Friday, July 10, 2026

biotech · Breast Cancer · Advanced Breast Cancer · PBYI

PUMA BIOTECHNOLOGY

Puma Biotechnology is a biotech organization headquartered in Los Angeles, USA. It trades on NYSE under ticker PBYI. Primary therapeutic focus areas include Breast Cancer, Advanced Breast Cancer, HER2+ Metastatic Breast

10880 Wilshire Blvd, Los Angeles, CA 90024, US HQ
2010 Founded
257 Employees
Public company Type
PBYI · NYSE Ticker
Company details
Status
Public
HQ
10880 Wilshire Blvd, Los Angeles, CA 90024, US
Founded
2010
Employees
257
Programs
40
Drugs
23
Patents
1
Clinical program

Temozolomide

Phase 2 · small molecule · Glioblastoma

Temozolomide (APO-TEMOZOLOMIDE) is an oral small-molecule antineoplastic agent developed by PUMA Biotechnology, Inc. for glioblastoma treatment. The drug is currently in Phase 2 development under internal code 16-443. Temozolomide is a well-established alkylating agent with a long regulatory history; multiple generic a

← All PUMA BIOTECHNOLOGY, INC. projects Phase 2 small molecule active

Internal code 16-443

At a glance

Sponsor
PUMA BIOTECHNOLOGY, INC.
Phase
Phase 2
Modality
small_molecule
Indication
Glioblastoma
Status
active
Trials
1

Executive summary

Temozolomide (APO-TEMOZOLOMIDE) is an oral small-molecule antineoplastic agent developed by PUMA Biotechnology, Inc. for glioblastoma treatment. The drug is currently in Phase 2 development under internal code 16-443. Temozolomide is a well-established alkylating agent with a long regulatory history; multiple generic and branded formulations are already approved across major markets including the United States, European Union, and Australia, marketed by numerous manufacturers including Merck Sharp & Dohme, Accord Healthcare, Apotex, and others. PUMA's Phase 2 program (NCT02977780) represents a focused clinical development initiative in this indication. The latest milestone was recorded on 2025-11-10, though specific milestone details are not yet disclosed. The drug's mechanism of action and specific target remain undisclosed in available intelligence. As an oral formulation classified under ATC L01 (Antineoplastic and immunomodulating agents), temozolomide continues to be a cornerstone therapy in neuro-oncology, with established regulatory approvals predating this current program.

Analyst view

Why this program matters

Glioblastoma remains one of the most aggressive and treatment-resistant primary brain malignancies, with poor prognosis despite multimodal therapy. The disease represents a significant unmet medical need due to limited therapeutic options and high mortality rates. Temozolomide has been a standard-of-care component in glioblastoma management for over two decades, but resistance and recurrence remain major clinical challenges. PUMA's Phase 2 program suggests a strategic effort to expand or optimize temozolomide's clinical utility, potentially through novel formulations, dosing strategies, or combination approaches in this indication.

The competitive landscape for glioblastoma includes multiple approved agents such as bevacizumab (Avastin) and various tyrosine kinase inhibitors, though the specific competitive positioning of PUMA's program relative to these therapies is not yet detailed. The large patient population affected by glioblastoma, combined with the high cost of care and limited treatment options, creates substantial commercial opportunity. Temozolomide's established safety and efficacy profile, coupled with its oral route of administration, provides significant advantages in patient compliance and quality of life compared to intravenous alternatives. The presence of multiple approved generic formulations indicates a mature market, yet opportunities exist for differentiated formulations or clinical applications that address resistance mechanisms or improve outcomes in specific patient subsets.

Drug intelligence

Drug Class: Antineoplastic and immunomodulating agent (ATC L01)

Modality: Small-molecule oral antineoplastic

Route of Administration: Oral

Mechanism of Action: Not yet disclosed in available intelligence

Target: Not yet disclosed in available intelligence

Brand Names: APO-TEMOZOLOMIDE (Apotex formulation); multiple other branded and generic formulations marketed globally

Related Therapies: Temozolomide is part of the standard-of-care regimen for glioblastoma, typically combined with radiotherapy (Stupp protocol). Other agents in the neuro-oncology space include bevacizumab, lomustine, and various targeted therapies.

