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7. Quantification of the spread of SARS-CoV-2 variant B.1.1.7 in Switzerland

Author

Chen, Chaoran, Nadeau, Sarah Ann, Topolsky, Ivan, Manceau, Marc, Huisman, Jana S., Jablonski, Kim Philipp, Fuhrmann, Lara, Dreifuss, David, Jahn, Katharina, Beckmann, Christiane, Redondo, Maurice, Noppen, Christoph, Risch, Lorenz, Risch, Martin, Wohlwend, Nadia, Kas, Sinem, Bodmer, Thomas, Roloff, Tim, Stange, Madlen, Egli, Adrian, Eckerle, Isabella, Kaiser, Laurent, Denes, Rebecca, Feldkamp, Mirjam, Nissen, Ina, Santacroce, Natascha, Burcklen, Elodie, Aquino, Catharine, de Gouvea, Andreia Cabral, Moccia, Maria Domenica, Grüter, Simon, Sykes, Timothy, Opitz, Lennart, White, Griffin, Neff, Laura, Popovic, Doris, Patrignani, Andrea, Tracy, Jay, Schlapbach, Ralph, Dermitzakis, Emmanouil T., Harshman, Keith, Xenarios, Ioannis, Pegeot, Henri, Cerutti, Lorenzo, Penet, Deborah, Blin, Anthony, Elies, Melyssa, Althaus, Christian L., Beisel, Christian, Beerenwinkel, Niko, Ackermann, Martin, and Stadler, Tanja

Published
2021
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13. Respiratory viruses and severe lower respiratory tract complications in hospitalized patients *

Author

Garbino, Jorge, Gerbase, Margaret W., Wunderli, Werner, Kolarova, Lenka, Nicod, Laurent P., Rochat, Thierry, and Kaiser, Laurent

Subjects
Health
Abstract

Background: Acute respiratory viral infections are generally self-limited in healthy subjects but can lead to severe complications in immunocompromised hosts. We report the clinical impact of acute lower respiratory tract [...]

Published
2004

14. Orthopox viruses: is the threat growing?

Author

Boehm, Erik, Summermatter, Kathrin, and Kaiser, Laurent

Subjects
*SMALLPOX, *MONKEYPOX, *SCIENTIFIC literature, *MORTALITY, *TREATIES, *INTERNATIONAL cooperation
Abstract

Smallpox was a major cause of human mortality until its eradication, but the threat of orthopox viruses has not disappeared. Since the eradication of smallpox and the cessation of the related vaccination campaigns, the threat has been growing, as evidenced by the currently ongoing worldwide Mpox outbreak. In addition to threats of an evolving Mpox, we must also be aware of a myriad of other threats that remain. Many countries still lack biosecurity regulations reflecting the recent technological advances, and the threat of bioterrorism remains ever present. Reconstruction of smallpox is a distinct possibility, as are other scenarios whereby other orthopox viruses may be made more fit for transmission in humans. To outline and discuss potential biosafety and biosecurity threats posed by orthopox viruses. Published scientific literature, news articles, and international agreements. It would be wise to take steps to mitigate these threats now. Vaccination campaigns should be considered in areas with frequent orthopox outbreaks, and more efforts must be made to put a final end to the Mpox outbreak. In many countries, national biosafety and biosecurity regulations may need to be revised and strengthened to better reflect the threats posed by new technologies, including controls on synthesis of smallpox sequences. Furthermore, more international cooperation and aid is needed. The present global Mpox outbreak could likely have been prevented had areas where Mpox is endemic not been neglected. Future outbreaks could be much worse. [ABSTRACT FROM AUTHOR]

Published
2024
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16. Propagation of respiratory viruses in human airway epithelia reveals persistent virus-specific signatures.

Author

Essaidi-Laziosi, Manel, Brito, Francisco, Benaoudia, Sacha, Royston, Léna, Cagno, Valeria, Fernandes-Rocha, Mélanie, Piuz, Isabelle, Zdobnov, Evgeny, Huang, Song, Constant, Samuel, Boldi, Marc-Olivier, Kaiser, Laurent, and Tapparel, Caroline

Abstract

Background The leading cause of acute illnesses, respiratory viruses, typically cause self-limited diseases, although severe complications can occur in fragile patients. Rhinoviruses (RVs), respiratory enteroviruses (EVs), influenza virus, respiratory syncytial viruses (RSVs), and coronaviruses are highly prevalent respiratory pathogens, but because of the lack of reliable animal models, their differential pathogenesis remains poorly characterized. Objective We sought to compare infections by respiratory viruses isolated from clinical specimens using reconstituted human airway epithelia. Methods Tissues were infected with RV-A55, RV-A49, RV-B48, RV-C8, and RV-C15; respiratory EV-D68; influenza virus H3N2; RSV-B; and human coronavirus (HCoV)–OC43. Replication kinetics, cell tropism, effect on tissue integrity, and cytokine secretion were compared. Viral adaptation and tissue response were assessed through RNA sequencing. Results RVs, RSV-B, and HCoV-OC43 infected ciliated cells and caused no major cell death, whereas H3N2 and EV-D68 induced ciliated cell loss and tissue integrity disruption. H3N2 was also detected in rare goblet and basal cells. All viruses, except RV-B48 and HCoV-OC43, altered cilia beating and mucociliary clearance. H3N2 was the strongest cytokine inducer, and HCoV-OC43 was the weakest. Persistent infection was observed in all cases. RNA sequencing highlighted perturbation of tissue metabolism and induction of a transient but important immune response at 4 days after infection. No majority mutations emerged in the viral population. Conclusion Our results highlight the differential in vitro pathogenesis of respiratory viruses during the acute infection phase and their ability to persist under immune tolerance. These data help to appreciate the range of disease severity observed in vivo and the occurrence of chronic respiratory tract infections in immunocompromised hosts. [ABSTRACT FROM AUTHOR]

Published
2018
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17. Anti-apolipoprotein A-1 autoantibodies are associated with immunodeficiency and systemic inflammation in HIV patients.

