enfermedad avanzada ¿qué hacemos con el triple negativo? · ¿qué hacemos con el triple...

ENFERMEDAD AVANZADA

¿Qué hacemos con el triple negativo?

Nuevas aproximaciones

Javier Cortes,

Hospital Universitario Ramon y Cajal, Madrid

Vall d´Hebron Institute of Oncology (VHIO), Barcelona

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“Triple Negative” Breast Cancer

PR HER2 • ER and PR <1%

nuclear

• HER2 “negative”:

IHC 0 or 1+

staining or 2+ IHC

staining with

negative FISH

ER

Histology

Immunohistochemistry

• High grade ductal

Poor Outcome of Metastatic TNBC

(N=112)

Kassam F, Enright K, Dent et al. Clin Breast Cancer 2009

Initial

therapy

First distant

relapse

First

line

chemo

Median D.F.I.

Second

line

chemo

Third

line

chemo

“Time on Treatment”

4 weeks 9 weeks 12 weeks

What is ‘Standard Therapy’ For TNBC?

• No specific systemic regimen guidelines exist

• Little data on which to base decisions

• Few historical controls making it challenging to

design clinical trials for this subgroup

TNBC: Current Treatment Strategies

Anthracyclines Taxanes

Capecitabine Platinum agents

Biologic agents

• TNBC paradox: chemo-

sensitive…but relapse more

aggressive with worse OS

• Cannot treat with existing

targeted therapies (hormonal

therapy or trastuzumab)

• Manage same as other BCs

with same grade & stage

• Limited data available from

prospective trials in this

population

• Best available data mostly

subpopulation analyses

CMTN: Antraciclinas vs. Docetaxel

CMTN HER2 Luminal B

Docetaxel 100

mg/m2 x 4 ciclos 29 33 14

Doxorrubicin 75

mg/m2 x 4 ciclos 10 55 16

Single agent Neoadjuvant Chemotherapy study with Doxorubicin or

Docetaxel for 4 cycles in Stage II-IIIa (> 3 cm)

pCR rate by phenotype

Martin et al, ASCO 2009

Taxanes For Metastatic TNBC?

Trial Phase N Setting Taxane Outcome in TNBC

CALGB 93421

III

44 First- or second-line metastatic

Paclitaxel weekly and q3w

ORR = 26% TTF = 2.8 months OS = 8.6 months

ECOG 21002 III

110 First-line metastatic

Paclitaxel weekly

ORR = 11.7%4

PFS = 5.3 months

AVADO3 III

52 First-line metastatic

Docetaxel q3w

ORR = 23.1%

PFS = 6.1 months

1. Harris, et al. Br Cancer Res 2006

2. O’Shaughnessy, et al. SABCS 2009

3. Glaspy, et al. EBCC 2010

Retrospective subgroup analyses

Placebo arm data

Capecitabine For Metastatic TNBC?

Trial Phase N Setting Treatment Outcome in TNBC

Pooled analysis1 III 208 Third-line or greater metastatic

Capecitabine ORR = 15% PFS = 1.7 months

RIBBON-12 III 50 First-line metastatic

Capecitabine + placebo

ORR = 24%

PFS = 4.2 months

1. Rugo, et al. SABCS 2008

2. Glaspy, et al. EBCC 2010

Retrospective subgroup analyses

Placebo arm data

TNT: Carboplatin vs Docetaxel in

Advanced TNBC or BRCA1/2+ BC

• Primary endpoint: ORR in ITT population

• Secondary endpoints: PFS, OS, ORR (crossover), toxicity

• Subgroup analyses: BRCA1/2 mutation, basal-like subgroups,

HRD biomarkers

Tutt A, et al. SABCS 2014

Patients with ER-,

PgR-/unknown, and

HER2- or BRCA1/2+

metastatic or

recurrent LA BC

(N = 376)

Carboplatin AUC6 q3w

x 6 cycles (n = 188)

Docetaxel 100 mg/m2 q3w

x 6 cycles ( n = 188)

For both arms, crossover upon progression allowed

Carboplatin vs Docetaxel in Advanced

TNBC or BRCA1/2+ BC (TNT): ORR

0

10

20

30

40

50

60

70

80

90

Response a

t C

ycle

3 o

r 6 (

%)

All Pts (n = 376)

C→D D→C Crossover*

(All pts; n = 182)

BRCA1/2 Mutation (n = 43)

No BRCA1/2 Mutation (n = 273)

31.4% 35.6%

22.8% 25.6%

P = .44

P = .73

68.0%

33.3%

P = .03

28.1%

36.6%

P = .16

Carboplatin

Docetaxel

Crossover


Carboplatin vs Docetaxel in Advanced

TNBC or BRCA1/2+ BC (TNT): Survival

Survival, Mos Carboplatin Docetaxel

Median PFS 3.1 4.5

BRCA 1/2 mutated 6.8 4.8

BRCA 1/2 not mutated 3.1 4.6

Median OS 12.4 12.3


Bevacizumab-based Therapy: Significant

Improvement in PFS

Time (months)

