MMP activities are controlled by a combination of proteolytic pro-enzyme activation steps and inhibition by endogenous inhibitors like α2-macroglobulin and the tissue inhibitors of metalloproteinases (TIMPs). TIMPs are the key inhibitors in tissue. The expression of both MMPs and TIMPs is controlled during tissue remodeling to maintain a balance in the turnover of extracellular matrix. Disruption of this balance may result in a broad spectrum of diseases. Additionally, TIMP-2 has been reported to have growth factor activities. To further study the function of TIMP-2 in development, we utilized zebrafish as an experimental model system. We have successfully isolated a TIMP-2 homologue from zebrafish (zTIMP-2). This zebrafish TIMP-2 showed high similarity to human TIMP-2 with all critical features conserved. Whole-mount in situ analysis showed that zTIMP-2 was expressed as early as the one-cell stage indicating a maternal origin. This expression continued through later stages of development. RT-PCR analysis confirmed the early expression pattern from the 16-cell stage through blastula, gastrula and 24-h stages. In addition, at the protein level, immunoreactive zTIMP-2 was detected using antibody against recombinant human TIMP-2. RFP-reporter analysis indicated that TIMP-2 can be secreted into the extracellular space where ECM is forming. Functional studies showed that the balance of TIMP-2 expression is important to normal development as reflected by the fact that both blockage of TIMP-2 translation using antisense morpholino oligonculeotides or increased translation of TIMP-2 using a mRNA microinjection approach resulted in abnormal zebrafish development. This is in contrast to murine knockout studies that indicate that TIMP-2 does not have a major role in mouse embryogenesis.
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Univ Copenhagen, Dept Biomed Sci, DK-2200 Copenhagen, Denmark
Univ Copenhagen, BRIC, DK-2200 Copenhagen, DenmarkUniv Cambridge, Dept Oncol, Canc Res Inst, Li Ka Shing Ctr, Cambridge CB2 ORE, England
Kveiborg, Marie
Jacobsen, Jonas
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Univ Copenhagen, Dept Biomed Sci, DK-2200 Copenhagen, Denmark
Univ Copenhagen, BRIC, DK-2200 Copenhagen, DenmarkUniv Cambridge, Dept Oncol, Canc Res Inst, Li Ka Shing Ctr, Cambridge CB2 ORE, England
Jacobsen, Jonas
Lee, Meng-Huee
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Univ Cambridge, Dept Oncol, Canc Res Inst, Li Ka Shing Ctr, Cambridge CB2 ORE, EnglandUniv Cambridge, Dept Oncol, Canc Res Inst, Li Ka Shing Ctr, Cambridge CB2 ORE, England
Lee, Meng-Huee
Nagase, Hideaki
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Univ London Imperial Coll Sci Technol & Med, Fac Med, Kennedy Inst, Div Rheumatol, London W6 8LH, EnglandUniv Cambridge, Dept Oncol, Canc Res Inst, Li Ka Shing Ctr, Cambridge CB2 ORE, England
Nagase, Hideaki
Wewer, Ulla M.
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Univ Copenhagen, Dept Biomed Sci, DK-2200 Copenhagen, Denmark
Univ Copenhagen, BRIC, DK-2200 Copenhagen, DenmarkUniv Cambridge, Dept Oncol, Canc Res Inst, Li Ka Shing Ctr, Cambridge CB2 ORE, England
Wewer, Ulla M.
Murphy, Gillian
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Univ Cambridge, Dept Oncol, Canc Res Inst, Li Ka Shing Ctr, Cambridge CB2 ORE, EnglandUniv Cambridge, Dept Oncol, Canc Res Inst, Li Ka Shing Ctr, Cambridge CB2 ORE, England