Tim Varney, PhD, CIH, RS, CHMM & Bob DeMott, PhD, DABT ENVIRON International, Corp

Toxicological Dose, Effect and Non-Monotonic Responses Implications For I.H. Health Risk Assessment Tim Varney, PhD, CIH, RS, CHMM & Bob DeMott, PhD, DABT ENVIRON International, Corp

Course Objectives • Establishing key toxicological fundamentals • The concept of dose • Dose response • Influencing variables • Identifying individual/group differences • Advanced dose response concepts • Non-monotonic dose response • Implications for I.H. health risk assessment

Exposure ? The concentration of a substance and/or agent in air, water, soil, and/or food associated with ones occupational, home or ambient environment that may or may not result in intake, dose and response.

Dose ? The amount/volume of a substance and/or agent taken into the body per unit of time.

Effective/Target Dose? The amount/volume of a substance/agent that elicits an observed response and/or that which is associated within specific tissues/organs

Dose Response The outcome of intake associated with biological process/defense mechanisms that may have no measurable effect, beneficial effects or effects that may lead to increased morbidity and/or mortality.

Exposure does not always=dose It is an agent concentration in air, water, soil, food, etc. It can be acute, chronic, alternating in character Intake must occur before dosing is realized Dose may be a one time or recurring events Dose can be partitioned to whole body, target organ or tissue specific Exposure Versus Dose

Dose--------------------Response • Is measurable if concentration and intake of the agent are known • Is a fundamental concept in pharmacology, toxicology and health risk assessment • May originate from exposures to toxicants in air, water, soil, food, etc. • May be derived from animal models, direct measurements and/or exposure assessments • Is often expressed as mg/kg/day • Is central to I.H. health risk assessment

Toxicant Interactions That Modify Dose Response • Antagonism: antidotes to bacterial, reptilian or insect toxins/venoms • Potentiation: ethanol and barbiturates • Synergistic: cigarette smoking and coincidental exposures to asbestos and radon decay daughters

Factors That Drive Dose-Response & Host Variability • Toxicity • Persistence • Magnitude of the dose • Frequency and duration of intake • Route of exposure • Age • Functional status • Gender • Ethnicity • Other agents in the mix: intrinsic/extrinsic

Importance of Functional Status • Respiratory-FEV1, FVC, FEV1/FVC, CO2-02 gas exchange/saturation, mucosiliary clearance • Renal clearance time • Hepatic enzyme activity/levels • Cardiovascular/peripheral circulatory output/efficiency

Atypical or Unusual Dose Reactions • Overt Tolerance: may be innate or acquired • Idiosyncratic responses: outside the norm of what is expected or reported • Chemical allergy: “simple” immune response • Type I&II Hypersensitivity: immune system marshals a progressively pronounced response that can become life threatening

How Do These Impact Dose-Response Affect/Effect Skin on hands versus skin on head or back Alveolar insult and intake of PM2.5 versus PM10 Intake of Cr III versus Cr VI and latency Relative humidity and intake of formaldehyde Intake of lead at age <5 versus 35 years Lipid versus water solubility

Early & Late-Term Dose Responses • Dose response can be immediate: chlorine gas/RADS, bee sting/anaphylaxis, H2S/tissue hypoxia • Dose response can be late: extensive acid burns/renal failure, high levels of NO2/pulmonary edema, Amanita toxin/hepatic necrosis

Working With Surrogate I.H. Measures of Exposure/Dose • Job descriptions • Occupational exposure cohorts • Temporal Exposure cohorts • Spatial/geographical exposure cohorts • Ambient toxicant concentrations • Can be subject to marked variation and uncertainty

Important ! Exposure and dose will always have temporal and spatial components that can be highly variable and host/cohort specific…understand the exposure setting

Or Risk = toxicity x exposure Or Risk = toxicity x intake Risk = Dose

What Must be Known Before Dose Can be Determined • Agent & agent characteristics • Exposure concentration • Routes of exposure • Exposure frequency • Exposure duration • Body weight

Route of Exposure Is A Critical Dose Factor • Respiratory-DRIVERS? (300-1000 ft2) • Ingestion-DRIVERS? • Dermal-DRIVERS? (12-30 ft2) • Percutaneous-DRIVERS?

Computing Average Daily Particle Dose ADD=PM2.5 x INF x EF x ED ÷ BW x EAT Where: PM2.5 = particle concentration INF=inhalation intake factor-resp. rate EF=exposure frequency ED=exposure duration BW=body weight EAT=exposure averaging time

Computing Average Daily Vapor/Gas Dose ADD=Cx x INF X EF x ED ÷ BW x EAT Where: Cx=concentration of agent INF=inhalation intake factor EF=exposure frequency ED=exposure duration BW=body weight EAT=exposure averaging time

Computing Average DailyDermal Dose ADD=Cx x SSAE x EF x ED ÷ BW x EAT Where: Cx=concentration of agent SSAE=skin surface area exposed EF=exposure frequency ED=exposure duration BW=body weight AT=exposure averaging time

Body Burden and Dose Computation/Dose-Response 1.Toxicant burden fluctuates with time and functional status 2. Differential release from body tissue 3. Bone: long-term slow release 4. Adipose tissue: sensitive to change in body weight 5. Blood & Lymph: short lived but subject to releases from bone and adipose tissue 6. Interferes with estimations of dose 7. Complicates dose estimates and dose affect

A. D. M. E.---AD ME---ADME • A=adsorption and movement-skin, lungs & digestive tract • D=distribution via blood & lymph • M=metabolism/chemical alteration • E=excretion via lungs, skin, bladder intestines

The Myth of The Average 70kg Male And Importance of Left Tail Sensitivity

PELs, TLVs, MCLs and Dose • What are PELs, TLVs and MCLs • Are PELs,TLVs and MCLs dose values? • What must be done/known before dose can be accurately determined? • Are PEL,TLV and MCL levels universally protective? • How do occupational PEL/TLV values differ from MCLs

Importance of I.H. Exposure Monitoring • Accurate estimations of dose-response hinge on “good” exposure data • Exposure monitoring should be representative of the exposure setting • Exposure monitoring should address both spatial and temporal components • The methods of exposure monitoring should be consonant with practice guidelines

Biomedical Monitoring • Choosing the agent and/or metabolite to measure • Choosing the body tissue and/or fluid to sample/collect • Deciding on the time and number of samples • Pre/post shift sampling • Sampling after a weekend, holiday, vacation • Lifestyle choices that confound/modify dose response

Gold Standard Measures • Experimental animal models • Epidemiological Clinical trials • Controlled real-time exposure monitoring • Measurement of toxicants and/or their metabolites in tissue, body fluids or waste

Working With Markers of Dose Response/Effect • Adverse/potentially adverse/susceptibility • Original agent/toxicant-lead/lead • Metabolites-phenol/benzene • Conjugates-immune components • Adducts-antigen/antibody • Enzymes-SGOT/liver

Working With Causal Inference • Biological plausibility • Dose response trends • Temporality of exposure/response-exposure precedes effect • Specificity of the response • Can it be generalized to other exposure settings • Is it supported by a body of peer reviewed literature

Children Are Not Small Adults Implications For Dose/Effect • Developing immune & reproductive systems • Rates of intake for food and water greater on a body weight basis than adults • Air intake of infants twice that of adults • Rate and contribution of dermal exposure • Children play closer to sources of contamination • Subject to parental take-home contamination

But!What happens When Up Is Down and Down Is Up?

Break

Tim Varney, PhD, CIH, RS, CHMM & Bob DeMott, PhD, DABT ENVIRON International, Corp