Your search keyword '"Koopmans D.V.M., M.P.G. (Marion)"' showing total 200 results

151. Middle east respiratory syndrome coronavirus (MERS-CoV) infections in two returning travellers in the Netherlands, May 2014

Author

Kraaij-Dirkzwager, M. (Marleen), Timen, A. (Aura), Dirksen, K. (Kees), Gelinck, L.B.S. (Luc), Leyten, E.M.S. (Eliane), Groeneveld, P.H.P. (Paul), Jansen, C., Jonges, M. (Marcel), Raj, S., Thurkow, I., Gageldonk-Lafeber, A.B. (Rianne) van, Eijck, A.A. (Annemiek), Koopmans D.V.M., M.P.G. (Marion), Kraaij-Dirkzwager, M. (Marleen), Timen, A. (Aura), Dirksen, K. (Kees), Gelinck, L.B.S. (Luc), Leyten, E.M.S. (Eliane), Groeneveld, P.H.P. (Paul), Jansen, C., Jonges, M. (Marcel), Raj, S., Thurkow, I., Gageldonk-Lafeber, A.B. (Rianne) van, Eijck, A.A. (Annemiek), and Koopmans D.V.M., M.P.G. (Marion)

Abstract

Two patients, returning to the Netherlands from pilgrimage in Medina and Mecca, Kingdom of Saudi Arabia, were diagnosed with Middle East respiratory syndrome coronavirus (MERS-CoV) infection in May 2014. The source and mode of transmission have not yet been determined. Hospital-acquired infection and community-acquired infection are both possible.

Published

2014

152. The hanta hunting study: Underdiagnosis of puumala hantavirus infections in symptomatic non-travelling leptospirosis-suspected patients in the Netherlands, in 2010 and April to November 2011

Author

Goeijenbier, M. (Marco), Hartskeerl, R.A., Reimerink, J.H.J. (Johan), Verner-Carlsson, J., Wagenaar, J.F., Goris, M.G.A. (Marga), Martina, B.E.E. (Byron), Lundkvist, Å. (Åke), Koopmans D.V.M., M.P.G. (Marion), Osterhaus, A.D.M.E. (Albert), Gorp, E.C.M. (Eric) van, Reusken, C.B.E.M. (Chantal), Goeijenbier, M. (Marco), Hartskeerl, R.A., Reimerink, J.H.J. (Johan), Verner-Carlsson, J., Wagenaar, J.F., Goris, M.G.A. (Marga), Martina, B.E.E. (Byron), Lundkvist, Å. (Åke), Koopmans D.V.M., M.P.G. (Marion), Osterhaus, A.D.M.E. (Albert), Gorp, E.C.M. (Eric) van, and Reusken, C.B.E.M. (Chantal)

Abstract

Leptospirosis and haemorrhagic fever with renal syndrome (HFRS) are hard to distinguish clinically since these two important rodent-borne zoonoses share hallmark symptoms such as renal failure and haemorrhage. Leptospirosis is caused by infection with a spirochete while HFRS is the result of an infection with certain hantaviruses. Both diseases are relatively rare in the Netherlands. Increased incidence of HFRS has been observed since 2007 in countries that border the Netherlands. Since a similar rise in incidence has not been registered in the Netherlands, we hypothesise that due to overlapping clinical manifestations, hantavirus infections may be confused with leptospirosis, leading to underdiagnosis. Therefore, we tested a cohort of non-travelling Dutch patients with symptoms compatible with leptospirosis, but with a negative diagnosis, during 2010 and from April to November 2011. Sera were screened with pan-hantavirus IgG and IgM enzyme-linked immunosorbent assays (ELISAs). Sera with IgM reactivity were tested by immunofluorescence assay (IFA). ELISA (IgM positive) and IFA results were confirmed using focus reduction neutralisation tests (FRNTs). We found hantavirus-specific IgG and/or IgM antibodies in 4.3% (11/255) of samples taken in 2010 and in 4.1% (6/146) of the samples during the 2011 period. After FRNT confirmation, seven patients were classed as having acute Puumala virus infections. A review of hantavirus diagnostic requests revealed that at least three of the seven confirmed acute cases as well as seven probable acute cases of hantavirus infection were missed in the Netherlands during the study period.

Published

2014

153. Preparedness for admission of patients with suspected Ebola virus disease in European hospitals: A survey, August-September 2014

Author

Jong, M.D. (Menno) de, Reusken, C.B.E.M. (Chantal), Horby, P., Koopmans D.V.M., M.P.G. (Marion), Bonten, M., Chiche, J.D., Giaquinto, C., Welte, T., Leus, F., Schotsman, J., Goossens, H., Jong, M.D. (Menno) de, Reusken, C.B.E.M. (Chantal), Horby, P., Koopmans D.V.M., M.P.G. (Marion), Bonten, M., Chiche, J.D., Giaquinto, C., Welte, T., Leus, F., Schotsman, J., and Goossens, H.

Abstract

In response to the Ebola virus disease (EVD) outbreak in West Africa, the World Health Organization has advised all nations to prepare for the detection, investigation and management of confirmed and suspected EVD cases in order to prevent further spread through international travel. To gain insights into the state of preparedness of European hospitals, an electronic survey was circulated in August–September 2014 to 984 medical professionals representing 736 hospitals in 40 countries. The survey addressed the willingness and capacity to admit patients with suspected EVD as well as specific preparedness activities in response to the current Ebola crisis. Evaluable responses were received from representatives of 254 (32%) hospitals in 38 countries, mostly tertiary care centres, of which 46% indicated that they would admit patients with suspected EVD. Patient transfer agreements were in place for the majority of hospitals that would not admit patients. Compared with non-admitting hospitals, admitting hospitals were more frequently engaged in various preparedness activities and more often contained basic infrastructural characteristics such as admission rooms and laboratories considered important for infection control, but some gaps and concerns were also identified. The results of this survey help to provide direction towards further preparedness activities and prioritisation thereof.

Published

2014

154. Reply to Pawar et al

Author

Todd, S. (Stephen), Bruin, E.I. (Esther) de, Nhat, N.T.D. (Nguyen Thi Duy), Koopmans D.V.M., M.P.G. (Marion), Boni, A. (Alejandro), Todd, S. (Stephen), Bruin, E.I. (Esther) de, Nhat, N.T.D. (Nguyen Thi Duy), Koopmans D.V.M., M.P.G. (Marion), and Boni, A. (Alejandro)

Published

2014

155. Middle east respiratory syndrome coronavirus (MERS-CoV) RNA and neutralising antibodies in milk collected according to local customs from dromedary camels, Qatar, April 2014

Author

Reusken, C.B.E.M. (Chantal), Farag, E. (Elmoubasher), Jonges, M. (Marcel), Godeke, G-J. (Gert-Jan), El-Sayed, A.M. (Ahmed M.), Pas, S.D. (Suzan), Raj, V.S. (Stalin), Mohran, K.A. (Khaled A.), Moussa, H.A., Ghobashy, H. (Hazem), Alhajri, F. (Farhoud), Ibrahim, A.K., Bosch, B.J. (Berend Jan), Pasha, S.K., Al Romaihi, H.E. (Hamad), Al-Thani, M. (Mohamed), Al-Marri, S.A. (Salih), AlHajri, M.M. (Mohd), Haagmans, B.L. (Bart), Koopmans D.V.M., M.P.G. (Marion), Reusken, C.B.E.M. (Chantal), Farag, E. (Elmoubasher), Jonges, M. (Marcel), Godeke, G-J. (Gert-Jan), El-Sayed, A.M. (Ahmed M.), Pas, S.D. (Suzan), Raj, V.S. (Stalin), Mohran, K.A. (Khaled A.), Moussa, H.A., Ghobashy, H. (Hazem), Alhajri, F. (Farhoud), Ibrahim, A.K., Bosch, B.J. (Berend Jan), Pasha, S.K., Al Romaihi, H.E. (Hamad), Al-Thani, M. (Mohamed), Al-Marri, S.A. (Salih), AlHajri, M.M. (Mohd), Haagmans, B.L. (Bart), and Koopmans D.V.M., M.P.G. (Marion)

Published

2014

156. Exploring the potential of next-generation sequencing in detection of respiratory Viruses

Author

Prachayangprecha, S. (Slinporn), Schapendonk, C.M.E. (Claudia), Koopmans D.V.M., M.P.G. (Marion), Osterhaus, A.D.M.E. (Albert), Schürch, A. (Anita), Pas, S.D. (Suzan), Eijck, A.A. (Annemiek), Poovorawan, Y. (Yong), Haagmans, B.L. (Bart), Smits, S.L. (Saskia), Prachayangprecha, S. (Slinporn), Schapendonk, C.M.E. (Claudia), Koopmans D.V.M., M.P.G. (Marion), Osterhaus, A.D.M.E. (Albert), Schürch, A. (Anita), Pas, S.D. (Suzan), Eijck, A.A. (Annemiek), Poovorawan, Y. (Yong), Haagmans, B.L. (Bart), and Smits, S.L. (Saskia)

Abstract

Efficient detection of human respiratory viral pathogens is crucial in the management of patients with acute respiratory tract infection. Sequence-independent amplification of nucleic acids combined with next-generation sequencing technology and bioinformatics analyses is a promising strategy for identifying pathogens in clinical and public health settings. It allows the characterization of hundreds of different known pathogens simultaneously and of novel pathogens that elude conventional testing. However, major hurdles for its routine use exist, including cost, turnaround time, and especially sensitivity of the assay, as the detection limit is dependent on viral load, host genetic material, and sequencing depth. To obtain insights into these aspects, we analyzed nasopharyngeal aspirates from a cohort of 81 Thai children with respiratory disease for the presence of respiratory viruses using a sequence-independent next-generation sequencing approach and routinely used diagnostic real-time reverse transcriptase PCR (real-time RT-PCR) assays. With respect to the detection of rhinovirus and human metapneumovirus, the nextgeneration sequencing approach was at least as sensitive as diagnostic real-time RT-PCR in this small cohort, whereas for bocavirus and enterovirus, next-generation sequencing was less sensitive than real-time RT-PCR. The advantage of the sequencing approach over real-time RT-PCR was the immediate availability of virus-typing information. Considering the development of platforms capable of generating more output data at declining costs, next-generation sequencing remains of interest for future virus diagnosis in clinical and public health settings and certainly as an additional tool when screening results from real-time RT-PCR are negative. Copyright

