系统性硬化症患者自体造血干细胞移植后的免疫重建:临床获益与免疫抑制强度之间的关系
Immunological reconstitution after autologous hematopoietic stem cell transplantation in patients with systemic sclerosis: relationship between clinical benefits and intensity of immunosuppression.
作者信息
Bohgaki Toshiyuki, Atsumi Tatsuya, Bohgaki Miyuki, Furusaki Akira, Kondo Makoto, Sato-Matsumura Kazuko C, Abe Riichiro, Kataoka Hiroshi, Horita Tetsuya, Yasuda Shinsuke, Amasaki Yoshiharu, Nishio Mitsufumi, Sawada Ken-Ichi, Shimizu Hiroshi, Koike Takao
机构信息
Department of Medicine II, Hokkaido University Graduate School of Medicine, N15, W7, Kita-ku, Sapporo 060-8638, Japan.
出版信息
J Rheumatol. 2009 Jun;36(6):1240-8. doi: 10.3899/jrheum.081025. Epub 2009 May 15.
OBJECTIVE
To analyze the relationship between clinical benefits and immunological changes in patients with systemic sclerosis (SSc) treated with autologous hematopoietic stem cell transplantation (HSCT).
METHODS
Ten patients with SSc were treated with high-dose cyclophosphamide followed by highly purified CD34+ cells (n=5) or unpurified grafts (n=5). Two groups of patients were retrospectively constituted based on their clinical response (good responders, n=7; and poor responders, n=3). As well as clinical findings, immunological reconstitution through autologous HSCT was assessed by fluorescence-activated cell sorter analysis, quantification of signal joint T cell receptor rearrangement excision circles (sjTREC), reflecting the thymic function, and foxp3, a key gene of regulatory T cells, mRNA levels.
RESULTS
Patients' clinical and immunological findings were similar between good and poor responders, or CD34-purified and unpurified groups at inclusion. The sjTREC values were significantly suppressed at 3 months after autologous HSCT in good responders compared with poor responders (p=0.0152). Reconstitution of CD4+CD45RO- naive T cells was delayed in good responders compared with poor responders. The phenotype of other lymphocytes, cytokine production in T cells, and foxp3 gene expression levels after autologous HSCT did not correlate with clinical response in good or poor responders. Clinical and immunological findings after autologous HSCT were similar between CD34-purified and unpurified groups.
CONCLUSION
Our results suggest that immunosuppression intensity, sufficient to induce transient suppression of thymic function, is attributable to the feasible clinical response in patients with SSc treated with autologous HSCT. Appropriate monitoring of sjTREC values may predict clinical benefits in transplanted SSc patients after autologous HSCT.
目的
分析自体造血干细胞移植(HSCT)治疗系统性硬化症(SSc)患者的临床获益与免疫变化之间的关系。
方法
10例SSc患者接受大剂量环磷酰胺治疗,随后分别输注高度纯化的CD34+细胞(n = 5)或未纯化的移植物(n = 5)。根据临床反应将两组患者进行回顾性分组(反应良好者,n = 7;反应不佳者,n = 3)。除临床检查结果外,还通过荧光激活细胞分选分析、反映胸腺功能的信号接头T细胞受体重排切除环(sjTREC)定量分析以及调节性T细胞的关键基因foxp3的mRNA水平,评估自体HSCT后的免疫重建情况。
结果
在纳入时,反应良好者与反应不佳者之间,或CD34纯化组与未纯化组之间,患者的临床和免疫检查结果相似。与反应不佳者相比,反应良好者在自体HSCT后3个月时sjTREC值显著降低(p = 0.0152)。与反应不佳者相比,反应良好者中CD4+CD45RO-初始T细胞的重建延迟。自体HSCT后其他淋巴细胞的表型、T细胞中的细胞因子产生以及foxp3基因表达水平与反应良好或不佳者的临床反应均无相关性。CD34纯化组与未纯化组自体HSCT后的临床和免疫检查结果相似。
结论
我们的结果表明,足以诱导胸腺功能短暂抑制的免疫抑制强度,是自体HSCT治疗SSc患者获得可行临床反应的原因。对sjTREC值进行适当监测可能有助于预测自体HSCT后移植SSc患者的临床获益。
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