Predictors of Repeated Wheeze in the First Year of Life . The Relative Roles of Cockroach, Birth Weight, Acute Lower Respiratory Illness, and Maternal Smoking

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Predictors of Repeated Wheeze in the First Year of Life
The Relative Roles of Cockroach, Birth Weight, Acute Lower Respiratory Illness, and Maternal Smoking

DIANE R. GOLD, HARRIET A. BURGE, VINCENT CAREY, DONALD K. MILTON, THOMAS PLATTS-MILLS, and SCOTT T. WEISS

Channing Laboratory, Department of Medicine, Brigham and Women's Hospital and the Harvard Medical School; Departments of Environmental Health, Environmental Science and Engineering, and Occupational Health Programs, Harvard School of Public Health, Boston, Massachusetts; and Division of Asthma, Allergy, and Immunology, Department of Medicine, University of Virginia, Charlottesville, Virginia

ABSTRACT

TOP
ABSTRACT
INTRODUCTION
METHODS
RESULTS
DISCUSSION
REFERENCES

While more than 80% of childhood asthmatics are allergic to one or more inhaled allergens, the role of inhaled allergens inthe induction of wheeze in the first year of life is unknown.In a prospective birth-cohort study of 499 children of asthmatic/allergicparents from metropolitan Boston, we examined home allergen concentrationsmeasured within the first 3 mo of life as predictors of repeatedwheeze episodes in the first year of life. In multivariate analysesadjusting for maternal asthma and dog in the home, predictorsof two or more wheeze episodes in the first year of life includedmaternal smoking during pregnancy (relative risk [RR] = 1.83;95% confidence limit [CL]: 1.12, 3.00), lower respiratory illnessin the first year of life (croup, bronchitis, bronchiolitis, orpneumonia) (RR = 2.25; 95% CL:1.58, 3.19), low birthweight (RR= 1.28, 95% confidence interval [CI]: 1.04, 1.58 for an interquartiledifference), and Bla g 1 or 2 (cockroach) allergen level in thefamily room > 0.05 U/g dust (RR = 1.76; 95% CL: 1.20, 2.57). Cockroachallergen in the family room and repeated wheeze remained significantafter adjustment for socioeconomic factors including race andincome (RR = 1.63; 95% CL: 1.05, 2.55). It is unknown whetherthe association between cockroach and repeated wheeze in infancyrepresents a cockroach-related increased risk of bronchial inflammationthrough nonallergenic or allergenicmechanisms.

	INTRODUCTION

TOP ABSTRACT INTRODUCTION METHODS RESULTS DISCUSSION REFERENCES

the cockroach lives

in peace and plenty

while the human race

hustles to support him

all the social institutions

of all time have existed

for the purpose

of forming a pyramid

on the apex of which

perches the cockroach triumphant

it has taken us a long

time but we point

with pride to the achievement

archy the cockroach (from Don Marquis, the lives and time of archy and mehitabel. Doubleday & Company, Inc., New York,1940).

More than 80% of childhood asthmatics are allergic to one or more inhaled allergens. Recent studies suggest that two-thirdsof childhood asthma cases in the United States are diagnosed by5 yr of age (1). Repeated or persistent wheeze is the chiefsymptom leading to doctor-diagnosed asthma, yet not all childrenwho wheeze are allergic, nor are they necessarily destined tobecome asthmatic. Particularly in the first year of life, childrenwith relatively small airways may develop airway inflammationand symptoms of wheeze in response to viral illnesses, yet maynot develop allergy or persistent wheeze that lasts beyond thefirst year of life (2).

A few prospective studies suggest an association between allergen exposure in the first year of life and subsequent developmentof specific allergic sensitization and asthma. In a cohort of67 British children with a parental history of asthma or hay fever,the relative risk of asthma at age 11 was 4.8 for those childrenexposed in the first year of life to more than 10 µg of Der p1 (dust mite allergen) per gram of dust (3). The age at whichthe first episode of wheezing occurred was inversely related tothe level of allergen measured in the first year of life. Wasthe association between early infancy allergen exposure and subsequentexpression of asthma significant by age 11 and not earlier becausethe study had insufficient power to detect earlier associations?Or is there a relatively long lag between exposure and subsequentdiseaseexpression?

Well documented predictors of wheeze in the first year of life include maternal smoking during pregnancy (4, 5), lowbirth weight, prematurity (6), and lower respiratory infections(7). Socioeconomic status and race/ethnicity are also strongpredictors of early childhood wheeze (8, 9), but these factorsmay, in part, be indicators of as yet poorly defined environmentalexposures, including allergenexposure.

In a birth cohort of children of parents with asthma or allergy, we tested the hypothesis that, even after the effects ofthese other predictors of early wheeze are taken into account,home allergen levels measured within the first 3 mo of an infant'slife predict repeated wheeze episodes in the first year oflife.

	METHODS

TOP ABSTRACT INTRODUCTION METHODS RESULTS DISCUSSION REFERENCES

Study Cohort

Participants were part of a metropolitan Boston prospective birth cohort study designed to examine relationships between exposureto indoor allergens and the development of allergic sensitizationand asthma. The 505 infants (including six sets of twins) andtheir 499 families with a history of asthma or allergy in at leastone parent were recruited between September 1994 and June 1996.Monday through Friday, all mothers who delivered at a large Bostonhospital were approached for screening within 24 to 48 h afterdelivery if they lived within Route 128 (encircling the metropolitanarea), were $>=$ 18 yr old, and were able to speak English or Spanish.To reduce the chance of prematurity or respiratory distress syndromeas a potential confounder, families were not screened if the childwas < 36 wk of gestation, had a major congenital anomaly, or wasin the neonatal intensive care unit. Mothers were asked: (1) Haveyou ever had a doctor's diagnosis of asthma, hay fever, or allergies?(2) Has the biological father of your child ever had a doctor'sdiagnosis of asthma, hay fever, or allergies? Women who answeredyes to any of these questions were asked to complete a screeningquestionnaire. One month after birth, a questionnaire regardingthe child's health was administered by telephone to families whohad initially expressed interest in participating in the studyand who fit the inclusion criteria. At 1 mo, parents who expressedplans to move or lack of interest in the study were also excluded.Of the 1,405 families initially screened, 906 were excluded fromthe study before the first home visit. Reasons for exclusion werereluctance to participate in a longitudinal study (51% of thoserefusing), plans to move within 1 yr (39%), early loss to follow-up(9%), and other (1%). Mothers gave consent for screening; at thetime of the first home visit, when the index child was 2 to 3mo of age, they gave consent for participation in the longitudinalstudy. Every 2 mo the primary caregiver was asked a follow-uptelephone questionnaire regarding respiratory symptoms and illnessesin the index child; changes in infant feeding and select homecharacteristics were alsorecorded.

