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Clinical Trial Details — Status: Suspended

Administrative data

NCT number NCT04675827
Other study ID # IJB-EBC-Decrescendo-2020
Secondary ID
Status Suspended
Phase Phase 2
First received
Last updated
Start date January 17, 2022
Est. completion date March 2029

Study information

Verified date February 2023
Source Jules Bordet Institute
Contact n/a
Is FDA regulated No
Health authority
Study type Interventional

Clinical Trial Summary

DECRESCENDO is a multicentre, open-label, dual-phase single-arm phase II de-escalation study evaluating neoadjuvant treatment with 12 administrations of weekly IV paclitaxel 80 mg/m2 (or IV docetaxel 75 mg/m2 every 3 weeks for 4 cycles) combined with subcutaneous (SC) fixed dose combination (FDC) of pertuzumab and trastuzumab (loading dose of 1200 mg pertuzumab and 600 mg trastuzumab, followed by 600 mg pertuzumab and 600 mg trastuzumab) every 3 weeks for 4 cycles. Surgery will be performed according to local guidelines in all subjects after neoadjuvant treatment. After surgery, subjects who achieve a pCR (defined as pT0/Tis pN0) will receive adjuvant pertuzumab and trastuzumab FDC SC for additional 14 cycles. Subjects with residual invasive disease will receive salvage adjuvant trastuzumab emtansine (T-DM1, 3.6 mg/kg, IV every 3 weeks) for 14 cycles. In subjects whose residual invasive disease is classified per RCB score as ≥2, 3 to 4 cycles of anthracycline-based chemotherapy may be administered, at the investigator's discretion, before the 14 cycles of T-DM1. If histopathological analysis finds that the surgical specimen from a subject with residual disease is ER-positive and/or PR-positive, adjuvant endocrine therapy may be administered concomitantly with study treatment, at the investigator's discretion and according to local guidelines. Adjuvant radiotherapy will be mandatory after breast-conserving surgery, whereas it will be performed according to local guidelines after mastectomy, and it will be administered concomitantly with pertuzumab and trastuzumab FDC SC in subjects who achieve a pCR, and concomitantly with T-DM1 in subjects with residual invasive disease (after anthracycline-based chemotherapy in subjects assigned to receive this treatment).


Description:

DECRESCENDO is a multicentre, open-label, dual-phase single-arm phase II de-escalation study evaluating neoadjuvant treatment with 12 administrations of weekly intravenous (IV) paclitaxel 80 mg/m2 (or IV docetaxel 75 mg/m2 every 3 weeks for 4 cycles) combined with subcutaneous (SC) fixed dose combination (FDC) of pertuzumab and trastuzumab (loading dose of 1200 mg pertuzumab and 600 mg trastuzumab, followed by 600 mg pertuzumab and 600 mg trastuzumab) every 3 weeks for 4 cycles. Surgery will be performed according to local guidelines in all subjects after neoadjuvant treatment. After surgery, subjects who achieve a pathologic complete response (pCR, defined as pT0/Tis pN0) will receive adjuvant pertuzumab and trastuzumab FDC SC for additional 14 cycles. Subjects with residual invasive disease will receive salvage adjuvant trastuzumab emtansine (T-DM1, 3.6 mg/kg, IV every 3 weeks) for 14 cycles. In subjects whose residual invasive disease is classified per Residual Cancer Burden (RCB) score as ≥2, 3 to 4 cycles of anthracycline-based chemotherapy may be administered, at the investigator's discretion, before the 14 cycles of T-DM1. If histopathological analysis finds that the surgical specimen from a subject with residual disease is ER-positive and/or PR-positive, adjuvant endocrine therapy may be administered concomitantly with study treatment, at the investigator's discretion and according to local guidelines. Adjuvant radiotherapy will be mandatory after breast-conserving surgery, whereas it will be performed according to local guidelines after mastectomy, and it will be administered concomitantly with pertuzumab and trastuzumab FDC SC in subjects who achieve a pCR, and concomitantly with T-DM1 in subjects with residual invasive disease (after anthracycline-based chemotherapy in subjects assigned to receive this treatment). Patients' tumour intrinsic subtype will be determined based on analysis of the PAM50 gene signature. The PAM50 gene signature, which measures the expression of 50 genes to classify tumours into 1 of 4 intrinsic subtypes (luminal A, luminal B, HER2-enriched, and basal-like), will be assessed in formalin-fixed paraffin embedded (FFPE) samples obtained at baseline. While a tumour biopsy sample must be available prior to enrolment, the PAM50 results will be generated centrally post enrolment and subsequently used to assess the primary endpoint of the study, which is the 3-year recurrence-free survival (RFS) rate in the subpopulation of subjects with HER2-enriched tumours who achieve a pCR after the neoadjuvant phase of the study. Sub-study: The flexible care sub-study is an open-label, randomised phase II study to be conducted in selected sites from some of the countries that participate in DECRESCENDO. After completion of neoadjuvant treatment and surgery in the main study, 121 of the subjects who achieved a pCR and thus are assigned to continue treatment with pertuzumab and trastuzumab FDC SC will be randomised at a 1:1 ratio to receive 3 cycles of pertuzumab and trastuzumab FDC SC every 3 weeks in the hospital, followed by 3 cycles in another setting outside the hospital, or to the same treatment starting with 3 cycles outside the hospital followed by 3 cycles in the hospital (treatment cross-over period). After the first 6 cycles of adjuvant treatment, subjects will be asked to choose between continuing treatment (for the remaining 8 cycles, for a total of 14 cycles) within or outside the hospital, according to their preference (treatment continuation period). Subjects can request to change from outside the hospital to in the hospital administration (and vice-versa) at any moment during the treatment continuation period, but not in the treatment cross-over period.


