ATEMPT 2.0: Adjuvant T-DM1 vs TH

• ClinicalTrials.gov Identifier: NCT04893109
• Recruitment Status: Recruiting
• First Posted: May 19, 2021
• Last Update Posted: April 25, 2024
• Sponsor: Dana-Farber Cancer Institute
• Collaborator: Genentech, Inc.
• Information provided by (Responsible Party): Sara Tolaney, MD, Dana-Farber Cancer Institute

Study Description

Brief Summary:

This research study is studying how well newly diagnosed breast cancer that has tested positive for a protein called HER2 responds using one of two different combination of HER2-directed therapies as a treatment after surgery.

The name of the study drugs involved are:

• Trastuzumab-emtansine (T-DM1, Kadcyla)
• Trastuzumab SC (Herceptin Hylecta)
• Paclitaxel

Condition or disease	Intervention/treatment	Phase
Breast Cancer; HER2-positive Breast Cancer	Drug: trastuzumab-emtansine; Drug: Trastuzumab SC; Drug: Paclitaxel	Phase 2

Detailed Description:

This is a randomized phase II adjuvant study for women and men with Stage I HER2-positive invasive breast cancer. Participants will be randomized into one of two treatment arms in this study and receive:

• Arm 1: trastuzumab-emtansine (T-DM1, Kadcyla) and trastuzumab SC (Herceptin Hylecta)
• Arm 2: paclitaxel and trastuzumab SC (Herceptin Hylecta) This research study is looking to see if the study drug T-DM1 followed by trastuzumab SC will have less side-effects than traditional HER2-positive breast cancer treatment of trastuzumab and paclitaxel.The study is also looking to learn about the long-term benefits and disease-free survival of participants who are treated with T-DM1 followed by trastuzumab SC.

T-DM1 is an antibody-drug conjugate; it is made up of an antibody (trastuzumab) linked to a cytotoxic drug, DM1 (chemotherapy). T-DM1 functions as a targeted cancer therapy because it targets HER2-positive breast cancer cells directly, limiting exposure of the rest of the body to chemotherapy. More specifically, the trastuzumab in T-DM1 first binds to the HER2 protein on the surface of the breast cancer cells and the DM1 then enters the cells and can cause them to die, preventing tumor growth. The FDA (the U.S. Food and Drug Administration) has not approved T-DM1 for use on its own in patients with stage I, II, or III breast cancer. However, it has been approved for use in (a) advanced or metastatic, previously treated breast cancer and (b) in some patients receiving postoperative treatment after preoperative chemotherapy and surgery have been completed.

Trastuzumab SC is a subcutaneous form of trastuzumab.Trastuzumab is a monoclonal antibody, which are disease-fighting proteins made by cloned immune cells. Paclitaxel and trastuzumab are considered a standard-of-care regimen in early breast cancer. Trastuzumab is FDA-approved to be administered as an IV (intravenous) or subcutaneous (muscular injection).

The research study procedures include screening for eligibility and study treatment including laboratory evaluations and follow up visits.

Participants will receive study treatment for a year in total and will be followed for 5 years after treatment.

It is expected that about 500 people will take part in this research study.

Genentech is supporting this research study by providing funding for the study and supplying trastuzumab-emtansine (T-DM1) and trastuzumab SC (subcutaneous).

Study Design

• Study Type: Interventional (Clinical Trial)
• Estimated Enrollment: 500 participants
• Allocation: Randomized
• Intervention Model: Parallel Assignment
• Intervention Model Description: participants are randomized in a 2-1 fashion to Arm A vs. Arm B
• Masking: None (Open Label)
• Primary Purpose: Treatment
• Official Title: A Randomized Phase II Trial of Adjuvant Trastuzumab Emtansine (T-DM1) Followed by Subcutaneous Trastuzumab Versus Paclitaxel in Combination With Subcutaneous Trastuzumab for Stage I HER2-positive Breast Cancer (ATEMPT 2.0)
• Actual Study Start Date: June 16, 2021
• Estimated Primary Completion Date: May 1, 2025
• Estimated Study Completion Date: May 1, 2028

