PDF herunterladen
Z Gastroenterol 2000; 38(8): 647-652
DOI: 10.1055/s-2000-7517
Übersichten
© Karl Demeter Verlag im Georg Thieme Verlag Stuttgart · New York

Modulation of gastrointestinal inflammation by chimeric proteins in experimental models

A. Stallmach, B. M. Wittig, M. Zeitz
  • Department of Internal Medicine II, Saarland University
Weitere Informationen

Publikationsverlauf

Publikationsdatum:
31. Dezember 2000 (online)

Auch verfügbar auf
    Lizenzen und Reprints

Summary

Conventional drug therapy in patients with chronic gastrointestinal inflammation is clinically effective in the majority of patients. However, in a relevant group of patients with highly active disease refractory to conventional drugs and for patients with severe side effects new therapeutic strategies are necessary. An advanced understanding of the immune mechanisms underlying chronic diseases resulted in the possibility to use chimeric proteins, in which the variable domains of an immunoglobulin are replaced by extracellular domains of cell surface molecules or cytokines for specific immunomodulation. The immunomodulating effects of chimeric proteins such as CTLA- 4-IgG, interleukin- 10-IgG, IL- 2-IgG or tumour necrosis factor (TNF)-receptor IgG have been proven beneficial in a variety of in vitro and in vivo models of chronic gastrointestinal inflammation and autoimmune diseases. It thus seems likely that genetically engineered fusion proteins targeting specific elements of the immune response may become an essential element in new clinical treatment protocols.

Key words: Cytokine Fusion Proteins - Inflammation - Inflammatory Bowel Disease

Modulation der gastrointestinalen Entzündung durch chimäre Proteine in experimentellen Modellen

Die me-dikamentöse Standardthe­rapie bei Patienten mit chronisch entzündlichen Darmerkrankungen ist in der Regel aus­reichend. Bei Patienten mit chronischer Krankheitsaktivität oder bei Patienten mit relevanten Nebenwirkungen der etablierten Medikamente sind jedoch neue therapeutische Strate­gien notwendig. Das bessere Verständnis der immunologischen Reaktionen bei chronischen Entzündungen führte in jüngster Zeit zur Entwicklung von chimären Proteinen, bei denen die variable Domäne eines Immunglobulins durch den extrazellulären Teil eines Zelloberflächenantigens oder durch funktionell-aktive Sequenzen von Zytokinen ersetzt wurden. Die immunmodulatorischen Effekte dieser Fusionsproteine, wie z. B. des CTLA- 4-IgG, des Interleukin- 10-IgG, des IL- 2-IgG oder des Tumor-Nekrose-Faktor (TNF)-Rezeptor-IgG sind erfolgreich in verschiedenen In-vitro- und In-vivo-Modellen getestet worden. Aufbauend auf diese Ergebnisse könnten genetisch her­gestellte Fusionsproteine zentrale Bestandteile zukünftiger klinischer Therapiestudien werden.

Schlüsselwörter: Zytokinfusionsproteine - Entzündung - Chronisch-entzündliche Darmerkrankung

