Effects of prophylactic ibuprofen and paracetamol administration on the immunogenicity and reactogenicity of the 10-valent pneumococcal non-typeable<i>Haemophilus influenzae</i>protein D conjugated vaccine (PHiD-CV) co-administered with DTPa-combined vaccines in children: An open-label, randomized, controlled, non-inferiority trial

Falup‐Pecurariu, Oana; Man, Sorin Claudiu; Neamtu, ML; Chicin, Gratiana; Baciu, Ginel; Pitic, Carmen; Cara, Alexandra C; Neculau, Andrea Elena; Burlea, Marin; Brinza, Ileana L; Schnell, Cristina Nicoleta; Sas, Valentina; Lupu, Vasile Valeriu; François, Nancy; Swinnen, Kristien; Borys, Dorota

doi:10.1080/21645515.2016.1223001

Cited by 21 publications

(24 citation statements)

References 32 publications

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“…Lower impact after dose 2. 105, 106, 112, 113 ↓ Fever↓ Swelling↓ PainAdministered therapeutically↓ FeverNo impact.↓ Pain Oral ibuprofen b Administered prophylactically at the time of vaccination and within the following 24 hLimited impact↓ pertussis toxin, tetanus. No impact after the second dose. 103, 112 Administered therapeutically↓ FeverNo impact.↓ Pain a One publication in older adults (mean ages 73–75 years). Results showed no impact on antibody levels and limited impact on symptoms b No data in older adults…”

Section: Symptom Managementmentioning

confidence: 99%

The how’s and what’s of vaccine reactogenicity

Hervé

Laupèze

Giudice³

et al. 2019

npj Vaccines

372

361

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Reactogenicity represents the physical manifestation of the inflammatory response to vaccination, and can include injection-site pain, redness, swelling or induration at the injection site, as well as systemic symptoms, such as fever, myalgia, or headache. The experience of symptoms following vaccination can lead to needle fear, long-term negative attitudes and non-compliant behaviours, which undermine the public health impact of vaccination. This review presents current knowledge on the potential causes of reactogenicity, and how host characteristics, vaccine administration and composition factors can influence the development and perception of reactogenicity. The intent is to provide an overview of reactogenicity after vaccination to help the vaccine community, including healthcare professionals, in maintaining confidence in vaccines by promoting vaccination, setting expectations for vaccinees about what might occur after vaccination and reducing anxiety by managing the vaccination setting.

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Section: Symptom Managementmentioning

confidence: 99%

The how’s and what’s of vaccine reactogenicity

Hervé

Laupèze

Giudice³

et al. 2019

npj Vaccines

372

361

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show abstract

“…For PCV10, a decreased immune response was noted in Prymula et al, and Falup et al [ 21 , 23 ]. Particularly, in Prymula et al, significantly lower antibody titers for all ten vaccine serotypes were observed one month after the primary vaccination in the group of children who received paracetamol with vaccination (t:0 h) compared with the group that did not receive paracetamol.…”

Section: Resultsmentioning

confidence: 97%

“…OPA GMTs detected no differences. Post booster: No effect Falup et al 2017 [ 23 ] Romania, 2016, RCT, Open label, unblinded 850 PCV10 (Synflorix™, GSK) DTPa-HBV-IPV/Hib (Infanrix Hexa™, GSK) 3, 4, 5 m/12–15 m Paracetamol Syr (15 mg/kg/dose) Ibuprofen Syr (10 mg/kg/dose) 3 doses/ 6–8 h for 24 h. t:0 h or t: 4-6 h ΙgG GMCs 1 m post-primary and booster dose (sp cut off: GMCs ≥0,2 μg/ml-22F-inhibition ELISA) Post primary: % GMCs ≥0.2 μg/mL lower in IPARA and DPARA vs NPARA (highest difference for 6B serotype) GMCS for serotypes 1, 4, 5, 9 V, 14, 18C in IPARA and 1,6B in DPARA lower vs NPARA. Post booster: GMCs in IPARA-ΝPARA and the majority of participants in DPARA-IPARA lower vs NPARA-NPARA Prymula et al 2014 [ 22 ] Czech Republic, 2014, RCT, Open label, unblinded 558 PCV7 (Prevenar™, Pfizer) 4CMenB (Bexsero™, Novartis) DTaP-HBV-IPV/Hib (Infanrix Hexa GSK) 2, 3, 4 m/12 m Paracetamol Syr (10-15 mg/kg) 3 doses/ 4–6 h for 24 h. t:0 h ΙgG GMCs 1 m post-primary and booster dose (sp cut-off: GMCs ≥0.35 μg/ml non-22F ELISA) GMCs for all serotypes in PARA lower vs NPARA (no statistical significance) Prymula et al 2013 [ 17 ] Czech Republic, 2012, RCT, unblinded (Follow up of Prymula et al 2009) 443 PCV10 (Synflorix GSK) 31–44 m (2nd booster dose) Paracetamol only at primary and 1st booster dose ΙgG GMCs before and 7–10 days after 2nd booster dose (sp cut-off: GMCs ≥0,2 μg/ml-22F-inhibition ELISA) OPA GMTs Before the 2nd booster: GMCs for serotypes 1, 4, 5 in PARA lower vs NPARA (borderline statistical significance).…”