Published

2014

157. Evaluation of yield of currently available diagnostics by sample type to optimize detection of respiratory pathogens in patients with a community-acquired pneumonia

Author

Huijskens, E. (Elisabeth), Rossen, J.W. (John), Kluytmans, J.A.J.W. (Jan), Zanden, A.G.M. (Adri) van der, Koopmans D.V.M., M.P.G. (Marion), Huijskens, E. (Elisabeth), Rossen, J.W. (John), Kluytmans, J.A.J.W. (Jan), Zanden, A.G.M. (Adri) van der, and Koopmans D.V.M., M.P.G. (Marion)

Abstract

Background: For the detection of respiratory pathogens, the sampling strategy may influence the diagnostic yield. Ideally, samples from the lower respiratory tract are collected, but they are difficult to obtain. Objectives: In this study, we compared the diagnostic yield in sputum and oropharyngeal samples (OPS) for the detection of respiratory pathogens in patients with community-acquired pneumonia (CAP), with the objective to optimize our diagnostic testing algorithm. Methods: Matched sputum samples, OPS, blood cultures, serum, and urine samples were taken from patients (>18 years) with CAP and tested for the presence of possible respiratory pathogens using bacterial cultures, PCR for 17 viruses and five bacteria and urinary antigen testing. Results: When using only conventional methods, that is, blood cultures, sputum culture, urinary antigen tests, a pathogen was detected in 49·6% of patients (n = 57). Adding molecular detection assays increased the yield to 80%. A pathogen was detected in 77 of the 115 patients in OPS or sputum samples by PCR. The sensitivity of the OPS was lower than that of the sputum samples (57% versus 74%). In particular, bacterial pathogens were more often detected in sputum samples. The sensitivity of OPS for the detection of most viruses was higher than in sputum samples (72% versus 66%), except for human rhinovirus and respiratory syncytial virus. Conclusion: Addition of PCR on both OPS and sputum samples significantly increased the diagnostic yield. For molecular detection of bacterial pathogens, a sputum sample is imperative, but for detection of most viral pathogens, an OPS is sufficient.

Published

2014

158. The value of signs and symptoms in differentiating between bacterial, viral and mixed aetiology in patients with community-acquired pneumonia

Author

Huijskens, E. (Elisabeth), Koopmans D.V.M., M.P.G. (Marion), Palmen, F.M.H. (Fernand M.), Erkel, A.J.M. (Adriana J.) van, Mulder, P.G.H. (Paul), Rossen, J.W. (John), Huijskens, E. (Elisabeth), Koopmans D.V.M., M.P.G. (Marion), Palmen, F.M.H. (Fernand M.), Erkel, A.J.M. (Adriana J.) van, Mulder, P.G.H. (Paul), and Rossen, J.W. (John)

Abstract

Current diagnostics for community-acquired pneumonia (CAP) include testing for a wide range of pathogens, which is costly and not always informative. We compared clinical and laboratory parameters of patients with CAP caused by different groups of pathogens to evaluate the potential for targeted diagnostics and directed treatment. In a prospective study, conducted between April 2008 and April 2

Published

2014

159. Emergence of the virulence-associated PB2 E627K substitution in a fatal human case of highly pathogenic avian influenza virus A(H7N7) infection as determined by illumina ultra-deep sequencing

Author

Jonges, M. (Marcel), Welkers, M.R.A. (Matthijs), Jeeninga, R.E. (Rienk), Meijer, A. (Adam), Schneeberger, P.M. (Peter), Fouchier, R.A.M. (Ron), Jong, M.D. (Menno) de, Koopmans D.V.M., M.P.G. (Marion), Jonges, M. (Marcel), Welkers, M.R.A. (Matthijs), Jeeninga, R.E. (Rienk), Meijer, A. (Adam), Schneeberger, P.M. (Peter), Fouchier, R.A.M. (Ron), Jong, M.D. (Menno) de, and Koopmans D.V.M., M.P.G. (Marion)

Abstract

Avian influenza viruses are capable of crossing the species barrier and infecting humans. Although evidence of human-to-human transmission of avian influenza viruses to date is limited, evolution of variants toward more-efficient human-to-human transmission could result in a new influenza virus pandemic. In both the avian influenza A(H5N1) and the recently emerging avian influenza A(H7N9) viruses, the polymerase basic 2 protein (PB2) E627K mutation appears to be of key importance for human adaptation. During a large influenza A(H7N7) virus outbreak in the Netherlands in 2003, the A(H7N7) virus isolated from a fatal human case contained the PB2 E627K mutation as well as a hemagglutinin (HA) K416R mutation. In this study, we aimed to investigate whether these mutations occurred in the avian or the human host by Illumina Ultra-Deep sequencing of three previously uninvestigated clinical samples obtained from the fatal case. In addition, we investigated three chicken samples, two of which were obtained from the source farm. Results showed that the PB2 E627K mutation was not present in any of the chicken samples tested. Surprisingly, the avian samples were characterized by the presence of influenza virus defective RNA segments, suggestive for the synthesis of defective interfering viruses during infection in poultry. In the human samples, the PB2 E627K mutation was identified with increasing frequency during infection. Our results strongly suggest that human adaptation marker PB2 E627K has emerged during virus infection of a single human host, emphasizing the importance of reducing human exposure to avian influenza viruses to reduce the likelihood of viral adaptation to humans.

Published

2014

160. Randomized controlled ferret study to assess the direct impact of 2008-09 trivalent inactivated influenza vaccine on A(H1N1)pdm09 disease risk

Author

Skowronski, D.M. (Danuta), Hamelin, M.E. (Marie Ève), Serres, G. (Gaston) de, Janjua, N.Z. (Naveed), Li, G. (Guiyun), Sabaiduc, S. (Suzana), Bouhy, X. (Xavier), Couture, C. (Christian), Leung, A. (Anders), Kobasa, D. (Darwyn), Embury-Hyatt, C. (Carissa), Bruin, E.I. (Esther) de, Balshaw, R. (Robert), Lavigne, S. (Sophie), Petric, M. (Martin), Koopmans D.V.M., M.P.G. (Marion), Boivin, G. (Guy), Skowronski, D.M. (Danuta), Hamelin, M.E. (Marie Ève), Serres, G. (Gaston) de, Janjua, N.Z. (Naveed), Li, G. (Guiyun), Sabaiduc, S. (Suzana), Bouhy, X. (Xavier), Couture, C. (Christian), Leung, A. (Anders), Kobasa, D. (Darwyn), Embury-Hyatt, C. (Carissa), Bruin, E.I. (Esther) de, Balshaw, R. (Robert), Lavigne, S. (Sophie), Petric, M. (Martin), Koopmans D.V.M., M.P.G. (Marion), and Boivin, G. (Guy)

Abstract

During spring-summer 2009, several observational studies from Canada showed increased risk of medically-attended, laboratory-confirmed A(H1N1)pdm09 illness among prior recipients of 2008-09 trivalent inactivated influenza vaccine (TIV). Explanatory hypotheses included direct and indirect vaccine effects. In a randomized placebo-controlled ferret study, we tested whether prior receipt of 2008-09 TIV may have directly influenced A(H1N1)pdm09 illness. Thirty-two ferrets (16/group) received 0.5 mL intra-muscular injections of the Canadian-manufactured, commercially-available, non-adjuvanted, split 2008-09 Fluviral or PBS placebo on days 0 and 28. On day 49 all animals were challenged (Ch0) with A(H1N1)pdm09. Four ferrets per group were randomly selected for sacrifice at day 5 post-challenge (Ch+5) and the rest followed until Ch+14. Sera were tested for antibody to vaccine antigens and A(H1N1)pdm09 by hemagglutination inhibition (HI), microneutralization (MN), nucleoprotein-based ELISA and HA1-based microarray assays. Clinical characteristics and nasal virus titers were recorded pre-challenge then post-challenge until sacrifice when lung virus titers, cytokines and inflammatory scores were determined. Baseline characteristics were similar between the two groups of influenza-naïve animals. Antibody rise to vaccine antigens was evident by ELISA and HA1-based microarray but not by HI or MN assays; virus challenge raised antibody to A(H1N1)pdm09 by all assays in both groups. Beginning at Ch+2, vaccinated animals experienced greater loss of appetite and weight than placebo animals, reaching the greatest between-group difference in weight loss relative to baseline at Ch+5 (7.4% vs. 5.2%; p = 0.01). At Ch+ 5 vaccinated animals had higher lung virus titers (log-mean 4.96 vs. 4.23pfu/mL, respectively; p = 0.01), lung inflammatory scores (5.8 vs. 2.1, respectively; p = 0.051) and cytokine levels (p.0.05). At Ch+14, both groups had recovered. Findings in influenza-naïve, systematic

Published

2014

161. Middle east respiratory syndrome coronavirus (MERS-CoV) serology in major livestock species in an affected region in Jordan, june to September 2013

Author

Reusken, C.B.E.M. (Chantal), Ababneh, M., Raj, V.S. (Stalin), Meyer, B. (Bernhard), Eljarah, A., Abutarbush, S., Godeke, G-J. (Gert-Jan), Bestebroer, T.M. (Theo), Zutt, I. (I.), Müller, M.A. (Marcel), Bosch, B.J. (Berend Jan), Rottier, P.J.M. (Peter), Osterhaus, A.D.M.E. (Albert), Drosten, C. (Christian), Haagmans, B.L. (Bart), Koopmans D.V.M., M.P.G. (Marion), Reusken, C.B.E.M. (Chantal), Ababneh, M., Raj, V.S. (Stalin), Meyer, B. (Bernhard), Eljarah, A., Abutarbush, S., Godeke, G-J. (Gert-Jan), Bestebroer, T.M. (Theo), Zutt, I. (I.), Müller, M.A. (Marcel), Bosch, B.J. (Berend Jan), Rottier, P.J.M. (Peter), Osterhaus, A.D.M.E. (Albert), Drosten, C. (Christian), Haagmans, B.L. (Bart), and Koopmans D.V.M., M.P.G. (Marion)

Abstract

Between June and September 2013, sera from 11 dromedary camels, 150 goats, 126 sheep and 91 cows were collected in Jordan, where

Published

2013

162. Specific serology for emerging human coronaviruses by protein microarray

Author

Reusken, C.B.E.M. (Chantal), Mou, H. (Huihui), Godeke, G-J. (Gert-Jan), Hoek, L. (Lia) van der, Meyer, B. (Bernhard), Müller, M.A. (Marcel), Haagmans, B.L. (Bart), Sousa, R. (Rita) de, Schuurman, N., Dittmer, U., Rottier, P.J.M. (Peter), Osterhaus, A.D.M.E. (Albert), Drosten, C. (Christian), Bosch, B.J. (Berend Jan), Koopmans D.V.M., M.P.G. (Marion), Reusken, C.B.E.M. (Chantal), Mou, H. (Huihui), Godeke, G-J. (Gert-Jan), Hoek, L. (Lia) van der, Meyer, B. (Bernhard), Müller, M.A. (Marcel), Haagmans, B.L. (Bart), Sousa, R. (Rita) de, Schuurman, N., Dittmer, U., Rottier, P.J.M. (Peter), Osterhaus, A.D.M.E. (Albert), Drosten, C. (Christian), Bosch, B.J. (Berend Jan), and Koopmans D.V.M., M.P.G. (Marion)

Abstract

We present a serological assay for the specific detection of IgM and IgG antibodies against the emerging human coronavirus hCoV-EMC and the SARS-CoV based on protein microarray technology. The assay uses the S1 receptor-binding subunit of the spike protein of hCoV-EMC and SARS-CoV as antigens. The assay has been validated extensively using putative cross-reacting sera of patient cohorts exposed to the four common hCoVs and sera from convalescent patients infected with hCoV-EMC or SARS-CoV.

