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Akt inhibition improves long-term tumour control following radiotherapy by altering the microenvironment. | LitMetric

AI Article Synopsis

  • Radiotherapy is a key cancer treatment, but many tumors still come back after treatment, leading researchers to explore combining targeted anti-cancer drugs with radiotherapy.
  • The study focuses on AZD5363, an Akt inhibitor, showing that giving it after radiotherapy improves long-term tumor control by positively affecting the tumor microenvironment.
  • AZD5363 reduces certain proteins linked to tumor growth and decreases the number of specific immune cells in the tumors when given post-radiotherapy, leading to less tumor vascular density and preventing tumor regrowth.

Article Abstract

Radiotherapy is an important anti-cancer treatment, but tumour recurrence remains a significant clinical problem. In an effort to improve outcomes further, targeted anti-cancer drugs are being tested in combination with radiotherapy. Here, we have studied the effects of Akt inhibition with AZD5363. AZD5363 administered as an adjuvant after radiotherapy to FaDu and PE/CA PJ34 tumours leads to long-term tumour control, which appears to be secondary to effects on the irradiated tumour microenvironment. AZD5363 reduces the downstream effectors VEGF and HIF-1α, but has no effect on tumour vascularity or oxygenation, or on tumour control, when administered prior to radiotherapy. In contrast, AZD5363 given after radiotherapy is associated with marked reductions in tumour vascular density, a decrease in the influx of CD11b myeloid cells and a failure of tumour regrowth. In addition, AZD5363 is shown to inhibit the proportion of proliferating tumour vascular endothelial cells which may contribute to improved tumour control with adjuvant treatment. These new insights provide promise to improve outcomes with the addition of AZD5363 as an adjuvant therapy following radiotherapy.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC5709765PMC
http://dx.doi.org/10.15252/emmm.201707767DOI Listing

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