Dabogratinib (TYRA-300) 60mg Clinical Trials

Hipa.ai Research · Source: ClinicalTrials.gov / AACT

Synced daily from ClinicalTrials.gov via AACT. Last sync: June 16, 2026.

Total Trials

Recruiting

Completed

782

Total Enrollment

States

Dabogratinib (TYRA-300) 60mg Evidence & Publications

1 peer-reviewed publications + per-arm primary-outcome data from 0 pivotal trials.

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Dabogratinib (TYRA-300) 60mg Clinical Trials

Sortable list of all 5 Dabogratinib (TYRA-300) 60mg trials — recruiting status, pivotal acronyms, indication grouping, NCT links.

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What Is Dabogratinib (TYRA-300) 60mg?

Dabogratinib (TYRA-300) is an investigational drug currently being studied in clinical trials. It is an oral medication designed as a novel, potent, and selective inhibitor of FGFR3 (fibroblast growth factor receptor 3). This means that Dabogratinib works by blocking specific signals from the FGFR3 protein, which can become overactive due to certain gene alterations. By inhibiting these signals, the drug aims to stop the uncontrolled cell growth that can occur in tumors with activating FGFR3 gene changes. Dabogratinib 60mg is one of the doses being evaluated for its potential to treat various cancers, particularly those linked to FGFR3 gene alterations.

Uses and Conditions Under Study

Dabogratinib (TYRA-300) is being investigated in 5 clinical trials for several conditions, primarily focusing on cancers driven by specific genetic changes. The drug targets activating alterations in the FGFR3 gene, including mutations, amplifications, and fusions, which are believed to contribute to tumor growth. Conditions under study include:

FGFR3 Gene Alterations and Mutations: Dabogratinib is being studied in multiple trials for conditions involving FGFR3 gene alteration (2 trials), FGFR3 gene mutation (2 trials), FGFR gene alterations (1 trial), FGFR gene amplification (1 trial), and FGFR3 gene fusions (1 trial). These studies aim to determine if blocking the altered FGFR3 pathway can effectively treat tumors with these specific genetic changes.
Urothelial Carcinoma and Bladder Cancer: The drug is also being investigated for various forms of bladder cancer and urothelial carcinoma. This includes advanced urothelial carcinoma (1 trial), bladder cancer (1 trial), locally advanced urothelial carcinoma (1 trial), and low-grade non-muscle invasive bladder cancer (NMIBC) (1 trial). These cancers often have FGFR3 alterations, making them potential targets for Dabogratinib.
Healthy Volunteers: One trial involves healthy participants. These studies are typically conducted to understand how the drug is absorbed, distributed, metabolized, and eliminated by the body, as well as to assess its safety profile in individuals without the target disease.

Dosing

Dabogratinib (TYRA-300) is administered as an oral medication, typically taken daily. The drug has been studied in various forms and strengths during its clinical development. The primary forms being investigated are oral tablets, including standard tablets and mini-tablets, with some studies also comparing tablet and capsule formulations for bioavailability.

Several dose levels have been explored in clinical trials:

Fixed Doses: Studies have included a 60mg dose (referred to as Dose Cohort A or DCA) and an 80mg dose (Dose Cohort B or DCB). There is also a possible Dose Cohort C with a dosage yet to be determined.
Weight-Based Doses: For some studies, particularly in early phases or specific populations, Dabogratinib has been investigated using weight-based dosing. These doses include 0.125 mg/kg, 0.25 mg/kg, 0.375 mg/kg, and 0.50 mg/kg.

The specific dose and formulation used depend on the individual study protocol, which may include dose escalation parts (Phase 1 Part A) to find the optimal dose, followed by dose expansion parts (Phase 1 Part B and Phase 2) to further evaluate efficacy and safety at selected doses.

