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DOI: 10.1055/s-2008-1074549
© Georg Thieme Verlag KG Stuttgart · New York
Elastase Inhibition Assay with Peptide Substrates – An Example for the Limited Comparability of in vitro Results
Publikationsverlauf
Received: December 21, 2007
Revised: April 24, 2008
Accepted: April 25, 2008
Publikationsdatum:
06. Juni 2008 (online)
Abstract
Many factors such as buffer, pH, or enzyme concentration influence the inhibitory activity of test compounds in in vitro enzyme inhibition assays. The purpose of this study was to evaluate whether the variation of the synthetic substrate has an influence on the IC50 values as well. As an exemplary enzyme, we have chosen polymorphonuclear neutrophil elastase (PMNE), which is considered as a promising target in the therapy for inflammatory and tumour diseases. A well established, validated in vitro PMNE inhibition assay was performed with three different synthetic peptide substrates (S-2484, L-1335, I-1270). As inhibitors ursolic acid, unfractionated heparin (UFH), the semisynthetic glucan sulfate PS3, and sulfated polysaccharides from the red algae Delesseria sanguinea (D.s.-SP), were used. The maximum achievable PMNE inhibition by the test compounds was shown to be determined by the substrate: 60 to 70 % (L-1335 and S-2484) or 90 % (I-1270). Furthermore, the IC50 values of the inhibitors turned out to strongly vary in dependence on the substrate, although the used peptide substrates are structurally very similar. The derived activities differed by up to 480 %. In addition, the potencies of the test compounds in relation to each other altered considerably. In conclusion, by the choice of the enzyme substrate, both the apparent maximum activity and the IC50 of an inhibitor can be influenced. Therefore, only results from identical test systems should be compared.
Abbreviations
D.s.-SP:sulfated polysaccharides from the red alga Delesseria sanguinea
I-1270:methoxysuccinyl-alanine-alanine-proline-valine-7-amido-4-metyhlcoumarin
L-1335:methoxysuccinyl-alanine-alanine-proline-valine-p-nitroanilide
PMN:polymorphonuclear neutrophil
PMNE:polymorphonuclear neutrophil elastase
S-2484:L-pyroglutamyl-proline-valine-p-nitroanilide
UFH:unfractionated heparin
Key words
elastase - PMNE - synthetic substrate - chromogenic assay - enzyme inhibition assay - sulfated polysaccarides - ursolic acid
References
- 1 Borregaard N, Cowland J B. Granules of the human neutrophilic polymorphonuclear leukocyte. Blood. 1997; 89 3503-21
- 2 Bank U, Ansorge S. More than destructive: neutrophil-derived serine proteases in cytokine bioactivity control. J Leukoc Biol. 2001; 69 197-206
- 3 Janoff A. Elastase in tissue injury. Annu Rev Med. 1985; 36 207-16
- 4 Bernstein P R, Edwards P D, Williams J C. Inhibitors of human leukocyte elastase. Prog Med Chem. 1994; 31 59-120
- 5 Döring G. The role of neutrophil elastase in chronic inflammation. Am J Resp Crit Care. 1994; 150 S114-7
- 6 Wiedow O, Wiese F, Streit V, Kalm C, Christophers E. Lesional elastase activity in psoriasis, contact dermatitis, and atopic dermatitis. J Invest Dermatol. 1992; 99 306-9
- 7 Siedle B, Hrenn A, Merfort I. Natural compounds as inhibitors of human neutrophil elastase. Planta Med. 2007; 73 401-20
- 8 Ohbayashi H. Neutrophil elastase inhibitors as treatment for COPD. Expert Opin Inv Drug. 2002; 11 965-80
- 9
Melzig M F, Loser B, Ciesielski S.
Inhibition of neutrophil elastase activity by phenolic compounds from plants.
Pharmazie.
2001;
56
967-70
MissingFormLabel
- 10 Skiles J W, Miao C, Sorcek R, Jacober S, Mui P W, Chow G. et al . Inhibition of human leukocyte elastase by N-substituted peptides containing alpha,alpha-difluorostatone residues at P1. J Med Chem. 1992; 35 4795-808
- 11 Steinmeyer J, Kalbhen D A. Pharmacological influence on polymorphonuclear granulocytes elastase under various test conditions. Arzneimittelforschung. 1990; 40 196-200
- 12 Lestienne P, Bieth J G. Activation of human leukocyte elastase activity by excess substrate, hydrophobic solvents, and ionic strength. J Biol Chem. 1980; 255 9289-94
- 13 Sartor L, Pezzato E, Dell′Aica I, Caniato R, Biggin S, Garbisa S. Inhibition of matrix-proteases by polyphenols: chemical insights for anti-inflammatory and anti-invasion drug design. Biochem Pharmacol. 2002; 64 229-37
- 14 Becker M, Franz G, Alban S. Inhibition of PMN-elastase activity by semisynthetic glucan sulfates. Thromb Haemost. 2003; 89 915-25
- 15 Yvin J, Alban S, Franz G. Anti-inflammatory and healing medicine based on laminarin sulfate. PCT Int Appl Patent No WO 2 002 036 132 May 2002
MissingFormLabel
- 16 Grünewald N, Alban S. Optimized isolation and structural characterization of biologically active sulfated polysaccharides from the red alga Delesseria sanguinea (Hudson) Lamouroux. Planta Med. 2007; 73 932
- 17 Macdonald S JF, Dowle M D, Harrison L A, Shah P, Johnson M R, Inglis G GA. et al . The discovery of a potent, intracellular, orally bioavailable, long duration inhibitor of human neutrophil elastase – GW311616A a development candidate. Bioorg Med Chem Lett. 2001; 11 895-8
- 18 Pannell R, Johnson D, Travis J. Isolation and properties of human plasma α-1-proteinase inhibitor. Biochemistry. 1974; 13 5439-45
- 19 Redini F, Tixier J M, Petitou M, Choay J, Robert , Hornebeck W. Inhibition of leucocyte elastase by heparin and its derivatives. Biochem J. 1988; 252 515-9
- 20 Ying Q L, Rinehart A R, Simon S R, Cheronis J C. Inhibition of human leucocyte elastase by ursolic acid. Evidence for a binding site for pentacyclic triterpenes. Biochem J. 1991; 277 521-6
- 21 Padrines M, Bieth J G. Elastin decreases the efficiency of neutrophil elastase inhibitors. Am J Respir Cell Mol Biol. 1991; 4 187-93
- 22 Stein R L. Catalysis by human leukocyte elastase: Substrate structural dependence of rate-limiting protolytic catalysis and operation of the charge relay system. J Am Chem Soc. 1983; 105 5111-6
- 23 Stein R L. Catalysis by human leukocyte elastase. 4. Role of secondary-subsite interactions. J Am Chem Soc. 1985; 107 5767-75
- 24 Shin J S, Yu M H. Kinetic dissection of alpha1-antitrypsin inhibition mechanism. J Biol Chem. 2002; 277 11 629-35
- 25 Huntington J A, Read R J, Carrell R W. Structure of a serpin-protease complex shows inhibition by deformation. Nature. 2000; 407 923-6
- 26 Spencer J L, Stone P J, Nugent M A. New insights into the inhibition of human neutrophil elastase by heparin. Biochemistry. 2006; 45 9104-20
Inken Groth
Pharmaceutical Institute
Department of Pharmaceutical Biology
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24118 Kiel
Germany
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eMail: igroth@pharmazie.uni-kiel.de