Oral Cancer Clinical Trial
Official title:
Biomarker-driven Approach to Develop Population-wide Cost-effective Prevention Strategies for High-risk Oral Premalignancies
Oral cancer is a major health problem worldwide, accounting for 274,000 new cases and
145,000 deaths annually. On average, half of the patients die within 5 years of an oral
cancer diagnosis. Most troubling, however, is the lack of significant change in prognosis
for this disease over the last 4 decades, even in developed nations. Even when successful,
treatment of oral cancer can be devastating due to diminished quality of life and
disfigurement. The key to controlling this disease is early identification of lesions that
are at high risk of progression and provide effective treatment. The overall objective of
the team is to integrate clinical, pathological, molecular, and imaging data to create a
robust oral cancer risk model to predict the risk of progression of OPLs and to develop
population-wide cost-effective prevention strategies for high-risk oral premalignancies. The
project will involve 4 specific aims as described in detail below.
Aim 1. To use molecular data to stratify low-grade OPLs into high- and low-risk groups.
Aim 2. To evaluate the cost-effectiveness of various follow-up frequency that use LOH at
chromosome 9p21 as a risk marker.
Aim 3: To evaluate the specificity and sensitivity of using imaging technologies as a tool
for the decision of the high-grade or high-risk biopsy site.
Aim 4. To assess the clinical utility of a miRNA expression signature derived from serum
collected from patients with oral cancer and OPLs.
1. Patient accrual This study will be occurring at the Otolaryngology Clinic, Vancouver
General Hospital. Three hundred and sixty volunteer subjects will be enrolled to
participate in the study. Detailed steps of the study patient accrual are provided
below.
1. The establishment of referral pipelines for a true population-based OPL cohort in
BC.
In BC, the BC Oral Biopsy Service (OBS) and the Pathology Department at Vancouver
General Hospital (VGH) receive biopsy and surgical specimens from the dental and
medical communities, respectively. These centralized biopsy services offer a very
rare opportunity to establish a population-based cohort of OPLs. The pathologists
team will identify eligible patients through the pathology sign-out process and
call the submitting physicians to notify the potential referral pipeline as an
alternative management for these patients. Currently, a referral pipeline for
severe dysplasia or more advanced oral malignancy using this model exists and has
been established to refer surgical patients for the TFRI-funded COOLS trial (by
Drs. Durham and Poh; H09-03090). This same system/pipeline will be used to
identify eligible patients diagnosed with mild and/or moderate dysplasias
identified from both medical and dental communities.
2. Eligibility Subjects over the age of 19 attend the Dental or Otolaryngology clinic
at the Vancouver General Hospital (Vancouver Acute) for assessment of oral lesions
diagnosed with mild or moderate dysplasia; are willing to give the informed
consent.
3. Recruitment & informed consent procedures A letter of invitation regarding this
study will be mailed to the potentially eligible patients a week before their
appointment date along with the consent document. On the day of the clinical
visit, the research assistant will explain the study to the eligible subject and
acquire signed consent from the participants. 400 subjects will be recruited.
These patients will be monitored once every six months (the current standard of
care). When clinically warranted due to signs of disease progression or at the
2-year follow-up mark, two 5-mm punch biopsies will be performed on lesion areas
with different severity (as determined by imaging technologies). Two-year
comparative biopsy at a stable lesion is current standard of care.
2. Study procedures The study is a longitudinal study following the follow-up schedule of
the current standard of care for such lesions, i.e., once per 6 months and comparative
biopsy once per 2-3 years. The important time points are initial visit (baseline), at
the end of second, 5th and 8th year of follow up visits. However, the time of biopsy is
solely based on the clinical judgment of the clinicians, i.e., signs of disease
progression.
1. Clinical data collection After the subject has consented, they will be asked to
complete a set of questionnaires for the collection of demographics and risk
factor information. The subject will be assigned a study ID and no unique
identifier will be linked to the data collected. A separate file will be used to
link the study ID and patient identifiers. This is important to facilitate patient
management and capture the outcome information. This file with patients' unique
identifier will be kept in the pass-word protected file in the BC Cancer Research
Centre (BCCRC) computer in a locked office in the BCCCRC and only PIs can access
the file. The health status and HAI questionnaire is not for diagnostic purposes.
