Zusammenfassung
Die Wirksamkeit verschiedener Substanzen auf Schubparameter ist bei Patienten mit
schubhaft remittierender Multipler Sklerose (MS) gut belegt. Patienten mit progredienten
MS-Verläufen profitieren dagegen von Immuntherapie kaum. Gegenwärtig wird daher der
Behandlungsbeginn nach dem ersten Schub propagiert, auch mit dem Ziel, Degeneration
und Behinderung entgegenzuwirken. In der vorliegenden Übersicht wird diese Vorstellung
einer kritischen Prüfung unterzogen. Tatsächlich gibt es keine Evidenz, dass durch
frühen Beginn einer Immuntherapie die sekundäre Progression verzögert oder abgeschwächt
werden kann. Ausgedehnte Degeneration lässt sich früh im Krankheitsverlauf und unabhängig
von Entzündungsaktivität fassen. Autoimmunität per se stellt offensichtlich kein ausreichendes
pathogenetisches Konzept für MS dar. Alternativ wird ein Virus-Superantigen-Dualismus
als Ursache der unterschiedlichen Pathomechanismen der MS vorgestellt. Zusammenfassend
ist eine Evidenz-basierte Immuntherapie an der tatsächlichen Entzündungsaktivität
der Erkrankung auszurichten. Geeignet ist dafür insbesondere der Abstand zwischen
zwei Schüben.
Abstract
It is well established that relapses can be suppressed by different substances in
patients with relapsing-remitting multiple sclerosis (MS). In contrast, patients with
progressive forms of MS do hardly respond to immune therapy. Therefore, start of immune
therapy after the first relapse has been proposed, especially in order to prevent
degeneration and disability. This view is challenged in the present review. Actually
no evidence exists in support of a retardation or an attenuation of secondary progression
by early immune therapy. Widespread degeneration occurs early and progresses independently
from inflammatory plaques. Therefore, autoimmunity per se is no adequate paradigm
to explain MS-pathogenesis entirely. A virus/superantigen-dualism is proposed to explain
the different parts of MS, instead. It is concluded that evidence-based immune therapy
should be adapted to the actual inflammatory activity of the disease. A suitable parameter
for this purpose is the interval between 2 relapses.
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Dr. med. M. E. Kornhuber
Neurologische Klinik der Universität Halle-Wittenberg
Ernst-Grube-Str. 40
6097 Halle (Saale), Deutschland
Email: malte.kornhuber@medizin.uni-halle.de