1. New Perspectives in Cancer Therapy
Óren Smaletz
Programa de Oncologia
Hospital Israelita Albert Einstein
2. Disclosure of Potential Conflicts of Interest Honoraria: Pfizer, Merck KGaA
Research Funding: Pfizer
Scientific Funding: Merck KGaA, Roche
3. A 72-year-old man presented for evaluation of progressive dyspnea and cough. He reported smoking one to two packs of cigarettes a day since the age of 15 years. Standard chest radiography showed a suspicious lesion in the right thoracic cavity. Computed tomography of his chest revealed bullous emphysema (thick arrow), a tumor involving the middle lobe of the right lung (thin arrow), and a pack of cigarettes in his shirt pocket (asterisk). Biopsy of the lesion confirmed the presence of non-small-cell lung cancer.A 72-year-old man presented for evaluation of progressive dyspnea and cough. He reported smoking one to two packs of cigarettes a day since the age of 15 years. Standard chest radiography showed a suspicious lesion in the right thoracic cavity. Computed tomography of his chest revealed bullous emphysema (thick arrow), a tumor involving the middle lobe of the right lung (thin arrow), and a pack of cigarettes in his shirt pocket (asterisk). Biopsy of the lesion confirmed the presence of non-small-cell lung cancer.
4. Change in the US Death Rates* by Cause, �1950 & 2002 Compared to the rate in 1950, the cancer death rate was about the same in 2002, while rates for other major chronic diseases decreased during this period. Compared to the rate in 1950, the cancer death rate was about the same in 2002, while rates for other major chronic diseases decreased during this period.
5. Fight Against Cancer Surgery
Radiotherapy
Chemotherapy
Targeted Therapy Agents
6. FDA Approved New Molecules for Solid Tumor Use per Year
8. Hanahan D, Cell 2000
9. The EGFR (erbB) Family and Ligands The EGFR family consists of four members, HER1/erbB-1 through HER4/erbB-4. They all share the same structure – an extracellular domain that interacts with specific ligands, a short transmembrane domain and a tyrosine kinase domain within the cell, which is the activator of downstream signaling. Each receptor has some homology with the others but they vary in terms of ligand binding and tyrosine kinase activity.The EGFR family consists of four members, HER1/erbB-1 through HER4/erbB-4. They all share the same structure – an extracellular domain that interacts with specific ligands, a short transmembrane domain and a tyrosine kinase domain within the cell, which is the activator of downstream signaling. Each receptor has some homology with the others but they vary in terms of ligand binding and tyrosine kinase activity.
10. Família EGFR (Her)
11. Trastuzumab – mecanismo de ação
12. Trastuzumab in Breast Cancer
13. Trastuzumab – metastatic breast cancer
14. Trastuzumab – metastatic breast cancer
15. Trastuzumab – adjuvant treatment
16. Trastuzumab – adjuvant treatment
17. EGFR Signaling Pathways
18. EGFR Expression in Human Cancer Overexpression associated with:
Invasion
Metastasis
Advanced disease
Poor outcome
Resistance to chemotherapy, hormonotherapy radiotherapy
EGFR is generally expressed in a wide range of human solid tumors. Expression is very variable due to the different detection assays used, since there is no standardized method of measuring EGFR expression.EGFR is generally expressed in a wide range of human solid tumors. Expression is very variable due to the different detection assays used, since there is no standardized method of measuring EGFR expression.
19. Disease-free Survival and EGFR and �TGF-a Levels in Head and Neck Cancer
20. EGFR Mab Currently Approved
21. Cetuximab (Erbitux®) IgG1 (chimerized antibody)
Exclusive for EGFR and its heterodimers
Prevents ligand binding to EGFR
High affinity. Kd = 0.39 nM �(M-225 Kd = 1 nM)
1 log > natural ligand
Stimulates receptor internalization
Blocks receptor dimerization, tyrosine kinase phosphorylation, signal transduction
M225, a murine monoclonal antibody, competitively binds to the EGFR and inhibits EGFR pathways. Clinical trials using murine monoclonal antibodies have been complicated by the development of the human antimouse antibody (HAMA) immune response. The HAMA response not only carries the risk of serious allergic reactions but also increases the clearance of the murine proteins. Thus, the clinical utility of murine monoclonal antibodies has been limited.
Cetuximab is a human:murine chimeric anti-EGFR IgG monoclonal antibody that binds exclusively to the EGFR. Chimeric antibodies are composed of the variable regions of murine antibody (the regions responsible for antigen binding) and the constant region of the human Fc fragment.[1] Chimeric monoclonal antibodies have demonstrated specificity and a diminished incidence of immunologic reactions.[2,3]
Cetuximab binds to the EGFR with a binding affinity that is approximately one log higher than natural ligands.[4] Cetuximab prevents binding of endogenous ligands and induces receptor internalization, which ultimately blocks the activities of the EGFR pathway.
