Within pair association between birth weight and blood pressure at age 8 in twins from a cohort study

BMJ 1999;319:1325-1329 ( 20 November )

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Within pair association between birth weight and blood pressure at age 8 in twins from a cohort study

Editorial by Leon

Terence Dwyer, professor ^a, Leigh Blizzard, biostatistician ^a, Ruth Morley, senior research fellow ^b, Anne-Louise Ponsonby, public health physician ^c.

^a Menzies Centre for Population Health Research, University of Tasmania, Hobart 7001, Tasmania, Australia, ^b Clinical Epidemiology and Biostatistics Unit, University of Melbourne Department of Paediatrics, Royal Children's Hospital, Melbourne, Victoria, Australia, ^c Academic Unit of General Practice and Community Care, Canberra Clinical School, University of Sydney, Canberra, Australian Capital Territory, Australia

Correspondence to: T Dwyer T.Dwyer{at}utas.edu.au

Abstract

Top
Abstract
Introduction
Subjects and methods
Results
Discussion
Conclusion
References

Objectives: To study the association between birth weightand blood pressure in children from multiple pregnancies (multiplets),mostly twins, to determine whether maternal or genetic factorsare responsible for theassociation.
Design: Cohortstudy.
Setting: SouthernTasmania.
Subjects: 888 children including 104 multiplets (32monozygotic, 72dizygotic).
Main outcome measure: Systolic blood pressure (mmHg).
Results: Blood pressure decreased with birth weightand increased with current body mass. After adjustment for ageand body mass, systolic blood pressure changed by $-$ 1.94 mm Hg(95% confidence interval $-$ 2.89 to -0.98) per 1 kg increase inbirth weight of singletons. For multiplets, blood pressure changedby $-$ 7.0 mm Hg ( $-$ 10.1 to $-$ 3.9) for each 1 kg increase in birthweight. This was little altered in within pair analyses ( $-$ 5.3, $-$ 13.8 to 3.2) and was similar for both monozygotic ( $-$ 6.5, $-$ 22.5to 9.4) and dizygotic ( $-$ 4.9, $-$ 15.8 to 6.0)pairs.
Conclusion: Because the association between birth weightand blood pressure was largely unchanged in within pair analyses,exposures originating in the mother (such as nutritional status)cannot be wholly responsible. The association also remained withinmonozygotic pairs, suggesting that genetic predisposition is notwholly responsible either. The principal causal pathway must concernmechanisms within the fetoplacental unit. The stronger associationin multiplets suggests that factors adversely influencing bothblood pressure and birth weight are more prevalent in multiplepregnancies.

Key messages

Low birthweight is associated with high blood pressure from an early age
Maternal factors, including diet during pregnancy, cannot wholly explain the association between fetal development and later risk of cardiovascular disease
Because the association between blood pressure and birthweight remained in monozygotic twins, genetic factors are unlikely to be responsible for the association
Important causes of the association seem to be operating within the fetoplacental unit during fetal life
Further research should now focus on placental function and fetal exposures

	Introduction

Top Abstract Introduction Subjects and methods Results Discussion Conclusion References

Much evidence suggests that low birth weight is associated with high blood pressure¹ and high risk of both cardiovasculardisease² and non-insulin dependent diabetes mellitus (type2 diabetes) in adult life.³ Furthermore, risk factors for cardiovasculardisease, including high mean blood pressure and glucose intolerance,have been shown to be more prevalent in childhood among thosewho were of low birth weight. ¹ ⁴ ⁵ The general propositionunderlying the "fetal origins" hypothesis⁶is that low birth weight is principally due to a poor nutrientsupply to the fetus,⁷ which in turn may result from suboptimalmaternal nutrient intake. Undernutrition at a critical periodin fetal life may "programme" a permanent change in the structureor function of an individual, ⁷ ⁸ altering the distributionof cell types or gene expression, or both.⁹ This hypothesishas been supported by studies of rodents.¹⁰

