Developmental Perchlorate Exposure and Synaptic Transmission in Hippocampus

In “Developmental Exposure to Perchlorate Alters Synaptic Transmission in Hippocampus of the Adult Rat,” Gilbert and Sui (2008) reported results of exposure of pregnant rat dams to perchlorate in drinking water, with the purpose of evaluating neurologic development in rat pups after in utero exposure to perchlorate.


Perspectives | Correspondence
Developmental Perchlorate Exposure and Synaptic Transmission in Hippocampus doi:10.1289/ehp.0800532 In "Developmental Exposure to Perchlorate Alters Synaptic Transmission in Hippocampus of the Adult Rat," Gilbert and Sui (2008) reported results of exposure of pregnant rat dams to perchlorate in drinking water, with the purpose of evaluating neurologic develop ment in rat pups after in utero exposure to perchlorate.
We cannot agree with the authors' con clusion that their findings indicate that neurologic impairment is associated with modest degrees of thyroid hormone insuf ficiency and support previous animal studies of neuro developmental sequelae associated with low levels of perchlorate exposure. Also, we do not agree that their data (Gilbert and Sui 2008) "provide evidence in a rodent model that modest degrees of thyroid hormone reduction induced by per chlorate result in persistent decrements in brain function." The "association" of the electro physio logic anomalies meas ured in the hippo campus [interpreted by Gilbert and Sui (2008) as "neurologic impairment" or "per sistent decrements in brain function"] with "modest degrees of thyroid hormone insuf ficiency" in the pups is not, in our opin ion, a credible interpretation of the authors' results, because the evidence for "thyroid hormone insufficiency" is questionable, the electro physio logic anomalies did not demon strate a consistent dose-response relationship, and behavioral tests, chosen for their sensitivity to hippocampal deficiencies, did not show any behavioral changes associ ated with the meas ured electro physiologic anomalies.
Pregnant rat dams were exposed to perchlorate in drinking water in four experimental dose groups (0, 30, 300, and 1,000 ppm) from gestational day 6 until pups were weaned on postnatal day (PND) 30. The active thyroid hormone triiodo thyronine (T 3 ), its inactive precur sor thyroxine (T 4 ), and thyroidstimulat ing hormone (TSH) were meas ured in the serum of rat pups on PNDs 4, 14, and 21. Hormonal levels were not affected on PNDs 4 or 14, with the exception of a marginal but statistically signifi cant increase in serum TSH on PND14 in the two lower dose groups (30 and 300 ppm perchlorate). The statistical significance of these results is ques tionable because changes of similar or greater magnitude in serum TSH on PND14 in the highest dose group (1,000 ppm) were not statistically significant.
On PND21, serum T 3 was reduced approximately 10-14% in the two higher dose groups (Gilbert and Sui 2008). These changes are similar to the intra and inter assay variations in these meas ure ments, stated in the "Methods" to be 9-12%. Serum T 4 at PND21 was reduced by approximately 11% in the 300ppm dose group and 27% in the 1,000ppm dose group. The authors observed no statistically significant change in TSH in any of the dose groups on PND21.
Thus, in three dose groups at three time points for three serum thyroid hormones-a total of 27 data points- Gilbert and Sui (2008) found no changes in the active serum thyroid hormone T 3 that were greater than the intra and inter assay variations. Only 3 of 27 possible data points showed changes in any of the serum thyroid hormones: TSH at PND14 increased marginally in the two lower dose groups (but not in the highest dose group), and T 4 (the precursor to the active hormone T 3 ) decreased by 27% on PND21 in the highest dose group.
Because Gilbert and Sui (2008) found no changes in the active thyroid hormone T 3 and questionable changes in other serum thyroid hormones measured in rat pups, we cannot agree with their interpretation that these data denote "thyroid hormone insuf ficiency" or "thyroid hormone reduction." The implication by Gilbert and Sui (2008) that the development of the hippo campus in rat pups is impaired as a result of perchlorate exposure of pregnant dams is weakened by the lack of consistent dose responses in the electro physiologic param eters measured in the hippocampus of the rat pups. For example, the essentially iden tical curves for the 30 and 300ppm dose groups shown in their Figure 4B, and the statistical equivalence of these curves with the control curve, leads us to question the relationship of these changes to perchlo rate dosage. In Figure 5, the lack of dose dependence is evident as the changes in 300ppm dose values often exceed or equal the changes in the 1,000ppm dose values. The apparently random nature of the results of the various electro physiologic tests used undermines any claim of reproducibility of their findings.
