmyr, Lars, Pateras, Ioannis S., Mickert, Matthias J., Franklin, Oskar, Forsell, Mattias N. E., Arnberg, Niklas, Dongre, Mitesh, Patthey, Cedric, Öhlund, Daniel, Lidström, Tommy, Cumming, Joshua, Gaur, Rahul, Frängsmyr, Lars, Pateras, Ioannis S., Mickert, Matthias J., Franklin, Oskar, Forsell, Mattias N. E., Arnberg, Niklas, Dongre, Mitesh, Patthey, Cedric, and Öhlund, Daniel

Abstract

Pancreatic ductal adenocarcinoma (PDAC) is characterized by rich deposits of extracellular matrix (ECM), affecting the pathophysiology of the disease. Here, we identified galectin 4 (gal 4) as a cancer cell produced protein deposited into the ECM of PDAC tumors and detected high circulating levels of gal 4 in PDAC patients. In orthotopic transplantation experiments we observed increased infiltration of T-cells and prolonged survival in immunocompetent mice transplanted with cancer cells with reduced expression of gal 4. Increased survival was not observed in immunodeficient RAG1-/- mice, demonstrating that the effect was mediated by the adaptive immune system. Furthermore, by performing single-cell RNA-sequencing we found that the myeloid compartment and cancer-associated fibroblast (CAF) subtypes were altered in the transplanted tumors. Reduced gal 4 expression was associated with higher proportion of myofibroblastic CAFs and reduced numbers of inflammatory CAFs. We also found higher proportions of M1 macrophages, T-cells and antigen presenting dendritic cells in tumors with reduced gal 4 expression. Using a co-culture system, we observed that extracellular gal 4 induced apoptosis in T-cells by binding N-glycosylation residues on CD3 epsilon/delta. Hence, we show that gal 4 is involved in immune evasion and identify gal 4 as a promising drug target for overcoming immunosuppression in PDAC., Originally included in thesis in manuscript form.

Published
2023
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15. At-home sampling to meet geographical challenges for serological assessment of SARS-CoV-2 exposure in a rural region of northern Sweden, March to May 2021 : a retrospective cohort study

Author

Wigren, Julia, Vikström, Linnea, Rosendal, Ebba, Gröning, Remigius, Gwon, Yong-Dae, Nilsson, Emma, Sharma, Atin, Espaillat, Akbar, Hanke, Leo, McInerney, Gerald, Puhar, Andrea, Cava, Felipe, Karlsson Hedestam, Gunilla B., Thunberg, Therese, Monsen, Tor, Elgh, Fredrik, Evander, Magnus, Johansson, Anders F., Överby, Anna K., Ahlm, Clas, Normark, Johan, Forsell, Mattias N. E., Wigren, Julia, Vikström, Linnea, Rosendal, Ebba, Gröning, Remigius, Gwon, Yong-Dae, Nilsson, Emma, Sharma, Atin, Espaillat, Akbar, Hanke, Leo, McInerney, Gerald, Puhar, Andrea, Cava, Felipe, Karlsson Hedestam, Gunilla B., Thunberg, Therese, Monsen, Tor, Elgh, Fredrik, Evander, Magnus, Johansson, Anders F., Överby, Anna K., Ahlm, Clas, Normark, Johan, and Forsell, Mattias N. E.

Abstract

Background: The current SARS-CoV-2 pandemic has highlighted a need for easy and safe blood sampling in combination with accurate serological methodology. Venipuncture for testing is usually performed by trained staff at healthcare centres. Long travel distances to healthcare centres in rural regions may introduce a bias of testing towards relatively large communities with closer access. Rural regions are therefore often not represented in population-based data. Aim: The aim of this retrospective cohort study was to develop and implement a strategy for at-home testing in a rural region of Sweden during spring 2021, and to evaluate its role to provide equal health care for its inhabitants. Methods: We developed a sensitive method to measure antibodies to the S-protein of SARS-CoV-2 and optimised this assay for clinical use together with a strategy of at-home capillary blood sampling. Results: We demonstrated that our ELISA gave comparable results after analysis of capillary blood or serum from SARS-CoV-2-experienced individuals. We demonstrated stability of the assay under conditions that reflected temperature and humidity during winter or summer. By assessment of capillary blood samples from 4,122 individuals, we could show both feasibility of the strategy and that implementation shifted the geographical spread of testing in favour of rural areas. Conclusion: Implementation of at-home sampling enabled citizens living in remote rural areas access to centralised and sensitive laboratory antibody tests. The strategy for testing used here could therefore enable disease control authorities to get rapid access to information concerning immunity to infectious diseases, even across vast geographical distance.

Published
2023
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16. Immune response to SARS-CoV-2 mRNA vaccination in multiple sclerosis patients after rituximab treatment interruption

Author

Gröning, Remigius, Dernstedt, Andy, Ahlm, Clas, Normark, Johan, Sundström, Peter, Forsell, Mattias N. E., Gröning, Remigius, Dernstedt, Andy, Ahlm, Clas, Normark, Johan, Sundström, Peter, and Forsell, Mattias N. E.

Abstract

Peripheral B cell depletion via anti-CD20 treatment is a highly effective disease-modifying treatment for reducing new relapses in multiple sclerosis (MS) patients. A drawback of rituximab (RTX) and other anti-CD20 antibodies is a poor immune response to vaccination. While this can be mitigated by treatment interruption of at least six months prior to vaccination, the timing to resume treatment while maintaining subsequent vaccine responses remains undetermined. Here, we characterized SARS-CoV-2 S-directed antibody and B cell responses throughout three BNT162b2 mRNA vaccine doses in RTX-treated MS patients, with the first two doses given during treatment interruption. We examined B-cell mediated immune responses in blood samples from patients with RTX-treated MS throughout three BNT162b2 vaccine doses, compared to an age- and sex-matched healthy control group. The first vaccine dose was given 1.3 years (median) after the last RTX infusion, the second dose one month after the first, and the third dose four weeks after treatment re-initiation. We analyzed SARS-CoV-2 S-directed antibody levels using enzyme-linked immunosorbent assay (ELISA), and the neutralization capacity of patient serum against SARS-CoV-2 S-pseudotyped lentivirus using luciferase reporter assay. In addition, we assessed switched memory (CD19+CD20+CD27+IgD-), unswitched memory (CD19+CD20+CD27+IgD+), naïve (CD19+CD20+CD27-IgD+), and double negative (DN, CD19+CD20+CD27-IgD-) B cell frequencies, as well as their SARS-CoV-2 S-specific (CoV+) and Decay Accelerating Factor-negative (DAF-) subpopulations, using flow cytometry. After two vaccine doses, S-binding antibody levels and neutralization capacity in SARS-CoV-2-naïve MS patients were comparable to vaccinated healthy controls, albeit with greater variation. Higher antibody response levels and CoV+-DN B cell frequencies after the second vaccine dose were predictive of a boost effect after the third dose, even after re-initiation of rituximab treatment.