Home Visit and Dust Collection

At the home visit, questionnaires regarding home characteristics, home environmental exposures (including smoking) and demographicand socioeconomic characteristics of the family were administeredby trained research assistants. Methods used for the collectionof dust samples and the processing and assay of allergens in thisstudy have been detailed previously (10). In brief, four separatedust samples were collected in standardized fashion by vacuumingthe following areas: (1) the baby's bedroom floor, (2) the baby'sbed, (3) the parent's bed (if the child slept there $>=$ 50% of thetime), (4) the family/living room chair or sofa most commonlyused by the caregiver when holding or feeding the infant as wellas the family room floor around the chair or sofa and in high-trafficareas, and (5) the kitchen floor. If a rug was present in anyof the rooms, half of the time was devoted to sampling therug.

Dust Extraction and Allergen Analysis

Dust extract was assayed for allergens including house dust mite (Der p 1, Der f 1), cat (Fel d 1), and cockroach (Bla g 1,Bla g 2). Two-site monoclonal antibody (MAB) immunoassays forDer p 1, Der f 1, and Fel d 1, and MAB/polyclonal immunoassaysfor Bla g 1 and Bla g 2 were used (10). Allergen concentrationswere reported as micrograms per gram (µg/g) of dust except forBla g 1 and 2 which were reported as units/gram (U/g) of dust.When limited dust was available from the bed, bedroom floor, orfamily room, Der f 1 (more prevalent than Der p in Boston) wasanalyzed first, and the remaining extract was then analyzed forDer p 1, Fel d 1, and Bla g 1, in that order. A limited numberof assays for Bla g 2 were performed in locations other than thekitchen. In the kitchen Bla g 1 was analyzed first and then (inorder) Bla g 2, Fel d 1, Der f 1, and finally Der p1.

Definition of Predictor Variables

The race/ethnicity of the child was defined according to parental self-reporting of race/ethnicity, which was considered asa socioeconomic factor. If either parent was black, the childwas defined as being black; if no parent was black but a parentwas Hispanic, the child was defined as being Hispanic; if no parentwas black or Hispanic but a parent was Asian, the child was definedas being Asian; children with two white parents were defined asbeing white. Zip code boundaries were used to define the levelsof poverty in areas within the greater Boston vicinity. The percentof the population below the poverty level was determined for eachof the zip code areas (based on data from the 1990 U.S. Census).Zip code areas were then combined to form three poverty area categories:low (less than 5% of individuals below the poverty level, basedon 1990 U.S. Census data), medium (5-20% of individuals belowthe poverty level), and high (> 20% of individuals below the povertylevel). Parental asthma was considered active if the parent hada report of wheeze in the past year. Smoking variables consideredincluded: maternal smoking during pregnancy; maternal smokingduring pregnancy or the first year of the child's life; currentmaternal smoking reported at the home visit; and total numberof cigarettes smoked in the home reported at the home visit. Seasonof birth was defined as winter (December-February), spring (March-May),summer (June-August), or fall (September-November). Birth weightand head circumference were considered both as continuous andas categorical variables. Any breast-feeding and number of monthsof breast-feeding (0 to < 2, 2 to < 8, 8 to $=<$ 12) in the first12 mo were considered as predictor variables. Lower respiratoryillness was defined as doctor diagnosed croup, bronchitis, bronchiolitis,or pneumonia. Furry/feathered pets were defined as pet hamsters,pet mice, other furry pets other than cats and dogs, andbirds.

As in previous analyses, allergen concentrations were grouped in categories with potential relevance to sensitization anddevelopment of allergy-related repeated wheeze (13). The maximalconcentration in the home and the specific room concentrations(bed, bedroom floor, living room, and kitchen) were assessed aspredictors of repeated wheeze to determine whether location influencedthe magnitude or strength of association between the allergenandwheeze.

Dust mite exposure was categorized as Der f 1 or Der p 1 at the following levels: (1) $>=$ 10 µg/g (including concentrationsexceeding detectable limits); (2) 2 to < 10 µg/g; (3) 0.05 to< 2 µg/g; and (4) < 0.05 µg/g (including assays "below the limitsof detection"). Those samples with "no dust" in the bed, bedroomfloor, and living room were also assigned to category (4) becauseif any dust was available, the measure of dust mite concentrationwas first priority. The correlation between dust mite concentrationper unit area and per unit mass in 484 living room samples was0.98, also supporting the assumption that homes with no dust wouldhave levels < 0.05 µg/g. We also checked whether exclusion of"no dust" from category 4 significantly altered the analyticresults.

Cockroach exposure was categorized as Bla g 1 or Bla g 2 at the following levels: (1) $>=$ 2 U/g (including concentrations exceedingdetectable limits); (2) 0.05 to < 2 U/g; (3) < 0.05 U/g (includingconcentrations below the limits of detection). Samples with nodust available for Bla g assay were assigned to a separate category(4) given that if any dust was available, measurement of cockroachantigens was not first priority except in the kitchen. Cat exposurewas categorized as Fel d 1 at the following levels: (1) $>=$ 8 µg/g(including concentrations exceeding detectable limits); (2) $>=$ 1 to < 8 µg/g; (3) < 1 µg/g (including concentrations below thelimits of detection), and (4) no dust available. A combined variablemeasuring Fel d 1 concentrations in either the bedroom bed orbedroom floor was created to represent bedroom exposure becausethe result was fewer cases in which "no dust" was available forthe assay. Dog allergen exposure, measured only in the livingroom, was categorized as Can f 1 at the following levels: (1) $>=$ 200 µg/g; (2) 20 to < 200 µg/g; and (3) < 20 µg/g.