Interpretation of the reported electro physiologic anomalies in the hippocampus as "neurologic impairment" or "decrements in brain function" by Gilbert and Sui (2008) was not supported by the results of behav ioral testing. The authors chose four different behavioral tests for motor activity, spatial learning, and fear conditioning because of their sensitivity to hippocampal deficien cies. Rat pups in the three experimental dose groups performed equivalently to those in the control (unexposed) group on all behav ioral tests. Thus, none of these tests dem onstrated any "neurologic impairment" or "decrements in brain function." We also wish to comment on the rele vance of this study (Gilbert and Sui 2008) to human health risk assessment. The per chlorate concentrations in drinking water the authors used (30-1,000 ppm) are 2-3 orders of magnitude higher than envi ronmental concentrations, which range up to a maximum of 200 ppb in the United States (National Research Council 2005). The lack of biologically functional effects observed at the 30ppm drinking water dose (Gilbert and Sui 2008) indicate that the environmental concentrations found in the United States have a 150fold margin (30 ppm ÷ 200 ppb) of safety against any effects suggested by these authors, based on water concentrations alone. Considering that rats consume approximately 5 times more water per kilogram body weight than humans would increase the margin of safety to 600fold (5 × 150).
In addition to the shortcomings of the study noted above, the rat is questionable as a model for the sensitivity of the human thyroid system to perchlorate because of differences in thyroid hormone storage. Humans are less sensitive than rats to inhi bition of thyroid hormone synthesis by perchlorate because humans are capable of storing several months supply of seques tered T 4 and T 3 , whereas rats are capable of storing only a few days supply of these hormones. Given the inadequacies of the experimental model, the absence of a dose response in the findings, and lack of cor roboration of alleged hippocampal defi ciency by behavioral tests, we believe that Gilbert and Sui's (2008)  I welcome the opportunity to respond to the comments of Mavis and DeSesso regard ing our article on the developmental effects of perchlorate exposure on brain function (Gilbert and Sui 2008). Although couched in strong terms, their criticisms are not per tinent to the under lying physiologic pro cesses that we investigated, and many of the points they raised were addressed in our original article. The comments of Mavis and De Sesso alter neither the significance of our study nor the integrity of our conclusions. Mavis and DeSesso opine that the "evi dence for 'thyroid hormone insufficiency' is questionable." They base this opinion on two points. First, they argue that there is no "dose-response" effect of perchlorate, and second, they focus on serum triiodo thyronine (T 3 ) as the biologically active hormone. They completely ignore the effect of perchlorate in the dams, and they do not acknowledge that circulating levels of T 3 do not reflect thy roid function. More than 80% of serum T 3 is derived from peripheral deiodination of thyroxine (T 4 ) and is not tightly linked to thyroid hormone action in the developing brain. Tissue (not serum) concentration of T 3 , as well as the criti cal window over which the T 3 is required, dictates the nuclear action of thyroid hormone. Different tissues, includ ing brain, can be deficient in T 3 while serum levels of this hormone are unchanged. In addition T 4 and other iodo thyronines interact with membranebound hormone receptors and can directly affect, through non nuclear actions, the biological activity in the cells of many tissues. Mavis and DeSesso also inac curately limit the discussion of thyroid hor mones and tissue function to circulating serum levels of T 3 in developing pups.
Mavis and DeSesso confuse analytical vari ability of the hormone measures with biologi cal effect size: One characterizes the precision and accuracy of the specific assay (inter and intraassay variation); the other characterizes the variation among animals attributable to treatment. The performance of the T 3 and T 4 assays we reported (Gilbert and Sui 2008) fall well within the manufacturer's recom mended limits, and variation between rep licate samples was typically < 3%. Although thyroidstimulating hormone (TSH) assays are inherently more variable, performance also fell within acceptable limits (9-12%). These sources of variance, as Mavis and DeSesso portend, do not under lie the reported effects on serum hormones in pups.
