Current
Topics in Medicinal Chemistry
ISSN: 1568-0266
Current Topics
in Medicinal Chemistry
Volume 6, Number 17, 2006
Contents
Neurotransmitter Transporters
Guest Editor: Dr. Anders A. Jensen
Editorial Pp. 1799-1800
Serotonin Reuptake Inhibitors: The Corner
Stone in Treatment of Depression for Half a Century –
A Medicinal Chemistry Survey Pp. 1801-1823
Ejner K. Moltzen and Benny Bang-Andersen
[Abstract]
Dopamine Transporter Ligands: Recent Developments
and Therapeutic Potential Pp. 1825-1843
Scott P. Runyon and F. Ivy Carroll
[Abstract]
Therapeutic Potential of Monoamine Transporter
Substrates Pp. 1845-1859
Richard B. Rothman and Michael H. Baumann
[Abstract]
Structure-Activity Relationships of Selective
GABA Uptake Inhibitors Pp. 1861-1882
Signe Høg, Jeremy R. Greenwood, Karsten B. Madsen,
Orla M. Larsson, Bente Frølund, Arne Schousboe, Povl
Krogsgaard Larsen and Rasmus P. Clausen
[Abstract]
Progress in the Preparation and Testing of Glycine
Transporter Type-1 (GlyT1) Inhibitors Pp. 1883-1896
Craig W. Lindsley, Scott E. Wolkenberg and Gene G. Kinney
[Abstract]
Ligands Targeting the Excitatory Amino Acid Transporters
(EAATs) Pp. 1897-1906
John Dunlop and John A. Butera
[Abstract]
Abstracts
[Back to top]
Editorial
Neurotransmitter transporters can be
divided into two types: the vesicular transporters mediating
the uptake and storage of neurotransmitters in vesicles in
the presynaptic terminal and two families of membrane-bound
transporters responsible for the transport of neurotransmitters
from the synaptic cleft back into the presynaptic terminal
or glia cells. One of these families, the Na+/Cl--dependent
transporters, contains transporters mediating the synaptic
reuptake of the monoamines norepinephrine, dopamine and serotonin
and the major inhibitory neurotransmitters γ-aminobutyric
acid (GABA) and glycine, and other transporters in this family
have creatine, taurine and proline as their substrates. The
other transporter family consists of five Na
+-dependent excitatory amino acid transporters
responsible for the synaptic reuptake of glutamate, the major
excitatory neurotransmitter in the mammalian CNS.
Being essential regulators of the synaptic activity in these
important neurotransmitter systems, the membrane-bound neurotransmitter
transporters constitute highly interesting targets for pharmacological
intervention in a wide range of psychiatric and neurological
disorders. Drugs targeting transporters are already being
administered in the clinic for depression, attention-deficit
hyperactivity disorder (ADHD), obesity and epilepsy and as
smoking cessation aids. The present issue of Current Topics
in Medicinal Chemistry is focused on medicinal chemistry
and pharmacology aspects of ligands targeting membrane-bound
neurotransmitter transporters and the possibilities and challenges
in connection with the development of novel drugs acting at
these transporters or the improvement of already existing
ones.
The serotonin transporter (SERT) is the key molecular target
in the treatment of depression and is thus by far the most
successful drug target amongst the neurotransmitter transporters.
Selective serotonin reuptake inhibitors (SSRIs) hold significant
advantages to older classes of antidepressants, in particular
when it comes to their relatively mild side effects. However,
the obvious clinical benefits of SSRIs are hampered by their
characteristic slow onset of action and the fact that a considerable
fraction of depression patients are non-responders to SSRI
therapy. In the first review of this issue Moltzen and Bang-Andersen
outline the add-on and augmentation strategies currently being
pursued in the industry to address these problems through
the development of compounds combining SERT inhibition with
activities at other monoamine transporters or at various different
neurotransmitter receptors [1].
The dopamine transporter (DAT) is a potentially interesting
target for a wide range of neurodegenerative and psychiatric
disorders, and furthermore it is the key mediator of the psychostimulant
effects of recreational drugs such as amphetamine and cocaine.