Definition of Outcome Variables

Every 2 mo the primary caregiver (usually the mother) was asked, "Since we last spoke with you on (date given), has your childhad symptoms of wheeze?" The primary categorical outcome variablewas two or more reports of wheeze in the first year of life comparedwith fewer than two. Any wheeze versus no wheeze report and twoor more reports of wheeze versus no wheeze report were also examinedfor their relationship to exposure. Because the symptom questionnairewas scheduled to be administered when the index child was 1, 2,3, 4, 6, 8, 10, and 12 mo of age, there were potentially sevenquestionnaires per child. Of the 505 children, 94.5% had a completedata set and 97% had their 12-mo questionnaire completed; thesechildren were included in the analysis. Of the 14 children missingtheir 12-mo questionnaire, three had a 10-mo and a 14-mo questionnaireand two children had a 10-mo questionnaire; their data were includedin the analyses. Because their repeated wheeze (outcome) classificationwas known, three children with two or more reports of wheeze wereincluded despite missing wheeze information from Months 10 through14. Thus six children were excluded from theanalysis.

Statistical Methods

SAS statistical software (SAS Institute, Inc., Cary, NC) was used to evaluate univariate and multivariate associations betweenpredictor variables and wheeze. Univariate associations betweencategorical predictor variables and two or more episodes of wheezewere examined with 2 × 2 contingency tables; the logit methodwas used to calculate relative risk for a cohort. Log relativerisk parameters were estimated directly (not approximated by thelog odds ratio) with use of SAS PROC GENMOD (SAS Institute, 1997),with log link and binomial variancefunction.

Variables were chosen for the multivariate models because they entered into both forward and backward stepwise logistic regressionat a level of p $=<$ 0.1, estimating odds ratios rather than relativerisks, since these procedures were not practically applicableto relative risk estimation. Because odds ratio estimations uniformlyresulted in a slight overestimation of the magnitude and precisionof risk, somewhat more variables were included in final modelsestimating relative risk. Socioeconomic variables (race/ethnicity,income, area) were considered because they were potential confoundersof the relationship between cockroach allergen level and repeatedwheeze.

	RESULTS

TOP ABSTRACT INTRODUCTION METHODS RESULTS DISCUSSION REFERENCES

Wheeze Experience

Of the 499 children, 288 (58%) never wheezed, 115 (23%) had a report of wheeze in only one questionnaire, 55 (11%) had reportsof wheeze in two questionnaires, 25 (5%) had reports of wheezein three questionnaires, and 16 (3%) had reports of wheeze inmore than three questionnaires in the first year of life. Of thosewho had two or more reports of wheeze in the first year of life,43% had their first wheeze episode within the first 2 to 3 moof life, but only one child had both episodes in that earlyperiod.

Cohort Characteristics as Wheeze Predictors: Univariate Analyses

Tables 1 and 2 show the cohort characteristics and their univariate relationship to two or more wheeze reports. Boys didnot have a higher risk than girls of two or more reports of wheeze.Multiple wheeze reports were higher among children of black, Hispanic,and "other" backgrounds than among those whose parents were bothwhite. Maternal history of asthma was a stronger predictor ofmultiple wheeze reports than paternal history of asthma. Childrenof asthmatic mothers with current wheeze had a higher risk ofmultiple wheeze reports than children of asthmatic mothers withoutcurrent wheeze.

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TABLE 1

UNIVARIATE PREDICTORS OF TWO OR MORE REPORTS OF WHEEZE IN THE FIRST YEAR OF LIFE: HEREDITARY, PRENATAL, AND PERINATAL FACTORS

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TABLE 2

UNIVARIATE PREDICTORS OF TWO OR MORE REPORTS OF WHEEZE IN THE FIRST YEAR OF LIFE: NUTRITIONAL, INFECTIOUS, AND SOCIOECONOMIC FACTORS

Children in the lowest quartile for birth weight had a significantly higher risk of multiple wheeze reports than childrenin the highest quartile, despite the narrow range of birth weightthat resulted from the selection of children who were not prematureand who did not require placement in the neonatal intensive careunit. Children in the lowest quartile for head circumference hada greater risk of multiple wheeze than those in the highest quartile.Analyses regarding head circumference were somewhat limited becauseof missing data. The relationship between maternal age and multiplewheeze reports was not linear; children whose mothers were inthe highest and lowest quartiles were more likely to have multiplewheeze reports than children of mothers in the midrange forage.

Children born in the winter had a lower rate of multiple wheeze reports than those born in the spring, summer, or fall. Childrenborn in the fall were at greatest risk forwheeze.

Maternal smoking during pregnancy, which was reported at low rates, was a strong predictor of multiple wheeze reports. Inclusionof paternal smoking or other sources of passive smoke exposurein the household did not add to the predictive power of maternalsmoking duringpregnancy.

Children of mothers who breast-fed (Table 2) had a somewhat lower risk of multiple wheeze episodes, though this associationdid not remain significant in multivariate analyses. Various socioeconomicfactors were associated with a higher risk of multiple wheezereports including residence in an area of Boston in which 20%or more of households were below the poverty level and an incomeof less than $30,000. Minority participants were overrepresentedamong socioeconomically disadvantaged studyparticipants.

The strongest predictor of multiple wheeze episodes was lower respiratory illness (Table 2), with or without bronchiolitis.However 51% of children with both lower respiratory illness andrepeated wheeze had wheeze in months before their first reportof lower respiratory illness (croup, bronchitis, bronchiolitis,orpneumonia).