Should the clinicians believe there is depression or anxiety present in the
participant (clinicians' clinical judgment), the study clinicians in charge of
this specific participant will communicate with patient's family doctor and refer
the participant to a proper source for further evaluation and management.
2. Data collection using study device
- The clinicians will examine the patients using WL, VELScope VX for FV
(previously approved, R05-0116), OCT (previously approved, H09-01955), and a
hand-held confocal microscope (H11-00011).
- OCT imaging: After identifying the abnormal areas for biopsy using WL and FV
examination, the clinician will place a fiber-optic probe of the OCT on the
oral mucosal areas of interest. The site for placement of the probe will be
determined by PIs (Otolaryngology-head and neck surgeons (SD/DA) and/or Oral
Medicine/Oral Pathology Specialist (Ng/Poh)). The images will be recorded by
the machine for later analysis.
- Confocal microscope imaging: After OCT imaging, the clinician will apply
0.05% Acriflavine Hydrochloride solution topically on the oral mucosal areas
of interest for 30 seconds prior to imaging. The clinician will place a
hand-held confocal microscope on the mucosal surface to record the
observation for later analysis.
- All necessary efforts will be taken to reduce any mild discomfort that could
be associated with the probe placement inside the oral cavity of a subject.
The OCT probe or the confocal microscope will be covered by a plastic barrier
and disinfected by standard methods used for oral cavity instruments before
and after subject usage. The device examination will take no more than 15
minutes in addition to the subject's appointment time for their routine
visits. The maximum intensity of tissue illumination for each measurement
will be less than the Threshold Limit Value (TLV) established by the American
Conference of Governmental Industrial Hygienists (ACGIH)11 for exposure to
broadband light.
- The information obtained from polarized reflectance measurements will be
compared with the histology and quantitative pathology (nuclear phenotype
score) of the tissue sections from the lesion. The collected spectra data
from normal looking areas from adjacent normal looking mucosa and
contralateral mucosa will be used to determine patient to patient variation
in the polarized reflectance of oral mucosa.
3. Exfoliative brushing sample collection (previously approved, R05-0116) An
Innovatec cytology brush (Arcona Inc) is used to collect exfoliated cells from the
oral lesion. These brushings are transferred into PreservCyt® Solution (Cytyc
Corp.) and keep in 4ºC fridge.
4. Blood sample collection In total, 12 ml (3/4 of a tablespoon) of blood sample will
be collected in 1 SST and 1 EDTA vacutainers in the clinic by trained research
personnel. The blood sample will be processed and serum, plasma and puffy coat
samples will be aliquot and frozen in -80ºC for future analysis. The DNA samples
in the puffy coat will be extracted and used as the normal control sample for the
loss of heterozygosity (LOH) analysis. A separate consent will be used for this
purpose. We anticipate that all aliquots of serum, plasma and puffy coat will be
used up. Any remaining tissue will not be discarded or sold, but will be stored in
a locked freezer room at the BC Cancer Agency for a period of up to fifteen years
so that results of this study can be confirmed.
5. Frozen tissue collection In the event of biopsy, tissue will be bisected. Half of
the sample will be fixed in the formalin solution and sent to the pathology
laboratory for analysis as a normal part of medical diagnosis procedure. Part of
this tissue will be kept and used only after the diagnosis has been made. At no
time will tissue be removed solely for the purpose of research. The donated tissue
will be given a code for identification by the project leader, and will be kept in
secure freezers at the BC Cancer Agency until genetic material (DNA and RNA) has
been extracted for analysis. A separate consent will be used for this purpose. We
anticipate that all donated tissue will be used up. Any remaining tissue will not
be discarded or sold, but will be stored in a locked freezer room at the BC Cancer
Agency for a period of up to fifteen years so that results of this study can be
confirmed.