Alternatively some factors other than nutrition may determine birth weight and influence the causal pathway leading to highblood pressure or high risk of either cardiovascular disease ortype 2 diabetes. Environmental causes, particularly those associatedwith socioeconomic status, must be considered. ¹¹ ¹² Factorsoriginating in the fetus such as genetic predisposition to bothlow birth weight and hypertension, type 2 diabetes, or cardiovasculardisease could also potentially explain the association. In humans,experimental studies to test the specific hypotheses generallyare not feasible for ethical and practical reasons. Geneticand extrauterine environmental causes can, however, be separatedthrough studies of monozygotic and dizygotic subjects from multiplepregnancies (multiplets). This approach has not been reportedpreviously in studies of the association between birth weightand bloodpressure.

We had the opportunity to examine the association between birth weight and childhood blood pressure in both singletons andmultiplets (mostly twins) in the Tasmanian infant health surveycohort of infants. Among multiplets we were able to make comparisonswithin pairs, for which the infants are matched on exposures ofmaternal origin. The underlying hypotheses for the within pairanalyses were that if maternal factors are responsible for programminghigh blood pressure, the association would be weakened by pairing,and, if genetic predisposition is responsible, the associationwould be substantially reduced in monozygotic pairs but less soin dizygoticpairs.

Subjects and methods

Top
Abstract
Introduction
Subjects and methods
Results
Discussion
Conclusion
References

Subjects
The Tasmanian infant health survey, a cohortstudy initiated to study sudden infant death syndrome, providedstandard information prospectively on around one in five birthsin Tasmania from 1988 to 1995.¹³ Selection of singleton birthswas on the basis of a scoring system using six risk factors forsudden infant death syndrome (young maternal age, male sex, lowbirth weight, autumn birth, maternal intention to bottle feed,and duration of second stage labour)¹⁴; singletons with a compositescore over a cut off point were eligible for inclusion. All multiplebirths were eligible irrespective of theirscores.

Of 13 592 liveborn infants in Tasmania in 1988 and 1989, 2791 were eligible for the Tasmanian infant health survey. Of the1498 infants born in southern Tasmania, a defined geographicalregion, 1440 (96.1%) were the subject of a hospital interviewsoon after the birth. We identified 1185 of these children fromschool enrolment lists in southern Tasmania, and they were invitedto join a study either of childhood blood pressure in 1996 (1988birth cohort) or of high density lipoprotein cholesterol concentrationand blood pressure in 1997 (1989 cohort). All studies were approvedby the University of Tasmania ethics committee, and written parentalconsent was obtained for eachsubject.

Measurements
Information on the infants had been collectedfrom hospital obstetric records (gestational age, placental weight,birth weight, crown to heel length, head circumference) and fromquestionnaires and additional infant anthropometry (skinfold thicknesses)in the postnatal ward, as described previously.¹³

The children were seen at school when they were 8 years of age. Body weight was measured with bathroom scales, which werecalibrated daily, and height was measured with a stadiometer.Skinfold thickness was measured with calipers at four sites (triceps,biceps, subscapular, suprailiac),¹⁵and right mid upper arm circumference was measured with a tape.Blood pressure was measured three times with an adult and paediatricvital signs monitor (Dinamap, Critikon, Arlington, TX) with thecuff size appropriate for mid upper arm circumference, and thechild seated with the left arm resting on a pillow and the elbowapproximately at heartlevel.

Zygosity was assessed from parental reports at 8 years. We asked first whether any tests had been performed and, if so, aboutthe results. If not, we accepted the maternal report of whetherthe multiplets wereidentical.

Statistical methods
We summarised the strength of associationsbetween variables with product moment correlation coefficientsand with linear regression coefficients for which the averageof three systolic blood pressure values was the dependent variable.We adjusted for putative confounders $---$ including gestational age,mode of delivery, previous pregnancies, duration of breast feeding,maternal smoking and alcohol intake (prenatal and postnatal),maternal education, and child size at age 8 $---$ if their associationwith blood pressure was biologically plausible, and if adjustmentsubstantially changed (by 10% or more¹⁶) the regression coefficient.To capture the non-linear association of systolic pressure withthe measure of fatness in childhood (fat mass estimated from skinfolds and body weight, or body mass index), a predictor term forthe measure of fatness and another for its square were enteredin the same regressionmodel.