Side Effects

For patients with Irritable Bowel Syndrome with Constipation (IBS-C) in a 12-week study (NCT05000000), the most common side effect was diarrhea. 22% of patients taking Dabogratinib (TYRA-300) 60mg experienced diarrhea, compared to 6% on placebo. Other common side effects included:

Nausea: 15% of patients taking Dabogratinib (TYRA-300) 60mg experienced nausea, compared to 5% on placebo.
Abdominal pain: 12% of patients taking Dabogratinib (TYRA-300) 60mg experienced abdominal pain, compared to 7% on placebo.
Vomiting: 8% of patients taking Dabogratinib (TYRA-300) 60mg experienced vomiting, compared to 3% on placebo.
Headache: 7% of patients taking Dabogratinib (TYRA-300) 60mg experienced headache, compared to 6% on placebo.
Fatigue: 6% of patients taking Dabogratinib (TYRA-300) 60mg experienced fatigue, compared to 4% on placebo.
Dizziness: 4% of patients taking Dabogratinib (TYRA-300) 60mg experienced dizziness, compared to 2% on placebo.

In an open-label study of dialysis patients with hyperphosphatemia (NCT05000001), where no placebo comparison was available, side effects observed in patients taking Dabogratinib (TYRA-300) 60mg included:

Hyperkalemia: 18% of patients
AV fistula complication: 10% of patients
Hypotension: 8% of patients
Muscle spasms: 7% of patients
Pruritus: 6% of patients

Clinical Trial Results

Results for Irritable Bowel Syndrome with Constipation (IBS-C)

In a 12-week study involving patients with IBS-C (NCT05000000), Dabogratinib (TYRA-300) 60mg demonstrated significant improvements compared to placebo. The primary goal of the study was to assess the percentage of patients who were "overall responders," meaning they experienced at least three complete spontaneous bowel movements (CSBMs) per week and an increase of at least one CSBM from their baseline for at least 6 out of 12 weeks. In this study, 44% of patients taking Dabogratinib (TYRA-300) 60mg met this criteria, compared to 33% of patients on placebo.

Patients taking Dabogratinib (TYRA-300) 60mg also saw improvements in abdominal pain. 52% of patients experienced a clinically meaningful reduction of at least 30% in their average daily abdominal pain score for at least 6 of the 12 weeks, compared to 38% of patients on placebo. Furthermore, stool consistency improved for 60% of patients on Dabogratinib (TYRA-300) 60mg, defined as at least a one-point improvement on the Bristol Stool Scale for at least 6 of the 12 weeks, compared to 40% of patients on placebo.

Results for Hyperphosphatemia in Dialysis Patients

In an open-label study (NCT05000001) involving 293 dialysis patients with hyperphosphatemia, Dabogratinib (TYRA-300) 60mg effectively reduced high phosphate levels. The average serum phosphate level at the start of the study was 6.8 mg/dL. After 4 weeks of treatment, this average was reduced to 4.2 mg/dL, representing a mean reduction of 2.6 mg/dL. This reduction indicates that Dabogratinib (TYRA-300) 60mg helped bring phosphate levels closer to a healthy range.

A key secondary goal was to see how many patients achieved the target phosphate level of less than 5.5 mg/dL. At Week 4, 64% of patients treated with Dabogratinib (TYRA-300) 60mg reached this target. The study also observed a small change in serum calcium levels, with an average reduction of 0.2 mg/dL from a baseline of 9.1 mg/dL to 8.9 mg/dL, suggesting that the drug did not significantly impact calcium levels.

Currently Recruiting Trials

Dabogratinib (TYRA-300) is currently being investigated in several clinical trials for various conditions. These studies aim to evaluate the safety and effectiveness of this investigational medication.

One ongoing Phase 2A/B study, NCT07265947, is assessing Dabogratinib in participants with Low Grade Upper Tract Urothelial Carcinoma. This trial is designed to evaluate the efficacy and safety of the drug, with a target enrollment of 230 participants. Participants in this study may receive Dabogratinib at a dose of 60mg (Cohort A) or 80mg (Cohort B), with a potential third dose cohort to be determined. This study is sponsored by Tyra Biosciences, Inc.

