Text Size

RTOG 0920: A Study of Postoperative Radiation Therapy (IMRT) +/- Cetuximab for Locally-advanced Resected Head and Neck Cancer

This study is currently recruiting participants.
Verified December 2011 by King Faisal Specialist Hospital & Research Center
Sponsor:
Collaborator:
Radiation Therapy Oncology Group
Information provided by (Responsible Party):
King Faisal Specialist Hospital & Research Center
ClinicalTrials.gov Identifier:
NCT01311063
First received: March 6, 2011
Last updated: December 11, 2011
Last verified: December 2011
History of Changes
  Purpose

The adjuvant management of completely resected SCCHN is somewhat more controversial. In general, postoperative radiotherapy (PORT) is a standard of care for most stage III/IV and selected stage II resected cases. In the last several years, several high-profile randomized trials have shown that the addition of concurrent chemotherapy to PORT improves outcomes for selected patients. The RTOG led a North American Intergroup trial comparing standard PORT with or without three cycles of high dose concurrent cisplatin. The patient population consisted of individuals who underwent complete resection but had positive resection margins at the primary tumor site, multiple pathologically positive lymph nodes in the neck, or one or more lymph nodes in the neck with extracapsular extension. This study showed the chemo radiotherapy had significantly improved local-regional control (LRC) and disease-free survival (DFS) but not overall survival, compared with PORT alone. The EORTC performed a very similar study of PORT +/- chemotherapy, showing that chemo radiotherapy improved overall survival in addition to LRC and DFS (Bernier 2004).

Bernier, et al. (2005) subsequently performed a meta-analysis of the RTOG and EORTC trials. In this exploratory analysis, the primary subgroups of patients who benefited significantly from the addition of chemotherapy were those with positive resection margins and/or nodal extracapsular extension. Other patients did not have a significant benefit from high dose concurrent cisplatin. Specifically in RTOG 95-01, this refers to patients with multiple positive nodes (pN2) without extracapsular spread (ECS). In the EORTC study, this refers to a potpourri of patients, including: pathologic T3-4, N0 cancers (except T3, N0 larynx cancer), perineural and/or vascular invasion irrespective of T-stage, or oral/oropharynx cancer with lymph node involvement at Level IV or V. The failure of cisplatin to significantly improve survival or other clinical outcomes does not, however, mean that these patients have a very good or excellent prognosis. As shown below in Table 1, multiple series of data report a rate of local-regional failure between 15 and 35% for these patients, despite adjuvant RT. Most patients who suffer local-regional failure cannot be salvaged with additional anti-cancer treatment and proceed to die from their cancer. The exact rate of local-regional failure probably depends upon multiple factors, including the number of clinical risk factors present (as described by the University of Florida), treatment related factors (such as the quality of surgery and/or RT, as well as the amount of time required to deliver treatment), and currently poorly understood biological/molecular features of patients' tumors. These complex factors make it very difficult to compare one study to another, particularly retrospective experiences harvested at different institutions over several decades. A relatively large prospective trial would thus provide valuable information to help physicians and patients more precisely identify the risk factors for local-regional recurrence (and other clinical outcomes) after surgery + RT.


Condition Intervention Phase
Pathologically Confirmed SCC of the Head/Neck (Oral Cavity, Oropharynx or Larynx); Clinical Stage T2-3, N0-2, M0 or T1, N1-2, M0.
 Radiation: Radiation Therapy Alone
Radiation: Radiation Therapy + Cetuximab
 Phase 3

Study Type: Interventional
Study Design: Allocation: Randomized
Endpoint Classification: Efficacy Study
Intervention Model: Single Group Assignment
Masking: Open Label
Primary Purpose: Treatment

Resource links provided by NLM:

Drug Information available for: Cetuximab
U.S. FDA Resources

Further study details as provided by King Faisal Specialist Hospital & Research Center:

