2024
DOI: 10.20935/acadmed6168
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Understanding cancer from an evolutionary perspective: high-risk reprogramming of genome-damaged stem cells

Vladimir F. Niculescu

Abstract: Background: One of the most astounding discoveries of recent times is the recognition that cancer embodies a transition from a higher level of metazoan cell organization to a more foundational premetazoic state. This shift is steered by genes housed within the ancestral genome compartment, pervasive across all metazoan genomes, encompassing humans, and governed by a premetazoic ancestral gene regulatory network. This work aims to highlight the emerging field of evolutionary cancer cell biology (ECCB), which po… Show more

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Cited by 2 publications
(11 citation statements)
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“…Human DSCDs can enter a state of transient quiescence or slow cycling within their niche. However, they can exit the quiescence niche and continue to proliferate through aberrant symmetric cell cycles [9][10][11]. Environmental changes inside the niche or exposure to more oxygenated regions can induce increased proliferation, causing DSCD progeny to become fusible and form cell aggregates (MGRS).…”
Section: Dysfunctional Dscd Cells Prior Malignizationmentioning
confidence: 99%
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“…Human DSCDs can enter a state of transient quiescence or slow cycling within their niche. However, they can exit the quiescence niche and continue to proliferate through aberrant symmetric cell cycles [9][10][11]. Environmental changes inside the niche or exposure to more oxygenated regions can induce increased proliferation, causing DSCD progeny to become fusible and form cell aggregates (MGRS).…”
Section: Dysfunctional Dscd Cells Prior Malignizationmentioning
confidence: 99%
“…Thus, DNA damage repair and genome reprogramming proceed in a unicellular manner under the control of the ancient gene regulatory network (aGRN) that transforms the precancerous high-risk tetraploid DSCD phenotype into a cancerous asymmetric cell division (ACD) phenotype, with stemness, differentiation potential, and the ability to initiate germ and soma (G+S) life cycles of pre-metazoan imprinting. The NG germline of cancer contains all the hallmarks of the ancestral Urgermline, producing naive CSCs as GSCs [9][10][11].…”
Section: Dysfunctional Dscd Cells Prior Malignizationmentioning
confidence: 99%
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“…In tumors, metastases, and recurrences, PGCCs function as mechanisms for genome repair (reprogramming) and serve as reproductive entities for the generation of CSCs. 10. PGCCs serve as an overarching term encompassing hyperpolyploidization through both cell and nuclear fusion (MGRS-like) and defective lower polyploidization processes such as tetraploidization and aneuploidization.…”
Section: Introductionmentioning
confidence: 99%