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Towards understanding cancer dormancy over strategic hitching up mechanisms to technologies

Authors
Yang SuminSeo JieunChoi JeonghyeonKim Sung-HyunKuk YunminPark Kyung ChanKang MingonByun SangwonJoo Jae-Yeol
Issue Date
Feb-2025
Publisher
BMC
Citation
MOLECULAR CANCER, v.24, no.1, pp 1 - 23
Pages
23
Indexed
SCIE
SCOPUS
Journal Title
MOLECULAR CANCER
Volume
24
Number
1
Start Page
1
End Page
23
URI
https://scholarworks.bwise.kr/erica/handle/2021.sw.erica/126395
ISSN
1476-4598
Abstract
Delving into cancer dormancy has been an inherent task that may drive the lethal recurrence of cancer after primary tumor relief. Cells in quiescence can survive for a short or long term in silence, may undergo genetic or epigenetic changes, and can initiate relapse through certain contextual cues. The state of dormancy can be induced by multiple conditions including cancer drug treatment, in turn, undergoes a life cycle that generally occurs through dissemination, invasion, intravasation, circulation, immune evasion, extravasation, and colonization. Throughout this cascade, a cellular machinery governs the fate of individual cells, largely affected by gene regulation. Despite its significance, a precise view of cancer dormancy is yet hampered. Revolutionizing advanced single cell and long read sequencing through analysis methodologies and artificial intelligence, the most recent stage in the research tool progress, is expected to provide a holistic view of the diverse aspects of cancer dormancy.
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