| Literature DB >> 27903863 |
Daniel L J Thorek1,2, Philip A Watson3, Sang-Gyu Lee2, Anson T Ku2, Stylianos Bournazos4, Katharina Braun5, Kwanghee Kim6, Kjell Sjöström7, Michael G Doran2, Urpo Lamminmäki8, Elmer Santos2, Darren Veach2,9, Mesruh Turkekul10, Emily Casey11, Jason S Lewis11,12, Diane S Abou1, Marise R H van Voss1,13, Peter T Scardino6,14, Sven-Erik Strand15, Mary L Alpaugh16, Howard I Scher17,18, Hans Lilja19,17,20,21,22, Steven M Larson23,9, David Ulmert19,11,24.
Abstract
Targeting the androgen receptor (AR) pathway prolongs survival in patients with prostate cancer, but resistance rapidly develops. Understanding this resistance is confounded by a lack of noninvasive means to assess AR activity in vivo. We report intracellular accumulation of a secreted antigen-targeted antibody (SATA) that can be used to characterize disease, guide therapy, and monitor response. AR-regulated human kallikrein-related peptidase 2 (free hK2) is a prostate tissue-specific antigen produced in prostate cancer and androgen-stimulated breast cancer cells. Fluorescent and radio conjugates of 11B6, an antibody targeting free hK2, are internalized and noninvasively report AR pathway activity in metastatic and genetically engineered models of cancer development and treatment. Uptake is mediated by a mechanism involving the neonatal Fc receptor. Humanized 11B6, which has undergone toxicological tests in nonhuman primates, has the potential to improve patient management in these cancers. Furthermore, cell-specific SATA uptake may have a broader use for molecularly guided diagnosis and therapy in other cancers.Entities:
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Year: 2016 PMID: 27903863 PMCID: PMC5568040 DOI: 10.1126/scitranslmed.aaf2335
Source DB: PubMed Journal: Sci Transl Med ISSN: 1946-6234 Impact factor: 17.956