Abraxane (paclitaxel albumin)

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Abraxane (paclitaxel albumin)

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Title: Abraxane (paclitaxel albumin)

1
nab-paclitaxel in monoterapia
Dati clinici e safety
2
nab-paclitaxel in monoterapia
Studi clinici che hanno portato allindicazione
3
Gli studi pre-registrativi nell MBC
1. Ibrahim et al. Clin Cancer Res.
2002810381044 2. American BioScience, Inc.
Data on File3.Ibrahim et al. J Clin Oncol.
200523601960264. Gradishar et al. J Clin
Oncol. 20052377947803
4
Studi di Fase 1

Phase I
MTD, PK, etc.
Phase II
Phase III
Registration RCT
Other

5
Studio fase I DOSE FINDING

No premedicazione steroidea
No reazioni acute di ipersensibilità
Tossicità Dose-limitanti da taxano a 375
mg/m2 (neuropatia, cheratite, stomatite)
Dose Massima Tollerata 300 mg/m2
Durata infusione tollerabile 30 minuti
AUCs lineari nel range di dose clinicamente
rilevante

6
A new paradigm in cancer therapy the nabTM
platform
Phase I and Pharmacokinetic Study of ABI-007, a
cremophore-free, protein-stabilized, nanoparticle
formulation of paclitaxel

Receptor-mediated transport (via gp60) and
specific protein (SPARC) binding in tumour with
the goal of improving efficacy and the
therapeutic index
Phase I studies were conducted to determine the
safety, MTD and PK profile of this novel
formulation

100 80 60 40 20 0
140 120 100 80 60 40
Paclitaxel
Mortality ()
Paclitaxel (nCi/g)
0 20 40 60 80 100
0.01 0.1 1 10 100
Dose (mg/kg)
Hrs
50 higher paclitaxel dose
33 higher intra-tumour paclitaxel
Ibrahim et al. Clin Cancer Res. 2002810381044
7
NAB-P was administered safely over 30 minu with
no HSR

19 patients treated
No HSRs observed during the infusion period
Haematological toxicity (characterised by ANC and
PLT nadirs) mild and dose-dependent
DLTs (in three of six patients treated at dose
level 3) sensory neuropathy (n 3), stomatitis
(n 2) and superficial keratopathy (n 2)
MTD defined as 300 mg/m2

Dose level ANC nadir x 103/mm3 (range) PLT nadir x 103/mm3 (range)
0 2.229 (1.8505.040) 204 (174292)
1 1.845 (0.5863.729) 197 (118270)
2 0.960 (0.2643.680) 200 (105609)
3 0.966 (0.0181.804) 173 (25251)
ANC, absolute neutrophil count DLT,
dose-limiting toxicity HSR, hypersensitivity
reaction PLT, platelet
Ibrahim et al. Clin Cancer Res. 2002810381044
8
Paclitaxel PK for nab-Paclitaxel are Linear
Paclitaxel
nab-Paclitaxel
Paclitaxel AUC 3 hr1 Paclitaxel AUC 3
hr2 Paclitaxel AUC 1 hr3
nab-Paclitaxel4
50 000 45 000 40 000 35 000 30 000 25 000 20
000 15 000 10 000 5000 0
35 000 30 000 25 000 20 000 15 000 10 000 5000 0
y 3213e0.0095x R2 0.9328
y 3023.2e0.0089x R2 0.9683
AUCinf (ng hr/mL)
Mean AUCinf (ng hr/ml)
N 3 6 5 1 3 3 12 5 4
100 150 200 250 300
75 100 125 150 175 200 225 250 275 300 325 350 37
5
Dose (mg/m2)
nab-Paclitaxel dose (mg/m2)
1Kearns. Pharmacotherapy. 199717105S109S2Taxol
package insert3Ross et al. Cancer Chemother
Pharm. 20004nab-paclitaxel NDA
9
Studi di fase II

Phase I
MTD, PK, etc.
Phase II
Phase III
Registration RCT
Other

nab-paclitaxel 300mg/m2 q 3w
MBC w measurable disease
No taxanes within past 6 months

11
nab-Paclitaxel Phase II Trial Purpose

To evaluate the safety and antitumor activity of
nab-Paclitaxel in MBC patients
Treatment Regimen
nab-paclitaxel 300 mg/m2 q3w, no standard
pre-medication
Primary endpoint
tumor response rate (CR or PR)
Secondary endpoints
TTP
OS
Antitumor activity in anthracycline-naïve vs.
anthracycline-exposed patients
Changes in quality of life from baseline

Ibrahim NK et al. J Clin Oncol. 2005 23
6019-6026
12

Metodi Statistici
Endpoint primario di efficacia basato su
popolazione ITT
Criteri Successo / Fallimento
30 tasso di risposta (ORR) per nab-paclitaxel in
pazienti pre-trattati con anthracycline
Tutti i pazienti che ricevevano una dose erano
inclusi in analisi di risposta e tossicità

13
nab-paclitaxel Trial Fase II

Pazienti
N 63 pazienti con malattia misurabile CMM
Precedente Taxano gt 6 mesi
Caratteristiche
Lesioni Metastatiche gt 3 41
Polmone / Fegato 57
1a Linea di Terapia per CMM 62
Naïve Chemoterapia 24
Precedente Anthraciclina 59
Precedente Taxano 17

Ibrahim NK et al. J Clin Oncol. 2005 23
6019-6026
14
nab-paclitaxel Trial Fase II

Risultati primari
ORR 48
WHO criteri RECIST
1a Linea 64
Pretrattate con antracicline 41
3a Linea 22
Risultati secondari
TTP 26.6 settimane
Responders 48.1 settimane
OS 63.6 settimane

