淋巴周围白细胞介素-2治疗口腔和口咽鳞状细胞癌:临床和病理相关性。

A De Stefani, G Valente, G Forni, W Lerda, R Ragona, G Cortesina
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引用次数: 33

摘要

我们描述了60例口腔或口咽部T2-4、N0-3、M0鳞状细胞癌(SCC)患者的临床和组织学表现之间的相关性,这些患者参加了一项随机试验,以评估当淋巴周围注射重组白细胞介素-2 (il -2)联合常规手术和放疗时,无病间隔和生存期是否延长。29例患者仅接受手术治疗(对照组)。另外31名患者在手术前10天每天接受两次2500 U il -2注射,一次在肿瘤同一侧乳突附近,另一次在下巴下方,并在手术后4周(或必要时进行放疗)开始1年的时间里,每月在未手术一侧注射一次il -2,以提高免疫系统水平并延缓复发。他们的手术标本显示明显更大的炎症反应,更大的坏死区域和更严重的硬化。炎性肿瘤浸润由嗜酸性粒细胞、浆细胞、CD25+和人白细胞抗原(HLA)-DR+淋巴细胞组成。然而,在坏死强度、嗜酸性粒细胞浸润、DR+细胞数量和临床结果方面没有明显的相关性。相比之下,CD25+细胞与更长的无病生存期之间的相关性表明,诱导t细胞反应性,也许是特异性免疫,是il -2诱导的抗肿瘤反应性的唯一重要方面。
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Treatment of oral cavity and oropharynx squamous cell carcinoma with perilymphatic interleukin-2: clinical and pathologic correlations.

We describe the correlations between the clinical and histologic findings in an initial series of 60 patients with T2-4, N0-3, M0 squamous cell carcinoma (SCC) of the oral cavity or oropharynx enrolled in a randomized trial set up to evaluate whether the disease-free interval and survival are extended when perilymphatic injections of recombinant interleukin-2 (rIL-2) are combined with routine surgery and radiotherapy. Twenty-nine patients were operated on only (controls). The other 31 received two daily injections of 2,500 U rIL-2, one near the mastoid process on the same side as the tumor and the other under the chin, for 10 days before surgery, and further injections on the nonoperated-on side on a monthly basis for 1 year starting 4 weeks after surgery (or radiotherapy, where necessary) in an effort to upregulate the immune system and delay recurrence. Their surgical specimens displayed a significantly greater inflammatory reaction, larger areas of necrosis, and more intense sclerosis. The inflammatory tumor infiltration consisted of eosinophils, plasma cells, and CD25+ and human leukocyte antigen (HLA)-DR+ lymphocytes. However, no correlations were apparent with regard to the intensity of necrosis, eosinophil infiltration, and the number of DR+ cells and the clinical outcome. By contrast, the correlation between CD25+ cells and a significantly longer disease-free survival suggests that induction of T-cell reactivity, and perhaps specific immunity, is the only important aspect of rIL-2-induced antitumor reactivity.

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