Chapter 2: Introduction/Background
2.1 General Background
Since the publication of Rachel Carson’s Silent Spring (Carson,
1962), there has been increasing awareness that chemicals in the
environment can exert profound and deleterious effects on wildlife
populations and that human health is inextricably linked to the
health of the environment. The last two decades, in particular, have
witnessed a growing scientific concern, public debate, and media
attention over the possible deleterious effects in humans and wildlife
that may result from exposure to chemicals that have the potential to
interfere with the endocrine system. The intensity of the concerns
and lack of consensus among scientists can best be ameliorated by an
objective evaluation of the available scientific data on the potential
adverse effects of these chemicals from a global perspective.
Countries lacking the necessary infrastructure to monitor and
evaluate these chemicals expressed a particular need for an objective
international assessment. The document builds on existing
assessment documents and reviews (see Table 2.1) and is not
intended as a thorough, comprehensive literature review. Only peer-
reviewed literature or publicly available reports were evaluated. It is
not a risk assessment or consensus document. Neither is it an
assessment of available test methodologies for detecting EDCs. Both
the OECD and a number of national organizations are addressing
these issues (ECETOC, 1996; OECD, 1998a, 1998b, 1999a; US
EPA, 1998a; Kanno et al., 2000).
EDCs encompass a variety of chemical classes, including natural
and synthetic hormones, plant constituents, pesticides, compounds
used in the plastics industry and in consumer products, and other
industrial by-products and pollutants. They are often pervasive and
widely dispersed in the environment. Some are persistent, can be
transported long distances across national boundaries, and have been
found in virtually all regions of the world. Others are rapidly degraded
in the environment or human body or may be present for only short
periods of time but at critical periods of development.
List of Abbreviations
AhR Aryl hydrocarbon receptor
DDE Dichlorodiphenyl dichloroethylene
DDT Dichlorodiphenyl trichloroethane
EDCs Endocrine-disrupting chemicals
ECETOC European Centre for Ecotoxicology and Toxicology of Chemicals
ER Estrogen receptor (α and β isoforms)
IUPAC International Union of Pure and Applied Chemistry
JEA Japan Environment Agency
LH Luteinizing hormone
MRC Medical Research Council
NRC National Research Council
NTP National Toxicology Program
OECD Organisation for Economic Co-operation and Development
PCBs Polychlorinated biphenyls
PCDDs Polychlorinated dibenzodioxins
PCDFs Polychlorinated dibenzofurans
POPs Persistent organic pollutants
SETAC Society for Environmental Toxicology and Chemistry
TCDD 2,3,7,8-Tetrachlorodibenzyl-p-dioxin
UBA Umweltbundesamt (German Environmental Agency)
UNEP United Nations Environment Programme
US EPA United States Environmental Protection Agency
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2.2 Generic Issues
There are a number of complex issues that must be considered when
evaluating the effects of endocrine disruptors (Ashby et al., 1997b;
Ashby, 2000). These are summarized in this chapter and are
discussed in detail in subsequent chapters (detailed references are also
provided in subsequent chapters). Studies that clearly address
exposure–outcome relationships are the most valuable in assessing
the impact of EDCs on wildlife and human health. Unfortunately,
many of the epidemiological or wildlife studies do not have good
measures of exposure, which limits our ability to draw firm
conclusions from them. This problem is especially prevalent for
those EDCs that are rapidly degraded in the environment or in the
human body. This means that the exposure that might have caused
an adverse outcome (e.g., a reproductive deficit) is not detectable at
the time that clinical manifestations become evident. For this reason,
most of the EDCs that are relied on to draw cause-and-effect
relationships are those that are biologically and ecologically persistent
(e.g., PCBs, DDT, and dioxins). A number of these POPs are
known to endanger human health and ecosystems and have been the
subject of global conventions. Twelve POPs were singled out for
elimination and/or reduction in a legally binding global treaty,
which was signed by 115 countries in Stockholm in May 2001.
These initial 12 high-priority POPs were selected based on data that
demonstrate adverse exposure–outcome relationships in humans and
wildlife, and processes are being implemented to add additional
chemicals to the list.
