AI Article Synopsis
- Rapid loss of the Rb1 pathway may lead to quick cancer mutations, but recent studies show retinoblastomas have little genomic instability, indicating a possible role of epigenetic changes.
- Research suggests the Rb1 pathway loss could be enough to trigger cancer, but mutations alone in Rb1 genes typically don't initiate tumors on their own.
- Our findings reveal that traditional testing methods using nude mice create environments that hinder tumor formation, but when we bypass these limitations, Rb1-mutated fibroblasts can successfully develop sarcomas and advance to invasive tumors via the Ras-ZEB1-Akt pathway.
Article Abstract
It is thought that genomic instability precipitated by Rb1 pathway loss rapidly triggers additional cancer gene mutations, accounting for rapid tumour onset following Rb1 mutation. However, recent whole-genome sequencing of retinoblastomas demonstrated little genomic instability, but instead suggested rapid epigenetic activation of cancer genes. These results raise the possibility that loss of the Rb1 pathway, which is a hallmark of cancers, might be sufficient for cancer initiation. Yet, mutation of the Rb1 family or inactivation of the Rb1 pathway in primary cells has proven insufficient for tumour initiation. Here we demonstrate that traditional nude mouse assays impose an artificial anoikis and proliferation barrier that prevents Rb1 family mutant fibroblasts from initiating tumours. By circumventing this barrier, we show that primary fibroblasts with only an Rb1 family mutation efficiently form sarcomas in nude mice, and a Ras-ZEB1-Akt pathway then causes transition of these tumours to an invasive phenotype.
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| http://dx.doi.org/10.1038/ncomms3650 | DOI Listing |
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