Author

Satta, Nathalie, Pagano, Sabrina, Montecucco, Fabrizio, Gencer, Baris, Mach, François, Kaiser, Laurent, Calmy, Alexandra, Vuilleumier, Nicolas, and Swiss HIV Cohort Study

Subjects
HIV infections, AUTOANTIBODIES, IMMUNOGLOBULINS, INFLAMMATION, RNA, APOPTOSIS, IMMUNOLOGICAL deficiency syndromes, APOLIPOPROTEINS, ODDS ratio, T cells, CELL lines, HIV, LONGITUDINAL method
Abstract

Objectives: To determine the existence of autoantibodies against apolipoprotein A-1 (anti-apoA-1 IgG) in HIV patients and explore their association with biological features of HIV infection and different inflammatory biomarkers. We also evaluated their impact on CD4+ lymphocytes survival.Methods: Anti-apoA-1 IgG plasma levels were assessed by ELISA in 237 HIV positive patients from a national prospective cohort with no current lipid-lowering therapy.Results: 58% of patients were found positive for anti-apoA-1 IgG and were associated with lower CD4+ counts, but higher viremia and systemic inflammation. Logistic regression analyses indicated that high anti-apoA-1 IgG levels were associated with a 16-fold increased risk of displaying low CD4+ levels, independent of HIV RNA levels and treatment (adjusted Odds ratio [OR]:16.1, 95% Confidence Interval [95%CI]:1.80-143.6; p = 0.01), and a 6-fold increased risk of having a detectable viremia, independent of antiretroviral treatment (OR:5.47; 95% CI:1.63-18.36; p = 0.006). In vitro, anti-apoA-1 IgG induced dose and time-dependent CD4+ apoptosis that was increased by exposure to HIV RNA.Conclusions: In HIV patients, anti-apoA-1 IgG levels are associated with low CD4+ counts, high viremia and a pro-inflammatory systemic profile. Anti-apoA-1 IgG can promote CD4+ lymphocyte apoptosis via undefined pathways. [ABSTRACT FROM AUTHOR]

Published
2018
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21. Cerebral Rhizomucor Infection Treated by Posaconazole Delayed-Release Tablets in an Allogeneic Stem Cell Transplant Recipient.

Author

Andrey, Diego O., Kaiser, Laurent, Emonet, Stéphane, Erard, Veronique, Chalandon, Yves, and van Delden, Christian

Subjects
*MUCORMYCOSIS, *MYCOSES, *HEMATOPOIETIC stem cell transplantation, *LEUKEMIA, *PATIENTS, *THERAPEUTICS
Abstract

Summary Mucormycosis (zygomycosis) is an emerging fungal disease in allogeneic hematopoietic stem cell transplant (allo-HSCT) recipients. A 30-year-old woman diagnosed with acute myelomonocytic leukemia and needing allo-HSCT presented pulmonary and cerebral infection due to Rhizomucor pusillus. This fungal infection was treated with surgical treatment and posaconazole delayed-release tablets. This strategy allowed reaching high drug levels that could not be obtained with the posaconazole solution. [ABSTRACT FROM AUTHOR]

Published
2017
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22. The neural correlates of maternal sensitivity: An fMRI study.

Author

Musser, Erica D., Kaiser-Laurent, Heidemarie, and Ablow, Jennifer C.

Subjects
BRAIN function localization, MAGNETIC resonance imaging of the brain, PSYCHOLOGY of mothers, SENSITIVITY (Personality trait), PSYCHOLOGICAL distress, CRYING in infants
Abstract

Abstract: Research on maternal neural response to infant distress highlights circuits that may underlie differences in quality of maternal behavior. However, it is far from clear which circuits are relevant to maternal sensitivity, as opposed to other maternal behavioral dimensions, particularly after the early postpartum. This study examined maternal sensitivity, intrusiveness, and mother–infant dyadic harmony as correlates of mothers’ neural responses to the cries of their own infants. Twenty-two primiparous mothers were observed during an interaction with their infants at 18 months postpartum. In a separate functional neuroimaging session, mothers were exposed to their own infant''s cry sound, as well as unfamiliar infant''s cry and control sounds. Mothers who displayed more sensitive behaviors with their infant exhibited greater activation to their own infant''s cry compared to that of an unfamiliar infant in the right frontal pole and inferior frontal gyrus. Mothers who displayed more intrusive behaviors with their infant showed greater activation in the left anterior insula and temporal pole, while mothers who had more harmonious interactions with their infant displayed greater activation in left hippocampal regions. The roles of these areas in the regulation of maternal emotion and stress, self and other awareness, and empathy are examined. [Copyright &y& Elsevier]

Published
2012
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23. Robust innate responses to SARS-CoV-2 in children resolve faster than in adults without compromising adaptive immunity.

Author

Vono, Maria, Huttner, Angela, Lemeille, Sylvain, Martinez-Murillo, Paola, Meyer, Benjamin, Baggio, Stephanie, Sharma, Shilpee, Thiriard, Anais, Marchant, Arnaud, Godeke, Gert-Jan, Reusken, Chantal, Alvarez, Catia, Perez-Rodriguez, Francisco, Eckerle, Isabella, Kaiser, Laurent, Loevy, Natasha, Eberhardt, Christiane S., Blanchard-Rohner, Geraldine, Siegrist, Claire-Anne, and Didierlaurent, Arnaud M.

Abstract

SARS-CoV-2 infection in children is less severe than it is in adults. We perform a longitudinal analysis of the early innate responses in children and adults with mild infection within household clusters. Children display fewer symptoms than adults do, despite similar initial viral load, and mount a robust anti-viral immune signature typical of the SARS-CoV-2 infection and characterized by early interferon gene responses; increases in cytokines, such as CXCL10 and GM-CSF; and changes in blood cell numbers. When compared with adults, the antiviral response resolves faster (within a week of symptoms), monocytes and dendritic cells are more transiently activated, and genes associated with B cell activation appear earlier in children. Nonetheless, these differences do not have major effects on the quality of SARS-CoV-2-specific antibody responses. Our findings reveal that better early control of inflammation as observed in children may be key for rapidly controlling infection and limiting the disease course. [Display omitted] • Innate response against SARS-CoV-2 is robust in children despite limited symptoms • Resolution of inflammation and onset of B cell response occur faster in children • Antibody response is not compromised by the shorter antiviral inflammatory response SARS-CoV-2 infection in children is less severe than it is in adults. Vono et al. find that children mount a potent, but more transient, antiviral innate response with a more rapid onset of B cell response. A more efficient early control of inflammation may be key to limiting disease severity. [ABSTRACT FROM AUTHOR]

Published
2021
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26. Sequelae of Ebola virus disease: the emergency within the emergency.

Author

Vetter, Pauline, Kaiser, Laurent, Schibler, Manuel, Ciglenecki, Iza, and Bausch, Daniel G

Subjects
*EBOLA virus disease prevention, *DISEASE complications, *EMERGENCY medicine, *EPIDEMICS, *SEVERITY of illness index, *PREVENTION of epidemics, *EBOLA virus disease, *UVEITIS, *JOINT pain, *EBOLA virus, *PSYCHOLOGY
Abstract

As the massive outbreak of Ebola virus disease (EVD) in west Africa wanes, it has become increasingly clear that thousands of survivors have many sequelae, some of which might be very severe, such as arthritis and vision-threatening uveitis. The mental health effects of EVD on survivors and other family and community members is similarly profound. Furthermore, it is increasingly being recognised that Ebola virus might persist for weeks or months in selected body compartments of survivors, most notably in the semen of men, bringing risk of renewed transmission where it has previously been eliminated. These challenges to EVD survivors constitute a new emergency in terms of addressing individual patient need and to control the disease spread. In this Review, we assess what is known regarding the sequelae of EVD, including possible delayed virus clearance. We discuss some of the key challenges regarding the provision of care to survivors and implementation of necessary future research. [ABSTRACT FROM AUTHOR]

Published
2016
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27. Characteristics of long-COVID among older adults: a cross-sectional study.

