Erratum: Corrigendum: Positively selected enhancer elements endow osteosarcoma cells with metastatic competence

Morrow, James J.; Bayles, Ian; Funnell, Alister P. W.; Miller, Tyler E.; Saiakhova, Alina; Lizardo, Michael M.; Bartels, Cynthia F.; Kapteijn, Maaike Y.; Hung, Stevephen; Mendoza, Arnulfo; Dhillon, Gursimran; Chee, Daniel R.; Myers, Jay; Allen, Frederick H.; Gambarotti, Marco; Righi, Alberto; DiFeo, Analisa; Rubin, Brian P.; Huang, Alex Yee-Chen; Meltzer, Paul S.; Helman, Lee J.; Picci, Piero; Versteeg, Henri H.; Stamatoyannopoulos, J; Khanna, Chand; Scacheri, Peter C.

doi:10.1038/nm0418-525c

Cited by 5 publications

(3 citation statements)

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“…TF expression is also up to 1000-fold greater in metastatic cells than in non-metastatic cells [163]. An unbiased shRNA screen showed that TF is one of the most powerful drivers of metastasis in osteosarcoma [164]. Such correlative findings have been verified by functional studies in vivo [23,163,165].…”

Section: Invasion and Metastasismentioning

confidence: 86%

Beyond thrombosis: the impact of tissue factor signaling in cancer

Unruh

Horbinski

2020

J Hematol Oncol

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Tissue factor (TF) is the primary initiator of the coagulation cascade, though its effects extend well beyond hemostasis. When TF binds to Factor VII, the resulting TF:FVIIa complex can proteolytically cleave transmembrane G protein-coupled proteaseactivated receptors (PARs). In addition to activating PARs, TF:FVIIa complex can also activate receptor tyrosine kinases (RTKs) and integrins. These signaling pathways are utilized by tumors to increase cell proliferation, angiogenesis, metastasis, and cancer stem-like cell maintenance. Herein, we review in detail the regulation of TF expression, mechanisms of TF signaling, their pathological consequences, and how it is being targeted in experimental cancer therapeutics.

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Section: Invasion and Metastasismentioning

confidence: 86%

Beyond thrombosis: the impact of tissue factor signaling in cancer

Unruh

Horbinski

2020

J Hematol Oncol

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“…Osteosarcoma (OS), the most common and aggressive type of primary malignant bone tumor, arises most often in children and adolescents 1,2 . It is derived from interstitial tissue and is characterized by heterogeneity, rapid progression, and a high risk of metastasis, primarily to the lungs 3 . Nevertheless, the underlying molecular mechanisms of OS pathogenesis remain elusive.…”

Section: Introductionmentioning

confidence: 99%

“… 1 , 2 It is derived from interstitial tissue and is characterized by heterogeneity, rapid progression, and a high risk of metastasis, primarily to the lungs. 3 Nevertheless, the underlying molecular mechanisms of OS pathogenesis remain elusive. Hence, it is imperative to investigate the underlying mechanism and develop novel effective targets for the treatment of OS.…”

Section: Introductionmentioning

confidence: 99%

LncRNA‐HOTAIRM1 promotes aerobic glycolysis and proliferation in osteosarcoma via the miR‐664b‐3p/Rheb/mTOR pathway

Duan

et al. 2023

Cancer Science

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Osteosarcoma (OS), which is a common and aggressive primary bone malignancy, occurs mainly in children and adolescent. Long noncoding RNAs (lncRNAs) are reported to play a pivotal role in various cancers. Here, we found that the lncRNA HOTAIRM1 is upregulated in OS cells and tissues. A set of functional experiments suggested that HOTAIRM1 knockdown attenuated the proliferation and stimulated the apoptosis of OS cells. A subsequent mechanistic study revealed that HOTAIRM1 functions as a competing endogenous RNA to elevate ras homologue enriched in brain (Rheb) expression by sponging miR‐664b‐3p. Immediately afterward, upregulated Rheb facilitates proliferation and suppresses apoptosis by promoting the mTOR pathway‐mediated Warburg effect in OS. In summary, our findings demonstrated that HOTAIRM1 promotes the proliferation and suppresses the apoptosis of OS cells by enhancing the Warburg effect via the miR‐664b‐3p/Rheb/mTOR axis. Understanding the underlying mechanisms and targeting the HOTAIRM1/miR‐664b‐3p/Rheb/mTOR axis are essential for OS clinical treatment.

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