Saturday, July 11, 2026

pharma · Hepatocellular Carcinoma · Obesity

Hospital Authority

Hospital Authority, Hong is a pharma organization headquartered in CN. Primary therapeutic focus areas include Hepatocellular Carcinoma, Obesity, Acute Kidney Injury, Nasopharyngeal Carcinoma, Coronary Artery Disease. No

Hospital Authority Building, 147B Argyle Street, Kowloon, Hong Kong, 852, HK, CN HQ
1991 Founded
12,669 Employees
NMPA registrant Type
Company details
Status
Public
HQ
Hospital Authority Building, 147B Argyle Street, Kowloon, Hong Kong, 852, HK, CN
Founded
1991
Employees
12,669
Programs
322
Drugs
301
Patents
0
Clinical program

Atorvastatin

Phase 2 · small molecule · Vitiligo

Atorvastatin (APO-ATORVASTATIN) is an HMG-CoA reductase inhibitor—a small-molecule statin originally developed for cholesterol management—being investigated by Hospital Authority, Hong Kong for an off-label indication in vitiligo treatment. The program, identified as 15-AOI-01, is currently in Phase 2 development and h

← All Hospital Authority, Hong Kong projects Phase 2 small molecule completed

Internal code 15-AOI-01

At a glance

Sponsor
Hospital Authority, Hong Kong
Phase
Phase 2
Modality
small_molecule
Indication
Vitiligo
Status
completed
Trials
1

Executive summary

Atorvastatin (APO-ATORVASTATIN) is an HMG-CoA reductase inhibitor—a small-molecule statin originally developed for cholesterol management—being investigated by Hospital Authority, Hong Kong for an off-label indication in vitiligo treatment. The program, identified as 15-AOI-01, is currently in Phase 2 development and has completed its trial phase as of March 2026. Atorvastatin is already approved in multiple jurisdictions including Australia, where it has been marketed since 1998 under various generic and branded formulations by multiple sponsors including Alphapharm, Apotex, and Arrow Pharma.

The mechanism of action in vitiligo remains undisclosed in available data, though the HMG-CoA reductase inhibition pathway is the known pharmacological basis of the drug class. The program represents a potential repurposing strategy for an established pharmaceutical agent into dermatology. Hospital Authority's sponsorship indicates an academic or institutional research focus rather than a commercial pharmaceutical company development pathway. With Phase 2 completion reported at March 2026, the program status suggests transition toward next-stage evaluation, though specific efficacy and safety outcomes from the completed trial have not been disclosed.

Atorvastatin competes in a crowded vitiligo landscape dominated by JAK inhibitors and other immunomodulatory agents in Phase 3 development from companies including Incyte, AbbVie, Pfizer, and others. The regulatory pathway and commercial viability of this statin repurposing strategy remain to be clarified through publication of trial results and regulatory feedback.

Analyst view

Why this program matters

Vitiligo is a chronic depigmentation disorder affecting approximately 0.5–2% of the global population, with significant psychosocial burden including depression, anxiety, and social stigma. Current treatment options are limited, with topical corticosteroids and calcineurin inhibitors providing modest efficacy and phototherapy requiring sustained commitment. The disease remains largely unmet medically, particularly for generalized or rapidly progressive vitiligo, creating substantial market opportunity for effective systemic therapies.

Atorvastatin's investigation in vitiligo represents a potential low-cost repurposing strategy for an off-patent, widely available medication. If efficacy is demonstrated, such an approach could offer significant advantages in accessibility and affordability compared to novel molecular entities. The competitive landscape includes multiple Phase 3 JAK inhibitors (povorcitinib, upadacitinib from Incyte and AbbVie), Pfizer's investigational compounds, and Clinuvel's SCENESSE implant, indicating substantial pharmaceutical industry investment in vitiligo therapeutics.

The patient population spans all ages and ethnicities, with particular impact on individuals with darker skin tones where depigmentation is more visually apparent. Commercial significance depends on demonstrating efficacy superior to or comparable with emerging JAK inhibitors while leveraging cost advantages. Hospital Authority's sponsorship suggests potential pathway toward academic publication and possible adoption in healthcare systems rather than traditional commercial pharmaceutical development, which may limit but not eliminate market relevance in institutional and emerging-market settings.

Drug intelligence

Drug Class: HMG-CoA reductase inhibitor (statin)

Mechanism of Action: HMG-CoA reductase inhibition; mechanism in vitiligo not yet disclosed

Modality: Small molecule

Route of Administration: Not yet disclosed

Molecular Target: Not yet disclosed for vitiligo indication

Related Therapies: Atorvastatin is an established cholesterol-lowering agent approved globally since the 1990s. In vitiligo, it competes with JAK inhibitors (povorcitinib, upadacitinib), topical immunomodulators, phototherapy agents, and other investigational small molecules.

