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Clinical Trial Details — Status: Completed

Administrative data

NCT number NCT00387127
Other study ID # EGF105884
Secondary ID
Status Completed
Phase Phase 2
First received October 10, 2006
Last updated May 28, 2015
Start date November 2006
Est. completion date January 2014

Study information

Verified date February 2015
Source GlaxoSmithKline
Contact n/a
Is FDA regulated No
Health authority France: Afssaps - Agence française de sécurité sanitaire des produits de santé (Saint-Denis)United States: Food and Drug Administration
Study type Interventional

Clinical Trial Summary

This is a phase II study comparing the effects of lapatinib versus placebo when administered concurrently with cisplatin and radiotherapy followed by 1 year monotherapy with lapatinib or placebo. The study is designed to evaluate and compare the two treatment groups with respect to complete response rate at 6 months following chemoradiation completion.


Recruitment information / eligibility

Status Completed
Enrollment 67
Est. completion date January 2014
Est. primary completion date June 2009
Accepts healthy volunteers No
Gender Both
Age group 18 Years and older
Eligibility Inclusion criteria:

- Willing and able to sign a written informed consent;

- Histologically confirmed diagnosis of SCCHN of one or more of the following sites:

oral cavity, oropharynx, hypopharynx and larynx;

Multiple primary tumours will:

Have to be histologically proven; Have to be anatomically distant and surrounded by normal tissue; Exclude distant metastasis.

- Prior to enrolment subjects must have ErbB1 over-expression determined by immunohistochemistry (IHC) 3+ as assessed by a central laboratory;

- Subjects with stage III and IVA/IVB disease, who are to receive cisplatin chemotherapy and radiation therapy as primary treatment (total dose 65 - 70 Gy); Subjects with any Tis, T1 or T2 disease regardless of N stage, are excluded. Subjects with distant metastases, ie Stage IVC, are excluded.

- Willing and able to have a tumour biopsy taken at screening; For patients who have had prior tumour biopsy, an adequate archived specimen must be available.

- Male or female =18 years of age;

Criteria for female subjects or female partners of male subjects:

Non-child-bearing potential (i.e., women with functioning ovaries who have a GM2005/00448/00 CONFIDENTIAL EGF105884 22 current documented tubal ligation or hysterectomy, or women who are postmenopausal); Child-bearing potential (i.e., women with functioning ovaries and no documented impairment of oviductal or uterine function that would cause sterility.) This category includes women with oligomenorrhoea (severe), women who are perimenopausal, and young women who have begun to menstruate. These subjects must have a negative serum pregnancy test at screening and agree to one of the following: Complete abstinence from intercourse from 2 weeks prior to administration of the first dose of study medication until 28 days after the final dose of study medication; or Consistent and correct use of one of the following acceptable methods of birth control: male partner who is sterile prior to the female subject's entry into the study and is the sole sexual partner for that female subject; implants of levonorgestrel; injectable progestogen; any intrauterine device (IUD) with a documented failure rate of less than

1% per year; oral contraceptives (either combined or progestogen only); or barrier methods, including diaphragm or condom with a spermicide.

- ECOG performance status 0, 1 or 2;

- Subjects must have adequate haematological, renal and hepatic function; Calculated creatinine clearance =50 ml/min as determined by the modified method of Cockcroft and Gault or by the EDTA method. Absolute neutrophil count =1,500/µl, platelets =100,000/µl. Haemoglobin =9gm/dL (5mmol/L). Aspartate (AST) and alanine transaminase (ALT) less than 4 times the upper limit of the normal range (ULN). Total bilirubin =2.0 mg/dL.

- Left ventricular ejection fraction (LVEF) within the institutional normal ranges as measured by echocardiogram (ECHO) or Multigated Acquisition (MUGA) scan;

- Able to swallow tablets whole or swallow a suspension of tablets dissolved in water at study inclusion; The use and timing of feeding tube is optional. If necessary, the suspension may be administered via percutaneous endoscopic gastrostomy (PEG), percutaneous jejunostomy tube (J- Tube), or a nasogastric tube (NG or Dobhoff type tube).

- Life expectancy of at least 6 months in the best judgment of the investigator.