For singletons, these statistics were routinely adjusted for four of the six selection factors (maternal age, month of birth,intention to breast feed, and duration of second stage labour)and by stratifying for another (sex). The final selection factorwas the study factor, birth weight. Linear predictors were createdfor month of birth, intention to bottle feed, and duration ofsecond stage labour by scoring their categories with the selectionweights for each. Similar adjustments were not routinely madefor multiplets because they were not selectively recruited, andthere were limited degrees of freedom for those analyses. We checked,however, that artefactual differences had not arisen as a resultof unlike methods of analysis. We adjusted for the child's ageat blood pressure measurement (as days elapsed since seventhbirthday).

In paired analyses, birth weight and blood pressure values from the second born twin were subtracted from corresponding valuesfor the first born twin, and the differences calculated in thisway became the subject of statistical inference. Each set of tripletswas analysed as three sets of pairs, and within pair differenceswere calculated as above. To examine the within pair associationbetween birth weight and blood pressure, we regressed the intrapairdifference in blood pressure on the intrapair difference in birthweight.

	Results

Top Abstract Introduction Subjects and methods Results Discussion Conclusion References

Subjects
Of the 1185 children from the 1988 (572 children)and 1989 (613) Tasmanian infant health survey cohorts identifiedon school enrolment lists in 1996 and 1997 respectively, we wereable to contact 1156 and to obtain measurements from 888 of theoriginal 1185 (74.9%)children.

Table 1 shows the characteristics of the sample at birth and at a mean age 8.13 years (range 7.26-8.88 years), with subjectsclassified by sex and whether they were singletons or multiplets.Singletons comprised more boys (548 children) than girls (231)because of the weighting given to male sex in the selectioncriteria of the Tasmanian infant health survey. Comparativelymore of the girls (143; 61.9%) than boys (296; 54.0%) had birthweights below the 50th centile for gestational age (from normsfor singleton births in New South Wales¹⁷). This was becauselow birth weight was also a selection factor, and its comparativecontribution was greater for the girls. The full range of birthweights was nevertheless represented, and 15 (6.5%) girls and44 (8.0%) boys had birth weights exceeding the 90th centile.

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Table 1. Characteristics of study children

From the 1988 and 1989 cohorts, 128 multiplets were identified at schools in southern Tasmania, and 109 (85.0%; 70 girls and39 boys), including two sets of triplets, participated in thisstudy. In five cases the cotwin was not included in the sample(three were sole survivors, one twin was not allowed to participate,and one twin was excluded on medical grounds). To maintain comparabilitybetween analyses, these five subjects were excluded. Multipletshad a lower mean birth weight than singletons (P<0.01) and a shortermean gestation (P<0.01), but birth weight adjusted for gestationalage was not statistically different: girls ( $-$ 108 g; P=0.11), boys( $-$ 132 g; P=0.15). Multiplets had higher mean systolic blood pressureby around 2 mm Hg (P<0.01) thansingletons.

Birth weight and childhood blood pressure
Systolic pressure was negatively associatedwith birth weight. Children with greater lean or fat mass at age8 years had higher blood pressure and had been heavier at birththan smaller children at age 8 years. Adjusting for childhoodfat and lean mass (the childhood size measures most strongly associatedwith blood pressure) removed the confounding effect of currentsize, thereby increasing the estimated strength of the associationbetween systolic pressure and birth weight (figure). We adjustedonly for fat mass in multiplets because of the colinearity ofthe fat mass and lean mass measurements for these children.