Published
2023
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17. Risk factors for impaired respiratory function post COVID-19 : a prospective cohort study of nonhospitalized and hospitalized patients

Author

Björsell, Tove, Sundh, Josefin, Lange, Anna, Ahlm, Clas, Forsell, Mattias N. E., Tevell, Staffan, Blomberg, Anders, Edin, Alicia, Normark, Johan, Cajander, Sara, Björsell, Tove, Sundh, Josefin, Lange, Anna, Ahlm, Clas, Forsell, Mattias N. E., Tevell, Staffan, Blomberg, Anders, Edin, Alicia, Normark, Johan, and Cajander, Sara

Abstract

Background: Severe COVID-19 increases the risk for long-term respiratory impairment, but data after mild COVID-19 are scarce. Our aims were to determine risk factors for reduced respiratory function 3–6 months after COVID-19 infection and to investigate if reduced respiratory function would relate to impairment of exercise performance and breathlessness. Methods: Patients with COVID-19 were enrolled at the University Hospitals of Umeå and Örebro, and Karlstad Central Hospital, Sweden. Disease severity was defined as mild (nonhospitalized), moderate (hospitalized with or without oxygen treatment), and severe (intensive care). Spirometry, including diffusion capacity (DLCO), was performed 3–6 months after hospital discharge or study enrollment (for nonhospitalized patients). Breathlessness (defined as ≥1 according to the modified Medical Research Council scale) and functional exercise capacity (1-min sit-to-stand test; 1-MSTST) were assessed. Results: Between April 2020 and May 2021, 337 patients were enrolled in the study. Forced vital capacity and DLCO were significantly lower in patients with severe COVID-19. Among hospitalized patients, 20% had reduced DLCO, versus 4% in nonhospitalized. Breathlessness was found in 40.6% of the participants and was associated with impaired DLCO. A pathological desaturation or heart rate response was observed in 17% of participants during the 1-MSTST. However, this response was not associated with reduced DLCO. Conclusion: Reduced DLCO was the major respiratory impairment 3–6 months following COVID-19, with hospitalization as the most important risk factor. The lack of association between impaired DLCO and pathological physiological responses to exertion suggests that these physiological responses are not primarily related to decreased lung function.

Published
2023
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18. Vaccine-induced correlate of protection against fatal COVID-19 in older and frail adults during waves of neutralization-resistant variants of concern : an observational study

Author

Vikström, Linnea, Fjällström, Peter, Gwon, Yong-Dae, Sheward, Daniel J., Wigren-Byström, Julia, Evander, Magnus, Bladh, Oscar, Widerström, Micael, Molnar, Christian, Rasmussen, Gunlög, Bennet, Louise, Åberg, Mikael, Björk, Jonas, Tevell, Staffan, Thålin, Charlotte, Blom, Kim, Klingström, Jonas, Murrell, Ben, Ahlm, Clas, Normark, Johan, Johansson, Anders F., Forsell, Mattias N. E., Vikström, Linnea, Fjällström, Peter, Gwon, Yong-Dae, Sheward, Daniel J., Wigren-Byström, Julia, Evander, Magnus, Bladh, Oscar, Widerström, Micael, Molnar, Christian, Rasmussen, Gunlög, Bennet, Louise, Åberg, Mikael, Björk, Jonas, Tevell, Staffan, Thålin, Charlotte, Blom, Kim, Klingström, Jonas, Murrell, Ben, Ahlm, Clas, Normark, Johan, Johansson, Anders F., and Forsell, Mattias N. E.

Abstract

Background: To inform future preventive measures including repeated vaccinations, we have searched for a clinically useful immune correlate of protection against fatal COVID-19 among nursing homes residents. Methods: We performed repeated capillary blood sampling with analysis of S-binding IgG in an open cohort of nursing home residents in Sweden. We analyzed immunological and registry data from 16 September 2021 to 31 August 2022 with follow-up of deaths to 30 September 2022. The study period included implementation of the 3rd and 4th mRNA monovalent vaccine doses and Omicron virus waves. Findings: A total of 3012 nursing home residents with median age 86 were enrolled. The 3rd mRNA dose elicited a 99-fold relative increase of S-binding IgG in blood and corresponding increase of neutralizing antibodies. The 4th mRNA vaccine dose boosted levels 3.8-fold. Half-life of S-binding IgG was 72 days. A total 528 residents acquired their first SARS-CoV-2 infection after the 3rd or the 4th vaccine dose and the associated 30-day mortality was 9.1%. We found no indication that levels of vaccine-induced antibodies protected against infection with Omicron VOCs. In contrast, the risk of death was inversely correlated to levels of S-directed IgG below the 20th percentile. The death risk plateaued at population average above the lower 35th percentile of S-binding IgG. Interpretation: In the absence of neutralizing antibodies that protect from infection, quantification of S-binding IgG post vaccination may be useful to identify the most vulnerable for fatal COVID-19 among the oldest and frailest. This information is of importance for future strategies to protect vulnerable populations against neutralization resistant variants of concern.

Published
2023
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19. Progress in vaccine development for infectious diseases : a Keystone Symposia report

Author

Cable, Jennifer, Graham, Barney S., Koup, Richard A., Seder, Robert A., Karikó, Katalin, Pardi, Norbert, Barouch, Dan H., Sharma, Bhawna, Rauch, Susanne, Nachbagauer, Raffael, Forsell, Mattias N. E., Schotsaert, Michael, Ellebedy, Ali H., Loré, Karin, Irvine, Darrell J., Pilkington, Emily, Tahtinen, Siri, Thompson, Elizabeth A., Feraoun, Yanis, King, Neil P., Saunders, Kevin, Alter, Galit, Moin, Syed M., Sliepen, Kwinten, Karlsson Hedestam, Gunilla B., Wardemann, Hedda, Pulendran, Bali, Doria-Rose, Nicole A., He, Wan-Ting, Juno, Jennifer A., Ataca, Sila, Wheatley, Adam K., McLellan, Jason S., Walker, Laura M., Lederhofer, Julia, Lindesmith, Lisa C., Wille, Holger, Hotez, Peter J., Bekker, Linda-Gail, Cable, Jennifer, Graham, Barney S., Koup, Richard A., Seder, Robert A., Karikó, Katalin, Pardi, Norbert, Barouch, Dan H., Sharma, Bhawna, Rauch, Susanne, Nachbagauer, Raffael, Forsell, Mattias N. E., Schotsaert, Michael, Ellebedy, Ali H., Loré, Karin, Irvine, Darrell J., Pilkington, Emily, Tahtinen, Siri, Thompson, Elizabeth A., Feraoun, Yanis, King, Neil P., Saunders, Kevin, Alter, Galit, Moin, Syed M., Sliepen, Kwinten, Karlsson Hedestam, Gunilla B., Wardemann, Hedda, Pulendran, Bali, Doria-Rose, Nicole A., He, Wan-Ting, Juno, Jennifer A., Ataca, Sila, Wheatley, Adam K., McLellan, Jason S., Walker, Laura M., Lederhofer, Julia, Lindesmith, Lisa C., Wille, Holger, Hotez, Peter J., and Bekker, Linda-Gail

Abstract

The COVID-19 pandemic has taught us many things, among the most important of which is that vaccines are one of the cornerstones of public health that help make modern longevity possible. While several different vaccines have been successful at stemming the morbidity and mortality associated with various infectious diseases, many pathogens/diseases remain recalcitrant to the development of effective vaccination. Recent advances in vaccine technology, immunology, structural biology, and other fields may yet yield insight that will address these diseases; they may also help improve societies' preparedness for future pandemics. On June 1-4, 2022, experts in vaccinology from academia, industry, and government convened for the Keystone symposium "Progress in Vaccine Development for Infectious Diseases" to discuss state-of-the-art technologies, recent advancements in understanding vaccine-mediated immunity, and new aspects of antigen design to aid vaccine effectiveness.

