Your search keyword '"Waight, Pauline"' showing total 14 results

1. Monitoring the emergence of community transmission of influenza A/H1N1 2009 in England: a cross sectional opportunistic survey of self sampled telephone callers to NHS Direct

Author

Elliot, Alex J, Powers, Cassandra, Thornton, Alicia, Obi, Chinelo, Hill, Caterina, Simms, Ian, Waight, Pauline, Maguire, Helen, Foord, David, Povey, Enid, Wreghitt, Tim, Goddard, Nichola, Ellis, Joanna, Bermingham, Alison, Sebastianpillai, Praveen, Lackenby, Angie, Zambon, Maria, Brown, David, Smith, Gillian E, Gill, O Noel, Elliot, Alex J, Powers, Cassandra, Thornton, Alicia, Obi, Chinelo, Hill, Caterina, Simms, Ian, Waight, Pauline, Maguire, Helen, Foord, David, Povey, Enid, Wreghitt, Tim, Goddard, Nichola, Ellis, Joanna, Bermingham, Alison, Sebastianpillai, Praveen, Lackenby, Angie, Zambon, Maria, Brown, David, Smith, Gillian E, and Gill, O Noel

Subjects

H1N1 influenza Epidemiology 21st century. Great Britain, H1N1 influenza Research 21st century. Great Britain, Grippe A (H1N1) Épidémiologie 21e siècle. Grande-Bretagne, Grippe A (H1N1) Recherche 21e siècle. Grande-Bretagne

Abstract

Objective To evaluate ascertainment of the onset of community transmission of influenza A/H1N1 2009 (swine flu) in England during the earliest phase of the epidemic through comparing data from two surveillance systems.

Published

2009

2. CD4(+) T cell responses to cytomegalovirus in early life: a prospective birth cohort study.

Author

Miles, David J C, Sande, Marianne van der, Kaye, Steve, Crozier, Sarah, Ojuola, Olubukola, Palmero, Melba, Sanneh, Mariama, Touray, Ebrima S, Waight, Pauline, Rowland-Jones, Sarah, Whittle, Hilton, Marchant, Arnaud, Miles, David J C, Sande, Marianne van der, Kaye, Steve, Crozier, Sarah, Ojuola, Olubukola, Palmero, Melba, Sanneh, Mariama, Touray, Ebrima S, Waight, Pauline, Rowland-Jones, Sarah, Whittle, Hilton, and Marchant, Arnaud

Abstract

We compared cytomegalovirus (CMV)-specific interferon-gamma (IFN-gamma), interleukin 2 (IL-2), and CD154 CD4(+) T cell responses of infants to those from chronically infected adults and from children aged 4-5 years. Magnitudes of the responses were similar, although coexpression of IFN-gamma plus CD154 occurred more than coexpression of IFN-gamma plus IL-2 or IL-2 plus CD154. Responses remained constant during infancy, although the proportion of IFN-gamma-producing cells increased from infancy to adulthood. Most responding cells in infants were undifferentiated (i.e. CD27(+)CD28(+)), although IFN-gamma-producing cells were disproportionately CD27(-). By 12 months after diagnosis, viremia was rarely detectable, indicating that CMV was controlled despite the slow development of CMV-specific CD4(+) T cell responses., Journal Article, Research Support, Non-U.S. Gov't, SCOPUS: ar.j, info:eu-repo/semantics/published

Published

2008

3. Maintenance of large subpopulations of differentiated CD8 T-cells two years after cytomegalovirus infection in Gambian infants.

Author

Miles, David J C, van der Sande, Marianne, Jeffries, David, Kaye, Steve, Ojuola, Olubukola, Sanneh, Mariama, Cox, M. L., Palmero, Melba, Touray, Ebrima S, Waight, Pauline, Rowland-Jones, Sarah, Whittle, Hilton, Marchant, Arnaud, Miles, David J C, van der Sande, Marianne, Jeffries, David, Kaye, Steve, Ojuola, Olubukola, Sanneh, Mariama, Cox, M. L., Palmero, Melba, Touray, Ebrima S, Waight, Pauline, Rowland-Jones, Sarah, Whittle, Hilton, and Marchant, Arnaud