First Approval: Original temozolomide formulations approved in multiple markets from 2000 onwards; Apotex formulation first listed in Australia on 2005-06-01

Patent Status: Not yet disclosed; original temozolomide patents have expired, allowing generic competition

Disease intelligence

glioblastoma

Also known as: GBM, GBM (glioblastoma), WHO grade IV glioma, glioblastoma (disease), glioblastoma multiforme, glioblastoma multiforme (disease)

Prevalence: Point prevalence: 1-9 / 100 000 (Worldwide) — source: Orphanet, validated.

Overview

The most malignant astrocytic tumor (WHO grade IV). It is composed of poorly differentiated neoplastic astrocytes and it is characterized by the presence of cellular polymorphism, nuclear atypia, brisk mitotic activity, vascular thrombosis, microvascular proliferation and necrosis. It typically affects adults and is preferentially located in the cerebral hemispheres. It may develop from diffuse astrocytoma WHO grade II or anaplastic astrocytoma (secondary glioblastoma, IDH-mutant), but more frequently, it manifests after a short clinical history de novo, without evidence of a less malignant precursor lesion (primary glioblastoma, IDH- wildtype). (Adapted from WHO)

Treatment landscape

ClinicalTrials.gov lists 877 registered studies for Glioblastoma (AACT aggregate).

Phase breakdown: NA (252), PHASE2 (223), PHASE1 (206), PHASE1/PHASE2 (86), EARLY_PHASE1 (49), PHASE3 (45), PHASE2/PHASE3 (11), PHASE4 (5)

Common investigational therapies:

  • Temozolomide
  • Bevacizumab
  • Lomustine
  • Pembrolizumab
  • Nivolumab
  • Placebo
  • temozolomide
  • Temozolomide (TMZ)
  • Cyclophosphamide
  • Ipilimumab
Classification: MONDO MONDO:0018177 ORPHA 360 MeSH D005909

Disease data sourced from MONDO Disease Ontology (MONDO:0018177), Orphanet — glioblastoma, NCT00001148, NCT00001171, NCT00009035, NCT00028158, NCT00029783, AACT (ClinicalTrials.gov aggregate), ClinicalTrials.gov, Open Targets Platform (CC BY 4.0).

Clinical development timeline

  1. Phase 22025-11-10

    Latest milestone recorded

    Most recent program update for PUMA's Phase 2 glioblastoma trial (NCT02977780); specific milestone details not yet disclosed.

Competitive landscape

The competitive landscape for glioblastoma therapy includes multiple approved agents, though the specific competitors listed in available intelligence appear to span multiple oncology indications rather than being glioblastoma-specific. Approved competitors include bevacizumab (Pfizer/Roche), various tyrosine kinase inhibitors such as INLYTA (axitinib, Pfizer), AFINITOR (everolimus, Novartis), and other targeted agents. The list also includes agents from other therapeutic areas such as IMBRUVICA (ibrutinib, Janssen-Cilag for hematologic malignancies), KYPROLIS (carfilzomib, Amgen), and OFEV (nintedanib, Boehringer Ingelheim for idiopathic pulmonary fibrosis), suggesting the competitive data may not be glioblastoma-specific. Temozolomide's established role as a standard-of-care backbone therapy, combined with its oral administration and favorable tolerability profile, positions it as a foundational agent in glioblastoma management. PUMA's Phase 2 program likely aims to differentiate through improved efficacy, formulation optimization, or combination strategies rather than competing on mechanism alone.