Arms and Interventions

Arm	Intervention/treatment
Experimental: Arm A. T-DM1 followed by Trastuzumab SC; Randomized participants will receive intravenous T-DM1 every 3 weeks for 6 cycles (18 weeks) and then Trastuzumab SC (subcutaneous) every 3 weeks for 11 cycles	Drug: trastuzumab-emtansine; intravenous infusion; Other Names: T-DM1; Kadcyla; Drug: Trastuzumab SC; Muscular injection; Other Name: Herceptin Hylecta
Experimental: Arm B: Paclitaxel with Trastuzumab SC, followed by Trastuzumab SC alone; Randomized participants will receive weekly intravenous Paclitaxel for 12 weeks (4 cycles) and Trastuzumab SC (subcutaneous) every 3 weeks for 17 cycles. The first 4 doses Trastuzumab SC are given with Paclitaxel.	Drug: Trastuzumab SC; Muscular injection; Other Name: Herceptin Hylecta; Drug: Paclitaxel; intravenous infusion; Other Names: Taxol; Onxal

Outcome Measures

Primary Outcome Measures :

1. Incidence of clinically relevant toxicities (CRT) [ Time Frame: First 18 weeks of treatment ]
   Compare the incidence of clinically relevant toxicities (CRT) in patients with Stage I HER2-positive breast cancer treated with trastuzumab emtansine followed by trastuzumab SC to the incidence in those treated with paclitaxel in combination with trastuzumab SC as assessed by PRO-CTCAE
2. Disease Free Survival (DFS) [ Time Frame: Time from randomization to first Disease Free Survival (DFS) event up to 72 months ]
   Evaluate disease-free survival in the T-DM1 followed by trastuzumab SC arm

Secondary Outcome Measures :

