Michael B. Berman scite author profile

The role of tissue-type plasminogen activator (tPA) in the 'spontaneous' as well as 'experimental' metastasis of ocular melanomas in mice was evaluated by transfecting the D5.1G4 murine melanoma cell line that possesses low metastatic activity and low tPA activity with a full length cDNA encoding human tPA. For comparison, a highly metastatic melanoma cell line (Queen's) that constitutively expresses high tPA production, was transfected with a cDNA coding for human plasminogen activator inhibitor type 1 (PAI-1). Unlike non-transfected controls, transfected D5.1G4 melanoma cells expressed high levels of tPA and produced extensive pulmonary metastases following intravenous injection. By contrast, PAI-1 transfected Queen's melanoma cells expressed low tPA activity and displayed significantly reduced metastatic potential compared with nontransfected controls. Moreover, PAI-1 transfected Queen's melanoma cells did not metastasize from the eye while nontransfected parental cells produced extensive spontaneous metastases. Expression of tPA activity in transfected and nontransfected cell lines was completely blocked by an anti-tPA antibody. This antibody significantly inhibited the organ localization and frequency of lung metastases of both Queen's and tPA-transfected D5.1G4 melanomas. This study demonstrates that tPA is involved in the metastasis of murine intraocular melanomas.

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The pathogenesis of corneal epithelial defects

Berman

1989

Acta Ophthalmologica

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Michael B. Berman

Effect of Topical Corticosteroids on Ulceration in Alkali-Burned Corneas

Regulation of Corneal Fibroblast MMP-1 Collagenase Secretion by Plasmin

Corneal ulceration and the serum antiproteases. II. Complexes of corneal collagenases of α-macroglobulins

Tissue-type plasminogen activator-induced invasion and metastasis of murine melanomas

The pathogenesis of corneal epithelial defects

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