Published
2023
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20. Structural and mechanistic basis of neutralization by a pan-hantavirus protective antibody

Author

Mittler, Eva, Serris, Alexandra, Esterman, Emma S., Florez, Catalina, Polanco, Laura C., O'Brien, Cecilia M., Slough, Megan M., Tynell, Janne, Gröning, Remigius, Sun, Yan, Abelson, Dafna M., Wec, Anna Z., Haslwanter, Denise, Keller, Markus, Ye, Chunyan, Bakken, Russel R., Jangra, Rohit K., Dye, John M., Ahlm, Clas, Rappazzo, C. Garrett, Ulrich, Rainer G., Zeitlin, Larry, Geoghegan, James C., Bradfute, Steven B., Sidoli, Simone, Forsell, Mattias N. E., Strandin, Tomas, Rey, Felix A., Herbert, Andrew S., Walker, Laura M., Chandran, Kartik, Guardado-Calvo, Pablo, Mittler, Eva, Serris, Alexandra, Esterman, Emma S., Florez, Catalina, Polanco, Laura C., O'Brien, Cecilia M., Slough, Megan M., Tynell, Janne, Gröning, Remigius, Sun, Yan, Abelson, Dafna M., Wec, Anna Z., Haslwanter, Denise, Keller, Markus, Ye, Chunyan, Bakken, Russel R., Jangra, Rohit K., Dye, John M., Ahlm, Clas, Rappazzo, C. Garrett, Ulrich, Rainer G., Zeitlin, Larry, Geoghegan, James C., Bradfute, Steven B., Sidoli, Simone, Forsell, Mattias N. E., Strandin, Tomas, Rey, Felix A., Herbert, Andrew S., Walker, Laura M., Chandran, Kartik, and Guardado-Calvo, Pablo

Abstract

Emerging rodent-borne hantaviruses cause severe diseases in humans with no approved vaccines or therapeutics. We recently isolated a monoclonal broadly neutralizing antibody (nAb) from a Puumala virus-experienced human donor. Here, we report its structure bound to its target, the Gn/Gc glycoprotein heterodimer comprising the viral fusion complex. The structure explains the broad activity of the nAb: It recognizes conserved Gc fusion loop sequences and the main chain of variable Gn sequences, thereby straddling the Gn/Gc heterodimer and locking it in its prefusion conformation. We show that the nAb's accelerated dissociation from the divergent Andes virus Gn/Gc at endosomal acidic pH limits its potency against this highly lethal virus and correct this liability by engineering an optimized variant that sets a benchmark as a candidate pan-hantavirus therapeutic.

Published
2023
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22. High prevalence of persistent symptoms and reduced health-related quality of life 6 months after COVID-19

Author

Ahmad, Irma, primary, Edin, Alicia, additional, Granvik, Christoffer, additional, Kumm Persson, Lowa, additional, Tevell, Staffan, additional, Månsson, Emeli, additional, Magnuson, Anders, additional, Marklund, Ingela, additional, Persson, Ida-Lisa, additional, Kauppi, Anna, additional, Ahlm, Clas, additional, Forsell, Mattias N. E., additional, Sundh, Josefin, additional, Lange, Anna, additional, Cajander, Sara, additional, and Normark, Johan, additional

Published
2023
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23. Immune response to SARS-CoV2 mRNA vaccination in multiple sclerosis patients after rituximab treatment interruption.

Author

Gröning, Remigius, Dernstedt, Andy, Ahlm, Clas, Normark, Johan, Sundström, Peter, and Forsell, Mattias N. E.

Subjects
IMMUNE response, IMMUNOLOGIC memory, MULTIPLE sclerosis, BOOSTER vaccines, RITUXIMAB, SLEEP interruptions
Abstract

Peripheral B cell depletion via anti-CD20 treatment is a highly effective diseasemodifying treatment for reducing new relapses in multiple sclerosis (MS) patients. A drawback of rituximab (RTX) and other anti-CD20 antibodies is a poor immune response to vaccination. While this can be mitigated by treatment interruption of at least six months prior to vaccination, the timing to resume treatment while maintaining subsequent vaccine responses remains undetermined. Here, we characterized SARS-CoV-2 S-directed antibody and B cell responses throughout three BNT162b2 mRNA vaccine doses in RTX-treated MS patients, with the first two doses given during treatment interruption. We examined B-cell mediated immune responses in blood samples from patients with RTX-treated MS throughout three BNT162b2 vaccine doses, compared to an age- and sexmatched healthy control group. The first vaccine dose was given 1.3 years (median) after the last RTX infusion, the second dose one month after the first, and the third dose four weeks after treatment re-initiation. We analyzed SARSCoV-2 S-directed antibody levels using enzyme-linked immunosorbent assay (ELISA), and the neutralization capacity of patient serum against SARS-CoV-2 Spseudotyped lentivirus using luciferase reporter assay. In addition, we assessed switched memory (CD19+CD20+CD27+IgD- ), unswitched memory (CD19+CD20+CD27+IgD+), naïve (CD19+CD20+CD27- IgD+), and double negative (DN, CD19+CD20+CD27- IgD- ) B cell frequencies, as well as their SARS-CoV-2 S-specific (CoV+) and Decay Accelerating Factor-negative (DAF- ) subpopulations, using flow cytometry. After two vaccine doses, S-binding antibody levels and neutralization capacity in SARS-CoV-2-naïve MS patients were comparable to vaccinated healthy controls, albeit with greater variation. Higher antibody response levels and CoV+-DN B cell frequencies after the second vaccine dose were predictive of a boost effect after the third dose, even after re-initiation of rituximab treatment. MS patients also exhibited lower frequencies of DAF- memory B cells, a suggested proxy for germinal centre activity, than control individuals. S-binding antibody levels in RTX-treated MS patients after two vaccine doses could help determine which individuals would need to move up their next vaccine booster dose or postpone their next RTX infusion. Our findings also offer first indications on the potential importance of antigenic stimulation of DN B cells and long-term impairment of germinal centre activity in rituximab-treated MS patients. [ABSTRACT FROM AUTHOR]

Published
2023
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25. Serum concentration of extracellular cold-inducible RNA-binding protein is associated with respiratory failure in COVID-19

Author

Schagatay, Felix, primary, Diamant, Klara, additional, Lidén, Mats, additional, Edin, Alicia, additional, Athlin, Simon, additional, Hultgren, Olof, additional, Ahlm, Clas, additional, Forsell, Mattias N. E., additional, Savilampi, Johanna, additional, Normark, Johan, additional, Lange, Anna, additional, and Cajander, Sara, additional

Published
2022
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27. Serum concentration of extracellular cold-inducible RNA-binding protein is associated with respiratory failure in COVID-19

Author

Schagatay, Felix, Diamant, Klara, Lidén, Mats, Edin, Alicia, Athlin, Simon, Hultgren, Olof, Ahlm, Clas, Forsell, Mattias N. E., Savilampi, Johanna, Normark, Johan, Lange, Anna, Cajander, Sara, Schagatay, Felix, Diamant, Klara, Lidén, Mats, Edin, Alicia, Athlin, Simon, Hultgren, Olof, Ahlm, Clas, Forsell, Mattias N. E., Savilampi, Johanna, Normark, Johan, Lange, Anna, and Cajander, Sara

