2. Letter from Prof Rolf Stahel
Dear Colleagues It is my pleasure to present this ETOP slide set which has been designed to highlight and summarise key findings in thoracic cancers from the major congresses in This slide set specifically focuses on the ESMO 2016 Congress and is available in 4 languages – English, French, Japanese and Chinese. The area of clinical research in oncology is a challenging and ever changing environment. Within this environment we all value access to scientific data and research which helps to educate and inspire further advancements in our roles as scientists, clinicians and educators. I hope you find this review of the latest developments in thoracic cancers of benefit to you in your practice. If you would like to share your thoughts with us we would welcome your comments. Please send any correspondence to I would like to thank our ETOP members Drs Solange Peters and Martin Reck for their roles as Editors – for prioritising abstracts and reviewing slide content. The slide set you see before you would not be possible without their commitment and hard work. And finally, we are also very grateful to Lilly Oncology for their financial, administerial and logistical support in the realisation of this complex yet rewarding activity. Yours sincerely, Rolf Stahel President, ETOP Foundation Council

3. ETOP Medical Oncology Slide Deck Editors 2016
Focus: Advanced NSCLC (not radically treatable stage III & stage IV) and related biomarker data
Dr Solange Peters
Multidisciplinary Oncology Center, Lausanne Cancer Center, Lausanne, Switzerland
Focus: Early and locally advanced NSCLC (stage I–III) and related biomarker data / other malignancies
Dr Martin Reck
Department of Thoracic Oncology, Hospital Grosshansdorf, Grosshansdorf, Germany

4. Contents Biomarkers and screening
Early stage and locally advanced NSCLC – Stages I, II and III
Advanced NSCLC – Not radically treatable stage III and stage IV
1st line
Later lines
Other malignancies
SCLC and mesothelioma
Rare tumours

5. Biomarkers and screening

6. 1055O: Changes in serum IL8 levels reflect and predict response to anti-PD-1 treatment in melanoma and non-small cell lung cancer patients – Sanmamed MF, et al
Study objective
To evaluate the use of serum IL-8 as a biomarker during anti-PD-1 mAb treatment of metastatic melanoma and NSCLC patients
Methods
Serum IL-8 levels were determined in 44 metastatic melanoma and 19 metastatic NSCLC patients undergoing anti-PD-1 mAb therapy
Key results
In responding NSCLC patients, compared with baseline levels (16.3 pg/mL), serum IL-8 levels decreased significantly at the moment of best response (6 pg/mL; p<0.05) and increased upon progression (53 pg/mL; NS)
In non-responding NSCLC patients, IL-8 levels significantly increased at the moment of progression vs. baseline levels (51 vs. 12 pg/mL; p<0.05)
Changes in serum IL-8 levels are associated with OS in NSCLC, change <9.2% vs. >9.2% HR 7.7 (95%CI 1.1, 55.8); p=0.004
Conclusions
Changes in serum IL-8 levels reflect the response to anti-PD-1 mAbs in melanoma and NSCLC patients
Early decrease in serum IL-8 levels is associated with longer survival in metastatic melanoma and NSCLC patients treated with anti-PD-1 mAbs
Sanmamed et al. Ann Oncol 2016; 27 (suppl 6): abstr 1055O

7. 1521PD: Clinical evaluation of the utility of a liquid biopsy (circulating tumoral cells and ctDNA) to determine the mutational profile (EGFR, KRAS, ALK, ROS1 and BRAF) in advanced NSCLC patients – Barrera L, et al
Study objective
To assess the utility of a liquid biopsy for mutation detection in advanced NSCLC
Methods
Patients with advanced NSCLC who had either a new diagnosis or developed resistance to an EGFR TKI were eligible for inclusion
62 patients were screened for EGFR, KRAS, ROS1, ALK and BRAF mutations via plasma genotyping (by the Target-SelectorTM ctDNA assay) and compared with tissue biopsies
Key results
The plasma assay showed a 90% (95%CI 82.83, 95.10) sensitivity for the detection of EGFR mutations and 100% (95%CI 96.38, 100) specificity
Of those who were enrolled with EGFR TKI resistance (n=52), 57% of those with polymetastatic disease had a T790M mutation, while 16% of those with oligometastatic disease had a T790M mutation, and none with loco-regional disease
Conclusion
EGFR mutations can be rapidly detected with a noninvasive ctDNA assay; however, conclusions regarding other driver alterations will require additional data
Barrera et al. Ann Oncol 2016; 27 (suppl 6): abstr 1521PD

8. 1202O: Clinical and biological characteristics of non-small cell lung cancer (NSCLC) harbouring EGFR mutation: Results of the nationwide programme of the French Cooperative Thoracic Intergroup (IFCT) – Leduc C, et al
Study objective
To analyse the EGFR mutation status of patients with EGFR-mutated NSCLC
Methods
The Biomarkers France database (containing data on 17,664 patients at time of study) was used to identify patients with EGFR-mutated NSCLC
Overall, 1837 (10.3%) patients were eligible for inclusion in this analysis
Key results
EGFR mutations were identified as follows:
Exon 18: 102 (5.6%) patients
Exon 19: 931 (50.6%) patients
Exon 20: 102 (5.6%) patients
Exon 21: 702 (38.2%) patients
70 of these mutations were novel
There was a higher proportion of smokers displaying exon 18 (20%) or exon 20 (19%) mutations compared with exon 19 (11%) or exon 21 (11%) (p=0.002)
In total, 226 patients had a personal history of cancer; this was not linked to exon mutation status
Patients displaying a T790M mutation were excluded from the survival analysis
Median follow-up time was 36.7 (36.4–37) months
Leduc et al. Ann Oncol 2016; 27 (suppl 6): abstr 1202O

9. 1202O: Clinical and biological characteristics of non-small cell lung cancer (NSCLC) harbouring EGFR mutation: Results of the nationwide programme of the French Cooperative Thoracic Intergroup (IFCT) – Leduc C, et al
Key results (cont.)
Median OS improved for exon 19 deletions vs. L858 mutations (26.5 vs months, p=0.045); deletion length had no impact on OS
For exon 21, median OS was longer for L858R compared with L861Q, other substitutions or wild-type (22.4 vs vs vs. 11.8, respectively; p<0.0001)
For mutations further classified as common, rare or complex, DCR was 82%, 77% and 54.5%, respectively, under first-line EGFR-TKI therapy (p=0.05)
No difference in DCR under EGFR-TKI therapy was observed according to mutation type for exon 19 or 21
Conclusions
Distinct clinical characteristics were observed for common and uncommon EGFR mutations
Patients with common exon 19 mutations tended to have better outcomes
Wild-type
Exon 18
Exon 19
Exon 20
Exon 21
p-value
OS, months [95%CI]
11.8 [10.1, 13.3] (n=1270)
14.2 [12.4, NR] (n=44)
27.0 [23.4, 29.1] (n=555)
16.0 [8.1, 19.1] (n=50)
21.3 [18.5, 27.8] (n=439)
<0.001
PFS (first-line EGFR TKI), months [95%CI]
7.2 [6.3, 7.9] (n=1243)
12.4 [5.8, NR] (n=44)
16.3 [13.9, 18.0] (n=560)
6.4 [2.9, 9.0] (n=48)
13.7 [11.6, 16.1] (n=442)
<0.0001
DCR (TKI), %
21 (n=14)
78 (n=9)
82 (n=235)
20 (n=5)
81 (n=201)
Leduc et al. Ann Oncol 2016; 27 (suppl 6): abstr 1202O

10. Early and locally advanced NSCLC Stages I, II and III

11. Standard of care post-op treatment
LBA41_PR: Neoadjuvant anti-PD1, nivolumab, in early stage resectable non-small-cell lung cancer – Forde RM, et al
Study objective
To assess neoadjuvant nivolumab in patients with early stage NSCLC
Key patient inclusion criteria
Newly diagnosed resectable stage I (>2 cm)/II/IIIA NSCLC
(n=19)
Nivolumab 3 mg/kg IV Days -28 and -14 with repeat CT prior to planned surgical resection on Day 0
Standard of care post-op treatment
30 days
Primary endpoint
Safety and feasibility
Exploratory endpoints
Pathologic regression, radiographic response
Forde et al. Ann Oncol 2016; 27 (suppl 6): abstr LBA41_PR

12. LBA41_PR: Neoadjuvant anti-PD1, nivolumab, in early stage resectable non-small-cell lung cancer – Forde RM, et al
Key results
The single grade 3–4 TRAE discontinuation was related to fever and lung tumour cavitation, the patient underwent an uncomplicated surgery and postoperative follow-up
Treatment-related AEs
Any grade
Grade 3–4
Any treatment-related AE, % 32 5
Treatment-related AEs leading to discontinuation, %
Treatment-related delays to surgery
None
Specific treatment-related AEs
Grade 1–2
GI, % 21
Skin/musculoskeletal, % 11
Pulmonary, %
Other, %
Forde et al. Ann Oncol 2016; 27 (suppl 6): abstr LBA41_PR

13. LBA41_PR: Neoadjuvant anti-PD1, nivolumab, in early stage resectable non-small-cell lung cancer – Forde RM, et al
Key results (cont.)
At resection, 7 (39 %) patients had <10% residual viable tumour cells (defined as major pathologic response); 1 patient had a pathological complete response
Conclusions
Nivolumab administered preoperatively in early stage NSCLC is well tolerated, and radiologic and/or pathologic regression was observed in several patients
Many pathological responses were observed independently of radiological responses
Radiographic response (n=18)
Response, %
Partial response 22
Stable disease 72
Progressive disease 6
Pathologic downstaging from pre-treatment clinical stage (n=17)*
Yes 39 No 61
*Only resected patients included in analysis
Forde et al. Ann Oncol 2016; 27 (suppl 6): abstr LBA41_PR