Ibrahim NK et al. J Clin Oncol. 2005 23
6019-6026
15
Treatment-related toxicities
Treatment-related grade 3 and 4 toxicities/AEs (N 63) Treatment-related grade 3 and 4 toxicities/AEs (N 63) Treatment-related grade 3 and 4 toxicities/AEs (N 63)
Grade 3 Grade 4
Haematological toxicities No. () No. ()
Neutropaenia 17 (27) 15 (24)
Leucopoenia 12 (19) 3 (5)
Infection with unknown absolute neutrophil count 4 (6) 0 (0)
Febrile neutropaenia 0 (0) 3 (5)
Anaemia 3 (5) 1 (2)
Thrombocytopenia 3 (5) 0 (0)
N 62
Note if a patient reported the same toxicity
more than once, that patient was only counted
once for the summary of that toxicity, using the
most severe intensity. Haematological toxicities
were based on laboratory values others were
based on AE reports from the clinical
investigators
Ibrahim NK et al. J Clin Oncol. 2005 23
6019-6026
16
Treatment-related toxicities (cont.)
Treatment-related grade 3 and 4 toxicities/AEs (N 63) Treatment-related grade 3 and 4 toxicities/AEs (N 63) Treatment-related grade 3 and 4 toxicities/AEs (N 63)
Grade 3 Grade 4
Non-haematological toxicities No. () No. ()
Fatigue 8 (13) 0 (0)
Sensory neuropathy 7 (11) 0 (0)
Myalgia 5 (8) 0 (0)
Diarrhoea 3 (5) 0 (0)
Cardiac - ischaemia/infarction 0 (0) 1 (2)
Jaundice 0 (0) 1 (2)
Vomiting 1 (2) 0 (0)
Nausea 1 (2) 0 (0)
Headache 1 (2) 0 (0)
Mucositis 1 (2) 0 (0)
Rash/desquamation 1 (2) 0 (0)
Stomatitis/pharyngitis 1 (2) 0 (0)
Ibrahim NK et al. J Clin Oncol. 2005 23
6019-6026
17
Treatment-related toxicities
100 90 80 70 60 50 40 30 20 10 0
Grade 1 Grade 2 Grade 3 Grade 4
Percentage of patients
Nausea
Myalgia
Vomiting
Alopecia
Anaemia
Leukopenia
Neutropenia
Sensory neuropathy
Stomatitis/pharyngitis
Fatigue
Infection with unknown ANC
Ibrahim NK et al. J Clin Oncol. 2005 23
6019-6026
18
Treatment-Related Toxicities

Grade 4 neutropeenia
Primarily during the first treatment cycle and
managed with dose reductions
Grade 3 neuropathy
All occurrences were sensory neuropathy
Five patients discontinued due to neuropathy (8)
Myalgia
Episodes were worse immediately after dosing and
resolved by next dose (no discontinuation)
Ocular/visual
Mostly dry eye and blurred vision (no G3)

Ibrahim NK et al. J Clin Oncol. 2005 23
6019-6026
19
Conclusioni

NAB-P demonstrated significant antitumour
activity and a favourable safety profile in
patients with MBC
No premedication, prolonged infusions or special
IV infusion sets are required with NAB-P
The significant antitumour activity and
favourable safety profile of NAB-P may be related
to both
exploitation of albumin to obtain high
intratumoral concentration via gp60 and SPARC
the absence of polyethylated castor oil
The low incidence of neutropaenia makes NAB-P a
good candidate for combination treatment regimens

Ibrahim NK et al. J Clin Oncol. 2005 23
6019-6026
20

Conclusioni Review Punti principali

Popolazione Eterogenea 63 pazienti con CMM (1a -
3a Linea), (Precedentemente trattati con/senza
Anthracicline)
ORR 48 (1a Linea 64), (Antrac. 41)
Effetti collaterali (Grado 4 Neutropenia 24),
(NF 5), (Grado 3 Neuropatia 11)

Ibrahim NK et al. J Clin Oncol. 2005 23
6019-6026
21
Studi di Fase III

Phase I
MTD, PK, etc.
Phase II
Phase III
Registration RCT
Other

22
Phase III Trial of Nanoparticle Albumin-bound
Paclitaxel Compared with Polyethylated Castor
Oil- based Paclitaxel in Women with Breast Cancer
CA-O12 nab-paclitaxel Trial Pivotal Fase III
William J. Gradishar, Sergei Tjulandin, Neville
Davidson, Heather Shaw, Neil Desai, Paul Bhar,
Michael Hawkins, and Joyce OShaughnessy
Gradishar et al. J Clin Oncol 23 7794-7803. Nov
2005.
23
Phase III Trial of nab-Paclitaxel Compared with
Polyethylated Castor Oil-Based Paclitaxel in
Women with Breast Cancer
Gradishar et al. J Clin Oncol. 20052377947803
24
Fase III obiettivi

Goals
Confrontare lattività anti-tumorale di
nab-paclitaxel e paclitaxel convenzionale in
pazienti con carcinoma mammario metastatico.
Valutare la safety e tollerabilità di
nab-paclitaxel confrontata al paclitaxel
convenzionale.