Abstract

Uncontrolled release of damage-associated molecular patterns (DAMPs) is suggested to be a major trigger for the dysregulated host immune response that leads to severe COVID-19. Cold-inducible RNA-binding protein (CIRP), is a newly identified DAMP that aggravates inflammation and tissue injury, and induces respiratory failure in sepsis. Whether CIRP contributes to the pathogenesis of respiratory failure in COVID-19 has not yet been explored. Aim: To investigate if the concentration of extracellular CIRP (eCIRP) in serum associates with respiratory failure and lung involvement by chest computed tomography (CT) in COVID-19. Methods: Herein we report a prospective observational study of patients with COVID-19 included at two University Hospitals in Sweden between April 2020 and May 2021. Serum from hospitalized patients in Örebro (N=97) were used to assess the association between eCIRP and the level of respiratory support and its correlation with pulmonary involvement on chest CT and inflammatory biomarkers. A cohort of hospitalized and non-hospitalized patients from Umeå (N=78) was used as an external validation cohort. The severity of disease was defined according to the highest degree of respiratory support; mild disease (no oxygen), non-severe hypoxemia (conventional oxygen or high-flow nasal oxygen, HFNO <50% FiO2), and severe hypoxemia (HFNO ≥50% FiO2, mechanical ventilation). Unadjusted and adjusted linear regression was used to evaluate peak eCIRP day 0-4 in respect to severity, age, sex, Charlson comorbidity score, symptom duration, and BMI. Results: Peak eCIRP concentrations were higher in patients with severe hypoxemia and were independently associated with the degree of respiratory support in both cohorts (Örebro; p=0.01, Umeå; p<0.01). The degree of pulmonary involvement measured by CT correlated with eCIRP, rs=0.30, p<0.01 (n=97). Conclusion: High serum levels of eCIRP are associated with acute respiratory failure in COVID-19. Experimental studies

Published
2022
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28. Probabilistic classification of anti-SARS-CoV-2 antibody responses improves seroprevalence estimates

Author

Castro Dopico, Xaquin, Muschiol, Sandra, Grinberg, Nastasiya F., Aleman, Soo, Sheward, Daniel J., Hanke, Leo, Ahl, Marcus, Vikström, Linnea, Forsell, Mattias N. E., Coquet, Jonathan M., McInerney, Gerald, Dillner, Joakim, Bogdanovic, Gordana, Murrell, Ben, Albert, Jan, Wallace, Chris, Karlsson Hedestam, Gunilla B., Castro Dopico, Xaquin, Muschiol, Sandra, Grinberg, Nastasiya F., Aleman, Soo, Sheward, Daniel J., Hanke, Leo, Ahl, Marcus, Vikström, Linnea, Forsell, Mattias N. E., Coquet, Jonathan M., McInerney, Gerald, Dillner, Joakim, Bogdanovic, Gordana, Murrell, Ben, Albert, Jan, Wallace, Chris, and Karlsson Hedestam, Gunilla B.

Abstract

Objectives: Population-level measures of seropositivity are critical for understanding the epidemiology of an emerging pathogen, yet most antibody tests apply a strict cutoff for seropositivity that is not learnt in a data-driven manner, leading to uncertainty when classifying low-titer responses. To improve upon this, we evaluated cutoff-independent methods for their ability to assign likelihood of SARS-CoV-2 seropositivity to individual samples. Methods: Using robust ELISAs based on SARS-CoV-2 spike (S) and the receptor-binding domain (RBD), we profiled antibody responses in a group of SARS-CoV-2 PCR+ individuals (n = 138). Using these data, we trained probabilistic learners to assign likelihood of seropositivity to test samples of unknown serostatus (n = 5100), identifying a support vector machines-linear discriminant analysis learner (SVM-LDA) suited for this purpose. Results: In the training data from confirmed ancestral SARS-CoV-2 infections, 99% of participants had detectable anti-S and -RBD IgG in the circulation, with titers differing > 1000-fold between persons. In data of otherwise healthy individuals, 7.2% (n = 367) of samples were of uncertain serostatus, with values in the range of 3-6SD from the mean of pre-pandemic negative controls (n = 595). In contrast, SVM-LDA classified 6.4% (n = 328) of test samples as having a high likelihood (> 99% chance) of past infection, 4.5% (n = 230) to have a 50–99% likelihood, and 4.0% (n = 203) to have a 10–49% likelihood. As different probabilistic approaches were more consistent with each other than conventional SD-based methods, such tools allow for more statistically-sound seropositivity estimates in large cohorts. Conclusion: Probabilistic antibody testing frameworks can improve seropositivity estimates in populations with large titer variability.

Published
2022
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29. Broad anti–SARS-CoV-2 antibody immunity induced by heterologous ChAdOx1/mRNA-1273 vaccination

Author

Kaku, Chengzi I., Champney, Elizabeth R., Normark, Johan, Garcia, Marina, Johnson, Carl E., Ahlm, Clas, Christ, Wanda, Sakharkar, Mrunal, Ackerman, Margaret E., Klingström, Jonas, Forsell, Mattias N. E., Walker, Laura M., Kaku, Chengzi I., Champney, Elizabeth R., Normark, Johan, Garcia, Marina, Johnson, Carl E., Ahlm, Clas, Christ, Wanda, Sakharkar, Mrunal, Ackerman, Margaret E., Klingström, Jonas, Forsell, Mattias N. E., and Walker, Laura M.

Abstract

Heterologous prime-boost immunization strategies have the potential to augment COVID-19 vaccine efficacy We longitudinally profiled severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2) spike (S)–specific serological and memory B cell (MBC) responses in individuals who received either homologous (ChAdOx1: ChAdOx1) or heterologous (ChAdOx1:mRNA-1273) prime-boost vaccination. Heterologous messenger RNA (mRNA) booster immunization induced higher serum neutralizing antibody and MBC responses against SARS-CoV-2 variants of concern (VOCs) compared with that of homologous ChAdOx1 boosting. Specificity mapping of circulating B cells revealed that mRNA-1273 boost immunofocused ChAdOx1-primed responses onto epitopes expressed on prefusion-stabilized S. Monoclonal antibodies isolated from mRNA-1273–booste participants displayed overall higher binding affinities and increased breadth of reactivity against VOCs relativ to those isolated from ChAdOx1-boosted individuals. Overall, the results provide molecular insight into the enhanced quality of the B cell response induced after heterologous mRNA booster vaccination.

Published
2022
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30. Human antibody recognizing a quaternary epitope in the Puumala virus glycoprotein provides broad protection against orthohantaviruses

Author

Mittler, Eva, Wec, Anna Z., Tynell, Janne, Guardado-Calvo, Pablo, Wigren, Julia, Polanco, Laura C., O'Brien, Cecilia M., Slough, Megan M., Abelson, Dafna M., Serris, Alexandra, Sakharkar, Mrunal, Pehau-Arnaudet, Gerard, Bakken, Russell R., Geoghegan, James C., Jangra, Rohit K., Keller, Markus, Zeitlin, Larry, Vapalahti, Olli, Ulrich, Rainer G., Bornholdt, Zachary A., Ahlm, Clas, Rey, Felix A., Dye, John M., Bradfute, Steven B., Strandin, Tomas, Herbert, Andrew S., Forsell, Mattias N. E., Walker, Laura M., Chandran, Kartik, Mittler, Eva, Wec, Anna Z., Tynell, Janne, Guardado-Calvo, Pablo, Wigren, Julia, Polanco, Laura C., O'Brien, Cecilia M., Slough, Megan M., Abelson, Dafna M., Serris, Alexandra, Sakharkar, Mrunal, Pehau-Arnaudet, Gerard, Bakken, Russell R., Geoghegan, James C., Jangra, Rohit K., Keller, Markus, Zeitlin, Larry, Vapalahti, Olli, Ulrich, Rainer G., Bornholdt, Zachary A., Ahlm, Clas, Rey, Felix A., Dye, John M., Bradfute, Steven B., Strandin, Tomas, Herbert, Andrew S., Forsell, Mattias N. E., Walker, Laura M., and Chandran, Kartik

