LUNG CANCER

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LUNG CANCER

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Title: Targeted Therapies for Advanced Non-Small Cell Lung Cancer Author: Can Ozturk Last modified by: CAN OZTURK Created Date: 9/29/2005 4:26:22 AM – PowerPoint PPT presentation

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Title: LUNG CANCER

1

LUNG CANCER
MOLECULAR THERAPY
Prof. Dr. Can ÖZTÜRK
Gazi University School of
Medicine
Department of Pulmonology

2
Turkey - Male (All ages)
Crude Rate ASR (World)
Lung 37.3 47.7
Stomach 9.6 12.2
Bladder 8.6 11.0
Colorectal 7.4 9.1
Larinx 6.4 8.0
Prostate 6.1 8.0
Leukemia 5.1 5.8
Brain,CNS 3.9 4.5
NHL 3.3 3.8
Oral cavity 2.6 3.2
Total(except skin) 110.3 137.3
per 100.000
3
Turkey - Female (All Ages)
Crude Rate ASR (World)
Breast 19.9 22.0
Colorectal 7.6 8.5
Stomach 5.7 6.4
Ovarium 4.8 5.4
Lung 4.6 5.3
Leukemia 4.4 4.7
Corpus-Uterus 4.1 4.8
Cervix- Uterus 4.0 4.5
Brain, CNS 3.5 3.8
Non-Hodgkin lenfoma 2.9 3.1
Total(except skin) 82.0 91.2
per 100.000
4
UNTREATED NSCLC- PROGNOSIS
STAGE MS(Mts) 1yr. Sur.() 2yr. Sur.()
c I, II 13 56 8
c III 4-9 16-30 0-4
c IV 3 - -
5
UNTREATED SCLC- PROGNOSIS
STAGE MEDIAN SUR. 1 YR. SURVIVAL
LIMITED Supportive Care 12 weeks 18 weeks 7
EXTENSIVE Supportive Care 5 weeks 8 weeks
6
Treatment- Prognosis

Status of treatment is dismal
Five year survival approx. 15
61 for Colon
86 for Breast
96 for Prostate

7
NSCLC Survival based on stages
Greene et al, eds. AJCC Cancer Staging Manual.
6th ed. 2002.
8
5 year survival - TARGETS

NSCLC CURRENT TARGET
STAGE
IA 70-85 85-95
IB 60-70 70-85
IIA 35-45 45-60
IIB 25-35 35-45
IIIA 5-20 20-30
IIIB 3-7 10-20
IV lt1 2-5

SCLC CURRENT TARGET
STAGE
LTD 15-25 25-30
EXT lt1 2-5

Langer CJ, Fox Chase Cancer Center-2006
9
NSCLC- Systemic Therapy

Uptodate standart therapies
Epidermal Growth Factor Receptor (EGFR)
Inhibitors
Gefitinib (Iressa)
Erlotinib (Tarceva)
Anti-EGFR Monoclonal antibodies
Cetuximab (Erbitux)
Anti-Vascular Endothelial Growth Factor (VEGF)
Monoclonal antibody
Bevacizumab (Avastin-Altuzan)

10
Systemic Therapy First Line

2-drug platinum-based combinations

2 drug platinum based regimens
Schiller JH. NEJM 2002 34692-98
11
Results- First Line
Survival
Medan survival 8 months
Response rate 19
TTP
MedianTTP 3.7 months
Schiller JH. NEJM 2002 34692-98
12
Second Line Therapies

Docetaxel is superior than best supportive care
Response rate 7
Median survival 7.0 vs 4.6 months
Median TTP 10.6 vs. 6.7 weeks
Pemetrexed (Alimta) is effective as docetaxel,
but less toxicity profile

Shepherd et al. JCO 2000182095-2103 Hanna et
al. JCO 2004 221589-97
13
Targeted Therapies in Lung Cancer
General Spesific
Cell Cycle cdks
Apoptosis Bcl-2 Survivin XIAP P53 clusterin
Others DNA MTase HDAC proteosom
Extracellular MMP
Receptors/ kinases C-kit PDGFR abl
General Spesific
Angiogenesis VEGF VEGFR FGF Integrin
EGFR family EGFR HER2
Signal Ras Raf kinaz MEK mTOR PKC
14
Targeted Therapies