1. Grade 3 and 4 adverse events [ Time Frame: Enrollment to end of treatment up to 1 year ]
   Compare the incidence of all grade 3 and 4 adverse events in patients treated with adjuvant trastuzumab emtansine followed by trastuzumab SC to the incidence in those receiving paclitaxel in combination with trastuzumab SC
2. Quality of Life Assessment: FACT B [ Time Frame: Enrollment to end of treatment up to 1 year ]
   Compare responses to FACT-B quality of life (QOL) questionnaire in patients receiving trastuzumab emtansine followed by trastuzumab SC to that experienced by patients receiving paclitaxel in combination with trastuzumab SC.
3. Symptoms related to therapy [ Time Frame: Enrollment to end of treatment up to 1 year ]
   Evaluate symptoms related to therapy in patients receiving trastuzumab emtansine followed by trastuzumab SC compared to those receiving paclitaxel in combination with trastuzumab SC using the Rotterdam Symptom Checklist (RSCL)
4. Symptoms related to therapy [ Time Frame: Enrollment to end of treatment up to 1 year ]
   Evaluate symptoms related to therapy in patients receiving trastuzumab emtansine followed by trastuzumab SC compared to those receiving paclitaxel in combination with trastuzumab SC using the Patient Neurotoxicity Questionnaire (PNQ)
5. Effects of therapy on work productivity [ Time Frame: Enrollment to end of treatment up to 1 year ]
   Evaluate effects of therapy on work productivity and activity using the Work Productivity and Activity Impairment Questionnaire (WPAI-SHP) in patients receiving trastuzumab emtansine followed by trastuzumab SC compared to those receiving paclitaxel in combination with trastuzumab SC
6. Effect of alopecia on patients [ Time Frame: Enrollment to end of treatment up to 1 year ]
   Evaluate the effects of alopecia on patients receiving paclitaxel in combination with trastuzumab SC using an alopecia questionnaire
7. Incidence of Side Effects [ Time Frame: Enrollment to end of treatment up to 1 year ]
   Compare incidence of sensory neuropathy, headache, arthralgia and myalgia using PRO-CTCAE criteria in patients receiving trastuzumab emtansine followed by trastuzumab SC to that experienced by patients receiving paclitaxel in combination with trastuzumab SC
8. Incidence of grade 3-4 cardiac left ventricular dysfunction [ Time Frame: Enrollment to end of treatment up to 1 year ]
   Evaluate the incidence of grade 3-4 cardiac left ventricular dysfunction in patients treated with adjuvant trastuzumab emtansine followed by trastuzumab SC compared to those receiving paclitaxel with trastuzumab SC
9. Incidence of trastuzumab-emtansine-induced grade 2-4 thrombocytopenia [ Time Frame: Enrollment to end of treatment up to 1 year ]
   Evaluate the incidence of trastuzumab-emtansine-induced grade 2-4 thrombocytopenia
10. Percentage of patients with amenorrhea [ Time Frame: Enrollment to end of treatment up to 1 year ]
    Investigate the percentage of patients with amenorrhea at various time points after the start of treatment in premenopausal women receiving treatment with trastuzumab emtansine followed by trastuzumab SC and paclitaxel with trastuzumab SC
11. Evaluation of gene predictors of trastuzumab-emtansine-induced grade 2-4 [ Time Frame: Enrollment to end of treatment up to 1 year ]
    Evaluate gene biomarkers predictive of trastuzumab-emtansine-induced grade 2-4 thrombocytopenia
12. Gene Profiling [ Time Frame: Enrollment to end of treatment up to 1 year ]
    Utilize genomic profiling to query a large panel of cancer gene mutations and gene expression in patients with Stage I HER2-positive breast cancer
13. Radiation therapy Toxicity [ Time Frame: Enrollment to end of treatment up to 1 year ]
    Evaluate the incidence of toxicities attributed to radiation therapy when given concurrently with trastuzumab SC after receipt of either trastuzumab emtansine or paclitaxel
14. Overall survival [ Time Frame: Enrollment to end of treatment up to 1 year ]
    Describe overall survival in patients with Stage I HER2-positive breast cancer treated with trastuzumab emtansine followed by trastuzumab SC

Eligibility Criteria

• Ages Eligible for Study: 18 Years and older (Adult, Older Adult)
• Sexes Eligible for Study: All
• Accepts Healthy Volunteers: No

Criteria

Inclusion Criteria:

• Patients must have HER2-positive Stage I histologically confirmed invasive carcinoma of the breast. Patients must have node-negative (N0) or micrometastases (N1mic) breast cancer according to the AJCC 8th edition anatomic staging table.

  • If the patient has had a negative sentinel node biopsy, then no further axillary dissection is required, and the patient is determined to be node-negative. If an axillary dissection without sentinel lymph node biopsy is performed to determine nodal status, at least six axillary lymph nodes must be removed and analyzed, and determined to be negative, for the patient to be considered node-negative. Axillary nodes with single cells or tumor clusters ≤ 0.2 mm by either H&E or immunohistochemistry (IHC) will be considered node-negative.
  • Any axillary lymph node with tumor clusters between 0.02 and 0.2 cm is considered a micrometastasis. Patients with a micrometastasis are eligible. An axillary dissection is not required to be performed in patients with a micrometastasis found by sentinel node evaluation. In cases where the specific pathologic size of lymph node involvement is subject to interpretation, the principal investigator will make the final determination as to eligibility. The investigator must document approval in the patient medical record.
  • Patients who have an area of a T1aN0, ER+ (defined as >10%), HER2-negative cancer in addition to their primary HER2-positive tumor are eligible.
• HER2-positive by ASCO CAP 2018 guidelines, confirmed by central testing. NOTE: HER-2 status must be confirmed to be positive by central review by NeoGenomics prior to patient starting protocol therapy. Patients previously having had HER2 immunohistochemical testing by NeoGenomics do not need to undergo retesting for central confirmation of HER2 status.

