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Antiangiogénicos de segunda generación
Dra. Marga Majem
Hospital de la Santa Creu i Sant Pau Barcelona
AGENDA
• Introduction
• Tumor angiogenesis
• Antiangiogenic agents
– Bevacizumab
– New antiangiogenics
• Ramucirumab
• Nintedanib
• Who benefits most from the antiangiogenic strategies?
• Lung cancer is the leading cause of cancer-related mortality worldwide, with about 85% patients diagnosed NSCLC.
• Locally advanced or metastatic NSCLC accounts for 80% patients. 5-year survival rates for patients with stage IV NSCLC is < 5%.
• The standard care for advanced NSCLC is CT, which prolongs survival, controls symptoms and improves quality of life. Regardless of the emergence of new agents, CT provides only marginal benefit in overall survival.
• Another treatment option is to inhibit tumor angiogenesis (tumor-associated vasculature).
INTRODUCTION
• Essential for the development and
progression of malignant tumours.
• Tumor-associated vessels provide
oxygen and nutrients that favor tumor
growth and favor tumor metastasis.
• VEGF pathway: one of the best
characterized proangiogenic pathways
stimulate downstream signaling
cascades that coordinate endothelial cell
proliferation, differentiation,
permeability and migration to
generate new blood vessels
TUMOR ANGIOGENESIS
• The fibroblast growth factor (FGF) and platelet-derived growth factor (PDGF) signaling pathways might be involved in adaptive resistance to VEGF therapy
ANTIANGIOGENIC AGENTS
Nintedanib
Inhibition of VEGF ligand • Blocks VEGF binding • Inhibits signaling due to
VEGF(s) Antibody to VEGFR-2 •Blocks ligand binding •Blocks receptor activation and signaling
Tyrosine kinase inhibitor to VEGFR. •Blocks receptor kinase activity and signaling
Inhibition of VEGF ligand
• Bevacizumab: humanized monoclonal antibody that binds to VEGF.
• Aflibercept: recombinant human fusion protein (VEGF-trap) that binds to VEGF and
PlGF.
Antibody to VEGFR-2
• Ramucirumab, a fully human monoclonal antibody that specifically binds VEGFR2.
Tyrosine kinase inhibitor to VEGFR-2
• Simultaneous inhibition of other pathways concerning angiogenesis and tumor
proliferation: PDGF, FGF, EGF,...
• Multi-targeted antiangiogenic tyrosine kinase inhibitors:
– Sunitinib: inhibits VEGF1–3, PDGFR-a and b, and RET.
– Sorafenib: inhibits VEGFR2–3, PDGFR-b, c-kit, Raf and flt-3.
– Cediranib: inhibits VEGFR1–3, PDGFR-a/b, FGFR1 and c-kit.
– Vandetanib: inhibits VEGFR2 and 3, RET and EGFR.
– Motesanib: inhibits VEGFR1–3, PDGFR, c-kit and RET.
– Nintedanib: inhibits VEGF1–3, PDGF-a/b, and FGFR1–3
– Axitinib: inhibits VEGFR1–3, PDGFR-b and c-kit.
– Pazopanib: inhibits VEGFR1–3, PDGFR-a/b and c-kit.
– Linifanib: inhibits VEGFR1–3, PDGFR-b, c-Kit and FLT-3.
ANTIANGIOGENIC AGENTS
Inhibition of VEGF ligand
• Bevacizumab: humanized monoclonal antibody that binds to VEGF.
• Aflibercept: recombinant human fusion protein (VEGF-trap) that binds to VEGF and PlGF.
Antibody to VEGFR-2
• Ramucirumab, a fully human monoclonal antibody that specifically binds VEGFR2.
Tyrosine kinase inhibitor to VEGFR-2
• Simultaneous inhibition of other pathways concerning angiogenesis and tumor
proliferation: PDGF, FGF, EGF,...
• Multi-targeted antiangiogenic tyrosine kinase inhibitors:
– Sunitinib: inhibits VEGF1–3, PDGFR-a and b, and RET.
– Sorafenib: inhibits VEGFR2–3, PDGFR-b, c-kit, Raf and flt-3.
– Cediranib: inhibits VEGFR1–3, PDGFR-a/b, FGFR1 and c-kit.
– Vandetanib: inhibits VEGFR2 and 3, RET and EGFR.
– Motesanib: inhibits VEGFR1–3, PDGFR, c-kit and RET.
– Nintedanib: inhibits VEGF1–3, PDGF-a/b, and FGFR1–3
– Axitinib: inhibits VEGFR1–3, PDGFR-b and c-kit.
– Pazopanib: inhibits VEGFR1–3, PDGFR-a/b and c-kit.
– Linifanib: inhibits VEGFR1–3, PDGFR-b, c-Kit and FLT-3.
ANTIANGIOGENIC AGENTS
Bevacizumab
• Humanized monoclonal antibody that binds to VEGF.
