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Current
Drug Targets
ISSN: 1389-4501
Current Drug Targets
Volume 9, Number 6, June 2008
Contents
Animal Models of Asthma
Guest Editor: Armin Braun
Editorial Pp. 436-437
Animal Models for Human Asthma: The Perspective of
a Clinician
Pp. 438-442
N. Krug and K.F. Rabe
[Abstract] [Purchase
Article]
The Preclinical Testing Strategy for the Development
of Novel Chemical Entities for the Treatment of Asthma Pp.
443-451
C. Hahn and K.J. Erb
[Abstract] [Purchase
Article]
The Guinea Pig as an Animal Model for Asthma Pp.
452-465
F.L.M. Ricciardolo, F. Nijkamp, V. De Rose and
G. Folkerts
[Abstract] [Purchase
Article]
Experimental Bronchial Asthma – The Strength
of the Species Ratb Pp. 466-469
T. Tschernig, D. Neumann, A. Pich, M. Dorsch
and R. Pabst
[Abstract] [Purchase
Article]
Use of Alternative Animals as Asthma Models
Pp. 470-484
N. Kirschvink and P. Reinhold
[Abstract] [Purchase
Article]
The "Classical" Ovalbumin Challenge
Model of Asthma in Mice Pp. 485-494
R.K. Kumar, C. Herbert and P.S. Foster
[Abstract] [Purchase
Article]
Improved Mouse Models of Allergy and Allergic
Asthma - Chances Beyond Ovalbumin Pp. 495-502
B. Fuchs and A. Braun
[Abstract] [Purchase
Article]
Transgenic Models in Allergic Responses
Pp. 503-510
M. Hausding, K. Sauer, J.H. Maxeiner and S. Finotto
[Abstract] [Purchase
Article]
Abstracts
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Editorial
Allergic bronchial asthma is a disease of high prevalence
in societies with western lifestyle. In recent years, substantial
progress has been made in understanding the underlying mechanisms,
and explanations have been developed why the disease prevalence
has increased dramatically over the past decades. The most
popular explanation is the so-called hygiene hypothesis, postulating
that decreased bacterial infection and microbiological contact
are responsible for an imbalanced immune response leading
to an allergic predisposition. However, the physiological
and immunological mechanisms in the lung leading to bronchial
asthma are still not fully understood. Therefore, animal models
of asthma have been established and improved to study the
complex cellular and physiological interactions in vivo.
It is the aim of this issue of CDT to give an overview
of the current status of different models of asthma. In a
first contribution, the clinicians Krug and Rabe describe
their demands on a valuable animal model from a clinical point
of view [1, this issue]. They state: "There is a marked
discrepancy between numerous successful studies in animals
and very few, rather disappointing clinical trials in patients.
The currently available models are usually uniform models
of an acute asthmatic attack in adult animals, which do not
spontaneously develop asthma." None of the animal models
described so far is able to represent all features of the
disease.
In spite of these difficulties, pharmaceutical companies are
interested in using predictive disease models to be able to
develop new drugs for asthma treatment. Hahn and Erb [2, this
issue] describe how companies deal with the complex drug discovery
and development process. They state: "A particularly
challenging aspect of developing novel chemical entities for
the treatment of asthma is choosing and setting up in
vivo models believed to be predictive of human disease,"
and add: "An optimal animal disease model should accurately
reproduce the clinical human disease pathology." Since
no single model at present completely fulfils this requirement,
researchers have to choose models which reproduce the relevant
aspects of the disease for a given specific compound or question
they want to test.
An approximated asthma phenotype can only be seen in larger
animals, e.g. monkeys, dogs, cats, rats, or guinea pigs. Until
the eighties, most of the pre-clinical research was performed
using these physiologically relevant models showing a clear
asthma phenotype [3]. Fabio et al. [4, this issue]
explain that the guinea pig is one of the oldest and best
models of asthma: "The guinea pig is the preferred choice
for use as a model of allergic bronchial asthma in the evaluation
of anti-asthmatic drugs, since the airway anatomy and the
response to inflammatory mediators is similar to humans. Further,
the great strength of this model is the direct anaphylactic
bronchoconstriction upon antigen challenge. Under certain
conditions a late asthmatic response can be measured, and
airway hyperresponsiveness is observed in vitro and
in vivo." However, the major shortcoming of this
model is that "guinea pigs are limited in terms of mechanistic
studies, particularly those involving genetics, due to the
low number of inbred strains and lack of guinea pig-specific
reagents available".
The rat is another classical asthma model. Rats are used preferentially
for the investigation of pharmacological and toxicological
aspects of therapeutics for the disease [3]. Tschernig et
al. [5, this issue] state: "The rat offers advantages
in comparison to other species: the anatomical feature of
the proprietary bronchial circulation, genetics and proteomics,
lung function, and finally economical considerations."
