Terapia sistemica neoadiuvante: in quali tumori? Quali ... · Neoadjuvant Treatment A window of...

42
Terapia sistemica neoadiuvante: in quali tumori? Quali risultati? Dott. Giacomo Pelizzari

Transcript of Terapia sistemica neoadiuvante: in quali tumori? Quali ... · Neoadjuvant Treatment A window of...

Page 1: Terapia sistemica neoadiuvante: in quali tumori? Quali ... · Neoadjuvant Treatment A window of opportunity Rational: Historically proposed to enable breast-conserving surgery in

Terapia sistemica neoadiuvante:

in quali tumori? Quali risultati?

Dott. Giacomo Pelizzari

Page 2: Terapia sistemica neoadiuvante: in quali tumori? Quali ... · Neoadjuvant Treatment A window of opportunity Rational: Historically proposed to enable breast-conserving surgery in

Neoadjuvant Treatment

A window of opportunity

Rational:

Historically proposed to enable breast-conserving surgery in stage II-III, in

particular for triple negative and HER2-positive EBC

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Neoadjuvant Treatment

A window of opportunity

Rational:

Historically proposed to enable breast-conserving surgery in stage II-III, in

particular for triple negative and HER2-positive EBC ➥ this strategy could fail in reducing the mastectomy rate!

Criscitiello C, et al. European Journal of Cancer 97 (2018) 1-6

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Neoadjuvant Treatment

A window of opportunity

Rational:

Historically proposed to enable breast-conserving surgery in stage II-III, in

particular for triple negative and HER2-positive EBC ➥ this strategy could fail in reducing the mastectomy rate!

In vivo evaluation of tumor dynamic response as early outcome

Page 5: Terapia sistemica neoadiuvante: in quali tumori? Quali ... · Neoadjuvant Treatment A window of opportunity Rational: Historically proposed to enable breast-conserving surgery in

Neoadjuvant Treatment

A window of opportunity

Rational:

Historically proposed to enable breast-conserving surgery in stage II-III, in

particular for triple negative and HER2-positive EBC ➥ this strategy could fail in reducing the mastectomy rate!

In vivo evaluation of tumor dynamic response as early outcome ➥ Tailored post-neoadjuvant treatment

Neoadjuvant

Treatment

NO pCR Escalation

Strategies

Surg

ery

pCR De-Escalation

Strategies

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Pathological complete response Definition and clinical meaning

Clinical meaning of pCR:

Achievement of pCR at time of surgery is correlated with favourable patient

outcome in all breast cancer subtype: prognostic relevance

Cortazar P, et al. Lancet 2014

Page 7: Terapia sistemica neoadiuvante: in quali tumori? Quali ... · Neoadjuvant Treatment A window of opportunity Rational: Historically proposed to enable breast-conserving surgery in

Neoadjuvant Treatment

A window of opportunity

Rational:

Historically proposed to enable breast-conserving surgery in stage II-III, in

particular for triple negative and HER2-positive EBC ➥ this strategy could fail in reducing the mastectomy rate!

In vivo evaluation of tumor dynamic response as early outcome ➥ Tailored post-neoadjuvant treatment

Ideal scenario for drug development and biomarker discovery ➥ shorter follow-ups and smaller sample sizes

➥ translational research

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Cortazar P, et al. Lancet 2014

Surrogate endpoint:

pCR has been proposed as a surrogate endpoint for prediction of long-term

clinical benefit, such as DFS and OS

SURROGACY

➥ Incremental gains of pCR should also result in a significant extensions of

survival outcomes at trial-level comparison of different treatmets

Prognostic relevance of pCR Enough for surrogacy?

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Which is the best candidate for neoadjuvant therapy?

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Neoadjuvant chemotherapy Identifying the best candidate

Cortazar P, et al. Lancet 2014

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Cortazar P, et al. Lancet 2014

Neoadjuvant chemotherapy Identifying the best candidate

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Cortazar P, et al. Lancet 2014

Neoadjuvant chemotherapy Identifying the best candidate

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Curigliano G, et al, Annals of Oncology 28: 1700–1712, 2017

“The Panel strongly endorsed the use of neoadjuvant therapy for

stage II or III, HER2 positive or triple-negative breast cancer as the

preferred initial treatment approach, particularly when there is any

suggestion that treatment response might enable de- escalation of

surgery or radiotherapy”

Neoadjuvant chemotherapy Identifying the best candidate

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Ellis, et al, JCO 2017

Neoadjuvant chemotherapy Luminal disease

ITT NO CT

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Recent advances in the neoadjuvant treatment of BC

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Escalating strategies

pCR

surgery

AC T Observation

Neoadjuvant Follow-up

DFS

+ CT (capecitabine, carboplatin)

+ Bevacizumab

+ Double HER2-blockage

+ PARPi

+ ET + CDK4/6i

+ Immunotherapy

We have a plan!

