Key Events Dose-Response Analysis. Part 1: Conceptual ...€¦ · Key Events and MoA (II) •The...
Transcript of Key Events Dose-Response Analysis. Part 1: Conceptual ...€¦ · Key Events and MoA (II) •The...
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ILSI Research Foundation
® Key Events Dose-Response Analysis.
Part 1: Conceptual Frameworkand Application to Chemicals
SOT RASS TeleconferenceJanuary 13, 2010
Alan Boobis (Imperial College London)George Daston (Procter & Gamble)Steve Olin (ILSI Research Foundation)
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ILSI Research Foundation
®
Dose-Response and Thresholds
• Recognition of the centrality of dose-response concept in life sciences
• QUESTION: Can our increasing understanding of modes of action provide insights for characterizing dose-response relationships at low doses (including thresholds) ?
• Not only for chemicals but also for other bioactive agents.
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ILSI Research Foundation
®
ILSI RF Threshold Working Group
• Characterizing fundamental biology of human health effects for chemicals, pathogens, allergens, nutrients
• Implications for dose-response, practical thresholds, public health standards
• Fostering cross-disciplinary discussion• → Key Events Dose-Response Framework
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ILSI Research Foundation
®
ILSI RF Threshold Working Group
• Chemical Group: Alan Boobis (Imperial College London), George Daston (Procter & Gamble), and Julian Preston (EPA).
• Nutrient Group: Sanford Miller (U Maryland), Joseph Rodricks (ENVIRON), Ian Munro (CANTOX), A. Catharine Ross (Pennsylvania State), Robert Russell (Tufts), and Elizabeth Yetley (retired NIH).
• Allergen Group: Steven Gendel (FDA CFSAN), Geert Houben (TNO), and Steve Taylor (U Nebraska).
• Pathogen Group: Bob Buchanan (U Maryland), Arie Havelaar (RIVM), Mary Alice Smith (U Georgia), and Richard Whiting (Exponent).
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ILSI Research Foundation
®
Work Products and Next Steps
• 5 papers – Crit Rev Food Sci Nutr, 49 (8), Sept 2009 (Overview, Chemicals, Nutrients, Pathogens, Allergens) – open access.
• Next Steps• Encourage the development of additional case studies
illustrating and evaluating the utility of the Framework• Organize small meetings and workshops to work through
specific examples• Explore application and integration of the Framework into
MOA analysis for risk assessment• CONTACT: Steve Olin ([email protected])
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Acknowledgements
Chemical Group: George Daston (Procter &
Gamble) and Julian Preston (EPA)
ILSI RF: Stephen Olin and Elizabeth Julien
All others in ILSI RF Threshold Working Group
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Derivation of reference values (RfDs, etc) for effects exhibiting non-linear dose-response relationships
Reference Dose (a reference value (RV)): “An
estimate, with uncertainty spanning perhaps an
order of magnitude, of a daily oral exposure to
the human population (including sensitive
subgroups) that is likely to be without an
appreciable risk of deleterious effects during a
lifetime”
The RV approach is based on the premise that
most toxicological endpoints have a true
biological threshold, although this is not
identifiable with accuracy
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Traditional approach to hazard characterization
Identify point of departure (NOAEL/BMDL), from
epidemiological or experimental evidence, to serve as
reference point, and apply default uncertainty factors
The POD is not a no-effect level and derivation of
“acceptable” doses requires assumptions about
thresholds and variability in those thresholds
In studies of inherently limited power, it is implicit that
there is uncertainty as to the magnitude of the
response, if any, at the POD
Are the assumptions in risk assessment conservative
overall?
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Derivation of reference valuesToxic effect
NOAEL
0 0.1 1 10 100 1000
1010
RV
UF
Test speciesAveragehumanSensitive
human
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Key Events Dose-Response Framework
ILSI Research Foundation established a tripartite,
multidisciplinary activity to develop an integrated
framework to incorporate advances in scientific
knowledge to support sound scientific decisions
Based on mode of action concept, with focus on
understanding the fundamental biology and dose-
response (including possible thresholds) at each
key event, to inform hazard characterization and
risk assessment
Crit. Rev. Food Sci. Nutr. 49(8), September 2009
– open access
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Mode of action and key events
Toxicological effect of concern
KEY EVENT (absorption)
EXTERNAL DOSE (exposure)
KEY EVENT (target tissue exposure
to ultimate toxic species )
KEY EVENT[S] (biological perturbation[s])
KEY EVENT[S] (pathological change[s])
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Factors operating at the level of a key event
DOSE
BIOLOGICAL INTERACTION OR PROCESS
Host characteristics(e.g.lifestage)
PROBABILITY OF EFFECTOF CONCERN MODIFIED
PROGRESSION TOWARDSEFFECT OF CONCERN
Physiological mechanisms(e.g.homeostatic, immune)
may operate to maintain normal
environment
Effects on shape of dose-response curve
Consequences for biological threshold
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Address each key event systematically
Is a minimum dose level required in order for this key event to
occur? What data would be needed to demonstrate this?