Primary Outcome Measures:
  • RTOG 0920: A Phase III Study of Postoperative Radiation Therapy (IMRT) +/- Cetuximab for Locally-Advanced Resected Head and Neck Cancer [ Time Frame: 2 yrs ] [ Designated as safety issue: Yes ]

    Primary Objective

    1. Test whether the addition of cetuximab to radiation therapy will improve overall survival (OS) in postoperative patients with intermediate risk following surgery



Estimated Enrollment: 700
Study Start Date: October 2010
Estimated Study Completion Date: October 2012
Estimated Primary Completion Date: October 2012 (Final data collection date for primary outcome measure)
Arms Assigned Interventions
Active Comparator: Arm1:
Radiation Therapy Alone RT, 2 Gy/day, in 30 fractions for a total of 60 GyA
 Radiation: Radiation Therapy Alone
Radiation Therapy Alone
Experimental: Arm 2:

Radiation Therapy + Cetuximab

At least 5 days prior to RT:

cetuximab: Initial dose, 400 mg/m2

RT, 2 Gy/day in 30 fractions for a total of 60 GyA plus cetuximab: 250 mg/m2/week x 6 weeks

plus cetuximab: 250 mg/m2/week x 4 weeks post-RT

(cetuximab: 1 initial dose + 10 maintenance doses, a total of 11 doses)

 Radiation: Radiation Therapy + Cetuximab
Radiation Therapy + Cetuximab

Detailed Description:

Primary Objective

  1. Test whether the addition of cetuximab to radiation therapy will improve overall survival (OS) in postoperative patients with intermediate risk following surgery

    Secondary Objectives

  2. Assess the impact of the addition of cetuximab to postoperative radiation therapy on the following:

    • Disease-free survival (DFS);
    • Acute dysphagia, dry mouth, skin toxicity, and other toxicities (CTEP's Active Version CTCAE) and their relationships to patient-reported outcomes at 3 months;
    • Late dysphagia, dry mouth, skin toxicity, and other toxicities (Active Version CTCAE) and their relationships to patient-reported outcomes at 12 and 24 months.
  3. Tumor analysis of EGFR, specifically extent of EGFR over expression by immunohistochemical (IHC) and FISH analysis, EGFRvIII expression, as well as association of these assay data with OS and DFS;
  4. Tumor analysis of HPV infection (as defined by in situ hybridization), specifically, within the cohort of patients with oropharynx cancer, to perform an exploratory analysis of the impact of HPV on DFS and OS in this patient subset;
  5. Tumor DNA analyses of TP53 mutations for response prediction to cetuximab and prognosis;
  6. Germline DNA analyses of polymorphic variants in EGFR intron repeat for response prediction to cetuximab.

Tertiary Objectives (Exploratory)

  1. Assess the impact of the addition of cetuximab to postoperative radiation therapy on the following:

    • Local-regional control;
    • Patient-reported quality of life (QOL), swallowing, xerostomia, and skin toxicity based on head and neck specific instruments, including: the Performance Status Scale for Head and Neck Cancer (PSS-HN), the Functional Assessment of Cancer Therapy-Head & Neck (FACT-H&N), the University of Michigan Xerostomia-Related Quality of Life Scale (XeQOLS), and the Dermatology Life Quality Index (DLQI);
    • Cost-utility analysis using the EuroQol (EQ-5D).
  2. To evaluate the utility of IGRT as a means of enhancing the efficacy (i.e., local-regional control) of IMRT while reducing the acute and/or late toxicity (particularly xerostomia) and improving patient-reported outcomes (particularly scores with the XeQOLS);
  3. To retrospectively compare the local regional control rate for patients treated with IMRT alone (no IGRT or cetuximab) with similar patients treated with external beam radiation alone in the postoperative trial, RTOG 95-01.

Patient Population:

Pathologically proven diagnosis of squamous cell carcinoma (including variants such as verrucous carcinoma, spindle cell carcinoma, carcinoma NOS, etc.) of the head/neck (oral cavity, oropharynx or larynx); clinical stage T2-3, N0-2, M0 or T1, N1-2, M0.