Abstract

BACKGROUND: In a previously published study, we found that large differentiated subpopulations of CD8 T-cells emerged rapidly after CMV infection in young infants and persisted throughout the following year. Here we describe a follow-up study conducted on the same infants to establish whether the differentiated subpopulations continued through the second year post-infection. METHODOLOGY / PRINCIPAL FINDINGS: CMV-specific cells identified using tetramers remained more activated and differentiated than the overall CD8 population. The large subpopulation of differentiated cytotoxic (CD28(-)CD62L(-)Bcl-2(low)CD95(+)perforin(+)) cells that emerged rapidly after infection remained stable after two years. No similar subpopulation was found in CMV-uninfected infants indicating that two years after infection, CMV remained a major factor in driving CD8 T-cell differentiation. Although markers of activation (CD45R0 and HLA-D) declined throughout the first year, HLA-D expression continued to decline during the second year and CD45R0 expression increased slightly. The age-related increase in IFNgamma response observed during the first year continued but was non-significant during the second year, indicating that the rate of functional improvement had slowed substantially. CONCLUSIONS / SIGNIFICANCE: The large differentiated subpopulations of CD8 T-cells that had emerged immediately after CMV infection persisted through the second year post-infection, while levels of activation and functional capacity remained fairly constant., Journal Article, Research Support, Non-U.S. Gov't, SCOPUS: ar.j, info:eu-repo/semantics/published

Published

2008

4. Maintenance of large subpopulations of differentiated CD8 T-cells two years after cytomegalovirus infection in Gambian infants.

Author

Miles, David J C, van der Sande, Marianne, Jeffries, David, Kaye, Steve, Ojuola, Olubukola, Sanneh, Mariama, Cox, M. L., Palmero, Melba, Touray, Ebrima S, Waight, Pauline, Rowland-Jones, Sarah, Whittle, Hilton, Marchant, Arnaud, Miles, David J C, van der Sande, Marianne, Jeffries, David, Kaye, Steve, Ojuola, Olubukola, Sanneh, Mariama, Cox, M. L., Palmero, Melba, Touray, Ebrima S, Waight, Pauline, Rowland-Jones, Sarah, Whittle, Hilton, and Marchant, Arnaud

Abstract

BACKGROUND: In a previously published study, we found that large differentiated subpopulations of CD8 T-cells emerged rapidly after CMV infection in young infants and persisted throughout the following year. Here we describe a follow-up study conducted on the same infants to establish whether the differentiated subpopulations continued through the second year post-infection. METHODOLOGY / PRINCIPAL FINDINGS: CMV-specific cells identified using tetramers remained more activated and differentiated than the overall CD8 population. The large subpopulation of differentiated cytotoxic (CD28(-)CD62L(-)Bcl-2(low)CD95(+)perforin(+)) cells that emerged rapidly after infection remained stable after two years. No similar subpopulation was found in CMV-uninfected infants indicating that two years after infection, CMV remained a major factor in driving CD8 T-cell differentiation. Although markers of activation (CD45R0 and HLA-D) declined throughout the first year, HLA-D expression continued to decline during the second year and CD45R0 expression increased slightly. The age-related increase in IFNgamma response observed during the first year continued but was non-significant during the second year, indicating that the rate of functional improvement had slowed substantially. CONCLUSIONS / SIGNIFICANCE: The large differentiated subpopulations of CD8 T-cells that had emerged immediately after CMV infection persisted through the second year post-infection, while levels of activation and functional capacity remained fairly constant., Journal Article, Research Support, Non-U.S. Gov't, SCOPUS: ar.j, info:eu-repo/semantics/published

Published

2008

5. CD4(+) T cell responses to cytomegalovirus in early life: a prospective birth cohort study.

Author

Miles, David J C, Sande, Marianne van der, Kaye, Steve, Crozier, Sarah, Ojuola, Olubukola, Palmero, Melba, Sanneh, Mariama, Touray, Ebrima S, Waight, Pauline, Rowland-Jones, Sarah, Whittle, Hilton, Marchant, Arnaud, Miles, David J C, Sande, Marianne van der, Kaye, Steve, Crozier, Sarah, Ojuola, Olubukola, Palmero, Melba, Sanneh, Mariama, Touray, Ebrima S, Waight, Pauline, Rowland-Jones, Sarah, Whittle, Hilton, and Marchant, Arnaud