This document emphasizes those chemical exposures and
adverse human and ecological outcomes where an indication of cause
and effect via multiple mechanisms of endocrine disruption has been
demonstrated or hypothesized. These case studies also illustrate the
types of interferences that are of importance and the variety of
adverse health outcomes that can be exhibited.
One of the major issues that needs to be addressed when
evaluating the impact of EDCs on human health and the
environment is whether effects reported in the literature represent
isolated cases or more global responses. For example, diminished
wildlife populations adjacent to a significant point source may not be
indicative of global responses. In contrast, relatively small effects on
wildlife or human health points might have great impact if those
responses are global in nature. Another problem in assessing the
health impacts of EDCs is that some of these chemicals have been
shown to contribute to the incidence of common diseases of
multifactorial etiology (e.g., infertility, cancer, neurobehavioral
deficits). Therefore, it will be difficult to attribute effects in
traditional epidemiology studies to EDCs unless those effects are
seen in large numbers of people.
2.3 Mechanisms of Endocrine Disruption in
Humans and Wildlife
There are a number of mechanisms whereby EDCs can modulate
endocrine systems and potentially cause adverse effects (see also
Chapter 3). The generally accepted paradigm for receptor-
mediated responses includes binding of hormone to its receptor at
the cell surface, cytoplasm, or nucleus, followed by a complex series
of events that lead to changes in gene expression characteristic for a
specific hormone (Birnbaum, 1994). It is thought that changes in
gene expression represent an early but critical step in the regulation
IPCS GLOBAL ASSESSMENT OF EDCS

Table 2.1 - Selected Workshop/Committee/Assessment Reports on Endocrine Disruption

Year Organization Purpose/Scope Reference
1992 World Wildlife Fund Examination of the commonalities of adverse effects in wildlife, experimental animals, Colborn and Clement, 1992
and humans. Produced the “Wingspread Consensus Statement”
1994 National Institute of Review of cellular biology, developmental effects, sources, and global health implications Maclachlan and Korach, 1995
Environmental Health Sciences of environmental estrogens
1995 German Federal Environmental Discussion about the occurrence and impact of endocrine disruptors and the potential German Federal Environment
Agency risks that may arise to humans and the environment Agency, 1996
1995 Ministry of Environment Evaluation of the effects of estrogens on male reproductive development and function Toppari et al., 1996
and Energy, Denmark
1995 US EPA Workshop on research needs for the Risk Assessment of health and environmental Kavlock et al., 1996
effects of endocrine disruptors (April 1995)
1995 Chemical Manufacturer’s Association; Workshop on screening methods for chemicals that alter thyroid hormone homeostasis, Ankley et al., 1998a
World Wildlife Fund; US EPA action, and function
1995 UK Medical Research Council Assessment on Environmental Estrogens: Consequences to Human Health and Wildlife MRC Institute for Environment
Institute for Environment & Health and Health, 1995
1996 European Commission European workshop on the impact of endocrine disruptors on human health and wildlife, European Commission, 1996
Wyebridge U.K.
1996 ECETOC Compendium of test methods for environmental estrogens ECETOC, 1996
1996 SETAC Workshop on principles and processes for evaluating endocrine disruption in wildlife Kendall et al., 1998
1996 US Committee on the Environment Development of a national planning framework for endocrine disruptor research and Reiter et al., 1998
and Natural Resources analysis of the existing federally funded research projects to help identify information gaps
1996 US EPA Workshop on the development of a risk strategy for assessing the ecological risk of Ankley et al., 1997
endocrine disruption
1997 UNEP, US EPA, White House Office International workshop on endocrine disruptors UNEP, 1997
of Science and Technology;
Alton Jones Foundation
1997 Federal Environment Agency, Germany Workshop on effects of endocrine disruptors on neuronal development and behavior UBA, 1997
1997 SETAC, OECD, European Commission Expert Workshop on Endocrine Modulators and Wildlife: Assessment and Testing SETAC, 1997
1997 US EPA Special report on environmental endocrine disruption: an effects assessment and analysis US EPA, 1997
1997 OECD Critical assessment of the ability of existing OECD test methods to detect sex hormones OECD, 1997
disrupting potential
1997 Health Council of the Netherlands Evaluation of the effects of endocrine disruptors on human reproduction and development Health Council, Netherlands,
1997
1997 International Life Sciences Institute; Scientific evaluation of the potential for substances in the diet to influence the ILSI, 1998
US EPA human endocrine system
1997 Japan Chemical Industry Association Evaluation of status and research needs of endocrine disrupting compounds in Japan Japan Chemical Industry
Association, 1997
