Skip to main content
Download PDF

Risk factors and prognosis of recurrent wheezing in Chinese young children: a prospective cohort study

Allergy, Asthma & Clinical Immunology volumeĀ 15, ArticleĀ number:Ā 38 (2019) Cite this article

Abstract

Background

Nearly all the investigations into the risk factors for wheezing and asthma were conducted in developed countries with a high prevalence rate of asthma and allergy, but the studies in developing countries are limited. In this study, we aimed to investigate the risk factors for different wheezing phenotypes in Chinese young children and to explore the prognosis of recurrent wheezing.

Methods

This cohort study contained the recruitment stage and the follow-up stage conducted by phone questionnaire survey. According to the information collected at the follow-up for wheezing episodes and remission age, our cohort was divided into transient wheezing, persistent wheezing and late-onset wheezing. The wheezing symptoms and potential risk factors were compared between these three wheezing groups.

Results

From the initial 109 participants, 78.0% completed the follow-up survey. The frequency of current wheezing at followup was significantly reduced in all three groups compared to the recruitment stage (pā€‰<ā€‰0.01). We observe a trend that the rhinovirus (RV) and respiratory syncytial virus (RSV) infection rates were higher in the persistent wheezing group, and the overall infection rates appear to be the lowest in late-onset wheezing group at recruitment. At follow-up stage, the rates of rhinitis ever and current rhinitis were both higher in the persistent wheezing (63.0%, 50.0%) and late-onset wheezing groups (88.2%, 58.8%), compared to the transient wheezing group (14.3%, 14.3%). The incidence of current wheezing episodes increased cumulatively if the participant had concomitant risk factors of rhinitis ever, aeroallergens sensitization at recruitment, either alone or together with previous RV infection at the time of recruitment.

Conclusion

While the incidence of wheezing declined overall with age, but in addition to transient wheezers, additional subsets of children manifest persistent wheeze or late onset wheeze, and moreover the risk factors for wheezing display phenotypic variability between these subgroups. Rhinitis ever and aeroallergens sensitization, either alone or together with previous RV infection, were the most significant predictors for persistent wheezing in children in an eastern environment, such as in China.

Background

Recurrent wheezing among infant/preschoolers is very prevalent. This not only has an impact on the affected children and their families but also on the society due to increased utilization of ED visits and hospitalizations [1]. Although many young wheezers outgrow their symptoms, a significant proportion of these young children will keep wheezing throughout school age years, or even into adulthood [2]. Studies have shown that the years at preschool are crucial for asthma development as lungs and immune system develop and mature functionally [3, 4]. However, it is very difficult to identify which children with wheezing symptoms will develop asthma in later years. Early identification of recurrent wheezing in children could help physicians to improve the secondary preventive measures and suitable treatments.

To date, multiple risk factors have been identified that contribute to the development of persistent wheezing and susceptibility to asthma. These are: a family history of asthma or atopy, childhood eczema, allergic rhinitis, allergic sensitization (skin prick test and specific IgE), and early life infection with viruses [5, 6]. Notably, viral respiratory infections have been strongly associated with wheezing and susceptibility to asthma. Especially human rhinoviruses (RVs) are gaining recognition as an important risk factor for wheezing and asthma [7]. Jackson et al. found that wheezing RV illness in infancy is the most significant predictor of the development of pre-school wheezing at the age of 3Ā years, and also a predictor of the development of asthma at age of 6Ā years [8, 9]. Another recent study showed that sensitization, eczema, and RV infection are predictors for atopic asthma at the school age [10].

Nearly all the investigations into the risk factors for wheezing and asthma were conducted in developed countries with a high prevalence rate of asthma and allergy [11]. In contrast, there have been limited studies in developing countries. Although the prevalence of childhood asthma and allergy is increasing in developing countries, like China, it is still relatively low compared to that of the Western developed countries, like Australia, the UK, etc. [11, 12]. We hypothesize that the risk profiles for the prognosis of recurrent wheezing are different in developing countries, compared to developed countries. In this study, we aimed to investigate the risk factors for different wheezing phenotypes in Chinese young children and to explore the prognosis of recurrent wheezing.

