Friday, July 10, 2026

pharma · Hepatitis B · Mixed Dyslipidemia · ARWR

Arrowhead Pharmaceuticals Ireland

Arrowhead Pharmaceuticals is a pharma organization headquartered in Pasadena, USA. It trades on NYSE under ticker ARWR. Primary therapeutic focus areas include Hepatitis B, Mixed Dyslipidemia, Severe Hypertriglyceridemia

177 E Colorado Blvd, Suite 700, Pasadena, California 91105, US HQ
746 Employees
Public company Type
ARWR · NYSE Ticker
Company details
Clinical program

ARO-INHBE

Phase 2 · small molecule · Obesity

ARO-INHBE is a small-molecule program in Phase 2 development by Arrowhead Pharmaceuticals Ireland Limited for the treatment of obesity. The program is currently active with a latest milestone recorded on 2026-04-24. The mechanism of action and specific molecular target have not yet been disclosed. ARO-INHBE represents

Internal code AROINHBE-1001

At a glance

Sponsor
Arrowhead Pharmaceuticals Ireland Limited
Phase
Phase 2
Modality
small_molecule
Indication
Obesity
Status
active
Trials
1

Executive summary

ARO-INHBE is a small-molecule program in Phase 2 development by Arrowhead Pharmaceuticals Ireland Limited for the treatment of obesity. The program is currently active with a latest milestone recorded on 2026-04-24. The mechanism of action and specific molecular target have not yet been disclosed. ARO-INHBE represents Arrowhead's entry into the obesity therapeutic space, a market experiencing significant clinical and commercial attention. The program is supported by clinical trial NCT06700538. No partnership arrangements or licensing details have been disclosed to date. The obesity indication represents a substantial unmet medical need with growing treatment options entering the market. ARO-INHBE's development trajectory and regulatory pathway remain under active evaluation as the program advances through Phase 2 evaluation.

Analyst view

Why this program matters

Obesity represents a significant global health burden with substantial unmet medical need. The therapeutic landscape has expanded considerably with multiple approved pharmacological interventions now available, yet patient access, efficacy variability, and tolerability concerns persist. ARO-INHBE's entry into this space reflects Arrowhead's strategic focus on metabolic disease. The competitive environment includes established therapies such as semaglutide-based products and combination approaches like naltrexone/bupropion (Mysimba), alongside emerging candidates. The obesity market has demonstrated strong commercial potential, with approved therapies achieving substantial uptake. ARO-INHBE's small-molecule modality may offer distinct advantages in terms of manufacturing, formulation flexibility, and potential oral bioavailability compared to injectable GLP-1 receptor agonists dominating current market share. Phase 2 progression will be critical in establishing the program's efficacy profile, safety characteristics, and differentiation within an increasingly crowded therapeutic landscape. Success could position ARO-INHBE as a meaningful addition to the obesity treatment armamentarium, particularly if the program demonstrates advantages in patient tolerability, convenience, or efficacy in specific patient subpopulations.

Drug intelligence

Drug Class: Small-molecule therapeutic agent

Modality: Small molecule

Indication: Obesity

Mechanism of Action: Not yet disclosed

Molecular Target: Not yet disclosed

Route of Administration: Not yet disclosed

Development Stage: Phase 2

Sponsor: Arrowhead Pharmaceuticals Ireland Limited

Related Therapies: The obesity therapeutic class includes GLP-1 receptor agonists (semaglutide, tirzepatide), combination therapies (naltrexone/bupropion), and metabolic modulators. ARO-INHBE's small-molecule approach differentiates it from the injectable GLP-1 agonist-dominated market.

Patent Status: Not yet disclosed

First Approval: Not applicable; program remains in clinical development

Disease intelligence

obesity disorder

Also known as: obesity, obesity disease

Overview

A disorder involving an excessive amount of body fat.

Treatment landscape

ClinicalTrials.gov lists 50 registered studies for Obesity (Disorder) (AACT aggregate).

Phase breakdown: NA (46), PHASE4 (3), PHASE3 (1)

Common investigational therapies:

  • Tirzepatide
  • Placebo
  • Semaglutide Pen Injector
  • Semaglutide
  • Gradual dose reduction of semaglutide
  • Abrupt cessation of semaglutide
  • GLP-1 Receptor Agonists
  • GLP-1 Therapy
  • Semaglutide (SEMA)
  • Metoclopramide

Disease data sourced from MONDO Disease Ontology (MONDO:0011122), Orphanet — obesity disorder, NCT03412149, NCT06787001, NCT06852391, NCT06881485, NCT06911918, AACT (ClinicalTrials.gov aggregate), ClinicalTrials.gov, Open Targets Platform (CC BY 4.0).

Clinical development timeline

  1. Phase 22026-04-24

    Latest Milestone

    Most recent program milestone recorded; specific milestone detail not yet disclosed.

