Dianthus Therapeutics (DNTH) Corporate presentation summary
Event summary combining transcript, slides, and related documents.
Corporate presentation summary
26 Mar, 2026Strategic focus and pipeline overview
Advancing two clinical-stage autoimmune therapeutics: claseprubart (aC1s mAb) and DNTH212 (BDCA2 and BAFF/APRIL bifunctional fusion protein), both with best-in-class, pipeline-in-a-product potential and patient-friendly, infrequent subcutaneous self-administration.
Claseprubart targets the classical complement pathway with a long half-life and is positioned for first-line use in neuromuscular diseases, showing positive Phase 2 results in gMG and early Phase 3 progress in CIDP.
DNTH212 targets both innate and adaptive immune systems, demonstrating superior in vitro efficacy compared to competitors and offering broad potential across multiple autoimmune diseases.
Strong financial position with ~$1.2B in cash and runway expected into 2030, supporting multiple near- and long-term milestones.
Clinical data and efficacy highlights
Claseprubart Phase 2 MaGic trial in gMG showed rapid, sustained, and statistically significant improvements in MG-ADL and QMG scores versus placebo, with robust responder rates and a favorable safety profile.
Over 60% of patients on claseprubart achieved ≥5-point improvement in MG-ADL and QMG, and 37% reached minimal symptom expression at Week 13.
Safety profile was comparable to placebo, with no serious infections, autoimmune activation, or drug-induced lupus observed.
Open-label extension and PK/PD data support convenient Q2W and Q4W dosing, with sustained efficacy and consistent symptom control.
Market opportunity and competitive positioning
Claseprubart is positioned to compete as a first-line biologic in large, growing US markets for gMG (>100,000 patients), CIDP (>40,000), and MMN (>10,000), with potential to expand biologic use due to differentiated efficacy, safety, and convenience.
Current biologic penetration in gMG is <20%, with significant opportunity for growth as the market is expected to exceed $8B by 2035.
Surveyed US neurologists confirm high unmet need for more durable, convenient, and safer therapies in gMG, CIDP, and MMN.
Claseprubart’s upstream inhibition may offer efficacy advantages over C5 inhibitors, with a lower risk of infection and no boxed warning or REMS.
Latest events from Dianthus Therapeutics
- Early GO decision in CAPTIVATE CIDP trial after high responder rate; key data readouts expected 2026–2028.DNTH
Study result9 Mar 2026 - Early Phase 3 success and robust cash reserves drive late-stage autoimmune pipeline progress.DNTHQ4 20259 Mar 2026
- Rapidly advancing CIDP and MMN trials with robust efficacy, safety, and patient-friendly design.DNTHTD Cowen 46th Annual Health Care Conference3 Mar 2026
- Key 2026 clinical milestones and strong commercial outlook drive optimism for pipeline success.DNTHGuggenheim Securities Emerging Outlook: Biotech Summit 202612 Feb 2026
- DNTH103 shows superior potency and convenience, with Phase II data expected in 2025.DNTHJefferies 2024 Global Healthcare Conference1 Feb 2026
- Biotech seeks to raise $600M for autoimmune drug development via flexible shelf registration.DNTHRegistration Filing28 Jan 2026
- Advancing next-gen complement therapy in neuromuscular diseases, with major data readouts ahead.DNTH2024 Cantor Fitzgerald Global Healthcare Conference20 Jan 2026
- Advancing a potent, patient-friendly classical pathway inhibitor in three key autoimmune indications.DNTHStifel 2024 Immunology and Inflammation Virtual Summit20 Jan 2026
- Claseprubart and DNTH212 advance with strong efficacy, safety, and major 2026 milestones ahead.DNTH44th Annual J.P. Morgan Healthcare Conference16 Jan 2026