Abstract

We compared cytomegalovirus (CMV)-specific interferon-gamma (IFN-gamma), interleukin 2 (IL-2), and CD154 CD4(+) T cell responses of infants to those from chronically infected adults and from children aged 4-5 years. Magnitudes of the responses were similar, although coexpression of IFN-gamma plus CD154 occurred more than coexpression of IFN-gamma plus IL-2 or IL-2 plus CD154. Responses remained constant during infancy, although the proportion of IFN-gamma-producing cells increased from infancy to adulthood. Most responding cells in infants were undifferentiated (i.e. CD27(+)CD28(+)), although IFN-gamma-producing cells were disproportionately CD27(-). By 12 months after diagnosis, viremia was rarely detectable, indicating that CMV was controlled despite the slow development of CMV-specific CD4(+) T cell responses., Journal Article, Research Support, Non-U.S. Gov't, SCOPUS: ar.j, info:eu-repo/semantics/published

Published

2008

6. Cytomegalovirus infection in Gambian infants leads to profound CD8 T-cell differentiation.

Author

Miles, David J C, van der Sande, Marianne, Jeffries, David, Kaye, Steve, Ismaili, Jamila, Ojuola, Olubukola, Sanneh, Mariama, Touray, Ebrima S, Waight, Pauline, Rowland-Jones, Sarah, Whittle, Hilton, Marchant, Arnaud, Miles, David J C, van der Sande, Marianne, Jeffries, David, Kaye, Steve, Ismaili, Jamila, Ojuola, Olubukola, Sanneh, Mariama, Touray, Ebrima S, Waight, Pauline, Rowland-Jones, Sarah, Whittle, Hilton, and Marchant, Arnaud

Abstract

Cytomegalovirus (CMV) infection is endemic in Gambian infants, with 62% infected by 3 months and 85% by 12 months of age. We studied the CD8 T-cell responses of infants to CMV following primary infection. CMV-specific CD8 T cells, identified with tetramers, showed a fully differentiated phenotype (CD28(-) CD62L(-) CD95(+) perforin(+) granzyme A(+) Bcl-2(low)). Strikingly, the overall CD8 T-cell population developed a similar phenotype following CMV infection, which persisted for at least 12 months. In contrast, primary infection was accompanied by up-regulation of markers of activation (CD45R0 and HLA-D) on both CMV-specific cells and the overall CD8 T-cell population and division (Ki-67) of specific cells, but neither pattern persisted. At 12 months of age, the CD8 T-cell population of CMV-infected infants was more differentiated than that of uninfected infants. Although the subpopulation of CMV-specific cells remained constant, the CMV peptide-specific gamma interferon response was lower in younger infants and increased with age. As the CD8 T-cell phenotype induced by CMV is indicative of immune dysfunction in the elderly, the existence of a similar phenotype in large numbers of Gambian infants raises the question of whether CMV induces a similarly deleterious effect., Journal Article, Research Support, Non-U.S. Gov't, SCOPUS: ar.j, info:eu-repo/semantics/published

Published

2007

7. Risk factors for and clinical outcome of congenital cytomegalovirus infection in a peri-urban West-African birth cohort.

Author

van der Sande, Marianne A B, Kaye, Steve, Miles, David J C, Waight, Pauline, Jeffries, David, Ojuola, Olubukola, Palmero, Melba, Pinder, Margaret, Ismaili, Jamila, Flanagan, Katie L., Aveika, Akum A, Zaman, Akram, Rowland-Jones, Sarah, McConkey, Samuel J, Whittle, Hilton C, Marchant, Arnaud, van der Sande, Marianne A B, Kaye, Steve, Miles, David J C, Waight, Pauline, Jeffries, David, Ojuola, Olubukola, Palmero, Melba, Pinder, Margaret, Ismaili, Jamila, Flanagan, Katie L., Aveika, Akum A, Zaman, Akram, Rowland-Jones, Sarah, McConkey, Samuel J, Whittle, Hilton C, and Marchant, Arnaud