Published

2013

163. Guiding outbreak management by the use of influenza a(H7NX) virus sequence analysis

Author

Jonges, M. (Marcel), Meijer, A. (Adam), Fouchier, R.A.M. (Ron), Koch, G. (Guus), Li, J., Pan, J.C., Chen, H. (Hong), Shu, Y.L. (Yue-Long), Koopmans D.V.M., M.P.G. (Marion), Jonges, M. (Marcel), Meijer, A. (Adam), Fouchier, R.A.M. (Ron), Koch, G. (Guus), Li, J., Pan, J.C., Chen, H. (Hong), Shu, Y.L. (Yue-Long), and Koopmans D.V.M., M.P.G. (Marion)

Abstract

The recently identified human infections with avian influenza A(H7N9) viruses in China raise important questions regarding possible source and risk to humans. Sequence comparison with an influenza A(H7N7) outbreak in the Netherlands in 2003 and an A(H7N1) epidemic in Italy in 1999-2000 suggests that widespread circulation of A(H7N9) viruses must have occurred in China. The emergence of human adaptation marker PB2 E627K in human A(H7N9) cases parallels that of the fatal A(H7N7) human case in the Netherlands.

Published

2013

164. Ability to cause erythema migrans differs between Borrelia burgdorferi sensu lato isolates

Author

Tijsse-Klasen, E. (Ellen), Pandak, N. (Nenad), Hengeveld, P. (Paul), Takumi, K. (Katsuhisa), Koopmans D.V.M., M.P.G. (Marion), Sprong, H. (Hein), Tijsse-Klasen, E. (Ellen), Pandak, N. (Nenad), Hengeveld, P. (Paul), Takumi, K. (Katsuhisa), Koopmans D.V.M., M.P.G. (Marion), and Sprong, H. (Hein)

Abstract

Background: Lyme borreliosis is a tick-borne disease caused by Borrelia burgdorferi sensu lato. The variety of characteristic and non-specific clinical manifestations is partially explained by its genetic diversity. We investigated the ability of B. burgdorferi sl isolates to cause erythema migrans. Methods. The genetic constellation of isolates from ticks was compared to isolates found in erythema migrans. PCR and sequence analysis was performed on the plasmid-encoded ospC and the chromosomal 5S-23S rDNA spacer region (IGS). Results: Seven different B. burgdorferi sl genospecies were identified in 152 borrelia isolates from ticks and erythema migrans biopsies. B afzelii (51%) and B. garinii (27%) were the most common in ticks. From the 44 sequences obtained from erythema migrans samples 42 were B. afzelii, one B. garinii and one B. bavariensis. Significant associations with erythema migrans formation were found for four IGS and two ospC types. Five from 45 ospC types were associated with more than one genospecies. Conclusions: B. burgdorferi sl isolates differ in their propensity to cause erythema migrans. These differences were also found within genospecies. In other words, although B. afzelii was mostly associated with erythema migrans, some B. afzelii isolates had a low ability to cause erythema migrans. Our data further support the occurrence of plasmid exchange between borrelia genospecies under natural conditions.

Published

2013

165. Authors' reply: Application of Bayesian methods to the inference of phylogeny for enterovirus surveillance

Author

Koopmans D.V.M., M.P.G. (Marion), Niesters, H.G.M. (Bert), Benschop, K. (Kimberley), Wolthers, K.C. (Katja), Schuurman, R. (Rob), Pas, S.D. (Suzan), Claas, E.C.J. (Eric), Kroneman, A. (Annelies), Rahamat-Langendoen, J. (Janette), Vennema, H. (Harry), Avoort, H.G.A.M. (Harrie) van der, Koopmans D.V.M., M.P.G. (Marion), Niesters, H.G.M. (Bert), Benschop, K. (Kimberley), Wolthers, K.C. (Katja), Schuurman, R. (Rob), Pas, S.D. (Suzan), Claas, E.C.J. (Eric), Kroneman, A. (Annelies), Rahamat-Langendoen, J. (Janette), Vennema, H. (Harry), and Avoort, H.G.A.M. (Harrie) van der

Published

2013

166. Profiling of Humoral Response to Influenza A(H1N1)pdm09 Infection and Vaccination Measured by a Protein Microarray in Persons with and without History of Seasonal Vaccination

Author

Huijskens, E. (Elisabeth), Reimerink, J.H.J. (Johan), Mulder, P.G.H. (Paul), Beek, J.J. (Hans) van, Meijer, A.C. (Sander), Bruin, E. (Erwin) de, Friesema, I.H.M., Jong, M.D. (Menno) de, Rimmelzwaan, G.F. (Guus), Peeters, M. (Marcel), Rossen, J.W. (John), Koopmans D.V.M., M.P.G. (Marion), Huijskens, E. (Elisabeth), Reimerink, J.H.J. (Johan), Mulder, P.G.H. (Paul), Beek, J.J. (Hans) van, Meijer, A.C. (Sander), Bruin, E. (Erwin) de, Friesema, I.H.M., Jong, M.D. (Menno) de, Rimmelzwaan, G.F. (Guus), Peeters, M. (Marcel), Rossen, J.W. (John), and Koopmans D.V.M., M.P.G. (Marion)

Abstract

Background: The influence of prior seasonal influenza vaccination on the antibody response produced by natural infection or vaccination is not well understood. Methods: We compared the profiles of antibody responses of 32 naturally infected subjects and 98 subjects vaccinated with a 2009 influenza A(H1N1) monovalent MF59-adjuvanted vaccine (Focetria®, Novartis), with and without a history of seasonal influenza vaccination. Antibodies were measured by hemagglutination inhibition (HI) assay for influenza A(H1N1)pdm09 and by protein microarray (PA) using the HA1 subunit for seven recent and historic H1, H2 and H3 influenza viruses, and three avian influenza viruses. Serum samples for the infection group were taken at the moment of collection of the diagnostic sample, 10 days and 30 days after onset of influenza symptoms. For the vaccination group, samples were drawn at baseline, 3 weeks after the first vaccination and 5 weeks after the second vaccination. Results: We showed that subjects with a history of seasonal vaccination generally exhibited higher baseline titers for the various HA1 antigens than subjects without a seasonal vaccination history. Infection and pandemic influenza vaccination responses in persons with a history of seasonal vaccination were skewed towards historic antigens. Conclusions: Seasonal vaccination is of significant influence on the antibody response to subsequent infection and vaccination, and further research is needed to understand the effect of annual vaccination on protective immunity.

Published

2013

167. Infectious disease transmission as a forensic problem: Who infected whom?

Author

Teunis, P.F.M. (Peter), Heijne, J.C.M. (Janneke ), Sukhrie, F.H.A. (Faizel), Eijkeren, J. (Jan) van, Koopmans D.V.M., M.P.G. (Marion), Kretzschmar, M.E.E. (Mirjam), Teunis, P.F.M. (Peter), Heijne, J.C.M. (Janneke ), Sukhrie, F.H.A. (Faizel), Eijkeren, J. (Jan) van, Koopmans D.V.M., M.P.G. (Marion), and Kretzschmar, M.E.E. (Mirjam)

Abstract

Observations on infectious diseases often consist of a sample of cases, distinguished by symptoms, and other characteristics, such as onset dates, spatial locations, genetic sequence of the pathogen and/or physiological and clinical data. Cases are often clustered, in space and time, suggesting that they are connected. By defining kernel functions for pairwise analysis of cases, a matrix of transmission probabilities can be estimated.We set up a Bayesian framework to integrate various sources of information to estimate the transmission network. The method is illustrated by analysing data from a multi-year study (2002-2007) of nosocomial outbreaks of norovirus in a large university hospital in the Netherlands. The study included 264 cases, the norovirus genotype was known in approximately 60 per cent of the patients. Combining all the available data allowed likely identification of individual transmission links between most of the cases (72%). This illustrates that the proposed method can be used to accurately reconstruct transmission networks, enhancing our understanding of outbreak dynamics and possibly leading to new insights into how to prevent outbreaks.

