Pentachlorophenol and hydroxylated polychlorinated biphenyl metabolites in umbilical cord plasma of neonates from coastal populations in Quebec. (Children's Health).Concentrations of polychlorinated biphenyls polychlorinated biphenyls, (pol´ēklôr´  nā´tid bīfē´n (PCBs), hydroxylated
metabolites MetabolitesSubstances produced by metabolism or by a metabolic process. Mentioned in: Interactions of PCBs (HO-PCBs) and octachlorostyrene (4-HO-HpCS), and pentachlorophenol pentachlorophenol a wood preservative with great capacity to enter the body by any route, including percutaneously; causes weight loss, low milk production and general debility. (PCP PCP abbr. 1. phencyclidine 2. primary care physician Pneumocystis carinii pneumonia (PCP) ) were determined in umbilical cord umbilical cord (ŭmbĭl`ĭkəl), cordlike structure about 22 in. (56 cm) long in the pregnant human female, extending from the abdominal wall of the fetus to the placenta. plasma samples from three different regions of Quebec. The regions studied included two coastal areas where exposure to PCBs is high because of marine-food-based diets--Nunavik (Inuit people) and the Lower North Shore of the Gulf of St. Lawrence Noun 1. Gulf of St. Lawrence - an arm of the northwest Atlantic Ocean off the southeastern coast of Canada Gulf of Saint Lawrence Atlantic, Atlantic Ocean - the 2nd largest ocean; separates North and South America on the west from Europe and Africa on the east (subsistence fishermen)--and a southern Quebec urban center where PCB PCB: see polychlorinated biphenyl. PCB in full polychlorinated biphenyl Any of a class of highly stable organic compounds prepared by the reaction of chlorine with biphenyl, a two-ring compound. exposure is at background levels (Quebec City). The main chlorinated chlorinated /chlo·ri·nat·ed/ (klor´i-nat?ed) treated or charged with chlorine. chlorinated charged with chlorine. chlorinated acids some, e.g. phenolic phe·no·lic adj. Of, relating to, containing, or derived from phenol. n. Any of various synthetic thermosetting resins, obtained by the reaction of phenols with simple aldehydes and used as adhesives. compound in all regions was PCP. Concentrations of PCP were not significantly different among regions (geometric mean (mathematics) geometric mean - The Nth root of the product of N numbers. If each number in a list of numbers was replaced with their geometric mean, then multiplying them all together would still give the same result. concentration 1,670 pg/g, range 628-7,680 pg/g wet weight in plasma). The ratio of PCP to polychlorihated biphenyl biphenyl /bi·phen·yl/ (-fen´il) diphenyl. polychlorinated biphenyl (PCB) any of a group of chlorinated derivatives of biphenyl, used as heat-transfer agents and electrical insulators; they are congener congener /con·ge·ner/ (kon´je-ner) something closely related to another thing, as a member of the same genus, a muscle having the same function as another, or a chemical compound closely related to another in composition and exerting number 153 (CB153) concentration ranged from 0.72 to 42.3. Sum HO-PCB ([SIGMA]HO-PCBs) concentrations were different among regions, with geometric mean concentrations of 553 (range 238-1,750), 286 (103-788), and 234 (147-464) pg/g wet weight plasma for the Lower North Shore, Nunavik, and the southern Quebec groups, respectively. Lower North Shore samples also had the highest geometric mean concentration of sum PCBs (sum of 49 congeners; [SIGMA]PCBs), 2,710 (525-7,720) pg/g wet weight plasma. [SIGMA]PCB concentrations for Nunavik samples and southern samples were 1,510 (309-6,230) and 843 (290-1,650) pg/g wet weight plasma. Concentrations (log transformed) of [SIGMA]HO-PCBs and [SIGMA]PCBs were significantly correlated (r = 0.62, p < 0.001), as were concentrations of all major individual HO-PCB congeners and individual PCB congeners. In Nunavik and Lower North Shore samples, free thyroxine ([T.sub.4]) concentrations (log transformed) were negatively correlated with the sum of quantitated chlorinated phenolic compounds (sum PCP and [SIGMA]HO-PCBs; r = -0.47, p = 0.01, n = 20) and were not correlated with any PCB congeners or [SIGMA]PCBs. This suggests that PCP and HO-PCBs are possibly altering thyroid hormone Thyroid hormone Any of the chemical messengers produced by the thyroid gland, including thyrocalcitonin, a polypeptide, and thyroxine and triiodothyronine, which are iodinated thyronines. See Hormone, Thyrocalcitonin, Thyroid gland, Thyroxine status in newborns, which could lead to new rodevelopmental effects in infants. Further studies are needed to examine the effects of chlorinated phenolic compounds on thyroid hormone status in newborns. Key words: hydroxylated metabolites, pentachlorophenol, polychlorinated biphenyls, retinol retinol: see Vitamin A under vitamin. , thyroxine, umbilical cord plasma. Environ Health Perspect 110:411-417 (2002). [Online 12 March 2002] http://ehpnet1.niehs.nih.gov/docs/2002 /110p411-417sandau/abstract.html ********** Polychlorinated biphenyls (PCBs) have been well studied for possible effects on newborns and infants after it was determined that PCBs could effectively pass through the placental barrier placental barrier n. The semipermeable layer of tissue in the placenta that serves as a selective membrane to substances passing from maternal to fetal blood. and that they were associated with lower birth weights (1). Jacobson et al. (2) found that children exposed in utero in utero (in u´ter-o) [L.] within the uterus. in u·ter·o adj. In the uterus. in utero adv. to PCBs had delayed central nervous system functioning. Subsequent studies then confirmed that for this same cohort, reductions in cognitive function cognitive function Neurology Any mental process that involves symbolic operations–eg, perception, memory, creation of imagery, and thinking; CFs encompasses awareness and capacity for judgment were associated with higher in utero PCB exposure at 4 years of age (3), followed by lower IQs at 11 years of age (4). These studies seem to indicate a potential