DT2216—a Bcl-xL-specific degrader is highly active against Bcl-xL-dependent T cell lymphomas

He, Yonghan; Koch, Raphael; Budamagunta, Vivekananda; Zhang, Peiyi; Zhang, Xuan; Khan, Sajid; Thummuri, Dinesh; Ortiz, Yuma T.; Zhang, Xin; Lv, Dongwen; Wiegand, Jan; Li, Wen; Palmer, Adam C.; Zheng, Guangrong; Weinstock, David M.; Zhou, Daohong

doi:10.1186/s13045-020-00928-9

Cited by 68 publications

(66 citation statements)

References 41 publications

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“…Crystal structures of the small molecule bound to VHL provided insight into suitable attachment points to create PROTACs ( 56 ). Indeed, several studies have now shown that this ligand can be incorporated to produce successful PROTACs ( 17 , 24 , 25 , 57 , 58 , 59 , 60 , 61 , 62 , 63 ). In fact, the VHL ligand is one of the most used E3 ligase recruiting elements in the PROTAC field to date.…”

Section: Hijacking Of the Ups: Protacsmentioning

confidence: 99%

Major advances in targeted protein degradation: PROTACs, LYTACs, and MADTACs

Alabi

Crews

2021

Journal of Biological Chemistry

128

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Of late, targeted protein degradation (TPD) has surfaced as a novel and innovative chemical tool and therapeutic modality. By co-opting protein degradation pathways, TPD facilitates complete removal of the protein molecules from within or outside the cell. While the pioneering Proteolysis-Targeting Chimera (PROTAC) technology and molecular glues hijack the ubiquitin-proteasome system, newer modalities co-opt autophagy or the endo-lysosomal pathway. Using this mechanism, TPD is posited to largely expand the druggable space far beyond small-molecule inhibitors. In this review, we discuss the major advances in TPD, highlight our current understanding, and explore outstanding questions in the field.

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Section: Hijacking Of the Ups: Protacsmentioning

confidence: 99%

Major advances in targeted protein degradation: PROTACs, LYTACs, and MADTACs

Alabi

Crews

2021

Journal of Biological Chemistry

128

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“…This intervention reduced disease progression and increased survival in a TCL PDX mouse model dependent on both Bcl-2 and Bcl-xl. (He et al, 2020;Zhang et al, 2020). The same PROTAC approach has been used to reduce platelet toxicity of navitoclax, a known Bcl-2 and Bcl-xl dual inhibitor (He et al, 2020).…”

Section: Fsfc Contributions To Cancer Immunotherapy Researchmentioning

confidence: 99%

“…(He et al, 2020;Zhang et al, 2020). The same PROTAC approach has been used to reduce platelet toxicity of navitoclax, a known Bcl-2 and Bcl-xl dual inhibitor (He et al, 2020). In these studies, FSFC was implemented to evaluate T cells, B cells, myeloid cells, hematopoietic progenitors and hematopoietic stem cells in bone marrow.…”

Section: Fsfc Contributions To Cancer Immunotherapy Researchmentioning

confidence: 99%

Full Spectrum Flow Cytometry as a Powerful Technology for Cancer Immunotherapy Research

Bonilla¹,

Reinin²,

Chua³

2021

Front. Mol. Biosci.

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The Nobel Prize-deserving concept of blocking inhibitory pathways in T cells, to unleash their anti-tumoral capacity, became one of the pillars of cancer treatment in the last decade and has resulted in durable clinical responses for multiple cancer types. Currently, two of the most important goals in cancer immunotherapy are to understand the mechanisms resulting in failure to checkpoint blockade and to identify predictive immunological biomarkers that correlate to treatment response, disease progression or adverse effects. The identification and validation of biomarkers for routine clinical use is not only critical to monitor disease or treatment progression, but also to personalize and develop new therapies. To achieve these goals, powerful research tools are needed. Flow cytometry stands as one of the most successful single-cell analytical tools used to characterize immune cell phenotypes to monitor solid tumors, hematological malignancies, minimal residual disease or metastatic progression. This technology has been fundamental in diagnosis, treatment and translational research in cancer clinical trials. Most recently, the need to evaluate simultaneously more features in each cell has pushed the field to implement more powerful adaptations beyond conventional flow cytometry, including Full Spectrum Flow Cytometry (FSFC). FSFC captures the full emission spectrum of fluorescent molecules using arrays of highly sensitive light detectors, and to date has enabled characterization of 40 parameters in a single sample. We will summarize the contributions of this technology to the advancement of research in immunotherapy studies and discuss best practices to obtain reliable, robust and reproducible FSFC results.

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“…To avoid the on-target toxicity of BCL-X L inhibitors to platelets, we have recently reported the development of the first-in-class BCL-X L degrader—a proteolysis-targeting chimera (PROTAC) referred to as DT2216—targets BCL-X L to the von Hippel-Lindau (VHL) E3 ligase for ubiquitination and subsequent proteasomal degradation 16 . Because platelets express a low level of VHL E3 ligase, DT2216 has minimal effect on platelets but exhibits an improved cytotoxicity against various cancer cells that are dependent on BCL-X L for survival 16 , 17 . We also developed another similar PROTAC PZ15227 that uses cereblon (CRBN) E3 ligase to induce BCL-X L polyubiquitination and degradation 18 .…”

Section: Introductionmentioning

confidence: 99%

Proteolysis-targeting chimera against BCL-XL destroys tumor-infiltrating regulatory T cells

Kolb

Khan

et al. 2021

Nat Commun

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Regulatory T cells (Tregs) play an important role in maintaining immune homeostasis and, within tumors, their upregulation is common and promotes an immunosuppressive microenvironment. Therapeutic strategies that can eliminate Tregs in the tumor (i.e., therapies that do not run the risk of affecting normal tissues), are urgently needed for the development of cancer immunotherapies. Here we report our discovery of B-cell lymphoma extra-large (BCL-XL) as a potential molecular target of tumor-infiltrating (TI) Tregs. We show that pharmacological degradation of BCL-XL using a newly developed platelet-sparing BCL-XL Proteolysis-targeting chimera (PROTAC) induces the apoptosis of TI-Tregs and the activation of TI-CD8+ T cells. Moreover, these activities result in an effective suppression of syngeneic tumor growth in immunocompetent, but not in immunodeficient or CD8+ T cell-depleted mice. Notably, treatment with BCL-XL PROTAC does not cause detectable damage within several normal tissues or thrombocytopenia. These findings identify BCL-XL as a target in the elimination of TI-Tregs as a component of cancer immunotherapies, and that the BCL-XL-specific PROTAC has the potential to be developed as a therapeutic for cancer immunotherapy.

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DT2216—a Bcl-xL-specific degrader is highly active against Bcl-xL-dependent T cell lymphomas

Cited by 68 publications

References 41 publications

Major advances in targeted protein degradation: PROTACs, LYTACs, and MADTACs

Major advances in targeted protein degradation: PROTACs, LYTACs, and MADTACs

Full Spectrum Flow Cytometry as a Powerful Technology for Cancer Immunotherapy Research

Proteolysis-targeting chimera against BCL-XL destroys tumor-infiltrating regulatory T cells

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