A phase II multicentre study of ziv-aflibercept in combination with cisplatin and pemetrexed in patients with previously untreated advanced/metastatic non-squamous non-small cell lung cancer.

BACKGROUND: This study evaluated the efficacy and safety of ziv-aflibercept in combination with cisplatin and pemetrexed in non-small cell lung cancer (NSCLC).
METHODS: This single arm, multicentre phase II trial enrolled patients with previously untreated, locally advanced or metastatic non-squamous NSCLC. Patients received intravenous ziv-aflibercept 6 mg kg(-1), pemetrexed 500 mg m(-2), and cisplatin 75 mg m(-2), every 21 days for up to six cycles. Maintenance administration of ziv-aflibercept was to continue until disease progression, intolerable toxicity or other cause for withdrawal. The co-primary end points were objective response rate (ORR) and progression-free survival (PFS). Planned sample size was 72 patients.
RESULTS: The study was closed prematurely because of three confirmed and two suspected cases of reversible posterior leukoencephalopathy syndrome (RPLS). A total of 42 patients were enrolled. Median age was 61.5 years; 55% were male, 86% Caucasian and 50% had Eastern Cooperative Oncology Group performance status (ECOG PS)=0. A median of four cycles of ziv-aflibercept was administered. The most common treatment-emergent adverse events (TEAEs) of any grade were nausea (69%) and fatigue (67%), with hypertension (36%) as the most common grade 3/4 TEAE. Of the 38 evaluable patients, ORR was 26% and median PFS was 5 months.
CONCLUSION: Cases of RPLS had been observed in other studies in the ziv-aflibercept clinical development programme but the rate observed in this study was higher than previously observed. This might be related to declining renal function and/or hypertension. Although ORR and PFS were in accordance with most historical first-line NSCLC studies, this combination of ziv-aflibercept/cisplatin/pemetrexed will not be further explored in NSCLC.

Cancer growth is dependent upon angiogenesis to maintain a source of nutrition and oxygen (Folkman, 1995), and vascular endothelial growth factor (VEGF) has a key role in tumour angiogenesis (Ferrara and Davis-Smyth, 1997). Non-small cell lung cancer (NSCLC) produces VEGF, and high serum levels of VEGF are correlated with poor prognosis (Korpanty ). Anti-angiogenic therapy thus aims to disrupt blood supply to tumours and has proven clinical benefit in non-squamous NSCLC (Jain, 2001).

Combination chemotherapy is used for the first-line treatment of advanced/metastatic NSCLC (Schiller ). The addition of the anti-VEGF antibody, bevacizumab, to carboplatin/paclitaxel in this setting improved response rate, progression-free survival (PFS), and overall survival (OS; Sandler ). Similarly, bevacizumab improved PFS when added to cisplatin/gemcitabine, although OS was not significantly prolonged as a secondary end point in this case (Reck ). For non-squamous histology, cisplatin/pemetrexed is a very active combination chemotherapy (Scagliotti ), and thus combinations of platinum/pemetrexed with bevacizumab or other anti-angiogenics are of strong interest for the first-line treatment of advanced/metastatic non-squamous NSCLC (Patel ).

Ziv-aflibercept (ZALTRAP, Sanofi, Bridgewater, NJ, USA and Regeneron Pharmaceuticals, Tarrytown, NY, USA) is a recombinant fusion protein consisting of portions of human VEGF receptor extracellular domains fused to the Fc portion of human immunoglobulin (Gaya and Tse, 2012). Ziv-aflibercept binds VEGF-A by acting as a high-affinity ligand trap to prevent binding to its endogenous receptor VEGFR-2, thereby inhibiting VEGF-induced angiogenesis in preclinical models (Lassoued ). Endothelial cells expressing high levels of VEGFR-2 were highly susceptible to blockade by ziv-aflibercept (Sitohy ). In addition, ziv-aflibercept binds PIGF (placental growth factor) and VEGF-B, which could potentially inhibit cancer invasion (Dowlati, 2010). Studies have investigated ziv-aflibercept as a single agent or in combination with other chemotherapeutic agents in treatment of various types of cancers (Lockhart ; Tew ; de Groot ; Isambert ). In August 2012, ziv-aflibercept was approved by the US FDA for use in metastatic colorectal cancer based on the results of VELOUR trial (Van Cutsem ). A phase II study using ziv-aflibercept as monotherapy demonstrated objective responses in heavily pretreated patients with advanced adenocarcinoma of the lung (Leighl ), and improvement in response and PFS (but not OS) was observed in combination with docetaxel as second-line treatment of NSCLC (Ramlau ).

