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“Benchmarking” Exposure Priority Setting Tools U.S. EPA Exposure Based Chemical Prioritization Workshop April 6 th /10 M.E. (Bette) Meek McLaughlin Centre.

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Presentation on theme: "“Benchmarking” Exposure Priority Setting Tools U.S. EPA Exposure Based Chemical Prioritization Workshop April 6 th /10 M.E. (Bette) Meek McLaughlin Centre."— Presentation transcript:

1 “Benchmarking” Exposure Priority Setting Tools U.S. EPA Exposure Based Chemical Prioritization Workshop April 6 th /10 M.E. (Bette) Meek McLaughlin Centre University of Ottawa

2 Outline Context –Increasing Efficiency What We’ve Learned from Exposure Profiling –Drawing on Canadian experience “Benchmarking” –“Groundtruthing” Some Potential Options in Moving Forward 2

3 The 4-Step Paradigm Risk Assessment Hazard Identification Risk Assessment & Characterization Exposure Assessment & Characterization Dose Response Assessment & Characterization Introduced in the mid 1980’s by the U.S. National Academy of Sciences

4 4 Risk Assessment – Qualitative/Quantitative Hazard Identification (qualitative - is it toxic?) –Effects seen in animals and/or humans Dose Response Analyses (quantitative – how toxic to humans?) –Shape of the dose response curve Range of observation & inference –Quantitative relevance to humans Exposure Estimation Risk Characterization –Comparison of Exposure and Effect

5 McLaughlin Centre University of Ottawa 5 Risk Assessment (organizing & analyzing to set priorities & guide management) hazard identification/ characterization dose-response exposure estimation risk characterization political social economic Engineering Risk Management (decision & action) Increased Efficiency

6 Keep in Mind: The appropriate performance indicator for chemicals programs is not priority setting, testing nor assessment but rather: Effective and efficient management of risk –Now 6

7 Evolving Mandates for Existing Chemicals Dealing with “grandfathered” chemicals Canada –“Categorization” (i.e., systematic priority setting) for 23, 000 chemicals by Sept., 2006 under the Canadian Environmental Protection Act (CEPA) Environmental, Consumer Europe –Registration, Evaluation and Authorization of Chemicals (REACH) (2007) Volume trigger and hazard based Consistency between Existing and New Chemicals Industry Responsibility U.S. –Voluntary Testing Initiatives –Renewal of the Toxic Substances Control Act (TOSCA) 7

8 Implications of Regulatory Developments to Consider All Chemicals Need for increased efficiency in risk assessment & management –Processing much larger numbers of substances Requires more integrated approach across compounds (less chemical-specific; more contextually relevant) More/better predictive tools & more efficient testing –Drawing on new technologies Requires a shift in approaches, testing and assessment strategies 8

9 The NAS 4-Step Paradigm The Need to Move On Hazard Characterization Risk Assessment & Characterization Exposure Assessment & Characterization Dose Response Assessment & Characterization Earlier focus on exposure & how effects are induced (mode of action)

10 The Challenge to the Risk Assessment Community We need to be much more: Efficient Predictive Application Driven (i.e., risk management) Reponsive, & Communicative McLaughlin Centre University of Ottawa 10

11 The Challenge to the Risk Assessment Community (Cont/d) Broadly drawing upon the existing experience on relatively limited numbers of chemicals, to “inform” efficient assessment and management of the remainder Essential basis for “benchmarking” CEPA “Categorization” of Existing Chemicals offered unique opportunity –Required consideration of “all” 11

12 CATEGORIZATION of the Domestic Substances List (DSL) (First Phase) (n=23,000) Decisions of Other Jurisdictions Public Nominations No further action under this program CEPA-Toxic No further action under this program CEPA-Toxic IN-DEPTH ASSESSMENT - Priority Substances List (Third Phase) Risk Management Greatest Potential for Human Exposure Substances that are Persistent or Bioaccumulative “Inherently Toxic” to Humans “Inherently Toxic” to non-Human Organisms SCREENING ASSESSMENT (Second Phase) CEPA 1999 Existing Substances Program INCREASING REFINEMENT OF PRIORITIES + COMPLEXITY OF ASSESSMENT 12 DECREASING NUMBERS OF SUBSTANCES DECREASING UNCERTAINTY