Author

Daitch, Vered, Yelin, Dana, Awwad, Muhammad, Guaraldi, Giovanni, Milić, Jovana, Mussini, Cristina, Falcone, Marco, Tiseo, Giusy, Carrozzi, Laura, Pistelli, Francesco, Nehme, Mayssam, Guessous, Idris, Kaiser, Laurent, Vetter, Pauline, Bordas-Martínez, Jaume, Durà-Miralles, Xavier, Peleato-Catalan, Dolores, Gudiol, Carlota, Shapira-Lichter, Irit, and Abecasis, Donna

Subjects
*POST-acute COVID-19 syndrome, *OLDER people, *COUGH, *NATURAL history, *PULMONARY function tests, *FATIGUE (Physiology)
Abstract

• This study evaluated 2333 individuals at hospital-based COVID-19 recovery clinics. • Older adults are more likely to report long-COVID symptoms. • The most common long-COVID symptoms among older adults are fatigue and dyspnea. • Older age does not correlate with long-COVID fatigue or dyspnea. • Obesity is an independent risk factor for both long-COVID fatigue and dyspnea. To describe long-COVID symptoms among older adults and to assess the risk factors for two common long-COVID symptoms: fatigue and dyspnea. This is a multicenter, prospective cohort study conducted in Israel, Switzerland, Spain, and Italy. Individuals were included at least 30 days after their COVID-19 diagnosis. We compared long-COVID symptoms between elderly (aged >65 years) and younger individuals (aged 18-65 years) and conducted univariate and multivariable analyses for the predictors of long-COVID fatigue and dyspnea. A total of 2333 individuals were evaluated at an average of 5 months (146 days [95% confidence interval 142-150]) after COVID-19 onset. The mean age was 51 years, and 20.5% were aged >65 years. Older adults were more likely to be symptomatic, with the most common symptoms being fatigue (38%) and dyspnea (30%); they were more likely to complain of cough and arthralgia and have abnormal chest imaging and pulmonary function tests. Independent risk factors for long-COVID fatigue and dyspnea included female gender, obesity, and closer proximity to COVID-19 diagnosis; older age was not an independent predictor. Older individuals with long-COVID have different persisting symptoms, with more pronounced pulmonary impairment. Women and individuals with obesity are at risk. Further research is warranted to investigate the natural history of long-COVID among the elderly population and to assess possible interventions aimed at promoting rehabilitation and well-being. [ABSTRACT FROM AUTHOR]

Published
2022
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28. Impact of interactive computerised decision support for hospital antibiotic use (COMPASS): an open-label, cluster-randomised trial in three Swiss hospitals.

Author

Catho, Gaud, Sauser, Julien, Coray, Valentina, Da Silva, Serge, Elzi, Luigia, Harbarth, Stephan, Kaiser, Laurent, Marti, Christophe, Meyer, Rodolphe, Pagnamenta, Francesco, Portela, Javier, Prendki, Virginie, Ranzani, Alice, Centemero, Nicolò Saverio, Stirnemann, Jerome, Valotti, Roberta, Vernaz, Nathalie, Suter, Brigitte Waldispuehl, Bernasconi, Enos, and Huttner, Benedikt D

Subjects
*HOSPITAL utilization, *ANTIMICROBIAL stewardship, *INTRAVENOUS therapy, *HOSPITALS, *DRUG prescribing, *ANTIBIOTICS, *RESEARCH, *RESEARCH methodology, *ANTI-infective agents, *EVALUATION research, *COMPARATIVE studies, *RANDOMIZED controlled trials
Abstract

Background: Computerised decision-support systems (CDSSs) for antibiotic stewardship could help to assist physicians in the appropriate prescribing of antibiotics. However, high-quality evidence for their effect on the quantity and quality of antibiotic use remains scarce. The aim of our study was to assess whether a computerised decision support for antimicrobial stewardship combined with feedback on prescribing indicators can reduce antimicrobial prescriptions for adults admitted to hospital.Methods: The Computerised Antibiotic Stewardship Study (COMPASS) was a multicentre, cluster-randomised, parallel-group, open-label superiority trial that aimed to assess whether a multimodal computerised antibiotic-stewardship intervention is effective in reducing antibiotic use for adults admitted to hospital. After pairwise matching, 24 wards in three Swiss tertiary-care and secondary-care hospitals were randomised (1:1) to the CDSS intervention or to standard antibiotic stewardship measures using an online random sequence generator. The multimodal intervention consisted of a CDSS providing support for choice, duration, and re-evaluation of antimicrobial therapy, and feedback on antimicrobial prescribing quality. The primary outcome was overall systemic antibiotic use measured in days of therapy per admission, using adjusted-hurdle negative-binomial mixed-effects models. The analysis was done by intention to treat and per protocol. The study was registered with ClinicalTrials.gov (identifier NCT03120975).Findings: 24 clusters (16 at Geneva University Hospitals and eight at Ticino Regional Hospitals) were eligible and randomly assigned to control or intervention between Oct 1, 2018, and Dec 31, 2019. Overall, 4578 (40·2%) of 11 384 admissions received antibiotic therapy in the intervention group and 4142 (42·8%) of 9673 in the control group. The unadjusted overall mean days of therapy per admission was slightly lower in the intervention group than in the control group (3·2 days of therapy per admission, SD 6·2, vs 3·5 days of therapy per admission, SD 6·8; p<0·0001), and was similar among patients receiving antibiotics (7·9 days of therapy per admission, SD 7·6, vs 8·1 days of therapy per admission, SD 8·4; p=0·50). After adjusting for confounders, there was no statistically significant difference between groups for the odds of an admission receiving antibiotics (odds ratio [OR] for intervention vs control 1·12, 95% CI 0·94-1·33). For admissions with antibiotic exposure, days of therapy per admission were also similar (incidence rate ratio 0·98, 95% CI 0·90-1·07). Overall, the CDSS was used at least once in 3466 (75·7%) of 4578 admissions with any antibiotic prescription, but from the first day of antibiotic treatment for only 1602 (58·9%) of 2721 admissions in Geneva. For those for whom the CDSS was not used from the first day, mean time to use of CDSS was 8·9 days. Based on the manual review of 1195 randomly selected charts, transition from intravenous to oral therapy was significantly more frequent in the intervention group after adjusting for confounders (154 [76·6%] of 201 vs 187 [87%] of 215, +10·4%; OR 1·9, 95% CI 1·1-3·3). Consultations by infectious disease specialists were less frequent in the intervention group (388 [13·4%] of 2889) versus the control group (405 [16·9%] of 2390; OR 0·84, 95% CI 0·59-1·25).Interpretation: An integrated multimodal computerised antibiotic stewardship intervention did not significantly reduce overall antibiotic use, the primary outcome of the study. Contributing factors were probably insufficient uptake, a setting with relatively low antibiotic use at baseline, and delays between ward admission and first CDSS use.Funding: Swiss National Science Foundation.Translations: For the French and Italian translations of the abstract see Supplementary Materials section. [ABSTRACT FROM AUTHOR]

Published
2022
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29. The role of mitochondrial biogenesis and ROS in the control of energy supply in proliferating cells.