Competitive landscape

The obesity therapeutic landscape includes multiple approved small-molecule and biologic options. Established competitors include semaglutide-based products (referenced as Semaglutide B 3.0 mg/ml PDS290 by Disc Medicine and Mounjaro solution by The George Institute), naltrexone/bupropion combination (Mysimba 8 mg/90 mg by Disc Medicine), and pioglitazone (Takeda). The competitive set also includes various metabolic agents such as candesartan/hydrochlorothiazide (Takeda) and other small-molecule therapeutics. Several entries in the competitive list appear to represent non-obesity-specific agents or may reflect data classification anomalies (simvastatin, esomeprazole, intravenous ibuprofen, rimegepant). The market is dominated by GLP-1 receptor agonists, which have achieved substantial clinical uptake and market penetration. ARO-INHBE's small-molecule approach may offer differentiation through oral administration, manufacturing scalability, and potential cost advantages compared to injectable biologics, though efficacy and safety profiles remain to be established in Phase 2 trials.

TherapyCompanyMechanismStatus
SimvastatinHospital Authority, Hong Kongsmall_moleculeapproved
PioglitazoneTakedasmall_moleculeapproved
Semaglutide B 3.0 mg/ml PDS290Disc Medicinesmall_moleculeapproved
Mounjaro solution for injection in pre-filled... for ObesityThe George Institutesmall_moleculeapproved
ESOMEPRAZOLE, ESOMEPRAZOLEFondazione Telethon ETSsmall_moleculeapproved
Candesartan and HydrochlorothiazideTakedasmall_moleculeapproved
NN9838-4968NovoThirteensmall_moleculeapproved
Intravenous IbuprofenCUMBERLAND PHARMACEUTICALS INCsmall_moleculeapproved
NN9536-7752NovoThirteensmall_moleculeapproved
ANGELOThe George Institutesmall_moleculeapproved
Mysimba 8 mg/90 mg prolonged-release tabletsDisc Medicinesmall_moleculeapproved
RIMEGEPANT , CapsaicinDisc Medicinesmall_moleculeapproved
SIBUTRAMINEMonoamine transporter inhibitorApproved
SETMELANOTIDE ACETATEMelanocortin receptor 4 agonistApproved
SETMELANOTIDEMelanocortin receptor 4 agonistApproved
RIMONABANTCannabinoid CB1 receptor antagonistApproved
PHENTERMINE HYDROCHLORIDENorepinephrine transporter releasing agentApproved
PHENTERMINENorepinephrine transporter releasing agentApproved
PHENDIMETRAZINE TARTRATENorepinephrine transporter inhibitorApproved
ORLISTATPancreatic lipase inhibitorApproved

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

Regulatory intelligence

FDA Status: Not yet disclosed. Program remains in Phase 2 clinical development.

EMA Status: Not yet disclosed.

PMDA (Japan) Status: Not yet disclosed.

NMPA (China) Status: Not yet disclosed.

Regulatory Pathway: ARO-INHBE has not yet entered formal regulatory submission processes. Advancement to Phase 3 and subsequent regulatory filings will depend on Phase 2 efficacy and safety outcomes. No breakthrough designation, fast-track status, or other expedited pathways have been disclosed.

Clinical evidence summary

NCT06700538

Objective
Not yet disclosed
Design
Not yet disclosed
Participants
Not yet disclosed
Primary endpoint
Not yet disclosed
Results
Results not yet reported

Key questions answered

What is ARO-INHBE and what is it used for?

ARO-INHBE is a small-molecule therapeutic program developed by Arrowhead Pharmaceuticals Ireland Limited for the treatment of obesity. It is currently in Phase 2 clinical development.

Who manufactures or sponsors ARO-INHBE?

ARO-INHBE is sponsored by Arrowhead Pharmaceuticals Ireland Limited. No manufacturing partners or co-development arrangements have been disclosed.

What is the mechanism of action of ARO-INHBE?

The mechanism of action of ARO-INHBE has not yet been disclosed by the sponsor.

What is the molecular target of ARO-INHBE?

The specific molecular target of ARO-INHBE has not yet been disclosed.

What is the current development phase of ARO-INHBE?

ARO-INHBE is currently in Phase 2 clinical development as of the latest available information.

Is ARO-INHBE approved by the FDA?

No, ARO-INHBE is not yet approved. The program remains in Phase 2 clinical development and has not entered regulatory submission processes.

What clinical trials are supporting ARO-INHBE?

ARO-INHBE is supported by clinical trial NCT06700538. Specific trial design, endpoints, and results have not yet been disclosed.

What is the route of administration for ARO-INHBE?

The route of administration for ARO-INHBE has not yet been disclosed.

How does ARO-INHBE compare to semaglutide or other obesity treatments?

ARO-INHBE is a small-molecule approach, which differs from GLP-1 receptor agonists like semaglutide that are injectable biologics. Comparative efficacy and safety data are not yet available from Phase 2 trials.

When was ARO-INHBE first disclosed?

The initial disclosure date for ARO-INHBE has not been specified in available records.

