Neoadjuvant Breast Cancer

Question 1

Why would we consider neoadjuvant therapy?

Answer 1

1) Survival outcomes are equal
Neoadjuvant = adjuvant

2) Improved tumor down-staging
- Converts inoperable to operable (LABC)
- Mastectomy to breast conserving (Primary operable Breast CA/Subset LABC)

3) Provides opportunity to assess surrogate biological end-points
4) May expedite new drug development
5) Provides in Vivo assessment of anti-tumor effects
6) Early initiation of systemic therapy

Question 2

What is the evidence showing neoadjuvant = adjuvant ?

Answer 2

1) NSABP B18
Using AC pre- vs post-op
- 16yOS: 55% vs 55%
- 16y DFS 42% vs 39%
- pCR 13%
- BCS 68% vs 60%

2) NSABP B27: AC–> S vs AC–> T–>S vs AC–>S–>T
- 8yOS 74% vs 75%
- 8yDFS 59% vs62%
- pCR 14% vs 26% (without or with Taxanes)

3) Meta-analyses
- Mauri JNCI
- Mielog Cochrane

Question 3

What is considered pCR?

Answer 3

• ypT0 ypN0
• ypT0/is ypN0
• ypT0

Question 4

What are the strongest association between pCR and long-term clinical outcome?

Answer 4

1) ER-/Her2+
2) Triple negative
3) High grade ER+/Her2-

Question 5

What does pCR assess?

Answer 5

pCR assess treatment given pre-operatively and not post-operatively

Question 6

Who are the candidates for BCS after neo-adjuvant chemotherapy?

Answer 6

1) Unifocal disease
2) No skin changes
3) Imaging abnormalities resectable with lumpectomy
4) Candidate for radiotherapy
5) Accepting of increased local recurrence rate
6) No metastatic disease

Question 7

What are the factors resulting in poorer outcome after neoadjuvant therapy?

Answer 7

1) Advanced disease before treatment
2) Poor clinical response to chemotherapy
3) Axillary nodal status after chemotherapy.
- must achieve both ypT0N0

Question 8

Tell me about the mechanisms of action for Trastuzumab

Answer 8

Acts extracellularly
on the sub domain IV of HER2

Does not inhibit HER2 dimerisation, thus blocking HER2:HER3

Prevents HER2 receptor shedding

Blocks HER2 signaling and elicits ADCC

Question 9

What is the MoA for Pertuzumab?

Answer 9

Works extra-cellularly
Works on the dimerisation domain of HER2

Inhibits HER2 forming of dimmer pairs
Activates ADCC
Does not prevent HER2 receptor shedding

Question 10

What is the MoA of Lapatinib?

Answer 10

Works on the intracellular kinase domain of HER2

Induces HER2 accumulation at Cell surface, stabilizing inactive HER2 homodimers and heterodimers

Accumulation of HER2 enhances Trastuzumab-dependent cytotoxicity

Question 11

What is the evidence that Herceptin is necessary to achieve better pCR in Her2+ patients in the neoadjuvant setting?

Answer 11

(A) MD Anderson Study
(B) NOAH study
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(A) MD Anderson Study
Buzdar Clin Cancer Res 2007

Breast cancer patients n=40
HER2+
M0, T1-3, N0-1

2arms:

1) 4# Paclitaxel Q3w –> 4#FEC
2) 4# Paclitaxel Q3w + 12#Herceptin –> 4#FEC + 12#Herceptin

RESULTS:
1) pCR with inclusion of Trastuzumab is almost 3x that without.
66% vs 26%

==============
(B) NOAH Study
Gianni Lancet 2010
N=300

Divided into Her2+ LABC and Her2- LABC
3 arms:
(1) HER2+ = 3#(H+AT)q3w –> 4#(H+T)q3w –> 4#Hq3w + 3#CMF q4w –> Surgery–>RT–>Hq3w until week 52
(2) HER2+ = 3#AT q3w –> 4#T q3w –> 3#CMF q4w –> Sx–>RT
(3) HER2- = 3#AT q3w –> 4#T q3w –> 3#CMF q4w –> Sx–> RT

RESULTS:

1) pCR rates with Herceptin : Without Herceptin = 40% : 20%
2) EFS HR 0.60 in favor of Herceptin

Question 12

What are the Anti-Her2 Neoadjuvant trials?

Answer 12

1) NeoSphere (n=400)
4arms:
(A) Trastuzumab + Docetaxel
(B) Pertuzumab + Docetaxel
(C) Pertuzumab + Trastuzumab + Docetaxel 
(D) Pertuzumab + Trastuzumab

2) Neo-ALTTO (n=450)
3 arms:
(A) Trastuzumab –> Trastuzumab+Paclitaxel
(B) Lapatinib –> Lapatinib+Paclitaxel
(C) Trastuzumab/Lapatinib –> Trastuzumab/Lapatnib + Paclitaxel

3) GeparQuinto (n=600)
2arms:
(A) Epirubicin + Cyclophosphamide + Trastuzumab –> Docetaxel +Trastuzumab + GCSF
(B) Epirubicin + Cyclophosphamide + Lapatinib –> Docetaxel + Lapatinib + GCSF

