Corporate presentation
Logotype for Nuvectis Pharma Inc

Nuvectis Pharma (NVCT) Corporate presentation summary

Event summary combining transcript, slides, and related documents.

Logotype for Nuvectis Pharma Inc

Corporate presentation summary

12 May, 2026

Precision medicine strategy and pipeline

  • Focus on developing targeted therapies for serious oncology conditions with unmet needs.

  • NXP900 is a novel, highly selective YES1/SRC kinase inhibitor discovered at the University of Edinburgh.

  • Phase 1a dose escalation and drug-drug interaction (DDI) studies completed; Phase 1b program ongoing with monotherapy and combination arms.

  • Potential indications include YES1/SRC-driven solid tumors, squamous cell cancers, and ALK/EGFR-mutated NSCLC.

  • Management team has a strong track record with three approved drugs in four indications in the US and EU.

Clinical progress and safety

  • Phase 1a study in advanced solid tumors showed robust pharmacodynamic response with ~90% SRC inhibition at ≥150 mg/day.

  • Acceptable safety profile; no dose-limiting toxicity identified.

  • Most common adverse events: diarrhea, fatigue, nausea, decreased appetite, and dyspnea, mostly mild to moderate.

  • DDI study in healthy volunteers showed NXP900 is a weak inhibitor of CYP3A and CYP2B6, with no serious adverse events.

  • Rapid and sustained reduction of pSRC in PBMCs observed after dosing.

Scientific rationale and preclinical validation

  • Hippo pathway mutations and YES1 amplification linked to NXP900 sensitivity; strong preclinical efficacy in lung, esophageal, and head and neck cancer models.

  • NXP900 achieves complete shut-down of YES1/SRC pathways, differentiating it from other multi-kinase inhibitors.

  • More selective and potent SRC inhibition compared to saracatinib, with enrichment strategy for patient selection.

  • Preclinical synergy demonstrated with ALK/EGFR inhibitors and RAS inhibitors, reversing resistance in NSCLC models.

  • SRC, YES1, and YAP1 activation validated as drivers of resistance to targeted therapies.

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