Author

Yoboue, Edgar D., Mougeolle, Alexis, Kaiser, Laurent, Averet, Nicole, Rigoulet, Michel, and Devin, Anne

Subjects
*MITOCHONDRIA formation, *REACTIVE oxygen species, *CELL proliferation, *ADENOSINE triphosphate, *OXIDATIVE phosphorylation, *CELLULAR signal transduction
Abstract

Abstract: In yeast, there is a constant growth yield during proliferation on non-fermentable substrate where the ATP generated originates from oxidative phosphorylation. This constant growth yield is due to a tight adjustment between the growth rate and the cellular mitochondrial amount. We showed that this cellular mitochondrial amount is strictly controlled by mitochondrial biogenesis. Moreover, the Ras/cAMP pathway is the cellular signaling pathway involved in the regulation of mitochondrial biogenesis, with a direct relationship between the activity of this pathway and the cellular amount of mitochondria. The cAMP protein kinase Tpk3p is the catalytic subunit specifically involved in the regulation of mitochondrial biogenesis through regulation of the mitochondrial ROS production. An overflow of mitochondrial ROS decreases mitochondrial biogenesis through a decrease in the transcriptional co-activator Hap4p, which can be assimilated to mitochondria quality control. Moreover, the glutathione redox state is shown as being an intermediate in the regulation of mitochondrial biogenesis. This article is part of a Special Issue entitled: 18th European Bioenergetic Conference. [Copyright &y& Elsevier]

Published
2014
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31. Low incidence of severe respiratory syncytial virus infections in lung transplant recipients despite the absence of specific therapy

Author

Uçkay, Ilker, Gasche-Soccal, Paola M., Kaiser, Laurent, Stern, Richard, Mazza-Stalder, Jesica, Aubert, John-David, and van Delden, Christian

Subjects
*LUNG transplantation, *RESPIRATORY syncytial virus, *DISEASE incidence, *COMMUNITY-acquired infections, *MORTALITY, *PLACEBOS, *RANDOMIZED controlled trials, *IMMUNOGLOBULINS, *PATIENTS
Abstract

Background: Respiratory syncytial virus (RSV) infections in lung transplant recipients (LTRs) have been associated with significant morbidity and mortality. Immunoglobulins, ribavirin, and palivizumab are suggested treatments for both pre-emptive and therapeutic purposes. However, in the absence of randomized, placebo-controlled trials, efficacy is controversial and there is toxicity as well as cost concerns. Methods: We retrospectively reviewed cases of lower respiratory tract RSV infections in adult LTRs. Diagnosis was based on clinical history, combined with a positive polymerase chain reaction (PCR) and/or viral cultures of bronchoalveolar lavage (BAL) specimens. Results: Ten symptomatic patients were identified (7 men and 3 women, age range 28 to 64 years). All were hospitalized for community-acquired respiratory tract infections. Two patients had a concomitant acute Grade A3 graft rejection, and 1 patient had a concomitant bacterial pneumonia. Eight patients did not receive a specific anti-RSV treatment because of clinical stability and/or improvement at the time of RSV diagnosis. Only 2 patients (1 with Grade A3 allograft rejection and 1 requiring mechanical ventilation) received ribavirin and palivizumab. All patients recovered without complications and with no persistent RSV infection. However, bronchiolitis obliterans (BOS) staging worsened in 6 patients during the mean follow-up of 45 months. Conclusions: Our data suggest that mild RSV infections in LTRs might evolve favorably in the absence of specific anti-viral therapy. However, this observation needs confirmation in a large clinical trial specifically investigating the development of BOS in untreated vs treated patients. [Copyright &y& Elsevier]

Published
2010
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32. Novel SARS-CoV-2 variants: the pandemics within the pandemic.

Author

Boehm, Erik, Kronig, Ilona, Neher, Richard A., Eckerle, Isabella, Vetter, Pauline, and Kaiser, Laurent

Subjects
*COVID-19, *SARS-CoV-2, *COVID-19 pandemic, *PANDEMICS, *VACCINE effectiveness, *CELL receptors
Abstract

Many new variants of the severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2) have been termed variants of concern/interest (VOC/I) because of the greater risk they pose due to possible enhanced transmissibility and/or severity, immune escape, diagnostic and/or treatment failure, and reduced vaccine efficacy. We sought to review the current knowledge of emerging SARS-CoV-2 variants, particularly those deemed VOC/Is: B.1.351, B.1.1.7, and P.1. MEDLINE and BioRxiv databases, as well as the grey literature, were searched for reports of SARS-CoV-2 variants since November 2020. Relevant articles and their references were screened. Mutations on the spike protein in particular may affect both affinity for the SARS-CoV-2 cell receptor ACEII and antibody binding. These VOC/Is often share similar mutation sets. The N501Y mutation is shared by the three main VOCs: B.1.1.7, first identified in the United Kingdom, P.1, originating from Brazil, and B.1.351, first described in South Africa. This mutation likely increases transmissibility by increasing affinity for ACEII. The B.1.351 and P.1 variants also display the E484K mutation which decreases binding of neutralizing antibodies, leading to partial immune escape; this favours reinfections, and decreases the in vitro efficacy of some antibody therapies or vaccines. Those mutations may also have phenotypical repercussions of greater severity. Furthermore, the accumulation of mutations poses a diagnostic risk (lowered when using multiplex assays), as seen for some assays targeting the S gene. With ongoing surveillance, many new VOC/Is have been identified. The emergence of the E484K mutation independently in different parts of the globe may reflect the adaptation of SARS-CoV-2 to humans against a background of increasing immunity. These VOC/Is are increasing in frequency globally and pose challenges to any herd immunity approach to managing the pandemic. While vaccination is ongoing, vaccine updates may be prudent. The virus continues to adapt to transmission in humans, and further divergence from the initial Wuhan sequences is expected. [ABSTRACT FROM AUTHOR]

Published
2021
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33. Definitions for coronavirus disease 2019 reinfection, relapse and PCR re-positivity.

Author

Yahav, Dafna, Yelin, Dana, Eckerle, Isabella, Eberhardt, Christiane S., Wang, Jianwei, Cao, Bin, and Kaiser, Laurent

Subjects
*COVID-19, *MIDDLE East respiratory syndrome
Abstract

SARS-CoV-2 RT-PCR re-positivity SARS-CoV-2 RT-PCR re-positivity describes positive RT-PCR following negative tests in an asymptomatic patient up to 90 days from the first episode. Keywords: COVID-19; PCR re-positivity; Reinfection; Relapse EN COVID-19 PCR re-positivity Reinfection Relapse 315 318 4 03/03/21 20210301 NES 210301 Introduction Defining reinfection, relapsed infection and recurrence of positive (re-positive) nucleic acid detection might have clinical and epidemiological implications for treatment and infection control measures, respectively. (b) Proof of a reinfection with two positive SARS-CoV-2 RT-PCR tests with Ct < 35 (or proof of replicating virus by cell culture or detection of subgenomic RNA) at different time-points. COVID-19 reinfection In August 2020, To et al. described an asymptomatic patient from Hong Kong with a positive SARS-CoV-2 PCR test from a sample collected 142 days after a first symptomatic COVID-19 episode. [Extracted from the article]

Published
2021
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34. Long-term consequences of COVID-19: research needs.

