TheraRadar
Landscape / Oncology
Page updated Jul 4, 2026 · using data updated on Jun 28, 2026

Triple Negative Breast Cancer Clinical Trial Landscape

Triple Negative Breast Cancer is being studied across 592 clinical trials registered since 2008, with 332 programs currently active. The competitive pipeline includes 43 active Phase 3 trials, 210 active Phase 2 trials, and 76 active Phase 1 trials.

Top industry sponsors include Gilead, Novartis, AstraZeneca.

Trial activity

332 active / 592 total since 2008
Active by phase 43 Ph3 / 66 210 Ph2 / 362 76 Ph1 / 161 3 Ph4 / 3

Competitive Intelligence

This Triple Negative Breast Cancer competitive landscape maps 7 companies against 5 mechanisms of action (MOA) across 7 active drug-development programs. Each cell is the lead program for a company–mechanism pair — its trial phase, modality, combination, and nearest readout. Read down a column to see who is competing on the same mechanism in Triple Negative Breast Cancer, across a row to see one company's mechanistic spread, and click any cell for the full program list and trial links.

Beta 7 companies 5 mechanisms 7 programs mapped all shown mechanisms rule/db-classified ⏰ 1 due ≤6 mo click any cell → asset tearsheet
At a glance

Breast shows 7 programs across 7 companies and 5 mechanisms. The most contested mechanism is Trop-2 ADC (8 programs).

Key findings
  • 90% of Trop-2 ADC programs (9 of 10) are combos with novel agents — class-extension work, not class-validation.
  • Top 3 mechanisms (Trop-2 ADC, TROP-2 ADC (next-gen), EGFR / HER3 bispecific ADC) account for ~37% of programs — class concentration is low.
  • AstraZeneca runs 5 programs — the deepest pipeline in this view.
  • Sichuan Kelun-Biotech Biopharmaceutical has the highest composite score (100) — most-imminent / most-advanced asset weighted higher than program count.
  • 9 hot readouts in next 6 months — most imminent: Sichuan Kelun-Biotech Biopharmaceutical (TROP-2 ADC (next-gen)).
  • 9 trials are stale (overdue without status change) — possible class-maturity inflection or operational issue.
  • 25 single-program mechanisms in the long tail — 0 are Ph2+ first-in-class first-mover bets.
  • 19 NME candidates in the long tail.

Forward catalysts next 18 months⏰ 1 due ≤6 mo

Nearest first. ⚖ Confirmed FDA PDUFA dates (curated calendar, primary sources) and 📅 estimated readouts (ClinicalTrials.gov primaryCompletionDate — a timing proxy, not a confirmed action date). Red = due within 6 months.

Company × Mechanism

Each cell = a company’s most-advanced program in that mechanism. Click for the asset tearsheet.
Unverified (lowTrust) cells:
Ph1 Ph2 Ph3 Ph4 ⚠ lowTrust +combo
Select & Focus Pro 🔒 Transpose, filtering, selection & export are Pro (search & sort are free) — start a free trial, or try them free on our showcase →
Trop-2 ADC
TROP-2 ADC (next-gen)
Nectin-4 ADC
EGFR / HER3 bispecific ADC
PD-L1 / VEGF-A bispecific antibody
AstraZeneca
Gilead Sciences
Merck & Co.
🇨🇳Mabwell (Shanghai) Bioscience
🇨🇳Sichuan Baili
BioNTech
🇨🇳Sichuan Kelun-Biotech Biophar…

Phase 3 leaders · most advanced

  1. recruiting Sichuan Kelun-Biotech Biopharmaceutical Co., Ltd. NCT06279364
  2. active Sichuan Kelun-Biotech Biopharmaceutical Co., Ltd. NCT05347134
  3. recruiting Merck Sharp & Dohme LLC NCT06393374
  4. recruiting Gilead Sciences NCT05633654
  5. active GBG Forschungs GmbH NCT04595565

Beyond the grid Beta

What the matrix leaves out — rare mechanisms with only one player, small & emerging sponsors, and programs we haven’t classified yet.

