Boehringer Ingelheim Showcases Expanding Presence In Lung Cancer At ASCO With New Data Including Presentation Of Gilotrif (Afatinib) Overall Survival Results For Squamous Cell Carcinoma Of The Lung
RIDGEFIELD, Conn., May 14, 2015 /PRNewswire/ -- Boehringer Ingelheim today announced that the latest data from its oncology portfolio will be presented at the Annual Meeting of the American Society of Clinical Oncology (ASCO) in Chicago, IL, on May 29 June 2, 2015. A total of nine abstracts, including new data for afatinib and nintedanib, will emphasize the growing presence of Boehringer Ingelheim in lung and other cancer types.
The LUX-Lung 8 Phase III trial directly compared the efficacy and safety of two EGFR-directed treatments, afatinib and erlotinib, in patients with advanced squamous cell carcinoma (SCC) of the lung, progressing after treatment with first-line chemotherapy. The study met its primary endpoint of progression-free survival, as well as its key secondary endpoint of overall survival (OS). Overall safety findings for afatinib were consistent with previous reports. The OS data will be unveiled in an oral presentation on Sunday, May 31 from 8:24 8:36 a.m. in N Hall B1. The outcome of the trial is highly anticipated due to the current poor prognosis and high level of unmet need for patients with this specific type of lung cancer.
"Boehringer Ingelheim is proud to present the overall survival results from the LUX-Lung 8 trial as well as data on other investigational compounds from our growing oncology pipeline," said Tunde Otulana, M.D., senior vice president, Clinical Development and Medical Affairs, Boehringer Ingelheim Pharmaceuticals, Inc. "Our ongoing research program with Gilotrif and other compounds underscores our commitment to advancing the care of people affected by cancer, particularly lung cancer."
Data for Boehringer Ingelheim Oncology Compounds at ASCO 2015
Title | Authors | Abstract Details |
Gilotrif® (afatinib)* | ||
Afatinib (A) vs erlotinib (E) as second-line treatment of patients (pts) with advanced squamous cell carcinoma (SCC) of the lung following first-line platinum-based chemotherapy: overall survival analysis from the LUX-Lung 8 Phase III global trial | J.C. Soria, E. Felip, M. Cobo, S. Lu, K.N. Syrigos, K.H. Lee, E. Goker, V. Georgoulias, K.W. Li, D. Isla, S.Z. Guclu, A. Morabito, YJ Min, A. Ardizzoni, S. Gadgeel, B Wang, V.K. Chand, G.D. Goss for the LUX-Lung 8 Investigators | Sunday, 31 May, 8:00 am 11:00 am |
Biomarker analysis in recurrent and/or metastatic head and neck squamous cell carcinoma (R/M HNSCC) patients (pts) treated with afatinib vs methotrexate (MTX): LUX-Head & Neck 1 (LUX-H&N1) | E.E.W. Cohen, L.F. Licitra, J. Fayette, T. Gauler, P.l.M. Clement, J.J. Grau, J.M. del Campo, A. Mailliez, R.I. Haddad, J.B. Vermorken, M. Tahara, J. Guigay, L.l. Geoffrois, M.oC. Merlan, N.F. Dupuis, X.J. Cong, N. Gibson, F. Solca, E. Ehrnrooth, J-P.H. Machiels | Saturday, 30 May, 1:15 pm 4:45 pm |
Afatinib (A) vs erlotinib (E) as second-line treatment of patients (pts) with advanced squamous cell carcinoma (SCC) of the lung following first-line platinum-based chemotherapy: patient-reported outcome (PRO) data from the LUX-Lung 8 Phase III global trial | S. Gadgeel, M. Cobo, E. Felip, J.C. Soria, K.H. Lee, S. Lu, V. Georgoulias, A. Fulop, E. Goker, K.N. Syrigos, A. Morabito, H.S. Coskun, S.Z. Guclu, W. Li, S. Popat, A. Ardizzoni, J Lungershausen, B. Wang, V.K. Chand, G.D. Goss for the LUX-Lung 8 Investigators | Monday, 1 June, 8:00 am 11:30 am |
