First in human phase 1 study of DT2216, a selective BCL-xL degrader, in patients with relapsed/refractory solid malignancies

Small molecule inhibition of BCL-XL with navitoclax resulted in on-target dose-limiting thrombocytopenia. DT2216 was more effective than navitoclax and reduced platelet toxicity in preclinical models by selectively degrading BCL-XL via the VHL E3 ligase, which is minimally expressed in platelets. A dose escalation study using a 3 + 3 design with doses ranging from 0.04 to 0.4 mg/kg IV twice weekly (BIW) was performed. Eligible subjects had solid tumors of any histology that had progressed on standard treatment and had measurable tumor by RECIST v1.1. Tumor assessment was performed at 8-week intervals. BCL-XL levels were measured in peripheral leukocytes by western blotting. Twenty patients were enrolled, with a median age of 60.5 year; 60% were female. Only one dose-limiting toxicity was observed, grade 4 thrombocytopenia that resolved within 48 h. Stable disease, observed in 20% of the patients. The lowest platelet count in the first cycle ranged from 24,000 to 297,000. In all cases, the platelet count recovered to > 50,000 within 4 days and > 75,000 within 1 week. There were no episodes of bleeding or treatment emergent adverse events leading to death. The median overall survival was 7.9 months. The plasma AUC of DT2216 was dose proportional with no dose accumulation. Patients receiving 0.4 mg/kg DT2216 demonstrated rapid and sustained degradation of BCL-XL. Based on the rapid recovery of transient thrombocytopenia that occurred only in the first cycle and the degradation of BCL-XL in peripheral leukocytes, the RP2D of DT2216 is 0.4 mg/kg IV BIW. (NCT04886622)

• Publication year

  2025

• Venue

  Journal of Hematology & Oncology

• Publication date

  2025-11-12

• Fields of study

  Medicine

• Identifiers
  DOI 10.1186/s13045-025-01753-8PMID 41225624PMCID 12613848
• External record

  Open on Semantic Scholar

• Source metadata

  Semantic Scholar, PubMed

• No claims are published for this paper.

• No concepts are published for this paper.

• Efficacy of a novel BCL-xL degrader, DT2216, in preclinical models of JAK2-mutated post-MPN AML

  2025cited by this paper
• Paclitaxel-induced mitotic arrest results in a convergence of apoptotic dependencies that can be safely exploited by BCL-XL degradation to overcome cancer chemoresistance

  2025cited by this paper
• A pan-KRAS degrader for the treatment of KRAS-mutant cancers

  2024cited by this paper
• TMEM63B channel is the osmosensor required for thirst drive of interoceptive neurons

  2024cited by this paper
• Corrigendum to Targeting apoptotic pathways for cancer therapy

  2024cited by this paper
• Targeting Ikaros and Aiolos: reviewing novel protein degraders for the treatment of multiple myeloma, with a focus on iberdomide and mezigdomide

  2024cited by this paper
• Oral Estrogen Receptor PROTAC Vepdegestrant (ARV-471) Is Highly Efficacious as Monotherapy and in Combination with CDK4/6 or PI3K/mTOR Pathway Inhibitors in Preclinical ER+ Breast Cancer Models

  2024cited by this paper
• PROTAC-Mediated Dual Degradation of BCL-xL and BCL-2 Is a Highly Effective Therapeutic Strategy in Small-Cell Lung Cancer

  2024cited by this paper
• First Results from a Phase 1, First-in-Human Study of the Bruton's Tyrosine Kinase (BTK) Degrader Bgb-16673 in Patients (Pts) with Relapsed or Refractory (R/R) B-Cell Malignancies (BGB-16673-101)

  2023cited by this paper
• Targeting BCL-XL in fibrolamellar hepatocellular carcinoma

  2022cited by this paper
• BCL-XL PROTAC degrader DT2216 synergizes with sotorasib in preclinical models of KRASG12C-mutated cancers

  2022cited by this paper
• Strategies to Reduce the On‐Target Platelet Toxicity of Bcl‐xL Inhibitors: PROTACs, SNIPERs and Prodrug‐Based Approaches

  2022cited by this paper
• Co-targeting BCL-XL and MCL-1 with DT2216 and AZD8055 synergistically inhibit small-cell lung cancer growth without causing on-target toxicities in mice

  2022cited by this paper
• Overcoming Gemcitabine Resistance in Pancreatic Cancer Using the BCL-XL–Specific Degrader DT2216

  2021cited by this paper
• A selective BCL-XL PROTAC degrader achieves safe and potent antitumor activity

  2019cited by this paper
• From basic apoptosis discoveries to advanced selective BCL-2 family inhibitors

  2017cited by this paper
• Bcl-2 family of proteins as drug targets for cancer chemotherapy: the long way of BH3 mimetics from bench to bedside.

  2015cited by this paper
• Structure-guided design of a selective BCL-X(L) inhibitor.

  2013cited by this paper
• ABT-199, a potent and selective BCL-2 inhibitor, achieves antitumor activity while sparing platelets

  2013cited by this paper
• Programmed anuclear cell death delimits platelet life span.

  2007cited by this paper
• An informatics approach identifying markers of chemosensitivity in human cancer cell lines.

  2000cited by this paper

• The combination of BCL-xL PROTAC and mTOR inhibitor sensitizes pancreatic ductal adenocarcinoma to KRASG12D inhibitor treatment by enhancing apoptosis induction

  2026cites this paper
• PROTAC-mediated degradation of Bcl-xL potentiates target therapy in preclinical melanoma models

  2026cites this paper
• The ubiquitination–autophagy axis in cancer therapy resistance: mechanistic insights and therapeutic opportunities

  2026cites this paper
• New-generation advanced nano-PROTACs as potential therapeutic agents in cancer therapy.

  2026cites this paper