Current
Topics in Medicinal Chemistry
ISSN: 1568-0266
Current Topics
in Medicinal Chemistry
Volume 8, Number 3, 2008
Contents
The Medicinal Chemistry of Agents Targeting
the Endogenous Cannabinoid System
Guest Editor: Outi M. H. Salo-Ahen
Editorial Pp. 172
CB Receptor Ligands from Plants
Pp. 173-186
Karin Wölkart, Outi M. H. Salo-Ahen and Rudolf Bauer
[Abstract]
Recent Advances in the Development of Selective Ligands
for the Cannabinoid CB2
Receptor Pp. 187-204
Karla-Sue C. Marriott and John W. Huffman
[Abstract]
CB1
Cannabinoid Antagonists: Structure-Activity Relationships
and Potential Therapeutic Applications Pp. 205-330
Nadine Jagerovic, Cristina Fernandez-Fernandez and Pilar
Goya
[Abstract]
The Medicinal Chemistry of Agents Targeting Monoacylglycerol
Lipase Pp. 231-246
Alma Viso, José A. Cisneros and Silvia Ortega-Gutiérrez
[Abstract]
Overview of the Chemical Families of Fatty Acid Amide
Hydrolase and Monoacylglycerol Lipase Inhibitors
Pp. 247-267
Séverine Vandevoorde
[Abstract]
Molecule of Month Pp. 268
Abstracts
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Editorial
The utilization of the hemp plant, Cannabis sativa
L. has a millenia long history. The therapeutic potential
of the plant was recognized early and most parts of the plant
have been exploited, for example, in medicine or in various
religious rituals. The major psychoactive substance of cannabis,
Δ9-tetrahydrocannabinol
(THC), was isolated only in the 1960s. THC and other structurally
similar compounds characterized from this plant were all named
cannabinoids. Over the years, numerous cannabinoid analogues
have been synthesized in the hope of developing potential
drugs for therapeutic use. Unfortunately, the unwanted psychotropic
effects of the cannabimimetic molecules have limited their
medical application. However in the 1990s, the discovery of
the endogenous cannabinoid system revolutionized the cannabinoid
research field. This complex lipid signaling system in humans
includes specific cannabinoid receptors (at least CB1 and
CB2), their endogenous ligands (endocannabinoids) and the
enzymes responsible for synthesizing or degrading the endocannabinoids
(e.g. fatty acid amide hydrolase, FAAH, or monoacylglycerol
lipase, MAGL), and it provides an intriguing target for the
design and development of selective cannabinoid drugs. The
current journal issue focuses on the chemical agents that
have been discovered or developed to target the endogenous
cannabinoid system.
The review by Wölkart et al. introduces us to the world
of phytocannabinoids. Phytocannabinoids from Cannabis
sativa L. are the best known cannabinoid compounds and
have contributed greatly to the discovery of the endogenous
cannabinoid system and understanding its functions. However,
cannabinoid-type compounds have also been found in Echinacea
species and liverwort, as well as in Helichrysum umbraculigerum.
The authors present the phytocannabinoids as useful templates
for drug design and especially discuss current studies of
their effects on the immune system.
Unlike the central CB1 receptors, CB2 receptors are mainly
located in the immune system. Therefore, selective CB2 receptor
ligands are potential immunotherapeutic agents and they do
not cause the unwanted psychotrophic effects related to the
CB1 agonism of the non-selective cannabinoids. Marriott and
Huffman give a comprehensive review of selective CB2 ligands
developed to date. Especially the structure-activity relationships
of traditional cannabinoid and indole analogues have been
studied extensively.
Another way of avoiding the unwanted psychotrophic effects
is to block the CB1 receptors. Jagerovic et al. review the
structure-activity relationships of CB1 selective antagonists/inverse
agonists, which are potential therapeutic agents for the treatment
of obesity and nicotine addiction. In addition to the extensively
studied analogues of rimonabant (Acomplia®),
there are also some other structural scaffolds that have been
shown to have antagonistic/inverse agonistic effects at CB1.
