Rx License-Rx

NAI02-03

Topical Inhibition of HIF-1a as a Novel Therapeutic Strategy for Inflammatory Skin Diseases

An effective, differentiated, and targeted therapeutic strategy for the treatment of inflammatory skin diseases such as psoriasis, atopic dermatitis, and hidradenitis suppurativa.

Intelligence Memo

Owner: University-originated technology office

Core category: Therapeutics

Therapeutic area: Inflammation

Indication: Inflammatory disease

Modality: Drug Delivery

Focus tags: Inflammation

Technology tags: Drug Delivery

Mechanism:

Development stage: Early / Discovery

Patent status: Needs review

Availability: Available for license

Risk Flags

  • Human validation and clinical path require diligence.
  • Patent scope and remaining exclusivity need review with counsel.
  • Inventor readiness and licensing terms are not yet verified.

Strategic Pharma Attractiveness

Large pharma would care if this becomes more than an interesting university-originated technology: it needs a crisp Inflammation wedge, a measurable value inflection, and a diligence package that makes the first deal feel like an option on upside rather than a blind research bet.

Most logical pharma targets Novartis — Broad modality appetite and academic-origin BD history. Takeda — Translational science focus and partnership-friendly structure. Sanofi — Immunology, rare disease, and platform-technology BD appetite.

Development Strategy to Increase PoS

First indication: Inflammatory disease

Study design: One decisive preclinical or analytical validation package with a hard go/no-go threshold.

Key experiments Validate the AI-optimized pivot: Turn delivery into the asset by choosing a toxicity-sensitive local indication Run independent replication of the core claim with pre-specified success criteria Generate a partner-facing risk register that separates solved, testable, and unresolved risks

Final Recommendation

Proceed with repositioning: Interesting science, but the next dataset should be funded before committing to a full license. The most investable version is: Turn delivery into the asset by choosing a toxicity-sensitive local indication

Best next experiment: Run the smallest independent study that validates: Run biodistribution and local tolerability first, then attach the platform to a known active payload instead of inventing a new drug story.

Best licensing timing: Begin BD conversations after the next validation package; pursue a license, option, or asset sale once the first value inflection is visible.