Published

2013

168. Course of pandemic influenza A(H1N1) 2009 virus infection in Dutch patients

Author

Friesema, I.H.M., Meijer, A. (Adam), Gageldonk-Lafeber, A.B. (Rianne) van, Lubben, M. (Mariken) van der, Beek, J.H.G.M. (Janko) van, Donker, G.A. (Gé), Prins, J.M. (Jan), Jong, M.D. (Menno) de, Boskamp, V. (Victor), Isken, L. (Leslie), Koopmans D.V.M., M.P.G. (Marion), Sande, M.A.B. (Marianne) van der, Friesema, I.H.M., Meijer, A. (Adam), Gageldonk-Lafeber, A.B. (Rianne) van, Lubben, M. (Mariken) van der, Beek, J.H.G.M. (Janko) van, Donker, G.A. (Gé), Prins, J.M. (Jan), Jong, M.D. (Menno) de, Boskamp, V. (Victor), Isken, L. (Leslie), Koopmans D.V.M., M.P.G. (Marion), and Sande, M.A.B. (Marianne) van der

Abstract

The clinical dynamics of influenza A(H1N1) 2009 infections in 61 laboratory-confirmed Dutch cases were examined. An episode lasted a median of 7·5days of which 2days included fever. Respiratory symptoms resolved slowly, while systemic symptoms peaked early in the episode and disappeared quickly. Severity of each symptom was rated highest in the first few days. Furthermore, dia

Published

2012

169. Unrecognized norovirus infections in health care institutions and their clinical impact

Author

Beersma, M.F.C. (Thijs), Sukhrie, F.H.A. (Faizel), Bogerman, J. (Jolanda), Verhoef, L. (Linda), Melo, M.M. (Mariana ) de, Vonk, A.G. (Alieke), Koopmans D.V.M., M.P.G. (Marion), Beersma, M.F.C. (Thijs), Sukhrie, F.H.A. (Faizel), Bogerman, J. (Jolanda), Verhoef, L. (Linda), Melo, M.M. (Mariana ) de, Vonk, A.G. (Alieke), and Koopmans D.V.M., M.P.G. (Marion)

Abstract

Noroviruses (NoVs) have emerged as the leading cause of acute viral gastroenteritis (GE) in humans. Although diagnostic facilities have greatly improved, significant underdiagnosis of NoV in hospitals may still occur, thereby increasing clinical burden and nosocomial spread. We evaluated the underdiagnosis of sporadic NoV infections in a tertiary care hospital and estimated its clinical impact. From December 2008 until July 2009, fecal samples specifically referred for bacterial but not viral examination were retrospectively tested for NoV by real-time PCR. The clinical and virological data from patients with undiagnosed NoV infection (missed patients) were evaluated and compared with those from patients with recognized NoV. During the study period, 45 patients with undiagnosed NoV were detected, whereas 50 patients were regularly diagnosed. The missed NoV cases were more frequently adults than children (80% versus 46%; P < 0.001). The viral load levels did not differ between the diagnosed and missed patients, but missed patients more frequently presented without diarrhea (20% versus 4%; P < 0.07). The newly admitted missed NoV cases with GE underwent more diagnostic imaging (24% versus 4%; P < 0.01) and tended to be hospitalized longer. When missed-NoV patients were included, the number of nosocomial clusters doubled and missed patients were index cases in 5 of the 6 clusters. These data indicate that NoV infections are frequently missed despite routine laboratory testing and demonstrate that underdiagnosis of NoV patients is associated with costly abdominal ima

Published

2012

170. Oseltamivir-resistant influenza A(H1N1)pdm09 virus in Dutch travellers returning from Spain, August 2012

Author

Meijer, A. (Adam), Jonges, M. (Marcel), Beek, P. (Paul) van, Swaan, C. (Corien), Osterhaus, A.D.M.E. (Albert), Daniels, R.S. (Rodney S.), Hurt, A.C. (Aeron), Koopmans D.V.M., M.P.G. (Marion), Meijer, A. (Adam), Jonges, M. (Marcel), Beek, P. (Paul) van, Swaan, C. (Corien), Osterhaus, A.D.M.E. (Albert), Daniels, R.S. (Rodney S.), Hurt, A.C. (Aeron), and Koopmans D.V.M., M.P.G. (Marion)

Abstract

Two Dutch travellers were infected with oseltamivirresistant influenza A(H1N1)pdm09 viruses with an H275Y neuraminidase substitution in early August 2012. Both cases were probably infected during separate holidays at the Catalonian coast (Spain). No epidemiological connection between the two cases was found, and neither of them was treated with oseltamivir before specimen collection. Genetic analysis of the neuraminidase gene revealed the presence of previously described permissive mutations that may increase the likelihood of such strains emerging and spreading widely.

Published

2012

171. Hepatitis E virus infection among solid organ transplant recipients, the Netherlands

Author

Pas, S.D. (Suzan), Man, R.A. (Robert) de, Mulders, C. (Claudia), Balk, A.H.M.M. (Aggie), Hal, P.Th.W. (Peter) van, Weimar, W. (Willem), Koopmans D.V.M., M.P.G. (Marion), Osterhaus, A.D.M.E. (Albert), Eijck, A.A. (Annemiek), Pas, S.D. (Suzan), Man, R.A. (Robert) de, Mulders, C. (Claudia), Balk, A.H.M.M. (Aggie), Hal, P.Th.W. (Peter) van, Weimar, W. (Willem), Koopmans D.V.M., M.P.G. (Marion), Osterhaus, A.D.M.E. (Albert), and Eijck, A.A. (Annemiek)

Abstract

We screened 1,200 living heart, lung, liver, and kidney transplant recipients for hepatitis E virus infection by reverse transcription PCR. In 12 (1%) patients, hepatitis E virus infection was identified; in 11 patients, chronic infection developed. This immunocompromised population is at risk for hepatitis E virus infection.

Published

2012

172. Macrolide resistance determination and molecular typing of Mycoplasma pneumoniae in respiratory specimens collected between 1997 and 2008 in the Netherlands

Author

Spuesens, E.B.M. (Emiel), Meijer, A. (Adam), Bierschenk, D. (Damien), Hoogenboezem, T. (Theo), Donker, G.A. (Gé), Hartwig, N.G. (Nico), Koopmans D.V.M., M.P.G. (Marion), Vink, C. (Cornelis), Rossum, A.M.C. (Annemarie) van, Spuesens, E.B.M. (Emiel), Meijer, A. (Adam), Bierschenk, D. (Damien), Hoogenboezem, T. (Theo), Donker, G.A. (Gé), Hartwig, N.G. (Nico), Koopmans D.V.M., M.P.G. (Marion), Vink, C. (Cornelis), and Rossum, A.M.C. (Annemarie) van

Abstract

An important role in the treatment regimens for Mycoplasma pneumoniae infections is played by macrolide (ML) antibiotics. In the past few years, however, a steady increase has been detected in the worldwide prevalence of ML-resistant (MLr) M. pneumoniae strains. It is obvious that this increase necessitates a continuous monitoring of MLr and, when detected, modification of antibiotic treatment modalities. Previously, we developed a pyrosequencing-based assay system for the genetic determination of MLr as well as molecular typing of M. pneumoniae. In this study, the sensitivity of this system was improved by the inclusion of a nested-PCR protocol. The modified system was applied to 114 M. pneumoniae-positive specimens that were obtained from a collection of 4,390 samples from patients with acute respiratory tract infections. These samples were collected between 1997 and 2008 in The Netherlands. The pyrosequencing system produced reliable data in 86% of the specimens that contained >500 M. pneumoniae genome copies/ml of patient sample. Each of these samples contained DNA of the ML-sensitive genotype. While 43% of the samples were found to harbor the M. pneumoniae subtype 1 genotype, 57% contained the subtype 2 genotype. We conclude that the pyrosequencing-based assay system is a useful tool for MLr determination and molecular typing of M. pneumoniae in patient samples. ML r-associated M. pneumoniae genotypes, however, were not found in the current study population. Copyright

Published

2012

173. Comparing pandemic to seasonal influenza mortality: Moderate impact overall but high mortality in young children

Author

Wijngaard, C.C. (Cees) van den, Asten, L. (Liselotte) van, Koopmans D.V.M., M.P.G. (Marion), Pelt, W. (Wilfrid) van, Nagelkerke, N.J.D. (Nico), Wielders, C.C.H. (Cornelia), Lier, A. (Alies) van, Hoek, W. (Wim) van der, Meijer, A. (Adam), Donker, G.A. (Gé), Dijkstra, F. (Frederika), Harmsen, C. (Carel), Sande, M.A.B. (Marianne) van der, Kretzschmar, M.E.E. (Mirjam), Wijngaard, C.C. (Cees) van den, Asten, L. (Liselotte) van, Koopmans D.V.M., M.P.G. (Marion), Pelt, W. (Wilfrid) van, Nagelkerke, N.J.D. (Nico), Wielders, C.C.H. (Cornelia), Lier, A. (Alies) van, Hoek, W. (Wim) van der, Meijer, A. (Adam), Donker, G.A. (Gé), Dijkstra, F. (Frederika), Harmsen, C. (Carel), Sande, M.A.B. (Marianne) van der, and Kretzschmar, M.E.E. (Mirjam)

Abstract

Background: We assessed the severity of the 2009 influenza pandemic by comparing pandemic mortality to seasonal influenza mortality. However, reported pandemic deaths were laboratory-confirmed - and thus an underestimation - whereas seasonal influenza mortality is often more inclusively estimated. For a valid comparison, our study used the same statistical methodology and data types to estimate pandemic and seasonal influenza mortality. Methods and Findings: We used data on all-cause mortality (1999-2010, 100% coverage, 16.5 million Dutch population) and influenza-like-illness (ILI) incidence (0.8% coverage). Data was aggregated by week and age category. Using generalized estimating equation regression models, we attributed mortality to influenza by associating mortality with ILI-incidence, while adjusting for annual shifts in association. We also adjusted for respiratory syncytial virus, hot/cold weather, other seasonal factors and autocorrelation. For the 2009 pandemic season, we estimated 612 (range 266-958) influenza-attributed deaths; for seasonal influenz

Published

2012

174. Comparative analysis of avian influenza virus diversity in poultry and humans during a highly pathogenic avian influenza A (H7N7) virus outbreak

Author

Jonges, M. (Marcel), Bataille, A. (Arnaud), Enserink, R. (Remko), Meijer, A. (Adam), Fouchier, R.A.M. (Ron), Stegeman, A. (Arjan), Koch, G. (Guus), Koopmans D.V.M., M.P.G. (Marion), Jonges, M. (Marcel), Bataille, A. (Arnaud), Enserink, R. (Remko), Meijer, A. (Adam), Fouchier, R.A.M. (Ron), Stegeman, A. (Arjan), Koch, G. (Guus), and Koopmans D.V.M., M.P.G. (Marion)

Abstract

Although increasing data have become available that link human adaptation with specific molecular changes in nonhuman influenza viruses, the molecular changes of these viruses during a large highly pathogenic avian influenza virus (HPAI) outbreak in poultry along with avian-to-human transmission have never been documented. By comprehensive virologic analysis of combined veterinary and human samples obtained during a large HPAI A (H7N7) outbreak in the Netherlands in 2003, we mapped the acquisition of human adaptation markers to identify the public health risk associated with an HPAI outbreak in poultry. Full-length hemagglutinin (HA), neuraminidase (NA), and PB2 sequencing of A (H7N7) viruses obtained from 45 human cases showed amino acid variations at different codons in HA (n = 20), NA (n = 23), and PB2 (n = 23). Identification o

