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J. Aerts

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MO24 - NSCLC - Chemotherapy III (ID 110)

Event: WCLC 2013
Type: Mini Oral Abstract Session
Track: Medical Oncology
Presentations: 1

Moderators:R. Feld, S. Peters
Coordinates: 10/30/2013, 10:30 - 12:00, Parkside Ballroom A, Level 1

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MO24.08 - Survival outcomes among NSCLC patients in Europe receiving platinum-based therapies as first-line treatment: results from the FRAME observational study (ID 1944)

10:30 - 12:00 | Author(s): J. Aerts

Abstract
Presentation
Slides

Background
FRAME was a European non-interventional prospective observational study of patients with advanced or metastatic non-small cell lung cancer (NSCLC) initiating platinum-based therapies as first-line treatment (FLT).

Methods
Patients were enrolled between April 2009 and February 2011. Consenting adult NSCLC (Stage III/IV) patients initiating FLT with a platinum-based doublet chemotherapy, with or without an additional targeted agent, were eligible for the study. The choice of FLT was left to physician discretion, as per routine clinical practice. The primary objective of FRAME was to evaluate overall survival (OS) among different platinum-based treatment cohorts in patients with and without additional targeted therapy. Secondary objectives included the evaluation of OS in patients with different histological subtypes of NSCLC. Survival outcomes were assessed using Kaplan-Meier analysis, and unadjusted estimates are presented.

Results
A total of 1564 eligible patients from 11 EU countries were observed. Patient cohorts were: pemetrexed + platinum, gemcitabine + platinum, vinorelbine + platinum, taxanes + platinum and other therapy + platinum. Table 1 shows a subset of baseline patient characteristics, which varied across several parameters in the treatment cohorts, including age, performance status (PS), stage and histology. The median OS across the 4 main treatment cohorts was 10.3 months (95% CI: 9.5-11.2). A subset of overall survival estimates in the different treatment cohorts is shown in Table 1.

Table 1. Select baseline patient characteristics and overall survival

	Baseline Patient Characteristics				Overall Survival Estimates (unadjusted)
Treatment Cohort[a]	Age ≥70 Years (%)	ECOG PS of 2/3 (%)	Stage IV (%)	Non-squamous Histology (%)	All patients Median OS in Months (95% CI)	Non-squamous Median OS in Months (95% CI)	Non-squamous Cisplatin[b] Median OS in Months (95% CI)
Pemetrexed + Platinum[b ](n=569)	23	18	86	97	10.7 (9.4-12.3) [n=569]	10.6 (9.4-12.0) [n=553]	11.6 (9.9-13.8) [n=374]
Gemcitabine + Platinum[b] (n=360)	35	11	74	56	10.0 (8.4-11.8) [n=360]	8.4 (7.0-10.6) [n=201]	8.4 (6.7-10.8) [n=107]
Taxanes + Platinum[b ](n=295)	36	23	75	64	9.1 (8.0-11.3) [n=295]	8.1 (7.4-10.1) [n=189]	9.6 (7.1-14.1) [n=44]
Vinorelbine + Platinum[b] (n=300)	28	15	67	53	10.7 (8.9-12.8) [n=300]	10.1 (8.0-13.1) [n=160]	9.9 (7.2-13.4) [n=91]

[a]A fifth cohort, the ‘other’ + platinum cohort contained a small number of subjects (n=40) and it was not included in the analyses presented here [b]Cisplatin is the platinum agent in the EMA approved prescription drug label

Conclusion
This observational study of first-line treatment for advanced NSCLC provides data describing patients and their survival outcomes in a real-world European practice setting between 2009 and 2012.

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P1.09 - Poster Session 1 - Combined Modality (ID 212)

Event: WCLC 2013
Type: Poster Session
Track: Combined Modality
Presentations: 1

Moderators:
Coordinates: 10/28/2013, 09:30 - 16:30, Exhibit Hall, Ground Level

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P1.09-009 - Preliminary Safety and Treatment Delivery Data During Concurrent Phase of Chemoradiation Therapy of the PROCLAIM Trial: A Phase 3 Trial of Pemetrexed, Cisplatin, and Radiotherapy Followed by Consolidation Pemetrexed Versus Etoposide, Cisplatin, and Radiotherapy Followed by Consolidation Cytotoxic Chemotherapy of Choice in Patients With Stage III Nonsquamous Cell Lung Cancer. (ID 1196)

09:30 - 16:30 | Author(s): J. Aerts

Abstract

Background
Pemetrexed platinum regimens, unlike other regimens, can be given at full systemic doses with thoracic radiation therapy (TRT) in locally advanced stage III nonsquamous non–small cell lung cancer (NSCLC). Study JMIG was initiated to determine if this finding would translate into a survival advantage versus contemporary standard of care.