NOTE: DCIS components will not be counted in the determination of HER2 status

• ER/PR determination is required. ER and PR assays should be performed by immunohistochemical methods according to the local institution standard protocol.
• Bilateral breast cancers that individually meet eligibility criteria are allowed.
• Patients with multifocal or multicentric disease are eligible, as long as each tumor individually meets eligibility criteria. Central confirmation is needed for any site of disease that is tested to be HER2-positive by local testing (unless testing was previously done by NeoGenomics).
• Patients with a history of ipsilateral DCIS are eligible if they were treated with wide excision alone, without radiation therapy, or treated with a mastectomy for this current breast cancer. Patients with a history of contralateral DCIS are not eligible.
• ≤ 90 days between the planned treatment start date and the patient's most recent breast surgery for this breast cancer
• ≥ 18 years of age with any menopausal status.
• ECOG Performance Status 0 or 1

• All tumor should be removed by either a modified radical mastectomy or a segmental mastectomy (lumpectomy), with either a sentinel node biopsy or axillary dissection

  • All margins should be clear of invasive cancer or DCIS (i.e. no tumor on ink). The local pathologist must document negative margins of resection in the pathology report. If all other margins are clear, a positive posterior (deep) margin is permitted, provided the surgeon documents that the excision was performed down to the pectoral fascia and all tumor has been removed. Likewise, if all other margins are clear, a positive anterior (superficial; abutting skin) margin is permitted provided the surgeon documents that all tumor has been removed.
• Patients undergoing breast conservation therapy (i.e. lumpectomy) must not have any contraindications to radiation therapy. Radiation to the conserved breast is required.
• Patients may have received up to 4 weeks of tamoxifen therapy, or other hormonal therapy, for adjuvant therapy for this cancer. Patients cannot receive adjuvant hormonal therapy during protocol treatment for the first 12 weeks.
• Prior oophorectomy for cancer prevention is allowed.
• Patients who have undergone partial breast radiation (duration ≤ 14 days) prior to registration are eligible. Partial breast radiation must be completed prior to 2 weeks before starting protocol therapy. Patients who have undergone whole breast radiation are not eligible.
• Patients who have participated in a window study (treatment with an investigational agent prior to surgery for ≤ 2 weeks) are eligible. Patients must have discontinued the investigational agent at least 14 days before participation.

• Adequate bone marrow function:

  • ANC ≥ 1000/mm3,
  • Hemoglobin ≥ 9 g/dl
  • Platelets ≥ 100,000/mm3

• Adequate hepatic function:

  • Total bilirubin ≤ 1.2mg/dL
  • AST and ALT ≤ 1.5x Institutional ULN
  • For patients with Gilbert syndrome, the direct bilirubin should be within the institutional normal range. Serum alkaline phosphatase should be ≤ 1.5x Institutional ULN.
• Left ventricular ejection fraction (LVEF) ≥ 50%
• Premenopausal patients must have a negative serum or urine pregnancy test, including women who have had a tubal ligation and for women less than 12 months after the onset of menopause.
• Women of childbearing potential and men with partners of childbearing potential must be willing to use one highly effective form of nonhormonal contraception or two effective forms of nonhormonal contraception by the patient and/or partner. Contraceptive use must be continued for the duration of the study treatment and for 7 months after the last dose of study treatment. Hormonal birth control methods are not permitted.
• Patients should have tumor tissue available, and a tissue block of sufficient size to make 15 slides, which must be sent to DFCI for correlative research. If a tissue block is unavailable, sites may send one H&E-stained slide and 15 unstained sections of paraffin-embedded tissue on uncharged slides. Slide sections should be 4-5 microns in thickness. It is also acceptable to submit 2 cores from a block of invasive tissue using a 1.2 mm diameter coring tool. If tumor is not available, the investigator must document why tissue is not available in the patient medical record, and that efforts have been made to obtain tissue.
• Willing and able to sign informed consent
• Must be able to read and understand English in order to participate in the quality of life surveys. If patient does not read and understand English, the patient is still eligible, but cannot participate in the quality of life surveys.

