4.6 Review

Ecology and evolution of dormant metastasis

Journal

TRENDS IN CANCER
Volume 8, Issue 7, Pages 570-582

Publisher

CELL PRESS
DOI: 10.1016/j.trecan.2022.03.002

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Funding

  1. Gobierno de Espana
  2. AECC (Spanish Cancer Association) postdoctoral grant
  3. Institucio Catalana de Recerca i Estudis Avancats
  4. Generalitat de Catalunya [SGR-2017-557]
  5. BBVA Foundation
  6. ISCIII/FEDER-CIBERONC
  7. 'la Caixa' Foundation [100010434]
  8. Spanish Ministerio de Economia y Competitividad (MINECO)
  9. FEDER funds (CIBERONC)
  10. FEDER funds [PID2019104948RB-I00]

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Metastatic cancer cells may remain dormant after primary metastasis and eventually spread to other organs, causing incurable metastasis. The stationary nature of metastatic tumor cells prevents effective treatment, ultimately leading to relapse and the development of treatment resistance in metastatic lesions.
Genetic studies suggest that sequential dissemination from a primary metastasis, usually at the bone, is a major route of metastatic progression in early, radically resected cancer. Disseminated tumor cells (DTCs) can likely infiltrate but not grow, and may remain dormant once disseminated for extended intervals (from months to decades). The stationary nature of DTCs prevents them from being successfully treated as an asymptomatic residual disease in the adjuvant setting; critically, they can eventually relapse, adapt, and develop therapy resistance, causing incurable overt metastasis. Metastatic lesions usually first appear in one tissue, which invigorates metastatic cells for further dissemination to other organs, with a fatal outcome. Clinical and genetic data now indicate that metastatic lesions in one organ can seed secondary metastases in other organs: in other words, metastasis arising from metastasis. Herein we discuss recent insight into metastasis cell dormancy mechanisms, survival, communication with the local microenvironment, and eventual changes that endow DTCs with the capacity to expand and colonize to other metastatic sites.

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