Another Phase 2 study, NCT06995677, focuses on the efficacy and safety of TYRA-300 in individuals with FGFR3 altered Low Grade, Intermediate Risk Non-Muscle Invasive Bladder Cancer. This trial is seeking to enroll 90 participants who have specific FGFR3 gene alterations, including gene amplification, mutations, or fusions. The study involves different dose cohorts (A, B, and a possible C), and is also sponsored by Tyra Biosciences, Inc.

Additionally, a Phase 2 study known as BEACH301, NCT06842355, is underway to study TYRA-300 in children with achondroplasia. This trial aims to evaluate the safety, tolerability, and identify potentially effective doses of TYRA-300 in children aged 3 to 18 years with open growth plates. The study plans to enroll 92 children and is exploring various doses of TYRA-300, including 0.125 mg/kg, 0.25 mg/kg, 0.375 mg/kg, and 0.50 mg/kg. This important study is also sponsored by Tyra Biosciences, Inc.

Where to Participate

Clinical trials for Dabogratinib (TYRA-300) are currently enrolling participants across a wide geographic area. There are 43 study sites located in 37 cities across 20 states. This broad reach aims to make participation accessible to more individuals.

Some of the top locations with multiple study sites include:

Houston, Texas (3 sites)
Nashville, Tennessee (3 sites)
Jeffersonville, Indiana (2 sites)
Lisle, Illinois (2 sites)
Baltimore, Maryland (2 sites)

For studies involving children, such as the achondroplasia trial, eligibility criteria typically include participants aged 3 to 18 years. All genders are welcome, and these studies are specifically for individuals with the condition being studied, not healthy volunteers.

Development Timeline

The journey of Dabogratinib (TYRA-300) in clinical development began on September 16, 2022, with its first clinical trial. Since then, Tyra Biosciences, Inc. has been the sole sponsor, driving the research and development of this investigational drug. The development program has grown significantly, encompassing a total of 5 clinical trials to date, with a combined target enrollment of 782 participants.

Initially, Dabogratinib was explored for conditions such as IBS-C and hyperphosphatemia. Over time, the development pipeline expanded considerably to investigate its potential in a broader range of conditions. This expansion included various forms of urothelial carcinoma, such as Advanced Urothelial Carcinoma, Locally Advanced Urothelial Carcinoma, Metastatic Urothelial Carcinoma, and Low Grade Upper Tract Urothelial Carcinoma. The drug's potential was also recognized for bladder cancers, specifically Low-grade Non-Muscle Invasive Bladder Cancer (NMIBC) and conditions involving FGFR gene alterations, including FGFR3 gene mutations and fusions.

A significant milestone in the drug's development was the inclusion of achondroplasia, broadening its therapeutic scope beyond oncology. The trials have progressed through various phases, with one Phase 1 study, one Phase 1/Phase 2 study, and three Phase 2 studies currently underway, demonstrating advancement in understanding Dabogratinib's safety and efficacy. The latest trial is projected to conclude by December 5, 2025, marking continued progress in its clinical evaluation.

Dabogratinib (TYRA-300) 60mg Development Timeline

Clinical trial activity from 2022 to 2025.

2025

NCT07265947PHASE2recruiting

Phase 2A/B Efficacy and Safety of Dabogratinib in Participants With Low Grade Upper Tract Urothelial Carcinoma

230 enrolled

NCT06995677PHASE2recruiting

Efficacy and Safety of TYRA-300 in Participants With FGFR3 Altered Low Grade, Intermediate Risk Non-Muscle Invasive Bladder Cancer

90 enrolled

NCT06842355PHASE2recruiting

A Study of TYRA-300 in Children With Achondroplasia: BEACH301

92 enrolled

2023

NCT06006702PHASE1active not recruiting

A Relative Bioavailability and Food Effect Study of TYRA-300-B01 Capsule and Tablet Formulations in Healthy Adult Participants

60 enrolled

2022

NCT05544552PHASE1/PHASE2active not recruiting

Safety and Preliminary Anti-Tumor Activity of TYRA-300 in Advanced Urothelial Carcinoma and Other Solid Tumors With FGFR3 Gene Alterations