Endpoints Primari
Objective response rates (ORR) Tutti I pazienti trattati 1 linea (analisi pianificata) RECIST criteria Safety e tollerabilità
Endpoints Secondari
Time to tumour progression (TTP) Overall survival (OS)
Gradishar et al. J Clin Oncol. 20052377947803
25
Phase III inclusion criteria

Females 18 yrs of age
Measurable MBC
ECOG PS 1 or 2
Patients stratified for prior anthracycline
exposure
No prior taxane for metastatic disease
No limit on number of prior therapies in the
metastatic setting

Gradishar et al. J Clin Oncol. 20052377947803
26
Select Baseline Characteristics
Primary Site of Measurable Disease
nab-Paclitaxel n229 Paclitaxel n225
Mean Age (yr) 53 53
Liver 40 43
Lung 32 35
LN, soft tissue only 16 13
Abdominal 4 3
Bone involvement 6 6
Unknown 1 0
Gradishar et al. J Clin Oncol 23 7794-7803. Nov
2005.
27
DemographicsTerapie precedenti
nab-Paclitaxel n229 Paclitaxel n225
Anthracycline-adiuvante e/o metastatico 77 78
Anthracycline per malattia metastatica 50 58
Precedente CT per malattia metastatica Nessuna 1 regime 2 regimi gt2 regimi 42 41 10 7 40 43 16 2
Gradishar et al. J Clin Oncol 23 7794-7803. Nov
2005.
28
Overall Response Rate (RECIST)
Tutti i pazienti Tutti i pazienti Pazienti 1a linea Pazienti 1a linea
nab-paclitaxel (N 229) Standard paclitaxel (N 225) nab-paclitaxel (N 97) Standard paclitaxel (N 89)
CRPR 33 19 42 27
95 CI 27-39 14-24 32-52 18-36
P-value P 0.001 P 0.001 P 0.029 P 0.029
Cochran-Mantel-Haenszel testCR, complete
responsePR, partial response
Gradishar WJ et al. J Clin Oncol 200523
7794-7803
29
Phase III NAB-P improved ORR independent of line
of therapy and across various subgroups
60
P 0.001
P 0.029
P 0.006
P 0.002
P 0.002
50
42.3
40
34.1
33.2
33.5
ORR ( 95 CI)
30
27.0
26.5
18.7
18.3
18.7
20
13.2
10
0
All First-line gt First-line Anthracycline Viscera
l patients therapy therapy exposed
disease
NAB-P 229 97 132 176 176Paclitaxel 225 89 136 175
182
Greater ORR was confirmed by an independent
review committee
Gradishar et al. J Clin Oncol. 20052377947803
30
Phase III NAB-P was associated with increased
paclitaxel intensity and improved outcome

Cross trial comparison (consistent with phase III
data)

CALGB 93421 (n 474) CALGB 93421 (n 474) CALGB 93421 (n 474) Pivotal phase III trial2 (n 454) Pivotal phase III trial2 (n 454) Pivotal phase III trial2 (n 454)
q3w regimen (mg/m2) Paclitaxel175 Paclitaxel 210 Paclitaxel 250 NAB-P260 Paclitaxel 175
ORR () 23 26 21 33 19 P 0.001
TTP 3.9 mo(16.8 wks) 4.1 mo(17.6 wks) 4.9 mo (21.1 wks) P 0.045 23.0 wks 16.9 wks P 0.006
Neutropaenia grade 4 () 34 44 53 9 22 P 0.001
Neuropathy grade 3 () 7 19 32 10 2 P 0.001
Wks mo x 4.3
Cancer and leukaemia group B 9342 data with
paclitaxel may not reflect on the active
ingredient per se, but rather on the increased
concentrations of Cremophor EL implicated in
drug entrapment in micelles and added toxicities
1. Winer et al. J Clin Oncol. 200422206120682.
Gradishar et al. J Clin Oncol. 20052377947803
31
Fase III nab-paclitaxel prolungato time to
disease progression in tutti i pazienti

Median TTP was significantly longer with NAB-P
vs. solvent-based paclitaxel for all patients
(23.0 vs. 16.6 weeks HR 0.726 P 0.002)

P 0.006 HR 0.75
NAB-P (n 229)
Paclitaxel (n 224)
Median 23.0 wks (19.426.1)
Proportion not progressed
Median 16.9 wks (15.120.9)
120
0 8 16 24 32 40 48 56 64 72 80 88 96
104
112
Wk
Note P value from log-rank test
Gradishar et al. J Clin Oncol. 20052377947803
32
Phase III OS in tutti i pazienti

All patients treated with NAB-P showed a trend
for greater median OS vs. solvent-based
paclitaxel (65 vs. 55.7 weeks P0.374)

NAB-P (n 229)
Paclitaxel (n 225)
P 0.374 HR 0.90
Median 65.0 wks (52.176.9)
Probability of survival
Median 55.7 wks (48.066.4)
0 8 16 24 32 40 48 56 64 72 80 88 96
104
112
120
128
136
144
Wk
Gradishar et al. J Clin Oncol. 20052377947803
Note P value from log-rank test
33
Phase III NAB-P significantly prolonged OS in gt
first-line patients

NAB-P significantly prolonged median OS in
patients receiving gt first-line therapy vs.
solvent-based paclitaxel (56.4 vs 46.7 weeks
HR0.73 P0.024)

Gradishar et al. J Clin Oncol. 20052377947803
Note P value from log-rank test
34
Phase III tossicità ematologiche nab-paclitaxel
ben tollerato
NAB-Pn 229 NAB-Pn 229 Paclitaxeln 225 Paclitaxeln 225
AE () Grade Grade Grade Grade
3 4 3 4 P value
Neutropaenia 25 9 32 22 lt 0.001
Thrombocytopaenia lt 1 0 lt 1 0 0.290
Anaemia lt 1 lt 1 0 lt 1 0.279
Febrile neutropaenia lt 1 lt 1 lt 1 0 0.491
Septic deaths 0 0
Gradishar et al. J Clin Oncol. 20052377947803
Cochran-Mantel-Haenszel test based upon all
grades
35
Phase III NAB-P was associated with increased
sensory neuropathy
NAB-Pn 229 NAB-Pn 229 NAB-Pn 229 Paclitaxel n 225 Paclitaxel n 225 Paclitaxel n 225
AE () Grade Grade Grade Grade Grade Grade
2 3 4 2 3 4 P value
Hypersensitivity lt 1 0 0 0 1 0 0.150
Flushing lt 1 0 0 5 0 0 lt 0.001
Sensory neuropathy 20 10 0 10 2 0 lt 0.001
Fatigue 13 8 lt 1 16 3 lt 1 0.062
Myalgias 12 7 0 15 2 0 0.567
Vomiting 4 3 lt 1 4 1 0 0.022
Oedema 2 0 0 lt 1 lt 1 0 0.851
Gradishar et al. J Clin Oncol. 20052377947803
Cochran-Mantel-Haenszel test based upon all
grades
36
Phase III sensory neuropathy following NAB-P
260 mg/m2 q3w improved rapidly