Author

Yelin, Dana, Wirtheim, Eytan, Vetter, Pauline, Kalil, Andre C, Bruchfeld, Judith, Runold, Michael, Guaraldi, Giovanni, Mussini, Cristina, Gudiol, Carlota, Pujol, Miquel, Bandera, Alessandra, Scudeller, Luigia, Paul, Mical, Kaiser, Laurent, and Leibovici, Leonard

Subjects
*COVID-19, *COVID-19 pandemic, *SARS-CoV-2, *DISEASE complications, *MEDICAL research, *VIRAL pneumonia, *CLINICAL pathology, *PROGNOSIS, *EPIDEMICS
Published
2020
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35. Novel human astroviruses: Novel human diseases?

Author

Vu, Diem-Lan, Cordey, Samuel, Brito, Francisco, and Kaiser, Laurent

Subjects
*ASTROVIRUSES, *RNA, *DIARRHEA, *CROSS-species amplification, *CEREBROSPINAL fluid, *IMMUNOCOMPROMISED patients
Abstract

Astroviruses are small, non-enveloped, single-stranded positive RNA viruses that belong to the Astroviridae family. While classical human astroviruses (HAstV) are a well-recognized cause of acute non-bacterial diarrhea among young children worldwide, novel astroviruses, named HAstV-MLB and HAstV-VA/HMO, have been identified recently in humans by molecular assays. They are phylogenetically more related to animal astroviruses than to classical human astroviruses, thus suggesting cross-species transmission. Serological studies demonstrated a surprisingly high seroprevalence in certain populations and highlighted a high infection rate in the early years of life. Although their pathogenic role has not yet been clearly determined, novel astrovirus RNA sequences have been identified in different biological specimens of symptomatic patients, including the feces, plasma, cerebrospinal fluid, and brain biopsies. Thus, there is evidence that they could contribute not only to digestive tract infection, but also to unexpected clinical syndromes, notably encephalitis and meningitis. Severe infections affect mainly immunocompromised patients. These findings indicate that novel astroviruses should be considered in the differential diagnosis of immunocompromised patients with meningitis or encephalitis of unknown origin. [ABSTRACT FROM AUTHOR]

Published
2016
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36. The E119D neuraminidase mutation identified in a multidrug-resistant influenza A(H1N1)pdm09 isolate severely alters viral fitness in vitro and in animal models.

Author

Abed, Yacine, Bouhy, Xavier, L’Huillier, Arnaud G., Rhéaume, Chantal, Pizzorno, Andrés, Retamal, Miguel, Fage, Clément, Dubé, Karen, Joly, Marie-Hélène, Beaulieu, Edith, Mallett, Corey, Kaiser, Laurent, and Boivin, Guy

Subjects
*NEURAMINIDASE, *INFLUENZA treatment, *MULTIDRUG resistance, *GENETIC mutation, *RELENZA (Drug), *RECOMBINANT viruses, *IMMUNOCOMPROMISED patients, *ANIMAL models in research, *THERAPEUTICS
Abstract

We recently isolated an influenza A(H1N1)pdm09 E119D/H275Y neuraminidase (NA) variant from an immunocompromised patient who received oseltamivir and zanamivir therapies. This variant demonstrated cross resistance to zanamivir, oseltamivir, peramivir and laninamivir. In this study, the viral fitness of the recombinant wild-type (WT), E119D and E119D/H275Y A(H1N1)pdm09 viruses was evaluated in vitro and in experimentally-infected C57BL/6 mice and guinea pigs. In replication kinetics experiments, viral titers obtained with the E119D and E119D/H275Y recombinants were up to 2- and 4-log lower compared to the WT virus in MDCK and ST6GalI-MDCK cells, respectively. Enzymatic studies revealed that the E119D mutation significantly decreased the surface NA activity. In experimentally-infected mice, a 50% mortality rate was recorded in the group infected with the WT recombinant virus whereas no mortality was observed in the E119D and E119D/H275Y groups. Mean lung viral titers on day 5 post-inoculation for the WT (1.2 ± 0.57 × 10 8 PFU/ml) were significantly higher than those of the E119D (9.75 ± 0.41 × 10 5 PFU/ml, P < 0.01 ) and the E119D/H275Y (1.47 ± 0.61 × 10 6 PFU/ml, P < 0.01 ) groups. In guinea pigs, comparable seroconversion rates and viral titers in nasal washes (NW) were obtained for the WT and mutant index and contact groups. However, the D119E reversion was observed in most NW samples of the E119D and E119D/H275Y animals. In conclusion, the E119D NA mutation that could emerge in A(H1N1)pdm09 viruses during zanamivir therapy has a significant impact on viral fitness and such mutant is unlikely to be highly transmissible. [ABSTRACT FROM AUTHOR]

Published
2016
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37. Ebola virus disease diagnosis by real-time RT-PCR: A comparative study of 11 different procedures.

Author

Cherpillod, Pascal, Schibler, Manuel, Vieille, Gaël, Cordey, Samuel, Mamin, Aline, Vetter, Pauline, and Kaiser, Laurent

Subjects
*EBOLA virus disease, *REVERSE transcriptase polymerase chain reaction, *EPIDEMICS, *MEDICAL practice, *VIRAL load, *BIOLOGICAL reagents, *DIAGNOSIS
Abstract

Background The diagnosis of Ebola virus disease relies on the detection of viral RNA in blood by real-time reverse-transcription PCR. While several of these assays were developed during the unprecedented 2013–2015 Ebola virus disease outbreak in West Africa, few were applied in the field. Objectives To compare technical performances and practical aspects of 11 Ebola virus real-time reverse-transcription PCR procedures. Study design We selected the most promising assays using serial dilutions of culture-derived Ebola virus RNA and determined their analytical sensitivity and potential range of quantification using quantified in vitro transcribed RNA; viral load values in the serum of an Ebola virus disease patient obtained with these assays were reported. Finally, ease of use and turnaround times of these kits were evaluated. Results Commercial assays were at least as sensitive as in-house tests. Five of the former (Altona, Roche, Fast-track Diagnostics, and Life Technologies) were selected for further evaluation. Despite differences in analytical sensitivity and limits of quantification, all of them were suitable for Ebola virus diagnosis and viral load estimation. The Lifetech Lyophilized Ebola Virus (Zaire 2014) assay (Life Technologies) appeared particularly promising, displaying the highest analytical sensitivity and shortest turnaround time, in addition to requiring no reagent freezing. Conclusions Commercial kits were at least as sensitive as in-house tests and potentially easier to use in the field than the latter. This qualitative comparison of real-time reverse transcription PCR assays may serve as a basis for the design of future Ebola virus disease diagnostics. [ABSTRACT FROM AUTHOR]

Published
2016
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38. Human three-dimensional engineered neural tissue reveals cellular and molecular events following cytomegalovirus infection.