Single-company mechanisms — BD white space 3 found

Mechanisms only ONE company is pursuing in this indication — the uncrowded / first-in-class bets the matrix cap hides. ⚡ first-in-class · ⚠ unverified mechanism. ⚡ first-in-class is computed across 61 mapped landscapes — scope-limited, not a global claim.
⚡ first-in-class · 🌱 first-in-indication · 🆕 NME candidate · ✅ AI-classified + verified · ⚙️ AI-classified, unverified · first-in-class computed across 61 mapped landscapes
Single-program mechanisms (25) — one program each — earliest-stage, sorted by phase
PhaseMechanismCompanyModalityReadoutTrial
Ph3 AKT inhibitor 🌱 AstraZeneca IV 1Q26 NCT03997123
Ph3 GLOBOH 🌱 🆕 OBI Pharma 4Q25 NCT03562637
Ph3 Nanoparticle-encapsulated taxane 🌱 ⚙️ Jina IV 2Q25 NCT03671044
Ph3 PD-1 / VEGF bispecific 🌱 🆕 Akeso IV ⏰ 4Q26 NCT06767527
Ph3 PD-L1 (adebrelimab) 🌱 🆕 Suzhou Suncadia Biopharma… IV 1Q28 NCT07111832
Ph2 Anti-PD-1 (mAb) 🌱 🆕 ⚙️ Biocad 4Q25 NCT07108309
Ph1+Ph2 AURORA A 🌱 🆕 Jacobio ⏰ 3Q26 NCT05490472
Ph1+Ph2 Botanical extract (BioLite) 🌱 🆕 BioLite Oral 2Q28 NCT02802423
Ph2 DPD inhibitor 🌱 ⚙️ Processa Oral ⏰ 3Q26 NCT06568692
Ph2 HER2 ADC 🌱 Pfizer IV 3Q29 NCT06157892
Ph2 HER3 ADC 🌱 Merck & Co. IV 4Q29 NCT06797635
Ph1+Ph2 Integrin αvβ3 🌱 ProDa IV ⏰ 3Q26 NCT06460298
Ph2 NECTIN4 🌱 🆕 Tianjin ConjuStar Biologi… 3Q27 NCT07080619
Ph1+Ph2 Neoantigen cancer vaccine 🌱 🆕 ⚙️ NEC Bio B.V Oral 4Q27 NCT06631092
Ph2 PD-L1 ADC 🌱 🆕 Shanghai Henlius 2Q27 NCT07487519
Ph2 PI3K inhibitor 🌱 🆕 Rhizen ⏰ 4Q26 NCT06189209
Ph2 Topoisomerase I inhibitor 🌱 🆕 ⚙️ JenKem Technology ⏰ 2Q26 NCT06586866
Ph1+Ph2 TROP2 × CD3 bispecific 🌱 🆕 ⚙️ Shenzhen Majory 3Q28 NCT07208149
Ph1+Ph2 Undisclosed target 🌱 🆕 Telomir Oral 2Q27 NCT07581314
Ph1 B7-H4 ADC 🌱 🆕 ⚙️ Mersana ⏰ 4Q26 NCT05377996
Ph1 FOLR1 🌱 🆕 Epsilogen ⏰ 3Q26 NCT06547840
Ph1 MELK 🌱 🆕 OncoTherapy Science 3Q27 NCT02926690
Ph1 Nectin-4 bispecific 🌱 🆕 Context 1Q30 NCT07545122
Ph1 Phospholipid radioligand (I-131) 🌱 🆕 Cellectar 1Q28 NCT07311993
Ph1 TROP2 ADC 🌱 🆕 Sichuan Baili 4Q25 NCT05339685
Emerging & small-cap sponsors (4) — few programs here — partnering / M&A radar
PhaseMechanismCompanyModalityReadoutTrial
Ph3 PD-L1 / VEGF-A bispecific antibody Biotheus IV 3Q27 NCT06419621
Ph2+Ph3 EGFR / HER3 bispecific ADC Bristol-Myers Squibb IV 1Q28 NCT06926868
Ph3 🇨🇳 Trop-2 ADC Jiangsu Alphamab Biopharm… IV 1Q29 NCT07533123
Ph3 🇨🇳 Trop-2 ADC Qilu 2Q27 NCT06732323
Unclassified programs (14) — mechanism not captured yet
PhaseMechanismCompanyModalityReadoutTrial
Ph2+Ph3 BEBT-209 capsules, Carboplatin Injection, Gemcitabine Hydrochlo…unclassified BeBetter Med Inc NCT07544056
Ph3 FDA018-ADC, Eribulin, Capecitabineunclassified Shanghai Fudan-Zhangjiang… NCT06519370
Ph3 Nuvastatic 300, Placebounclassified Natureceuticals Sdn Bhd NCT07669467
Ph1+Ph2 Durvalumab, Capivasertib, Oleclumabunclassified AstraZeneca NCT03742102
Ph1+Ph2 Dual-target CAR-NK cells, Lymphodepletingunclassified Beijing Biotech NCT07510802
Ph1+Ph2 Dual-target CAR-NK cells (EB-DT-CAR-NK), Lymphodepleting chemot…unclassified Beijing Biotech NCT07486089
Ph2 Tobemstomig, Pembrolizumab, Nab-Paclitaxelunclassified Hoffmann-La Roche NCT05852691
Ph2 AK117, AK112, Nab paclitaxelunclassified Akeso NCT05227664
Ph1+Ph2 LBL-024 for Injection, albumin-bound Paclitaxel injection, Tori…unclassified Nanjing Leads Biolabs Co.… NCT07281976
Ph1+Ph2 STAR0602, Sacituzumab Govitecan (SG)unclassified Marengo Therapeutics, Inc. NCT06827613
Ph2 BEBT-209 capsules, Carboplatin injection, Gemcitabine hydrochlo…unclassified BeBetter Med Inc NCT06685796
Ph1 PF-08032562, Fulvestrant, Cetuximabunclassified Pfizer NCT07318805
Ph1 Datopotamab Deruxtecan (Dato-DXd), Steroid Containing Mouthwashunclassified Daiichi Sankyo Co., Ltd. NCT03401385
Ph1 ITI-5000 mRNA Vaccine, Pembrolizumabunclassified Immunomic Therapeutics, I… NCT07652242

Sponsor activity

Who is running trials now — green active, blue completed, red failed/terminated.

