targeted agents in breast cancer: examining advances in management of breast cancer - dr. peter...
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Targeted Agents In Breast Cancer
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Wonderful Music With New Instruments
Peter M Ravdin, MD, PhD
San Antonio, Texas
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Trends In Cancer Mortality In Women in US At This Rate We Will Beat Breast Cancer In 2040
Is the cause screening ??
Is the cause better therapy ??
Probably some of both.
Not yet prevention.
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Targeted Agents In Breast Cancer
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Accelerated Progress
1. Its expression is only found to a limited extent in
normal adult tissues
2. Its expression in cancer correlates with its anti-
cancer effects.
3. It can be combined with other agents without
unexpected toxicity
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Targeted Agents In Breast Cancer
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Why All The Excitement Now
1. Knowledge about metabolic, signalling, and
control pathways is advancing
2. Methodologies for detecting and quantitating
macromolecules are improving
3. Methods for screening large libraries of compounds
are maturing.
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Targets In Breast Cancer
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The Estrogen Receptor.
ER (Discovery late 1970s)
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Targets In Breast Cancer
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The Grandmother of Them All
The Estrogen Receptor.
Restricted expression in tissues in the adult.
Toxicity issues: Expression in endometrium
Expression in bone
Expression in CNS
Methodologies for detecting
Still an issue
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Targets In Breast Cancer
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Tamoxifen: An Agent Targeting The
Estrogen Receptor.
Useful In
Metastatic Disease 50 % RR
Adjuvant Therapy 40 % HR
Prevention 40 % RR
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Targets In Breast Cancer
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Tamoxifen Effects Are Long Term
45 % 32 % 7%
Relapse Reductions
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Targets In Breast Cancer
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HER2
(Discovery late 1980s)
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Targets Agents In Breast Cancer
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Second Major Target
Her2
Restricted expression in the adult
Expression in heart ?
Methodologies for detecting
Still an issue
In adjuvant therapy do Her2
“negative“ cases respond
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NSABP B-47 Chemotherapy With or Without Trastuzumab After Surgery in Treating
Women With Invasive Breast Cancer
Groups: Arm 1. DC q3w * 6
Arm 2. AC qw2 or 3w * 4 then P qw * 12
Arm 3. DC and Trastuzumab q3w * 6 and then Tras. q3w * 11
Arm 4. AC qw2 or 3w * 4 then P and Tras. qw * 12 then Tras . Q3w * 12
Eligibility
1. HER2 0 or 1 by IHC. If Her2 = 2, FISH negative. If Her2 = 3 ineligible
2. Node positive. If Node Negative. N0 with ER/PgR negative or Grade 3
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Targets/Agents In Breast Cancer
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Active Classes (1990‘s)
HER2-targeted agents
Pertuzumab and trastuzumab-maytansine immunoconjugate)
VEGF-targeted agents aflibercept
anti-VEGF monoclonal antibody bevacizumab
Dual EGFR/HER2-targeted agents
afatinib [BIBW 2992] and neratinib,
Multitargeted tyrosine kinase inhibitors
sunitinib, pazopanib
Mammalian target of rapamycin (mTOR)
everolimus
Poly (ADPribose) polymerase 1 inhibitors
iniparib, olaparib.
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Targets In Breast Cancer
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Development of A New Agent
Metastatic Disease
NeoAdjuvant Therapy
Adjuvant Therapy
Prevention
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Adjuvant Treatment: What Is Involved ? Lots of variations but this is a common way.
Chemotherapy: 3-6 months
Unacceptable risk of dying of cancer
Tolerable, but obnoxious.
Hormone therapy: 5 years
Only if ER (estrogen receptor positive
Usually low toxicity pills.
Biological Therapy: 1 year
Only if Her2 positive
Usually low toxicity antibodies.
Radiation: 4-6 weeks
High risk of local recurrence
Inconvenient, bothersome.
XRT
Chemo
Bio
Hormone
Time (yrs)
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PFS Results in MBC of A Trial
Letrozole + Lapatinib vs Letrozole
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OS Results of A Trial
Letrozole + Lapatinib vs Letrozole
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QOL Results of A Trial
Letrozole + Lapatinib vs Letrozole
10% of the L + L patients had Grade 3 / 4 diarrhea
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AI’s +/- Everolimus
Exemestane + Everolimus (Pending)
Exemestane
Letrozole + Everolimus (Better Response)
More Toxicity
Letrozole Gr 3/4 23 % vs 4 %)
Neoadjuvant Study
1st Line MBC Study
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Bisphosphonates ? !