Abstract

The rodent-borne hantavirus Puumala virus (PUUV) and related agents cause hemorrhagic fever with renal syndrome (HFRS) in humans. Other hantaviruses, including Andes virus (ANDV) and Sin Nombre virus, cause a distinct zoonotic disease, hantavirus cardiopulmonary syndrome (HCPS). Although these infections are severe and have substantial case fatality rates, no FDA-approved hantavirus countermeasures are available. Recent work suggests that monoclonal antibodies may have therapeutic utility. We describe here the isolation of human neutralizing antibodies (nAbs) against tetrameric Gn/Gc glycoprotein spikes from PUUV-experienced donors. We define a dominant class of nAbs recognizing the "capping loop" of Gn that masks the hydrophobic fusion loops in Gc. A subset of nAbs in this class, including ADI-42898, bound Gn/Gc complexes but not Gn alone, strongly suggesting that they recognize a quaternary epitope encompassing both Gn and Gc. ADI-42898 blocked the cell entry of seven HCPS- and HFRS-associated hantaviruses, and single doses of this nAb could protect Syrian hamsters and bank voles challenged with the highly virulent HCPS-causing ANDV and HFRS-causing PUUV, respectively. ADI-42898 is a promising candidate for clinical development as a countermeasure for both HCPS and HFRS, and its mode of Gn/Gc recognition informs the development of broadly protective hantavirus vaccines.

Published
2022
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31. Convalescent plasma treatment in severely immunosuppressed patients hospitalized with COVID-19 : an observational study of 28 cases

Author

Ljungquist, Oskar, Lundgren, Maria, Iliachenko, Elena, Månsson, Fredrik, Böttiger, Blenda, Landin-Olsson, Mona, Wikén, Christian, Rosendal, Ebba, Överby, Anna K., Wigren, Julia, Forsell, Mattias N. E., Kjeldsen-Kragh, Jens, Rasmussen, Magnus, Kahn, Fredrik, Holm, Karin, Ljungquist, Oskar, Lundgren, Maria, Iliachenko, Elena, Månsson, Fredrik, Böttiger, Blenda, Landin-Olsson, Mona, Wikén, Christian, Rosendal, Ebba, Överby, Anna K., Wigren, Julia, Forsell, Mattias N. E., Kjeldsen-Kragh, Jens, Rasmussen, Magnus, Kahn, Fredrik, and Holm, Karin

Abstract

Background: Immunosuppressed patients are particularly vulnerable to severe infection from the severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2), risking prolonged viremia and symptom duration. In this study we describe clinical and virological treatment outcomes in a heterogeneous group of patients with severe immunosuppression due to various causes suffering from COVID-19 infection, who were all treated with convalescent plasma (CCP) along with standard treatment. Methods: We performed an observational, retrospective case series between May 2020 to March 2021 at three sites in Skåne, Sweden, with a population of nearly 1.4 million people. All patients hospitalized for COVID-19 who received CCP with the indication severe immunosuppression as defined by the treating physician were included in the study (n = 28). Results: In total, 28 severely immunocompromised patients, half of which previously had been treated with rituximab, who had received in-hospital convalescent plasma treatment of COVID-19 were identified. One week after CCP treatment, 13 of 28 (46%) patients had improved clinically defined as a decrease of at least one point at the WHO-scale. Three patients had increased score points of whom two had died. For 12 patients, the WHO-scale was unchanged. Conclusion: As one of only few studies on CCP treatment of COVID-19 in hospitalized patients with severe immunosuppression, this study adds descriptive data. The study design prohibits conclusions on safety and efficacy, and the results should be interpreted with caution. Prospective, randomized trials are needed to investigate this further.

Published
2022
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32. Hierarchical Clustering and Trajectory Analyses Reveal Viremia-Independent B-Cell Perturbations in HIV-2 Infection

Author

Johansson, Emil, Kerkman, Priscilla, Scharf, Lydia, Lindman, Jacob, Szojka, Zsófia I., Månsson, Fredrik, Biague, Antonio, Medstrand, Patrik, Norrgren, Hans, Buggert, Marcus, Karlsson, Annika C., Forsell, Mattias N. E., Esbjörnsson, Joakim, Jansson, Marianne, Johansson, Emil, Kerkman, Priscilla, Scharf, Lydia, Lindman, Jacob, Szojka, Zsófia I., Månsson, Fredrik, Biague, Antonio, Medstrand, Patrik, Norrgren, Hans, Buggert, Marcus, Karlsson, Annika C., Forsell, Mattias N. E., Esbjörnsson, Joakim, and Jansson, Marianne

Abstract

Time to AIDS in HIV-2 infection is approximately twice as long compared to in HIV-1 infection. Despite reduced viremia, HIV-2-infected individuals display signs of chronic immune activation. In HIV-1-infected individuals, B-cell hyperactivation is driven by continuous antigen exposure. However, the contribution of viremia to B-cell perturbations in HIV-2-infected individuals remains largely unexplored. Here, we used polychromatic flow cytometry, consensus hierarchical clustering and pseudotime trajectory inference to characterize B-cells in HIV-1- or HIV-2-infected and in HIV seronegative individuals. We observed increased frequencies of clusters containing hyperactivated T-bethighCD95highCD27int and proliferating T-bet+CD95highCD27+CD71+ memory B-cells in viremic HIV-1 (p < 0.001 and p < 0.001, respectively), viremic HIV-2 (p < 0.001 and p = 0.014, respectively) and in treatment-naïve aviremic HIV-2 (p = 0.004 and p = 0.020, respectively)-infected individuals, compared to seronegative individuals. In contrast, these expansions were not observed in successfully treated HIV-1-infected individuals. Finally, pseudotime trajectory inference showed that T-bet-expressing hyperactivated and proliferating memory B-cell populations were located at the terminal end of two trajectories, in both HIV-1 and HIV-2 infections. As the treatment-naïve aviremic HIV-2-infected individuals, but not the successfully ART-treated HIV-1-infected individuals, showed B-cell perturbations, our data suggest that aviremic HIV-2-infected individuals would also benefit from antiretroviral treatment.

Published
2022
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33. Recall of preexisting cross-reactive B cell memory after Omicron BA.1 breakthrough infection

Author

Kaku, Chengzi I., Bergeron, Alan J., Ahlm, Clas, Normark, Johan, Sakharkar, Mrunal, Forsell, Mattias N. E., Walker, Laura M., Kaku, Chengzi I., Bergeron, Alan J., Ahlm, Clas, Normark, Johan, Sakharkar, Mrunal, Forsell, Mattias N. E., and Walker, Laura M.

Abstract

Understanding immune responses after severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2) breakthrough infection will facilitate the development of next-generation vaccines. Here, we profiled spike (S)-specific B cell responses after Omicron/BA.1 infection in messenger RNA-vaccinated donors. The acute antibody response was characterized by high levels of somatic hypermutation and a bias toward recognition of ancestral SARS-CoV-2 strains, suggesting the early activation of vaccine-induced memory B cells. BA.1 breakthrough infection induced a shift in B cell immunodominance hierarchy from the S2 subunit, which is highly conserved across SARS-CoV-2 variants of concern (VOCs), and toward the antigenically variable receptor binding domain (RBD). A large proportion of RBD-directed neutralizing antibodies isolated from BA.1 breakthrough infection donors displayed convergent sequence features and broadly recognized SARS-CoV-2 VOCs. Together, these findings provide insights into the role of preexisting immunity in shaping the B cell response to heterologous SARS-CoV-2 variant exposure.