EGFR Inhibitors
Gefitinib (Iressa)
Erlotinib (Tarceva)
Anti-EGFR Monoclonal antibody
Cetuximab (Erbitux)
Anti-VEGF Monoclonal antibody
Bevacizumab (Avastin-Altuzan)

15
Epidermal Growth Factor Receptor (EGFR) Human
Cancer

EGFR critically regulates tumor cell division,
proliferation, repair
EGFR may play a critical role in metastasis,
angiogenesis, invasion
Binding of specific ligands to EGFR (eg, EGF,
TGF-a) activates the receptor and triggers signal
transduction cascades that affect cell
proliferation
EGFR is expressed in a significant percentage of
human tumors and is correlated with poor
prognosis, decreased survival, and/or increased
metastasis
Inhibition of EGFR on tumor cells may inhibit the
growth or progression of EGFR-expressing tumors

16
EGFR structure
Extracellular area
Transmembranous area
Intracellular area
17
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18
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19
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20
EGFR expression in human tumors
Tumors showing high EGFR expression
High expression generallyassociated with

Invasion
Metastasis
Late-stage disease
Chemotherapy resistance
Hormone-therapy resistance
Poor outcome

NSCLC 40-80
Prostate 40-80
Gastric 33-74
Breast 14-91
Colorectal 25-77
Pancreatic 30-50
Ovarian 35-70

21
NSCLC- EGFR HER2
Lung Cancer- EGFR expression
F. Hirsch et al. Semin Oncol, 2002
22
NSCLC- EGFR HER2Survival
J. Brabender et al. Clin Cancer Res, 2001
23
EGFR Targeted Therapies

Inhibition of EGFR signalling with either the
monoclonal Ab or the tyrosine kinase
inhibitors(TKI) reduces proliferation in a
variety of epithelial tumor cells and blocks cell
cycle progression in the G1 phase
Inhibition of cell cycle progression is an
effective mechanism for modulating the growth of
tumors
EGFR inhibition, using TKI induce apoptosis (in
human tumor cells and vascular endothelial cells)
Ongoing trials are evaluating the clinical
utility of EGFR inhibitors for the treatment of
EGFR-expressing cancers

24
Acquired spesifications of Cancer Cells

Spesifications
Autocrine growth signal Yes
Yes
Insensitivity to anti-growth signals
Yes Yes
Awareness of cell death Yes
Yes
Uncontrolled proliferation Yes
Yes
Continious angiogenesis Yes
Yes
Tissue invasion and Metastasis Yes
Yes

Increase by EGFR activation
Decrease by EGFR Inhibition
Hanahan ve Weinberg, Cell, 2000
25
TKI-Small molecules mechanism of action
TKI
Proliferation
Apoptosis
Invasion
Sensitivity to chemotherapy
Metastasis
Adhesion
Angiogenesis
Etessami A, et al. Drugs Fut 2000258959 Moyer
J, et al. Cancer Res 199757483848Harari PM,
et al. Semin Radiat Oncol 200212(Suppl. 2)216
26
Growth Factors Cell Cycle
Receptors
27
Targeted Therapies

EGFR Inhibitors
Gefitinib (Iressa)
Erlotinib (Tarceva)
Anti-EGFR Monoclonal antibody
Cetuximab (Erbitux)
Anti-VEGF Monoclonal antibody
Bevacizumab (Avastin-Altuzan)

28
Gefitinib- with ChemotherapyFirst Line-Phase III
INTACT 1 2
Untreated advanced NSCLC Stratification Weigh
t loss in last 6 months(?5 vs gt5) PS 0 - 1
vs 2
Chemo x 6 cycles
250 mg gefitinib
Gefitinib / Placebo until progression
Chemo x 6 cycles
Randomise
500 mg gefitinib
Chemoi x 6 cycles
Placebo
Evre IIIB/IV KHDAKINTACT IRESSA NSCLC Trial
Assessing Combination Therapy INTACT 1 (N1093)
gemcitabin (1250 mg/m2)/cisplatin (80 mg/m2)
INTACT 2 (N1037) paclitaxel (225
mg/m2)/carboplatin (AUC6).
29
Gefitinib- with ChemotherapyFirst Line-Phase III
Med. survival
10 months
10 months
30
Gefitinib Second Third Line-Phase II
(250mg vs. 500mg)
Patient no. Response Rate () Median survival (Mts)
IDEAL-1 Japan, Europe, Australia, S. Africa 208 18.4 (total) 27.5 (Japan) 10.4 (Non-Japan) 7.6
IDEAL-2 United States 216 12 7

