2. HER2: beyond Herceptin
3. “Non esiste vento favorevole per il marinaio che non sa dove andare”��(there is no favourable wind for a sailor �who does not know where to go) Seneca (5 aC-65 dC)
4. Why targeting HER2 beyond Trastuzumab in Breast Cancer? � Efficacy
Primary resistance
Secondary resistance
Cardiac safety
HER2 + molecular subtypes
5. FIRST-LINE SINGLE-AGENT TRIAL RESPONSE ACCORDING TO HER2 STATUS
6. Efficacy data from Phase II and III trials of trastuzumab combined with chemotherapy
9. HER2+ Advanced Breast Cancer ~ 60 – 70% of patients exhibit a primary resistance to Trastuzumab monotherapy
~ 30 – 50% of patients show a primary resistance to Trastuzumab plus chemotherapy
Eventually, all the patients become resistant to Trastuzumab within months or years
CNS MTS are frequent
Trastuzumab is ineffective for CNS MTS ( CSF levels 300-fold lower than in the serum)
10. The Censored DFS analysis, censoring pts switching to delayed trastuzumab at the time of the switch –
Also shows a highly significant benefit, very similar to the ITT, with a HR of 0.63 and an absolute 3 yr DFS gain of 6.6%The Censored DFS analysis, censoring pts switching to delayed trastuzumab at the time of the switch –
Also shows a highly significant benefit, very similar to the ITT, with a HR of 0.63 and an absolute 3 yr DFS gain of 6.6%
12. HER2+ Early Breast Cancer > 50% of patients do not need HER2 targeted therapy
> 50% of patients show a primary resistance to Trastuzumab plus chemotherapy
CNS relapse as 1st event is more frequent in patients on adjuvant trastuzumab
13. Management of trastuzumab resistance�Lesson # 1 Check HER2 positivity on original tumor blocks
Whenever possible, test HER2 status on recurrent disease
Trastuzumab and chemotherapy can act synergically on apoptotic pathway
Other proteins in the EFGR-mediated signalling pathways are important
Other EGFRs (i.e.HER1) can be important
14. Trastuzumab resistance Trastuzumab can induce apoptosis through inhibition of PI3K/Akt pathway
PTEN normally opposes PI3K/Akt signaling
trastuzumab stabilizes PTEN and downregulates Akt signaling
loss of PTEN can induce trastuzumab resistance
15. ErbB2/ErbB3 Expression and Estrogen �Receptor Status in Breast Carcinomas Signaling through either the estrogen receptor (ER) or ErbB receptors is often discussed as if they were discrete pathways, but experimental evidence suggests there is considerable interplay between them. Overexpression of ErbB2 has been found to decrease responsiveness to hormonal therapy in patients with breast cancer,1 and estrogen depletion can increase the expression of ErbB1 in breast cancer cell lines.2
This evidence of crosstalk raises the question of the relationship between ER and ErbB expression in primary tumors. In a study conducted by Witton and colleagues, ErbB and estrogen receptor (ER) levels were determined by immunohistochemistry in 220 breast carcinomas.3 An inverse relationship was detected between ER expression and expression of ErbB1, ErbB2, and/or ErbB3.
1. De Placido S, De Laurentiis M, Carlomagno C, et al. Twenty-year results of the Naples GUN randomized trial: predictive factors of adjuvant tamoxifen efficacy in early breast cancer. Clin Cancer Res 2003; 9:1039-46.
2. Yarden RI, Wilson MA, Chrysogelos SA. Estrogen suppression of EGFR expression in breast cancer cells: A possible mechanism to modulate growth. J Cell Biochem 2001; 81:232-246.
3. Witton CJ, Reeves JR, Going JJ, et al. Expression of the HER1-4 family of receptor tyrosine kinases in breast cancer. J Pathol 2003; 200:290-7.