14. 1178O: Multi-centre randomized controlled study comparing adjuvant vs neo-adjuvant chemotherapy with docetaxel plus carboplatin in resectable stage IB to IIIA NSCLC: final results of CSLC0501 – Wu Y, et al
Study objective
To compare DFS between adjuvant and neoadjuvant chemotherapy in resectable NSCLC
Key patient inclusion criteria
Histologically/cytologically confirmed stage IB–IIIA NSCLC
No prior chemotherapy, radiotherapy or target therapy
ECOG PS 0–1
(n=198)
Adjuvant: Docetaxel 75 mg/m2 + carboplatin AUC5 q3w
(n=101) PD
Stratification
Gender
Centre
Stage (1B vs. II vs. IIIA)
Pathology (adeno vs. non-adeno) R
Neoadjuvant: Docetaxel 75 mg/m2 + carboplatin AUC5 q3w
(n=97) PD
Primary endpoint
3-year DFS
Secondary endpoints
5-year OS, safety
Wu et al. Ann Oncol 2016; 27 (suppl 6): abstr 1178O

15. In the neoadjuvant arm ORR was 34.4% and DCR was 34.4%
1178O: Multi-centre randomized controlled study comparing adjuvant vs neo-adjuvant chemotherapy with docetaxel plus carboplatin in resectable stage IB to IIIA NSCLC: final results of CSLC0501 – Wu Y, et al
Key results
Chemotherapy was completed in 100% of the neoadjuvant arm vs % of the adjuvant arm, with a mean of 3 cycles for each
There was no surgery in 15.5% of the neoadjuvant arm vs. 0% of the adjuvant arm
In the neoadjuvant arm ORR was 34.4% and DCR was 34.4%
Neoadjuvant
Adjuvant
HR (95%CI)
p-value
3-year DFS, years, median (95%CI)
2.3 (1.6, 3.0) NR
0.73 (0.49, 1.09)
0.126
Total DFS, years, median (95%CI)*
5.2 (1.3, 9.0)
0.70 (0.49, 1.01)
0.057
5-year OS, years, median (95%CI)
4.2 (3.2, 5.2)
0.66 (0.44, 1.00)
0.050
Total OS, years, median (95%CI)*
7.3
0.71 (0.48, 1.05)
0.087
*The study was closed early due to slow accrual and the phase 1b proportion was stopped as adjuvant therapy was no longer feasible
Wu et al. Ann Oncol 2016; 27 (suppl 6): abstr 1178O

16. 1178O: Multi-centre randomized controlled study comparing adjuvant vs neo-adjuvant chemotherapy with docetaxel plus carboplatin in resectable stage IB to IIIA NSCLC: final results of CSLC0501 – Wu Y, et al
Key results (cont.)
Grade 3–4 events occurred in 45.4% and 35.6% of patients, respectively, in the neoadjuvant and adjuvant arms (p=0.21)
The most common grade 3–4 event was granulocytopenia occurring in 41.2% (neoadjuvant) and 31.7% (adjuvant) of patients
Conclusions
Docetaxel + carboplatin is safe as either adjuvant or neoadjuvant chemotherapy in resectable clinical stage IB–IIIA NSCLC
There was no statistically significant difference between the adjuvant and neoadjuvant arms in OS or 3-year DFS, with a trend in favour of adjuvant therapy for DFS and 5-year OS
Wu et al. Ann Oncol 2016; 27 (suppl 6): abstr 1178O

17. Advanced NSCLC Not radically treatable stage III and stage IV
1st line

18. LBA43: Afatinib (A) vs gefitinib (G) in patients (pts) with EGFR mutation-positive (EGFRm+) non-small-cell lung cancer (NSCLC): overall survival (OS) data from the phase IIb trial LUX-Lung 7 (LL7) – Paz-Ares L, et al
Study objective
A head-to-head trial of two EGFR-directed therapies, afatinib and gefitinib, as first-line therapy in EGFR+ NSCLC
Key patient inclusion criteria
Stage IIIB/IV lung adenocarcinoma
EGFR mutation (Del19 and/or L858R) in the tumour tissue
No prior treatment for advanced/metastatic disease
ECOG PS 0/1
(n=319)
Afatinib 40 mg/day
(n=160)
PD / toxicity
Stratification
Mutation type (Del19 vs. L858R)
Brain metastases (present vs. absent) R
1:1
Gefitinib 250 mg/day
(n=159)
PD / toxicity
Co-primary endpoints
PFS (IR), TTF, OS
Secondary endpoints
ORR, TTR, DoR, tumour shrinkage, HRQoL
Paz-Ares et al. Ann Oncol 2016; 27 (suppl 6): abstr LBA43

19. LBA43: Afatinib (A) vs gefitinib (G) in patients (pts) with EGFR mutation-positive (EGFRm+) non-small-cell lung cancer (NSCLC): overall survival (OS) data from the phase IIb trial LUX-Lung 7 (LL7) – Paz-Ares L, et al
Key results
Treatment discontinuation due to drug-related AEs was low in each arm (6%)
Conclusions
In patients with EGFR m+ NSCLC, afatinib significantly improved PFS, TTF and ORR compared with gefitinib, with no significant difference in OS
AEs were tolerable and resulted in equally low rates of treatment discontinuation
Afatinib (n=160)
Gefitinib (n=159)
HR (95%CI)
p-value
Median PFS (independent review), months
11.0
10.9
0.74 (0.57, 0.95)
0.0178
Median TTF, months
13.7
11.5
0.75 (0.60, 0.94)
0.0136
Median DoR, months
10.1
8.3
Median OS, months
27.9
24.5
0.86 (0.66, 1.12)
0.2580
Paz-Ares et al. Ann Oncol 2016; 27 (suppl 6): abstr LBA43

20. Pembrolizumab + chemotherapy
LBA46_PR: Randomized, phase 2 study of carboplatin and pemetrexed with or without pembrolizumab as first-lie therapy for advanced NSCLC: KEYNOTE-021 cohort G – Langer C, et al
Study objective
To compare the efficacy and safety pembrolizumab + carboplatin and pemetrexed vs. carboplatin and pemetrexed alone as first-line therapy for patients with advanced nonsquamous NSCLC histology in KEYNOTE-021
Key patient inclusion criteria
Untreated stage IIIB/IV nonsquamous NSCLC
No EGFR mutation or ALK translocation
Provision of sample for PD-L1 assessment
ECOG PS 0–1
No untreated brain metastases
(n=123)
Pembrolizumab + chemotherapy
Pembrolizumab 200 mg q3w (2 years) +
carboplatin AUC5 mg/mL/min +
pemetrexed 500 mg/m2 q3w (4 cycles)*
(n=60) R
1:1
Stratification
PD-L1 status (TPS ≥1 vs. <1%)
Chemotherapy
Carboplatin AUC5 mg/mL/min +
pemetrexed 500 mg/m2 q3w (4 cycles)*
(n=63) PD
Pembro 200 mg q3w (2 years)
Primary endpoint
ORR (RECIST)
Secondary endpoints
PFS, OS, safety, relationship between anti-tumor activity and PD-L1 TPS
*Pemetrexed 500 mg/m2 q3w permitted as maintenance therapy
Langer et al. Ann Oncol 2016; 27 (suppl 6): abstr LBA46_PR

21. Pembro + chemo responders (n=33) Chemo alone responders (n=18)
LBA46_PR: Randomized, phase 2 study of carboplatin and pemetrexed with or without pembrolizumab as first-lie therapy for advanced NSCLC: KEYNOTE-021 cohort G – Langer C, et al
Key results
Pembrolizumab + chemotherapy significantly improved the proportion of patients who achieved an ORR compared with chemotherapy alone
Confirmed ORR
∆26%
100
p=0.0016
Pembro + chemo responders (n=33)
Chemo alone responders (n=18)
TTR, months median (range)
1.5 (1.2–12.3)
2.7 (1.1–4.7)
DoR, months median (range)
NR (1.4+–13.0+)
NR (1.4+– 15.2+)
Ongoing response, n (%)
29 (88)
14 (78) 80
55% 60
ORR, % (95%CI)
29% 40 20
Pembro +
chemo
Chemo
alone
Langer et al. Ann Oncol 2016; 27 (suppl 6): abstr LBA46_PR

22. PFS (RECIST by Central Review)
LBA46_PR: Randomized, phase 2 study of carboplatin and pemetrexed with or without pembrolizumab as first-lie therapy for advanced NSCLC: KEYNOTE-021 cohort G – Langer C, et al
Key results (cont.)
PFS was significantly longer with pembrolizumab + chemotherapy compared with chemotherapy alone
PFS, %
100 80 60 40 20 5 10 15
Time, months
Pembro + chemo 23 33
Chemo alone
Events, n HR
(95%CI)
0.53
(0.31, 0.91)
p=0.0102
Number at risk: 63 43 32 13 1
Median PFS,
months
PFS (RECIST by Central Review)
13.0
8.9
Langer et al. Ann Oncol 2016; 27 (suppl 6): abstr LBA46_PR

23. LBA46_PR: Randomized, phase 2 study of carboplatin and pemetrexed with or without pembrolizumab as first-lie therapy for advanced NSCLC: KEYNOTE-021 cohort G – Langer C, et al
Key results (cont.)
At data cut-off, there was no difference in OS between the treatment groups (p=0.39), with few events in either arm
Events, n
HR (95%CI) OS
100
Pembro + chemo 13
0.90
Chemo alone 14
(0.42, 1.91) 80 60
OS, % 40 20 5 10 15 20
Time, months
Number at risk: 60 63 43 57 20 31 5 6
Langer et al. Ann Oncol 2016; 27 (suppl 6): abstr LBA46_PR

24. Pembrolizumab + chemotherapy (n=59)
LBA46_PR: Randomized, phase 2 study of carboplatin and pemetrexed with or without pembrolizumab as first-lie therapy for advanced NSCLC: KEYNOTE-021 cohort G – Langer C, et al
Key results (cont.)
Exposure was 1.6 times longer in the pembrolizumab + chemotherapy group
Most treatment-related AEs were mild and grade 1−2 severity
Conclusions
In chemotherapy-naïve advanced nonsquamous NSCLC, pembrolizumab + carboplatin and pemetrexed resulted in improved ORR and PFS vs. carboplatin and pemetrexed alone as first-line therapy
Pembrolizumab + carboplatin and pemetrexed have a manageable safety profile
OS data are awaited after a longer follow-up period
Pembrolizumab + chemotherapy (n=59)
Chemotherapy alone
(n=62)
Exposure, months median (range)
8.0 (1 d–16.1 mo)
4.9 (1 d–15.3 mo)
Treatment-related AEs, n (%)
Grade 3–4
Led to discontinuation
Led to death
55 (93)
23 (39)
6 (10)
1 (2)
56 (90)
16 (26)
8 (13)
2 (3)
Langer et al. Ann Oncol 2016; 27 (suppl 6): abstr LBA46_PR