Phase Ib study of afatinib plus standard-dose cetuximab in patients (pts) with advanced solid tumors | A. Gazzah, V. Boni, J.C. Soria, E. Holgado, C. Even, M. Ould-Kaci, S. Nazabadioko, W. Xue, E. Calvo | Saturday, 30 May, 8:00 am 11:30 am |
Influence of dose adjustment on afatinib safety and efficacy in patients (pts) with advanced EGFR mutation-positive (EGFRm+) non-small cell lung cancer (NSCLC) | J.C-H. Yang, M-J. Ahn, N.J. Dickgreber, B. Halmos, V. Hirsh, M.J. Hochmair, B.P. Levy, F. de Marinis, T. Mok, K. O'Byrne, I. Okamoto, M. Schuler, M. Sebastian, R. Shah, E-H. Tan, N. Yamamoto, A. Märten, D. Massey, S. Wind, D.P. Carbone | Monday, 1 June, 8:00 am 11:30 am |
Mechanisms of acquired afatinib resistance in HER2-positive breast cancer cells. | A. Canonici | Saturday, 30 May, 8:00 am 11:30 am |
Nintedanib* | ||
LUME-Colon 1: a double-blind, randomized Phase III study of nintedanib plus best supportive care (BSC) versus placebo plus BSC in patients with colorectal cancer (CRC) refractory to standard therapies | H.J. Lenz, J. Tabernero , T. Yoshino, Z. Oum'Hamed, S. Vlassak, M. Sassi, E. Van Cutsem | Monday, 1 June, 8:00 am 11:30 am |
Efficacy and safety of nintedanib (N) versus sorafenib (S) in Caucasian and Asian patients with advanced hepatocellular carcinoma (HCC): pooled analysis of two randomized Phase II trials | T. Meyer, D. Palmer, Y. Chao, C. Choi, A. Deptala, L. Fartoux, Y-H. Feng, J. Graham, J. Hocke, T-Y. Kim, D-Y Lin, Y.T. Ma, M. Peck-Radosavljevic, P. Ross, B-Y Ryoo, A. Wenz, C-J. Yen, A-B. Loembé, A-L. Cheng | Monday, 1 June, 8:00 am 11:30 am |
BI 853520 (focal adhesion kinase (FAK) inhibitor*) | ||
A phase I study of BI 853520, an inhibitor of focal adhesion kinase (FAK), in patients with advanced or metastatic solid tumors | A. Zer, R.B. Verheijen, F. De Vos, S. Hotte, F. Eskens, L.C. Pronk, L.L. Siu, D. Schnell, N. Steeghs, M. Langenberg, H. Hirte, M. de Jonge | Saturday, 30 May. 8:00 am 11:30 am |
*All compounds are either investigational or studied in new indications to evaluate safety and efficacy.
About Gilotrif® (afatinib) tablets
GILOTRIF is indicated for the first-line treatment of patients with metastatic non-small cell lung cancer (NSCLC) whose tumors have epidermal growth factor receptor (EGFR) exon 19 deletions or exon 21 (L858R) substitution mutations as detected by an FDA-approved test.
Limitation of Use: Safety and efficacy of GILOTRIF have not been established in patients whose tumors have other EGFR mutations.
GILOTRIF is an oral, once-daily kinase inhibitor that is designed to irreversibly bind and inhibit the following receptors: EGFR (ErbB1), HER2 (ErbB2) and ErbB4.
IMPORTANT SAFETY INFORMATION
WARNINGS AND PRECAUTIONS
Diarrhea
- Diarrhea has resulted in dehydration with or without renal impairment; some of these cases were fatal. In the pivotal study, diarrhea occurred in 96% of patients treated with GILOTRIF (n=229), of which 15% was Grade 3 in severity and occurred within the first 6 weeks. Renal impairment as a consequence of diarrhea occurred in 6.1% of patients treated with GILOTRIF, out of which 3 (1.3%) were Grade 3.
- For patients who develop prolonged Grade 2 diarrhea lasting more than 48 hours or greater than or equal to Grade 3 diarrhea, withhold GILOTRIF until diarrhea resolves to Grade 1 or less, and resume GILOTRIF with appropriate dose reduction. Provide patients with an anti-diarrheal agent (e.g., loperamide) for self-administration at the onset of diarrhea and instruct patients to continue anti-diarrheal therapy until loose bowel movements cease for 12 hours.
