PO.ET02.11 · 实验与分子治疗

Evaluation of HERV-K as an unusual cancer therapeutic target

海报缩略图:Evaluation of HERV-K as an unusual cancer therapeutic target
编号 445 展板 15 时间 4/19 02:00–05:00 区域 Section 18 主讲 Monica Gordon, PhD
分会场 Novel Therapeutics and Drug Targets 1
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作者与单位

Monica Gordon1, James H. Torpey2, Andy D. Martin2, Benjamin R. Miller2, Marica Speranza3, Kenneth W. Hance4

1Oncology ETCT BU, GlaxoSmithKline plc, Stevenage, United Kingdom,2GlaxoSmithKline plc, Stevenage, United Kingdom,3Oncology ETCT BU, Glaxosmithkline, Boston, MA,4GlaxoSmithKline, Malvern, PA

摘要 Abstract

Human endogenous retroviruses (HERVs) are abundant genomic elements, transcriptionally repressed under normal physiological conditions. However, epigenetic alterations during disease reactivate HERV expression. HERV-K, specifically, has been identified as prevalent in numerous tumor types, including prostate, lung, breast, colon, and ovarian cancers and its presence correlates with tumor progression and protumoral signalling. In addition, HERV-K's immunosuppressive role in the placenta, where it is usually expressed, points to a potential similar function within the tumor microenvironment, making it an attractive therapeutic target. We have comprehensively evaluated HERV-K as a potential target for T-cell Engagers (TCEs) and Antibody-Drug Conjugates (ADCs). This evaluation has been limited by the availability of tool antibodies. Employing flow cytometry and immunohistochemistry (IHC), HERV-K expression on the tumor cell surface was consistently low and unstable, often lost upon enzymatic cell detachment, indicating susceptibility to proteolytic cleavage. Receptor quantification on HERV-K+ tumor cell lines varied from 0-25,000 receptors per cell. IHC results confirmed low membranous staining across various tumor types, with a significant proportion of the protein detected in the cytoplasm, and thus, not available for antibody engagement. In vitro functional evaluation was performed by generating HERV-K tool TCEs and ADCs. While HERV-K TCEs demonstrated moderate and specific tumor cytotoxicity, HERV-K tool ADCs did not elicit HERV-K-dependent cytotoxic effects. In conclusion, while HERV-K presents an intriguing opportunity due to its tumor-selective expression, its inconsistent and labile surface presentation poses considerable challenges. Our findings suggest that HERV-K may be a viable target for TCE-based therapies, but less so for ADCs, primarily due to insufficient receptor density. Future efforts necessitate the development of high-quality specific antibodies to fully harness HERV-K's therapeutic potential in cancer. Note: Human biological samples were sourced ethically, and their research use was in accord with the terms of the informed consents. IHC experiments were done by DLS.
利益披露 Disclosure
M. Gordon, GSK Employment. J. H. Torpey, GSK Employment. A. D. Martin, GSK Employment. B. R. Miller, GSK Employment. M. Speranza, GSK Employment.

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