抗原呈递细胞8015 (Provenge®)在雄激素依赖性生化复发前列腺癌患者中的应用

Garth Beinart , Brian I. Rini , Vivian Weinberg , Eric J. Small
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引用次数: 61

摘要

抗原呈递细胞8015 (APC8015;Provenge®)是一种免疫治疗产品,旨在启动t细胞介导的针对前列腺酸性磷酸酶的免疫应答,前列腺酸性磷酸酶是一种在95%的前列腺癌细胞中过表达的抗原。在I/II期试验中,APC8015在雄激素非依赖性前列腺癌患者中显示出免疫和临床反应。该II期临床试验旨在评估APC8015在生化进展的雄激素依赖性前列腺癌(ADPC)患者中的前列腺特异性抗原(PSA)调节作用。患者和方法纳入了PSA水平升高(0.4-6.0 ng/mL)且既往接受过明确手术或放疗的非转移性复发性疾病患者。治疗包括在第0、2和4周输注APC8015(即3次输注)。在基线和每月测量前列腺特异性抗原,直到疾病进展,定义为基线或最低点PSA值(以低者为准)加倍至≥4 ng/mL或远处转移。结果18例患者中有13例显示PSA倍增时间(PSADT)增加,中位增加62%(治疗前4.9个月vs.治疗后7.9个月;P = 0.09;符号秩检验)。结论治疗耐受性良好。APC8015作为单药免疫疗法用于ADPC和生化进展患者,并没有导致PSA从基线水平下降≥50%,但确实可以调节一些患者的PSADT。为了达到显著的抗肿瘤效果,可能需要进一步操纵宿主免疫。
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Antigen-Presenting Cells 8015 (Provenge®) in Patients with Androgen-Dependent, Biochemically Relapsed Prostate Cancer

Background

Antigen-presenting cells 8015 (APC8015; Provenge®) is an immunotherapeutic product designed to initiate a T-cell–mediated immune response against prostatic acid phosphatase, an antigen overexpressed in 95% of prostate cancer cells. In phase I/II trials, APC8015 has shown immunologic and clinical responses in patients with androgen- independent prostate cancer. This phase II trial was conducted to assess the prostate-specific antigen (PSA)–modulating effects of APC8015 in patients with androgen-dependent prostate cancer (ADPC) with biochemical progression.

Patients and Methods

Patients with nonmetastatic recurrent disease as manifested by increasing PSA levels (0.4-6.0 ng/mL) and who had undergone previous definitive surgical or radiation therapy were enrolled. Therapy consisted of APC8015 infusion on weeks 0, 2, and 4 (ie, 3 infusions). Prostate-specific antigen was measured at baseline and monthly until disease progression, defined as a doubling of the baseline or nadir PSA value (whichever was lower) to ≥ 4 ng/mL or development of distant metastases.

Results

Thirteen of 18 patients demonstrated an increase in PSA doubling time (PSADT), with a median increase of 62% (4.9 months before treatment vs. 7.9 months after treatment; P = 0.09; signed-rank test).

Conclusion

Therapy was well tolerated. APC8015 as single-agent immunotherapy for patients with ADPC and biochemical progression did not result in ≥ 50% decrease in PSA from baseline levels but did appear to modulate PSADT in some patients. Further manipulations of host immunity may be required to achieve a significant antitumor effect.

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