Antibody response and intra‐host viral evolution after plasma therapy in <scp>COVID</scp>‐19 patients pre‐exposed or not to B‐cell‐depleting agents

Gachoud, David; Pillonel, Trestan; Tsilimidos, Gerasimos; Battolla, Dunia; Dumas, Dominique; Opota, Onya; Fontana, Stefano; Vollenweider, Péter; Manuel, Oriol; Greub, Gilbert; Bertelli, Claire; Rufer, Nathalie

doi:10.1111/bjh.18450

Cited by 9 publications

(5 citation statements)

References 69 publications

(162 reference statements)

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“…Patients were classified according to whether they had Vax-CCP treatment once or twice (Figure 1B) and presented various Phylogenetic Assignment of Named Global Outbreak (PANGO) lineages, depending on the predominant circulating strain(s) at the time of diagnosis (Figure 1C). Our data indicate that seven out nine patients were able to clear the virus within the same time-range (<35 days, Figure 1D,E) as reported for patients with endogenous anti-SARS-CoV-2 responses, 6 among them two had received two serial transfusions. Hence, our tailored approach is consistent with the relative low number of refractory cases (six of 36) previously observed 6 and enables sparing Vax-CCP resources of high anti-SARS-CoV-2 titres, which heavily rely on the continuous collection of donor plasma.…”

supporting

confidence: 77%

“…Our data indicate that seven out nine patients were able to clear the virus within the same time-range (<35 days, Figure 1D,E) as reported for patients with endogenous anti-SARS-CoV-2 responses, 6 among them two had received two serial transfusions. Hence, our tailored approach is consistent with the relative low number of refractory cases (six of 36) previously observed 6 and enables sparing Vax-CCP resources of high anti-SARS-CoV-2 titres, which heavily rely on the continuous collection of donor plasma.…”

supporting

confidence: 77%

“… 5 From March to July 2021, we treated 19 immunosuppressed patients with plasma collected from COVID‐naive two‐dose mRNA‐vaccinated donors, under a compassionate use protocol, according to the Swiss regulation rules. 6 No relevant difference was observed between patients receiving CCP ( n = 17) versus vaccinated plasma (VP, n = 19), indicating that VP therapy is safe and effective in patients with B‐cell lymphopenia. In the meantime, CCP donors are increasingly getting vaccinated, and three‐dose VP donors are being boosted by a breakthrough infection (defined as ‘hybrid plasma’, Vax‐CCP or CP/VP).…”

mentioning

confidence: 99%

“…Understanding which parameter(s) may be predictive of complete viral clearance would likely help adjusting Vax‐CCP treatment. As such, the question of whether basal viral load is typically higher in B‐cell‐depleted patients than in B‐cell‐undepleted ones and thus represents a red‐flag could alas not be addressed in the dataset initially reported, 6 as both cohorts differed substantially in terms of the underlying viral variant (pre‐alpha vs. alpha predominance respectively). Still, we recently observed that patients transfused twice with Vax‐CCP had higher levels of initial SARS‐CoV‐2 viral loads than those receiving only one‐time plasma (Figure 1D ).…”

mentioning

confidence: 99%

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Understanding the parameters guiding the best practice for treating B‐cell‐depleted patients with COVID‐19 convalescent plasma therapy