Signaling through either the estrogen receptor (ER) or ErbB receptors is often discussed as if they were discrete pathways, but experimental evidence suggests there is considerable interplay between them. Overexpression of ErbB2 has been found to decrease responsiveness to hormonal therapy in patients with breast cancer,1 and estrogen depletion can increase the expression of ErbB1 in breast cancer cell lines.2
This evidence of crosstalk raises the question of the relationship between ER and ErbB expression in primary tumors. In a study conducted by Witton and colleagues, ErbB and estrogen receptor (ER) levels were determined by immunohistochemistry in 220 breast carcinomas.3 An inverse relationship was detected between ER expression and expression of ErbB1, ErbB2, and/or ErbB3.
1. De Placido S, De Laurentiis M, Carlomagno C, et al. Twenty-year results of the Naples GUN randomized trial: predictive factors of adjuvant tamoxifen efficacy in early breast cancer. Clin Cancer Res 2003; 9:1039-46.
2. Yarden RI, Wilson MA, Chrysogelos SA. Estrogen suppression of EGFR expression in breast cancer cells: A possible mechanism to modulate growth. J Cell Biochem 2001; 81:232-246.
3. Witton CJ, Reeves JR, Going JJ, et al. Expression of the HER1-4 family of receptor tyrosine kinases in breast cancer. J Pathol 2003; 200:290-7.
16. Survival Interrelationship Between �ER/PR Status and ErbB Expression Dr. Witton and colleagues reported that there was a significant survival difference
among the patients with ER+ tumors depending on ErbB receptor status
(P = .0016).1 The 10-year survival rate was lower for the patients with tumors
that were ER+ and positive for ErbB1, ErbB2, or ErbB3 (35%) than for those
with ER+ tumors that were negative for all ErbB receptors (55%). However, survival
rates were significantly higher in the patients with ER+ tumors that were
positive for ErbB4 (80%). No significant difference was seen in 10-year survival
in the patients with ER– tumors that were either positive or negative for ErbB1,
ErbB2, or ErbB3.
Witton CJ, Reeves JR, Going JJ, et al. Expression of the HER1–4 family of receptor tyrosine kinases in breast cancer. J Pathol 2003; 200:290-7.
Dr. Witton and colleagues reported that there was a significant survival difference
among the patients with ER+ tumors depending on ErbB receptor status
(P = .0016).1 The 10-year survival rate was lower for the patients with tumors
that were ER+ and positive for ErbB1, ErbB2, or ErbB3 (35%) than for those
with ER+ tumors that were negative for all ErbB receptors (55%). However, survival
rates were significantly higher in the patients with ER+ tumors that were
positive for ErbB4 (80%). No significant difference was seen in 10-year survival
in the patients with ER– tumors that were either positive or negative for ErbB1,
ErbB2, or ErbB3.
Witton CJ, Reeves JR, Going JJ, et al. Expression of the HER1–4 family of receptor tyrosine kinases in breast cancer. J Pathol 2003; 200:290-7.
17. Effect on survival of the expression of other EGF-r family members
18. Lapatinib Mechanism of Action Binds to intracellular ATP binding site of EGFR (ErbB-1) and HER2 (ErbB-2) preventing phosphorylation and activation
Blocks downstream signaling through homodimers and heterodimers of EGFR (ErbB-1) and HER2 (ErbB-2)
Dual blockade of signaling may be more effective than the single-target inhibition provided by agents such as trastuzumab As a dual-kinase inhibitor with specificity for both ErbB1 and ErbB2, lapatinib can block signaling through homodimers composed of either of these receptors.1,2 In theory, lapatinib may also be able to inhibit or decrease signaling through other heterodimer combinations, such as ErbB2/ErbB3.
1. Rusnak DW, Lackey K, Affleck K, et al. The effects of the novel, reversible epidermal growth factor receptor/ErbB-2 tyrosine kinase inhibitor, GW2016, on the growth of human normal and tumor-derived cell lines in vitro and in vivo. Mol Cancer Ther 2001; 1:85-94.
Xia W, Mullin RJ, Keith BR, et al. Anti-tumor activity of GW572016: a dual tyrosine kinase inhibitor blocks EGF activation of EGFR/erbB2 and downstream Erk1/2 and AKT pathways. Oncogene 2002; 21:6255-63.
