CALGB 90401: A randomized double-blind placebo controlled phase III trial comparing docetaxel,

prednisone and placebo with docetaxel, prednisone and bevacizumab in men with metastatic castrate resistant

prostate cancer (mCRPC).

Wm. Kevin Kelly, Susan Halabi, Michael Carducci, Daniel George, John F. Mahoney, Walter M. Stadler, Michael

Morris, Philip Kantoff, Paul Monk, Eric J. Small

for the Cancer and Leukemia Group B (CALGB) and Eastern Cooperative Oncology Group (ECOG)

Role of Vascular Endothelial Growth Factor (VEGF) in CRPC

Lower baseline urinary VEGF levels are associated with improved survival (P = 0.024). (Bok, R. A. et al. Cancer Res 2001;61:2533-2536)

Multivariate model of plasma VEGF levels predicting survival time among 197 CRPC patients(George DJ, et al. Clin Cancer Res. 2001 7:1932-6)

Factor HR P

VEGF(>260 vs ≤260)

2.42 .006

Measurable disease( Y vs N)

2.01 <.001

Alkakine phosphatase(>170 vs ≤170)

1.60 .030

Baseline PSA(>150 vs ≤150)

1.48 .050

Cancer and Leukemia Group B:Phase II Studies in CRPC

Authors N ObjectiveResponse

50% PSA Decline

TTP-PSA(Months)

Median Survival(Months)

Savarese et al.1

EstramustineDocetaxel

47 50% 68% 7 20

Oh et al.2

EstramustineDocetaxelCarboplatin

40 55% 68% 9 18

Picus et al.3

EstramustineDocetaxelBevacizumab

77 59% 75% 8 24

1J Clin Oncol. 2001 May 1;19(9):2509-16 2Cancer. 2003 Dec 15;98(12):2592-83Picus et al. Cancer in press

CALGB 90401

• Primary Objective– To determine if the addition of bevacizumab to

docetaxel and prednisone increases overall survival compared to docetaxel and prednisone alone in patients with CRPC.

• Secondary Objectives– To compare the PFS of these two regimens in patients

with CRPC.– To compare the proportion of patients who experience

50% post-therapy PSA decline from baseline.– To compare proportion of patients who have grade 3 or

higher toxicities

CALGB 90401: Eligibility Criteria • Progressive adenocarcinoma of the prostate by consensus criteria • No prior cytotoxic chemotherapy or anti- angiogenic agents • Four or more weeks since major surgery or radiation therapy• Eight or more weeks from radio-isotope therapy• ECOG performance status of 0-2• Signed Informed Consent

• Patient with HTN were to be well controlled (< 160/90)• No significant history of bleeding within 6 months of registration• No GI perforation or arterial thrombotic event within 12 months

of registration

Required initial laboratory values:

– Absolute neutrophil count: ≥ 1500/ µL– Platelet count ≥ 100,000/ µL – Creatinine ≤ 1.5 x ULN– Bilirubin* ≤ 1.5 x ULN– AST ≤ 1.5 x ULN– PSA ≥ 5 ng/ml (non-measurable ds.)– UPC ratio < 1.0– Serum Testosterone ≤ 50 ng/dl

*Patient with Gilbert’s Disease, ≤ 2.5 x ULN is allowed

CALGB 90401: Eligibility Criteria

CALGB 90401: Stratification Factors

1. Predicted 24 month survival probability using the nomogram developed by Halabi et al*.

• Group 1: < 10%• Group 2: 10-29.9% • Group 3: ≥ 30%

2. Age• < 65 years• ≥ 65 years

3. Prior history of arterial events (cardiac ischemia/infarction, cerebral ischemia, peripheral arterial ischemia or CNS hemorrhage.

