Late pregnancy exposures to disinfection by-products and growth-related birth outcomes.Toxicologic studies have demonstrated associations between growth-related birth outcomes and exposure to high concentrations of disinfection disinfection, n the process of destroying pathogenic organisms or rendering them inert. disinfection, full oral cavity, n a procedure used to reduce active periodontal disease, usually completed within a certain short time frame. by-products (DBPs), including specific trihalomethane tri·hal·o·meth·ane n. A chemical compound containing three halogen atoms substituted for the three hydrogen atoms normally present in a methane molecule. (THM) and haloacetic acid (HAA HAA Harvard Alumni Association HAA Houston Apartment Association HAA High Altitude Airship HAA Haloacetic Acid HAA HIV/AIDS Administration (District of Columbia) HAA Heavy Anti-Aircraft HAA Height Above Airport ) chemical subspecies subspecies, also called race, a genetically distinct geographical subunit of a species. See also classification. . Few prior investigations of DBPs have evaluated exposure during the third trimester Noun 1. third trimester - time period extending from the 28th week of gestation until delivery trimester - a period of three months; especially one of the three three-month periods into which human pregnancy is divided of pregnancy, the time period of gestation GESTATION, med. jur. The time during which a female, who has conceived, carries the embryo or foetus in her uterus. By the common consent of mankind, the term of gestation is considered to be ten lunar months, or forty weeks, equal to nine calendar months and a week. when fetal growth may be most sensitive to environmental influences. We conducted a retrospective cohort study A cohort study is a form of longitudinal study used in medicine and social science. It is one type of study design. In medicine, it is usually undertaken to obtain evidence to try to refute the existence of a suspected association between cause and disease; failure to refute to examine the effects of exposure to THMs and HAAs during the third trimester and during individual weeks and months of late gestation on the risks for term low birth weight, intrauterine growth retardation Intrauterine Growth Retardation Definition Intrauterine growth retardation (IUGR) occurs when the unborn baby is at or below the 10th weight percentile for his or her age (in weeks). , and very preterm preterm /pre·term/ (-term´) before completion of the full term; said of pregnancy or of an infant. pre·term adj. and preterm births. The study population (n = 48,119) included all live births and fetal deaths occurring from January 1998 through March 2003 to women whose residence was served by one of three community water treatment facilities. We found evidence of associations between exposure to specific HAAs and term low birth weight as well as intrauterine growth retardation and for exposure to the five regulated HAAs (HAAS) and term low birth weight. Our findings suggest a critical window of exposure with respect to fetal development during weeks 33-40 for the effects of dibromoacetic acid and during weeks 37-40 for the effects of dichloroacetic acid Dichloroacetic acid, often abbreviated DCA, is a chemical compound, an acid, and an analogue of acetic acid in which two of the three hydrogen atoms of the methyl group have been replaced by chlorine atoms. . Adjustment for potential confounders did not affect the conclusions. Key words: birth weight, disinfection by-products, epidemiology, haloacetic acids Haloacetic acids are carboxylic acids in which a halogen atom takes the place of a hydrogen atom in acetic acid. Thus, in a monohaloacetic acid, a single halogen would replace a hydrogen atom. , pregnancy, preterm birth, trihalomethanes. Environ Health Perspect 113:1808-1813 (2005). doi: 10.1289/ehp.8282 available via http://dx.doi.org/[Online 17 August 2005] ********** The chemical mixture of disinfection by-products (DBPs) has not been fully characterized but is known to contain trihalomethanes (THMs), haloacetic acids (HAAs), haloacetonitriles, and other classes of chemicals, some of which are mutagenic mutagenic inducing genetic mutation. or carcinogenic carcinogenic having a capacity for carcinogenesis. in laboratory animals (Nieuwenhuijsen et al. 2000). Total THMs (TTHMs) are the sum of the concentrations of the THM species chloroform chloroform (klôr`əfôrm) or trichloromethane (trī'klôrōmĕth`ān), CHCl3 , bromodichloromethane (BDCM BDCM Bromodichloromethane BDCM Bulk Distribution Carton Metric (shipping, supply chain) ), dibromochloromethane (DBCM DBCM Data Base Configuration Management ), and bromoform. The five regulated HAAs (HAA5) include monochloroacetic acid (MCAA MCAA Mason Contractors Association of America (Oakbrook Terrace, Illinois) MCAA Messenger Courier Association of the Americas MCAA Marine Corps Aviation Association MCAA Mechanical Contractors Association of America, Inc. ), dichloroacetic acid (DCAA DCAA Defense Contract Audit Agency DCAA Dansk Center Vedrørende Alkoholisme Og Andre Afhængighedssygdomme (Danish) DCAA Danish Civil Aviation Administration DCAA Derby City Agility Association DCAA Dual Call Auto Answer ), trichloroacetic acid trichloroacetic acid /tri·chlo·ro·ace·tic ac·id/ (tri-klor?o-ah-se´tik) an extremely caustic acid, used in clinical chemistry to precipitate proteins and applied topically in chemabrasion and to remove warts. (TCAA TCAA Traditional Cowboy Arts Association TCAA Texas Clay Arts Association TCAA Truck Cap & Accessory Alliance (now Light Truck Accessory Alliance) TCAA Trichloro Acetic Acid TCAA Tile Contractors Association of America, Inc. ), monobromoacetic acid (MBAA MBAA Master Brewers' Association of the Americas MBAA Mortgage Bankers Association of America MBAA Medical Billing Advocates of America MBAA Melty Blood Actress Again (game) MBAA Mississippi Bail Agents Association ), and dibromoacetic acid (DBAA DBAA Discount Buyers Association of America DBAA Duplicate Bridge Association of Atlanta (Atlanta, GA) DBAA Detail Business Area Analysis ). Concerns have been raised regarding the potential effects of by-products on reproductive outcomes, supported in part by the findings that some by-products cause reproductive and developmental toxicity in laboratory animals, albeit at doses much higher than those encountered by humans. In addition, exposure to DBPs has been associated with an increased risk of impaired fetal growth in several epidemiologic studies epidemiologic study A study that compares 2 groups of people who are alike except for one factor, such as exposure to a chemical or the presence of a health effect; the investigators try to determine if any factor is associated with the health effect (Bove et al. 1995; Dodds et al. 1999; Gallagher et al. 1998; Kramer et al. 1992; Savitz et al. 1995; Wright et al. 2003). The third trimester of pregnancy is considered the period of human fetal development during which fetal growth and birth weight are maximally max·i·mal adj. 1. Of, relating to, or consisting of a maximum. 