Bullous and Exfoliative Skin Disorders
- Grade 3 cutaneous reactions characterized by bullous, blistering, and exfoliating lesions occurred in 6 (0.15%) of the 3865 patients who received GILOTRIF across clinical trials. In the pivotal study, the overall incidence of cutaneous reactions consisting of rash, erythema, and acneiform rash was 90%, and the incidence of Grade 3 cutaneous reactions was 16%. In addition, the incidence of Grade 1-3 palmar-plantar erythrodysesthesia syndrome was 7%. Discontinue GILOTRIF in patients who develop life-threatening bullous, blistering, or exfoliating lesions. For patients who develop prolonged Grade 2 cutaneous adverse reactions lasting more than 7 days, intolerable Grade 2, or Grade 3 cutaneous reactions, withhold GILOTRIF until the adverse reaction resolves to Grade 1 or less, and resume GILOTRIF with appropriate dose reduction.
Interstitial Lung Disease (ILD)
- ILD or ILD-like adverse reactions (e.g., lung infiltration, pneumonitis, acute respiratory distress syndrome, or alveolitis allergic) occurred in 1.5% of the 3865 patients who received GILOTRIF across clinical trials; of these, 0.4% were fatal. The incidence of ILD appeared to be higher in patients of Asian ethnicity (2.1%) as compared to non-Asians (1.2%). In the pivotal study, the incidence of Grade >/= 3 ILD was 1.3% and resulted in death in 1% of GILOTRIF-treated patients.
- Withhold GILOTRIF during evaluation of patients with suspected ILD, and discontinue GILOTRIF in patients with confirmed ILD.
Hepatic Toxicity
- In 3865 patients who received GILOTRIF across clinical trials, 10.1% had liver test abnormalities, of which 7 (0.18%) were fatal. In the pivotal study, liver test abnormalities of any grade occurred in 17.5% of the patients treated with GILOTRIF.
- Obtain periodic liver testing in patients during treatment with GILOTRIF. Withhold GILOTRIF in patients who develop worsening of liver function. In patients who develop severe hepatic impairment while taking GILOTRIF, treatment should be discontinued.
Keratitis
- Keratitis, characterized as acute or worsening eye inflammation, lacrimation, light sensitivity, blurred vision, eye pain, and/or red eye occurred in 0.8% of patients treated with GILOTRIF among 3865 patients across clinical trials. Keratitis was reported in 5 (2.2%) patients in the pivotal study, with Grade 3 in 1 (0.4%). Withhold GILOTRIF during evaluation of patients with suspected keratitis, and if diagnosis of ulcerative keratitis is confirmed, treatment with GILOTRIF should be interrupted or discontinued. If keratitis is diagnosed, the benefits and risks of continuing treatment should be carefully considered. GILOTRIF should be used with caution in patients with a history of keratitis, ulcerative keratitis, or severe dry eye. Contact lens use is also a risk factor for keratitis and ulceration.
Embryofetal Toxicity
- GILOTRIF is Pregnancy Category D. Based on its mechanism of action; GILOTRIF can cause fetal harm when administered to a pregnant woman. If this drug is used during pregnancy, or if the patient becomes pregnant while taking this drug, the patient should be apprised of the potential hazard to the fetus.
- Advise females of reproductive potential to use highly effective contraception during treatment, and for at least 2 weeks after the last dose of GILOTRIF. Advise patients to contact their healthcare provider if they become pregnant, or if pregnancy is suspected, while taking GILOTRIF.
ADVERSE REACTIONS
- In GILOTRIF-treated patients (n=229) the most common adverse reactions in the pivotal study (>/= 20% all grades & vs pemetrexed/cisplatin-treated patients (n=111)) were diarrhea (96% vs 23%), rash/dermatitis acneiform (90% vs 11%), stomatitis (71% vs 15%), paronychia (58% vs 0%), dry skin (31% vs 2%), decreased appetite (29% vs 55%), pruritus (21% vs 1%).
- Serious adverse reactions were reported in 29% of patients treated with GILOTRIF.
The most frequent serious adverse reactions reported in patients treated with GILOTRIF were diarrhea (6.6%); vomiting (4.8%); and dyspnea, fatigue, and hypokalemia (1.7% each). Fatal adverse reactions in GILOTRIF-treated patients included pulmonary toxicity/ILD-like adverse reactions (1.3%), sepsis (0.43%), and pneumonia (0.43%). - More GILOTRIF-treated patients (2.2%; n=5) experienced ventricular dysfunction (defined as diastolic dysfunction, left ventricular dysfunction, or ventricular dilation; all < Grade 3) compared to chemotherapy-treated patients (0.9%; n=1).
