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Implications of Systemic Dysfunction for the Etiology of Malignancy

机译:系统性功能障碍对恶性肿瘤病因的影响

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The current approach to treatment in oncology is to replace the generally cytotoxic chemotherapies with pharmaceutical treatment which inactivates specific molecular targets associated with cancer development and progression. The goal is to limit cellular damage to pathways perceived to be directly responsible for the malignancy. Its underlying assumptions are twofold: (1) that individual pathways are the cause of malignancy; and (2) that the treatment objective should be destruction—either of the tumor or the dysfunctional pathway. However, the extent to which data actually support these assumptions has not been directly addressed. Accumulating evidence suggests that systemic dysfunction precedes the disruption of specific genetic/molecular pathways in most adult cancers and that targeted treatments such as kinase inhibitors may successfully treat one pathway while generating unintended changes to other, non-targeted pathways. This article discusses (1) the systemic basis of malignancy; (2) better profiling of pre-cancerous biomarkers associated with elevated risk so that preventive lifestyle modifications can be instituted early to revert high-risk epigenetic changes before tumors develop; (3) a treatment emphasis in early stage tumors that would target the restoration of systemic balance by strengthening the body's innate defense mechanisms; and (4) establishing better quantitative models of systems to capture adequate complexity for predictability at all stages of tumor progression.
机译:当前的肿瘤治疗方法是用药物治疗代替通常的细胞毒性化学疗法,该药物治疗可使与癌症发生和发展有关的特定分子靶失活。目的是将细胞损伤限于认为直接导致恶性肿瘤的途径。其基本假设是双重的:(1)个别途径是恶性肿瘤的原因; (2)治疗目标应该是消灭肿瘤或功能障碍途径。但是,数据实际支持这些假设的程度尚未得到直接解决。越来越多的证据表明,在大多数成年癌症中,系统功能障碍先于特定基因/分子途径的破坏,而靶向治疗(例如激酶抑制剂)可能成功治疗了一种途径,同时对其他非靶向途径产生了意外改变。本文讨论(1)恶性肿瘤的系统基础; (2)更好地分析与升高的风险相关的癌前生物标志物,以便可以提早进行预防性生活方式改变,以在肿瘤发展之前逆转高危表观遗传学改变; (3)重视早期肿瘤的治疗,其目标是通过增强机体的先天防御机制来恢复全身平衡; (4)建立更好的系统定量模型,以捕获足够的复杂性以在肿瘤进展的所有阶段进行可预测性。

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