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An Overview of Risk Assessment and Issues

An Overview of Risk Assessment and Issues. Lynne Haber Toxicology Excellence for Risk Assessment Presentation to the CPSC April 8, 2010. Outline of Talk. Risk assessment paradigm Overview Exposure assessment Hazard characterization Dose-response assessment Risk characterization

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An Overview of Risk Assessment and Issues

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  1. An Overview ofRisk Assessment and Issues Lynne Haber Toxicology Excellence for Risk Assessment Presentation to the CPSC April 8, 2010

  2. Outline of Talk • Risk assessment paradigm • Overview • Exposure assessment • Hazard characterization • Dose-response assessment • Risk characterization • Children’s risk issues

  3. hazard identification/ characterization dose-response exposure estimation risk characterization social economic public response political Risk Assessment(organizing & analyzing to set priorities & guide management) Risk Management(decision & action)

  4. NAS 2008 Approach

  5. Risk Assessment/Management Components • Hazard characterization: Is this toxic to humans? • Dose-response assessment: How toxic is it? • Exposure assessment: Who is exposed, how much, how often, and for how long each time? • Risk characterization: So what? • Risk management: So what will be done about it? Don Barnes, 1993

  6. “The Dose Makes the Poison” • Even seemingly safe substances can be toxic at the “right” dose (e.g., water) • Organisms respond to toxic substances according to the dose that gets into the body; in toxicology this is called dose-response • Increasing the dose or exposure to the substance generally causes more effects • Example RfDs: acetone - 0.9 mg/kg-day, zinc - 0.3 mg/kg-day, Aroclor 1016 - 7 x 10-5 mg/kg-day

  7. Exposure Assessment • What are the sources and routes of exposure? (exposure pathway) • What is the magnitude, duration and frequency of the exposure? • What are the characteristics of the exposed population? • The exposure portion of the paradigm – sources, activity patterns, containment approaches, etc. – provide much of the opportunities for risk management • CPSC does nice research to evaluate potential exposure from specific products – e.g., leaching to mimic effects of mouthing or swallowing, wipe tests to mimic handling

  8. Hazard Characterization • Considers: • Data on toxicity • Various endpoints • Mechanistic data/Mode of action • How a chemical induces an effect • Kinetics – what the body does to the chemical • Dynamics – what the chemical does to the body • Uses weight of evidence approach

  9. Types of Data – Chronic Limits • Human data – case reports, epidemiology, controlled studies in limited cases (e.g., air pollutants) • Animal data – e.g.: • Carcinogenicity • Neurotoxicity • Reproductive/developmental toxicity • Immunotoxicity • General system toxicity – e.g., effects on liver, kidney • Bioavailability – how much enters the body • In vitro studies – mechanistic, “omics”

  10. Types of Data – Acute Limits • Data typically much more limited • Lethality data (e.g., LD50) commonly available, but are of limited use for identifying safe levels • Some research has been done and studies published on extrapolation approaches – e.g., from LC50 – but involve assumptions and larger uncertainties • May have data on some effects – sensitive endpoints typically not evaluated • Developmental toxicity still relevant – potential short windows of susceptibility • Steepness of dose-response curve is important

  11. Importance of Mode of Action • Hazard characterization • Determining human relevance (e.g., alpha-2u-globulin related kidney tumors in male rats) • Determining conditions of carcinogenicity and other effects (e.g., route-specific at portal of entry; dose-relationship) • Dose-response assessment • Determining approach for risk characterization/low-dose extrapolation • Informing specific aspects of quantitation (e.g., dosimetry, UFs, data needs, childrens’ risk)

  12. Non-Cancer Dose Response Assessment…As Defined by EPA Reference Dose (RfD) is ... an estimate (with uncertainty spanning perhaps an order of magnitude) of a daily exposure to the human population (includingsensitive subgroups) that islikely to be withoutan appreciable risk of deleterious effects during a lifetime. (Barnes and Dourson, 1988)