1.00 0.75 0.50 0.25 0.00

NAB-P (n 24)

Proportion not resolved
NAB-P median time to resolution to a lesser
grade 22 days (95 CI 1722 days) vs. 79 days
with solvent-based paclitaxel
0 10 20 30 40 50 60 70 80 90 100 110 120 130
Days since grade 3 to lower grade
Gradishar et al. J Clin Oncol. 20052377947803
Censored
37
Fase III neuropatia migliorata rapidamente nella
maggior parte dei pazienti
24 pazienti (10) con nab-paclitaxel hanno
sviluppato grado 3 neuropatia

14 / 24 rapido miglioramento con una mediana di
22 giorni
71 (10/14) con miglioramento hanno ripreso
nab-paclitaxel ad una dose ridotta
solo 3 (6/233) interrotto nab-paclitaxel a
causa della neuropatia sensoriale
no neuropatia motoria in entrambi I bracci di
trattamento

Gradishar et al. J Clin Oncol. 20052377947803
38
Phase III nab-paclitaxel ben tollerato in
pazienti 65 aa

AEs erano simili in pazienti lt 65 e 65 aa in
entrambi I gruppi

AE () NAB-Pn 229 Paclitaxeln 225
Neutropenia 23 59
Leucopenia 10 31
Nausea 20 38
Iperglicemia 0 19
Flushing 0 16
NO effetti collaterali addizionali per
nab-paclitaxel in pazienti 65 aa rispetto a
pazienti più giovani
Gradishar et al. J Clin Oncol. 20052377947803
39
Conclusioni

Confronto con solvent-based paclitaxel
nab-paclitaxel ha dimostrato un
significativamente maggiore tasso di risposta e
prolungato TTP
nab-paclitaxel ha prolungato sopravvivenza in
pazienti con CMM trattati come seconda linea
Lincidenza di grade 4 neutropenia è stata
significativamente più bassa per nab-paclitaxel
Maggiore tasso di neuropatia sensoriale grade 3
con nab-paclitaxel ma risolta rapidamente con
una mediana di 22 giorni verso 79 giorni per
solvent-based taxano
no Severe HSRs con nab-paclitaxel con assenza
di premedicazione e più breve tempo di infusione

HSR, hypersensitivity reaction
Gradishar et al. J Clin Oncol. 2005 23
77947803
40
Phase III Subgroup Analysis Comparing
nab-paclitaxel with Paclitaxel in Patients with
MBC Previously Treated with Anthracycline
Davidson et al.EBCC. 2008. Poster 569
41
Phase III prior anthracycline patient
demographics
Metastatic anthracycline(n 245) Metastatic anthracycline(n 245) Metastatic or adjuvant anthracycline(n 351) Metastatic or adjuvant anthracycline(n 351)
nab-paclitaxel(n 115) Paclitaxel(n 130) nab-paclitaxel(n 176) Paclitaxel(n 175)
Age (yrs)
mean 53.3 53.8 52.6 52.8
range 2779 3483 2779 3083
Race, n ()
white 111 (97) 128 (98) 169 (96) 169 (97)
other 4 (3) 2 (2) 7 (4) 6 (3)
ECOG PS, n ()
1 109 (95) 127 (98) 165 (94) 172 (98)
2 6 (5) 3 (2) 10 (6) 3 (2)
3 0 (0) 0 (0) 1 (lt 1) 0 (0)
Davidson et al. EBCC. 2008. Poster 569
42
Phase III CA012 nab-paclitaxel significantly
improved ORR by 16 over paclitaxel
Sub-analysis of anthracycline pretreated patients
nab-paclitaxel
P 0.002
Paclitaxel
P 0.01
ORR ()
Davidson et al. EBCC. 2008. Poster 569
43
Phase III CA012 nab-paclitaxel had a
significantly longer TTP compared with
paclitaxel
Prior anthracycline in metastaticsetting only
Prior anthracycline (adjuvant or metastatic
setting)
1.00
1.00
P 0.004
P 0.011
0.75
0.75
nab-paclitaxel Paclitaxel
Proportion not progressed
0.50
0.50
Proportion not progressed
0.25
0.25
0.00
0.00
0 16 32 48 64 80 96 120
0 16 32 48 64 80 96 120
Wks
Wks
Davidson et al. EBCC 2008. Poster 569
44
Phase III CA012 nab-paclitaxel significantly
prolonged OS compared with paclitaxel
Prior anthracycline in metastaticsetting onlyB
Prior anthracycline (adjuvant or metastatic
setting)A
1.00
1.00
P 0.049
P 0.049
0.75
0.75
nab-paclitaxel Paclitaxel
0.50
Probability of survival
0.50
Probability of survival
0.25
0.25
0.00
0.00
0 16 32 48 64 80 96 112 128 152
0 16 32 48 64 80 96 112 128 152
Wks
Wks
Davidson et al. EBCC 2008. Poster 569
45
CA012 conclusions from subgroup analysis