250mg ve 500mg doses- no difference in efficacy
Adverse effects- acceptable (rash and diarrhea)
more frequent in 500 mg group
IDEAL-1 M. Fukuoka et al. JCO
2003 212237-2246
IDEAL-2 MG Kris et al. JAMA
2003 2149-2158

31
Gefitinib Second Third Line-Phase III ISEL
Iressa Survival Evaluation in Lung Cancer
R A N D O M I Z E
Gefitinib 250 mg/gün

Inclusion Criteria
Stage IIIB veya IV NSCLC
Treated with platinum based CT( 1 or 2 times)
PS 0-3

N1692
Placebo
Thatcher et al. Lancet 2005
32
Gefitinib Second Third Line-Phase III ISEL -
Survival
Placebo
Gefitinib
(n1129)
(n563)
1.0
Median survival (mts)
5.6
5.1
0.8
1-year survival ()
27
22
0.6
HR0.89 (95 CI, 0.78-1.03) Plt0.11
Probability
0.4
Gefitinib
0.2
Placebo
0.0
0
16
2
14
4
10
12
8
6
Months
Thatcher et al. Lancet 2005
33
Targeted Therapies

EGFR Inhibitors
Gefitinib (Iressa)
Erlotinib (Tarceva)
Anti-EGFR Monoclonal antibody
Cetuximab (Erbitux)
Anti-VEGF Monoclonal antibody
Bevacizumab (Avastin-Altuzan)

34
Erlotinib-With Chemotherapy-First Line - Phase
III

TALENT study - Cisplatin/gemcitabine (tarceva
or placebo)
1172 pts, chemo-naive

Tarceva Placebo
Med. survival (days) 301 309
TTP (days) 167 179
Gatzemeier U. ASCO 2004 Abstract
35
Erlotinib-with chemotherapy-First Line-Phase III

TRIBUTE study - Carboplatin/paclitaxel (tarceva
or placebo)
1059 pts, chemo-naive

Tarceva Placebo
Med. survival (mts) 10.8 10.6
RR () 21.5 19.3
TTP (mts) 5.1 4.9
Herbst R. J Clin Oncol 2005
36
Erlotinib-with chemotherapy-First Line-Phase III

TRIBUTE study Subgroup analysis
Nonsmokers
tarceva vs placebo
Median survival 23 mts vs. 10 mts

Miller VA et al. ASCO 2004 Abstract
37
Why are TALENT and TRIBUTE negative studies?
Possible explanations

Concurrent use may be antagonistic
in vitro evidence of antagonism with combination
chemotherapy regimens
Remarkable benefit in the non-smoker subset
smoking potentially reduces exposure to Tarceva
via induction of metabolising enzymes1
Triplets are redundant doublets Tarceva kills
the same tumour cell population?

1Hamilton M, et al. Proc Am Assoc Cancer Res
200543 (Abs. 6165)
38
Erlotinib Second or Third Line
BR.21 Phase III
39
Erlotinib Second or Third LineBR.21 Phase III
40
Erlotinib Second or Third LineBR.21 Phase III