Exclusion criteria:

- Nasopharyngeal, paranasal sinuses or nasal cavity tumours;

- Any prior or current treatment for invasive head and neck cancer of any kind. This will include but is not limited to: prior tyrosine kinase inhibitors, prior neoadjuvant therapy, prior surgical resection, or use of any investigational agent;

- Concurrent use of CYP3A4 inducers or inhibitors. A standard 3-day course of dexamethasone for the prevention of cisplatin-induced nausea and vomiting is permitted;

- Subjects with known history of uncontrolled or symptomatic angina, arrhythmias, or congestive heart failure;

- History of another malignancy within the last 5 years, with the exception of completely resected basal or squamous cell skin cancer, or successfully treated in-situ carcinoma. History of non-invasive lesion or in-situ carcinoma, including in the head and neck region that was successfully treated with surgery, photodynamics or laser, will be permitted;

- Peripheral neuropathy = grade 2;

- Pregnant or lactating females (female subjects of child-bearing potential will undertake pregnancy testing at screening and during study completion/withdrawal visits);

- Malabsorption syndrome, disease significantly affecting GI function, that could affect absorption of lapatinib;

- History of allergic reactions to appropriate antiemetics (e.g. 5-HT3 antagonists) to be administered with platinum chemotherapy;

- The investigator considers the subject unfit for the study as a result of the medical interview, physical examinations, or screening investigations;

Study Design

Allocation: Randomized, Endpoint Classification: Safety/Efficacy Study, Intervention Model: Parallel Assignment, Masking: Double Blind (Subject, Investigator), Primary Purpose: Treatment


Related Conditions & MeSH terms


Intervention

Drug:
Lapatinib oral tablets
Lapatinib is administered orally once daily.
radiotherapy
Radiotherapy is given either as conventional fractionation using Two-dimensional (2D) or conformal techniques, or as Intensity Modulated Radiation Therapy (IMRT). Radiation therapy will be standardised throughout the study. Radiation therapy is given only once daily, with a dose/fraction not exceeding 2.5Gy, to a total dose of 65 Gy (IMRT) or 70 Gy (2D or 3D RT) to the gross site of disease .
cisplatin chemotherapy
Cisplatin is administered intravenously at a dose of 100mg/m2 on days 1, 22 and 43 of radiotherapy (approximately Study Days 8, 29 and 50).

Locations

Country Name City State
Canada GSK Investigational Site Hamilton Ontario
Canada GSK Investigational Site Quebec
Canada GSK Investigational Site Sherbrooke Quebec
France GSK Investigational Site Lens
France GSK Investigational Site Lille
France GSK Investigational Site Lyon
France GSK Investigational Site Paris cedex 15
France GSK Investigational Site Vandoeuvre-Les-Nancy
Hungary GSK Investigational Site Budapest
Hungary GSK Investigational Site Gyor
India GSK Investigational Site Ahemdabad
India GSK Investigational Site Mumbai
India GSK Investigational Site Thiruvananthapuram
Netherlands GSK Investigational Site Amsterdam
Netherlands GSK Investigational Site Leiden
Peru GSK Investigational Site Lima
Peru GSK Investigational Site Lima
Spain GSK Investigational Site Barcelona
Spain GSK Investigational Site Madrid
United Kingdom GSK Investigational Site Cambridge Cambridgeshire
United Kingdom GSK Investigational Site Coventry
United Kingdom GSK Investigational Site Leeds
United Kingdom GSK Investigational Site London
United Kingdom GSK Investigational Site London
United Kingdom GSK Investigational Site Newcastle upon Tyne
United Kingdom GSK Investigational Site Northwood Middlesex
United Kingdom GSK Investigational Site Sheffield
United States GSK Investigational Site Charlotte North Carolina
United States GSK Investigational Site Kansas City Missouri
United States GSK Investigational Site Minneapolis Minnesota

Sponsors (1)

Lead Sponsor Collaborator
GlaxoSmithKline

Countries where clinical trial is conducted

United States,  Canada,  France,  Hungary,  India,  Netherlands,  Peru,  Spain,  United Kingdom, 

References & Publications (1)

Harrington K, Berrier A, Robinson M, Remenar E, Housset M, de Mendoza FH, Fayette J, Mehanna H, El-Hariry I, Compton N, Franklin N, Biswas-Baldwin N, Lau M, Legenne P, Kumar R. Randomised Phase II study of oral lapatinib combined with chemoradiotherapy in patients with advanced squamous cell carcinoma of the head and neck: rationale for future randomised trials in human papilloma virus-negative disease. Eur J Cancer. 2013 May;49(7):1609-18. doi: 10.1016/j.ejca.2012.11.023. Epub 2012 Dec 19. — View Citation

