The Role of Time as a Quantifiable Variable of Toxicity and the Experimental Conditions When Haber's c x t Product Can Be Observed: Implications for Therapeutics

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Vol. 296, Issue 3, 663-668, March 2001

The Role of Time as a Quantifiable Variable of Toxicity and the Experimental Conditions When Haber's c × t Product Can Be Observed: Implications for Therapeutics

Karl K. Rozman and John Doull

Department of Pharmacology, Toxicology and Therapeutics, University of Kansas Medical Center, Kansas City, Kansas (K.K.R, J.D.); Section of Environmental Toxicology, GSF-Institut für Toxikologie, Neuherberg, Germany (K.K.R.)

	Abstract

Top Abstract Introduction Examination of the c... Kinetics Dynamics Conclusions References

One hundred years ago, Warren established for the first time a quantitative link between dose and time while studying thetoxicity of sodium chloride in Daphnia magna (Straus). Duringthis century, many toxicologists in different contexts returnedto this idea, which has become known as Haber's Rule of inhalationtoxicology. Most attempts to explore this relationship ended infrustration because of the observed deviations from it, whichwere unfortunately called exceptions. Thus, toxicologists concentratedon the quantitative relationship between dose and effect undermostly isotemporal conditions, while time was assigned such arbitrary,semiquantitative designations as acute, subacute, subchronic,and chronic. Time itself as a quantifiable variable of toxicitywas seldom studied and when it was examined, it was often notdone under isodosic (steady-state) conditions. A recent analysisof time as a variable of toxicity indicated the existence of atleast three independent time scales (toxicokinetic, toxicodynamic,exposure frequency/duration) in toxicological studies, which interactwith dose and effect to yield the enormous complexity known toevery toxicologist. Based on prototypical examples when toxicokinetic(dioxins, chloroacetic acid), toxicodynamic (nitrosamines, soman,sarin, tabun), exposure frequency (methylene chloride), or otherexperimental design-related conditions (HgCl₂, CdCl₂) representthe critical time scale, the general validity of the c × t = kconcept will be discussed as a starting point for a theory oftoxicology. As endpoints of toxicity, (delayed) acute toxicity,blood dyscrasias, and cancer will be used to illustrate the criticalconditions needed to demonstrate the validity of this theory.The relevance of this theory to the pharmacologic action of chemicalsand its implication for the therapeutic index are alsodiscussed.

	Introduction

Top Abstract Introduction Examination of the c... Kinetics Dynamics Conclusions References

This year is the centennial of Warren's (1900) article on the toxicity of sodium chloride in Daphnia magna (Straus), linking,for the first time, dose and time in a quantitative relationship:(c $-$ c_o) × t = k. Problems with this simple formula were notedsoon thereafter, and Ostwald and Dernoscheck (1910) suggestedin analogy to an adsorption isotherm that c^x × t = k provides a better description of experimental data. Haber(1924) used the simplest form of the dose/time relationship (c× t = k) to estimate the toxicity of war gases, and Flury andcoworkers examined this phenomenon further when studying the toxicityof solvents (e.g., Flury and Wirth, 1934). Entomologists werethe ones who confirmed most frequently the simplest c × t = krelationship, but they also reported departures from it. Bliss(1940) dealt with the deviations mathematically and concludedthat departures from c × t = k can be described either by c^x × t = k or c × t^x = k. Druckrey et al. (1967) studied the carcinogenicity of alarge number of nitrosamines and came to the conclusion that thelatency to cancer can be best characterized by c × t^x = k, where in some instances x = 1. The relationship kept reappearingin different experimental contexts (e.g., Gardner et al., 1977,1979), but each time anomalies showed up and the claim for generalizationwas given up because of the occurrence of presumedexceptions.

Claiming exceptions to an often observed phenomenon is detrimental to the scientific approach since it puts an end to furtherinquiry. The more appropriate question is why does a particularexperiment show departure from the frequently made observationof c × t = k? This generalized question arose as a result of experiencewith studying the toxicity of dioxins. Why was the remarkablyconsistent c × t = k of 1,2,3,4,6,7,8-heptachlorodibenzo-p-dioxin(HpCDD) for delayed acute toxicity (Rozman, 1999) not observedwith 2,3,7,8-tetracholorodibenzo-p-dioxin (TCDD)? It was entirelyimplausible that TCDD would be an "exception" from something thatapplies to HpCDD considering the perfect structure/activity relationshipsin terms of all other aspects of their effects. Therefore, thechallenge was to identify a critical step(s) that was responsiblefor the manifestation of c × t = k in the case of HpCDD and thelack thereof in the case of TCDD.