link between PCBs and neurodevelopment. Although many theories exist about how PCBs affect neurodevelopment, the main hypothesis involves disruption of thyroid hormone homeostasis homeostasis Any self-regulating process by which a biological or mechanical system maintains stability while adjusting to changing conditions. Systems in dynamic equilibrium reach a balance in which internal change continuously compensates for external change in a feedback (5). Thyroid hormones Thyroid Hormones Definition Thyroid hormones are artificially made hormones that make up for a lack of natural hormones produced by the thyroid gland. regulate neuronal proliferation and cell migration and differentiation, including control over when differentiation begins and when cell proliferation ends (6). Studies in the rat showed that transport of thyroid hormones to the brain requires thyroxine ([T.sub.4]) to pass through the blood-brain barrier blood-brain barrier n. Abbr. BBB A physiological mechanism that alters the permeability of brain capillaries so that some substances, such as certain drugs, are prevented from entering brain tissue, while other substances are allowed to bound to the thyroid hormone transport protein transthyretin (TTR TTR Transthyretin TTR Ticket To Ride (World Snowboard Tour) TTR Transformer Turns Ratio (electric power transmission and distribution) TTR Time To Repair TTR Time to Read ) (7). Although PCBs show some binding affinity for TTR (8), hydroxylated metabolites of PCBs (HO-PCBs) have much higher in vitro in vitro /in vi·tro/ (in ve´tro) [L.] within a glass; observable in a test tube; in an artificial environment. in vi·tro adj. In an artificial environment outside a living organism. binding affinities that can be as high as 12 times the binding affinity of the natural ligand [T.sub.4] (9). Binding to TTR is not limited to HO-PCBs. Other halogenated halogenated pertaining to a substance to which a halogen is added. halogenated salicylanilides see rafoxanide, clioxanide. phenolic compounds such as pentachlorophenol (PCP), halogenated phenols phenols (fēˑ·n  lz),n. , and tetrabromobisphenol A Tetrabromobisphenol A (TBBPA) is a brominated flame retardant. Synthesis TBBPA is a derivative of bisphenol A and is synthesized from this substance. Most commercial TBBPA products are of a relatively low purity, in fact containing a mixture of products brominated to (10,11) also have strong affinities for TTR. Recently, PCP was found to be the dominant phenolic compound in whole blood from Inuit (12) and Latvian and Swedish fish Swedish Fish are a type of quasi-gummi chewy candies shaped like fish. Originally colored red with a flavor unique to the candy, they are now also available in orange, yellow and green; the flavor varies with color. The fish come in two different sizes. eaters (13). Thus, we must consider the combined effect of halogenated phenolic compounds in plasma that exhibit similar toxicological properties to HO-PCBs (10,14,15). A recent review described the formation and retention of HO-PCBs and the main metabolites that have been previously identified in plasma (16). HO-PCBs decrease circulating levels of thyroid hormones in rats through competitive binding to TTR (17). TTR is also responsible for retinol transport by forming a dimer dimer /di·mer/ (di´mer) 1. a compound formed by combination of two identical molecules. 2. a capsomer having two structural subunits. di·mer n. 1. with retinol-binding protein. Thus, circulating retinol concentrations can also be affected by PCB and HO-PCB exposure (18). The fetus may be especially vulnerable to PCB and HO-PCB exposure. When fetal mice were exposed in utero to 4'-HO-CB79, a metabolite metabolite, organic compound that is a starting material in, an intermediate in, or an end product of metabolism. Starting materials are substances, usually small and of simple structure, absorbed by the organism as food. of polychlorinated biphenyl polychlorinated biphenyl or PCB, any of a group of organic compounds originally widely used in industrial processes but later found to be dangerous environmental pollutants. congener number 77 (CB77), both maternal and fetal plasma [T.sub.4] levels decreased significantly compared to controls (19). In this same study, fetal plasma had twice the 4'-HO-CB79 concentration of the maternal plasma (20). These experiments were recently repeated on pregnant rats orally exposed to 4-HO-CB107 (21), one of the main HO-PCBs found in human plasma (12,13). In that study, both maternal and fetal plasma concentrations of thyroid hormones were reduced by exposure to 4-HO-CB107. Fetal total [T.sub.4] concentrations decreased by 89% of that of the controls (21). The decreased plasma [T.sub.4] levels also decreased forebrain forebrain: see brain. and cerebellum cerebellum (sĕr'əbĕl`əm), portion of the brain that coordinates movements of voluntary (skeletal) muscles. It contains about half of the brain's neurons, but these particular nerve cells are so small that the cerebellum accounts for [T.sub.4] concentrations compared to controls (21), which may lead to a neurodevelopmental effect. PCP also decreases brain T4 availability in rats (22). Another interesting finding of the 4-HO-CB107 rat dosing study was an accumulation of 4-HO-CB107 in fetal plasma, liver, and brain (21). Thus, prenatal exposure to PCBs, HO-PCBs, and PCP may all lead to thyroid hormone disruption and possibly neurodevelopmental effects. Analysis of umbilical cord plasma is of special interest became it provides a direct indication of in utero exposure to developmental toxicants. PCBs have been measured previously in umbilical cord plasma (23,24), but the present study, to our knowledge, is one of the first studies to examine chlorinated phenolic compounds in this biological medium. Participants were from populations with different PCB exposures caused by differences in dietary habits. Retinol and thyroid hormone status [triiodothyronine triiodothyronine /tri·io·do·thy·ro·nine/ (tri?i-o?do-thi´ro-nen) one of the thyroid hormones, an