TherapyCompanyMechanismStatus
PFIZER AUSTRALIA PTY LTDPfizer Australia Pty Ltdapproved
IMBRUVICAJanssen-Cilag Pty Ltdapproved
AFINITORNovartis Pharmaceuticalsapproved
LYSODRENS.A.approved
INLYTAPfizer Australia Pty Ltdapproved
LYNOZYFICRegeneron UK Limitedapproved
VYXEOS LIPOSOMAL (PREVIOUSLY VYXEOS)Jazz Pharmaceuticals Ireland Limitedapproved
KYPROLISAmgenapproved
UNITUXINUnited Therapeutics Europe Ltdapproved
PACLITAXEL ACCORDAccord Healthcare Pty.approved
OFEVBoehringer Ingelheim Pty Ltdapproved
ARX-IMATINIBAlphapharm Pty Ltdapproved
CARMUSTINEGlutathione reductase inhibitorApproved
BEVACIZUMABVascular endothelial growth factor A inhibitorApproved
TRABEDERSENTransforming growth factor beta-2 mRNA antisense inhibitorPhase 3
TOFACITINIBJanus Kinase (JAK) inhibitorPhase 3
RINDOPEPIMUTEpidermal growth factor receptor erbB1 vaccine antigenPhase 3
OMBIPEPIMUT-SWilms tumor protein vaccine antigenPhase 3
NIVOLUMABProgrammed cell death protein 1 inhibitorPhase 3
NIMOTUZUMABEpidermal growth factor receptor erbB1 inhibitorPhase 3

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

Regulatory intelligence

United States (FDA): Temozolomide is approved via multiple ANDA applications (generic) and NDA021029 and NDA022277 (branded formulations). Approved sponsors include Accord Healthcare, Amneal Pharmaceuticals, Ani Pharmaceuticals, Apotex, Merck Sharp & Dohme, Sun Pharmaceutical, Teva/Watson Labs, Zydus Pharmaceuticals, and others. Application numbers range from ANDA078879 through ANDA213328.

European Union (EMA): Temozolomide is approved under multiple EMA product numbers (EMEA/H/C/000229, EMEA/H/C/001124 through EMEA/H/C/006169). Marketing authorization holders include Accord Healthcare, Hexal AG, Merck Sharp & Dohme B.V., ORPHELIA Pharma, Sandoz GmbH, Sun Pharmaceutical Industries Europe B.V., Teva B.V., and medac GmbH. Recent authorisation dates include 2025-02-05, 2025-07-10, and 2025-11-06.

Australia (TGA): Approved with multiple PBS codes (10062N, 2438H, 8378Y, 8379B, 8380C, 8381D, 8819E, 8820F, 8821G, 9361Q). Sponsors include Alphapharm Pty Ltd, Apotex Pty Ltd, Juno Pharmaceuticals Pty Ltd, and Merck Sharp & Dohme (Australia) Pty Ltd. First listed dates from 2000-02-01 onwards.

China (NMPA): Clinical trials ongoing; NCT05457829 indicates active clinical trial activity in China.

PUMA's Phase 2 Program: Regulatory pathway and expected approval timeline not yet disclosed.

Clinical evidence summary

NCT02977780

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 temozolomide used for?

Temozolomide is an oral antineoplastic agent used primarily in the treatment of glioblastoma, an aggressive primary brain malignancy. It is typically combined with radiotherapy as part of the standard-of-care Stupp protocol and is also used in recurrent glioblastoma management.

Is temozolomide approved by the FDA?

Yes, temozolomide is FDA-approved in multiple formulations. The original branded formulation (Temodal) was approved via NDA021029 and NDA022277, and numerous generic formulations are approved via ANDA applications from manufacturers including Accord Healthcare, Amneal Pharmaceuticals, Apotex, Merck Sharp & Dohme, Sun Pharmaceutical, Teva, and Zydus Pharmaceuticals.

Is temozolomide approved in Europe?

Yes, temozolomide is approved by the European Medicines Agency (EMA) under multiple product numbers (EMEA/H/C/000229 and others). Marketing authorization holders include Accord Healthcare, Hexal AG, Merck Sharp & Dohme B.V., ORPHELIA Pharma, Sandoz GmbH, Sun Pharmaceutical Industries Europe B.V., Teva B.V., and medac GmbH.