Can f 1, Fel d 1, and Reports of Animals as Predictors of Wheeze

The presence of Can f 1 concentrations of > 200 µg/g of dust in the living room and the reported presence of a dog in thehousehold were both associated with increased risk of multiplereports of wheeze, with estimates of similar magnitude (Table3). The relatively small number of living room samples assayedfor Can f 1 likely reduced the precision of the estimate for theactual allergen concentrations as compared with the precisionof the estimate for the association between the presence of adog in the household and wheeze. Neither Fel d 1 concentrationsnor the reported presence of a cat in the household predictedmultiple wheeze episodes. Mouse or rat allergen levels were notmeasured, but households with other furry/ feathered pet animalsor households in which wild mice or rats had been seen tendedto have a higher univariate risk of multiple wheeze reports inthe children. Of the 15 homes with other furry/feathered pet animals,six had dogs, resulting in collinearity between the two variables;multivariate analyses focused on associations between dog andwheeze, because of the specificity of the exposure, the largernumbers, and the corroborative allergen data.

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TABLE 3

UNIVARIATE PREDICTORS OF TWO OR MORE REPORTS OF WHEEZE IN THE FIRST YEAR OF LIFE: CAT ALLERGEN (Fel d 1), DOG ALLERGEN (Can f 1), AND REPORTS OF ANIMAL EXPOSURE

Cockroach Allergen (Bla g 1 or 2) and Dust Mite Allergen (Der f 1 or Der p 1) as Predictors of Wheeze

In each tested site in the home (child's bedroom bed and floor, family room, and kitchen), the presence of cockroach allergenlevels predicted two or more episodes of wheeze in the children(Table 4). The magnitude of the relationship was highest forcockroach allergen measured in the bed. Compared with homes withno detectable cockroach allergen, the univariate data suggesteda possible dose response, with a relative risk (RR) of 3.68 (95%confidence interval [CI]: 1.50, 9.02) for an exposure level of $>=$ 2 U/g and RR of 2.59 (95% CI: 1.21, 5.56) for exposure levelbetween 0.05 and 2 U/g. The estimated risk of wheeze when Blag concentrations were $>=$ 2 U/g on the bedroom floor was slightlylower than for comparable levels in the bed, with a similar suggestionof dose response. Whereas many more homes had cockroach allergenlevels of $>=$ 2 U/g in the kitchen than had such concentrationsin the bedroom (bed or floor), the magnitude and strength of theunivariate association with wheeze were smaller. In univariateanalyses, compared with Bla g concentrations of < 0.05 U/g, theRR of two or more episodes of wheeze was 1.79 (95% confidencelimit [CL]: 1.06, 3.00) if the maximal concentration in the homewas > 2 U/g (n = 62). The estimate for the risk of two or moreepisodes of wheeze with exposure to family room Bla g concentrationsof > 0.05 U/g (combining the categories $>=$ 2 and $>=$ 0.05 to < 2)was found to be the most precise and representative estimate ofcockroach effect in multivariate analyses (Table 5), becauseof the small numbers of missing ("no dust available") data, becauseof the large numbers exposed, and because of the lack of strongcollinearity between socioeconomic factors and exposure. The maximalBla g concentrations in the family room were more modest thanthose in the kitchen, but were still at levels generally associatedwith overt cockroach infestation. For the family room categoryBla g 0.05 to < 2 U/g, the median value was 0.32 U/g with a rangeof 0.05 to 1.6 U/g. For the category Bla g $>=$ 2 U/g, the medianfamily room value was 7.8 U/g (range 2.0 to 29 U/g), comparedwith a median bed value of 3.0 U/g (range 2.0 to 31 U/g), a medianbedroom floor value of 8.7 U/g (range 3.0 to 140 U/g) and a mediankitchen value of 10.5 U/g (range 2.0 to 412 U/g).

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TABLE 4

COCKROACH (Bla g 1 OR 2) AND DUST MITE (Der f 1 OR Der p 1) ALLERGENS AS PREDICTORS OF TWO OR MORE REPORTS OF WHEEZE IN THE FIRST YEAR OF LIFE

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TABLE 5

COCKROACH ALLERGEN (Bla g 1 OR 2) IN THE FAMILY ROOM AS A PREDICTOR OF TWO OR MORE REPORTS OF WHEEZE IN THE FIRST YEAR OF LIFE, MULTIVARIATE MODELS

Dust mite allergen concentrations (Der f 1 or Der p 1) were not associated with an increased risk of multiple wheeze reportsin the first year of life. Results were inconsistent across rooms,with univariate family room data actually suggesting an inverserelationship whereas bedroom floor data suggested an elevated(but not significant) estimate of risk of wheeze withexposure.

Persistence of the Association of Multiple Wheeze Reports with Cockroach Allergen in Multivariable Analyses

Compared with no detectable cockroach allergen, concentrations of living room Bla g 1 or 2 of $>=$ 0.05 U/g were associated with1.76 (95% CL: 1.20, 2.57) times the risk of two or more wheezeepisodes in a model (Table 5, Model 1) including smoking whilepregnant, lower respiratory illness, low birth weight, maternalasthma, and dog exposure. The magnitude of the risk was not significantlyreduced from the univariate estimate. This result suggested thatthe effect of cockroach exposure was independent of the effectsof these other variables. Multivariate analyses including familyroom Der f or Der p in addition to the variables in Model 1 confirmedthe absence of an inverse or positive association between dustmite exposure and wheeze (p = 0.95 for Der f 1 or Der p 1 concentrationsof $>=$ 10 µg/g). When the socioeconomic variables (race/ethnicityand income) were included, cockroach allergen in the family roomremained a significant predictor of repeated wheeze, but the magnitudeof the estimate of effect was somewhat reduced (Table 5). Areaof residence did not further reduce the estimate of the estimateof the effect of cockroach. Area was a weak (p > 0.1) predictorof repeated wheeze in multivariate analyses and had no associationwith wheeze in models including race and income. The estimatedrisk of wheeze with cockroach exposure was of similar magnitudeto the estimated risk with maternalsmoking.