What response mechanisms (e.g. homeostasis, repair) are
involved? At what dose would these be overwhelmed?
What modifying factors (e.g. lifestage, disease state, nutritional
status) can potentially reduce the effectiveness of response
mechanisms? What factors can increase the effectiveness of
response mechanisms?
Do such modifying factors change the dose level at which
response mechanisms become overwhelmed? What data would
be needed to demonstrate this?
Is any one key event rate limiting, driving the shape of the
overall dose-response curve?
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Chloroform as a case study to investigate the KEDRF
Chloroform is hepatocarcinogenic
Mode of action (MOA) involves
hepatotoxicity
Risk assessment is based on evidence
that cancer arises only after a certain
degree of liver damage is produced and
maintained
Analyze MOA for mechanistic evidence
of thresholds
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Chloroform
Regenerative cell proliferation
Postulated MOA for CHCl3
Sustained cytoxicity
Tumor development
Key events
Cl H
Cl
Cl
C
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Key events for chloroform carcinogenicity
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Cytotoxicity
Homeostatic „steady state‟
Cellular adaptations
Reversible cell injury
Irreversible cell injury
Cell death
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Critical determinant of threshold
There is evidence that several of the key events in
chloroform carcinogenesis exhibit a threshold
It is not possible to determine which of these is the
critical determinant (if any), from available data
For this, studies in which each event was studied in
isolation would be necessary
Information from all biologically relevant models
should be used in such analyses. This is of particular
value for more distal key events, which will be less
compound specific
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Individual vs. population thresholds
Thresholds will vary among individuals
Once the determining key events are understood,
research to study contributions to population variability
(including identification of susceptible subpopulations)
can be targeted on those events
The goal is to understand how various factors (age,
gender, disease state, nutritional status, etc.) may
quantitatively affect the doses at which those
determining events occur
Some key events are likely to show absolute population
bounds, thus determining population thresholds
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Conclusions
Identify key events at the appropriate level of
biological organization
Contribution of toxicogenomics
Ensure that all important events are included,
and that non-essential events are not included
Understand interindividual variability in the rate
determining molecular events involved, to
enable a true population threshold(s) to be
identified
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Key Events Dose-Response Analysis:
Carcinogens and Estrogens
George P. Daston
The Procter & Gamble Company
SOT RASS Teleconference, January 13, 2010
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Testing the Threshold Assumption:
New Research
• Research on the basis of cancer has led to
the understanding that multiple cellular
changes are needed to progress from
normal to a cancerous state
• Research in gene expression at a genomic
level is helping to provide experimental
data at the low end of the dose-response
curve
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Evidence of Thresholds for
Mutations- Mice
0
10
20
30
40
50
60
70
80
0 25 50 75 100 150 200 250
Muta
tions/ Locus
ENU (mg/kg)
(Russell et al., 1982)
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Evidence for Mutation Thresholds
in Drosophila
0
0.1
0.2
0.3
0.4
0.5
0.6
0.7
0.8
0.9
1
0 0.02 0.04 0.06 0.14
Sperm
Oogonia
No. Leth
al M
uta
tions
ENU (nmol/fly)
(Zimmering et al., 1989)
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Mechanisms of Carcinogenesis
Cancer is a multistep process based on the requirement of a cell to develop a set of 6 acquired characteristics leading to uncontrolled cell division and a survival advantage. These “steps” require genetic alterations (gene mutations and chromosome alterations). Specific phenotypes are selected based on growth advantage in a Darwinian selection model. The substrate is cells with an unstable genome
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a1 a2 a3
m1 m2
d1 d2
Normal
Cell
Initiated
CellMalignant
Cell
Multistage Model of Carcinogenesis
d3
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Key Events for Tumor Development:
DNA-reactive MoA
• Exposure of target cells to ultimate DNA-reactive and mutagenic
species
• Reaction with DNA in target cells to produce DNA damage
• (For Non DNA-reactive MoA DNA damage produced by other
processes but remaining key events the same)
• Replication or repair errors from damaged template
• Mutations in critical genes in replicating target cell
• Enhanced cell proliferation
• Additional mutations induced from DNA damage and replication
• Clonal expansion of mutant cells
• Preneoplastic lesions and neoplasms develop
• Malignant behavior
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Mode-of-Action and Cancer Risk
Assessment
The use of mechanistic data to define
mode-of-action for cancer risk
assessment is described in the current
U.S. EPA’s Guidelines for Carcinogen
Risk Assessment (2005). This provides a
framework for considering approaches to extrapolations from high to low doses and from biomarkers to tumors
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Key Events and MoA (I)
• To produce a gene mutation or a
chromosome structural alteration it is
necessary to have some form of DNA
damage (e.g., a DNA strand break, an
adduct) and to have DNA and cell
replication. Enhanced DNA damage
and/or enhanced cell proliferation will
increase the probability of producing a
genetic alteration.