Tarceva (n488) Placebo (n243)
RR () 8.9 lt1
Median survival 6.7 mts 4.7 mts
PFS 2.2 mts 1.8 mts
En sik yan etki kizariklik, diyare
Shepherd FA et al. NEJM 2005
41
BR.21 Study-Survival
100
Median Survival (mts)
1-year Survival ()
80
Erlotinib Placebo
6.7
31.2
4.7
21.5
60
Survival
HR0.73, Plt0.001
40
20
0
0 5 10 15 20 25 30
Months
42
BR.21 Toxicity
Patients Patients Patients Patients Patients Patients
Erlotinib(n485) Erlotinib(n485) Erlotinib(n485) Placebo(n242) Placebo(n242) Placebo(n242)
Total Grade 3 Grade 4 Total Grade 3 Grade 4
Rash 75 8 lt1 17 0 0
Diarrhea 54 6 lt1 18 lt1 0
Anoreksia 52 8 1 38 5 lt1
Fatigue 52 14 4 45 16 4
Dyspne 41 17 11 35 15 11
Cough 33 4 0 29 2 0
Emesis 33 3 0 24 2 0
Infection 24 4 0 15 2 0
Vomitting 23 2 lt1 19 2 0
Tarceva? (erlotinib) PI.
43
BR.21 Summary

Erlotinib has confered a survival advantage in
previously treated and relapsed NSCLC patients
Erlotinib is effective in both subgroups
Therapy is well tolerated
Most frequent toxicity is rash and diarrhea
Pulmonary toxicity is rare, but 30 fetal

44
BR.21 ISEL
No. of patients 731 1692
Response rate Overall survival 1 year survival HR P value 8.9 Tarceva 6.7 mts Plasebo 4.7 mts 31 vs. 21 0.73 lt0.001 8 Iressa 5.6 mts Plasebo 5.1 mts 27 vs. 22 0.89 0.11
45
Response to TKI- Important factors
Group Response rate () p
Male vs. Female 19 vs. 3 0.001
Asian vs. Non-Asian 27.5 vs. 10.4 0.0023
Adeno. vs. others 13 vs. 4 0.046
BAC vs. adeno 38 vs 14 lt0.001
Nonsmoker vs. smoker 36 vs. 8 lt0.001
Fukuoka JCO 2003212237-46. Kris JAMA
20032902149-58. Miller JCO 2004221103-09.
46
Erlotinib - Faz II Survival Grade of Rash
1.00
Grade 2/3 (n17)
0.75
Survival
0.50
Grade 1 (n26)
Yok (n14)
0.25
0.00
Perez-Soler R, et al. Am Soc Clin Oncol Mol Ther
Symp. 2002
47

NSCLC EGFR Mutations
48
Gefitinib-EGFR mutation and amplification

EGFR EGFR
amplification mutation
- -
33 67 17 83
Obj. response() 36 3
(lt.001) 53 5 (lt.001)
Med. Survival (ay) 18.7 7.0
(.03) 20.8 8.4 (.09)
1 year survival () 57 33
(.03) 57 38 (.22)

Cappuzzo JNCI 97643,2005
49
Targeted Therapies

EGFR Inhibitors
Gefitinib (Iressa)
Erlotinib (Tarceva)
Anti-EGFR Monoclonal antibody
Cetuximab (Erbitux)
Anti-VEGF Monoclonal antibody
Bevacizumab (Avastin-Altuzan)

50
Single agent Cetuximab

Phase II study
(n60, 1 chemo)
Response rate 3.3
Median TTP 2.3 ay
Median survival 8.1 mo.
Well tolerated (Most frequent adverse effect
rash)

Lilenbaum ASCO 2005
51
Cetuximab-with chemotherapy
Docetaxel 75 mg/m2 Every 3
weeks Cetuximab 400 mg/m2 every week then, 250
mg/m2 every week

Patients (no.47)
Stage IIIB/IV
1 previous CT
Median KPS 80
Faz II study

RR 28,SD 17
TTP 3 mts
Well tolerated
(rash, neutropenia)

Kim ES. 2005 ASCO
52
Cetuximab- With chemotherapy
Cisplatin 80 mg/m2 Day 1 Vinorelbin 25
mg/m2 Day 1,8. Every 3 weeks Cetuximab
400 mg/m2 week 1, then 200 mg/m2
week 2 and 3
RANDOMISATION