	Examination of the c × t Concept

Top Abstract Introduction Examination of the c... Kinetics Dynamics Conclusions References

Rozman and Doull (2000) recently suggested a decision tree-type analysis to identify critical steps in the toxicity of chemicals.Use of this analysis revealed that the critical difference betweenHpCDD and TCDD resided in their differential kinetics. In otherinstances, the analysis revealed dynamic step(s) as the crucialone(s) in the manifestation of toxicity. In either instance, frequency/durationof exposure needed to be carefully considered as an additionalindependent time scale. In the following discussion, exampleswill be used to illustrate under what circumstances Haber's Productwill be obtainable when either kinetics, dynamics, or exposurefrequency represents the rate-determining step in the developmentoftoxicity.

	Kinetics

Top Abstract Introduction Examination of the c... Kinetics Dynamics Conclusions References

If the kinetic half-life of a compound (as determined from its plasma disappearance profile) is longer than the dynamic half-lifeof the effect (as determined from its effect recovery profile),it will dominate the overall process of toxicity under conditionsof intermittentexposure.

Case 1: Very Long Kinetic Half-Life. HpCDD yielded c × t = k in terms of delayed acute toxicity (Rozman, 1999), whereas TCDD did not (Stahl et al., 1992). Thehalf-life of TCDD in female Sprague-Dawley rats is about 20 daysand that of HpCDD about 200 to 300 days (Viluksela et al., 1997,1998). Rats died as a result of wasting for up to 70 days aftertreatment with a single dose (rate) of HpCDD, but no rat diedafter 30 days when treated with a single dose (rate) of TCDD.The reason for this difference is that 70 days represents lessthan <FR><NU>1</NU><DE>3</DE></FR> of one half-life for HpCDD, whereas30 days amounts to about 11/2 half-lives for TCDD. Consequentlythere is a minimum departure from steady state (at the most 16%)regarding the body burden of HpCDD during the observation period,but there is a major departure from it (about 62%) in terms ofthat of TCDD. As a result, the single dose (rate) experiment withHpCDD was being conducted under nearly ideal conditions (nearkinetic steady state), allowing for little recovery to occur during70 days after dosing, whereas in TCDD-treated animals, a sufficientamount of chemical has been removed from the organism for significantrecovery to have occurred during 30 days after dosing. When TCDDwas administered to female rats under isoeffective conditionsas a loading dose followed by maintenance doses every 4 days thec × t = k relationship emerged with clarity also for this dioxincongener (Fig. 1). It should be noted that this study was conductedunder isoeffective conditions (100% mortality), which representsthe "ideal" condition to study the relationship between dose andtime. Variability is larger in this experiment than in the experimentwith HpCDD (Rozman, 1999). The reason for this is that differentrats of the same dose group often received a different numberof maintenance dose rates and with that different doses due todifferent times to death of individual animals. The lesson fromthese and other experiments (lower doses) was that the slightestdeparture from ideal conditions (kinetic steady state or monotonicdeparture from it) has a major impact on the c × t = k product,making it indiscernible in most toxicological experiments. Itappears that there are no exceptions to the c × t = k relationshipunder ideal conditions and that most toxicological experimentsdo have uncontrolled (hidden) variables. For example, the kineticsof chemicals have virtually never been controlled in toxicologicalexperiments unless nature did it in the form of medium to longerkinetic half-lives when routine laboratory dosing regimens resultedin reasonably good steady-state concentrations.

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Fig. 1. Time to death and dose × time (c × t) in TCDD-treated female Sprague-Dawley rats depicted on two separate scales as indicated by different ordinates. Time to death decreased significantly and incrementally with increasing dose (rates). The c × t product did not change much with increasing dose (rates). $black-square$ , time to death (days);

, c × t (µg/kg × day); *p < 0.05.