25. LBA8_PR: KEYNOTE-024: Pembrolizumab (pembro) vs platinum-based chemotherapy (chemo) as first-line therapy for advanced NSCLC with a PD-L1 tumor proportion score (TPS) ≥50% – Reck M, et al
Study objective
To compare pembrolizumab vs. platinum-doublet chemotherapy as first-line therapy for advanced NSCLC of PD-L1 TPS ≥50% without treatable EGFR mutations or ALK translocations
Pembrolizumab 200 mg q3w (2 years)
(n=154)
Key patient inclusion criteria
Untreated stage IV NSCLC
PD-L1 TPS ≥50%
No activating EGFR mutation or ALK translocation
No untreated brain metastases
(n=305)
PD / toxicity / other R
Platinum-doublet chemotherapy*
(n=151)
PD / toxicity / other
Primary endpoint
PFS
Secondary endpoints
OS, ORR, safety
*Carboplatin or cisplatin + pemetrexed, carboplatin or cisplatin + gemcitabine, or carboplatin + paclitaxel, with optional pemetrexed maintenance for nonsquamous NSCLC
Reck et al. Ann Oncol 2016; 27 (suppl 6): abstr LBA8_PR

26. LBA8_PR: KEYNOTE-024: Pembrolizumab (pembro) vs platinum-based chemotherapy (chemo) as first-line therapy for advanced NSCLC with a PD-L1 tumor proportion score (TPS) ≥50% – Reck M, et al
Key results
Pembrolizumab demonstrated superior PFS over chemotherapy in patients whose tumours express high levels of PD-L1
PFS
Events, n
Median,
months
HR (95%CI)
p-value
100
Pembro 73
10.3
0.50
<0.001 80
Chemo
116
6.0
(0.37, 0.68) 60
PFS, % 40 20 3 6 9 12 15 18
Time, months
Number at risk:
154
151
104 99 89 70 44 18 22 9 3 1 1
Reck et al. Ann Oncol 2016; 27 (suppl 6): abstr LBA8_PR

27. LBA8_PR: KEYNOTE-024: Pembrolizumab (pembro) vs platinum-based chemotherapy (chemo) as first-line therapy for advanced NSCLC with a PD-L1 tumor proportion score (TPS) ≥50% – Reck M, et al
Key results (cont.)
Significant OS benefit was observed despite a 50% total crossover from chemotherapy to anti-PD-L1 therapy
Events, n
Median,
months
HR (95%CI) OS
p-value
Pembro 44 NR
0.60
100
0.005
Chemo 64 NR
(0.41, 0.89) 80 60
OS, % 40 20 3 6 9 12 15 18 21
Time, months
Number at risk:
154
151
136
123
121
106 82 64 39 34 11 7 2 1
Reck et al. Ann Oncol 2016; 27 (suppl 6): abstr LBA8_PR

28. Pembrolizumab responders (n=69) Chemotherapy responders (n=42)
LBA8_PR: KEYNOTE-024: Pembrolizumab (pembro) vs platinum-based chemotherapy (chemo) as first-line therapy for advanced NSCLC with a PD-L1 tumor proportion score (TPS) ≥50% – Reck M, et al
Key results (cont.)
There was an improvement in ORR with pembrolizumab over chemotherapy
6 CRs were observed with pembrolizumab
Confirmed ORR
ORR, % (95%CI) 60 40 20
Pembrolizumab
Chemotherapy
45%
28%
∆17%
p=0.0011
n=6
n=63
n=41
n=1 CR PR
Pembrolizumab responders (n=69)
Chemotherapy responders (n=42)
TTR, months median (range)
2.2 (1.4−8.2)
2.2 (1.8–12.2)
DoR, months median (range) NR
(1.9+–14.5+)
6.3
(2.1+–12.6+)
Reck et al. Ann Oncol 2016; 27 (suppl 6): abstr LBA8_PR

29. LBA8_PR: KEYNOTE-024: Pembrolizumab (pembro) vs platinum-based chemotherapy (chemo) as first-line therapy for advanced NSCLC with a PD-L1 tumor proportion score (TPS) ≥50% – Reck M, et al
Key results (cont.)
Incidence of treatment-related AEs was lower with pembrolizumab compared with chemotherapy
Conclusions
Pembrolizumab demonstrated improved PFS, OS and ORR over chemotherapy, with a lower incidence of AEs
PD-L1 TPS ≥50% is observed in ~1/3 of patients with advanced NSCLC and identifies those most likely to benefit from anti-PD-1 therapy
Pembrolizumab
(n=154)
Chemotherapy
(n=150)
Exposure, months median (range)
7.0 (1 d–18.7 mo)
3.5 (1 d–16.8 mo)
Treatment-related AEs, n (%)
Grade 3–4
Serious
Led to discontinuation
Led to death
113 (73)
40 (26)
33 (21)
11 (7)
1 (<1)
135 (90)
77 (51)
31 (21)
16 (11)
3 (2)
Reck et al. Ann Oncol 2016; 27 (suppl 6): abstr LBA8_PR

30. LBA7_PR: CheckMate 026: A phase 3 trial of nivolumab vs investigator's choice (IC) of platinum-based doublet chemotherapy (PT-DC) as first-line therapy for stage IV/recurrent programmed death ligand 1 (PD-L1)–positive NSCLC – Socinski M, et al
Study objective
To evaluate the efficacy of first-line nivolumab vs. investigator choice of platinum-based doublet chemotherapy in stage IV/recurrent PD-L1-positive NSCLC
Key patient inclusion criteria
Stage IV or recurrent NSCLC
No prior systemic therapy for advanced disease
No EGFR/ALK mutations sensitive to targeted inhibitor therapy
PD-L1 expression of ≥1%
ECOG PS 0–1
(n=541)
Nivolumab 3 mg/kg IV q2w (n=271)
PD / toxicity
Stratification
PD-L1 expression (<5% vs. ≥5%)
Histology (squamous vs. nonsquamous) R
Nivolumab
(optional)
Chemotherapy* for 6 cycles (n=270) PD
Primary endpoint
PFS (≥5% PD-L1+)
Secondary endpoints
PFS (≥1% PD-L1+), OS, ORR
*Investigator choice – histology dependent
Socinski et al. Ann Oncol 2016; 27 (suppl 6): abstr LBA7_PR

31. LBA7_PR: CheckMate 026: A phase 3 trial of nivolumab vs investigator's choice (IC) of platinum-based doublet chemotherapy (PT-DC) as first-line therapy for stage IV/recurrent programmed death ligand 1 (PD-L1)–positive NSCLC – Socinski M, et al
Key results
PFS per IRRC in ≥5% PD-L1+ 24 21 18 15 12 9 6 3 27
100 80 60 40 20
Nivolumab
(n=211)
Chemotherapy
(n=212)
mPFS, months
(95%CI)
4.2
(3.0, 5.6)
5.9
(5.4, 6.9)
1-year PFS rate, %
23.6
23.2
Months
PFS, %
HR 1.15 (95%CI 0.91, 1.45); p=0.2511
Nivolumab
Chemotherapy
Number at risk:
Nivolumab
211
104 71 49 35 24 6 3 1
Chemotherapy
212
144 74 47 28 21 8
All randomised patients (≥1% PD-L1+): HR 1.17 (95%CI 0.95, 1.43)
Socinski et al. Ann Oncol 2016; 27 (suppl 6): abstr LBA7_PR

32. All randomised patients (≥1% PD-L1+): HR 1.07 (95%CI 0.86, 1.33)
LBA7_PR: CheckMate 026: A phase 3 trial of nivolumab vs investigator's choice (IC) of platinum-based doublet chemotherapy (PT-DC) as first-line therapy for stage IV/recurrent programmed death ligand 1 (PD-L1)–positive NSCLC – Socinski M, et al
Key results (cont.)
OS (≥5% PD-L1+)
Months
OS, % 24 21 18 15 12 9 6 3 30
100 80 60 40 20 27
Nivolumab
Chemotherapy
Nivolumab
(n=211)
Chemotherapy
(n=212)
Median OS, months
(95%CI)
14.4
(11.7, 17.4)
13.2
(10.7, 17.1)
1-year OS rate, %
56.3
53.6
HR 1.02 (95%CI 0.80, 1.30)
60.4% in the chemotherapy arm had subsequent nivolumab therapy
43.6% in the nivolumab arm had subsequent systemic therapy
Number at risk:
Nivolumab
211
186
156
133
118 98 49 14 4
Chemotherapy
212
153
137
112 91 50 15 3 1
All randomised patients (≥1% PD-L1+): HR 1.07 (95%CI 0.86, 1.33)
Socinski et al. Ann Oncol 2016; 27 (suppl 6): abstr LBA7_PR

33. LBA7_PR: CheckMate 026: A phase 3 trial of nivolumab vs investigator's choice (IC) of platinum-based doublet chemotherapy (PT-DC) as first-line therapy for stage IV/recurrent programmed death ligand 1 (PD-L1)–positive NSCLC – Socinski M, et al
Key results (cont.)
Nivolumab (n=211)
Chemotherapy (n=212)
ORR, % (95%CI)
26.1 (20.3, 32.5)
33.5 (27.2, 40.3)
Best overall response, % CR PR SD PD
Not determined
1.9
24.2
38.4
27.5
8.1
0.5
33.0
47.2
9.9
9.4
Median time to response, months (range)
2.8 (1.2, 13.2)
2.6 (1.2, 9.8)
Median duration of response, months (95%CI)
12. 1 (8.8, NE)
5.7 (4.2, 8.5)
Socinski et al. Ann Oncol 2016; 27 (suppl 6): abstr LBA7_PR

