Immunogenicity of the inactivated influenza vaccine in children who have undergone allogeneic haematopoietic stem cell transplant.

Influenza vaccination is recommended for children following allogeneic haematopoietic stem cell transplant (HSCT), however there is limited evidence regarding its benefit. A prospective multicentre study was conducted to evaluate the immunogenicity of the inactivated influenza vaccine in children who have undergone HSCT compared with healthy age-matched controls. Participants were vaccinated between 2013 and 2016 according to Australian guidelines. Influenza-specific hemagglutinin inhibition antibody titres were performed prior to each vaccination and 4 weeks following the final vaccination. A nasopharyngeal aspirate for influenza was performed on participants that developed influenza-like illness. There were 86 children recruited; 43 who had undergone HSCT and 43 controls. For the HSCT group, seroprotection and seroconversion rates were 81.4% and 60.5% for H3N2, 41.9% and 32.6% for H1N1, and 44.2% and 39.5% for B strain respectively. There was a significant geometric mean fold increase to the H3N2 (GMFI 5.80, 95% CI 3.68-9.14, p < 0.001) and B (GMFI 3.44, 95% CI 2.36-5.00, p = 0.048) strains. Serological response was superior in age-matched controls to all vaccine strains. There were no serious adverse events following vaccination. For children who underwent HSCT, incidence of laboratory-proven influenza infection was 2.3%. Overall, this study provides evidence to support annual inactivated influenza vaccine administration to children following HSCT.

Introduction

Influenza infection can result in significant morbidity and mortality following allogeneic haematopoietic stem cell transplantation (HSCT) [1-3]. In children, the incidence of influenza following allogeneic HSCT ranges between 0.9 and 9.9% [4-8]. Administration of one dose of the seasonal inactivated influenza vaccine is recommended for children commencing 6 months following HSCT. Children aged 6 months to 8 years who have never previously been vaccinated should receive two doses, 4 or more weeks apart [9, 10]. However, these recommendations are based on adult studies [10], with a distinct paucity of paediatric-specific data assessing the immunogenicity of the inactivated influenza vaccine following HSCT [11]. Given the lack of evidence, we undertook a prospective multicentre study to evaluate the immunogenicity of the seasonal inactivated influenza vaccine in children who have undergone allogeneic HSCT compared with healthy matched controls, and to identify risk factors that predict vaccine response in this population.

Methods

Patient selection

Children between the ages of 6 months and 18 years who were ≥6 months and ≤2 years post allogeneic HSCT were eligible. Recruitment was undertaken during the Southern Hemisphere influenza seasons of 2013–2016 (March to September) from four tertiary paediatric haematology, oncology and bone marrow transplant units in Australia (Princess Margaret Hospital for Children, Perth; Queensland Children’s Hospital, Brisbane; Women’s and Children’s Hospital, Adelaide; The Royal Children’s Hospital, Melbourne). Healthy siblings were recruited as age-matched controls. Exclusion criteria included anaphylaxis to previous doses of any influenza vaccine, a history of egg anaphylaxis, receipt of intravenous immunoglobulin within the last 3 months, a history of Guillain-Barre syndrome or current medical condition that would be compromised by inclusion in the study. Informed consent was obtained from the parents of each child prior to recruitment.

Study design

Participants were vaccinated with inactivated influenza vaccine according to national Australian guidelines [12]. Children receiving influenza vaccine for the first time post allogeneic HSCT were given two doses of the vaccine 4 weeks apart, with one dose given to vaccine-experienced children. For healthy age-matched controls, children less than 10 years of age receiving influenza vaccine for the first time, were given two doses of the influenza vaccine 4 weeks apart; children less than 10 years of age who had previously received the influenza vaccine and children who were 10 or older were given a single dose of the vaccine. A 0.25 mL dose was administered to children less than 3 years of age and 0.5 mL to children older than 3. The inactivated trivalent vaccine was given for the 2013–2015 seasons and the inactivated quadrivalent vaccine for the 2016 season. The specific strains included in each annual influenza vaccine were A/Victoria/362/2011 (H3N2), A/California/7/2009 (H1N1), B/Hubei-Wujiagang/158/2009 (B) for 2013; A/Texas/50/2012 (H3N2), A/California/7/2009 (H1N1), B/Massachusetts/2/2012 (B) for 2014; A/South Australia/55/2014 (H3N2), A/California/7/2009 (H1N1), B/Phuket/3073/2013 (B) for 2015; and A/Hong Kong/480/2014 (H3N2), A/California/7/2009 (H1N1), B/Phuket/3073/2013 (B), B/Brisbane/60/2008 (B) for 2016.