References

  • 1 Fiocchi C. Inflammatory bowel disease: Etiology and pathogenesis.  Gastroenterology. 1998;  115 182-205
    Google Scholar
  • 2 Duchmann R, Neurath M, Märker-Hermann E, Meyer z um Büschenfelde KH. Immune responses towards intestinal bacteria-current concepts and future perspectives.  Z Gastroenterol. 1997;  35 337-46
    Google Scholar
  • 3 Evans R C, Clarke L, Heath P. et al . Treatment of ulcerative colitis with an engineered human anti-TNFalpha antibody CDP571.  Aliment Pharmacol Ther. 1997;  11 1031-5
    Google Scholar
  • 4 Harding F A, McArthur J G, Gross J A, Raulet D H, Allison J P. CD28-mediated signalling co-stimulates murine T cells and prevents induction of anergy in T-cell clones.  Nature. 1992;  356 607-9
    Google Scholar
  • 5 Gulwani A B, Akolkar P N, Minassian A. et al . Selective expansion of specific T cell receptors in the inflamed colon of Crohn’s disease.  J Clin Invest. 1996;  98 1344-54
    Google Scholar
  • 6 Probert C S, Chott A, Turner J. et al . Persistent clonal expansions of peripheral blood CD4+ lymphocytes in chronic inflammatory bowel disease.  J Immunol. 1996;  157 3183-91
    Google Scholar
  • 7 Leach M W, Bean A G, Mauze S, Coffman R L, Powrie F. Inflammatory bowel disease in C.B- 17 scid mice reconstituted with the CD45RBhigh subset of CD4+ T cells.  Am J Pathol. 1996;  148 1503-15
    Google Scholar
  • 8 Claesson M H, Rudolphi A, Kofoed S, Poulsen S S, Reimann J. CD4+ T lymphocytes injected into severe combined immunodeficient (SCID) mice lead to an inflammatory and lethal bowel disease.  Clin Exp Immunol. 1996;  104 491-500
    Google Scholar
  • 9 Romagnani S. Th1 and Th2 in human diseases.  Clin Immunol Immunopathol. 1996;  80 225-35
    Google Scholar
  • 10 Weiner H L, Friedman A, Miller A. et al . Oral tolerance: Immunologic mechanisms and treatment of animal and human organ-specific autoimmune diseases by oral administration of autoantigens.  Annu Rev Immunol. 1994;  12 809-37
    Google Scholar
  • 11 Marth T, Strober W, Kelsall B L. High dose oral tolerance in ovalbumin TCR-transgenic mice: Systemic neutralization of IL- 12 augments TGF-beta secretion and T cell apoptosis.  J Immunol. 1996;  157 2348-57
    Google Scholar
  • 12 Stallmach A, Strober W, MacDonald T T, Lochs H, Zeitz M. Induction and modulation of gastrointestinal inflammation.  Immunology Today. 1998;  19 438-41
    Google Scholar
  • 13 Robinson M. Optimizing therapy for inflammatory bowel disease.  Am J Gastroenterol. 1997;  92 (Suppl) 12S-17S
    Google Scholar
  • 14 Emmrich J, Seyfarth M, Fleig W E, Emmrich F. Treatment of inflammatory bowel disease with anti-CD4-monoclonal antibody.  Lancet. 1991;  338 570-1
    Google Scholar
  • 15 Otto G, Thies J, Kraus T. et al . Monoclonal anti-CD25 for acute rejection after liver transplantation.  Lancet. 1991;  338 195
    Google Scholar
  • 16 Vincenti F, Kirkman R, Light S. et al . Interleukin- 2-receptor blockade with daclizumab to prevent acute rejection in renal transplantation.  N Engl J Med. 1998;  338 161-5
    Google Scholar
  • 17 Lenschow D J, Zeng Y, Thistlethwaite J. et al . Long-term survival of xenogeneic pancreatic islet grafts induced by CTLA4lg.  ­Science. 1992;  257 789-92
    Google Scholar
  • 18 Bogers W M, Lang F, Parker K E. et al . Rat interleukin- 2 immunoglobulin M fusion proteins are cytotoxic in vitro for cells expressing the IL- 2 receptor and can abolish cell-mediated immunity in vivo.  Transplantation. 1994;  58 932-9
    Google Scholar
  • 19 Finck B K, Linsley P S, Wofsy D. Treatment of murine lupus with CTLA4Ig.  Science. 1994;  265 1225-7
    Google Scholar
  • 20 Kunzendorf U, Pohl T, Bulfone P S. et al . Suppression of cell-mediated and humoral immune responses by an interleukin- 2-immunoglobulin fusion protein in mice.  J Clin Invest. 1996;  97 1204-10
    Google Scholar
  • 21 Capon D J, Chamow S M, Mordenti J. et al . Designing CD4 immunoadhesins for AIDS therapy.  Nature. 1989;  337 525-31
    Google Scholar
  • 22 Traunecker A, Schneider J, Kiefer H, Karjalainen K. Highly efficient neutralization of HIV with recombinant CD4-immunoglobulin molecules.  Nature. 1989;  339 68-70