Patients (No.86)
Stage IV (92)
Chemo-naive
Median KPS 90
Faz II study

Cisplatin 80 mg/m2 Day 1 Vinorelbin 25
mg/m2 Day 1,8 Every 3 weeks
Rosell 2004 ASCO
53
Cetuximab- With chemotherapy
RR () (GA) Median survival (mts) Median TTP (mts)
Cisplatin/Vinor. 20 (7.6-32.4) 7.0 4.2
Cisplatin/Vinor. Cetuximab 32 (17.5-46.0) 8.3 4.7
Rosell 2004 ASCO
54
Targeted Therapies

EGFR Inhibitors
Gefitinib (Iressa)
Erlotinib (Tarceva)
Anti-EGFR Monoclonal antibody
Cetuximab (Erbitux)
Anti-VEGF Monoclonal antibody
Bevacizumab (Avastin-Altuzan)

55
What is VEGF?

Key driver of angiogenesis
Stimulates angiogenic remodelling and sprouting
Stimulates growth of endothelial cells, promotes
endothelial cell survival (i.e prevents
endothelial cell apoptosis and vessel regression)
Also known as VEGF-A
Related molecules are VEGF-B, C and D, placental
growth factor (PlGF)
When angiogenesis is stimulated , a region of the
mature vessel becomes destabilized and undergoes
angiogenic sprouting if VEGF is present
Binds VEGF receptor-2

56
VEGF Receptors

The biological effects of VEGF appear to be
exerted through binding to VEGF receptor-2, which
is expressed predominantly on vascular
endothelial cells
VEGF-2 receptor consists of 7 extracellular Ig
like domains, a transmembrane region and an
intracellular domain having tyrosine kinase
activity

57
VEGF

This binding to trans-membrane receptors
activates
Proliferation of vascular endothelial cells
Migration of vascular endothelial cells
Survival of immature endothelial cells
Increased vascular permeability

58
Angiogenesis

The primary factor controlling vessel formation
is lack of oxygen
This triggers the secretion of pro-angiogenic
factors, principally vacular endothelial growth
factor (VEGF)
TGF alfa/beta, fibroblast growth factor(FGF) are
other two pro-angiogenic growth factors

59
Angiogenesis

Tumor angiogenesis can be considered to
involve two phases
Avascular phase lesions remain dormant and are
not more than 1-2 mm diameter, proliferation and
apoptosis are balanced
Vascularization phase new vessels continue to
form as long the tumor grows

60
Why inhibit angiogenesis in NSCLC?

Angiogenesis plays a role at several stages in
the growth and progression of all types of solid
tumour
tumours are incapable of growth beyond 12mm in
the absence of vasculature1
Expression of high levels of VEGF, the key
mediator of angiogenesis, is associated with poor
prognosis in NSCLC24
Novel combinations of existing chemotherapy
agents are not predicted to provide increased
survival benefit in advanced NSCLC, suggesting
that new therapeutic strategies are required5

1Folkman J. J Natl Cancer Inst 19908246 2Volm
M, et al. Int J Cancer 199774648 3OByrne KJ,
et al. Br J Cancer 200082142732 4Fontanini G,
et al. Br J Cancer 20028655863 5Socinski MA.
Respir Care Clin N Am 2003920736
61
Why inhibit angiogenesis in NSCLC?

Inhibition of angiogenesis, using antiangiogenic
agents has shown to be effective in preventing
tumor growth
In some cases tumor regression has also been
shown
Many antiangiogenic agents are currently in
devolopment, targeting various factors and stages
in the regulation of angiogenesis

