C4 Therapeutics (CCCC) Status Update summary
Event summary combining transcript, slides, and related documents.
Status Update summary
8 Jul, 2026Portfolio and Pipeline Progress
Achieved significant milestones in targeted protein degradation, advancing multiple clinical programs and collaborations, with the TORPEDO platform validated by internal pipeline expansion and partnerships with Biogen, Merck, and Betta Pharmaceuticals.
Cemsidomide advanced rapidly as a best-in-class IKZF1/3 degrader, showing compelling activity in multiple myeloma (MM) and non-Hodgkin's lymphoma (NHL), with ongoing clinical programs.
Initial clinical data for CFT1946 (BRAF V600X degrader) and CFT8919 (EGFR L858R degrader) demonstrated proof of mechanism and activity, with further readouts planned for 2025.
C4T aims to become a fully integrated biotech company focused on orally bioavailable degraders in oncology and non-oncology indications.
Clinical Progress and Trial Updates
Cemsidomide showed strong anti-tumor and immunomodulatory activity in heavily pre-treated MM and NHL, including patients with prior CAR-T, BCMA, and T-cell engager therapies.
In MM, cemsidomide plus dexamethasone achieved a 36% overall response rate at 75 μg and 26% across all doses, with durable responses and a wide therapeutic index.
In NHL, cemsidomide monotherapy achieved a 38% overall response rate, with 44% in PTCL and 100% in AITL subtype, and a 25% complete metabolic response rate in PTCL.
Responses were observed across all dose levels, with deepening and durable responses up to 18 months.
Ongoing dose escalation and combination studies are planned in MM and NHL.
Safety and Tolerability
Cemsidomide was well-tolerated in both MM and NHL, with manageable neutropenia and low rates of infections and febrile neutropenia.
Most neutropenia events occurred in the first two cycles, with limited G-CSF use (26%) and no dose reductions due to adverse events in MM.
In NHL, 48% experienced grade ≥3 neutropenia, but cases were manageable and did not lead to discontinuation.
Safety profile compares favorably to mezigdomide, with fewer neutropenic events, lower G-CSF use, and lower rates of grade ≥3 infections.
Only one dose-limiting toxicity was observed, and the maximum tolerated dose has not been exceeded.
Latest events from C4 Therapeutics
- Cemsidomide shows strong efficacy and safety in late-line myeloma, with pivotal trials in 2026.CCCC
Status Update8 Jul 2026 - All proposals, including director elections and stock plan amendment, passed by majority vote.CCCC
AGM 202624 Jun 2026 - Cemsidomide shows best-in-class potential as a foundational therapy for multiple myeloma.CCCC
KOL event18 Jun 2026 - Cemsidomide shows strong efficacy in MM, with a pipeline targeting oncology and INN diseases.CCCC
Corporate presentation15 Jun 2026 - Up to $400 million in securities registered to fund oncology pipeline, with $200 million ATM led by TD Securities.CCCC
Registration Filing14 Jun 2026 - Cemsidomide shows best-in-class potential in efficacy and safety, targeting a $4B+ market.CCCC
Jefferies Global Healthcare Conference 20264 Jun 2026 - Cemsidomide demonstrates robust late-line efficacy and safety, with pivotal data expected in 2027.CCCC
7th Annual Oncology Innovation Summit: Insights for ASCO & EHA26 May 2026 - Net loss narrowed to $25.1M in Q1 2026; cash runway extends to 2028 after Roche deal.CCCC
Q1 202612 May 2026 - Advancing best-in-class protein degraders for oncology and INN, led by cemsidomide in MM.CCCC
Investor presentation12 May 2026