Blood was taken prior to each vaccination and 4 weeks following the final vaccination to assess influenza-specific immune responses. Following collection, blood samples were centrifuged and sera stored at −20 °C. At the end of each influenza season, the samples were sent to the World Health Organization (WHO) Collaborating Centre for Reference and Research on Influenza, Victorian Infectious Diseases Reference Laboratory where standardised hemagglutinin inhibition (HI) assays were performed to determine specific influenza antibody titres towards each virus in the vaccine [13]. Viruses used for HI analysis were egg propagated; specifically for A(H1N1)pdm NYMC-X-179A (A/California/7/2009) was used for seasons 2013–2016. For A(H3N2) IVR-165 (A/Victoria/361/2011), NYMC X-223A (hy A/Texas/50/2012), IVR-175 (A/South Australia/55/2014) and NYMC X-263 (hy A/Hong Kong/4801/2014) were used for the 2013, 2014, 2015 and 2016 seasons, respectively. Split B/Yamagata viruses B/Hubei-Wujiagang/158/2009, NYMC BX-51B (B/Massachusetts/02/2012) and B/Phuket/3073/2013 were used for the 2013, 2014 and 2015 seasons, respectively. Split viruses B/Yamagata (B/Phuket/3073/2013) and B/Victoria (B/Brisbane/60/2008) were both used for the 2016 season.

Susceptibility to a vaccine-like strain was defined as a prevaccination HI titre of <40. Seroprotection in an individual was defined as a post vaccination HI titre of ≥40. Seroconversion was defined as either a fourfold increase in HI antibody titre if the prevaccination titre was ≥10 or a rise in HI titre from <10 to ≥40 following vaccination [14]. The percentage (95% confidence interval [CI]) of patients who individually met the criteria for seroprotection and seroconversion to each strain of the vaccine was calculated.

Criteria as established by the Committee for Proprietary Medicinal Products (CPMP) were used to determine whether the vaccine was considered effective as to elicit an overall immunogenic response [15]. According to these criteria the influenza vaccine is considered effective if it meets one or more of the following three criteria: seroprotection in >70% of patients; seroconversion in >40% of patients; or a geometric mean fold increase (GMFI) of >2.5. These criteria were used to calculate one-sided p values in relation to the null hypothesis for overall seroprotection and seroconversion to each strain of the vaccine. GMFI was calculated for each strain as the geometric mean of the fold increase in antibody level after vaccination, with CI and one-sided p values estimated using a log-normal approximation for the distribution of antibody levels pre- and post-vaccination and the CPMP defined threshold of GMFI >2.5.

Linear regression models, with change in log antibody level as the dependent variable, were used to assess the influence of clinically relevant predictors on vaccine response to each strain. The predictor variables included within the models were age at receipt of first vaccination, the number of vaccination doses received, time since transplant, and the absolute lymphocyte count at the time of first vaccination. Lower than normal limits for absolute lymphocyte counts according to age were defined as 1.7 × 109/L for children <5 years of age, 1.1 × 109/L for 5 to ≤10 years, and 1.0 × 109/L for ≥10 years [16].

All patients enroled on the study that developed influenza-like illness were instructed to present for clinical review. Influenza detection was performed on a nasopharyngeal aspirate using polymerase chain reaction. Influenza-like illness was defined as an elevated temperature (≥37.5 °C) or a clear history of fever (e.g. chills, rigors); the presence of at least one constitutional symptom from irritability, myalgia, headache, vomiting, diarrhoea or malaise; and the presence of at least one respiratory symptom from cough, sore throat or rhinorrhoea; with the onset of symptoms occurring greater than 72 h after vaccine administration. Clinical features of all children with laboratory-proven influenza infection were documented.

This study was approved by the Child and Adolescent Health Service Ethics Committee (Ethics Approval Number 1988/EP), with ethical approval granted at all sites under the National Mutual Acceptance agreement. It conforms to the provisions of the Declaration of Helsinki in 1995 (as revised in Tokyo, 2004) and the National Statement on Ethical Conduct in Human Research, Australian National Health and Medical Research Council. The study was registered on the Australian New Zealand Clinical Trials Registry (ACTRN12614000240640).

