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Putative Origins of Cell-Free DNA in Humans: A Review of Active and Passive Nucleic Acid Release Mechanisms

Through various pathways of cell death, degradation, and regulated extrusion, partial or complete genomes of various origins (e.g., host cells, fetal cells, and infiltrating viruses and microbes) are continuously shed into human body fluids in the form of segmented cell-free DNA (cfDNA) molecules. W...

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Autores principales: Grabuschnig, Stefan, Bronkhorst, Abel Jacobus, Holdenrieder, Stefan, Rosales Rodriguez, Ingund, Schliep, Klaus Peter, Schwendenwein, Daniel, Ungerer, Vida, Sensen, Christoph Wilhelm
Formato: Online Artículo Texto
Lenguaje:English
Publicado: MDPI 2020
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7662960/
https://www.ncbi.nlm.nih.gov/pubmed/33137955
http://dx.doi.org/10.3390/ijms21218062
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author Grabuschnig, Stefan
Bronkhorst, Abel Jacobus
Holdenrieder, Stefan
Rosales Rodriguez, Ingund
Schliep, Klaus Peter
Schwendenwein, Daniel
Ungerer, Vida
Sensen, Christoph Wilhelm
author_facet Grabuschnig, Stefan
Bronkhorst, Abel Jacobus
Holdenrieder, Stefan
Rosales Rodriguez, Ingund
Schliep, Klaus Peter
Schwendenwein, Daniel
Ungerer, Vida
Sensen, Christoph Wilhelm
author_sort Grabuschnig, Stefan
collection PubMed
description Through various pathways of cell death, degradation, and regulated extrusion, partial or complete genomes of various origins (e.g., host cells, fetal cells, and infiltrating viruses and microbes) are continuously shed into human body fluids in the form of segmented cell-free DNA (cfDNA) molecules. While the genetic complexity of total cfDNA is vast, the development of progressively efficient extraction, high-throughput sequencing, characterization via bioinformatics procedures, and detection have resulted in increasingly accurate partitioning and profiling of cfDNA subtypes. Not surprisingly, cfDNA analysis is emerging as a powerful clinical tool in many branches of medicine. In addition, the low invasiveness of longitudinal cfDNA sampling provides unprecedented access to study temporal genomic changes in a variety of contexts. However, the genetic diversity of cfDNA is also a great source of ambiguity and poses significant experimental and analytical challenges. For example, the cfDNA population in the bloodstream is heterogeneous and also fluctuates dynamically, differs between individuals, and exhibits numerous overlapping features despite often originating from different sources and processes. Therefore, a deeper understanding of the determining variables that impact the properties of cfDNA is crucial, however, thus far, is largely lacking. In this work we review recent and historical research on active vs. passive release mechanisms and estimate the significance and extent of their contribution to the composition of cfDNA.
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spelling pubmed-76629602020-11-14 Putative Origins of Cell-Free DNA in Humans: A Review of Active and Passive Nucleic Acid Release Mechanisms Grabuschnig, Stefan Bronkhorst, Abel Jacobus Holdenrieder, Stefan Rosales Rodriguez, Ingund Schliep, Klaus Peter Schwendenwein, Daniel Ungerer, Vida Sensen, Christoph Wilhelm Int J Mol Sci Review Through various pathways of cell death, degradation, and regulated extrusion, partial or complete genomes of various origins (e.g., host cells, fetal cells, and infiltrating viruses and microbes) are continuously shed into human body fluids in the form of segmented cell-free DNA (cfDNA) molecules. While the genetic complexity of total cfDNA is vast, the development of progressively efficient extraction, high-throughput sequencing, characterization via bioinformatics procedures, and detection have resulted in increasingly accurate partitioning and profiling of cfDNA subtypes. Not surprisingly, cfDNA analysis is emerging as a powerful clinical tool in many branches of medicine. In addition, the low invasiveness of longitudinal cfDNA sampling provides unprecedented access to study temporal genomic changes in a variety of contexts. However, the genetic diversity of cfDNA is also a great source of ambiguity and poses significant experimental and analytical challenges. For example, the cfDNA population in the bloodstream is heterogeneous and also fluctuates dynamically, differs between individuals, and exhibits numerous overlapping features despite often originating from different sources and processes. Therefore, a deeper understanding of the determining variables that impact the properties of cfDNA is crucial, however, thus far, is largely lacking. In this work we review recent and historical research on active vs. passive release mechanisms and estimate the significance and extent of their contribution to the composition of cfDNA. MDPI 2020-10-29 /pmc/articles/PMC7662960/ /pubmed/33137955 http://dx.doi.org/10.3390/ijms21218062 Text en © 2020 by the authors. Licensee MDPI, Basel, Switzerland. This article is an open access article distributed under the terms and conditions of the Creative Commons Attribution (CC BY) license (http://creativecommons.org/licenses/by/4.0/).
spellingShingle Review
Grabuschnig, Stefan
Bronkhorst, Abel Jacobus
Holdenrieder, Stefan
Rosales Rodriguez, Ingund
Schliep, Klaus Peter
Schwendenwein, Daniel
Ungerer, Vida
Sensen, Christoph Wilhelm
Putative Origins of Cell-Free DNA in Humans: A Review of Active and Passive Nucleic Acid Release Mechanisms
title Putative Origins of Cell-Free DNA in Humans: A Review of Active and Passive Nucleic Acid Release Mechanisms
title_full Putative Origins of Cell-Free DNA in Humans: A Review of Active and Passive Nucleic Acid Release Mechanisms
title_fullStr Putative Origins of Cell-Free DNA in Humans: A Review of Active and Passive Nucleic Acid Release Mechanisms
title_full_unstemmed Putative Origins of Cell-Free DNA in Humans: A Review of Active and Passive Nucleic Acid Release Mechanisms
title_short Putative Origins of Cell-Free DNA in Humans: A Review of Active and Passive Nucleic Acid Release Mechanisms
title_sort putative origins of cell-free dna in humans: a review of active and passive nucleic acid release mechanisms
topic Review
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7662960/
https://www.ncbi.nlm.nih.gov/pubmed/33137955
http://dx.doi.org/10.3390/ijms21218062
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