Methods
Study JMIG randomized patients with stage III unresectable nonsquamous NSCLC to experimental Pem+Cis (pemetrexed plus cisplatin and concurrent TRT for three 21-day cycles, followed by consolidation pemetrexed) or to control Etop+Cis (etoposide plus cisplatin and concurrent TRT for two 28-day cycles, followed by consolidation chemotherapy regimen of choice [excluding pemetrexed]). The primary objective was overall survival of Pem+Cis compared with Etop+Cis with safety as a secondary objective using Common Terminology Criteria for Adverse Events (CTCAE). Adverse event incidences were analyzed using Fisher’s exact test (2-sided α=0.05).

Results
Of 598 randomized patients, 555 received treatment: 283 Pem+Cis and 272 Etop+Cis. Baseline characteristics were similar (Pem+Cis/Etop+Cis); age (mean±SD) 59.2±9.5/58.7±9.3 years; women, n=114 (40.3%) / n=105 (38.6%); stage IIIB, n=153 (54.1%)/n=138 (50.7%); Eastern Cooperative Oncology Group performance standard of 1, n=138 (48.8%)/n=137 (50.4%); and planned target volume (mean±SD) 628.9 ±463.3/581.2±417.0 ml. Pem+Cis mean weekly dose intensities were 95.9% for both pemetrexed and cisplatin; Etop+Cis dose intensities were 96.4% and 94.1% for etoposide and cisplatin. TRT therapies were similar (Pem+Cis/Etop+Cis); TRT median (range) of 66.0 (2.0–66.3) gray (Gy)/66.0 (2.0–66.0) Gy, mean (SD) number of fractions 31.4 (4.3)/31.1 (5.2), V20 of 27.5% (6.5%)/26.7% (7.3%). Table 1 summarizes AEs during the concurrent phase by treatment. Few patients (n≤4) had grade 3 or 4 CTCAE of mucositis/stomatitis or rash. Pem+Cis had fewer SAEs of febrile neutropenia and pneumonia but increased vomiting compared with Etop+Cis. Nine patients died during the concurrent phase (not included in this safety analysis by treatment to preserve the integrity of final efficacy analysis).

Table 1. Summary of Common Terminology Criteria for Adverse Events Grade 3 Plus 4 Occurring in ≥2% of Patients Randomized and Treated
CTCAE (Grades 3 and 4)	Pem+Cis N=283 n (%)	Etop+Cis N=272 n (%)	p-value
Patients with ≥1 CTCAE*	170 (60.1)	186 (68.4)	0.042
Neutrophils/granulocytes*	52 (18.4)	78 (28.7)	0.005
Leukocytes*	44 (15.5)	65 (23.9)	0.014
Esophagitis	42 (14.8)	47 (17.3)	0.488
Lymphopenia	48 (17.0)	37 (13.6)	0.290
Hemoglobin	14 (4.9)	20 (7.4)	0.289
Febrile neutropenia	9 (3.2)	18 (6.6)	0.075
Dysphagia	18 (6.4)	16 (5.9)	0.861
Platelets	15 (5.3)	16 (5.9)	0.854
Vomiting	12 (4.2)	13 (4.8)	0.839
Hypokalemia	6 (2.1)	12 (4.4)	0.153
Infection—lung (pneumonia)*[a]	1 (0.4)	9 (3.3)	0.010
Dehydration	11 (3.9)	8 (2.9)	0.643
Nausea	13 (4.6)	8 (2.9)	0.376
Anorexia	10 (3.5)	7 (2.6)	0.625
Fatigue	9 (3.2)	6 (2.2)	0.603
Hyponatremia	5 (1.8)	6 (2.2)	0.768
Thrombosis/thrombus/embolism	7 (2.5)	5 (1.8)	0.772

Abbreviations: Cis = cisplatin; CTCAE = Common Terminology Criteria for Adverse Events, Version 3.0; Etop = etoposide; N = number of patients dosed; n = number of patients with at least one CTCAE; Pem = pemetrexed.
* Statistically significant; p<.05 based on Fisher’s exact test.
[a] CTCAE was defined as Infection (clinical/microbio)—Gr3/4 neutrophils—Pulmonary/upper respiratory—Lung (pneumonia).

