Department of Rheumatology and Inflammation Research, Sahlgrenska University Hospital, Guldhedsgatan 10A, 413 46 Göteborg, Sweden.
Rheumatology (Oxford). 2010 Oct;49(10):1911-9. doi: 10.1093/rheumatology/keq159. Epub 2010 Jun 14.
Viruses may contribute to RA. This prompted us to monitor viral load and response to anti-CD20 therapy in RA patients.
Blood and bone marrow from 35 RA patients were analysed for CMV, EBV, HSV-1, HSV-2, parvovirus B19 and polyomavirus using real-time PCR before and 3 months after rituximab (RTX) treatment and related to the levels of autoantibodies and B-cell depletion. Clinical response to RTX was defined as decrease in the 28-joint disease activity score (DAS-28) >1.3 at 6 months.
Before RTX treatment, EBV was identified in 15 out of 35 patients (EBV-positive group), of which 4 expressed parvovirus. Parvovirus was further detected in eight patients (parvo-positive group). Twelve patients were negative for the analysed viruses. Following RTX, EBV was cleared, whereas parvovirus was unaffected. Eighteen patients were responders, of which 12 were EBV positive. The decrease in the DAS-28 was significantly higher in EBV-positive group compared with parvo-positive group (P = 0.002) and virus-negative patients (P = 0.04). Most of EBV-negative patients that responded to RTX (75%) required retreatment within the following 11 months compared with only 8% of responding EBV-positive patients. A decrease of RF, Ig-producing cells and CD19(+) B cells was observed following RTX but did not distinguish between viral infections. However, EBV-infected patients had significantly higher levels of Fas-expressing B cells at baseline as compared with EBV-negative groups.
EBV and parvovirus genomes are frequently found in bone marrow of RA patients. The presence of EBV genome was associated with a better clinical response to RTX. Thus, presence of EBV genome may predict clinical response to RTX.
病毒可能与类风湿关节炎(RA)的发病相关。因此,我们对 RA 患者进行了病毒载量监测,并评估了抗 CD20 治疗对病毒的影响。
35 例 RA 患者在接受利妥昔单抗(RTX)治疗前和治疗后 3 个月,采用实时 PCR 检测其血液和骨髓中的巨细胞病毒(CMV)、EB 病毒、单纯疱疹病毒 1 型(HSV-1)、单纯疱疹病毒 2 型(HSV-2)、微小病毒 B19 和多瘤病毒,同时检测与自身抗体和 B 细胞耗竭相关的指标。以治疗后 6 个月时 28 关节疾病活动度评分(DAS-28)下降>1.3 定义为 RTX 临床应答。
在 RTX 治疗前,35 例患者中有 15 例(EBV 阳性组)存在 EBV,其中 4 例表达微小病毒。进一步检测发现,8 例患者存在微小病毒(微小病毒阳性组)。12 例患者病毒检测均为阴性。治疗后,EBV 被清除,但微小病毒未受影响。18 例患者为应答者,其中 12 例为 EBV 阳性。与微小病毒阳性组和病毒阴性组相比,EBV 阳性组的 DAS-28 下降更明显(P = 0.002 和 P = 0.04)。在随后的 11 个月内,大多数对 RTX 应答的 EBV 阴性患者(75%)需要再次治疗,而应答的 EBV 阳性患者仅为 8%。治疗后,RF、Ig 产生细胞和 CD19+B 细胞均减少,但不能区分病毒感染。然而,与 EBV 阴性组相比,EBV 感染患者在基线时 Fas 表达的 B 细胞明显更高。
RA 患者骨髓中经常存在 EBV 和微小病毒基因组。EBV 基因组的存在与 RTX 治疗的临床应答相关。因此,EBV 基因组的存在可能预测 RTX 的临床应答。
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