Outcome

Type Measure Description Time frame Safety issue
Other Number of Participants Classified as Responders, as Per Volumetric Tumor Response No analysis was not performed. From the date of randomization until 6 months post chemoradiation treatment, assessed for a median of 13 months No
Primary Number of Participants (Par.) With Complete Response (CR), as Assessed by Independent Radiological Review Participants with CR are defined as those who achieved a complete tumor response at 6 months after the completion of the chemoradiation treatment (CRT), as assessed by independent radiological review. Tumor response was assessed using modified Response Evaluation Criteria in Solid Tumors (RECIST) criteria. Per RECIST, CR is defined as the disappearance of all target and non-target lesions. Data are based on Week 24 scans from participants receiving study treatment at that time and on those in follow-up. From the date of randomization until 6 months post chemoradiation treatment, assessed for a median time of 13 months No
Secondary Number of Participants With CR, as Assessed by the Investigator Participants with CR are defined as those who achieved a complete tumor response at 6 months after the completion of the CRT, as determined by the investigator. Tumor response was assessed using modified RECIST criteria. Per RECIST, CR is defined as the disappearance of all target and non-target lesions. Data are based on Week 24 scans from participants receiving study treatment at that time and on those in follow-up. From the date of randomization until 6 months post chemoradiation treatment, assessed after a median time of 13 months of follow-up No
Secondary Progression-Free Survival (PFS), as Assessed by the Investigator PFS=the time from randomization until the earliest date of disease progression or death due to any cause, if sooner. Per RECIST, progressive disease=a >=20% increase in the sum of the longest diameter of target lesions (TLs), or the appearance of >=1 new L, symptomatic progression and/or unequivocal progression of existing non-TLs. For participants who did not progress or die at the time of reporting (data cut-off 1-Aug-2014), PFS data were censored at the time of the last investigator assessed radiological scan preceding the initiation of any alternative anti-cancer therapy. From the date of randomization until the date of disease progression or death due to any cause, assessed after a median of 22 months of follow-up No
Secondary Overall Survival (OS) OS is defined as the time from randomization until death due to any cause. Time to death (data cut-off 1-Aug-2014) was censored at the time of last contact for participants who did not die. From the date of randomization until the date of death due to any cause, assessed after a median of 30.9 months No
Secondary Number of Participants Who Died Due to Progressive Disease The number of participants who died due to progressive disease (a >=20% increase in the sum of the longest diameter of target lesions, or the appearance of >=1 new lesion, symptomatic progression and/or unequivocal progression of existing non-target lesions), or died due to head and neck cancer without evidence of disease progression, after randomization in the study is presented, using a data cut of 1 August 2014. From the date of randomization until the date of death due to disease under study, assessed after a median of 30.9 months No
Secondary Disease-specific Survival Disease-specific survival is defined as the time from randomization until death due to head and neck cancer. From the date of randomization until the date of death due to disease, assessed after a median of 13 months of follow-up No
Secondary Number of Participants With Loco-regional Recurrence of Initial Disease Participants with loco-regional recurrence were those who had progression of disease in the T and N sites. Per the Tumor, Node, and Metastases (TNM) staging of tumors: T describes the size of the tumor and whether it has invaded nearby tissue, and N describes regional lymph nodes that are involved. If a participant had progression in the T or N sites, then the participant was counted as having had an event of interest. From the date of randomization until progression in the T or N site or death due to any cause, assessed after a median of 30.9 months No
Secondary Loco-regional Control Loco-regional control is defined as the time from the date of randomization until progression in the T or N site. Participants who died or had secondary primary malignancies in the head and neck region outside of the T and N site or distant metastasis were not counted as an event and were instead treated as competing risks. Per the TNM staging of tumors: T describes the size of the tumor and whether it has invaded nearby tissue, and N describes regional lymph nodes that are involved. Due to the minimal events reported (data cut-off 30-Sep-2010), valid analysis could not be performed for loco-regional control rate. From the date of randomization until progression in the T or N site or death due to any cause, assessed after a median of 30.9 months No
