The immunoconjugate "icon" targets aberrantly expressed endothelial tissue factor causing regression of endometriosis

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This study reports that the immunoconjugate Icon, targeting aberrantly expressed endothelial tissue factor, largely destroyed endometriotic implants in a mouse model by disrupting existing blood vessels without toxicity or fertility effects.

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Abstract

Endometriosis is a major cause of chronic pain, infertility, medical and surgical interventions, and health care expenditures. Tissue factor (TF), the primary initiator of coagulation and a modulator of angiogenesis, is not normally expressed by the endothelium; however, prior studies have demonstrated that both blood vessels in solid tumors and choroidal tissue in macular degeneration express endothelial TF. The present study describes the anomalous expression of TF by endothelial cells in endometriotic lesions. The immunoconjugate molecule (Icon), which binds with high affinity and specificity to this aberrant endothelial TF, has been shown to induce a cytolytic immune response that eradicates tumor and choroidal blood vessels. Using an athymic mouse model of endometriosis, we now report that Icon largely destroys endometriotic implants by vascular disruption without apparent toxicity, reduced fertility, or subsequent teratogenic effects. Unlike antiangiogenic treatments that can only target developing angiogenesis, Icon eliminates pre-existing pathological vessels. Thus, Icon could serve as a novel, nontoxic, fertility-preserving, and effective treatment for endometriosis.

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Condition tags

endometriosisinfertility

MeSH descriptors

Endometriosis Immunoconjugates Neovascularization, Pathologic Peritoneal Diseases Thromboplastin Thromboplastin Adult Animals CHO Cells Cricetinae Cricetulus Drug Delivery Systems Endometriosis Endometriosis Endometriosis Endothelium, Vascular Endothelium, Vascular Endothelium, Vascular Female Humans

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Source provenance

europepmc
last seen: 2026-06-17T06:13:18.893374+00:00
pubmed
last seen: 2026-05-13T22:17:24.614948+00:00
unpaywall
last seen: 2026-05-14T19:30:52.867331+00:00
License: Public-Domain · commercial use OK · attribution required
Courtesy of the U.S. National Library of Medicine