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Clinical Trial Details — Status: Recruiting

Administrative data

NCT number NCT06103864
Other study ID # D7630C00001
Secondary ID
Status Recruiting
Phase Phase 3
First received
Last updated
Start date November 23, 2023
Est. completion date April 23, 2029

Study information

Verified date May 2024
Source AstraZeneca
Contact AstraZeneca Clinical Study Information Center
Phone 1-877-240-9479
Email information.center@astrazeneca.com
Is FDA regulated No
Health authority
Study type Interventional

Clinical Trial Summary

This is a Phase III, randomised, open-label, 3-arm, multicentre, international study assessing the efficacy and safety of Dato-DXd with or without durvalumab compared with investigator's choice chemotherapy in combination with pembrolizumab in participants with PD-L1 positive locally recurrent inoperable or metastatic TNBC.


Description:

The primary objective of the study is to demonstrate superiority of Dato-DXd + durvalumab relative to ICC + pembrolizumab by assessment of PFS as assessed by BICR in participants with PD-L1 positive locally recurrent inoperable or metastatic TNBC. The study will be stratified based on geographic location (US/Canada/Europe vs. Dato-DXd monotherapy enrolling countries vs. rest of world), disease-free interval (DFI) history (de novo vs. prior DFI 6 to 12 months vs. prior DFI > 12 months), and prior PD-1/PD-L1 treatment for early stage TNBC (yes vs. no). This study aims to see if Dato-DXd with durvalumab allows patients to live longer without their breast cancer getting worse, or simply to live longer, compared to patients receiving standard of care chemotherapy and pembrolizumab. This study is also looking to see how the treatment and the breast cancer affects patients' quality of life.


Recruitment information / eligibility

Status Recruiting
Enrollment 625
Est. completion date April 23, 2029
Est. primary completion date September 1, 2026
Accepts healthy volunteers No
Gender All
Age group 18 Years and older
Eligibility Key Inclusion Criteria - Histologically or cytologically documented locally recurrent inoperable, which cannot be treated with curative intent, or metastatic TNBC, as defined by the ASCO-CAP guidelines. - ECOG PS 0 or 1. - All participants must provide a FFPE metastatic or locally recurrent inoperable tumour sample. - PD-L1 positive TNBC based on results from an appropriately validated investigational PD-L1 (22C3) assay (CPS = 10) from a sponsor designated central laboratory. - No prior chemotherapy or targeted systemic anti-cancer therapy for metastatic or locally recurrent inoperable breast cancer. - Patients with recurrent disease will be eligible if they have completed treatment for Stage I-III breast cancer, if indicated, and =6 months have elapsed between completion of treatment with curative intent and the first documented recurrence. - Eligible for one of the chemotherapy options listed as ICC (paclitaxel, nab-paclitaxel, or gemcitabine + carboplatin). - Measurable disease as per RECIST 1.1. - Adequate bone marrow reserve and organ function. - Male and female participants of childbearing potential must agree to use protocol-specified method(s) of contraception. Key Exclusion Criteria - As judged by investigator, severe or uncontrolled medical conditions including systemic diseases, history of allogeneic organ transplant and active bleeding diseases, ongoing or active infection, significant cardiac or psychological conditions. - History of another primary malignancy except for malignancy treated with curative intent with no known active disease within 3 years before Cycle 1 Day 1 and of low potential risk for recurrence. - Neoplastic spinal cord compression or active brain metastases, leptomeningeal carcinomatosis or history of leptomeningeal carcinomatosis. - Participants with treated clinically inactive brain metastases that are no longer symptomatic, who require no treatment with corticosteroids or anticonvulsants, may be included in the study if they have recovered from acute toxic effects of radiotherapy. - Uncontrolled infection requiring IV antibiotics, antivirals or antifungals. - Active or uncontrolled hepatitis B or C virus infection. - Known HIV infection that is not well controlled. - Uncontrolled or significant cardiac disease. - History of non-infectious ILD/pneumonitis (including radiation pneumonitis) that required steroids, current ILD/pneumonitis, or suspected ILD/pneumonitis that cannot be ruled out by imaging at screening. - Severe pulmonary function compromise. - Clinically significant corneal disease. - Active or prior documented autoimmune or inflammatory disorders. - Prior exposure to any treatment including ADC containing a chemotherapeutic agent targeting topoisomerase I and TROP2-targeted therapy. - Any concurrent anti-cancer treatment. - Participants with a known severe hypersensitivity to PD-1/PD-L1 inhibitors or Dato-DXd. - Currently pregnant (confirmed with positive pregnancy test), breastfeeding or planning to become pregnant.

