Post on 18-Dec-2020
Antonino Musolino
Breast Unit Interaziendale
Provincia di Parma
La Ricerca Clinica e Traslazionale
Breast Cancer Subtypes
Perou et al. Nature 2000
Sorlie et al. PNAS 2001
Luminal A
Luminal B
Basal-Like
HER2+
ER+ 65-75%
ER- 15%
ER- 15-20%
Carcinoma mammario ER/PR+
(Luminal)
BIG 1-98 and ATAC Trials
20
15
10
5
0
Per
cen
t w
ith
ev
ent
1 2 3 4 5
8.1%
6.2%
13.6%
10.2%
Years
HR 95%CI P value
Let vs. Tam 0.81 .70-.93 0.0002
Letrozole
Tamoxifen
0 1 2 3 4 5 6
P value
0.005HR
0.83A vs T
95% CI
(0.73–0.94)
:
Years
0
5
10
15
20
25
Absolute
difference:1.6% 2.6% 2.5% 3.3%
Tamoxifen
Anastrozole
Slide 12
EBCTCG, NEJM 2017
EBCTCG metanalysis on long-term recurrence risk after 5yrs of ET
N=91 trials from individual ER9+ pts allocated to 5 yrs of ETN= 46000 pts still alive and disease-free after 5 yrs
Cooperation between ER and Cyclic D1 pathways enhances proliferation in luminal breast cancer
Cyclin D1
CDK4-6
ER
p RbInhibitory controlInhibitory control
Cell Cycle:
G1 S
proliferation
Inhibitors:
-Palbociclib
-Abemaciclib
-Ribociclib
-CDKN2A/p16
Hortobagyi GN, Ann Oncol 2018
MONALEESA-2: Progression-free Survival
Carcinoma mammario Triplo-negativo
(Basal-like)
Triple Negative Breast Cancer
• Some commonly
encountered features
• More frequent at youger age
• More frequent in black ethnicity
• Almost always High-Grade
• Often p53 positive
• Highly proliferative
• Often N0
• Poor prognosis
• Some unusual histologies are TN and
carry a better prognosis– Medullary
– Aprocrine
– Low grade adeno-squamous
– Low grade spindle cell
• BRCA1-mutated often display this
phenotype
• BRCA1 dysfunctional tumors often
display this phenotype
ERHER2
PgR
Immunohistochemistry
Hazard Functions for Disease Progression Among Patients with TNBC vs. non-TNBC
Liedtke et al. J Clin Oncol 2008
Triple
Negative
Basal
~75% of TNBC have
Basal gene
expression
1. Pal & Mortimer. Maturitas 2009
2. Gluz et al. Ann Oncol 2009
3. Anders & Carey. Oncology 2008
4. Young et al. BMC Cancer 2009
5. Schneider, B. P. et al. Clin Cancer Res 2008
Triple-Negative vs. Basal-Like: Definitions
ER- / PR- / HER2-
~15% of all breast carcinomas
Poorly differentiated
Express CK 5/6, 17, EGFR (+)
• BRCA1-2 mutated tumors
•~5% of Breast Cancer
• 50% BRCA-1 carriers are basal-like
• Basal but not triple negative
• Definition by gene expression
• Includes most BRCA1 mutated tumors
• 15-40% are ER+, PR+ or HER2+
• Triple negative but not basal
• Definition by IHC
• Includes other histologies(medullar, adenoid cystic)
• 10-30% can also include “claudin-low,” a subtype notable for high expression of stem cell markers
• 90% of TNBC do not have BRCA mutations
BRCA 1-2
Cortesi L., Current Cancer Drug Targets 2018
Primary endpoint: progression-free survival by BICR
Slide 8
Slide 9
Slide 10
Carcinoma mammario HER2+
Carcinoma mammario HER2-positivo
•Targets HER2 protein
•High affinity (Kd = 0.1 nM) and
specificity
•95% human, 5% murine
– Decreases potential
for immunogenicity
– Increases potential for
recruiting immune effector
mechanisms
HER2 epitopes recognized by hypervariable
murine
antibody fragment
Human
IgG-1
Trastuzumab:Humanized Anti-HER2 Antibody
Antibody Dependent Cell Mediated Cytotoxicity (ADCC)
HER2 Targeting With Trastuzumab And the Natural History of HER2-Positive Advanced Breast Cancer
Dawood S., et al. J Clin Oncol. 2009
Disease-free Survival
87%85%
67%
75%
N EventsAC T 1679 261AC TH 1672 134
%
HR=0.48, 2P=3x10-12
AC TH
AC T
Years From Randomization B31/N9831
First-in-human, phase I Study of Margetuximab, an Fc-optimized Chimeric mAb, in pts with HER2+ solid tumors
Burris, et al. ASCO 2015 #523
Trastuzumab continually
suppresses HER2 activity
Flags cells for destruction
by the immune system
• Activates ADCC
Trastuzumab and Pertuzumab Bind to Different Regions on HER2 and Have Synergistic Activity
Pertuzumab inhibits HER2 forming
dimer pairs
Suppresses multiple HER signaling
pathways
Flags cells for destruction
by the immune system
• Activates ADCC
HER2 receptor
TrastuzumabPertuzumab
Subdomain IV of HER2
Dimerization domain of HER2
Trastuzumab IV (8 mg/kg loading dose,
followed by 6 mg/kg) plus
Pertuzumab IV (840 mg loading dose,
followed by 420 mg) plus
Docetaxel IV (75→100 mg/m2),
every 3 weeks for 4 cycles
Eligibility (n 63)
Women with histologically
confirmed HER2-positive breast
cancer with locally advanced,
inflammatory, or early stage
tumor (either greater than 2 cm
in diameter or node positive)
with no evidence of metastatic
disease
Randomized Phase IIb Biomarker Study of Immune-mediated Mechanism of Action of Neoadjuvant Trastuzumab (either iv or sc) in Patients with HER2-
positive Breast Cancer (ImmunHER)
R
Pre-randomization phase:
FEC (5FU 500; epirubicin 75;
CTX 500) x 3 cycles
Trastuzumab SC
(fixed dose of 600 mg) plus
Pertuzumab IV (840 mg loading dose,
followed by 420 mg) plus
Docetaxel IV (75→100 mg/m2),
every 3 weeks for 4 cycles
Primary endpoint:
TIL rate on residual disease after either IV trastuzumab or
SC trastuzumab
Primary Objective:
To evaluate variations of host immune response
parameters to either trastuzumab SC or trastuzumab IV
given in combination with pertuzumab and chemotherapy.st
cancer.
Hallmarks of Cancer
Hanahan et al. Cell 2011
Una singola freccia si rompe facilmente, ma non
dieci frecce tenute assieme – Proverbio
giapponese
Email: breast-unit@ao.pr.it
Segreteria: 0521/702316