Monitoring der Therapie von Multiple-Sklerose-Patienten basierend auf Transkriptomuntersuchungen

 

 Buy Article Permissions and Reprints

Zusammenfassung

Die Multipe Sklerose (MS) stellt nach heutigem Erkenntnisstand eine multifaktorielle immunmediierte Erkrankung dar, deren Verlauf als auch Therapieansprechen von einer Reihe von Genen beeinflusst wird. Ein Ziel der biomedizinischen MS-Forschung ist die Bestimmung und Evaluierung der Expression prädisponierender Gene, die den Krankheitsverlauf und das Therapieansprechen vorhersagen (prognostische Biomarker). Solche Informationen können direkten Einfluss auf Auswahl und Optimierung von Therapeutika und für die Entwicklung von Behandlungsstrategien haben. Das genomweite RNA-Profil eines Individuums repräsentiert eine wichtige Komponente bei der umfassenden Bestimmung von krankheitsrelevanten oder Therapieresponse-assoziierten Faktoren. Es dient hiermit einem großangelegten Screening. Die vorliegende Arbeit liefert einen Überblick über den Stand der genomweiten Screeningmethoden auf Transkriptomebene in humanen peripheren Immunzellen bei MS.

Abstract

Multiple sclerosis (MS) is a multifactorial immune mediated disease; its course and response to therapy is influenced by various genes. A goal of the biomedical MS research is the discovery of sets of predisposing genes of which differential expression predict the disease course and outcomes of drug therapy. Such knowledge would have direct consequences for selection, refinement or development of treatments. The genome-wide RNA profile of an individual represents one component of the comprehensive determination of disease- or drug response-related elements; it serves as a large-scale approach. This work reviews the state of the art in MS research applying genomewide screening methods at the transcriptome level in peripheral immune cells of humans.

Literatur

• 1 Lassmann H, Bruck W, Lucchinetti C. Heterogeneity of multiple sclerosis pathogenesis: implications for diagnosis and therapy.  Trends Mol Med. 2001;  7 115-121
  Google Scholar
• 2 Goodin D S. Disease-modifying therapy in multiple sclerosis: update and clinical implications.  Neurology. 2008;  71 S8-S13
  Google Scholar
• 3 Rieckmann P, Toyka K V. Multiple Sclerosis Therapy Consensus Group . Immunmodulatorische Stufentherapie der Multiplen Sklerose.  Nervenarzt. 2002;  73 556-563
  Google Scholar
• 4 Hemmer B, Hartung H P. Toward the development of rational therapies in multiple sclerosis: what is on the horizon?.  Ann Neurol. 2007;  62 314-326
  Google Scholar
• 5 Villoslada P, Steinman L, Baranzini S E. Systems biology and its application to the understanding of neurological diseases.  Ann Neurol. 2009;  65 124-139
  Google Scholar
• 6 Vastag B. Gene chips inch toward the clinic.  JAMA. 2003;  289 155-159
  Google Scholar
• 7 Windeler J. Prognosis – what does the clinician associate with this notion?.  Stat Med. 2000;  19 425-430
  Google Scholar
• 8 Comabella M, Martin R. Genomics in multiple sclerosis – current state and future directions.  J Neuroimmunol. 2007;  187 1-8
  Google Scholar
• 9 Goertsches R H, Hecker M, Zettl U K. Monitoring of multiple sclerosis immunotherapy: from single candidates to biomarker networks.  J Neurol. 2008;  225 (Suppl 6) 48-57
  Google Scholar
• 10 Sturzebecher S, Wandinger K P, Rosenwald A. et al . Expression profiling identifies responder and non-responder phenotypes to interferon-beta in multiple sclerosis.  Brain. 2003;  126 1419-1429
  Google Scholar
• 11 Wandinger K P, Lunemann J D, Wengert O. et al . TNF-related apoptosis inducing ligand (TRAIL) as a potential response marker for interferon-beta treatment in multiple sclerosis.  Lancet. 2003;  361 2036-2043
  Google Scholar
• 12 Baranzini S E, Mousavi P, Rio J. et al . Transcription-based prediction of response to IFNbeta using supervised computational methods.  PLoS Biol. 2005;  3 e2
  Google Scholar
• 13 Goertsches R, Serrano-Fernández P, Möller S. et al . Multiple sclerosis therapy monitoring based on gene expression.  Curr Pharm Des. 2006;  12 3761-3779
  Google Scholar
• 14 Hecker M, Goertsches R H, Engelmann R. et al . Integrative Modelling of Transcriptional Regulation in Response to Antirheumatic Therapy.  BMC Bioinformatics. 2009;  (in Revision)
  Google Scholar
• 15 Fernald G H, Knott S, Pachner A. et al . Genome-wide network analysis reveals the global properties of IFN-beta immediate transcriptional effects in humans.  J Immunol. 2007;  178 5076-5085
  Google Scholar
• 16 Palacios R, Goni J, Martinez-Forero I. et al . A network analysis of the human T-cell activation gene network identifies JAGGED1 as a therapeutic target for autoimmune diseases.  PLoS ONE. 2007;  2 e1222
  Google Scholar
• 17 Weinstock-Guttman B, Bhasi K, Badgett D. et al . Genomic effects of once-weekly, intramuscular interferon-█1a treatment after the first dose and on chronic dosing: Relationships to 5-year clinical outcomes in multiple sclerosis patients.  J Neuroimmunol. 2008;  205 113-125
  Google Scholar
• 18 Goertsches R, Hecker M, Koczan D. et al . Biological function analyses of long-term genome wide blood RNA expression profiles yield novel molecular response candidates for interferon beta treatment in relapsing remitting multiple sclerosis.  Pharmacogenomics. 2009;  (in Revision)
  Google Scholar

Prof. Dr. med. Uwe K. Zettl

Klinik und Poliklinik für Neurologie, Universität Rostock

Gehlsheimer Str. 20

18147 Rostock

Email: uwe.zettl@med.uni-rostock.de