依那西普血清水平与强直性脊柱炎患者疗效无相关性
De Vries MK, Wolbink GJ, et al. EULAR 2007. Present ID: FRI0382.
背景:我们最近的一研究显示AS的Infliximab无效者与Infliximab外周血水平低以及和出现Infliximab抗体有关。
目的:评价AS的Etanercept疗效是否也与Etanercept水平以及出现Etanercept抗体有关。
方法: 用Etanercept 25mg x2/周治疗AS患者。基线时、治疗第3和6月时,随机挑选患者采集血清。 ASAS疗效的定义:BASDAI分数出现50%相对变化或绝对改变超过2 cm。用ELISA测定Etanercept血清水平。用经典的抗原结合试验检测Etanercept抗体。将临床疾病活动度数据与血清 Etanercept水平进行相关分析。
结果:共纳入72例患者。治疗后有50例(69.4%)出现ASAS应答。第3、6 月时,Etanercept中位数水平为2.4 mg/l (范围:0~7.5, N=63)、2.9 mg/l (范围:0.8~5.4, N=57)。应对组与非应答组Etanercept水平无显著差异。BMI、ESR、CRP水平与Etanercept水平之间无相关性。未发现 Etanercept抗体。
结论:Etanercept治疗3月后,69% AS患者被判为治疗有效。应答组与非应答组之间的Etanercept血清水平相似。而且与之前研究发现Infliximab抗体明显不同的是,本研究未发现Etanercept抗体。
[FRI0382] NO DIFFERENCE IN
ETANERCEPT LEVELS BETWEEN RESPONDERS AND NON-RESPONDERS IN PATIENTS
WITH ANKYLOSING SPONDYLITIS TREATED WITH 25 MG ETANERCEPT TWICE A
WEEK
M.K. de Vries 1, G.J. Wolbink 2, M.T.
Nurmohamed 3, L.A. Aarden 4, S.O. Stapel
4, M.J.L. Peters 3, J.C. van Denderen
3, B.A.C. Dijkmans 1, I.E. van der
Horst-Bruinsma 1. 1Rheumatology, VU
University Medical Center, 2Rheumatology, Sanquin
Research, 3Rheumatology, Jan van Breemen Institute,
4Immunopathology, Sanquin Research, Amsterdam,
Netherlands
Background: Recently we showed in patients with Ankylosing
Spondylitis (AS), who were treated with infliximab, that
non-response was correlated with undetectable infliximab levels and
presence of antibodies to infliximab.
Objectives: To evaluate whether clinical response of AS to
etanercept also correlates with etanercept levels, and the presence
of antibodies to etanercept.
Methods: AS patients were treated with etanercept 25 mg
twice weekly. Sera were collected randomly at baseline, after 3 and
6 months of treatment.
ASAS response was defined as 50% relative change of the BASDAI
score or absolute change of 2cm.
Etanercept levels were measured by a newly developed ELISA,
measuring binding of etanercept to TNFalpha. Antibodies to
etanercept were measured with an antigen binding test and a
classical two side assay. Clinical data were used to correlate
disease activity with serum etanercept levels.
Results: 72 patients were included. After 3 months of
treatment 50 patients (69.4%) were ASAS responders. Median
etanercept levels were 2.4 mg/l (range 0-7.5, N=63) and 2.9 mg/l
(range 0.8-5.4, N=57), after 3 and 6 months resp. No significant
differences were found between the etanercept levels of responders
and non-responders. No correlation was found between BMI, ESR, CRP
levels and etanercept levels. No antibodies to etanercept were
detected with any of the assays used.
Fig. 1. Mean etanercept levels (mg/l) and SD for ASA non-responders
and responders after 3 months of treatment of AS with
etanercept.
Conclusion: 69% of the patients was classified as responder after 3 months of treatment. Serum etanercept levels of responders and non-responders were similar. Moreover, no antibody formation against etanercept was detected in these patients which is in contrast with our prior study of infliximab in AS.
Citation: Ann
Rheum Dis 2007;66(Suppl II):395
Session: Spondylarthropathies