Secondary Number of Participants With Distant Recurrence of Initial Disease Participants were analyzed for the occurrence of distant metastasis (spread of a disease from one organ or part to another non-adjacent organ or part) after randomization in the study until data cut-off date 1-Aug-2014. Participants who died or had recurrence of disease in the T or N sites or secondary primary malignancies in the head and neck region outside of the original T and N site were not counted as an event and were instead treated as competing risks. From the date of randomization until the first occurrence of distant metastasis, assessed after a median of 30.9 months No
Secondary Distant Relapse Distant relapse is defined as the time from the date of randomization until the first occurrence of distant metastasis (spread of a disease from one organ or part to another non-adjacent organ of part). Participants who died or had recurrence of disease in the T or N sites or secondary primary malignancies in the head and neck region outside of the original T and N site were not counted as an event and were instead treated as competing risks. From the date of randomization until the first occurrence of distant metastasis, assessed after a median of 30.9 months No
Secondary Number of Participants With Overall Response (OR), as Assessed by the Investigator Participants with OR were those who achieved either a CR or partial response (PR) from the assessment of overall tumor response at 6 months (24 weeks) following completion of CRT (data cut-off 30-Sep-2010). Per RECIST, CR is defined as the disappearance of all target and non-target lesions; PR is defined as at least a 30% decrease in the sum of the long diameter (LD) of target lesions, taking as a reference, the baseline sum LD. Data are based on Week 24 scans from participants receiving study treatment at that time point. From the date of randomization until 6 months post chemoradiation treatment, assessed for a median of 13 months No
Secondary Number of Participants Positive and Negative for the Expression of Biomarkers in Tumor Tissue: Human Epidermal Growth Factor Receptor (HER)-1, HER2, HER3, HER4, P16, and Transforming Growth Factor (TGF-alpha) Paraffin-embedded tissue block (or sections) from archived tumor tissue sample, if available (from time of original diagnosis) or fresh tumor tissue, was sent for testing to determine intra-tumoral biomarker expression by immunohistochemistry (IHC) or fluorescent in situ hybridization (FISH) assay. Stained tumor slides or tissue micro arrays (TMAs) were scored by a pathologist from 0 (no expression) to 3+ (high expression). An expression level of >=2+ was considered positive. Up to 28 days prior to the date of the first dose of lapatinib/placebo start No
Secondary Plasma Proteome Analysis Proteomic analyses of blood plasma samples were to be conducted to identify any changes in the proteome profile that could be related to the treatment response. Examination of pre-dosing (screening) plasma protein profiles could uncover novel blood-borne protein candidate biomarkers/profiles, which could be used to predict drug response. From up to 28 days prior to the first dose of lapatinib/placebo start to 8 weeks after the first dose No
Secondary Analysis of Deoxyribonucleic Acid (DNA) and Ribonucleic Acid (RNA) From Tumor Samples No analysis was performed for tumor sample RNA/DNA. Screening No
Secondary Number of Participants Negative and Positive for Human Papilloma Virus (HPV) Infection, as Determined From Tumor Samples Analysis was performed for HPV infection analysis from the tumor biopsy samples obtained during the Screening period. p16 was used as a marker for HPV; thus, "negative" participants did not have the p16 marker. Up to 28 days prior to the first dose of lapatinib/placebo No
Secondary Number of Participants Positive and Negative for Biomarker HER1/ErbB1 Categorized in the Indicated Independent Review Panel-assessed Tumor Responses by Expression of Biomarkers From Tumor Tissue: Sensitivity Analysis - 0 Versus (1, 2, 3) Tumor tissue (fresh or archived) was sent to a central laboratory for biomarker HER1/ErbB1 and tumor genetics analysis up to 1 week after randomization. Per RECIST: CR, disappearance of all lesions; PR, a >=30% decrease in the sum of the longest dimensions (LD) of the target lesions (TLs) taking as a reference the baseline sum LD; Progressive disease (PD), a >=20% increase in the sum of the LD of TLs, or the appearance of >=1 new lesion; Stable Disease (SD), neither PR nor PD, persistence of >=1 non-TL. 0=negative; 1, 2, 3=positive (increasing level of biomarker expression). From the date of randomization until 6 months post chemoradiation treatment, assessed for up to 24 weeks No
Secondary Number of Participants Positive and Negative for Biomarker HER1/ErbB1 Categorized in the Indicated Independent Review Panel-assessed Tumor Responses by Expression of Biomarkers From Tumor Tissues: Sensitivity Analysis - 0, 1, 2 Versus 3 Tumor tissue (fresh or archived) was sent to a central laboratory for biomarker HER1/ErbB1 and tumor genetics analysis up to 1 week after randomization. Per RECIST: CR, disappearance of all lesions; PR, a >=30% decrease in the sum of the longest dimensions (LD) of the target lesions (TLs) taking as a reference the baseline sum LD; Progressive disease (PD), a >=20% increase in the sum of the LD of TLs, or the appearance of >=1 new lesion; Stable Disease (SD), neither PR nor PD, persistence of >=1 non-TL. 0=negative; 1, 2, 3=positive (increasing level of biomarker expression). From the date of randomization until 6 months post chemoradiation treatment, assessed for up to 24 weeks No
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