organic iodine-containing compound liberated from thyroglobulin by hydrolysis. It has several times the biological activity of thyroxine. ([T.sub.3]), free [T.sub.4], thyroid-stimulating hormone thyroid-stimulating hormone (TSH): see thyrotropin. (TSH TSH thyroid-stimulating hormone; see thyrotropin. TSH abbr. thyroid-stimulating hormone Thyroid-stimulating hormone (TSH) ), and thyroxine-binding globulin thyroxine-binding globulin TBG An α2-migrating protein that is the main–70% carrrier protein for thyroxine/T4 and triiodothryonine/T3 (TBG TBG abbr. thyroid-binding globulin TBG thyroxine-binding globulin. TBG Thyroxine-binding globulin, see there )] were determined in samples from remote maritime populations, so the relationship between chlorinated phenolic compounds and these biological markers could be explored. Materials and Methods Samples. Plasma samples were obtained during various umbilical cord blood umbilical cord blood Transplantation A source of primitive and stem cells that can be used to reconstitute BM destroyed by aplastic anemia or by RT or chemotherapy for CA, lymphoproliferative malignancies. See Bone marrow transplantation, Stem cell therapy. surveys conducted from 1993 to 1996 in Quebec (25,26). These surveys took place in Nunavik (northern Quebec), the Lower North Shore of the Gulf of St. Lawrence, and southern Quebec (Quebec City; Figure 1). The population in the Quebec City area receives background PCB exposure similar to that of the general population of Canada, whereas the former two coastal areas comprise small settlements of people with unusually high PCB exposure. The traditional diet of Nunavik Inuit include seal and beluga beluga (bəl  `gə) or white whale, small, toothed northern whale, Delphinapterus leucas. The beluga may reach a length of 19 ft (5. blubber, which contain concentrations of PCBs in
the order of several milligrams per kilogram (27,28). The diet of the
Lower North Shore subsistence fish-eating population includes fish, sea
mammals, and seabird eggs (28). Ten samples from each region were
randomly selected for chlorinated phenolic compound and PCB residue
analysis from all samples collected during the surveys. Nunavik samples
were all from Inuit newborns, southern Quebec samples from Caucasian
newborns, and Lower North Shore samples from three Caucasians and seven
aboriginal neonates.[FIGURE 1 OMITTED] Standards and chemicals. PCBs are numbered according to according to prep. 1. As stated or indicated by; on the authority of: according to historians. 2. In keeping with: according to instructions. 3. the numbering scheme There are many different numbering schemes for assigning nominal numbers to entities. These generally require an agreed set of rules, or a central coordinator. The schemes can be considered to be examples of a primary key of a database management system table, whose table as described by Ballschmiter and Zell (29). Hydroxylated PCBs and their methoxylated derivatives are given the appropriate Ballschmiter PCB number according to their chlorination chlorination Public health Addition of chlorinated compounds to drinking water as disinfectants. Cf Ozonation. pattern. The HO- or MeO-functional groups are numbered thereafter, as described by Letcher et al. (16). Note that the numbering of two congeners in our previous publication (12) has changed: 4-HO-CB109 is now 4-HO-CB107, and 4-HO-CB107 is now 4'-HO-CB108. The following [sup.13][C.sub.12]-labeled standards were acquired from Wellington Laboratories (Guelph, ON, Canada) and were used as an internal recovery standard mixture: 4'-HO-CB120, 4'-HO-CB159, 4'-HO-CB172, and 4-HO-CB187. [[sup.13][C.sub.6]]PCP was purchased from Cambridge Isotope Laboratories (Andover, MA, USA) and was used for PCP quantitation. Labeled PCBs ([[sup.13][C.sub.12]]CB-118, 153, 180, and 194) were used as internal recovery standards, and [[sup.13][C.sub.12]]CB-138 was used as the performance standard for PCB analysis. [[sup.13][C.sub.12]]PCB standards were purchased from Cambridge Isotope Laboratories (Andover, MA, USA). The HO-PCB performance standard, 4'-Me-4-MeO-CB112, was a custom synthesis by B. Wightman (Carleton University, Ottawa, ON, Canada). All solvents were residue-analysis grade and purchased from EM Science (Gibbstown, NJ, USA). Merck Silica gel (Grade 60, 70-230 mesh, 60[Angstrom angstrom (ăng`strəm), abbr. Å, unit of length equal to 10−10 meter (0.0000000001 meter); it is used to measure the wavelengths of visible light and of other forms of electromagnetic radiation, such as ultraviolet ]) was purchased from Aldrich Chemical Company, Inc. (Milwaukee, WI, USA). Sulfuric acid sulfuric acid, chemical compound, H2SO4, colorless, odorless, extremely corrosive, oily liquid. It is sometimes called oil of vitriol. Concentrated Sulfuric Acid (trace-metal grade) was purchased from Fisher Scientific (Pittsburgh, PA, USA). Methodology and instrumentation. A thorough description of the methodology and instrumentation used for these analyses was described previously (12). Methodology was altered slightly for this study. Umbilical cord plasma samples ranged from 1.63 to 10.4 g and samples were spiked with 20 [micro]L [[sup.13][C.sub.12]]HO-PCB internal standard mixture (100 pg/[micro]L), 20 [micro]L [[sup.13][C.sub.6]]PCP (100 pg/[micro]L), and with 10 [micro]L [[sup.13][C.sub.12]]PCB internal standard mixture (2.5 ng/[micro]L) before extraction. The final volume for the phenolic compound fraction was 25 [micro]L and was spiked with 4'-Me-4-MeO-2,3,3',5,6-pentachlorobiphenyl (5 [micro]L) as performance standard before analysis. The PCB fraction was reduced to a final volume of 100 [micro]L and spiked with [[sup.13][C.sub.12]]CB138 performance standard (10 [micro]L) before analysis. Because of low levels of PCBs in the umbilical cord plasma samples, we analyzed PCBs by GC-MS GC-MS Gas chromatography-mass spectroscopy. See there. electron capture negative chemical ionization mode using the same mass spectrometry mass spectrometry or mass spectroscopy Analytic technique by which chemical substances are identified by sorting gaseous ions by mass using electric and magnetic fields. conditions as described previously for HO-PCBs (12). Only pentachlorinated PCB congeners and higher are reported because tetrachlorinated congeners and lower do not respond well to this type of detection. Congener-specific analysis using a characterized Aroclor 1:1:1 quantitation mixture allowed the quantitation of 49 PCB congeners in most of the samples. Retinol analysis was performed at the Quebec Toxicology Centre (Sainte-Foy, Quebec, Canada). Ethanol was added to the plasma sample to denature de·na·ture v. 1. To change the nature or natural qualities of. 2. To render unfit to eat or drink without destroying usefulness in other applications, especially adding methyl alcohol to ethyl alcohol. 