Compared with no detectable cockroach allergen, the risk of two or more wheeze episodes were 1.47 (95% CL: 1.01, 2.14) formaximum Bla g in the home $>=$ 0.05 U/g (n = 297), 1.45 (95% CL:0.87, 2.41) for maximum Bla g in the home $>=$ 2 U/g (n = 62) and1.66 (95% CL: 0.85, 3.23) for maximum Bla g in the bedroom $>=$ 2U/g (n = 20), considered separately in models including smokingwhile pregnant, lower respiratory illness, low birth weight, maternalasthma, and dog exposure. After further adjustment for race/ethnicity,the risk of two or more wheeze episodes were 1.37 (95% CL: 0.93,2.01) for maximum Bla g in the home $>=$ 0.05 U/g, 1.18 (95% CL:0.69, 2.02) for maximum Bla g in the home $>=$ 2 U/g and 1.22 (95%CL: 0.53, 2.84) for maximum Bla g in the bedroom $>=$ 2 U/g. Nonwhiterace/ethnicity and Bla g $>=$ 2 U/g were highly collinear. Of the14 families with Bla g in the family room $>=$ 2 U/g, 11 (79%) wereeither black or Hispanic versus 3 (21%) who were white. In contrast,of the 947 families with Bla g in the family room $>=$ 0.05 but <2 U/g, 38% were nonwhite and 62% were white. Of the 20 familieswith bedroom Bla g $>=$ 2 U/g, 18 (90%) werenonwhite.

Substituting the individual LRI diagnoses for any LRI in Model 1, Table 5, significant predictors of repeated wheeze includedpneumonia (RR: 3.04; 95% CL: 1.70, 5.43) and bronchitis (RR: 1.79;95% CI: 1.09, 2.93), as well as bronchiolitis (RR: 3.10; 95% CL:2.03, 4.70). Croup had a positive association with repeated wheezethat did not reach p $=<$ 0.05 (RR: 1.22, 95% CL: 0.73, 2.02).

	DISCUSSION

TOP ABSTRACT INTRODUCTION METHODS RESULTS DISCUSSION REFERENCES

Cockroach Allergen Level as a Predictor of Repeated Wheeze in the First Year of Life

Cockroach exposure may increase the risk of repeated wheeze in the first year of life of children of allergic or asthmaticparents even when cockroach infestation is not obvious and themeasured concentration is relatively low. Although cockroachesare most abundant in kitchens, their presence in the bedroom andthe family room/living room may be more important for the inductionof repeated wheeze ininfancy.

Not all wheeze in the first year of life represents allergic sensitization and not all children who wheeze in the first yearof life continue to wheeze thereafter (16). We did not performskin prick testing or radioallergosorbent testing (RAST) at theend of the first year of life of the children in our cohort toevaluate whether the association between Bla g and repeated wheezerepresented an early expression of allergy. However, previousstudies suggest that IgE antibody to inhalant allergens (specificallyDer p) is rarely detected in the first year of life (17); skintesting responses to inhalant allergens in that period are oftennegative (18). The appropriate serologic or cellular tests ofthe sensitization process during that early period have not yetbeen fullyelucidated.

Many children wheeze in the first year of life if they are born with small airways and/or encounter a noninfectious or infectiousproinflammatory exposure (2). It is possible that in infancyexposure to insect and other animal feces may increase the riskof bronchial inflammation through nonallergenic as well as allergenicmechanisms. Like all insects (and acarids such as mites), cockroachescontain proteolytic digestive enzymes (16, 19). As well asbeing allergens, proteolytic enzymes may have direct proinflammatoryeffects on the lung (20). Cockroaches, which drink from sinks,bathtubs, and other residual sources of moisture, are also knownto be potential carriers of virus and enteric bacteria, thoughthey have never been strongly implicated epidemiologically assources of infectious disease (21, 22). Moreover, cockroachallergen levels in our study had no association with LRI. Toxicproducts of bacteria (e.g., endotoxin) in cockroach or dog fecesmay also have direct proinflammatory effects. In Belgium, homeendotoxin concentrations have been implicated in the worseningof asthma symptoms (23), but data are not yet available on endotoxinand the onset ofwheeze.

Few prospective studies are available on allergen exposure in infancy as a predictor of the development of sensitization,wheeze, and asthma. None are available in relation to cockroachallergen exposure. All suggest a lag of years between exposureto inhalant allergen in infancy and the development of allergen-associatedspecific sensitization and expression of allergic asthma. In aprospective English study, Rowntree and colleagues found thatlevels of Der p I > 5 µg/g of dust in infancy predicted positiveskin test results and elevated IgG to Der p by the fifth yearof life (17). In a prospective cohort study of 67 British childrenwith a family history of asthma or hay fever, Sporik and colleaguesfound that the age at first onset of wheeze was inversely proportionalto the level of Der p exposure in the first year of life, butthe association between Der p and asthma was not observed untilage 11. The RR of asthma at age 11 was 4.8 for those childrenexposed at age 1 to > 10 µg/g dust of Der p 1/g of dust (24).A cross-sectional analysis in a Dutch study of 104 infants suggestedthat, among children of allergic/asthmatic parents, mattress Derp 1 concentrations of > 2 µg/g of dust might be associated withwheeze and frequent cough in the first year of life (25). Itis not clear whether the dust mite-associated symptoms in infancyrepresented allergy. It may be that more follow-up time in ourstudy is required to detect an association between dust mite allergenand repeated wheeze, particularly because bed dust mite levelswere relatively low in this cohort, in which most infants slepton plastic encased mattresses. In England and the Netherlands,crib mattresses tended to be covered withcotton.

Our study found no association between cat allergen concentrations and risk of repeated wheeze, again perhaps because morefollow-up time must elapse for expression of allergic symptoms.Cats were less frequently kept in households where at least oneof the parents was asthmatic, and this factor may have decreasedthe risk of sensitization in the children at highest risk becauseof family history. The concentration of cat allergen in individualhouses may not define the risk of sensitization, because cat allergenexposure is widespread in the community. As suggested in the Reportof the Third International Workshop on Indoor Allergens and Asthma,"the question is whether sensitization of children in a communityrelates to exposure in individual houses or to total exposure"(16).