This subset analysis evaluating patients
previously treated with anthracycline shows that,
compared with paclitaxel, treatment with
nab-paclitaxel
significantly improved clinical outcomes in
patients with MBC
nab-paclitaxel achieved significantly higher
ORRs
nab-paclitaxel had a significantly longer TTP
nab-paclitaxel significantly prolonged survival
benefit
is effective for the treatment of patients with
MBC

46
nab-paclitaxel in monoterapia
Altri dati/studi pazienti pesantemente trattate
con taxani
47
November 2007

nab-paclitaxel 100 or 125mg/m2 qw
MBC w measurable disease
PD on taxanes or relapse within 12 months from
adjuvant taxanes

48
nab-Paclitaxel QW Regimen Phase II Trial in
Taxane-Refractory MBC Purpose

To explore whether nab-paclitaxel has antitumor
activity in patients with MBC that had progressed
on conventional taxane therapy
Primary Endpoint
Percentage of patients who achieved a confirmed
objective, complete, or partial response
Secondary Endpoints
SD after gt 16 weeks
PFS
OS
Safety

Blum et al. Clin Breast Cancer. 20077850856
49
nab-Paclitaxel QW Regimen Phase II Trial in
Taxane-Refractory MBC Trial Design

Heavily pre-treated, taxane-refractory patients

PATIENT COHORTS
nab-Paclitaxel 100 mg/m2 qw 3/4 n 106
nab-Paclitaxel 125 mg/m2 qw 3/4 n 75
Study initiated at 100 mg/m2 qw 3 of 4 wks.
Because minimal toxicities were observed at this
dose and schedule, protocol was amended to
include additional cohort of patients to receive
125 mg/m2 qw 3 of 4 wks. Each cohort was analyzed
separately.
Blum et al. Clin Breast Cancer. 20077850856
50
nab-Paclitaxel QW Regimen Phase II Trial in
Taxane-Refractory MBC Select Demographics and
Baseline Characteristics
100 mg/m2(n106) 125 mg/m2(n75)
Median (range) age, yrs 53 (3476) 53 (3374)
Visceral disease () 94 89
gt 3 metastatic sites () 65 69
Tumour progression while on taxane therapy for metastatic disease () 88 89
Previous taxane therapy on a qw schedule for metastatic disease (no. of pts) 58 41
paclitaxel () 40 44
docetaxel () 34 37
paclitaxel/docetaxel (sequential) () 26 20
Median (range) no. of previous chemotherapy regimens for metastatic disease 3 (07) 3 (114)
Previous adjuvant chemotherapy (no. of pts) 85 79
anthracycline-containing () 75 56
taxane-containing () 29 27
Blum et al. Clin Breast Cancer. 20077850856
51
nab-Paclitaxel QW Regimen Responses in
Taxane-Refractory MBC
100 mg/m2 100 mg/m2 100 mg/m2 125 mg/m2 125 mg/m2 125 mg/m2
n ORR () DiseaseControl () n ORR () DiseaseControl ()
Antitumour activity all patients 106 14 26 75 16 37
Prior taxane therapy for metastatic disease Docetaxel Paclitaxel Docetaxel and Paclitaxel 34 30 29 21 13 7 32 30 21 28 20 19 21 20 0 46 45 21
Cochran-Mantel-Haenszel test based upon all
grades
Blum et al. Clin Breast Cancer. 20077850856
52
nab-Paclitaxel QW Regimen Similar Survival
Between Patients Who Achieved SD 16 wks and
Those With a Confirmed Response
100
Survival curves for the 100 and 125 mg/m2 cohorts
combined (n 181)
Confirmed responders
75
SD 16 wks
Non-responders
50
Probability of survival ()
25
P 0.7106
0
0 3 6 9 12 15 18 21 24 27 30
Mo
Blum et al. Clin Breast Cancer. 20077850856
53
NAB-P qw regimen safety
100 mg/m2 100 mg/m2 125 mg/m2 125 mg/m2
NCI CTC toxicity/AE Grade 3 Grade 4 Grade 3 Grade 4
Haematological toxicities ()
leucopaenia 19 lt 1 33 3
neutropaenia (without G-CSF) 14 4 31 3
Non-haematological toxicities ()
fatigue 5 0 12 0
sensory neuropathy 8 0 19 0
nausea 4 0 3 0
diarrhoea 1 0 5 0
vomiting 3 0 1 0
alopaecia 0 0 0 0
41 of patients treated with NAB-P 100 mg/m2
and 35 of those treated with 125 mg/m2 had
pre-existing grade 1 peripheral
neuropathyG-CSF, granulocyte-colony stimulating
factor NCI CTC, National Cancer Institute common
toxicity criteria
Blum et al. Clin Breast Cancer. 2007 7 850856
54
NAB-P qw regimen peripheral neuropathy improved
rapidly

Grade 3 neuropathy
100 mg/m2 cohort, nine patients (8)
125 mg/m2 cohort, 14 patients (19)
grade 1 pre-existing neuropathy
three patients in 100 mg/m2 and three patients in
125 mg/m2
Of the 23 patients with grade 3 PN, 15 (65)
restarted NAB-P at a lower dose
patients who continued treatment were able to
resume dosing, typically in 12 wks

PN, peripheral neuropathy
Blum et al. Clin Breast Cancer. 2007 7 850856
55
Conclusions

