| Literature DB >> 31387672 |
Ainara Mira-Iglesias1, F Xavier López-Labrador1,2, Víctor Baselga-Moreno1, Miguel Tortajada-Girbés3, Juan Mollar-Maseres4, Mario Carballido-Fernández5,6, Germán Schwarz-Chavarri7, Joan Puig-Barberà1,8, Javier Díez-Domingo1.
Abstract
IntroductionInfluenza immunisation is recommended for elderly people each season. The influenza vaccine effectiveness (IVE) varies annually due to influenza viruses evolving and the vaccine composition.AimTo estimate, in inpatients ≥ 60 years old, the 2017/18 trivalent IVE, overall, by vaccine type and by strain. The impact of vaccination in any of the two previous seasons (2016/17 and 2015/16) on current (2017/18) IVE was also explored.MethodsThis was a multicentre prospective observational study within the Valencia Hospital Surveillance Network for the Study of Influenza and Respiratory Viruses Disease (VAHNSI, Spain). The test-negative design was applied taking laboratory-confirmed influenza as outcome and vaccination status as main exposure. Information about potential confounders was obtained from clinical registries and/or by interviewing patients; vaccine information was only ascertained by registries.ResultsOverall, 2017/18 IVE was 9.9% (95% CI: -15.5 to 29.6%), and specifically, 48.3% (95% CI: 13.5% to 69.1%), -29.9% (95% CI: -79.1% to 5.8%) and 25.7% (95% CI: -8.8% to 49.3%) against A(H1N1)pdm09, A(H3N2) and B/Yamagata lineage, respectively. For the adjuvanted and non-adjuvanted vaccines, overall IVE was 10.0% (95% CI: -24.4% to 34.9%) and 7.8% (95% CI: -23.1% to 31.0%) respectively. Prior vaccination significantly protected against influenza B/Yamagata lineage (IVE: 50.2%; 95% CI: 2.3% to 74.6%) in patients not vaccinated in the current season. For those repeatedly vaccinated against influenza A(H1N1)pdm09, IVE was 46.4% (95% CI: 6.8% to 69.2%).ConclusionOur data revealed low vaccine effectiveness against influenza in hospitalised patients ≥60 years old in 2017/18. Prior vaccination protected against influenza A(H1N1)pdm09 and B/Yamagata-lineage.Entities:
Keywords: Spain; epidemiology; hospitalisations; influenza; influenza virus; surveillance; vaccine; viral infections
Mesh:
Substances:
Year: 2019 PMID: 31387672 PMCID: PMC6685101 DOI: 10.2807/1560-7917.ES.2019.24.31.1800461
Source DB: PubMed Journal: Euro Surveill ISSN: 1025-496X
Figure 1Selection process and influenza status of hospitalised patients ≥ 60 years old for the influenza vaccine effectiveness study, Valencia Hospital Network for the Study of Influenza (VAHNSI), Spain, 2017/18 influenza season (n = 4,858 eligible patients)
Figure 2Admissions with laboratory-confirmed influenza in patients ≥ 60 years old, with influenza positivity percentages shown by epidemiological week, Valencia Hospital Network for the Study of Influenza (VAHNSI), Spain, 2017/18 influenza season (n = 483 patients)
Characteristics of patients ≥ 60 years old admitted to hospital and included in the influenza vaccine effectiveness study, Valencia Hospital Network for the Study of Influenza (VAHNSI), Spain, 2017/18 influenza season (n = 1,477 patients)
| Characteristics | Influenza | Influenza | p valuec | Number vaccinated in 2017/18 | Total | %d | p value | ||
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| n | %a | n | %b | ||||||
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| 483 | 32.7 | 994 | 67.3 | NA | 759 | 1,477 | 51.4 | NA |
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| 60–69 | 88 | 18.2 | 203 | 20.4 | 0.218 | 99 | 291 | 34.0 |
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| 70–79 | 166 | 34.4 | 289 | 29.1 | 244 | 455 | 53.6 | ||
| 80–89 | 177 | 36.6 | 384 | 38.6 | 327 | 561 | 58.3 | ||
| ≥ 90 | 52 | 10.8 | 118 | 11.9 | 89 | 170 | 52.4 | ||
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| Male | 234 | 48.4 | 526 | 52.9 | 0.107 | 420 | 760 | 55.3 |
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| Female | 249 | 51.6 | 468 | 47.1 | 339 | 717 | 47.3 | ||
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| None | 29 | 6.0 | 76 | 7.6 | 0.181 | 35 | 105 | 33.3 |
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| One | 122 | 25.3 | 214 | 21.5 | 154 | 336 | 45.8 | ||
| Two or more | 332 | 68.7 | 704 | 70.8 | 570 | 1,036 | 55.0 | ||
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| Yes | 140 | 29.0 | 346 | 34.8 |
| 485 | 991 | 48.9 |
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| No | 343 | 71.0 | 648 | 65.2 | 274 | 486 | 56.4 | ||
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| None | 145 | 30.0 | 314 | 31.6 | 0.814 | 223 | 459 | 48.6 | 0.126 |
