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人T细胞对柳氮磺胺吡啶的获得性耐药:耐药表型的稳定性及对非相关改善病情抗风湿药的敏感性

Acquired resistance of human T cells to sulfasalazine: stability of the resistant phenotype and sensitivity to non-related DMARDs.

作者信息

van der Heijden J, de Jong M C, Dijkmans B A C, Lems W F, Oerlemans R, Kathmann I, Scheffer G L, Scheper R J, Assaraf Y G, Jansen G

机构信息

Department of Rheumatology, Vrije Universiteit Medical Centre, Amsterdam, The Netherlands.

出版信息

Ann Rheum Dis. 2004 Feb;63(2):131-7. doi: 10.1136/ard.2003.006494.

Abstract

BACKGROUND

A recent study from our laboratory showed that induction of the multidrug resistance related drug efflux pump ABCG2 contributed to acquired resistance of human T cells to the disease modifying antirheumatic drug (DMARD) sulfasalazine (SSZ).

OBJECTIVES

To investigate the duration of SSZ resistance and ABCG2 expression after withdrawal of SSZ and rechallenging with SSZ, and to assess the impact of SSZ resistance on responsiveness to other DMARDs.

METHODS

Human CEM cells (T cell origin) with acquired resistance to SSZ (CEM/SSZ) were characterised for (a) SSZ sensitivity and ABCG2 expression during withdrawal and rechallenge of SSZ, and (b) antiproliferative efficacy of other DMARDs.

RESULTS

ABCG2 protein expression was stable for at least 4 weeks when CEM/SSZ cells were grown in the absence of SSZ, but gradually declined, along with SSZ resistance levels, to non-detectable levels after withdrawal of SSZ for 6 months. Rechallenging with SSZ led to a rapid (<2.5 weeks) resumption of SSZ resistance and ABCG2 expression as in the original CEM/SSZ cells. CEM/SSZ cells displayed diminished sensitivity to the DMARDs leflunomide (5.1-fold) and methotrexate (1.8-fold), were moderately more sensitive (1.6-2.0 fold) to cyclosporin A and chloroquine, and markedly more sensitive (13-fold) to the glucocorticoid dexamethasone as compared with parental CEM cells.

CONCLUSION

The drug efflux pump ABCG2 has a major role in conferring resistance to SSZ. The collateral sensitivity of SSZ resistant cells for some other (non-related) DMARDs may provide a further rationale for sequential mono- or combination therapies with distinct DMARDs upon decreased efficacy of SSZ.

摘要

背景

我们实验室最近的一项研究表明,多药耐药相关药物外排泵ABCG2的诱导导致人类T细胞对疾病修饰抗风湿药物(DMARD)柳氮磺胺吡啶(SSZ)产生获得性耐药。

目的

研究停用SSZ并再次使用SSZ后,SSZ耐药的持续时间和ABCG2的表达情况,并评估SSZ耐药对其他DMARDs反应性的影响。

方法

对获得SSZ耐药性的人CEM细胞(T细胞来源)(CEM/SSZ)进行如下特征分析:(a)在停用和再次使用SSZ期间的SSZ敏感性和ABCG2表达,以及(b)其他DMARDs的抗增殖效力。

结果

当CEM/SSZ细胞在无SSZ的情况下生长时,ABCG2蛋白表达至少4周保持稳定,但在停用SSZ 6个月后,随着SSZ耐药水平逐渐下降至无法检测到的水平。再次使用SSZ导致SSZ耐药和ABCG2表达迅速恢复(<2.5周),如同原始的CEM/SSZ细胞。与亲代CEM细胞相比,CEM/SSZ细胞对DMARDs来氟米特(5.1倍)和甲氨蝶呤(1.8倍)的敏感性降低,对环孢素A和氯喹的敏感性中度增加(增加1.6 - 2.0倍),对糖皮质激素地塞米松的敏感性显著增加(13倍)。

结论

药物外排泵ABCG2在赋予对SSZ的耐药性中起主要作用。SSZ耐药细胞对某些其他(非相关)DMARDs的旁系敏感性可能为在SSZ疗效降低时采用不同DMARDs进行序贯单药或联合治疗提供进一步的理论依据。

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