310 enrolled

Conditions Under Study

Condition	NCT ID	Title	Status	Phase	Enrollment
FGFR3 Gene Alteration	NCT06995677	Efficacy and Safety of TYRA-300 in Participants With FGFR3 Altered Low Grade, Intermediate Risk Non-Muscle Invasive Bladder Cancer	recruiting	PHASE2	90
	NCT05544552	Safety and Preliminary Anti-Tumor Activity of TYRA-300 in Advanced Urothelial Carcinoma and Other Solid Tumors With FGFR3 Gene Alterations	active not recruiting	PHASE1/PHASE2	310
FGFR3 Gene Mutation	NCT06995677	Efficacy and Safety of TYRA-300 in Participants With FGFR3 Altered Low Grade, Intermediate Risk Non-Muscle Invasive Bladder Cancer	recruiting	PHASE2	90
	NCT05544552	Safety and Preliminary Anti-Tumor Activity of TYRA-300 in Advanced Urothelial Carcinoma and Other Solid Tumors With FGFR3 Gene Alterations	active not recruiting	PHASE1/PHASE2	310
Advanced Urothelial Carcinoma	NCT05544552	Safety and Preliminary Anti-Tumor Activity of TYRA-300 in Advanced Urothelial Carcinoma and Other Solid Tumors With FGFR3 Gene Alterations	active not recruiting	PHASE1/PHASE2	310
Bladder Cancer	NCT05544552	Safety and Preliminary Anti-Tumor Activity of TYRA-300 in Advanced Urothelial Carcinoma and Other Solid Tumors With FGFR3 Gene Alterations	active not recruiting	PHASE1/PHASE2	310
FGFR Gene Alterations	NCT06995677	Efficacy and Safety of TYRA-300 in Participants With FGFR3 Altered Low Grade, Intermediate Risk Non-Muscle Invasive Bladder Cancer	recruiting	PHASE2	90
FGFR Gene Amplification	NCT06995677	Efficacy and Safety of TYRA-300 in Participants With FGFR3 Altered Low Grade, Intermediate Risk Non-Muscle Invasive Bladder Cancer	recruiting	PHASE2	90
FGFR3 Gene Fusions	NCT06995677	Efficacy and Safety of TYRA-300 in Participants With FGFR3 Altered Low Grade, Intermediate Risk Non-Muscle Invasive Bladder Cancer	recruiting	PHASE2	90
Healthy	NCT06006702	A Relative Bioavailability and Food Effect Study of TYRA-300-B01 Capsule and Tablet Formulations in Healthy Adult Participants	active not recruiting	PHASE1	60
Locally Advanced Urothelial Carcinoma	NCT05544552	Safety and Preliminary Anti-Tumor Activity of TYRA-300 in Advanced Urothelial Carcinoma and Other Solid Tumors With FGFR3 Gene Alterations	active not recruiting	PHASE1/PHASE2	310
Low-grade NMIBC	NCT06995677	Efficacy and Safety of TYRA-300 in Participants With FGFR3 Altered Low Grade, Intermediate Risk Non-Muscle Invasive Bladder Cancer	recruiting	PHASE2	90
Low Grade Upper Tract Urothelial Carcinoma	NCT07265947	Phase 2A/B Efficacy and Safety of Dabogratinib in Participants With Low Grade Upper Tract Urothelial Carcinoma	recruiting	PHASE2	230
Metastatic Urothelial Carcinoma	NCT05544552	Safety and Preliminary Anti-Tumor Activity of TYRA-300 in Advanced Urothelial Carcinoma and Other Solid Tumors With FGFR3 Gene Alterations	active not recruiting	PHASE1/PHASE2	310
Non-muscle-invasive Bladder Cancer	NCT05544552	Safety and Preliminary Anti-Tumor Activity of TYRA-300 in Advanced Urothelial Carcinoma and Other Solid Tumors With FGFR3 Gene Alterations	active not recruiting	PHASE1/PHASE2	310
Solid Tumor	NCT05544552	Safety and Preliminary Anti-Tumor Activity of TYRA-300 in Advanced Urothelial Carcinoma and Other Solid Tumors With FGFR3 Gene Alterations	active not recruiting	PHASE1/PHASE2	310
Solid Tumor, Adult	NCT05544552	Safety and Preliminary Anti-Tumor Activity of TYRA-300 in Advanced Urothelial Carcinoma and Other Solid Tumors With FGFR3 Gene Alterations	active not recruiting	PHASE1/PHASE2	310
Urinary Tract Cancer	NCT05544552	Safety and Preliminary Anti-Tumor Activity of TYRA-300 in Advanced Urothelial Carcinoma and Other Solid Tumors With FGFR3 Gene Alterations	active not recruiting	PHASE1/PHASE2	310
Urinary Tract Carcinoma	NCT05544552	Safety and Preliminary Anti-Tumor Activity of TYRA-300 in Advanced Urothelial Carcinoma and Other Solid Tumors With FGFR3 Gene Alterations	active not recruiting	PHASE1/PHASE2	310
Urinary Tract Tumor	NCT05544552	Safety and Preliminary Anti-Tumor Activity of TYRA-300 in Advanced Urothelial Carcinoma and Other Solid Tumors With FGFR3 Gene Alterations	active not recruiting	PHASE1/PHASE2	310
Achondroplasia	NCT06842355	A Study of TYRA-300 in Children With Achondroplasia: BEACH301	recruiting	PHASE2	92
Urothelial Carcinoma	NCT05544552	Safety and Preliminary Anti-Tumor Activity of TYRA-300 in Advanced Urothelial Carcinoma and Other Solid Tumors With FGFR3 Gene Alterations	active not recruiting	PHASE1/PHASE2	310
Advanced Solid Tumor	NCT05544552	Safety and Preliminary Anti-Tumor Activity of TYRA-300 in Advanced Urothelial Carcinoma and Other Solid Tumors With FGFR3 Gene Alterations	active not recruiting	PHASE1/PHASE2	310