Published

2011

175. Comparative analysis of avian influenza virus diversity in poultry and humans during a highly pathogenic avian influenza A (H7N7) virus outbreak

Author

Jonges, M. (Marcel), Bataille, A. (Arnaud), Enserink, R. (Remko), Meijer, A. (Adam), Fouchier, R.A.M. (Ron), Stegeman, A. (Arjan), Koch, G. (Guus), Koopmans D.V.M., M.P.G. (Marion), Jonges, M. (Marcel), Bataille, A. (Arnaud), Enserink, R. (Remko), Meijer, A. (Adam), Fouchier, R.A.M. (Ron), Stegeman, A. (Arjan), Koch, G. (Guus), and Koopmans D.V.M., M.P.G. (Marion)

Abstract

Although increasing data have become available that link human adaptation with specific molecular changes in nonhuman influenza viruses, the molecular changes of these viruses during a large highly pathogenic avian influenza virus (HPAI) outbreak in poultry along with avian-to-human transmission have never been documented. By comprehensive virologic analysis of combined veterinary and human samples obtained during a large HPAI A (H7N7) outbreak in the Netherlands in 2003, we mapped the acquisition of human adaptation markers to identify the public health risk associated with an HPAI outbreak in poultry. Full-length hemagglutinin (HA), neuraminidase (NA), and PB2 sequencing of A (H7N7) viruses obtained from 45 human cases showed amino acid variations at different codons in HA (n = 20), NA (n = 23), and PB2 (n = 23). Identification o

Published

2011

176. Evaluation of the antiviral response to zanamivir administered intravenously for treatment of critically ill patients with pandemic influenza A (H1N1) infection

Author

Fraaij, P.L.A. (Pieter), Vries, E. (Erhard) van der, Beersma, M.F.C. (Thijs), Riezebos-Brilman, A. (Annelies), Niesters, H.G.M. (Bert), Eijck, A.A. (Annemiek), Jong, M.D. (Menno) de, Reis Miranda, D. (Dinis) dos, Horrevorts, A.M., Ridwan, B.U., Wolfhagen, M.J.H.M., Houmes, R.J.M. (Robert Jan), Dissel, J.T. (Jaap) van, Fouchier, R.A.M. (Ron), Kroes, A. (Aloys), Koopmans D.V.M., M.P.G. (Marion), Osterhaus, A.D.M.E. (Albert), Boucher, C.A.B. (Charles), Fraaij, P.L.A. (Pieter), Vries, E. (Erhard) van der, Beersma, M.F.C. (Thijs), Riezebos-Brilman, A. (Annelies), Niesters, H.G.M. (Bert), Eijck, A.A. (Annemiek), Jong, M.D. (Menno) de, Reis Miranda, D. (Dinis) dos, Horrevorts, A.M., Ridwan, B.U., Wolfhagen, M.J.H.M., Houmes, R.J.M. (Robert Jan), Dissel, J.T. (Jaap) van, Fouchier, R.A.M. (Ron), Kroes, A. (Aloys), Koopmans D.V.M., M.P.G. (Marion), Osterhaus, A.D.M.E. (Albert), and Boucher, C.A.B. (Charles)

Abstract

A retrospective nationwide study on the use of intravenous (IV) zanamivir in patients receiving intensive care who were pretreated with oseltamivir in the Netherlands was performed. In 6 of 13 patients with a sustained reduction of the viral load, the median time to start IV zanamivir was 9 days (range, 4-11 days) compared with 14 days (range, 6-21 days) in 7 patients without viral load reduction (P = .052). Viral load response did not influence mortality. We conclude that IV zanamivir as late add-on therapy has limited effectiveness. The effect of an immediate start with IV zanamivir monotherapy or in combination with other drugs n

Published

2011

177. Prevalence of antibodies against seasonal influenza A and B viruses in children in Netherlands

Author

Bodewes, R. (Rogier), Mutsert, G. (Gerrie) de, Klis, F.R. (Fiona) van der, Ventresca, M., Wilks, S., Smith, D.J. (Derek James), Koopmans D.V.M., M.P.G. (Marion), Fouchier, R.A.M. (Ron), Osterhaus, A.D.M.E. (Albert), Rimmelzwaan, G.F. (Guus), Bodewes, R. (Rogier), Mutsert, G. (Gerrie) de, Klis, F.R. (Fiona) van der, Ventresca, M., Wilks, S., Smith, D.J. (Derek James), Koopmans D.V.M., M.P.G. (Marion), Fouchier, R.A.M. (Ron), Osterhaus, A.D.M.E. (Albert), and Rimmelzwaan, G.F. (Guus)

Abstract

To gain insight into the age at which children become infected with influenza viruses for the first time, we analyzed the seroprevalence of antibodies against influenza viruses in children 0 to 7 years of age in the Netherlands. Serum samples were collected during a cross-sectional population-based study in 2006 and 2007 and were tested for the presence of antibodies against influenza A/H1N1, A/H3N2, and B viruses representative of viruses present in previous influenza seasons using the hemagglutination inhibition assay. The seroprevalence of antibodies to influenza virus was higher in children 1 to 6 months of age than in children 7 to 12 months of age, which likely reflects the presence of maternally derived antibodies. The proportion of study subjects >1 year of age with detectable antibodies against influenza viruses gradually increased with age until they reached

Published

2011

178. Evaluation of Syndromic Surveillance in the Netherlands: Its Added Value and Recommendations for Implementation

Author

Wijngaard, C.C. (Cees) van den, Pelt, W. (Wilfred) van, Nagelkerke, N.J.D. (Nico), Kretzschmar, M.E.E. (Mirjam), Koopmans D.V.M., M.P.G. (Marion), Wijngaard, C.C. (Cees) van den, Pelt, W. (Wilfred) van, Nagelkerke, N.J.D. (Nico), Kretzschmar, M.E.E. (Mirjam), and Koopmans D.V.M., M.P.G. (Marion)

Abstract

In the last decade, syndromic surveillance has increasingly been used worldwide for detecting increases or outbreaks of infectious diseases that might be missed by surveillance based on laboratory diagnoses and notifications by clinicians alone. There is, however, an ongoing debate about the feasibility of syndromic surveillance and its potential added value. Here we present our perspective on syndromic surveillance, based on the results of a retrospective analysis of syndromic data from six Dutch healthcare registries, covering 1999–2009 or part of this period. These registries had been designed for other purposes, but were evaluated for their potential use in signalling infectious disease dynamics and outbreaks. Our results show that syndromic surveillance clearly has added value in revealing the blind spots of traditional surveillance, in particular by detecting unusual, local outbreaks independently of diagnoses of specific pathogens, and by monitoring disease burden and virulence shifts of common pathogens. Therefore we recommend the use of syndromic surveillance for these applications.

Published

2011

179. High probability of avian influenza virus (H7N7) transmission from poultry to humans active in disease control on infected farms

Author

Bos, M.E.H. (Marian), Beest, D.E. (Dennis) te, Boven, M. (Michiel) van, Holle, M.R.D.R.B. van, Meijer, A. (Adam), Bosman, A. (Arnold), Mulder, Y.M. (Yonne), Koopmans D.V.M., M.P.G. (Marion), Stegeman, A. (Arjan), Bos, M.E.H. (Marian), Beest, D.E. (Dennis) te, Boven, M. (Michiel) van, Holle, M.R.D.R.B. van, Meijer, A. (Adam), Bosman, A. (Arnold), Mulder, Y.M. (Yonne), Koopmans D.V.M., M.P.G. (Marion), and Stegeman, A. (Arjan)

Abstract

An epizootic of avian influenza (H7N7) caused a large number of human infections in The Netherlands in 2003. We used data from this epizootic to estimate infection probabilities for persons involved in disease control on infected farms. Analyses were based on databases containing information on the infected farms, person-visits to these farms, and exposure variables (number of birds present, housing type, poultry type, depopulation method, period during epizootic). Case definition was based on self-reported conjunctivitis and positive response to hemagglutination inhibition assay. A high infection probability was associated with clinical inspection of poultry in the area surrounding infected flocks (7.6%; 95% confidence interval [CI], 1.4%-18.9%) and active culling during depopulation (6.2%; 95% CI, 3.7%-9.6%). Low probabilities were estimated for management of biosecurity (0.0%; 95% CI, 0.0%-1.0%) and cleaning assistance during depopulation (0.0%; 95% CI, 0.0%-9.2%). No significant association was observed between the probability of infection and the exposure variables.

Published

2010

180. Clostridium difficile is not associated with outbreaks of viral gastroenteritis in the elderly in the Netherlands

Author

Svraka-Latifovic, S. (Sanela), Kuijper, E., Duizer, E. (Erwin), Bakker, D. (Dennis), Koopmans D.V.M., M.P.G. (Marion), Svraka-Latifovic, S. (Sanela), Kuijper, E., Duizer, E. (Erwin), Bakker, D. (Dennis), and Koopmans D.V.M., M.P.G. (Marion)

Abstract

The coincidental increase in norovirus outbreaks and Clostridium difficile infection (CDI) raised the question of whether these events could be related, e.g. by enhancing spread by diarrhoeal disease outbreaks. Therefore, we studied the prevalence of C. difficile in outbreaks of viral gastroenteritis in nursing homes for the elderly and characterised enzyme immunoassay (EIA)-positive stool samples. Stool samples from nursing home residents (n=752) in 137 outbreaks of viral aetiology were investigated by EIA for the presence of C. difficile toxins. Positive samples were further tested by a cell neutralisation cytotoxicity test, a second EIA and culture. Cultured isolates were tested for the presence of toxin genes, the production of toxins and characterised by 16S rRNA polymerase chain reaction (PCR) and sequencing. Twenty-four samples (3.2%) tested positive in the EIA. Of these 24 positive samples, only two were positive by cytotoxicity and three by a second EIA. Bacterial culture of 21 available stool samples yielded a toxinogenic C. difficile PCR ribotype 001 in one patient sample only. In conclusion, we found no evidence in this retrospective study for an association between viral gastroenteritis outbreaks and C. difficile. The high rate of false-positive EIA samples emphasises the need for second confirmation tests to diagnose CDI.