How confident are we that cockroach exposure, and not the other exposures of poverty associated with the presence of cockroaches,is responsible for the increase risk of repeated wheeze? Detectablelow levels of cockroach allergen were found throughout the Bostoncommunity, not just in the homes of socioeconomically disadvantagedfamilies in our cohort. Family room Bla g 1 or 2 concentrationsof > 0.05 U/g still predicted a higher risk of repeated wheezeafter adjustment for various socioeconomic factors; these resultssuggested that cockroach allergen was not just a proxy for otherexposures of poverty. It was more difficult to separate socioeconomicstatus from Bla g 1 or 2 concentrations of $>=$ 2 U/g, where mostexposure occurred in disadvantaged households and where the numberof observations of Bla g wassparse.

While we have most confidence in the independent association between detectable cockroach allergen in the living room andwheeze, we need to address issues regarding potential misclassificationof exposure to low levels of cockroach allergen. Misclassificationcan occur either because of variability in sampling or becauseof assay interference owing to the presence of other substancesin the dust. Chew has demonstrated that the presence of boricacid (used to kill cockroaches) can lead to an overestimationof Bla g levels and the presence of salt to an underestimation(26). However, cockroaches are usually present at some levelwhere boric acid has recently been applied. Although misclassificationof exposure is certainly possible, it is unlikely to be responsiblefor the association between detectable cockroach allergen andrepeatedwheeze.

When cockroach was detectable in the family room, it was also usually detectable elsewhere in the home, adding confidencethat detectable cockroach in the family room represented the presenceof cockroach in the home. Of the 111 homes with cockroach levelsof > 0.05 in the family room, 30% had cockroach levels of 2 ormore U/g in at least one other room and 86% had detectable levelsof cockroach allergen in at least one otherroom.

The decision to examine cockroach allergen levels as a categorical rather than continuous variable was dictated by the skewnessof the data and by the fact that a large proportion of the datawas censored, with values "below detectable limits." Both thesuggestion in the literature of concentrations above which sensitizationto cockroach allergen might occur (15) and a sparsity of datadictated the categories for Bla g levels. Categorization did notallow a detailed evaluation of the dose- response relationshipbetween allergen concentration and risk. The bedroom data on Blag 1 concentrations did, however, suggest a dose response; thefamily room data suggested the possibility of risk for early-liferepeated wheeze at levels of exposure below those demonstratedto increase risk for asthma morbidity in cockroach-sensitizedchildren (27).

At family room cockroach allergen levels between 0.05 and 2 U/g, 79/97 (81%) of families reported no sign of cockroaches inthe home, making reporting bias less of a potential issue thanin the homes with $>=$ 2 U/g Bla g, where 10/14 (71%) families hadseen cockroaches. However, fewer people related cockroach levelsto wheezing when this study began, prior to the Inner City AsthmaStudy article about asthma morbidity and cockroach allergen incockroach sensitized asthmatic children (27).

Allergen concentration was measured at 2 to 3 mo of life; in all but one child, the second episode of wheeze occurred afterthat period, though the first episode may have occurred in thesame period as measurement of the exposure. It is not known whetherexposure measured at 2 to 3 mo of life also represented exposureduring pregnancy, when T-cell function which can reflect the tendencyto allergy begins to develop (28). The relative contributionsof prenatal and early infancy allergen exposures to allergy/wheezerisk is an area of activeinvestigation.

Other Predictors of Wheeze in the First Year of Life

As we anticipated, exposures known to be associated with infectious and noninfectious nonallergic bronchial inflammation werethe strongest predictors of repeated wheeze in the first yearof life. The most prevalent of these exposures was lower respiratoryillness (LRI) as defined by a report of doctor-diagnosed croup,bronchiolitis, bronchitis, or pneumonia (7). Most of theseillnesses were presumably viral in etiology, though misclassificationis possible. The fact that specimens for viral analysis were nottaken from these children limits our knowledge about whether illnessesdiagnosed as bronchiolitis were caused by infections with respiratorysyncytial virus or were wheeze episodes without an associatedviral infection. Because wheeze symptoms preceded LRI in 51% ofcases (repeated wheeze preceded LRI in 18% of cases), it is possiblethat pathophysiologic factors predisposing children to wheezealso increased the risk that viral infections became lower respiratoryrather than upper respiratory or asymptomatic illnesses. Viralinfections may increase the risk of the persistence of wheezeor asthma in some infants, yet may protect against persistentwheeze, atopy, or asthma in others (29). Further follow-up isneeded to evaluate in this cohort whether the various kinds oflower respiratory illness in the first year of life are protectiveor predictive of allergicasthma.

Despite the exclusion of premature children from the cohort, low birth weight and small head circumference predicted repeatedwheeze. Prematurity, low birth weight, and respiratory distresssyndrome are well-documented predictors of persistent wheeze and/orasthma (34). Further research is needed to investigate whetherthis association is due solely to abnormalities in airway sizeand architecture or whether prematurity is associated with T-cellimmaturity at birth, which might lead to increased risk of atopyandasthma.

The association between maternal smoking in pregnancy and early wheeze has been well documented in other studies (4, 5)and was again seen in this study, despite the low number of smokers.Smoking increases the risk of developing small airways (35)and wheezing; whether or not it increases the risk of sensitizationand allergic asthma is more controversial. Although the effectof maternal smoking during pregnancy (n = 32) was greater thanthe effect of maternal smoking either during pregnancy or duringthe first year of the child's life (n = 41), small numbers andstudy design limited further investigation into interactions withsmoking or the relative effect of smoking before versus smokingafter the birth of thechild.

Season of birth has been a predictor of asthma in other studies (36, 37). A prospective birth cohort study of Swedishchildren found that asthma developed more often in children bornin August through October (38). In our univariate analyses,a winter birth was associated with the lowest risk of wheeze anda fall birth was associated with the highest. The low risk inwinter-born infants may relate to the fact that in Boston childrenborn in the winter have their nadir in immune protection againstviral illnesses in the spring, when fewer viral illnesses arecirculating. They also tend to enter daycare in the spring ratherthan the winter, when there are fewer outbreaks of viral illnessesin the classrooms. Spring and summer are the seasons of highest-levelexposure to pollen allergens, whereas outdoor fungal allergenexposure is generally greatest in the fall. Influences of theseexposures on repeated wheeze in this cohort areunknown.