Conclusion
During the concurrent treatment phase, patients with stage III locally advanced nonsquamous NSCLC in either treatment arm received comparable systemic therapy; however Pem+Cis had significantly lower incidences of some toxicities. Further toxicity differences may emerge with longer follow-up.

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P3.10 - Poster Session 3 - Chemotherapy (ID 210)
- Event: WCLC 2013
- Type: Poster Session
- Track: Medical Oncology
- Presentations: 1
- Moderators:
- Coordinates: 10/30/2013, 09:30 - 16:30, Exhibit Hall, Ground Level
- 12594
  
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  P3.10-002 - Resource utilization of NSCLC patients receiving platinum-based therapies across Europe; results from the FRAME observational study (ID 183)
  
  09:30 - 16:30 | Author(s): J. Aerts
  Abstract
  
  Background
  FRAME was a non-interventional, prospective observational study of advanced or metastatic non-small cell lung cancer (NSCLC) patients initiating first-line treatment (FLT) with platinum-based therapies in a routine practice setting across 11 European countries.
  
  Methods
  Patient enrollment occurred between April 2009 and February 2011. Consenting adults with Stage IIIB or IV NSCLC receiving platinum-based doublet chemotherapy with or without an additional targeted agent as FLT were eligible for this study. Patients were under routine treatment for NSCLC by their doctors and treatment choice and resource use were at the discretion of the treating physician. Secondary objectives of the study included determining resource use during FLT. Hospitalizations, outpatient visits, concomitant therapy use, transfusions and the use of colony stimulating factors (CSFs) are reported here. Cohorts were not adjusted for multivariate parameters prohibiting statistical comparisons.
  
  Results
  Evaluable patients (n=1564) were categorized into 4 main cohorts based on their FLTs: pemetrexed + platinum (n=569), gemcitabine + platinum (n=360), taxanes + platinum (n=295) or vinorelbine + platinum (n=300). Forty of the evaluable patients received other platinum-doublet treatments and were excluded from the analyses presented here.Across the four main cohorts, 55% of patients were hospitalized.A majority (61%) of hospitalizations were preplanned (71% in the pemetrexed cohort, 45% in the gemcitabine cohort, 67% in the taxanes cohort and 53% in the vinorelbine cohort). Among the unplanned hospitalizations, 54% were related to an adverse event (54% in the pemetrexed cohort, 54% in the gemcitabine cohort, 55% in the taxanes cohort, and 55% in the vinorelbine cohort). The mean (95%-confidence interval) duration of hospitalizations was 13 days (11.6 to 14.6) for pemetrexed (median=9 days), 11 days (9.4 to 12.8) for gemcitabine (median=7 days),17 days (14.0 to 19.7) for taxanes (median=12 days), and 13 days (11.3 to 15.0) for vinorelbine (median=9 days). Nearly half of patients (47%) were seen in an outpatient setting with most outpatient visits (82%)planned for scheduled treatments. Nineteen percent of patients received ≥1 transfusion (16% in the pemetrexed cohort, 24% in the gemcitabine cohort, 15% in the taxanes cohort and 24% in the vinorelbine cohort). Nearly all (94%) of these patients received packed red blood cells. Nineteen percent of patients received ≥1 colony stimulating factor (CSF), which included G-CSF (69%), or erythropoietin (39%). During therapy, 82% of patients used antiemetics and antinauseants, 58% used steroids, 40% used analgesics, and 24% used antibiotics. Twenty-eight percent of patients received radiation during FLT and most often radiation was delivered concurrently with chemotherapy (66% overall, 66% in the pemetrexed cohort, 54% in the gemcitabine cohort, 68% in the taxanes cohort, and 73% in the vinorelbine cohort).
  
  Conclusion
  The FRAME study provides unique, real-life data reflecting prospectively collected information on resource use not accessible in a clinical trial setting. This study revealed several important findings regarding real-world resource use during NSCLC therapy including data on hospitalizations, outpatient visits, transfusions, concomitant treatments, and radiation.