Methods

Study design

Recruitment

This longitudinal cohort study was undertaken at the Childrenā€™s Hospital of the Capital Institute of Pediatrics, Beijing, China. FigureĀ 1 shows the flow of the study. During phase 1 (Oct 2013ā€“May 2014) a total of 109 participants were recruited at the asthma outpatient clinic during their wheezing exacerbation. The criteria of recruitment were aged from 6Ā months and up to 6Ā years old with 3 or more episodes of doctor-diagnosed wheezing. The exclusion criteria were: history of congenital pulmonary airway malformation, bronchopulmonary dysplasia, trachea cannula, severe pneumonia, severe immunodeficiency disease, and cardiovascular disease. The parents/guardians were asked to fill in a questionnaire for their children during the recruitment. Blood was taken to measure serum total and specific IgE (sIgE) and eosinophil (EOS) count in peripheral blood. Nasopharyngeal aspirate (NPA) specimens were collected to detect virus infection, which included the detection of RV, Human Metapneumovirus (hMPV), Bocavirus, respiratory syncytial virus (RSV), parainfluenza viruses type I, II and III (PIV), influenza types A and B (Flu).

Fig.Ā 1
figure 1

The flow chat of the study design: a total number of 109 participant were recruited at phase 1, with all of them having medical record, and virus infection test, but 45 and 73 of them had got serum IgE and EOS count tested. 85 of the participants had finished the telephone survey at follow-up stage

Full size image

Follow-up stage

Phase 2 (Octā€“Nov 2017) was the follow-up of the phase 1 cohort. A specialist physician at the asthma clinic conducted a telephone questionnaire survey on the childā€™s current wheezing status, etc.

This study was approved by the Ethics Committee of the Capital Institute of Pediatrics (SHERLL-2013072). All parents of the recruited children gave informed consent.

Questionnaire survey

The questionnaire at phase 1 captured baseline information on the childā€™s date of birth, gender, birth history, siblings, breastfed history, pets ownership (at birth, and current), mother and other family members smoking history, onset age of wheezing, past-year wheezing episodes, rhinitis history, eczema history and parental history of asthma.

The telephone questionnaire during phase 2 recorded the following items, [1] current wheezing: Wheezing episodes in the past 12Ā months, [2] history of doctor-diagnosed rhinitis and eczema after recruitment, and [3] current rhinitis and eczema: Symptoms of doctor-diagnosed rhinitis and eczema in the past 12Ā months.

Serum IgE and peripheral blood eosinophil count

Serum was isolated for total IgE and specific IgE (sIgE) measurements using the ImmunoCapā„¢ assays (Phadia, Sweden) on PhadiaĀ® 250 System (Thermo Fisher Scientific). Any sensitization was defined as positive sIgE results against common food allergens FX5 (egg white, cowā€™s milk, codfish, wheat, peanut, soybean), and aeroallergens: Phad, mould mix (MX1), and house dust mite (HDM: Der p, Der f) with cutoff level of 0.35 kU/L [10]. Peripheral blood eosinophil count was obtained from XN-1000ā„¢ Hematology Analyzer (Sysmex Corporation).

Virus infection detection

The NPA specimens were processed within 3Ā h after collection. RV, hMPV and Bocavirus were screened by a reverse transcription-polymerase chain reaction. Direct detection of viral antigens by fluoroimmunoassay was carried out using UItraTMDFA Respiratory Virus Screening & ID Kit (Diagnostic Hybrids, USA) for RSV, PIV type I, II and III, Flu types A and B.

Grouping strategy

After the telephone survey of phase 2, our participants were assigned into 3 groups according to the study of Martinez et al. [5]:

  1. 1.

    Transient wheezing group: wheezing symptom started and remitted before age 3.

  2. 2.

    Persistent wheezing group: wheezing symptom started before age 3-year and persisted until age 6 or after.

  3. 3.

    Late-onset wheezing group: wheezing symptom started after age 3.

