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Shift from stochastic to spatially-ordered expression of serine-glycine synthesis enzymes in 3D microtumors

机译:3D微型肿瘤中丝氨酸-甘氨酸合成酶从随机表达到空间有序表达的转变

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摘要

Cell-to-cell differences in protein expression in normal tissues and tumors are a common phenomenon, but the underlying principles that govern this heterogeneity are largely unknown. Here, we show that in monolayer cancer cell-line cultures, the expression of the five metabolic enzymes of serine-glycine synthesis (SGS), including its rate-limiting enzyme, phosphoglycerate dehydrogenase (PHGDH), displays stochastic cell-to-cell variation. By contrast, in cancer cell line-derived three-dimensional (3D) microtumors PHGDH expression is restricted to the outermost part of the microtumors’ outer proliferative cell layer, while the four other SGS enzymes display near uniform expression throughout the microtumor. A mathematical model suggests that metabolic stress in the microtumor core activates factors that restrict PHGDH expression. Thus, intracellular enzyme expression in growing cell ecosystems can shift to spatially ordered patterns in 3D structured environments due to emergent cell-cell communication, with potential implications for the design of effective anti-metabolic cancer therapies.
机译:正常组织和肿瘤中蛋白质表达的细胞间差异是一种普遍现象,但是控制这种异质性的基本原理尚不清楚。在这里,我们显示了在单层癌细胞系培养物中,丝氨酸-甘氨酸合成(SGS)的五个代谢酶(包括其限速酶,磷酸甘油酸脱氢酶(PHGDH))的表达显示出随机的细胞间差异。相比之下,在源自癌细胞系的三维(3D)微肿瘤中,PHGDH表达仅限于微肿瘤外部增生细胞层的最外层,而其他四种SGS酶在整个微肿瘤中均表现出近乎均匀的表达。数学模型表明,微肿瘤核心中的代谢应激激活了限制PHGDH表达的因子。因此,由于新兴的细胞间通讯,生长中的细胞生态系统中的细胞内酶表达可能会转变为3D结构化环境中的空间有序模式,这对有效的抗代谢性癌症疗法的设计具有潜在的影响。

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