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Summary of PROTAC Degraders in Clinical Trials
EP39122
Poster Title: Summary of PROTAC Degraders in Clinical Trials
Submitted on 09 Aug 2022
Author(s): Sonia Li
Affiliations: Biopharma PEG Scientific Inc.
Poster Views: 199
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Poster Information
Abstract: Targeted protein degradation (TPD) is an emerging therapeutic modality that has attracted the substantial interest of drug developers in recent years, and major progress has been made in this area. A major class of molecules that may enable such proteins to be modulated through TPD are known as proteolysis-targeting chimera (PROTAC) protein degraders. PROTACs are heterobifunctional small molecules consisting of two ligands joined by a linker: one ligand recruits and binds a protein of interest (POI) while the other recruits and binds an E3 ubiquitin ligase.

PROTAC
Figure 1. PROTAC, source: https://xvivo.com/

In the 20 years since the concept of PROTAC molecules that use the ubiquitin-proteasome system to degrade target proteins was first reported, TPD has moved from academia to industry, where many companies have initiated preclinical and early clinical development programs. in 2019, the first PROTAC molecules enter clinical trials; in 2020, these trials provided the first clinical proof-of-concept for the modality against two well-established cancer targets: the estrogen receptor (ER) and the androgen receptor (AR). With this success, the TPD field is now ready and committed to tackling ‘undrugged’ targets.

Timeline of PROTAC discoveries
Timeline of PROTAC discoveries
Figure 2. Timeline of PROTAC discoveries, source: reference [1]

In 2008, the Crews team developed the first small molecule-based PROTAC that effectively degrades AR in cancer cells. This cell-permeable PROTAC contains Nutlin (an E3 ligase MDM2 inhibitor) and a non-steroidal AR ligand (SARM) and links the two through a PEG-based linker fragment.

In 2010, Itoh et al. synthesized another PROTAC molecule using methyl-ubenimex to recruit an E3 ligase (inhibitor of apoptosis protein (IAP)) to degrade POI. To improve potency and target selectivity, small molecules with high affinity and specificity (e.g., phthalimides that recruit the E3 ligase cereblon (CRBN) or VHL-1 recognizing the E3 ligase Von Hippel-Lindau (VHL)) into PROTAC molecules, which in turn down-regulate a variety of cancer targets, such as Ikaros family zinc finger protein 1/3 (IKZF1/3) and estrogen-related receptor alpha (ERRα). The breakthrough of small molecule-based PROTAC opens a new path for PROTAC as a cancer treatment strategy.

Since 2013, companies such as Arvinas, C4 Therapeutics, and Kymera Therapeutics have been established to focus on the development of this technology, and pharmaceutical giants such as Merck, Genentech, Pfizer, Novartis, and Boehringer Ingelheim have also laid out their plans for this field. But until 2020, four questions are long overdue for answers.

1) Whether PROTAC is safe in the body.
2) Whether PROTAC can act accurately at the target site in the body.
3) Whether PROTAC is therapeutically effective.
4) Whether PROTAC retains the pharmacokinetic properties of small molecules.

In 2019, Arvinas' ARV-110 and ARV-471 were the first to enter clinical phase 1, and in 2020 the company published study data that provided clear and positive answers to all four of these questions and also successfully pushed the pipeline into phase 2 accordingly.

PROTACs in Clinical Trials
protac-in-clinic-trials
Figure 3. PROTAC targeted protein degraders in clinical development, source: reference [1]

ARV-110
Androgen receptor (AR) activity is a major driver of prostate cancer, so the first line of treatment is "anti-androgen therapy" - lowering androgen levels or blocking the androgen receptor. However, "anti-androgen therapy" is ineffective in 15-25% of patients, who are left in a passive situation with no treatment after desmothering, and this group of patients was selected for the clinical trial of ARV-110, which was administered orally once daily.

Ligands targeting androgen receptors (green), linkers (red), and ligands targeting E3 CRBN (blue).

ARV-110
Figure 4. Structure of ARV-110, source: reference [1]

In February 2022, Arvinas released clinical phase 1 dose creep and clinical phase 2 interim data showing that a dose of 420 mg was determined to be safe and is being followed in the ongoing phase 2 clinic. ARV-110 is able to act on specific targets in vivo and has shown preliminary efficacy in treating tumors.