Statistical analysis

Results of the continuous variables (normal distribution) were expressed as meanā€‰Ā±ā€‰SD. Non-normal distribution data were expressed as the median and inter-quartile range. The Mannā€“Whitney U test was utilized to compare the past-year wheezing episodes between recruitment and follow-up stages and the Kruskalā€“Wallis H test was used for comparing the current wheezing episodes and the onset age of wheezing between the three wheezing phenotype groups. Variance analysis was utilized for the three groupsā€™ comparison of EOS and logarithmic transformation of total serum IgE. Categorical variables were compared using Ļ‡2 test. If the expected values in any of the cells of the contingency table were below 5, Fisherā€™s exact test was used. Poisson regression was used to determine the incidence rate ratio (IRR) of current wheezing episodes at the follow up and its association with concomitant risk factors adjusted for the confounders. SPSS 17.0 was used for the statistical analysis and RStudio (Version 1.0.153) was used for creating figures.

Results

Characteristics of the participants and the wheezing status comparison

The average age of the 109 participants at the start of the study (phase 1) was 2.6ā€‰Ā±ā€‰2.3Ā year and 80 (73.4%) were males. At phase 2, 85 (78.0%) of the participantsā€™ parents completed the telephone survey, and 66 (77.6%) of these children were boys. Forty-three (50.6%) of the participants were initially recruited in spring, while 24 (28.2%) and 18 (21.2%) were recruited in autumn and winter, respectively. The demographic information are shown in TableĀ 1. There was no significant difference in the gender frequency, birth history, recruitment season, siblings, breastfed history, childcare, pet ownership, mother and other family member smoking history between the different wheezing phenotypes.

TableĀ 1 Patientsā€™ characteristics and wheezing episode
Full size table

The number of current wheezing episodes had decreased in all groups, including those with persistent and late onset wheezing (both of the pā€‰<ā€‰0.01) (Fig.Ā 2). However, there was no significant difference in current wheezing between the different phenotypes of wheezing groups, both at recruitment (pā€‰=ā€‰0.925) and the follow-up stage (pā€‰=ā€‰0.323) (TableĀ 1). Comparison of the onset age of wheezing showed that the transient wheezing group started earlier than the persistent wheezing group (pā€‰=ā€‰0.039).

Fig.Ā 2
figure 2

The current wheezing episodes comparison between recruitment and follow-up stages in three different phenotypes: Notched boxes showed the inter quartile ranges, lines inside the boxes represented medians, and dots were outliers

Full size image

Risk factors for the three different wheezing phenotypes

We have compared the risk factors between the three different wheezing phenotypes (TableĀ 2). The total virus infection rates were 42.9%, 51.9%, and 29.4% for the transient, persistent, and late-onset wheezing groups, respectively. The RV infection rate was the highest among the tested viruses in all three groups, followed by the RSV positive rate. Although there was no significant difference between the three wheezing phenotype groups, we did observe a trend that the RV and RSV infection rates were higher in the persistent wheezing group, and the overall infection rate appear the lowest in late-onset wheezing group.

TableĀ 2 The comparison of wheezing risk factors between the three wheezing phenotypes
Full size table

There was a significant difference for ā€˜rhinitis everā€™ between the three groups (pā€‰<ā€‰0.01). The rhinitis rates of the persistent and late-onset wheezing groups were both higher than the transit wheezing group (both pā€‰<ā€‰0.01). We found that the current rhinitis rate of the persistent wheezing and late-onset wheezing groups was also higher than transient wheezing group at the follow-up stage (pā€‰=ā€‰0.016, pā€‰=ā€‰0.011).

The total IgE of the transient wheezing group was significantly lower than the other two groups (pā€‰<ā€‰0.05). However, there was no significant difference of total IgE level between the persistent and late-onset wheezing groups. The prevalence of a positive specific IgE to aeroallergen was highest in the late-onset wheezing group, but no difference was observed in the prevalence of mould mix, house dust mite (HDM) and food allergen sIgE positive. Significant difference was detected for the percentage of EOS in peripheral blood (pā€‰=ā€‰0.045) between the three wheezing groups, with the highest EOS percentage in late-onset wheezing group.

