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A catalytically inactive gelatinase B/MMP-9 mutant impairs homing of chronic lymphocytic leukemia cells by altering migration regulatory pathways

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dc.contributor.author Bailón, Elvira
dc.contributor.author Aguilera Montilla, Noemí
dc.contributor.author Gutiérrez González, Alejandra
dc.contributor.author Ugarte Berzal, Estefanía
dc.contributor.author Van den Steen, Philippe E.
dc.contributor.author Opdenakker, Ghislain
dc.contributor.author García Marco, José A.
dc.contributor.author García Pardo, Ángeles
dc.date.accessioned 2024-12-11T12:21:49Z
dc.date.available 2024-12-11T12:21:49Z
dc.date.created 2017
dc.identifier.uri https://hdl.handle.net/20.500.12080/44934
dc.description.abstract We previously showed that MMP-9 overexpression impairs migration of primary CLL cells and MEC- 1 cells transfected with MMP-9. To determine the contribution of non-proteolytic activities to this effect we generated MEC-1 transfectants stably expressing catalytically inactive MMP-9MutE (MMP-9MutE- cells). In xenograft models in mice, MMP-9MutE-cells showed impaired homing to spleen and bone marrow, compared to cells transfected with empty vector (Mock-cells). In vitro transendothelial and random migration of MMP-9MutE-cells were also reduced. Biochemical analyses indicated that RhoAGTPase and p-Akt were not downregulated by MMP-9MutE, at difference with MMP-9. However, MMP-9MutE-cells or primary cells incubated with MMP-9MutE had significantly reduced p-ERK and increased PTEN, accounting for the impaired migration. Our results emphasize the role of non-proteolytic MMP-9 functions contributing to CLL progression. es_ES
dc.format application/pdf es_ES
dc.language eng es_ES
dc.rights CC-BY es_ES
dc.rights.uri http://creativecommons.org/licenses/by/4.0/deed.es es_ES
dc.title A catalytically inactive gelatinase B/MMP-9 mutant impairs homing of chronic lymphocytic leukemia cells by altering migration regulatory pathways es_ES
dc.type info:eu-repo/semantics/article es_ES
dc.rights.accessrights info:eu-repo/semantics/restrictedAccess es_ES
dc.identifier.location N/A es_ES


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