A new challenger in target degradation
Ascentage hopes to become a new force in BTK.
Ascentage hopes to become a new force in BTK.
Until now BTK degradation has been a two-horse race, with BeOne and Nurix putting up near-identical datasets for their two clinical contenders. China’s Ascentage Pharma will hope to change this status quo, starting a first-in-human study of its BTK degrader APG-3288 this month.
Ascentage has been playing up this asset, announcing the clearance of its IND last month; now this study, to be carried out in the US as well as in China, is to start, according to its just revealed clinicaltrials.gov listing. With just a handful of BTK degraders in clinical trials any moves here are of note, especially given AbbVie’s apparent discontinuation of its contender ABBV-101.
The precise status of ABBV-101 is unclear, with the company keeping it in its R&D pipeline despite reportedly telling analysts it had ended its development in non-Hodgkin’s lymphoma last month. But it’s chronic lymphoblastic leukaemia where BTK degraders have battled, and this indication is included in the phase 1 study of APG-3288, alongside diffuse large B-cell and other lymphomas.
In CLL Ascentage will have a high bar to meet. BeOne’s BGB-16673 and Nurix’s bexobrutideg have shown response rates above 80% in their respective Cadance-101 and NX-5948-301 trials, and BeOne has already begun the pivotal Cadance-302, 303 and 304 studies in various CLL settings.
Though BTK as a whole is a highly competitive setting there are still only a few degraders in development. The clinical-stage pipeline includes HealZen’s HZ-Q1070, Chia Tai’s TQB3019, Ubix’s UBX-303061 and a back-up from Nurix, zelebrudomide, which is said to be cereblon-recruiting but which spent time on clinical hold.
Recently disclosed first-in-human studies*
| Project | Mechanism | Company | Trial | Scheduled start |
|---|---|---|---|---|
| 177Lu-BRP-020063 | Nectin-4 radioconjugate | Boomray | Solid tumours | 2 Mar 2026 |
| CT1390B | CLL1 Car-T | Carsgen | R/r AML | 2 Mar 2026 |
| GSK5533524 | Undisclosed ADC | GSK | Solid tumours | 31 Mar 2026 |
| APG-3288 | BTK degrader | Ascentage Pharma | R/r haematological malignancies | Mar 2026 |
| CKD-703 | cMet ADC | Chong Kun Dang | cMet+ve solid tumours, Met-amplified NSCLC | Mar 2026 |
| HRS-8364 | Undisclosed small molecule | Jiangsu HengRui | Solid tumours | Mar 2026 |
| ANO31905 | Claudin18.2-directed biological | Anova Innovation | Claudin18.2+ve pancreatic cancer | Mar 2026 |
| TAK-505 | Undisclosed | Takeda | Solid tumours | 15 Apr 2026 |
Note: *these projects were first listed on the clinicaltrials.gov database between 20 Feb and 3 Mar 2026.
Other first-in-human study entrants include Boomray’s anti-Nectin-4 radiotherapeutic BRP-020063, after Aktis took a similarly acting project, AKY-1189, into phase 1 last July.
However, while the Aktis study is in Nectin-4-positive patients, Boomray’s doesn’t appear to mandate any level of Nectin-4 expression. BRP-020063 uses lutetium-177 as its radioisotope, while Aktis is developing two forms of AKY-1189, one using lutetium-177 and the other actinium-225.
As ever, conjugates remain a popular modality, and intrigue surrounds the target of GSK’s GSK5533524, which for now remains under wraps. Meanwhile, Chong Kun Dang is advancing the cMet-directed ADC CKD-703 into a phase 1 trial in cMet-positive solid tumours including lung cancer, and Met-amplified NSCLC specifically.
The cMet ADC space saw the approval of AbbVie’s Emrelis last year, though another asset that appeared to have a promising and slightly different approach, Mythic Therapeutics’ MYTX-011, ended in failure when that private biotech found it impossible to raise additional cash.
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