13 13 Simple and Complex Priority Setting Tools EXPOSURE Simple Exposure Tool (SimET) - Relative ranking of all DSL substances based on submitters (S),quantity (Q) and expert ranked use (ERU) Complex Exposure Tool (ComET) - Quantitative plausible maximum age-specific estimates of environmental and consumer exposure for individuals based on use scenario (sentinel products), phys/chem properties & bioavailability HAZARD Simple Hazard Tool (SimHaz) - Identification of high or low hazard compounds by various agencies based on weight of evidence and expert opinion/consensus Complex Hazard Tool (ComHaz) - Hierarchical approach for multiple endpoints & data sources (e.g., (Q)SAR) including preliminary weight of evidence framework Potential for exposure influential in setting priorities Included simple use profiling for all 23, 000 chemicals, more complex use profiling for priorities

14 The Simple Exposure Tool - SimET SimET is the tool by which we “binned” and relatively ranked all 23,000 substances Based on three different lines of evidence, derived from the limited information provided for all substances on the DSL: –quantity (estimated annual quantity of use, Q), –number of submitters (S) –use (sum of normalized expert ranked use codes, U), reflecting two workshops “Ground-truthed” against more robust and recent data on use –Commercial chemical profiles –Mandated use surveys Use far more important than volume as the critical driver 14

15 Potential for Exposure (Greatest, Intermediate & Lowest) Quantity (kg/year) Number of Submitters Sum of Expert Ranked Use Codes GPE > 100 000Top 10% IPE > 10 000n.a.Top 30% LPE All Score for each substance = ∑ (use x relative ranking for PE ) – e.g., direct consumer use, dispersive environmental, industrial, etc. 15

16 16 Post Categorization Refinement of Exposure (Complex Tool) Objective: Multi-tiered approach for consumer and environmental exposure –generic scenarios, defaults and most common use/product categories in early stages E.g., sentinel products - consumer product that yields the highest exposure for one of its component substances –Increasing refinement in subsequent stages Methodology: –Comparison of algorithms and default values in consumer exposure tools as basis for iterative approach 8 models/algorithms Range of sources of default values –Development of use profiles for hundreds of chemicals based on robust search strategies

17 17 Chemical Identity Physical/ Chemical Properties Substance Profile Production Quantity Measures of Dose- Response for Critical Effects Priority for Assessment Production Quantity Bin + Release Factor Emissions Near-fieldFar-field Human Exposure Sentinel Products SP 1 SP 2 SP 3 SP n Far Field Age Specific Variables Overview of Early Tier

18 18 Tier 1 Model Comparison – Sample of Most Common Product Categories Product CategoryRoute of ExposureComETConsExpoECETOCCEMSDA Personal Care and Over-the-Counter Products Mucous membrane contact productsInhalation (lipstick, toothpaste/mouthwash, eye makeup, contact cleaner)Dermal XX X Oral X X Leave-on ProductsInhalation XX X (creams, deodorant, hair preparations, face make-up, powder)Dermal XX X Oral Rinse-off ProductsInhalation (soaps, shampoo/conditioner, cleansers)Dermal XX XX Oral Over-the-Counter ProductsInhalation (wipes, shaving aids, oral dosing, topical dosing, lubricants)Dermal XX X Oral X X

19 What Did We Learn re Exposure “Surrogates”? Simple use profiling can be discriminating Importance of consumer vs. environmental exposure Persistence/bioaccumulation ≠ exposure Volume ≠ exposure; use profiling more influential implications for selection criteria for current testing programs Importance of early and iterative use profiling Much of the information is publically available 19

20 What Did We Learn re Exposure Tools? Criteria for consideration of algorithms and default values: Transparency, Defensibility “Validation”/Acceptance and Use Scope Relevance Complexity for various iterations Observations: Transparency was limited –“expert judgment” No consistency in default values, or algorithms for “screening” vs. more robust models –Limited incentive to harmonize or draw upon the work of others Range of coverage is limited Early tiers for consumer exposure provided limited additional discrimination 20

21 The Challenge to the Risk Assessment Community (Cont/d) So, how do we get there? Broadly drawing upon the existing experience on relatively limited numbers of chemicals, to “inform” efficient assessment and management of the remainder Essential basis for “benchmarking” 21

22 Potential for “Benchmarking” Relative rankings for “potential for exposure” for 23, 000 substances (use “weighted”) More detailed use profiling for several hundred substances Detailed multimedia exposure estimates for a proportion (approx. 100 Priority Substances), including: –Compilation of phys/chem properties –Probabilistic estimates based on national monitoring data for a portion –Measured consumer exposure for a portion –Some with biomonitoring data 22

23 23 Individual sublists are then rank ordered using the PE Score (the highest score = the highest priority)