According to our experience, the choice of the appropriate
strain is critical. The widely used Brown Norway rat has significant
and variable problems with endogenous granulomatous pneumonia
[6]. Therefore, new models using e.g. Fischer rats have been
developed [7]. Compared to guinea pig more reagents are available
for the rat, but compared to mice the number of reagents especially
for immunological targets is still very limited.
Other, non-laboratory animal models involve similar problems
regarding the availability of reagents and scientific tools.
However, the article by Kirschvink and Reinhold [8, this issue]
describes the advantages of such models: "Large animal
species, however, present unique physiological and natural
preconditions as well as experimental advantages that are
of great value to develop alternative models of allergic and
non-allergic chronic airway diseases. Despite the known disadvantages
of being expensive and time consuming, large animal models
are worth to be considered for their possible role as ‘functional
models’. They offer the potential to perform long-term
studies allowing a simultaneous within-subject approach of
functional, inflammatory and morphological changes, and taking
the influence of co-factors into account." Despite these
advantages, they are not used widely at the moment.
Interestingly, the use of animal models completely changed
in the nineteen-nineties [3]. Asthma was newly defined as
an immunological disease, and models had to reflect immunological
features much more than the physiological outcome of asthma.
Due to the scientific revolution in molecular biology, leading
to a wide range of transgenic and knock-out animals and the
generation of specific tools such as monoclonal antibodies
and RNA probes, the mouse became the most frequently used
species for asthma research.
Although mice do not develop a perfect asthma phenotype with
chronic allergic inflammation and spontaneous airflow limitations,
the mouse reflects very well the immunological events believed
to lead to symptoms of asthma. The Th-2-dependent allergic
inflammation with eosinophilic influx into the lung and resulting
airway hyperresponsiveness can me mimicked very easily in
mouse models. In addition, parts of the remodelling processes
observed in asthma are also present in mouse models. This
improved knowledge about the mechanisms of asthma pathogenesis
generated from mouse models has led to a rapid identification
of novel pharmaceutical targets for treatment of the disease.
Progress in the past 10 years has demonstrated that the mouse
is indeed a suitable model for some aspects of the disease.
The current "chronic" asthma models using repetitive
allergen aerosol provocation mimic important features of human
disease. They show an allergen-dependent sensitisation with
IgE production, a Th-2-dependent allergic inflammation characterised
by eosinophilic influx into the airway mucosa, airway remodelling,
airway hyperreactivity, and allergen-specific early phase
response. However, other features of asthma such as allergen-independent
chronification or acute "asthma attacks" have not
been observed in mice. To date, models using ovalbumin as
a model allergen are most popular. Therefore, the article
by Kumar et al. [9, this issue] can conclude: "Models
of asthma based on ovalbumin challenge in mice have limitations,
which need to be recognised when attempting to interpret experimental
findings. Nevertheless, careful use of well-defined models
to answer specific questions can contribute to the understanding
of pathogenesis, as well as identifying and investigating
potential therapeutic targets in asthma."
During recent years, mouse models have been further developed,
using more human-relevant allergens, adjuvant-free protocols,
and clinically relevant routes of sensitisation, e.g. airway
sensitisation. This recent progress has been described in
our contribution [10, this issue]. The possibility to use
and generate transgenic animals is a further important step
forward. The contribution by Hausding et al. [11,
this issue] explains the advantages of using transgenic animals
to understand the pathophysiological mechanisms leading to
asthma. Special emphasis was given to the role of transcription
factors.
In conclusion, animal models of asthma are not perfect representations
of the human disease. Nevertheless, they are able to mimic
certain aspects of the disease. For the best choice of a model,
the advantages of this particular model for the specific question
must be taken into consideration. For pharmacological questions,
guinea pig and rat might be optimal models. For immunological
problems, the different mouse strains and protocols including
transgenic animals might be the right choice, whereas remodelling
in chronic studies might best be performed in large animals.
This work was supported by the German Research Foundation
(SFB 587, B4, Z2).
References
[1] Krug, N., Rabe, K. F. (2008). This issue.
[2] Hahn, C., Erb, J. K. (2008). This issue.
[3] Börger, J. A., Neye, N., Scutaru, C., Kreiter, C.,
Puk, C., Fischer, T. C., Groneberg-Kloft, B. (2008) J.
Occup. Med. Tox., 3(Suppl 1), S7.
[4] Ricciardolo, F. L. M., Nijkamp, F.M., De Rose, V., Folkerts,
G. (2008). This issue.
[5] Tschernig,T., Neumann, D., Pich, A., Dorsch, M., Pabst,
R. (2008). This issue.
[6] Germann, P. G., Häfner, D., Hanauer, G. and Drommer,
W. (1998) J. Exp. Animal. Sci., 39,
22-33
[7] Skripuletz, T., Schmiedl, A., Schade, J., Bedoui, S.,
Glaab, T., Pabst, R., von Hörsten, S., Stephan, M. (2007)
Am. J. Physiol. Lung Cell. Mol. Physiol., 292,
L1564-71.