Study Design


Intervention

Drug:
Dato-DXd
Provided in 100mg vials. IV infusion. Experimental drug.
Durvalumab
Provided in 500mg vials. IV infusion. Experimental drug.
Paclitaxel
IV infusion. Active comparator.
Nab-paclitaxel
IV infusion. Active comparator.
Gemcitabine
IV infusion. Active comparator.
Carboplatin
IV infusion. Active comparator.
Pembrolizumab
IV infusion. Active comparator.

Locations

Country Name City State
Argentina Research Site Buenos Aires
Argentina Research Site Caba
Argentina Research Site Caba
Argentina Research Site Caba
Argentina Research Site Ciudad Autonoma Bs As
Argentina Research Site Rosario
Argentina Research Site Rosario
Argentina Research Site San Nicolas de Los Arroyos
Australia Research Site Camperdown
Australia Research Site Darlinghurst
Australia Research Site Heidelberg
Australia Research Site Melbourne
Australia Research Site Nedlands
Australia Research Site Waratah
Brazil Research Site Barretos
Brazil Research Site Curitiba
Brazil Research Site Florianópolis
Brazil Research Site Goiânia
Brazil Research Site Itajai
Brazil Research Site Porto Alegre
Brazil Research Site Recife
Brazil Research Site Sao Paulo
Brazil Research Site São Paulo
Brazil Research Site Teresina
Canada Research Site Barrie Ontario
Canada Research Site Greenfield Park Quebec
Canada Research Site Montreal Quebec
Canada Research Site Montréal Quebec
Canada Research Site Quebec
Canada Research Site Regina Saskatchewan
Canada Research Site Saskatoon Saskatchewan
Canada Research Site Toronto Ontario
China Research Site Beijing
China Research Site Beijing
China Research Site Bengbu
China Research Site Changchun
China Research Site Changsha
China Research Site Changsha
China Research Site Chengdu
China Research Site Chengdu
China Research Site Chongqing
China Research Site Fuzhou
China Research Site Guangzhou
China Research Site Guangzhou
China Research Site Guangzhou
China Research Site Hangzhou
China Research Site Hangzhou
China Research Site Harbin
China Research Site Hefei
China Research Site Ji Nan
China Research Site Nanchang
China Research Site Nanjing
China Research Site Nanning
China Research Site Shandong
China Research Site Shanghai
China Research Site Shanghai
China Research Site Shenyang
China Research Site Tianjin
China Research Site Wenzhou
China Research Site Wuhan
China Research Site Wuhan
China Research Site Xi'an
China Research Site Xiamen
China Research Site Xintai
China Research Site Xuzhou
China Research Site Zhengzhou
China Research Site Zhengzhou
France Research Site Lille
France Research Site Lyon
France Research Site Paris
France Research Site Saint Herblain Cedex
France Research Site Toulouse Cedex 9
Germany Research Site Düsseldorf
Germany Research Site Essen
Germany Research Site Georgsmarienhütte
Germany Research Site Hamburg
Germany Research Site Hannover
Germany Research Site Heidelberg
Germany Research Site Heilbronn
Germany Research Site Leipzig
India Research Site Calicut
India Research Site Kochi
India Research Site Kolkata
India Research Site Marg Jaipur
India Research Site Mohali
India Research Site Mysuru
India Research Site Nagpur
India Research Site Nashik
India Research Site New Delhi
India Research Site New Delhi
India Research Site Pondicherry
India Research Site Surat
India Research Site Vadodara
India Research Site Vishakapatnam
Italy Research Site Empoli
Italy Research Site Milan
Italy Research Site Modena