Author

Cosset, Érika, Martinez, Yannick, Preynat-Seauve, Olivier, Lobrinus, Johannes-Alexander, Tapparel, Caroline, Cordey, Samuel, Peterson, Hedi, Petty, Tom J., Colaianna, Marilena, Tieng, Vannary, Tirefort, Diderik, Dinnyes, Andras, Dubois-Dauphin, Michel, Kaiser, Laurent, and Krause, Karl-Heinz

Subjects
*NERVE tissue, *TISSUE engineering, *CYTOMEGALOVIRUSES, *FETAL brain, *IMMUNOHISTOCHEMISTRY
Abstract

Human cytomegalovirus (HCMV) is the most common cause of congenital infection of the central nervous system (CNS). To overcome the limited access to human neural tissue and stringent species specificity of HCMV, we used engineered neural tissues to: (i) provide a technical advance to mimick features of HCMV infection in a human neural fetal tissue in vitro and (ii) characterize the molecular and cellular phenomenon following HCMV infection in this tissue. Herein, we infected hESC-derived engineered neural tissues (ENTs) whose organization resembles fetal brain. Transcriptome analysis of ENTs demonstrated that HCMV infection displayed features of the infection with the expression of genes involved in lipid metabolism, growth and development, as well as stress and host-response in a time-dependent manner. Immunohistochemical analysis demonstrated that HCMV did not firstly infect neural tubes ( i.e. radially organized, proliferating stem cell niches), but rather an adjacent side population of post-mitotic cells expressing nestin, doublecortin, Sox1, musashi and vimentin markers. Importantly, we observe the same tropism in naturally HCMV-infected fetal brain specimens. To the best of our knowledge this system represents the first human brain-like tissue able to provide a more physiologically model for studying HCMV infection. [ABSTRACT FROM AUTHOR]

Published
2015
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39. Role of rhinovirus load in the upper respiratory tract and severity of symptoms in lung transplant recipients.

Author

Ambrosioni, Juan, Bridevaux, Pierre-Olivier, Aubert, John-David, Soccal, Paola, Wagner, Ghislaine, and Kaiser, Laurent

Subjects
*RESPIRATORY infections, *RHINOVIRUSES, *VIRAL load, *LUNG transplantation, *SYMPTOMS, *REVERSE transcriptase polymerase chain reaction, *DIAGNOSIS
Abstract

Background Rhinovirus is the most common cause of respiratory viral infections and leads to frequent respiratory symptoms in lung transplant recipients. However, it remains unknown whether the rhinovirus load correlates with the severity of symptoms. Objectives This study aimed to better characterize the pathogenesis of rhinoviral infection and the way in which viral load correlates with symptoms. Study design We assessed rhinovirus load in positive upper respiratory specimens of patients enrolled prospectively in a cohort of 116 lung transplant recipients. Rhinovirus load was quantified according to a validated in-house, real-time, reverse transcription polymerase chain reaction in pooled nasopharyngeal and pharyngeal swabs. Symptoms were recorded in a standardised case report form completed at each screening/routine follow-up visit, or during any emergency visit occurring during the 3-year study. Results Rhinovirus infections were very frequent, including in asymptomatic patients not seeking a specific medical consultation. Rhinovirus load ranged between 4.1 and 8.3 log copies/ml according to the type of visit and clinical presentation. Patients with highest symptom scores tended to have higher viral loads, particularly those presenting systemic symptoms. When considering symptoms individually, rhinovirus load was significantly higher in the presence of symptoms such as sore throat, fever, sputum production, cough, and fatigue. There was no association between tacrolimus levels and rhinovirus load. Conclusions Rhinovirus infections are very frequent in lung transplant recipients and rhinoviral load in the upper respiratory tract is relatively high even in asymptomatic patients. Patients with the highest symptom scores tend to have a higher rhinovirus load. [ABSTRACT FROM AUTHOR]

Published
2015
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40. Seroprevalence of anti-SARS-CoV-2 antibodies after the second pandemic peak.

Author

Stringhini, Silvia, Zaballa, María-Eugenia, Perez-Saez, Javier, Pullen, Nick, de Mestral, Carlos, Picazio, Attilio, Pennacchio, Francesco, Wisniak, Ania, Richard, Aude, Baysson, Helene, Loizeau, Andrea, Balavoine, Jean-François, Trono, Didier, Pittet, Didier, Posfay-Barbe, Klara, Flahault, Antoine, Chappuis, François, Kherad, Omar, Vuilleumier, Nicolas, and Kaiser, Laurent

Subjects
*SEROPREVALENCE, *PANDEMICS, *IMMUNOGLOBULINS
Published
2021
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41. Comparative genetic analyses point to HCP5 as susceptibility locus for HCV-associated hepatocellular carcinoma.

Author

Lange, Christian M., Bibert, Stéphanie, Dufour, Jean-François, Cellerai, Cristina, Cerny, Andreas, Heim, Markus H., Kaiser, Laurent, Malinverni, Raffaele, Müllhaupt, Beat, Negro, Francesco, Semela, David, Moradpour, Darius, Kutalik, Zoltán, and Bochud, Pierre-Yves

Subjects
*COMPARATIVE genetics, *LIVER cancer, *DISEASE susceptibility, *HUMAN genetic variation, *SINGLE nucleotide polymorphisms, *HEPATITIS C virus, *JAPANESE people, *COHORT analysis, *PATIENTS, *DISEASES
Abstract

Background & Aims: Recently, genetic variations in MICA (lead single nucleotide polymorphism [SNP] rs2596542) were identified by a genome-wide association study (GWAS) to be associated with hepatitis C virus (HCV)-related hepatocellular carcinoma (HCC) in Japanese patients. In the present study, we sought to determine whether this SNP is predictive of HCC development in the Caucasian population as well. Methods: An extended region around rs2596542 was genotyped in 1924 HCV-infected patients from the Swiss Hepatitis C Cohort Study (SCCS). Pair-wise correlation between key SNPs was calculated both in the Japanese and European populations (HapMap3: CEU and JPT). Results: To our surprise, the minor allele A of rs2596542 in proximity of MICA appeared to have a protective impact on HCC development in Caucasians, which represents an inverse association as compared to the one observed in the Japanese population. Detailed fine-mapping analyses revealed a new SNP in HCP5 (rs2244546) upstream of MICA as strong predictor of HCV-related HCC in the SCCS (univariable p =0.027; multivariable p =0.0002, odds ratio=3.96, 95% confidence interval=1.90–8.27). This newly identified SNP had a similarly directed effect on HCC in both Caucasian and Japanese populations, suggesting that rs2244546 may better tag a putative true variant than the originally identified SNPs. Conclusions: Our data confirms the MICA/HCP5 region as susceptibility locus for HCV-related HCC and identifies rs2244546 in HCP5 as a novel tagging SNP. In addition, our data exemplify the need for conducting meta-analyses of cohorts of different ethnicities in order to fine map GWAS signals. [Copyright &y& Elsevier]

