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小鼠乳腺肿瘤微环境中种子和土壤依赖性差异决定抗PD-L1 IgG递送及治疗效果。

Seed- and Soil-Dependent Differences in Murine Breast Tumor Microenvironments Dictate Anti-PD-L1 IgG Delivery and Therapeutic Efficacy.

作者信息

Liu Yan Ting, Goel Shreya, Kai Megumi, Moran Guerrero Jose Alberto, Nguyen Thao, Mai Junhua, Shen Haifa, Ziemys Arturas, Yokoi Kenji

机构信息

Houston Methodist Research Institute, Houston, TX 77030, USA.

出版信息

Pharmaceutics. 2021 Apr 10;13(4):530. doi: 10.3390/pharmaceutics13040530.

Abstract

We sought to determine if Stephen Paget's "seed and soil" hypothesis of organ-preference patterns of cancer metastasis can explain the development of heterogeneity in a tumor microenvironment (TME) as well as immunotherapeutic delivery and efficacy. We established single-cell-derived clones (clones 1 and 16) from parental 4T1 murine breast cancer cells to create orthotopic primary and liver metastasis models to deconvolute polyclonal complexity cancer cells and the difference in TME-derived heterogeneities. Tumor-bearing mice were treated with anti-PD-L1 IgG or a control antibody, and immunofluorescent imaging and quantification were then performed to evaluate the therapeutic efficacy on tumor growth, the delivery of therapy to tumors, the development of blood vessels, the expression of PD-L1, the accumulation of immune cells, and the amount of coagulation inside tumors. The quantification showed an inverse correlation between the amount of delivered therapy and therapeutic efficacy in parental-cell-derived tumors. In contrast, tumors originating from clone 16 cells accumulated a significantly greater amount of therapy and responded better than clone-1-derived tumors. This difference was greater when tumors grew in the liver than the primary site. A similar trend was found in PD-L1 expression and immune cell accumulation. However, the change in the number of blood vessels was not significant. In addition, the amount of coagulation was more abundant in clone-1-derived tumors when compared to others. Thus, our findings reconfirmed the seed- and soil-dependent differences in PD-L1 expression, therapeutic delivery, immune cell accumulation, and tumor coagulation, which can constitute a heterogeneous delivery and response of immunotherapy in polyclonal tumors growing in different organs.

摘要

我们试图确定斯蒂芬·佩吉特(Stephen Paget)关于癌症转移器官偏好模式的“种子与土壤”假说是否能够解释肿瘤微环境(TME)中异质性的发展以及免疫治疗的递送和疗效。我们从亲本4T1小鼠乳腺癌细胞中建立了单细胞衍生克隆(克隆1和克隆16),以创建原位原发性和肝转移模型,从而解析多克隆复杂性癌细胞以及TME衍生异质性的差异。对荷瘤小鼠用抗PD-L1 IgG或对照抗体进行治疗,然后进行免疫荧光成像和定量分析,以评估对肿瘤生长的治疗效果、治疗药物向肿瘤的递送、血管生成、PD-L1的表达、免疫细胞的积累以及肿瘤内部的凝血量。定量分析显示,亲本细胞衍生肿瘤中递送的治疗药物量与治疗效果呈负相关。相比之下,源自克隆16细胞的肿瘤积累的治疗药物量显著更多,且比源自克隆1的肿瘤反应更好。当肿瘤在肝脏中生长时,这种差异比在原发部位时更大。在PD-L1表达和免疫细胞积累方面也发现了类似趋势。然而,血管数量的变化并不显著。此外,与其他肿瘤相比,源自克隆1的肿瘤中的凝血量更为丰富。因此,我们的研究结果再次证实了在PD-L1表达、治疗药物递送、免疫细胞积累和肿瘤凝血方面存在种子和土壤依赖性差异,这可能构成在不同器官中生长的多克隆肿瘤中免疫治疗的异质性递送和反应。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/1cfb/8069710/bfe0a4fc1f2e/pharmaceutics-13-00530-g001.jpg

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