Recruitment information / eligibility

Status Suspended
Enrollment 1065
Est. completion date March 2029
Est. primary completion date June 2027
Accepts healthy volunteers No
Gender All
Age group 18 Years and older
Eligibility Inclusion Criteria: 1. Male or female. 2. Age =18 years old. 3. Eastern Cooperative Oncology Group (ECOG) performance status =1. 4. Subjects whose tumour measures =15 mm and =50 mm, according to clinical staging performed with imaging exams (either mammography, ultrasound or breast magnetic resonance imaging [MRI]). 5. Must have histologically confirmed diagnosis of HER2-positive and ER-negative/PR-negative breast cancer (analysis performed by the local laboratory). 1. HER2-positive defined as a score of 3+ in IHC or a positive ISH (ratio of HER2 copy number/chromosome 17 =2 or average HER2 copy number =6 signals per cell). 2. ER-negative/PR-negative defined as estrogen receptor and progesterone receptor nuclear staining <1% by IHC. Note: patients with micro-invasive carcinoma or ductal carcinoma in situ (DCIS) without invasive disease are not eligible. 6. Subjects with multifocal or multicentric invasive disease are eligible as long as all the biopsiable lesions can be characterised and are confirmed to be HER2-positive and ER and PR negative. Note: In the case of multifocal or multicentric disease, only the biopsy from the largest lesion should be provided. 7. Node-negative disease (N0): no axillary lymph nodes identifiable at ultrasound, or in case of suspect axillary lymph nodes are identified, fine-needle aspiration or core biopsy must be carried out to confirm that axillary status is negative. Axillary micrometastases (i.e., if the greatest diameter of the nodal metastasis in a sentinel node is 0.2 mm or less) are not allowed. 8. Serum pregnancy test (for women of childbearing potential) negative within 7 days prior to treatment start. 9. Women of childbearing potential must agree to use 1 highly effective non-hormonal contraceptive method with a failure rate of less than 1% per year from the signing of the ICF until at least 7 months after last dose of study drugs; or they must totally abstain from any form of sexual intercourse. Men with a partner of childbearing potential must agree to use condom in combination with a spermicidal foam, gel, film, cream, or suppository, and agreement to refrain from donating sperm, during the course of this study and for at least 7 months after the last administration of study treatment. 10. Adequate bone marrow and coagulation functions as defined below: - Absolute neutrophil count =1500 /µL or 1.5x109/L - Haemoglobin =9 g/dL (blood transfusions to reach these levels of haemoglobin are allowed) - Platelets =100,000/µL or 100x109/L - International normalized ratio (INR) and activated partial thromboplastin time (aPTT) = 1.5 ×ULN 11. Adequate liver function as defined below: - Serum total bilirubin =1.5 x ULN. In case of known Gilbert's syndrome =3xUNL is allowed - AST (SGOT) and ALT (SGPT) =2.5 x ULN - Alkaline phosphatase =2.5 x ULN 12. Adequate renal function as defined below: • Creatinine =1.5 x UNL or creatinine clearance >60 mL/min/1.73 m2 13. Completion of all necessary screening procedures within 28 days prior to enrolment. 14. Adequate cardiac function, defined as a left ventricular ejection fraction =55% estimated by echocardiogram (ECHO) or multiple-gated acquisition scintigraphy (MUGA). 15. Availability of a pre-treatment tumour biopsy sample as specified below: - At least one FFPE tumour block must be available for central evaluation. Whenever possible, two FFPE tumour blocks should be available (preferred). - If a block cannot be provided, 25 unstained FFPE slides of 4 µm thickness from the pre-treatment tumour biopsy must be provided as an alternative. These slides must be freshly cut prior the shipment to the sponsor. - In either case, the local pathologist must evaluate an H&E stained slide to ensure that the tumour surface is at least 4 mm² and that tumour cellularity is =10%. Note 1: Tumour biopsy must be sent to the central research laboratory as soon as the patient is confirmed by the local investigator to be eligible for the study. Note 2: the inclusion of the subject is only based on local assessments. A central review of HER2, ER, and PR status will be performed at posteriori for quality control purposes. 