We report the results of a phase II trial of ziv-aflibercept in combination with cisplatin and pemetrexed in patients with advanced or metastatic non-squamous NSCLC. This study was conducted after a phase I trial using the same regimen of ziv-aflibercept/cisplatin/pemetrexed (Diaz-Padilla ). That phase I trial determined the recommended dose of ziv-aflibercept (6 mg kg−1 every 21 days) to be used in the current phase II trial, which aimed to evaluate the efficacy and safety of ziv-aflibercept in combination with cisplatin and pemetrexed in the first-line treatment of advanced/metastatic NSCLC.

Materials and methods

Eligibility

Patients eligible for this study had histologically/cytologically confirmed, untreated, locally advanced/metastatic NSCLC, and they had to have measurable disease as per the Response Evaluation Criteria in Solid Tumors (RECIST) criteria (Therasse ). Patients with squamous histology and/or cavitating lesions were excluded. Patients were 18 years of age or older, and had an Eastern Cooperative Oncology Group performance status (ECOG PS) of 0 or 1, with adequate bone marrow, renal, and hepatic functions and calculated creatinine clearance (CrCL) ⩾60 ml min−1. Patients were excluded from the study if they had brain or central nervous system metastases; systolic blood pressure (BP) >150 mm Hg and/or diastolic blood pressure >100 mm Hg; bleeding diathesis or evidence of active bleeding; or recent significant cardiovascular, cerebrovascular, or thromboembolic conditions.

The protocol was approved by the Institutional Review Boards at each participating institution. Informed consent was obtained from each patient.

Study design

This is a single arm, open label, multicentre phase II study (ClinicalTrials.gov identifier: NCT00794417). Patients received the three-drug combination intravenously on day 1 of every 21 days, with ziv-aflibercept (6 mg kg−1) first, followed by pemetrexed (500 mg m−2) and cisplatin (75 mg m−2). Premedications consisted of folic acid, vitamin B12, and dexamethasone as a prophylactic measure to reduce pemetrexed-related toxicities and standard anti-emetics. Patients could receive up to six cycles of combination therapy. For patients who completed the combined chemotherapy, maintenance ziv-aflibercept every 21 days was to continue until disease progression, intolerable toxicity, or withdrawal from the study.

End points and assessments

The two co-primary end points were objective response rate (ORR) and PFS. The ORR was defined as the proportion of patients with complete response plus partial response (CR+PR). The PFS was defined as the time interval from the first dose of combination chemotherapy to tumour progression or death, whichever occurred first. Secondary variables were the determination of the adverse events (AEs), pharmacokinetics (PK), and pharmacodynamic profiles (including anti-ziv-aflibercept antibody and hematopoiesis). Pharmacokinetic end points included the area under the concentration curve, maximum concentration (Cmax), clearance, and terminal half-life (t1/2).

Tumour imaging (CT or MRI) was performed at screening, on day 21 (±7 days) of every even numbered cycle (every 6 weeks), and when disease progression was suspected. Responses were assessed using RECIST, version 1.0 (Therasse ). Safety and tolerability were assessed at baseline and at least every 21 days, as evaluated by AEs and changes in laboratory parameters graded according to the Common Terminology Criteria for Adverse Events (CTCAE), version 3.0 (National Cancer Institute, 2006). Ziv-aflibercept (free or bound to VEGF) in plasma samples was quantified using a validated, direct enzyme-linked immunosorbent assay. A validated, non-quantitative, titre-based, bridging assay was used to detect anti-ziv-aflibercept antibodies in serum samples.