Runyon and Carroll summarize the findings in recent structure-activity
studies of 3-phenyltropane, 1,4-dialkylpiperazine, phenylpiperidine
and benztropine analogs as well as other classes of DAT ligands
[2]. Furthermore, the authors outline the results from studies
of DAT inhibitors in non-human primate models of psychostimulant
abuse, Parkinson’s Disease and ADHD.
In their review of monoamine transporter substrates Rothman
and Baumann elucidate how the basic inhibitor/substrate properties
and the NET/DAT/SERT selectivity profile of the psychostimulant
drug determine its pharmacological effects, including its
therapeutic potential and its abuse liability [3]. Since equipotent
DAT/SERT substrates do not appear to induce the cardiovascular
side-effects caused by ‘clean’ serotonin releasers
or the psychostimulant side-effects and abuse liabilities
characteristic for ‘clean’ dopamine releasers,
the authors propose these ligands as candidate drugs for the
treatment of cocaine abuse.
The GABA and glycine transporters have not attracted nearly
as much medicinal chemistry attention as the monoamine transporters.
In their review of the GABA transporter (GAT) field, Clausen
and colleagues present the structure-activity relationships
for different series of conformationally restricted GAT ligands
and propose a pharmacophore model for the GAT1 subtype [4].
Several selective GAT1 inhibitors have been published, whereas
no truly selective pharmacological tools have been identified
for the other three GAT subtypes. Considering the clinical
administration of the GAT1-inhibitor tiagabine in epilepsy
and the well-established therapeutic potential in augmentation
of GABAergic neurosignalling in other disorders like anxiety,
convulsive states, pain and sleeping disorders these three
subtypes could be interesting as drug targets as well.
In addition to having glycine, the co-agonist of the NMDA
receptors, as its substrate, the glycine transporter subtype
1 (GlyT1) is co-localized with these receptors in several
CNS regions. In keeping with the ’glutamate/NMDA dysfunction’
hypothesis of schizophrenia, inhibition of GlyT1 and the resulting
augmentation of NMDA receptor signaling have been proposed
as an alternate way to treat this disorder. Kinney and coworkers
present a selection of the sarcosine and non-sarcosine based
GlyT1 inhibitors published to date and outline the performances
of these ligands in in vivo models for schizophrenia
[5].
The major excitatory neurotransmitter glutamate plays key
roles in a wide range of processes in the CNS, and an exhaustive
numbers of ligands acting at ionotropic and metabotropic glutamate
receptors have been published over the years. In the last
review of this issue, Dunlop and Butera outline the relatively
limited medicinal chemistry work done in the field of excitatory
amino acid transporters (EAATs) [6]. While the therapeutic
potential in EAAT inhibitors may be limited, some β-lactam
antibiotics have recently been shown able to increase expression
levels of EAAT proteins and have displayed promising neuroprotective
effects in various in vitro and in vivo
models.
I would like to thank all the authors for their enthusiasm
and dedication in contributing to this CTMC issue, and the
insightful suggestions and constructive criticism of the reviewers
are also thankfully acknowledged. I hope this issue will be
an inspiring read for the scientist engaged in the neurotransmitter
transporter area and that it also will serve as an introduction
to this exciting field of research for the general reader.
REFERENCES
[1] Moltzen, E. K.; Bang-Andersen, B. Serotonin reuptake inhibitors:
The corner stone in treatment of depression for half a century
– A medicinal chemistry survey. Curr. Topics Med.
Chem. 2006, 6(17), 1801-1823.
[2] Runyon, S. P.; Carroll, F. I. Dopamine transporter ligands:
Recent developments and therapeutic potential. Curr. Topics
Med. Chem. 2006, 6(17), 1825-1843.
[3] Rothman, R. B.; Baumann, M. H. Therapeutic potential of
monoamine transporter substrates. Curr. Topics Med. Chem.
2006, 6(17), 1845-1859.
[4] Høg, S.; Greenwood, J. R.; Madsen, K. B.; Larsson,
O. M.; Frølund, B.; Schousboe, A.; Krogsgaard-Larsen,
P.; Clausen, R. P. Structure-activity relationships of selective
GABA uptake inhibitors. Curr. Topics Med. Chem. 2006,
6(17), 1861-1882.