Exclusion Criteria:

• Any of the following due to teratogenic potential of the study drugs:

  • Pregnant women
  • Nursing women
  • Women of childbearing potential who are unwilling to employ adequate contraception (condoms, diaphragms, IUDs, surgical sterilization, abstinence, etc.).
  • Men who are unwilling to employ adequate contraception (condoms, surgical sterilization, abstinence, etc.).
• Locally advanced tumors at diagnosis, including tumors fixed to the chest wall, peau d'orange, skin ulcerations/nodules, or clinical inflammatory changes (diffuse brawny cutaneous induration with an erysipeloid edge)
• Patients with a history of previous invasive breast cancer.
• History of prior chemotherapy in the past 5 years.
• History of paclitaxel therapy
• Patients with active liver disease, for example due to hepatitis B virus, hepatitis C virus, autoimmune hepatic disorder, or sclerosing cholangitis

• Individuals with a history of a different malignancy are ineligible except for the following circumstances:

  • Individuals with a history of other malignancies are eligible if they have been disease-free for at least 5 years and are deemed by the investigator to be at low risk for recurrence of that malignancy.
  • Individuals with the following cancer are eligible regardless of when they were diagnosed and treated: cervical cancer in situ, and non-melanoma cancer of the skin.
• Intercurrent illness including, but not limited to: ongoing or active, unresolved systemic infection, renal failure requiring dialysis, active cardiac disease, prior myocardial infarction (asymptomatic changes on EKG suggestive of old MI is not an exclusion), history of CHF, current use of any therapy specifically for CHF, uncontrolled hypertension, significant psychiatric illness, or other conditions that in the opinion of the investigator limit compliance with study requirements.

Contacts and Locations

Contacts

Contact: Sara Tolaney, MD, PhD; 617-632-2335; sara_tolaney@dfci.harvard.edu

Locations

United States, California

UCSF Helen Diller Family Comprehensive Cancer Center; Recruiting

San Francisco, California, United States, 94158

Contact: Hope Rugo, MD

Principal Investigator: Hope Rugo, MD

United States, Connecticut

Smilow Cancer Hospital Care center at Derby; Recruiting

Derby, Connecticut, United States, 06418

Contact: Clinical Trial Offcie Yale Cancer Center 203-734-1664

Principal Investigator: Daniel O'Neil, MD

Smilow Cancer Hospital Care center at Fairfield; Recruiting

Fairfield, Connecticut, United States, 06824

Contact: Clinical Trials Office Yale Cancer Center 203-255-2766

Principal Investigator: Daniel O'NEIL, MD

Smilow Cancer Hospital Care center at Glastonbury; Recruiting

Glastonbury, Connecticut, United States, 06033

Contact: Clinical Trial Office Yale Cancer Center 860-714-9170

Principal Investigator: Daniel O'Neil, MD

Smilow Cancer Hospital Care center at Greenwich; Recruiting

Greenwich, Connecticut, United States, 06830

Contact: Clinical Trials Office Yale Cancer Center 203-863-3700

Principal Investigator: Daniel O'Neil, MD

Smilow Cancer Hospital Care center at Guilford; Recruiting

Guilford, Connecticut, United States, 06437

Contact: Clinical Trial Office Yale Cancer Center 203-453-9192

Principal Investigator: Daniel O'Neil, MD

Smilow Cancer Hospital Care center at St. Francis; Recruiting

Hartford, Connecticut, United States, 06105

Contact: Clinical Trial Office Yale Cancer Center 860-714-4680

Principal Investigator: Daniel O'Neil, MD

Smilow Cancer Hospital Care center at Long Ridge; Recruiting

Long Ridge, Connecticut, United States, 06902

Contact: Clinical Trial Office Yale Center 203-863-3700

Principal Investigator: Daniel O'Neil, MD

Yale Cancer Center at Yale University School of Medicine; Recruiting

New Haven, Connecticut, United States, 06520-8028

Contact: Clinical Trial Office Clinical Trials Office - Yale Cancer Center 203-785-5702