Even in multivariate analyses, maternal history (not paternal history) of asthma was marginally associated with repeated wheeze,suggesting either reporting bias or early manifestations of theinfluence of inherited traits on the risk of early expressionof allergic asthma. In siblings of this cohort < 5 yr we foundthat maternal history of asthma predicted asthma (39). If allergenlevel in infancy ultimately predicts not only repeated wheezebut also asthma in our cohort, we hypothesize that a parental(particularly maternal) history of asthma will be found to influencethe timing and strength of the associations between allergen exposureand allergy-relatedwheeze.

Areas for Future Investigation

Additional follow-up of this cohort will reveal whether early-life exposure to cockroach or other allergens in the home predictssensitization and the development of childhood asthma. Furtherinvestigation is necessary to understand why low-level exposureto cockroach allergen, which occurs in many households under diversesocioeconomic circumstances, is a risk factor for wheeze in infants.Research is needed to assess whether cockroach allergen is morepotent than other allergens, whether it influences early wheezethrough additional proinflammatory nonallergenic mechanisms, andwhether there is an interaction between the other exposures ofpoverty and cockroach exposure on the risk of wheeze inchildren.

	Footnotes

Correspondence and requests for reprints should be addressed to Dr. Diane Gold, Channing Laboratory, Brigham and Women's Hospital, 181 Longwood Avenue, Boston, MA 02115.

(Received in original form July 20, 1998 and in revised form February 16, 1999).

Dr. Gold is a recipient of the Edward and Amalie Kass Fellowship at the Harvard MedicalSchool.

Acknowledgments: The authors thank Kathleen McGaffigan for her work in data management, computer programming and statistical analysis; MarisaBarr for coordinating and managing this project; Joanne Maldonisfor secretarial assistance; the research assistants (Matthew Agnew,Anne Beaven, Tom Castiglione, Sylvia Fischer, Jennifer Hawthorne,April Hulvershorn, Sammer Saleh, Meghan Syring, and Douglas Yuan);and the families who have taken time from their busy lives toparticipate in thisproject.

Supported by RO1 AI/EHS35786.

	References

TOP ABSTRACT INTRODUCTION METHODS RESULTS DISCUSSION REFERENCES

1. Croner, S., and N. I. M. Kjellman. 1992. Natural history of bronchial asthma in childhood. Allergy 47: 150-157 [Medline].

2. Martinez, F. D., A. L. Wright, L. M. Taussig, C. J. Holberg, M. Halonen, W. J. Morgan, and the Group Health Medical Associates. 1995. Asthma and wheezing in the first six years of life. N. Engl. J. Med. 352: 133-138 .

3. Sporik, R., S. T. Holgate, T. A. E. Platts-Mills, and J. J. Cogswell. 1990. Exposure to house dust mite allergen (Der p 1) and the development of asthma in childhood: a prospective study. N. Engl. J. Med. 323: 502-507 [Abstract].

4. Weitzman, M., S. Gortmaker, D. K. Walker, and A. Sobol. 1990. Maternal smoking and childhood asthma. Pediatrics 85: 505-511 [Abstract/Free Full Text].

5. Pedreira, F. A., V. L. Guandolo, E. J. Feroli, and et al. 1985. Involuntary smoking and incidence of respiratory illness during the first year of life. Pediatrics 75: 594-597 [Abstract/Free Full Text].

6. Bjorksten, B., and N. I. M. Kjellman. 1987. Perinatal factors influencing the development of allergy. Clin. Rev. Allergy 5: 339-347 [Medline].

7. Gold, D. R., I. B. Tager, S. T. Weiss, T. D. Tosteson, and F. E. Speizer. 1989. Acute lower respiratory illness in childhood as a predictor of lung function and chronic respiratory symptoms. Am. Rev. Respir. Dis. 140: 877-885 [Medline].

8. Schwartz, J., D. Gold, D. W. Dockery, S. T. Weiss, and F. E. Speizer. 1990. Predictors of asthma and persistent wheeze in a national sample of children in the United States. Am. Rev. Respir. Dis. 142: 555-562 [Medline].

9. Weitzman, M., S. Gortmaker, and A. Sobol. 1990. Racial, social, and environmental risks for childhood asthma. Am. J. Dis. Child. 144: 1189-1194 [Abstract/Free Full Text].

10. Chew, G. L., H. A. Burge, D. W. Dockery, M. L. Muilenberg, S. T. Weiss, and D. R. Gold. 1998. Limitations of a home characteristic's questionnaire as a predictor of indoor allergen levels: clinical and epidemiologic implications. Am. J. Respir. Crit. Care Med. 157: 1536-1541 [Abstract/Free Full Text].

11. Chapman, M. D., R. C. Aalberse, M. J. Brown, and T. A. E. Platts-Mills. 1988. Monoclonal antibodies to the feline allergen, Fel d I, N-terminal sequence analysis and development of a sensitive two-site immunoassay to assess Fel d I exposure. J. Immunol. 812-818.

12. Luczynska, C. M., L. Yin, M. D. Chapman, and T. A. E. Platts-Mills. 1989. A two-site ELISA for the quantification of the major Dermatophagoides spp allergens, Der p I and Der f I. J. Immunol. Methods 118: 227-235 [Medline].

13. Korsgaard, J.. 1983. Mite asthma and residency: a case-control study on the incidence of exposure to house-dust mites in dwellings. Am. Rev. Respir. Dis. 128: 231-235 [Medline].

14. Gelber, L., S. Pollart, M. Chapman, et al . 1990. Serum IgE antibodies and allergen exposure as risk factors for acute asthma (abstract). J. Allergy Clin. Immunol. 85: 193 .

15. Kang, B. J., and J. L. Chang. 1985. Allergenic impact of inhaled arthropod material. Clin. Rev. Allergy 3: 363-375 [Medline].