Konecny GE, Pegram MD, Venkatesan N, et al. Activity of the dual kinase inhibitor lapatinib (GW572016) against HER-2-overexpressing and trastuzumab-treated breast cancer cells. Cancer Res. 2006;66:1630-1639.
As a dual-kinase inhibitor with specificity for both ErbB1 and ErbB2, lapatinib can block signaling through homodimers composed of either of these receptors.1,2 In theory, lapatinib may also be able to inhibit or decrease signaling through other heterodimer combinations, such as ErbB2/ErbB3.
1. Rusnak DW, Lackey K, Affleck K, et al. The effects of the novel, reversible epidermal growth factor receptor/ErbB-2 tyrosine kinase inhibitor, GW2016, on the growth of human normal and tumor-derived cell lines in vitro and in vivo. Mol Cancer Ther 2001; 1:85-94.
Xia W, Mullin RJ, Keith BR, et al. Anti-tumor activity of GW572016: a dual tyrosine kinase inhibitor blocks EGF activation of EGFR/erbB2 and downstream Erk1/2 and AKT pathways. Oncogene 2002; 21:6255-63.
Konecny GE, Pegram MD, Venkatesan N, et al. Activity of the dual kinase inhibitor lapatinib (GW572016) against HER-2-overexpressing and trastuzumab-treated breast cancer cells. Cancer Res. 2006;66:1630-1639.
19. Dual kinase inhibitor lapatinib against HER-2 overexpressing and trastuzumab-treated breast cancer cell lines
20. Combined effect of �Trastuzumab and Lapatinib
21. Phase Ib Trial: EGF10004�Overview Study objectives:
Determine a dose or range of biologically active doses
Evaluate safety and tolerability
Examine dose pharmacokinetics and pharmacodynamics
Study design:
Patients randomized to doses of 500, 650, 900, 1200, or 1600 mg/day
Clinical response evaluated every 8 weeks
Biological effects examined by comparing biomarker results from biopsy samples obtained pretreatment and following 21 days of therapy The phase Ib trial EGF10004 was designed to determine the range of biologically effective doses for lapatinib. Additional goals of this study included evaluating safety and tolerability as well as pharmacokinetics and pharmacodynamics at different doses. Patients were required to have tumors with documented overexpression or activation of ErbB1 or ErbB2 (immunohistochemical data) or evidence of amplification of the ErbB2 gene. Tumors or ascites also needed to be amenable to baseline and repeat biopsies. In addition, patients were required to have adequate organ function with an LVEF >40%.
Eligible patients were randomized to 5 dose levels, with skin and tumor biopsies obtained prior to the start of the study and again on day 21. Clinical responses were determined every 8 weeks. The biological effects of lapatinib on skin and tumor tissue were evaluated by quantitative immunohistochemistry.
The phase Ib trial EGF10004 was designed to determine the range of biologically effective doses for lapatinib. Additional goals of this study included evaluating safety and tolerability as well as pharmacokinetics and pharmacodynamics at different doses. Patients were required to have tumors with documented overexpression or activation of ErbB1 or ErbB2 (immunohistochemical data) or evidence of amplification of the ErbB2 gene. Tumors or ascites also needed to be amenable to baseline and repeat biopsies. In addition, patients were required to have adequate organ function with an LVEF >40%.
Eligible patients were randomized to 5 dose levels, with skin and tumor biopsies obtained prior to the start of the study and again on day 21. Clinical responses were determined every 8 weeks. The biological effects of lapatinib on skin and tumor tissue were evaluated by quantitative immunohistochemistry.
22. EGF10004 Results: Frequency of Achieving = 75% Inhibition of p-EGFR, p-ErbB2, p-ERK1/2, or �p-AKT Expression in Tumors at Day 21 In order to determine the range of biologically effective doses of lapatinib, a panel of tumor biomarkers was examined by quantitative immunohistochemistry.1 Tumor samples were taken at day 0 and at day 21 following initiation of treatment. Potent inhibition of the phosphorylation of ErbB1, ErbB2, ERK1/2 or Akt occurred at dose levels greater than or equal to 650 mg/day. The greatest frequency of inhibition was observed in patients receiving 1600 mg daily (80%).