[5] Lindsley, C. W.; Wolkenberg, S. E.; Kinney, G. G. Progress
in the preparation and testing of glycine transporter type-1
(GlyT1) inhibitors. Curr. Topics Med. Chem. 2006,
6(17), 1883-1896.
[6] Dunlop, J.; Butera, J. A. Ligands targeting the excitatory
amino acid transporters (EAATs). Curr. Topics Med. Chem.
2006, 6(17), 1897-1906.
Anders A. Jensen, Ph.D.
Department of Medicinal Chemistry
The Danish University of Pharmaceutical Sciences
Universitetsparken 2
DK-2100 Copenhagen Denmark
Email: aaj@dfuni.dk
[Back to top]
Serotonin Reuptake Inhibitors: The Corner
Stone in Treatment of Depression for Half a Century –
A Medicinal Chemistry Survey
Ejner K. Moltzen and Benny Bang-Andersen
Inhibition of serotonin (5-HT) reuptake has been
a central theme in the therapy of depression for half a century.
Through the years these therapies have improved, particularly
with regard to side effects, and today’s selective serotonin
reuptake inhibitors (SSRIs) constitute a reasonably effective
offer for the patients. However, there is still room for major
improvement and considering that almost 20% of the population
in the western world will experience a depressive period in
their lifetime, there is a large need for improved therapies.
A large spectrum of targets and strategies are currently being
pursued, but so far none of these new approaches have been
successful, mainly due to lack of a deeper understanding of
the disease biology.
Since inhibition of 5-HT reuptake ensures a certain degree
of antidepressant efficacy, there has been a large interest
in various combinations with serotonin reuptake inhibitors
(SRIs) in order to improve on the shortcomings of treatment
with SSRIs. Some of these approaches have resulted in marketed
antidepressants, eg combinations of SRI with norepinephrine
(NE) reuptake inhibition, whereas other approaches are still
at an experimental stage. This review attempts to present
the current status of these add-on/combination approaches
with particular focus on the medicinal chemistry aspects.
[Back to top]
Dopamine Transporter Ligands: Recent Developments
and Therapeutic Potential
Scott P. Runyon and F. Ivy Carroll
The dopamine transporter (DAT) is a target for the
development of pharmacotherapies for a number of central disorders
including Parkinson’s disease, Alzheimer’s disease,
schizophrenia, Tourette’s syndrome, Lesch-Nyhan disease,
attention deficit hyperactivity disorder (ADHD), obesity,
depression, and stimulant abuse as well as normal aging. Considerable
effort continues to be devoted to the development of new ligands
for the DAT. In this review, we present some of the more interesting
ligands developed during the last few years from the 3-phenytropane,
1,4-dialkylpiperazine, phenylpiperidine, and benztropine classes
of DAT uptake inhibitors as well as a few less studied miscellaneous
DAT uptake inhibitors. Studies related to the therapeutic
potential of some of the more studied compounds are presented.
A few of the compounds have been studied as pharmacotherapies
for Parkinson’s disease, ADHD, and obesity. However,
most of the drug discovery studies have been directed toward
pharmacotherapies for stimulant abuse (mainly cocaine). A
number of the compounds showed decreased cocaine maintained
responding in rhesus monkeys trained to self-administer cocaine.
One compound, GBR 12,909, was evaluated in a Phase 1 clinical
trial.
[Back to top]
Therapeutic Potential of Monoamine Transporter Substrates
Richard B. Rothman and Michael H. Baumann
Monoamine transporter proteins are targets for many
psychoactive compounds, including therapeutic and abused stimulant
drugs. This paper reviews recent work from our laboratory
investigating the interaction of stimulants with transporters
in brain tissue. We illustrate how determining the precise
mechanism of stimulant drug action (uptake inhibitor vs. substrate)
can provide unique opportunities for medication discovery.