The concomitant risk factors for the incidence of current wheezing episodes

The incidence of current wheezing episodes increased cumulatively if the participant had concomitant risk factors (TableĀ 3). The significance did not change after adjustment for the confounders we investigated in this study, including gender, birth history, number of siblings, breastfed history, childcare, pets ownership, mother and other family membersā€™ smoking history, onset wheezing age (months), past-year wheezing episode at recruitment and parental asthma history. Four confounders were finally included in the regression model. The incidence rate ratios (IRRs) of wheezing increased from with either rhinitis or RV infection (3.61, pā€‰<ā€‰0.01) to both (4.54, pā€‰=ā€‰0.01), compared to neither, respectively. The IRRs were also significantly high with either aeroallergens positive or RV infection (2.54, pā€‰=ā€‰0.05), and marginally significant with both (3.44, pā€‰=ā€‰0.07). In addition, children with both rhinitis and aeroallergens positive were 4.36-fold higher of IRR than children with none of the risk factors (pā€‰<ā€‰0.01). Poisson regression showed concomitant rhinitis and/or RV infection strongly indicated an increased risk of wheezing at the follow up and Fig.Ā 3 visualizes the overlapping characteristics of these two risk factors among the three different wheezing phenotypes. The overlap of rhinitis and RV infection was 14 (25.9%) in persistent wheezing group compared to 0 (0.0%) and 2 (11.8%) in the transient and late-onset wheezing groups, respectively.

TableĀ 3 The incidence rate ratios (IRRs) of concomitant risk factors for the incidence of current wheezing episodes
Full size table
Fig.Ā 3
figure 3

Patient numbers of wheezing phenotypes with sole and overlapping risk factors (RV and rhinitis): Venn diagrams were draw to show the concomitant of RV infection and rhinitis in the three different wheezing phenotypes

Full size image

Discussion

The prevalence of wheezing has been increasing recently in China [13] but the prognosis of recurrent wheezing during young age is unknown in developing countries. To the best of our knowledge, this is the first longitudinal study conducted in China that investigates the prognosis of recurrent wheezing in young children and identifies risk factors for different wheezing phenotypes.

The strength of our study is that it includes the comprehensive collection of medical records, viral etiology, serum IgE test, and EOS count at study entry, and is combined with a 3.5-year follow-up by an experienced asthma clinic specialist practitioner. We found that rhinitis and aeroallergen sensitization, either alone or together with early RV infection, were the most significant predictors for subsequent persistent and late onset wheeze in China. Previously, an observational study conducted in Turkey investigated the short-term prognosis and risk factors of recurrent wheezing in the first 3Ā years of life [14]. Maternal smoking during pregnancy and emergency room admissions were significant risk factors for the persistence of wheezing. A study in Mozambique by Oā€™Callaghan-Gordo et al. showed that an initial episode of lower respiratory infection (LRI) with RV during infancy could increase the risk of wheezing [15].

We found that the number of wheezing episodes had decreased significantly during the follow-up stage and the onset age of wheezing was earlier in the transient wheezing than in the persistent wheezing group. The findings are consistent with earlier studies from Martinez et al. [5] and Matricardi et al. [16] showing that the incidence of wheezing declined with age. The respiratory system gradually undergoes development with age which may be an important reason for the decrease in the number of wheezing episodes [17]. In addition, our findings echo the previous reports that the risk factors of wheezing also show phenotypic variability [18, 19]. A large population-based cohort in the UK showed that episodic viral wheeze decreased with age, but multiple trigger wheeze (mainly due to exercise or aeroallergen-associated wheeze) increased [20]. Martinez suggested that transient wheezing in young children is not associated with an atopic predisposition [21].

It is well known that respiratory tract virus infection is an important cause for early childhood wheezing and asthma [22]. Jackson et al. revealed that RV and RSV are the main viruses that cause wheezing, and RV infection can affect the long-term prognosis of children with wheezing [23]. Early life RV-induced wheezing can increase the asthma risk at school age [24]. We observed 37% of RV in children with persistent wheezing and less than 20% of RV in children with the other wheezing phenotypes, although these differences were not statistically different due to the relatively small sample size. To date, studies on the mechanisms of respiratory virus-induced wheeze in children has surged, driven by efforts to find better interventions to reduce wheezing exacerbations. A recent review recapitulated that RV type C was associated with a decrease in expression of a cellular receptor specific for this virus-CDHR3, and a decrease in interferon-Ī² expression [25]. The shift to focus on the mechanisms and new intervention methods is promising.

