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Title: EC Contract: FI6RCT2004508847

1

Risk Characterisation
Institute for Radiological Protection and Nuclear
Safety
For the ERICA project
2
Table of Content

What is risk characterisation?
What are the methods to characterise the risk?
ERICA Tiered Approach and Risk Characterisation
Definitions of Benchmarcks
How to derive those safe levels ?
Principles and assumptions of SSD
The two methods adapted for radioactive
substances
Methodology Applied To FRED Data
Application to FRED(ERICA) data
Illustration Chronic g external exposure
conditions
Comparison of the benchmarks values obtained with
the two methods
ERICA screening values (SSD method)
Conclusions for Tiers 1 and 2
Tier 3 Effect analysis towards more realistic
estimates to reduce the uncertainty

3
What is risk characterisation?
Exposure analysis (pathways, transfers, dosimetry)
Effect analysis (dose-effect relationships, safe
levels)
PED(R) Predicted Exposure Dose (rate) (Gy or
Gy/time) Or PNEC Predicted Exposure Concentration
(Bq/L or Bq/kg)
PNED(R) Predicted No-Effect Dose (rate) (Gy or
Gy/time)
Risk

Risk characterisation is the final step of any
Ecological Risk Assessment.

It represents the synthesis of information
obtained during risk
assessment for use in management decisions.
It includes an estimation of the probability (or
incidence) and
magnitude (or severity) of the adverse effects
likely to occur in
an ecosystem or its sub-organisational levels,
together with
identification of uncertainties.

4
What are the methods to characterise the risk?
Predicted Exposure Dose (rate)
Predicted No-effect Dose (rate)

Deterministic method

PNED(R)
PED(R)
The risk index is expressed as the ratio
PED(R)PNED(R)

Semi-probabilistic method

pdf
Uncertainty is introduced only in the exposure
estimate. The risk index is expressed as a
probability that the exposure estimate exceeds
the PNED(R).
1
0
pdf

Probabilistic method

1
A statistical distribution is also alsigned to
PNED(R) (e.g. a species sensitivity
distribution). This allows to calculate the
probability of the risk.
0
5
ERICA Tiered Approach and Risk Characterisation

Tiers 1 and 2 use deterministic method through
the Risk Quotient.

PED(R)PNED(R)
Risk characterisation requires risk assessment
benchmarchs,
the so called PNED(R) Tier 2, and the
corresponding
environmental media limiting activities Tier
1.

Tier 3 uses probabilistic method.

Problem Formulation
Fixed values in Tiers 1 and 2 (PNED(R ) for
acute(chronic) exposure conditions)

risk?

Tier 1 media-specific benchmarks are
backcalculated (the lowest environmental media
limiting activity concentration (water,
sediment, soil) Tier 2 Direct use of PNEDR
corresponds to biota limiting benchmarck
Tier 1 Screening

risk?

Tier 2 Generic Assess.

Methods to derive appropriate risk
characterisation
risk?

Tier 3 Full Assess.
Tier 3 no fixed value - Receptor/site-specific

risk?

6
Definitions of Benchmarcks

Benchmarks are numerical values used to
guide risk assessors at various decision
points in a tiered approach.

These values need to be provided by a
transparent and scientific
reasoning.
They correspond to screening values when they
are used in
screening tiers (e.g. ERICA Tiers 1 and 2).

These screening values are concentration, dose
or
dose rate that are assumed to be safe based
on.
exposure response information (e.g.
ecotoxicity test
endpoints found in FREDERICA). They
represent safe
levels for the ecosystem.

For radioactive substances, concentration are
expressed in Bq per
unit of volume or mass, dose in Gy and dose
rate in Gy per unit
of time.

7
How to derive those safe levels ?(1/2)

Methods recommended by EC for chemicals,
adapted for radioactive substances

The EC recommends to develop an assessment of
effect and to characterise
risk on ecosystems with the minimum amount of
empirical information while
using extrapolation methodology (Technical
Guidance Document TGD, EC
2003).

All existing approaches are based on available
ecotoxicity data, typically EC50
for acute exposure conditions (short-term) and
EC10 (preferred to NOEC) for
chronic exposure conditions (long-term).

Exposure-response relationship from ecotoxicity
tests (stressor, species, endpoint)

Effect ()
100
Observed data
Regression model
50
LOEC Lowest observed effect concentration
NOEC No observed effect concentration
10
Concentration (Bq/L or kg) Dose (Gy) Dose Rate
(µGy/h)
EC50 ED50 EDR50
EC10 ED10 EDR10
8
How to derive those safe levels ?(2/2)

Methods recommended by EC for chemicals,
adapted for radioactive substances

Whatever the method, the ecotoxicity data
selection is of major importance
as the benchmark values greatly depend on their
relevancy, their quality and
their quantity.

Two main methods, recommended by EC (TGD,
revised in 2003) to derive
PNEC for chemicals.

Safety Factor Method (SF method)
based on the application of safety factors to
ecotoxicity data stringent method as the PNEC
value is obtained by dividing the lowest critical
data by an appropriate SF ranging from 10 to 1000.

(2) Species Sensitivity Distribution Method
(SSD) based on a statistical extrapolation model
to address variation between species in their
sensitivity to a stressor.
9
Principles and assumptions of SSD (1/2)

Safe levels can be calculated with statistical
extrapolation models. The
extrapolation is made from tested endpoint(s)
for a set of tested species to
the same endpoint(s) in the full set of the
potentially exposed species.

