Partner: Bozena Kamińska

Nencki Institute of Experimental Biology, Polish Academy of Sciences (PL)

Ostatnie publikacje
1.Was H., Barszcz K., Czarnecka J., Kowalczyk A., Bernas T., Uzarowska E., Koza P., Klejman A., Piwocka K., Kaminska B., Sikora E., Bafilomycin A1 triggers proliferative potential of senescent cancer cells in vitro and in NOD/SCID mice, Oncotarget, ISSN: 1949-2553, DOI: 10.18632/oncotarget.14066, Vol.8, No.6, pp.9303-9322, 2017

Streszczenie:

Anticancer therapies that induce DNA damage tend to trigger senescence in cancer cells, a process known as therapy-induced senescence (TIS). Such cells may undergo atypical divisions, thus contributing to tumor re-growth. Accumulation of senescent cancer cells reduces survival of patients after chemotherapy. As senescence interplays with autophagy, a dynamic recycling process, we sought to study whether inhibition of autophagy interferes with divisions of TIS cells. We exposed human colon cancer HCT116 cells to repeated cycles of a chemotherapeutic agent - doxorubicin (doxo) and demonstrated induction of hallmarks of TIS (e.g. growth arrest, hypertrophy, poliploidization and secretory phenotype) and certain properties of cancer stem cells (increased NANOG expression, percentages of CD24+ cells and side population). Colonies of small and highly proliferative progeny appeared shortly after drug removal. Treatment with bafilomycin A1 (BAF A1), an autophagy inhibitor, postponed short term in vitro cell re-population. It was associated with reduction in the number of diploid and increase in the number of poliploid cells. In a long term, a pulse of BAF A1 resulted in reactivation of autophagy in a subpopulation of HCT116 cells and increased proliferation. Accordingly, the senescent HCT116 cells treated with BAF A1 when injected into NOD/SCID mice formed tumors, in contrast to the controls. Our results suggest that senescent cancer cells that appear during therapy, can be considered as dormant cells that contribute to cancer re-growth, when chemotherapeutic treatment is stopped. These data unveil new mechanisms of TIS-related cancer maintenance and re-population, triggered by a single pulse of BAF A1 treatment.

Słowa kluczowe:

colon cancer, chemotherapy, senescence, autophagy, angiogenesis

Afiliacje autorów:

Was H.-Nencki Institute of Experimental Biology, Polish Academy of Sciences (PL)
Barszcz K.-Nencki Institute of Experimental Biology, Polish Academy of Sciences (PL)
Czarnecka J.-Nencki Institute of Experimental Biology, Polish Academy of Sciences (PL)
Kowalczyk A.-Nencki Institute of Experimental Biology, Polish Academy of Sciences (PL)
Bernas T.-Nencki Institute of Experimental Biology, Polish Academy of Sciences (PL)
Uzarowska E.-Nencki Institute of Experimental Biology, Polish Academy of Sciences (PL)
Koza P.-other affiliation
Klejman A.-Nencki Institute of Experimental Biology, Polish Academy of Sciences (PL)
Piwocka K.-Nencki Institute of Experimental Biology, Polish Academy of Sciences (PL)
Kaminska B.-Nencki Institute of Experimental Biology, Polish Academy of Sciences (PL)
Sikora E.-Nencki Institute of Experimental Biology, Polish Academy of Sciences (PL)
40p.
2.Kijewska M., Kocyk M., Kloss M., Stępniak K., Korwek Z., Polakowska R., Dąbrowski M., Gieryng A., Wojtas B., Ciechomska I.A., Kamińska B., The embryonic type of SPP1 transcriptional regulation is re-activated in glioblastoma, Oncotarget, ISSN: 1949-2553, DOI: 10.18632/oncotarget.14092, pp.1-16, 2016

Streszczenie:

Osteopontin (SPP1, a secreted phosphoprotein 1) is primarily involved in immune responses, tissue remodelling and biomineralization. However, it is also overexpressed in many cancers and regulates tumour progression by increasing migration, invasion and cancer stem cell self-renewal. Mechanisms of SPP1 overexpression in gliomas are poorly understood. We demonstrate overexpression of two out of five SPP1 isoforms in glioblastoma (GBM) and differential isoform expression in glioma cell lines. Up-regulated SPP1 expression is associated with binding of the GLI1 transcription factor to the promoter and OCT4 (octamer-binding transcription factor 4) to the first SPP1 intron of the SPP1 gene in human glioma cells but not in non-transformed astrocytes. GLI1 knockdown reduced SPP1 mRNA and protein levels in glioma cells. GLI1 and OCT4 are known regulators of stem cell pluripotency. GBMs contain rare cells that express stem cell markers and display ability to self-renew. We reveal that SPP1 is overexpressed in glioma initiating cells defined by high rhodamine 123 efflux, sphere forming capacity and stemness marker expression. Forced differentiation of human glioma spheres reduced SPP1 expression. Knockdown of SPP1, GLI1 or CD44 with siRNAs diminished sphere formation. C6 glioma cells stably depleted of Spp1 displayed reduced sphere forming capacity and downregulated stemness marker expression. Overexpression of the wild type Spp1, but not Spp1 lacking a Cd44 binding domain, rescued cell ability to form spheres. Our findings show re-activation of the embryonic-type transcriptional regulation of SPP1 in malignant gliomas and point to the importance of SPP1-CD44 interactions in self-renewal and pluripotency glioma initiating cells.

Słowa kluczowe:

osteopontin, glioma initiating cells, transcription factors, stemness factors, self-renewal

Afiliacje autorów:

Kijewska M.-other affiliation
Kocyk M.-Nencki Institute of Experimental Biology, Polish Academy of Sciences (PL)
Kloss M.-Nencki Institute of Experimental Biology, Polish Academy of Sciences (PL)
Stępniak K.-other affiliation
Korwek Z.-other affiliation
Polakowska R.-other affiliation
Dąbrowski M.-Nencki Institute of Experimental Biology, Polish Academy of Sciences (PL)
Gieryng A.-Nencki Institute of Experimental Biology, Polish Academy of Sciences (PL)
Wojtas B.-Nencki Institute of Experimental Biology, Polish Academy of Sciences (PL)
Ciechomska I.A.-Nencki Institute of Experimental Biology, Polish Academy of Sciences (PL)
Kamińska B.-Nencki Institute of Experimental Biology, Polish Academy of Sciences (PL)
35p.