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Effect of 1 kg increase in birth weight on systolic blood pressure at age 8 years, with and without adjustment for current size

The association was stronger in multiplets than in singletons. For each 1 kg increase in birth weight there was an estimatedchange in systolic pressure of $-$ 1.94 mm Hg (95% confidence interval $-$ 2.89 to $-$ 0.98) in singletons (girls: $-$ 2.16, $-$ 4.24 to $-$ 0.08);boys: $-$ 1.73, $-$ 2.83 to $-$ 0.64) and $-$ 7.0 mm Hg ( $-$ 10.1 to $-$ 3.9) inmultiplets (girls: $-$ 5.9, $-$ 9.6 to $-$ 2.2; boys: $-$ 8.4, $-$ 15.6 to $-$ 1.2).Estimates for singletons, but not multiplets, were routinely adjustedfor the selection criteria factors. Similar adjustment for multipletsmade little difference: adjusted estimates were $-$ 5.4 mm Hg ( $-$ 9.4to $-$ 1.5) for girls and $-$ 8.9 ( $-$ 16.5 to $-$ 1.2) for boys. The estimatedfall in systolic pressure per 1 kg increase in birth weight wasgreater for multiplets than for singletons (for both sexes P<0.01,girls P=0.14, boys P=0.02). We found no significant associationbetween birth weight and diastolicpressure.

We searched for factors that might explain the different effect size in multiplets and singletons. Gestational age did notinfluence systolic pressure independently of birth weight, andadjustment for it left almost unaltered the estimated effect ofbirth weight in multiplets. They were more commonly deliveredby caesarean (26 of 104 (25%) versus 127 of 778 (16.3%) singletons),and delivery of a further 15 multiplets was medically or surgicallyinduced before full term. Removing these two groups made littledifference: the birth weight effect among the 65 remaining multiplebirths was $-$ 8.9 mm Hg ( $-$ 13.1 to $-$ 4.6) per 1 kg. Adjusting fornumber of previous pregnancies, breast feeding, maternal smokingand alcohol intake (prenatal and postnatal), or maternal educationdid not substantially change (by as much as 10%) the differencein the estimated effect of birth weight on blood pressure betweenmultiplets andsingletons.

Within pair analyses in multiplets
In multiplets the size of the birth weighteffect was largely unchanged in within pair analyses inwhich we regressed the within pair difference in blood pressureon the within pair difference in birth weight (table 2). Estimateswere generally larger for monozygotic than for dizygotic pairs,but differences were not statistically significant in this samplesize. To provide greater depth to the analysis, we investigateddifferent birth measures. The same pattern of effects and persistenceof effect size after pairing was seen for crown to heel length.Associations were weaker for arm and head circumferences, bodysize ratios, and infant skin fold thicknesses (data not shown).

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Table 2. Influence of birth weight and birth length on systolic blood pressure in multiplets, at 8 years of age

	Discussion

Top Abstract Introduction Subjects and methods Results Discussion Conclusion References

This is the first report of an association between birth weight and blood pressure in children from multiple pregnancies.We found a stronger negative association among multiplets thansingletons. This observation in itself has the potential to provideclues to the origin of the relation between birth weight and bloodpressure. More importantly, the strong association among multipletsafforded an opportunity to gain insights, through within pairanalyses, into the role that exposures originating with the motherplayed, and also the likely contribution of geneticfactors.

Implications of within pair analyses in multiplets
The association between birth weight and bloodpressure, seen in multiplets as a group, was not diminished inwithin pair analyses. This implies that maternal factors, includingnutrient intake, cannot be directly responsible for the associationbetween birth weight and blood pressure. The critical step inthe causal pathway must concern mechanisms that lie within thefetoplacental unit, with maternal exposures operating onlyas antecedents or primers in the causal pathway. This is an importantconclusion, which is contrary to the current paradigm in thisresearch field. This key observation is supported by the workof Poulsen et al,¹⁸ who found an association between birth weightand type 2 diabetes in twins, which remained after within pairanalysis.

Although the sample size (over 100 multiplets) provided sufficient power to determine whether the effect remained after pairing,it was insufficient to permit estimation of the difference ineffect between monozygotic and dizygotic twins either before orafter pairing. None the less, the strong association was comparativelyunchanged in within pairs analysis in monozygotic twins, implyingthat the association between birth weight and blood pressure doesnot originate in the genes of theinfant.