Fine-tuning of the levels of the endocannabinoids is yet another
intelligent approach to overcome the problems associated with
direct CB1 activation. Viso and co-authors present the current
knowledge on MAGL, the enzyme hydrolyzing 2-arachidonoylglycerol,
the endocannabinoid. They focus especially on the enzyme structure
and catalytic mechanism, as well as on the therapeutic potential
of MAGL inhibitors. Séverine Vandevoorde compares different
structural families of FAAH and MAGL inhibitors. In addition
to the chemical features, modes of inhibition, potencies and
FAAH/MAGL selectivities of the inhibitors, their synthetic
pathways are also presented.
Outi M. H. Salo-Ahen
EML Research gGmbH
Schloss-Wolfsbrunnenweg 33
D-69118 Heidelberg,
Germany
E-mail: outi.salo-ahen@eml-r.villa-bosch.de
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CB Receptor Ligands from Plants
Karin Wölkart, Outi M. H. Salo-Ahen and Rudolf Bauer
Advances in understanding the physiology and pharmacology
of the endogenous cannabinoid system have potentiated the
interest of cannabinoid receptors as potential therapeutic
targets. Cannabinoids have been shown to modulate a variety
of immune cell functions and have therapeutic implications
on central nervous system (CNS) inflammation, chronic inflammatory
conditions such as arthritis, and may be therapeutically useful
in treating autoimmune conditions such as multiple sclerosis.
Many of these drug effects occur through cannabinoid receptor
signalling mechanisms and the modulation of cytokines and
other gene products. Further, endocannabinoids have been found
to have many physiological and patho-physiological functions,
including mood alteration and analgesia, control of energy
balance, gut motility, motor and co-ordination activities,
as well as alleviation of neurological, psychiatric and eating
disorders. Plants offer a wide range of chemical diversity
and have been a growing domain in the search for effective
cannabinoid ligands. Cannabis sativa L. with the
known plant cannabinoid, Δ9-tetrahydrocannabinol
(THC) and Echinacea species with the cannabinoid
(CB) receptor-binding lipophilic alkamides are the best known
herbal cannabimimetics. This review focuses on the state of
the art in CB ligands from plants, as well their possible
therapeutic and immunomodulatory effects.
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Recent Advances in the Development of Selective Ligands for
the Cannabinoid CB2 Receptor
Karla-Sue C. Marriott and John W. Huffman
Two subtypes of the mammalian cannabinoid receptor have
been identified and successfully cloned since 1990. The CB1
receptor is primarily located in the central nervous system
and the CB2 receptor is almost
exclusively expressed in cells of the immune system. The CB1
and CB2 receptors are both
G-protein coupled receptors and are involved in the inhibition
of adenylate cyclase. The CB2
receptor is of particular importance due to its involvement
in signal transduction in the immune system, making it a potential
target for therapeutic immune intervention. A number of these
selective ligands are derivatives of traditional dibenzopyran
based cannabinoids. These include the very recently synthesized
(2’R)-1-methoxy-3-(2’-methylbutyl)-Δ8-THC
(JWH-359) which has a 224 fold selectivity for the CB2
receptor, readily comparable to the well known 1-deoxy-3-(1’,1’-dimethylbutyl)-Δ8-THC
(JWH-133) which has 200 fold selectivity for the CB2
receptor. Several 9-hydroxyhexahydrocannabinols have also
been synthesized and are found to be selective high affinity
ligands for the CB2 receptor.These
are 1-deoxy-9β-hydroxy-dimethylhexylhexahydrocannabinol
(JWH-361, Ki = 2.7 nM) and 1-deoxy-9β-hydroxy-dimethylpentylhexahydrocannabinol
(JWH-300, Ki = 5.3 nM). CB2
selective cannabi-mimetic indoles include 1-(2,3-dichlorobenzoyl)-2-methyl-3-(2-[1-morpholine]ethyl)-5
methoxyindole (L768242), (R)-3-(2-Iodo-5-nitrobenzoyl)-1-(1
methyl-2-piperidinylmethyl)-1H-indole (AM1241) and 1-propyl-2
methyl-3-(1-naphthoyl) indole (JWH-015), which exhibit significant
selectivity for the CB2 receptor
coupled with weak affinity for the CB1receptor.
Bristol-Meyer Squibb has produced a phenylalanine derived
cannabimimetic indole which possesses high CB2
affinity (Ki = 8 nM) and
very low affinity for the CB1
receptor (Ki = 4000 nM).
This review will discuss the current advances and recent results
in the structure-activity relationships (SAR) of selective
ligands for the cannabinoid CB2
receptor.