1. Burris H, Hurwitz H, Dees C, et al. EGF 10004: a randomized, multicenter, phase Ib study of the safety, biologic activity and clinical efficacy of the dual kinase inhibitor GW572016 [abstract #39]. (SABCS Oral Presentation) Breast Cancer Res Treat. 2003;82 (suppl1):S18
In order to determine the range of biologically effective doses of lapatinib, a panel of tumor biomarkers was examined by quantitative immunohistochemistry.1 Tumor samples were taken at day 0 and at day 21 following initiation of treatment. Potent inhibition of the phosphorylation of ErbB1, ErbB2, ERK1/2 or Akt occurred at dose levels greater than or equal to 650 mg/day. The greatest frequency of inhibition was observed in patients receiving 1600 mg daily (80%).
1. Burris H, Hurwitz H, Dees C, et al. EGF 10004: a randomized, multicenter, phase Ib study of the safety, biologic activity and clinical efficacy of the dual kinase inhibitor GW572016 [abstract #39]. (SABCS Oral Presentation) Breast Cancer Res Treat. 2003;82 (suppl1):S18
23. EGF10004: Clinical Characteristics of Responders––�Breast Cancer Subset Sixty-seven patients with various solid tumors were entered on study with the largest proportion (n=30) having breast cancer. The patients were heavily pretreated having received a median of 5 prior lines of treatment (range, 1-14).
Four patients (of 59 evaluable) achieved a partial response, all of whom had breast cancer. Twenty-four patients showed stable disease (10 breast cancer, 5 NSCLC, 3 colorectal cancer, 3 SCCHN, and 1 each of ovarian, adenocarcinoma of unknown primary, and granular cell carcinoma).
Details of the 4 breast cancer patients who responded were assessed in detail so as to understand clinical parameters which may influence responsiveness. Two of the patients had inflammatory breast cancer.
Among these 4 patients all overexpressed ErbB2 (3+ by IHC) and histological evaluation of the tumor sample revealed that ErbB2 activity was inhibited by lapatinib. Three of the patients also overexpressed EGFR/ErbB1.
All patients had received prior therapy with trastuzumab, 3 had received taxanes and 3 had received anthracyclines.
Burris H, Hurwitz H, Dees EC et al. Phase I Safety, Pharmacokinetics, and Clinical Activity Study of Lapatinib (GW572016), a Reversible, Dual Inhibitor of Epidermal Growth Factor Receptor Tyrosine Kinases in Heavily Pretreated Patients With Metastatic Carcinomas J Clin Oncol 2005; 23:1-9
Sixty-seven patients with various solid tumors were entered on study with the largest proportion (n=30) having breast cancer. The patients were heavily pretreated having received a median of 5 prior lines of treatment (range, 1-14).
Four patients (of 59 evaluable) achieved a partial response, all of whom had breast cancer. Twenty-four patients showed stable disease (10 breast cancer, 5 NSCLC, 3 colorectal cancer, 3 SCCHN, and 1 each of ovarian, adenocarcinoma of unknown primary, and granular cell carcinoma).
Details of the 4 breast cancer patients who responded were assessed in detail so as to understand clinical parameters which may influence responsiveness. Two of the patients had inflammatory breast cancer.
Among these 4 patients all overexpressed ErbB2 (3+ by IHC) and histological evaluation of the tumor sample revealed that ErbB2 activity was inhibited by lapatinib. Three of the patients also overexpressed EGFR/ErbB1.
All patients had received prior therapy with trastuzumab, 3 had received taxanes and 3 had received anthracyclines.
Burris H, Hurwitz H, Dees EC et al. Phase I Safety, Pharmacokinetics, and Clinical Activity Study of Lapatinib (GW572016), a Reversible, Dual Inhibitor of Epidermal Growth Factor Receptor Tyrosine Kinases in Heavily Pretreated Patients With Metastatic Carcinomas J Clin Oncol 2005; 23:1-9
24. �EGF20009:�A Phase II, Randomized Trial Using the Small Molecule Tyrosine Kinase Inhibitor Lapatinib as a First-Line Treatment in Patients with FISH Positive Advanced or Metastatic Breast Cancer H. L. Gomez, M. A. Chavez, D. C. Doval, �L. W. Chow, B. Newstat, S. H. Stein, �M. S. Berger, G. W. Sledge
ASCO 2005
25. EGF20009: Phase II Randomized Trial of Lapatinib �as First-line Treatment in FISH-Positive �Metastatic Breast Cancer EGF20009 was undertaken to evaluate single agent lapatinib in previously untreated ErbB2-overexpressing MBC. Based upon activity observed with lapatinib in heavily pre-treated patients, it was hypothesized that greater activity would be observed in a chemotherapy-naïve population of MBC patients.