| One | 56 | 11.6 | 116 | 11.7 | 82 | 172 | 47.7 | ||
| Two or more | 282 | 58.4 | 564 | 56.7 | 454 | 846 | 53.7 | ||
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| Never | 256 | 53.0 | 427 | 43.0 |
| 350 | 683 | 51.2 |
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| Ex-smoker | 158 | 32.7 | 425 | 42.8 | 336 | 583 | 57.6 | ||
| Current smoker | 69 | 14.3 | 142 | 14.3 | 73 | 211 | 34.6 | ||
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| Professional | 57 | 11.8 | 119 | 12.0 | 0.953 | 88 | 176 | 50.0 | 0.527 |
| Skilled | 43 | 8.9 | 93 | 9.4 | 76 | 136 | 55.9 | ||
| Unskilled | 383 | 79.3 | 782 | 78.7 | 595 | 1,165 | 51.1 | ||
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| No | 356 | 73.7 | 733 | 73.7 | 0.988 | 556 | 1,089 | 51.1 | 0.669 |
| Yes | 127 | 26.3 | 261 | 26.3 | 203 | 388 | 52.3 | ||
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| 0–2 | 74 | 15.3 | 175 | 17.6 | 0.310 | 131 | 249 | 52.6 | 0.153 |
| 3–4 | 212 | 43.9 | 387 | 38.9 | 300 | 599 | 50.1 | ||
| 5–7 | 157 | 32.5 | 348 | 35.0 | 274 | 505 | 54.3 | ||
| > 7 | 40 | 8.3 | 84 | 8.5 | 54 | 124 | 43.5 | ||
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| Vaccinated 2017/18 | 242 | 50.1 | 517 | 52.0 | 0.491 | NA | NA | NA | NA |
| Vaccinated 2016/17 | 241 | 49.9 | 528 | 53.1 | 0.245 | 663 | 769 | 86.2 |
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| Vaccinated 2015/16 | 254 | 52.6 | 544 | 54.7 | 0.439 | 651 | 798 | 81.6 |
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| Negative | 0 | 0.0 | 994 | 100.0 | NA | 517 | 994 | 52.0 | 0.491 |
| A(H1N1)pdm09 | 81 | 16.8 | 0 | 0.0 | NA | 30 | 81 | 37.0 |
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| A(H3N2) | 232 | 48.0 | 0 | 0.0 | NA | 132 | 232 | 56.9 | 0.067 |
| B/Yamagata lineage | 150 | 31.1 | 0 | 0.0 | NA | 69 | 150 | 46.0 | 0.405 |
| B/Victoria lineage | 1 | 0.2 | 0 | 0.0 | NA | 1 | 1 | 0.0 | 0.272 |
GP: general practitioner.
a Except for the ‘Overall’ category line of the Table, where the percentages are calculated relative to the total number of patients included in the analysis (i.e. 1,477), the rest of the percentages presented in this column are based on the total of patients testing positive for influenza (i.e. 483).
b Except for the ‘Overall’ category line of the Table, where the percentages are calculated relative to the total number of patients included in the analysis (i.e. 1,477), the rest of the percentages presented in this column are based on the total of patients testing negative for influenza (i.e. 994).
c These p values identify whether there is a dependence between the laboratory-confirmed influenza variable and the characteristics on the left, e.g. age. P values < 0.05 indicate that influenza cases and influenza controls were not equally distributed according to the explored characteristics on the left.
d Percentages in this column are based on the numbers and totals displayed in the two previous columns.
e Socioeconomic status: ‘professional’ includes professionals, managers, medium or superior technicians, small entrepreneurs, middle managers, supervisors; ‘skilled’ includes skilled manual workers; ‘unskilled’ includes semi-skilled and unskilled manual workers.
f Obesity was defined as a body mass index (BMI) ≥ 30.
g Fifteen influenza A and four influenza B samples were not subtyped because of low viral loads.
Bold font is used to highlight p values indicating statistical significance.
Influenza vaccine effectiveness by vaccine type, regardless of vaccination history in patients ≥ 60 years old admitted to hospital, Valencia Hospital Network for the Study of Influenza (VAHNSI), Spain, 2017/18 influenza season (n = 1,477 patients)
| Types, subtypes or lineage of influenza | N | Casesa | Vaccinated cases | Controlsb | Vaccinated controls | Overall IVE | Overall IVE | Overall IVE | |||||||
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| Adjuvanted | Non-adjuvanted | Total | Adjuvanted | Non-adjuvanted | Total | IVE | 95% CI | IVE | 95% CI | IVE | 95% CI | ||||
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| A(H1N1)pdm09d | 684 | 77 | 12 | 16 | 28 | 607 | 137 | 189 | 326 | 48.33 | 13.51 to 69.13 | 34.38 | −34.58 to 68.00 | 54.12 | 15.32 to 75.14 |
| A(H3N2)e | 1,226 | 232 | 54 | 77 | 131 | 994 | 239 | 271 | 510 | −29.88 | −79.09 to 5.81 | −23.93 | −87.94 to 18.28 | −37.03 | −98.15 to 5.24 |
| B/Yamagataf | 916 | 150 | 29 | 39 | 68 | 766 | 180 | 228 | 408 | 25.75 | −8.83 to 49.35 | 30.09 | −15.94 to 57.85 | 21.10 | −24.43 to 49.97 |
CI: confidence interval; GP: general practitioner; IVE: influenza vaccine effectiveness; LCI: laboratory-confirmed influenza.