34. Nivolumab did not improve PFS or OS compared with chemotherapy
LBA7_PR: CheckMate 026: A phase 3 trial of nivolumab vs investigator's choice (IC) of platinum-based doublet chemotherapy (PT-DC) as first-line therapy for stage IV/recurrent programmed death ligand 1 (PD-L1)–positive NSCLC – Socinski M, et al
Key results (cont.)
Conclusions
Nivolumab did not improve PFS or OS compared with chemotherapy
High PD-L1 expression subset was not planed and cannot be accurately measured/reported related to clinical characteristics imbalances
AEs were consistent with reported data for nivolumab, with fewer grade 3–4 AEs than chemotherapy
Nivolumab (n=267)
Chemotherapy (n=263)
Any grade
Grade 3–4
Treatment-related AE, %
Any
SAE
AE leading to discontinuation
71.2
17.2
9.7
17.6
13.1
7.9
92.4
18.3
13.3
50.6
15.6
6.5
Treatment-related deaths, n (%)
2 (0.7)
3 (1.1)
Socinski et al. Ann Oncol 2016; 27 (suppl 6): abstr LBA7_PR

35. Advanced NSCLC Not radically treatable stage III and stage IV
Later lines

36. 359O: First-in-human study of AC0010, a novel irreversible, mutant-selective EGFR inhibitor in patients with 1st generation EGFR TKI-resistant non-small cell lung cancer (NSCLC) – Zhang L, et al
Study objective
To evaluate the safety and efficacy of AC0010 in NSCLC patients with EGFR-TKI resistance
Methods
52 EGFR mutation-positive advanced stage NSCLC patients who had resistance to EGFR TKIs were included; all patients had EGFR activated mutation and 87% had acquired T790M+
Oral administration of AC0010 either QD (50–350 mg), BID (175–300 mg) or TID (200 mg)
Key results
The majority of AEs were grade 1–2, and maximum tolerated dose was not reached
Among all evaluated patients (including T790M negative patients), the ORR was 38.9% and DCR was 73%
Dose exposure between 350 and 600 mg/day was considered as the efficacious dose, with ORR 55.6% and DCR 86.1%
Conclusions
AC0010 was well-tolerated with a good safety profile and showed promising anti-tumour activity in EGFR T790M+ NSCLC patients
Better anti-tumour activities were seen with 250 mg BID and 300 mg BID and was recommended as the dosage in phase 2 studies
Zhang et al. Ann Oncol 2016; 27 (suppl 6): abstr 359O

37. LBA42_PR: Ceritinib vs chemotherapy (CT) in patients (pts) with advanced anaplastic lymphoma kinase (ALK)-rearranged (ALK+) non-small cell lung cancer (NSCLC) previously treated with CT and crizotinib (CRZ): results from the confirmatory phase 3 ASCEND-5 study – Scagliotti G, et al
Study objective
To compare the efficacy of ceritinib vs. chemotherapy in ALK+ NSCLC patients pre-treated with chemotherapy and crizotinib
Key patient inclusion criteria
Locally advanced or metastatic ALK+ NSCLC
Progressive disease
WHO PS 0–2
Prior crizotinib (>1 course allowed)
1 or 2 prior chemotherapy regimens
Measurable disease at baseline
(n=231)
Ceritinib 750 mg/day
(n=115)
Crossover
following BIRC-confirmed PD
Stratification
WHO PS (0 vs.1–2)
Brain metastases (yes vs. no) R
1:1
Chemotherapy
Pemetrexed 500 mg/m2 (n=40) or docetaxel 75 mg/m2 (n=73) q3w
Primary endpoint
PFS (BIRC)
Secondary endpoints
OS, PFS (investigator), ORR, DCR, TTR
BIRC, blinded independent review committee
Scagliotti et al. Ann Oncol 2016; 27 (suppl 6): abstr LBA42_PR

38. LBA42_PR: Ceritinib vs chemotherapy (CT) in patients (pts) with advanced anaplastic lymphoma kinase (ALK)-rearranged (ALK+) non-small cell lung cancer (NSCLC) previously treated with CT and crizotinib (CRZ): results from the confirmatory phase 3 ASCEND-5 study – Scagliotti G, et al
Key results
Median OS was 18.1 months (95%CI 13.4, 23.9) for ceritinib and 20.1 months (95%CI 11.9, 25.1) for chemotherapy (HR 1.0; 95%CI 0.67, 1.49)
ORR (BIRC) was 39.1% (95%CI 30.2, 48.7) with ceritinib vs. 6.9% (95%CI 3.0, 13.1) with chemotherapy
PFS (BIRC)
100
Treatment
Median PFS, mo (95%CI)
Events, n (%)
Ceritinib 750 mg (n=115)
5.4 (4.1, 6.9)
83 (72.2)
Chemotherapy (n=116)
1.6 (1.4, 2.8)
89 (76.7) 80 60
HR 0.49 (95%CI 0.36, 0.67) p<0.001
Probability of PFS, % 40 20 2 4 6 8 10 12 14 16 18 20 22 24
Time, months
BIRC, blinded independent review committee
Scagliotti et al. Ann Oncol 2016; 27 (suppl 6): abstr LBA42_PR

39. LBA42_PR: Ceritinib vs chemotherapy (CT) in patients (pts) with advanced anaplastic lymphoma kinase (ALK)-rearranged (ALK+) non-small cell lung cancer (NSCLC) previously treated with CT and crizotinib (CRZ): results from the confirmatory phase 3 ASCEND-5 study – Scagliotti G, et al
Key results (cont.)
Diarrhoea, nausea and vomiting were higher with ceritinib than chemotherapy
AEs led to discontinuation in 5.2% of the ceritinib patients and 6.9% of the chemotherapy patients
Conclusions
Compared with chemotherapy, ceritinib significantly improved PFS in patients with ALK+ NSCLC
The safety profile of ceritinib was consistent with that reported in previous studies and compared unfavourably to chemotherapy in this trial
AEs (occurring in >50% any grade), n (%)
Ceritinib (n=115)
Chemotherapy (n=113)
All grades
Grades 3/4
Diarrhoea
83 (72.2)
5 (4.3)
20 (17.7)
1 (0.9)
Nausea
76 (66.1)
9 (7.8)
26 (23.0)
2 (1.8)
Vomiting
60 (52.2)
6 (5.3)
Scagliotti et al. Ann Oncol 2016; 27 (suppl 6): abstr LBA42_PR

40. Ceritinib 750 mg/day (fasting, PO)
1208O: Phase 2 study of ceritinib in ALKi-naïve patients (pts) with ALK-rearranged (ALK+) non-small cell lung cancer (NSCLC): Whole body responses in the overall pt group and in pts with baseline brain metastases (BM) – Felip E, et al
Study objective
To evaluate the long-term efficacy and safety of ceritinib in ALK+ NSCLC patients previously-treated with up to 3 lines of prior chemotherapy, but ALK inhibitor naïve
Key patient inclusion criteria
Advanced or metastatic ALK+ NSCLC
ALK inhibitor naïve
≤3 lines of chemotherapy with progression with last line
WHO PS 0–2
(n=124)
Ceritinib 750 mg/day (fasting, PO)
PD / toxicity / other
Primary endpoint
ORR (investigator)
Secondary endpoints
ORR (BIRC), DoR, TTR, DCR, PFS, OS
Felip et al. Ann Oncol 2016; 27 (suppl 6): abstr 1208O

41. Without brain metastases (n=75)
1208O: Phase 2 study of ceritinib in ALKi-naïve patients (pts) with ALK-rearranged (ALK+) non-small cell lung cancer (NSCLC): Whole body responses in the overall pt group and in pts with baseline brain metastases (BM) – Felip E, et al
Key results
Investigator assessment
Total population (n=124)
With brain metastases
(n=49)
Without brain metastases (n=75)
ORR, n (%) [95%CI]
84 (67.7) [58.8, 75.9]
28 (57.1) [42.2, 71.2]
56 (74.7) [63.3, 84.0]
DCR, n (%) [95%CI]
112 (90.3) [83.7, 94.9]
43 (87.8) [75.2, 95.4]
69 (92.0) [83.4, 97.0]
Median PFS, months [95%CI]
16.6 [11.0, 22.1]
10.8 [8.3, 16.6]
19.6 [14.5, NE]
Median DOR, months [95%CI]
22.1 [14.8, NE]
Median OS, months
Not yet reached
24-month OS rate, % [95%CI]
67.5 [58.0, 75.2]
BIRC assessment
79 (63.7) [54.6, 72.2]
107 (86.3) [79.0, 91.8]
18.4 [10.9, 26.3]
Felip et al. Ann Oncol 2016; 27 (suppl 6): abstr 1208O

42. 8.9% of patients discontinued treatment due to AEs Conclusions
1208O: Phase 2 study of ceritinib in ALKi-naïve patients (pts) with ALK-rearranged (ALK+) non-small cell lung cancer (NSCLC): Whole body responses in the overall pt group and in pts with baseline brain metastases (BM) – Felip E, et al
Key results (cont.)
Grade 3 or 4 AEs occurred in 85.5% of patients, the most common were ALT increased (21.0%), GGT increased (19.4%) and AST increased (9.7%)
Drug-related SAEs occurred in 11.3% patients, the most common were pericarditis, nausea and vomiting
8.9% of patients discontinued treatment due to AEs
Conclusions
In the long-term follow-up of the ASCEND-3 study, ceritinib resulted in robust ORR and exhibited a prolonged PFS and OS in ALK inhibitor- naive patients
Ceritinib was also shown to be active in patients with brain metastases
The AEs seen were consistent with the reported safety profile of ceritinib
Felip et al. Ann Oncol 2016; 27 (suppl 6): abstr 1208O

43. 1201O: Gefitinib/chemotherapy vs chemotherapy in EGFR mutation-positive NSCLC after progression on 1st line gefitinib (IMPRESS study): Final overall survival (OS) analysis – Soria J, et al
Study objective
To evaluate the impact of continuing gefitinib therapy in addition to cisplatin + pemetrexed chemotherapy in patients with advanced/metastatic NSCLC
Key patient inclusion criteria
Stage IIIB/IV EGFR+ advanced NSCLC
Chemotherapy naïve
Achieved CR/PR ≥4 months or SD >6 months with first-line gefitinib
Disease progression <4 weeks prior to study randomisation
WHO PS 0−1
(n=265)
Gefitinib 250 mg/day +
cisplatin 75 mg/m2 + pemetrexed 500 mg/m2
(n=133)
PD / toxicity R
1:1
Placebo + cisplatin 75 mg/m2 + pemetrexed 500 mg/m2 (n=132)
PD / toxicity
Primary endpoint
PFS
Secondary endpoints
OS, ORR, DCR, safety/tolerability, HRQoL
Soria et al. Ann Oncol 2016; 27 (suppl 6): abstr 1201O

