Publications by authors named "Alexandra P Cadena"

Purpose Acute radiation-induced esophagitis (ARIE) leads to treatment delays, decreased quality of life (QOL), and secondary adverse events such as weight loss. Grade 3 ARIE occurs in 15%-30% of patients undergoing radiotherapy to the esophagus, leading to disruption or discontinuation of treatment. The purpose of this study was to assess the effects of glutamine, a common nutritional supplement, on ARIE in patients with thoracic malignancies.

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Article Synopsis
  • - The study addresses the challenges of cancer treatment, particularly the resistance of tumors to checkpoint inhibitors, and introduces a novel combined approach using low-dose radiotherapy (XRT) alongside immunotherapy to enhance treatment effectiveness.
  • - Researchers tested this combination on mice with lung adenocarcinoma, revealing that high-dose XRT helps prepare T cells in primary tumors, while low-dose XRT allows for better immune responses in secondary tumors by modifying the tumor environment.
  • - Results showed that low-dose XRT boosts the effectiveness of immune cells, such as M1 macrophages and NK cells, and reduces inhibitory factors like TGF-β, with the lack of certain immune cells negating the treatment's benefits, suggesting a promising strategy for improving
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Purpose: Radiotherapy (RT) traditionally has been used for local tumor control in the treatment of cancer. The recent discovery that radiotherapy can have anticancer effects on the immune system has led to recognition of its ability to sensitize the tumor microenvironment to immunotherapy. However, radiation can also prompt adverse immunosuppressive effects that block aspects of systemic response at other tumor sites.

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Glycosylation and its by-product, the glycan, play a crucial role in many cellular processes. Aberrant glycan structures and mutations of the glycosylation pathway have been intricately linked with the development of cancer and more recently with cancer's ability to escape the innate immune system. This chapter aims to elucidate how glycosylation interacts with the immune system to promote tumor deviation through endogenous lectins, mutated glycosphingolipids, sialic acid domains, and more.

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Despite the potential to cure metastatic disease, immunotherapy on its own often fails outright or early on due to tumor immune evasion. To address this obstacle, we investigated combinations of anti-GITR, anti-PD1 and radiation therapy (XRT) in our previously developed anti-PD1 resistant 344SQ non-small cell lung adenocarcinoma preclinical tumor model. We hypothesized that targeting multiple mechanisms of immune evasion with this triple therapy would lead to an enhanced tumor-specific immune response and improve survival more so than any mono- or dual therapy.

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