Published
2022
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34. Immune responses after omicron infection in triple-vaccinated health-care workers with and without previous SARS-CoV-2 infection

Author

Blom, Kim, Marking, Ulrika, Havervall, Sebastian, Norin, Nina Greilert, Gordon, Max, García, Marina, Tecleab, Teghesti, Christ, Wanda, Forsell, Mattias N. E., Phillipson, Mia, Nilsson, Peter, Mangsbo, Sara, Hober, Sophia, Åberg, Mikael, Klingström, Jonas, Thålin, Charlotte, Blom, Kim, Marking, Ulrika, Havervall, Sebastian, Norin, Nina Greilert, Gordon, Max, García, Marina, Tecleab, Teghesti, Christ, Wanda, Forsell, Mattias N. E., Phillipson, Mia, Nilsson, Peter, Mangsbo, Sara, Hober, Sophia, Åberg, Mikael, Klingström, Jonas, and Thålin, Charlotte

Published
2022
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36. Human antibody recognizing a quaternary epitope in the Puumala virus glycoprotein provides broad protection against orthohantaviruses

Author

Mittler, Eva, primary, Wec, Anna Z., additional, Tynell, Janne, additional, Guardado-Calvo, Pablo, additional, Wigren-Byström, Julia, additional, Polanco, Laura C., additional, O’Brien, Cecilia M., additional, Slough, Megan M., additional, Abelson, Dafna M., additional, Serris, Alexandra, additional, Sakharkar, Mrunal, additional, Pehau-Arnaudet, Gerard, additional, Bakken, Russell R., additional, Geoghegan, James C., additional, Jangra, Rohit K., additional, Keller, Markus, additional, Zeitlin, Larry, additional, Vapalahti, Olli, additional, Ulrich, Rainer G., additional, Bornholdt, Zachary A., additional, Ahlm, Clas, additional, Rey, Felix A., additional, Dye, John M., additional, Bradfute, Steven B., additional, Strandin, Tomas, additional, Herbert, Andrew S., additional, Forsell, Mattias N. E., additional, Walker, Laura M., additional, and Chandran, Kartik, additional

Published
2022
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37. Broad anti–SARS-CoV-2 antibody immunity induced by heterologous ChAdOx1/mRNA-1273 vaccination

Author

Kaku, Chengzi I., primary, Champney, Elizabeth R., additional, Normark, Johan, additional, Garcia, Marina, additional, Johnson, Carl E., additional, Ahlm, Clas, additional, Christ, Wanda, additional, Sakharkar, Mrunal, additional, Ackerman, Margaret E., additional, Klingström, Jonas, additional, Forsell, Mattias N. E., additional, and Walker, Laura M., additional

Published
2022
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38. Convalescent plasma treatment in severely immunosuppressed patients hospitalized with COVID-19: an observational study of 28 cases

Author

Ljungquist, Oskar, primary, Lundgren, Maria, additional, Iliachenko, Elena, additional, Månsson, Fredrik, additional, Böttiger, Blenda, additional, Landin-Olsson, Mona, additional, Wikén, Christian, additional, Rosendal, Ebba, additional, Överby, Anna K., additional, Wigren, Byström J., additional, Forsell, Mattias N. E., additional, Kjeldsen-Kragh, Jens, additional, Rasmussen, Magnus, additional, Kahn, Fredrik, additional, and Holm, Karin, additional

Published
2021
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39. The Tonsil Lymphocyte Landscape in Pediatric Tonsil Hyperplasia and Obstructive Sleep Apnea

Author

Carrasco, Anna, Sjölander, Isabella, Van Acker, Aline, Dernstedt, Andy, Fehrm, Johan, Forsell, Mattias N. E., Friberg, Danielle, Mjösberg, Jenny, Rao, Anna, Carrasco, Anna, Sjölander, Isabella, Van Acker, Aline, Dernstedt, Andy, Fehrm, Johan, Forsell, Mattias N. E., Friberg, Danielle, Mjösberg, Jenny, and Rao, Anna

Abstract

Tonsil hyperplasia is the most common cause of pediatric obstructive sleep apnea (OSA). Despite the growing knowledge in tissue immunology of tonsils, the immunopathology driving tonsil hyperplasia and OSA remains unknown. Here we used multi-parametric flow cytometry to analyze the composition and phenotype of tonsillar innate lymphoid cells (ILCs), T cells, and B cells from pediatric patients with OSA, who had previous polysomnography. Unbiased clustering analysis was used to delineate and compare lymphocyte heterogeneity between two patient groups: children with small tonsils and moderate OSA (n = 6) or large tonsils and very severe OSA (n = 13). We detected disturbed ILC and B cell proportions in patients with large tonsils, characterized by an increase in the frequency of naïve CD27-CD21hi B cells and a relative reduction of ILCs. The enrichment of naïve B cells was not commensurate with elevated Ki67 expression, suggesting defective differentiation and/or migration rather than cellular proliferation to be the causative mechanism. Finally, yet importantly, we provide the flow cytometry data to be used as a resource for additional translational studies aimed at investigating the immunological mechanisms of pediatric tonsil hyperplasia and OSA.

Published
2021
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40. Generation of plasma cells and CD27-IgD- B cells during hantavirus infection is associated with distinct pathological findings

Author

Kerkman, Priscilla, Dernstedt, Andy, Tadala, Lalitha, Mittler, Eva, Dannborg, Mirjam, Sundling, Christopher, Maleki, Kimia T., Tauriainen, Johanna, Tuiskunen-Bäck, Anne, Wigren Byström, Julia, Ocaya, Pauline, Thunberg, Therese, Jangra, Rohit K, Román-Sosa, Gleyder, Guardado-Calvo, Pablo, Rey, Feilx A., Klingström, Jonas, Chandran, Kartik, Puhar, Andrea, Ahlm, Clas, Forsell, Mattias N. E., Kerkman, Priscilla, Dernstedt, Andy, Tadala, Lalitha, Mittler, Eva, Dannborg, Mirjam, Sundling, Christopher, Maleki, Kimia T., Tauriainen, Johanna, Tuiskunen-Bäck, Anne, Wigren Byström, Julia, Ocaya, Pauline, Thunberg, Therese, Jangra, Rohit K, Román-Sosa, Gleyder, Guardado-Calvo, Pablo, Rey, Feilx A., Klingström, Jonas, Chandran, Kartik, Puhar, Andrea, Ahlm, Clas, and Forsell, Mattias N. E.

Abstract

Objective: Human hantavirus infections can cause haemorrhagic fever with renal syndrome (HFRS). The pathogenic mechanisms arenot fully understood, nor if they affect the humoral immune system. The objective of this study was to investigate humoral immune responses to hantavirus infection and to correlate them to the typical features of HFRS: thrombocytopenia and transient kidney dysfunction. Methods: We performed a comprehensive characterisation of longitudinal antiviral B-cell responses of 26 hantavirus patients and combined this with paired clinical data. In addition, we measured extracellular adenosine triphosphate (ATP)and its breakdown products in circulation and performed in vitro stimulations to address its effect on B cells. Results: We found that thrombocytopenia was correlated to an elevated frequency of plasmablasts in circulation. In contrast, kidney dysfunction was indicative of an accumulation of CD27-IgD- B cells and CD27/low plasmablasts. Finally, we provide evidence that high levels of extracellular ATP and matrix metalloproteinase 8 can contribute to shedding of CD27 during human hantavirus infection. Conclusion: Our findings demonstrate that thrombocytopenia and kidneydysfunction associate with distinctly different effects on the humoral immune system. Moreover, hantavirus-infectedindividuals have significantly elevated levels of extracellular ATP incirculation.