Results

There were 86 children enroled in the study; 43 children who had undergone allogeneic HSCT and 43 healthy controls. The groups were frequency matched according to age (mean age: 7.7 versus 8.2 years, p = 0.65) and sex (females: 37.2% versus 41.9%, p = 0.66) Participant characteristics are listed in Table 1, with individualised characteristics listed in Supplementary Table 1. The percentage of patients in the allogeneic HSCT group that were susceptible to each strain of the vaccine prior to the first dose was 65% to H3N2, 88% to H1N1 and 91% to the B strain. Susceptibility of the healthy age-matched controls was 37% to H3N2, 70% to H1N1 and 79% to the B strain. Seroprotection occurred in 81.4% to H3N2, 41.9% to H1N1 and 44.2% to B strain in children who received allogeneic HSCT compared with 97.7%, 81.4% and 69.8% for healthy age-matched controls (Table 2). Seroconversion occurred in 60.5% for H3N2, 32.6% for H1N1 and 39.5% for B strain in children who received allogeneic HSCT, while 72.1%, 65.1% and 58.1% of healthy age-matched controls seroconverted to the respective strains (Table 2). For children in the HSCT group who received two doses of the vaccine and seroconverted, the second dose of the vaccine was required for seroconversion to occur in 47% of patients to H3N2, 70% to H1N1 and 81% to B strain.

Table 1

Patient demographics

Characteristic	Allogeneic HSCT(n = 43)	Healthy controls(n = 43)
Age at vaccination
6 months to <3 years	9	6
3 to <10 years	18	24
10 to <18 years	16	13
Number of vaccine doses
One dose	11	23
Two doses	32	20
Diagnosis
Malignant	26
Non-malignant	17
Donor type
Matched sibling	12
Matched unrelated	28
Haploidentical	3
Interval between allogeneic HSCT and influenza vaccine
6 to  <12 months	32
≥12 months	11
History of graft versus host disease
Yes	23
No	20
On immunosuppressive therapy at time of vaccination
Yes	13
No	30

Table 2

Overall immunogenicity to inactivated influenza vaccine in children who have undergone allogeneic HSCT and age-matched controls

Strain	GMFI (95% CI)	P valuea	Seroprotection % (95% CI)	P valuea	Seroconversion % (95% CI)	P valuea
Allogeneic HSCT (n = 43)
H3N2 (A)	5.80 (3.68–9.14)	<0.001	81.4 (69.8–93.0)	0.051	60.5 (45.9–75.1)	0.003
H1N1 (A)	3.75 (2.20–6.40)	0.069	41.9 (27.1–56.6)	>0.99	32.6 (18.6–46.6)	0.84
B	3.44 (2.36–5.00)	0.048	44.2 (29.3–59.0)	>0.99	39.5 (24.9–54.1)	0.53
B (2016)	1.46 (0.79–2.71)	0.96	44.4 (12.0–76.9)	0.95	33.3 (2.5–64.1)	0.66
Controls (n = 43)
H3N2 (A)	8.96 (5.96–13.45)	<0.001	97.7 (93.2–99.9)	<0.001	72.1 (58.7–85.5)	<0.001
H1N1 (A)	6.49 (4.40–9.56)	<0.001	81.4 (69.8–93.0)	0.051	65.1 (50.9–79.4)	<0.001
B	6.81 (4.41–10.53)	<0.001	69.8 (56.0–83.5)	0.51	58.1 (43.4–72.9)	0.008
B (2016)	5.88 (2.24–15.41)	0.041	66.7 (35.9–97.5)	0.59	44.4 (12.0–76.9)	0.39

aOne-sided P values in relation to CPMP criteria

According to CPMP criteria, children who had undergone allogeneic HSCT demonstrated a significant response to the H3N2 (GMFI 5.80, 95% CI 3.68–9.14, p < 0.001 and seroconversion 60.5%, 95% CI 45.9–75.1, p = 0.003) and B (GMFI 3.44, 95% CI 2.36–5.00, p = 0.048) strains (Table 2). Healthy age-matched controls demonstrated significant response to all vaccine strains: H3N2 (GMFI 8.96, 95% CI 5.96–13.45, p < 0.001; seroprotection 97.7%, 95% CI 93.2–99.9, p < 0.001 and seroconversion 72.1%, 95% CI 58.7–85.5, p < 0.001), H1N1 (GMFI 6.49, 95% CI 4.40–9.56, p < 0.001 and seroconversion 65.1%, 95% CI 50.9–79.4, p < 0.001) and B (GMFI 6.81, 95% CI 4.41–10.53, p < 0.001 and seroconversion 58.1%, 95% CI 43.4–72.9, p = 0.008) according to CPMP criteria (Table 2).

