Consensus micro RNAs governing the switch of dormant tumors to the fast-growing angiogenic phenotype.

Consensus micro RNAs governing the switch of dormant tumors to the fast-growing angiogenic phenotype.

Tumor dormancy refers to a critical stage in cancer development in which tumor cells remain occult for a prolonged period of time until they eventually progress and become clinically apparent. We previously showed that the switch of dormant tumors to fast-growth is angiogenesis dependent and require...

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Main Authors: Nava Almog, Lili Ma, Christian Schwager, Bastian G Brinkmann, Afshin Beheshti, Peter Vajkoczy, Judah Folkman, Lynn Hlatky, Amir Abdollahi
Format: Article
Language:English
Published: Public Library of Science (PLoS) 2012-01-01
Series:PLoS ONE
Online Access:http://europepmc.org/articles/PMC3432069?pdf=render
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spelling doaj-252efcd0b5cf401a919017eb0ada60192020-11-25T01:46:41ZengPublic Library of Science (PLoS)PLoS ONE1932-62032012-01-0178e4400110.1371/journal.pone.0044001Consensus micro RNAs governing the switch of dormant tumors to the fast-growing angiogenic phenotype.Nava AlmogLili MaChristian SchwagerBastian G BrinkmannAfshin BeheshtiPeter VajkoczyJudah FolkmanLynn HlatkyAmir AbdollahiTumor dormancy refers to a critical stage in cancer development in which tumor cells remain occult for a prolonged period of time until they eventually progress and become clinically apparent. We previously showed that the switch of dormant tumors to fast-growth is angiogenesis dependent and requires a stable transcriptional reprogramming in tumor cells. Considering microRNAs (miRs) as master regulators of transcriptome, we sought to investigate their role in the control of tumor dormancy. We report here the identification of a consensus set of 19 miRs that govern the phenotypic switch of human dormant breast carcinoma, glioblastoma, osteosarcoma, and liposarcoma tumors to fast-growth. Loss of expression of dormancy-associated miRs (DmiRs, 16/19) was the prevailing regulation pattern correlating with the switch of dormant tumors to fast-growth. The expression pattern of two DmiRs (miR-580 and 190) was confirmed to correlate with disease stage in human glioma specimens. Reconstitution of a single DmiR (miR-580, 588 or 190) led to phenotypic reversal of fast-growing angiogenic tumors towards prolonged tumor dormancy. Of note, 60% of angiogenic glioblastoma and 100% of angiogenic osteosarcoma over-expressing miR190 remained dormant during the entire observation period of ∼ 120 days. Next, the ability of DmiRs to regulate angiogenesis and dormancy-associated genes was evaluated. Transcriptional reprogramming of tumors via DmiR-580, 588 or 190 over-expression resulted in downregulation of pro-angiogenic factors such as TIMP-3, bFGF and TGFalpha. In addition, a G-CSF independent downregulation of Bv8 was found as a common target of all three DmiRs and correlated with decreased tumor recruitment of bone marrow-derived CD11b+ Gr-1+ myeloid cells. In contrast, antiangiogenic and dormancy promoting pathways such as EphA5 and Angiomotin were upregulated in DmiR over-expressing tumors. This work suggests novel means to reverse the malignant tumor phenotype into an asymptomatic dormant state and may provide promising targets for early detection or prevention of cancer.http://europepmc.org/articles/PMC3432069?pdf=render
collection DOAJ
language English
format Article
sources DOAJ
author Nava Almog
Lili Ma
Christian Schwager
Bastian G Brinkmann
Afshin Beheshti
Peter Vajkoczy
Judah Folkman
Lynn Hlatky
Amir Abdollahi
spellingShingle Nava Almog
Lili Ma
Christian Schwager
Bastian G Brinkmann
Afshin Beheshti
Peter Vajkoczy
Judah Folkman
Lynn Hlatky
Amir Abdollahi
Consensus micro RNAs governing the switch of dormant tumors to the fast-growing angiogenic phenotype.
PLoS ONE
author_facet Nava Almog
Lili Ma
Christian Schwager
Bastian G Brinkmann
Afshin Beheshti
Peter Vajkoczy
Judah Folkman
Lynn Hlatky
Amir Abdollahi
author_sort Nava Almog
title Consensus micro RNAs governing the switch of dormant tumors to the fast-growing angiogenic phenotype.
title_short Consensus micro RNAs governing the switch of dormant tumors to the fast-growing angiogenic phenotype.
title_full Consensus micro RNAs governing the switch of dormant tumors to the fast-growing angiogenic phenotype.
title_fullStr Consensus micro RNAs governing the switch of dormant tumors to the fast-growing angiogenic phenotype.
title_full_unstemmed Consensus micro RNAs governing the switch of dormant tumors to the fast-growing angiogenic phenotype.
title_sort consensus micro rnas governing the switch of dormant tumors to the fast-growing angiogenic phenotype.
publisher Public Library of Science (PLoS)
series PLoS ONE
issn 1932-6203
publishDate 2012-01-01
description Tumor dormancy refers to a critical stage in cancer development in which tumor cells remain occult for a prolonged period of time until they eventually progress and become clinically apparent. We previously showed that the switch of dormant tumors to fast-growth is angiogenesis dependent and requires a stable transcriptional reprogramming in tumor cells. Considering microRNAs (miRs) as master regulators of transcriptome, we sought to investigate their role in the control of tumor dormancy. We report here the identification of a consensus set of 19 miRs that govern the phenotypic switch of human dormant breast carcinoma, glioblastoma, osteosarcoma, and liposarcoma tumors to fast-growth. Loss of expression of dormancy-associated miRs (DmiRs, 16/19) was the prevailing regulation pattern correlating with the switch of dormant tumors to fast-growth. The expression pattern of two DmiRs (miR-580 and 190) was confirmed to correlate with disease stage in human glioma specimens. Reconstitution of a single DmiR (miR-580, 588 or 190) led to phenotypic reversal of fast-growing angiogenic tumors towards prolonged tumor dormancy. Of note, 60% of angiogenic glioblastoma and 100% of angiogenic osteosarcoma over-expressing miR190 remained dormant during the entire observation period of ∼ 120 days. Next, the ability of DmiRs to regulate angiogenesis and dormancy-associated genes was evaluated. Transcriptional reprogramming of tumors via DmiR-580, 588 or 190 over-expression resulted in downregulation of pro-angiogenic factors such as TIMP-3, bFGF and TGFalpha. In addition, a G-CSF independent downregulation of Bv8 was found as a common target of all three DmiRs and correlated with decreased tumor recruitment of bone marrow-derived CD11b+ Gr-1+ myeloid cells. In contrast, antiangiogenic and dormancy promoting pathways such as EphA5 and Angiomotin were upregulated in DmiR over-expressing tumors. This work suggests novel means to reverse the malignant tumor phenotype into an asymptomatic dormant state and may provide promising targets for early detection or prevention of cancer.
url http://europepmc.org/articles/PMC3432069?pdf=render
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