3. proteins, and retinol was extracted from the resulting solution with hexane hexane /hex·ane/ (hek´san) a saturated hydrogen obtained by distillation from petroleum. hex·ane n. . The hexane extract was concentrated under vacuum (Speed-Vac) and redissolved in ethanol. Retinol was determined by reverse-phase high-pressure liquid chromatography (Waters Corp., Milford, MA, USA) using a C-18 column and a UV detector (325 nm). Free [T.sub.4], [T.sub.3], TSH, and TBG were measured by heterogeneous competition magnetic separation assay (Immuno 1 System; Bayer Diagnostics, Leverkusen, Germany), and TBG was determined by radioimmunoassay (DiaSorin, Stillwater, MN, USA). Thyroid hormones and TBG determinations were conducted at the Unite de Recherche re·cher·ché adj. 1. Uncommon; rare. 2. Exquisite; choice. 3. Overrefined; forced. 4. Pretentious; overblown. en Genetique Humaine (CHUL-CHUQ, Sainte-Foy, Quebec, Canada). Thyroid hormone measurements were performed on Nunavik and Lower North Shore samples but not on southern Quebec samples. All statistical analyses were completed with STATISTICA for Windows, version 5.1, from StatSoft, Inc. (Tulsa, OK, USA). Results Recoveries of the internal recovery standards ([[sup.13][C.sub.6]]PCP and [[sup.13][C.sub.12]]HO-PCBs and PCBs) were in the range of 75-104%. Mean recovery of phenolic internal standards was better than 87%. All concentrations were recovery corrected. With the Liliefors test for normal distribution, the chemical residue data were not normally distributed. Thus, all data (including retinol and thyroid hormone concentrations) were log transformed before statistical analysis. The regional concentration data are summarized using geometric means along with minimum and maximum values (Tables 1-3) Thirty compounds were characterized as HO-PCBs in the umbilical cord plasma samples. Concentrations of PCP and identified HO-PCB congeners are listed in Table 1. Two congeners, 4-HO-CB 107 and 4'-HO-CB108, coelute and were quantitated as a single peak. The peak is likely 4-HO-CB107, as demonstrated in previous studies (16,30). [SIGMA]HO-PCBs represents a sum of all identified HO-PCBs and all compounds characterized as HO-PCBs. Unidentified HO-PCBs were quantitated using relative response factors as described previously (12). [SIGMA]HO-PCBs were analyzed for regional differences by multiple analysis of variance. Lower North Shore samples had the highest mean concentration of [SIGMA]HO-PCBs, which was significantly higher than concentrations in southern Quebec samples using the Sheffe test (p = 0.01). The Nunavik samples were not significantly different from southern samples (p = 0.8) or from Lower North Shore samples (p = 0.06). PCP concentrations were highest in Nunavik samples but were not significantly different among regions. We also found another compound recently identified as a major chlorinated phenolic compound in polar bear plasma, 4-hydroxy-heptachlorostyrene (4-HO-HpCS) (31), in the human umbilical cord plasma samples (Table 1). This compound was determined in all umbilical cord plasma samples. No quantitative standard was available at the time of analysis, so we estimated concentrations of 4-HO-HpCS using the average heptachlorinated MeO-PCB response factor. The geometric mean concentrations in Nunavik and Lower North Shore samples were about six times higher than in southern Quebec samples. Forty-nine PCB congeners with 5 or more chlorines were above the detection limit in most of the umbilical cord plasma samples. Concentrations of all 49 PCBs and [SIGMA]PCBs (sum of all congeners) are listed in Table 2. The ratio of [SIGMA]HO-PCBs to [SIGMA]PCBs is given in Table 1. [SIGMA]PCBs were highest in Lower North Shore plasma samples and Nunavik samples, but only Lower North Shore samples were significantly different (p = 0.01) from southern Quebec samples by the Sheffe test. The mean ratio of [SIGMA]HO-PCB metabolites to PCBs was highest in southern Quebec samples and lowest in Nunavik samples, but the ratio was not statistically different among regions. [SIGMA]HO-PCBs and [SIGMA]PCBs concentrations were highly correlated in umbilical cord plasma (r = 0.69, p < 0.001), as shown in Figure 2. Fractions of the main identified HO-PCBs of [SIGMA]HO-PCBs are shown in Figure 3. The PCBs from which the main metabolites may be formed are listed above each metabolite in Figure 3. [FIGURES 2-3 OMITTED] Figure 4 shows the correlation between one of the main HO-PCBs, 4-HO-CB146, and its potential precursor PCBs. The metabolite was significantly correlated (p < 0.001) with all possible precursor PCBs and was significantly correlated with many non-related PCBs (not shown). [FIGURE 4 OMITTED] Mean retinol concentrations were lowest in Nunavik samples and highest in southern Quebec samples, but differences between the regions were not statistically significant (Table 3). No significant correlations were observed between concentrations of retinol and any individual HO-PCB or PCB congeners, [SIGMA]HO-PCBs, sum of all chlorinated phenolic compounds, or [SIGMA]PCBs. Plasma concentrations of [T.sub.3], free [T.sub.4], TSH, and TBG were not significantly different between Lower North Shore and Nunavik samples (Table 3). Concentrations of main HO-PCBs