Clinical Epigenetics (Jul 2024)

Quantification method of ctDNA using cell-free DNA methylation profile for noninvasive screening and monitoring of colon cancer

  • Hyojung Ryu,
  • Ji-Hoon Kim,
  • Yeo Jin Kim,
  • Hahyeon Jeon,
  • Byoung-Chul Kim,
  • Yeonsu Jeon,
  • Yeonkyung Kim,
  • Hyebin Bak,
  • Younghui Kang,
  • Changjae Kim,
  • Hyojin Um,
  • Ji-Hye Ahn,
  • Hwi Hyun,
  • Byung Chul Kim,
  • Inho Song,
  • Sungwon Jeon,
  • Jong Bhak,
  • Eon Chul Han

DOI
https://doi.org/10.1186/s13148-024-01708-9
Journal volume & issue
Vol. 16, no. 1
pp. 1 – 11

Abstract

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Abstract Background Colon cancer ranks as the second most lethal form of cancer globally. In recent years, there has been active investigation into using the methylation profile of circulating tumor DNA (ctDNA), derived from blood, as a promising indicator for diagnosing and monitoring colon cancer. Results We propose a liquid biopsy-based epigenetic method developed by utilizing 49 patients and 260 healthy controls methylation profile data to screen and monitor colon cancer. Our method initially identified 901 colon cancer-specific hypermethylated (CaSH) regions in the tissues of the 49 cancer patients. We then used these CaSH regions to accurately quantify the amount of circulating tumor DNA (ctDNA) in the blood samples of these same patients, utilizing cell-free DNA methylation profiles. Notably, the methylation profiles of ctDNA in the blood exhibited high sensitivity (82%) and specificity (93%) in distinguishing patients with colon cancer from the control group, with an area under the curve of 0.903. Furthermore, we confirm that our method for ctDNA quantification is effective for monitoring cancer patients and can serve as a valuable tool for postoperative prognosis. Conclusions This study demonstrated a successful application of the quantification of ctDNA among cfDNA using the original cancer tissue-derived CaSH region for screening and monitoring colon cancer.

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