44. Time since randomisation, months
1201O: Gefitinib/chemotherapy vs chemotherapy in EGFR mutation-positive NSCLC after progression on 1st line gefitinib (IMPRESS study): Final overall survival (OS) analysis – Soria J, et al
Key results
Final OS (66% maturity)
Gefitinib (n=133)
Placebo (n=132)
Median OS, months
13.4
19.5
Number of events, n (%)
94 (71)
82 (62)
HR 1.44 (95%CI 1.07, 1.94); p=0.016
1.0
0.8
0.6
Probability of OS
0.4
0.2
Gefitinib + CT (n=133)
Placebo + CT (n=132)
0.0 4 8 12 16 20 24 28 32 36 40 44
Time since randomisation, months
Soria et al. Ann Oncol 2016; 27 (suppl 6): abstr 1201O

45. Time since randomisation, months
1201O: Gefitinib/chemotherapy vs chemotherapy in EGFR mutation-positive NSCLC after progression on 1st line gefitinib (IMPRESS study): Final overall survival (OS) analysis – Soria J, et al
Key results (cont.)
Conclusion
Final OS data from the IMPRESS study warn against continued treatment with first-generation EGFR TKIs beyond radiological disease progression
T790M mutation-positive
Gefitinib + CT (n=81)
Placebo + CT (n=61)
Median OS, months
10.8
14.1
Number of events, n (%)
63 (77.8)
44 (72.1)
HRa 1.49 (95%CI 1.02, 2.21)
OS by T790M mutation
1.0
0.8
0.6
0.4
0.2
0.0 4
Time since randomisation, months 8 12 16
Probability of OS 20 24 28 32 36 40 44
Gefitinib – T790M negative
Placebo – T790M negative
Gefitinib – T790M positive
Placebo – T790M positive
T790M mutation-negative
Gefitinib + CT (n=46)
Placebo + CT (n=59)
Median OS, months
21.4
22.5
Number of events, n (%)
27 (58.7)
30 (50.8)
HRa 1.15 (95%CI 0.68, 1.94)
Number at risk:
aPrimary Cox analysis with covariates
Soria et al. Ann Oncol 2016; 27 (suppl 6): abstr 1201O

46. 1203PD: LURET study: Phase 2 study of vandetanib in patients with advanced RET-rearranged non-small cell lung cancer (NSCLC) – Horiike A, et al
Study objective
To assess the efficacy and safety of vandetanib in advanced RET-rearranged NSCLC
Methods
A single-arm phase 2 study of vandetanib (300 mg/day orally) in patients with advanced RET-rearranged NSCLC with ≥1 prior chemotherapy
Key results
34 RET-positive patients were identified (2% of those screened); 19 were enrolled into the study (ITT population) with 17 in the primary analysis population
ORR was 53% (90%CI 31, 74; p=0.04) with 9 partial responses for the primary analysis; ORR was 47% (90%CI 24, 71) in the ITT population
In the ITT population, DCR was 90% (95%CI 67, 99), median PFS was 4.7 months (95%CI 2.8, 8.5) and 1-year OS rate was 47% (95%CI 21, 69)
In subgroup analyses, CCDC6-RET mutations had ORR 83% (95%CI 36, 99.6) and median PFS 8.3 months (95%CI 4.7, 8.5), and KIF5B-RET mutations had ORR 20% (95%CI 3, 56) and median PFS 2.9 months (95%CI 1.1, 15.7)
AEs grade ≥3 (occurring in >10%) included hypertension (58%), acneiform rash (16%), diarrhoea (11%) and QTc prolongation (11%)
Conclusions
Vandetanib showed anti-tumour activity in patients with advanced RET-rearranged NSCLC
Data suggest that tumours expressing CCDC6-RET mutations may respond better to vandetanib than tumours with KIF5B-RET
Horiike et al. Ann Oncol 2016; 27 (suppl 6): abstr 1203PD

47. 1204PD: Phase 2 study of lenvatinib (LN) in patients (pts) with RET fusion-positive adenocarcinoma of the lung – Velcheti V, et al
Study objective
To evaluate the efficacy and safety of lenvatinib, a multikinase inhibitor
Methods
Open-label, phase 2 study of lenvatinib (24 mg/day PO) in patients with RET fusion- positive lung adenocarcinoma
Key results
25 patients with RET fusion-positive NSCLC were enrolled; 28% had received previous RET-targeted therapy
ORR was 16% (all confirmed PRs) and DCR was 76%
mPFS was 7.3 months (95%CI 3.6, 10.2)
Grade ≥3 treatment-related AEs were reported in 21 (84.0%) patients. TEAEs of 20.0%, 64.0% and 76.0% were associated with drug withdrawal, dose reduction and dose interruption, respectively
Commonly reported AEs (any grade occurring in >50%) included hypertension (68%), nausea (60%), decreased appetite and diarrhoea (both 52%)
Conclusion
In patients with RET fusion-positive NSCLC lenvatinib showed clinical activity, including those who had previously received RET-targeted therapy
Velcheti et al. Ann Oncol 2016; 27 (suppl 6): abstr 1204PD

48. 1205PD: Ceritinib in ROS1-rearranged non-small-cell lung cancer: A Korean nationwide phase II study – Lim S, et al
Study objective
To evaluate the efficacy and safety of ceritinib in patients with advanced ROS1-rearranged NSCLC
Methods
A phase 2 study of ceritinib 750 mg/day PO after fasting, in patients with advanced NSCLC who tested positive for ROS1 rearrangement and had previously received ≥1 line of platinum-based chemotherapy
Key results
404 patients were screened and 32 ROS1-positive patients were enrolled
ORR was 62% with 1 CR and 19 PRs; median DoR was 18.4 months (95%CI 8.0, 18.4) and median PFS was 10.0 months (95%CI 2.5, 17.4)
Median OS was not reached by time of data cut-off
Seven ROS fusion partners (including ROS1-CD74, ROS1-SLC34A2 and ROS1-EZR) were identified in the 11 tumours tested
The most frequently reported AEs occurring in >50% were diarrhoea (78%), nausea (59%), anorexia (56%) and vomiting (53%), but drug-related AEs were mainly grades 1–2
Conclusion
Ceritinib showed significant clinical activity in advanced ROS1-positive NSCLC patients, with a safety profile consistent to that previously reported
Lim et al. Ann Oncol 2016; 27 (suppl 6): abstr 1205PD

49. No grade 4 or 5 TRAEs were reported
1206PD: Crizotinib in advanced ROS1-rearranged non-small cell lung cancer (NSCLC): Updated results from PROFILE 1001 – Shaw A, et al
Study objective
To assess the safety and anti-tumour activity of crizotinib in ROS1-positive NSCLC
Methods
Phase 1 study of crizotinib (250 mg BID PO) in patients with ROS1-positive advanced NSCLC
Key results
53 patients were enrolled with median treatment duration of 23.2 months
Vision disorder was the most frequently reported TRAE (84.9%), followed by nausea (49.1%), oedema (45.3%) and diarrhoea (41.5%)
No grade 4 or 5 TRAEs were reported
ORR by investigator was 69.8% (95%CI 55.7, 81.7), with 5 CRs and 32 PRs
Median PFS was 19.3 months (95%CI 14.8, not reached)
Median OS was not reached at median follow-up of 25.4 months
Conclusion
Crizotinib was well tolerated and showed significant clinical activity with acceptable safety profile in patients with ROS1-positive advanced NSCLC
Shaw et al. Ann Oncol 2016; 27 (suppl 6): abstr 1206PD

50. Atezolizumab 1200 mg IV q3w (n=425)
LBA44_PR: Primary analysis from OAK, a randomized phase III study comparing atezolizumab with docetaxel in 2L/3L NSCLC – Barlesi F, et al
Study objective
To evaluate the efficacy and safety of atezolizumab vs. docetaxel in patients with previously treated NSCLC
Atezolizumab 1200 mg IV q3w (n=425)
Key patient inclusion criteria
Locally advanced or metastatic NSCLC
1–2 prior lines of chemotherapy including at least 1 platinum based
Any PD-L1 status
(n=1225)
PD / loss of benefit
Stratification
PD-L1 status
Prior chemotherapy regimens (1 vs. 2)
Histology R
Docetaxel 75 mg/m2 IV q3w
(n=425) PD
Primary endpoint
OS in ITT and PD-L1-expression on ≥1% TC or IC
Secondary endpoints
ORR, PFS, DoR, safety
Barlesi et al. Ann Oncol 2016; 27 (suppl 6): abstr LBA44_PR

51. LBA44_PR: Primary analysis from OAK, a randomized phase III study comparing atezolizumab with docetaxel in 2L/3L NSCLC – Barlesi F, et al
Key results
OS, ITT (n=850)
OS, %
HR 0.73a
(95%CI 0.62, 0.87)
p=0.0003
Minimum follow-up = 19 months
(95%CI 8.6, 11.2)
(95%CI 11.8, 15.7)
Median 9.6 mo
Median 13.8 mo
Months
Atezolizumab
Docetaxel
Number at risk:
425
407
382
363
342
326
305
279
260
248
234
223
218
205
198
188
175
163
157
141
116 74 54 41 28 15 4 1
390
365
336
311
286
263
219
195
179
168
151
140
132
123
104 98 90 70 51 37 16 6 3
236
100 27 21 80 24 18 60 12 40 9 20
aStratified HR
Barlesi et al. Ann Oncol 2016; 27 (suppl 6): abstr LBA44_PR

