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干细胞分化阶段因素及其在触发癌症发展过程中对称性破缺过程中的作用:一种将癌细胞重编程为健康表型的量子场论模型。

Stem Cell Differentiation Stage Factors and their Role in Triggering Symmetry Breaking Processes during Cancer Development: A Quantum Field Theory Model for Reprogramming Cancer Cells to Healthy Phenotypes.

机构信息

Scientific Institute of Research and Care Multimedica, Via Milanese 300 Sesto S. G., Milano, Italy.

Associazione Medicina e Complessita, Trieste, Italy.

出版信息

Curr Med Chem. 2019;26(6):988-1001. doi: 10.2174/0929867324666170920142609.

Abstract

A long history of research has pursued the use of embryonic factors isolated during cell differentiation processes for the express purpose of transforming cancer cells back to healthy phenotypes. Recent results have clarified that the substances present at different stages of cell differentiation-which we call stem cell differentiation stage factors (SCDSFs)-are proteins with low molecular weight and nucleic acids that regulate genomic expression. The present review summarizes how these substances, taken at different stages of cellular maturation, are able to retard proliferation of many human tumor cell lines and thereby reprogram cancer cells to healthy phenotypes. The model presented here is a quantum field theory (QFT) model in which SCDSFs are able to trigger symmetry breaking processes during cancer development. These symmetry breaking processes, which lie at the root of many phenomena in elementary particle physics and condensed matter physics, govern the phase transitions of totipotent cells to higher degrees of diversity and order, resulting in cell differentiation. In cancers, which share many genomic and metabolic similarities with embryonic stem cells, stimulated redifferentiation often signifies the phenotypic reversion back to health and nonproliferation. In addition to acting on key components of the cellular cycle, SCDSFs are able to reprogram cancer cells by delicately influencing the cancer microenvironment, modulating the electrochemistry and thus the collective electrodynamic behaviors between dipole networks in biomacromolecules and the interstitial water field. Coherent effects in biological water, which are derived from a dissipative QFT framework, may offer new diagnostic and therapeutic targets at a systemic level, before tumor instantiation occurs in specific tissues or organs. Thus, by including the environment as an essential component of our model, we may push the prevailing paradigm of mutation-driven oncogenesis toward a closer description of reality.

摘要

长期以来,研究人员一直致力于利用细胞分化过程中分离出来的胚胎因子,专门将癌细胞转化为健康表型。最近的研究结果表明,细胞分化的不同阶段存在的物质——我们称之为干细胞分化阶段因子(SCDSFs)——是具有低分子量的蛋白质和调节基因组表达的核酸。本综述总结了这些物质在细胞成熟的不同阶段是如何能够抑制许多人类肿瘤细胞系的增殖,从而将癌细胞重新编程为健康表型的。这里提出的模型是一个量子场论(QFT)模型,其中 SCDSFs 能够在癌症发展过程中触发对称破缺过程。这些对称破缺过程是基本粒子物理和凝聚态物理中许多现象的根源,它们控制着全能细胞向更高程度的多样性和秩序的相变,从而导致细胞分化。在癌症中,由于与胚胎干细胞有许多基因组和代谢相似之处,受刺激的再分化通常标志着表型向健康和非增殖的恢复。除了作用于细胞周期的关键成分外,SCDSFs 还能够通过巧妙地影响癌症微环境来重新编程癌细胞,调节电化学,从而调节生物大分子中偶极网络之间和间质水场的集体电动力学行为。源于耗散 QFT 框架的生物水的相干效应可能会在肿瘤在特定组织或器官中发生之前,在系统水平上提供新的诊断和治疗靶点。因此,通过将环境作为我们模型的一个重要组成部分,我们可以将以突变驱动的致癌作用为主导的现有范式推向更接近现实的描述。

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