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HER2+

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Escalation Neoadjuvant therapy in HR+/HER2+ Phase II/III clinical trials

45% Double HER2 blockage

Harbeck N, et al. The Breast 34 (2017) S99eS103

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Escalation Neoadjuvant therapy in HR-/HER2+ Phase II/III clinical trials

70% Double HER2 blockage

Harbeck N, et al. The Breast 34 (2017) S99eS103

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Neoadjuvant therapy in HER2+ Does Double-blockage improve DFS/EFS?

Courtesy of Cortes J. Presented at ESMO 2018

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Neoadjuvant therapy in HER2+ Do we need anthracyclines?

Schneeweiss A, et al. Annals of Oncology 24: 2278–2284, 2013. Van Ramshorst et al. ASCO 2017

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Neoadjuvant therapy in HER2+ Concomitant anthracyclines and anti-HER2 therapies?

Buzdar et al. Jama Oncol 2018

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Neoadjuvant therapy in HER2+ De-escalation chemotherapy?

Harbeck N, et al. JCO 2017. Hurvitz S. Lancet Oncol 2017

ADAPT HR+ KRISTINE

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TNBC

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Escalation Neoadjuvant therapy in TNBC Phase II/III clinical trials

50%

Harbeck N, et al. The Breast 34 (2017) S99eS103

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Escalation Neoadjuvant therapy Platinum salts

Ref. Pop. Escalation Neoadjuvant Treatment Pz pCR HR DFS HR OS

Gepar IV

2010[1,2]

T≥2 cm,

or ER–,

or

ER+N+

4xEC 4xT

4xEC 4xTCape

4xEC 4xT 4xCape

471

471

479

22.3%

19.5%

22.3% ns

0.92 ns

0.97 ns

0.93

ns

0.97

ns

Gepar VI

2014[3,4,5]

TNBC

sub.

18wPacli/nPLD +Bev

18wPacli/nPLD/Cb1.5AUC +Bev

157

158

42.7%

53.2%*

0.56*

0.10

ns

CALGB40603

2015[6,7]

TNBC 12wPacli 4xddAC ±Bev

12wPacli+4xCb6AUC 4xddAC ±Bev

212

221

41%

54%*

0.84 ns

1.15

ns

[1] von Minckwitz, et al. JCO 2010; [2] von Minckwitz, et al. Ann Oncol 2014

[3] von Minckwitz, et al. Lancet Oncology 2014; [4] von Minckwitz, et al. ESMO 2017

1. [5] Loibl S, et al. Annals of Oncol 2018; [6] Sikov W, et al. JCO 2015; [7] Sikov W, et al. SABCS 2015

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Escalation Neoadjuvant therapy Final results of GeparSixto

Loibl S, et al. Annals of Oncol 2018

DFS OS

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Escalation Neoadjuvant therapy in TNBC Platinum salts

Poggio et al. Annals of Oncology. 29: 1497–1508, 2018

OR for pCR

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Escalation Neoadjuvant therapy in TNBC PARP Inhibitors

[1] Rugo HS, et al. NEJM 2016; [2] Loibl et al, Lancet Oncol 2018

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Escalation Neoadjuvant therapy Clinical trials

Ref. Pop. Escalation Neoadjuvant Treatment Pz pCR HR DFS HR OS

Gepar IV

2010[1,2]

T≥2 cm,

or ER–,

or

ER+N+

4xEC 4xT

4xEC 4xTCape

4xEC 4xT 4xCape

471

471

479

22.3%

19.5%

22.3% ns

0.92 ns

0.97 ns

0.93

ns

0.97

ns

Gepar VI

2014[3,4,5]

TNBC

sub.

18wPacli/nPLD +Bev

18wPacli/nPLD/Cb1.5AUC +Bev

157

158

42.7%

53.2%*

0.56*

0.10

ns

CALGB40603

2015[6,7]

TNBC 12wPacli 4xddAC ±Bev

12wPacli+4xCb6AUC 4xddAC ±Bev

212

221

41%

54%*

0.84 ns

1.15

ns

ISPY-2

2016[8]

TNBC

sub.

