Cholangiocarcinoma

A U B H O 2 0 1 5 , B A N G K O K , T H A I L A N D
R A C H N A T . S H R O F F , M D , M S
A S S I S T A N T P R O F E S S O R ,
D E P T O F G I M E D I C A L O N C O L O G Y
M . D . A N D E R S O N C A N C E R C E N T E R
R S H R O F F @ M D A N D E R S O N . O R G
Cholangiocarcinoma:
Changing the landscape for a rare
disease

Outline
 Overview of the disease
 Second-line therapy
 Retrospective data
 Phase Ib of pazopanib and trametinib
 The role of radiation
 Retrospective data
 Next steps
 Next generation sequencing for cholangiocarcinoma
 Profiling data
 Clinical trials at MD Anderson

The Magnitude of the Problem: U.S. Data
 >7,000 cases annually in 2009
 5-year survival is <15%
 Most patients present with locally advanced or metastatic
disease
 Treatment commonly administered in the community,
at low-volume centers.

Risk factors
 Obesity, Metabolic Syndrome
 Chronic inflammation (hepatitis, ETOH, smoking,
occupational)
 Parasitic infections
 Primary sclerosing cholangitis, Crohns disease
 Cysts, anomalous pancreatobiliary ducts
 Biliary polyps (>10 mm)

Rising incidence
J Hepatol. 2004;40(3):472-7

Cholangiocarcinoma: Site of Disease
Hilar Intrahepatic

Localized Cholangiocarcinoma
 Surgical resection is the standard of care
 Post operative radiation/ chemoradiation therapy improves
recurrence-free survival in R1 disease
 Role of adjuvant therapy in R0 resection is debatable
 Role of liver transplantation in unresectable hilar
cholangiocarcinoma.
NCCN Guidelines

Advanced biliary tract cancers
 Disease-related factors
 Uncommon malignancies
 Unwell, elderly population, infection/obstruction
 Histological / cytological confirmation difficult
 Lack of evidence
 Disease often not measurable
 Primarily small phase II and one phase III study of
gemcitabine-based combinations

ABC-02 - Study schema
Eligible patients (n=400*)
Arm A
Gem 1000 mg/m2 D1,8,15 q
28d, 24 weeks (6 cycles)
Arm B
Cisplatin 25 mg/m2
+ Gem 1000 mg/m2
24 weeks (8 cycles)
Randomized 1:1
(stratified by centre, primary site, PS, prior
therapy and locally advanced vs. metastatic)
Upon disease progression, management will be on clinician’s
discretion (mostly best supportive care)
D1,8 q 21d
+ QoL

Result
Gem
n (%)
Gem + Cis
n (%)
Not assessed * 74 (36%) 56 (27%)
Assessed * 132 (64%) 148 (73%)
Complete Response 1 (0.8%) 1 (0.7%)
Partial Response 20 (15.2%) 37 (25.0%)
Stable Disease 73 (55.3%) 79 (53.4%)
Progressive Disease 33 (25.0%) 28 (18.9%)
CR + PR + SD 94 (71.2%) 117 (79.1%)
p-value 0.256
* Patients not required to have measurable disease at study entry,
some patients still in follow-up
Radiologic Response

ABC-02 - Results:
Overall Survival (ITT)
Treatment arm Gem Gem + Cis
Number of patients n=206 n=204
Deaths n(%) 141 (68.5) 122 (59.8)
Median survival (mo) 8.3 11.7
Log rank p value 0.002
Hazard ratio (95% CI) 0.70 (0.54, 0.89)

ABC-02 Conclusions
 Cisplatin and gemcitabine significantly improves overall
survival compared with gemcitabine monotherapy (11.7
vs. 8.3 months)
 Benefit gained with no clinically significant added toxicity
 CisGem is recommended as a worldwide standard of care
and the backbone for further studies
 Caution required in patients with PS > 2

Agents Target Patients RR PFS Author
Combination Regimens First line therapy
GEMOX-
cetuximab
EGFR 51 - 61% (4 mths) Malka
GEMOX-
bevacizumab
VEGF 35 40
7 months
(median)
Zhu
Single Agent Regimens First or Second line
AZD6244
MEK1/2 22 14
5.4 months
(median)
Bekaii-Saab
Erlotinib
EGFR 43 7
2.6 months
(median)
Philip et al
Lapatinib
EGFR/HER2 17 0
1.8 months
(median)
Ramanathan
Sorafenib
BRAF/VEGFR 36 6
2 months
(median)
El-Khoueiry
Sorafenib
BRAF/VEGFR 46 2
2.3 months
(median)
Bengala
Zhu et al, JCO, 2009

Phase III GEMOX + Erlotinib
268 pts randomized: GEMOX +
Erlotinib
PR higher in erlotinib group (40
vs. 21, p=0.005)
Higher PFS with erlotinib (5·9
months vs 3·0 months) (p=0·049)
Median overall survival was the
same in both groups
Lancet Oncol. 2012;13(2):181-8.

