Oral Lichen Planus Clinical Trial
Official title:
Prospective Prediction of Malignant Transformation of Oral Leukoplakia Using a MAGE-A-based Immunoscore
Oral squamous cell carcinomas (OSCC) is among the most common malignancies worldwide. Early
detection and prevention of OSCC is thought to have the highest potential to reduce morbidity
and mortality. In prevention, the main focus is on precancerous lesions, especially oral
leukoplakia (OLP), as up to 67% of OSCC arise on the basis of OLP. The determination of the
transformation risk of OLP by histological determination of the degree of dysplasia is
unreliable.
A promising marker for the timely development of a OSCC is the detection of antigens of the
MAGE-A gene family. The special feature of MAGE-A is that they can be detected in 93% of all
OSCC and in approx. 85% of OLP that transform to OSCC. The detection of MAGE-A could also
indicate changes in the immunological environment that occur prior to malignant OLP
transformation and could be used for immunotherapies.
Aim of this study is to investigate MAGE-A as a predictive marker for the malignant
transformation of OLP in the setting of a prospective, multicenter study and to establish it
as a diagnostic parameter in addition to classical histology. In addition, the association of
MAGE-A expression with the occurrence of immunological changes in OLP will be investigated in
order to evaluate the possibility of minimally invasive immunotherapy of OLP.
The study is intended to include 500 biopsies of non-selected patients with OLP from
university institutions and private practices. The follow-up should be at least 3 years,
whereby it is examined whether an OSCC on the basis of the original OLP developed. After
three years, an interim evaluation of the results with statistical evaluation will be carried
out. In order to ensure that the course of the disease is monitored for at least three years
for all OLPs, an extension of the monitoring period to 5 years is planned.
The study could establish a routine diagnostic parameter to supplement the
histo-morphological diagnosis of OLP and evaluate the possibility of immunotherapy of OLP.
Oral squamous cell carcinomas (OSCC) is among the most common malignancies worldwide. Despite
the introduction of microsurgical reconstruction options and advances in multimodal tumor
therapy, the prognosis has not improved significantly in the last 30 years.
The most important aspect for increasing survival rate is seen in the early detection of OSCC
and its precursor lesions. Up to 67 % of OSCC develop on the basis of oral leukoplakia (OLP),
which frequently occur prior to the diagnosis of carcinoma. OLP treatment depends on the risk
of malignant transformation. Therapeutic approaches range from simple observation to complete
surgical excision of OLP. The scientific evidence regarding the handling of OLP is low.
Current literature outlines missing evidence in therapeutic management of OLP. The early
identification of OLP with a high risk of malignant degeneration is a relevant clinical
question, since approx. 2% of OLPs transform malignantly each year. In lesions with dysplasia
this rate increases to about 17%.
Gold standard for determining the risk of malignant transformation of OLP is the histologic
determination of the degree of dysplasia. As the histological degree of dysplasia increases,
so does the risk of developing PECM on the basis of OLP. The decision for a surgical or a
conservative therapy currently depends on the degree of dysplasia of the OLP. The
histopathological assessment of the degree of dysplasia is subjective and depends on the
experience of the pathologist making the assessment. However, the major disadvantage in
assessing the malignant transformation potential with this method is that many precursor
lesions do not follow the histopathologically determined degree of dysplasia. Thus, 0-3% of
hyperplasias (D0) and up to 30% of mild dysplasias (D1) transform to OSCC. D0 OLP are
lesions, which are usually only observed according to current therapy recommendations. Thus,
an assessment of the dignity of OLP and a long-term prediction of the risk for the
development of OSCC are not reliable. OLP with a histopathologically low malignancy potential
but a cell-biologically probable malignant transformation must be identified in order to
prevent undertreatment of these patients.
The aim of this explorative study is to investigate whether the malignant transformation of
OLP can be reliably predicted using immunohistochemical and molecular biological methods. A
significant association of the expression of MAGE-A expression with the malignant
transformation of OLP to OSCC has already been demonstrated in retrospective studies. It is
now necessary to further develop these available test procedures and evaluate them in a
prospective study in order to transfer them into clinical routine. Sensitivity and
specificity of the investigated markers will be investigated in a prospective, multicenter
setting. A non-selected group of patients will be examined. The aim is to establish a test
procedure that can be used cost-effectively. The MAGE-A expression should serve as an
indicator and for the application of new, innovative therapy concepts such as the
immunotherapy of OLP.
The following questions will be answered:
i) Do OLP with malignant transformation show an increased MAGE-A expression in a time
interval of 3 years (follow-up up to 5 years)? ii) How high is the sensitivity and
specificity of MAGE-A expression as a predictive diagnostic test? Is immunohistochemical or
molecular biological (RT-PCR) detection of MAGE-A better suited as a diagnostic test? iii)
Can MAGE-A be used successfully as a diagnostic test in practice? iv) Is there an association
between MAGE-A expression and immunological changes preceding malignant transformation
(macrophage polarization, T cell infiltration, checkpoint expression, TLR expression)? v) Are
the immunological changes in OLP potentially amenable to immunomodulatory therapy?
Short summary of the study protocol:
After the patient has been informed and included in the study, the first step is the photo
documentation and then the incision biopsy of the OLP. The treating physician is free to
choose whether to take a sample from one or more sites of the lesion. This procedure complies
with the standard diagnostic guidelines and is not a study-specific measure. Thus, there is
no deviation from the clinical routine for the study and no invasive measure required by the
study. The sample taken is then divided. The total amount of tissue taken corresponds to the
amount taken in the routine outside the study. One part of the sample is conventionally fixed
in formalin. The second part (max. 5x5x2mm) is preserved in RNA later for later PCR analysis.
Both samples will be sent to the study center in Erlangen. There the histological evaluation
of the tissue takes place in the Pathological Institute of the University Hospital Erlangen
within routine diagnostics. The result is communicated to the treating physician and the
study centre. The immunohistochemical and molecular biological analyses are carried out in
the laboratories of the Oral and Maxillofacial Surgery Erlangen. The results of the analyses
are not communicated to the attending physician (blinding). A therapy decision is only made
on the basis of clinical and classical histological parameters (degree of dysplasia). D0 and
D1 lesions are monitored. D2 and D3 lesions are treated surgically or with laser coagulation
depending on the decision of the treating physician and patient. This corresponds to the
current clinical standard. If the patient rejects the treatment of the lesion and wishes to
continue observing its progress, he remains included in the study. The follow-up time during
the study period is 3 years (evaluations also after 2 years). After completion of the study a
further follow-up of 2 years is planned in order to achieve a total follow-up of 5 years.
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