Breast Cancer Clinical Trial
Official title:
A Phase II Trial of Lapatinib and Trastuzumab With or Without Endocrine Therapy in Locally Advanced HER2 Overexpressing Breast Cancer Patients
We think that lapatinib will help to shrink your tumor when given prior to the main or
primary therapy for the kind of breast cancer you have been diagnosed with. When treatment is
given before the main or primary therapy, it is called neoadjuvant therapy. We will compare
lapatinib with lapatinib plus trastuzumab (herceptin) for 12 weeks. If your tumor is estrogen
receptor positive (ER positive), estrogen deprivation will also be given to you. Tumors that
are ER positive have a lot of estrogen receptors found in them. This is also called "over
expression" or amplification of estrogen receptors.
The most important information we will get from this study is to see the response to
"neoadjuvant" (treatment given before the main treatment), lapatinib with trastuzumab
(herceptin) in your tumor tissue sample.
The neoadjuvant setting is especially attractive for studies of predictive biologic
correlates for several reasons including early assessment of response to therapy, access to
the primary tumor, and reduced patient numbers compared to those required in the adjuvant
setting. Response to neoadjuvant therapy is a validated surrogate marker for improved
survival; it may be used to test the overall efficacy of neoadjuvant treatment regimens and
response in the primary tumor mirrors the effect of therapy on micrometastases.
Trastuzumab is an efficacious agent in HER2 overexpressing breast cancers. Our results with
neoadjuvant trastuzumab indicate that its efficacy may be better in patients with
treatment-naïve tumors compared to metastatic disease, with 26% of patients showing a partial
response after only 3 weeks of therapy. No patients progressed during this 3-week period. We
have also conducted a neoadjuvant lapatinib study given as a single agent for 6 weeks. The
response rates in this second study have been impressive with greater than 80% responses in
patients with HER2 positive locally advanced breast cancers. It is likely that the true
response rate to HER2 blockade would be higher had therapy been continued for longer. We
therefore hypothesize that lapatinib, a dual tyrosine kinase inhibitor, together with
trastuzumab, will result in tumor regression when given as neoadjuvant therapy in HER2
overexpressing breast cancer. We will compare lapatinib plus trastuzumab for 12 weeks, and if
the tumors express ER, estrogen deprivation will also be administered.
This is a phase II trial. Clinical efficacy will be assessed by bidimensional tumor
measurements of the primary cancer at baseline, and at the end of week 12. Objective tumor
response rate defined as objective bidimensional tumor measurements after neoadjuvant
treatment at 12 weeks will be calculated, and assessed according to standard RECIST criteria.
Pathologic responses will be graded as pathologic complete response if there is no invasive
cancer in the residual breast at the time of surgery. Near pathologic complete response will
also be documented as residual disease of less than 1 cm.
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