2. Being the greatest or highest possible. n. Mathematics An element in an ordered set that is followed by no other. sensitive to environmental influences (Kline et al. 1989). The third trimester lasts from approximately the 26th week of gestation to parturition parturition or birth or childbirth or labour or delivery Process of bringing forth a child from the uterus, ending pregnancy. It has three stages. , with the actual length of time dependent on the individual pregnancy. However, only a few prior investigations of DBPs have evaluated exposure during this period (Dodds et al. 1999; Gallagher et al. 1998; Savitz et al. 1995; Wright et al. 2003). Risks for adverse birth outcomes depend on the magnitude of exposure over critical time windows. Therefore, analyses over exposure windows that are too wide may bias risk estimates. Because the critical time period for the potential effects of DBP DBP Diastolic Blood Pressure DBP Development Bank of the Philippines DBP Database Project (Visual Studio File Extension) DBP DNA Binding Protein DBP Disinfection Byproduct DBP Deutsche Bundespost exposure on fetal growth is uncertain, the use of multiple, shorter exposure windows may provide less biased risk estimates (Hertz-Picciotto et al. 1996). The purpose of this study was to examine the effects of exposure to THMs and HAAs during the third trimester and during individual weeks and months of late gestation on the risks for term low birth weight, intrauterine growth retardation, and very preterm and preterm births. Materials and Methods We conducted a retrospective cohort study in a large Arizona community served by three water treatment facilities. This community of more than half a million residents living in 24 ZIP codes zip code System of postal-zone codes (zip stands for “zone improvement plan”) introduced in the U.S. in 1963 to improve mail delivery and exploit electronic reading and sorting capabilities. is located adjacent to a major metropolitan area. Most water used by this community originates from surface water sources by means of the Salt River and Central Arizona projects. The community was selected from the U.S. Environmental Protection Agency Environmental Protection Agency (EPA), independent agency of the U.S. government, with headquarters in Washington, D.C. It was established in 1970 to reduce and control air and water pollution, noise pollution, and radiation and to ensure the safe handling and (EPA EPA eicosapentaenoic acid. EPA abbr. eicosapentaenoic acid EPA, n.pr See acid, eicosapentaenoic. EPA, n. ) Information Collection Rule database (U.S. EPA 1999) because the distribution systems displayed large temporal fluctuations (range, 7-81 [micro]g/L) and low spatial variability Spatial variability is characterized by different values for an observed attribute or property that are measured at different geographic locations in an area. The geographic locations are recorded using GPS (global positioning systems) while the attribute's spatial variability is in TTHM TTHM Total Trihalomethanes (water contaminant) levels that permitted a natural experiment through intracommunity comparisons of exposures and outcomes. We determined spatial variability using the methods described by Hinckley et al. (2005). Briefly, we classified a facility as having low spatial variability if TTHM values measured at four points in the facility's distribution system consistently fell, each season, within established boundaries for low, medium, and high exposure as based on concentration cutpoints for TTHMs derived from prior epidemiologic studies of birth outcomes. The study population included all live births and fetal deaths for women whose residence was provided water by one of three facilities serving the community from January 1998 through December 2002. Table 1 summarizes the annual frequency of births in this population, as well as the distribution of TTHM and HAA5 concentrations by year over the period of the study. This study was approved by the human subjects institutional review boards of Colorado State University Colorado State University, at Fort Collins; land-grant with state and federal support; chartered 1870, opened 1879 as an agricultural college, assumed present name in 1957. There is a veterinary teaching hospital, an agricultural campus, and a research campus. and the Arizona Department of Health Services Department of Health Services may refer to:
Subjects were identified from Arizona birth records (n = 48,119) and were matched to a facility service area by residential ZIP code. In cases where two facilities shared the same distribution system, treatment facility employees identified service boundaries. Subjects who lived in ZIP codes that received water from more than one facility were excluded from the analysis. Maternal residence at birth was assumed to be the same as residence during the third trimester. We estimated exposure from data obtained from each facility (facilities A-C A-C Air Conditioning ) for the years 1998-2002. Total and individual THMs were measured quarterly during each of the 5 years, for each of the facilities. Facility A provided quarterly THM and HAA data for the entire study period, with monthly data available for 2001 and 2002. At facilities B and C, HAA5 data were available only for 2000 and 2002. Supplemental monthly and biweekly bi·week·ly adj. 1. Happening every two weeks. 2. Happening twice a week; semiweekly. n. pl. bi·week·lies A publication issued every two weeks. adv. 1. Every two weeks. TTHM and HAA5 data were provided by facility B for 2000 and 2002, respectively. DBP concentrations were monitored at two to four locations within the distribution system of each facility. The quarterly and monthly data indicated the presence of very low levels of bromoform, MBAA, and MCAA; therefore, these chemicals were not included in the analyses. To estimate DBP values for specific study periods corresponding to months when no data were available, we performed a spline In computer graphics, a smooth curve that runs through a series of given points. The term is often used to refer to any curve, because long before computers, a spline was a flat, pliable strip of wood or metal that was bent into a desired shape for drawing curves on paper. See Bezier and B-spline. regression (Greenland 1998) for each water facility to impute impute v. 1) to attach to a person responsibility (and therefore financial liability) for acts or injuries to another, because of a particular relationship, such as mother to child, guardian to ward, employer to employee, or business associates. the missing values In statistics, missing values are a common occurrence. Several statistical methods have been developed to deal with this problem. Missing values mean that no data value is stored for the variable in the current observation. using procedures similar to those used by investigators in Nova Scotia Nova Scotia (nō`və skō`shə) [Lat.,=new Scotland], province (2001 pop. 908,007), 21,425 sq mi (55,491 sq km), E Canada. Geography (Dodds et al. 1999; Dodds and King 2001; King et al. 2000). This nonlinear A system in which the output is not a uniform relationship to the input. nonlinear - (Scientific computation) A property of a system whose output is not proportional to its input. smoothing technique was applied to impute missing exposure data from existing data by generating a joined series of parabolic par·a·bol·ic also par·a·bol·i·cal adj. 1. Of or similar to a parable. 