Kymera Investor Presentation Deck
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Part C Summary
KT-474 administered to HS and AD patients at 75 mg QD for 28 days shown to have
safety, PK and PD comparable to healthy volunteers
Modest, non-adverse QTcF prolongation observed to spontaneously resolve back to
baseline during final 2 weeks of dosing in HS and AD patients
Robust degradation of IRAK4 in blood and skin was associated with systemic anti-
inflammatory effect in HS and AD patients
Promising clinical activity observed in HS and AD exceeding benchmark placebo rates
and comparing favorably to SOC biologics
Data presented here validate IRAK4 degradation as a potential best in class mechanism
in inflammatory diseases and its superior clinical potential over SMI
Results support advancing KT-474 into Phase 2 placebo-controlled trials, Sanofi
expects to start Ph2 clinical trials in HS and AD in 4Q23
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