The multivariate analysis of predictive variables revealed a significantly higher GMFI to the B strain for children who received two doses of the inactivated influenza vaccine (Two doses GMFI 4.23, 95% CI 2.74–6.53 versus One dose GMFI 1.88, 95% CI 0.90–3.94, p = 0.019) and who had a normal lymphocyte count at the time of vaccination (Normal range GMFI 4.22, 95% CI 2.78–6.39 versus Low GMFI 1.59, 95% CI 0.71–3.57, p = 0.07). Table 3 shows the multivariate analysis of factors predicting GMFI to each strain.

Table 3

Multivariate analysis of factors predicting GMFI to inactivated influenza vaccine in children who have undergone allogeneic HSCT

Variable	Influenza strain	H3N2 (A)		H1N1 (A)		B
		GMFI (95% CI)	P value	GMFI (95% CI)	P value	GMFI (95% CI)	P value
Time since transplant	<12 months	4.86 (2.84–8.33)	0.42	2.65 (1.44–4.87)	0.15	3.12 (1.99–4.89)	0.24
	≥12 months	9.66 (3.85–24.24)		10.29 (3.64–29.08)		4.54 (2.11–9.76)
Age at vaccination	<10 years	5.73 (3.15–10.43)	0.97	5.31 (2.69–10.48)	0.10	3.52 (2.15–5.76)	0.58
	≥10 years	5.91 (2.71–12.86)		2.09 (0.86–5.05)		3.30 (1.74–6.27)
Lymphocyte count at time of vaccination	Low	3.17 (1.15–8.76)	0.34	1.71 (0.52–5.62)	0.30	1.59 (0.71–3.57)	0.07
	Normal range	6.80 (4.03–11.46)		4.61 (2.51–8.49)		4.22 (2.78–6.39)
Doses of vaccine received	One	7.05 (2.77–17.98)	0.93	7.51 (2.57–21.96)	0.54	1.88 (0.90–3.94)	0.019
	Two	5.42 (3.13–9.38)		2.95 (1.57–5.54)		4.23 (2.74–6.53)

GMFIs are raw subgroup means; P values relate to a multivariate comparison of GMFIs between subgroup

There were no adverse effects following vaccination in either the allogeneic HSCT or healthy age-matched control group. There was a single case of laboratory-proven influenza infection in the allogeneic HSCT group (2.3%). This patient was typed as having H1N1pdm09 strain in 2014, with infection occurring 50 days following completion of a two dose immunisation schedule and absence of a serological response to any vaccine strain. The patient received a 5-day course of oseltamivir following confirmation of influenza infection and did not experience any significant influenza associated complications. There were no cases of laboratory confirmed influenza in the healthy age-matched control group.

Discussion

Influenza infection can result in significant morbidity and mortality following allogeneic HSCT [1-3]. Vaccination with inactivated influenza vaccine represents the main strategy to prevent infection. Several studies have been conducted to determine immunogenicity of the inactivated influenza vaccine in adults who have undergone HSCT, however, there is a distinct lack of paediatric-specific data [11]. Our study demonstrates that the inactivated influenza vaccine is safe and elicits a statistically significant serological response to H3N2 and B strains in children who have undergone allogeneic HSCT. However, serological response was limited in comparison with healthy age-matched controls. The only study from which meaningful paediatric-specific data can be extrapolated for comparison between children who have undergone allogeneic HSCT is from a mixed paediatric-adult study [17]. In this study, seroconversion rates in 27 of the study participants under the age of 18 years were 59.3% for H3N2, 55.6% for H1N1 and 40.7% for B strain. Our current study shows comparable seroconversion rates to the H3N2 and B strains, but showed an inferior seroconversion rate to H1N1. There were notable differences between the H1N1 viruses tested in both of these studies as the Yalcin et al. [17] study was conducted over the 2007–2008 influenza season, when the previous seasonal influenza H1N1 vaccine was used, in comparison with our study, which used a post-2009 H1N1 pandemic influenza virus.

The CPMP have defined criteria to assess whether influenza vaccines are effective within a population. Using these criteria, our study shows that the inactivated influenza vaccine can be considered immunologically effective against the H3N2 and B strains in children following allogeneic HSCT. For the H1N1 strain, statistical significance was not achieved according to GMFI criteria and the numerical thresholds of >70% for seroprotection and >40% for seroconversion were not attained. However, interpretation of these findings should also take into consideration that the CPMP criteria were defined based on applicability to immunocompetent populations, further emphasised by satisfaction of the criteria against all three strains in our age-matched healthy control population. This highlights the need for revised definitions according to different populations, such as immunocompromised children.