a Cases in this column were individuals included in the study with LCI who were admitted to hospital during the period when influenza viruses of the type or subtype in question circulated. For example, cases of all influenza comprised all LCI individuals admitted during the 2017/18 influenza season, while cases of influenza A(H1N1)pdm09, A(H3N2) and B/Yamagata lineage only included patients admitted during times when influenza A(H1N1)pdm09, A(H3N2) and B/Yamagata lineage viruses respectively circulated. For each virus type, the time of circulation was estimated as the period between the first of at least two consecutive weeks with two or more cases of this type and the previous week of the first of two consecutive weeks with no cases of this type.
b Controls in this column were individuals included in the study who tested negative for influenza in the laboratory and who were admitted to hospital during the time that viruses of the influenza type in question circulated. The time of circulation was estimated as described in the above footnote a.
c Adjusted by age, number of chronic conditions, sex, socioeconomic class (occupation), admission in the last 12 months, number of GP visits in the last 3 months, smoking habits, obesity status, days between symptoms onset and swab, hospital and epidemiological week at admission. Nine individuals vaccinated with a vaccine different from the ones under study were excluded from the IVE estimations by vaccine type (seven controls and two cases).
d Adjusted by age, sex and epidemiological week at admission. Four individuals vaccinated with a vaccine different from the ones under study were excluded from the IVE estimations by vaccine type; all four were controls.
e Adjusted by age, number of chronic conditions, sex, socioeconomic status (occupation), admission in the last 12 months, number of GP visits in the last 3 months, smoking habits, obesity status, days between symptoms onset and swab, hospital and epidemiological week at admission. Eight individuals vaccinated with a vaccine different from the ones under study were excluded from the IVE estimations by vaccine type (seven controls and one case).
f Adjusted by age, number of chronic conditions, sex, smoking habits and epidemiological week at admission. Seven individuals vaccinated with a vaccine different from the ones under study were excluded from the IVE estimations by vaccine type (six controls and one case).
Influenza vaccine effectiveness, considering vaccination history in the current and the two previous seasons in patients ≥ 60 years old admitted to hospital, Valencia Hospital Network for the Study of Influenza (VAHNSI), Valencia, Spain, 2017/18 influenza season (n = 1,477 patients)
| Types, subtypes or lineage of influenza | Vaccinated in either 2015/16 or 2016/17a | Vaccinated in 2017/18 | IVEb | 95% CI |
|---|---|---|---|---|
| All influenzac | No | Yes | 30.16 | −34.21 to 63.65 |
| Yes | Yes | 14.20 | −12.79 to 34.73 | |
| Yes | No | 22.98 | −16.64 to 49.14 | |
| A(H1N1)pdm09d | No | Yes | 80.11 | −53.74 to 97.43 |
| Yes | Yes | 46.41 | 6.78 to 69.20 | |
| Yes | No | 10.60 | −94.00 to 58.80 | |
| A(H3N2)e | No | Yes | −1.47 | −142.01 to 57.46 |
| Yes | Yes | −35.26 | −93.67 to 5.53 | |
| Yes | No | −7.52 | −84.80 to 37.44 | |
| B/Yamagataf | No | Yes | 4.48 | −142.60 to 62.39 |
| Yes | Yes | 39.61 | 8.13 to 60.31 | |
| Yes | No | 50.18 | 2.34 to 74.59 |
CI: confidence interval; GP: general practitioner; IVE: influenza vaccine effectiveness.
a The 2015/16 influenza vaccine comprised an A/California/7/2009 (H1N1)pdm09-like virus, an A/Switzerland/9715293/2013 (H3N2)-like virus and a B/Phuket/3073/2013-like virus (Yamagata lineage). The 2016/17 influenza vaccine comprised an A/California/7/2009 (H1N1)pdm09-like virus, an A/Hong Kong/4801/2014 (H3N2)-like virus and a B/Brisbane/60/2008-like virus (Victoria lineage).
b Taking those individuals not vaccinated in any of the three considered seasons as reference category.
c Adjusted by age, number of chronic conditions, sex, socioeconomic status (occupation), admission in the last 12 months, number of GP visits in the last 3 months, smoking habits, obesity status, days between symptoms onset and swab, hospital and epidemiological week at admission.
d Adjusted by age, sex and epidemiological week at admission.
e Adjusted by age, number of chronic conditions, sex, socioeconomic status (occupation), admission in the last 12 months, number of GP visits in the last 3 months, smoking habits, obesity status, days between symptoms onset and swab, hospital and epidemiological week at admission.
f Adjusted by age, number of chronic conditions, sex, smoking habits and epidemiological week at admission.