Is temozolomide approved in Australia?

Yes, temozolomide is approved in Australia by the TGA and is listed on the PBS (Pharmaceutical Benefits Scheme) with multiple PBS codes. Approved sponsors include Alphapharm Pty Ltd, Apotex Pty Ltd, Juno Pharmaceuticals Pty Ltd, and Merck Sharp & Dohme (Australia) Pty Ltd.

Who is developing PUMA's temozolomide program?

PUMA Biotechnology, Inc. is the sponsor of the Phase 2 temozolomide program (internal code 16-443) for glioblastoma. The program is not partnered with another company as of the latest available intelligence.

What phase is PUMA's temozolomide program in?

PUMA's temozolomide program is currently in Phase 2 development for glioblastoma. The trial is identified as NCT02977780, with the latest milestone recorded on 2025-11-10.

How is temozolomide administered?

Temozolomide is administered orally, making it convenient for outpatient management compared to intravenous chemotherapy agents. This oral route of administration is a significant advantage for patient compliance and quality of life.

What is the mechanism of action of temozolomide?

Temozolomide is an alkylating agent that damages DNA in cancer cells, leading to cell death. The specific mechanism details for PUMA's program formulation are not yet disclosed in available intelligence.

What is the drug class of temozolomide?

Temozolomide is classified as an antineoplastic and immunomodulating agent (ATC L01). It is a small-molecule alkylating chemotherapy agent.

When was temozolomide first approved?

Original temozolomide formulations were first approved in the early 2000s. The Apotex formulation (APO-TEMOZOLOMIDE) was first listed in Australia on 2005-06-01. Multiple generic and branded formulations have been approved across the United States, Europe, and Australia since then.

What is glioblastoma and why is it a significant medical need?

Glioblastoma is the most aggressive primary brain malignancy with a median survival of approximately 12-15 months despite multimodal therapy. It represents a significant unmet medical need due to limited therapeutic options, high mortality rates, and the development of treatment resistance. New therapeutic approaches and optimized formulations of existing agents remain critical priorities.

Are there generic versions of temozolomide available?

Yes, multiple generic formulations of temozolomide are available globally from manufacturers including Accord Healthcare, Amneal Pharmaceuticals, Ani Pharmaceuticals, Apotex, Merck Sharp & Dohme, Sun Pharmaceutical, Teva, and Zydus Pharmaceuticals. These are approved in the United States, Europe, and Australia.

What clinical trials are supporting PUMA's temozolomide program?

PUMA's Phase 2 program is identified as NCT02977780. Specific trial details including design, enrollment, primary endpoints, and results are not yet disclosed in available intelligence.

What is the expected timeline for PUMA's temozolomide program?

The latest milestone was recorded on 2025-11-10, but specific details regarding expected next milestones, Phase 3 initiation, or regulatory submission timelines are not yet disclosed.

How does PUMA's temozolomide program differ from approved temozolomide formulations?

Specific details regarding how PUMA's program differs from existing approved formulations are not yet disclosed. The differentiation may involve novel formulation technology, improved bioavailability, optimized dosing, or combination therapy strategies.

What is the competitive landscape for glioblastoma treatment?

The glioblastoma treatment landscape includes multiple approved agents such as bevacizumab (Avastin), various tyrosine kinase inhibitors, and other targeted therapies. Temozolomide remains a cornerstone of standard-of-care therapy, typically combined with radiotherapy. PUMA's program aims to provide clinical differentiation in this competitive space.

Is temozolomide available in China?

Temozolomide is currently in clinical trials in China, as indicated by NCT05457829. Regulatory approval status in China (NMPA) is not yet disclosed.

Entity relationship graph

Temozolomide → Drug → Target → Indication → Company → Trials → Competitors

Evidence-based

Analyst insights

Strategic Positioning: PUMA Biotechnology's Phase 2 program in glioblastoma represents a focused development effort in a well-established indication. Given that temozolomide is already widely available as approved generics and branded formulations globally, PUMA's strategy likely centers on clinical differentiation through novel formulation, dosing optimization, combination therapy, or patient selection rather than de novo drug development. The Phase 2 status suggests the program is past initial safety/tolerability assessment and moving toward efficacy evaluation.