1998 Swedish Environmental Protection Endocrine disrupting substances-impairment of reproduction and development Olsson et al., 1998
Agency
1998 International Union of Pharmacology Natural and anthropogenic environmental estrogens—the scientific basis for IUPAC, 1998
risk assessment
1998 Society of Environmental Toxicology Workshop on endocrine disruption in invertebrates DeFur et al., 1999
and Chemistry
1999 National Research Council Hormonally active agents in the environment NRC, 1999
1999 European Commission Scientific committee on toxicity, ecotoxicity, and the environment opinion on human Vos et al., 2000
and wildlife health effects of endocrine disruptors
2000 Health and Environment Canada Workshop on endocrine disrupting substances in the Canadian environment Servos and Van Der Kraak, 2001
2000 US National Toxicology Program Report of the endocrine disruptors low-dose peer review NTP, 2001a
2000 Finnish Environment Institute Research for Management of Environmental Risks from Endocrine Disruptors Assmuth and Louekari, 2000
2001 Federal Environment Agency, Germany Second status seminar on endocrine disruptors UBA, 2001a

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of normal biological function, including cell proliferation and
differentiation responses essential for normal development and
the function of multiple organ systems. Although there is
considerable information on the early molecular events involved
in hormone response, there is very little knowledge concerning
the relationship between those molecular events and adverse
health effects such as cancer or reproductive toxicity. This
knowledge gap is perhaps the most limiting factor in our ability to
evaluate exposure–response relationships, particularly following
low-level exposure to potential EDCs. The use of new approaches
in molecular epidemiology and animal model systems has the
potential to yield additional valuable information for elucidating
the role of these mechanistic determinants of specificity at low-
dose exposures to potential EDCs and for improved risk
evaluations for the adverse health effects of EDCs. There are
numerous experimental systems available for evaluating the
interactions of exogenous or synthetic chemicals with hormone
systems, particularly those that interact with the estrogen,
androgen, thyroid, and AhRs (Bolander, 1994). However, there is
a growing body of knowledge that interactions of chemicals with
other receptor systems also may be important in the EDC arena.
These include the retinoic acid receptor, cytokine systems, and a
number of so-called orphan receptors (receptors without
unknown ligands and/or functions) such as the peroxisome
proliferator receptor system. In general, these receptor systems are
remarkably well conserved phylogenetically, suggesting that data
from wildlife and experimental models should be useful, although
not necessarily definitive, for estimating risks from EDC exposure
to humans.
The mechanism or mode of action of EDCs is not limited to
those agents that interact directly with hormone receptors. Other
mechanisms of interest include inhibition of hormone synthesis,
transport, or metabolism and activation of receptor through
processors such as receptor phosphorylation or the release of cellular
complexes necessary for hormone action. In the case of hormone
synthesis, considerable research has been conducted on the
aromatase inhibitors that prevent the conversion of androgens to
estrogens through a cytochrome P450 system that is highly
conserved in many species. Several fungicides have been shown to
cause infertility by aromatase inhibition. In addition, there is a
growing awareness that multiple receptor systems act in concert to
regulate biological functions. For example, “cross talk” between the
ER and growth factor receptors appears necessary for estrogen
signaling of mammary cells to divide or differentiate. These events
are critical for explaining several risk factors for breast cancer such
as age at menarche, age at menopause, or effects of numbers of
pregnancies. There are numerous other kinds of cross talk between
various constituents of the endocrine system, and an understanding
of the mechanisms involved could improve our ability to produce
credible health assessments of EDCs. One well-known example of
“cross talk” involves antiandrogen-mediated elevation of
endogenous estrogen levels due to increased LH production.
Other examples of EDCs capable of acting at multiple cellular
sites via multiple endocrine mechanisms are discussed in detail in
Chapter 3. For example, the pesticide methoxychlor displays
estrogen agonist (ER-β) activity because some of its metabolites
bind to the ER. It also possesses antiandrogenic actions through a
more poorly defined mechanism involving the hypothalamic-
pituitary-gonadal axis. Another example is the ability of the DDT
metabolite DDE to act as an antiandrogen by inhibiting
testosterone binding with the androgen receptor, but these
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CHAPTER 2: INTRODUCTION/BACKGROUND
antiandrogenic effects may also be facilitated by the effects of DDE
on steroid-metabolizing enzyme expression.
