The non-targeted effects of radiation are perpetuated by exosomes

Ammar Al-Mayah; Scott Bright; Kim Chapman; Sarah Irons; Ping Luo; David Carter; Edwin Goodwin; Munira Kadhim

doi:10.1016/j.mrfmmm.2014.12.007

The non-targeted effects of radiation are perpetuated by exosomes

Mutat Res. 2015 Feb:772:38-45. doi: 10.1016/j.mrfmmm.2014.12.007. Epub 2014 Dec 30.

Authors

Ammar Al-Mayah¹, Scott Bright¹, Kim Chapman¹, Sarah Irons², Ping Luo³, David Carter⁴, Edwin Goodwin⁵, Munira Kadhim⁶

Affiliations

¹ Genomic Instability Group, Oxford Brookes University, Gipsy Lane Campus, Headington, Oxford OX3 0BP, United Kingdom.
² Insect Virus Research Group, Oxford Brookes University, Gipsy Lane Campus, Headington, Oxford OX3 0BP, United Kingdom.
³ Izon Science Ltd., The Oxford Science Park, Magdalen Centre, Robert Robinson Avenue, Oxford OX4 4GA, United Kingdom.
⁴ Chromatin and non-coding RNA, Oxford Brookes University, Gipsy Lane Campus, Headington, Oxford OX3 0BP, United Kingdom.
⁵ The New Mexico Consortium, Los Alamos, NM 87544, USA.
⁶ Genomic Instability Group, Oxford Brookes University, Gipsy Lane Campus, Headington, Oxford OX3 0BP, United Kingdom. Electronic address: mkadhim@brookes.ac.uk.

PMID: 25772109
DOI: 10.1016/j.mrfmmm.2014.12.007

Abstract

Exosomes contain cargo material from endosomes, cytosol, plasma membrane and microRNA molecules, they are released by a number of non-cancer and cancer cells into both the extracellular microenvironment and body fluids such as blood plasma. Recently we demonstrated radiation-induced non-targeted effects [NTE: genomic instability (GI) and bystander effects (BE)] are partially mediated by exosomes, particularly the RNA content. However the mechanistic role of exosomes in NTE is yet to be fully understood. The present study used MCF7 cells to characterise the longevity of exosome-induced activity in the progeny of irradiated and unirradiated bystander cells. Exosomes extracted from conditioned media of irradiated and bystander progeny were added to unirradiated cells. Analysis was carried out at 1 and 20/24 population doublings following medium/exosome transfer for DNA/chromosomal damage. Results confirmed exosomes play a significant role in mediating NTE of ionising radiation (IR). This effect was remarkably persistent, observed >20 doublings post-irradiation in the progeny of bystander cells. Additionally, cell progeny undergoing a BE were themselves capable of inducing BE in other cells via exosomes they released. Furthermore we investigated the role of exosome cargo. Culture media from cells exposed to 2 Gy X-rays was subjected to ultracentrifugation and four inoculants prepared, (a) supernatants with exosomes removed, and pellets with (b) exosome proteins denatured, (c) RNA degraded, and (d) a combination of protein-RNA inactivation. These were added to separate populations of unirradiated cells. The BE was partially inhibited when either exosome protein or exosome RNA were inactivated separately, whilst combined RNA-protein inhibition significantly reduced or eliminated the BE. These results demonstrate that exosomes are associated with long-lived signalling of the NTE of IR. Both RNA and protein molecules of exosomes work in a synergistic manner to initiate NTE, spread these effects to naïve cells, and perpetuate GI in the affected cells.

Keywords: Bystander effects; Exosome cargo; Exosomes; Genomic instability; Ionising radiation.

Publication types

Research Support, Non-U.S. Gov't

MeSH terms

Bystander Effect / radiation effects*
Cell Line, Tumor
Exosomes / metabolism*
Female
Genomic Instability / radiation effects*
Humans
RNA / metabolism*
Signal Transduction / radiation effects*
X-Rays

Substances

RNA