Abstract

BACKGROUND: Congenital cytomegalovirus (CMV) infection is the most prevalent congenital infection worldwide. Epidemiology and clinical outcomes are known to vary with socio-economic background, but few data are available from developing countries, where the overall burden of infectious diseases is frequently high. METHODOLOGY/PRINCIPAL FINDINGS: As part of an ongoing birth cohort study in The Gambia among term infants, urine samples were collected at birth and tested by PCR for the presence of CMV DNA. Risk factors for transmission and clinical outcome were assessed, including placental malaria infection. Babies were followed up at home monthly for morbidity and anthropometry, and at one year of age a clinical evaluation was performed. The prevalence of congenital CMV infection was 5.4% (40/741). A higher prevalence of hepatomegaly was the only significant clinical difference at birth. Congenitally infected children were more often first born babies (adjusted odds ratio (OR) 5.3, 95% confidence interval (CI) 2.0-13.7), more frequently born in crowded compounds (adjusted OR 2.9, 95%CI 1.0-8.3) and active placental malaria was more prevalent (adjusted OR 2.9, 95%CI 1.0-8.4). These associations were corrected for maternal age, bed net use and season of birth. During the first year of follow up, mothers of congenitally infected children reported more health complaints for their child. CONCLUSIONS/SIGNIFICANCE: In this study, the prevalence of congenital CMV among healthy neonates was much higher than previously reported in industrialised countries, and was associated with active placental malaria infection. There were no obvious clinical implications during the first year of life. The effect of early life CMV on the developing infant in the Gambia could be mitigated by environmental factors, such as the high burden of other infections., Journal Article, Research Support, Non-U.S. Gov't, info:eu-repo/semantics/published

Published

2007

8. Risk factors for and clinical outcome of congenital cytomegalovirus infection in a peri-urban West-African birth cohort.

Author

van der Sande, Marianne A B, Kaye, Steve, Miles, David J C, Waight, Pauline, Jeffries, David, Ojuola, Olubukola, Palmero, Melba, Pinder, Margaret, Ismaili, Jamila, Flanagan, Katie L., Aveika, Akum A, Zaman, Akram, Rowland-Jones, Sarah, McConkey, Samuel J, Whittle, Hilton C, Marchant, Arnaud, van der Sande, Marianne A B, Kaye, Steve, Miles, David J C, Waight, Pauline, Jeffries, David, Ojuola, Olubukola, Palmero, Melba, Pinder, Margaret, Ismaili, Jamila, Flanagan, Katie L., Aveika, Akum A, Zaman, Akram, Rowland-Jones, Sarah, McConkey, Samuel J, Whittle, Hilton C, and Marchant, Arnaud

Abstract

BACKGROUND: Congenital cytomegalovirus (CMV) infection is the most prevalent congenital infection worldwide. Epidemiology and clinical outcomes are known to vary with socio-economic background, but few data are available from developing countries, where the overall burden of infectious diseases is frequently high. METHODOLOGY/PRINCIPAL FINDINGS: As part of an ongoing birth cohort study in The Gambia among term infants, urine samples were collected at birth and tested by PCR for the presence of CMV DNA. Risk factors for transmission and clinical outcome were assessed, including placental malaria infection. Babies were followed up at home monthly for morbidity and anthropometry, and at one year of age a clinical evaluation was performed. The prevalence of congenital CMV infection was 5.4% (40/741). A higher prevalence of hepatomegaly was the only significant clinical difference at birth. Congenitally infected children were more often first born babies (adjusted odds ratio (OR) 5.3, 95% confidence interval (CI) 2.0-13.7), more frequently born in crowded compounds (adjusted OR 2.9, 95%CI 1.0-8.3) and active placental malaria was more prevalent (adjusted OR 2.9, 95%CI 1.0-8.4). These associations were corrected for maternal age, bed net use and season of birth. During the first year of follow up, mothers of congenitally infected children reported more health complaints for their child. CONCLUSIONS/SIGNIFICANCE: In this study, the prevalence of congenital CMV among healthy neonates was much higher than previously reported in industrialised countries, and was associated with active placental malaria infection. There were no obvious clinical implications during the first year of life. The effect of early life CMV on the developing infant in the Gambia could be mitigated by environmental factors, such as the high burden of other infections., Journal Article, Research Support, Non-U.S. Gov't, info:eu-repo/semantics/published