Allergic rhinitis (AR) is often associated with asthma and asthma is present in 15% to 38% of the patients with AR, and nasal symptoms are found in 6% to 85% patients with asthma [26]. Indeed we found that the incidence of rhinitis ever and current rhinitis were more common in the persistent and late-onset wheezing groups compared to the transient wheezing group. The sIgE results showed that a positive allergy response to aeroallergens was lower in the transient wheezing groups. Serum IgE levels has long been associated with asthma and allergic sensitization is an independent predictor for the persistence of wheezing [27, 28]. Interestingly, when we analyzed the concomitant risk factors we found that the increase of wheezing episodes in the year preceding follow up was associated with overlapping RV and/or rhinitis, RV and/or aeroallergens sensitization, rhinitis and aeroallergens sensitization. This confirms RV, aeroallergens and rhinitis, more likely working together are dominant risk factors for persistent wheezing in China. As noted above, this constellation of risk factors closely resembles those reported for developed countries, despite the fact that as a developing country China has different social/economic contexts and lower allergy prevalence compared to industrialized countries.

In this regard, a community-based birth cohort study demonstrated that viral infections interact with atopic sensitization in infancy to enhance the susceptibility to asthma development and the occurrence of both of the two factors is associated with maximal risk for subsequent asthma [29]. Jackson and colleagues also showed that asthma rate was highest in infants with both sensitization and RV-related wheezing, but RV-related wheezing was the most significant predictor of subsequent asthma in the Childhood Origins of ASThma (COAST) study [8]. Consistently, a recent cohort study revealed that first RV-induced wheezing alone or together with sensitization could predict atopic school-aged asthma [10]. Notably, in our result, children in persistent and late-onset wheezing groups are approximately equivalently ā€œatopicā€ relative to the children in transient wheezing group. We speculate that the reason why onset of asthma is faster in the persistent wheezing group is because the early impact of viral infections on them was higher, whereas it took longer time for the late-onset wheezing group to accumulate enough viral-associated tissue damage to catch up and start expressing symptoms. On the other hand, we suggest that the late-onset wheezing group could be driven by atopy alone and in the absence of high level viral infection, it takes longer for lung function to deteriorate. However, the wheezing symptom in transient wheezing group is simple and mainly due to the congenitally smaller airways not being able to manage viral inflammation and children in this group grow out of that because they donā€™t have the ā€œsecond hitā€ from atopy.

This study has limitations that should be taken into account. Firstly, we acknowledge the small sample size of this study. Nonetheless, the conclusion should be interpreted with caution. Secondly, not all the participants had serum IgE and EOS count measured at recruitment. This is because that not all patients were covered by health insurance for serum IgE test due to policy (e.g. outpatient clinic attendance in non-local tertiary hospitals). However, this novel Chinese cohort provided insights into the risk factors and prognosis of early life wheezing in an eastern environment. The focus for future researches should be larger, preferably multicentre, study cohorts with extensive follow-up to elucidate the risk factors in the development of asthma in children living in developing countries.

In conclusion, we show that while the incidence of wheezing declined overall with age, but in addition to transient wheezers, additional subsets of children manifest persistent wheeze or late onset wheeze, and moreover the risk factors for wheezing display phenotypic variability between these subgroups. Rhinitis ever and aeroallergens sensitization, either alone or together with previous RV infection, were the most significant predictors for persistent wheezing in children in China.

Availability of data and materials

The data that support the findings of this study are not publicly available due to the undergoing of more analysis, but are available from the corresponding author upon reasonable request.

Abbreviations

RV:

rhinovirus

RSV:

respiratory syncytial virus

hMPV:

human metapneumovirus

PIV:

parainfluenza virus

Flu:

influenza

EOS:

eosinophil

IRR:

incidence rate ratio

HDM:

house dust mite

LRI:

lower respiratory infection

AR:

allergic rhinitis

References

  1. Soh JE, Kim KM, Kwon JW, Kim HY, Seo JH, Kim HB, et al. Recurrent wheeze and its relationship with lung function and airway inflammation in preschool children: a cross-sectional study in South Korea. BMJ Open. 2017;7(10):e018010.