Target accrual for this trial was 130 patients and the patients were required to have ErbB2 positive disease as determined by FISH.
Patients were randomized to treatment with lapatinib 1500 mg/day or 500 mg PO BID. Treatment in either arm was administered for 12 weeks. Efficacy was assessed at 8 and 12 weeks and those benefiting from therapy were permitted to continue therapy. The primary endpoint for this study was objective response rates, with secondary endpoints of clinical benefit, time to response, duration of response, and time to treatment failure.
EGF20009 was undertaken to evaluate single agent lapatinib in previously untreated ErbB2-overexpressing MBC. Based upon activity observed with lapatinib in heavily pre-treated patients, it was hypothesized that greater activity would be observed in a chemotherapy-naïve population of MBC patients.
Target accrual for this trial was 130 patients and the patients were required to have ErbB2 positive disease as determined by FISH.
Patients were randomized to treatment with lapatinib 1500 mg/day or 500 mg PO BID. Treatment in either arm was administered for 12 weeks. Efficacy was assessed at 8 and 12 weeks and those benefiting from therapy were permitted to continue therapy. The primary endpoint for this study was objective response rates, with secondary endpoints of clinical benefit, time to response, duration of response, and time to treatment failure.
26. Efficacy in All Patients
27. EGF20009: Lapatinib Monotherapy for First-line �FISH-Positive Metastatic Breast Cancer�Safety
28. Patient C: Brain Lesion Baseline
29. Patient C: Brain Lesion Week 12
30. Lapatinib + Trastuzumab in Advanced �Pretreated Metastatic Breast Cancer �Phase I Study: EGF10023 Study objectives:
Safety of lapatinib in combination with trastuzumab
Optimally tolerated regimen of combination
Pharmacokinetic parameters
Clinical activity
Eligibility criteria:
Advanced ErbB2+ MBC
Prior treatment with trastuzumab allowed but not required
Treatment consisted of escalating doses of lapatinib 750, 1000, 1250, or 1500 mg/day with trastuzumab (4-mg/kg loading dose; 2 mg/kg/week) Responses to single agent lapatinib in patients with heavily pretreated MBC are limited, according to studies EGF20008 and EGF20002.1,2 In preclinical studies, the combination of lapatinib and trastuzumab demonstrated enhanced activity against an ErbB2-overexpressing cell line compared to either agent alone.3 Thus, to augment activity in these patients, combining lapatinib with trastuzumab may lead to enhanced responsiveness.
A phase I trial (EGF10023) was undertaken to assess the feasibility and to define an optimal regimen for treatment of advanced pretreated MBC using trastuzumab and lapatinib.4,5 Patients had ErbB2+ disease and prior therapy with trastuzumab was allowed but not required. Treatment with trastuzumab was administered with lapatinib in escalating doses of 750, 1000, 1250 or 1500 mg/day. Forty-six patients were enrolled of whom 45 (94%) were pretreated with trastuzumab
1. Blackwell et al. ESMO 2004; Abstract 103
Burstein et al. ESMO 2004; Abstract 104
Konecny et al. Proc AACR 2002; 42 (abstract 4974)
Storniolo A, et al. ECCO 2005; Abstract 278
Storniolo A, et al. SABCS 2005; Abstract 1075Responses to single agent lapatinib in patients with heavily pretreated MBC are limited, according to studies EGF20008 and EGF20002.1,2 In preclinical studies, the combination of lapatinib and trastuzumab demonstrated enhanced activity against an ErbB2-overexpressing cell line compared to either agent alone.3 Thus, to augment activity in these patients, combining lapatinib with trastuzumab may lead to enhanced responsiveness.