Question 13

Tell me about the NeoSphere study

Answer 13

Gianni SABCS 2010

N=400
Operable/LABC/inflammatory Her2+ breast cancer
Chemo-naive, primary tumor >2cm

4 arms:

1) Docetaxel/Trastuzumab –> op –> FEC/Trastuzumab
2) Docetaxel/Trastuzumab/Pertuzumab –> op –> FEC/Trastuzumab
3) Trastuzumab/Pertuzumab – op –> Docetaxel–>FEC/Trastuzumab
4) Docetaxel/Pertuzumab –> op –> FEC/Trastuzumab

RESULTS:
1) pCR: 
= THP> TH> TP> HP
- TH = 30%
- THP = 45%
- HP = 15%
- TP = 25%

Question 14

Tell me about the Neo-ALTTO trial

Answer 14

Jose Baselga 2010

Invasive operable Her2+ Breast Cancer
T>2cm, excluded inflammatory breast cancer
EF>50%
N=450

3arms:
1) 6w Lapatinib–>12w Lapatinib+Paclitaxel–>op–>3#FEC–>Lap
2) 6w Trastuzumab–>12w Trastuzumab+Pac–>op–>3#FEC–>Trast
3) 6w Lap/Trast –>12w Lap/Trast/Pac –>op–>3#FEC–>Lap/Trast

RESULTS:
1) pCR by Hormonal receptor status
(A) HR +
- Lap: 15%
- Trast: 20%
- Lap+Trast: 40% 
(B) HR -
- Lap: 35%
- Trast: 35%
- Lap+Trast: 60%

Question 15

Tell me about GeparSixto

Answer 15

Minckwitz Lancet Oncol 2014
N=300
TNBC

2 arms:

1) 18# Weekly Pac/Doxo + 6# Bev Q3w –> Surgery
2) 18# Weekly Pac/Doxo/Carboplatin + 6#Bev Q3w –> Surgery

RESULTS:
- pCR Rates PMCb>PM = 50+% vs 30+%

Question 16

What about CALGB 40603 ? The other trial for neoadjuvant TNBC?

Answer 16

CALGB 40603 SABC 2014
Sikov JCO 2014

N=400
2x2 factorial design
1) 12# weekly Pac –> 4# ddAC
2) 12# Weekly Pac/Bev Q2w –> 4#ddAC/BevQ2w
3) 12# weekly Pac/4# CarboQ3w —> 4#ddAC
4) 12# weekly Pac/4#CarboQ3w/BevQ2w–> 4#ddAC/BevQ2w

RESULTS:

1) pCR by No Bev vs Bev = 50% vs 60%
2) pCR by no Carbo vs Carbo = 45% vs 60%

Question 17

Between Letrozole and Tamoxifen as Neoadjuvant endocrine therapy, which is better?

Answer 17

Letrozole.

P024 trial
n=300
Ineligible for BCS 
2 arms:
- Letrozole vs Tamoxifen
- 4 months therapy 

RESULTS:
Higher ORR with Letrozole 55% vs 30%
Higher rate of BCS with Letrozole 45% vs 35%

Question 18

What are the risk factors for breast cancer?

Answer 18

Genetic predisposition
Exposure to estrogens (endogenous and exogenous)
Ionizing radiation
Low parity
Hx of atypical hyperplasia
Western-style diet
Obesity
Alcohol

Question 19

What are the risk factors for breast cancer in males?

How common?

Answer 19

~1%
Clinic disorders carrying hormonal imbalances 
- Gynaecomastia
- Cirrhosis
Radiation exposure
Family Hx
Genetic predisposition

Question 20

When is BCS not possible?

Answer 20

Tumor size (relative to breast size)
Tumor multicentricity
Inability to achieve negative surgical margins after multiple resections
Prior RT to chest wall/breast 
Other contraindications to RT
Patient choice

Question 21

If a sentinel LN has Micromets (0.2-2m), is further Axillary treatment required?

Answer 21

Based on IBCSG 23-01, no.

Question 22

Why is post-op RT strongly recommended after BCS?

Answer 22

WBRT alone reduces:
- the 10-year risk of any 1st recurrence by 15%
» including locoregional and distant
- 15y risk of breast cancer-related mortality by 4%

Boost irradiation gives a further 50% RR reduction.

Question 23

When is boost irradiation indicated?

Answer 23

Unfavorable risk factors for local control. Eg:

- Age

Question 24

Why is radiation after mastectomy important in N+ patients?

Answer 24

Reduces:

• 10y recurrence risk (anywhere) by 10%
• 20y risk of breast-cancer-related mortality by 8%

Should now consider routine use of PMRT for those with 1-3 LN + as well as the benefits of PMRT are independent from the no. Of involved Axillary LN and chemo.

Question 25

What is the usual RT schedule ?

Answer 25

45-50Gy in 25-28# of 1.8-2Gy each

Typical boost dose of 10-16Gy in 2Gy single doses

Question 26

Define ER positivity

Answer 26

1% or more of invasive cancer cells

Question 27

Name me a breast tumor marker that can suggest tumor invasiveness

Answer 27

uPA-PAI1