Owens RJ, Young RJ. The genetic engineering of monoclonal antibodies. J Immunol Methods 1994; 168:149–165.
Shitara K, Kuwana Y, Nakamura K, et al. A mouse/human chimeric anti-(ganglioside GD3) antibody with enhanced tumor activities. Cancer Immunol Immunother. 1993; 36:373–380.
LoBuglio AF, Wheeler RH, Trang J, et al. Mouse/human chimeric monoclonal antibody in man: kinetics and immune response. Proc Natl Acad Sci U S A. 1989; 86:4220–4224.
Goldstein NI, Prewett M, Zuklys K, et al. Biological efficacy of a chimeric antibody to the epidermal growth factor receptor in a human tumor xenograft model. Clin Cancer Res. 1995; 1:1311–1318.M225, a murine monoclonal antibody, competitively binds to the EGFR and inhibits EGFR pathways. Clinical trials using murine monoclonal antibodies have been complicated by the development of the human antimouse antibody (HAMA) immune response. The HAMA response not only carries the risk of serious allergic reactions but also increases the clearance of the murine proteins. Thus, the clinical utility of murine monoclonal antibodies has been limited.
Cetuximab is a human:murine chimeric anti-EGFR IgG monoclonal antibody that binds exclusively to the EGFR. Chimeric antibodies are composed of the variable regions of murine antibody (the regions responsible for antigen binding) and the constant region of the human Fc fragment.[1] Chimeric monoclonal antibodies have demonstrated specificity and a diminished incidence of immunologic reactions.[2,3]
Cetuximab binds to the EGFR with a binding affinity that is approximately one log higher than natural ligands.[4] Cetuximab prevents binding of endogenous ligands and induces receptor internalization, which ultimately blocks the activities of the EGFR pathway.
Owens RJ, Young RJ. The genetic engineering of monoclonal antibodies. J Immunol Methods 1994; 168:149–165.
Shitara K, Kuwana Y, Nakamura K, et al. A mouse/human chimeric anti-(ganglioside GD3) antibody with enhanced tumor activities. Cancer Immunol Immunother. 1993; 36:373–380.
LoBuglio AF, Wheeler RH, Trang J, et al. Mouse/human chimeric monoclonal antibody in man: kinetics and immune response. Proc Natl Acad Sci U S A. 1989; 86:4220–4224.
Goldstein NI, Prewett M, Zuklys K, et al. Biological efficacy of a chimeric antibody to the epidermal growth factor receptor in a human tumor xenograft model. Clin Cancer Res. 1995; 1:1311–1318.
22. Panitumumab (Vectibix®) fully human IgG2? mAb
high affinity (Kd ~ 0.05 nM)
Upon binding, internalized and donwregulates EGFR
Prevents
receptor dimerization
EGFR-tyrosine autophosphorylation
activation of downstream signaling molecules
23. Mechanism of Action of anti-EGFR �Monoclonal Antibodies This and the next slide show simple examples of the difference in mechanism of action between moAbs and TKIs.
In this slide it is shown that ligand binding is blocked by an anti-EGFR moAb. The moAb-EGFR is internalized, but cannot signal within the cell. In this way, the signal transduction cascade is blocked.
With a moAb such as cetuximab, ligand activation of the receptor, and therefore intracellular signaling, are blocked.This and the next slide show simple examples of the difference in mechanism of action between moAbs and TKIs.
In this slide it is shown that ligand binding is blocked by an anti-EGFR moAb. The moAb-EGFR is internalized, but cannot signal within the cell. In this way, the signal transduction cascade is blocked.
With a moAb such as cetuximab, ligand activation of the receptor, and therefore intracellular signaling, are blocked.
24. Cetuximab in Colorectal Cancer�(“Bond Trial”) Eligibility criteria
Pretreated metastatic colorectal cancer with irinotecan
All patients had to be EGF-R positive
Primary end-point
Tumor response
25. Cetuximab in Colorectal Cancer (“Bond Trial”)
28. Cetuximab in Colorectal Cancer (“Bond Trial”)
30. Panitumumab in Colon/Rectal Cancer
31. Panitumumab vs. BSC
33. Panitumumab vs. BSC
35. EGFR and K-RAS K-RAS mutation present in 40-45% patients
When K-ras gene is mutated, K-ras protein (p21 ras) is active independently of EGFR activation
36. K-RAS mutation detection PCR test for mutation in codons 12 and 13 kras
39. Take Home Message Moleculat Targeted Therapy – showtime
Benefit is evident – as well as costs
Who should receive? – Clinical oncology os meeting science
40. Thank you
osmaletz@einstein.br