First Approval: Approved in Australia as of February 1998 (earliest listed date); marketed under multiple brand names and generic formulations by Alphapharm Pty Ltd, Apotex Pty Ltd, Arrow Pharma Pty Ltd, Aspen Pharmacare Australia Pty Limited, and Medsurge Healthcare Pty Ltd

Patent Status: Not yet disclosed; atorvastatin is off-patent in most major markets

  • APO-ATORVASTATIN brand formulation identified in facts
  • Multiple PBS codes in Australia indicate multiple approved formulations and dosing strengths
  • Clinical trials ongoing in China (NCT01547455, NCT02496962, NCT02715726, NCT05790499, NCT07378228)
Disease intelligence

vitiligo

Overview

Generalized well circumscribed patches of leukoderma that are generally distributed over symmetric body locations and is due to autoimmune destruction of melanocytes.

Treatment landscape

ClinicalTrials.gov lists 225 registered studies for Vitiligo (AACT aggregate).

Phase breakdown: NA (128), PHASE2 (36), PHASE4 (18), PHASE1 (13), PHASE3 (13), PHASE2/PHASE3 (10), EARLY_PHASE1 (4), PHASE1/PHASE2 (3)

Common investigational therapies:

  • Placebo
  • Afamelanotide
  • Topical corticosteroid
  • Apremilast
  • Methotrexate
  • Ruxolitinib 1.5% Cream BID
  • Tofacitinib
  • Ruxolitinib cream
  • Vehicle
  • Tacrolimus ointment
Classification: MONDO MONDO:0008661 ORPHA 247871 ICD-10 L80MeSH D014820

Disease data sourced from MONDO Disease Ontology (MONDO:0008661), Orphanet — vitiligo, NCT00134368, NCT00167752, NCT00172939, NCT00177034, NCT00367224, AACT (ClinicalTrials.gov aggregate), ClinicalTrials.gov, Open Targets Platform (CC BY 4.0).

Clinical development timeline

  1. Approved1998-02-01

    First Australian approval

    Atorvastatin approved in Australia; earliest listed date in regulatory database.

  2. Approved2001-08-01

    Additional Australian approvals

    Further atorvastatin formulations approved in Australia by additional sponsors.

  3. Approved2012-04-01

    Continued market expansion

    Additional atorvastatin formulations approved in Australia.

  4. Phase 22026-03-24

    Phase 2 vitiligo trial completed

    Hospital Authority's Phase 2 investigation of atorvastatin in vitiligo (15-AOI-01) reported as completed.

Competitive landscape

Atorvastatin's vitiligo program competes in a therapeutically active landscape dominated by JAK inhibitors in Phase 3 development. Incyte leads with multiple candidates: povorcitinib (INCB054707-801, INCB 18424-309) and related formulations in Phase 3, representing the most advanced JAK inhibitor class in vitiligo. AbbVie's upadacitinib (Phase 3) represents another major JAK inhibitor competitor. Pfizer has two Phase 3 candidates (B7981080, B7981041) in development. Clinuvel's SCENESSE 16 mg implant (Phase 3) offers a distinct mechanism as an alpha-melanocyte-stimulating hormone analog.

In Phase 2, VYNE Therapeutics' VYN201 Gel, Merck's MK-6194, Takeda's zasocitinib, and Arcutis Biotherapeutics' ARQ-252 cream 0.3% represent additional small-molecule competitors at earlier development stages. Atorvastatin's competitive positioning is distinguished by its established safety profile, off-patent status, and potential cost advantage, but is disadvantaged by lack of disclosed efficacy data, uncertain mechanism in vitiligo, and positioning by an academic sponsor rather than a commercial pharmaceutical company. The Phase 2 completion status places atorvastatin behind multiple Phase 3 competitors in development timeline.