Two main assumptions
The species for wich results are known are
representative, in terms of sensitivity, of
the totality of the species in the ecosystem.
The endpoints measured in laboratory tests are
indicative of effects on populations in
field.

PAF ( of Affected Species)
Calculation of a dose(rate) that is assumed to
protect a given of species In the Technical
Guidance Document (2003) the agreed
concentration is the hazardous concentration
affecting 5 of species with 50
confidence. For radioactive substances -gtHD5 or
HDR5 useful to derive PNED or PNEDR
respectively.
100
80
60
40
Dose (Gy) or Dose Rate (µGy/h)
20
5
0
1
10
100
1000
10000
PNED(R) x SF
HD(R)5
10
Principles and assumptions of SSD (2/2)

This method requires the selection of an
appropriate level of protection (95
of species). This cut-off value selected as
protective level for the entire
ecosystem can be argued on the basis of
ecological theories.

The aim of the cut-off value selection is to
indirectly protect ecosystem
structure and processes by protecting the most
sensitive species.

The more functionally redundancy that there is
in a system, the more
overprotective such an assumption will be. This
is adequate when changes
in structure is more sensitive than changes in
process.
In the difficult case of keystone species
(species playing much larger
functional role than others), the only way to
deal with a cut-off value as
protection level is to identify those
unprotected species and to examine
whether they correspond to an engineer.

11
The two methods adapted for radioactive
substances (1/2)
SF from 10 to 1000 according to rules given in
the TGD (2003)

Safety Factor Method

12
The two methods adapted for radioactive
substances (2/2)

Species Sensitivity Distribution Method

HD(R)5 for acute(chronic) PNED(R) combined with
a SF ranging from 1 to 5 according to rules given
in the TGD (2003)
13
Methodology Applied To FRED Data

STEP 1 Extracting appropriate data sets
Data from FRED sorted per ecosystem, per
exposure condition, per bibliographic reference
and per test . Quality of data describing each
test
is assessed.

FRED FASSET Radiation Effect Database

STEP 2 Building dose(rate)-effect relationships
Dose-effect relationship was built for each
accepted
test. Estimated toxicity values are ED50 for
acute
exposure or EDR10 for chronic exposure.
The quality of the fitted model was judged.

STEP 3 Deriving PNED(R) values
The two methods recommended by EC were applied
on the basis
of the estimated toxicity values accepted after
Step 2.
Comparison of the obtained PNED(R) values.

14
Application to FRED(ERICA) data

Data allocation per ecosystem and per exposure
pathway (external or internal
irradiation) and duration (acute or chronic).

Only data devoted to effects induced by external
irradiation pathway are
quantitatively adequate to be mathematically
structured in terms of dose-effect
relationships (Hill model).

15
Illustration Chronic g external exposure
conditions (1/2)

Set of toxicity values EDR10
geometric means per species and
effect category - obtained for
terrestrial, freshwater and marine
ecosystems.
Application of the SF method and the
SSD method on the dataset.

Results
AF method 3 EDR10 for 3 trophic level and lowest
value (contributing to the geometric mean of
31.3) equal to 6.7 µGy/h -gtSF10 PNEDR 0.6
µGy/h
16
Illustration Chronic g external exposure
conditions (2/2)

Comparison of species radiosensitivity among
ecosystems gave no difference
(bilateral Wilcoxon test, a0.05). This allowed
the construction of a unique SSD
for generic ecosystems (SWFWTER) chronically
exposed to external ?
irradiation.

Results
SSD method

HDR581.8
SF 5
rounded down and keeping 1 digit
PNEDR
10 µGy/h

17
Comparison of the benchmarks values obtained with
the two methods

As expected, the SF method gave much more
stringent screening
values. ERICA preferred to apply the SSD method
due the use of the
whole data set (not the lowest one).

18
ERICA screening values (SSD method)

The present safe levels were derived to be used
in the first tiers (and
generic ecosystem) of the ERICA tiered approach
that can be applied
across the range of activities that use
radioactive substances.

As they were derived on the basis of ecotoxicity
data from external g
irradiation, it is suggested when needed to
apply a safety factor to take
account for the higher biological efficiency of
a and b emitters.

19
Conclusions for Tiers 1 and 2

The present safe levels were derived to be used
in the first tiers (and
generic ecosystem) of the ERICA tiered approach
that can be applied
across the range of activities that use
radioactive substances. Our
values are consistent with background and with
former guidelines at
which no significant effects were expected (see
Table 16 in ERICA D5).

As they were derived on the basis of ecotoxicity
data from external g
irradiation, it is suggested when needed to
apply a safety factor to take
account for the higher biological efficiency of
a and b emitters.

Selection of the 95 cut-off level for the
application of the SSD method is consistent
with the threshold level used for chemicals
assessments in the
TGD.

To take account for the possible existence of
keystone species among
the 5 that are unprotected, we suggest to
identify the species and
the effect endpoint present in the lowest
quartile of the distribution and
to consider the possible consequences of this.

20
Tier 3 Effect analysis towards more realistic
estimates to reduce the uncertainty

For Tier 3, the ERICA consortium decided that it
would not be
appropriate to make specific recommendations on
numeric values.
Rather, guidance on the sorts of approaches
that may be applied for
refined effect analysis has been provided.

In ERICA D5, examples are given for several cases
as follows

To apply the SSD methodology to introduce more
ecological realism by
(1) using more conservative levels of protection
(95 to 99 )
(2) applying trophic/taxonomic weightings that
better describe the structure of a specific
ecosystem
(3) restricting the statistical analysis to a
particular endpoint
(reproduction) and/or a
particular trophic/taxonomic group (fish).