Plasminogen binding and activation at the breast cancer cell surface: the integral role of urokinase activity

Stillfried, Gillian E.; Saunders, Darren N.; Ranson, Marie

doi:10.1186/bcr1647

Cited by 64 publications

(52 citation statements)

References 62 publications

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“…Peptide 18-36 blocked the cell surface binding by 45% compared to scrambled peptide ( Figure 3A). Because it had been shown before that a direct interaction between uPA and Plg was necessary for Plg activation on the cell surface, 30,31 we tested whether sM6P/IGF2R and peptide 18-36 were able to block this interaction. An in vitro binding assay revealed that similarly to TA, sM6P/IGF2R and peptide 18-36 both blocked the interaction between Plg and uPA ( Figure 3B).…”

Section: Sm6p/igf2r and Peptide 18-36 Have A Similar Negative Regulatmentioning

confidence: 99%

Soluble M6P/IGF2R Released by TACE Controls Angiogenesis via Blocking Plasminogen Activation

Leksa

Loewe

Binder

et al. 2011

Circulation Research

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Rationale:The urokinase plasminogen activator (uPA) system is among the most crucial pericellular proteolytic systems associated with the processes of angiogenesis. We previously identified an important regulator of the uPA system in the mannose 6-phosphate/insulin-like growth factor 2 receptor (M6P/IGF2R).Objective: Here, we wanted to clarify whether and how did the soluble form of M6P/IGF2R (sM6P/IGF2R) contribute to modulation of the uPA system. Methods and Results:

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Section: Sm6p/igf2r and Peptide 18-36 Have A Similar Negative Regulatmentioning

confidence: 99%

Soluble M6P/IGF2R Released by TACE Controls Angiogenesis via Blocking Plasminogen Activation

Leksa

Loewe

Binder

et al. 2011

Circulation Research

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“…It was found that the proteolytic activity of uPA is closely related to cell-surface events when incubated with the breast cancer cells. MCF-7 had low uPAR/uPA-expressing and low plasminogen-binding, whereas MDA-MB-231 had high uPAR/uPA expressing and high plasminogen binding 29 . Due to synthesized peptides would be rather nontoxic to MCF-7 cancer cells.…”

Section: Resultsmentioning

confidence: 99%

Tripeptides with non-code amino acids as potential serine proteases inhibitors

Markowska

Bruzgo²,

Surażyński

et al. 2012

Journal of Enzyme Inhibition and Medicinal Chemistry

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“…The interpretation of this result may be that cells of benign tissue lumps can expose a number of molecules, which participate in Plg/AS binding with cellular surface. A variety of proteins, including actin, annexin II, S100A10, cytokeratin 8, tetranectin and αenolase have been identified as potential Plg receptors on the surface of certain types of human breast cancer cells [30]. AS appeared to effectively interact with some Plg receptors.…”

Section: Fig 3 Gelatin Zymography Of Protein Samples Obtained From mentioning

confidence: 99%

Plasminogen and angiostatin levels in female benign breast lesions

Tykhomyrov¹,

Вовчук²,

Grinenko³

2015

Ukr.Biochem.J.

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Plasminogen binding and activation at the breast cancer cell surface: the integral role of urokinase activity

Cited by 64 publications

References 62 publications

Soluble M6P/IGF2R Released by TACE Controls Angiogenesis via Blocking Plasminogen Activation

Soluble M6P/IGF2R Released by TACE Controls Angiogenesis via Blocking Plasminogen Activation

Tripeptides with non-code amino acids as potential serine proteases inhibitors

Plasminogen and angiostatin levels in female benign breast lesions

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