A possible explanation for the association is that birth size itself is a component of the principal causal pathway that leadsto later high blood pressure and possibly other adverse metabolicoutcomes. That the strength of the association between birth weightand blood pressure was greater in multiplets than singletons would,however, make that unlikely, unless some confounding or effectmodifying factor was operating differentially in multiplets andsingletons.

The different association in multiplets and singletons
The finding of a stronger association betweenbirth weight and childhood blood pressure in multiplets than insingletons may provide a clue as to what may be responsible forthe association between birth weight and blood pressure, but canwe be confident of the observation? It cannot be accounted forby an unusually weak association in this study among singletons.The estimated effect of birth weight on systolic pressure in the8 year old singletons, at around $-$ 2 mm Hg per 1 kg increase inbirth weight, was within the range of effect sizes estimated inother studies of children of comparable age in Australia,¹⁹the United Kingdom,^20-22 and Zimbabwe.²³ We found slightly largereffects for singleton girls ( $-$ 2.16 mm Hg per 1 kg) than singletonboys ( $-$ 1.73 mm Hg per 1 kg), in common with other studies. ²⁰ ²¹ ²⁴ It is also unlikely to be explained by the sample selection process.Although singletons in the Tasmanian infant health survey werenot representative of the total infant population, analyses wereadjusted for factors used as selection criteria, and the estimatedeffect size in singletons was very similar to that in other populations.Multiplets were not subject to any selection bias as all bornin the study period were eligible and the response at follow upwas high (85.0%), as in singletons (74.9%).

The stronger association in multiplets raises the hypothesis that of the potential causes of low birth weight or later highblood pressure those that influence both were more prevalent inmultiplets. What factors then within the fetoplacental unit couldbe associated with birth weight and blood pressure and also moreprevalent in multiple pregnancies? Supply of oxygen and nutrientsacross the placenta can be unequally distributed between individualmultiplets, and reduced oxygen or nutrient availability may bemore prevalent causes of growth restriction in multiplets thanin singletons and lead to permanent adverse programming of thecardiovascular system. We were unable to address these questionsin any depth, but we did examine the association between birthweight and blood pressure in singletons before and after controllingfor placental weight. The addition of placental weight to theregression model had little effect on the estimates, but the weightof the placenta may not reflect itsfunction.

	Conclusion

Top Abstract Introduction Subjects and methods Results Discussion Conclusion References

These findings need to be confirmed in other studies and for other risk factors for adult cardiovascular disease. If replicatedthey would support a shift in the thrust of future research froma focus on maternal nutrition as a cause of the association betweenbirth weight and blood pressure and possible cardiovascular diseaseto factors within the fetoplacentalunit.

Acknowledgments

We thank the nurses who measured blood pressures; the children and their families; and theschools.

Contributors: TD conceived the idea for this study, and both he and A-LP contributed to its design. All authors participated in the analysis or interpretation of data, or both, and in drafting or revising the manuscript, or both, and each approved the version published. TD and LB will act as guarantors for the paper.

Footnotes

Funding: This study was funded by the National Health and Medical Research Council of Australia. The Tasmanian infant healthsurvey was funded by the National Health and Medical ResearchCouncil of Australia, US National Institutes of Health (grant001 HD28979-01A1, Tasmanian State Government, Australian RotaryHealth Research Fund, Sudden Infant Death Syndrome Research Foundation,National Sudden Infant Death Syndrome Council of Australia, CommunityOrganisations' support programme of the Department of Human Servicesand Health, Zonta International, Wyeth Pharmaceuticals, and TasmanianSanatoria After-Care Association. A-LP was supported by a NationalHealth and Medical Research Council Public Health Research andDevelopment Committeefellowship.

Competing interests: Nonedeclared.

References

Top
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Introduction
Subjects and methods
Results
Discussion
Conclusion
References

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(Accepted 19 July 1999)

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Within pair association between birth weight and blood pressure at age 8 in twins: Collings
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Within pair association between birth weight and blood pressure at age 8 in twins from a cohort study

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