A phase I trial (EGF10023) was undertaken to assess the feasibility and to define an optimal regimen for treatment of advanced pretreated MBC using trastuzumab and lapatinib.4,5 Patients had ErbB2+ disease and prior therapy with trastuzumab was allowed but not required. Treatment with trastuzumab was administered with lapatinib in escalating doses of 750, 1000, 1250 or 1500 mg/day. Forty-six patients were enrolled of whom 45 (94%) were pretreated with trastuzumab
1. Blackwell et al. ESMO 2004; Abstract 103
Burstein et al. ESMO 2004; Abstract 104
Konecny et al. Proc AACR 2002; 42 (abstract 4974)
Storniolo A, et al. ECCO 2005; Abstract 278
Storniolo A, et al. SABCS 2005; Abstract 1075
32. Lapatinib + Trastuzumab in Advanced �Pretreated Metastatic Breast Cancer: Results Optimally tolerated dose and dose-limiting toxicities:
Lapatinib 1000 mg/day with standard trastuzumab was defined as optimally tolerated regimen (OTR).
The most frequent adverse at OTR were diarrhea, rash, fatigue, nausea, anorexia, and vomiting.
Pharmacokinetics:
No effect on PK of lapatinib or trastuzumab was observed during coadministration.
Synergism of action of lapatinib and trastuzumab similar to preclinical studies reported.
Based on the prevalence of dose limiting toxicities and need for dose reduction, 1000 mg/day was identified as the dose for further study in combination with trastuzumab. Among 10 patients treated at 1250 mg/day, there were 2 DLTs and 3 dose reductions, and among 3 patients treated at 1500 mg/day, there were 2 DLTs and 2 dose reductions.
Storniolo A, et al. ECCO 2005; Abstract 278, and SABCS 2005; Abstract 1075Based on the prevalence of dose limiting toxicities and need for dose reduction, 1000 mg/day was identified as the dose for further study in combination with trastuzumab. Among 10 patients treated at 1250 mg/day, there were 2 DLTs and 3 dose reductions, and among 3 patients treated at 1500 mg/day, there were 2 DLTs and 2 dose reductions.
Storniolo A, et al. ECCO 2005; Abstract 278, and SABCS 2005; Abstract 1075
33. Management of trastuzumab resistance�Lesson # 2 Combining two MoAbs binding at different epitopes of HER2 receptor can inhibit more efficiently HER2-driven signalling (trastuzumab+Pertuzumab)
Combining an anti-ErbB2 antibody with small molecule tyrosine kinase inhibitor, that act at different sites of the receptor with distinct mechanisms of action, might enhance the efficacy of both drugs (trastuzumab +Lapatinib)
Inhibition of multiple EGFR-family receptors can be important (lapatinib)
34. A Phase III Randomized, Open-Label, International Study Comparing �Lapatinib and Capecitabine vs. Capecitabine in Women with Refractory Advanced or Metastatic Breast Cancer (EGF100151) C.E. Geyer, D. Cameron, D. Lindquist, S. Chan, T. Pienkowski, C.G. Romieu, A. Jagiello-Gruszfeld,�J. Crown, B. Kaufman, A. Chan, J.K. Forster
Allegheny General Hospital, Pittsburgh, PA; Western General Hospital, Edinburgh, UK; US Oncolgy Research Network, Houston,TX; Nottingham City Hospital, Nottingham, UK; Cancer Center, Warsaw, Poland; CRCC Val d’Aurelle Paul Lamarque, Montpellier, France; ZOZ MSWiA, Olsztyn, Poland; St. Vincent’s University Hospital, Dublin, Ireland; Sheba Medical Center, Tel Hashomer, Israel; Mount Medical Centre, Perth, Australia; GlaxoSmithKline, Greenford, UK
35. Study Design
36. EGF 100151 - Study Objectives Primary
TTP
Secondary
Overall survival
Progression free survival
6-month progression free survival
Overall tumor response rate
Clinical benefit (complete, partial response or stable disease for at least 6 months)
Time to response
Duration of response
37. Prior Therapy
38. Prior Trastuzumab for Metastatic Disease
39. Issued – Monday 3 April 2006, London, UK & Philadelphia, US -
LSE Announcement
GlaxoSmithKline Receives Positive Data and Halts Enrolment in Phase III Trial of Tykerb® (Lapatinib) in Advanced Breast Cancer ���
First Regulatory Filings now Planned for 2nd Half of 2006
Based on the unanimous recommendation of an Independent Data Monitoring Committee (IDMC), GlaxoSmithKline (GSK) announced today that it has halted enrolment in its Phase III clinical trial evaluating the combination of Tykerb (lapatinib ditosylate) and capecitabine (Xeloda®) versus capecitabine alone. The trial evaluated women with refractory advanced or metastatic breast cancer who have documented ErbB2 (HER2) overexpression and whose disease progressed following treatment with trastuzumab (Herceptin?) as well as other cancer therapies. A pre-planned interim analysis of 321 patients in the study yielded statistically significant results, exceeding the primary endpoint.