Correlative studies

The exploratory objective of the correlative studies was to evaluate changes in erythropoiesis in response to VEGF inhibition. It was hypothesised that VEGF inhibition would result in an increase in haemoglobin via increased hepatic erythropoietin production.

Statistical analysis

Statistical testing was done to determine whether the ORR was larger than 20% or whether the PFS was greater than 4.5 months. Exact test (one-sided) was used to test the null hypothesis that ORR was ⩽20% versus the alternative hypothesis that ORR was ⩾35%. Assuming type I error was not >2.5%, a sample of 72 patients would provide >80% power to test the hypothesis using exact binomial test. The calculated sample size of 72 patients would also provide >90% power to test the null hypothesis that median PFS was ⩽4.5 months versus the alternative hypothesis that PFS was ⩾6.5 months at one-sided alpha of 2.5% using one sample log-rank test.

Safety data were to be summarised. Concentrations of free ziv-aflibercept and adjusted bound ziv-aflibercept: VEGF complex were to be summarised every 21 days over the duration of the study by nominal time point. Noncompartmental parameters were calculated using WinNonlin (version 5.3, Pharsight Corporation, Mountain View, CA, USA) and model 202 (constant infusion) using nominal time points after a single dose of ziv-aflibercept. The noncompartmental analysis was performed over the dosing interval, 21 days following the first dose. All analyses used statistical software SAS (version 9.1.3, Cary, NC, USA).

Results

Patients

This study was closed prematurely because of three confirmed and two suspected but unconfirmed cases of reversible posterior leukoencephalopathy syndrome (RPLS). A total of 42 patients were enrolled from 17 participating sites across the United States and Canada between January, 2009 and December, 2010. Table 1 summarises the patient demographics. Median age was 61.5 years; 55% were male, 86% were Caucasian and 50% had ECOG PS of 0.

Table 1

Baseline demographics (N=42)

Age (years)
Median	61.5
Range (years)	38–77
Age (years) by category	N (%)
<65	23 (54.8)
⩾65	19 (45.2)
Gender	N (%)
Male	23 (54.8)
Female	19 (45.2)
Race	N (%)
African American	2 (4.8)
Asian American	4 (9.5)
Caucasian American	36 (85.7)
ECOG performance status	N (%)
0	21 (50.0)
1	21 (50.0)

Abbreviation: ECOG=Eastern Cooperative Oncology Group.

Safety evaluation

Treatment exposure and dose modifications

All 42 patients received at least one dose of each of the three study drugs, with a median of 92 days of treatment (range 21–288 days). Twenty-seven (64%) patients completed four or more cycles of the combination treatment. A median of 4.5 (range 1–6) cycles of pemetrexed and 4 (range 1–6) cycles of cisplatin were administered. The median dose intensity was 163.9 (range 110.1–175.5) mg m−2 per week for pemetrexed and 24.6 (range 15.3–26.3) mg m−2 per week for cisplatin. The delivered dose intensities were 98.3% for pemetrexed and 98.5% for cisplatin. Seventeen (40%) completed six or more cycles of ziv-aflibercept. The median dose intensity of ziv-aflibercept was 1.97 mg kg−1 per week, close to the planned intensity of 2 mg kg−1 per week. Reasons for treatment discontinuation were disease progression (33%), AEs (33%), and others (34%, including withdrawal of consent and investigator request). Seventeen patients had at least one cycle delayed. Eleven patients (26%) had at least 1 dose modification of ziv-aflibercept, 6 (14%) of pemetrexed, and 11 of cisplatin.