[8] Kirschvink, N., Reinhold, P. (2008). This issue.
[9] Kumar, R. K., Herbert, C., Foster, P. S. (2008). This
issue.
[10] Fuchs, B., Braun, A. (2008). This issue.
[11] Hausding, M., Sauer, K., Mayxeiner, J. H., Finotto, S.
(2008). This issue.
Armin Braun
Immunology, Allergology and Immunotoxicology
Fraunhofer Institute of Toxicology and Experimental Medicine
Nikolai-Fuchs-Str. 1
30625 Hannover, Germany
Phone: +49 511 5350-263
Fax: +49 511 5350-155
E-mail: armin.braun@item.fraunhofer.de
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Article]
Animal Models for Human Asthma: The Perspective of
a Clinician N. Krug and K.F. Rabe
The asthma animal model is still the only system that
is available for modelling in vivo processes of human
disease since for obvious ethical reasons these experiments
are not possible in humans. However, there is a marked discrepancy
between numerous successful studies in animals and very few
rather disappointing clinical trials in patients. The current
available models are usually uniform models of an acute asthmatic
attack in adult animals, which do not spontaneously develop
asthma. Major anatomical differences exist between human and
animal airways and comparable lung function measurements are
very difficult or impossible. The main reason why simplistic
animal models may be inadequate lies probably in the diversity
that exists within the different phenotypes of human asthma.
Whereas progress is made to develop chronic asthma models
with signs of airway remodelling, severe asthma and the role
of small airways is still poorly reflected in current animal
models.
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The Preclinical Testing Strategy for the Development
of Novel Chemical Entities for the Treatment of Asthma
C. Hahn and K.J. Erb
Identifying and developing novel chemical entities (NCE)
for the treatment of asthma is a time-consuming process and
liabilities that endanger the successful progression of a
compound from research into the patient are found throughout
all phases of drug discovery. In particular the failure of
advanced compounds in clinical studies due to lack of efficacy
and/or safety concerns is tremendously costly. Therefore,
in order to try and reduce the failure rate in clinical trials
various in vitro and in vivo tests are performed
during preclinical development, to rapidly identify liabilities,
eliminate high risk compounds and promote promising potential
drug candidates. To achieve this objective, numerous prerequisites
have to be met regarding the physico-chemical properties of
the compound, and bioactivity or model systems are needed
to rate the therapeutic potential of new compounds. Drug liabilities
such as target and species specificity, formulation issues,
pharmacokinetics as well as pharmacodynamics and the toxic
potential of the compound have to be analyzed in great detail
before a compound can enter a clinical trial. A particularly
challenging aspect of developing novel NCEs for the treatment
of asthma is choosing and setting up in vivo models
believed to be predictive for human disease. Numerous companies
have in the past and are currently developing NCEs targeting
many different pathways and cells with the aim to treat asthma.
However, currently the only NCE having a significant market
share are long-acting β-agonists
(LABA), inhaled and orally active steroids and leukotriene
receptor antagonists. In the past many novel NCE for the treatment
of asthma were effective in animal models but failed in the
clinic. In this review we outline the prerequisites of novel
NCE needed for clinical development.
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The Guinea Pig as an Animal Model for Asthma
F.L.M. Ricciardolo, F. Nijkamp, V. De Rose and
G. Folkerts
Experimental guinea pig asthma is a reliable and clinically
relevant facsimile of human disease. The guinea pig is the
preferred choice for use as a model of allergic bronchial
asthma in the evaluation of anti-asthmatic drugs, since the
airway anatomy and the response to inflammatory mediators
is similar to humans. Further, the great strength of this
model is the direct anaphylactic bronchoconstriction upon
antigen challenge. Under certain conditions a late asthmatic
response can be measured and airway hyperresponsiveness is
observed in vitro and in vivo. Moreover,
the inflammatory response is comparable with the human situation.
More recent studies describe a chronic model for asthma in
which airway remodeling is induced as can be observed in the
asthmatic patients. The focus here is to demonstrate that
guinea pig asthma models are useful for testing novel therapeutics.
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Experimental Bronchial Asthma – The Strength
of the Species Rat
T. Tschernig, D. Neumann, A. Pich, M. Dorsch
and R. Pabst
No single animal species reflects the complete range
of human respiratory anatomy, physiology and - often not mentioned
- age-related changes. The rat was the first experimental
asthma model, but was overtaken in numbers by murine models
many years ago. Data will be compiled to document that the
rat model still has an important role in the research of bronchial
asthma and other lung diseases. In pharmaceutical research
for new drugs the rat model is still indispensable. Here specific
aspects will be highlighted where the rat offers advantages
in comparison to other species: the anatomical feature of
the proprietary bronchial circulation, genetics and proteomics,
lung function and finally economical considerations.