Published

2007

9. Cytomegalovirus infection in Gambian infants leads to profound CD8 T-cell differentiation.

Author

Miles, David J C, van der Sande, Marianne, Jeffries, David, Kaye, Steve, Ismaili, Jamila, Ojuola, Olubukola, Sanneh, Mariama, Touray, Ebrima S, Waight, Pauline, Rowland-Jones, Sarah, Whittle, Hilton, Marchant, Arnaud, Miles, David J C, van der Sande, Marianne, Jeffries, David, Kaye, Steve, Ismaili, Jamila, Ojuola, Olubukola, Sanneh, Mariama, Touray, Ebrima S, Waight, Pauline, Rowland-Jones, Sarah, Whittle, Hilton, and Marchant, Arnaud

Abstract

Cytomegalovirus (CMV) infection is endemic in Gambian infants, with 62% infected by 3 months and 85% by 12 months of age. We studied the CD8 T-cell responses of infants to CMV following primary infection. CMV-specific CD8 T cells, identified with tetramers, showed a fully differentiated phenotype (CD28(-) CD62L(-) CD95(+) perforin(+) granzyme A(+) Bcl-2(low)). Strikingly, the overall CD8 T-cell population developed a similar phenotype following CMV infection, which persisted for at least 12 months. In contrast, primary infection was accompanied by up-regulation of markers of activation (CD45R0 and HLA-D) on both CMV-specific cells and the overall CD8 T-cell population and division (Ki-67) of specific cells, but neither pattern persisted. At 12 months of age, the CD8 T-cell population of CMV-infected infants was more differentiated than that of uninfected infants. Although the subpopulation of CMV-specific cells remained constant, the CMV peptide-specific gamma interferon response was lower in younger infants and increased with age. As the CD8 T-cell phenotype induced by CMV is indicative of immune dysfunction in the elderly, the existence of a similar phenotype in large numbers of Gambian infants raises the question of whether CMV induces a similarly deleterious effect., Journal Article, Research Support, Non-U.S. Gov't, SCOPUS: ar.j, info:eu-repo/semantics/published

Published

2007

10. Impact of outpatient neuraminidase inhibitor treatment in patients infected with influenza A(H1N1)pdm09 at high risk of hospitalization: an Individual Participant Data (IPD) meta-analysis

Author

Venkatesan, Sudhir, Myles, Puja R., Leonardi-Bee, Jo, Muthuri, Stella G., Al Masri, Malak, Andrews, Nick, Bantar, Carlos, Dubnov-Raz, Gal, Gérardin, Patrick, Koay, Evelyn S.C., Loh, Tze Ping, Memish, Ziad A., Miller, Elizabeth, Oliva, Maria E., Rath, Barbara A., Schweiger, Brunhilde, Tang, Julian W., Tran, Dat, Vidmar, Tjasa, Waight, Pauline A., Nguyen-Van-Tam, Jonathan S., Venkatesan, Sudhir, Myles, Puja R., Leonardi-Bee, Jo, Muthuri, Stella G., Al Masri, Malak, Andrews, Nick, Bantar, Carlos, Dubnov-Raz, Gal, Gérardin, Patrick, Koay, Evelyn S.C., Loh, Tze Ping, Memish, Ziad A., Miller, Elizabeth, Oliva, Maria E., Rath, Barbara A., Schweiger, Brunhilde, Tang, Julian W., Tran, Dat, Vidmar, Tjasa, Waight, Pauline A., and Nguyen-Van-Tam, Jonathan S.

Abstract

Background: While evidence exists to support the effectiveness of neuraminidase inhibitors (NAIs) in reducing mortality when given to hospitalized patients with A(H1N1)pdm09 virus infection, the impact of outpatient treatment on hospitalization has not been clearly established. We investigated the impact of outpatient NAI treatment on subsequent hospitalization in patients with A(H1N1)pdm09 virus infection. Methods: We assembled general community and outpatient data from 9 clinical centers in different countries collected between January 2009 and December 2010. We standardized data from each study center to create a pooled dataset and then used mixed-effects logistic regression modeling to determine the effect of NAI treatment on hospitalization. We adjusted for NAI treatment propensity and preadmission antibiotic use, including “study center” as a random intercept to account for differences in baseline hospitalization rate between centers. Results: We included 3376 patients with influenza A(H1N1)pdm09, of whom 3085 (91.4%) had laboratory-confirmed infection. Eight hundred seventy-three patients (25.8%) received outpatient or community-based NAI treatment, 928 of 2395 (38.8%) with available data had dyspnea or respiratory distress, and hospitalizations occurred in 1705 (50.5%). After adjustment for preadmission antibiotics and NAI treatment propensity, preadmission NAI treatment was associated with decreased odds of hospital admission compared to no NAI treatment (adjusted odds ratio, 0.24; 95% confidence interval, 0.20–0.30). Conclusions: In a population with confirmed or suspected A(H1N1)pdm09 and at high risk of hospitalization, outpatient or community-based NAI treatment significantly reduced the likelihood of requiring hospital admission. These data suggest that community patients with severe influenza should receive NAI treatment.