Some might argue that the finding with HpCDD was just coincidental for another short-term effect and as such is just an exceptionfrom the exceptions regarding Haber's Rule. Rozman (2000b)

showedthe major chronic toxic effects of HpCDD in the continuation ofthe experiment that first addressed its delayed acute toxicity.The experimental design of that study has been described in detailin a previous publication (Rozman, 1999

). Animals surviving theacutely toxic insult [including an acute no observable adverseeffect level (NOAEL) of 2.5 mg/kg] developed anemia, lung cancer,liver cancer, various kidney pathologies, and a variety of low-incidencepathologies toward the end of the animal's natural life span,in the sequence as listed. Figure 2 demonstrates the chronic timeresponse to various doses of HpCDD in terms of all causes of death.This chronic time response predicts with great accuracy the shorteningof the animal's life span by increasing doses of HpCDD. It istruncated at about an LD₈₀ by the delayed acute dose responsethat had killed most or all animals at higher doses. At leasttwo of the effects were concurrently present in many animals (anemiaand lung cancer), making separation of these two endpoints oftoxicity difficult other than by the time to occurrence of effectin the first subject to be affected. However, if each effect occursaccording to c × t = k, then the sum of all effects must alsobe c × t = k for all subjects. This indeed has been confirmedfor all chronic effects combined (Rozman, 2000b

). The remarkablylow variability is comparable to data obtained for delayed acutetoxicity (Rozman, 1999

). It should be noted that these chroniceffects developed while the animals were eliminating a significantportion of their body burden, allowing for increasing recoveryto occur. With a half-life of about 200 days, 75% of HpCDD waseliminated by day 400 and 87.5% by day 600, a period during whichmost chronic deaths occurred. To elucidate the role of recoveryin the toxicity of HpCDD, the compound was also administered asa loading dose rate (2.8 mg/kg) followed by biweekly maintenancedose rates (0.085 mg/kg) to maintain kinetic steady state. Eventhough this dosing regimen increased considerably the dose ofHpCDD, the c × t product remained approximately constant becauseof an entirely predictable shortening of the animal's life span(Rozman, 2000b

). The second important message of this experimentis the increased incidence of anemia and lung cancer and the unchanged/decreasedincidence of liver cancer and kidney pathologies with the completedisappearance of other pathologies (Rozman, 2000b

). This importantfinding is consistent with the notion that some rats recoveredsufficiently after the single dose rate to live considerably longerthan under conditions of kinetic steady state. Because of thisrecovery, they did not develop anemia and lung cancer but contractedother toxicities/pathologies, which could not develop under conditionsof kinetic steady state because of the shortening of the animal'slife span.

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Fig. 2. A plot of time to death versus dose in female Sprague-Dawley rats chronically exposed to HpCDD by administration of a single dose (rate). Increasing dose (rates) significantly and incrementally decreased time to death as compared with controls. *p < 0.05; **p < 0.01.

Case 2: Intermediate Kinetic Half-Life. Monochloroacetic acid (MCA) has a half-life of about 2 h in male rats and a time to effect (coma, death) of the same orderof magnitude. Therefore, in the course of the development of toxicity,a significant portion of a dose will be eliminated allowing forsome recovery to occur while toxicity is developing. Like TCDD,MCA does not obey Haber's Rule when administered as a single dose(rate), although it comes close to it after subcutaneous injection(Hayes et al., 1973) because of the slow release of MCA from thisdepot. To create ideal conditions, MCA had to be infused by osmoticmini pumps because repeated administration of maintenance doserates by most of the other commonly used methods would have severelydisturbed the animals, triggering convulsions (and death) andthereby off-setting their normal time schedule to develop comaaccording to c × t. Rozman (2000) demonstrated that this experimentaladjustment resulted in a reasonably good c × t = k relationshipalso for this compound and for still another endpoint of toxicity(coma). It must be recognized that it is not the "absolute" timescale that determines whether or not c × t = k will become manifestwhen steady state is not carefully controlled but the ratio betweenthe half-life of a compound and the observation period. If theobservation period is much shorter than the half-life of a compound,then c × t = k will be observable unless, for example, adaptationintroduces a "hidden" variable. However, the more unfavorablethis ratio becomes, the more recovery will be occurring concurrentlywith the development of toxicity. This will not only introducean uncontrolled variable but also flatten the dose-and-timeresponses.