There are many factors that should be considered when
utilizing mechanistic information on EDCs in health assessments.
Of particular concern are species, interindividual, and tissue
specificity in endocrine signaling pathways. Differential
responsiveness to EDCs has been observed between different
species and extends to interindividual differences within a species
and between different tissues as well. The biologic and molecular
mechanisms underlying this specificity are quite diverse.
Determinants of species specificity include differences that exist
between species in receptor binding, gene transcription patterns of
gene expression, and cellular responses to endocrine-active
compounds. Interindividual differences in responsiveness may be
determined at the level of genetic polymorphisms in hormone-
metabolizing enzymes, hormone receptors, and those genes that are
activated by these receptors. Our rapidly growing knowledge base
emerging from the human genome project will enable the design of
rational studies on the impact of EDC exposures on hormonally
sensitive end points in groups that may be genetically predisposed.
Extrinsic factors such as diet can also impact individual
susceptibility to endocrine-active agents.
The organochlorine chemicals provide interesting insights
regarding the mechanisms of action for EDCs. In the case of the
dioxins, the scientific consensus is that most, if not all, of their
effects require an initial interaction with a cellular protein termed
AhR (Poland and Glover, 1977). As discussed in Chapter 3, the
ligand-bound AhR is capable of interacting with a number of
critical signal transduction pathways, leading, for example, to
involvement with xenobiotic metabolizing enzymes, steroid
receptor signaling, growth factor expression, circadian clocks,
responses to hypoxia, and angiogenesis. Through these varied
interactions, such chemicals are able to induce a wide spectrum of
biological effects at a number of different life stages in a variety of
species, and some of these responses do not easily fit the traditional
definition of endocrine-mediated events. Although adverse
biological effects mediated via the activation of AhR are certainly of
concern, a higher burden of proof is needed to identify such effects
as due to endocrine disruption than merely the correlation between
ability to bind to the receptor and the elicitation of some biological
effect. In this regard, the considerations detailed in section 3.16
were used in evaluating the extent to which information would be
included in this document. Although information on the
involvement of the AhR in wildlife is limited, in our final
conclusions on the strength of the evidence for relationships
between chemicals and endocrine-mediated effects, the same
criteria were applied for both humans and wildlife.
2.4 Dose–Response Relationships
The issue of dose–response relationships is perhaps the most
controversial issue regarding EDCs. One of the reasons is that
EDCs often act by mimicking or antagonizing the actions of
naturally occurring hormones. These hormones are already at
physiologically functional concentrations, so the dose–response
considerations for EDCs are often different than for other
chemicals that are not acting directly on the endocrine system.
Reported low-dose effects for EDCs have come under intense
scrutiny regarding the question of the adequacy of traditional
toxicology testing paradigms for detecting low-dose effects. A recent
workshop on this issue (NTP, 2001a) concluded that although low-
dose effects may be occurring, those effects often are not replicated
IPCS GLOBAL ASSESSMENT OF EDCS
consistently, and the toxicological significance of the reported
effects is not known. Dose–response issues should be explicitly
considered when studies are designed for risk evaluation for health
or wildlife effects. Of particular relevance is the issue of dose
selection. Ideally, the doses used should span a wide range to
identify both toxic and mechanistic end points. The issue of dose
selection has become critical to the current controversies
surrounding the issue of biphasic dose–response curves for EDC
effects on end points such as prostate weight. Although there may
never be complete knowledge on the mechanism(s) of action for
any chemical, some knowledge of key events could help clarify
dose–response relationships.
Timing of exposure is also critical to the understanding of
dose–response relationships for EDCs. Numerous examples exist in
the literature where age at exposure is a known risk factor. For
example, endocrine disruption of the developing brain can
permanently alter behavior, whereas similar exposures to a fully
differentiated brain could be without effect. Ecological and wildlife
effects are also strongly influenced by the timing of exposure (e.g.,
during the breeding season).