2. Of or having the form of a parabola or paraboloid. curve segments. HAA exposure data were not estimated before the year 2000 for facilities B and C. Infant outcomes were identified through vital records. The date of last menstrual period last menstrual period Gynecology The most recent time that a ♀ notes menstruation, a datum recorded in a chart during a routine gynecologic visit. See Menstruation. was used to define the duration of gestation. We identified infants born at [greater than or equal to] 37 completed weeks of gestation and weighing < 2,500 g as being term low birth weight. We evaluated this outcome only among term births to separate children with true growth retardation retardation: see mental retardation. from babies that are small because of birth at a young gestational age ges·ta·tion·al age n. See estimated gestational age. Gestational age The estimated age of a fetus expressed in weeks, calculated from the first day of the last normal menstrual period. . We identified case infants with intrauterine growth retardation as term or preterm babies that fell below the published value for the lowest 10th percentile percentile, n the number in a frequency distribution below which a certain percentage of fees will fall. E.g., the ninetieth percentile is the number that divides the distribution of fees into the lower 90% and the upper 10%, or that fee level of birth weights by race, ethnicity, and gestation age (Alexander et al. 1999). In this investigation, term low birth weight and intrauterine growth retardation were not mutually exclusive Adj. 1. mutually exclusive - unable to be both true at the same time contradictory incompatible - not compatible; "incompatible personalities"; "incompatible colors" , and cases born at term may have been included in both outcome groups. Because published values for the lowest 10th percentile of birth weights were not available for extreme gestational ages, births before 23 weeks' gestation were excluded from intrauterine growth retardation analyses for Caucasians, African Americans African American Multiculture A person having origins in any of the black racial groups of Africa. See Race. , and Hispanics, and births before 29 weeks' gestation were excluded for Native Americans (Alexander et al. 1999). For intrauterine growth retardation and term low birth weight, estimated monthly DBP exposures were averaged over the third trimester. Additionally, for DBPs associated with intrauterine growth retardation or term low birth weight, we averaged and evaluated exposure during specific time windows, corresponding to gestation weeks 25-28, 29-32, 33-36, 37-40, and 41-44, using monthly DBP concentrations. Preterm births were defined as infants born at < 37 completed weeks of gestation. Very preterm births were defined as a birth occurring before 32 completed weeks of gestation (Martin et al. 2002). Because preterm birth outcomes are defined by time length of gestation, it was inappropriate to evaluate exposure averaged over the third trimester. Preterm births have shorter gestation lengths than the typical comparison group (term births), increasing the potential for bias (Hertz-Picciotto et al. 1996; Hinckley 2003; Hinckley et al. 2002). Therefore, for preterm and very preterm births, we evaluated exposure to DBPs only for the specific gestation week intervals mentioned above. We abstracted information on potential confounders from birth records. These variables included maternal age maternal age, n the age of the mother at the period of conception. , race, ethnicity, education, parity, smoking, and the Kessner index (a measure of prenatal care prenatal care, n the health care provided the mother and fetus before childbirth. adequacy) (Kotelchuck 1994). By comparing the outcomes over different exposure time windows within a single community, we attempted to control for potential residual confounders that could not be evaluated individually. We calculated tertiles of DBP concentrations using the species-specific data from all three water treatment regions in analyses for potential associations with each birth outcome. We used stratified stratified /strat·i·fied/ (strat´i-fid) formed or arranged in layers. strat·i·fied adj. Arranged in the form of layers or strata. chi-square and logistic regression In statistics, logistic regression is a regression model for binomially distributed response/dependent variables. It is useful for modeling the probability of an event occurring as a function of other factors. analyses to evaluate the associations among demographic variables, exposure variables, and adverse birth outcomes. In addition, all covariates significantly associated with growth outcomes at the < 0.20 level in univariate analyses were retained for inclusion in multivariable analyses. After adjustment for potential confounders, we calculated odds ratios (ORs) and 95% confidence intervals confidence interval, n a statistical device used to determine the range within which an acceptable datum would fall. Confidence intervals are usually expressed in percentages, typically 95% or 99%. (CIs) for the relationships between all individual THM species and growth and preterm birth outcomes. For gestation week and third-trimester analyses, a multivariate The use of multiple variables in a forecasting model. logistic regression model containing all individual HAAs as continuous variables was used to evaluate the possible relationship between individual HAAs in increasing the risk of growth-related outcomes. A similar model was not created for individual THMs because there was no evidence of any associations with growth-related outcomes. Results Table 2 summarizes characteristics of subjects and frequency of intrauterine growth retardation, term low birth weight, and preterm and very preterm births. Most mothers were white, non-Hispanic, nulliparous women with some college education. Most mothers received adequate prenatal care, and < 10% smoked during pregnancy. Subjects were excluded if there was no date for last menstrual period or no estimated date of conception. The estimated date of conception was used to estimate the last menstrual period when data on last menstrual period were missing or considered extreme (> 44 weeks before the birth date). The results were not different when using last menstrual period, estimated date of conception, or a combination of both methods; therefore, we used the combined method to minimize the number of subjects lost for this reason (n = 42). The ORs and 95% CIs for intrauterine growth retardation and term low birth weight and exposure to DBPs during the third trimester are shown in Table 3. We found no evidence of an association with either outcome for exposure to TTHMs or specific brominated and chlorinated chlorinated /chlo·ri·nat·ed/ (klor´i-nat?ed) treated or charged with chlorine. chlorinated charged with chlorine. chlorinated acids some, e.g. THMs. We also found no association between exposure to HAA5 and intrauterine growth retardation. The second and third tertiles of exposure to HAA5 showed evidence of a weak association with term low birth weight [OR = 1.26 (95% CI, 0.96-1.65), and OR = 1.25 (95% CI, 0.96-1.64), respectively] compared with referent ref·er·ent n. A person or thing to which a linguistic expression refers. Noun 1. referent - something referred to; the object of a reference exposure levels. Exposures to the highest tertiles of DCAA and TCAA were associated with an increased risk of intrauterine growth retardation [OR = 1.28 (95% CI, 1.08-1.51), and OR = 1.19 (95% CI, 1.01-1.41), respectively]. DCAA and TCAA were also associated with intrauterine growth retardation when analyzed as continuous variables. Weak associations were found for exposure to the highest tertile of DBAA and DBAA analyzed as a continuous variable, although the 95% CIs for those results all included 1.0. Analyses of intrauterine growth retardation were adjusted for parity, smoking, maternal education, and Kessner index. The risk of term low birth weight was increased (OR = 1.49; 95% CI, 1.09-2.04) among women exposed to average DBAA concentrations of [greater than or equal to] 5 [micro]g/L during the third trimester compared with those who were exposed to the referent category of < 4 [micro]g/L. Continuous (unit) increases in average exposure to DBAA also indicated a weak association with term low birth weight (OR = 1.17; 95% CI 1.03-1.32). Analyses of term low birth weight were adjusted for maternal age, parity, education, race, ethnicity, smoking, and Kessner index. Table 4 presents ORs and 95% CIs for exposure to HAA5 and individual HAAs over specific gestation time windows for intrauterine growth retardation and term low birth weight. Because the potential for bias due to averaging was reduced when examining shorter time intervals, exposure values were generally slightly higher or slightly lower over the specific gestation week intervals than over the third trimester. In analyses for intrauterine growth retardation, small increases in risk were observed for DBAA concentrations [greater than or equal to] 5 [micro]g/L (OR = 1.15; 95% CI, 0.98-1.35) and for DBAA analyzed as a continuous variable (OR = 1.06; 95% CI, 1.01-1.12) over gestation weeks 25-28. The largest risk was observed with exposure to DCAA [greater than or equal to] 8 [micro]g/L (OR = 1.27; 95% CI, 1.02-1.59) during gestation weeks 37-40. In addition, an increased risk was observed for exposure to moderate concentrations of TCAA (OR = 1.58; 95% CI, 1.02-2.46) and DCAA (OR = 1.51; 95% CI, 0.98-2.32) during gestation weeks 41-44, but the risk estimates were lower at higher levels of estimated exposure. Exposure to DBAA was associated with an increase in risk for term low birth weight in analyses by gestation week. Between gestation weeks 33 and 36, the second and third tertiles of exposure to DBAA showed evidence of a dose-dependent trend [OR = 1.29 (95% CI, 0.94-1.79), and OR = 1.49 (95% CI, 1.10-2.02), respectively] compared with referent exposure levels. Similarly, moderate exposure to DBAA between gestation weeks 37 and 40 was associated with an increased risk for term low birth weight (OR = 1.38; 95% CI, 1.02-1.86). No associations were observed between preterm or very preterm birth and exposure to TTHMs, HAA5, or specific DBPs during any gestation week interval. ORs for the associations between individual HAAs and term low birth weight and intrauterine growth retardation were not affected by inclusion of other HAAs in the logistic regression model. Discussion Reduced fetal weight is one of the most consistent developmental effects observed with exposure to high concentrations of DBPs in laboratory animals (Nieuwenhuijsen et al. 2000). The biologic mechanisms for DBP-induced growth retardation are not well understood. In animal studies, reductions in birth weight have been commonly described after exposure to THMs, especially chloroform (Murray et al. 1979; Ruddick et al. 1983; Schwetz et al. 1974; Thompson et al. 1974). Two studies by Smith et al. (1989, 1992) found reductions in rat pup body weight after exposure to DCAA and TCAA. Recently, Christian et al. (2001) found that DBAA administration (of 250, 500, and 1,000 mg/L) was associated with exposure-related decreases in rat pup body weight. This effect, however, was thought to be due to reduced parental water consumption. The epidemiologic evidence for an association between exposure to THMs and indicators of fetal growth is relatively sparse sparse - A sparse matrix (or vector, or array) is one in which most of the elements are zero. If storage space is more important than access speed, it may be preferable to store a sparse matrix as a list of (index, value) pairs or use some kind of hash scheme or associative memory. and inconsistent, and few studies have investigated this relationship with respect to HAAs. Four prior epidemiologic studies have evaluated exposure to total and individual THMs in relation to intrauterine growth retardation. In a study by Kramer et al. (1992), a dose-related trend was observed for intrauterine growth retardation at the 5th percentile for exposure to chloroform [greater than or equal to] 10 [micro]g/L and BDCM [greater than or equal to] 4 [micro]g/L, with ORs of 1.8 (95% CI, 1.1-2.9) and 1.7 (95% CI, 0.9-2.9), respectively. Bove et al. (1995) also found an increased risk of intrauterine growth retardation (adjusted OR = 1.50; 90% CI, 1.19-1.86) with exposure to TTHMs > 100 [micro]g/L during pregnancy. In a Massachusetts cohort, Wright et al. (2003) found increased risk of intrauterine growth retardation (10th percentile) for mean exposures to TTHMs > 80 [micro]g/L throughout pregnancy (adjusted OR = 1.14 95% CI, 1.02-1.26) and during the second trimester Noun 1. second trimester - time period extending from the 13th to the 27th week of gestation trimester - a period of three months; especially one of the three three-month periods into which human pregnancy is divided (adjusted OR = 1.13; 95% CI, 1.03-1.24). However, Dodds et al. (1999) found no association between intrauterine growth retardation (10th percentile) and TTHM exposure [greater than or equal to] 100 [micro]g/L in a large cohort of Nova Scotia women. Three studies have evaluated term low birth weight and exposure to TTHMs. Gallagher et al. (1998) found an adjusted OR of 5.9 (95% CI, 2.0-17.0) for term births, although only six cases were analyzed. Bove et al. (1995) also observed a positive, but smaller, association between TTHM exposures averaged over the entire pregnancy and term low birth weight with an OR of 1.42 (50% CI, 1.22-1.65). In a study by Wright et al. (2003), no associations were reported between term low birth weight and trimester-specific exposures or entire pregnancy exposures to TTHMs. Six studies have evaluated preterm birth or very preterm birth; none found a significant relationship with DBPs (Bove et al. 1995; Dodds et al. 1999; Gallagher et al. 1998; Kramer et al. 1992; Savitz et al. 1995; Wright et al. 2003). As a group, these studies differed in their selection of a referent group for exposure, in their ability to control for potential confounding confounding when the effects of two, or more, processes on results cannot be separated, the results are said to be confounded, a cause of bias in disease studies. confounding factor , and in their assessment of exposure during the third trimester or late stages of pregnancy. To evaluate the relationship between TTHMs and growth-related birth outcomes, Bove et al. (1995) averaged quarterly TTHM concentrations over each subject's entire pregnancy. In a study of miscarriage miscarriage: see abortion. miscarriage or spontaneous abortion Spontaneous expulsion of an embryo or fetus from the uterus before it can live outside the mother. , low birth weight and preterm delivery in North Carolina North Carolina, state in the SE United States. It is bordered by the Atlantic Ocean (E), South Carolina and Georgia (S), Tennessee (W), and Virginia (N). Facts and Figures Area, 52,586 sq mi (136,198 sq km). Pop. , Savitz et al. (1995) assigned exposure by using the quarterly value nearest the 28th week of pregnancy. Gallagher et al. (1998) used the median of all quarterly measurements taken during the third trimester. For children born in the second or third month of the quarter, Wright et al. (2003) used the average quarterly values for the third trimester; children born in the first month of the quarter were assigned the preceding quarterly averages. In Nova Scotia, Dodds et al. (1999) used linear regression Linear regression A statistical technique for fitting a straight line to a set of data points. of quarterly data to estimate average exposures during the last 3 months of pregnancy. Our method of assigning exposure included estimating some periodic study time exposures using a spline regression based on quarterly sampling values. Further, all data were interpolated interpolated /in·ter·po·lat·ed/ (in-ter´po-la?ted) inserted between other elements or parts. from month midpoint mid·point n. 1. Mathematics The point of a line segment or curvilinear arc that divides it into two parts of the same length. 