Published

2010

181. Detection of excess influenza severity: Associating respiratory hospitalization and mortality data with reports of influenza-like illness by primary care physicians

Author

Wijngaard, C.C. (Cees) van den, Asten, L. (Liselotte) van, Meijer, A. (Adam), Pelt, W. (Wilfrid) van, Nagelkerke, N.J.D. (Nico), Donker, G.A. (Gé), Sande, M.A.B. (Marianne) van der, Koopmans D.V.M., M.P.G. (Marion), Wijngaard, C.C. (Cees) van den, Asten, L. (Liselotte) van, Meijer, A. (Adam), Pelt, W. (Wilfrid) van, Nagelkerke, N.J.D. (Nico), Donker, G.A. (Gé), Sande, M.A.B. (Marianne) van der, and Koopmans D.V.M., M.P.G. (Marion)

Published

2010

182. Syndromic surveillance for local outbreaks of lower-respiratory infections: Would it work?

Author

Wijngaard, C.C. (Cees) van den, Asten, L. (Liselotte) van, Pelt, W. (Wilfrid) van, Doornbos, G. (Gerda), Nagelkerke, N.J.D. (Nico), Donker, G.A. (Gé), Hoek, W. (Wim) van der, Koopmans D.V.M., M.P.G. (Marion), Wijngaard, C.C. (Cees) van den, Asten, L. (Liselotte) van, Pelt, W. (Wilfrid) van, Doornbos, G. (Gerda), Nagelkerke, N.J.D. (Nico), Donker, G.A. (Gé), Hoek, W. (Wim) van der, and Koopmans D.V.M., M.P.G. (Marion)

Abstract

Background: Although syndromic surveillance is increasingly used to detect unusual illness, there is a debate whether it is useful for detecting local outbreaks. We evaluated whether syndromic surveillance detects local outbreaks of lower-respiratory infections (LRIs) without swamping true signals by false alarms. Methods and Findings: Using retrospective hospitalization data, we simulated prospective surveillance for LRI-elevations. Between 1999-2006, a total of 290762 LRIs were included by date of hospitalization and patients place of residence (>80% coverage, 16 million population). Two large outbreaks of Legionnaires disease in the Netherlands were used as positive controls to test whether these outbreaks could have been detected as local LRI elevations. We used a space-time permutation scan statistic to detect LRI clusters. We evaluated how many LRI-clusters were detected in 1999-2006 and assessed likely causes for the cluster-signals by looking for significantly higher proportions of specific hospital discharge diagnoses (e.g. Legionnaires disease) and overlap with regional influenza elevations. We also evaluated whether the number of space-time signals can be reduced by restricting the scan statistic in space or time. In 1999-2006 the scan-statistic detected 35 local LRI clusters, representing on average 5 clusters per year. The known Legionnaires' disease outbreaks in 1999 and 2006 were detected as LRI-clusters, since cluster-signals were generated with an increased proportion of Legionnaires disease patients (p:<0.0001). 21 other clusters coincided with local influenza and/or respiratory syncytial virus activity, and 1 cluster appeared to be a data artifact. For 11 clusters no likely cause was defined, some possibly representing as yet undetected LRI-outbreaks. With restrictions on time and spatial windows the scan statistic still detected the Legionnaires' disease outbreaks, without loss of timeliness and with less signals generated in time (up to 42% decl

Published

2010

183. Evolutionary trajectory of the VP1 gene of human enterovirus 71 genogroup B and C viruses

Author

Sanden, S.M.G. (Sabine) van der, Avoort, H.G.A.M. (Harrie) van der, Lemey, P. (Philippe), Uslu, G. (Gökhan), Koopmans D.V.M., M.P.G. (Marion), Sanden, S.M.G. (Sabine) van der, Avoort, H.G.A.M. (Harrie) van der, Lemey, P. (Philippe), Uslu, G. (Gökhan), and Koopmans D.V.M., M.P.G. (Marion)

Abstract

From 1963 to 1986, human enterovirus 71 (HEV71) infections in the Netherlands were successively caused by viruses of subgenogroups B0, B1 and B2. A genogroup shift occurred in 1987, after which viruses of subgenogroups C1 and C2 were detected exclusively. This is in line with HEV71 typing in Aust

Published

2010

184. Epidemiology and genotype analysis of emerging sapovirus-associated infections across Europe

Author

Svraka-Latifovic, S. (Sanela), Vennema, H. (Harry), Veer, B. (Bas) van der, Hedlund, K.O., Thorhagen, M. (Margareta), Siebenga, J.J. (Joukje), Duizer, E. (Erwin), Koopmans D.V.M., M.P.G. (Marion), Svraka-Latifovic, S. (Sanela), Vennema, H. (Harry), Veer, B. (Bas) van der, Hedlund, K.O., Thorhagen, M. (Margareta), Siebenga, J.J. (Joukje), Duizer, E. (Erwin), and Koopmans D.V.M., M.P.G. (Marion)

Abstract

Sapoviruses (SaVs) belong to the Caliciviridae family and can cause gastroenteritis in humans and swine. Despite extensive testing, human sapoviruses have been found only in sporadic cases and in one mixed outbreak in children between 1994 and 2007 in the Netherlands. Here we describe a change in sapovirus epidemiology in the Netherlands resulting in sapovirus outbreaks and infections in adults. From November 2007 to January 2009, 478 outbreaks of acute gastroenteritis were reported to the National Institute for Public Health and the Environment in the Netherlands as a part of ongoing surveillance. Sapoviruses were found to be the most likely cause of 19 outbreaks (4%). During the same 2-year period, sapovirus infections were reported in Sweden, Slovenia, and Hungary. In the Netherlands, further characterization of outbreak strains showed that 12 (63%) sapovirus outbreaks were caused by genotype I.2 viruses. Most patients were adults older than 60 years (range, 1 to 100 years). Phylogenetic analysis using all presently available SaV sequences showed high homology between genotype I.2 strains detected in different geographical regions (Sweden, Slovenia, Taiwan, Japan, and Russia) since 2007. These first reported outbreaks of sapovirus infections in adults in the Netherlands were remarkable. Detection of identical genotypes in many samples might suggest that these viruses have the same origin, and since the infection is spreading fast, the prevalence of sapovirus infection may be increasing. The incidence of sapovirus infections in these countries suggests that a substantial part of Europe is affected by this virus. Copyright

Published

2010

185. Phylodynamic reconstruction reveals norovirus GII.4 epidemic expansions and their molecular determinants

Author

Siebenga, J.J. (Joukje), Lemey, P. (Philippe), Pond, S.L.K. (Sergei), Rambaut, A. (Andrew), Vennema, H. (Harry), Koopmans D.V.M., M.P.G. (Marion), Siebenga, J.J. (Joukje), Lemey, P. (Philippe), Pond, S.L.K. (Sergei), Rambaut, A. (Andrew), Vennema, H. (Harry), and Koopmans D.V.M., M.P.G. (Marion)

Abstract

Noroviruses are the most common cause of viral gastroenteritis. An increase in the number of globally reported norovirus outbreaks was seen the past decade, especially for outbreaks caused by successive genogroup II genotype 4 (GII.4) variants. Whether this observed increase was due to an upswing in the number of infections, or to a surveillance artifact caused by heightened awareness and concomitant improved reporting, remained unclear. Therefore, we set out to study the population structu

Published

2010

186. Introduction of virulence markers in PB2 of pandemic swine-origin influenza virus does not result in enhanced virulence or transmission

Author

Herfst, S. (Sander), Chutinimitkul, S. (Salin), Ye, J. (Jian), Wit, E. (Emmie) de, Munster, V.J. (Vincent), Schrauwen, E.J.A. (Eefje), Bestebroer, T.M. (Theo), Jonges, M. (Marcel), Meijer, A. (Adam), Koopmans D.V.M., M.P.G. (Marion), Rimmelzwaan, G.F. (Guus), Osterhaus, A.D.M.E. (Albert), Perez, D.R. (Daniel), Fouchier, R.A.M. (Ron), Herfst, S. (Sander), Chutinimitkul, S. (Salin), Ye, J. (Jian), Wit, E. (Emmie) de, Munster, V.J. (Vincent), Schrauwen, E.J.A. (Eefje), Bestebroer, T.M. (Theo), Jonges, M. (Marcel), Meijer, A. (Adam), Koopmans D.V.M., M.P.G. (Marion), Rimmelzwaan, G.F. (Guus), Osterhaus, A.D.M.E. (Albert), Perez, D.R. (Daniel), and Fouchier, R.A.M. (Ron)

Abstract

In the first 6 months of the H1N1 swine-origin influenza virus (S-OIV) pandemic, the vast majority of infections were relatively mild. It has been postulated that mutations in the viral genome could result in more virulent viruses, leading to a more severe pandemic. Mutations E627K and D701N in the PB2 protein have previously been identified as determinants of avian and pandemic influenza virus virulence in mammals. These mutations were absent in S-OIVs detected early in the 2009 pandemic. Here, using reverse genetics, mutations E627K, D701N, and E677G were introduced into the prototype S-OIV A/Netherlands/602/2009, and their effects on virus replication, virulence, and transmission were investigated. Mutations E627K and D701N caused increased reporter gene expression driven by the S-OIV polymerase complex. None of the three mutations affected virus replication in vitro. The mutations had no major impact on virus replication in the respiratory tracts of mice and ferrets or on pathogenesis. All three mutant viruses were transmitted via aerosols or respiratory droplets in ferrets. Thus, the impact of key known virulence markers in PB2 in the context of current S-OIVs was surprisingly small. This study does not exclude the possibility of emergence of S-OIVs with other virulence-associated mutations in the future. We conclude that surveillance studies aimed at detecting S-OIVs with increased virulence or transmission should not rely solely on virulence markers identified in the past but should include detailed characterization of virus phenotypes, guided by genetic signatures of viruses detected in severe cases of disease in humans. Copyright

Published

2010

187. Response to imported case of Marburg hemorrhagic fever, the Netherlands

Author

Timen, A. (Aura), Koopmans D.V.M., M.P.G. (Marion), Vossen, A.C.Th.M. (Ann), Doornum, G.J.J. (Gerard) van, Günther, S. (Stephan), Berkmortel, F.W.P.J. (Franchette) van den, Verduin, C.M. (Cees), Dittrich, S. (Sabine), Emmerich, P. (Petra), Osterhaus, A.D.M.E. (Albert), Dissel, J.T. (Jaap) van, Coutinho, R.A. (Roel), Timen, A. (Aura), Koopmans D.V.M., M.P.G. (Marion), Vossen, A.C.Th.M. (Ann), Doornum, G.J.J. (Gerard) van, Günther, S. (Stephan), Berkmortel, F.W.P.J. (Franchette) van den, Verduin, C.M. (Cees), Dittrich, S. (Sabine), Emmerich, P. (Petra), Osterhaus, A.D.M.E. (Albert), Dissel, J.T. (Jaap) van, and Coutinho, R.A. (Roel)

Abstract

On July 10, 2008, Marburg hemorrhagic fever was con-firmed in a Dutch patient who had vacationed recently in Uganda. Exposure most likely occurred in the Python Cave (Maramagambo Forest), which harbors bat species that elsewhere in Africa have been found positive for Marburg virus. A multidisciplinary response team was convened to perform a structured risk assessment, perform risk classi-fication of contacts, issue guidelines for follow-up, provide information, and monitor the crisis response. In total, 130 contacts were identified (66 classified as high risk and 64 as low risk) and monitored for 21 days after their last possible exposure. The case raised questions specific to international travel, postexposure prophylaxis for Marburg virus, and laboratory testing of contacts with fever. We present lessons learned and results of the follow-up serosurvey of contacts and focus on factors that prevented overreaction during an event with a high public health impact.

