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Humoral response against heat shock proteins and other mycobacterial antigens after intravesical treatment with bacille Calmette–Guérin (BCG) in patients with superficial bladder cancer

机译:浅表性膀胱癌膀胱内注射杆菌卡介苗(BCG)后对热休克蛋白和其他分枝杆菌抗原的体液反应

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摘要

Few studies have analysed the antibody response during intravesical BCG immunotherapy for superficial bladder cancer. We have examined the evolution in serum antibody response against several heat shock proteins (hsp), including the recombinant mycobacterial hsp65 and the native protein P64 from BCG, GroEL from Escherichia coli (hsp60 family), recombinant mycobacterial hsp70 and the E. coli DnaK (hsp70 family), against purified protein derivative of tuberculin (PPD) and the AG85 complex of Mycobacterium bovis BCG, as well as against tetanus toxoid in 42 patients with a superficial bladder tumour, 28 treated with six intravesical BCG instillations and 14 patients used as controls. We also analysed the lymphoproliferative response of peripheral blood mononuclear cells against PPD in this population. Data of antibody responses at 6 weeks post BCG were available in all 28 patients, and at 4 month follow up in 17 patients. All patients who demonstrated a significant increase in IgG antibodies against PPD at 4 months follow up had a significant increase already at 6 weeks of follow up. In contrast, IgG antibodies against hsp increased significantly from 6 weeks to 4 months post-treatment. A significant increase in IgG antibodies against PPD, hsp65, P64, GroEL, and hsp70 at 4 months follow up was observed in 10/17, 8/17, 10/17, 4/17 and 8/17 patients. Native P64 protein elicited a higher antibody response than recombinant mycobacterial hsp65. No increase in antibody response was observed against Dnak from E. coli, against AG85 or tetanus toxoid after BCG therapy. An increase in IgG antibodies against P64 at 4 months follow up compared with pretreatment values was found to be a significant predictor of tumour recurrence (P< 0.01). Further studies with a larger number of patients are needed to confirm the value of the antibody response against P64 as a clinical independent prognostic factor.
机译:很少有研究分析浅表膀胱癌的膀胱内BCG免疫治疗期间的抗体反应。我们已经检查了针对几种热休克蛋白(hsp)的血清抗体反应的演变,包括重组分枝杆菌hsp65和BCG的天然蛋白P64,大肠杆菌(hsp60家族)的GroEL,重组分枝杆菌hsp70和大肠杆菌DnaK( hsp70家族),针对42例浅表性膀胱肿瘤患者,针对结核菌素(PPD)和牛分枝杆菌BCG的AG85复合物的纯化蛋白衍生物,针对破伤风类毒素的治疗,对28例患者进行了6次膀胱BCG灌注治疗,其中14例作为对照。我们还分析了该人群中外周血单核细胞对PPD的淋巴增生反应。 BCG术后6周的抗体应答数据在所有28例患者中可用,在4个月的随访中有17例患者。所有在随访4个月时显示抗PPD IgG抗体显着增加的患者在随访6周时已经显着增加。相反,抗hsp的IgG抗体从治疗后6周到4个月显着增加。在10 / 17、8 / 17、10 / 17、4 / 17和8/17患者中,随访4个月时,针对PPD,hsp65,P64,GroEL和hsp70的IgG抗体显着增加。天然P64蛋白比重组分枝杆菌hsp65引起更高的抗体反应。在BCG治疗后,未观察到针对大肠杆菌的Dnak,针对AG85或破伤风类毒素的抗体反应增加。与治疗前的值相比,在4个月的随访中抗P64的IgG抗体的增加被发现是肿瘤复发的重要预测指标(P <0.01)。需要对更多患者进行进一步研究,以确认针对P64的抗体应答作为临床独立预后因素的价值。

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