1.0

0.8

0.6

0.4

0.2

0

PF

S e

stim

ate

0 6 12 18 24 30

9.2 8.0

Bevacizumab + taxane/

anthracycline (n=415)

Placebo + taxane/anthracycline

(n=207)

HR=0.64* (0.52–0.80)

p<0.0001

RIBBON-1: taxane/anthracycline cohort3

HR=0.48* (0.39–0.61)

p<0.0001

1.0

0.8

0.6

0.4

0.2

0

PF

S e

stim

ate

0 6 12 18 24 30 36

Time (months)

Bevacizumab + paclitaxel (n=368)

Paclitaxel (n=354)

5.8

E2100 (IRF assessment)1

1.0

0.8

0.6

0.4

0.2

0 0 6 12 18 24 30

Time (months)

HR=0.69* (0.56–0.84)

p=0.0002

Bevacizumab + capecitabine

(n=409)

Placebo + capecitabine (n=206)

8.6 5.7

PF

S e

stim

ate

RIBBON-1: capecitabine cohort3

1. Gray, et al. JCO 2009; 2. Miles, et al. JCO 2010

3. Robert, et al. ASCO 2009

*Censored for non-protocol therapy before disease

progression ‡15mg/kg q3w; §Exploratory p-value

AVADO2

HR=0.67* (0.54–0.83)

p<0.001§

1.0

0.8

0.6

0.4

0.2

0

PF

S e

stim

ate

0 6 12 18 24 30 36

Time (months)

8.1

Bevacizumab‡ + docetaxel

(n=247)

Placebo + docetaxel (n=241)

10.0

11.3

Meta-analysis:Analysis of PFS by Subgroups

O’Shaughnessy et al. ASCO 2010

Miles DW, et al. ESMO, 2010

Meta-analysis of First-line Bevacizumab

Plus Chemotherapy in taxanes-pretreated

Triple-Negative Breast Cancer

Deconstructing the molecular portraits of

breast cancer

Luminal A and B Normal-like

HER2-enriched Basal-like

Prat & Perou Mol Oncol 2011; Prat et al. BCR 2010

Claudin-low

Basal-like 1: Cell cycle,

DNA repair and

proliferation genes

Basal-like 2: Growth factor

signaling (EGFR, MET, Wnt,

IGF1R)

IM: Immune cell

processes (medullary

breast cancer)

M: Cell motility and

differentiation, EMT

processes

MSL: Similar to M but

growth factor signaling, low

levels of proliferation genes

(metaplastic cancers)

LAR: Androgen receptor

and downstream genes,

luminal features

Lehmann BD, et al. J Clin Invest. 2011

Identification of Human TNBC Subtypes

How could TNBCs be stratified?

LAR

BL1, BL2

IM

M, MSL

LAR

• Triple negative breast cancer is comprised of 6 molecularly distinct subtypes

BL= Basal Like, IM = Immunomodulatory, ML= Mesenchymal-Like, MSL= Mesenchymal Stem-like, LAR = Luminal AR

• 10% are “Luminal AR” (LAR) • LAR express higher levels of AR

mRNA vs other TNBC subtypes • LAR breast cancers are heavily

enriched in hormonally-regulated pathways

• Luminal AR is more closely related to hormone receptor positive breast cancer (Luminal A and B) than to other subtypes

LAR

•All LAR cell lines had some

response to bicalutamide

•Not all of “AR+” cell lines

were LAR (40%)

•The majority (70%) of “AR+”

cell lines responded to

bicalutamide

Lehman et al CCR 2011

LAR

LAR Cell lines

•All LAR cell lines had some

response to bicalutamide

•Not all of “AR+” cell lines

were LAR (40%)

•The majority (70%) of “AR+”

cell lines responded to

bicalutamide

Lehman et al CCR 2011

LAR

L. Denne et al, SABC 2013

LAR

Traina TA, et al, SABC 2014

Progression-Free Survival

by PREDICT AR Status

ITT Population

0

80

40

20

n = 118

0 8 16 24 33 41 49 61 64

Weeks

100

60

80

Patients at risk

PREDICT AR+

PREDICT AR−

56

62

36

28

25

15

19

6

15

4

13

4

10

2

2

1

1

1

0

0

0–1 Prior Regimens

n = 63

27

36

20

18

17

11

14

6

11

4

10

4

7

2

2

1

1

1

0

0

0

80

40

20

0 8 16 24 33 41 49 61 64

Weeks

100

60

80

PREDICT AR+

mPFS 16.0 weeks

(95% CI: 10.4, 26.1)

PREDICT AR−

mPFS 8.0 weeks

(95% CI: 7.1, 12.6)

PREDICT AR+

mPFS 32.3 weeks

(95% CI: 14.7, 60.3)

PREDICT AR−

mPFS 8.3 weeks

(95% CI: 7.1, 15.7)

ITT = Intent to Treat; mPFS = median progression-free survival; CI = confidence interval

PF

S (

%)

PF

S (

%)

Cortes J, et al, ECCO 2015

Overall Survival by PREDICT AR Status

56

62

53

55

49

46

45

37

42

27

40

24

32

13

15

6

11

6

3

2

Data cutoff 1Jul2015

ITT = intent to treat; mOS = median survival; CI = confidence interval; .

