Prelude and premise to the special issue: disruption of homeostasis-induced signaling and crosstalk in the carcinogenesis paradigm “Epistemology of the origin of cancer”

4open Pub Date : 2019-01-01 DOI:10.1051/FOPEN/2019005
B. Brücher, I. Jamall
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引用次数: 2

Abstract

The vast majority of anticancer strategies are symptomatic but in order to achieve some tangible progress, we need to identify the cause(s) of the majority of cancers. There is a kind of zeitgeist that findings in genetics, namely somatic mutations, are reflexively viewed as being causative for carcinogenesis, although some 80% of all cancers are presently termed “sporadic” (i.e., with no proven cause). The observation that one inch of cancerous liver tissue can have more than 100 000 000 mutations and an identical mutation can result in different phenotypes, depending on the environment surrounding that mutation, makes it very unlikely that mutations by themselves are causative of most cancers. 4open debuts its Special Issue series with papers that provide strong evidence that carcinogenesis consists of a 6-step sequence (1) a pathogenic stimulus followed by (2) chronic inflammation from which develops (3) fibrosis with associated remodeling of the extracellular microenvironment, and from these changes a (4) precancerous niche (PCN), a product of fibrosis with remodeling by persistent inflammation develops which triggers the deployment of (5) a chronic stress escape strategy and when this fails to be resolved it results in (6) the normal cell to cancerous cell transition. This Special Issue contains separate papers discussing undervalued ubiquitous proteins, chronic inflammation, eicosanoids, microbiome and morbid obesity, PCN, cell transition, followed by altered signaling induced by Metformin, NF-κB signaling and crosstalk during carcinogenesis, and a brief synopsis. In essence, the available evidence, both in vitro and in vivo, lends credence to the proposition that the majority of cancers occur from a disruption of homeostasis-induced signaling and crosstalk in the carcinogenesis paradigm “Epistemology of the origin of cancer”.
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特刊的前奏和前提:癌变范式中体内平衡诱导的信号和串扰的破坏“癌症起源的认识论”
绝大多数的抗癌策略都是有症状的,但为了取得一些切实的进展,我们需要确定大多数癌症的病因。有一种时代思潮认为,遗传学上的发现,即体细胞突变,被反射性地视为致癌的诱因,尽管目前约80%的癌症被称为“散发性”(即没有证实的病因)。观察到一英寸的癌变肝组织可能有超过1亿个突变,一个相同的突变可能导致不同的表型,这取决于该突变周围的环境,这使得突变本身不太可能是大多数癌症的病因。4open首次推出其特刊系列论文,提供了强有力的证据,证明癌变包括6步序列(1)病原性刺激,随后(2)慢性炎症,由此发展(3)纤维化与细胞外微环境的相关重塑,以及从这些变化中形成(4)癌前生态位(PCN)。纤维化与持续炎症重塑的产物形成,触发慢性应激逃逸策略的部署,当这一策略无法解决时,就会导致正常细胞向癌细胞转变。本特刊包含单独的论文,讨论被低估的普遍存在的蛋白质,慢性炎症,类二十烷类,微生物组和病态肥胖,PCN,细胞转移,随后二甲双胍诱导的信号改变,NF-κB信号和癌变过程中的串扰,并简要介绍。从本质上讲,现有的体外和体内证据都支持这样一个命题,即大多数癌症发生于癌变范式“癌症起源认识论”中稳态诱导的信号和串扰的破坏。
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