11. Impact of outpatient neuraminidase inhibitor treatment in patients infected with influenza A(H1N1)pdm09 at high risk of hospitalization: an Individual Participant Data (IPD) meta-analysis

Author

Venkatesan, Sudhir, Myles, Puja R., Leonardi-Bee, Jo, Muthuri, Stella G., Al Masri, Malak, Andrews, Nick, Bantar, Carlos, Dubnov-Raz, Gal, Gérardin, Patrick, Koay, Evelyn S.C., Loh, Tze Ping, Memish, Ziad A., Miller, Elizabeth, Oliva, Maria E., Rath, Barbara A., Schweiger, Brunhilde, Tang, Julian W., Tran, Dat, Vidmar, Tjasa, Waight, Pauline A., Nguyen-Van-Tam, Jonathan S., Venkatesan, Sudhir, Myles, Puja R., Leonardi-Bee, Jo, Muthuri, Stella G., Al Masri, Malak, Andrews, Nick, Bantar, Carlos, Dubnov-Raz, Gal, Gérardin, Patrick, Koay, Evelyn S.C., Loh, Tze Ping, Memish, Ziad A., Miller, Elizabeth, Oliva, Maria E., Rath, Barbara A., Schweiger, Brunhilde, Tang, Julian W., Tran, Dat, Vidmar, Tjasa, Waight, Pauline A., and Nguyen-Van-Tam, Jonathan S.

Abstract

Background: While evidence exists to support the effectiveness of neuraminidase inhibitors (NAIs) in reducing mortality when given to hospitalized patients with A(H1N1)pdm09 virus infection, the impact of outpatient treatment on hospitalization has not been clearly established. We investigated the impact of outpatient NAI treatment on subsequent hospitalization in patients with A(H1N1)pdm09 virus infection. Methods: We assembled general community and outpatient data from 9 clinical centers in different countries collected between January 2009 and December 2010. We standardized data from each study center to create a pooled dataset and then used mixed-effects logistic regression modeling to determine the effect of NAI treatment on hospitalization. We adjusted for NAI treatment propensity and preadmission antibiotic use, including “study center” as a random intercept to account for differences in baseline hospitalization rate between centers. Results: We included 3376 patients with influenza A(H1N1)pdm09, of whom 3085 (91.4%) had laboratory-confirmed infection. Eight hundred seventy-three patients (25.8%) received outpatient or community-based NAI treatment, 928 of 2395 (38.8%) with available data had dyspnea or respiratory distress, and hospitalizations occurred in 1705 (50.5%). After adjustment for preadmission antibiotics and NAI treatment propensity, preadmission NAI treatment was associated with decreased odds of hospital admission compared to no NAI treatment (adjusted odds ratio, 0.24; 95% confidence interval, 0.20–0.30). Conclusions: In a population with confirmed or suspected A(H1N1)pdm09 and at high risk of hospitalization, outpatient or community-based NAI treatment significantly reduced the likelihood of requiring hospital admission. These data suggest that community patients with severe influenza should receive NAI treatment.