Published
2021
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41. Single-Dilution COVID-19 Antibody Test with Qualitative and Quantitative Readouts

Author

Bortz, Robert H., Florez, Catalina, Laudermilch, Ethan, Wirchnianski, Ariel S., Lasso, Gorka, Malonis, Ryan J., Georgiev, George I., Vergnolle, Olivia, Herrera, Natalia G., Morano, Nicholas C., Campbell, Sean T., Orner, Erika P., Mengotto, Amanda, Dieterle, M. Eugenia, Fels, J. Maximilian, Haslwanter, Denise, Jangra, Rohit K., Celikgil, Alev, Kimmel, Duncan, Lee, James H., Mariano, Margarette C., Nakouzi, Antonio, Quiroz, Jose, Rivera, Johanna, Szymczak, Wendy A., Tong, Karen, Barnhill, Jason, Forsell, Mattias N. E., Ahlm, Clas, Stein, Daniel T., Pirofski, Liise-Anne, Goldstein, D Yitzchak, Garforth, Scott J., Almo, Steven C., Daily, Johanna P., Prystowsky, Michael B., Faix, James D., Fox, Amy S., Weiss, Louis M., Lai, Jonathan R., Chandran, Kartik, Bortz, Robert H., Florez, Catalina, Laudermilch, Ethan, Wirchnianski, Ariel S., Lasso, Gorka, Malonis, Ryan J., Georgiev, George I., Vergnolle, Olivia, Herrera, Natalia G., Morano, Nicholas C., Campbell, Sean T., Orner, Erika P., Mengotto, Amanda, Dieterle, M. Eugenia, Fels, J. Maximilian, Haslwanter, Denise, Jangra, Rohit K., Celikgil, Alev, Kimmel, Duncan, Lee, James H., Mariano, Margarette C., Nakouzi, Antonio, Quiroz, Jose, Rivera, Johanna, Szymczak, Wendy A., Tong, Karen, Barnhill, Jason, Forsell, Mattias N. E., Ahlm, Clas, Stein, Daniel T., Pirofski, Liise-Anne, Goldstein, D Yitzchak, Garforth, Scott J., Almo, Steven C., Daily, Johanna P., Prystowsky, Michael B., Faix, James D., Fox, Amy S., Weiss, Louis M., Lai, Jonathan R., and Chandran, Kartik

Abstract

The coronavirus disease 2019 (COVID-19) global pandemic caused by severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2) continues to place an immense burden on societies and health care systems. A key component of COVID-19 control efforts is serological testing to determine the community prevalence of SARS-CoV-2 exposure and quantify individual immune responses to prior SARS-CoV-2 infection or vaccination. Here, we describe a laboratory-developed antibody test that uses readily available research-grade reagents to detect SARS-CoV-2 exposure in patient blood samples with high sensitivity and specificity. We further show that this sensitive test affords the estimation of viral spike-specific IgG titers from a single sample measurement, thereby providing a simple and scalable method to measure the strength of an individual's immune response. The accuracy, adaptability, and cost-effectiveness of this test make it an excellent option for clinical deployment in the ongoing COVID-19 pandemic.IMPORTANCE Serological surveillance has become an important public health tool during the COVID-19 pandemic. Detection of protective antibodies and seroconversion after SARS-CoV-2 infection or vaccination can help guide patient care plans and public health policies. Serology tests can detect antibodies against past infections; consequently, they can help overcome the shortcomings of molecular tests, which can detect only active infections. This is important, especially when considering that many COVID-19 patients are asymptomatic. In this study, we describe an enzyme-linked immunosorbent assay (ELISA)-based qualitative and quantitative serology test developed to measure IgG and IgA antibodies against the SARS-CoV-2 spike glycoprotein. The test can be deployed using commonly available laboratory reagents and equipment and displays high specificity and sensitivity. Furthermore, we demonstrate that IgG titers in patient samples can be estimated from a single measurement, enabling t

Published
2021
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42. Heterologous ChAdOx1 nCoV-19 and mRNA-1273 Vaccination

Author

Normark, Johan, Vikström, Linnea, Yong-Dae, Gwon, Persson, Ida-Lisa, Edin, Alicia, Björsell, Tove, Dernstedt, Andy, Christ, Wanda, Tevell, Staffan, Evander, Magnus, Klingström, Jonas, Ahlm, Clas, Forsell, Mattias N. E., Normark, Johan, Vikström, Linnea, Yong-Dae, Gwon, Persson, Ida-Lisa, Edin, Alicia, Björsell, Tove, Dernstedt, Andy, Christ, Wanda, Tevell, Staffan, Evander, Magnus, Klingström, Jonas, Ahlm, Clas, and Forsell, Mattias N. E.

Published
2021
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43. Evaluation of 11 SARS-CoV-2 antibody tests by using samples from patients with defined IgG antibody titers

Author

Lagerqvist, Nina, Maleki, Kimia T., Verner-Carlsson, Jenny, Olausson, Mikaela, Dillner, Joakim, Wigren Byström, Julia, Monsen, Tor J., Forsell, Mattias N. E., Eriksson, Jenny, Bogdanovic, Gordana, Muschiol, Sandra, Ljunggren, Joel, Repo, Johanna, Kjerstadius, Torbjörn, Muradrasoli, Shaman, Brytting, Mia, Szekely Björndal, Åsa, Åkerlund, Thomas, Nilsson, Charlotta, Klingström, Jonas, Lagerqvist, Nina, Maleki, Kimia T., Verner-Carlsson, Jenny, Olausson, Mikaela, Dillner, Joakim, Wigren Byström, Julia, Monsen, Tor J., Forsell, Mattias N. E., Eriksson, Jenny, Bogdanovic, Gordana, Muschiol, Sandra, Ljunggren, Joel, Repo, Johanna, Kjerstadius, Torbjörn, Muradrasoli, Shaman, Brytting, Mia, Szekely Björndal, Åsa, Åkerlund, Thomas, Nilsson, Charlotta, and Klingström, Jonas

Abstract

We evaluated the performance of 11 SARS-CoV-2 antibody tests using a reference set of heat-inactivated samples from 278 unexposed persons and 258 COVID-19 patients, some of whom contributed serial samples. The reference set included samples with a variation in SARS-CoV-2 IgG antibody titers, as determined by an in-house immunofluorescence assay (IFA). The five evaluated rapid diagnostic tests had a specificity of 99.0% and a sensitivity that ranged from 56.3 to 81.6% and decreased with low IFA IgG titers. The specificity was > 99% for five out of six platform-based tests, and when assessed using samples collected ≥ 22 days after symptom onset, two assays had a sensitivity of > 96%. These two assays also detected samples with low IFA titers more frequently than the other assays. In conclusion, the evaluated antibody tests showed a heterogeneity in their performances and only a few tests performed well with samples having low IFA IgG titers, an important aspect for diagnostics and epidemiological investigations.