Not really a
Specifically Targeted Agents
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Can Zoledronic Acid (An Osteoporosis Treatment) Improve Outcomes?
Inhibition of Multiple Steps in Tumor Cell Metastasis
Adapted from Mundy GR, et al. Nat Rev Cancer. 2002;2:584-593.
Invasion Angiogenesis Primary tumor
Metastases Adhesion &
extravasation Arrest in distant
capillary
Micrometastases
Inhibits
angiogenesis
Decreases
adhesion to bone
Synergy with
anticancer drugs
Induces
tumor cell
apoptosis
Stimulates immune
surveillance
Decreases
matrix invasion
20
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Austrian BC Study Group 12 Trial
Design Results Presented in 2008
• Accrual 1999-2006
• 1,803 premenopausal breast cancer patients
• Endocrine-responsive (ER and/or PR positive)
• Stage I&II, <10 positive nodes
• No chemotherapy except neoadjuvant
• Treatment duration: 3 years
21
Randomize
1 : 1 : 1: 1
Surgery
(+RT)
Tamoxifen 20 mg/d
Goserelin
3.6 mg q28d
Anastrozole 1 mg/d
+ Zoledronic acid 4 mg q6m
Anastrozole 1 mg/d
Tamoxifen 20 mg/d
+ Zoledronic acid 4 mg q6m
Endocrine Neoadjuvant
Therapy
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Secondary Endpoints: ZOL vs No ZOL
RFS OS
22
100
90
80
70
60
50
40
30
20
10
0 0 12 24 36 48 60 72 84
Time since randomization, months
Ove
rall
surv
ival
, %
No. of Hazard ratio (95% CI) events vs No ZOL P value
ZOL 16 0.595 (0.32 to 1.11) .101
No ZOL 26
100
90
80
70
60
50
40
30
20
10
0 0 12 24 36 48 60 72 84
Time since randomization, months
Rec
urr
ence
-fre
e su
rviv
al, %
No. of Hazard ratio (95% CI) events vs No ZOL P value
ZOL 54 0.653 (0.46 to 0.92) .014
No ZOL 82
Relative Reduction of Relapse
35 % ! Relative Reduction of Death
40 % !
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AZURE: Study Design
Standard therapy
Standard therapy +
Zoledronic acid 4 mg
3,360
patients
Stage II/III
Treatment duration 5 years
Accrual September 2003 - February 2006
R
174 centres • UK (123 centres; 2710 patients) • Eire (10 ; 247) • Australia (28 ; 226) • Spain (8 ; 107) • Portugal (1 ; 32)
• Thailand (2 ; 25) • Taiwan (2 ; 13)
6 doses 8 doses 5 doses
Q3-4 weeks Q 3 months Q 6 months
6 30 60
Months
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AZURE: Disease Free Survival
NO EFFECT ! BIG SURPRISE
1 2 3 4 5 6 7
20
40
60
80
TIME (YEARS)
Zoledronic acid: N= 1681
No. at risk:
1681 1591 1465 1354 1243 580 83
1678 1583 1445 1344 1252 561 71
Control: N= 1678
Adjusted HR = 0.98 95% CI [0.85,1.13] p=0.79
100
0
%
%
ZOL:
CONT: CONT:
0
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AZURE: Overall Survival by Menopausal Status
1 2 3 4 5 6 7
20
40
60
80
TIME (YEARS)
Zoledronic acid N= 1131 Control N= 1127
Adjusted HR = 1.01 95% CI [0.81,1.26] p=0.93 157 vs 156 deaths
Premenopausal
% Surviving
100
0 0 1 2 3 4 5 6 7
20
40
60
80
TIME (YEARS)
Zoledronic acid N= 550 Control N= 551
Adjusted HR = 0.71 95% CI [0.54,0.94] p=0.017 86 vs 120 deaths
Postmenopausal
0 0
29% Decrease in Deaths No Difference in Deaths
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There Are Many Promising Ideas
Some of these will be good