The invention describes methods for inhibiting angiogenesis in a tissue by
administering an antagonist that specifically binds to a proteolyzed or
denatured collagen type-IV with substantially greater affinity than to
the native triple helical form of collagen type-IV. Methods utilizing
such antagonists for therapeutic treatment of tumor growth, tumor
metastasis or of restenosis also are described, as are methods to use
such antagonists as diagnostic markers of angiogenesis in normal or
diseased tissues both in vivo and ex vivo.