Sorted by active Active Done Failed
Gilead 6 1 2
Novartis 4 7 5
AstraZeneca 3 3 0
AbbVie 3 1 1
Eli Lilly 3 0 2
Sichuan Kelun-Biotech Biopharmaceutical Co., Ltd. 3 0 0
Mabwell (Shanghai) Bioscience Co., Ltd. 3 0 0
Exelixis 2 1 1
NiKang Therapeutics, Inc. 2 0 1
Exscientia AI Ltd., a wholly owned subsidiary of Recursion Pharmaceuticals, Inc. 2 0 0
BeBetter Med Inc 2 0 0
Sichuan Baili Pharmaceutical Co., Ltd. 2 0 0
Beijing Biotech 2 0 0
Radiopharm Theranostics, Ltd 2 0 0
Shanghai Henlius Biotech 2 0 0

All 15 active Triple Negative Breast Cancer sponsors

Unlock the remaining 7 sponsors with active / completed / failed counts — sortable and exportable.

Unlock with Pro

How the field has grown

New-trial starts peaked in 2024 (78 registered); 2025 saw 59. The right-hand chart shows median Phase 3 enrollment by start year — the number in parentheses is that year's Phase 3 trial count (58 in total), so single-trial years (and years with no Phase 3 starts) are obvious. Both are by trial start date; the current year is partial.

New trials started by year

2016
25
2017
37
2018
41
2019
44
2020
41
2021
47
2022
54
2023
46
2024
78
2025
59
2026
53

TheraRadar.com

Median Phase 3 enrollment by start year

2016 (4)
462
2017 (3)
653
2018 (5)
575
2019 (3)
184
2020 (5)
522
2021 (2)
211
2022 (7)
443
2023 (7)
223
2024 (8)
355
2025 (7)
440
2026 (7)
446

TheraRadar.com

Full trial pipeline

Every active and completed trial across Phase 1–4, with enrollment analytics. Sortable, filterable, exportable with Pro.