[Back to top]
CB1 Cannabinoid Antagonists:
Structure-Activity Relationships and Potential Therapeutic
Applications
Nadine Jagerovic, Cristina Fernandez-Fernandez and Pilar
Goya
During the last decade there has been a growing interest
towards the modulation of the cannabinoid CB1
receptor. The identification of CB1
cannabinoid receptor antagonists has been one of the major
advances in cannabinoid research. Thus, the development of
these ligands has opened new therapeutic applications. Since
the discovery of the first cannabinoid receptor antagonist,
rimonabant, by Sanofi in 1994, a large number of structural
variations within this chemical series of 1,5-diarylpyrazoles
have been described. So far, all attempts to identify novel
structures for CB1 antagonists
have been based on one or more pharmacophoric elements of
the rimonabant structure. The advanced clinical trials of
rimonabant confirm the therapeutic potential value of CB1
antagonists for the treatment of obesity. In addition, the
results of pharmacological and clinical studies reveal other
effective pharmacotherapeutic applications. The current review
will mainly focus on the structure-activity relationships
that have been established for antagonists/inverse agonists
that bind to the CB1 cannabinoid
receptors and on their therapeutic applications.
[Back to top]
The Medicinal Chemistry of Agents Targeting Monoacylglycerol
Lipase
Alma Viso, José A. Cisneros and Silvia Ortega-Gutiérrez
Monoacylglycerol lipase (MAGL) has been recently proposed
as the main enzymatic activity responsible for the in
vivo hydrolysis of the most abundant endocannabinoid
in the brain, the 2-arachidonoylglycerol (2-AG). The endocannabinoids,
mainly anandamide (AEA) and 2-AG, are a class of lipid messengers
that modulate a broad number of physiological processes both
in the central nervous system and in the periphery. To date,
AEA has been by far the most studied endocannabinoid, although
increasing evidence is pointing out the prominent, and sometimes
underestimated, role of 2-AG in the regulation of different
functions. Therefore, it is of outmost importance to dissect
the specific cellular pathways in which these two endocannabinoids
are involved. Nonetheless, little is known about the structural
requirements of MAGL. Here we review the current knowledge
on MAGL, with special focus on its structure and catalytic
mechanism as the rational basis for the design of potent and
selective compounds able to interact with it; the inhibitors
that have been described to date, and the therapeutic applications
that make MAGL an attractive therapeutic target.
[Back to top]
Overview of the Chemical Families of Fatty Acid Amide Hydrolase
and Monoacylglycerol Lipase Inhibitors
Séverine Vandevoorde
The family of the endogenous agonists of the cannabinoid
receptors – i.e., the endocannabinoids - includes several
polyunsaturated fatty acid amides and esters. Arachidonoylethanolamide
(anandamide, AEA) and 2-arachidon-oylglycerol (2-AG) are,
respectively, the leads of these chemical families. So far,
two enzymes responsible for the metabolism of AEA and 2-AG
have been described: Fatty Acid Amide Hydrolase (FAAH) which
hydrolyzes AEA and in some cells 2-AG, and Monoacylglycerol
Lipase (MAGL) which hydrolyzes 2-AG. In spite of the early
characterisation of MAGL and the nearly simultaneous clonings
of the two enzymes, most of the efforts were dedicated to
the study of FAAH and consequentially, the range of FAAH inhibitors
available nowadays exceeds the number of compounds active
upon MAGL. FAAH inhibitors can be divided in two major groups,
the first one includes the inhibitors inspired by the chemical
structures of FAAH substrates, which carry an arachidonoyl-,
oleoyl- or palmitoyl-carbon chain that mimic the fatty acid
chains of anandamide, oleamide and palmitoylethanolamide.
The second group involves compounds that do not share similarities
with the endocannabinoids, such as the carbamates, oxazolopyridins,
2-thioxoimidazolidin-4-ones, imidazolidine-2,4-diones and
the non-steroidal anti-inflammatory drugs. However, the family
of MAGL inhibitors contains few members and most of them exhibit
a lack of selectivity.
The purpose of this review is to give an overview of the families
of synthetic inhibitors of FAAH and MAGL. The synthetic pathways,
the chemical features, potencies, selectivities and modes
of inhibition are listed and discussed in order to facilitate
their comparison.
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