Adverse events

Thirty-five patients (83%) experienced a treatment-emergent adverse event (TEAE) of grade 3 or 4 (3/4), and 16 patients (38%) experienced a serious TEAE. The most common TEAEs were nausea (69%), fatigue (67%), and hypertension (57%). Hypertension, neutropaenia, and hypokalaemia were the most common grade 3/4 TEAEs in 36%, 14%, and 10% of patients, respectively. Table 2 summarised the most common TEAEs. Thirty-nine patients (93%) experienced at least one haematologic abnormality, with grade 3/4 in eight patients (19%), mostly neutropaenia. Every patient experienced at least one abnormal chemistry value, with grade 3/4 in 15 (36%), most commonly hyponatraemia.

Table 2

Summary of most common (>10%) TEAEs by NCI CTCAE grade (N=42)

	All grades N (%)	Grade 3/4 N (%)
Number of patients with most common TEAE with NCI grade	40 (95.2)	27 (64.3)
Nausea	29 (69.0)	0
Fatigue	28 (66.7)	3 (7.1)
Hypertension	24 (57.1)	15 (35.7)
Constipation	21 (50.0)	0
Diarrhoea	16 (38.1)	1 (2.4)
Dysgeusia	15 (35.7)	0
Stomatitis	15 (35.7)	0
Dysphonia	14 (33.3)	0
Headache	14 (33.3)	1 (2.4)
Proteinuria	14 (33.3)	1 (2.4)
Anorexia	13 (31.0)	0
Dehydration	12 (28.6)	3 (7.1)
Dyspepsia	12 (28.6)	0
Epistaxis	11 (26.2)	0
Vomiting	10 (23.8)	0
Weight loss	10 (23.8)	0
Blood creatinine increased	8 (19.0)	0
Cough	8 (19.0)	0
Dyspnoea	7 (16.7)	1 (2.4)
Hyponatraemia	7 (16.7)	2 (4.8)
Neutropaenia	7 (16.7)	6 (14.3)
Thrombocytopaenia	7 (16.7)	3 (7.1)
Dizziness	6 (14.3)	0
Hyperglycaemia	6 (14.3)	1 (2.4)
Hypokalaemia	6 (14.3)	4 (9.5)
Hypomagnesaemia	6 (14.3)	0
Insomnia	6 (14.3)	0
Rhinorrhaea	6 (14.3)	0
Anaemia	5 (11.9)	2 (4.8)
Dry mouth	5 (11.9)	0
Hiccups	5 (11.9)	0
Hyperkalaemia	5 (11.9)	2 (4.8)
Hypocalcaemia	5 (11.9)	1 (2.4)
Musculoskeletal pain	5 (11.9)	0
Oedema peripheral	5 (11.9)	0
Pain in extremity	5 (11.9)	0
Pneumonia	5 (11.9)	2 (4.8)

Abbreviations: CTCAE=Common Terminology Criteria for Adverse Events; TEAE=treatment-emergent adverse events.

Seven patients (17%) died before clinical cutoff of the study. Five died due to disease progression and two due to TEAEs: 1 pneumonia and 1 sepsis.

Neurological toxicities

Between 26 September, 2010 and 30 December, 2010, five patients experienced neurological symptoms, including altered mental status in four, slurred speech in one, seizure in two, and headache in four patients. Three patients had a brain MRI that was consistent with RPLS (Figure 1B). Brain MRI was negative for RPLS in two other patients. The three patients diagnosed with RPLS were all Caucasian women, aged 38, 51, and 72 years, respectively. One of the three patients with RPLS entered the study with a history of hypertension. All three patients experienced elevated BP and two patients had reduced CrCL during the therapy: one patient's CrCL decreased by 45% from baseline (141 to 78 ml min−1) after one cycle, and the other's decreased by 20% (64 to 51 ml min−1) after four cycles. They were diagnosed with RPLS after one, two, and five cycles of ziv-aflibercept, respectively. Two patients recovered from RPLS, and one died due to disease progression before RPLS resolution. Pharmacokinetic information was available for two of the three RPLS patients and for one suspected case: systemic concentrations of free ziv-aflibercept were within the range of other patients in the treatment cohort.