16. Signed Informed Consent form (ICF) obtained prior to any study related procedure. 17. Subject is willing and able to comply with the protocol for the duration of the study including treatment and scheduled visits and examinations. Inclusion criterion applicable to FRANCE only: 18. Affiliated to the French Social Security System. Exclusion Criteria: 1. Pregnant and/or lactating women. 2. Bilateral invasive breast cancer. 3. Evidence of metastatic breast cancer: all subjects must have had a CT/MRI scan of the thorax/abdomen/pelvis to rule out metastatic breast cancer prior to enrolment. FDG/PET-CT can be used as an alternative to replace all the exams above. A screening bone scan must have been done if ALP and/or corrected calcium levels were above the institutional upper limits at screening (if PET/CT was used as an alternative imaging exam, a bone scan and/or CT/MRI is not required). 4. Subject with a significant medical, neuro-psychiatric, or surgical condition, currently uncontrolled by treatment, which, in the investigator's opinion, may interfere with completion of the study. 5. Previous exposure to any anti-HER2 treatment. 6. Concomitant exposure to any investigational products as part of a clinical trial within 30 days prior to enrolment. 7. Subject with second primary malignancies diagnosed = 5 years before enrolment in the study. Exceptions are: adequately treated non-melanoma skin cancer, in situ cancer of the cervix, ductal carcinoma in situ of the breast, and any other solid or haematological tumour diagnosed > 5 years before enrolment and for which no chemotherapy and no systemic treatment were necessary, with no evidence of disease recurrence. 8. Resting electrocardiogram (ECG) with QTc >470 msec detected on at 2 or more time points within a 24-hour period, or family history of long QT syndrome. 9. Serious cardiac illness or medical conditions including, but not confined to, the following: - History of NCI CTCAE (v4) Grade = 3 symptomatic congestive heart failure (CHF) or New York Heart Association (NYHA) Class = II - High-risk uncontrolled arrhythmias (i.e., atrial tachycardia with a heart rate = or > 100/min at rest, significant ventricular arrhythmia [ventricular tachycardia], or higher-grade atrioventricular [AV]-block, such as second degree AV-block Type 2 [Mobitz 2] or third-degree AV-block) - Serious cardiac arrhythmia not controlled by adequate medication, severe conduction abnormality - Angina pectoris requiring anti-anginal medication - Clinically significant valvular heart disease - Evidence of transmural infarction on ECG - Evidence of myocardial infarction within 12 months prior to randomization - Poorly controlled hypertension (i.e., systolic > 180 mm Hg or diastolic > 100 mmHg) 10. History of ventricular dysrhythmias or risk factors for ventricular dysrhythmias, such as structural heart disease (e.g., severe LVSD, left ventricular hypertrophy), coronary heart disease (symptomatic or with ischemia demonstrated by diagnostic testing), clinically significant electrolyte abnormalities (e.g., hypokalemia, hypomagnesemia, hypocalcemia), or family history of sudden unexplained death or long QT syndrome. 11. Peripheral neuropathy (CTCAE version 5) grade =2. 12. Major surgery within 14 days prior to enrolment. 13. Subject with HIV, Hepatitis B or Hepatitis C infection documented by serology, except for those subjects with a previous exposure to Hepatitis B who developed an effective immune response (HBSAg-negative and anti-HBS-positive). 14. Previous allogeneic bone marrow transplant. 15. Known prior severe hypersensitivity to investigational product or any component in its formulations, including known severe hypersensitivity reactions to monoclonal antibodies (CTCAE grade =3). 16. Subjects who received live attenuated vaccines within 14 days before enrolment. Exclusion criterion applicable to FRANCE only: 17. Vulnerable persons according to the article L.1121-6 of the CSP, adults who are the subject of a measure of legal protection or unable to express their consent according to article L.1121-8 of the CSP.