    ArticleĀ  Google ScholarĀ 

  2. Sears MR. Predicting asthma outcomes. J Allergy Clin Immunol. 2015;136(4):829ā€“36.

    ArticleĀ  Google ScholarĀ 

  3. Grad R, Morgan WJ. Long-term outcomes of early-onset wheeze and asthma. J Allergy Clin Immunol. 2012;130(2):299ā€“307.

    ArticleĀ  Google ScholarĀ 

  4. Savenije OE, Kerkhof M, Koppelman GH, Postma DS. Predicting who will have asthma at school age among preschool children. J Allergy Clin Immunol. 2012;130(2):325ā€“31.

    ArticleĀ  Google ScholarĀ 

  5. Martinez FD, Wright AL, Taussig LM, Holberg CJ, Halonen M, Morgan WJ. Asthma and wheezing in the first six years of life. The Group Health Medical Associates. N Engl J Med. 1995;332(3):133ā€“8.

    ArticleĀ  CASĀ  Google ScholarĀ 

  6. Rodriguez-Martinez CE, Sossa-Briceno MP, Castro-Rodriguez JA. Factors predicting persistence of early wheezing through childhood and adolescence: a systematic review of the literature. J Asthma Allergy. 2017;10:83ā€“98.

    ArticleĀ  Google ScholarĀ 

  7. Kusel MM, Kebadze T, Johnston SL, Holt PG, Sly PD. Febrile respiratory illnesses in infancy and atopy are risk factors for persistent asthma and wheeze. Eur Respir J. 2012;39(4):876ā€“82.

    ArticleĀ  CASĀ  Google ScholarĀ 

  8. Jackson DJ, Gangnon RE, Evans MD, Roberg KA, Anderson EL, Pappas TE, et al. Wheezing rhinovirus illnesses in early life predict asthma development in high-risk children. Am J Respir Crit Care Med. 2008;178(7):667ā€“72.

    ArticleĀ  Google ScholarĀ 

  9. Lemanske RF Jr, Jackson DJ, Gangnon RE, Evans MD, Li Z, Shult PA, et al. Rhinovirus illnesses during infancy predict subsequent childhood wheezing. J Allergy Clin Immunol. 2005;116(3):571ā€“7.

    ArticleĀ  Google ScholarĀ 

  10. Lukkarinen M, Koistinen A, Turunen R, Lehtinen P, Vuorinen T, Jartti T. Rhinovirus-induced first wheezing episode predicts atopic but not nonatopic asthma at school age. J Allergy Clin Immunol. 2017;140(4):988ā€“95.

    ArticleĀ  Google ScholarĀ 

  11. Mallol J, Crane J, von Mutius E, Odhiambo J, Keil U, Stewart A, et al. The international study of asthma and allergies in childhood (ISAAC) phase three: a global synthesis. Allergol Immunopathol. 2013;41(2):73ā€“85.

    ArticleĀ  CASĀ  Google ScholarĀ 

  12. Chen YZ, National Cooperation Group On Childhood Asthma China. Third nationwide survey of childhood asthma in urban areas of China. Zhonghua er ke za zhi Chinese J Pediatrics. 2013;51(10):729ā€“35.

    Google ScholarĀ 

  13. Liu CH, Hong JG, Shang YX, Sun J, Duolikun M, Shan MN, et al. Comparison of asthma prevalence in children from 16 cities of China in 20 years. Chin J Pract Pediatr. 2015;30(8):596ā€“600.

    CASĀ  Google ScholarĀ 

  14. Sahiner UM, Buyuktiryaki B, Cavkaytar O, Arik Yilmaz E, Soyer O, Sackesen C, et al. Recurrent wheezing in the first three years of life: short-term prognosis and risk factors. J Asthma. 2013;50(4):370ā€“5.