  13. Acceptable Daily Intake (ADI) NOAEL, LOAEL or BMD ADI = UF Where: NOAEL is the No Observed Adverse Effect Level LOAEL is the Lowest Observed Adverse Effect Level BMD is the benchmark dose UF is one or more uncertainty factors needed for data deficiencies

  14. Determining the Point of Departure • The numerator of the ADI identifies a threshold for toxicity in the experimental species • Traditionally, as default, agencies assumed that for most types of effects, there is a dose level below which a response is unlikely • Homeostatic, compensation and adaptive mechanisms in the cell protect against toxic effects • Critical effect is the first adverse effect or known precursor relevant to humans that occurs as dose increases

  15. Areas of Uncertainty Addressed in ADIs and Similar “Safe Doses” – Uncertainty Factors • Variability • Extrapolating from animals to humans • Human variability and sensitive populations • Uncertainty • Extrapolation from above threshold to below threshold (“LOAEL to NOAEL”) • Extrapolation from less than lifetime exposure • Consideration of data gaps

  16. Dose Response Assessment at CPSC: Non-Carcinogens • No-observed adverse effect level (NOAEL) • Acceptable Daily Intake (ADI) = • NOAEL  10 if human data • NOAEL  100 if animal data • LOAEL  1000 if NOAEL not established • Benchmark dose may also be used

  17. The Continuum Default  Data-Informed • Default – 10 x 10 • Database - Derived - databases of information, not group or chemical-specific • Categorical - applies to categories of substances/species based on their characteristics (BSA correction; RfC - gases/particles) • Chemical Specific Adjustment Factors - addressing kinetic or dynamic aspects with chemical specific or compound-related information (e.g., PBPK) • Fully Data-Derived – biologically-based dose-response modeling addressing kinetic and dynamic aspects (BBDR)

  18. CPSC - Dose Response Assessment: Carcinogens • Linear dose response • No threshold • Unless there is convincing evidence to the contrary (mode of action) • Surface area scaling • Humans are 5- to 10-fold more sensitive than rodents

  19. Risk Characterization • Integrates exposure data and dose-response (informed by hazard characterization) to obtain risk estimates • Provides risk managers with information regarding the probable nature and distribution of health risks • Has both quantitative and qualitative components • Clearly delineates uncertainty and data gaps

  20. Risk Characterization at CPSC • Non-Carcinogens • “Hazardous” if exposure > ADI • Carcinogens • “Hazardous” if cancer risk > 10-6 • That is, the ADI is the dose at 10-6 risk

  21. Childrens’ Risk Issues

  22. Available Frameworks • ILSI 2003, Workshop to Develop a Framework for Assessing Risks to Children from Exposure to Environmental Agents • EPA 2006, A Framework for Assessing Health Risks of Environmental Exposures to Children • WHO 2006 (draft), Principles for evaluating health risks in children associated with exposure to chemicals • CalEPA 2008, Technical Support Document For the Derivation of Noncancer Reference Exposure Levels

  23. Children’s Differences in Exposure • Different exposure scenarios • Mouthing behavior – age-dependent • Important for child-related products (toys, clothing) • Hand-to-mouth activity • Near the floor • More active • More food and water ingested per kg body weight • Accounted for in 1-day and 10-day health advisories for water (EPA) • Higher breathing rate – may or may not affect internal dose • Child –Specific Exposure Factors Handbook. EPA. 2008. http://cfpub.epa.gov/ncea/CFM/recordisplay.cfm?deid=199243

  24. Where is Children’s Risk Considered in the Paradigm? • Specific exposure scenarios • As part of human variability – this can be refined based on data, as noted in following slides • As part of consideration of overall database – consider whether have identified the critical effect, with particular attention to reproductive and developmental toxicity studies – quantitatively or qualitatively