What is the latest milestone for ARO-INHBE?

The latest recorded milestone for ARO-INHBE is dated 2026-04-24. Specific details of this milestone have not been disclosed.

Does ARO-INHBE have any partnership agreements?

No partnership arrangements have been disclosed for ARO-INHBE. The program is being developed solely by Arrowhead Pharmaceuticals Ireland Limited.

What is the projected peak sales potential for ARO-INHBE?

Projected peak sales figures for ARO-INHBE have not been disclosed.

What is the unmet medical need that ARO-INHBE addresses?

ARO-INHBE addresses the substantial unmet medical need in obesity treatment, where current options include injectable GLP-1 agonists and combination therapies, with potential advantages offered by an oral small-molecule approach.

What are the key competitive therapies in the obesity space?

Key competitive therapies include semaglutide-based products, tirzepatide (Mounjaro), naltrexone/bupropion (Mysimba), and pioglitazone. GLP-1 receptor agonists currently dominate the market.

What is the internal code for ARO-INHBE?

The internal code for ARO-INHBE is AROINHBE-1001.

Entity relationship graph

ARO-INHBE → Drug → Target → Indication → Company → Trials → Competitors

Evidence-based

Analyst insights

Strategic Positioning: Arrowhead's entry into obesity with a small-molecule approach reflects recognition of the market's therapeutic and commercial significance. The Phase 2 stage suggests early-to-mid stage clinical validation is underway.

Competitive Implications: ARO-INHBE faces a well-established competitive environment dominated by GLP-1 receptor agonists with proven efficacy and market penetration. Differentiation will be critical; small-molecule modality offers potential advantages in oral bioavailability and manufacturing but must demonstrate comparable or superior efficacy and tolerability.

Clinical Development Catalysts: Phase 2 data readout will be the primary near-term catalyst. Key metrics will include weight loss efficacy, safety/tolerability profile, and any signals of differentiation from existing therapies. Progression to Phase 3 and regulatory interactions will follow positive Phase 2 outcomes.

Future Milestones: Expected catalysts include Phase 2 data presentation/publication, regulatory guidance meetings, Phase 3 initiation, and potential partnership announcements if Arrowhead seeks to expand development or commercialization reach.

Unmet Needs Addressed: If ARO-INHBE demonstrates oral bioavailability with efficacy comparable to injectable GLP-1 agonists, it could address patient preferences for oral administration and reduce injection burden, a recognized barrier to adherence in obesity treatment.

Quick answers

Concise, citable answers optimized for AI answer engines.

What is ARO-INHBE?
Small-molecule Phase 2 program for obesity by Arrowhead Pharmaceuticals Ireland Limited.
What indication does ARO-INHBE treat?
Obesity.
Who manufactures ARO-INHBE?
Arrowhead Pharmaceuticals Ireland Limited.
What is the development phase of ARO-INHBE?
Phase 2.
Is ARO-INHBE approved?
No, it is in Phase 2 clinical development.
What modality is ARO-INHBE?
Small molecule.
What is the mechanism of action?
Not yet disclosed.
What is the molecular target?
Not yet disclosed.
What is the route of administration?
Not yet disclosed.
Does ARO-INHBE have a partner?
No partner disclosed; developed by Arrowhead alone.
What clinical trial supports ARO-INHBE?
NCT06700538; trial details not yet disclosed.
What is the internal code?
AROINHBE-1001.
When was the latest milestone?
2026-04-24; specific details not disclosed.
What is the peak sales projection?
Not yet disclosed.
How does it compare to semaglutide?
Small-molecule vs. injectable biologic; comparative data not yet available.
Is there FDA breakthrough designation?
Not disclosed; no expedited pathway status reported.
What is the competitive landscape?
Faces GLP-1 agonists, Mysimba, pioglitazone, and other metabolic agents.
When was ARO-INHBE first disclosed?
Initial disclosure date not specified in available records.
What is the status of ARO-INHBE?
Active Phase 2 development.
Are results from NCT06700538 available?
Results not yet reported.
What is the patent status?
Patent information not yet disclosed.
Is ARO-INHBE oral or injectable?
Route of administration not yet disclosed.

Evidence & sources

Reviewed by NovaPharmaNews Intelligence Desk. Last reviewed .

  1. ClinicalTrials.gov NCT06700538 (clinicaltrials)
  2. Source: phase (source_attribution)
  3. MONDO Disease Ontology (MONDO:0011122) (mondo)
  4. Orphanet — obesity disorder (orphanet)
  5. NCT03412149 (clinicaltrials_gov)
  6. NCT06787001 (clinicaltrials_gov)
  7. NCT06852391 (clinicaltrials_gov)
  8. NCT06881485 (clinicaltrials_gov)
  9. NCT06911918 (clinicaltrials_gov)
  10. AACT (ClinicalTrials.gov aggregate) (aact)
  11. ClinicalTrials.gov (clinicaltrials_gov)
  12. 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.