and PCBs were not significantly correlated with thyroid hormone markers. In contrast, PCP concentrations were negatively correlated with [T.sub.3] (r = -0.55, p = 0.01), TBG (r = -0.44, p = 0.05), and free [T.sub.4] levels (r = -0.51, p = 0.02). Figure 5 shows the statistically significant inverse correlation (r = -0.47, p = 0.01) between free [T.sub.4] concentrations and log-transformed sum of all chlorinated phenolic compounds (sum of PCP and [SIGMA]HO-PCBs). The relationship was not improved using log-free [T.sub.4] and log-sum molar concentration of phenolic compounds. The sum of all chlorinated phenolic compounds was also negatively associated with [T.sub.3] concentrations (r = -0.48, p = 0.03). Concentrations of [SIGMA]PCBs and [SIGMA]HO-PCBs were both negatively correlated with TSH concentrations (r = -0.46, p = 0.04 and r = -0.45, p = 0.04, respectively). [FIGURE 5 OMITTED] Discussion Hydroxylated metabolites and other chlorinated phenolic compounds, to our knowledge, have never been examined in umbilical cord plasma. We found that PCP was the most abundant phenolic compound in all three regions, representing an average of 78%, 66%, and 82% of the concentration of the sum of all quantitated chlorinated phenolic compounds in the Nunavik, Lower North Shore, and southern Quebec groups, respectively. Mean PCP concentrations were similar among groups, and individual values ranged from 628 to 7,680 pg/g wet weight. We previously reported PCP as the dominant chlorinated phenolic compound in blood samples from Nunavik and southern Quebec adults (12). Thus, PCP may supersede To obliterate, replace, make void, or useless. Supersede means to take the place of, as by reason of superior worth or right. A recently enacted statute that repeals an older law is said to supersede the prior legislation. HO-PCBs as the chlorinated phenolic compound of highest concern in humans. PCP and its salts have been used extensively as wood preservatives, biocides, and disinfectants (32). PCP use has been curtailed since the late 1970s and has been banned in some countries, such as Sweden (1977) and Germany (1987) (32). The use of PCP has been restricted in Canada since 1981. The main exposure to PCP for nonoccupationally exposed individuals is through the diet (33). Another significant source of PCP may occur through the metabolism of hexachlorobenzene (34). Plasma is the most important compartment for PCP storage. In dosed rats, 99% of PCP is bound to plasma proteins (35). In human volunteers, the percentage of PCP bound to plasma proteins was estimated to be 96% (36). PCP can induce deleterious effects on several organs or tissues. Increased lymphocyte lymphocyte: see blood; immunity. lymphocyte Type of leukocyte fundamental to the immune system, regulating and participating in acquired immunity. Each has receptor molecules on its surface that bind to a specific antigen. responses were noted in patients with high PCP blood levels (37). PCP can be metabolized to reactive quinone quinone Any member of a class of cyclic organic compounds comprising a six-membered unsaturated ring (see saturation) to which two oxygen atoms are bonded as carbonyl groups (−C=O; see functional group). metabolites (38) with possible covalent co·va·lent adj. Of or relating to a chemical bond characterized by one or more pairs of shared electrons. binding to crude liver homogenates and isolated liver proteins in vitro (39). PCP has twice the affinity of [T.sub.4] to TTR (10) and has been shown to decrease circulating [T.sub.4] levels in rams exposed from conception (40). PCP also affects thyroid hormone metabolism by competitively inhibiting iodothyronine sulfation in vitro (41). In the present study, the sum of plasma concentrations of phenolic compounds, the major part being PCP, were negatively correlated to free [T.sub.4] and [T.sub.3] plasma levels. This suggests that PCP and perhaps other chlorinated phenolic compounds can alter thyroid hormone status in newborns, which in turn could lead to adverse neurodevelopmental effects in infants. Another chlorinated phenolic compound recently identified by our laboratory in polar bear plasma, 4-HO-HpCS (31), was also found in all umbilical cord plasma samples analyzed. This is the first time this compound has been shown to be present in human plasma. The likely precursor for this compound is octachlorostyrene, all industrial byproduct by·prod·uct or by-prod·uct n. 1. Something produced in the making of something else. 2. A secondary result; a side effect. Noun 1. . The fact that lower concentrations of 4-HO-HpCS were found in the southern Quebec group than in the Nunavik and Lower North Shore groups suggests that the likely source of exposure is the consumption of species from the marine food chain. Sandau et al. (31) showed that this compound had air affinity similar to [T.sub.4] for binding to TTR, which is slightly less than PCP (10) and lower than most HO-PCBs that have been determined (42). Concentrations of [SIGMA]HO-PCBs in umbilical plasma were highest in the Lower North Shore samples. More than 30 compounds were identified as HO-PCBs, of which 11 were positively identified with authentic standards. Three more HO-PCBs found in humans (16) were tentatively identified but could not be confirmed because no authentic standards were available. The main metabolite in 27 of the 30 samples was 4-HO-CB187. This compound was also the dominant metabolite in fish eaters from Sweden, Black-footed and Laysan albatross, and polar bear (13,43,44). Two possible parent PCBs can form 4-HO-CB187 through two different hydroxylation hydroxylation addition of -OH groups to a molecule. mechanisms. The first involves the direct insertion (45) of a hydroxyl group hydroxyl group (hīdrŏk`sĭl), in chemistry, functional group that consists of an oxygen atom joined by a single bond to a hydrogen atom. An alcohol is formed when a hydroxyl group is joined by a single bond to an alkyl group or aryl group. onto the para position of CB187. Direct insertion has been demonstrated to occur