Moschos Stergios J, Edington Howard D, Land Stephanie R, Rao Uma N, Jukic Drazen, Shipe-Spotloe Janice, Kirkwood John M
Melanoma and Skin Cancer Program, University of Pittsburgh School of Medicine, Pittsburgh, PA, USA.
J Clin Oncol. 2006 Jul 1;24(19):3164-71. doi: 10.1200/JCO.2005.05.2498.
Adjuvant high-dose interferon-alfa-2b (HDI) improves disease-free and overall survival in patients with high-risk melanoma. However, its mechanism of action is largely unknown. Therefore, HDI was investigated in the neoadjuvant setting to assess clinical and pathologic responses after 4 weeks of HDI and to perform immunohistochemical evaluation of immune cell subsets and melanoma-associated antigens.
Patients with palpable regional lymph node metastases from melanoma (American Joint Committee on Cancer stage IIIB-C) underwent surgical biopsy at study entry and then received standard intravenous HDI (20 million units/m2, 5 days per week) for 4 weeks followed by complete lymphadenectomy and standard maintenance subcutaneous HDI (10 million units/m2 3 times per week) for 48 weeks. Biopsy samples were obtained before and after intravenous HDI and subjected to immunohistochemical analysis as well as routine pathologic study.
Twenty patients were enrolled, and biopsy samples were informative for 17. Eleven patients (55%) demonstrated objective clinical response, and 3 patients (15%) had complete pathologic response. At a median follow-up of 18.5 months (range, 7 months to 50 months) 10 patients had no evidence of recurrent disease. Clinical responders had significantly greater increases in endotumoral CD11c+ and CD3+ cells and significantly greater decreases in endotumoral CD83+ cells compared with nonresponders. No changes in the expression of melanoma-associated lineage antigens, tumor cell proliferation, angiogenesis, or apoptosis were evident.
Neoadjuvant HDI is highly effective for the treatment of palpable stage IIIB-C melanoma, and the findings of this study implicate an indirect immunomodulatory mechanism rather than a direct antitumor mechanism.
辅助性大剂量干扰素-α-2b(HDI)可改善高危黑色素瘤患者的无病生存期和总生存期。然而,其作用机制尚不清楚。因此,在新辅助治疗中对HDI进行研究,以评估HDI治疗4周后的临床和病理反应,并对免疫细胞亚群和黑色素瘤相关抗原进行免疫组化评估。
有可触及的黑色素瘤区域淋巴结转移的患者(美国癌症联合委员会III B - C期)在研究开始时接受手术活检,然后接受标准静脉注射HDI(2000万单位/m²,每周5天),持续4周,随后进行根治性淋巴结清扫,并接受标准维持性皮下注射HDI(1000万单位/m²,每周3次),持续48周。在静脉注射HDI前后获取活检样本,进行免疫组化分析以及常规病理研究。
纳入20例患者,17例患者的活检样本提供了有效信息。11例患者(55%)表现出客观临床反应,3例患者(15%)有完全病理反应。在中位随访18.5个月(范围7个月至50个月)时,10例患者无疾病复发证据。与无反应者相比,临床反应者肿瘤内CD11c⁺和CD3⁺细胞显著增加,肿瘤内CD83⁺细胞显著减少。黑色素瘤相关谱系抗原的表达、肿瘤细胞增殖、血管生成或凋亡均无明显变化。
新辅助HDI对可触及的IIIB - C期黑色素瘤治疗非常有效,本研究结果提示其作用机制为间接免疫调节机制而非直接抗肿瘤机制。