  25. Differences in Toxicokinetics • Toxicokinetics = absorption (entering the body), distribution (where it goes), metabolism (how it is transformed), excretion (how it is removed) • There are age-related differences in all of these aspects, but the focus is primarily on absorption/deposition for inhalation exposures, and on metabolism. E.g.: • Infants have higher body water • Lower levels of key metabolic enzymes • Kidney excretion low in first year • All of these differences approach adult levels by end of first year or earlier

  26. Aspirin (salicylates) • Differences in metabolism between children and adults • Children are more susceptible to toxicity of methyl salicylate (oil of wintergreen) • Metabolic differences: Children have increased risk of acidosis when overdosed • Reye’s syndrome thought to be related to aspirin and age. Children seem to be particularly at risk

  27. Differences in metabolism between children and adults Different “safe and effective” OTC dose. (Children allowed ~ 30% more per unit body weight) Adults more susceptible to hepatotoxicity when overdosed Children have no significant risk of hepatotoxicity (Increased excretion of sulfate-acetaminophen) Difference in metabolism Children (<12 years) 45-55% sulfate, 15-30% glucuronide Adults 30% sulfate, 50% glucuronide Acetaminophen

  28. Implications of Age-Related Toxicokinetic Differences • Interpretation depends on the time period of focus – neonates differ in sensitivity by >3x for some chemicals, but duration of exposure as neonate is short, difference in sensitivity drops rapidly and is small by 1 year • Difference in sensitivity for neonates may be critical for acute exposures, need to look at mode of action for chronic interpretation • If toxicity is due to cumulative exposure, and average dose is important, increased internal dose to neonate has small impact, due to short duration • If chronic toxicity is due to peak exposure, the higher internal dose for neonates may be important

  29. Conclusions • Little information is available to refine considerations of toxicodynamic differences, but consideration of mode of action and pathways affected can be useful. • Toxicokinetic differences are largest the first year of life. • The quantitative implications of those differences depends on the exposure duration of interest and whether peak exposure is important • The ratio of mean child:mean adult dose was generally 2 or less, but the ratio can get large for certain combinations of active chemical form and age-related differences in clearance • After the first year of life, estimated mean child and mean adult doses are within ~50%.

  30. Cadmium

  31. Acute Effects at High Levels • Weak and brittle bones “itai – itai disease” • Bone become soft, lose mineral density, susceptible to fracture • Kidney tubular failure • Irreversible • Children’s risk? • Developing bones may be at higher risk

  32. Chronic Effects of Cadmium Exposure • Kidney is the most sensitive target • Cadmium accumulates in the kidney, and cumulative exposure across all routes (oral, inhalation, dermal) determines toxicity • Urinary excretion is related to total body burden, and can be used to estimate cumulative dose • Toxicity measured as a biomarker of effect – protein in urine

  33. Child Susceptibility to Chronic Effects • Because of the cumulative nature of the effect, children tend not to be at higher risk while children, but have more time to accumulate cadmium, and so may be at risk later in life • There is some evidence that adults exposed to cadmium as children may be more susceptible (for same internal dose) than people exposed only as adults

  34. Cancer • Inhalation exposure to cadmium associated with lung cancer in some worker studies and in laboratory animals • Several organizations consideration cadmium a known human carcinogen; others say “probable.” • Neither animal nor human data are adequate to determine whether cadmium is carcinogenic via oral route • Note route difference – mode of action

  35. Any Questions?

  36. Toxicodynamics: WHO 2006 Key Conclusions Regarding Critical Windows of Development • The greatest concern: agents that influence key signalling pathways, affect cell fate, or react with DNA • Different effects may result from exposure during early life stages and following adult exposure. • Effects shortly after fertilization are hard to identify and evaluate • Transient changes in physiology or endocrinology at critical periods of development can result in permanent changes in organ function.

  37. Impact of Adult/Child Differences in Ventilation Rate (Adapted from Clewell et al. 2004) • Uptake of vapors depends on ventilation rate only until steady state is achieved • At steady state, variation in ventilation rate (e.g., difference between adults and children) does not produce a significant variation in vapor uptake • Impact of ventilation rate is different for reactive gases – for those, normalized by surface area

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