Case 3: Very Short Kinetic Half-Life. Methylene chloride is an example for such compounds, having an estimated kinetic half-life of 5 to 40 min. The following considerations,however, also apply to compounds of even shorter half-lives likeozone, although for ozone the dynamics of recovery may be rate-determining.For compounds of very short kinetic or dynamic half-lives, thedistinction between kinetics/dynamics becomes less important becauserapid elimination/recovery reduces time dependence of toxicity.Such compounds will be more concentration-dependent after anytype of discontinuous exposure regimen, and only continuous exposuretill the actual occurrence of an effect will yield c × t = k.This is probably the origin of the notion that Haber's Rule appliesto inhalation toxicology only, when in fact inhalation happensto be the only practical way (intravenous infusion for days tomonths is clearly not) to provide continuous exposure for compoundshaving very short kinetic or dynamic half-lives. Here, the importantfactor is not inhalation but the need for continuous exposure.Intermittent exposure (6 h per day) to kinetically acting compoundswill yield c × t = k only if their kinetic half-lives are at leasta day or longer to allow for a reasonable steady state with littlekinetic recovery (elimination) occurring between exposure episodes.If intermittent exposure is further fragmented by weekends, thehalf-life has to be correspondinglylonger.

It needs to be emphasized that c × t = k may not be observable for compounds of very short kinetic half-life, but not becausethey are exceptions from this law of toxicology as claimed bysome scientists (Boyes et al., 2000

). If exposure is not continuousuntil the actual measurement of an effect, then the departurefrom c × t = k will depend on the ratio between the half-lifeof a compound and the elapse of time between cessation of exposureand the actual measurement taken. Often the lack of a good timeresolution will make it difficult to design experiments to demonstratec × t = k. However, when time resolution is good, as in the pungencyof acids, clear summation effect can be observed on a time scaleof seconds (Cometto-Muñiz and Cain, 1984

	Dynamics

Top Abstract Introduction Examination of the c... Kinetics Dynamics Conclusions References

For compounds causing effects such that the effect recovery half-life is longer (slower recovery) than the kinetic half-life,the former will dominate the dynamics of the effect. These arethe hit-and-run type poisons, which can be eliminated very rapidlyand yet produce an effect in accordance with c × t = k.

Case 1: Very Long Dynamic Half-Life. There are few examples of recovery taking place on a time scale of years or longer. Chemical neuropathies are the closestexamples that come to mind. Because of the enormous reserve capacityand plasticity of the nervous system, it is difficult to conductconclusive studies in this area. As is the case for compoundswith very long kinetic half-lives, both the frequency/durationand the recovery can be critical for these compounds, dependingon the dynamics of the effect. If the damage is highly irreversibleas occurs with Ginger Jake paralysis (Morgan and Penovich, 1978),or with methanol's damage to the retina/optic nerve, accumulationof injury will occur according to a triangular geometry afterrepeated above-threshold exposures in spite of the short kinetichalf-lives of these compounds. If an essentially irreversibleinjury is very severe, it is very difficult to titrate the dose/injuryto assure reproducible survival, which is necessary when studyingtime to effectphenomena.

Case 2: Intermediate Dynamic Half-Life. Diethylnitrosamine (DENA) has a short kinetic half-life of about 10 min in rats (Druckrey et al., 1967). Feeding rats a dietwith different daily dose rates resulted in a reasonably goodc × t = k relationship with cancer as endpoint of toxicity (Druckreyet al., 1963; Rozman, 2000b). The daily dose rate was a poor surrogateof dose (cumulative) because of the vastly different life spanof the animals receiving the various daily dose rates. It is worthwhileto note that c × t = k is less variable under isoeffective conditionsthan when departure from it takes place (see 91 and 64 mg/kg doses).Again, with a kinetic half-life of 10 min for DENA and two boutsof feeding per day, no good c × t = k relationship should be expectedif kinetics were rate-determining because of very rapid kineticrecovery (elimination) after completion of absorption of eachdaily dose rate. However, in general, the half-life of DNA adductsof potent carcinogens is in the order of weeks to months (Szafarzand Weisburger, 1969; Swenberg et al., 1985; Pitot and Dragan,1996), which provides the key to understanding the reasonablygood c × t = k obtained (Rozman, 2000b). The dynamics of DENA-inducedcancer are dominated by the long dynamic half-life of the effectand not by the short kinetic half-life of the causative agent.Thus, animals exposed to DENA in the diet are not at kinetic steadystate at all, but they are at dynamic steady state with regardto the DNA damage, which is the reason for the good c × t = krelationship.

