Squamous Cell Carcinoma of the Skin Clinical Trial
Official title:
Chemoprevention of Squamous Cell Cancer of the Skin in High Risk Patients
This study is proposed based on our work showing that the diabetes drug Pioglitazone strongly inhibits growth of tissue cultured squamous cell carcinoma (SCC) of the skin. This occurs at concentrations readily achievable by oral administration of this drug using doses currently approved for the treatment of diabetes. In our study, we propose to enroll 40 non-diabetic adult subjects (18-80 yrs of age inclusive) with a documented clinical history of frequent occurrence of skin squamous cell cancer to receive Pioglitazone (Actos®,Takeda Pharmaceuticals). Each subject will receive usual care for all new tumors they develop while on study (i.e, excision and plastic repair). The study protocol will randomize (1:1) patients for 6 months of observation followed by 6 months of treatment (group 1) or 6 months of treatment with drug followed by observation for 6 months (to examine washout effects). The biopsy specimens collected on and off therapy will be examined to determine if they express AKR1C3, an enzyme we believe increases resistance of SCC to prostaglandin inflammatory mediators. We will also examine the histologic grade of the removed tumors and study whether Pioglitazone treatment can decrease the number of aggressive versus well differentiated tumors in study patients. This pilot study is designed to detect a statistically significant change in SCC tumor numbers but is not sponsored by the drug manufacturer. The data obtained will not be used to effect a change in the product label.
This is a single center open label feasibility pilot project based at the University of
Rochester. This study is proposed based on our work showing that the diabetes drug
Pioglitazone strongly inhibits growth of tissue cultured squamous cell carcinoma (SCC) of the
skin. This occurs at concentrations readily achievable by oral administration of this drug
using doses currently approved for the treatment of diabetes. In our study, we propose to
enroll 40 non-diabetic adult subjects (18-80 yrs of age inclusive) with a documented clinical
history of frequent occurrence of skin squamous cell cancer to receive Pioglitazone
(Actos®,Takeda Pharmaceuticals). Patients followed in the University of Rochester Dermatology
Clinic who have had greater than 3 or more SCCs treated in the past year, without
contraindication for the use of pioglitazone, and are on a stable drug treatment regimen will
be offered participation .The study has a cross-over design, so patients will be enrolled and
randomized to one arm of two treatment protocols: 1) six months of usual care while
documenting and characterizing any new tumors that occur followed by 6 months of pioglitazone
treatment plus usual care for the next 6 months or 2) six months of pioglitazone treatment
followed by 6 months off treatment receiving usual care. The second group will offer the
opportunity to assess whether there is any persistent beneficial effect after pioglitazone
treatment ends, while tumors from the first group that occur during the initial 6 months of
usual care will be characterized by study parameters for comparison to tumors arising while
on treatment. At the end of the one year treatment period, the number of biopsy-proven new
tumors that patients develop while taking pioglitazone will be counted and compared with the
number that patients developed during the 6 month period they were not receiving treatment as
well as the numbers that occurred during the 6 months after treatment (washout effect). This
information will be used as the basis for a larger multicenter study. We will also examine
the histologic grade of the removed tumors and study whether Pioglitazone treatment can
decrease the number of aggressive versus well differentiated tumors in study patients. This
pilot study is designed to detect a statistically significant change in SCC tumor numbers but
is not sponsored by the drug manufacturer. The data obtained will not be used to effect a
change in the product label.
This study will also assess secondary endpoints. First, we will examine whether the ratio of
well-differentiated to poorly differentiated SCC is influenced while subjects are on
treatment. This endpoint is included because it is unknown whether there may be more
signaling mediated by PPARγ in one tumor morphology vs. another. Second, we will determine
whether patients on treatment might have different numbers of "borderline" lesions biopsied;
precancerous lesions are often suspicious enough to biopsy. It may be that there will be
fewer lesions in this category, as well as fewer squamous cell cancers. Basal cell cancers
and other forms of skin cancer will also be documented. Third, we will test tumors that are
excised after they are processed for routine diagnostic pathology to see if markers of
proliferation or apoptosis that are influenced by PPARγ activity or the presence of AKR1C3
are altered. These endpoints would support the idea that any changes produced in tumor
incidence while patients are on study drug are related to the mechanistic effect on PPARγ
that is proposed.
Subjects will be excluded from study if they have NYHA class I - IV cardiac status because of
concerns that thiazolidinediones, such as Pioglitazone, may exacerbate congestive heart
failure.
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