24 Considerations for “Benchmarking” Select chemicals for quantitative “anchoring” of “surrogates” balancing: –broadest representation of “chemical space” i.e., range and nature of uses, physical/chemical properties Availability of data, as a basis for robust exposure estimates –Monitoring, biomonitoring Objective is to select for the simplest and most discriminating “determinants” of exposure “Designing” to limit exposure 24

25 Evolution of Risk Assessment RA/RM Paradigm Guidelines/Methods Dosimetry/PbPK RA/RM Paradigm Guidelines/Methods Dosimetry/PbPK 1980s Mode of Action Susceptible Populations Mixtures Mode of Action Susceptible Populations Mixtures Toxicity Pathways Integrated Approaches CompTox Toxicity Pathways Integrated Approaches CompTox 1990s 2000s 21 st Century 1983 1994 2007 2009

26 How Quickly does Risk Assessment Evolve? In 1984, the “benchmark dose” was introduced –Now receiving widespread acceptance 25 yrs. later Much guidance, many recommendations on analysis of uncertainty since the 1980’s –Several NAS & EPA reports Incorporation of PBPK modelling –Since the late 1980’s Formal consideration of mode of action; chemical specific adjustment factors (National & International) –Since the late 1990’s Tiered assessment (‘94 NAS report) Problem formulation –EPA Guidance on Risk Characterization (2000) 26

27 Barriers to Change A function (in part) of: –The past focus on “Hazard” –Traditional approaches “codified” “institutionalized” (requiring limited expert interpretation), easy to explain to stakeholders & somewhat consistent –Lack of long term planning for regulatory science Meeting short term deadlines for numbers of assessments vs. longer term investment in predictive methodology –Communication: Lack of “user friendly” tools –Lack of coordination of regulatory risk assessment/research 27

28 The Future of Chemical Risk Assessment Optimistic re the availability of more predictive tools drawing on greater exposure and biological knowledge Less optimistic re the will and capability to efficiently implement change –Collective leadership 28

29 IPCS Framework for Combined Exposure to Multiple Chemicals Early and Continuing Consideration of Exposure Criteria for Considering an Assessment Group What is the nature of exposure and are the components known? Is exposure unlikely or very low taking into account the context? Is there a likelihood of co-exposure within a relevant time frame ? What is the reason to believe that components act similarly or interact? –Information on chemical structure –Hazard or other biological data (tox or efficacy) 29

30 Yes, no further action required No, continue Input from exposure or hazard assessments (iterative process) Is the margin of exposure adequate ? Increasing refinement of exposure models Increasing refinement of hazard models (MOA) Sample Tiered Exposure and Hazard Considerations Mixture or Component Based Tier 0 Simple semi- quantitative estimates of exposure Tier 1 Generic exposure scenarios using conservative point estimates Tier 2 Tier 3 Probabilistic Exposure Estimates Tiered Exposure Assessments Tier 0 Dose addition for all components Tier 2 More refined potency (RPF) and grouping based on MOA Tier 3 PBPK or BBDR; probabilistic estimates of risk Tier 1 Refined potency based on individual POD, refinement of POD Tiered Hazard Assessments Refined exposure assessment, increased use of actual measured data See text for details 30

31 More Information? Existing Substances Division Website – http://www.hc-sc.gc.ca/exsd-dse http://www.hc-sc.gc.ca/exsd-dse IPCS Harmonization Website http://www.who.int/ipcs/methods/harmonization/i ndex.html 31

32 A.1 Models and Sources of Algorithms Considered ComET (developed by Health Canada and The LifeLine Group) ConsExpo v. 4.0 ECETOC (from Targeted Risk Assessment 2004 Technical Report No. 93) Soap and Detergent Association 2005 EAU – Cosmetic Workbooks (Health Canada’s Environmental Assessment Unit) CEM v. 1.2 (from US EPA E-FAST) U.S. EPA 1997 (Exposure Factors Handbook Volume I) Health Canada 1995 (Handbook for Exposure Calculations) 32

33 A.2 Default Values Considered Versar Inc., 1986. Standard Scenarios for Estimating Exposure to Chemical Substances During Use of Consumer Products, Volume I and II ConsExpo v 4.0 (and RIVM Factsheets) SDA (Soap and Detergent Association) 2005. Exposure and Risk Screening Methods for Consumer Product Ingredients ECETOC 2004. Targeted Risk Assessment, Technical Report No. 93 ComET (Health Canada/LifeLine) US EPA 1997. Exposure Factors Handbook Volume III – General Factors EAU (Environmental Assessment Unit – Health Canada) 2005. The Cosmetics Exposure Workbook Various books on product formulations to obtain weight fractions 33


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