TherapyCompanyMechanismStatus
INCB054707-801Incytesmall_moleculephase_3
INCB 18424-309Incytesmall_moleculephase_3
Placebo to Povorcitinib, PovorcitinibIncytesmall_moleculephase_3
Upadacitinib Placebo, UpadacitinibAbbVie Deutschland GmbH & Co. KGsmall_moleculephase_3
B7981080Pfizer Australia Pty Ltdsmall_moleculephase_3
SCENESSE 16 mg implantClinuvel Europe Limitedsmall_moleculephase_3
Povorcitinib, Placebo to PovorcitinibIncytesmall_moleculephase_3
B7981041Pfizer Australia Pty Ltdsmall_moleculephase_3
VYN201 GelVYNE Therapeuticssmall_moleculephase_2
Placebo to MK-6194, MK-6194Merck Sharp and Dohmesmall_moleculephase_2
ZasocitinibTakedasmall_moleculephase_2
ARQ-252 cream 0.3%Arcutis Biotherapeuticssmall_moleculephase_2
UPADACITINIBTyrosine-protein kinase JAK2 inhibitorPhase 3
TACROLIMUS ANHYDROUSFK506-binding protein 1A inhibitorPhase 3
RUXOLITINIBTyrosine-protein kinase JAK1 inhibitorPhase 3
RITLECITINIBTEC family kinase inhibitorPhase 3
METHOTREXATEDihydrofolate reductase inhibitorPhase 3
DEUCRAVACITINIBTyrosine-protein kinase TYK2 negative allosteric modulatorPhase 3
CRAVACITINIBTyrosine-protein kinase TYK2 negative allosteric modulatorPhase 3
TRIAMCINOLONE ACETONIDEGlucocorticoid receptor agonistPhase 2

Additional associated therapies sourced from Open Targets Platform (CC0), linked to NovaPharmaNews drug profiles where matched.

Regulatory intelligence

Australia (TGA): Atorvastatin approved; marketed under multiple formulations and PBS codes (13374X, 13468W, 13495G, 13529C, 8213G, 8214H, 8215J, 8521L) by Alphapharm Pty Ltd, Apotex Pty Ltd, Arrow Pharma Pty Ltd, Aspen Pharmacare Australia Pty Limited, and Medsurge Healthcare Pty Ltd. First listed dates: February 1, 1998; August 1, 2001; April 1, 2012.

China (NMPA): Atorvastatin in clinical trials; multiple NCT registrations indicate ongoing investigational activity (NCT01547455, NCT02496962, NCT02715726, NCT05790499, NCT07378228).

Vitiligo Indication Regulatory Status: Not yet disclosed. No FDA, EMA, or PMDA approvals for atorvastatin in vitiligo are evident from facts provided. Regulatory pathway for vitiligo indication remains unknown.

  • Phase 2 trial completion (March 2026) suggests potential transition toward regulatory discussions, but no filing or approval status disclosed
  • Academic sponsorship by Hospital Authority may indicate pathway toward publication and institutional adoption rather than traditional NDA/BLA filing
  • Mechanism of action in vitiligo not disclosed, which may impact regulatory strategy

Clinical evidence summary

NCT02432534

Objective
Not yet disclosed
Design
Not yet disclosed
Participants
Not yet disclosed
Primary endpoint
Not yet disclosed
Results
Results not yet reported; trial reported as completed as of March 2026

Key questions answered

What is atorvastatin being investigated for in this program?

Atorvastatin is being investigated for vitiligo, a chronic depigmentation disorder, in a Phase 2 trial sponsored by Hospital Authority, Hong Kong.

Is atorvastatin approved for vitiligo?

No. Atorvastatin is approved for cholesterol management in multiple countries including Australia, but approval status for vitiligo has not been disclosed.

How does atorvastatin work?

Atorvastatin is an HMG-CoA reductase inhibitor (statin) that lowers cholesterol. Its mechanism of action in vitiligo has not been disclosed.

Who is sponsoring the vitiligo trial?

Hospital Authority, Hong Kong is the sponsor of the Phase 2 vitiligo program (15-AOI-01).

What is the current development status?

The Phase 2 trial is reported as completed as of March 26, 2026. Next-stage development plans have not been disclosed.

What is the clinical trial identifier?

The primary trial identifier is NCT02432534.

What type of drug is atorvastatin?

Atorvastatin is a small-molecule HMG-CoA reductase inhibitor belonging to the statin drug class.

Who manufactures atorvastatin?

Multiple manufacturers produce atorvastatin globally. In Australia, approved sponsors include Alphapharm Pty Ltd, Apotex Pty Ltd, Arrow Pharma Pty Ltd, Aspen Pharmacare Australia Pty Limited, and Medsurge Healthcare Pty Ltd.

When was atorvastatin first approved?

Atorvastatin was first approved in Australia on February 1, 1998, and has been approved in multiple markets since then.

What are the main competitors in vitiligo?

Competitors include JAK inhibitors (povorcitinib and upadacitinib in Phase 3), Pfizer's investigational compounds, Clinuvel's SCENESSE implant, and other small molecules in Phase 2–3 development.

Is there a partner company involved?

No partner company is listed; Hospital Authority is the sole sponsor.

What is the projected peak sales figure?

Peak sales projections have not been disclosed.

What is the route of administration?

The route of administration for the vitiligo indication has not been disclosed.

