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本文引用的文献

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Cancer cells mimic in vivo spatial-temporal cell-cycle phase distribution and chemosensitivity in 3-dimensional Gelfoam® histoculture but not 2-dimensional culture as visualized with real-time FUCCI imaging.通过实时FUCCI成像观察发现,癌细胞在三维明胶海绵组织培养中模拟体内时空细胞周期阶段分布和化学敏感性,但在二维培养中则不然。
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Tumor mechanics and metabolic dysfunction.肿瘤力学与代谢功能障碍
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Tumor-targeting Salmonella typhimurium A1-R decoys quiescent cancer cells to cycle as visualized by FUCCI imaging and become sensitive to chemotherapy.肿瘤靶向性鼠伤寒沙门氏菌A1-R诱使静止癌细胞进入细胞周期,这可通过FUCCI成像观察到,并且使癌细胞对化疗敏感。
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Spatial-temporal FUCCI imaging of each cell in a tumor demonstrates locational dependence of cell cycle dynamics and chemoresponsiveness.肿瘤中每个细胞的时空FUCCI成像显示了细胞周期动力学和化学敏感性的位置依赖性。
Cell Cycle. 2014;13(13):2110-9. doi: 10.4161/cc.29156. Epub 2014 May 8.
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Bacterial delivery of Staphylococcus aureus α-hemolysin causes regression and necrosis in murine tumors.金黄色葡萄球菌α-溶血素的细菌递送可导致小鼠肿瘤消退和坏死。
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Rapid uptake of glucose and lactate, and not hypoxia, induces apoptosis in three-dimensional tumor tissue culture.葡萄糖和乳酸的快速摄取,而非缺氧,在三维肿瘤组织培养中诱导细胞凋亡。
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Lipid A controls the robustness of intratumoral accumulation of attenuated Salmonella in mice.脂 A 控制减毒沙门氏菌在小鼠肿瘤内积累的稳健性。
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Microfluidic technique to measure intratumoral transport and calculate drug efficacy shows that binding is essential for doxorubicin and release hampers Doxil.微流控技术测量肿瘤内转运并计算药物疗效表明,阿霉素的结合是必需的,而释放则会阻碍 Doxil 的作用。
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Motility is critical for effective distribution and accumulation of bacteria in tumor tissue.运动性对于细菌在肿瘤组织中的有效分布和积累至关重要。
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In tumors Salmonella migrate away from vasculature toward the transition zone and induce apoptosis.在肿瘤中,沙门氏菌从血管迁移到过渡区并诱导细胞凋亡。
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工程细菌可检测实体肿瘤细胞团内葡萄糖浓度的空间分布。

Engineered bacteria detect spatial profiles in glucose concentration within solid tumor cell masses.

作者信息

Panteli Jan T, Forbes Neil S

机构信息

Department of Chemical Engineering, University of Massachusetts, 686 North Pleasant Street, Amherst, Massachusetts, 01003.

出版信息

Biotechnol Bioeng. 2016 Nov;113(11):2474-84. doi: 10.1002/bit.26006. Epub 2016 Sep 20.

DOI:10.1002/bit.26006
PMID:27159665
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC5037000/
Abstract

Tumor heterogeneity makes cancer difficult to treat. Many small molecule cancer drugs target rapidly dividing cells on the periphery of tumors but have difficulty in penetrating deep into tumors and are ineffective at treating entire tumors. Targeting both rapidly dividing and slower growing regions of tumors is essential to effectively treat cancer. A cancer drug carrier that penetrates deep into tumors and identifies metabolically activity could supply treatment to those areas based on the local microenvironment. We hypothesized that glucose sensing bacteria could identify sugar gradients in solid tumors. To test this hypothesis, a genetic circuit was designed to trigger expression of a green fluorescent protein (GFP) reporter through the chemotaxis-osmoporin fusion protein, Trz1, a receptor for sensing glucose and ribose sugars. E. coli equipped with the Trz1-GFP expression system, were administered to an in vitro model of a continuously perfused tumor tissue that mimics systemic delivery and clearance of bacteria through a blood vessel adjacent to a solid tumor. The level of GFP expressed, per bacterium, was time independent and indicated the glucose concentration as a function of penetration depth within the microfluidic tumors. The measured glucose concentration, correlated (P-value = 2.6 × 10(-5) ) with tumor cell viability as a function of depth. Mathematical analysis predicted drug delivery by glucose-sensing bacteria would eliminate a higher percentage of the viable tumor cell population than a systemically administered drug. Glucose-sensing bacteria could deliver cancer therapies with increased drug penetration and nutrient-dependent dosing to continuously treat viable regions of cancer tissue that have a higher prevalence for metastatic dissemination. Biotechnol. Bioeng. 2016;113: 2474-2484. © 2016 Wiley Periodicals, Inc.

摘要

肿瘤异质性使得癌症难以治疗。许多小分子抗癌药物靶向肿瘤周边快速分裂的细胞,但难以深入渗透到肿瘤内部,对整个肿瘤的治疗效果不佳。靶向肿瘤快速分裂和生长较慢的区域对于有效治疗癌症至关重要。一种能够深入渗透到肿瘤内部并识别代谢活性的抗癌药物载体,可以根据局部微环境向这些区域提供治疗。我们推测葡萄糖感应细菌能够识别实体瘤中的糖梯度。为了验证这一假设,设计了一个基因回路,通过趋化渗透蛋白融合蛋白Trz1(一种用于感应葡萄糖和核糖糖的受体)来触发绿色荧光蛋白(GFP)报告基因的表达。将配备Trz1-GFP表达系统的大肠杆菌应用于连续灌注肿瘤组织的体外模型,该模型模拟了细菌通过与实体瘤相邻的血管进行全身递送和清除的过程。每个细菌表达的GFP水平与时间无关,并表明葡萄糖浓度是微流控肿瘤内渗透深度的函数。测得的葡萄糖浓度与肿瘤细胞活力随深度的变化相关(P值 = 2.6 × 10(-5))。数学分析预测,与全身给药的药物相比,葡萄糖感应细菌进行药物递送将消除更高比例的存活肿瘤细胞群体。葡萄糖感应细菌可以通过增加药物渗透和营养依赖性给药来递送癌症治疗药物,以持续治疗转移性扩散发生率较高的癌症组织的存活区域。《生物技术与生物工程》2016年;113:2474 - 2484。© 2016威利期刊公司