NCT06279364 RECRUITING
A Study of SKB264 Versus Investigator's Choice Chemotherapy in Patients With Unresectable Recurrent or Metastatic Triple-Negative Breast Cancer
Sichuan Kelun-Biotech Biopharmaceutical Co., Ltd. n=524
NCT05347134 ACTIVE NOT RECRUITING
SKB264 Injection vs Investigator Selected Regimens to Treat Locally Advanced, Recurrent or Metastatic Triple-negative Breast Cancer
Sichuan Kelun-Biotech Biopharmaceutical Co., Ltd. n=254
NCT07178730 NOT YET RECRUITING
NeoAdjuvant Therapy Comparing Sacituzumab Govitecan+Pembrolizumab vs. SoC Chemotherapy in Clinical Stage II-III, Triple-negative Early Breast Cancer
West German Study Group n=765
NCT06393374 RECRUITING
Sacituzumab Tirumotecan (MK-2870) Plus Pembrolizumab Versus TPC in TNBC Who Did Not Achieve pCR (MK-2870-012)
Merck Sharp & Dohme LLC n=1,530
NCT05633654 RECRUITING
Study of Sacituzumab Govitecan-hziy and Pembrolizumab Versus Treatment of Physician's Choice in Patients With Triple Negative Breast Cancer Who Have Residual Invasive Disease After Surgery and Neoadjuvant Therapy (ASCENT-05/AFT-65 OptimICE-RD/GBG 119/NSABP B-63)
Gilead Sciences n=1,514
NCT07556848 NOT YET RECRUITING
A Study of 9MW2821 Versus Chemotherapy in Participants With Previously Treated Locally Advanced or Metastatic Triple-Negative Breast Cancer
Mabwell (Shanghai) Bioscience Co., Ltd. n=356
NCT04595565 ACTIVE NOT RECRUITING
Sacituzumab Govitecan in Primary HER2-negative Breast Cancer
GBG Forschungs GmbH n=1,332
NCT07544056 NOT YET RECRUITING
A Study of BEBT-209 Plus Chemotherapy in Patients With Locally Advanced or Metastatic Triple-Negative Breast Cancer
BeBetter Med Inc n=446
NCT06382142 ACTIVE NOT RECRUITING
A Study Comparing BL-B01D1 With Chemotherapy of Physician's Choice in Patients With Unresectable Locally Advanced or Metastatic Triple-Negative Breast Cancer(PANKU-Breast02)
Sichuan Baili Pharmaceutical Co., Ltd. n=418
NCT07533123 RECRUITING
A Phase III Study of JSKN016 Versus Treatment of Physician's Choice in Patients With Triple-Negative Breast Cancer Who Have Failed Standard of Care
Jiangsu Alphamab Biopharmaceuticals Co., Ltd n=364
NCT05382299 ACTIVE NOT RECRUITING
Study of Sacituzumab Govitecan-hziy Versus Treatment of Physician's Choice in Patients With Previously Untreated Locally Advanced Inoperable or Metastatic Triple-Negative Breast Cancer
Gilead Sciences n=623
NCT05806060 RECRUITING
Precise Treatment for BLIS Subtype of TNBC in the First-line Treatment of Locally Advanced or Metastatic Breast Cancer
Fudan University n=134
NCT07486687 NOT YET RECRUITING
Pembrolizumab Adjuvant in Patients With Early-stage Triple Negative Breast Cancer With Residual Disease After Neoadjuvant Pembrolizumab Plus Chemotherapy
The Netherlands Cancer Institute n=1,000
NCT06767527 RECRUITING
AK112 or Placebo Plus Nab-Paclitaxel as First-line Treatment in Inoperable Locally Advanced/ Metastatic Triple-negative Breast Cancer
Akeso n=416
NCT07407517 NOT YET RECRUITING
Adjuvant Intensification for LAR
Fudan University n=904
NCT06627712 RECRUITING
SBRT Combined With PD-1 Inhibitor and Chemotherapy in Early-stage TNBC
West China Hospital n=318
NCT06519370 ACTIVE NOT RECRUITING
FDA018-ADC vs Investigator's Choice Chemotherapy to Treat Locally Advanced, Recurrent or Metastatic Triple-negative Breast Cancer
Shanghai Fudan-Zhangjiang Bio-Pharmaceutical Co., Ltd. n=350
NCT05909332 RECRUITING
Study of Antivascular Therapy Combined With Chemotherapy Versus Chemotherapy in Adjuvant Therapy of TNBC-BLIS Patients (BCTOP-T-A03)
Fudan University n=764
NCT07111832 RECRUITING
A Clinical Trial of SHR-A1811 in the Treatment of Triple-negative Breast Cancer
Suzhou Suncadia Biopharmaceuticals Co., Ltd. n=400
NCT04722978 RECRUITING
Standard Chemotherapy Plus Moxifloxacin as First-line Treatment for Metastatic Triple-negative Breast Cancer
Sun Yat-Sen University Cancer Center n=228
NCT06081244 RECRUITING
NeoAdj. Therapy Comparing Sacituzumab Govitecan (SG) vs. SG+Pembrolizumab in Low-risk, Triple-neg. EBC (ADAPT-TN-III)
West German Study Group n=348
NCT06732323 RECRUITING
A Phase III Study of ESG401 for Unresectable Recurrent or Metastatic Triple-Negative Breast Cancer
Qilu Pharmaceutical Co., Ltd. n=504
NCT05382286 ACTIVE NOT RECRUITING
Study of Sacituzumab Govitecan-hziy and Pembrolizumab Versus Treatment of Physician's Choice and Pembrolizumab in Patients With Previously Untreated, Locally Advanced Inoperable or Metastatic Triple-Negative Breast Cancer