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Use of Alternative Animals as Asthma Models
N. Kirschvink and P. Reinhold
This review focuses on the availability, advantages and
non-advantages of asthma models in non-laboratory animals
(cats, dogs, sheep, swine, cattle, horses, and monkey). Physiology
and pathophysiology of the respiratory system as well as methodological
aspects differ significantly between species and must be taken
into account before evaluating the usefulness of a single
species to serve as model for either asthma or chronic airway
obstruction. Allergic asthma models have been described in
cats, dogs, pigs, sheep, and monkeys. Among these species,
the feline one is of particular interest because cats spontaneously
develop idiopathic asthma. Currently available allergic feline
models are well characterized with respect to lung function,
bronchial responsiveness, airway inflammation and lung morphology
(remodeling). Other species lacking for collateral airways
(i.e. porcine and bovine lungs) are most sensitive to functional
consequences of airway obstruction and are therefore suitable
to study any obstructive lung disease. Animals of body weights
comparable to humans (pigs, sheep, calves) offer the possibility
to evaluate pulmonary functions using the same principles
and techniques that are applicable to either children or adults
during spontaneous breathing (generating lung function data
in a directly comparable range). Despite the known disadvantages
of being expensive and time consuming and despite limited
availability of immunological or molecular tools, large animal
models offer the great potential to perform long-term functional
studies allowing a simultaneous within-subject approach of
functional, inflammatory and morphological changes. This may
add valuable information to the present knowledge about the
complexity of asthma or other chronic airway diseases.
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The "Classical" Ovalbumin Challenge
Model of Asthma in Mice
R.K. Kumar, C. Herbert and P.S. Foster
Ovalbumin challenge models of asthma offer many opportunities
for increasing our understanding of the pathogenetic mechanisms
underlying this disease, as well as for identifying novel
therapeutic targets. There is no single "classical"
model, because numerous alternatives exist with respect to
the choice of mouse strain, method of sensitisation, route
and duration of challenge, and approach to assessing the host
response. Moreover, the limitations of these models need to
be recognised when attempting to interpret experimental findings.
Nevertheless, careful use of well-defined models allows investigators
to answer specific questions that are otherwise difficult
to address.
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Improved Mouse Models of Allergy and Allergic
Asthma - Chances Beyond Ovalbumin
B. Fuchs and A. Braun
Allergic asthma is defined as a hypersensitivity reaction
of the lung towards per se harmless antigens, e.g.
pollen and house dust mite, accompanied with a chronic eosinophilic
inflammation of the lung. During the course of the disease,
physiological and structural changes in the lung occur, i.e.
airway hyperresponsiveness, restricted airflow and airway
remodelling. In addition to ovalbumin-induced mouse models
of acute asthma, recently new models were developed, which
show a closer resemblance to human asthma, both regarding
the induction of characteristics of chronic allergic inflammation
and the use of clinical relevant allergens. Moreover, attention
is paid on the influence of adjuvants or the route of sensitisation
on the protocol outcomes. The effort spent in development
of these new models will be worthwhile, especially for research
in the field of immuno-therapy. These improved animal models
may broaden the knowledge of the disease and thereby provide
new strategies for preventive and therapeutic interventions.
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Transgenic Models in Allergic Responses
M. Hausding, K. Sauer, J.H. Maxeiner and S. Finotto
The immunoresponses are mediated by cells presenting
the antigen to T cells. The transcription factors involved
in the differentiation of T helper cells enclose T-bet (Th1),
c-maf (Th2), GATA-3 (Th2), Foxp3 (T reg) and RORγT
(Th17). They are regulated in allergic asthma. The use of
murine models either as germline or as tissue specific transgenic
mice has given decisive immunological tools to understand
the importance of selected transcription factors or cytokines.
Tissue specific transgenic lines have been generated into
the Clara Cell or CD2 promoter directing tissue- and immune
cells specific expression of the gene of interest. We identified
T cell transcription factors important for asthma –
such as T-bet, c-maf, GATA-3. Transgenic and knockout
murine models of these transcription factors provided very
important information for the human disease. Regarding to
the pathogenesis of chronic asthma, we generated transgenic
lines overexpressing IL-18 and analyzed a dominant negative
mutant of the TGF-β
receptor II. These models will offer to us a great
input for the understanding of the T cell memory and the processes
like airway remodelling. Beside DNA microinjection and stem
cell transfer the On/Off systems like Cre-lox models have
helped to understand the role of selected genes in different
steps of experimental disease. Moreover, the transgenic model
provide reliable models for the preclinical approval of therapy
for allergic asthma to develop more efficient compounds and
functional antibodies.
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