• The only antiangiogenic agent approved for the first-line treatment of
NSCLC.
• Restricted to patients with non-squamous NSCLC (70% of patients)
Bevacizumab in first-line + CT
BEVACIZUMAB. New roles
Maintenance beyond progression:
• AvaALL trial: phase III, patients with advanced non-squamous NSCLC who
have progressed following bevacizumab plus platinum-based CT to
standard second-line therapy with or without bevacizumab.
• Primary end-point: overall survival.
Adjuvant setting:
• ECOG E1505: impact of adding bevacizumab to adjuvant chemotherapy in
patients with completely resected stage IB–IIIA NSCLC.
EGFR mutation:
• Bevacizumab + Erlotinib fase II trial. JO 25567 trial
• Ramucirumab
• Nintedanib
NEW ANTIANGIOGENICS IN NSCLC.
NEW ANTIANGIOGENICS IN NSCLC. Ramucirumab
• RAMUCIRUMAB (LY3009806):
– Fully human IgG1 monoclonal Ab.
– Selectively blocks VEGFR-2.
• VEGFR-2 signaling:
– Involved in proliferation, migration, and survival of endothelial cells
– Mediating the increased endothelial permeability associated with cancer
angiogenesis.
• Ramucirumab inhibit VEGF ligand binding and subsequent activation and
downstream signaling of pathways (permeability, migration, and proliferation)
RAMUCIRUMAB in second-line + CT
Med OS: 10.5m (R) vs 9.1m (P)
RESPONSE RATE
PFS
Med PFS: 4,5 m (R) vs 3,0 m (P)
Med PFS: 4,5 m (R) vs 3,0 m (P)
Med OS: 10.5m (R) vs 9.1m (P)
RESPONSE RATE
PFS OVERALL SURVIVAL
Med OS: 10,5 m (R) vs 9.1 m (P)
Med OS: 11.1 m (R) vs 9.7 m (P) Med OS: 9.5 m (R) vs 8.2 m (P)
Comments to the REVEL trial
• REVEL met its primary endpoint of OS improvement in the total population (including ADK and SCC). Also RAM+DOC showed significant improvement in PFS and ORR compared to PL+DOC.
• Better outcome of the control group: Only PS 0-1.
• Exclusion criteria excluded patients at increased risk from anti-angiogenic therapy (major blood vessel encasement or invasion and intratumour cavitation) able for docetaxel.
• The addition of RAM to DOC did not result in an increase of SAEs and AEs leading to death.
• Safety profile was as expected for an anti-VEGFR agent.
• Ramucirumab
• Nintedanib
SECOND GENERATION ANTIANGIOGENICS.
1. Hilberg F, et al. Cancer Res 2008;68:4774–8; 2. Boehringer Ingelheim Data on file; 3. Stopfer P, et al. Xenobiotica. 2011;41:297–311; 4. Bousquet G, et al. Br
J Cancer 2011;105:1640–5; 5. Ellis PM, et al. Clin Cancer Res 2010;16:2881–9; 6. Doebele RC, et al. Ann Oncol 2012;23:2094–102.
IC50
(nmol/L)
VEGFR
1 / 2 / 3
34/ 21/ 13
PDGFR
α / β
59/ 65
FGFR
1 / 2 / 3
69/ 37/ 108
NINTEDANIB in LUNG CANCER
• Nintedanib inhibits VEGFR, PDGFR y FGFR, all participating in angiogenesis.
• Inhinition of VEGFR and FGFR new vessels
• Inhibition of FGFR y PDGFR former vessels
NINTEDANIB in second-line + CT
Nintedanib 200mg BID PO, D2–21, + Docetaxel 75mg/m2 IV, D1,
21-day cycles (n=655)
Placebo BID PO, D2–21, + Docetaxel 75mg/m2 IV, D1,
21-day cycles (n=659)
N=1314
RANDOMISE
•Stage IIIB/IV* or recurrent NSCLC
•Failed 1st-line chemotherapy
•Any histology
•ECOG PS 0 or 1
•No prior docetaxel or VEGF/VEGFR inhibitors**
•No active brain metastases
1:1
PD
PD
Number of docetaxel cycles not restricted Monotherapy allowed after ≥4 cycles of combination therapy
** Other than bevacizumab
EXCLUSION CRITERIA: • Active Brain Mets • Cavitary/ necrotic tumours, centrally located tumours with radiographic
evidence of invasion of major blood vessels
• Recent history of clinically signifi cant haemoptysis or a major thrombotic. • Clinically relevant major bleeding event
Primary endpoint:
PFS by independent central
review
Key secondary endpoint: OS
pre-planned analyses of
adenocarcinoma and ITT
LUME-Lung 1: hierarchical analysis used to reduce error rate and maintain power for the
important OS endpoint
*Hanna N, et al. ASCO 2013. Abstract #8034; Hanna N, et al. ESMO 2013. Abstract #3418;
Kaiser R, et al. ESMO 2013. Abstract #3479.