62
Anti-angiogenic agents in clinical development
for NSCLC
Drug Mechanism of action Molecular target(s) Stage of development
Bevacizumab Anti-VEGF antibody VEGF Phase III
Sorafenib (BAY43-9006) TKI Raf-1, VEGFR-2, -3, PDGFR-?, Flt-3, c-Kit Phase III
Sunitinib (SU11248) TKI VEGFR-1, -2, -3, Flt-3, PDGFR-?, -?, c-Kit Phase II
Vatalanib (PTK787) TKI VEGFR-1, -2, -3, PDGFR-?, c-Kit, c-Fms Phase II
CP-547,632 TKI VEGFR-2 Phase II
ZD6474 TKI VEGFR-2, -3, EGFR Phase II
AG-013736 TKI VEGFR-1, -2, -3 Phase II
63
Different mechanisms of anti-angiogenesis VEGF
versus VEGF receptor
Monoclonal antibodies against VEGF Inhibitors of VEGF receptor tyrosine kinases
Directly block interaction between VEGF and its receptors Block signalling by activated VEGF receptors
Prevent activation of downstream signals Down-regulate signalling pathways which are already activated
Bind specifically to VEGF Interact with other receptor tyrosine kinases effects are not all specific to angiogenesis inhibition
Specific action on VEGF minimal effects on normal physiology Non-specific action could produce unexpected side effects
Inhibit all functions of VEGF May not inhibit all functions of VEGF
64
Angiogenesis is involved throughout tumour
formation, growth and metastasis
Premalignant stage
Malignant tumour
Tumourgrowth
Vascularinvasion
Dormantmicrometastasis
Overtmetastasis
(Avascular tumour)
(Angiogenicswitch)
(Vascularisedtumour)
(Tumour cellintravasation)
(Seeding indistant organs)
(Secondary angiogenesis)
Stages at which angiogenesis plays a role in
tumour progression
Adapted from Poon RT, et al. J Clin Oncol
200119120725
65
Effects of VEGF inhibitionregression of
microvasculature

Reduction in tumour blood flow after 1 day of
anti-VEGF therapy

Inai T, et al. Am J Pathol 20041653552
66
Effects of VEGF inhibitionnormalisation of
existing vasculature

Abnormal vasculature is normalised following
VEGF inhibition

Inai T, et al. Am J Pathol 20041653552
67
Summary mechanism of action of anti-VEGF therapy
EARLY BENEFIT
CONTINUED BENEFIT
Regression of existing microvasculature
Inhibition of vessel regrowth and
neovascularisation
Normalisation of surviving microvasculature

Inhibition of VEGF may act against tumours in
three ways
regression of existing microvasculature
normalisation of mature vasculature
inhibition of production of new vasculature

68
Bevacizumab
Anti-VEGF antibody (Bevacizumab)
VEGF
VEGFR-1
VEGFR-2
Endothel
Presta et al. Cancer Res. 1997574593.
69
Phase II trial of bevacizumab in NSCLC summary

Addition of bevacizumab to carboplatin and
paclitaxel improved response rate, time to
progression and overall survival in patients with
advanced NSCLC
Patients with non-squamous cell histology appear
to be a subpopulation with improved outcome and
acceptable safety risks
Recommended dose of bevacizumab for further
evaluation is 15mg/kg every 3 weeks
The promising benefit of bevacizumab with
chemotherapy in this trial warrants further
investigation

70
Phase III trial of bevacizumab in NSCLC(ECOG
4599) study design
Previously untreated stage IIIB/IV non-squamous
NSCLC (n878)
CP ? 6 (n444)
PD
Bevacizumab (15mg/kg) every 3 weeks CP ? 6
(n434)
Bevacizumab every 3 weeks until progression
PD

Primary objective to assess overall survival in
patients with advanced non-squamous NSCLC treated
with CP (carboplatin/paclitaxel) versus CP
bevacizumab
Secondary objective to assess response rates,
time to progression and toxicity

Sandler A, et al. J Clin Oncol 200523(Suppl 16
Pt I)2s (Abs. 4)
No cross over will be permitted
71
Phase III trial of bevacizumab in NSCLC(ECOG
4599) key eligibility criteria

Chemotherapy-naïve stage IIIB (pleural or
pericardial effusion only) or stage IV
non-squamous NSCLC
Measurable or non-measurable disease
ECOG PS 01
INR lt1.5 and a PTT no greater than upper limits
of normal within 1 week prior to randomisation
No history of thrombotic or haemorrhagic
disorders
No gross haemoptysis (defined as bright red blood
of a 1/2 teaspoon or more)
Brain metastases were not allowed

Sandler A, et al. J Clin Oncol 200523(Suppl. 16
Pt I)2s (Abs. LBA4)
72
Phase III trial of bevacizumab in NSCLC(ECOG
4599) patient population
CP bevacizumab n424 ()
CPn431 ()

