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Tumor infiltrating lymphocytes in ovarian cancer

机译:卵巢癌中的肿瘤浸润淋巴细胞

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The accumulation of tumor infiltrating lymphocytes (TILs) in ovarian cancer is prognostic for increased survival while increases in immunosuppressive regulatory T-cells (Tregs) are associated with poor outcomes. Approaches that bolster tumor-reactive TILs may limit tumor progression. However, identifying tumor-reactive TILs in ovarian cancer has been challenging, though adoptive TIL therapy in patients has been encouraging. Other forms of TIL immunomodulation remain under investigation including Treg depletion, antibody-based checkpoint modification, activation and amplification using dendritic cells, antigen presenting cells or IL-2 cytokine culture, adjuvant cytokine injections, and gene-engineered T-cells. Many approaches to TIL manipulation inhibit ovarian cancer progression in preclinical or clinical studies as monotherapy. Here, we review the impact of TILs in ovarian cancer and attempts to mobilize TILs to halt tumor progression. We conclude that effective TIL therapy for ovarian cancer is at the brink of translation and optimal TIL activity may require combined methodologies to deliver clinically-relevant treatment.
机译:卵巢癌中肿瘤浸润淋巴细胞(TILs)的积累预示着生存率的提高,而免疫抑制性T细胞(Tregs)的增加与不良预后相关。支持肿瘤反应性TIL的方法可能会限制肿瘤的进展。然而,尽管在患者中采用过继性TIL治疗一直令人鼓舞,但在卵巢癌中鉴定肿瘤反应性TIL一直具有挑战性。 TIL免疫调节的其他形式仍在研究中,包括Treg耗竭,基于抗体的检查点修饰,使用树突状细胞,抗原呈递细胞或IL-2细胞因子培养物的活化和扩增,佐剂细胞因子注射和基因工程T细胞。在临床前或临床研究中,作为单一疗法,许多TIL操纵方法都可抑制卵巢癌的进展。在这里,我们回顾了TILs在卵巢癌中的影响,并尝试动员TILs阻止肿瘤的进展。我们得出的结论是,有效的TIL治疗卵巢癌正处于翻译的边缘,最佳的TIL活性可能需要组合的方法来提供临床相关的治疗。

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