AI Article Synopsis
- Most solid tumors often have irregular blood flow, leading to low oxygen levels (hypoxia) that make radiotherapy less effective.
- Research has focused on ways to boost oxygen levels in tumors, especially during post-surgery radiotherapy, which is a common treatment for various cancers.
- This review discusses drugs that target how the body uses glucose and lactate, nitric oxide, and certain cell signaling pathways to improve oxygen availability, showing promise for supporting radiotherapy and encouraging further clinical studies.
Article Abstract
Most solid tumors are characterized by unstable perfusion patterns, creating regions of hypoxia that are detrimental to radiotherapy treatment response. Because postsurgical radiotherapy, alone or in combination with other interventions, is a first-line treatment for many malignancies, strategies aimed at homogeneously increasing tumor pO2 have been the focus of intense research over the past decades. Among other approaches of demonstrable clinical and preclinical utility, this review focuses on those directly targeting oxygen consumption to redirect oxygen from a metabolic fate to the stabilization of radiation-induced DNA damage, more particularly drugs targeting glucose and lactate metabolism, nitric oxide donors or inducers, and mitogen-activated protein kinase pathway inhibitors. Their utility as adjuvant treatments with radiotherapy has been proven preclinically, which should foster further their clinical development and evaluation.
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| http://dx.doi.org/10.1016/j.semradonc.2013.05.008 | DOI Listing |
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