52. LBA44_PR: Primary analysis from OAK, a randomized phase III study comparing atezolizumab with docetaxel in 2L/3L NSCLC – Barlesi F, et al
Key results (cont.)
OS by PD-L1 expression
mOS, months
Atezolizumab
Docetaxel
Subgroup
n=425
TC3 or IC3
TC2 / 3 or IC2 / 3
TC1 / 2 / 3 or IC1 / 2 / 3a
TC0 and IC0
20.5
16.3
15.7
12.6
8.9
10.8
10.3
13.8
9.6
ITTa
0.2 1 2
Hazard Ratioa
In favour of
atezolizumab
docetaxel
0.41
0.67
0.74
0.75
0.73
On-study prevalence 0%
20%
40%
80%
60%
100%
16%
31%
55%
45%
aStratified HRs for ITT and TC1 / 2 / 3 or IC1 / 2 / 3. Unstratified HR for subgroups
Barlesi et al. Ann Oncol 2016; 27 (suppl 6): abstr LBA44_PR

53. LBA44_PR: Primary analysis from OAK, a randomized phase III study comparing atezolizumab with docetaxel in 2L/3L NSCLC – Barlesi F, et al
Key results (cont.)
PFS, ITT
mPFS, months
100
HR 0.95a
Atezolizumab
Docetaxel
Median 2.8 mo
(95%CI 2.6, 3.0)
(95%CI 0.82, 1.10) 80
p=0.4928b
Subgroup
n=425
n=425
0.63 60
Median 4.0 mo
(95%CI 3.3, 4.2)
TC3 or IC3
TC2 / 3 or IC2 / 3
TC1 / 2 / 3 or IC1 / 2 / 3a
TC0 and IC0
4.2
4.1
2.8
2.6
3.3
3.6
4.1
4.0
PFS, %
Atezolizumab
0.76 40
Docetaxel
0.91 20
1.00
0.95 3 6 9 12 15 18 21 24 27
ITTa
2.8
4.0
Months
Number at risk
Atezolizumab
Docetaxel
425
395
385
243
283
190
223
181
198
139
142
128
110
119 91
111 81 99 60 92 50 80 41 75 38 64 29 59 27 53 23 51 19 49 17 45 16 29 13 22 11 12 5 9 4 7 2 2 1 1
0.4 1 2
Hazard Ratioa
In favour of
atezolizumab
In favour of
docetaxel
Investigator-assessed PFS per RECIST v1.1
aStratified HRs for ITT and TC1 / 2 / 3 or IC1 / 2 / 3. Unstratified HR for subgroups; bp-values for descriptive purposes only
Barlesi et al. Ann Oncol 2016; 27 (suppl 6): abstr LBA44_PR

54. LBA44_PR: Primary analysis from OAK, a randomized phase III study comparing atezolizumab with docetaxel in 2L/3L NSCLC – Barlesi F, et al
Key results (cont.)
Conclusions
Atezolizumab improved OS in all patients, and benefit was seen regardless of PD-L1 expression levels (HR 0.75 in <1% PD-L1 expression population and 0.41 in ≥50% TC or ≥10% IC expression population)
OS benefit was consistent across subgroups, including histology (HR 0.73 for both), patients with CNS mets (HR 0.54) and never smokers (HR 0.71)
Atezolizumab was well tolerated and had a favourable safety profile compared with docetaxel
Atezolizumab
Docetaxel
ORR, %
TC3 or IC3
TC2 / 3 or IC2 / 3
TC1 / 2 / 3 or IC1 / 2 / 3
TC0 or IC0 14 31 22 18 8 13 11 16
Duration of response
ITT
Ongoing response, %
Median, months
TC0 and IC0 52
16.3 47
16.0 71 NE
6.2 29
Barlesi et al. Ann Oncol 2016; 27 (suppl 6): abstr LBA44_PR

55. Placebo + docetaxel 75 mg/m2 IV q3w (up to 6 cycles)
LBA45: Top-line results from SUNRISE: A phase III, randomized, double-blind, placebo-controlled multicenter trial of bavituximab plus docetaxel in patients with previously treated stage IIIb/IV non-squamous non small cell lung cancer – Spigel DR, et al
Study objective
To evaluate bavituximab + docetaxel compared with placebo + docetaxel in patients with previously treated stage IIIb/IV nonsquamous NSCLC
Key patient inclusion criteria
Stage IIIb/IV nonsquamous NSCLC
1 prior platinum-based doublet for advanced disease
Progressed on appropriate targeted therapy if known EGFR/ALK mutation
ECOG PS 0–1
Prior immunotherapy allowed
(n=597)
Bavituximab 3 mg/kg qw + docetaxel 75 mg/m2 IV q3w (up to 6 cycles) (n=425)
PD / toxicity
Stratification
Region
Disease stage
Prior maintenance/targeted therapy R
Placebo + docetaxel 75 mg/m2 IV q3w (up to 6 cycles)
(n=425)
PD / toxicity
Primary endpoint OS
Secondary endpoints
ORR, PFS, safety, PK, QoL, β2-GP1 as exploratory biomarker
Spigel et al. Ann Oncol 2016; 27 (suppl 6): abstr LBA45

56. LBA45: Top-line results from SUNRISE: A phase III, randomized, double-blind, placebo-controlled multicenter trial of bavituximab plus docetaxel in patients with previously treated stage IIIb/IV non-squamous non small cell lung cancer – Spigel DR, et al
Key results
Safety profile was generally similar between the two treatment groups
Grade 3/4 febrile neutropenia was slightly higher for bavituximab vs. docetaxel (8% vs. 5%)
Trend for prolonged survival with bavituximab in subgroups with high β2-GP1 at baseline (exploratory analysis only)
Conclusions
The safety profile of bavituximab + docetaxel is similar to placebo + docetaxel
The addition of bavituximab to docetaxel did not result in improvement in OS
Preliminary data suggest β2-GP1 levels may provide a biomarker for patients who may be more likely to benefit from treatment with bavituximab
1.0
OS (ITT population)
Treatment
Median, months
No. of events
Bavituximab
10.7 (8.6, 11.5)
169
Placebo
10.8 (9.2, 12.6)
161
0.8
0.6
OS, %
0.4
HR (95%CI) 1.10 (0.89, 1.37)
p-value
0.2 3 6 9 12 15 18 21 24 27
Time, months
Spigel et al. Ann Oncol 2016; 27 (suppl 6): abstr LBA45

57. LBA47_PR: Selumetinib in combination with docetaxel as second-line treatment for patients with KRAS-mutant advanced NSCLC: Results from the phase III SELECT-1 trial – Jänne PA, et al
Study objective
To assess the clinical benefit of selumetinib + docetaxel compared with placebo + docetaxel in patients with locally advanced or metastatic KRAS-mutant NSCLC
Key patient inclusion criteria
KRAS-mutant stage IIIb/IV NSCLC
Failed first-line therapy
WHO PS 0–1
Excluded if >1 previous anti-cancer drug regimen for advanced disease
(n=510)
Selumetinib 75 mg BID PO + docetaxel 75 mg/m2 IV D1 q3w (up to 6 cycles)* (n=254)
PD / toxicity / other
Stratification
WHO PS (0/1)
Histology (squamous/nonsquamous) R
Selumetinib or placebo
Placebo + docetaxel 75 mg/m2 IV D1 q3w (up to 6 cycles)*
(n=256)
PD / toxicity / other
Primary endpoint
PFS
Secondary endpoints
OS, ORR, DoR, safety
*All received prophylactic G-CSF
Jänne et al. Ann Oncol 2016; 27 (suppl 6): abstr LBA47_PR

58. Time from randomisation, months
LBA47_PR: Selumetinib in combination with docetaxel as second-line treatment for patients with KRAS-mutant advanced NSCLC: Results from the phase III SELECT-1 trial – Jänne PA, et al
Key results
OS was not significantly improved with selumetinib + docetaxel compared with placebo + docetaxel, 8.7 vs. 7.9 months (HR 1.05 [95%CI 0.85,1.30]) in KRAS- mutant advanced NSCLC
PFS
Time from randomisation, months
254
256 1
219
231 2
164
154 3
128
112 4
109 97 5 74 68 6 48 50 7 31 33 8 27 28
SEL + DOC
PBO + DOC 9 20 10 15 13 11 14 12 16 17 18 19 21 22 23 24 25 26
SEL + DOC (n=254)
PBO + DOC (n=254)
Events, n (%)
218 (86)
229 (89)
Median, months
3.9
2.8
HR (95%CI) 2-sided p-value
0.93 (0.77, 1.12)
0.44
1.0
0.8
0.6
Probability of PFS
0.4
0.2
Patients at risk:
SEL + DOC
PBO + DOC
Jänne et al. Ann Oncol 2016; 27 (suppl 6): abstr LBA47_PR

59. Selumetinib + docetaxel (n=251) Placebo + docetaxel (n=254)
LBA47_PR: Selumetinib in combination with docetaxel as second-line treatment for patients with KRAS-mutant advanced NSCLC: Results from the phase III SELECT-1 trial – Jänne PA, et al
Key results (cont.)
Conclusions
Selumetinib + docetaxel did not significantly improve PFS or OS compared with docetaxel + placebo in KRAS-mutant advanced NSCLC
The safety profile of selumetinib + docetaxel was consistent with data for docetaxel and selumetinib
Selumetinib + docetaxel (n=251)
Placebo + docetaxel (n=254)
Any AE
Grade 3
249 (99)
169 (67)
242 (95)
115 (45)
Any SAE
Related to selumetinib/placebo
Related to docetaxel
124 (49)
50 (20)
42 (17)
82 (32)
14 (6)
24 (9)
Any AE leading to hospitalisation
116 (46)
76 (30)
Any AE with outcome of death
16 (6)
9 (4)
Grade 3 AE occurring in ≥5%, n (%)
Diarrhoea
Asthenia
Dyspnoea
Anaemia
Neutropenia
18 (7)
22 (9)
20 (8)
12 (5)
7 (3)
6 (2)
11 (4)
10 (4)
Jänne et al. Ann Oncol 2016; 27 (suppl 6): abstr LBA47_PR