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Key Events and MoA (II)
• The great majority of carcinogens that induce DNA damage will also induce cell killing that can lead to regenerative proliferation as noted by the key events for a DNA-reactive MoA. Thus, unique MoAs are quite unlikely; “combined” MoAs will be common. Thus, incorporating MoA into the tumor dose-response characterization requires consideration of key events with different dose-response curve shapes.
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Key Events and MoA (III)
• In the absence of sufficient data, EPA assumes a linear low dose response for tumors
• However, based on key events and MoA, it is very likely that other forms of dose-response are feasible. This view is enhanced by the fact that cancer is a complex process that is unlikely to be defined mathematically by a single mechanism.
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Genomics to Address Thresholds
• Intermediate step between initial molecular
interaction and frank effect
• High degree of sensitivity
• We have used this to demonstrate a lack
of a low-dose effect of estrogens on rat
testicular development
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1
10
100
1000
10000
100000
0.01 0.1 1 10 100 1000 10000
Antisense-Oligonucleotide (attomol)
Flu
ore
sc
en
ce
In
ten
sit
y M13
ICAP
CYP17
PPIB9
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Estrogen: Mechanism of Action
EE
/b
Estrogen-responsive genes
Organ Response
TransportersExtracellular matrix Enzymes
Cellular Response
Cytosol
Receptors
Specific mRNAs (Up- or Down-regulated)
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Key Events for an Estrogen-
Mediated Developmental Effect
• Binding of ligand to receptor
• Translocation to DNA and initiation of
gene transcription
• Cell and tissue responses
– Proliferation
– Changes in differentiation
– Physiological changes
– Angiogenesis
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1 2 8 24 48 72 96
Time (h)
Fluid imbibition
CellProliferation
Epitheliumremodeling
Regression to basal level
Transcription factors, cell signaling, vascular permeability, growth factors
mRNA and protein synthesis
Cell growth, differentiation, suppression apoptosis,
Cell cycle regulators
DNA replication and cell division
Tissue remodeling and cytoarchitecture
Immune response
Adapted from Fertuck et al. (2003); Moggs et al. (2004); and Naciff et al. (2007)
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Low Dose Issue
Is there a different transcript profile at low doses than at high doses?
What is the threshold for gene expression changes induced by exposure to estrogens?
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0
20
40
60
80
100
120
140
160
0.001 0.01 0.1 1.0 10.0
EE (mg/kg/day)
Nu
mb
er
of
gen
es a
ffecte
d
0
10
20
30
40
50
60
70
80
LL L M MH H
Doses
Nu
mb
er
of
Gen
es a
ffecte
d
Ges
BPA
Dose-Response of Gene Expression Changes Induced by EE, Ges or BPA in
Testis/Epididymis of the Developing Rat
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Genes whose expression is modified by EE
-8.0
-6.0
-4.0
-2.0
0.0
2.0
4.0
6.0
0.001 0.010 0.1 1.0 10.0
mg EE/kg/day
Fo
ld c
han
ge
ESTs, BF403853,
PgR
EST, S43529
IL4R
ESTs, AI029175
S100A8
ESTs, AI029175
ESTs, BE099979
Epsilon 1 globin
Series13
InCaBP
Cyp11a
Calbindin 2
CPA1
RLF or Isl3
StAR
Svs5
StAR (2)
Cyp17Genes whose expression is modified by BPA
-20.0
-15.0
-10.0
-5.0
0.0
5.0
10.0
0.002 0.020 0.500 50.0 400.0
mg BPA/kg/day
Fo
ld C
ha
ng
e
InCaBP
Epsilon 1 globin
HMGCS2
SLC16A2
EST, SCARB1
SCARB1
GSTA1 (K01932)
Gsta1 (S72505)
Cyp11a
CPA5
Svs5
StAR(AB006007)
StAR (AB001349)
Cyp17
Dose-response: Fetal Testis
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Population Threshold”
• Population Threshold: a dose below
which an effect will very likely not occur in
a population
• Must consider the mechanisms underlying
individual thresholds as well as the
variability of the population, and
background exposures
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Individuals may have differing
susceptibilities
Min
Min
Min
Max
Max
Max
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Conclusions
• New information about the mechanism of toxicity or disease production can be used to inform about the nature of the dose-response at low exposure levels.
• Detailed understanding of the steps from exposure through pathogenesis can be displayed in a key events framework to facilitate the development of models describing the quantitative behavior of critical steps in pathogenesis
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Conclusions 2
• New technologies will make it possible to empirically test for biological responses at low doses and may be useful in setting pragmatic thresholds
• Better information about the nature of biological responses at low exposure levels will make risk assessment less uncertain