2. A position midway between two extremes. and converted to ordinal (mathematics) ordinal - An isomorphism class of well-ordered sets. study time, to better align with gestation time (Yang yang (yang) [Chinese] in Chinese philosophy, the active, positive, masculine principle that is complementary to yin; see yin, under principle. et al. 2005). This regression method, which is similar to that used in the Nova Scotia studies, permitted estimation of exposure for time periods when data were missing or when sampling was not performed. We performed a sensitivity analysis by systematically repeating the spline regression with varying subsets of exposure data. By this method, we found that the model consistently predicted existing data points to within [+ or-] 5%. However, the spline regression technique requires additional validation in other distribution systems. Our study is the first to examine associations between exposures to specific HAAs and impaired fetal growth. We found evidence of associations between exposure to specific HAAs and term low birth weight and intrauterine growth retardation. The second and third tertiles of exposure to HAA5 were also associated with a small increase in risk for term low birth weight when evaluated over the third trimester (Table 3). The increased risk in the second tertile did not seem to be due to a higher risk from DBAA, DCAA, or TCAA. HAA5 concentration is currently regulated in the United States United States, officially United States of America, republic (2005 est. pop. 295,734,000), 3,539,227 sq mi (9,166,598 sq km), North America. The United States is the world's third largest country in population and the fourth largest country in area. , but concentrations of specific HAAs are not. Our findings suggest a critical window of exposure during weeks 33-40 for the effects of DBAA on fetal development. To our knowledge, this is the first time that DBAA has been investigated in an epidemiologic study of developmental outcomes. Studies of exposure to HAAs are relatively new, and none have been performed in communities where DBAA concentrations in drinking water drinking water supply of water available to animals for drinking supplied via nipples, in troughs, dams, ponds and larger natural water sources; an insufficient supply leads to dehydration; it can be the source of infection, e.g. leptospirosis, salmonellosis, or of poisoning, e.g. were above detection (King et al. 2005; Wright et al. 2004). In this investigation, the levels of DBAA were well above the 90th percentile concentrations reported by the U.S. EPA (1998). We also observed evidence of an association between intrauterine growth retardation and exposure to chlorinated HAAs during specific critical time windows of gestation, with modest increases in risk for third-trimester exposure to DCAA and slightly lower estimates for TCAA. When analyzed as continuous variables, exposure to DCAA and TCAA also showed slight increases in risk of intrauterine growth retardation between weeks 29 and 40 of gestation. The risk estimates remained consistent during the gestation week windows comprising this time period. Our study is the first to examine exposure to DBPs during specific gestation week intervals of exposure. In previous studies, exposure for fetal development was usually averaged over the longer third-trimester window. Averaging a variable exposure over longer time periods such as the third trimester is likely to introduce misclassification over the critical time periods and lead to biased risk estimates (Hertz-Picciotto et al. 1996). However, for the highest level of exposure to DBAA, we observed the same OR for exposure averaged over the third trimester as for exposure averaged over gestation weeks 33-36. The CIs were narrower for DBAA exposure during weeks 33-36 than for the entire third trimester, reflecting increased precision due to the slightly larger sample population retained for analysis of gestation week intervals. Because the third trimester is a longer time period, it is more likely to fall outside of the study initiation and termination (or beginning and end) date than are single week-long periods (Hinckley 2003; Hinckley et al. 2002). Windows of exposure have been historically important in epidemiologic investigations of thalidomide thalidomide (thəlĭd`əmĭd'), sleep-inducing drug found to produce skeletal defects in developing fetuses. The drug was marketed in Europe, especially in West Germany and Britain, from 1957 to 1961, and was thought to be so safe that , retinoic acid retinoic acid /ret·i·no·ic ac·id/ (ret?i-no´ik) an oxidized derivative of retinol, believed to be the form of vitamin A that plays a role in the development and growth of bone and in the maintenance of normal epithelial structures. (vitamin A vitamin A also called retinol Fat-soluble alcohol, most abundant in fatty fish and especially in fish-liver oils. It is not found in plants, but many vegetables and fruits contain beta-carotene (see ), maternal rubella rubella or German measles, acute infectious disease of children and young adults. It is caused by a filterable virus that is spread by droplet spray from the respiratory tract of an infected individual. , and radiation (O'Rahilly and Muller Mul·ler , Hermann Joseph 1890-1967. American geneticist. He won a 1946 Nobel Prize for the study of the hereditary effect of x-rays on genes. Mül·ler , Johannes Peter 1801-1858. 2001). For exposures during the first 2 weeks of gestation, few congenital abnormalities Noun 1. congenital abnormality - a defect that is present at birth birth defect, congenital anomaly, congenital defect, congenital disorder ablepharia - a congenital absence of eyelids (partial or complete) are observed because the teratogen teratogen /ter·a·to·gen/ (ter´ah-to-jen) any agent or factor that induces or increases the incidence of abnormal prenatal development.teratogen´ic te·rat·o·gen n. either damages most cells, resulting in cell and embryonic em·bry·on·ic or em·bry·on·al adj. Of, relating to, or being an embryo. Embryonic In the life cycle of the round worm, a very early life stage occurring within the uterus of the female round worm. death, or affects only a few cells that can be repaired without resultant birth defects birth defects, abnormalities in physical or mental structure or function that are present at birth. They range from minor to seriously deforming or life-threatening. A major defect of some type occurs in approximately 3% of all births. (Moore and Persaud 1998). After the first 2 weeks, the tissue or organ that is most susceptible to malformation malformation /mal·for·ma·tion/ (-for-ma´shun) 1. a type of anomaly. 2. a morphologic defect of an organ or larger region of the body, resulting from an intrinsically abnormal developmental process. is the part undergoing critical development when the teratogen is active. Exposures that occur later in gestation have a less drastic effect and are thought to primarily affect fetal growth. The strengths of this study include the large number of birth records, high quantity of exposure data (including some biweekly data), and the ability to evaluate multiple time periods of exposure to specific THMs and HAAs. By comparing subjects within the same community with respect to exposure levels, we may have reduced potential residual confounding. We also selected this community to minimize misclassification due to spatial variability within the distribution systems (Hinckley et al. 2005). Our study was limited by the use of birth records to ascertain individual exposure information. Maternal residence was identified from birth records to assign the appropriate water service, but residential mobility during pregnancy may have introduced exposure misclassification. Potential exposure misclassification could also have resulted from lack of information regarding exposures from inhalation inhalation /in·ha·la·tion/ (in?hah-la´shun) 1. the drawing of air or other substances into the lungs.inhala´tional 2. the drawing of an aerosolized drug into the lungs with the breath. 