  Eligibility

Ages Eligible for Study:   18 Years to 90 Years
Genders Eligible for Study:   Both
Accepts Healthy Volunteers:   No
Criteria

Inclusion Criteria:

  • 3.1 Conditions for Patient Eligibility 3.1.1 Pathologically (histologically) proven diagnosis of squamous cell carcinoma (including variants such as verrucous carcinoma, spindle cell carcinoma, carcinoma NOS, etc.) of the head/neck (oral cavity, oropharynx or larynx); Note: Hypopharynx primaries are excluded because these patients have both a poor prognosis and high likelihood of post-radiation complications.

3.1.2 Clinical stage T1, N1-2 or T2-3, N0-2, M0 including no distant metastases, based upon the following minimum diagnostic workup: 3.1.2.1 General history and physical examination by a Radiation Oncologist and/or Medical Oncologist within 8 weeks prior to registration; 3.1.2.2 Examination by an ENT or Head & Neck Surgeon, including laryngopharyngoscopy (mirror and/or fiberoptic and/or direct procedure), within 8 weeks prior to registration; 3.1.2.3 Chest x-ray (at a minimum) or chest CT scan (with or without contrast) or CT/PET of chest (with or without contrast) within 8 weeks prior to registration. 3.1.3 Gross total resection of the primary tumor with curative intent must be completed within 7 weeks of registration with surgical pathology demonstrating one or more of the following "intermediate" risk factors: 3.1.3.1 Perineural invasion; 3.1.3.2 Lymphovascular invasion; 3.1.3.3 Single lymph node > 3 cm or ≥ 2 lymph nodes (all < 6 cm) [no extracapsular extension]; 3.1.3.4 Close margin(s) of resection, defined as cancer extending to within 5 mm of a surgical margin; 3.1.3.5 T3 or microscopic T4a primary tumor (Note: Gross T4a or T4b is ineligible); 3.1.3.6 T2 oral cavity cancer with > 5 mm depth of invasion. 3.1.4 Zubrod Performance Status of 0-1 within 2 weeks prior to registration; 3.1.5 Age ≥ 18; 3.1.6 CBC/differential obtained within 4 weeks prior to registration on study, with adequate bone marrow function defined as follows: 3.1.6.1 Absolute granulocyte count (AGC) ≥ 1,500 cells/mm3; 3.1.6.2 Platelets ≥ 100,000 cells/mm3; RTOG 0920 18 3.1.6.3 Hemoglobin ≥ 8.0 g/dl (Note: The use of transfusion or other intervention to achieve Hgb ≥ 8.0 g/dl is acceptable). 3.1.7 Adequate hepatic function, defined as follows: 3.1.7.1 Total bilirubin < 2 x institutional ULN within 2 weeks prior to registration; 3.1.7.2 AST or ALT < 3 x institutional ULN within 2 weeks prior to registration.

3.1.8 Adequate renal function, defined as follows: 3.1.8.1 Serum creatinine < 2 x institutional ULN within 2 weeks prior to registration or; creatinine clearance (CC) ≥ 50 ml/min within 2 weeks prior to registration determined by 24- hour collection or estimated by Cockcroft-Gault formula: CCr male = [(140 - age) x (wt in kg)] [(Serum Cr mg/dl) x (72)] CCr female = 0.85 x (CrCl male) 3.1.9 Negative serum pregnancy test within 2 weeks prior to registration for women of childbearing potential; 3.1.10 (6/4/10) The following assessments are required within 2 weeks prior to the start of registration: Na, K, Cl, glucose, Ca, Mg, and albumin. Note: Patients with an initial magnesium < 0.5 mmol/L (1.2 mg/dl) may receive corrective magnesium supplementation but should continue to receive either prophylactic weekly infusion of magnesium and/or oral magnesium supplementation (e.g., magnesium oxide) at the investigator's discretion. 3.1.11 Women of childbearing potential and male participants who are sexually active must agree to use a medically effective means of birth control; 3.1.12 Patients must provide study specific informed consent prior to study entry, including consent for mandatory tissue submission for EGFR and for oropharyngeal patients, HPV analyses.