12wPacli 4xddAC

12wPacli+4xCb6AUC+Veliparib 4xddAC

21

39

26%

51%*

- -

BRIGHTNES

S

2017[9]

TNBC 12wPacli 4xddAC

12wPacli+Cb 4xddAC

12wPacli+Cb+Veliparib 4xddAC

158

160

361

31%

57.5%*

53.2%*

[1] von Minckwitz, et al. JCO 2010; [2] von Minckwitz, et al. Ann Oncol 2014

[3] von Minckwitz, et al. Lancet Oncology 2014; [4] von Minckwitz, et al. ESMO 2017

[5] Loibl S, et al. Annals of Oncol 2018; [6] Sikov W, et al. JCO 2015; [7] Sikov W, et al. SABCS 2015

[8] Rugo HS, et al. NEJM 2016; [9] Loibl et al, Lancet Oncol 2018

1. Escalation-NeoAdjuvant therapy increases pCR from 30-40% to 55%

2. Lack of proven survival benefit.

3. Patient selection (gBRCAm?)

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Escalation Neoadjuvant therapy in TNBC Parp trapping potency

Presented by Litton J at ASCO 2018

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Escalation Neoadjuvant therapy in TNBC Parp trapping potency

Presented by Litton J at ASCO 2018

Page 33: Terapia sistemica neoadiuvante: in quali tumori? Quali ... · Neoadjuvant Treatment A window of opportunity Rational: Historically proposed to enable breast-conserving surgery in

Escalation Neoadjuvant therapy in TNBC Parp trapping potency

Presented by Litton J at ASCO 2018

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Escalation Neoadjuvant therapy in TNBC Carboplatin vs Parp Inhibitors

Courtesy of Tutt A, at al. Presented at ESMO 2018

GEPAR-OLA Study

Page 35: Terapia sistemica neoadiuvante: in quali tumori? Quali ... · Neoadjuvant Treatment A window of opportunity Rational: Historically proposed to enable breast-conserving surgery in

Escalation Neoadjuvant therapy Clinical trials

Ref. Pop. Escalation Neoadjuvant Treatment Pz pCR HR DFS HR OS

Gepar IV

2010[1,2]

T≥2

cm, or

ER–,

or

ER+N+

4xEC 4xT

4xEC 4xTCape

4xEC 4xT 4xCape

471

471

479

22.3%

19.5%

22.3%

ns

0.92 ns

0.97 ns

0.93

ns

0.97

ns

Gepar VI

2014[3,4,5]

TNBC

sub.

18wPacli/nPLD +Bev

18wPacli/nPLD/Cb1.5AUC +Bev

157

158

42.7%

53.2%*

0.56*

0.10

ns

CALGB40603

2015[6,7]

TNBC 12wPacli 4xddAC ±Bev

12wPacli+4xCb6AUC 4xddAC ±Bev

212

221

41%

54%*

0.84 ns

1.15

ns

ISPY-2

2016[8]

TNBC

sub.

12wPacli 4xddAC

12wPacli+4xCb6AUC+Veliparib 4xddAC

21

39

26%

51%*

- -

BRIGHTNESS

2017[9]

TNBC 12wPacli 4xddAC

12wPacli+Cb 4xddAC

12wPacli+Cb+Veliparib 4xddAC

158

160

361

31%

57.5%*

53.2%*

-

GeparNuevo[10]

TNBC 12wNabPacli 4xAC

12wNabPacli ±Durv 4xAC ±Durv

Durvx2w+12wNabPacli±Durv4xAC ±Durv

44.2%

53.4%

61vs41

%

-

[1] von Minckwitz, et al. JCO 2010; [2] von Minckwitz, et al. Ann Oncol 2014

[3] von Minckwitz, et al. Lancet Oncology 2014; [4] von Minckwitz, et al. ESMO 2017

[5] Loibl S, et al. Annals of Oncol 2018; [6] Sikov W, et al. JCO 2015; [7] Sikov W, et al. SABCS 2015

[8] Rugo HS, et al. NEJM 2016; [9] Loibl S, et al. Lancet Oncol 2018; Loibl S, et al. ASCO 2018

1. Escalation-NeoAdjuvant therapy increases pCR from 30-40% to 55%

2. Lack of proven survival benefit.

3. Patient selection (gBRCAm?)

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Escalating strategies

We have a plan!