In patients with tumors carrying the AR T878X/H875Y mutation, ARV-110 reduced prostate-specific antigen (PSA) levels by ≥50% (PSA50) in 46% of patients. Of the seven patients who met RECIST criteria and were evaluable, six had tumor reduction and two achieved partial remission. Arvinas plans to conduct a pivotal clinical phase 3 trial in late 2022 to further evaluate ARV-110 in patients with tumors carrying the AR T878X/H875Y mutation.

avr-110-phase2
Figure 5. ARV-110 Phase 2 clinical trials, source: reference [2]
avr-110
Figure 6. ARV-110 Phase 2 clinical trials, source: reference [2]


ARV-471
ARV-471 is an estrogen receptor (ER) PROTAC degrader co-developed by Arvinas and Pfizer for the treatment of ER+/HER2- breast cancer.

ARV-471
Figure 7. structure of AVR-471, source: reference [1]

Based on clinical phase 1 results published by Arvinas on December 10, 2021, ARV-471 had a favorable safety profile, with no dose-limiting toxicity observed with a once-daily oral dose of 700 mg in a dose creep trial, provided that the patients had received multiple treatments prior to enrollment.

The average degradation rate of ARV-471 was 64% with a maximum of 89% compared to the 40-50% degradation rate of fulvestrant, an ER degrader currently used in clinical practice. Of the 47 evaluable patients enrolled, 19 had clinical benefits (including partial remission and stable disease) with a benefit rate of 40%, including 3 patients in partial remission.

avr-471-phase1
Figure 8. ARV-471 Phase 2 clinical trials, source: reference [3]
avr-471
Figure 9. ARV-471 Phase 2 clinical trials, source: reference [3]


ARV-471 is currently in 2 concurrent trials, clinical phase 2 monotherapy for metastatic breast cancer and clinical phase 1b in combination with the CDK4/6 inhibitor palbociclib.

NX-2127 & NX-5948
NX-2127 and NX-5948 from NurixTheraputics is a BTK degrader used to treat a variety of immune inflammatory conditions such as rheumatoid arthritis.

There are several marketed BTK drugs, however, the emergence of the C481S drug resistance mutation has diminished the effectiveness of first-generation BTK inhibitors. Yet, this presents a new opportunity for PROTAC therapy, which does not rely on long-term covalent binding of small molecules to BTK and is therefore not affected by mutations in the binding site on BTK. PROTAC only required relatively weaker non-covalent binding to BTK to recruit E3 proteases to modify and ultimately degrade BTK. Both of NurixTheraputics' BTK degraders are currently in clinical phase 1: NX-2127 for malignant hematomas and NX-5948 for hematomas and autoimmune diseases.

btk degrader
Figure 10. BTK degrader, source: https://www.nurixtx.com/

NX-2127 data released by Nurix in October 2021 showed that BTK levels in peripheral blood were significantly reduced in the first six patients enrolled from Day 1 and remained suppressed throughout the dosing period. BTK degradation levels exceeded 80% and 90% in the 100mg/200mg dose groups, respectively.

According to data from a preclinical study of NX-5948 presented by Nurix at the 2021 American Society of Hematology (ASH) annual meeting, NX-5948 significantly reduced BTK protein levels in TMD8 tumor cells and microglia in the brain.

KT-474
KT-474 is an IRAK4 degrader. No drugs targeting IRAK4 are currently available worldwide, but studies demonstrating that IRAK4 plays a key role in inflammatory responses, B-cell lymphomas are well established and there are several traditional small molecule inhibitors in development, targeting autoimmune diseases.

IRAK4 mediates the IL-1R/TLR downstream signaling pathway and participates in immune monitoring through two pathways: on the one hand, IRAK4 has kinase activity and is able to phosphorylate the downstream proteins IRF5/7; on the other hand, IRAK4 acts as a scaffold structure responsible for the formation of the protein multimer myddosome complex.

Traditional small-molecule inhibitors can only block its kinase activity but not its scaffold structure, a characteristic that determines the inadequate inhibition of IRAK4 by small-molecule inhibitors. In contrast, PROTAC is able to completely degrade IRAK4, blocking both kinase activity and scaffold structure, which theoretically provides better inhibition.
Summary: A major class of molecules that may enable such proteins to be modulated through TPD are known as proteolysis-targeting chimera (PROTAC) protein degraders. Here we talk about the summary of PROTAC degraders in clinical trials.References: [1] Békés, M., Langley, D.R. & Crews, C.M. PROTAC targeted protein degraders: the past is prologue. Nat Rev Drug Discov 21, 181–200 (2022). https://doi.org/10.1038/s41573-021-00371-6
[2] https://sec.report/Document/0001193125-22-044926/
[3] https://www.streetinsider.com/dr/news.php?id=19335892
[4] https://sec.report/Document/0001193125-21-308787/
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