in in vitro metabolism studies of halobenzenes (46) and CB52 (47). CB187 is an abundant congener found in biota biota /bi·o·ta/ (bi-o´tah) all the living organisms of a particular area; the combined flora and fauna of a region. bi·o·ta n. The flora and fauna of a region. and accounted for a mean of 3.4% of the [SIGMA]PCBs in all the umbilical cord plasma samples. It is found as a small percentage (0.54%) in the Aroclor 1254 mixture, but is more abundant in Aroclor 1260 (5.4%) (48). The second mechanism of oxidation is the formation of a 3,4 (meta-para)-epoxide in CB183 followed by a 3,4 shift of chlorine to the meta position similar to the National Institutes of Health (NIH) shift of [sup.2]H first described by Guroff et al. (49). Epoxide epoxide /epox·ide/ (e-pok´sid) an organic compound containing a reactive group resulting from the union of an oxygen atom with two other atoms, usually carbon, that are themselves joined together. formation in the metabolism of PCBs has been demonstrated in in vitro studies (50) as well as in vivo in vivo /in vi·vo/ (ve´vo) [L.] within the living body. in vi·vo adj. Within a living organism. in vivo adv. studies (17) using CB77 as substrate. CB183 composed a mean of 0.8% of the [SIGMA]PCBs in the umbilical cord plasma and constitutes approximately 0.2% and 2.4% of Aroclor 1254 and 1260 mixtures, respectively (48). Interestingly, the major PCB metabolite in umbilical cord plasma, 4-HO-CB187, is formed from PCBs that make up a small percentage of the [SIGMA]PCBs in the samples. The second most abundant metabolite in umbilical cord plasma was 4-HO-CB146. This metabolite can be formed by direct insertion onto CB146 or by NIH shift of chlorine in the metabolism of CB138 or CB153. These three parent PCBs compose a large percentage of the [SIGMA]PCBs (between 11 and 47%) quantitated in all the samples. CB153 (mean 15% of [SIGMA]PCBs) and CB138 (mean 8.3% of [SIGMA]PCBs) are the two most abundant PCBs determined in the plasma samples and are major components in Aroclor mixtures (48). All three potential parent PCBs were significantly (p < 0.001) correlated with 4-HO-CB 146 (Figure 4). The third most abundant metabolite was 4-HO-CB107, which can be formed from CB107 (direct insertion), CB105 (NIH-Cl shift), or CB118 (NIH-Cl shift). Both CB105 and CB118 are major congeners in Aroclor 1254, composing 5.2% and 10.5% of the total (48). CB107 is a minor congener in Aroclor 1254 (0.6%), and it is rarely found in environmental samples, including these umbilical cord plasma samples. Concentrations of the potential parent PCBs CB105 (mean 1.3% of [SIGMA]PCBs) and CB118 (mean 4.8% of [SIGMA]PCBs) were significantly correlated (r = 0.69, r = 0.81, respectively; p < 0.001) with 4-HO-CB 107 concentrations. In contrast to our study results, 4-HO-CB107 was previously found to be the main metabolite in adult Inuit whole blood, Latvian fish consumers, Baltic seals, white-tailed eagles, and rats dosed with Aroclor 1254 (12,13,16,30). The relationship between metabolites and their potential precursor PCBs could not be resolved further using multiple-step regression analysis In statistics, a mathematical method of modeling the relationships among three or more variables. It is used to predict the value of one variable given the values of the others. For example, a model might estimate sales based on age and gender. (forward or backward). Concentrations of major metabolites were highly correlated with all PCBs, even unrelated congeners. Therefore, it is not possible from the present data to determine which congeners are the precursors of the metabolites--that is, the relative importance of NIH chlorine shift to direct insertion. Hydroxylated PCB patterns vary among individuals (12,13). This variation can be caused by selective retention or selective formation of metabolites or by differences in PCB exposure. The retention of specific HO-PCBs is probably similar for all humans. The main structural requirement for retention is the capability to bind to to contract; as, to bind one's self to a wife s>. See also: Bind TTR (9). This requirement is thought to involve a hydroxyl group with adjacent chlorines (42). The hydroxyl group is often in the para position of the biphenyl ring, but not exclusively, because meta-substituted metabolites are also found in plasma. Humans have varying concentrations of TTR in plasma, and some genetic abnormalities are known (51). Generally, concentrations are in excess molar concentration to HO-PCBs (12). Thus, the main determinant of the pattern of HO-PCBs in blood is likely the formation of metabolites from the parent PCB congeners. It was interesting to note that the geometric mean ratio of [SIGMA]HO-PCBs to [SIGMA]PCBs concentrations was similar (~0.2) among regions. The ratio was twice that found in a previous study involving whole blood of Canadian Inuit (0.11) (12). Because the relationship of the log-transformed concentrations in umbilical cord plasma had a slope of between 0.5 and 0.6 (Figures 2 and 4), the ratio of metabolites to PCBs decreased with increasing PCB concentrations. The range was from approximately 0.4 at low PCB concentrations (500 pg/g; Figure 2) to approximately 0.1 at high PCB concentrations (5,000 pg/g; Figure 2), similar to that found in adult whole blood. There was no apparent effect of PCB concentration on the ratio of metabolites to PCBs in adult whole blood (15). The generally higher ratio in umbilical cord plasma samples may reflect the difference in composition of fetal and adult blood. For example, umbilical cord plasma has approximately half the lipid content and less transthyretin than adult plasma (52). It has been shown previously that PCBs are most concentrated in plasma lipoproteins Lipoproteins The packages in which cholesterol and triglycerides travel throughout the body. Mentioned in: Lipoproteins Test lipoproteins (lip´ōprō´tēns), n. (53). Another possible explanation for the differences in the metabolite/PCB ratio in adult and fetal blood could involve enhanced placental placental