RD

surgery

AC T

Neoadjuvant Follow-up

DFS Adjuvant

+ CT (capecitabine, carboplatin)

+ Target therapies (PARPi, T-DM1)

+ ET + CDK4/6i

+ Immunotherapy

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Post-Neoadjuvant therapy CREATE X

Masuda N, et al. NEJM 2017

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CREATE X

Masuda N, et al. NEJM 2017

Trial Design

-HER2

negative

-Stage I-IIIB

-Age 20-74yr

-ECOG 0-1

NO pCR

Stratification:

ER- vs ER+

Age >50

Taxane use

N0 vs N1 vs N2

Fluorouracil use

Center

Standard treatment

Observation

Capecitabine 1250 mg/mq BD

d1-14 q21 x6-8 cycles

Ne

oa

dju

va

nt

CT

(at

least 4xA

nth

racycline)

Surg

ery

Random

ization 1

:1

End Points & Statistical Analysis:

Primary end point: DFS

Secondary end point: OS, Safety

With a power of the 80%, and a type I error set at

0.05, to see the hypothesized 0.74 hazard for

recurrence, second cancer or death, the required

sample size was estimated to be 900 patients.

Follow-up: 5 years.

Prespecified subgroup analysis (TNBC)

Page 39: Terapia sistemica neoadiuvante: in quali tumori? Quali ... · Neoadjuvant Treatment A window of opportunity Rational: Historically proposed to enable breast-conserving surgery in

CREATE X

Masuda N, et al. NEJM 2017

Results

• mFU: 3.9 years

All comers:

• 3-year DFS rate:

82.2% vs 73.9% with

Cape

• 5-year OS rate: 89.2%

vs 83.6% with Cape

• HR for recurrence 0.70

(0.53-0.92; P=0.01)

• HR for death 0.59

(0.39-0.90; P=0.01)

TNBC:

• 5-year DFS rate:

69.8% vs 56.1% with

Cape

• 5-year OS rate: 78.8%

vs 70.3% with Cape

• HR for recurrence 0.58

(0.39-0.87)

• HR for death 0.52

(0.30-0.90)

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CREATE X Conclusions

Capecitabine showed effectiveness as adjuvant treatment in patients with residual

disease after neoadjuvant therapy:

Methodological issues Previous trials in the adjuvant setting were negative (FINXX, GEICAM).

Statistical enrichment? In the FINXX trial, an exploratory analysis in the TNBC

subgroup showed that TX/CEX was more effective than T/CEF.

Treatment sequence? In preclinical models, agents such as paclitaxel,

cyclophosphamide increase cancer thymidine-phosphorylase concentration.

In subgroup analysis the survival benefit was significative only among TNBC patients.

Applicability issues Concern about the applicability and safety among non-Asian population.

Japanase have a 36% lower Cmax and 24% lower AUC than Caucasian.

The study dose was 1250mg/mq BD (Tolerability?).

Clinical issues Tailored therapies or Clinical Trials are preferred in this setting. Precision medicine?

Post-Neoadjuvant Carboplatin?

Warnings about Capecitabine use in adjuvant setting.

DPYD variants.

About 20% pts discontinued, 30% had dose reduction.

Off-lable?

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Ongoing Clinical Trials Post-Neoadjuvant therapy

Ref. Ph Post-NAT Population Ongoing Post-Neoadjuvant Treatment

ECOG-ACRIN III TNBC with RD1 cm 4xCis 75mg/mq q21

4xCb6AUC q21

6xCape 1000mg/mq BID d1-14 q21

A-BRAVE III TNBC with RD Observation

Avelumab 10 mg/kg IV q14 x 1 yr

SWOG S1418 III TNBC with RD1 cm or yN+

Observation

Pembrolizumab 200 mg q21 x 1yr

OlympiA III HER2– BC with gBRCAm Placebo

Olaparib 300 mg BID x 1yr

KATHERINE III HER2+ BC with RD Trastuzumab 6 mg/kg q21 x14

TDM-1 3.6 mg/kg q21 x14

PENELOPE-B III HR+/HER2– BC with RD and

CPSEG≥3, or 2 if ypN+

Placebo + ET

Palbociclib 125 mg d1-21 q28 x 13 + ET

CLEE011G2301

III HR+/HER2– BC with RD1

cm or yN12 mm

Placebo + ET

Ribociclib 600 mg d1-21 q28 x 26 + ET

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Dott. Giacomo Pelizzari

[email protected]