CD25-Targeted Aptamer-Drug Conjugate for the Treatment of CD25-Expressing Hematological Malignancies

  • Pharmaceutics. 2026 Feb 9;18(2):217. doi: 10.3390/pharmaceutics18020217.
Sanghyeok Woo  1 Ju-Hyung Kang  1 Inu Song  1 Soryong Lim  1 Hwarim Ryu  1 Yujin Lee  1 Daekyun Lee  1
Affiliations
  • 1. Aptamer Sciences Inc., 15, Pangyo-ro 228beon-gil, Seongnam-si 13487, Republic of Korea.
Abstract

Background: CD25, the α-chain of the interleukin-2 (IL-2) receptor, is highly expressed on malignant cells and tumor-infiltrating regulatory T-cells (Tregs) in hematologic malignancies, making it an attractive therapeutic target for tumor elimination and immunomodulation. Methods: We developed a CD25-specific aptamer-drug conjugate (CD25-ApDC) by linking a CD25 aptamer to monomethyl Auristatin E via a Cathepsin B-cleavable Val-Cit linker. Results: The aptamer exhibited high affinity for CD25 (Kd = 16.4 ± 0.29 nM), rapid receptor-mediated uptake (half-time = 9.6 min), and selective inhibition of IL-2 signaling in CD25high cells, with no activity in CD25low cells. In vitro, CD25-ApDC induced selective cytotoxicity, confirmed by Apoptosis and G2/M arrest in CD25-positive Cancer cells while having no effect on CD25-negative cells. Co-culture studies confirmed selective depletion of CD25high Treg-like cells, suggesting potential to relieve immune suppression within the tumor microenvironment. In vivo, CD25-ApDC achieved complete tumor remission in xenograft and disseminated models with optimized dosing, showing efficacy and tolerability comparable to Brentuximab vedotin. Increasing drug-to-aptamer ratios further enhanced outcomes, supporting flexible dosing strategies. Conclusions: These findings highlight CD25-ApDC as a promising therapeutic modality for hematologic malignancies, offering advantages in specificity, tissue penetration, and manufacturability over conventional antibody-based therapies.

Keywords
CD25; SELEX; aptamer; aptamer–drug conjugate; hematologic malignancies; monomethyl auristatin E; targeted therapy.
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