Monitoring circulating tumor DNA revealed dynamic changes in KRAS status in patients with metastatic colorectal cancer

mutated circulating tumor DNA (MctDNA) can be monitored in the blood of patients with metastatic colorectal cancer (mCRC), but dynamic changes have not been determined. Four hundred and fifty-seven plasma samples were collected prospectively from 85 mCRC patients who underwent chemotherapy. MctDNA i...

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Veröffentlicht in:Oncotarget 2018-05, Vol.9 (36), p.24398-24413
Hauptverfasser: Takayama, Yuji, Suzuki, Koichi, Muto, Yuta, Ichida, Kosuke, Fukui, Taro, Kakizawa, Nao, Ishikawa, Hideki, Watanabe, Fumiaki, Hasegawa, Fumi, Saito, Masaaki, Tsujinaka, Shingo, Futsuhara, Kazushige, Miyakura, Yasuyuki, Noda, Hiroshi, Konishi, Fumio, Rikiyama, Toshiki
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Sprache:eng
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Zusammenfassung:mutated circulating tumor DNA (MctDNA) can be monitored in the blood of patients with metastatic colorectal cancer (mCRC), but dynamic changes have not been determined. Four hundred and fifty-seven plasma samples were collected prospectively from 85 mCRC patients who underwent chemotherapy. MctDNA in plasma was detected by droplet digital PCR, and the percentage of MctDNA in total circulating cell-free DNA was calculated. assessment in tumor tissues showed 29 patients with the mutant-type (MT) and 56 patients with the wild-type (WT). Twenty-three of 29 MT patients (79.3%) and 28 of 56 WT patients (50.0%) showed MctDNA. Emergence of MctDNA was recognized during treatments with various drugs. Regardless of status in tumor tissues, patients with MctDNA in blood showed poor progression-free survival with first-line treatment. Median percentage of MctDNA accounted for 10.10% in MT patients and 0.22% in WT patients. These differences between MT and WT likely affected patterns of changes in MctDNA. monitoring identified dynamic changes in MctDNA, such as continuous, intermittent, and transient changes (quick elevation and disappearance). Emergence of MctDNA involved drug resistance, except for transient changes, which were seen in WT patients and likely corresponded with the drug response. Transient changes could be involved in recovery of sensitivity to anti-EGFR antibody in WT patients. Monitoring MctDNA during various treatments showed dynamic changes in status and could provide useful information for determining treatments for patients with mCRC.
ISSN:1949-2553
1949-2553
DOI:10.18632/oncotarget.25309