Italy Research Site Napoli
Italy Research Site Padova
Italy Research Site Roma
Italy Research Site Rozzano
Japan Research Site Akashi-shi
Japan Research Site Bunkyo-ku
Japan Research Site Bunkyo-ku
Japan Research Site Chiba-shi
Japan Research Site Chuo-ku
Japan Research Site Fukuoka-shi
Japan Research Site Fukushima-shi
Japan Research Site Gifu-shi
Japan Research Site Hidaka-shi
Japan Research Site Hiroshima-shi
Japan Research Site Hiroshima-shi
Japan Research Site Isehara-shi
Japan Research Site Kamogawa-shi
Japan Research Site Kashiwa
Japan Research Site Kitaadachi-gun
Japan Research Site Koto-ku
Japan Research Site Kumamoto-shi
Japan Research Site Kurume-shi
Japan Research Site Matsuyama-shi
Japan Research Site Nagoya-shi
Japan Research Site Nagoya-shi
Japan Research Site Niigata-shi
Japan Research Site Nishinomiya-shi
Japan Research Site Okayama-shi
Japan Research Site Osaka-shi
Japan Research Site Osakasayama-shi
Japan Research Site Ota-shi
Japan Research Site Sapporo-shi
Japan Research Site Sendai-shi
Japan Research Site Shinagawa-ku
Japan Research Site Shinjuku-ku
Japan Research Site Shinjuku-ku
Japan Research Site Tsu-shi
Japan Research Site Tsukuba
Japan Research Site Yokohama-shi
Korea, Republic of Research Site Busan
Korea, Republic of Research Site Daegu
Korea, Republic of Research Site Goyang-si
Korea, Republic of Research Site Seoul
Korea, Republic of Research Site Seoul
Korea, Republic of Research Site Seoul
Korea, Republic of Research Site Seoul
Korea, Republic of Research Site Seoul
Korea, Republic of Research Site Seoul
Korea, Republic of Research Site Seoul
Mexico Research Site CD Mexico
Mexico Research Site Guadalajara
Mexico Research Site Guadalajara
Mexico Research Site Mexico
Mexico Research Site México
Mexico Research Site Mexico City
Mexico Research Site Tuxtla Gutierrez
Philippines Research Site Bacolod
Philippines Research Site Cebu City
Philippines Research Site Manila
Philippines Research Site Muntinlupa City
Philippines Research Site Quezon City
Philippines Research Site San Juan
Poland Research Site Bialystok
Poland Research Site Bydgoszcz
Poland Research Site Gdansk
Poland Research Site Gdynia
Poland Research Site Konin
Poland Research Site Kraków
Poland Research Site Kraków
Poland Research Site Legnica
Poland Research Site Lódz
Poland Research Site Lublin
Poland Research Site Przemysl
Poland Research Site Warszawa
Poland Research Site Wroclaw
Singapore Research Site Singapore
Singapore Research Site Singapore
Singapore Research Site Singapore
South Africa Research Site Cape Town
South Africa Research Site Johannesburg
South Africa Research Site Johannesburg
South Africa Research Site Johannesburg
South Africa Research Site Pretoria
Spain Research Site Barcelona
Spain Research Site Barcelona
Spain Research Site Granada
Spain Research Site Hospitalet deLlobregat
Spain Research Site Madrid
Spain Research Site Madrid
Spain Research Site Pamplona
Spain Research Site Santander
Taiwan Research Site Hsinchu
Taiwan Research Site Kaohsiung
Taiwan Research Site Taichung
Taiwan Research Site Tainan
Taiwan Research Site Taipei
Taiwan Research Site Taipei
Taiwan Research Site Taipei
Taiwan Research Site Taoyuan
Thailand Research Site Bangkok
Thailand Research Site Bangkok
Thailand Research Site Bangkok
Thailand Research Site Chiang Mai
Thailand Research Site Dusit
Thailand Research Site Khon Kaen
Thailand Research Site Songkhla
Turkey Research Site Ankara