Population heterogeneity is another important factor in
dose–response evaluation. For human health, a number of factors
contribute to a wide range of risks, including genetic
predisposition, age, gender, diet, disease conditions, and past
exposures. The range of risk modulators may be even greater for
complex ecosystems, but little information is available in this area.
Evaluation of the dose–response relationships for health and
environmental effects of endocrine disruptors will be most credible
when information is available from several sources (e.g., toxicity
studies, mechanistic and epidemiological studies, and field studies).
There are a number of issues that are helpful to consider when
embarking on dose–response assessment. These include, but are not
limited to, 1) the adequacy of relevant experimental models for
evaluating potential human effects of low-dose exposure to endocrine
disruptors, 2) state of knowledge concerning quantitative relationships
among the various processes maintaining homeostasis for the tissue,
organ, or function being studied, 3) how perturbations in homeostasis
lead to disease or dysfunction, 4) whether these changes can be
quantified, 5) an understanding of the mechanisms through which
endocrine disruptors perturb homeostasis and endocrine function and
alter the risks from that of normal levels of endogenous hormones, 6)
consideration of how differences in lifestyle factors (diet, nutrition,
etc.) affect sensitivity to endocrine disruption, 7) an understanding of
how the age of the endocrine system alters sensitivity to endocrine
disruption, and 8) how interindividual differences (based on genetic
variation) in constituents of endocrine pathways (e.g., receptor
variants) alter responses to endocrine-sensitive end points caused by
exposure to EDCs. Most of these considerations are relevant to both
human and wildlife effects of EDCs.
A common dose–response relationship for all effects and for
all endocrine disruption mechanisms should not be expected.
This conclusion is based on the knowledge that there are many
different kinds of hormonal actions of chemicals categorized as
endocrine disruptors. These activities include estrogenic,
antiestrogenic, antiandrogenic, growth factor modulation,
cytokine and thyroid modulation, modulation of hormone
metabolism, among many others.
2.5 Exposure Issues
There are numerous chemicals in the environment (e.g., pesticides,
industrial chemicals, and natural products) that are hormonally
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active, and these can be detected in people and wildlife as well as in
environmental samples. Some of these persist in the environment
and others do not. Some are lipophilic, sequestered in adipose tissue
and secreted in milk, and others may only be present for short
periods of time but at critical periods of development. Our
knowledge about the magnitude of human or wildlife exposure
remains very limited. Most of the more definitive studies on
chemically mediated effects, including those on EDCs, have been
conducted on highly exposed groups in various occupations or from
accidental exposures. In only a few cases, appropriate exposure
information is available from lower level environmental exposures
because of analytical sensitivity and the latency in outcome after
exposure has occurred.
Hormonally active environmental chemicals are
extraordinarily diverse in their structure and potency. For example,
some organohalogens, such as the PCBs, DDT, PCDDs, and
PCDFs, are suspected endocrine-disrupting agents, but various
members of these groups of chemicals exhibit profound differences
in potency, biological and ecological persistence, and mechanisms
of action. For example, 75 PCDD congeners and 135 PCDF
congeners vary tremendously in their potency to exhibit TCDD-
like activity (see Chapter 6). This kind of diversity creates obvious
problems in human and ecological health assessments, and it also
increases the complexity and costs of analyzing for concentrations
of these chemicals in biological samples. In addition to the PCBs,
PCDDs, and PCDFs, many other kinds of chemical modulators of
endocrine function are examined in this report. These include
phthalate acid esters, DDT and DDE, alkylphenols,
methoxychlor, bisphenol, diethylstilbestrol, estradiol as an
ecological contaminant, the fungicide vinclozolin, and several
other synthetic chemicals that are reported to interact with various
components of the endocrine system.
Synthetic chemicals are not the only exogenous agents that
have caused health concerns because of their hormonelike activity.
