| Literature DB >> 28126926 |
Paul Yeh1,2,3, Michael Dickinson2, Sarah Ftouni1, Tane Hunter1,3, Devbarna Sinha1, Stephen Q Wong1, Rishu Agarwal1,3, Ravikiran Vedururu1, Kenneth Doig1,3, Chun Yew Fong1,3, Piers Blombery1,2, David Westerman1,2, Mark A Dawson1,2,3,4, Sarah-Jane Dawson1,2,3,4.
Abstract
The diagnosis and monitoring of myelodysplastic syndromes (MDSs) are highly reliant on bone marrow morphology, which is associated with substantial interobserver variability. Although azacitidine is the mainstay of treatment in MDS, only half of all patients respond. Therefore, there is an urgent need for improved modalities for the diagnosis and monitoring of MDSs. The majority of MDS patients have either clonal somatic karyotypic abnormalities and/or gene mutations that aid in the diagnosis and can be used to monitor treatment response. Circulating cell-free DNA is primarily derived from hematopoietic cells, and we surmised that the malignant MDS genome would be a major contributor to cell-free DNA levels in MDS patients as a result of ineffective hematopoiesis. Through analysis of serial bone marrow and matched plasma samples (n = 75), we demonstrate that cell-free circulating tumor DNA (ctDNA) is directly comparable to bone marrow biopsy in representing the genomic heterogeneity of malignant clones in MDS. Remarkably, we demonstrate that serial monitoring of ctDNA allows concurrent tracking of both mutations and karyotypic abnormalities throughout therapy and is able to anticipate treatment failure. These data highlight the role of ctDNA as a minimally invasive molecular disease monitoring strategy in MDS.Entities:
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Year: 2017 PMID: 28126926 DOI: 10.1182/blood-2016-09-740308
Source DB: PubMed Journal: Blood ISSN: 0006-4971 Impact factor: 22.113