Published
2013
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42. Picornavirus and enterovirus diversity with associated human diseases

Author

Tapparel, Caroline, Siegrist, Fredy, Petty, Tom J., and Kaiser, Laurent

Subjects
*PICORNAVIRUSES, *ENTEROVIRUSES, *GENETIC mutation, *RNA viruses, *CAPSIDS, *PHENOTYPES, *RNA polymerases, *HAND, foot & mouth disease
Abstract

Abstract: Members of the Picornaviridae family are non-enveloped, positive-stranded RNA viruses with a 30nm icosahedral capsid. This virus family exhibits a considerable amount of genetic variability driven both by mutation and recombination. Recently, three previously unknown human picornaviruses, namely the human Saffold cardiovirus, cosavirus and salivirus, have been identified in stools or respiratory samples from subjects presenting symptoms ranging from gastroenteritis to acute flaccid paralysis. However, these viruses were also frequently detected in asymptomatic subjects and their clinical relevance remains to be elucidated. The Enterovirus genus is a prototype example of the Picornaviridae heterogeneity at both genetic and phenotypic levels. This genus is divided into 10 species, seven of which contain human viruses, including three Rhinovirus species. Both human rhino- and enteroviruses are also characterized by high levels of genetic variability, as exemplified by the existence of over 250 different serotypes and the recent discovery of new enterovirus genotypes and the Rhinovirus C species. Despite their common genomic features, rhinoviruses are restricted to the respiratory tract, whereas the vast majority of enteroviruses infect the gastrointestinal tract and can spread to other organs, such as the heart or the central nervous system. Understanding the genetic determinants of such phenotypic diversity is an important challenge and a field for future investigation. Better characterization of these ubiquitous human pathogens may help to develop vaccines or antiviral treatments and to monitor the emergence of new strains. [Copyright &y& Elsevier]

Published
2013
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43. Influenza Virus Partially Counteracts Restriction Imposed by Tetherin/BST-2.

Author

Mangeat, Bastien, Cavagliotti, Lorris, Lehmann, Martin, Gers-Huber, Gustavo, Kaur, Inderdeep, Thomas, Yves, Kaiser, Laurent, and Piguet, Vincent

Subjects
*INFLUENZA viruses, *INTERFERONS, *PROTEINS, *ANTIVIRAL agents, *VIRION
Abstract

Influenza virus infections lead to a burst of type I interferon (IFN) in the human respiratory tract, which most probably accounts for a rapid control of the virus. Although in mice, IFNinduced Mx1 factor mediates a major part of this response, the situation is less clear in humans. Interestingly, a recently identified IFN-induced cellular protein, tetherin (also known as CD317, BST-2, or HM1.24), exerts potent antiviral activity against a broad range of retroviruses, as well as several other enveloped viruses, by impeding the release of newly generated viral particles from the cell surface. Here we show that influenza virus belongs to the targets of this potent antiviral factor. Ectopic expression of tetherin strongly inhibited fully replicative influenza virus. In addition, depleting endogenous tetherin increased viral production of influenza virions, both in cells constitutively expressing tetherin and upon its induction by IFN. We further demonstrate, by biochemical and morphological means, that tetherin exerts its antiviral action by tethering newly budded viral particles, a mechanism similar to the one that operates against HIV-1. In addition, we determined that the magnitude of tetherin antiviral activity is comparable with or higher than the one of several previously identified anti-influenza cellular factors, such as MxA, ADAR1, ISG15, and viperin. Finally, we demonstrate that influenza virus reduces the impact of tetherin-mediated restriction on its replication by several mechanisms. First, the influenza virus NS1 protein impedes IFN-mediated tetherin induction. Second, influenza infection leads to a decrease of tetherin steady state levels, and the neuraminidase surface protein partly counteracts its activity. Overall, our study helps to delineate the intricate molecular battle taking place between influenza virus and its host cells. [ABSTRACT FROM AUTHOR]

Published
2012
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44. Antibody responses to natural influenza A/H1N1/09 disease or following immunization with adjuvanted vaccines, in immunocompetent and immunocompromised children

Author

Meier, Sara, Bel, Michael, L’Huillier, Arnaud, Crisinel, Pierre-Alex, Combescure, Christophe, Kaiser, Laurent, Grillet, Stéphane, Pósfay-Barbe, Klara, and Siegrist, Claire-Anne

Subjects
*INFLUENZA A virus, H1N1 subtype, *H1N1 influenza, *IMMUNOLOGICAL adjuvants, *ANTIBODY titer, *VACCINATION of children, *COHORT analysis, *BLOOD agglutination, *CHRONIC diseases, *REVERSE transcriptase polymerase chain reaction, *VACCINATION
Abstract

Abstract: Objectives: To compare antibody responses elicited by influenza A/H1N1/09 disease and immunization with adjuvanted vaccines, in immunocompetent or immunocompromised children. Study design: Prospective parallel cohort field study enrolling children with confirmed influenza A/H1N1/09 disease or immunized with 1 (immunocompetent) or 2 (immunocompromised) doses of influenza A/H1N1/09 squalene-based AS03- or MF59-adjuvanted vaccines. Antibody geometric mean titers (GMT) were measured by hemagglutination inhibition (HAI) and microneutralization (MN) assays 4–6 weeks after vaccination/disease. Vaccine adverse events were self-recorded in a 7-day diary. Results: Antibody titers were as high in 48 immunocompetent children after a single immunization (HAI and MN seroprotection rates: 98%; HAI-GMT: 395, MN-GMT: 370) as in 51 convalescent children (seroprotection rates: 98% (HAI) and 92% (MN); GMT: 350 (HAI) and 212 (MN). Twenty-seven immunocompromised children reached slightly lower seroprotection rates (HAI: 89%, MN: 85%) but similar antibody titers (HAI-GMT: 306, MN-GMT: 225) after 2 immunizations. Adverse events increased with age (P =0.01) and were more frequent with Pandemrix® than Focetria® (P =0.03). Conclusions: Similarly high seroresponses may be expected in immunocompetent children after a single dose of adjuvanted vaccines as responses of convalescent children. Two vaccine doses were sufficient for most immunocompromised children. Trial registration: NCT0102293 and NCT01022905. [Copyright &y& Elsevier]

Published
2011
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45. Persistence of anti-SARS-CoV-2 antibodies: immunoassay heterogeneity and implications for serosurveillance.