QW nab-paclitaxel at 100 mg/m2 and 125 mg/m2
achieved
Disease control in 26 and 36 of pts,
respectively
PFS of 3.0 mo and 3.5 mo
OS of 9.2 mo and 9.1 mo
There was no significant difference in OS between
patients who achieved an objective response and
non-responders who had SD 16 wks
nab-Paclitaxel 100 mg/m2 was well tolerated with
no HSR and a low rate of treatment cessation for
peripheral neuropathy
Minimal myelosuppression grade 4 neutropenia and
leukopaenia occurred in lt 5 of patients in both
cohorts

Blum et al. Clin Breast Cancer. 20077850856
56
nab-paclitaxel in monoterapia
Altri dati/studi confronto verso docetaxel
57
nab-paclitaxel JCO Editorial
58
nab-paclitaxel JCO Editoriale
CA-012 nab-paclitaxel vs Taxol
TAX 311 Taxotere vs Taxol
nab-paclitaxel 260mg/m2 (30min) q 3 wk No
premedicazione No special tubing
DOCETAXEL 100mg/m2 (1h) q 3 wk Dexametasone 8mg
po bid x 5 d Dal giorno precedente all infusione
R
R
PACLITAXEL 175mg/m2 (3h) q 3 wk Dexametasone
20mg po 12 6 h Difenidramine 50mg IV
Cimetidine 300mg or Ranitidine 50mg IV 30-60
min prima dell infusione
PACLITAXEL 175mg/m2 (3h) q 3 wk Dexametasone
20mg po 12 6 h Difenidramine 50mg IV
Cimetidine 300mg or Ranitidine 50mg IV 30-60
min prima dell infusione
59
JCO Editorial CA-012 vs. TAX 311

Entrambi i trials mostrano avere simili
caratteristiche di pazienti e malattia
Simile numero di pazienti in ogni trial
Mix di pazienti trattati e non trattati per CMM
Precedente trattamento con antracicline
Simili Fattori Prognostici
Sia nab-paclitaxel che Taxotere confrontati con
Taxol alla dose di 175mg/m2 ogni 3 settimane

60
nab-paclitaxel JCO Editoriale
61
Significantly Longer Progression-Free Survival
with nab-Paclitaxel Compared with Docetaxel as
First-Line Therapy for Metastatic Breast Cancer

W.J. Gradishar, D. Krasnojon, S. Cheporov, A.N.
Makhson, G.M. Manikhas, A. Clawson, P. Bhar

Gradishar W, et al. J Clin Oncol, 2009 27(22)
3611-3619.
62
Study Objectives

To obtain comparative safety and preliminary
antitumor response data for
nab-paclitaxel vs docetaxel
weekly (QW) vs every-3-week (Q3W)
nab-paclitaxel
lower vs higher dose QW nab-paclitaxel
Design open-label, randomized, phase II,
multi-center study

Gradishar W, et al. J Clin Oncol, 2009 27(22)
3611-3619.
63
qw or q3w NAB-P vs q3w docetaxel study design

302 first-line MBC patients randomised to four
arms (300 pts received study drug and were
evaluable)

R A N D OMI S E
Arm A NAB-P 300 mg/m2 q3w
Comparisons
NAB-P vs docetaxel(A, B, C vs D)
Arm B NAB-P 100 mg/m2 3q4w
qw vs q3w NAB-P (B, C vs A)
Arm C NAB-P 150 mg/m2 3q4w
low- vs high-dose qw NAB-P (B vs C)
Arm D docetaxel 100 mg/m2 q3w
Arms A, C and D administered at the MTD3q4w,
repeated wkly for 3 wks out of 4
Gradishar W, et al. J Clin Oncol, 2009 27(22)
3611-3619.
64
qw or q3w nab-paclitaxel vs q3w docetaxel
obiettivi dello studio

Ottenere confronto tossicità e dati preliminari
di risposta antitumorale per
nab-paclitaxel vs docetaxel
qw vs q3w nab-paclitaxel
lower- vs higher-dose qw nab-paclitaxel
Utilizzare dati di questo trial per disegnare
futuri trials con nab-paclitaxel

Gradishar W, et al. J Clin Oncol, 2009 27(22)
3611-3619.
65
qw or q3w nab-paclitaxel vs q3w docetaxel
analisi finale - status dello studio
nab-paclitaxel nab-paclitaxel nab-paclitaxel Docetaxel
300 mg/m2 q3w (n 76) 100 mg/m2 3q4w(n 76) 150 mg/m2 3q4w(n 74) 100 mg/m2q3w (n 76)
Terapia in corso () 4 (5) 6 (8) 14 (19) 3 (4)
Interrotta () 72 (95) 70 (92) 60 (81) 71 (96)
Motivi per interruzione ()
PD 37 (51) 48 (69) 33 (55) 27 (38)
tossicità inaccettabile 10 (14) 5 (7) 10 (17) 15 (21)
AEs 0 1 (1) 2 (3) 2 (3)
decisione investigatore 7 (10) 5 (7) 6 (10) 14 (20)
decisione paziente 18 (25) 11 (16) 8 (13) 13 (18)
PD, progressive disease
Gradishar W, et al. J Clin Oncol, 2009 27(22)
3611-3619.
66
qw or q3w nab-paclitaxel vs q3w docetaxel
(RECIST) sperimentatore-ORR
C vs D P lt 0.001
B vs D P 0.002
A vs D NS
ORR
300 mg/m2q3w(A n 76)
100 mg/m23q4w(B n 76)
150 mg/m23q4w(C n 74)
Docetaxel100 mg/m2q3w(D n 74)
nab-paclitaxel
A vs B P 0.024A vs C P 0.002B vs C
NSNS, not significant
Gradishar W, et al. J Clin Oncol, 2009 27(22)
3611-3619.
67
qw or q3w nab-paclitaxel vs q3w docetaxel
controllo della malattia (ORR SD gt 16 wks)
P 0.009
Disease Control Rate stable disease for 16 weeks
or confirmed overall PR or CR
P 0.017