2022

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The commentary by Focosi et al. 1 highlights two key aspects of the patient-blood management for coronavirus disease 2019 (COVID-19) convalescent plasma (CCP) therapy in seronegative patients who are pre-exposed to B-cell-depleting agents. The first one relates to the qualitative composition of CCP used for patient treatment. The efficacy of CCP is strongly affected by the titres of neutralising antibodies (nAb) present at the time of donation. 2,3 Moreover, there is growing evidence that the nAb activity of plasma units collected from unvaccinated donors infected during the former COVID-19 waves is reduced against novel variants such as Omicron. 4 Hence, the efficacy of collected plasma is likely evolving alongside the exposure of potential donors to successive variant outbreaks and vaccination campaigns against severe acute respiratory syndrome coronavirus-2 (SARS-CoV-2).At the beginning of the pandemic, CCP was used as a front-line treatment; however, its wide heterogeneity in nAb titres made it difficult to recruit suitable donors of high neutralising titres, as defined by the United States Food and drug Administration (FDA). In contrast, nAb induced after two doses of mRNA vaccination have generally higher and more homogenous titres, which further remain effective against Omicron following a booster dose. 5 From March to July 2021, we treated 19 immunosuppressed patients with plasma collected from COVID-naive two-dose mRNA-vaccinated donors, under a compassionate use protocol, according to the Swiss regulation rules. 6 No relevant difference was observed between patients receiving CCP (n = 17) versus vaccinated plasma (VP, n = 19), indicating that VP therapy is safe and effective in patients with B-cell lymphopenia. In the meantime, CCP donors are increasingly getting vaccinated, and three-dose VP donors are being boosted by a breakthrough infection (defined as 'hybrid plasma', Vax-CCP or CP/VP). Their plasmas contain higher nAb titres and broader antibody specificity than CCP, 4,7,8 as shown by the increase in anti-spike immunoglobulin G titres between 2021 and 2022 (Figure 1A). Thus, Vax-CCP is emerging as the most convenient available source of polyclonal antibody plasma, given the failure of many monoclonal antibody therapies, due to the Omicron immune escape variants. 9

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supporting

confidence: 77%

supporting

confidence: 77%

mentioning

confidence: 99%

mentioning

confidence: 99%

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Understanding the parameters guiding the best practice for treating B‐cell‐depleted patients with COVID‐19 convalescent plasma therapy

2022

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“…It is biologically plausible that IC individuals who fail to produce an appropriate antibody response to COVID-19 and/or SARS-CoV-2 vaccination are likely to benefit from the SARS-CoV-2 antibodies provided by CCP. Established high risk groups that would qualify for CCP based on this definition include—but are not limited to—organ transplant recipients, patients with auto-immune diseases treated by B-cell depleting agents, and patients with cancer diagnoses, especially those with B-cell deficiency or depletion that may be primary (eg, due to malignancy) or acquired (eg, due to treatment with B-cell depleting agents such as Rituximab) [ 27 , 28 ]. Practically, these patients are likely to have a minimal or absent response to SARS-CoV-2 vaccination.…”

Section: Definition Of Immunocompromisementioning

confidence: 99%

Guidance on the Use of Convalescent Plasma to Treat Immunocompromised Patients With Coronavirus Disease 2019

Bloch

Focosi²,

Shoham

et al. 2023

Clinical Infectious Diseases

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COVID-19 convalescent plasma (CCP) is a safe and effective treatment for COVID-19 in immune compromised (IC) patients. IC patients have a higher risk of persistent infection, severe disease and death from COVID-19. Despite the continued clinical use of CCP to treat IC patients, the optimal dose, frequency/schedule, and duration of CCP treatment has yet to be determined, and related best practices guidelines are lacking. A group of individuals with expertise spanning infectious diseases, virology and transfusion medicine was assembled to render an expert opinion statement pertaining to the use of CCP for IC patients. For optimal effect, CCP should be recently and locally collected to match circulating variant. CCP should be considered for the treatment of IC patients with acute and protracted COVID-19; dosage depends on clinical setting (acute vs protracted COVID-19). CCP containing high-titer SARS-CoV-2 antibodies, retains activity against circulating SARS-CoV-2 variants, which have otherwise rendered monoclonal antibodies ineffective.

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Mortality Rates Among Hospitalized Patients With COVID-19 Treated With Convalescent Plasma: A Systematic Review and Meta-Analysis

Senefeld,

Gorman,

Johnson

et al. 2023

Mayo Clinic Proceedings: Innovations, Quality & Outcomes

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Antibody response and intra‐host viral evolution after plasma therapy in COVID‐19 patients pre‐exposed or not to B‐cell‐depleting agents

Cited by 9 publications

References 69 publications

Understanding the parameters guiding the best practice for treating B‐cell‐depleted patients with COVID‐19 convalescent plasma therapy

Understanding the parameters guiding the best practice for treating B‐cell‐depleted patients with COVID‐19 convalescent plasma therapy

Guidance on the Use of Convalescent Plasma to Treat Immunocompromised Patients With Coronavirus Disease 2019

Mortality Rates Among Hospitalized Patients With COVID-19 Treated With Convalescent Plasma: A Systematic Review and Meta-Analysis

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