Tímár József, Forster-Horváth C, Lukits J, Döme B, Ladányi A, Remenár E, Kásler M, Bencsik M, Répássy G, Szabó G, Velich N, Suba Z, Elõ J, Balatoni Z, Bajtai A, Chretien P, Talor Eyal
National Institute of Oncology, Semmelweis University, Budapest, Hungary.
Laryngoscope. 2003 Dec;113(12):2206-17. doi: 10.1097/00005537-200312000-00031.
OBJECTIVES/HYPOTHESIS: The main objective of this study was to investigate the effect of the administration of a novel immunoadjuvant, leukocyte interleukin injection, as part of an immuno-augmenting treatment regimen on the peritumoral and intratumoral subpopulations of the tumor infiltrating mononuclear cells and on the epithelial and stromal components, when administered to patients with advanced primary oral squamous cell carcinoma classified as T2-3N0-2M0, as compared with disease-matched control patients (not treated with leukocyte interleukin injection).
Multicenter Phase I/II clinical trial. Fifty-four patients from four clinical centers were included in the dose-escalating study (27 in each group [leukocyte interleukin injection-treated and control groups]). Cumulative leukocyte inter-leukin injection doses were 2400, 4800, and 8000 IU (as interleukin-2 equivalent).
Paraffin-embedded tumor samples obtained at surgical resection of the residual tumor (between days 21 and 28 after treatment initiation) were used. Histological analysis, necrosis evaluation, and American Joint Committee on Cancer grading were performed from H&E-stained sections. Immunohistochemical analysis was performed on three different tumor regions (surface, zone 1; center, zone 2; and tumor-stroma interface, zone 3). Trichrome staining was used to evaluate connective tissue, and morphometric measurements were made using ImagePro analysis software. Cell cycling was determined by the use of Ki-67 marker.
Leukocyte interleukin injection treatment induced a shift from stromal infiltrating T cells toward intraepithelial T cells and posted a significant (P <.05) increase in intraepithelial CD3-positive T cells independent of the leukocyte interleukin injection dose, whereas the increase in CD25 (interleukin-2 receptor alpha [IL-2Ralpha])-positive lymphoid cells was significant only at the lowest leukocyte interleukin injection dose (P <.05). Furthermore, both low- and medium-dose leukocyte interleukin injection treatment induced a significant (P <.05) increase in the number of cycling tumor cells, as compared with control values.
The results could be highly beneficial for patients with oral squamous cell carcinoma. First, leukocyte interleukin injection treatment induces T-cell migration into cancer nests and, second, noncycling cancer cells may enter cell cycling on administration of leukocyte interleukin injection. This latter effect may modulate the susceptibility of cancer cells to radiation therapy and chemotherapy. The findings may indicate a need to re-evaluate the way in which follow-up treatment (with radiation therapy and chemotherapy) of patients with head and neck cancer is currently approached.
目的/假设:本研究的主要目的是,调查一种新型免疫佐剂白细胞介素注射液作为免疫增强治疗方案的一部分,在给予T2 - 3N0 - 2M0期晚期原发性口腔鳞状细胞癌患者时,对肿瘤浸润单核细胞的瘤周和瘤内亚群以及上皮和基质成分的影响,并与疾病匹配的对照患者(未接受白细胞介素注射液治疗)进行比较。
多中心I/II期临床试验。来自四个临床中心的54名患者纳入剂量递增研究(每组27名[白细胞介素注射液治疗组和对照组])。白细胞介素注射液的累积剂量为2400、4800和8000 IU(以白细胞介素-2等效剂量计)。
使用在手术切除残留肿瘤时(治疗开始后21至28天之间)获取的石蜡包埋肿瘤样本。对苏木精-伊红染色切片进行组织学分析、坏死评估和美国癌症联合委员会分级。对三个不同肿瘤区域(表面,区域1;中心,区域2;肿瘤-基质界面,区域3)进行免疫组织化学分析。使用三色染色评估结缔组织,并使用ImagePro分析软件进行形态测量。通过使用Ki-67标记物确定细胞周期。
白细胞介素注射液治疗导致基质浸润T细胞向上皮内T细胞转变,且上皮内CD3阳性T细胞显著增加(P <.05),与白细胞介素注射液剂量无关,而CD25(白细胞介素-2受体α[IL-2Rα])阳性淋巴细胞仅在最低白细胞介素注射液剂量时显著增加(P <.05)。此外,与对照值相比,低剂量和中剂量白细胞介素注射液治疗均导致循环肿瘤细胞数量显著增加(P <.05)。
这些结果可能对口腔鳞状细胞癌患者非常有益。首先,白细胞介素注射液治疗诱导T细胞迁移至癌巢,其次,给予白细胞介素注射液后非循环癌细胞可能进入细胞周期。后一种效应可能调节癌细胞对放射治疗和化疗的敏感性。这些发现可能表明需要重新评估目前对头颈部癌患者进行后续治疗(放射治疗和化疗)的方式。