Gilead Sciences n=443
NCT06606730 RECRUITING
Personalizing the Use of Pembrolizumab for Patients Who Have a Strong Response in Early Triple Negative Breast Cancer
UNICANCER n=2,454
NCT05862064 RECRUITING
A Multi-center, Randomized, Open-label, Phase III Study Comparing PD-1 Inhibitor Combined With Antivascular Therapy and Anthracycline/Taxane-based Adjuvant Chemotherapy Versus Anthracycline/Taxane-based Adjuvant Chemotherapy Alone in Patients With Operable Triple-negative Breast Cancer
Fudan University n=606
NCT07021261 NOT YET RECRUITING
Comparing UTD2 Combined With Capecitabine to Capecitabine as Adjuvant Therapy for Non-pCR TNBC Patients
Fudan University n=440
NCT05552001 RECRUITING
Safety and Efficacy Analysis of an Antibody Associated With a Chemotherapy for Patients With a Triple Negative Metastatic Breast Cancer
UNICANCER n=96
NCT05078047 RECRUITING
Study Comparing the Standard Administration of IO Versus the Same IO Administered Each 3 Months in Patients in Response After 6 Months of Standard IO
UNICANCER n=646
NCT03562637 ACTIVE NOT RECRUITING
Study of Adagloxad Simolenin (OBI-822)/OBI-821 in the Adjuvant Treatment of Patients With Globo H Positive TNBC
OBI Pharma, Inc n=575
NCT03168880 ACTIVE NOT RECRUITING
A Randomized Controlled Trial of Neoadjuvant Weekly Paclitaxel Versus Weekly Paclitaxel Plus Weekly Carboplatin In Women With Large Operable or Locally Advanced, Triple Negative Breast Cancer
Tata Memorial Hospital n=720
NCT06910072 NOT YET RECRUITING
Paclitaxel Polymeric Micelles and Carboplatin in Combination With Iparomilimab and Tuvonralimab Neoadjuvant Therapy for Triple-negative Breast Cancer
Cancer Institute and Hospital, Chinese Academy of Medical Sciences n=32
NCT04296175 ACTIVE NOT RECRUITING
Carboplatin Intensified Chemotherapy for TRIple NEgative Breast Cancer(CITRINE)
Fudan University n=808
NCT03671044 RECRUITING
A Study to Evaluate the Efficacy and Safety of Nanosomal Docetaxel Lipid Suspension in Triple Negative Breast Cancer Patients
Jina Pharmaceuticals Inc. n=657
NCT06419621 RECRUITING
PM8002 or Placebo Plus Nab-Paclitaxel as First-line Treatment in Inoperable Locally Advanced/Metastatic TNBC
Biotheus Inc. n=360
NCT06795503 NOT YET RECRUITING
Non-Inferiority Study on MRNA-lncRNA Model in Low-Risk Triple-Negative Breast Cancer Patients
Fudan University n=1,462
NCT06533384 RECRUITING
PARPi or Capecitabine Combined With PD-1 Inhibitors as Adjuvant Therapy in High-risk TNBC
Guangdong Provincial People's Hospital n=310
NCT03281954 ACTIVE NOT RECRUITING
Clinical Trial of Neoadjuvant Chemotherapy With Atezolizumab or Placebo in Patients With Triple-Negative Breast Cancer Followed After Surgery by Atezolizumab or Placebo
NSABP Foundation Inc n=1,550
NCT05999149 RECRUITING
A Study of Camrelizumab Plus Chemotherapy in Combination With or Without Famitinib as Neoadjuvant Therapy in Participants With Triple Negative Breast Cancer (BCTOP-T-N01)
Fudan University n=424
NCT05760378 RECRUITING
Famitinib in Combination With Camrelizumab and TPC in The First-line Treatment of Immunomodulatory Locally Advanced or Metastatic TNBC.
Fudan University n=223
NCT02641847 ACTIVE NOT RECRUITING
TA(E)C-GP Versus A(E)C-T for the High Risk TNBC Patients and Validation of the mRNA-lncRNA Signature
Fudan University n=503
NCT05954442 RECRUITING
Everolimus With Investigator's Choice of Chemotherapy in Advanced Triple-Negative Breast Cancer (TNBC) With Luminal Androgen Receptor (LAR) Subtype
Fudan University n=203
NCT04301739 NOT YET RECRUITING
to Evaluate Efficacy and Safety of HLX10 in Combination With Chemotherapy Versus Placebo in Combination With Chemotherapy as Neoadjuvant Therapy and HLX10 Versus Placebo as Adjuvant Therapy in Patients With Triple Negative Breast Cancer (TNBC)
Shanghai Henlius Biotech n=522
NCT07669610 NOT YET RECRUITING
An Open-Label, Randomized Phase III Study of Trastuzumab Rezetecan With or Without Bevacizumab in First to Third Line BLIS Subtype TNBC
Fudan University n=140
NCT04085276 COMPLETED
Toripalimab in Combination With Nab-Paclitaxel For Patients With Metastatic or Recurrent Triple-Negative Breast Cancer (TNBC) With or Without Systemic Treatment
Shanghai Junshi Bioscience Co., Ltd. n=531
NCT04148911 COMPLETED
A Study of Atezolizumab Plus Nab-Paclitaxel in the Treatment of Unresectable Locally Advanced or Metastatic PD-L1-Positive Triple-Negative Breast Cancer
Hoffmann-La Roche n=184
NCT01805076 COMPLETED