Previously, only two small studies assessing responses to influenza vaccination following HSCT have been exclusively performed in children [18, 19]. Haining et al. identified an increase in influenza A-specific CD4+ T-cell proliferation but no increase in influenza A-specific serum antibody levels in four children following vaccination with trivalent inactivated influenza vaccine 4–22 months following allogeneic HSCT [18]. Guerin-El Khourouj et al. identified a cellular proliferative response to H1N1 strain in 11 of 14 children following vaccination 76–336 days post allogeneic HSCT. H1N1 antibody titres were also measured in eight participants, with seroconversion only occurring in one patient following vaccination [19]. Although small numbers, both studies are important as they demonstrate that despite the absence of an influenza-specific antibody response, there was generation of an influenza-specific T-cell response. This finding is supported by an adult study, which identified a strong cell-mediated immune response to a single dose of the trivalent inactivated influenza vaccine in 14 patients following allogeneic HSCT, despite a poor influenza-specific antibody response [20]. This further highlights the potential to consider alternative measures to determine vaccine efficacy in immunocompromised populations, in addition to those defined by the CPMP.

Receipt of two doses of the inactivated influenza vaccine and a normal lymphocyte count at the time of vaccination were identified as significant predictors of vaccine response to B strain. Two studies with combined adult and paediatric populations have identified time from transplantation to vaccination as one of the strongest predictors of response to trivalent inactivated influenza vaccine following HSCT [21, 22], with one of the studies also identifying absolute CD19+ cell counts as being predictive of response [22]. Although both studies were not able to identify a significant benefit for administration of two doses of the trivalent inactivated influenza vaccine compared with one dose [21, 22], the benefit of a second vaccine dose has been demonstrated in several studies which have assessed response to the AS03-adjuvanted 2009 H1N1 vaccine in adults post HSCT [23-25], while another study identified comparable response to two doses of the AS03-adjuvanted 2009 H1N1 vaccine in adults post allogeneic HSCT to a single dose received by healthy controls [26]. Transplant to vaccination interval [24, 26], presence of graft versus host disease [26], donor type [23] and receipt of immunosuppressive therapy [25] have all been shown to be predictive of response to the AS03-adjuvanted 2009 H1N1 vaccine within these studies. Although this is the largest paediatric study to assess immunogenicity of the inactivated influenza vaccine following allogeneic HSCT, greater patient numbers are required to further validate the variables that have been assessed and to identify whether additional variables, such as presence of graft versus host disease, receipt of immunosuppressive therapy, donor type and stem cell source, predict response to vaccination.

To determine whether a vaccine is clinically effective traditionally relies on comparison of infection rate between unvaccinated and vaccinated subjects. In a previous retrospective study, the clinical efficacy of influenza vaccination in HSCT recipients was identified as 80% [27]. However, in the modern era, all patients who have undergone allogeneic HSCT are recommended to receive inactivated influenza vaccination [10], thus precluding assessment of vaccine efficacy due to the low number of unvaccinated patients. This highlights the need for alternative measures to determine the clinical efficacy of influenza vaccine for patients receiving HSCT. Incidence of laboratory-proven influenza infection was defined as the clinical endpoint for this study, limited to one case occurring in the HSCT cohort (2.3%). This patient was typed as having H1N1pdm09 infection in 2014, occurring 50 days following completion of a two dose immunisation schedule, and did not mount protective antibody titres to any strain. The published data regarding clinical effectiveness of the influenza vaccine in HSCT recipients is limited, with reported incidence rates of 10.5% following one dose of the trivalent inactivated influenza vaccine and 4.6% following administration of two doses of AS03-adjuvanted 2009 H1N1 vaccine post allogeneic HSCT [26, 27]. The low incidence of influenza infection in our study may also be influenced by minimising risk of exposure to infection, which is considered standard practice for children who have undergone HSCT [28].

In summary, our data demonstrate that the inactivated influenza vaccine is safe and provides immunogenicity to the H3N2 and B strains in children who have received allogeneic HSCT. We identify the need for further research to improve overall vaccine response and immunogenicity to the H1N1 pandemic strain. Receipt of two doses of the inactivated influenza vaccine and a normal lymphocyte count at the time of vaccination were both predictive of response to the B strain, however larger global collaborative studies are required to validate these findings and investigate a greater number of predictive variables. A high proportion of children who received two vaccine doses and seroconverted, required the second dose of the vaccine for seroconversion to each strain. In conclusion, our study provides evidence to support the recommendation for annual administration of inactivated influenza vaccine to children following allogeneic HSCT.

Supplementary Table 1