What is the molecular target in vitiligo?

The molecular target in vitiligo has not been disclosed; the HMG-CoA reductase target is known for cholesterol indication only.

Are there other trials ongoing?

Multiple atorvastatin trials are ongoing in China (NCT01547455, NCT02496962, NCT02715726, NCT05790499, NCT07378228), though their specific indications are not detailed in available facts.

What is the unmet medical need in vitiligo?

Vitiligo affects 0.5–2% of the global population with limited effective treatments; current options (topical corticosteroids, phototherapy) have modest efficacy and significant psychosocial burden remains.

Entity relationship graph

Atorvastatin → Drug → Target → Indication → Company → Trials → Competitors

Evidence-based

Analyst insights

Strategic Implications: Hospital Authority's Phase 2 completion in March 2026 represents a potential inflection point toward Phase 3 initiation or publication of efficacy/safety data. The academic sponsorship model suggests prioritization of scientific evidence generation and institutional adoption over rapid commercialization. Success would validate statin repurposing in autoimmune/inflammatory dermatology and potentially lower barriers to adoption in resource-constrained healthcare systems.

Competitive Implications: Atorvastatin faces substantial competitive pressure from multiple Phase 3 JAK inhibitors with disclosed efficacy signals. Unless Phase 2 data demonstrate compelling efficacy advantages or superior safety, the program risks being outpaced by faster-moving competitors. However, off-patent status and established safety profile provide cost and accessibility advantages if efficacy is confirmed.

Future Catalysts:

  • Publication of Phase 2 trial results (primary efficacy and safety endpoints)
  • Announcement of Phase 3 initiation or regulatory feedback from health authorities
  • Comparative efficacy/safety analysis versus JAK inhibitors
  • Mechanism of action elucidation in vitiligo
  • Regulatory pathway clarification (NDA, institutional adoption, or other)

Expected Milestones: Next milestone label and date not yet disclosed. Clinical trial completion in March 2026 suggests potential data readout or regulatory meeting within 6–12 months, though timeline remains speculative absent formal disclosure.

Quick answers

Concise, citable answers optimized for AI answer engines.

Program name?
Atorvastatin (internal code 15-AOI-01)
Indication?
Vitiligo
Current phase?
Phase 2 (completed as of March 2026)
Sponsor?
Hospital Authority, Hong Kong
Partner?
None disclosed
Modality?
Small molecule
Mechanism of action?
HMG-CoA reductase inhibitor; mechanism in vitiligo not disclosed
Molecular target?
Not disclosed for vitiligo indication
Route of administration?
Not disclosed
Brand name?
APO-ATORVASTATIN
First approval date?
February 1, 1998 (Australia)
Approved jurisdictions?
Australia (multiple formulations); vitiligo approval status not disclosed
Trial identifier?
NCT02432534
Latest milestone?
Phase 2 completion, March 24, 2026
Peak sales projection?
Not disclosed
Consensus position?
Not disclosed
Lead investigator?
Not disclosed
First disclosure date?
Not disclosed
Expected next milestone?
Not disclosed
License type?
Not disclosed
Main competitors?
Incyte povorcitinib, AbbVie upadacitinib, Pfizer compounds (Phase 3)
Competitive advantage?
Off-patent, established safety, cost; disadvantaged by Phase 2 status vs Phase 3 competitors
Regulatory pathway?
Not disclosed; academic sponsorship suggests potential institutional adoption model
Patent status?
Off-patent in most major markets
Development status summary?
Phase 2 completed; next steps not disclosed

Evidence & sources

Reviewed by NovaPharmaNews Intelligence Desk. Last reviewed .

  1. ClinicalTrials.gov NCT02432534 (clinicaltrials)
  2. atorvastatin AU status (fda)
  3. atorvastatin CN status (fda)
  4. statin CN status (fda)
  5. Source: phase (source_attribution)
  6. MONDO Disease Ontology (MONDO:0008661) (mondo)
  7. Orphanet — vitiligo (orphanet)
  8. NCT00134368 (clinicaltrials_gov)
  9. NCT00167752 (clinicaltrials_gov)
  10. NCT00172939 (clinicaltrials_gov)
  11. NCT00177034 (clinicaltrials_gov)
  12. NCT00367224 (clinicaltrials_gov)
  13. AACT (ClinicalTrials.gov aggregate) (aact)
  14. ClinicalTrials.gov (clinicaltrials_gov)
  15. Open Targets Platform (opentargets)

Intelligence compiled from public regulatory and clinical sources (FDA, EMA, ClinicalTrials.gov and company disclosures). Figures may be editorial or analyst estimates; verify against primary sources before relying on them.