    Google Scholar
  • 23 Meuer S, Schraven B, Samstag Y. An alternative pathway of T cell activation.  Int Arch Allergy Immunol. 1994;  104 216-21
    Google Scholar
  • 24 Endler-Jobst B, Schrawen B, Hutmacher B, Meuer S. Human T cell response to IL- 1 and IL- 6 are dependent on signals mediated through CD2.  J Immunol. 1991;  146 1736
    Google Scholar
  • 25 Meuer S C, Samstag Y, Schraven B. Accessory signals for growth and differentiation of human T lymphocytes.  Cancer Surv. 1995;  22 63-73
    Google Scholar
  • 26 Jenkins M K, Taylor P S, Norton S D, Urdahl K B. CD28 delivers a costimulatory signal involved in antigen-specific IL- 2 production by human T cells.  J Immunol. 1991;  147 2461-6
    Google Scholar
  • 27 Maiuri L, Auricchio S, Coletta S. et al . Blockage of T-cell costimulation inhibits T-cell action in celiac disease.  Gastroenterology. 1998;  115 564-72
    Google Scholar
  • 28 Schuppan D, Dieterich W, Riecken E O. Exposing gliadin as a tasty food for lymphocytes.  Nat Med. 1998;  4 666-7
    Google Scholar
  • 29 Stallmach A, Belitz H D, Gellermann B. et al . Effects of gliadin peptides B1-B4 in celiac disease. I. Organ culture studies.  J Pediatr Gastroenterol Nutr. 1987;  6 335-40
    Google Scholar
  • 30 de R itis G, Auricchio S, Jones H W. et al . In vitro (organ culture) studies of the toxicity of specific A-gliadin peptides in celiac disease.  Gastroenterology. 1988;  94 41-9
    Google Scholar
  • 31 Picarelli A, Maiuri L, Frate A. et al . Production of antiendomysial antibodies after in-vitro gliadin challenge of small intestine biopsy samples from patients with coeliac disease.  Lancet. 1996;  348 1065-7
    Google Scholar
  • 32 Stüber E, Strober W, Neurath M. Blocking the CD40L-CD40 interaction in vivo specifically prevents the priming of T helper 1 cells through the inhibition of interleukin 12 secretion.  J Exp Med. 1996;  183 693-8
    Google Scholar
  • 33 Stallmach A, Wittig B M, Giese T. et al . Protection of Trinitrobenzene Sulfonic Acid-induced Colitis by an Interleukin- 2-IgG2b Fusion Protein in Mice.  Gastroenterology. 1999; 117: 866-76; 
    Google Scholar
  • 34 Sutterwala F S, Noel G J, Clynes R, Mosser D M. Selective suppression of interleukin- 12 induction after macrophage receptor ligation.  J Exp Med. 1997;  185 1977-85
    Google Scholar
  • 35 Sutterwala F S, Noel G J, Salgame P, Mosser D M. Reversal of proinflammatory responses by ligating the macrophage Fcgamma receptor type I.  J Exp Med. 1998;  188 217-22
    Google Scholar
  • 36 Kühn R, Lohler J, Rennick D, Rajewsky K, Müller W. Interleukin- 10-deficient mice develop chronic enterocolitis.  Cell. 1993;  75 263-74
    Google Scholar
  • 37 Powrie F, Leach M W, Mauze S. et al . Inhibition of Th1 responses prevents inflammatory bowel disease in scid mice reconstituted with CD45RBhi CD4+ T cells.  Immunity. 1994;  1 553-62
    Google Scholar
  • 38 Ribbons K A, Thompson J H, Liu X. et al . Anti-inflammatory properties of interleukin- 10 adminstration in hapten-induced colitis.  Eur J Pharmacol. 1997;  323 245-54
    Google Scholar
  • 39 Pender S LF, Breese E J, Günther U. et al . Suppression of T cell-mediated injury in human gut by interleukin 10: Role of matrix metalloproteinases.  Gastroenterology. 1998;  115 573-83
    Google Scholar
  • 40 Chernoff A E, Granowitz E V, Shapiro L. et al . A randomized, controlled trial of IL- 10 in humans. Inhibition of inflammatory cytokine production and immune responses.  J Immunol. 1995;  154 5492-9
    Google Scholar
  • 41 Zheng X X, Steele A W, Hancock W W. et al . A noncytolytic IL- 10/Fc fusion protein prevents diabetes, blocks autoimmunity, and promotes suppressor phenomena in NOD mice.  J Immunol. 1997;  158 4507-13
    Google Scholar
  • 42 Williams D P, Parker K, Bacha P. et al . Diphtheria toxin receptor binding domain substitution with interleukin- 2: Genetic construction and properties of a diphtheria toxin-related interleukin- 2 fusion protein.  Protein Eng. 1987;  1 493-8