13
14
Stage IIIB
91
91
Measurable disease
28
28
Prior weight loss ?5
43
44
Age ?65 years
40
38
ECOG PS 0
50
58
Male
90
91
Caucasian
Sandler A, et al. J Clin Oncol 200523(Suppl. 16
Pt I)2s (Abs. LBA4)
73
Phase III trial of bevacizumab in NSCLC (E4599)
efficacy
CP CP bevacizumab p value (HR)
Complete response, n () 0 (0) 5 (1.4)
Partial response, n () 35 (10) 92 (25.8)
Overall response rate, n () 35 (10) 97 (27.2) lt0.0001
Median OS (months) 10.2 12.5 0.007 (0.77)
Median PFS (months) 4.5 6.4 lt0.0001 (0.62)
Sandler A, et al. J Clin Oncol 200523(Suppl. 16
Pt I)2s (Abs. 4)
74
ECOG 4599 - Survival
75
ECOG 4599 - PFS
76
Phase III trial of bevacizumab in NSCLC(ECOG
4599) haematological toxicity
CP(n427)Grade 4 CP bevacizumab(n420)Grade 4 p value
Neutropenia () 16.4 24 0.006
Thrombocytopenia () 0 1.4 0.01
Anaemia () 0.7 0 NS
Febrile neutropenia () 1.9 3.3 NS
Includes one death on each arm due to
neutropenic fever
Sandler A, et al. J Clin Oncol 200523(Suppl. 16
Pt I)2s (Abs. LBA4)
77
Phase III trial of bevacizumab in NSCLC(ECOG
4599) non-haematological toxicity

CP

CP bevacizumab

n ()

n ()

gtGrade 3

gtGrade 3

p
value

Haemorrhage

3 (0.7)
19 (4.5)
lt0.00
1
Haemoptysis

1 (0.2)
8 (1.9)
0.04
CNS

0
4 (1.0)
0.03
GI

2 (0.5)
5 (1.2)
NS
Other

1 (0.2)
4 (1.0)
NS
Hypertension

3 (0.7)
25 (6.0)
lt0.001
Ve
nous thrombosis

13 (3.0)
16 (3.8)
NS
Arterial thrombosis

4 (1.0)
8 (1.9)
NS
Sandler A, et al. J Clin Oncol 200523(Suppl. 16
Pt I)2s (Abs. LBA4)
78
Phase III trial of bevacizumab in NSCLC(ECOG
4599) treatment-related deaths
CP

CP bevacizumab

(n427)

(n420)

Haemorrhage

Haemoptysis
0
5

GI bleed
1
2

Neutropenic fever
1
1

Total
2
8
Sandler A, et al. J Clin Oncol 200523(Suppl. 16
Pt I)2s (Abs. LBA4)
79
Phase III trial of bevacizumab in NSCLC(ECOG
4599) conclusions

The addition of bevacizumab (15mg/kg every 3
weeks) to CP improves OS, RR and PFS in patients
with NSCLC
In certain patients, bevacizumab plus CP is
associated with life-threatening and fatal
haemorrhage
event is associated with squamous cell histology
patients with squamous cell NSCLC excluded from
ongoing trials

80
Bevacizumab in first-line advanced NSCLC

Bevacizumab is the first novel agent combined
with standard chemotherapy to significantly
improve overall survival in unselected patients
with advanced NSCLC in the first-line setting
Bevacizumab plus CP is now the ECOG reference
standard for the first-line treatment of advanced
non-squamous NSCLC

81
Bevacizumab ErlotinibPhase II study

Patients (No.40)
Stage IIIB/IV
Nonsquamous type
Previously treated with chemo
Median KPS 80

Erlotinib 150 mg/day Bevacizumab 15mg/kg every 3
weeks

RR 20
Med. survival 12.6 mts
TTP 6.2 mts
Well tolerated

Herbst RS. JCO 2005 232544-55.
82
Recurrent NSCLC Erlotinib ? Bevacizumab
83
Results

Gefitinib does not prolong survival
Erlotinib prolongs survival
There is no advantage when added to standard
chemo
Efficacy is better in nonsmokers, asians,
adenocarcinomas, females
Response rates are higher in patients who have
Exon 19 - 21 mutations and gene amplification
If there is K-ras mutation response rates are
lower

84
Results