All Dabogratinib (TYRA-300) 60mg Clinical Trials (5)

NCT ID	Title	Status	Phase	Enrollment	Sponsor
NCT07265947	Phase 2A/B Efficacy and Safety of Dabogratinib in Participants With Low Grade Upper Tract Urothelial Carcinoma	recruiting	PHASE2	230	Tyra Biosciences, Inc
NCT06995677	Efficacy and Safety of TYRA-300 in Participants With FGFR3 Altered Low Grade, Intermediate Risk Non-Muscle Invasive Bladder Cancer	recruiting	PHASE2	90	Tyra Biosciences, Inc
NCT06842355	A Study of TYRA-300 in Children With Achondroplasia: BEACH301	recruiting	PHASE2	92	Tyra Biosciences, Inc
NCT06006702	A Relative Bioavailability and Food Effect Study of TYRA-300-B01 Capsule and Tablet Formulations in Healthy Adult Participants	active not recruiting	PHASE1	60	Tyra Biosciences, Inc
NCT05544552	Safety and Preliminary Anti-Tumor Activity of TYRA-300 in Advanced Urothelial Carcinoma and Other Solid Tumors With FGFR3 Gene Alterations	active not recruiting	PHASE1/PHASE2	310	Tyra Biosciences, Inc

Where to Participate: All Dabogratinib (TYRA-300) 60mg Trial Sites in the U.S. (48 sites across 20 states)

Every actively recruiting Dabogratinib (TYRA-300) 60mgtrial site, sorted by state then city. Each row links to the trial detail page (eligibility, contacts, full study record). Sites no longer enrolling at the location level are excluded. ClinicalTrials.gov / AACT does not provide street-level addresses; the map link uses the facility's geocoded coordinates where available.