Figure 1

(A) The Kaplan–Meier curve of PFS ( Median PFS: 5 months (95% CI, 4.3–7.1). (B) Brain MRI of a patient diagnosed with RPLS. Extensive increased T2 signal of a few scattered areas of restricted diffusion and vasogenic oedema in the frontal cortex/subcortical regions near the vertex, and the parietal and occipital regions bilaterally (arrows). No focal enhancing lesions to suggest metastatic disease.

In the phase I study using the same regimen (N=18), five patients experienced a mild neurocognitive disturbance but no RPLS was diagnosed (Diaz-Padilla ). Rare cases of RPLS have been observed in the ziv-aflibercept clinical development programme but the rate observed in this study (3 out of 42=7%) was much higher than previously reported (i.e., 0.5% of 3795 patients treated with ziv-aflibercept as monotherapy or in combination with chemotherapy, ZALTRAP product insert). As a result, this study was permanently closed to enrolment. Patients who remained on study were re-consented with updated safety information regarding RPLS in addition to continued close monitoring.

Hypertension and renal insufficiency are two risk factors for RPLS. Twenty-four patients (57%) experienced hypertension (15 grade 3 but no grade 4) during the study, 15 of whom had a history of hypertension and 12 had taken antihypertensive medications before entering the study. Eight patients with hypertension also experienced proteinuria. Fourteen patients (33%) experienced proteinuria (all grades 1 or 2 except a single grade 3), none of whom had a history of renal disease. Fourteen patients experienced CrCL decreases during treatment, with six patients having CrCL decreases below 60 ml min−1 after treatment cycle 4.

Efficacy evaluation

As the study was closed prematurely, there was no statistical power to test the primary hypothesis. Of the 42 patients enrolled, 4 patients discontinued early from the study due to AEs (2), consent withdrawal (1), and investigator decision (1). As they did not have a post-baseline tumour assessment, they were excluded from the efficacy assessment per predefined statistical analysis plan. Of the 38 patients evaluable for efficacy, the median PFS was 5 months (95% CI, 4.3–7.1; Figure 1A), and ORR was 26% (95% CI, 12–40%), all of which (10/38) were PR. The disease control rate (PR+stable disease) was 89% (26%+63%). A mean reduction of 20% was observed in average percentage changes over time in tumour burden (sum of largest diameters of target lesions) from baseline.

Of the 38 patients evaluable for efficacy, 22 (58%) developed hypertension as AE during the study. Seven (7 out of 22=32%) had a PR compared with only three with no hypertension (3 out of 16=18%), suggesting that patients who developed hypertension may have had a higher likelihood of response to this treatment.

Participation in the correlative studies was optional. Erythropoietin levels were obtained from 16 patients. No trend towards increase in haemoglobin or change in erythropoietin level was seen over time.

Pharmacokinetic and antibody evaluation

Twenty-three patients participated in blood sampling for PK analysis. Mean observed noncompartmental PK parameters for free ziv-aflibercept are presented in Table 3. The concentration–time profiles and PK of free ziv-aflibercept and adjusted bound ziv-aflibercept: VEGF were consistent with results in the phase I study (Diaz-Padilla ). Mean trough concentrations after the second ziv-aflibercept dose plateaued and remained at ∼10 mg l−1. The mean adjusted bound ziv-aflibercept:VEGF complex Cmax was 7.81 mg l−1. Trough concentrations plateaued after day 42 and remained constant for the remainder of the study.