Published
2021
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44. MAIT cell activation is associated with disease severity markers in acute hantavirus infection

Author

Maleki, Kimia T., Tauriainen, Johanna, García, Marina, Kerkman, Priscilla, Christ, Wanda, Dias, Joana, Wigren, Julia, Leeansyah, Edwin, Forsell, Mattias N. E., Ljunggren, Hans-Gustaf, Ahlm, Clas, Björkström, Niklas K., Sandberg, Johan K., Klingström, Jonas, Maleki, Kimia T., Tauriainen, Johanna, García, Marina, Kerkman, Priscilla, Christ, Wanda, Dias, Joana, Wigren, Julia, Leeansyah, Edwin, Forsell, Mattias N. E., Ljunggren, Hans-Gustaf, Ahlm, Clas, Björkström, Niklas K., Sandberg, Johan K., and Klingström, Jonas

Abstract

Hantaviruses are zoonotic RNA viruses that cause severe acute disease in humans. Infected individuals have strong inflammatory responses that likely cause immunopathology. Here, we studied the response of mucosal-associated invariant T (MAIT) cells in peripheral blood of individuals with hemorrhagic fever with renal syndrome (HFRS) caused by Puumala orthohantavirus, a hantavirus endemic in Europe. We show that MAIT cell levels decrease in the blood during HFRS and that residual MAIT cells are highly activated. This activation correlates with HFRS severity markers. In vitro activation of MAIT cells by hantavirus-exposed antigen-presenting cells is dependent on type I interferons (IFNs) and independent of interleukin-18 (IL-18). These findings highlight the role of type I IFNs in virus-driven MAIT cell activation and suggest a potential role of MAIT cells in the disease pathogenesis of viral infections.

Published
2021
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45. Regulation of Decay Accelerating Factor Primes Human Germinal Center B Cells for Phagocytosis

Author

Dernstedt, Andy, Leidig, Jana, Holm, Anna, Kerkman, Priscilla, Mjösberg, Jenny, Ahlm, Clas, Henriksson, Johan, Hultdin, Magnus, Forsell, Mattias N. E., Dernstedt, Andy, Leidig, Jana, Holm, Anna, Kerkman, Priscilla, Mjösberg, Jenny, Ahlm, Clas, Henriksson, Johan, Hultdin, Magnus, and Forsell, Mattias N. E.

Abstract

Germinal centers (GC) are sites for extensive B cell proliferation and homeostasis is maintained by programmed cell death. The complement regulatory protein Decay Accelerating Factor (DAF) blocks complement deposition on host cells and therefore also phagocytosis of cells. Here, we show that B cells downregulate DAF upon BCR engagement and that T cell-dependent stimuli preferentially led to activation of DAF(lo) B cells. Consistent with this, a majority of light and dark zone GC B cells were DAF(lo) and susceptible to complement-dependent phagocytosis, as compared with DAF(hi) GC B cells. We could also show that the DAF(hi) GC B cell subset had increased expression of the plasma cell marker Blimp-1. DAF expression was also modulated during B cell hematopoiesis in the human bone marrow. Collectively, our results reveal a novel role of DAF to pre-prime activated human B cells for phagocytosis prior to apoptosis.

Published
2021
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46. Single-Dilution COVID-19 Antibody Test with Qualitative and Quantitative Readouts

Author

Bortz, Robert H., primary, Florez, Catalina, additional, Laudermilch, Ethan, additional, Wirchnianski, Ariel S., additional, Lasso, Gorka, additional, Malonis, Ryan J., additional, Georgiev, George I., additional, Vergnolle, Olivia, additional, Herrera, Natalia G., additional, Morano, Nicholas C., additional, Campbell, Sean T., additional, Orner, Erika P., additional, Mengotto, Amanda, additional, Dieterle, M. Eugenia, additional, Fels, J. Maximilian, additional, Haslwanter, Denise, additional, Jangra, Rohit K., additional, Celikgil, Alev, additional, Kimmel, Duncan, additional, Lee, James H., additional, Mariano, Margarette C., additional, Nakouzi, Antonio, additional, Quiroz, Jose, additional, Rivera, Johanna, additional, Szymczak, Wendy A., additional, Tong, Karen, additional, Barnhill, Jason, additional, Forsell, Mattias N. E., additional, Ahlm, Clas, additional, Stein, Daniel T., additional, Pirofski, Liise-anne, additional, Goldstein, D. Yitzchak, additional, Garforth, Scott J., additional, Almo, Steven C., additional, Daily, Johanna P., additional, Prystowsky, Michael B., additional, Faix, James D., additional, Fox, Amy S., additional, Weiss, Louis M., additional, Lai, Jonathan R., additional, and Chandran, Kartik, additional

Published
2021
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47. Platelets mediate serological memory to neutralize viruses in vitro and in vivo

Author

Waltraud, Schrottmaier C., Salzmann, Manuel, Badrnya, Sigrun, Mussbacher, Marion, Kral-Pointner, Julia B., Morava, Susanne, Pirabe, Anita, Brunnthaler, Laura, Yaiw, Koon C., Heber, Ulrike M., Pereyra, David, Andersen, Jan T., Bergthaler, Andreas, Söderberg-Nauclér, Cecilia, Karlsson, Mikael C., I, Assinger, Alice, Forsell, Mattias N. E., Waltraud, Schrottmaier C., Salzmann, Manuel, Badrnya, Sigrun, Mussbacher, Marion, Kral-Pointner, Julia B., Morava, Susanne, Pirabe, Anita, Brunnthaler, Laura, Yaiw, Koon C., Heber, Ulrike M., Pereyra, David, Andersen, Jan T., Bergthaler, Andreas, Söderberg-Nauclér, Cecilia, Karlsson, Mikael C., I, Assinger, Alice, and Forsell, Mattias N. E.

Published
2020
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48. Longitudinal dynamics of the human B cell response to the yellow fever 17D vaccine

Author

Wec, Anna Z., Haslwanter, Denise, Abdiche, Yasmina N., Shehata, Laila, Pedreno-Lopez, Nuria, Moyer, Crystal L., Bornholdt, Zachary A., Lilov, Asparouh, Nett, Juergen H., Jangra, Rohit K., Brown, Michael, Watkins, David I., Ahlm, Clas, Forsell, Mattias N. E., Rey, Felix A., Barba-Spaeth, Giovanna, Chandran, Kartik, Walker, Laura M., Wec, Anna Z., Haslwanter, Denise, Abdiche, Yasmina N., Shehata, Laila, Pedreno-Lopez, Nuria, Moyer, Crystal L., Bornholdt, Zachary A., Lilov, Asparouh, Nett, Juergen H., Jangra, Rohit K., Brown, Michael, Watkins, David I., Ahlm, Clas, Forsell, Mattias N. E., Rey, Felix A., Barba-Spaeth, Giovanna, Chandran, Kartik, and Walker, Laura M.

Abstract

A comprehensive understanding of the development and evolution of human B cell responses duced by pathogen exposure will facilitate the design of next-generation vaccines. Here, we utilized a gh-throughput single B cell cloning technology to longitudinally track the human B cell response to the llow fever virus 17D (YFV-17D) vaccine. The earlymemory B cell (MBC) response was mediated by both assical immunoglobulin M (IgM) (IgM(+)CD27(+)) and switched immunoglobulin (swIg(+)) MBC pulations; however, classical IgM MBCs waned rapidly, whereas swIg(+) and atypical IgM(+) and IgD(+) MBCs were stable over time. Affinity maturation continued for 6 to 9 mo following vaccination, providing evidence for the persistence of germinal center activity long after the period of active viral replication in peripheral blood. Finally, a substantial fraction of the neutralizing antibody response was mediated by public clones that recognize a fusion loop-proximal antigenic site within domain II of the viral envelope glycoprotein. Overall, our findings provide a framework for understanding the dynamics and complexity of human B cell responses elicited by infection and vaccination.

Published
2020
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