Detection of cell‐free DNA fragmentation and copy number alterations in cerebrospinal fluid from glioma patients

Florent Mouliere; Richard Mair; Dineika Chandrananda; Francesco Marass; Christopher G Smith; Jing Su; James Morris; Colin Watts; Kevin M Brindle; Nitzan Rosenfeld

doi:10.15252/emmm.201809323

Detection of cell‐free DNA fragmentation and copy number alterations in cerebrospinal fluid from glioma patients

Florent Mouliere, Richard Mair, Dineika Chandrananda, Francesco Marass, Christopher G Smith, Jing Su, James Morris, Colin Watts, Kevin M Brindle, Nitzan Rosenfeld

Department of Physics & Astronomy

Research output: Contribution to journal › Article › peer-review

Abstract

Glioma is difficult to detect or characterize using current liquid biopsy approaches. Detection of cell‐free tumor DNA (cftDNA) in cerebrospinal fluid (CSF) has been proposed as an alternative to detection in plasma. We used shallow whole‐genome sequencing (sWGS, at a coverage of < 0.4×) of cell‐free DNA from the CSF of 13 patients with primary glioma to determine somatic copy number alterations and DNA fragmentation patterns. This allowed us to determine the presence of cftDNA in CSF without any prior knowledge of point mutations present in the tumor. We also showed that the fragmentation pattern of cell‐free DNA in CSF is different from that in plasma. This low‐cost screening method provides information on the tumor genome and can be used to target those patients with high levels of cftDNA for further larger‐scale sequencing, such as by whole‐exome and whole‐genome sequencing.

Original language	English
Article number	e9323
Pages (from-to)	1-6
Number of pages	6
Journal	EMBO Molecular Medicine
Volume	10
Issue number	12
DOIs	https://doi.org/10.15252/emmm.201809323
Publication status	Published - 6 Nov 2018

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10.15252/emmm.201809323

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title = "Detection of cell‐free DNA fragmentation and copy number alterations in cerebrospinal fluid from glioma patients",

abstract = "Glioma is difficult to detect or characterize using current liquid biopsy approaches. Detection of cell‐free tumor DNA (cftDNA) in cerebrospinal fluid (CSF) has been proposed as an alternative to detection in plasma. We used shallow whole‐genome sequencing (sWGS, at a coverage of < 0.4×) of cell‐free DNA from the CSF of 13 patients with primary glioma to determine somatic copy number alterations and DNA fragmentation patterns. This allowed us to determine the presence of cftDNA in CSF without any prior knowledge of point mutations present in the tumor. We also showed that the fragmentation pattern of cell‐free DNA in CSF is different from that in plasma. This low‐cost screening method provides information on the tumor genome and can be used to target those patients with high levels of cftDNA for further larger‐scale sequencing, such as by whole‐exome and whole‐genome sequencing.",

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T1 - Detection of cell‐free DNA fragmentation and copy number alterations in cerebrospinal fluid from glioma patients

AU - Mouliere, Florent

AU - Mair, Richard

AU - Chandrananda, Dineika

AU - Marass, Francesco

AU - Smith, Christopher G

AU - Su, Jing

AU - Morris, James

AU - Watts, Colin

AU - Brindle, Kevin M

AU - Rosenfeld, Nitzan

PY - 2018/11/6

Y1 - 2018/11/6

N2 - Glioma is difficult to detect or characterize using current liquid biopsy approaches. Detection of cell‐free tumor DNA (cftDNA) in cerebrospinal fluid (CSF) has been proposed as an alternative to detection in plasma. We used shallow whole‐genome sequencing (sWGS, at a coverage of < 0.4×) of cell‐free DNA from the CSF of 13 patients with primary glioma to determine somatic copy number alterations and DNA fragmentation patterns. This allowed us to determine the presence of cftDNA in CSF without any prior knowledge of point mutations present in the tumor. We also showed that the fragmentation pattern of cell‐free DNA in CSF is different from that in plasma. This low‐cost screening method provides information on the tumor genome and can be used to target those patients with high levels of cftDNA for further larger‐scale sequencing, such as by whole‐exome and whole‐genome sequencing.

AB - Glioma is difficult to detect or characterize using current liquid biopsy approaches. Detection of cell‐free tumor DNA (cftDNA) in cerebrospinal fluid (CSF) has been proposed as an alternative to detection in plasma. We used shallow whole‐genome sequencing (sWGS, at a coverage of < 0.4×) of cell‐free DNA from the CSF of 13 patients with primary glioma to determine somatic copy number alterations and DNA fragmentation patterns. This allowed us to determine the presence of cftDNA in CSF without any prior knowledge of point mutations present in the tumor. We also showed that the fragmentation pattern of cell‐free DNA in CSF is different from that in plasma. This low‐cost screening method provides information on the tumor genome and can be used to target those patients with high levels of cftDNA for further larger‐scale sequencing, such as by whole‐exome and whole‐genome sequencing.

U2 - 10.15252/emmm.201809323

DO - 10.15252/emmm.201809323

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Detection of cell‐free DNA fragmentation and copy number alterations in cerebrospinal fluid from glioma patients

Abstract

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