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(DIR) Return to: TECFIDERA (dimethyl fumarate, BG-12, Fumaderm)
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#Post#: 240--------------------------------------------------
How Tecfidera works explained
By: agate Date: April 4, 2014, 3:20 pm
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From Medical News Today, April 3, 2014:
[quote]Research may lead to development of novel therapeutic
agents for multiple sclerosis
Just a few short weeks ago, dimethyl fumarate was approved in
Europe as a basic therapy for multiple sclerosis. Although its
efficacy has been established in clinical studies, its
underlying mode of action was still unknown, but scientists from
Bad Nauheim's Max Planck Institute for Heart and Lung Research
and the University of Lubeck have now managed to decode it. They
hope that this knowledge will help them develop more effective
therapeutic agents.
...
Basic MS therapy to date generally involved beta interferons or
the active substance glatiramer acetate. In both cases, the drug
was administered by injections under the skin or into the
muscle, which is a cause of considerable discomfort and
annoyance to many patients.
By contrast, the active substance dimethyl fumarate (DMF),
approved in Europe for MS treatment only a few weeks ago, brings
a ray of hope to those affected since it can be taken in tablet
form. The efficacy of DMF in clinical studies was at least
comparable to that of the more established substances, while its
side effects were moderate by comparison.
DMF has been in use for some twenty years as a successful
treatment for psoriasis, but little was known about how it
influences immune function. Scientists from Nina Wettschureck's
research groups at the Max Planck Institute for Heart and Lung
Research in Bad Nauheim and Markus Schwaninger from the
Institute of Experimental and Clinical Pharmacology and
Toxicology at the University of Lübeck have explained
significant aspects of how DMF works.
In their study, the researchers used a standardised mouse model
of multiple sclerosis, whereby drugs trigger an autoimmune
response, leading to characteristic reactions within days. In
this way, they induced neurological deficits comparable to those
observed in MS. "In the group we treated with DMF, the problems
with motor function were considerably lower than in the control
group," says Wettschureck.
The researchers uncovered the mode of action by treating
genetically modified mice in the same way. "In mice that don't
have the gene for the receptor called HCA2, DMF was unable to
prevent the signs of paralysis," explains Schwaninger. This
means that the HCA2 receptor must mediate the therapeutic effect
of DMF. HCA2 is a so-called G protein-coupled membrane receptor
which occurs, among other places, on a certain type of white
blood cells, neutrophil granulocytes. "In animals treated with
DMF, the number of granulocytes that infiltrated the nervous
system was much lower than in untreated animals. In animals
without the HCA2 receptor, the number of invasive granulocytes
remained equally high despite treatment with DMF," stated
Wettschureck.
In other experiments involving cell cultures, the scientists
found that activation of the HCA2 receptor is responsible for
infiltration of the central nervous system by white blood cells.
DMF blocks this infiltration, thereby preventing the associated
inflammation. "Our study has enabled us to provide the first
evidence that DMF's protective effect is due to the HCA2
receptor. However, we are not ruling out the possibility that
there may also be other mechanisms," observed Wettschureck.
As a next step, the scientists want to find out why patients
respond differently to treatment with DMF. "It may be that
individual genetic differences influence the efficacy of DMF,"
states Schwaninger. Consequently, future therapies could be
specifically designed for individual patients, an approach known
as personalised medicine.
The researchers also intend to search for additional substances
that bind to the HCA2 receptor. "Ideally, we would find a
substance of comparable or even greater efficacy, but with fewer
side effects," says Wettschureck. The colleagues in Bad Nauheim
and Lübeck hope this will lead to the development of novel
therapeutic agents for MS with an improved profile in terms of
efficacy and adverse effects.
[/quote]
[quote]Original publication:
Hui Chen, Julian C. Assmann, Antje Krenz, Mahbubur Rahman,
Myriam Grimm, Christian M. Karsten, Jörg Köhl, Stefan
Offermanns, Nina Wettschureck, Markus Schwaninger
Hydroxycarboxylic acid receptor 2 mediates dimethyl fumarate’s
protective effect in EAE. The Journal of Clinical Investigation,
2 April 2014 (doi:10.1172/JCI72151)
Max-Planck-Gesellschaft[/quote]
The entire article can be seen here
(HTM) http://www.medicalnewstoday.com/releases/274939.php?tw.
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