Author

Perez-Saez, Javier, Zaballa, María-Eugenia, Yerly, Sabine, Andrey, Diego O., Meyer, Benjamin, Eckerle, Isabella, Balavoine, Jean-François, Chappuis, François, Pittet, Didier, Trono, Didier, Kherad, Omar, Vuilleumier, Nicolas, Kaiser, Laurent, Guessous, Idris, Stringhini, Silvia, and Azman, Andrew S.

Subjects
*IMMUNOASSAY, *IMMUNOGLOBULINS, *COVID-19 pandemic, *VIRAL antibodies, *SARS-CoV-2, *SENSITIVITY & specificity (Statistics), *SEROPREVALENCE
Abstract

Serological studies have been critical in tracking the evolution of the COVID-19 pandemic. Data on anti-SARS-CoV-2 antibodies persistence remain sparse, especially from infected individuals with few to no symptoms. The objective of the study was to quantify the sensitivity for detecting historic SARS-CoV-2 infections as a function of time since infection for three commercially available SARS-CoV-2 immunoassays and to explore the implications of decaying immunoassay sensitivity in estimating seroprevalence. We followed a cohort of mostly mild/asymptomatic SARS-CoV-2-infected individuals (n = 354) at least 8 months after their presumed infection date and tested their serum for anti-SARS-CoV-2 antibodies with three commercially available assays: Roche-N, Roche-RBD and EuroImmun-S1. We developed a latent class statistical model to infer the specificity and time-varying sensitivity of each assay and show through simulations how inappropriately accounting for test performance can lead to biased serosurvey estimates. Antibodies were detected at follow-up in 74–100% of participants, depending on immunoassays. Both Roche assays maintain high sensitivity, with the EuroImmun assay missing 40% of infections after 9 months. Simulations reveal that without appropriate adjustment for time-varying assay sensitivity, seroprevalence surveys may underestimate infection rates. Antibodies persist for at least 8 months after infection in a cohort of mildly infected individuals with detection depending on assay choice. Appropriate assay performance adjustment is important for the interpretation of serological studies in the case of diminishing sensitivity after infection. [ABSTRACT FROM AUTHOR]

Published
2021
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46. Clinical, virologic and immunologic features of a mild case of SARS-CoV-2 reinfection.

Author

Vetter, Pauline, Cordey, Samuel, Schibler, Manuel, Vieux, Laure, Despres, Lena, Laubscher, Florian, Andrey, Diego O., Martischang, Romain, Harbarth, Stephan, Cuvelier, Clémence, Bekliz, Meriem, Eckerle, Isabella, Siegrist, Claire-Anne, Didierlaurent, Arnaud M., Eberhardt, Christiane S., Meyer, Benjamin, and Kaiser, Laurent

Subjects
*COVID-19, *SARS-CoV-2, *REINFECTION, *MEDICAL personnel, *REVERSE transcriptase, *NUCLEOPROTEINS
Abstract

To report a case of severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2) reinfection 6 months after the first infection in a young healthy female physician. Both episodes led to mild coronavirus disease 2019 (COVID-19). SARS-CoV-2 infections were detected by real-time reverse transcriptase PCR (RT-PCR) on nasopharyngeal specimens. Reinfection was confirmed by whole-genome sequencing. Kinetics of total anti-S receptor binding domain immunoglobulins (Ig anti–S RBD), anti-nucleoprotein (anti-N) and neutralizing antibodies were determined in serial serum samples retrieved during both infection episodes. Memory B-cell responses were assessed at day 12 after reinfection. Whole-genome sequencing identified two different SARS-CoV-2 genomes both belonging to clade 20A, with only one nonsynonymous mutation in the spike protein and clustered with viruses circulating in Geneva (Switzerland) at the time of each of the corresponding episodes. Seroconversion was documented with low levels of total Ig anti–S RBD and anti-N antibodies at 1 month after the first infection, whereas neutralizing antibodies quickly declined after the first episode and then were boosted by the reinfection, with high titres detectable 4 days after symptom onset. A strong memory B-cell response was detected at day 12 after onset of symptoms during reinfection, indicating that the first episode elicited cellular memory responses. Rapid decline of neutralizing antibodies may put medical personnel at risk of reinfection, as shown in this case. However, reinfection leads to a significant boosting of previous immune responses. Larger cohorts of reinfected subjects with detailed descriptions of their immune responses are needed to define correlates of protection and their duration after infection. [ABSTRACT FROM AUTHOR]

Published
2021
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47. Antibody persistence in the first 6 months following SARS-CoV-2 infection among hospital workers: a prospective longitudinal study.

Author

L'Huillier, Arnaud G., Meyer, Benjamin, Andrey, Diego O., Arm-Vernez, Isabelle, Baggio, Stephanie, Didierlaurent, Arnaud, Eberhardt, Christiane S., Eckerle, Isabella, Grasset-Salomon, Carole, Huttner, Angela, Posfay-Barbe, Klara M., Royo, Irene Sabater, Pralong, Jacques A., Vuilleumier, Nicolas, Yerly, Sabine, Siegrist, Claire-Anne, and Kaiser, Laurent

Subjects
*COVID-19, *SARS-CoV-2, *NOSOCOMIAL infections, *HOSPITAL personnel, *VIRAL antibodies, *VIRAL proteins, *NUCLEOPROTEINS
Abstract

To evaluate longitudinally the persistence of humoral immunity for up to 6 months in a cohort of hospital employees with mild coronavirus disease 2019 (COVID-19). We measured anti-RBD (receptor binding domain of viral spike protein), anti-N (viral nucleoprotein) and neutralizing antibodies at 1, 3 and 6 months after mostly mild COVID-19 in 200 hospital workers using commercial ELISAs and a surrogate virus neutralization assay. Antibodies specific for severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2) persisted in all participants for up to 6 months. Anti-RBD geometric mean concentrations (GMCs) progressively increased between months 1 (74.2 U/mL, 95%CI: 62.7–87.8), 3 (103.2 U/mL, 95%CI: 87.9–121.2; p < 0.001), and 6 (123.3 U/mL, 95%CI: 103.4–147.0; p < 0.001) in the whole cohort. Anti-N antibodies were detectable in >97% at all times. Neutralizing antibodies were detectable in 99.5% of participants (195/196) at 6 months post infection. Their GMC progressively decreased between months 1 (20.1 AU/mL, 95%CI: 16.9–24.0), 3 (15.2 AU/mL, 95%CI: 13.2–17.6; p < 0.001) and 6 (9.4 AU/mL, 95%CI: 7.7–11.4; p < 0.001). RBD-ACE2-inhibiting antibody titres and anti-RBD antibody concentrations strongly correlated at each timepoint (all r > 0.86, p < 0.001). Disease severity was associated with higher initial anti-RBD and RBD-ACE2-inhibiting antibody titres, but not with their kinetics. Neutralizing antibodies persisted at 6 months in almost all participants, indicating more durability than initially feared. Anti-RBD antibodies persisted better and even increased over time, possibly related to the preferential detection of progressively higher-affinity antibodies. [ABSTRACT FROM AUTHOR]

Published
2021
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