An important lesson learned from this work is that drugs which
display equipotent substrate activity at dopamine (DA) and
serotonin (5-HT) transporters have minimal abuse liability
and few stimulant side-effects, yet are able to suppress ongoing
drug-seeking behavior. As a specific example, we describe
the development of PAL-287 (α
methylnapthylethylamine), a dual DA/5-HT releasing
agent that suppresses cocaine self-administration in rhesus
monkeys, without the adverse effects associated with older
phenylethylamine 5-HT releasers (e.g., fenfluramine) and DA
releasers (e.g., amphetamine). Our findings demonstrate the
feasibility of developing non-amphetamine releasing agents
as potential treatments for substance abuse disorders and
other psychiatric conditions.
[Back to top]
Structure-Activity Relationships of Selective GABA
Uptake Inhibitors
Signe Høg, Jeremy R. Greenwood, Karsten
B. Madsen, Orla M. Larsson, Bente Frølund, Arne Schousboe,
Povl Krogsgaard Larsen and Rasmus P. Clausen
For more than four decades there has been a search
for selective inhibitors of GABA transporters. This has led
to potent and selective inhibitors of the cloned GABA transporter
subtype GAT1, which is responsible for a majority of neuronal
GABA transport. The only clinically approved compound with
this mechanism of action is Tiagabine. Other GABA transporter
subtypes have not been targeted with comparable selectivity
and potency. We here review a comprehensive series of competitive
inhibitors that provide information about the GABA recognition
site and summarise the structure-activity relations in a ligand-based
pharmacophore model that suggests how future compounds could
be designed. Finally, some of the recent results on subtype-characterised
competitive inhibitors and recent lipophilic aromatic GABA
uptake inhibitors are reviewed.
[Back to top]
Progress in the Preparation and Testing of Glycine
Transporter Type-1 (GlyT1) Inhibitors
Craig W. Lindsley, Scott E. Wolkenberg and Gene
G. Kinney
Clinically utilized antipsychotic agents share as
a common mechanism the ability to antagonize dopamine D2 receptors
and it is widely assumed that this activity contributes to
their efficacy against the positive symptoms of schizophrenia.
The efficacy of currently marketed antipsychotic agents on
the negative and cognitive symptoms of this disease, however,
is not optimal. One alternate hypothesis to the “dopamine
hypothesis” of schizophrenia derives from the observation
that antagonists of NMDA receptor activity better mimic the
symptomatology of schizophrenia in its entirety than do dopamine
agonists. Findings from this line of research have led to
the NMDA receptor hypofunction (or glutamate dysfunction)
hypothesis of schizophrenia, which complements existing research
implicating dopamine dysfunction in the disease. According
to the NMDA receptor hypofunction hypothesis, any treatment
that enhances NMDA receptor activity may prove useful for
the treatment of the complex symptoms that define schizophrenia.
This idea is now supported by numerous clinical studies that
have reported an efficacious response following treatment
with activators of the NMDA receptor co-agonist glycineB site.
One area of study, aimed at potentiating the NMDA receptor
via activation of the glycineB site is small molecule blockade
of the glycine reuptake transporter type 1 (GlyT1). Broadly,
these efforts have focused on derivatives of the substrate
inhibitor, sarcosine, and non-sarcosine based GlyT1 inhibitors.
Accordingly, the following review discusses the development
of both sarcosine and non-sarcosine based GlyT1 inhibitors
and their current status as putative treatments for schizophrenia
and other disorders associated with NMDA receptor hypoactivity.
[Back to top]
Ligands Targeting the Excitatory Amino Acid Transporters
(EAATs)
John Dunlop and John A. Butera
This review provides an overview of ligands for the
excitatory amino acid transporters (EAATs), a family of high-affinity
glutamate transporters localized to the plasma membrane of
neurons and astroglial cells. Ligand development from the
perspective of identifying novel and more selective tools
for elucidating transporter subtype function, and the potential
of transporter ligands in a therapeutic setting are discussed.
Acute pharmacological modulation of EAAT activity in the form
of linear and conformationally restricted glutamate and aspartate
analogs is presented, in addition to recent strategies aimed
more toward modulating transporter expression levels, the
latter of particular significance to the development of transporter
based therapeutics.
|
