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首页> 外文期刊>Urologic oncology >Infiltration of CD3+ and CD68+ cells in bladder cancer is subtype specific and affects the outcome of patients with muscle-invasive tumors
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Infiltration of CD3+ and CD68+ cells in bladder cancer is subtype specific and affects the outcome of patients with muscle-invasive tumors

机译:膀胱癌中CD3 +和CD68 +细胞的浸润是亚型特异性的,并会影响肌肉浸润性肿瘤患者的预后

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Objectives: Urothelial carcinoma (UC) aggressiveness is determined by tumor inherent molecular characteristics, such as molecular subtypes, as well as by host reactions directed toward the tumor. Cell types responsible for the host[U+05F3]s response include tumor-infiltrating lymphocytes (TILs) and tumor-associated macrophages (TAMs). The aim of the present investigation was to explore the immunological response in relation to UC molecular subtypes and to evaluate the prognostic effect of TIL and TAM counts in tissue sections from muscle-invasive (MI) tumors. Methods and materials: Tissue microarrays with 296 tumors spanning all pathological stages and grades were analyzed with antibodies for CD3, CD8, FOXP3, CD68, and CD163. Cases were classified into the following molecular subtypes: urobasal, genomically unstable, and squamous cell carcinoma-like using a combination of immunohistochemistry and histology. The Cox regression and Kaplan-Meier analyses were performed with progression-free survival and disease-specific survival as end points. Results: UC molecular subtypes demonstrate different degrees of immunological responses; the urobasal subtype induces a weak response, the genomically unstable subtype induces an intermediate response, and the squamous cell carcinoma-like subtype induces a strong response. These subtype specific responses are independent of tumor stage and include both TILs and TAMs. The presence of infiltrating CD3+ TILs was significantly associated with good prognosis in the MI cases (P0.01). This positive association was modulated by the presence of CD68+ TAMs. The strongest association with poor survival was observed for a high ratio between CD68 and CD3 (P = 7×10-5). Conclusion: UC molecular subtypes induce immunological responses at different levels. A high CD68/CD3 ratio identifies a bad prognosis group among MI UC cases.
机译:目的:尿路上皮癌(UC)的侵袭性取决于肿瘤固有的分子特征,例如分子亚型,以及针对肿瘤的宿主反应。负责宿主[U + 05F3]反应的细胞类型包括肿瘤浸润淋巴细胞(TIL)和肿瘤相关巨噬细胞(TAM)。本研究的目的是探讨与UC分子亚型有关的免疫应答,并评估TIL和TAM计数在肌肉浸润性(MI)肿瘤组织切片中的预后效果。方法和材料:用CD3,CD8,FOXP3,CD68和CD163抗体分析了涵盖所有病理阶段和等级的296个肿瘤的组织微阵列。结合免疫组织化学和组织学方法,将病例分为以下分子亚型:尿路基底型,基因组不稳定型和鳞状细胞癌样。以无进展生存期和疾病特异性生存期为终点,进行Cox回归和Kaplan-Meier分析。结果:UC分子亚型表现出不同程度的免疫反应。尿路基底亚型诱导弱反应,基因组不稳定亚型诱导中等反应,鳞状鳞癌样亚型诱导强反应。这些亚型特异性应答与肿瘤分期无关,包括TIL和TAM。浸润的CD3 + TILs的存在与MI患者的良好预后显着相关(P <0.01)。 CD68 + TAM的存在调节了这种正向关联。 CD68与CD3的比例较高时,观察到与不良存活之间的最强关联(P = 7×10-5)。结论:UC分子亚型在不同水平上诱导免疫反应。高CD68 / CD3比表明MI UC病例中预后不良。

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