Turkey Research Site Ankara
Turkey Research Site Besevler Ankara
Turkey Research Site Izmir
Turkey Research Site Küçükçekmece
Turkey Research Site Samsun
United Kingdom Research Site Cardiff
United Kingdom Research Site Chelsea
United Kingdom Research Site Leicester
United Kingdom Research Site Liverpool
United Kingdom Research Site London
United Kingdom Research Site London
United Kingdom Research Site Oxford
United Kingdom Research Site Surrey
United Kingdom Research Site Sutton
United States Research Site Albany New York
United States Research Site Albuquerque New Mexico
United States Research Site Atlanta Georgia
United States Research Site Aurora Colorado
United States Research Site Baltimore Maryland
United States Research Site Baton Rouge Louisiana
United States Research Site Baton Rouge Louisiana
United States Research Site Boston Massachusetts
United States Research Site Charlottesville Virginia
United States Research Site Chicago Illinois
United States Research Site Cincinnati Ohio
United States Research Site Cincinnati Ohio
United States Research Site Columbia Maryland
United States Research Site Dallas Texas
United States Research Site Dallas Texas
United States Research Site Dallas Texas
United States Research Site Daphne Alabama
United States Research Site Decatur Illinois
United States Research Site Des Moines Iowa
United States Research Site Detroit Michigan
United States Research Site Duarte California
United States Research Site El Paso Texas
United States Research Site Elmhurst Illinois
United States Research Site Flower Mound Texas
United States Research Site Fort Worth Texas
United States Research Site Glendale California
United States Research Site Grand Rapids Michigan
United States Research Site Hattiesburg Mississippi
United States Research Site Honolulu Hawaii
United States Research Site Houston Texas
United States Research Site Houston Texas
United States Research Site Jacksonville Florida
United States Research Site Kingwood Texas
United States Research Site Lexington Kentucky
United States Research Site Louisville Kentucky
United States Research Site Louisville Kentucky
United States Research Site Louisville Kentucky
United States Research Site Madison Wisconsin
United States Research Site McKinney Texas
United States Research Site Miami Florida
United States Research Site Midlothian Virginia
United States Research Site Naperville Illinois
United States Research Site Nashville Tennessee
United States Research Site New Albany Indiana
United States Research Site New Haven Connecticut
United States Research Site New York New York
United States Research Site Norfolk Virginia
United States Research Site Palm Bay Florida
United States Research Site Plantation Florida
United States Research Site Providence Rhode Island
United States Research Site Roanoke Virginia
United States Research Site Sacramento California
United States Research Site Saint Louis Missouri
United States Research Site Saint Paul Minnesota
United States Research Site Santa Rosa California
United States Research Site Springdale Arkansas
United States Research Site Stony Brook New York
United States Research Site Sugar Land Texas
United States Research Site Tacoma Washington
United States Research Site Worcester Massachusetts
United States Research Site York Pennsylvania
Vietnam Research Site Hanoi
Vietnam Research Site Ho Chi Minh City
Vietnam Research Site Vinh