Of particular interest are the phytoestrogens (such as genistein and
equol) and the fungal estrogens (such as zearalenone). The
phytoestrogens and fungal estrogens are diverse in structure,
undergo complex metabolic processes, and are ubiquitous in the
environment. They can be found in blood and urine samples of
virtually every person and animal on this planet, often in high
concentrations. They pose difficult analytical issues, yet if
exposure–response relationships for the phytoestrogens remain
uncertain, health assessments for many endocrine-disrupting
agents, particularly the environmental estrogens, will also remain
uncertain. This is because several of the phytoestrogens, mostly
notably genistein and its analogs, possess binding affinities for the
ER far greater than many of the EDCs of concern, such as the
alkylphenols, bisphenol A, and DDE. From a potency standpoint,
the phytoestrogens exert a far greater impact on human exposure to
exogenous estrogens than do the synthetic chemicals. This does not
mean that we should not be concerned about synthetic estrogens,
but it does emphasize that exposure assessments for EDCs need to
consider both the magnitude of exposure and relative potencies of
the array of EDCs that may be encountered in the home,
workplace, and general environment.
Information is needed to more accurately quantify the human,
wildlife, and environmental burden of hormonally active
environmental chemicals so that quantitative comparisons can be
made between body levels of natural and exogenous hormones
based on potency, not just absolute amount. This kind of
information is essential if we ever hope to properly evaluate

exposure–response relationships in field and epidemiology studies
and to use those relationships to produce credible risk assessments.
Data on historical and geographic trends of exposure to EDCs are
generally lacking. Knowledge of the fate and transport of new and
existing chemicals is also limited, particularly among the different
environmental compartments (water, sediment, and biota).
Exposure assessment, particularly as it involves human health,
must focus on vulnerable groups, in terms of both life stage and
lifestyle. Exposure assessment for the critical development stages
remains a high research priority. These stages include gestation,
lactation, adolescence, and senescence. The endocrine system,
through a developmentally regulated pattern of expression, controls
the pathways essential for cell proliferation, differentiation, and
organ development, so it is not surprising that perturbations of the
endocrine system during critical windows of sensitivity create the
greatest potential for adverse health effects.
Vulnerability of different groups in the population will be
affected by lifestyle factors (e.g., subsistence hunting and fishing,
and avid sportsmen who consume fish and wildlife), genetic factors
(e.g., metabolic differences that can determine sensitivity), special
dietary habits, and age (e.g., the types and rates of food
consumption in children). Although there is general agreement that
diet would likely be the major exposure route for exposure to the
EDCs, an approach based on integrated exposure assessment needs
to be taken. All routes should be examined (e.g., dermal, inhalation,
and ingestion). Examining the exposure of humans or wildlife to
multiple chemicals (especially for chemicals with a common mode
of action and/or common target sites) that may function as EDCs
is also critical.
Exposure assessment encompasses both external measurements
(levels in air, water, soil, food, etc.) and internal measurements
(levels in blood, urine, and tissue samples). Both kinds of
measurements provide critical information for wildlife,
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CHAPTER 2: INTRODUCTION/BACKGROUND
epidemiological, and experimental studies. Internal measurements
are often confounded by the rapid metabolism of some EDCs
(Elsby et al., 2001). This means that quantification of metabolites
or degradation products in biological samples is necessary for
endocrine disruptor research. Some of the rapidly metabolized
chemicals reviewed in this document are the phthalate acid esters,
alkylphenols, diethylstilbestrol, some PCBs, phytoestrogens, and
methoxychlor.
Other complications in exposure assessment include time lags,
seasonality, and multiple chemical exposures. a) Time lags between
exposure and effect: The transgenerational nature of some EDC
effects may be the single most complicating factor. All of the
potential latent effects that may occur from short-term exposures
during critical development windows have not yet been identified.
b) Seasonality: Because of the sensitivity of reproductive stages to
EDCs, seasonality will be extremely important to wildlife. In
addition, the association of EDCs with the aquatic environment is
complicated by seasonal rainfall, storm runoff, and water releases.
c) Multiple chemical exposures: This, too, is a factor for any toxic
chemical, but it is especially identified here because of the potential
for effect modification (e.g., synergy, additivity, or antagonism).
The most critical need on status and trends is for the
continuation and improvement of monitoring of the environment
for the presence and magnitude of contaminants. Although
environmental and tissue levels of certain EDCs (e.g., PCBs) have
declined in some countries in response to regulations, they remain
of concern in other countries, and uncertainty still exists regarding
future trends. For most EDCs, data on trends are not available.
Long-term data using harmonized collection and analysis methods
are needed. Existing programs that furnish repeated measures of
chemical contamination in the environment or in food provide our
only indication of whether exposure is increasing or decreasing, and
to what magnitude.