| Literature DB >> 33120014 |
Nevena B Ognjenovic1, Meisam Bagheri1, Gadisti Aisha Mohamed1, Ke Xu2, Youdinghuan Chen3, Mohamed Ashick Mohamed Saleem4, Meredith S Brown1, Shivashankar H Nagaraj5, Kristen E Muller6, Scott A Gerber7, Brock C Christensen8, Diwakar R Pattabiraman9.
Abstract
Differentiation therapy utilizes our understanding of the hierarchy of cellular systems to pharmacologically induce a shift toward terminal commitment. While this approach has been a paradigm in treating certain hematological malignancies, efforts to translate this success to solid tumors have met with limited success. Mammary-specific activation of PKA in mouse models leads to aberrant differentiation and diminished self-renewing potential of the basal compartment, which harbors mammary repopulating cells. PKA activation results in tumors that are more benign, exhibiting reduced metastatic propensity, loss of tumor-initiating potential, and increased sensitivity to chemotherapy. Analysis of tumor histopathology revealed features of overt differentiation with papillary characteristics. Longitudinal single-cell profiling at the hyperplasia and tumor stages uncovered an altered path of tumor evolution whereby PKA curtails the emergence of aggressive subpopulations. Acting through the repression of SOX4, PKA activation promotes tumor differentiation and represents a possible adjuvant to chemotherapy for certain breast cancers.Entities:
Keywords: epithelial-mesenchymal transition; mammary development; tumor differentiation; tumor evolution; tumor metastasis
Year: 2020 PMID: 33120014 PMCID: PMC7726035 DOI: 10.1016/j.devcel.2020.10.004
Source DB: PubMed Journal: Dev Cell ISSN: 1534-5807 Impact factor: 12.270