MRI and Mammography Before Surgery in Patients With Stage I-II Breast Cancer
Alliance for Clinical Trials in Oncology n=319
NCT05555706 COMPLETED
Study of B013 and Nab-Paclitaxel for Locally Advanced or Metastatic Triple Negative Breast Cancer
Shanghai Jiaolian Drug Research and Development Co., Ltd n=62
NCT02819518 COMPLETED
Study of Pembrolizumab (MK-3475) Plus Chemotherapy vs. Placebo Plus Chemotherapy for Previously Untreated Locally Recurrent Inoperable or Metastatic Triple Negative Breast Cancer (MK-3475-355/KEYNOTE-355)
Merck Sharp & Dohme LLC n=882
NCT03498716 TERMINATED
A Study Comparing Atezolizumab (Anti PD-L1 Antibody) In Combination With Adjuvant Anthracycline/Taxane-Based Chemotherapy Versus Chemotherapy Alone In Patients With Operable Triple-Negative Breast Cancer
Hoffmann-La Roche n=2,199
NCT04799249 COMPLETED
Trilaciclib, a CDK 4/6 Inhibitor, in Patients Receiving Gemcitabine and Carboplatin for Metastatic Triple-Negative Breast Cancer (TNBC)
G1 Therapeutics, Inc. n=194
NCT05134194 TERMINATED
A Study of Camrelizumab in Combination With Chemotherapy Regimen Comparative Chemotherapy Regimen for Metastatic Triple-negative Breast Cancer
Suzhou Suncadia Biopharmaceuticals Co., Ltd. n=1
NCT04613674 COMPLETED
A Study of Camrelizumab Plus Chemotherapy vs Placebo Plus Chemotherapy as Neoadjuvant Therapy in Participants With Triple Negative Breast Cancer (TNBC)
Jiangsu HengRui Medicine Co., Ltd. n=441
NCT04177108 COMPLETED
A Study of Ipatasertib in Combination With Atezolizumab and Paclitaxel as a Treatment for Participants With Locally Advanced or Metastatic Triple-Negative Breast Cancer
Hoffmann-La Roche n=242
NCT03125902 COMPLETED
A Study of Atezolizumab and Paclitaxel Versus Placebo and Paclitaxel in Participants With Previously Untreated Locally Advanced or Metastatic Triple Negative Breast Cancer (TNBC)
Hoffmann-La Roche n=653
NCT03197935 COMPLETED
A Study to Investigate Atezolizumab and Chemotherapy Compared With Placebo and Chemotherapy in the Neoadjuvant Setting in Participants With Early Stage Triple Negative Breast Cancer
Hoffmann-La Roche n=333
NCT04335006 TERMINATED
A Phase 3 Study Comparing Carelizumab Plus Nab-paclitaxel and Apatinib, Carelizumab Plus Nab-paclitaxel, and Nab-paclitaxel in Patients With Advanced Triple Negative Breast Cancer.
Jiangsu HengRui Medicine Co., Ltd. n=80
NCT03002103 SUSPENDED
A Trial Evaluating the Efficacy and Safety of EndoTAG®-1 in Combination With Paclitaxel and Gemcitabine Compared With Paclitaxel and Gemcitabine as First-line Therapy in Patients With Visceral Metastatic Triple-negative Breast Cancer
SynCore Biotechnology Co., Ltd. n=420
NCT03674242 TERMINATED
Study of Eryaspase in Combination With Chemotherapy Versus Chemotherapy Alone for the Treatment of TNBC (TRYbeCA-2)
ERYtech Pharma n=27
NCT02425891 COMPLETED
A Study of Atezolizumab in Combination With Nab-Paclitaxel Compared With Placebo With Nab-Paclitaxel for Participants With Previously Untreated Metastatic Triple-Negative Breast Cancer (IMpassion130)
Hoffmann-La Roche n=902
NCT02555657 COMPLETED
Study of Single Agent Pembrolizumab (MK-3475) Versus Single Agent Chemotherapy for Metastatic Triple Negative Breast Cancer (MK-3475-119/KEYNOTE-119)
Merck Sharp & Dohme LLC n=622
NCT03055312 TERMINATED
Bicalutamide in Treatment of Androgen Receptor (AR) Positive Metastatic Triple Negative Breast Cancer
Sun Yat-sen University n=36
NCT02032277 COMPLETED
A Study Evaluating Safety and Efficacy of the Addition of ABT-888 Plus Carboplatin Versus the Addition of Carboplatin to Standard Chemotherapy Versus Standard Chemotherapy in Subjects With Early Stage Triple Negative Breast Cancer
AbbVie n=634
NCT01216111 COMPLETED
Adjuvant Platinum and Taxane in Triple-negative Breast Cancer (PATTERN)
Fudan University n=647
NCT03777579 SUSPENDED
A Study of First-line JS001 and Nab-paclitaxel Versus Palcelbo and Nab-Paclitaxel in Participants With Advanced Recurrent or Metastatic TNBC
CSPC ZhongQi Pharmaceutical Technology Co., Ltd. n=375
NCT01881230 COMPLETED
Evaluate Risk/Benefit of Nab Paclitaxel in Combination With Gemcitabine and Carboplatin Compared to Gemcitabine and Carboplatin in Triple Negative Metastatic Breast Cancer (or Metastatic Triple Negative Breast Cancer)
Celgene n=191
NCT02225470 COMPLETED
Eribulin Versus Vinorelbine in Subjects With Locally Recurrent or Metastatic Breast Cancer Previously Treated With Anthracyclines and Taxanes
Eisai Co., Ltd. n=530