Patients at risk

PREDICT AR+

PREDICT AR−

0

80

40

20

n = 118

PREDICT AR−

mOS 32.3 weeks

(95% CI: 20.7, 48.3)

PREDICT AR+

mOS 75.6 weeks

(95% CI: 51.6, 91.4)

0 8 16 24 33 41 49 61 64

Weeks

100

60

Overa

ll S

urv

ival

(%)

85

ITT Population

PREDICT AR+ mOS 18.0 months

PREDICT AR – mOS 7.5 months

Cortes J, et al, ECCO 2015

IM

Dendritic cell

T cell

Lung

Anti-PDL1 X X

Tumor cell

X X

X X

Anti-PDL1

T cell

Akbari O, et al. Mucosal Immunol. 2010;

Matsumoto K, et al. Biochem Biophys Res Commun. 2008;

Chen, et al. Immunity, 2013

Mutational load:

somatic mutations act as tumor antigens

Lawrence et al, Nature 2013

Breast cancer has fewer mutations

p<0.0001

Objective responses to PD-1/PD-L1

blockade in advanced TNBC

Merck anti-PD1 Ab Genentech anti-PD-L1 Ab

ORR 18% centrally reviewed

N=32

58% PDL1+ ≥1%

Three ORRs >1 year duration

ORR 19% centrally reviewed

N=21 (4 ORR +3 pseudoprogression)

23% PDL1+ IHC 2+/3+ ≥5%/10%

Nanda 2014; Emens 2015

ML, MSL

Eribulin Mesylate (E7389): A Novel Tubulin

Targeted Agent

ML, MSL

Eribulin Mesylate (E7389):

EMT to MET phenoype

Yoshida T, et al. Br J Cancer 2014

Migration Invation

ML, MSL

Eribulin Mesylate (E7389):

EMT to MET phenoype

Yoshida T, et al. Br J Cancer 2014

Hazard ratio (95% CI)

<40 (n=51) Age ≥40 - <65 (n=560) ≥65 (n=151)

Caucasian (n=703) Race Non-Caucasian (n=59)

ER/PR + (n=528) Receptor status ER/PR - (n=187) Unknown (n=47)

ER/PR/HER2-negative (n=144)

≤2 (n=537) No. of organs involved >2 (n=217)

Visceral (n=624) Sites of disease Non-Visceral (n=130)

0.2 0.5 1.0 2 5 Favors ERIBULIN Favors TPC

Overall results (n=762)

EMBRACE Trial: Eribulin vs TPC

Based upon a stratified Cox analysis including geographic region, HER2 status, and prior capecitabine therapy as strata TPC: Treatment of Physician's Choice

Cortes et al. Lancet 2011

Eribulin vs Capecitabine (Study 301)

TN population

Kaufman P, et al. JCO 2015


DNA repair and

proliferation genes



IGF1R)

IM: Immune cell


breast cancer)



processes







luminal features

TNBC Subtypes: (Some) Research Strategies


DNA repair and

proliferation genes



IGF1R)

IM: Immune cell


breast cancer)



processes







luminal features

TNBC Subtypes: (Some) Research Strategies PARPi, ± DNA damaging agents

homologous recombination

deficiency assay (BRCA-1 ness)


DNA repair and

proliferation genes



IGF1R)

IM: Immune cell


breast cancer)



processes







luminal features




EGFR (cetuximab, lapatinib)

Self-renewal pathways (stem cell)

Wnt

Notch (PF03084014, AACR 2012


DNA repair and

proliferation genes



IGF1R)

IM: Immune cell


breast cancer)



processes







luminal features






Wnt

Notch (PF03084014, AACR 2012

Immune check point

PD1/PDL1, CTLA4

Vaccines: MUC1, NYO-ESO1


DNA repair and

proliferation genes



IGF1R)

IM: Immune cell


breast cancer)



processes







luminal features






Wnt

Notch (PF03084014, AACR 2012

Immune check point

PD1/PDL1, CTLA4


Agents targeting androgen receptor

(enzalutamide, bicalutamide, etc)


DNA repair and

proliferation genes



IGF1R)

IM: Immune cell


breast cancer)



processes







luminal features






Wnt

Notch (PF03084014, AACR 2012

Immune check point

PD1/PDL1, CTLA4


Agents targeting androgen receptor

(enzalutamide, bicalutamide, etc)

(eribulin?) Plus

PI3Ki, RAS/MEK/Erk,

MET, PTEN

etc, etc

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