    ArticleĀ  Google ScholarĀ 

  15. Oā€™Callaghan-Gordo C, Bassat Q, Diez-Padrisa N, Morais L, Machevo S, Nhampossa T, et al. Lower respiratory tract infections associated with rhinovirus during infancy and increased risk of wheezing during childhood. A cohort study. PLoS ONE. 2013;8(7):e69370.

    ArticleĀ  Google ScholarĀ 

  16. Matricardi PM, Illi S, Gruber C, Keil T, Nickel R, Wahn U, et al. Wheezing in childhood: incidence, longitudinal patterns and factors predicting persistence. Eur Respir J. 2008;32(3):585ā€“92.

    ArticleĀ  CASĀ  Google ScholarĀ 

  17. Fu L, Freishtat RJ, Gordish-Dressman H, Teach SJ, Resca L, Hoffman EP, et al. Natural progression of childhood asthma symptoms and strong influence of sex and puberty. Ann Am Thorac Soc. 2014;11(6):939ā€“44.

    ArticleĀ  Google ScholarĀ 

  18. Caudri D, Savenije OE, Smit HA, Postma DS, Koppelman GH, Wijga AH, et al. Perinatal risk factors for wheezing phenotypes in the first 8Ā years of life. Clin Exp Allergy. 2013;43(12):1395ā€“405.

    ArticleĀ  CASĀ  Google ScholarĀ 

  19. Kutzora S, Weber A, Heinze S, Hendrowarsito L, Nennstiel-Ratzel U, von Mutius E, et al. Asthmatic/wheezing phenotypes in preschool children: influential factors, health care and urbanā€“rural differences. Int J Hyg Environ Health. 2018;221(2):293ā€“9.

    ArticleĀ  Google ScholarĀ 

  20. Jurca M, Pescatore AM, Goutaki M, Spycher BD, Beardsmore CS, Kuehni CE. Age-related changes in childhood wheezing characteristics: a whole population study. Pediatr Pulmonol. 2017;52(10):1250ā€“9.

    ArticleĀ  Google ScholarĀ 

  21. Martinez FD. Role of respiratory infection in onset of asthma and chronic obstructive pulmonary disease. Clin Exp Allergy. 1999;29(Suppl 2):53ā€“8.

    PubMedĀ  Google ScholarĀ 

  22. Holt PG, Strickland DH, Sly PD. Virus infection and allergy in the development of asthma: what is the connection? Curr Opin Allergy Clin Immunol. 2012;12(2):151ā€“7.

    ArticleĀ  CASĀ  Google ScholarĀ 

  23. Jackson DJ, Evans MD, Gangnon RE, Tisler CJ, Pappas TE, Lee WM, et al. Evidence for a causal relationship between allergic sensitization and rhinovirus wheezing in early life. Am J Respir Crit Care Med. 2012;185(3):281ā€“5.

    ArticleĀ  Google ScholarĀ 

  24. Rubner FJ, Jackson DJ, Evans MD, Gangnon RE, Tisler CJ, Pappas TE, et al. Early life rhinovirus wheezing, allergic sensitization, and asthma risk at adolescence. J Allergy Clin Immunol. 2017;139(2):501ā€“7.

    ArticleĀ  Google ScholarĀ 

  25. Le Souef P. Viral infections in wheezing disorders. Eur Respir Rev. 2018;27:147.

    ArticleĀ  Google ScholarĀ 

  26. Brozek JL, Bousquet J, Agache I, Agarwal A, Bachert C, Bosnic-Anticevich S, et al. Allergic rhinitis and its impact on asthma (ARIA) guidelinesā€”2016 revision. J Allergy Clin Immunol. 2017;140(4):950ā€“8.

    ArticleĀ  Google ScholarĀ 

  27. Martinez FD, Stern DA, Wright AL, Taussig LM, Halonen M. Differential immune responses to acute lower respiratory illness in early life and subsequent development of persistent wheezing and asthma. J Allergy Clin Immunol. 1998;102(6 Pt 1):915ā€“20.

    ArticleĀ  CASĀ  Google ScholarĀ 

  28. Kusel MM, de Klerk NH, Kebadze T, Vohma V, Holt PG, Johnston SL, et al. Early-life respiratory viral infections, atopic sensitization, and risk of subsequent development of persistent asthma. J Allergy Clin Immunol. 2007;119(5):1105ā€“10.