12. Impact of outpatient neuraminidase inhibitor treatment in patients infected with influenza A(H1N1)pdm09 at high risk of hospitalization: an Individual Participant Data (IPD) meta-analysis

Author

Venkatesan, Sudhir, Myles, Puja R., Leonardi-Bee, Jo, Muthuri, Stella G., Al Masri, Malak, Andrews, Nick, Bantar, Carlos, Dubnov-Raz, Gal, Gérardin, Patrick, Koay, Evelyn S.C., Loh, Tze Ping, Memish, Ziad A., Miller, Elizabeth, Oliva, Maria E., Rath, Barbara A., Schweiger, Brunhilde, Tang, Julian W., Tran, Dat, Vidmar, Tjasa, Waight, Pauline A., Nguyen-Van-Tam, Jonathan S., Venkatesan, Sudhir, Myles, Puja R., Leonardi-Bee, Jo, Muthuri, Stella G., Al Masri, Malak, Andrews, Nick, Bantar, Carlos, Dubnov-Raz, Gal, Gérardin, Patrick, Koay, Evelyn S.C., Loh, Tze Ping, Memish, Ziad A., Miller, Elizabeth, Oliva, Maria E., Rath, Barbara A., Schweiger, Brunhilde, Tang, Julian W., Tran, Dat, Vidmar, Tjasa, Waight, Pauline A., and Nguyen-Van-Tam, Jonathan S.

Abstract

Background: While evidence exists to support the effectiveness of neuraminidase inhibitors (NAIs) in reducing mortality when given to hospitalized patients with A(H1N1)pdm09 virus infection, the impact of outpatient treatment on hospitalization has not been clearly established. We investigated the impact of outpatient NAI treatment on subsequent hospitalization in patients with A(H1N1)pdm09 virus infection. Methods: We assembled general community and outpatient data from 9 clinical centers in different countries collected between January 2009 and December 2010. We standardized data from each study center to create a pooled dataset and then used mixed-effects logistic regression modeling to determine the effect of NAI treatment on hospitalization. We adjusted for NAI treatment propensity and preadmission antibiotic use, including “study center” as a random intercept to account for differences in baseline hospitalization rate between centers. Results: We included 3376 patients with influenza A(H1N1)pdm09, of whom 3085 (91.4%) had laboratory-confirmed infection. Eight hundred seventy-three patients (25.8%) received outpatient or community-based NAI treatment, 928 of 2395 (38.8%) with available data had dyspnea or respiratory distress, and hospitalizations occurred in 1705 (50.5%). After adjustment for preadmission antibiotics and NAI treatment propensity, preadmission NAI treatment was associated with decreased odds of hospital admission compared to no NAI treatment (adjusted odds ratio, 0.24; 95% confidence interval, 0.20–0.30). Conclusions: In a population with confirmed or suspected A(H1N1)pdm09 and at high risk of hospitalization, outpatient or community-based NAI treatment significantly reduced the likelihood of requiring hospital admission. These data suggest that community patients with severe influenza should receive NAI treatment.

13. Impact of outpatient neuraminidase inhibitor treatment in patients infected with influenza A(H1N1)pdm09 at high risk of hospitalization: an Individual Participant Data (IPD) meta-analysis

Author

Venkatesan, Sudhir, Myles, Puja R., Leonardi-Bee, Jo, Muthuri, Stella G., Al Masri, Malak, Andrews, Nick, Bantar, Carlos, Dubnov-Raz, Gal, Gérardin, Patrick, Koay, Evelyn S.C., Loh, Tze Ping, Memish, Ziad A., Miller, Elizabeth, Oliva, Maria E., Rath, Barbara A., Schweiger, Brunhilde, Tang, Julian W., Tran, Dat, Vidmar, Tjasa, Waight, Pauline A., Nguyen-Van-Tam, Jonathan S., Venkatesan, Sudhir, Myles, Puja R., Leonardi-Bee, Jo, Muthuri, Stella G., Al Masri, Malak, Andrews, Nick, Bantar, Carlos, Dubnov-Raz, Gal, Gérardin, Patrick, Koay, Evelyn S.C., Loh, Tze Ping, Memish, Ziad A., Miller, Elizabeth, Oliva, Maria E., Rath, Barbara A., Schweiger, Brunhilde, Tang, Julian W., Tran, Dat, Vidmar, Tjasa, Waight, Pauline A., and Nguyen-Van-Tam, Jonathan S.