• Yes• No

*Halabi et al JCO.2:1232-7, 2003

CALGB 90410: Treatment SchemaR

AN

DO

MIZ

E (1

:1)

RA

ND

OM

IZE

(1:1

)

Arm 2Dexamethasone 8 mg po x 3 doses Docetaxel 75 mg/m2 on day 1 q 21 daysPrednisone 10 mg po dailyPlacebo1 IV on day 1 q 21 days

Arm 1Dexamethasone 8 mg po x 3 dosesDocetaxel 75 mg/m2 on day 1 q 21 daysPrednisone 10 mg po dailyBevacizumab1 15 mg/kg IV on day 1 q 21 days

•ASA 325 mg encouraged in all patients that can tolerate 1In the event of intolerable toxicity to Docetaxel the Bevacizumab\placebo may be continued alone until POD

CALGB 90410: Study Evaluation

Baseline Frequency•Physical exam•Toxicity assessment •Routine chemistry, CBC, Urine protein\creatinine ratio•Prostate specific antigen (PSA)•Testosterone

•Chest x-ray•Bone Scan•CT or MRI of abdomen\pelvis

q cycleq cycleq cycle *q cycle

*Every 3 cycles*Every 3 cycles*Every 3 cycles

*Every 3 months until evidence of progression or relapse for a maximum of 5 years from the time of registration

• Primary endpoint: Overall Survival (OS) • Secondary endpoint:

–50% decline in PSA1

–Progression Free Survival (PFS)1

–Toxicity

• 1050 men randomized • 86% power to detect a hazard ratio (HR) of 1.26 (assume an

increase in median OS from 19 mo. in DP to 24 mo. with DP+B)–Final analysis was based on 748 deaths

• Primary analysis an intent-to-treat approach using the stratified log-rank statistic adjusting for the stratification factors

• Trial was monitored for efficacy and safety by the CALGB DSMB1PSAWG Criteria, J.Clin.Oncol. 22:537-556, 2004

CALGB 90401:Trial Design and Data Analysis

Baseline Clinical Characteristics(N =1050)

May 2005 – December 2007

Arm 1DP + BN=524

Arm 2DP

N=526RaceWhite 88% 87%

Age<6565+ years

34%66%

33%67%

Prior history of arterial eventsYesNo

7%93%

8%92%

24-Month Predicted Survival Probability<10%10%-29.9%30%+

18%34%47%

18%35%47%

ECOG PS 0, 12

96%4%

95%5%

Measurable Disease 48% 52%

Percent on opioid pain medication 35% 35%

Median Number of Treatment Cycles

0 2 4 6 8 10

ARM 1: DB + B

ARM 2: DP

Overall

Bev or Placebo Docetaxel

Range

(0-40)(0-40)

(0-40)(0-40)

(0-38)(0-37)

0 6 12 18 24 30 36 42Time(months)

0.0

0.2

0.4

0.6

0.8

1.0

Ove

rall

Sur

viva

l (pr

obab

ility)

Placebo+DoceBev+Doce, log-rank p=0.181

Kaplan-Meier Overall Survival Curves by Treatment Arm

526 480 390 305 199 100 44 22524 484 417 327 217 117 52 23

Placebo+DoceBev+Doce

Number of Patients at Risk

Median DP = 21.5 (20.0-23.0)Median DPB=22.6 (21.1-24.5) HR= 0.91 (0.78-1.05)

0 6 12 18 24 30 36 42Time(months)

0.0

0.2

0.4

0.6

0.8

1.0

PFS

(pro

babi

lity)

Placebo+DoceBev+Doce, log-rank p<0.0001

Kaplan-Meier PFS Curves by Treatment Arm

526 303 134 75 34 8 4 0524 381 194 97 44 15 5 1

Placebo+DoceBev+Doce

Number of Patients at Risk

Median DP = 7.5 (6.7-8.0)Median DPB=9.9 (9.1-10.6) HR= 0.77 (0.68-0.88)

Secondary Endpoints: Objective Response and 50% Decline in PSA

Clinical Endpoint

Arm 1DP+B

(N=524)

Arm 2 DP

(N=526)

p-value

≥50% decline in PSA(95% CI)

69.5% (65.2-73.5)

57.9% (53.3-62.3)

0.0002

Objective Response(95% CI) (# with measurable disease)

53.2%(46.8-59.6)

(248)

42.1% (36.2-48.2)

(273)