    Google Scholar
  • 43 Bousvaros A, Stevens A C, Strom T B, Murphy J, Lamont J T. Interleukin- 2 fusion protein (DAB389IL- 2) selectively targets activated human peripheral blood and lamina propria lymphocytes.  Dig Dis Sci. 1997;  42 1542-8
    Google Scholar
  • 44 Bastos M G, Pankewycz O, Rubin K V, Murphy J R, Strom T B. ­Concomitant administration of hapten and IL- 2-toxin (DAB486-IL- 2) results in specific deletion of antigen-activated T cell clones.  J Immunol. 1990;  145 3535-9
    Google Scholar
  • 45 Sewell K L, Parker K C, Woodworth T G. et al . DAB486IL- 2 fusion toxin in refractory rheumatoid arthritis.  Arthritis Rheum. 1993;  36 1223-33
    Google Scholar
  • 46 Tepler I, Schwartz G, Parker K. et al . Phase I trial of an interleukin- 2 fusion toxin (DAB486IL- 2) in hematologic malignancies: Complete response in a patient with Hodgkin’s disease refractory to chemotherapy.  Cancer. 1994;  73 1276-85
    Google Scholar
  • 47 LeMaistre C F, Saleh M N, Kuzel T M. et al . Phase I trial of a ligand fusion-protein (DAB389IL- 2) in lymphomas expressing the receptor for interleukin- 2.  Blood. 1998;  91 399-405
    Google Scholar
  • 48 Ullrich R, Schneider T, Schieferdecker H L. et al .Cell activation and proliferation in the large intestine of patients with Crohn’s disease or ulcerative colitis and controls. In: Mestecky J, Russell MW, Jackson S, Michalek SM, Tlaskalová-Hogenová, Sterzl J Plenum Press New York; 1995: 1281-2
    Google Scholar
  • 49 Stallmach A, Schäfer F, Weber S. et al . Increased state of activation of CD4-positive T cells and elevated interferon-γ production in pouchitis.  Gut. 1998;  43 499-505
    Google Scholar
  • 50 MacDonald T T, Hutchings P, Choy M Y, Murch S, Cooke A. Tumour necrosis factor-alpha and interferon-gamma production measured at the single cell level in normal and inflamed human intestine.  Clin Exp Immunol. 1990;  81 301-5
    Google Scholar
  • 51 Murch S H, Braegger C P, Walker S J, MacDonald T T. Location of tumour necrosis factor alpha by immunohistochemistry in chronic inflammatory bowel disease.  Gut. 1993;  34 1705-9
    Google Scholar
  • 52 van D ullemen HM, van D eventer SJ, Hommes D W. et al . Treatment of Crohn's disease with anti-tumor necrosis factor chimeric monoclonal antibody (cA2).  Gastroenterology. 1995;  109 129-35
    Google Scholar
  • 53 Stack W A, Mann S D, Roy A J. et al . Randomised controlled trial of CDP571 antibody to tumour necrosis factor-alpha in Crohn's disease.  Lancet. 1997;  349 521-4
    Google Scholar
  • 54 Targan S R, Hanauer S B, van D S. et al . A short-term study of chimeric monoclonal antibody cA2 to tumor necrosis factor alpha for Crohn's disease. Crohn's Disease cA2 Study Group.  N Engl J Med. 1997;  337 1029-35
    Google Scholar
  • 55 Mohler K M, Torrance D S, Smith C A. et al . Soluble tumor necrosis factor (TNF) receptors are effective therapeutic agents in lethal endotoxemia and function simultaneously as both TNF carriers and TNF antagonists.  J Immunol. 1993;  151 1548-61
    Google Scholar
  • 56 Pender S L, Fell J M, Chamow S M, Ashkenazi A, MacDonald T T. A p55 TNF receptor immunoadhesin prevents T cell-mediated intestinal injury by inhibiting matrix metalloproteinase production.  J Immunol. 1998;  160 4098-103
    Google Scholar
  • 57 Edwards C K. PEGylated recombinant human soluble tumour necrosis factor receptor type I (r-Hu-sTNF-RI): Novel high affinity TNF receptor deigned for chronic inflammatory diseases.  Ann Rheum Dis. 1999;  58 (Suppl 1) 173-81
    Google Scholar
  • 58 Neurath M F, Fuss I, Kelsall B, Meyer z um Büschenfelde KH, Strober W. Effect of IL- 12 and antibodies to IL- 12 on established granulomatous colitis in mice.  Ann N Y Acad Sci. 1996;  795 368-70
    Google Scholar
  • 59 Groux H, OGara A, Bigler M. A CD4+ T cell subset inhibits antigen-specific T-cell response and prevents colitis.  Nature. 1997;  389 737-41
    Google Scholar

Address for correspondence

Andreas Stallmach, MD 

Clinic for Internal Medicine II Saarland University

D-66421 Homburg/Saar, Germany

Fax: 0 49/68 41/16 32 64

      >