[HTML][HTML] Reprogramming the immunological microenvironment through radiation and targeting Axl

TA Aguilera, M Rafat, L Castellini, H Shehade… - Nature …, 2016 - nature.com
TA Aguilera, M Rafat, L Castellini, H Shehade, MS Kariolis, ABY Hui, H Stehr, R Von Eyben…
Nature communications, 2016nature.com
Increasing evidence suggests that ionizing radiation therapy (RT) in combination with
checkpoint immunotherapy is highly effective in treating a subset of cancers. To better
understand the limited responses to this combination we analysed the genetic,
microenvironmental, and immune factors in tumours derived from a transgenic breast cancer
model. We identified two tumours with similar growth characteristics but different RT
responses primarily due to an antitumour immune response. The combination of RT and …
Abstract
Increasing evidence suggests that ionizing radiation therapy (RT) in combination with checkpoint immunotherapy is highly effective in treating a subset of cancers. To better understand the limited responses to this combination we analysed the genetic, microenvironmental, and immune factors in tumours derived from a transgenic breast cancer model. We identified two tumours with similar growth characteristics but different RT responses primarily due to an antitumour immune response. The combination of RT and checkpoint immunotherapy resulted in cures in the responsive but not the unresponsive tumours. Profiling the tumours revealed that the Axl receptor tyrosine kinase is overexpressed in the unresponsive tumours, and Axl knockout resulted in slower growth and increased radiosensitivity. These changes were associated with a CD8+ T-cell response, which was improved in combination with checkpoint immunotherapy. These results suggest a novel role for Axl in suppressing antigen presentation through MHCI, and enhancing cytokine release, which promotes a suppressive myeloid microenvironment.
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