HNSCC Clinical Trial
Official title:
A Phase I Study Evaluating the Combination Afatinib With Docetaxel and Cisplatin (TPA) in Induction Chemotherapy in Locally Advanced Squamous Cell Carcinoma of the Upper Aerodigestive Tract
The purpose of the study is to determine the maximum tolerated dose (MTD) of afatinib
administrated in combination with docetaxel (Taxotere®) and cisplatin in induction
chemotherapy of locally advanced head and neck carcinoma in order to move to a phase II,
allowing the comparison with standard induction chemotherapy TPF.
It is a multicentric, national, opened, not-randomized phase Ib. Three doses of afatinib (20,
30 and 40 Mg per day) will be studied in combination with the fixed standard doses of
docetaxel and cisplatin. For each dose level, beginning with smallest (20 Mg per day of
afatinib), 3 to 6 patients will be treated at maximum, i.e. 3 cycles of three weeks treatment
each one (9 weeks on the whole). The next dose level will be studied only if the previous
dose is well tolerated for the period of the first 4 weeks observation of the treatment (1st
cycle more first week of the 2nd cycle). Once the MTD is determined, four additional patients
will be treated with this dose. A maximum of 22 patients should be included in this study.
The total duration of the study is estimated at 18 months. In case of major safety problems,
the study may be stopped earlier. In short, the preclinical data, pharmacological and
clinical on afatinib indicate that the benefit-risk ratio can be regarded as positive and
that the association of afatinib with cisplatin and docetaxel could be effective in patients
with head and neck squamous cell carcinoma potentially resulting in an extension of time to
progression.
Cancers of the upper aerodigestive tract correspond in the Western countries about 5% of
cancers. They are treated by surgery, radiotherapy, and chemotherapy. Although progress in
radio chemotherapy have reduced mortality and increase the rates of organ preservation in
patients with locally advanced head and neck cancers, they have metastatic risk or
particularly high local recurrence. The induction chemotherapy is a first-line treatment of
cancer in which the patient receives doses of chemotherapy allowing to obtain a significant
reduction in tumor size, and thus to avoid the surgery and to treat the tumor then by
radiotherapy alone or combine by certain drugs. The standard treatment of induction
chemotherapy currently used for the carcinoma of aerodigestive tract is TPF compose of 3
drugs: the docetaxel (or Taxotere®, T), the cisplatin (P) and the 5-fluorouracil (or 5FU, F).
Despite of the relative efficacy of this treatment, which provides a survival benefit, it is
necessary to find a combination of induction to be more effective and less toxic. That is why
this study intended to check if a new combination called TPA in which the fluorouracil (F) is
replaced by the afatinib (A), will be more beneficial. The afatinib is a powerful and
irreversible inhibitor of the EGFR (human Epidermal Growth Factor Receptor type 1), HER2 and
HER 4. The EGFR is associated with a pejorative prognosis and resistance to the treatments
through its role in the proliferation (multiplication of tumoral cells), the cell survival
and replication and angiogenesis (process of growth of new blood-vessels, vital in the growth
of the malignant tumors). Afatinib has proved effective in patients in with local recurrence
or metastatic squamous cell carcinoma of the head and neck after first line cisplatin based
and tolerance is correct.
The rational of this study is based on the following elements:
- Cisplatin and docetaxel on the one hand and the afatinib on the other hand have proved
effectiveness in head and neck cancers. The tolerance of their association is not known.
- In addition, several broad randomized trials have shown that it is possible to improve
the effectiveness of induction chemotherapy in locally advanced head and neck carcinoma
by the addition of Taxotere® to the cisplatin-5FU.
- Independently, it has been shown in carcinoma of the upper aerodigestive tract with
recurrence or metastatic, that an anti-EGFR targeted therapy by cetuximab could improve
the effectiveness of chemotherapy with cisplatin-5FU More recently, Taxotere® and
Cisplatin + Cetuximab (or Erbitux®) combination for the treatment of head and neck
squamous cell carcinoma has been tested in a broad study of phase II showing the good
feasibility of this combination and a particularly high rate of tumoral response.
- Finally a comparative study of cetuximab versus afatinib showed an advantage in terms of
tumoral response in support of afatinib.
From all these observations, the investigators can hypothesize that the addition of afatinib
to the docetaxel and the cisplatin could be an induction treatment for locally advanced
carcinoma both innovating and promising. Indeed, this regimen appears optimized in terms of
efficiency, incorporating both the combination of the most active cytotoxic agents, Taxotere®
and the cisplatin, but also potentially more effective than Erbitux®.
The purpose of the study is to determine the Maximum Tolerated Dose (MTD) of afatinib
administrated in combination with docetaxel (Taxotere®) and cisplatin in induction
chemotherapy of locally advanced head and neck carcinoma in order to move to a phase II,
allowing the comparison with standard induction chemotherapy TPF.
It is a multicentric, national, opened, not-randomized phase Ib. Three doses of the afatinib
(20, 30 and 40 Mg per day) will be studied in combination with the fixed standard doses of
the docetaxel and the cisplatin. For each dose level, beginning with smallest (20 Mg per day
of afatinib), 3 to 6 patients will be treated at maximum, i.e. 3 cycles of three weeks
treatment each one (9 weeks on the whole). The next dose level will be studied only if the
previous dose is well tolerated for the period of the first 4 weeks observation of the
treatment (1st cycle and first week of the 2nd cycle). Once the MTD is determine, four
additional patients will be treated with this dose. A maximum of 22 patients should be
included in this study. The total duration of the study is estimated at 18 months. In case of
major safety problems, the study may be stopped earlier. In short, the preclinical data,
pharmacological and clinical on afatinib indicate that the benefit-risk ratio can be regarded
as positive and that the association of afatinib with cisplatin and docetaxel could be
effective in patients with head and neck squamous cell carcinoma potentially resulting in an
extension of time to progression.
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