ACR Meeting Abstracts

ACR Meeting Abstracts

Abstract Number: 479

Active Immunization with TNF-Kinoid in Rheumatoid Arthritis Patients with Secondary Resistance to Tumor Necrosis Factor-Alpha Antagonists Is Safe and Immunogenic

Patrick Durez1, Pedro Miranda2, Antoaneta Toncheva3, Alberto Berman Sr.4, Oscar L. Rillo5, Yves Boutsen6, Tatjana Kehler7, Eugenia Mociran8, LiAn Soto Saez9, Bruno Fautrel10, Xavier Mariette11, Panayot Solakov12, Eleonora Lucero13, Tonko Vlak14, Simeon Grazio15, Ksenija Mastrovic16, Rodica Chiriac17, Géraldine Grouard-Vogel18, Olivier Dhellin18, Stéphane Ouary18, Pierre Vandepapeliere18 and Marie-Christophe Boissier19, 1Department of Rheumatology, Université Catholique de Louvain, Brussels, Belgium, 2Universidad de Chile and Centro de Estudios Reumatologicos, Santiago de Chile, Chile, 3National Multiprofile Transport Hospital, Sofia, Bulgaria, 4Internal Medicine, Hospital Padilla, Tucuman, Argentina, 5Rheumatology, Hospital General de Agudos "Dr. E. Tornú", Buenos Aires, Argentina, 6UCL Mont-Godinne, Godinne, Belgium, 7Thalassotherapia Opatija, Opatija, Croatia, 8Emergency County Hospital Dr Constantin Opis, Maramures, Romania, 9Sociedad Medica del Aparato Locomotor SA, Santiago de Chile, Chile, 10Rheumatology / GRC08-EEMOIS, APHP-Pitie Salpetriere Hospital / UPMC, Paris, France, 11Rheumatology, Université Paris-Sud, Le Kremlin Bicetre, France, 12Plovdiv, Diagnostic and Consulting Center, Plovdiv, Bulgaria, 13Rheumatology Unit, Padilla Hospital, Tucumán, Argentina, 14University Hospital Split, Split, Croatia, 15Clinical Hospital Center Sestre Milosrdnice, Zagreb, Croatia, 16Clinical Hospital Sveti Duh, Zagreb, Croatia, 17Rehabilitation clinical Hospital Iasi, Iasi, Romania, 18NEOVACS SA, Paris, France, 19Dept of Rheumatology, Hopital Avicenne, Bobigny, France

Meeting: 2012 ACR/ARHP Annual Meeting

Keywords: , ,

Session Information

Title: Rheumatoid Arthritis Treatment - Small Molecules, Biologics and Gene Therapy

Session Type: Abstract Submissions (ACR)

Background/Purpose: Blocking TNF alpha (TNFα) with monoclonal antibodies (mAbs) has been successful in the treatment of rheumatoid arthritis. However secondary resistances are frequent and impose treatment changes. Active immunization with a TNF-Kinoid that safely induces self polyclonal anti-TNFα antibodies (Abs) could be an alternative to anti-TNFα mAbs. We evaluated the immunogenicity and safety of TNF-K in patients with rheumatoid arthritis and secondary resistance to TNF blockers.

Methods: TNFα-Kinoid (TNF-K, Neovacs SA, Paris, France) is an immunotherapeutic composed of recombinant human TNFα conjugated to KLH, inactivated and adjuvanted with ISA-51 emulsion. 40 patients with active rheumatoid arthritis (DAS28≥3.2) with history of positive clinical response to at least one TNF-blocker followed by secondary failure (35% IFX, 30 % ADA, 42.5% ETA) were enrolled in a double-blind, placebo-controlled, phase 2 study to evaluate three different intramuscular doses of TNF-K (90, 180, 360 mcg) and two immunization schedules (D0 and 28 or D0, 7 and 28). Humoral immune responses were evaluated through titration of anti-TNFα and anti-KLH Abs and neutralization assay. The T cell response was assessed by lymphoproliferative assay with tritiated thymidine incorporation. Clinical response was evaluated by the ACR and EULAR core set response.

Results: No related serious adverse event has been reported. Few minor transient local and systemic reactions have been recorded following immunization. Anti-TNFα Abs were induced in 50%, 75% and 91% of patients at 90 mcg, 180 mcg and 360 mcg, respectively. 100% of patients with three injections of 180 or 360 mcg had immunogenic response against TNF versus 67% in the groups receiving two injections. The anti-TNF antibody geometric mean titres were higher in patients who received 3 injections of 360 mcg. No lymphoproliferative response could be measured after stimulation with native TNF.  Among the 21 patients who developed anti-TNF Abs, 48% present a moderate to good response according to EULAR score as opposed to only 31% of the 16 patients without Abs. A mean decrease of -14% of the C reactive protein level is measured in patients with Abs while in patients without Abs, the mean CRP level increased by 5%.

Conclusion: Active immunization with TNFα kinoid to induce a polyclonal, self-anti-TNFα antibody response is safe and immunogenic. A clear dose-response was observed for the dose of kinoid as well as  for the number of administrations. Association of anti-TNF Abs induced by the kinoid with clinical and biological responses were observed in patients included in this preliminary phase 2 study. Further studies are needed to confirm this new approach in RA.

Disclosure:

P. Durez,
None;

P. Miranda,
None;

A. Toncheva,
None;

A. Berman Sr.,
None;

O. L. Rillo,
None;

Y. Boutsen,
None;

T. Kehler,
None;

E. Mociran,
None;

L. Soto Saez,
None;

B. Fautrel,
None;

X. Mariette,

Neovacs SA,

5;

P. Solakov,
None;

E. Lucero,
None;

T. Vlak,
None;

S. Grazio,
None;

K. Mastrovic,
None;

R. Chiriac,
None;

G. Grouard-Vogel,

Neovacs SA,

3;

O. Dhellin,

Neovacs SA,

3;

S. Ouary,

Neovacs SA,

3;

P. Vandepapeliere,

Neovacs SA,

3;

M. C. Boissier,

Neovacs SA,

5.

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