Table 3

Mean (s.d.) observed noncompartmental pharmacokinetic parameters for free ziv-aflibercept

		Ziv-aflibercept
Parameter		N	Mean	s.d.
t1/2	Day	7	4.62	1.46
CL	l per day per kg	7	0.016	0.004
Vss	l kg−1	7	0.081	0.015
Cmax	mg l−1	21	104	26.2
Clast	mg l−1	21	65.2	50.8
tmax	Day	21	0.0695	0.019
tlast	Day	21	7.02	9.32
AUCinf	Day × mg l−1	7	402	100
MRTinf	Day	7	5.35	1.28

Abbreviations: AUCinf=area under the concentration curve from time zero extrapolated to infinity; CL=clearance; Clast=last positive plasma concentration; Cmax=maximal plasma concentration; MRTinf=mean residence time extrapolated to infinity; tlast=time of the last positive plasma concentration; tmax=time required to reach maximal plasma concentration; t1/2=observed half-life; Vss=volume of distribution at steady state.

Two patients had one sample each that was positive in the anti-drug antibody (ADA) assay. One was positive at baseline, but did not have an antibody titre drawn at the end of treatment (EOT) visit. This patient completed all six cycles of combination treatment without dose delay/reduction or grade 3/4 AEs and had stable disease. The other one was negative at baseline but positive at the EOT visit. This patient experienced anaphylaxis 20 minutes after start of the ziv-aflibercept infusion on day 1 of the second cycle. Study drug was permanently withdrawn. This patient had PK parameters and a concentration–time profile different from ADA-negative patients, probably because of the ADA formation.

Discussion

Ziv-aflibercept has been tested as a single agent and in combination with chemotherapy in the treatment of NSCLC (Leighl ; Ramlau ). On the basis of activity and safety profile, we conducted the current phase II study to explore the efficacy of ziv-aflibercept in the first-line setting. Similar to ECOG 4599, AVAiL, and PointBreak trials (Sandler ; Patel ; Reck ), this study was designed to test a three-drug regimen including an anti-angiogenesis agent, in this case ziv-aflibercept/cisplatin/pemetrexed. In addition, maintenance therapy with single-agent ziv-aflibercept was intended to prolong the benefits and delay the development of resistance. This approach was first tested in a phase I dose-escalation study that used the same regimen of ziv-aflibercept/cisplatin/pemetrexed in 18 patients with advanced solid tumours (Diaz-Padilla ).

Our study population was representative of patients with advanced NSCLC. Overall, the median ziv-aflibercept dose intensity was similar to the planned intensity. The delivered dose intensities of pemetrexed/cisplatin in this study were over 98%, higher than those in the pemetrexed/cisplatin arm (94.8% and 95.0%, respectively) of the phase III trial (Scagliotti ). The PK of ziv-aflibercept in this study was characterised as nonlinear and similar to that observed in the phase I study. The mean observed terminal t1/2 was independent of ziv-aflibercept dose. Administration of ziv-aflibercept did not alter pemetrexed PK. Development of ADA was a rare event, leading to reduced drug concentration in one patient who experienced anaphylaxis. As with all therapeutic proteins, there is a potential for immunogenicity; however, severe hypersensitivity reactions are rare. Although this study was terminated early, the two co-primary end points, ORR of 26% and median PFS of 5 months, were in accordance with most historical first-line NSCLC studies (Schiller ; Scagliotti ) and slightly less than triplet regimens incorporating another anti-VEGF agent (Sandler ; Reck ). However, there was no statistical power to test the primary hypothesis that ziv-aflibercept would enhance the efficacy of standard chemotherapy in NSCLC.

Biomarkers that can reliably predict the degree of VEGF blockade in vivo are currently not available. Preclinical studies identified increased erythropoietin production and erythropoiesis as a possible surrogate marker of VEGF inhibition, as animal data indicate that stringent VEGF inhibition, including by ziv-aflibercept, modulates erythropoiesis via increased hepatic erythropoietin synthesis (Tam ). Bevacizumab has also been associated with increased haemoglobin in NSCLC (Riess ) and reduced anaemia (Sher and Wu, 2011). Therefore, this study explored whether the increase in haemoglobin observed previously could be reproduced in the presence of chemotherapy and would correlate with anti-angiogenic activity. No trend towards increase in haemoglobin or change in erythropoietin level was found in a small subset of patients. However, as in the phase I study, a stabilisation of median haemoglobin values for multiple cycles as well as low rate of all-grade anaemia was observed. The result provides some support for the hypothesis that VEGF is a negative regulator of erythropoiesis, and its inhibitors may have a role in the management of anaemia.