3. or dermal dermal /der·mal/ (der´mal) pertaining to the dermis or to the skin. der·mal or der·mic adj. Of or relating to the skin or dermis. exposure from showering, bathing, and washing. Exposure estimates were based on distribution system DBP concentrations and did not account for variability in personal habits affecting ingestion ingestion /in·ges·tion/ (-chun) the taking of food, drugs, etc., into the body by mouth. in·ges·tion n. 1. The act of taking food and drink into the body by the mouth. 2. , such as the use of bottled water (Zender et al. 2001). Finally, exposure misclassification could have resulted from exposures outside the service area (e.g., at work) of the designated water treatment system. In summary, despite toxicologic evidence of growth retardation after exposure to DBPs, few human studies have been conducted on this relationship. The pervasive nature of the exposure suggests that even small effects may be important. This work explored this relationship using seasonal variability and intracommunity comparisons to define a natural experiment. We improved on previous exposure assessments by considering total and individual THMs and HAAs, and multiple time periods of exposure in late gestation. Further studies are needed to confirm our observations for DBAA, TCAA, and DCAA as well as other relationships between DBPs and growth outcomes. We thank water facility departments in Tempe and Mesa, Arizona Mesa is a city in Maricopa County, Arizona and part of the Phoenix-Mesa-Scottsdale Metropolitan Area. It is the third-largest city in Arizona, after Phoenix and Tucson. Mesa is one of the United States' fastest-growing cities, and currently ranks as the 38th-largest. , for assistance in data collection and exposure assignment. We also thank J. Nuckols and the Environmental Health Advanced Systems Laboratory for support of this work. Funding was provided by the College Research Council, College of Veterinary Medicine veterinary medicine, diagnosis and treatment of diseases of animals. An early interest in animal diseases is found in ancient Greek writings on medicine. Veterinary medicine began to achieve the stature of a science with the organization of the first school in the and Biomedical Sciences Noun 1. biomedical science - the application of the principles of the natural sciences to medicine bioscience, life science - any of the branches of natural science dealing with the structure and behavior of living organisms , Colorado State University. 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To draw (air or smoke, for example) into the lungs by breathing; inspire. 2. chloroform in pregnant mice and their offspring. Toxicol Appl Pharmacol 50:515-522. Nieuwenhuijsen MJ, Toledano MB, Eaton NE, Fawell J, Elliott P. 2000. Chlorination disinfection byproducts in water and their association with adverse reproductive outcomes: a review. Occup Environ Med 57:73-85. O'Rahilly R, Muller F. 2001. Human Embryology and Teratology teratology /ter·a·tol·o·gy/ (ter?ah-tol´ah-je) that division of embryology and pathology dealing with abnormal development and the production of congenital anomalies.teratolog´ic ter·a·tol·o·gy n. . 3rd ed. New York:John Wiley John Wiley may refer to:
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Table 1. Distribution of births/fetal deaths and
TTHM and HAA5 concentrations [mean (range)] by
year for the Arizona study community.
No. of births/ TTHM HAA5
fetal concentrations concentrations
Year deaths ([micro]g/L) ([micro]g/L)
1998 9,117 56.9 (30.1-80.8) 31.8 (9.8-48.9) (a)
1999 9,571 45.8 (15.7-71.3) 20.6 (13.9-25.2) (a)
2000 9,976 48.9 (27.8-65.9) 17.0 (7.5-25.7)
2001 10,149 46.1 (16.6-68.0) 14.4 (4.2-22.3) (a)
2002 9,306 43.4 (7.8-70.3) 13.7 (3.1-23.0)
(a) Based on data from one facility.
Table 2. Characteristics of subjects and frequency
of intrauterine growth retardation, term low birth
weight, and preterm births [n (%)].
Study Intrauterine
population growth Term low
Characteristic (% of total) retardation (a) birth weight
Total births (% of 48,119 (100) 4,346 (9.5) 1,010 (2.1)
total)
Maternal age (years)
<20 5,609 (11.7) 671 (15.4) 150 (14.9)
20-29 28,366 (59.0) 2,536 (58.4) 573 (56.7)
[greater than or 14,076 (29.3) 1,135 (26.1) 285 (28.2)
equal to] 30
Unknown 68 (0.1) 4 (0.1) 2 (0.2)
Maternal race
Caucasian 43,026 (89.4) 4,085 (94.0) 844 (83.6)
African American 1,347 (2.8) 114 (2.6) 52 (5.1)
Native American 1,715 (3.6) 147 (3.4) 33 (3.3)
Other 1,701 (3.5) -- 64 (6.3)
Unknown 330 (0.7) -- 17 (1.7)
Maternal ethnicity
Non-Hispanic 30,803 (64.0) 2,741 (63.1) 623 (61.7)
Hispanic 15,140 (31.5) 1,453 (33.4) 340 (33.7)
Unknown 2,176 (4.5) 152 (3.5) 47 (4.7)
Maternal education
[greater than or 22,435 (46.6) 1,769 (40.7) 391 (38.7)
equal to] 1 year
of college
High school 13,427 (27.9) 1,266 (29.1) 281 (27.8)
graduate
< 12th grade 11,172 (23.2) 1,220 (28.1) 293 (29.0)
Unknown 1,085 (2.3) 91 (2.1) 45 (4.5)
Parity
0 18,886 (39.3) 2,023 (46.5) 440 (43.6)
1 14,341 (29.8) 1,180 (27.2) 291 (28.8)
2 8,348 (17.4) 653 (15.0) 158 (15.6)
3 3,728 (7.8) 282 (6.5) 67 (6.6)
[greater than or 2,724 (5.7) 198 (4.6) 53 (5.2)
equal to] 4
Unknown 92 (0.2) 10 (0.2) 1 (0.0)
Prenatal care
(Kessnerindex)
Adequate 36,271 (75.4) 3,059 (70.4) 663 (65.6)
Intermediate 9,117 (19.0) 941 (21.7) 243 (24.1)
Inadequate 2,731 (5.7) 346 (8.0) 104 (10.3)
Maternal smoking
No 44,139 (91.7) 3,741 (86.1) 856 (84.7)
Yes 3,409 (7.1) 540 (12.4) 136 (13.4)
Unknown 571 (1.2) 651 (1.5) 18 (1.8)
Maternal alcohol
No 47,176 (98.0) 4,233 (97.4) 976 (96.6)
Yes 291 (0.6) 39 (0.9) 11 (1.1)
Unknown 652 (1.4) 74 (1.7) 23 (2.3)
Very
Characteristic preterm birth Preterm birth
Total births (% of 564 (1.2) 4,008 (8.3)
total)
Maternal age (years)
<20 100 (17.7) 527 (13.1)
20-29 299 (53.0) 2,190 (54.6)
[greater than or 164 (29.1) 1,281 (32.0)
equal to] 30
Unknown 1 (0.2) 10 (0.3)
Maternal race
Caucasian 493 (87.4) 3,490 (87.1)
African American 41 (7.3) 173 (4.3)
Native American 7 (1.2) 146 (3.6)
Other 14 (2.5) 151 (3.8)
Unknown 91 (1.6) 48 (1.2)
Maternal ethnicity
Non-Hispanic 349 (61.9) 2,575 (64.2)
Hispanic 191 (33.9) 1,228 (30.6)
Unknown 24 (4.2) 205 (5.1)
Maternal education
[greater than or 217 (38.5) 1,779 (44.4)
equal to] 1 year
of college
High school 171 (30.3) 1,139 (28.4)
graduate
< 12th grade 153 (27.1) 970 (24.2)
Unknown 23 (4.1) 120 (2.99)
Parity
0 249 (44.1) 1,560 (39.9)
1 165 (29.3) 1,121 (28.0)
2 70 (12.4) 682 (17.0)
3 40 (7.1) 342 (8.5)
[greater than or 37 (6.5) 285 (7.1)
equal to] 4
Unknown 3 (0.5) 18 (0.5)
Prenatal care
(Kessnerindex)
Adequate 350 (62.1) 2,604 (65.0)
Intermediate 124 (22.0) 948 (23.7)
Inadequate 90 (16.0) 456 (11.4)
Maternal smoking
No 484 (85.8) 3,527 (88.0)
Yes 71 (12.6) 417 (10.4)
Unknown 9 (1.6) 64 (1.6)
Maternal alcohol
No 547 (97.0) 3,906 (97.5)
Yes 5 (0.9) 29 (0.7)
Unknown 12 (2.1) 73 (1.8)
(a) Does not include births at < 23 weeks' gestation for Caucasians,
African Americans, and Hispanics or births at less than 29 weeks'
gestation for Native Americans. Does not include Asian or "other"
births. For intrauterine growth retardation analyses, total number
of births in data set = 41,682.
