Journal of Ovarian Research (Apr 2024)

Sialyl-Tn serves as a potential therapeutic target for ovarian cancer

  • Linah Al-Alem,
  • Jillian M. Prendergast,
  • Justin Clark,
  • Bianca Zarrella,
  • Dominique T. Zarrella,
  • Sarah J. Hill,
  • Whitfield B. Growdon,
  • Venkatesh Pooladanda,
  • David R. Spriggs,
  • Daniel Cramer,
  • Kevin M. Elias,
  • Rawan I. Nazer,
  • Steven J. Skates,
  • Jeff Behrens,
  • Daniel T. Dransfield,
  • Bo R. Rueda

DOI
https://doi.org/10.1186/s13048-024-01397-1
Journal volume & issue
Vol. 17, no. 1
pp. 1 – 16

Abstract

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Abstract Background Ovarian cancer remains the deadliest of the gynecologic cancers in the United States. There have been limited advances in treatment strategies that have seen marked increases in overall survival. Thus, it is essential to continue developing and validating new treatment strategies and markers to identify patients who would benefit from the new strategy. In this report, we sought to further validate applications for a novel humanized anti-Sialyl Tn antibody-drug conjugate (anti-STn-ADC) in ovarian cancer. Methods We aimed to further test a humanized anti-STn-ADC in sialyl-Tn (STn) positive and negative ovarian cancer cell line, patient-derived organoid (PDO), and patient-derived xenograft (PDX) models. Furthermore, we sought to determine whether serum STn levels would reflect STn positivity in the tumor samples enabling us to identify patients that an anti-STn-ADC strategy would best serve. We developed a custom ELISA with high specificity and sensitivity, that was used to assess whether circulating STn levels would correlate with stage, progression-free survival, overall survival, and its value in augmenting CA-125 as a diagnostic. Lastly, we assessed whether the serum levels reflected what was observed via immunohistochemical analysis in a subset of tumor samples. Results Our in vitro experiments further define the specificity of the anti-STn-ADC. The ovarian cancer PDO, and PDX models provide additional support for an anti-STn-ADC-based strategy for targeting ovarian cancer. The custom serum ELISA was informative in potential triaging of patients with elevated levels of STn. However, it was not sensitive enough to add value to existing CA-125 levels for a diagnostic. While the ELISA identified non-serous ovarian tumors with low CA-125 levels, the sample numbers were too small to provide any confidence the STn ELISA would meaningfully add to CA-125 for diagnosis. Conclusions Our preclinical data support the concept that an anti-STn-ADC may be a viable option for treating patients with elevated STn levels. Moreover, our STn-based ELISA could complement IHC in identifying patients with whom an anti-STn-based strategy might be more effective.

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