Case 3: Short Dynamic Half-Life. The kinetic half-life of soman, sarin, and tabun is about 10 min to 1 h in all species studied, but the recovery half-lifefrom intoxication is about 12 h (Lintern et al., 1998; Rozman,2000b). Considering the ratio between observation period (6 h)and kinetic half-life (10 to 60 min) suggests extremely unfavorableconditions for c × t = k to occur due to virtually complete kineticrecovery by the end of the observation period. In fact, thereis an excellent c × t = k relationship (Sivam et al. 1984), atleast for those organophosphates (OP) that display slow recovery,because it is the dynamic half-life of the effect and not thekinetic half-life of the compound that determines c × t = k.

There are two important issues here that indicate the relevance of time as a variable also of therapeutics. A case in pointis antidotal therapy in OP poisonings. In terms of dose alone,soman is the most toxic OP among the three OPs listed above; however,in terms of dose and time, both tabun and sarin are more dangerousthan soman because the time to death is shorter for sarin andmuch shorter for tabun than for soman (Rozman, 2000b

). Indeed,a severely intoxicated person's life was saved by administeringatropin sulfate and PAM (pralidoxime, 2-formyl-N-methyl-pyridiniumchloride oxime) within 5 to 10 min of an accident with soman (Sidell,1974

). It is unlikely that this person's life could have beensaved if the agent in this intoxication episode had been tabunbecause of the short therapeutic window (15 min) in terms oftime.

Many if not most therapeutic agents belong to the last two cases discussed (short to intermediate dynamic half-life). Considerthe H⁺-ion pump inhibitor omeprazole. The binding half-life to its receptoris 24 h. Its kinetic half-life is about 1 h or less. If the therapeuticdose would be based on its kinetic half-live, the conclusion wouldbe that after 6.64 half-lives (6.64 h) 99% of the drug would beeliminated. Therefore, a dosing regimen entailing the administrationof the drug every 6 h still would yield a very poor steady stateand, with that, moderate to low therapeutic efficacy. Omeprazole,in fact, is given daily once or every other day in accordancewith its pharmacodynamic half-life of 24 h. It has been reportedthat it takes 3 days for maximum effect (clinically indistinguishablefrom 3.32 dynamic half-lives equaling 90% of steady state) and3 to 5 days for cessation of effect, which is clinically alsoindistinguishable from 3.32 reversibility half-lives. The actionof this drug is entirely dominated by dynamics, and any opinionbased on kinetics would be inerror.

Special Cases: Experiment-Driven Steady State. Any time an experiment is conducted under conditions of kinetic steady state (e.g., continuous inhalation until observationbeyond four to seven kinetic and/or dynamic half-lives) the outcomewill be in accordance with Haber's Rule unless some hidden variablesare impeding the outcome. In vitro studies, experiments involvingthe use of aquatic species (fish, pond snails, etc.), or any instancewhen continuous exposure is implicitly part of the experimentaldesign will result in experiments showing simple or more complexc × t = k relationships unless kinetic or dynamic adaptation(s)occur during measurement of toxicity (Verhaar et al., 1999). Infact, Rozman (2000b) provided an indication for the accuracy ofthe c × t = k relationship using sea urchin sperm motility asendpoint of toxicity and divalent cations astoxicants.

	Conclusions

Top Abstract Introduction Examination of the c... Kinetics Dynamics Conclusions References

If physicists would have claimed the occurrence of exceptions to what later became Boyle's Law of ideal gases as deviationsfrom it started accumulating after some initial confirmatory evidence,mankind would not possess perhaps the most profound theory everdevised, which is thermodynamics. The greatest impediment in thedevelopment of the discipline of toxicology was to view deviationsfrom the c × t = k concept as exceptions. Claiming that an exceptionexists stifles any attempt at generalization, which eventuallyis needed to develop a theory, which in turn is a preconditionof a scientific discipline. If the discipline of toxicology isto develop into a science, then the prerequisite is to changethis notion about exceptions. There are no exceptions to a fundamentallaw of nature, and if we assumed that c × t = k under isoeffectiveconditions or c × t = k × E (effect) under isodosic or isotemporalconditions represents a law of toxicology, then there should beno exceptions to it either (for detail, see Rozman, 2000a andRozman and Doull, 2000). What we then need to understand are theconditions under which c × t = k or c × t = k × E can be experimentallyobserved to begin to explore apparent departures from it by askingthe followingquestions.