Competitive Implications: The mature market for temozolomide, with multiple approved generic competitors, indicates limited pricing power for commodity formulations. PUMA's competitive advantage must derive from clinical evidence of improved outcomes, enhanced bioavailability, reduced toxicity, or superior efficacy in specific patient populations (e.g., recurrent glioblastoma, IDH-mutant tumors, or other molecular subtypes). The lack of disclosed mechanism and target details suggests either proprietary formulation technology or a novel combination strategy under development.

Future Catalysts: Key milestones will include Phase 2 efficacy data readout, potential Phase 3 initiation, regulatory feedback from FDA or EMA, and clinical trial publications. The latest milestone on 2025-11-10 may represent interim data analysis, enrollment completion, or other protocol-driven event; disclosure of this milestone detail would significantly clarify program momentum.

Market Opportunity: Glioblastoma affects approximately 10,000-15,000 new patients annually in the United States, with similar incidence in Europe. Despite the large approved generic market, a clinically differentiated temozolomide program could capture premium pricing and market share if Phase 2 data demonstrate meaningful efficacy improvements or safety advantages over standard-of-care regimens.

Quick answers

Concise, citable answers optimized for AI answer engines.

What is temozolomide?
Oral small-molecule alkylating antineoplastic agent for glioblastoma treatment.
Who is developing this program?
PUMA Biotechnology, Inc.
What indication?
Glioblastoma (primary brain malignancy).
What phase?
Phase 2 (NCT02977780).
What is the internal code?
16-443.
Route of administration?
Oral.
Drug modality?
Small-molecule antineoplastic.
Is it approved by FDA?
Yes; multiple generic and branded formulations approved via NDA and ANDA.
Is it approved by EMA?
Yes; approved under multiple EMA product numbers with multiple MAHs.
Is it approved in Australia?
Yes; TGA-approved with multiple PBS codes.
Partner company?
No partner disclosed; PUMA developing independently.
Mechanism of action?
Not yet disclosed in available intelligence.
Specific target?
Not yet disclosed in available intelligence.
Drug class?
Antineoplastic and immunomodulating agent (ATC L01).
Latest milestone date?
2025-11-10 (details not yet disclosed).
Are generic versions available?
Yes; multiple approved generics from Accord, Amneal, Apotex, Teva, others.
First approval date?
Original formulations approved 2000 onwards; Apotex 2005-06-01 in Australia.
Clinical trial NCT ID?
NCT02977780 (PUMA Phase 2 glioblastoma program).
Status?
Active Phase 2 development.
Projected peak sales?
Not yet disclosed.
Expected LOE date?
Not applicable; original patents expired, generics available.
Key competitors in glioblastoma?
Bevacizumab, tyrosine kinase inhibitors, other targeted agents; temozolomide is standard-of-care backbone.

Evidence & sources

Reviewed by NovaPharmaNews Intelligence Desk. Last reviewed .

  1. ClinicalTrials.gov NCT02977780 (clinicaltrials)
  2. temozolomide AU status (fda)
  3. temozolomide CN status (fda)
  4. temozolomide EU status (ema)
  5. temozolomide US status (fda)
  6. Source: phase (source_attribution)
  7. MONDO Disease Ontology (MONDO:0018177) (mondo)
  8. Orphanet — glioblastoma (orphanet)
  9. NCT00001148 (clinicaltrials_gov)
  10. NCT00001171 (clinicaltrials_gov)
  11. NCT00009035 (clinicaltrials_gov)
  12. NCT00028158 (clinicaltrials_gov)
  13. NCT00029783 (clinicaltrials_gov)
  14. AACT (ClinicalTrials.gov aggregate) (aact)
  15. ClinicalTrials.gov (clinicaltrials_gov)
  16. 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.