Principal Investigator: Daniel O'Niel, MD

Smilow Cancer Hospital Care center at North Haven; Recruiting

North Haven, Connecticut, United States, 06510

Contact: Clinical Trials Office Yale Cancer Center 203-407-8002

Principal Investigator: Daniel O'neil, MD

Stamford Hospital; Recruiting

Stamford, Connecticut, United States, 06904

Contact: K.M. Steve Lo, MD slo@stamhealth.org

Principal Investigator: K. M. Steve Lo, MD

Smilow Cancer Hospital Care center at Torrington; Recruiting

Torrington, Connecticut, United States, 06790

Contact: Clinical Trial Office Yale Cancer Center 860-482-5384

Principal Investigator: Daniel O'Neil, MD

Smilow Cancer Hospital Care center at Trumbull; Recruiting

Trumbull, Connecticut, United States, 06611

Contact: Clinical Trials Office Cancer Trial 203-502-8400

Principal Investigator: Daniel O'Neil, MD

Smilow Cancer Hospital Care center at Waterbury; Recruiting

Waterbury, Connecticut, United States, 06708

Contact: Clinical Trials Office Yale Cancer Center 203-755-6311

Principal Investigator: Daniel O'Neil, MD

Smilow Cancer Hospital Care center at Waterford; Recruiting

Waterford, Connecticut, United States, 06385

Contact: Clinical Trials Office Yale Cancer Center 860-444-3744

Principal Investigator: Daniel O'Neil, MD

United States, Florida

Miami Cancer Institute/Baptist Hospital of Miami; Recruiting

Miami, Florida, United States, 33176

Contact: Reshma Mahtani, DO

Sub-Investigator: Reshma Mahtani, DO

Miami Cancer Institute - Plantation (MCIP); Recruiting

Plantation, Florida, United States, 33324

Contact: Reshma Mahtani, DO reshma.mahtani@baptisthealth.net

Principal Investigator: Reshma Mahtani, DO

United States, Indiana

Indiana University Health Joe & Shelly Schwarz Cancer Center; Recruiting

Carmel, Indiana, United States, 46032

Contact: Kathy Miller, MD kathmill@iu.edu

Principal Investigator: Kathy Miller, MD

IU Health North Hospital; Recruiting

Carmel, Indiana, United States, 46032

Contact: Kathy Miller, MD kathmill@iu.edu

Principal Investigator: Kathy Miller, MD

Indiana University Melvin and Bren Simon Comprehensive Cancer Center; Recruiting

Indianapolis, Indiana, United States, 46202

Contact: Kathy Miller, MD kathmill@iu.edu

Principal Investigator: Kathy Miller, MD

Indiana University Sidney and Lois Eskenazi Hospital; Recruiting

Indianapolis, Indiana, United States, 46202

Contact: Kathy Miller, MD kathmill@iu.edu

Principal Investigator: Kathy Miller, MD

United States, Maine

Eastern Maine Medical Center (Northern Light); Recruiting

Brewer, Maine, United States, 04412

Contact: Laurie Lewis 207-973-4249 llewis@northernlight.org

Principal Investigator: Sarah J Sinclair, DO

New England Cancer Specialists; Recruiting

Scarborough, Maine, United States, 04074

Contact: Rachael Farris research@newecs.org

Principal Investigator: Chiara Battelli, MD

United States, Massachusetts

Beth Israel Deaconess Medical Center; Recruiting

Boston, Massachusetts, United States, 02215

Contact: Nadine Tung, MD 617-667-7081 ntung@bidmc.harvard.edu

Principal Investigator: Nadine Tung, MD

Dana Farber Cancer Institute; Recruiting

Boston, Massachusetts, United States, 02215

Contact: Sara M. Tolaney, MD MPH 617-632-2335 Sara_Tolaney@dfci.harvard.edu

Principal Investigator: Sara M. Tolaney, MD MPH

Massachusetts General Hospital; Recruiting