Study Design


Intervention

Drug:
Pertuzumab and tratuzumab fixed dose combination
Treatment administration: adjuvant pertuzumab and trastuzumab fixed dose combination SC for 14 cycles
Trastuzumab emtansine
Treatment administration: adjuvant T-DM1 for 14 cycles.

Locations

Country Name City State
Australia Icon Cancer Centre Wesley Auchenflower
Australia Ballarat Health Services Ballarat
Australia Bendigo Hospital Bendigo
Australia Sunshine Coast University Hospital Birtinya
Australia Box Hill Hospital Box Hill
Australia Chris O'Brien Lifehouse Camperdown
Australia Monash Medical Centre (Clayton) Clayton
Australia Coffs Harbour Health Campus Coffs Harbour
Australia Concord Repatriation General Hospital Concord
Australia Townsville University Hospital Douglas
Australia Lake Macquarie Private Hospital Gateshead
Australia Gosford Hospital Gosford
Australia Royal Brisbane and Women's Hospital Herston
Australia Icon Cancer Centre Hobart Hobart
Australia Liverpool Hospital Liverpool
Australia Peter MacCallum Cancer Centre Melbourne
Australia Sir Charles Gairdner Hospital Nedlands
Australia Macquarie University North Ryde
Australia Mater Hospital North Sydney
Australia Sunshine Hospital Saint Albans
Australia Calvary Mater Newcastle Waratah
Australia Westmead Hospital Westmead
Australia Princess Alexandra Hospital Woolloongabba
Belgium OLV ziekenhuis Aalst
Belgium GZA Ziekenhuisen Campus Sint-Augustinus - Iridium Kankernetwerk Antwerp Wilrijk
Belgium Ziekenhuisnetwerk Jan Palfijn Antwerp
Belgium AZ Klina VZW Brasschaat
Belgium Cliniques Universtaires Saint-Luc Brussels
Belgium Institut Jules Bordet Bruxelles
Belgium Grand Hôpital de Charleroi Charleroi
Belgium Centre Hospitalier Chretien MontLegia Liège
Belgium Heilig Hartziekenhuis Lier
Belgium CHU UCL Namur Sainte-Elisabeth Namur
France Institut de Cancérologie de l'Ouest - Angers Angers
France Institut Sainte Catherine Avignon
France Centre Hospitalier de la Côte Basque Bayonne
France CHRU Jean Minjoz Besançon
France Institut Bergonié Bordeaux
France Polyclinique Bordeaux Nord Aquitaine Bordeaux
France CHU Morvan Brest
France Centre François Baclesse Caen
France Centre Jean Perrin Clermont-Ferrand
France Centre Georges François Leclerc Dijon
France Hopital Michallon Grenoble
France Centre Oscar Lambret Lille
France CHU de Limoges Limoges
France GHBS Lorient Lorient
France Centre Léon Bérard Lyon
France Institut Paoli Calmettes Marseille
France CH Annecy Genevois Metz-Tessy
France Centre de Cancerologie du Grand Montpellier Montpellier
France Hopital privé du Confluent Nantes
France Groupe Hospitalier Diaconesses Croix Saint-Simon Paris
France Hopital Tenon Paris
France Institut Curie - Paris Paris
France CH Perpignan Perpignan
France Hopital Lyon Sud Pierre-Bénite
France CHU Poitiers Poitiers
France Institut Godinot Reims
France Centre Henri Becquerel Rouen
France Institut Curie - Saint-Cloud Saint-Cloud
France Clinique Saint Anne Strasbourg
France Institut Claudius Regaud Toulouse
France Institut Gustave Roussy Villejuif
Israel Sheba Medical Center Ramat Gan
Korea, Republic of Soon Chun Hyang University Cheonan Hospital Cheonan
Korea, Republic of Keimyung University Dongsan Hospital Daegu
Korea, Republic of National Cancer Center Goyang-si
Korea, Republic of Gachon University Gil Medical Center Incheon
Korea, Republic of Inha University Hospital Incheon
Korea, Republic of Seoul National University Bundang Hospital Seongnam
Korea, Republic of CHA bundang Medical Center Seongnam-si
Korea, Republic of Asan Medical Center Seoul
Korea, Republic of Ewha Womans University Mokdong Hospital Seoul
Korea, Republic of Korea university anam hospital Seoul
Korea, Republic of Samsung Medical Center Seoul
Korea, Republic of Seoul National University Hospital Seoul
Korea, Republic of Seoul ST. Mary's Hospital Seoul
Korea, Republic of Severance Hospital Seoul
Korea, Republic of Ajou University Hospital Suwon si
Korea, Republic of Ulsan University Hospital Ulsan
Switzerland Hirslanden Klinik - Tumor Zentrum Aarau
Switzerland Kantonsspital Baden Baden
Switzerland Universitatsspital Basel Basel
Switzerland Kantonsspital Frauenfeld/Frauenklinik Frauenfeld
Switzerland Hopital Daler - Centre du Sein Fribourg
Switzerland Kantonsspital Winterthur Winterthur