Section: Resultsmentioning

confidence: 99%

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Effect of prophylactic administration of antipyretics on the immune response to pneumococcal conjugate vaccines in children: a systematic review

2021

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Background Prophylactic administration of antipyretics at the time of immunization seems to decrease some side effects, however reduced immune responses have been reported in some studies. This systematic review aimed to investigate the effect of prophylactic use of antipyretics on the immune response following administration of pneumococcal conjugate vaccines (PCVs). Methods A systematic review of randomized controlled trials and observational studies concerning the immune response to PCVs after antipyretic administration was performed up to November 2020 in the electronic databases of Pubmed and Scopus. Results Of the 3956 citations retrieved, a total of 5 randomized control trials including 2775 children were included in the review. Included studies were referred to PCV10 (3 studies), PCV7 and PCV13 (one study each). The prophylactic administration of paracetamol decreased the immune response to certain pneumococcal serotypes in all included studies. The effect was more evident following primary vaccination and with immediate administration of paracetamol. Despite the reductions in antibody geometric mean concentrations, a robust memory response was observed following the booster dose. Besides, antibody titers remained above protective levels in 88–100% of participants. The use of ibuprofen, that was evaluated in two studies, did not seem to affect the immunogenicity of PCVs . Conclusion Although the reviewed studies had significant heterogeneity in design, paracetamol administration seems to affect the immune response for certain serotypes. The clinical significance of reduced immunogenicity especially before booster dose needs further investigation.

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“…Most of the preventable AEFI reports were due to the potential interaction between the components of the vaccines or between the vaccines and concomitant medications administered to the patients. Previous studies have documented poor immunologic response to conjugated Pneumococcus vaccine following acetaminophen administration (Prymula et al, 2009; Falup-Pecurariu et al, 2017; Wysocki et al, 2017). We also reported one case of interaction between varicella, live-attenuated vaccine, and the glucocorticoid betamethasone, which may result in an inadequate immunological response to the live vaccine (Infectious Diseases and Immunization Committee, Canadian Paediatric Society, 2000; Liu et al, 2013).…”

Section: Discussionmentioning

confidence: 99%

Vaccines Safety in Children and in General Population: A Pharmacovigilance Study on Adverse Events Following Anti-Infective Vaccination in Italy

et al. 2019

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Background: The concern for adverse events following immunization (AEFI) and anti-vaccination movements that lacked scientific evidence-based supports may reduce vaccine uptake in the general population. Thus, the aims of the present study were to characterize AEFI in general population (all age groups), in terms of frequency, preventability, and seriousness and to define predictors of their seriousness in children. Methods: A retrospective study was performed on suspected AEFI reports for children and adults who received any form of vaccinations, collected in Tuscany, Italy, between 1 January and 31 December 2017. Patients’ characteristics, suspected vaccines, and AEFI description were collected. Causality and preventability were assessed using WHO and Schumock and Thornton algorithms, respectively. Logistic regression was used to estimate the reporting odds ratios of potential predictors of AEFI seriousness in children. Results: A total of 223 suspected AEFI reports were collected, and the majority of them were defined as non-serious (76.7%). Reports were mostly related to one vaccine, and to a median of two to five strains/toxoids. The total number of simultaneously administered strains/toxoids and the presence of allergens did not correlate with AEFI seriousness. Considering vaccines with a high number of administered doses (≥60,000 doses), the rates estimated for serious AEFI reports were always very low, ranging between 0.01 and 0.2/1,000 doses. Twenty-four vaccines (8,993 doses) were not related to any AEFI. Conclusion: Results of present study showed that AEFI were very rare; the vast majority of them was non-serious and, despite the claims of anti-vaccination movements, the simultaneous administration of vaccines was safe and did not influence the risk of reporting a serious AEFI, particularly in children.

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Cited by 21 publications

References 32 publications

The how’s and what’s of vaccine reactogenicity

The how’s and what’s of vaccine reactogenicity

Effect of prophylactic administration of antipyretics on the immune response to pneumococcal conjugate vaccines in children: a systematic review

Vaccines Safety in Children and in General Population: A Pharmacovigilance Study on Adverse Events Following Anti-Infective Vaccination in Italy

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