Boston, Massachusetts, United States, 02215

Contact: Laura Spring, MD 617-724-4000 Lspring2@partners.org

Principal Investigator: Laura Spring, MD

Dana-Farber at St. Elizabeth's Medical Center; Recruiting

Brighton, Massachusetts, United States, 02135

Contact: Wendy Loeser Wendy_Loeser@DFCI.HARVARD.EDU

Principal Investigator: Sara Giordano, MD

Mass General North Shore Cancer Center; Recruiting

Danvers, Massachusetts, United States, 01923

Contact: Meegan Petersen mpetersen1@partners.org

Principal Investigator: Katherine Harris, MD

Dana-Farber Brigham Cancer Center - Foxborough; Recruiting

Foxboro, Massachusetts, United States, 02035

Contact: Natalie Sinclair 781-624-4800 nsinclair1@partners.org

Principal Investigator: Natalie Sinclair, MD

Dana-Farber Cancer Instiute - Merrimack Valley; Recruiting

Methuen, Massachusetts, United States, 01844

Contact: Saida Hussein saida_hussein@dfci.harvard.edu

Principal Investigator: Pedro Sanz-Altamira, MD

Dana-Farber at Milford; Recruiting

Milford, Massachusetts, United States, 01757

Contact: Natalie Sinclair, MD NSINCLAIR1@PARTNERS.ORG

Principal Investigator: Natalie Sinclair, MD

Newton Wellesley Hospital; Recruiting

Newton, Massachusetts, United States, 02462

Contact: Natassia Mazzola NAMAZZOLA@mgh.harvard.edu

Principal Investigator: Aron Rosenstock, MD

Berkshire Medical Center; Recruiting

Pittsfield, Massachusetts, United States, 01201

Contact: Lori O'Brien lobrien@bhs1.org

Principal Investigator: Thomas Fynan, MD

Dana Farber at South Shore Hospital; Recruiting

Weymouth, Massachusetts, United States, 02190

Contact: Meredith Faggen meredith_faggen@dfci.harvard.edu

Contact 7816244800

Principal Investigator: Meredith Faggen, MD

United States, New Hampshire

NH Oncology-Hematology, PA - Payson Center for Cancer Care; Recruiting

Concord, New Hampshire, United States, 03301

Contact: Ali Fleury 603-224-2556 a.fleury@nhoh.com

Principal Investigator: Douglas Weckstein, MD

Dana-Farber Cancer Insitute at Londonderry Hospital; Recruiting

Londonderry, New Hampshire, United States, 03053

Contact: Stefani Freeman, RN StefaniD_Freeman@DFCI.HARVARD.EDU

Principal Investigator: Jeanna Walsh, MD

Solinsky Center for Cancer Care (NH Oncology-Hematology, PA); Recruiting

Manchester, New Hampshire, United States, 03103

Contact: Ali Fleury 603-224-2556 a.fleury@nhoh.com

Principal Investigator: Douglas Weckstein, MD

United States, New York

State University of New York Downstate Medical Center; Recruiting

Brooklyn, New York, United States, 11220

Contact: Gurinder Sidhu, MD gurinder@downstate.edu

Principal Investigator: Gurinder Sidhu, MD

New York University Langone Hospital - Long Island; Recruiting

Mineola, New York, United States, 11501

Contact: Mehwash "Mahi" Muhammad mehwash.muhammad@nyulangone.org

Principal Investigator: Sylvia Adams, MD

New York University Langone Health; Recruiting

New York, New York, United States, 10016

Contact: Sylvia Adams, MD sylvia.adams@nyulangone.org

Principal Investigator: Sylvia Adams, MD

United States, North Carolina

Duke University Medical Center; Recruiting

Durham, North Carolina, United States, 27710

Contact: Gretchen Kimmick, MD gretchen.kimmick@duke.edu

Principal Investigator: Gretchen Kimmick, MD

Duke Women's Cancer Care Raleigh; Recruiting

Raleigh, North Carolina, United States, 27710