6. Tissue microdissection and DNA extraction. The formalin-fixed, paraffin-embedded
tissue blocks of the initial biopsy and biopsy from the follow-up visit will be
obtained from the Department of Anatomical Pathology, the Vancouver General
Hospital. at the time of clinical change or at 24 months follow-up visit will be
requested for processing. Ten 10-µm thick sections for DNA sample, 2 4-µm
unstained tissue sections for quantitative histological analysis. Areas of
dysplasia on the thick sections will be identified and microdissected. The DNA
sample from the epithelium will be extracted and used for the LOH analysis.
;
| Status | Clinical Trial | Phase | |
|---|---|---|---|
| Recruiting |
NCT06031337 -
Salivary Expression of SOX7 in Oral Squamous Cell Carcinoma: Diagnostic Accuracy Study
|
||
| Completed |
NCT00158678 -
IMRT Plus Cisplatin Versus Conventional Radiotherapy Plus Cisplatin in Stage III-IV HNSCC
|
Phase 3 | |
| Completed |
NCT00933387 -
A Study of Neoadjuvant Bio-C/T Followed by Concurrent Bio-R/T in High-risk Locally Advanced Oral Squamous Cell Carcinoma
|
Phase 2 | |
| Enrolling by invitation |
NCT05030597 -
Exploring the Application Value of PET Molecular Imaging Targeting FAP in Oral Squamous Cell Carcinoma
|
N/A | |
| Completed |
NCT03682562 -
Diagnostic Accuracy of Salivary DNA Integrity Index in Oral Malignant and Premalignant Lesions
|
||
| Recruiting |
NCT03684707 -
Cancer Chemoprevention by Metformin Hydrochloride Compared to Placebo in Oral Potentially Malignant Lesions
|
Phase 4 | |
| Recruiting |
NCT06130332 -
Neoadjuvant Tirellizumab Combined With Chemotherapy for Early Oral Squamous Cell Carcinoma(HNC-SYSU-004)
|
Phase 2 | |
| Recruiting |
NCT04372914 -
Prevention of Oral DNA Damage by Black Raspberries
|
N/A | |
| Active, not recruiting |
NCT03529422 -
Durvalumab With Radiotherapy for Adjuvant Treatment of Intermediate Risk SCCHN
|
Phase 2 | |
| Recruiting |
NCT03686020 -
Sensitivity and Specificity of Serum and Salivary CYFRA21-1 in the Detection of Malignant Transformation in Oral Potentially Malignant Mucosal Lesions (Diagnostic Accuracy Study)
|
||
| Not yet recruiting |
NCT06060288 -
Diagnostic Accuracy of Mobile Phone Imaging Compared to Conventional Clinical Examination for Oral Cancer Screening
|
||
| Withdrawn |
NCT00951470 -
Complete Decongestive Therapy (CDT) for Treatment of Head and Neck Lymphedema
|
N/A | |
| Completed |
NCT00964977 -
Effectiveness of Adjuvant Radiotherapy in Small Oropharyngeal Squamous Cell Cancer and Single Lymph Node Metastasis.
|
Phase 3 | |
| Completed |
NCT01418118 -
Assessment of the Effects of Pressors on Graft Blood Flow After Free Tissue Transfer Surgery
|
Phase 4 | |
| Active, not recruiting |
NCT00232960 -
Postoperative Radiotherapy According to Molecular Analysis of Surgical Margins of Oral and Oropharyngeal SCC
|
N/A | |
| Recruiting |
NCT05429099 -
Mandibular Reconstruction Preplanning (ViPMR)
|
Phase 2/Phase 3 | |
| Completed |
NCT04614896 -
Use of Ultrasound for Measuring Size of Oral Tongue Cancers
|
N/A | |
| Recruiting |
NCT03685409 -
Cancer Chemoprevention by Metformin Hydrochloride in Oral Potentially Malignant Lesions
|
Phase 3 | |
| Completed |
NCT00402779 -
Erlotinib Prevention of Oral Cancer (EPOC)
|
Phase 3 | |
| Recruiting |
NCT05153733 -
Improved Implant for Reconstruction Purposes After Mandibular Resection
|
N/A |