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Clonal Hematopoiesis in Liquid Biopsy: From Biological Noise to Valuable Clinical Implications

机译:液体活检中的克隆造血:从生物噪声到有价值的临床意义

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摘要

The use of blood liquid biopsy is being gradually incorporated into the clinical setting of cancer management. The minimally invasive nature of the usage of cell-free DNA (cfDNA) and its ability to capture the molecular alterations of tumors are great advantages for their clinical applications. However, somatic mosaicism in plasma remains an immense challenge for accurate interpretation of liquid biopsy results. Clonal hematopoiesis (CH) is part of the normal process of aging with the accumulation of somatic mutations and clonal expansion of hematopoietic stem cells. The detection of these non-tumor derived CH-mutations has been repeatedly reported as a source of biological background noise of blood liquid biopsy. Incorrect classification of CH mutations as tumor-derived mutations could lead to inappropriate therapeutic management. CH has also been associated with an increased risk of developing cardiovascular disease and hematological malignancies. Cancer patients, who are CH carriers, are more prone to develop therapy-related myeloid neoplasms after chemotherapy than non-carriers. The detection of CH mutations from plasma cfDNA analysis should be cautiously evaluated for their potential pathological relevance. Although CH mutations are currently considered as “false-positives” in cfDNA analysis, future studies should evaluate their clinical significance in healthy individuals and cancer patients.
机译:血液液体活检的使用逐渐掺入癌症管理的临床环境中。使用无细胞DNA(CFDNA)的使用的微创性质及其捕获肿瘤的分子改变的能力对其临床应用具有很大的优势。然而,血浆中的体细胞果皮仍然是患液体活检结果的准确解释的巨大挑战。克隆造血(CH)是随着造血干细胞的体细胞突变和克隆膨胀的积累的正常过程的一部分。这些非肿瘤衍生的CH-突变的检测已被反复报告为血液活检的生物背景噪声源。作为肿瘤衍生突变的CH突变分类不正确可能导致不适当的治疗管理。 CH也与发育心血管疾病和血液恶性恶性肿瘤的风险增加有关。癌症患者是CH携带者的患者,更容易发生化疗后的治疗相关的骨髓肿瘤,而不是非载体。应致考虑来自血浆CFDNA分析的CH突变的潜在病理相关性。虽然CH突变目前在CFDNA分析中被视为“假阳性”,但未来的研究应评估其健康个体和癌症患者的临床意义。

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