Published

2009

188. Pathogenesis and transmission of swine-origin 2009 A(H1N1) influenza virus in ferrets

Author

Munster, V.J. (Vincent), Wit, E. (Emmie) de, Brand, J.M.A. (Judith) van den, Herfst, S. (Sander), Schrauwen, E.J.A. (Eefje), Bestebroer, T.M. (Theo), Vijver, D.A.M.C. (David) van de, Boucher, C.A.B. (Charles), Koopmans D.V.M., M.P.G. (Marion), Rimmelzwaan, G.F. (Guus), Kuiken, T. (Thijs), Osterhaus, A.D.M.E. (Albert), Fouchier, R.A.M. (Ron), Munster, V.J. (Vincent), Wit, E. (Emmie) de, Brand, J.M.A. (Judith) van den, Herfst, S. (Sander), Schrauwen, E.J.A. (Eefje), Bestebroer, T.M. (Theo), Vijver, D.A.M.C. (David) van de, Boucher, C.A.B. (Charles), Koopmans D.V.M., M.P.G. (Marion), Rimmelzwaan, G.F. (Guus), Kuiken, T. (Thijs), Osterhaus, A.D.M.E. (Albert), and Fouchier, R.A.M. (Ron)

Abstract

The swine-origin A(H1N1) influenza virus that has emerged in humans in early 2009 has raised concerns about pandemic developments. In a ferret pathogenesis and transmission model, the 2009 A(H1N1) influenza virus was found to be more pathogenic than a seasonal A(H1N1) virus, with more extensive virus replication occurring in the respiratory tract. Replication of seasonal A(H1N1) virus was confined to the nasal cavity of ferrets, but the 2009 A(H1N1) influenza virus also replicated in the trachea, bronchi, and bronchioles. Virus shedding was more abundant from the upper respiratory tract for 2009 A(H1N1) influenza virus as compared with seasonal virus, and transmission via aerosol or respiratory droplets was equally efficient. These data suggest that the 2009 A(H1N1) influenza virus has the ability to persist in the human population, potentially with more severe clinical consequences.

Published

2009

189. Shedding of vaccine viruses with increased antigenic and genetic divergence after vaccination of newborns with monovalent type 1 oral poliovirus vaccine

Author

Sanden, S.M.G. (Sabine) van der, Pallansch, M.A. (Mark), Kassteele, J. (Jan) van de, El-Sayed, N. (Nasr), Sutter, R.W. (Roland), Koopmans D.V.M., M.P.G. (Marion), Avoort, H.G.A.M. (Harrie) van der, Sanden, S.M.G. (Sabine) van der, Pallansch, M.A. (Mark), Kassteele, J. (Jan) van de, El-Sayed, N. (Nasr), Sutter, R.W. (Roland), Koopmans D.V.M., M.P.G. (Marion), and Avoort, H.G.A.M. (Harrie) van der

Abstract

For the final stages in the eradication of poliovirus type 1 (P1), the World Health Organization advocates the selective use of monovalent type 1 oral poliovirus vaccine (mOPV1). To compare the immunogenicity of mOPV1 with that of trivalent OPV (tOPV) in infants, a study was performed in Egypt in 2005. Newborns were vaccinated with mOPV1 or tOPV immediately after birth and were challenged with mOPV1 after 1 month. Vaccination with mOPV1 at birth resulted in significantly higher seroconversion against P1 viruses and lower excretion of P1 viruses than vaccination with tOPV. Intratypic differentiation of the viruses shed by the newborns revealed the presence of remarkably high numbers of antigenically divergent (AD) P1 isolates, especially in the mOPV1 study group. The majority of these AD P1 isolates (71%) were mOPV1 challenge derived and were shed by newborns who did not seroconvert to P1 after the birth dose. Genetic characterization of the viruses revealed that amino acid 60 of the VP3 region was mutated in all AD P1 isolates. Isolates with substitution of residue 99 of the VP1 region had significantly higher numbers of nonsynonymous mutations in the VP1 region than isolates without this substitution and were preferentially shed in the mOPV1 study group. The widespread use of mOPV1 has proven to be a powerful tool for fighting poliovirus circulation in the remaining areas of endemicity. This study provides another justification for the need to achieve high vaccination coverage in order to prevent the circulation of AD strains. Copyright

Published

2009

190. High prevalence of prolonged norovirus shedding and illness among hospitalized patients: A model for in vivo molecular evolution

Author

Siebenga, J.J. (Joukje), Beersma, M.F.C. (Thijs), Vennema, H. (Harry), Biezen, P. (Paula) van, Hartwig, N.G. (Nico), Koopmans D.V.M., M.P.G. (Marion), Siebenga, J.J. (Joukje), Beersma, M.F.C. (Thijs), Vennema, H. (Harry), Biezen, P. (Paula) van, Hartwig, N.G. (Nico), and Koopmans D.V.M., M.P.G. (Marion)

Abstract

During a 2-year survey in an academic hospital, 8 (8.4%) of all norovirus (NoV)-positive patients showed prolonged norovirus illness and shedding (duration, 21-182 days). All patients had underlying illnesses, resulting in some level of immunodeficiency in 5. Four patients were admitted to the hospital with gastroenteritis, 2 acquired norovirus while hospitalized, and 2 were outpatients. Genotypes GII.4 and GIIb-GII.3 were found. Rei

Published

2008

191. Prevalence of human parechovirus in The Netherlands in 2000 to 2007

Author

Sanden, S.M.G. (Sabine) van der, Bruin, E. (Erwin) de, Vennema, H. (Harry), Swanink, C. (Caroline), Koopmans D.V.M., M.P.G. (Marion), Avoort, H.G.A.M. (Harrie) van der, Sanden, S.M.G. (Sabine) van der, Bruin, E. (Erwin) de, Vennema, H. (Harry), Swanink, C. (Caroline), Koopmans D.V.M., M.P.G. (Marion), and Avoort, H.G.A.M. (Harrie) van der

Abstract

Infection with human parechovirus 3 (HPeV3) was described for the first time in Japan in 2004 and reportedly is more often associated with severe disease than infection with HPeV1 or HPeV2. In 2004, infections with HPeV3 were observed for the first time in The Netherlands. Genetic analysis showed several different lineages, suggesting endemic circulation. We analyzed 163 cell culture isolates from the same number of patients tested in routine virological laboratories as part of the national enterovirus surveillance program. Isolates were collected between 2000 and 2007 and could not be characterized by routine methods. In total, 155 isolates (95%) were found positive for HPeV by a reverse transcription-PCR assay targeting the 5′ untranslated region, explaining the majority of the diagnostic deficit in enterovirus surveillance for these years. Typing of the isolates by use of partial genome sequencing of the VP1/2A region revealed the presence of 55 HPeV1, 2 HPeV2, 89 HPeV3, 1 HPeV4, and 8 HPeV5 isolates. We compared isolation dates, age groups affected, and clinical pictures, which were reported as part of the routine surveillance. Clear differences in epidemiology were observed, with HPeV3 occurring at intervals of 2 years and in the spring-summer season, whereas HPeV1 was observed in small numbers throughout each year, with a low in the summer months. HPeV3 infection affected younger children than HPeV1 infection and was significantly more often associated with fever, meningitis, and viremia. Copyright

Published

2008

192. Bolletjes slikken

Author

Koopmans D.V.M., M.P.G. (Marion) and Koopmans D.V.M., M.P.G. (Marion)

Abstract

Rede, in verkorte vorm uitgesproken ter gelegenheid van het aanvaarden van het ambt van bijzonder hoogleraar in de virologie aan het Erasmus faculteit van de Erasmus Universiteit Rotterdam op 8 maart 2007

Published

2007

193. Epochal evolution of GGII.4 norovirus capsid proteins from 1995 to 2006

Author

Siebenga, J.J. (Joukje), Vennema, H. (Harry), Renckens, B. (Bernadet), Bruin, E. (Erwin) de, Veer, B. (Bas) van der, Siezen, R.J. (Roland), Koopmans D.V.M., M.P.G. (Marion), Siebenga, J.J. (Joukje), Vennema, H. (Harry), Renckens, B. (Bernadet), Bruin, E. (Erwin) de, Veer, B. (Bas) van der, Siezen, R.J. (Roland), and Koopmans D.V.M., M.P.G. (Marion)

Abstract

Noroviruses are the causative agents of the majority of viral gastroenteritis outbreaks in humans. During the past 15 years, noroviruses of genotype GGII.4 have caused four epidemic seasons of viral gastroenteritis, during which four novel variants (termed epidemic variants) emerged and displaced the resident viruses. In order to understand the mechanisms and biological advantages of these epidemic variants, we studied the genetic changes in the capsid proteins of GGII.4 strains over this period. A representative sample was drawn from 574 GGII.4 outbreak strains collected over 15 years of systematic surveillance in The Netherlands, and capsid genes were sequenced for a total of 26 strains. The three-dimensional structure was predicted by homology modeling, using the Norwalk virus (Hu/NoV/GGI.1/Norwalk/1968/US) capsid as a reference. The highly significant preferential accumulation and fixation of mutations (nucleotide and amino acid) in the protruding part of the capsid protein provided strong evidence for the occurrence of genetic drift and selection. Although subsequent new epidemic variants differed by up to 25 amino acid mutations, consistent changes were observed in only five positions. Phylogenetic analyses showed that each variant descended from its chronologic predecessor, with the exception of the 2006b variant, which is more closely related to the 2002 variant than to the 2004 variant. The consistent association between the observed genetic findings and changes in epidemiology leads to the conclusion that population immunity plays a role in the epochal evolution of GGII.4 norovirus strains. Copyright