Why does it appear that this or that experiment deviates from the c × t concept? What are the uncontrolled (hidden) variables?What experiments are needed to findout?

Short of changing our experiments to accommodate these questions, there will be little real progress in toxicology as a science.Toxicology was first marginalized by risk assessment because ofthe claim that it could not answer conclusively questions abouthigh to low dose extrapolation and species-to-species interpretation.Unfortunately, toxicologists did not challenge forcefully enoughthis notion on grounds of the c × t concept, which does allowto define both the dose and the time threshold within biologicalvariability (normal distribution). This led risk assessors tothe absurd assumption (from the biological point of view) thattime is not important at low doses (Crump et al., 1976) when infact time is less important at high doses but it dominates thelow dose end of the c × t relationship. The recently emergingprecautionary principle (to lower exposure as much as possible)will complete this process by making the large scale toxicologicaltesting/evaluations of environmental chemicals a matter of thepast. Perhaps this is the only way to confront currently acceptedexperimental designs (acute, subchronic, chronic toxicity), whichignore time as a quantifiable variable of toxicity. The analysisprovided in this article suggests that it is possible to understandthe conditions under which Haber's Rule can be experimentallydemonstrated that would make this relationship into a law of toxicology.Toxicology has benefited from pharmacology immensely both methodologicallyand theoretically. As continuous long-term therapies become moreand more common, perhaps pharmacology can take advantage of theseinsights gained in toxicological investigations and examine itsimplications for beneficial rather than adverse effects, bothof which are clearly subject to the same fundamental laws ofnature.

One such pharmacological principle that could benefit from application of Haber's Rule is the therapeutic index. The therapeuticindex is traditionally defined as the ratio of the toxic doseto the therapeutic dose (LD₅₀/ED₅₀). Dose in this expression couldbe viewed as a surrogate for exposure, but generally time is ignoredalthough it is an equally important variable of exposure. Doseis a simple variable (number of molecules reaching the receptor),whereas time is a complex variable with kinetic, dynamic, andfrequency/durationscales.

If we establish the minimal combinations of dose and time that are required to produce a specific toxic or therapeutic effectwith continuous exposure, we can plot the logs of these time anddose values to obtain a slope of $-$ 1 (Fig. 3). Parallel lines willbe obtained for all other effects of an agent, and all of theselines can be described by Haber's Rule (c × t = k) under idealexposure conditions. Each of these lines defines the individualor population exposure threshold for a specific therapeutic ortoxic effect, and the ends of these lines are defined by thosecombinations where further increases of dose no longer reducetime to effect or conversely where further increases in time nolonger reduce the dose required to produce the specific effect.The k values for specific toxic and therapeutic effects can beused as surrogates for exposure to define the therapeutic indexof an agent in the same way as is done currently with dose (therapeuticindex = k^toxic
effect/k^{therapeutic effect}). When the effects are the result of long-lasting or slowly reversibledynamics or kinetics, continuous exposure is not needed to establishHaber's k values. Fractionation of the time or dose will resultin lines with different slopes and k values (c × t^y = k^t, c^y × t = k^c) as will fractionation of both dose and time (c^x × t^y = k^ct) (Fig. 3), but these k values could also be used to characterizethe therapeutic index by comparing conditions of intended usageversus minimum toxicity under conditions of continuous exposure.

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Fig. 3. Relationship between dose and time under different conditions of exposure.

Many more examples of the potential importance of time as a quantifiable variable of therapeutics could be provided, but theintent of this article is not comprehensiveness but the stimulationof discussion with pharmacologists regarding the applicabilityof Haber's Product to bothdisciplines.

	Footnotes

Accepted for publication November 2, 2000.

Received for publication September 9, 2000.

Send reprint requests to: Dr. Karl K. Rozman, Department of Pharmacology, Toxicology and Therapeutics, 3901 Rainbow Blvd., Kansas City, KS 66160-7417. E-mail: krozman{at}kumc.edu

	Abbreviations

HpCDD, 1,2,3,4,6,7,8-heptachlorodibenzo-p-dioxin; TCDD, 2,3,7,8-tetracholorodibenzo-p-dioxin; MCA, monochloroacetic acid; DENA, diethylnitrosamine; OP, organophosphates.

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