of Patients
100 mg/m2 q3w
300 mg/m2 q3w
100 mg/m2 qw 3/4
150 mg/m2 qw 3/4
Docetaxel
nab-Paclitaxel
P-Values for Investigator-assessed DCR are not
shown
Gradishar W, et al. J Clin Oncol, 2009 27(22)
3611-3619
68
qw or q3w nab-paclitaxel vs q3w docetaxel PFS
(Investigator Review)
1.00
Regimen Median PFS (mo) P value vs docetaxel
nab-paclitaxel (A) 300 mg/m2 q3w 10.9 NS
nab-paclitaxel (B) 100 mg/m2 3q4w 7.5 NS
nab-paclitaxel (C) 150 mg/m2 3q4w(n 74) 14.6 P 0.012 HR 0.568
Docetaxel (D) 100 mg/m2 q3w 7.8 NA
0.75
Proportion not progressed
0.50
0.25
0.00
0 3 6 9 12 15 18 21 24
Mo
A vs B P 0.076, HR 0.702 B vs C P 0.001
HR 1.972
Gradishar W, et al. J Clin Oncol, 2009 27(22)
3611-3619.
69
qw or q3w nab-paclitaxel vs q3w docetaxel
tossicità
nab-paclitaxel nab-paclitaxel nab-paclitaxel Docetaxel
300 mg/m2 q3w (n 76) 100 mg/m2 qw (n 76) 150 mg/m2 qw (n 74) 100 mg/m2 q3w (n 74)
Neuropatia, n ()
grade 2 17 (22) 11 (14) 19 (26) 14 (19)
grade 3 13 (17) 6 (8) 10 (14) 9 (12)
grade 4 0 (0) 0 (0) 0 (0) 0 (0)
Fatigue, n ()
grade 2 17 (22) 5 (7) 15 (20) 12 (16)
grade 3 4 (5) 0 (0) 2 (3) 14 (19)
grade 4 0 (0) 0 (0) 0 (0) 0 (0)
Tossicità legate al trattamento riportate in
25 dei pazienti
Gradishar W, et al. J Clin Oncol, 2009 27(22)
3611-3619.
70
qw or q3w nab-paclitaxel vs q3w docetaxel
tossicità
nab-paclitaxel nab-paclitaxel nab-paclitaxel Docetaxel
300 mg/m2 q3w (n 76) 100 mg/m2 qw (n 76) 150 mg/m2 qw (n 74) 100 mg/m2 q3w (n 74)
Artralgia
grade 2 20 (26) 5 (7) 14 (19) 10 (14)
grade 3 1 (1) 0 (0) 0 (0) 0 (0)
grade 4 0 (0) 0 (0) 0 (0) 0 (0)
Neutropenia
grade 2 22 (29) 25 (33) 24 (32) 2 (3)
grade 3 29 (39) 15 (20) 26 (35) 14 (19)
grade 4 4 (5) 4 (5) 7 (9) 54 (75)
Medio nadir SD, x 109/l 1.21 1.00 1.51 0.96 1.11 0.63 0.38 0.34
Tossicità legate al trattamento riportate in
25 dei pazienti
Gradishar W, et al. J Clin Oncol, 2009 27(22)
3611-3619.
71
qw or q3w nab-paclitaxel vs q3w docetaxel grade
3 neuropatia migliorata più rapidamente con
nab-paclitaxel
Proportion not improved

Neuropatia con simile frequenza in tutti i
bracci di trattamento
Tempo mediano al miglioramento
per nab-paclitaxel 300 mg/m2, 100 mg/m2, 150
mg/m2 22, 22, 19 giorni
vs docetaxel 37 giorni

1.00
nab-paclitaxel 300 mg/m2 q3w (A) nab-paclitaxel
100 mg/m2 qw (B) nab-paclitaxel 150 mg/m2 qw
(C) Docetaxel 100 mg/m2 q3w (D)
0.75
0.50
0.25
0.00
0 10 20 30 40 50 60
70 80 90 100
Giorni
Gradishar W, et al. J Clin Oncol, 2009 27(22)
3611-3619.
72
Conclusioni

nab-paclitaxel ha dimostrato migliore
tollerabilità ed efficacia rispetto a docetaxel
Tutti e tre i bracci di nab-paclitaxel con più
bassi tassi di neutropenia, neutropenia febbrile
e fatigue
Il braccio più efficace di nab-paclitaxel
basato su PFS e ORR è risultato 150 mg/m2 qw
nab-paclitaxel 150 mg/m2 qw è risultato
superiore in maniera statisticamente
significativa in termini di ORR e PFS rispetto a
docetaxel
nab-paclitaxel 100 mg/m2 qw è risultato
associato con la minore tossicità
Gradishar W, et al. J Clin Oncol, 2009
27(22) 3611-3619.