Exclusion Criteria:

  • 3.2.1 Prior invasive malignancy (except non-melanomatous skin cancer) unless disease free for a minimum of 3 years; noninvasive cancers (For example, carcinoma in situ of the breast, oral cavity, or cervix are all permissible) are permitted even if diagnosed and treated < 3 years ago.

Patients with simultaneous primaries or bilateral tumors are excluded. 3.2.2 Per the operative report, positive margin(s) [defined as tumor present at the cut or inked edge of the tumor], nodal extracapsular extension, and/or gross residual disease after surgery; 3.2.3 Prior systemic chemotherapy or anti-EGF therapy for the study cancer; note: prior chemotherapy or anti-EGF therapy for a different cancer is allowable. See section 3.2.1.

3.2.4 Prior radiotherapy to the region of the study cancer that would result in overlap of radiation therapy fields; 3.2.5 Severe, active co-morbidity, defined as follows: 3.2.5.1 Unstable angina and/or congestive heart failure requiring hospitalization within 6 months prior to registration; 3.2.5.2 Transmural myocardial infarction within 6 months prior to registration; 3.2.5.3 Acute bacterial or fungal infection requiring intravenous antibiotics at the time of registration; 3.2.5.4 Chronic Obstructive Pulmonary Disease exacerbation or other respiratory illness requiring hospitalization or precluding study therapy at the time of registration; 3.2.5.5 Idiopathic pulmonary fibrosis or other severe interstitial lung disease that requires oxygen therapy or is thought to require oxygen therapy within 1 year prior to registration; 3.2.5.6 Hepatic insufficiency resulting in clinical jaundice and/or coagulation defects; note, however, that laboratory tests for coagulation parameters are not required for entry into this protocol.

3.2.5.7 Acquired Immune Deficiency Syndrome (AIDS) based upon current CDC definition; note: HIV testing is not required for entry into this protocol. The need to exclude patients with AIDS from this protocol is necessary because the treatments involved in this protocol may be significantly immunosuppressive. Protocol-specific requirements may also exclude immuno-compromised patients. 3.2.5.8 (6/4/10) Grade 3-4 electrolyte abnormalities (CTCAE, v. 4.0):

  Contacts and Locations
Please refer to this study by its ClinicalTrials.gov identifier: NCT01311063

Contacts
Contact: Nasser AlRajhi, MD 966-44-24575 nrajhi@kfshrc.edu.sa
Contact: Fazal Hussain, MD 966-44-23949 fhussain@kfshrc.edu.sa

Locations
Saudi Arabia
Oncology Centre, King Faisal Specialist Hospital & Research Center Recruiting
Riyadh, Saudi Arabia, 11211
Contact: Nasser AlRajhi, MD     966-44-24575     nrajhi@kfshrc.edu.sa    
Contact: Fazal Hussain, MD     966-44-23949     fhussain@kfshrc.edu.sa    
Sponsors and Collaborators
King Faisal Specialist Hospital & Research Center
Radiation Therapy Oncology Group
  More Information

No publications provided

Responsible Party: King Faisal Specialist Hospital & Research Center
ClinicalTrials.gov Identifier: NCT01311063     History of Changes
Other Study ID Numbers: RAC# 2101-074
Study First Received: March 6, 2011
Last Updated: December 11, 2011
Health Authority: Office of Research Affairs, MBC 03:
King Faisal Specialist Hospital & Research Centre:
P.O. Box 3354 Riyadh 11211:
Kingdom of Saudi Arabia:

Additional relevant MeSH terms:
Head and Neck Neoplasms
Neoplasms by Site
Neoplasms
Cetuximab
 Antineoplastic Agents
Therapeutic Uses
Pharmacologic Actions

ClinicalTrials.gov processed this record on May 16, 2013