Sponsors (5)

Lead Sponsor Collaborator
Jules Bordet Institute Breast International Group, Hoffmann-La Roche, Institut Curie, International Drug Development Institute

Countries where clinical trial is conducted

Australia,  Belgium,  France,  Israel,  Korea, Republic of,  Switzerland, 

Outcome

Type Measure Description Time frame Safety issue
Primary 3-year RFS in HER2-enriched subjects who achieve a pCR 3-year RFS, defined as the time from enrolment until the first occurrence of one of the following events: invasive ipsilateral breast tumour recurrence, local/regional invasive recurrence, distant recurrence, death from breast cancer, death attributable to any cause other than breast cancer, death from unknown cause; in subjects with HER2-enriched, ER-negative/PR-negative, clinically node-negative breast cancers who achieve a pCR after neoadjuvant treatment. 3 years
Secondary 3-year RFS in all subjects who achieve a pCR. 3-year RFS in all subjects who achieve a pCR. 3 years
Secondary 5-year RFS in all subjects who achieve a pCR. 5-year RFS in all subjects who achieve a pCR. 5 years
Secondary pCR (in the overall population) To assess pCR rates in the overall population and by primary tumour dimension. pCR (in the overall population) is defined as the absence of residual invasive tumour in the breast and axillary lymph nodes (pT0/Tis pN0) at surgery as per the local anatomo-pathological report. during procedure
Secondary 3-year RFS (survival rates) In all population, the sub-group analysis according to the pathological response (pCR versus residual disease) and stratified by tumour size (T1 versus T2) for following outcomes:
Survival rates: - 3-year RFS The RFS is defined as the time from enrolment until the first occurrence of one of the following events: invasive ipsilateral breast tumour recurrence, local/regional invasive recurrence, distant recurrence, death from breast cancer, death attributable to any cause other than breast cancer, death from unknown cause
3 years
Secondary 3-year invasive disease-free survival (iDFS) (survival rates) In all population, the sub-group analysis according to the pathological response (pCR versus residual disease) and stratified by tumour size (T1 versus T2) for following outcomes:
Survival rates: - 3-year invasive disease-free survival (iDFS) The iDFS is defined as the time from enrolment until the first occurrence of one of the following events: invasive ipsilateral breast tumour recurrence, local/regional invasive recurrence, distant recurrence, death from breast cancer, death attributable to any cause other than breast cancer, death from unknown cause, invasive contralateral breast cancer, second primary invasive cancer (non-breast)
3 years
Secondary 3-year distant disease-free survival (dDFS) (survival rates) In all population, the sub-group analysis according to the pathological response (pCR versus residual disease) and stratified by tumour size (T1 versus T2) for following outcomes:
urvival rates: - 3-year distant disease-free survival (dDFS) The dDFS defined as the time from enrolment until the first occurrence of one of the following events: distant recurrence; death from breast cancer; death from non-breast cancer cause; death from unknown cause; second primary invasive cancer (non-breast);
3 years
Secondary 3-year overall survival (OS) (survival rates) In all population, the sub-group analysis according to the pathological response (pCR versus residual disease) and stratified by tumour size (T1 versus T2) for following outcomes:
Survival rates: - 3-year overall survival (OS) The OS defined as the time from enrolment until the first occurrence of one of the following events: death from breast cancer, death from non-breast cancer cause, death from unknown cause
3 years
Secondary Recurrence-free interval (RFI) (Time) In all population, the sub-group analysis according to the pathological response (pCR versus residual disease) and stratified by tumour size (T1 versus T2) for following outcomes:
Time: Recurrence-free interval (RFI) The RFI is defined as the time interval between enrolment and the occurrence of one of the following events: invasive ipsilateral breast tumour recurrence, local/regional invasive recurrence, distant recurrence; death from breast cancer
3 years