Reck M, et al. Lancet Oncol 2014;15:143–155.
Prim
ary
en
dp
oin
t K
ey s
eco
nd
ary
en
dp
oin
t
Independently
assessed PFS All histologies
OS
Adenocarcinoma
Time since start of first-
line therapy <9 months
OS
All adenocarcinoma
OS
All histologies
Significant
finding for
PFS at time
of OS
Significant
finding
Significant
finding
Previously analysed trial, LUME-Lung 2, showed enhanced benefit in early progressing
adenocarcinoma tumours, so stepwise testing was used to preserve power and reduce error*
PATIENT CHARACTERISTICS
RESPONSE RATE
PFS total population: 3.4 months vs 2.7 months;
HR 0·79 (95% CI 0.68–0.92), p=0.0019).
PFS Adenocarcinoma: 4,0 months vs 2.8 months;
HR 0.77, (95%CI 0.62–0.96), p=0.0193
PFS Squamous: 2,9 months vs 2.6 months;
HR 0.77, (95% CI 0.62–0.96), p=0.0200
Progression Free Survival
ADK PD<9m: 10.9 months vs 7.9 months; HR 0.75 (95% CI 0.60–0.92), p=0.0073.
(PFS 4.2 months vs 1.5 months;
HR 0·68 [95% CI 0·54–0·84], p=0.0005).
All ADK: 12.6 months vs 10.3 months; HR 0·83 (95% CI 0.70–0.99), p=0.0359.
Total: 10.1 months vs 9.1 months; HR 0.94 (95% CI 0.83–1.05), p=0.2720.
Overall Survival
33
45
40
35
30
25
20
15
10
5
0
Pa
tie
nts
(%
)
All CTCAE grades ≥15% incidence
CTCAE grades ≥3 ≥1% incidence
Nintedanib + docetaxel
Placebo + docetaxel
50
45
40
35
30
25
20
15
10
5
0
50
Patients with AE, %
Nintedanib +
docetaxel (n=652)
Placebo +
docetaxel (n=655)
Any AE leading to discontinuation 22.7 21.7
Any serious AE 34.4 31.5
VEGF/VEGFR inhibitor-associated adverse events P
ati
en
ts (
%)
20
15
10
5
0
20
15
10
5
0
Nintedanib + docetaxel
Placebo + docetaxel
CTCAE Grade ≥3 (%)
All CTCAE grades (%)
Nintedanib + docetaxel
Placebo + docetaxel
EJC; 17 December 2014
No differences in cough, dyspnoea, pain
between the two arms
No differences in function scores
between the two arms
The significant improvement in PFS and
the significant OS benefit in
adenocarcinoma with nintedanib +
docetaxel had no detrimental effect on
patient-reported QoL.
• Docetaxel plus Nintedanib significantly improved PFS independently of histology in second line NSCLC patients.
• There is evidence of improved OS in patients with adenocarcinoma including those patients with a poor prognosis (refractory to first-line CT or had a very short response).
• This may reflect the biologic mechanism behind tumor progression fast-progressing tumors are more dependent on new vasculature that are driven by growth factors where Nintedanib works on.
• The significant improvement in PFS and the significant OS benefit in adenocarcinoma with Nintedanib + docetaxel had no detrimental effect on patient-reported QoL.
Comments to the LUME-Lung 1 trial
Who benefits most from the antiangiogenic strategies?
• ECOG PS 0-1.
• < 65 years (65% REVEL, LUME-Lung 1)
• Adenocarcinoma histology. – Bevacizumab
– Ramucirumab (subgroup analysis)
– Nintedanib
• No/stable BRAIN Mets.
• Patients that not meet Key exclusion criteria for antiangiogenics: – Cavitary/ necrotic tumours, radiographic evidence of invasion of major blood vessels.
– Recent significant haemoptysis / bleeding.
– Therapeutic anticoagulation.
• Patients with a poor prognosis (refractory or very short response) – Nintedanib.
• Second line: Previous Bevacizumab is allowed.
Who benefit most from the antiangiogenic strategies?
Predictive factors for antiangiogenic therapy
• To date, no validated biomarker has been identified for any angiogenesis inhibitor. Several studies in various cancer types have failed to identify a relevant biomarker for antiangiogenic drugs.
• A major challenge is to develop robust biomarkers that can guide selection of patients for whom antiangiogenic therapy is most beneficial.
• In the absence of a predictive biomarker, which patients will benefit from antiangiogenics is not known.
CONCLUSIONS
• To identify a useful biomarker that allow us to determine specific patients who might benefit from antiangiogenics is crucial to do a step forward in the antiangiogenic strategies.
Antiangiogénicos de segunda generación
Dra. Marga Majem
Hospital de la Santa Creu i Sant Pau Barcelona
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