40. EGF100151: Phase III Trial of Capecitabine ± Lapatinib in Advanced or Metastatic Breast Cancer Efficacy
41. Time to Progession – ITT Population
42. EGF100151: Phase III Trial of Capecitabine ± Lapatinib in Advanced or Metastatic Breast Cancer�Brain Metastases as Site of Progression
43. EGF 100151-�Most Frequent Adverse Events � All Grades
44. EGF 100151-Mean LVEF at Scheduled Assessments
45. Conclusions Lapatinib with capecitabine is an effective new regimen for advanced HER2+ breast cancer and should be considered a new standard of care for women meeting eligibility criteria of this trial
46. Summary: Cardiac Effects Associated with Lapatinib Therapy (n = 3558) 1097 pts with > 6 mo exposure to lapatinib
In 598 patients pre-treated with A but no H
1.2% LVEF decrease; 0.3% symptomatic
In 759 patients pre-treated with H and chemotherapy
1.7% LVEF decrease; 0.1% symptomatic
In 2201 A and H naïve patients
1.7% LVEF decrease; 0.2% symptomatic
47. Effect of tumor selection and treatment selection on response
48. EGF109085/CHERLOB�STUDY DESIGN
49. DOSES AND TREATMENT REGIMENS� Arm A: Paclitaxel 80 mg/m2 weekly for 12 weeks ? FE75C q 21 X 4 courses plus trastuzumab 4 mg/kg loading dose followed by 2mg/kg weekly
Arm B: Paclitaxel 80 mg/m2 weekly for 12 weeks ? FE75C q 21 X 4 courses plus Lapatinib 1500 mg po daily
Arm C: Paclitaxel 80 mg/m2 weekly for 12 weeks ? FE75C q 21 X 4 courses plus trastuzumab 4 mg/kg loading dose followed by 2mg/kg weekly plus Lapatinib 1000 mg po daily
Lapatinib and trastuzumab administration will start on the same day of the 1st infusion of CT, will continue throughout all the duration of the treatment and will be discontinued 1 week before surgery
50. EGF109077/LET-LOB�STUDY DESIGN
51. BIOMARKER EVALUATION The following biomarkers will be evaluated, to define the inhibition of the down-stream pathways of EGFR-family:
- EGFR, HER2
- pTEN, pAKT, pMAPK
- Apoptosis with TUNEL Test
- Ki 67
These parameters will be evaluated by IHC, on paraffin-embedded specimens obtained from diagnostic core biopsy of the primary lesion and from surgical specimens.
Fresh tumor tissue from core-biopsy must be snap frozen, to perform a microarray analysis of the gene expression profile before treatment and to evaluate its correlation with response.
53. Molecular subtypes of breast cancer and clinical management Her2+ represents a distinct molecular subtype
Her2+ tumors have a unique clinical behaviour (shorter DFI, more visceral and CNS metastases)
Her2 + tumors exhibit a peculiar pattern of sensitivity to chemo and hormonal therapy
Her2 targeting agents have dramatically changed the course of this disease and represent now the foundation of treatment in early and advanced disease