Gastrointest Cancer Res. 2011;4(5-6):155-60.
First line regimens at MD Anderson

Second-line therapy
 Retrospective review of MD Anderson experience:
 Patients with advanced cholangiocarcinoma who received 2nd
line therapy from 2009-2012
 56 patients evaluated, majority were intrahepatic
cholangiocarcinoma
 Primary objective: PFS with second-line therapy
 Secondary objectives: OS, disease control rate
 80% received gemcitabine-based first-line therapy
 Majority of patients received 5-fluorouracil in the second-line
setting

Second-line therapy
Rogers JE, et al. J Gastrointest Oncol 2014
Median PFS: 2.7 months
Median OS: 13.8 months
DCR: 50%

Pazopanib and trametinib – a phase Ib study
 Collaboration between MD Anderson and Johns
Hopkins
 Phase I showed one prolonged PR and one SD with
cholangiocarcinoma
 Expansion to 25 patients (MD Anderson n = 18)
 Primary endpoint: PFS
 Secondary endpoints: OS, RR, DCR
 Highly refractory population (median # prior
therapies: 2)
 Median follow-up: 8.9 months
Shroff RT, et al, ASCO Annual Meeting 2015

Pazopanib and trametinib – a phase Ib study
 Overall response rate – 5%
 Disease control rate – 75% (15/20 patients)
 Median PFS 4.3 months
 4-month PFS – 56%
 p<0.002 compared with a pre-specified null hypothesis rate of
25%
 Median OS was 6.7 mths
 Next steps: In development

The role of radiation
 Retrospective review of MD Anderson experience
 114 patients from 2009-2013, majority intrahepatic
 Primary objectives
 Determine first-line therapy given to unresectable
cholangiocarcinoma (uCC) patients
 Determine the percentage of patients that received chemoradiation
(CRT)
 Secondary objectives
 Disease response with first-line therapy
 Evaluate the median number of chemotherapy cycles received prior
to CRT
 Duration of CRT control
 Progression-free survival (PFS) with or without CRT
 Overall survival (OS) with or without CRT
Rogers JE, et al, Cholangiocarcinoma Foundation Annual Meeting 2015

 66% received gemcitabine plus platinum (cisplatin or
oxaliplatin)
First-Line Therapy Percentage
Gemcitabine + Cisplatin 63.2 %
Gemcitabine + Cisplatin +
Erlotinib
5.3%
Gemcitabine monotherapy 3.5%
Others (Gemcitabine +
capecitabine; Gemcitabine +
Oxaliplatin, etc)
11.4%
CRT 16.7%
Shroff RT, et al, Cholangiocarcinoma Foundation Annual Meeting 2015

Patient group Median PFS (95% CI) Median OS (95% CI)
No CRT
(N= 40)
11.4 months (9.1-15.3) 22.4 months (12.6-37.5)
CRT
(N =74)
14.5 months (12.1-16.6) 29.4 months (23.8-38.2)
CRT with disease control
on first-line treatment
(N= 62)
15.7 months (13.5-19.0) 32.0 months (24.0-44.1)
CRT with progression on
first-line treatment
(N=12)
4.2 months (2.3-9.0) 6.9 months (7.0-30.2)

The role of radiation - PFS
0.00
0.25
0.50
0.75
1.00
0 12 24 36 48 60 72 84 96
Months
No CRT
CRT
p = 0.105
Progression-free Survival
0.00
0.25
0.50
0.75
1.00
ProportionProgression-free
0 12 24 36 48 60 72 84 96
Months
No CRT
CRT with First-line Treatment Disease Control
CRT with First-line Treatment Progression
p < 0.001
Progression-free Survival
CRT vs. No CRT: 14.5 vs. 11.4 mths
CRT (DC) vs. CRT (PD): 15.7 vs. 4.2 mths

The role of radiation - OS
0.00
0.25
0.50
0.75
1.00
0 12 24 36 48 60 72 84 96
Months
No CRT
CRT
p = 0.005
Overall Survival
0.00
0.25
0.50
0.75
1.00
ProportionSurviving
0 12 24 36 48 60 72 84 96
Months
No CRT
CRT with First-line Treatment Disease Control
CRT with First-line Treatment Progression
p = 0.001
Overall Survival
CRT vs. No CRT: 29.4 vs. 22.4 mths
CRT (DC) vs. CRT (PD): 32 vs. 6.9 mths

Unresectable
Cholangiocarcinoma
-liver confined
-no cirrhosis or CPC A
-up to 2 satellite lesions
-12 cm or less
Stratify:
Largest tumor > 6 cm
-satellite y/n
Gem/Cis x 4
Liver Directed Radiation
Therapy
Followed by maintenance
Gem/Cis x 4
Gem/Cis x 4
Re-staging
AND
Randomization
after cycle 3
Radiation
Planning
during cycle 4
NRG GI-001 Phase III Trial
Hong, PI, Activated 8/2014

Next generation sequencing (NGS)
 NGS on all cholangiocarcinoma patients with
available tissue
 Standard practice at MD Anderson since 2013
 Important differences between intrahepatic and
extrahepatic cholangiocarcinoma
 75 patients
Churi CR, et al. PLoS One 2014.

Next generation sequencing (NGS)

Next generation sequencing (NGS) –
BRAF inhibition

MD Anderson Approach
Unresectable Cholangiocarcinoma
Localized
Induction Chemo
followed by
ChemoRT
Disseminated
Systemic
Chemotherapy
NGS
Add targeted agents
based on molecular
phenotype
Clinical trials:
GAP
FGFR Inhibitor
Radiation Therapy
Select cases
with SD/PR> 6
mos on chemo,
consider OLT
(investigational)

Clinical Trials at MD Anderson
 First-line therapy
 GAP trial – multicenter, phase II study of Nab-Paclitaxel with
gemcitabine and cisplatin in advanced, untreated biliary cancers
 15 of 50 patients enrolled thus far and all remain on study
 Therapy for refractory disease
 Ramucirumab for advanced biliary cancers
 FGFR inhibitor for patients with known FGFR alterations
 IDH inhibitors for IDH1 and IDH2 mutations
 Pilot study with anti-PD-1 planned
 Radiation therapy
 NRG-GI001
 Pre-clinical work
 PDX models
 BAP1, KRAS mutant models

Q U E S T I O N S ?
Thank you!

Cholangiocarcinoma

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