DRUG INTERACTIONS
Effect of P-glycoprotein (P-gp) Inhibitors and Inducers
- Concomitant taking of P-gp inhibitors (including but not limited to ritonavir, cyclosporine A, ketoconazole, itraconazole, erythromycin, verapamil, quinidine, tacrolimus, nelfinavir, saquinavir, and amiodarone) with GILOTRIF can increase exposure to afatinib.
- Concomitant taking of P-gp inducers (including but not limited to rifampicin, carbamazepine, phenytoin, phenobarbital, and St. John's wort) with GILOTRIF can decrease exposure to afatinib.
USE IN SPECIFIC POPULATIONS
Nursing Mothers
- It is not known whether afatinib is present in human milk. Because many drugs are present in human milk and because of the potential for serious adverse reactions in nursing infants from GILOTRIF, a decision should be made whether to discontinue nursing or to discontinue the drug, taking into account the importance of the drug to the mother.
Renal Impairment
- GILOTRIF has not been studied in patients with severely impaired renal function.
Closely monitor patients with moderate (CLcr 30-59 mL/min) to severe (CLcr <30 mL/min) renal impairment and adjust GILOTRIF dose if not tolerated.
Hepatic Impairment
- GILOTRIF has not been studied in patients with severe (Child Pugh C) hepatic impairment. Closely monitor patients with severe hepatic impairment and adjust GILOTRIF dose if not tolerated.
About nintedanib
Nintedanib is an oral triple angiokinase inhibitor which simultaneously inhibits vascular endothelial growth factor receptor (VEGFR), platelet-derived growth factor receptors (PDGFR) and fibroblast growth factor receptor (FGFR) signaling pathways, the three receptors crucially involved in angiogenesis and tumor growth. Growing scientific evidence shows these three different angiokinase receptors play an important role not only in angiogenesis, but also in tumor growth and metastasis.
Nintedanib is currently being investigated in patients with various solid tumors including Phase III studies in advanced NSCLC, colon cancer (metastatic colorectal cancer) and ovarian cancer, and also in Phase II studies in mesothelioma, kidney cancer (renal cell carcinoma) and liver cancer (hepatic cell carcinoma).
About Boehringer Ingelheim in Oncology
Building on scientific expertise and excellence in the fields of pulmonary and cardiovascular medicine, metabolic disease, neurology, virology and immunology, Boehringer Ingelheim has embarked on a major research program to discover and develop innovative cancer treatments. Working in close collaboration with the international scientific community and a number of the world's leading cancer centers, Boehringer Ingelheim's commitment to oncology is underpinned by using advances in science to develop a range of targeted therapies for various solid tumors and hematological cancers. The current focus of late-stage research includes compounds in three areas: signal transduction inhibition, angiogenesis inhibition and cell-cycle kinase inhibition. The company is also evaluating a robust and growing pipeline of early-stage oncology compounds in areas including growth/survival signaling, immunotherapy and epigenetics.
For information about participating in a Boehringer Ingelheim clinical trial, please visit www.bicancertrials.com or call 1.866.725.7110.
About Boehringer Ingelheim Pharmaceuticals, Inc.
Boehringer Ingelheim Pharmaceuticals, Inc., based in Ridgefield, CT, is the largest U.S. subsidiary of Boehringer Ingelheim Corporation.
Boehringer Ingelheim is one of the world's 20 leading pharmaceutical companies. Headquartered in Ingelheim, Germany, the company operates globally with 146 affiliates and more than 47,000 employees. Since its founding in 1885, the family-owned company has been committed to researching, developing, manufacturing and marketing novel treatments for human and veterinary medicine.
Boehringer Ingelheim is committed to improving lives and providing valuable services and support to patients and families. Our employees create and engage in programs that strengthen our communities. To learn more about how we make more health for more people, visit our Corporate Social Responsibility Report.
In 2014, Boehringer Ingelheim achieved net sales of about $16.96 billion dollars (13.3 billion euros). R&D expenditure corresponds to 19.9 percent of its net sales.
For more information please visit www.us.boehringer-ingelheim.com, or follow us on Twitter @BoehringerUS.
Contact:
Boehringer Ingelheim Pharmaceuticals, Inc.
Name: Paul Wynn
Public Relations
Office: 203-798-4887
Mobile: 203-482-4512
Email: paul.wynn@boehringer-ingelheim.com
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SOURCE Boehringer Ingelheim Pharmaceuticals, Inc.
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