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Diagnostic value of inflammatory cell infiltrates tumor stroma percentage and disease-free survival in patients with colorectal cancer

机译:炎症细胞浸润肿瘤基质百分比和无病生存对大肠癌的诊断价值

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摘要

The anticancer immune defense mechanism involves humoral and cellular responses. The main effector mechanisms of antitumor responses involve the following: the activity of cytotoxic T cells; the activation of macrophages and neutrophils; the activity of cytokines secreted by T cells; and natural killer cell activity. Selected cell populations are responsible for the stimulation or suppression of the immune system against tumor cells. Therefore, the aim of the present study was to evaluate the location, extent and composition of the cellular inflammatory infiltration of tumors in patients with colorectal cancer (CRC). In addition, the correlation between cellular inflammatory infiltration, and anatomoclinical and histopathological features of patients was evaluated. The study involved 160 patients diagnosed with primary operable CRC. The local inflammatory infiltrate was assessed in the invasive front and center of the tumor using light microscopy with hematoxylin and eosin (H&E) staining, according to the Klintrup-Makinen criteria, tumor stroma percentage, and Glasgow microenvironment score. The inflammatory infiltrate in the invasive front of the tumor was correlated with gender (P=0.018), the invasion of blood vessels (P=0.020) and lymph vessels (P=0.038), the presence of tumor-infiltrating lymphocytes in the invasive front (P=0.033) and center (P<0.001) of the tumor, fibrosis (P<0.001), and the degree of desmoplasmic stroma (P=0.004). In contrast, inflammatory infiltration in the center of the tumor was associated with the tumor node metastasis stage (P=0.012), Dukes' stage (P=0.009), primary tumor stage (P=0.036), lymph node status (P=0.005), number of lymph nodes (P=0.006), invasion of lymph node pouches (P=0.021), size of lymph node metastasis (P=0.025) and the degree of desmoplasmic stroma (P=0.002). The low-group, who demonstrated an absent or weak inflammatory cell infiltrate in the invasive front of the tumor, had a statistically significant shorter disease-free survival (DFS) time (P=0.004). Inflammatory cell infiltrate in the invasive front was identified as an independent predictive factor in CRC (P=0.041). In conclusion, the degree of inflammatory cell infiltration in the invasive front of the primary tumor significantly affects various variables that determine disease progression and DFS rates of patients with CRC. Furthermore, the routine histopathological assessment of this parameter in tissue stained with H&E may have potential prognostic value.
机译:抗癌免疫防御机制涉及体液和细胞反应。抗肿瘤反应的主要效应机制涉及以下方面:细胞毒性T细胞的活性;巨噬细胞和嗜中性粒细胞的活化; T细胞分泌的细胞因子的活性;和自然杀伤细胞活性。选择的细胞群负责刺激或抑制针对肿瘤细胞的免疫系统。因此,本研究的目的是评估结直肠癌(CRC)患者肿瘤细胞炎性浸润的位置,程度和组成。此外,还评估了细胞炎性浸润与患者的解剖学和组织病理学特征之间的相关性。该研究涉及160名被诊断患有原发性可操作性CRC的患者。根据Klintrup-Makinen标准,肿瘤基质百分率和格拉斯哥微环境评分,使用苏木精和曙红(H&E)染色,使用光学显微镜对肿瘤的浸润前部和中心进行局部炎症浸润评估。肿瘤浸润前部的炎性浸润与性别(P = 0.018),血管浸润(P = 0.020)和淋巴管(P = 0.038),浸润前部肿瘤浸润淋巴细胞的存在有关。 (P = 0.033)和肿瘤中心(P <0.001),纤维化(P <0.001)和非质膜基质程度(P = 0.004)。相比之下,肿瘤中心的炎性浸润与肿瘤淋巴结转移阶段(P = 0.012),Dukes'阶段(P = 0.009),原发肿瘤阶段(P = 0.036),淋巴结状态(P = 0.005)相关。 ),淋巴结数目(P = 0.006),淋巴结袋浸润(P = 0.021),淋巴结转移的大小(P = 0.025)和非质性基质的程度(P = 0.002)。这个低水平的人群在肿瘤的浸润前线中没有炎性细胞浸润或浸润较弱,在统计学上显着缩短了无病生存期(DFS)(P = 0.004)。浸润前区的炎性细胞浸润被确定为CRC的独立预测因素(P = 0.041)。总之,在原发性肿瘤的浸润前部中炎性细胞浸润的程度会显着影响决定CRC患者疾病进展和DFS率的各种变量。此外,在H&E染色的组织中对该参数进行常规组织病理学评估可能具有潜在的预后价值。

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