    ArticleĀ  Google ScholarĀ 

  29. Holt PG, Rowe J, Kusel M, Parsons F, Hollams EM, Bosco A, et al. Toward improved prediction of risk for atopy and asthma among preschoolers: a prospective cohort study. J Allergy Clin Immunol. 2010;125(3):653ā€“9.

    ArticleĀ  Google ScholarĀ 

Download references

Acknowledgements

We sincerely thank Prof. Peter Le Souƫf (School of Paediatrics and Child Health, the University of Western Australia) for his assistance of the questionnaire design.

Funding

This research was supported by Special Scientific Research Fund of Public Welfare Profession of China from National Health and Family Planning Commission of the PRC [Grant Number 201502025] and Key Medical Specialty Development Plan of Beijing Hospital Administration [ZYLX201829].

Author information

Authors and Affiliations

  1. Department of Allergy, Childrenā€™s Hospital of Capital Institute of Pediatrics, Beijing, China

    Jing Guo,Ā Wenjing Zhu,Ā Huimin WangĀ &Ā Chuanhe Liu

  2. School of Public Health, Curtin University, Perth, Australia

    Jing GuoĀ &Ā Guicheng Zhang

  3. The Curtin UWA Centre for Genetic Origins of Health and Disease, Faculty of Health and Medical Sciences, Curtin University, The University of Western Australia, Perth, Australia

    Jing GuoĀ &Ā Guicheng Zhang

  4. Telethon Kids Institute, University of Western Australia, Perth, Australia

    Patrick G. Holt

Authors
  1. Jing Guo
    View author publications

    You can also search for this author in PubMedĀ Google Scholar

  2. Wenjing Zhu
    View author publications

    You can also search for this author in PubMedĀ Google Scholar

  3. Huimin Wang
    View author publications

    You can also search for this author in PubMedĀ Google Scholar

  4. Patrick G. Holt
    View author publications

    You can also search for this author in PubMedĀ Google Scholar

  5. Guicheng Zhang
    View author publications

    You can also search for this author in PubMedĀ Google Scholar

  6. Chuanhe Liu
    View author publications

    You can also search for this author in PubMedĀ Google Scholar

Contributions

JG and CL contributed to the study design, data analysis and interpretation, and drafting and revising the manuscript. WZ and HW contributed to the study design, recruitment, and data acquisition. PGH and GZ contributed to the data analysis, interpretation, and critical revision of the manuscript. All authors read and approved the final manuscript.

Corresponding author

Correspondence to Chuanhe Liu.

Ethics declarations

Ethics approval and consent to participate

This study was approved by the Ethics Committee of the Capital Institute of Pediatrics (SHERLL-2013072). All parents of the recruited children gave informed consent.

Competing interests

The authors declare that they have no competing interests.

Additional information

Publisher's Note

Springer Nature remains neutral with regard to jurisdictional claims in published maps and institutional affiliations.

Rights and permissions

Open Access This article is distributed under the terms of the Creative Commons Attribution 4.0 International License (http://creativecommons.org/licenses/by/4.0/), which permits unrestricted use, distribution, and reproduction in any medium, provided you give appropriate credit to the original author(s) and the source, provide a link to the Creative Commons license, and indicate if changes were made. The Creative Commons Public Domain Dedication waiver (http://creativecommons.org/publicdomain/zero/1.0/) applies to the data made available in this article, unless otherwise stated.

Reprints and permissions

About this article

Check for updates. Verify currency and authenticity via CrossMark

Cite this article

Guo, J., Zhu, W., Wang, H. et al. Risk factors and prognosis of recurrent wheezing in Chinese young children: a prospective cohort study. Allergy Asthma Clin Immunol 15, 38 (2019). https://doi.org/10.1186/s13223-019-0351-4

Download citation

  • Received:

  • Accepted:

  • Published:

  • DOI: https://doi.org/10.1186/s13223-019-0351-4

Keywords

Allergy, Asthma & Clinical Immunology

ISSN: 1710-1492

Contact us