0.0113

DP + B better DP better

Variable

PS0 1

HGB<=12.8>12.8

ALK<=118>118

LDH<=205>205

PSA<=85>85

TEST<=20>20

TotalN = 1050

ARM 1 DP +B

26.716.7

19.3 26.7

27.9 19.7

26.0 19.4

26.6 20.1

22.6 22.8

22.6

Median Survival (months)

Arm 2DP23.817.2

17.0 26.7

26.6 16.3

26.5 16.3

24.5 18.4

19.9 23.4

21.5

HR

0.8320.996

0.8151.045

1.0140.793

1.0190.802

0.8960.892

0.7891.074

0.906

p-value

0.0810.971

0.040.145

0.9020.02

0.870.029

0.3230.267

0.0160.549

0.181

0 0.25 0.5 0.75 1 1.25 1.5 1.75 2

Forest Plot of Overall Survival in Select Subgroups

DP + B better DP better

Variable

PS0 1

HGB<=12.8>12.8

ALK<=118>118

LDH<=205>205

PSA<=85>85

TEST<=20>20

TotalN = 1050

ARM 1 DP +B

26.716.7

19.3 26.7

27.9 19.7

26.0 19.4

26.6 20.1

22.6 22.8

22.6

Median Survival (months)

Arm 2DP23.817.2

17.0 26.7

26.6 16.3

26.5 16.3

24.5 18.4

19.9 23.4

21.5

HR

0.8320.996

0.8151.045

1.0140.793

1.0190.802

0.8960.892

0.7891.074

0.906

p-value

0.0810.971

0.040.145

0.9020.02

0.870.029

0.3230.267

0.0160.549

0.181

0 0.25 0.5 0.75 1 1.25 1.5 1.75 2

Forest Plot of Overall Survival in Select Subgroups

Significant Grade ≥ 3 Adverse Events

ARM 1DP +B

ARM 2DP

Neutrophils 30% 24%Fatigue 18% 10%Leukocytes 17% 13%Febrile Neutropenia 7% 4%Hypertension 7% 1%Hemorrhage, GI 6% 2%GI, Perforation 4% 0%Mucositis\stomatitis 3% 0%Pneumonitis 2% 0%Thrombosis\embolism 4% 7%

Adverse Events Summary

Arm Grade 3# (%)

Grade 4# (%)

*Grade 5# (%)

Maximum Hematologic AE DP + BDP

11%12%

24%17%

0%0%

Maximum non-Hematologic AE

DP + BDP

53%35%

11%10%

3.8%1.1%

Maximum Overall AE DP + BDP

41%31%

30%23%

3.8%1.1%

* Infection major cause of treatment related deaths

Conclusions• The addition of bevacizumab to docetaxel/prednisone

did not significantly prolong survival in men with metastatic CRPC, although a trend towards improved survival was observed (22.6 vs 21.5 m, p = 0.18).

• The addition of bevacizumab to docetaxel/prednisone DID have a significant impact on:PFS 9.9 mo. vs. 7.5 mo. p < 0.0001 Objective RR 53.2% vs. 42.1% p= 0.0113PSA decline ≥ 50% 69.5% vs. 57.9% p= 0.0002

Conclusions• OS with docetaxel/prednisone is longer than previously reported (21.5

mos vs 19.2 mos in TAX327) and may be due to:•Stage migration•A good risk population (47% of pts had a 24 mo predicted survival of > 30%)

• Discrepancy between OS and other markers of clinical benefit such as PFS and RR may be due to:

•Impact of longer-than-expected survival in the control group on power calculations

•Impact of subsequent therapy on OS•True disconnect between PFS/RR and OS

Discordance between OS and PFS\overall response

• The addition of bevacizumab to docetaxel/prednisone resulted in more severe toxicities.

• The role of anti-angiogenic therapeutics in metastatic CRPC remains to be defined.

• Exploratory analysis of patient subsets that may have a clinical benefit from bevacizumab are underway.

Conclusions

Acknowledgements

• Patients and families that participated in the study

• All colleagues and investigators that contributed to the success of CALGB 90401.

• Cancer and Leukemia Group B central office and

statistical staff– Eleanor Leung, Ellen Kaplan, Jennifer Williams, John

Taylor

Thank You