Secondary 5-year RFS (survival rates) In all population, the sub-group analysis according to the pathological response (pCR versus residual disease) and stratified by tumour size (T1 versus T2) for following outcomes:
Survival rates: - 5-year RFS The RFS is defined as the time from enrolment until the first occurrence of one of the following events: invasive ipsilateral breast tumour recurrence, local/regional invasive recurrence, distant recurrence, death from breast cancer, death attributable to any cause other than breast cancer, death from unknown cause
5 years
Secondary 5-year invasive disease-free survival (iDFS) (survival rates) In all population, the sub-group analysis according to the pathological response (pCR versus residual disease) and stratified by tumour size (T1 versus T2) for following outcomes:
Survival rates: - 5-year invasive disease-free survival (iDFS) The iDFS is defined as the time from enrolment until the first occurrence of one of the following events: invasive ipsilateral breast tumour recurrence, local/regional invasive recurrence, distant recurrence, death from breast cancer, death attributable to any cause other than breast cancer, death from unknown cause, invasive contralateral breast cancer, second primary invasive cancer (non-breast)
5 years
Secondary 5-year distant disease-free survival (dDFS) (survival rates) In all population, the sub-group analysis according to the pathological response (pCR versus residual disease) and stratified by tumour size (T1 versus T2) for following outcomes:
Survival rates: - 5-year distant disease-free survival (dDFS) The dDFS defined as the time from enrolment until the first occurrence of one of the following events: distant recurrence; death from breast cancer; death from non-breast cancer cause; death from unknown cause; second primary invasive cancer (non-breast);
5 years
Secondary 5-year overall survival (OS)(survival rates) In all population, the sub-group analysis according to the pathological response (pCR versus residual disease) and stratified by tumour size (T1 versus T2) for following outcomes:
Survival rates: - 5-year overall survival (OS) The OS defined as the time from enrolment until the first occurrence of one of the following events: death from breast cancer, death from non-breast cancer cause, death from unknown cause
5 years
Secondary Recurrence-free interval (RFI) (time) In all population, the sub-group analysis according to the pathological response (pCR versus residual disease) and stratified by tumour size (T1 versus T2) for following outcomes:
Time: Recurrence-free interval (RFI) The RFS is defined as the time from enrolment until the first occurrence of one of the following events: invasive ipsilateral breast tumour recurrence, local/regional invasive recurrence, distant recurrence, death from breast cancer, death attributable to any cause other than breast cancer, death from unknown cause
5 years
Secondary Number of participants experiencing an Adverse Event An adverse event (AE) is any untoward medical occurrence in a subject or clinical investigation subject receiving/undergoing the study treatments (paclitaxel (or docetaxel), pertuzumab and trastuzumab FDC SC, T-DM1, surgery, radiotherapy) and which does not necessarily have a causal relationship with these study treatments. The number of participants who experience an AE (including 1 month of safety follow up) will be presented. The intensity of all AEs will be graded according to the CTCAE version 5 on a five-point scale (Grade 1 to 5). study treatment plus follow-up of 30 days ( Time Frame: Up to approximately 17 months )
Secondary Number of participants experiencing an Serious Adverse Event A serious adverse event (SAE) is any untoward medical occurrence that results in any of the following outcomes: Death; Life-threatening; Subject hospitalisation or prolongation of existing hospitalisation; Persistent or significant disability/incapacity; Congenital anomaly/birth defect. The number of participants who experience any SAE while receiving paclitaxel (or docetaxel), pertuzumab and trastuzumab FDC SC, T-DM1, surgery, radiotherapy (including 1 months of safety follow up) with or without the relationship to IMPs will be presented. During survival follow-up, only SAE related to IMPs will be presented. through study completion estimated 60 months
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