Published

2007

194. General practitioner practices in requesting laboratory tests for patients with gastroenteritis in the Netherlands, 2001–2002

Author

Brandhof, W.E. van den, Bartelds, A.I.M. (Aad), Koopmans D.V.M., M.P.G. (Marion), Duynhoven, I.T.H.P. van, Brandhof, W.E. van den, Bartelds, A.I.M. (Aad), Koopmans D.V.M., M.P.G. (Marion), and Duynhoven, I.T.H.P. van

Abstract

Background: The objective of this study was to estimate the (selective) proportion of patients consulting their GP for an episode of gastroenteritis for whom laboratory tests were requested. In addition adherence of GPs to the guidelines for diagnostic test regime was ascertained. Methods: Data were collected from a GP network in the Netherlands. Information was also collected on the reason for requesting the test, test specifications, and test results. Results: For 12% of the GP patients with gastroenteritis, a stool sample was requested and tested for enteric pathogens. In most patients, the duration, followed by severity of complaints or a visit to a specific, high-risk country were reported as reasons to request laboratory diagnostics. Tests were requested most often in summer months and in February. Campylobacter (requested for 87% of the tests), Salmonella (84%), Shigella (78%) and Yersinia (56%) were most frequently included in the stool tests. Campylobacter was detected most often in patients. Conclusion: Test requests did not always comply with existing knowledge of the etiology of gastroenteritis in GP patients and were not always consistent with the Dutch GP guidelines. Therefore, the data of this study can be used to develop educational approaches for GP's as well as for revision of the guidelines.

Published

2006

195. Inactivation of caliciviruses

Author

Duizer, E. (Erwin), Bijkerk, P. (Paul), Rockx, B. (Barry), De Groot, A. (Astrid), Twisk, F. (Fleur), Koopmans D.V.M., M.P.G. (Marion), Duizer, E. (Erwin), Bijkerk, P. (Paul), Rockx, B. (Barry), De Groot, A. (Astrid), Twisk, F. (Fleur), and Koopmans D.V.M., M.P.G. (Marion)

Abstract

The viruses most commonly associated with food- and waterborne outbreaks of gastroenteritis are the noroviruses. The lack of a culture method for noroviruses warrants the use of cultivable model viruses to gain more insight on their transmission routes and inactivation methods. We studied the inactivation of the reported enteric canine calicivirus no. 48 (CaCV) and the respiratory feline calicivirus F9 (FeCV) and correlated inactivation to reduction in PCR units of FeCV, CaCV, and a norovirus. Inactivation of suspended viruses was temperature and time dependent in the range from 0 to 100°C. UV-B radiation from 0 to 150 mJ/cm2 caused dose-dependent inactivation, with a 3 D (D = 1 log10) reduction in infectivity at 34 mJ/cm2 for both viruses. Inactivation by 70% ethanol was inefficient, with only 3 D reduction after 30 min. Sodium hypochlorite solutions were only effective at >300 ppm. FeCV showed a higher stability at pH <3 and pH >7 than CaCV. For all treatments, detection of viral RNA underestimated the reduction in viral infectivity. Norovirus was never more sensitive than the animal caliciviruses and profoundly more resistant to low and high pH. Overall, both animal viruses showed similar inactivation profiles when exposed to heat or UV-B radiation or when incubated in ethanol or hypochlorite. The low stability of CaCV at low pH suggests that this is not a typical enteric (calici-) virus. The incomplete inactivation by ethanol and the high hypochlorite concentration needed for sufficient virus inactivation point to a concern for decontamination of fomites and surfaces contaminated with noroviruses and virus-safe water.

Published

2004

196. Avian influenza A virus (H7N7) associated with human conjunctivitis and a fatal case of acute respiratory distress syndrome.

Author

Fouchier, R.A.M. (Ron), Schneeberger, P.M. (Peter), Rozendaal, F.W. (Frans), Broekman, J.M. (Jan), Kemink, S.A. (Stiena), Munster, V.J. (Vincent), Rimmelzwaan, G.F. (Guus), Schutten, M. (Martin), Doornum, G.J.J. (Gerard) van, Koch, G. (Guus), Bosman, A. (Arnold), Koopmans D.V.M., M.P.G. (Marion), Osterhaus, A.D.M.E. (Albert), Kuiken, T. (Thijs), Fouchier, R.A.M. (Ron), Schneeberger, P.M. (Peter), Rozendaal, F.W. (Frans), Broekman, J.M. (Jan), Kemink, S.A. (Stiena), Munster, V.J. (Vincent), Rimmelzwaan, G.F. (Guus), Schutten, M. (Martin), Doornum, G.J.J. (Gerard) van, Koch, G. (Guus), Bosman, A. (Arnold), Koopmans D.V.M., M.P.G. (Marion), Osterhaus, A.D.M.E. (Albert), and Kuiken, T. (Thijs)

Abstract

Highly pathogenic avian influenza A viruses of subtypes H5 and H7 are the causative agents of fowl plague in poultry. Influenza A viruses of subtype H

Published

2004

197. Changes in small intestinal homeostasis, morphology, and gene expression during rotavirus infection of infant mice

Author

Boshuizen, J.A. (Jos), Reimerink, J.H., Korteland-van Male, A.M. (Anita), Ham, V.J. van, Büller, H.A. (Hans), Dekker, J. (Jan), Einerhand, A.W.C. (Sandra), Koopmans D.V.M., M.P.G. (Marion), Boshuizen, J.A. (Jos), Reimerink, J.H., Korteland-van Male, A.M. (Anita), Ham, V.J. van, Büller, H.A. (Hans), Dekker, J. (Jan), Einerhand, A.W.C. (Sandra), and Koopmans D.V.M., M.P.G. (Marion)

Abstract

Rotavirus is the most important cause of infantile gastroenteritis. Since in vivo mucosal responses to a rotavirus infection thus far have not been extensively studied, we related viral replication in the murine small intestine to alterations in mucosal structure, epithelial cell homeostasis, cellular kinetics, and differentiation. Seven-day-old suckling BALB/c mice were inoculated with 2 x 10(4) focus-forming units of murine rotavirus and were compared to mock-infected controls. Diarrheal illness and viral shedding were recorded, and small intestinal tissue was evaluated for rotavirus (NSP4 and structural proteins)- and enterocyte-specific (lactase, SGLT1, and L-FABP) mRNA and protein expression. Morphology, apoptosis, proliferation, and migration were evaluated (immuno)histochemically. Diarrhea was observed from days 1 to 5 postinfection, and viral shedding was observed from days 1 to 10. Two peaks of rotavirus replication were observed at 1 and 4 days postinfection. Histological changes were characterized by the accumulation of vacuolated enterocytes. Strikingly, the number of vacuolated cells exceeded the number of cells in which viral replication was detectable. Apoptosis and proliferation were increased from days 1 to 7, resulting in villous atrophy. Epithelial cell turnover was significantly higher (<4 days) than that observed in controls (7 days). Since epithelial renewal occurred within 4 days, the second peak of viral replication was most likely caused by infection of newly synthesized cells. Expression of enterocyte-specific genes was downregulated in infected cells at mRNA and protein levels starting as early as 6 h after infection. In conclusion, we show for the first time that rotavirus infection induces apoptosis in vivo, an increase in epithelial cell turnover, and a shutoff of gene expression in enterocytes showing viral replication. The shutoff of enterocyte-specific gene expression, together with the loss of mature enterocytes through apoptosis an

Published

2003

198. Natural history of human Calicivirus infection: A prospective cohort study

Author

Rockx, B. (Barry), De Wit, M. (Matty), Vennema, H. (Harry), Vinjé, J. (Jan), Bruin, E.I. (Esther) de, Duynhoven, Y.T.H.P. van, Koopmans D.V.M., M.P.G. (Marion), Rockx, B. (Barry), De Wit, M. (Matty), Vennema, H. (Harry), Vinjé, J. (Jan), Bruin, E.I. (Esther) de, Duynhoven, Y.T.H.P. van, and Koopmans D.V.M., M.P.G. (Marion)

Abstract

We investigated the natural history of human Calicivirus infection in the community. Clinical information was obtained from 99 subjects infected with Norwalk-like viruses (NLV) and 40 subjects infected with Sapporo-like viruses (SLV) in a prospective, community-based cohort study. NLV infection was common in all age groups, whereas SLV infection was mainly restricted to children aged <5 years. Symptoms lasted for a median of 5 and 6 days for NLV and SLV infections, respectively. Disease was characterized by diarrhea during the first 5 days (87% of patients with NLV infection and 95% of patients with SLV infection) and vomiting on the first day (74% for NLV and 60% for SLV). Vomiting was less common in children aged <1 year (59% for NLV and 44% for SLV) than it was among children aged ≤1 year (>75% for NLV and >67% for SLV). Overall, NLV was detected in 26% of patients up to 3 weeks after the onset of illness. This proportion was highest (38%) for children aged <1 year. SLV shedding subsided after 14 days. These data show that the durations of disease and viral shedding of caliciviruses are longer than has been described elsewhere. Therefore, the impact of these infections may have been underestimated.

Published

2002

199. The Incidence and Genetic Variability of Small Round-Structured Viruses in Outbrreaks of Gastroenteritis in The Netherlands

Author

Vinjé, J., Altena, S.A., Koopmans D.V.M., M.P.G. (Marion), Vinjé, J., Altena, S.A., and Koopmans D.V.M., M.P.G. (Marion)

Published

1997

200. The Role of Small Round-Structured Viruses (SRSV) in Outbreaks of Gastroenteritis in The Netherlands

Author

Vinjé, J., Koopmans D.V.M., M.P.G. (Marion), Vinjé, J., and Koopmans D.V.M., M.P.G. (Marion)

Published

1996