60. Interim analysis Final analysis
LBA38: Interim safety and clinical activity in patients with advanced NSCLC from a multi-cohort phase 1 study of ramucirumab (R) plus pembrolizumab (P) – Herbst RS, et al
Study objective
To assess the safety and tolerability of adding ramucirumab to pembrolizumab
Phase 1a: DLT assessment (n=6–12) Primary: Safety and tolerability
Secondary: PK
Phase 1b: Cohort expansion (n=155)
Treatment up to 35 cycles, until PD or discontinuation for other reason
Schedule 1: Gastric/GEJ, BTC
3+3 design (n=3–6)
Ramucirumab 8 mg/kg D1, 8
Pembrolizumab 200 mg D1
Both IV q3w
Cohort A: 15 Gastric/GEJ (2nd-3rd line)
Cohort A1: 25 BTC (2nd-3rd line)
Cohort A2: 25 Gastric/GEJ (1st line)
Schedule 2: Gastric/GEJ, NSCLC, UC
3+3 design (n=3–6)
Ramucirumab 10 mg/kg D1
Pembrolizumab 200 mg D1
Both IV q3w
Interim analysis
Final analysis
Cohort B: 15 Gastric/GEJ (2nd-3rd line)
Cohort C: 25 NSCLC (2nd-4th line)
Cohort D: 25 UC (2nd-4th line)
Cohort E: 25 NSCLC (1st line)
Key inclusion criteria
ECOG PS 0–1, squamous or nonsquamous NSCLC with PD on prior therapy (Cohort C)
Patients with known EGFR or ALK mutations eligible only if they have received prior targeted therapy
Herbst et al. Ann Oncol 2016; 27 (suppl 6): abstr LBA38

61. There were no grade 4/5 TRAEs
LBA38: Interim safety and clinical activity in patients with advanced NSCLC from a multi-cohort phase 1 study of ramucirumab (R) plus pembrolizumab (P) – Herbst RS, et al
Key results
There were no grade 4/5 TRAEs
Objective response occurred in 8 (30%) patients (1 unconfirmed) and are ongoing in all responders; DCR was 85%
Conclusions
There were no new safety signals with ramucirumab + pembrolizumab, with a low incidence of grade 3 AEs
In squamous and nonsquamous NSCLC there was promising clinical activity with the ramucirumab + pembrolizumab combination
TRAE of interest, n (%)
Cohort C: NSCLC (n=27)
Any grade
Grade 3
Endocrine disorders
6 (22)
1 (4)
Hypertension
5 (19) -
Diarrhoea
3 (11)
Infusion-related reaction
2 (7)
Elevated transaminase
Proteinuria
Herbst et al. Ann Oncol 2016; 27 (suppl 6): abstr LBA38

62. Other malignancies
SCLC and mesothelioma

63. Placebo BID PO (3 days on/4 days off) + paclitaxel 80 mg/m2 D1, 8, 15
1423O: Randomized phase 2 study of investigational aurora A kinase (AAK) inhibitor alisertib (MLN8237) + paclitaxel (P) vs placebo + P as second line therapy for small-cell lung cancer (SCLC) – Owonikoko TK, et al
Study objective
To investigate the efficacy and safety of alisertib + paclitaxel in SCLC
Key patient inclusion criteria
Histologically/cytologically confirmed SCLC
Relapse <180 days after last dose of platinum-based chemotherapy
ECOG PS 0–1
(n=178)
Alisertib 40 mg BID PO (3 days on/4 days off) + paclitaxel 60 mg/m2 D1, 8, 15
(n=89)
PD / toxicity
Stratification
Type of relapse (sensitive vs. resistant/refractory)
Brain metastases at baseline R
1:1
Placebo BID PO (3 days on/4 days off) + paclitaxel 80 mg/m2 D1, 8, 15
(n=89)
PD / toxicity
Primary endpoint
PFS (ITT population)
Secondary endpoints
Safety/tolerability, OS, ORR, DCR, DoR, biomarkers (c-Myc expression)
Owonikoko et al. Ann Oncol 2016; 27 (suppl 6): abstr 1423O

64. Primary endpoint: PFS (ITT population) Median PFS, days (months)
1423O: Randomized phase 2 study of investigational aurora A kinase (AAK) inhibitor alisertib (MLN8237) + paclitaxel (P) vs placebo + P as second line therapy for small-cell lung cancer (SCLC) – Owonikoko TK, et al
Key results
Primary endpoint: PFS (ITT population)
1.0
Treatment
Median PFS, days (months)
Alisertib + paclitaxel
101 (3.32)
Placebo + paclitaxel
66 (2.17)
0.8
0.6
IVRS HR (95%CI) 0.77 (0.557, 1.067) Log rank p=0.113
Corrected* HR (95%CI) 0.71 (0.509, 0.985) Log rank p=0.038
Survival probability
0.4
0.2
0.0 30 60 90
120
150
180
210
240
270
300
Survival time, days
89 89
74 65
55 45
41 27
28 19
13 12
10 8
6 4
3 3
0 3
0 0
Group
Alisertib
Placebo
HR (95%CI)
p-value
PFS (resistant/refractory relapse patients), days 87 50
0.659 (0.442, 0.983)
0.0372
OS, days
186
165
0.93 (0.652, 1.341)
0.714
ORR, % 22 18
DCR, % 58 46
*Stratification definition of sensitive was amended after 30% of patients had been enrolled but prior to analysis to better reflect the guidelines
Owonikoko et al. Ann Oncol 2016; 27 (suppl 6): abstr 1423O

65. Rates of AEs were higher with alisertib
1423O: Randomized phase 2 study of investigational aurora A kinase (AAK) inhibitor alisertib (MLN8237) + paclitaxel (P) vs placebo + P as second line therapy for small-cell lung cancer (SCLC) – Owonikoko TK, et al
Key results (cont.)
Rates of AEs were higher with alisertib
Conclusions
Alisertib + paclitaxel showed favourable PFS vs. paclitaxel alone with a significant difference observed in the protocol redefined subgroup of resistant/refractory tumours
The combination did not reach statistical significance for OS, ORR and DCR
Greater toxicity was observed with alisertib + paclitaxel vs. paclitaxel alone
Alisertib
(n=87)
Placebo
(n=89)
Grade >3 AEs, % 76 51
Drug-related grade >3 AEs, % 67 25
Drug-related serious AEs, % 32 7
AEs leading to discontinuation of study drug, % 15 6
Owonikoko et al. Ann Oncol 2016; 27 (suppl 6): abstr 1423O

66. 1425PD: Clinical activity, safety and predictive biomarkers results from a phase Ia atezolizumab (atezo) trial in extensive-stage small cell lung cancer (ES-SCLC) – Sequist LV, et al
Study objective
To assess the safety and clinical therapy of atezolizumab in extensive stage (ES)-SCLC
Methods
Phase 1a study of atezolizumab monotherapy 15 mg/kg or 1200 mg q3w IV in ES-SCLC
Tumours were assessed by RECIST v1.1 criteria and irRC assessments
Key results
As of March 31, 2016, 17 patients were enrolled and had a minimum follow-up of 10 months
There were seven grade 3–4 TRAEs in 2 patients and one grade 5 (hepatic failure)
The ORR was 5.9% (95%CI 0.2, 28.7) by RECIST and 17.6% (95%CI 3.8, 43.4) by irRC
mPFS was 1.5 months (95%CI 1.2, 2.7) by RECIST and 2.9 months (95%CI 1.2, 6.1) by irRC
mOS was 5.9 months (95%CI 4.3, 12.6)
There was a trend toward improved PFS (per irRC) and OS in tumours with higher expression (≥median) of PD-L1 mRNA and T-effector gene signature
Conclusions
Atezolizumab in ES-SCLC had a tolerable safety profile
Modest single-agent activity of atezolizumab in ES-SCLC is reported
Sequist et al. Ann Oncol 2016; 27 (suppl 6): abstr 1425PD

67. 1426PD: Phase II study of roniciclib in combination with cisplatin/etoposide or carboplatin/etoposide as first-line therapy in subjects with extensive-disease small cell lung cancer (ED-SCLC) – Reck M, et al
Study objective
To evaluate the efficacy and safety of roniciclib in combination with cisplatin + etoposide or carboplatin + etoposide in extensive-disease (ED)-SCLC
Roniciclib 5 mg BID 3 days-on/4 days-off q3w*
(n=70)
PD / toxicity / other
Key patient inclusion criteria
Histologically or cytologically confirmed ED-SCLC
ECOG 0–1
Life expectancy ≥12 weeks
Serum sodium ≥120 mmol/L
(n=140)
Stratification
Gender
Serum lactate dehydrogenase (≤2.5/>2.5 x upper limit of normal) R
Placebo BID 3 days-on/4 days-off q3w*
(n=70)
PD / toxicity / other
Primary endpoint
PFS
Secondary endpoints
OS, TTP, ORR and safety
*For 6 cycles combined with standard chemotherapy (etoposide [100 mg/m2 D1, 2, 3] with either cisplatin [75 mg/m2 D1] or carboplatin [5 mg/mL/min D1] q3w) followed by roniciclib or placebo monotherapy
Reck et al. Ann Oncol 2016; 27 (suppl 6): abstr 1426PD

68. 1426PD: Phase II study of roniciclib in combination with cisplatin/etoposide or carboplatin/etoposide as first-line therapy in subjects with extensive-disease small cell lung cancer (ED-SCLC) – Reck M, et al
Key results
No significant differences with roniciclib vs. placebo were seen in the efficacy endpoints
Median PFS 4.9 vs. 5.5 months (HR 1.242; 95%CI 0.820, 1.881; p=0.8653)
Median OS 10.6 vs months (HR 1.430; 95%CI 0.785, 2.606; p=0.8691)
Median TTP 5.4 vs. 5.5 months (HR 1.047; 95%CI 0.665, 1.648; p=0.5900)
ORR 60.6% vs. 74.6% (p=0.9685)
The incidence of serious AEs was higher in the roniciclib group (55.7% vs. 34.3%)
There were 9 fatal AEs in the roniciclib arm (2 attributed to roniciclib: sepsis and bronchopulmonary haemorrhage) vs. 1 in the placebo arm
Conclusion
Addition of roniciclib to standard-of-care chemotherapy in ED-SCLC patients increased toxicity without improving efficacy
TEAEs (occurring in >50% any grade), n (%)
Roniciclib (n=70)
Placebo (n=70)
Any
Grade 3
Grade 4
Nausea
46 (65.7)
5 (7.1)
33 (47.1)
2 (2.9)
Vomiting
43 (61.4)
7 (10.0)
14 (20.0)
1 (1.4)
Fatigue
39 (55.7)
27 (38.6)
4 (5.7)
Decreased neutrophil count
38 (54.3)
13 (18.6)
22 (31.4)
45 (64.3)
18 (25.7)
23 (32.9)
Reck et al. Ann Oncol 2016; 27 (suppl 6): abstr 1426PD