16. Platts-Mills, T. A. E., D. Vervloet, W. R. Thomas, R. C. Aalberse, M. D. Chapman, et al. 1997. Indoor allergens and asthma: report of the third international workshop 1997. J. Allergy Clin. Immunol. S1-S24.

17. Rowntree, S., T. A. E. Platts-Mills, J. J. Cogswell, and E. B. Mitchell. 1987. A subclass IgG4-specific antigen-binding radioimmunoassay (RIA): comparison between IgG and IG4 antibodies to food and inhaled antigens in adult atopic dermatitis after desensitization treatment and during development of antibody responses in children. J. Allergy Clin. Immunol. 80: 622-630 [Medline].

18. Zeiger, R. S.. 1985. Atopy in infancy and early childhood: natural history and role of skin testing. J. Allergy Clin. Immunol. 75: 633-639 [Medline].

19. Arruda, L. K., L. D. Vailes, B. J. Mann, J. Shannon, J. W. Fox, T. S. Vedvick, M. L. Hayden, and M. D. Chapman. 1995. Molecular cloning of a major cockroach (Blatella germanica) allergen, Bla g 2: sequence homology to the aspartic proteases. J. Biol. Chem. 270: 19563-19568 [Abstract/Free Full Text].

20. Baur, X., G. Konig, K. Bencze, and G. Fruhmann. 1982. Clinical symptoms and results of skin test, RAST and bronchial provocation test in thirty-three papain workers: evidence for strong immunogenic potency and clinically relevant "proteolytic effects of airborne papain". Clin. Allergy 12: 9-17 [Medline].

21. Roth and Willis. 1957. The Medical and Veterinary Importance of Cockroaches. Smithsonian Institution.

22. Cockran, D. Cockroaches $---$ Biology and Control. World Health Organization, 1975.

23. Michel, O., J. Kips, J. Duchateaie, T. Vertongen, R. L. Collet, R. Pauwels, and R. Sergysels. 1998. Severity of asthma is related to endotoxin in housedust. Am. J. Respir. Crit. Care Med. 154: 164-166 .

24. Sporik, R., S. T. Holgate, T. A. E. Platts-Mills, and J. J. Cogswell. 1990. Exposure to house dust mite allergen (Der p 1) and the development of asthma in childhood: a prospective study. N. Engl. J. Med. 323: 502-507 .

25. Van Stien, R. T., A. P. Verhoeff, J. H. van Wijnen, G. Doekes, G. de Meer, and B. Brunekreef. 1996. Infant respiratory symptoms in relation to mite allergen exposure. Eur. Respir. J. 9: 926-931 [Abstract].

26. Chew, G. L. 1997. Exposure assessment of allergen and culturable fungi in residential environments. Doctoral thesis.

27. Rosenstreich, D. L., P. Eggleston, M. Kattan, D. Baker, R. G. Slavin, P. Gergen, H. Mitchell, K. McNiff-Mortimer, H. Lunn, D. Ownby, and F. Malveaux. 1997. The role of cockroach allergy and exposure to cockroach allergen in causing morbidity among inner-city children with asthma. N. Engl. J. Med. 336: 1356-1363 [Abstract/Free Full Text].

28. Wegmann, T. G., H. Lin, L. Guilbert, and T. R. Mosmann. 1993. Bidirectional cytokine interactions in the maternal-fetal relationship: is successful pregnancy a T_H2 phenomenon? Immunol. Today 14: 353-356 [Medline].

29. Martinez, F. D.. 1994. Role of viral infections in the inception of asthma and allergies during childhood: could they be protective? (Editorial). Thorax 49: 1189-1191 [Free Full Text].

30. Martinez, F. D., D. A. Stern, A. L. Wright, L. M. Taussig, and M. Halonen. 1995. Association of non-wheezing lower respiratory tract illnesses in early life with persistently diminished serum IgE levels. Group Health Medical Associates. Thorax 50: 1067-1072 [Abstract/Free Full Text].

31. Welliver, R. C., T. N. Kaul, and P. L. Ogra. 1980. The appearance of cell-bound IgE on respiratory tract epithelium after respiratory-syncytial virus infection. N. Engl. J. Med. 303: 1198-1202 [Abstract].

32. Shaheen, S. O., P. Aaby, A. J. Hall, D. J. Barker, C. B. Heyes, A. W. Shiell, and A. Goudiaby. 1996. Measles and atopy in Guinea-Bissau. Lancet 347: 1792-1796 [Medline].

33. Wjst, M., S. Dold, P. Reitneir, C. Fritzsch, E. von Mutius, and H.-H. Thiemann. 1994. Pertussis infection and allergic sensitization. Ann. Allergy 73: 450-454 [Medline].

34. Bjorksten, B., and N. I. M. Kjellman. 1987. Perinatal factors influencing the development of allergy. Clin. Rev. Allergy 5: 339-347 .

35. Hanrahan, J. P., I. B. Tager, M. R. Segal, T. D. Tosteson, R. G. Castile, H. Van Vanakis, S. T. Weiss, and F. E. Speizer. 1992. The effect of maternal smoking during pregnancy on early infant lung function. Am. Rev. Respir. Dis. 145: 1129-1135 [Medline].

36. Aberg, N.. 1989. Birth season variation in asthma and allergic rhinitis. Clin. Exp. Allergy 19: 643-648 [Medline].

37. Singh, B. P., M. Malhotra, S. Sridhara, and S. N. Gaur. 1997. Relevance of birth month in respiratory allergy. Allergy 52: 232-233 [Medline].

38. Croner, S., and N. Kjellman. 1992. Natural history of bronchial asthma in childhood: a prospective study from birth up to 12-14 years of age. Allergy 47: 150-157 .

39. Litonjua, A., V. J. Carey, H. A. Burge, S. T. Weiss, and D. R. Gold. 1998. Parental history of asthma and allergies as predictors of childhood asthma: does mother confer more risk than father? Am. J. Respir. Crit. Care Med. 158: 176-181 [Abstract/Free Full Text].

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