pertaining to or emanating from placenta. placental barrier the placental separation of maternal and fetal blood which varies in its structure and permeability between the species. transfer of HO-PCBs from the mother. The transfer of PCB metabolites from dosed mice to the fetus was tested b3, Sinjari et al. (20). They showed that 4'-HO-CB79 concentrations in fetal plasma were twice that of the maternal plasma, 24 hr after exposure, indicating enhanced transport of the metabolite, which likely occurs through binding to TTR. When the individual chemical residue data were compared to thyroid hormone markers, only PCP concentration was significantly related to [T.sub.3], free [T.sub.4], and TBG concentrations. PCP has twice the affinity of [T.sub.4] to TTR (10) and can affect thyroid hormone concentrations in rats (54). PCP has also been shown to affect thyroid hormone metabolism by competitively inhibiting iodothyronine sulfation in vitro (41). When concentrations of all phenolic compounds were summed and correlated with the thyroid hormone markers, only [T.sub.3] and free [T.sub.4] concentrations were negatively associated, and the significance of the regression increased. The negative association between free [T.sub.4] and the sum of all phenolic compounds is in agreement with the theory that HO-PCBs and other chlorinated phenolic compounds disrupt thyroid hormone transport through the common mechanism of binding to TTR. In addition to binding to TTR, halogenated phenolic compounds may disrupt thyroid hormone metabolism (14,41). Morse et al. (55) found that both maternal and neonatal rats showed decreased total and free [T.sub.4] levels with exposure to CB169 and/or CB77 in a dose-dependent manner. They concluded that fetal [T.sub.4] levels were affected by both reduced transplacental transplacental /trans·pla·cen·tal/ (-plah-sen´tal) through the placenta. trans·pla·cen·tal adj. Relating to or involving passage through or across the placenta. delivery of [T.sub.4] and increased [T.sub.4] metabolism by the induced glucuronyltransferase enzymes. Darnerud et al. (56) also demonstrated fetal reduction in total [T.sub.4] and free [T.sub.4] when pregnant mice were dosed with CB77. Furthermore, Dutch infants showed decreased free and total [T.sub.4] levels with increased PCB/dioxinlike compound exposure (23). Thus, many studies indicate that [T.sub.4] concentrations can be decreased by exposure to PCBs, and this study supports the theory that HO-PCBs, and perhaps other halogenated phenolic compounds, may be partly responsible for this decrease. TTR has been shown to be important in [T.sub.4] transport in cerebral spinal fluid spinal fluid n. See cerebrospinal fluid. (7). If chlorinated phenolic compounds can significantly alter plasma levels of TTR-bound [T.sub.4], this may lead to brain thyroid hormone deficiencies in utero, possibly affecting brain development (57). TTR is also important in thyroid hormone transport across the placental barrier (58). Maternal sources of thyroid hormones are thought to influence fetal brain development (59). The binding of metabolites to TTR may also improve transport of halogenated phenolic compounds across the placenta placenta (pləsĕn`tə) or afterbirth, organ that develops in the uterus during pregnancy. It is a unique characteristic of the higher (or placental) mammals. In humans it is a thick mass, about 7 in. , as has been shown in mice (19). Thus, phenolic compounds may be able to disrupt maternal sources of thyroid hormones, penetrate into fetal circulation fetal circulation Embryology Prenatal circulation which bypasses the lung and right heart, and is returned to the systemic circulation at the aorta via a patent ductus arteriosus, which usually closes at or shortly after birth, after which the blood flows to the lungs , and disrupt local thyroid hormone supply in the developing fetus. The potential of PCP and HO-PCBs to disrupt thyroid hormone homeostasis in the developing fetus warrants further investigation to confirm the effects observed in the present study. A study is currently underway that will examine the relationship between halogenated phenolic compounds, thyroid hormones, and retinol concentrations in newborns from a larger cohort.
Table 1. Concentrations (picograms per gram wet weight plasma) of
halogenated phenolic compounds and [SIGMA]PCBs in umbilical cord
plasma from three regions in Quebec (n = 10 for each region).
Lower North
Nunavik Shore
Compound GM Min Max GM Min
PCP 1,870 889 7,680 1,430 628
4-HO-HpCS 31 3 177 34 9
HO-PCBs
4-HO-CB187 47 13 155 95 54
4-HO-CB146 37 4 134 81 16
3-HO-CB153 19 4 65 23 10
4-HO-CB107/ 12 3 44 49 6
4'-H0-C8108
3'-HO-CB138 10 3 35 22 9
4'-HO-CB172 10 3 43 20 8
4,4'-diHO-CB202 (a) 6 3 15 5 1
3-HO-CB187 4 ND 34 7 2
4-HO-CB193 3 1 17 3 1
4'-HO-CB120 2 1 4 7 3
4'-HO-CB208 (a) 2 1 5 3 1
3'-HO-CB180 2 ND 14 5 1
4'-HO-CB130 1 ND 3 2 ND
4'-HO-CB199 (a) < 1 ND 4 < 1 ND
Sum HO-PCBs 286 103 788 553 238
HO-PCBs:PCBs 0.19 0.08 0.41 0.20 0.08
Lower
North
Shore Southern Quebec
Compound Max GM Min Max
PCP 3,640 1,740 1,020 4,090
4-HO-HpCS 139 5 2 21
HO-PCBs
4-HO-CB187 250 28 10 97
4-HO-CB146 507 12 4 58
3-HO-CB153 74 6 3 14
4-HO-CB107/ 168 11 3 43
4'-H0-C8108
3'-HO-CB138 92 5 3 16
4'-HO-CB172 75 4 1 11
4,4'-diHO-CB202 (a) 13 4 3 17
3-HO-CB187 21 1 ND 3
4-HO-CB193 8 1 0 5
4'-HO-CB120 20 2 ND 6
4'-HO-CB208 (a) 11 1 ND 3
3'-HO-CB180 23 1 ND 3
4'-HO-CB130 27 1 ND 3
4'-HO-CB199 (a) 7 < 1 ND < 1
Sum HO-PCBs 1,750 234 147 464
HO-PCBs:PCBs 0.56 0.19 0.04 0.46
Abbreviations: GM, geometric mean; Max, maximum; Min, minimum; ND,
not detected.
(a) Tentative identifications based on information in the review
by Letcher et al. (16). Note that 4-HO-CB107 and
4'-HO-CB108 coelute and were quantitated as a single peak.
The 4-hydroxy-heptachlorostyrene (4-HO-HpCS) was quantitated using
relative response factors from the heptachlorinated MeO-PCB standards.
Table 2. Concentrations (picograms per gram wet weight plasma)
of 49 PCB congeners in umbilical cord plasma from three regions
in Quebec (n = 10 for each region).
