Mechanism of the anti-inflammatory effect of colchicine in rheumatic diseases: a possible new outlook through microarray analysis

doi:10.1093/rheumatology/kei140

Rheumatology Advance Access originally published online on September 27, 2005
Rheumatology 2006 45(3):274-282; doi:10.1093/rheumatology/kei140

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Mechanism of the anti-inflammatory effect of colchicine in rheumatic diseases: a possible new outlook through microarray analysis

E. Ben-Chetrit, S. Bergmann¹^,2 and R. Sood

Department of Biochemistry, School of Medicine, Stanford University, CA, USA, ¹ Department of Molecular Genetics, Weizmann Institute for Science, Rehovot, Israel and ² Department of Medical Genetics, University of Lausanne, Switzerland.

Correspondence to: E. Ben-Chetrit, Department of Medicine, Hadassah University Hospital, PO Box 12000, Jerusalem, Israel. E-mail: eldad{at}hadassah.org.il

Objective. Colchicine is an alkaloid that is used to alleviateacute gout and to prevent acute attacks of familial Mediterraneanfever (FMF). However, it is not beneficial when given duringthe occurrence of an acute episode of FMF. It is believed thatcolchicine exerts its anti-inflammatory effect through directinteraction with microtubules. We aim to study the molecularbasis of colchicine action by analysing the effect of this drugon global gene expression of HUVEC (human umbilical vein endothelialcell line) cells.

Methods. HUVEC cells were exposed to various concentrationsof colchicine and were harvested at different time points. Ribonucleicacid was extracted, amplified, reverse transcribed and hybridizedto complementary deoxyribonucleic acid microarrrays containingmore than 40,000 probes to human expressed sequence tags. Thisapproach enabled us to have a global look at the transcriptionalresponse induced by colchicine treatment.

Results. Colchicine changed the expression of many genes inHUVEC cells following exposure to a concentration of 100 ng/mlor higher. Following short exposure (30 or 120 min), colchicineaffected genes known to be involved in the cell cycle and itsregulation. However, change in expression of genes involvedin neutrophil migration or other inflammatory processes wereobserved mainly after 12 to 24 h.

Conclusions. The anti-inflammatory effect of colchicine maybe mediated not only through direct interaction with microtubulesbut also through changes at the transcriptional level. Thislatter effect apparently requires a higher concentration anda longer time to occur. This can explain the observation thatcolchicine does not have an immediate effect when given duringan acute attack of FMF.

KEY WORDS: Colchicine, Familial Mediterranean fever, HUVEC cells, Anti-inflammatory

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