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Combinations of TLR Ligands: A Promising Approach in Cancer Immunotherapy

机译:TLR配体的组合:癌症免疫治疗中的有前途的方法。

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Toll-like receptors (TLRs), a family of pattern recognition receptors recognizing molecules expressed by pathogens, are typically expressed by immune cells. However, several recent studies revealed functional TLR expression also on tumor cells. Their expression is a two-sided coin for tumor cells. Not only tumor-promoting effects of TLR ligands are described but also direct oncopathic and immunostimulatory effects. To clarify TLRs’ role in colorectal cancer (CRC), we tested the impact of the TLR ligands LPS, Poly IC, R848, and Taxol on primary human CRC cell lines (HROC40, HROC60, and HROC69) in vitro and in vivo (CT26). Taxol, not only a potent tumor-apoptosis-inducing, but also TLR4-activating chemotherapeutic compound, inhibited growth and viability of all cell lines, whereas the remaining TLR ligands had only marginal effects (R848 > LPS > Poly IC). Combinations of the substances here did not improve the results, whereas antitumoral effects were dramatically boosted when human lymphocytes were added. Here, combining the TLR ligands often diminished antitumoral effects. In vivo, best tumor growth control was achieved by the combination of Taxol and R848. However, when combined with LPS, Taxol accelerated tumor growth. These data generally prove the potential of TLR ligands to control tumor growth and activate immune cells, but they also demonstrate the importance of choosing the right combinations.
机译:Toll样受体(TLR)是识别病原体表达的分子的模式识别受体家族,通常由免疫细胞表达。但是,最近的一些研究表明,肿瘤细胞上也有功能性TLR表达。它们的表达是肿瘤细胞的两面硬币。不仅描述了TLR配体的肿瘤促进作用,而且还描​​述了直接的癌性和免疫刺激作用。为了阐明TLR在结直肠癌(CRC)中的作用,我们在体外和体内(CT26)测试了TLR配体LPS,Poly IC,R848和紫杉醇对人类主要CRC细胞系(HROC40,HROC60和HROC69)的影响)。紫杉酚不仅能有效诱导肿瘤细胞凋亡,而且还能激活TLR4的化学治疗化合物抑制所有细胞系的生长和活力,而其余的TLR配体仅具有边际效应(R848> LPS> Poly IC)。这里的物质组合并不能改善结果,而当添加人淋巴细胞时,抗肿瘤作用会大大增强。在这里,结合TLR配体经常减少抗肿瘤作用。在体内,紫杉醇和R848的组合可实现最佳的肿瘤生长控制。但是,当与LPS结合使用时,紫杉醇可促进肿瘤生长。这些数据通常证明了TLR配体控制肿瘤生长和激活免疫细胞的潜力,但它们也表明选择正确组合的重要性。

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