Lower North
Nunavik Shore
Congener GM Min Max GM Min
CB92 9 ND 60 7 ND
CB84 27 5 141 36 6
CB101/90 49 11 262 87 13
CB99 100 16 1,120 174 17
CB97 10 ND 167 12 ND
CB87 28 5 236 63 8
CB85 6 2 115 14 2
CB110 42 8 403 79 10
CB118 67 19 402 155 30
CB105 19 6 300 37 7
CB136 13 1 316 15 2
CB151 7 3 34 11 4
CB144/135 17 ND 97 27 ND
CB149 20 9 71 33 ND
CB134 8 1 35 11 2
CB146 23 5 98 54 15
CB153 262 49 1,340 430 107
CB141 3 2 20 5 3
CB130 6 2 20 9 3
CB137 4 1 13 6 2
CB138/163 157 36 712 232 62
CB158 5 2 18 8 2
CB178 1 ND 9 1 ND
CB128 7 3 27 16 6
CB156 27 5 94 40 17
CB157 8 2 28 17 7
CB179 2 1 5 2 ND
CB176 1 ND 2 1 ND
CB178 2 < 1 27 1 < 1
CB187/182 39 7 146 102 24
CB183 14 4 135 23 6
CB185 < 1 < 1 2 1 ND
CB174 3 2 12 4 2
CB177 5 2 13 10 4
CB171 3 1 7 6 2
CB172 2 < 1 10 6 2
CB180 118 33 663 146 43
CB193 3 < 1 53 5 1
CB191 < 1 < 1 5 1 < 1
CB170/190 21 4 74 39 13
CB202 4 1 21 5 3
CB200 1 < 1 22 2 1
CB199 1 ND 4 1 ND
CB201 4 1 17 10 2
CB196/203 8 2 26 33 7
CB195 3 1 28 5 1
CB194 9 2 23 17 7
CB206 3 1 10 6 3
CB209 1 < 1 1 1 < 1
Sum PCBs 1,510 309 6,230 2,710 525
Lower
North
Shore Southern Quebec
Congener Max GM Min Max
CB92 167 9 ND 13
CB84 251 16 ND 31
CB101/90 786 44 17 181
CB99 1,630 38 ND 116
CB97 232 8 ND 19
CB87 436 13 ND 27
CB85 150 6 ND 86
CB110 709 44 18 502
CB118 673 35 9 81
CB105 155 11 2 31
CB136 651 12 1 536
CB151 68 8 ND 14
CB144/135 713 13 ND 22
CB149 96 30 14 103
CB134 86 3 ND 18
CB146 178 11 6 54
CB153 1,350 104 30 199
CB141 13 5 1 8
CB130 30 2 ND 4
CB137 15 2 ND 3
CB138/163 704 54 11 110
CB158 17 3 1 6
CB178 3 1 ND 1
CB128 47 4 ND 7
CB156 104 11 2 19
CB157 45 5 ND 8
CB179 4 2 ND 5
CB176 1 1 ND 2
CB178 20 1 ND 4
CB187/182 297 38 13 226
CB183 57 7 2 12
CB185 1 1 ND 2
CB174 9 6 1 11
CB177 18 4 1 7
CB171 13 2 1 4
CB172 14 1 ND 3
CB180 501 40 8 84
CB193 23 1 < 1 4
CB191 7 1 < 1 2
CB170/190 87 13 3 22
CB202 10 2 ND 3
CB200 4 1 ND 2
CB199 4 2 ND 6
CB201 31 7 4 11
CB196/203 113 15 6 95
CB195 32 2 ND 2
CB194 55 11 2 21
CB206 12 1 ND 2
CB209 2 < 1 ND 1
Sum PCBs 7,720 843 290 1,650
Abbreviations: GM, geometric mean; Max, maximum; Min, minimum; ND,
not detected.
Table 3. Concentrations of retinol, thyroid hormones, and TBG in
umbilical cord plasma samples from three regions in Quebec (n = 10
for each region).
Lower North
Nunavik Shore
GM Min Max GM Min
Retinol ([micro]g/L) 160 61 250 160 89
F[T.sub.4] (pmol/L) 16 13 22 17 9.6
[T.sub.3] (nmol/L) 0.64 0.45 1.20 0.49 0.20
TSH ([micro]mol/L) 7.7 3.9 19 6.7 3.9
TBG (nmol/L) 920 590 1,300 880 620
Lower
North
Shore Southern Quebec
Max GM Min Max
Retinol ([micro]g/L) 290 190 110 330
F[T.sub.4] (pmol/L) 21 NA NA NA
[T.sub.3] (nmol/L) 0.78 NA NA NA
TSH ([micro]mol/L) 15 NA NA NA
TBG (nmol/L) 1,300 NA NA NA
Abbreviations: GM, geometric mean; Max, maximum; NA, not analyzed.
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Lu M-H M-H Miami Herald (Miami, FL newspaper) , Anderson RR. Thyroxine secretion rates during pregnancy in the rat. Endocr Res 20:343-364 (1994). (59.) Porterfield SP, Hendrich CE. The role of thyroid hormones in prenatal and neonatal neurological development--current perspectives. Endocr Rev 14:94-106 (1993). Courtney D. Sandau, (1) Pierre Ayotte, (2) Eric Dewailly, (2) Jason Duffe, (3) and Ross J. Norstrom (1,3) (1) Centre for Analytical and Environmental Chemistry, Department of Chemistry, Carleton University, Ottawa, Ontario, Canada; (2) Unite de Recherche en Sante Publique, Centre de Recherche du CHUL-Centre Hospitalier Universitaire de Quebec and Universite Laval, Beauport, Quebec, Canada; (3) Environment Canada, Canadian Wildlife Service The Canadian Wildlife Service or CWS (French: Service canadien de la faune, SCF) is an agency of the Government of Canada, administered by the Department of the Environment, also known as Environment Canada. , National Wildlife Research Centre, Hull, Quebec, Canada Address correspondence to C. Sandau, Centers for Disease Control and Prevention Centers for Disease Control and Prevention (CDC), agency of the U.S. Public Health Service since 1973, with headquarters in Atlanta; it was established in 1946 as the Communicable Disease Center. , National Center for Environmental Health, 4770 Buford Highway NE, Mail stop F17, Atlanta, GA 30341-3724 USA. Telephone: (770) 488-4299. Fax: (770) 488-4609. E-mail: csandau@cdc.gov The project was funded by the Canadian Chlorine Coordinating Committee (C4) and the Canadian Chemical Producers Association. Funding for cord blood studies was provided by Hydro-Quebec, Indian and Northern Affairs Canada The Department of Indian Affairs and Northern Development (FIP: Indian and Northern Affairs Canada, French: Affaires indiennes et du Nord Canada, DIAND (Northern Contaminants Program), and Health Canada (St. Lawrence Vision 2000 Health Program). Informed consent was obtained from all volunteers prior to their participation in this study. Received 16 May 2001; accepted 24 July 2001. |
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