The consequences of small reductions in serum T 4 on brain development in pups and dams are not trivial and should not be dismissed (for review, see Zoeller and Rovet 2004). Unless perchlorate is acting through a non thyroidal mechanism, our study fully supports recent data indicating that small changes in maternal and/or neonatal serum thyroid hormone can impact brain development.
We are perplexed by Mavis and DeSesso's erroneous characterization of in vivo field potentials as "electro physiologic anomalies." This seems to reflect a mis conception of the value of these measures as functional indi ces of integrated physiologic responses in an intact neural circuit. These end points are widely acknowledged to reflect the func tional integrity of the hippocampus. Our data (Gilbert and Sui 2008) go beyond the more commonly reported acute response in an isolated hippocampal brain slice to reveal impairments in the fundamentals of neuronal communication in living ani mals, and the changes were demonstrated months after exposure to perchlorate had ceased. Certainly a permanent impairment in the synaptic function of any brain struc ture must be considered an adverse neuro toxicologic insult. Input/output (I/O) functions [Figure 4 (Gilbert and Sui 2008)] reflect the ability of a population of neurons to transmit signals across a monosynaptic connection. Synaptic plasticity, the ability to adapt to stimuli, tested in the form of paired pulse (PP) depression and facilitation meas ure the influence of local circuit neurons to modulate that synaptic output [Figure 5 (Gilbert and Sui 2008)]. The clear relation ship between increasing stimulus strength and increases in the amplitude of the physio logic response, evident in both the I/O and PP data, validates the high degree of experi mental control maintained over these bio logical responses. Contrary to the allegations of Mavis and DeSesso, both sets of meas ures demon strate dosedependent perturbations as a function of peri natal perchlorate expo sure and represent important contributions to a literature largely lacking examinations of dose-response relationships. Furthermore, these findings are in complete agreement with observations using graded levels of the known goitrogen propylthio uracil (PTU) over a similar dosing regimen.
Mavis and DeSesso state that electro physiologic anomalies are not evidence of neuro logic impairment as they occurred in the absence of behavioral changes (Gilbert and Sui 2008). As discussed in our article, the neuro science literature holds many instances where molecular, neurochemical, anatomical, and electro physiologic indices do not correlate with apical behavioral mea sures. This does not negate the significance of these downstream observations, but rather reveals the relative bluntness of some of the behavioral tools available to assess cognitive function in rodent models. Attempts to eval uate subtle perturbations of the thyroid axis will require further refinement of existing paradigms to increase sensitivity or the uti lization of more sophisticated evaluations of behavioral dysfunction. This paradigm shift is not dissimilar from what was necessary in the behavioral evaluation of developmental lead exposure two decades ago.
Mavis and DeSesso state that the con centrations used in our study (Gilbert and Sui 2008) bear no relevance to the human health risk assessment for perchlorate. However, the purpose of our study was not to emulate human exposures to perchlorate. Rather, percholorate was used to disrupt the thyroid axis via a mechanism distinct from standard model compounds (i.e., PTU and methimazole) to examine the impact of mild perturbations of the thyroid axis on neuro development. Nonetheless, the results revealed a significant reduction in synap tic function at a dose (30 ppm = 4.5 mg/ kg body weight per day) consistent with the lowest observable adverse effect levels identified from the review of all available animal data and summarized in the U.S. Environmental Protection Agency's perchlo rate risk assessment document (U.S. EPA 2002). As such, these findings corroborate previous findings and add additional weight to the existing evidence from animal studies on the negative impact of perchlorate on brain development.
Finally, according to Mavis and DeSesso, the rat model is questionable for sensitivity of the human thyroid system to perchlorate because of differences in thy roid hormone storage. The hypothalamicpituitary-thyroid axis is very similar in its chemis try and its function in rodents and humans, and rodent models have provided important information on the fundamen tal biology of endocrine systems informing medical practice and public health protec tion. Although differences in thyroid hor mone economy of adult rats make rodents less than ideal for the assessment of thy roid tumors, the dependence of the fetus on