The toxicity profile of this trial was consistent with published data on cisplatin plus pemetrexed and with the known effects of ziv-aflibercept with the exception of a higher than anticipated rate of RPLS (Gadgeel, 2012). Hypertension was the third most frequent TEAE and is a known adverse effect of anti-VEGF therapies. However, higher response rate was observed among patients who developed hypertension during the treatment than among those who did not in a post hoc analysis. This observation is consistent with data from ECOG 4599 that suggested improved outcomes associated with bevacizumab in patients developing hypertension on therapy (Dahlberg ).

Although cases of RPLS have been observed in other ziv-aflibercept studies, the 7% rate observed in this study was much higher. It should be noted that the dose and schedule of ziv-aflibercept in this study at 6 mg kg−1 every 21 days is different from the one approved in colorectal cancer at 4 mg kg−1 every 14 days (Van Cutsem ), although the dose intensity is the same at 2 mg kg−1 per week. At the recommended phase II dose of 6 mg kg−1 for ziv-aflibercept, no RPLS was reported in the phase I study that used the same regimen (N=7 at that dose level; Diaz-Padilla ), or in another phase I study of ziv-aflibercept/cisplatin/docetaxel (N=17 at that dose level; Freyer ), nor in combination with docetaxel in the VITAL study (N=456 in the combination arm; Ramlau ). A meta-analysis of safety data from three large placebo-controlled studies reported no RPLS among 1333 patients treated with ziv-aflibercept in combination with standard chemotherapy (Allegra ). It is likely that the development of RPLS may be regimen dependent rather than dose or schedule dependent.

Reversible posterior leukoencephalopathy syndrome is described as a brain-capillary leak syndrome frequently related to hypertension, fluid retention, and possibly the cytotoxic effects of immunosuppressive agents on the vascular endothelium (Hinchey ). Risk factors include female sex, hypertension, and renal dysfunction (Vaughn ), as well as anticancer agents: 75% were diagnosed in women and 71% were associated with combination regimens (Marinella and Markert, 2009). Bevacizumab and gemcitabine have been most commonly associated with RPLS. Treatment including cisplatin without concomitant anti-VEGF therapy has been associated with RPLS (Ito ), whereas pemetrexed, before this study, was not. Consistent with the literature, the three cases of RPLS were all diagnosed in women, which may be related to an anticancer drug–oestrogen interaction inducing altered cerebral vasoreactivity and endothelial dysfunction. Agents that decrease VEGF signalling increases the risk of RPLS (including bevacizumab, sunitinib, sorafenib, and ziv-aflibercept), suggesting a class effect toxicity (Glusker ). Clinical features of RPLS are neurological symptoms characterized by headaches, altered mental status, visual disturbances, or seizures, and systemic signs such as hypertension. Onset is variable ranging from hours to 1 month after completing therapy (Lee ). Characteristic findings in brain MRI demonstrate bilateral, symmetric parieto-occipital subcortical and cortical vasogenic oedema (Bartynski, 2008). Removal of the causative agent and treatment of hypertension and renal insufficiency are indicated for RPLS, which is usually, but not always, reversible clinically.

In conclusion, this phase II study was designed to evaluate ziv-aflibercept in combination with cisplatin and pemetrexed in patients with untreated, advanced/metastatic non-squamous NSCLC. However, three confirmed and two suspected but unconfirmed cases of RPLS led to the early termination of the trial. The reason for the increased incidence of RPLS might be related to declining CrCL and/or increased BP. Although ORR and median PFS were in accordance with most historical first-line NSCLC studies, this combination of ziv-aflibercept/cisplatin/pemetrexed will not be further pursued in NSCLC. Future efforts to identify predictive biomarkers of anti-VEGF agents are warranted.