73
Ultimi Aggiornamenti- Dati di Overall Survival
- Older patients with MBC
74
Nab- Paclitaxel Versus Docetaxel for the
First-line Treatment of Metastatic Breast Cancer
(MBC) Final Overall Survival (OS) Analysis of a
Randomized Phase 2 Trial
ASCO Breast Symposium, September 8-10 , 2011,
California Abstract 275
75
Overall Survival
Median OS (mo) P HR
AB-Pac 150mg/m2 qw (C) 33.8 Overall 0.047 C vs B 0.008 C vs D - - 0.575 0.688
AB-Pac 300mg/m2 q3w (A) 27.7 Overall 0.047 C vs B 0.008 C vs D - - 0.575 0.688
Taxotere 100mg/m2 q3w (D) 26.6 Overall 0.047 C vs B 0.008 C vs D - - 0.575 0.688
AB-Pac 100mg/m2 qw (B) 22.2 Overall 0.047 C vs B 0.008 C vs D - - 0.575 0.688

The 150 mg/m2 qw albumin-bound paclitaxel arm
demonstrated
A significantly longer median OS versus the 100
mg/m2 arm
A longer OS versus docetaxel, although this
difference was not statistically significant
The OS benefit of the 150 mg/m2 arm was
consistent among patient subgroups
Age lt65 vs 65 years
Visceral vs non-visceral disease
No. of visceral lesion sites lt5 vs 5
Pre-menopausal vs post-menopausal

ASCO Breast Symposium, Abstract 275
76
Overall Efficacy Analyses

A significant (P .047) treatment effect on OS
was observed among the 4 tratment arms
The OS benefit of 150 mg/mq qw nab-paclitaxel arm
was consistent with results observed in
investigator-assessed ORR and PFS

ASCO Breast Symposium, Abstract 275
77
Conclusion

Based on event-driven analysis of final OS, the
nab-paclitaxel 150 mg/m2 qw 3/4 regimen provided
the best clinical benefit for the forst-line
treatment of patients with MBC
The median OS of 33.8 months compares favorably
with historical values for taxane monotherapy for
MBC
The OS benefit of the 150 mg/mq qw regimen in
consistent with trends seen in investigator-assess
ed ORR and PFS
nab.-paclitaxel was generally well tolerated, and
the safety profile is consistent with previous
reports
These results support further eveluation of the
150 mg/mq qw dosing schedule of nab-paclitaxel in
a randomized, phase 3 trial for the first-line
treatment on MBC

ASCO Breast Symposium, Abstract 275
78
Weekly nab-paclitaxel is safe and effective in 65
years old patientswith metastatic breast cancer
A post-hoc analysis

Matti Aapro, Sergei Tjulandin, Paul Bhar, William
Gradishar

79
Purpose

This post-hoc analysis of 2 studies (Gradishar
W. 2005 and Gradishar W. 2009) investigated the
safety and efficacy of weekly and every-3-week
(q3w) nanoparticle albumin-bound paclitaxel
(nab-paclitaxel) in older patients with
metastatic breast cancer (MBC) compared with q3w
solvent-based paclitaxel and docetaxel.

Aapro M et al, The Breast 2011
80
Patient Population
Among the total treatment population in the 2
studies 114 (15) were 65 years old (phase 2, n
52 phase 3, n 62)

In the phase 2 study
33 pt randomized to nab-paclitaxel n 9 300
mg/m2 q3w
n 14 100 mg/m2 weekly
n 10 150 mg/m2 weekly
19 pt randomized to docetaxel

In the phase 3 study 30 pt randomized to
nab-paclitaxel 32 pt randomized to paclitaxel
Aapro M et al, The Breast 2011
81
Demographics/Baseline Characteristics
Aapro M et al, The Breast 2011
82
Efficacy (1)

In the phase 2 study
ORR nab-paclitaxel 22 300 mg/m2 q3w
64 100 mg/m2 weekly
60 150 mg/m2 weekly
docetaxel 32 100 mg/m2 q3w
In the phase 3 study
ORR nab-paclitaxel 27 260 mg/m2 q3w
paclitaxel 19 175 mg/m2 q3w

In the phase 2 study DCR nab-paclitaxel 56 300
mg/m2 q3w 86 100 mg/m2 weekly 90 150
mg/m2 weekly docetaxel 79 100 mg/m2 q3w In
the phase 3 study DCR nab-paclitaxel 53 260
mg/m2 q3w paclitaxel 41 175 mg/m2 q3w
Aapro M et al, The Breast 2011
83
Efficacy (2)
In the phase 2 study PFS median nab-paclitaxel
13.8 300 mg/m2 q3w 9.2 100
mg/m2 weekly 18.9 150 mg/m2
weekly docetaxel 8.5 100 mg/m2
q3w

In the phase 3 study
PFS median nab-paclitaxel 5.6 260
mg/m2 q3w
paclitaxel 3.5 175 mg/m2 q3w

Aapro M et al, The Breast 2011
84
Response and Survival
Aapro M et al, The Breast 2011
85
Safety and Tolerability
In general, treatment related grade 3 and 4 AEs
were similar for the elderly patients compared
with results from all patients in the 2 studies.
Aapro M et al, The Breast 2011
86
Conclusion
Weekly nab-paclitaxel was safe and more
efficacious compared with the q3w schedule and
with solvent-based taxanes in older patients with
MBC.

In particular, the 150 mg/m2 weekly for 3 weeks
followed by 1 week of rest nab-paclitaxel
resulted in 60 ORR and 21 months of median OS
along with no SAEs and no deaths thus, it may be
the optimal dose of nab-paclitaxel therapy in
patients 65 years old. These findings warrant
further examination of weekly nab-paclitaxel in
older patients with MBC.

Aapro M et al, The Breast 2011
87
nab-PaclitaxelOngoing Study in MBC
88
Cooperative Group Trial with Biomarker Analysis
Tumor biopsy on accessible tissue
RANDOMI ZE
Paclitaxel 90 mg/m2 qw 3/4
Bevacizumab 10 mg/kg q2w
nab-Paclitaxel 150 mg/m2 qw 3/4
Ixabepilone 16 mg/m2 qw 3/4
Serum for Caveolin-1 Tumor block for SPARC,
tubulin mutations, Circulating Tumor Cells (CTC)
and Circulating Endothelial Cells (CEC)
Serial serum measurement of caveolin-1 Serial
measurement of CTC and CEC
CALGB and NCCTG, PI Hope Rugo, Alvino Moreno
N900

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