Table 3. ORs and 95% CIs for the association between exposure to
DBPs averaged over the entire third trimester and intrauterine
growth retardation and term low birth weight.
Intrauterine growth
retardation (a)
DBP ([micro]g/L) Cases (n) OR (95% CI)
TTHMs (n) (c) 39,954 --
< 40 1,208 --
40-53 1,198 0.98 (0.90-1.07)
[greater than or equal to] 53 1,354 1.09 (1.00-1.18)
Continuous 3,760 1.00 (1.00-1.01)
Chloroform
< 10 1,216 --
10-16 1,258 1.02 (0.94-1.11)
[greater than or equal to] 16 1,286 1.01 (0.93-1.10)
Continuous 3,760 1.00 (1.00-1.01)
BDCM
< 13 1,251 --
13-18 1,173 0.93 (0.85-1.01)
[greater than or equal to] 18 1,336 1.03 (0.95-1.12)
Continuous 3,760 1.00 (1.00-1.01)
DBCM
< 12 1,288 --
12-16 1,164 0.96 (0.89-1.05)
[greater than or equal to] 16 1,308 1.01 (0.94-1.10)
Continuous 3,760 1.01 (1.00-1.01)
HAA5 (n) 14,350
< 15 462 --
15-19 466 1.00 (0.87-1.15)
[greater than or equal to] 19 513 1.08 (0.94-1.23)
Continuous 1,441 1.00 (1.00-1.01)
DBAA (n) (d) 9,576
< 4 322 --
4-5 301 1.04 (0.88-1.23)
[greater than or equal to] 5 347 1.12 (0.95-1.32)
Continuous 970 1.05 (0.98-1.12)
DCAA
<6 268 --
6-8 332 1.15 (0.97-1.36)
[greater than or equal to] 8 370 1.28 (1.08-1.51)
Continuous 970 1.05 (1.02-1.09)
TCAA
< 4 277 --
4-6 309 1.00 (0.84-1.18)
[greater than or equal to] 6 384 1.19 (1.01-1.41)
Continuous 970 1.04 (1.02-1.07)
Term low birth
weight (b)
DBP ([micro]g/L) Cases (n) OR (95% CI)
TTHMs (n) (c) 38,096
< 40 269 --
40-53 284 1.06 (0.89-1.25)
[greater than or equal to] 53 306 1.11 (0.94-1.31)
Continuous 859 1.00 (1.00-1.01)
Chloroform
< 10 265 --
10-16 312 1.18 (1.00-1.39)
[greater than or equal to] 16 282 1.04 (0.88-1.23)
Continuous 859 1.00 (1.00-1.01)
BDCM
< 13 274 --
13-18 290 1.05 (0.89-1.24)
[greater than or equal to] 18 295 1.04 (0.88-1.23)
Continuous 859 1.00 (0.99-1.02)
DBCM
< 12 286 --
12-16 269 1.00 (0.84-1.18)
[greater than or equal to] 16 304 1.05 (0.89-1.24)
Continuous 859 1.01 (0.99-1.02)
HAA5 (n) 13,981
< 15 97 --
15-19 124 1.26 (0.96-1.65)
[greater than or equal to] 19 126 1.25 (0.96-1.64)
Continuous 347 1.01 (1.00-1.02)
DBAA (n) (d) 9,312
< 4 70 --
4-5 71 1.01 (0.72-1.41)
[greater than or equal to] 5 103 1.49 (1.09-2.04)
Continuous 244 1.17 (1.03-1.32)
DCAA
<6 76 --
6-8 81 1.04 (0.75-1.43)
[greater than or equal to] 8 87 1.10 (0.80-1.50)
Continuous 244 1.02 (0.96-1.08)
TCAA
< 4 73 --
4-6 81 0.94 (0.68-1.30)
[greater than or equal to] 6 90 1.00 (0.73-1.37)
Continuous 244 1.01 (0.96-1.05)
(a) Adjusted for parity, education, smoking, and Kessner index.
(b) Adjusted for maternal age, parity, education, race, ethnicity,
smoking, and Kessner index. (c) Sample sizes used in analysis of
chloroform, BDCM, and DBCM were equal for third-trimester analyses.
(d) Sample sizes used in analysis of DBAA, DCAA, and TCAA were
equal for third-trimester analyses.
Table 4. ORs (95% CIs) for term low birth weight and intrauterine
growth retardation by gestation week (GW) according to level of
DBP exposure.