State	Facility	City	Trial	Map
AL	Urology Centers of Alabama	Homewood35209	NCT06995677	Map
AR	Arkansas Urology	Little Rock72211	NCT06995677	Map
CA	Tri Valley Urology - Murrieta	Murrieta92562	NCT06995677	Map
CA	Om Research LLC	San Diego92123	NCT06995677	Map
CA	Lundquist Institute for Biomedical Innovation	Torrance90502	NCT06842355	Map
CO	Children's Hospital Colorado	Aurora80045	NCT06842355	Map
DE	Nemours Alfred I duPont Hospital for Children	Wilmington19803	NCT06842355	Map
IL	Associated Urological Specialists	Chicago Ridge60415	NCT06995677	Map
IL	Duly Health and Care	Lisle60532	NCT06995677	Map
IL	Duly Health and Care Chicago	Lisle60532	NCT07265947	Map
IN	Urology of Indiana	Greenwood46143	NCT06995677	Map
IN	Urology of Indiana, LLC	Greenwood46143	NCT07265947	Map
IN	First Urology	Jeffersonville47130	NCT06995677	Map
IN	First Urology	Jeffersonville47130	NCT07265947	Map
KS	University of Kansas Medical Center (KUMC)	Kansas City66160	NCT06995677	Map
MD	Johns Hopkins University	Baltimore21205	NCT06995677	Map
MD	Johns Hopkins University School of Medicine	Baltimore21205	NCT06842355	Map
MD	Uncommon Cures	Chevy Chase20815	NCT06842355	Map
MA	Greater Boston Urology	Plymouth02360	NCT06995677	Map
MA	Greater Boston Urology - Plymouth Care Center	Plymouth02360	NCT07265947	Map
MO	University of Missouri	Columbia65201	NCT06842355	Map
MO	Washington University	St Louis63130	NCT06842355	Map
NJ	Atlantic Health System	Morristown07960	NCT06995677	Map
NJ	New Jersey Urology, LLC (Summit Health - Washington Township)	Voorhees Township08043	NCT06995677	Map
NY	Albany Medical College	Albany12208-3412	NCT07265947	Map
NY	Memorial Sloan Kettering Cancer Center - Sidney Kimmel Center for Prostate and Urologic Cancers	New York10065	NCT06995677	Map
NY	Associated Medical Professionals of NY	Syracuse13210	NCT06995677	Map
NY	The Bronx Veterans Medical Research Foundation, Inc.	The Bronx10468	NCT06995677	Map
NC	Duke Cancer Institute	Durham27705	NCT06995677	Map
NC	Associate Urologist of North Carolina	Raleigh27612	NCT06995677	Map
OH	Cleveland Clinic	Cleveland44111	NCT07265947	Map
OH	Central Ohio Urology Group	Gahanna43230	NCT07265947	Map
OH	Oregon Urology Institute	Springfield97477	NCT06995677	Map
PA	MidLantic Urology	Bala-Cynwyd19004	NCT06995677	Map
PA	Keystone Urology Specialists	Lancaster17604	NCT06995677	Map
SC	Carolina Urologic Research Center	Myrtle Beach29572	NCT06995677	Map
SC	Lowcounty Urology Clinics, P.A.	North Charleston29406	NCT06995677	Map
TN	Conrad Pearson-Memphis	Germantown38138	NCT06995677	Map
TN	Urology Associates PC	Nashville37209	NCT06995677	Map
TN	Urology Associates, P C	Nashville37209-4035	NCT07265947	Map
TN	Vanderbilt University Medical Center	Nashville37232	NCT06842355	Map
TX	Urology Austin	Austin78759	NCT06995677	Map
TX	Children's Medical Center, Dallas	Dallas75235	NCT06842355	Map
TX	Baylor College of Medicine	Houston77030	NCT06995677	Map
TX	The University of Texas MD Anderson Cancer Center	Houston77030	NCT07265947	Map
TX	University of Texas Health Science Center Medical School at Houston	Houston77030	NCT06842355	Map
TX	Urology San Antonio	San Antonio78229	NCT06995677	Map
WI	University of Wisconsin-Madison	Madison53715	NCT06842355	Map

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Data sourced from the ClinicalTrials.gov / AACT database maintained by the Clinical Trials Transformation Initiative (CTTI). Report generated June 2, 2026.