Contact: Gretchen Kimmick, MD gretchen.kimmick@duke.edu

Principal Investigator: Gretchen Kimmick, MD

United States, Ohio

Stefanie Spielman Comprehensive Breast Center; Recruiting

Columbus, Ohio, United States, 43212

Contact: Breast Cancer Clinical Trials 800-293-5066

Principal Investigator: Gilbert Bader, MD

United States, Pennsylvania

University of Pennsylvania, Abramson Cancer Center; Recruiting

Philadelphia, Pennsylvania, United States, 19104

Contact: Igor Makhlin, MD igor.makhlin@pennmedicine.upenn.edu

Principal Investigator: Igor Makhlin, MD

United States, Rhode Island

Smilow Cancer Hospital Care center at Westerly; Recruiting

Westerly, Rhode Island, United States, 02891

Contact: Clinical Trials Office Yale Cancer Center 401-656-4950

Principal Investigator: Daniel O'Neil, MD

United States, Tennessee

Sarah Cannon Research Institute; Recruiting

Nashville, Tennessee, United States, 37203

Contact: Denise A Yardley, MD dyardley@tnonc.com

Principal Investigator: Denise A Yardley, MD

United States, Texas

MD Anderson Cancer Center; Recruiting

Houston, Texas, United States, 77030

Contact: Vicente Valero, MD 713-563-0751 vvalero@mdanderson.org

Principal Investigator: Vicente Valero, MD

Sponsors and Collaborators

Dana-Farber Cancer Institute

Genentech, Inc.

Investigators

• Principal Investigator: Sara Tolaney, MD, PhD; Dana-Farber Cancer Institute

More Information

• Responsible Party: Sara Tolaney, MD, Principal Investigator, Dana-Farber Cancer Institute
• ClinicalTrials.gov Identifier: NCT04893109
• Other Study ID Numbers: 21-159
• First Posted: May 19, 2021
• Last Update Posted: April 25, 2024
• Last Verified: April 2024

Individual Participant Data (IPD) Sharing Statement:

• Plan to Share IPD: Yes
• Plan Description: The Dana-Farber / Harvard Cancer Center encourages and supports the responsible and ethical sharing of data from clinical trials. De-identified participant data from the final research dataset used in the published manuscript may only be shared under the terms of a Data Use Agreement. Requests may be directed to: [contact information for Sponsor Investigator or designee]. The protocol and statistical analysis plan will be made available on Clinicaltrials.gov only as required by federal regulation or as a condition of awards and agreements supporting the research.
• Supporting Materials: Study Protocol; Statistical Analysis Plan (SAP); Informed Consent Form (ICF)
• Time Frame: Data can be shared no earlier than 1 year following the date of publication
• Access Criteria: Contact the Belfer Office for Dana-Farber Innovations (BODFI) at innovation@dfci.harvard.edu

• Studies a U.S. FDA-regulated Drug Product: Yes
• Studies a U.S. FDA-regulated Device Product: No

Keywords provided by Sara Tolaney, MD, Dana-Farber Cancer Institute:

Breast Cancer; HER2-positive Breast Cancer

Additional relevant MeSH terms:

Breast Neoplasms; Neoplasms by Site; Neoplasms; Breast Diseases; Skin Diseases; Paclitaxel; Maytansine; Ado-Trastuzumab Emtansine; Trastuzumab; Antineoplastic Agents, Phytogenic; Antineoplastic Agents; Tubulin Modulators; Antimitotic Agents; Mitosis Modulators; Molecular Mechanisms of Pharmacological Action; Antineoplastic Agents, Immunological; Immunotoxins; Immunoconjugates; Immunologic Factors; Physiological Effects of Drugs