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      Detection of chromosomal alterations in the circulation of cancer patients with whole-genome sequencing.

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          Abstract

          Clinical management of cancer patients could be improved through the development of noninvasive approaches for the detection of incipient, residual, and recurrent tumors. We describe an approach to directly identify tumor-derived chromosomal alterations through analysis of circulating cell-free DNA from cancer patients. Whole-genome analyses of DNA from the plasma of 10 colorectal and breast cancer patients and 10 healthy individuals with massively parallel sequencing identified, in all patients, structural alterations that were not present in plasma DNA from healthy subjects. Detected alterations comprised chromosomal copy number changes and rearrangements, including amplification of cancer driver genes such as ERBB2 and CDK6. The level of circulating tumor DNA in the cancer patients ranged from 1.4 to 47.9%. The sensitivity and specificity of this approach are dependent on the amount of sequence data obtained and are derived from the fact that most cancers harbor multiple chromosomal alterations, each of which is unlikely to be present in normal cells. Given that chromosomal abnormalities are present in nearly all human cancers, this approach represents a useful method for the noninvasive detection of human tumors that is not dependent on the availability of tumor biopsies.

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          Author and article information

          Journal
          Sci Transl Med
          Science translational medicine
          American Association for the Advancement of Science (AAAS)
          1946-6242
          1946-6234
          Nov 28 2012
          : 4
          : 162
          Affiliations
          [1 ] Ludwig Center for Cancer Genetics and Howard Hughes Medical Institutions, Johns Hopkins Kimmel Cancer Center, Baltimore, MD 21287, USA.
          Article
          4/162/162ra154 NIHMS440630
          10.1126/scitranslmed.3004742
          3641759
          23197571
          9d0bbe48-b686-492e-b9a8-94d28107095d
          History

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