Abstract

Background: While evidence exists to support the effectiveness of neuraminidase inhibitors (NAIs) in reducing mortality when given to hospitalized patients with A(H1N1)pdm09 virus infection, the impact of outpatient treatment on hospitalization has not been clearly established. We investigated the impact of outpatient NAI treatment on subsequent hospitalization in patients with A(H1N1)pdm09 virus infection. Methods: We assembled general community and outpatient data from 9 clinical centers in different countries collected between January 2009 and December 2010. We standardized data from each study center to create a pooled dataset and then used mixed-effects logistic regression modeling to determine the effect of NAI treatment on hospitalization. We adjusted for NAI treatment propensity and preadmission antibiotic use, including “study center” as a random intercept to account for differences in baseline hospitalization rate between centers. Results: We included 3376 patients with influenza A(H1N1)pdm09, of whom 3085 (91.4%) had laboratory-confirmed infection. Eight hundred seventy-three patients (25.8%) received outpatient or community-based NAI treatment, 928 of 2395 (38.8%) with available data had dyspnea or respiratory distress, and hospitalizations occurred in 1705 (50.5%). After adjustment for preadmission antibiotics and NAI treatment propensity, preadmission NAI treatment was associated with decreased odds of hospital admission compared to no NAI treatment (adjusted odds ratio, 0.24; 95% confidence interval, 0.20–0.30). Conclusions: In a population with confirmed or suspected A(H1N1)pdm09 and at high risk of hospitalization, outpatient or community-based NAI treatment significantly reduced the likelihood of requiring hospital admission. These data suggest that community patients with severe influenza should receive NAI treatment.

14. Impact of outpatient neuraminidase inhibitor treatment in patients infected with influenza A(H1N1)pdm09 at high risk of hospitalization: an Individual Participant Data (IPD) meta-analysis

Author

Venkatesan, Sudhir, Myles, Puja R., Leonardi-Bee, Jo, Muthuri, Stella G., Al Masri, Malak, Andrews, Nick, Bantar, Carlos, Dubnov-Raz, Gal, Gérardin, Patrick, Koay, Evelyn S.C., Loh, Tze Ping, Memish, Ziad A., Miller, Elizabeth, Oliva, Maria E., Rath, Barbara A., Schweiger, Brunhilde, Tang, Julian W., Tran, Dat, Vidmar, Tjasa, Waight, Pauline A., Nguyen-Van-Tam, Jonathan S., Venkatesan, Sudhir, Myles, Puja R., Leonardi-Bee, Jo, Muthuri, Stella G., Al Masri, Malak, Andrews, Nick, Bantar, Carlos, Dubnov-Raz, Gal, Gérardin, Patrick, Koay, Evelyn S.C., Loh, Tze Ping, Memish, Ziad A., Miller, Elizabeth, Oliva, Maria E., Rath, Barbara A., Schweiger, Brunhilde, Tang, Julian W., Tran, Dat, Vidmar, Tjasa, Waight, Pauline A., and Nguyen-Van-Tam, Jonathan S.

Abstract

Background: While evidence exists to support the effectiveness of neuraminidase inhibitors (NAIs) in reducing mortality when given to hospitalized patients with A(H1N1)pdm09 virus infection, the impact of outpatient treatment on hospitalization has not been clearly established. We investigated the impact of outpatient NAI treatment on subsequent hospitalization in patients with A(H1N1)pdm09 virus infection. Methods: We assembled general community and outpatient data from 9 clinical centers in different countries collected between January 2009 and December 2010. We standardized data from each study center to create a pooled dataset and then used mixed-effects logistic regression modeling to determine the effect of NAI treatment on hospitalization. We adjusted for NAI treatment propensity and preadmission antibiotic use, including “study center” as a random intercept to account for differences in baseline hospitalization rate between centers. Results: We included 3376 patients with influenza A(H1N1)pdm09, of whom 3085 (91.4%) had laboratory-confirmed infection. Eight hundred seventy-three patients (25.8%) received outpatient or community-based NAI treatment, 928 of 2395 (38.8%) with available data had dyspnea or respiratory distress, and hospitalizations occurred in 1705 (50.5%). After adjustment for preadmission antibiotics and NAI treatment propensity, preadmission NAI treatment was associated with decreased odds of hospital admission compared to no NAI treatment (adjusted odds ratio, 0.24; 95% confidence interval, 0.20–0.30). Conclusions: In a population with confirmed or suspected A(H1N1)pdm09 and at high risk of hospitalization, outpatient or community-based NAI treatment significantly reduced the likelihood of requiring hospital admission. These data suggest that community patients with severe influenza should receive NAI treatment.