Full Triple Negative Breast Cancer Pipeline

Every trial across Phase 1–4, plus enrollment analytics. Sortable, filterable, exportable.

Unlock with Pro

Frequently asked

Common questions about the Triple Negative Breast Cancer landscape

How many companies are developing Breast treatments?
7 companies have active or registered Breast programs in TheraRadar's competitive landscape (49 classified trials). The most active are AstraZeneca, Gilead Sciences, and Merck & Co..
What mechanisms of action are being developed for Breast?
5 distinct mechanisms of action appear across the Breast pipeline, including Trop-2 ADC, TROP-2 ADC (next-gen), Nectin-4 ADC, EGFR / HER3 bispecific ADC, and PD-L1 / VEGF-A bispecific antibody.
What is the most crowded mechanism in Breast?
Trop-2 ADC is the most contested mechanism in Breast, with 8 programs mapped to it.
Are there upcoming Breast clinical readouts or FDA decisions?
Near-term Breast catalysts include SKB264 (data readout, Jul '26); Sacituzumab govitecan- (data readout, Jun '27); Dato-DXd (data readout, Jul '27). Dates combine estimated trial primary-completion readouts and confirmed FDA decision dates.
Where does TheraRadar's Breast landscape data come from?
Programs are derived from industry-sponsored ClinicalTrials.gov registrations (2008–present) and classified by mechanism of action using a curated rule set plus an LLM pipeline. Every cell links to its underlying trials, so each program is verifiable.
Is the Breast heatmap free to use?
Yes — viewing and searching the Breast heatmap is free. A TheraRadar Pro subscription adds advanced filters, row/column selection, and one-click export to PowerPoint, PDF, and CSV.
How this is built — methodology & limits

These grids are only as good as the data and the classification behind them — so here is exactly what goes in, what stays out, how every assignment is made, and where the limits are.

Where the data comes from

Every heatmap is built from the public ClinicalTrials.gov registry, via its official API — interventional drug and biologic trials with a start date of 2008 or later. The master index holds over 145,000 trials and is refreshed weekly (see the “updated” date on this page). A disease landscape draws only from the active, Phase 1–3, industry-sponsored slice of that index.

  • In scope: industry-sponsored trials in Phase 1, 2, or 3, with an active status (recruiting, active-not-recruiting, not-yet-recruiting, or enrolling by invitation). Phase 4 sits in the index but is left out of the landscapes.
  • Filtered out: deeply stale programs (a primary completion date more than two years past with no update to completed or terminated); basket trials and incidental mentions (a trial counts toward a disease only when that disease is genuinely the subject of study — not a secondary cohort, an organ-of-origin overlap, or a passing mention); and healthy-volunteer studies.

We do not exclude trials by sponsor geography. Where a sponsor is based in China, the program is flagged on the page rather than hidden, so you can weigh it yourself. An automated test fails the weekly refresh if the underlying index is more than 14 days old, so a published grid is never built on a stale index.

How a trial is matched to a disease

Matching uses a structured medical ontology, not keyword guessing, and is designed so that no trial is ever silently dropped — every trial that clears the filters gets a classification, even if that is just “Other.” It runs as an ordered sequence of steps, stopping at the first that applies:

  1. Healthy-volunteer studies are set aside as non-disease trials.
  2. Ontology match — each tracked disease is linked to its official identifiers in the standard medical taxonomy (MeSH), so a trial can be matched even when its text uses a synonym.
  3. Curated disease patterns — a hand-maintained library of over 150 disease-name patterns covers the more granular indications across oncology, hematology, infectious disease, cardiometabolic, immunology, and neuropsychiatry.
  4. Basket guard — a trial matching four or more distinct diseases, or carrying explicit basket language (“tumor-agnostic,” “all solid tumors,” “pan-cancer”), is grouped into a single advanced-solid-tumor category rather than over-counted across every cancer it touches.
  5. Therapeutic-area roll-up — a trial with no specific match, but which the taxonomy still places under a broad area, is assigned to that area (“Oncology — other,” “Immunology — other,” …), checking cancers first so a site-specific tumor isn’t filed under its anatomical system.

A “drop-if-parent-present” rule keeps a generic name from drowning out a subtype: a trial matching both lupus and lupus nephritis is reported only as lupus nephritis. Internal abbreviations are translated to the plain disease names used across the site (for example, “CRC” becomes “Colorectal Cancer”), and the same classifier is shared by every heatmap, so the same trial always maps to the same disease wherever it appears.

How a drug is matched to its mechanism

Mechanism of action is the hardest part to get right, so it is assigned in layers — leaning on curated and public data first, with AI as a last resort:

  1. Curated rulebook (first). A rulebook we maintain — over 600 drug-to-mechanism rules — is checked first, matching on drug names, trial acronyms, sponsor trial identifiers, and intervention lists. First match wins, which stops a combination trial from being counted several times.
  2. Public molecular-target data. Where no rule applies, each intervention’s target is looked up in a public target database, with verbose or gene-symbol labels normalized into consistent short forms so one target isn’t split across several columns.
  3. Standard-of-care backbones. A small set of rules recognizes common combination scaffolds (checkpoint-inhibitor monotherapy, standard chemotherapy regimens, established standard-of-care agents) so they aren’t mistaken for the experimental arm.
  4. AI as a last resort, then cross-checked. Only for genuinely opaque sponsor code-names that none of the first three steps can resolve do we ask an AI model to propose a mechanism — applied only above a fixed confidence bar, then automatically cross-checked against the sponsor’s own pipeline page. Where AI and the sponsor agree, the program is marked sponsor-verified. Where they contradict, the label is discarded entirely — not shown, not counted.

