免疫疗法治疗持续性生殖器疣的随机试验。
A randomized trial of immunotherapy for persistent genital warts.
机构信息
Princess Alexandra Sexual Health, Princess Alexandra Hospital, Brisbane, QLD, Australia.
出版信息
Hum Vaccin Immunother. 2012 May;8(5):623-9. doi: 10.4161/hv.19319. Epub 2012 May 1.
AIM
To determine whether immunotherapy with HPV6 L1 virus like particles (VLPs) without adjuvant (VLP immunotherapy) reduces recurrence of genital warts following destructive therapy.
TRIAL DESIGN
A randomized placebo controlled blinded study of treatment of recurrent genital warts amenable to destructive therapy, conducted independently in Australia and China.
METHODS
Patients received conventional destructive therapy of all evident warts together with intramuscular administration of 1 µg, 5 µg or 25 µg of VLP immunotherapy, or of placebo immunotherapy (0.9% NaCl), as immunotherapy at week 0 and week 4. Primary outcome, assessed at week 8, was recurrence of visible warts.
RESULTS
Of 33 protocol compliant Brisbane recipients of placebo immunotherapy, 11 were disease free at two months, and a further 9 demonstrated reduction of > 50% in total wart area. Wart area reduction following destructive treatment correlated with prior duration of disease. Among 102 protocol compliant Brisbane recipients of VLP immunotherapy, disease reduction was significantly greater than among the placebo immunotherapy (50% ± s.e.m. 7%) recipients for subjects receiving 5 µg or 25 µg of VLP immunotherapy/dose (71% ± s.e.m. 7%) but not for those receiving 1 µg VLP immunotherapy/dose (42% ± 7%). Of 52 protocol compliant placebo immunotherapy recipients in Wenzhou, 37 were disease free at two months, and a further 8 had > 50% disease reduction. Prior disease duration was much shorter in Wenzhou subject (8.1 ± 1.1 mo) than in Brisbane subjects (53.7 ± 5.5 mo). No significant reduction in mean wart area was observed for the 168 Wenzhou protocol compliant subjects who also received VLP immunotherapy.
CONCLUSIONS
This study confirms the findings in a previous open label trial that administration of VLP immunotherapy may assist in clearance of recurrent genital warts in patients for whom destructive therapy is unsuccessful and that unsuccessful destructive therapy is more common with increasing prior disease duration.
目的
确定是否在没有佐剂的情况下使用 HPV6 L1 病毒样颗粒(VLPs)进行免疫疗法(VLP 免疫疗法)可以减少破坏性治疗后生殖器疣的复发。
试验设计
这是一项在澳大利亚和中国独立进行的针对可接受破坏性治疗的复发性生殖器疣的随机安慰剂对照双盲研究。
方法
患者接受所有可见疣的常规破坏性治疗,并在第 0 周和第 4 周接受 1μg、5μg 或 25μg 的 VLP 免疫疗法或安慰剂免疫疗法(0.9%NaCl)的肌肉内给药作为免疫疗法。主要结局评估于第 8 周,为可见疣的复发。
结果
在接受安慰剂免疫疗法的 33 名符合方案的布里斯班患者中,11 名在两个月时无病,另有 9 名患者的总疣面积减少了>50%。破坏性治疗后的疣面积减少与疾病的先前持续时间相关。在 102 名符合方案的布里斯班 VLP 免疫疗法接受者中,与接受安慰剂免疫疗法的患者(50%±s.e.m.7%)相比,接受 5μg 或 25μg VLP 免疫疗法/剂量(71%±s.e.m.7%)的患者疾病减轻明显更大,但接受 1μg VLP 免疫疗法/剂量的患者(42%±7%)则不然。在接受安慰剂免疫疗法的 52 名符合方案的温州患者中,37 名在两个月时无病,另有 8 名患者的疾病减少了>50%。温州患者的疾病持续时间明显短于布里斯班患者(8.1±1.1 个月)。168 名接受 VLP 免疫疗法的温州符合方案患者的平均疣面积也没有明显减少。
结论
本研究证实了先前开放标签试验的结果,即给予 VLP 免疫疗法可能有助于清除对破坏性治疗不成功的复发性生殖器疣患者的疣,且破坏性治疗的成功率随着先前疾病持续时间的增加而降低。
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