Sponsors (2)

Lead Sponsor Collaborator
AstraZeneca Daiichi Sankyo

Countries where clinical trial is conducted

United States,  Vietnam,  Argentina,  Australia,  Brazil,  Canada,  China,  France,  Germany,  India,  Italy,  Japan,  Korea, Republic of,  Mexico,  Philippines,  Poland,  Singapore,  South Africa,  Spain,  Taiwan,  Thailand,  Turkey,  United Kingdom, 

Outcome

Type Measure Description Time frame Safety issue
Primary Progression Free Survival (PFS) PFS is defined as time from randomisation until progression per RECIST 1.1 as assessed by BICR, or death due to any cause. The comparison will include all randomised participants, as randomised, regardless of whether the participant withdraws from randomised therapy, receives another anticancer therapy or clinically progresses prior to RECIST 1.1 progression.
However, if the participant progresses or dies immediately after 2 or more consecutive missed visits, the participant will be censored at the time of the latest evaluable assessment prior to the 2 missed visits.
The measure of interest is the HR of PFS.
From randomisation until progression per RECIST 1.1 as assessed by BICR, or death due to any cause (anticipated to be up to 33 months).
Secondary Overall Survival (OS) OS is defined as the time from randomisation until the date of death due to any cause. From randomisation until the date of death due to any cause (anticipated to be up to 64 months).
Secondary Objective Response Rate (ORR) ORR is defined as the proportion of participants who have a CR or PR, as determined by the BICR/investigator assessment, per RECIST 1.1. From randomisation up until progression (anticipated to be up to 33 months).
Secondary Duration of Response (DoR) DoR is defined as the time from the date of first documented response until date of documented progression per RECIST 1.1, as assessed by BICR/investigator assessment or death due to any cause. From the date of first documented response until date of documented progression per RECIST 1.1, as assessed by BICR/investigator assessment or death due to any cause (anticipated to be up to 33 months).
Secondary Progression-Free Survival (PFS) by Investigator assessment PFS is defined as time from randomisation until progression per RECIST 1.1 as assessed by investigator, or death due to any cause. From randomisation until progression per RECIST 1.1 as assessed by the investigator, or death due to any cause (anticipated to be up to 33 months).
Secondary Clinical Benefit Rate (CBR) at 24 weeks CBR at 24 weeks is defined as the percentage of participants who have a CR or PR or who have SD, per RECIST 1.1, as assessed by BICR/per investigator assessment and derived from the raw tumour data for at least 23 weeks after randomisation. From randomisation up until progression, or the last evaluable assessment in the absence of progression (anticipated to be up to 33 months).
Secondary Time to deterioration (TTD) in breast and arm symptoms in participants treated with Dato-DXd + durvalumab compared with ICC + pembrolizumab TTD in breast symptoms and arm symptoms as measured by the arm symptoms scale from EORTC IL116 TTD is defined as time from the date of randomisation to the date of deterioration.
Deterioration is defined as change from baseline that reaches a clinically meaningful deterioration threshold.
From the date of randomisation to the date of deterioration (from randomization to 18 weeks post-progression).
Secondary Time to deterioration (TTD) in pain in participants treated with Dato-DXd + durvalumab compared with ICC + pembrolizumab TTD in pain as measured by the EORTC IL199. Time from the date of randomisation to the date of deterioration (from randomization to 18 weeks post-progression).
Secondary Time to deterioration (TTD) in physical functioning in participants treated with Dato-DXd + durvalumab compared with ICC + pembrolizumab TTD in physical function as measured by the PROMIS Short Form v2.0 - Physical Function 8c. From the date of randomisation to the date of deterioration (from randomization to 18 weeks post-progression).
Secondary Time to deterioration (TTD) in GHS/QoL in participants treated with Dato-DXd + durvalumab compared with ICC + pembrolizumab TTD in GHS/QoL as measured by the GHS/QoL scale from EORTC IL172. From the date of randomisation to the date of deterioration (from randomization to 18 weeks post-progression).
Secondary Time to First Subsequent Therapy (TFST) TFST is defined as the time from randomisation until the start date of the first subsequent anticancer therapy after discontinuation of randomised treatment, or death due to any cause. From randomisation until the start date of the first subsequent anticancer therapy after discontinuation of randomised treatment, or death due to any cause (anticipated to be up to 64 months).
Secondary Time to Second Subsequent Therapy (TSST) TSST is defined as the time from randomisation until the start date of the second subsequent anticancer therapy after discontinuation of first subsequent treatment, or death due to any cause. From randomisation until the start date of the second subsequent anti cancer therapy after discontinuation of first subsequent treatment, or death due to any cause (anticipated to be up to 64 months).
Secondary Progression Free Survival 2 (PFS2) PFS2 will be defined as the time from the randomisation to the earliest progression event (following the initial progression), subsequent to first subsequent therapy, or death. The date of second progression will be recorded by the investigator in the eCRF and defined according to local standard clinical practice based on radiological or clinical progression. From the randomisation to the earliest of the progression event (following the initial progression), subsequent to first subsequent therapy, or death (anticipated to be up to 64 months).
Secondary Pharmacokinetics of Dato-DXd in combination with durvalumab Concentration of Dato-DXd, total anti-TROP2 antibody, and DXd (payload) in plasma. From first dose to end of treatment (anticipated to be up to 33 months).
Secondary Immunogenicity of Dato-DXd in combination with durvalumab Presence of antidrug antibodies for Dato-DXd (confirmatory results: positive or negative, titres). From first dose to end of treatment safety follow-up (anticipated to be up to 33 months).
Secondary Safety and tolerability of Dato-DXd + durvalumab as compared with ICC + pembrolizumab Safety and tolerability will be evaluated in the safety population in terms of AEs. From first dose to end of treatment safety follow-up (anticipated to be up to 33 months).
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