New mechanism rules are independently double-verified before they’re trusted — a second, adversarial pass set up to disprove the first — and each is checked so it can’t mislabel an unrelated trial. Drugs whose mechanism isn’t publicly disclosed are shown openly as “Emerging — not yet disclosed” rather than guessed at: for a tool meant to support real decisions, “we don’t yet know” is a more trustworthy answer than a confident guess.

Where AI is used — and where it isn’t

The disease and mechanism matching above is driven first by deterministic rules and public ontologies, not AI. AI plays three bounded, disclosed roles: (1) an optional extra check that a trial genuinely studies the disease, on top of the ontology match; (2) inferring a trial’s treatment setting on the competitive grids when the rules don’t cover it, only above a fixed confidence bar; and (3) the last-resort mechanism step above, always cross-checked against the sponsor’s disclosures. Wherever an AI label reaches a cell, the page marks it (⚙️ or ✅) — AI is never the silent, sole source of what you see.

What the on-page markers mean

  • ✅ Sponsor-verified — AI proposed the mechanism and it matched the sponsor’s own pipeline page. High-trust.
  • ⚙️ AI-classified — AI proposed it above the confidence bar but it has not yet been cross-checked against the sponsor. Useful; verify before citing. It never means a person reviewed it.
  • ⚡ First-in-class — the mechanism hasn’t appeared in any other disease landscape we’ve built. This reflects the scope of landscapes published so far (the tooltip lists exactly which were scanned), not an absolute claim about the whole market.
  • 🌱 First-in-indication — the only program competing on that mechanism within this disease.
  • 🆕 NME candidate — the interventions match no drug in our approved-drug index, suggesting a new molecular entity. The index is incomplete — a signal, not a regulatory fact.
  • 🔗 Combination · 👶 Pediatric · 🔥 Hot (readout within six months) · ⏳ Stale (completion date passed but still marked active — often a stalled program).

Sponsor names are resolved through a curated parent/subsidiary map; unrecognized sponsors appear under their raw registry name. The registry records the sponsor at a trial’s inception, so names are as originally filed and may not reflect later acquisitions. To keep large grids legible, mechanisms with a single program are listed separately rather than crowding the main grid, and very small players are listed below it — presentation choices only; nothing is removed from the underlying counts.

How we score programs — “what’s about to move”

Each program carries a 0–100 score that deliberately ranks imminence over raw stage — the most decision-relevant signal on a competitive grid. It is the sum of:

  • Clinical phase — up to 40 points (Phase 3 = 40, Phase 2 = 25, Phase 1 = 10).
  • Readout proximity — up to 60 points (next readout <6 months = 60, 6–12 months = 45, 1–2 years = 30, distant = 5).
  • Stale penalty — the score is halved if a trial is past its expected readout but still listed as active.

Cell colour on the grid is driven by this score, so a Phase 2 program about to read out can — correctly — outrank a dormant Phase 3 one. It answers “what’s about to move,” not just “what’s furthest along.”

What each grid plots

  • Indication landscape (this page) — one disease — companies (rows) × mechanism of action (columns): who is competing, and on what mechanism.
  • Company portfolio — one company — diseases (rows) × mechanism (columns): where it is active, and what it is betting on.
  • MOA platform — one mechanism family — drugs (rows) × diseases (columns): who is working on this class, and where.
  • Competitive landscape — one disease — mechanism (rows) × clinical setting (columns), aggregated across companies; setting columns are tailored per disease (e.g. lines of therapy in oncology; biologic-naïve vs. biologic-experienced in IBD).

What we don’t claim

  • First-in-class is editorial, not absolute — “not seen in the landscapes we’ve built,” not “novel across the industry.”
  • NME candidate is a signal, not a filing — absent from our (incomplete) approved-drug index.
  • Disease matching is automated and not exhaustively validated per disease — ontology and pattern matching can occasionally include or miss a trial.
  • AI-classified mechanisms are machine-proposed — unconfirmed unless they also carry ✅.
  • Sponsor names are as-filed and may lag current ownership.
  • Grids are as fresh as their last rebuild from the weekly index — no faster continuous refresh is claimed.

Data: ClinicalTrials.gov v2 API + FDA Drugs@FDA (approved-drug index). Spot an error? [email protected].

Data: ClinicalTrials.gov · Trials registered 2008 onwards · Industry sponsors only