69. 1179PD: Low dose CT scan screening versus empiric surveillance in asbestos exposed subjects: Update of ATOM 002 study – Fasola G, et al
Study objective
To evaluate low-dose CT scan screening in reducing mortality for lung cancer and/or malignant pleural mesothelioma in asbestos-exposed former workers
Methods
Prospective non-randomised study of 2433 occupationally asbestos-exposed men with follow-up from 2002 to 2011
A Cox regression model was used for all-cause, all cancers, lung cancer and pleural mesothelioma survival
Multivariate models were adjusted for smoking habits, age, level of asbestos exposure and Charlson-Quan comorbidity index
Key results
926 men were allocated to the low-dose CT scan screening cohort and 1507 to the standard follow-up cohort
Lung cancer crude mortality was 99.4 per 100,000 person-year in the low-dose CT scan screening cohort compared with per 100,000 person-year in the standard follow-up cohort
Fasola et al. Ann Oncol 2016; 27 (suppl 6): abstr 1179PD

70. Hazard ratio (multivariate)
1179PD: Low dose CT scan screening versus empiric surveillance in asbestos exposed subjects: Update of ATOM 002 study – Fasola G, et al
Key results (cont.)
There was a significant reduction in lung cancer and all-cause mortality with low-dose CT scan screening, with no difference in all cancers or pleural mesothelioma mortality
There was also a reduction in lung cancer mortality compared to the general Italian population in the CT scan screening population (standardised mortality ratio 0.51; 95%CI 0.22, 1.01)
Conclusion
In this observational study, compared with national figures, low-dose CT scan screening reduced the risk of death from lung cancer in asbestos exposed men
All causes
HR 0.61; 95%CI 0.44, 0.84
All cancers
HR 0.97; 95%CI 0.62, 1.50
Lung cancer
HR 0.41; 95%CI 0.17, 0.96
Cancer of pleura
HR 0.86; 95%CI 0.31, 2.41
0.0
0.5
1.0
1.5
2.0
2.5
3.0
Hazard ratio (multivariate)
Fasola et al. Ann Oncol 2016; 27 (suppl 6): abstr 1179PD

71. Other malignancies
Rare tumours

72. 1509PD: Quality of resection and outcome in stage III thymic epithelial tumors (TET): A retrospective analysis of 150 cases from the national network RYTHMIC experience – Bluthgen MV, et al
Study objective
To evaluate the value of recommendations made by the board of the RYTHMIC network for the management of stage III thymic epithelial tumours (TET)
Methods
A retrospective analysis of 150 patients with stage III TET was conducted; this analysis included patients whose cases were discussed at the RYTHMIC board between January and December 2015
Clinical, pathologic and surgical data were prospectively collected in a central database
Survival rates were based on Kaplan-Meier estimation, and DFS and OS were evaluated using Cox proportional hazard models
Baseline characteristics
The majority of patients were male (57%); median age was 62 [range 18–91] years
Thymoma A–B2 and thymoma B3–thymic carcinoma were reported in 51% and 47% of patients, respectively
Overall, 23% of patients displayed autoimmune disease (predominantly myasthenia 26 of 34 patients)
Bluthgen et al. Ann Oncol 2016; 27 (suppl 6): abstr 1509PD

73. 1509PD: Quality of resection and outcome in stage III thymic epithelial tumors (TET): A retrospective analysis of 150 cases from the national network RYTHMIC experience – Bluthgen MV, et al
Key results
A total of 134 (89%) patients received surgery
Rate of complete resection (R0) was 53%
90 (60%) patients received postoperative radiotherapy
26 (68%) patients received induction chemotherapy
Overall survival for overall population
Disease-free survival for overall population
1.0
1.0
0.8
0.8
0.6
0.6
Probability of overall survival
Probability of disease-free survival
0.4
5-year OS: 88% 10-year OS: 68%
Median follow-up: 23.4 months (range 0.3–266.5)
0.4
5-year DFS: 32% 10-year DFS: 8%
Median DFS: 43.9 months (95%CI 35.4, 52.3)
0.2
0.2
0.0
0.0 12 24 36 48 60 72 84 96
108
120 12 24 36 48 60 72 84 96
108
120
Time, months
Time, months
Number at risk
Number
at risk
150 97 24 54 39 32 25 21 19 16 11
150 90 57 36 21 13 11 8 5 4 3
Bluthgen et al. Ann Oncol 2016; 27 (suppl 6): abstr 1509PD

74. Disease-free survival
1509PD: Quality of resection and outcome in stage III thymic epithelial tumors (TET): A retrospective analysis of 150 cases from the national network RYTHMIC experience – Bluthgen MV, et al
Key results (cont.)
Conclusions
Improved outcomes are observed with surgery followed by radiotherapy, regardless of R0
Patients with stage III TET initially considered ineligible for surgery should be reassessed for resection following induction chemotherapy
Multivariate analysis in overall population
Overall survival
HR (95%CI)
p-value
Histology (A–B2 vs. B3–TC)
0.19 (0.05, 0.70)
0.02
Modality surgery (vs. no surgery)
0.04 (0.01, 0.20)
<0.001
Multivariate analysis in surgical population
Disease-free survival
HR (95%CI)
p-value
Histology (A–B2 vs. B3–TC)
0.50 (0.30, 0.90)
0.02
Adjuvant radiotherapy (vs. no radiotherapy)
0.40 (0.20, 1.00)
0.05
Bluthgen et al. Ann Oncol 2016; 27 (suppl 6): abstr 1509PD

75. 1510PD: Pathological central review of 400 thymic epithelial tumors (TET): The national network RYTHMIC experience – Molina T, et al
Study objective
To describe the discordances in institution and review panel diagnoses of thymic epithelial tumours (TET) and the impact on disease management
Methods
A central review of 400 patients diagnosed with TET between January 2012 and December 2015 was conducted by a panel of 10 expert pathologists
Agreement or disagreement between the initial institution and the panel review was assessed according to WHO 2004/2015 guidelines for histologic typing, and Masaoka- Koga and the new ITMIG proposals for staging
Discordances were classified as:
“Major” when disagreement between panel review and the initial institution would have changed the therapy or management of patients
“Minor” when disagreement between panel review and the initial institution would not have changed the therapy or management of patients
Key results
Overall, 178 discordances were identified in 159 (40%) patients
118 discordances concerned histological diagnosis
60 discordances concerned stage
Molina et al. Ann Oncol 2016; 27 (suppl 6): abstr 1510PD

76. Total discordances according to stage before and after central review
1510PD: Pathological central review of 400 thymic epithelial tumors (TET): The national network RYTHMIC experience – Molina T, et al
Key results (cont.)
Sub-diagnosis of stage III was the most frequently observed discordance
31 occurrences of major discordances were observed in 29 (7%) patients
In 17 cases, adjuvant radiotherapy should have been recommended
In 1 case, adjuvant radiotherapy should not have been recommended
In 7 cases, primary treatment should have been modified
In 4 cases, follow-up treatment should have been modified
Conclusion
These results indicate the importance of expert histopathological panel diagnosis for thymic malignancies and the need for improved decision making, particularly with regard to the application of postoperative radiotherapy
Total discordances according to stage before and after central review
Total discordances according to histology before and after central review
Local
Review I
IIA
IIB
III
IVA
IVB A AB B1 B2 B3 TC
NOS
Other
Other diagnosis
-30
-20
-10 10 20 30
-40
-30
-20
-10 10 20 30 40
Molina et al. Ann Oncol 2016; 27 (suppl 6): abstr 1510PD

77. Pasireotide 60 mg/month + everolimus 10 mg/day
416O: Efficacy and safety of pasireotide LAR or everolimus alone, or in combination in patients with advanced carcinoids (NET) of the lung/thymus: Results from the randomized, phase 2 LUNA study – Ferolla P, et al
Study objective
To evaluate the efficacy and safety of everolimus, pasireotide and pasireotide + everolimus in patients with progressive carcinoids of lung/thymus
Pasireotide
60 mg/month IM
(n=41) PD
Key patient inclusion criteria
Metastatic RECIST progressive carcinoids of lung/thymus
(n=124)
Everolimus
10 mg/day PO
(n=42) R
1:1:1 PD
Pasireotide 60 mg/month + everolimus 10 mg/day
(n=41) PD
Primary endpoint
PFR at 9 months
Secondary endpoints
PFS, DCR, safety
Ferolla et al. Ann Oncol 2016; 27 (suppl 6): abstr 416O

78. Pasireotide + everolimus
416O: Efficacy and safety of pasireotide LAR or everolimus alone, or in combination in patients with advanced carcinoids (NET) of the lung/thymus: Results from the randomized, phase 2 LUNA study – Ferolla P, et al
Key results
Progression-free rate at 9 months was: pasireotide 39.0% (95%CI 24.2, 55.5); everolimus 33.3% (95%CI 19.6, 49.5); pasireotide + everolimus 58.5% (95%CI 42.1, 73.7)
Most common AEs in the pasireotide + everolimus arm were: hyperglycaemia (88%), diarrhoea (78%), weight decrease (56%), asthenia (37%), and stomatitis (34%)
Conclusions
In the treatment of advanced lung/thymus carcinoids, promising 9-month PFR was seen in all treatment arms, and particularly in the combination arm
No new safety signals were observed for pasireotide or everolimus
Best overall response (9-month)
Pasireotide
Everolimus
Pasireotide + everolimus
CR, %
PR, % 2
SD, % 34 31 49
PD, % 17
Not assessed, % 44 60 42
Ferolla et al. Ann Oncol 2016; 27 (suppl 6): abstr 416O