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Phase I/II Study of Intrathecal/Ommaya T-DXd in HER2-Expressing Breast Cancer With Leptomeningeal/Brain Metastases

Evaluating Safety and Efficacy of INtrathecal or Ommaya ReserVoir Administration of T-DXd in Patients With HER2-Expressing Breast Cancer With Active Leptomeningeal and/or Brain Metastases Based on Systemic Therapy: Phase I/II Study

Status
Recruiting
Phases
Phase 1Phase 2
Study type
Interventional
Source
ClinicalTrials.gov
Registry ID
NCT07134153
Acronym
INOVATE
Enrollment
139
Registered
2025-08-21
Start date
2025-04-18
Completion date
2027-02-28
Last updated
2025-08-21

For informational purposes only — not medical advice. Sourced from public registries and may not reflect the latest updates. Terms

Conditions

Breast Cancer

Brief summary

Multiple trials confirm systemic T-DXd efficacy in HER2+ breast cancer with leptomeningeal/brain metastases, yet median LM survival remains 3-4 months, highlighting unmet needs. While systemic therapies improve survival, intracranial disease control remains limited due to poor BBB penetration. Preclinical data show no detectable T-DXd/DXd in CSF, though intrathecal trastuzumab demonstrates preliminary safety/efficacy in HER2+ LM. This study evaluates intrathecal/intra-Ommaya T-DXd plus systemic therapy in active HER2+ meningeal/brain metastases, assessing safety, intracranial efficacy, and CSF/peripheral blood T-DXd distribution to clarify BBB penetration potential. Findings may guide novel therapeutic strategies for this high-need population.

Detailed description

Multiple clinical trials have demonstrated the efficacy of systemic T-DXd in advanced HER2-expressing breast cancer with leptomeningeal and/or brain metastases. However, the median survival of leptomeningeal metastasis (LM) patients remains only 3-4 months, and treatment options for isolated brain metastases are limited, underscoring the need for more effective therapeutic strategies. While systemic therapies have prolonged survival in advanced breast cancer, intracranial disease management remains constrained by a lack of effective local treatments. As the use of T-DXd increases, the progression of intracranial lesions in patients who have received prior local therapy or lack indications for radiotherapy has become a critical unmet clinical challenge. Conventional understanding holds that large biologic molecules poorly penetrate the blood-brain barrier (BBB). Preclinical studies detected neither T-DXd nor free DXd (payload) in cerebrospinal fluid (CSF), and the distribution of T-DXd in human CSF remains uncharacterized. However, preliminary data suggest that intrathecal trastuzumab-alone or combined with pertuzumab-exhibits acceptable safety and efficacy in HER2-positive LM.

Interventions

DRUGT-DXd

Evaluating safety and efficacy of intrathecal or ommaya reservoir administration of T-DXd in patients with HER2-expressing breast cancer with active leptomeningeal and/or brain metastases based on systemic therapy

Sponsors

Fudan University
Lead SponsorOTHER

Study design

Allocation
NON_RANDOMIZED
Intervention model
PARALLEL
Primary purpose
TREATMENT
Masking
NONE

Eligibility

Sex/Gender
ALL
Age
18 Years to No maximum
Healthy volunteers
No

Inclusion criteria

* Age ≥18 years, regardless of gender. * HER2-expressing advanced or metastatic breast cancer * Leptomeningeal metastasis * Subjects with active brain metastases only must have at least one intracranially measurable lesion (RANO-BM criteria). * Adequate organ and bone marrow function * No radiotherapy, chemotherapy, targeted therapy, immunotherapy, endocrine therapy, or surgery within 2 weeks prior to enrollment (or within 5 half-lives of prior therapy, whichever is shorter). * All prior treatment-related toxicities must have resolved to ≤Grade 1