DBP ([micro]g/L) GW 25-28 GW 29-32
Intrauterine growth
retardation (a)
HAA5 (n) 14,350 14,953
< 14 --
14-19 1.02 (0.89-1.17) 1.00 (0.86-1.13)
[greater than or 1.12 (0.98-1.29) 1.11 (0.98-1.27)
equal to] 19
Continuous 1.01 (1.00-1.01) 1.01 (1.00-1.01)
DBAA (n) (b) 9,576 10,302
< 3 --
3.5-5 1.00 (0.84-1.18) 0.97 (0.82-1.14)
[greater than or 1.15 (0.98-1.35) 1.06 (0.91-1.24)
equal to] 5
Continuous 1.06 (1.01-1.12) 1.03 (0.99-1.08)
DCAA
< 6 --
6-8 1.00 (0.85-1.18) 1.06 (0.90-1.25)
[greater than or 1.04 (0.85-1.29) 1.11 (0.90-1.35)
equal to] 8
Continuous 1.02 (0.99-1.04) 1.03 (1.01-1.05)
TCAA
< 4 --
4-6 0.96 (0.81-1.14) 1.05 (0.85-1.24)
[greater than or 1.01 (0.86-1.19) 1.15 (0.98-1.34)
equal to] 6
Continuous 1.01 (1.00-1.03) 1.02 (1.01-1.04)
Term low birth
weight (c)
HAA5 (n) 13,981 14,593
< 14 --
14-19 0.91 (0.69-1.18) 1.04 (0.79-1.36)
[greater than or 1.05 (0.81-1.36) 1.30 (1.00-1.69)
equal to] 19
Continuous 1.01 (0.99-1.02) 1.01 (1.00-1.02)
DBAA (n) (b) 9,312 10,043
< 3 --
3.5-5 0.97 (0.69-1.35) 1.05 (0.77-1.45)
[greater than or 1.16 (0.86-1.58) 1.18 (0.87-1.61)
equal to] 5
Continuous 1.03 (0.94-1.12) 1.07 (0.98-1.17)
DCAA
< 6 --
6-8 0.80 (0.58-1.09) 0.84 (0.61-1.15)
[greater than or 0.87 (0.64-1.18) 0.99 (0.74-1.32)
equal to] 8
Continuous 1.01 (0.97-1.05) 1.02 (0.98-1.06)
TCAA
< 4 --
4-6 0.79 (0.57-1.09) 0.91 (0.67-1.24)
[greater than or 0.89 (0.66-1.20) 0.98 (0.73-1.33)
equal to] 6
Continuous 1.01 (0.98-1.05) 1.01 (0.98-1.04)
DBP ([micro]g/L) GW 33-36 GW 37-40
Intrauterine growth
retardation (a)
HAA5 (n) 15,414 14,929
< 14
14-19 0.93 (0.81-1.06) 0.99 (0.86-1.13)
[greater than or 1.00 (0.88-1.14) 0.98 (0.85-1.13)
equal to] 19
Continuous 1.00 (0.99-1.01) 1.00 (0.99-1.01)
DBAA (n) (b) 10,945 10,875
< 3
3.5-5 1.14 (0.97-1.34) 0.95 (0.81-1.12)
[greater than or 1.08 (0.93-1.27) 0.90 (0.77-1.06)
equal to] 5
Continuous 1.01 (0.96-1.06) 0.99 (0.94-1.04)
DCAA
< 6
6-8 0.92 (0.78-1.08) 1.00 (0.85-1.18)
[greater than or 1.03 (0.84-1.26) 1.27 (1.02-1.59)
equal to] 8
Continuous 1.03 (1.01-1.05) 1.03 (1.01-1.05)
TCAA
< 4
4-6 0.91 (0.78-1.07) 1.12 (0.95-1.32)
[greater than or 1.07 (0.92-1.24) 1.15 (0.98-1.35)
equal to] 6
Continuous 1.03 (1.01-1.05) 1.02 (1.01-1.04)
Term low birth
weight (c)
HAA5 (n) 15,195 15,780
< 14
14-19 1.04 (0.80-1.36) 1.12 (0.87-1.44)
[greater than or 1.20 (0.93-1.55) 1.08 (0.83-1.40)
equal to] 19
Continuous 1.00 (1.01-1.02) 1.00 (0.99-1.02)
DBAA (n) (b) 10,778 11,484
< 3
3.5-5 1.29 (0.94-1.79) 1.38 (1.02-1.86)
[greater than or 1.49 (1.10-2.02) 1.22 (0.90-1.66)
equal to] 5
Continuous 1.11 (1.01-1.21) 1.10 (1.01-1.20)
DCAA
< 6 --
6-8 0.94 (0.69-1.27) 0.98 (0.74-1.32)
[greater than or 0.98 (0.73-1.30) 0.91 (0.68-1.211
equal to] 8
Continuous 1.00 (0.96-1.04) 1.01 (0.97-1.05)
TCAA
< 4
4-6 1.05 (0.77-1.42) 1.15 (0.86-1.53)
[greater than or 1.05 (0.78-1.41) 0.93 (0.69-1.25)
equal to] 6
Continuous 1.00 (0.96-1.03) 1.00 (0.96-1.03)
DBP ([micro]g/L) GW 41-44
Intrauterine growth
retardation (a)
HAA5 (n) 2,634
< 14
14-19 1.22 (0.86-1.72)
[greater than or 0.91 (0.63-1.33)
equal to] 19
Continuous 1.00 (0.98-1.01)
DBAA (n) (b) 1,913
< 3
3.5-5 1.23 (0.82-1.85)
[greater than or 0.91 (0.60-1.40)
equal to] 5
Continuous 0.97 (0.85-1.10)
DCAA
< 6
6-8 1.51 (0.98-2.32)
[greater than or 1.41 (0.85-2.33)
equal to] 8
Continuous 1.03 (0.98-1.08)
TCAA
< 4
4-6 1.58 (1.02-2.46)
[greater than or 1.48 (0.96-2.31)
equal to] 6
Continuous 1.02 (0 98-106)
Term low birth
weight (c)
HAA5 (n) 2,755
< 14
14-19 0.74 (0.28-1.98)
[greater than or 1.03 (0.39-2.72)
equal to] 19
Continuous 0.99 (0.95-1.04)
DBAA (n) (b) 2,003
< 3
3.5-5 0.99 (0.34-2.85)
[greater than or 0.38 (0.10-1.43)
equal to] 5
Continuous 0.88 (0.62-1.23)
DCAA
< 6
6-8 0.45 (0.13-1.60)
[greater than or 0.93 (0.33-2.57)
equal to] 8
Continuous 0.94 (0.81-1.09)
TCAA
< 4
4-6 0.40 (0.11-1.30)
[greater than or 0.64 (0.23-1.79)
equal to] 6
Continuous 0.93 (0.80-1.09)
(a) Adjusted for parity, education, smoking, and Kessner index.
(b) Sample sizes used in analysis of DBAA, DCAA, and TCAA were
equal for each gestation age interval. (c) Adjusted for maternal
age, parity, education, race, ethnicity, smoking, and Kessner
index.
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