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Review
. 2018 Aug;93(3):1649-1683.
doi: 10.1111/brv.12413. Epub 2018 Apr 14.

The diverse origins of circulating cell-free DNA in the human body: a critical re-evaluation of the literature

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Review

The diverse origins of circulating cell-free DNA in the human body: a critical re-evaluation of the literature

Janine Aucamp et al. Biol Rev Camb Philos Soc. 2018 Aug.

Abstract

Since the detection of cell-free DNA (cfDNA) in human plasma in 1948, it has been investigated as a non-invasive screening tool for many diseases, especially solid tumours and foetal genetic abnormalities. However, to date our lack of knowledge regarding the origin and purpose of cfDNA in a physiological environment has limited its use to more obvious diagnostics, neglecting, for example, its potential utility in the identification of predisposition to disease, earlier detection of cancers, and lifestyle-induced epigenetic changes. Moreover, the concept or mechanism of cfDNA could also have potential therapeutic uses such as in immuno- or gene therapy. This review presents an extensive compilation of the putative origins of cfDNA and then contrasts the contributions of cellular breakdown processes with active mechanisms for the release of cfDNA into the extracellular environment. The involvement of cfDNA derived from both cellular breakdown and active release in lateral information transfer is also discussed. We hope to encourage researchers to adopt a more holistic view of cfDNA research, taking into account all the biological pathways in which cfDNA is involved, and to give serious consideration to the integration of in vitro and in vivo research. We also wish to encourage researchers not to limit their focus to the apoptotic or necrotic fraction of cfDNA, but to investigate the intercellular messaging capabilities of the actively released fraction of cfDNA and to study the role of cfDNA in pathogenesis.

Keywords: active DNA release; cellular breakdown mechanisms; circulating mitochondrial DNA; in vitro cell culture; lateral information transfer.

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