Exclusion criteria

* Diagnosis of other malignancies within the past 5 years, except for cured carcinoma in situ of the cervix, basal cell carcinoma or squamous cell carcinoma of the skin, other in situ carcinomas, or papillary thyroid carcinoma. * Uncontrolled concurrent illnesses including, but not limited to: persistent or active infections, uncontrolled or clinically significant cardiovascular diseases, severe chronic gastrointestinal disorders with diarrhea, or psychiatric/social conditions that may compromise compliance with study requirements, significantly increase AE risks, or impair the subject's ability to provide written informed consent. * History of (non-infectious) ILD/non-infectious pneumonitis requiring steroid therapy, current ILD/non-infectious pneumonitis, or suspected ILD/non-infectious pneumonitis that cannot be ruled out by imaging during screening. * Clinically significant pulmonary comorbidities * Use of immunosuppressants or systemic corticosteroids (\>10 mg/day prednisone equivalent) for immunosuppression within 2 weeks prior to first dose (excluding intranasal/inhaled corticosteroids). * Any active autoimmune disease or history of autoimmune disease with potential recurrence. * Uncontrolled infections requiring IV antibiotics, antivirals, or antifungals. * Active primary immunodeficiency, known HIV infection, active HBV (HBsAg+ with HBV DNA ≥500 IU/mL) or HCV infection. HCV antibody-positive subjects are eligible only if PCR confirms HCV RNA negativity. * Radiographic evidence of tumor encasement/invasion of major blood vessels, or investigator-determined high risk of fatal hemorrhage due to probable vascular invasion during treatment. * Pregnant/lactating women, or subjects of reproductive potential unwilling/unable to use effective contraception. * Any other condition deemed by investigators to potentially affect trial conduct or outcome interpretation.

Design outcomes

Primary

MeasureTime frameDescription
Phase II Stage Cohorts A: LM-OS18 monthsCohorts A: leptomeningeal metastasis-overall survival(LM-OS)
Phase II Stage Cohorts B: LM-OS18 monthsCohorts B: leptomeningeal metastasis-overall survival(LM-OS)
Phase II Stage Cohorts C: LM-ORR18 monthsCohorts C: leptomeningeal metastasis-Objective Response Rate(LM-ORR)
Phase I Stage Cohort A: Maximum Tolerated Dose (MTD)Up to 21 days after the first doseCohort A: Maximum Tolerated Dose (MTD) of intracapsular administration,In the dose increment stage, the highest dose whose estimated DLT rate is closest to the target DLT rate but does not exceed the upper bound of the equivalent interval of DLT rate is selected as MTD.
Phase I Stage Cohort B: Maximum serum concentration (Cmax)Up to 21 days after the first doseCohort B: Maximum serum concentration (Cmax) of T-DXd in cerebrospinal fluid and blood will be investigated.
Phase I Stage Cohort B:Time to maximum serum concentration (Tmax)Up to 21 days after the first doseCohort B: Time to maximum serum concentration (Tmax) of T-DXd in cerebrospinal fluid and blood will be investigated.
Phase I Stage Cohort B:Half-life (T1/2)Up to 21 days after the first doseCohort B: Half-life (T1/2) of T-DXd in cerebrospinal fluid and blood will be investigated.
Phase II Stage Cohorts D: LM-ORR18 monthsCohorts D: leptomeningeal metastasis-Objective Response Rate(LM-ORR)
Phase II Stage Cohorts E: LM-OS18 monthsCohorts E: leptomeningeal metastasis-overall survival(LM-OS)
Phase II Stage Cohorts F: LM-OS18 monthsCohorts F: leptomeningeal metastasis-overall survival(LM-OS)
Phase II Stage Cohorts G: LM-ORR18 monthsCohorts G: leptomeningeal metastasis-Objective Response Rate(LM-ORR)
Phase II Stage Cohorts H: LM-ORR18 monthsCohorts H: leptomeningeal metastasis-Objective Response Rate(LM-ORR)

Countries

China

Contacts

Primary ContactJian Zhang, MD, PhD
syner2000@163.com+8664175590
Backup ContactYanchun Meng, MD
ycmclinicaltrials@126.com+8664175590

Outcome results

None listed

Source: ClinicalTrials.gov · Data processed: Feb 4, 2026