Background: Most patients diagnosed with renal carcinoma developed met
astatic disease at some time during their course, with available thera
py inducing response in only a small proportion of patients. Docetaxel
(Taxotere(R), RP56976) a semisynthetic analogue of paclitaxel with a
broad range of in vitro antitumor activity, was evaluated in a phase I
I study. Methods: Eligibility criteria included histologically proven
metastatic or advanced, bidimensionally measurable disease, no prior c
hemotherapy, immunotherapy, or hormonal therapy, adequate hematologic
(neutrophils greater-than-or-equal-to 2.0 x 10(9)/L, platelets greater
-than-or-equal-to 100 x 10(9)/L) and biochemical (serum creatinine and
bilirubin less-than-or-equal-to 1.5 x normal, transaminases less-than
-or-equal-to 3 x normal) parameters, WHO performance status of at leas
t 2, and a life expectancy of > 12 weeks. Docetaxel was administered i
n a dose of 100 mg/m2 as a 1 hour intravenous infusion every 3 weeks.
The first 2 patients entered onto the study were not premedicated for
hypersensitivity reactions; subsequent patients received dexamethasone
10 mg and diphenhydramine 50 mg i.v. 30 minutes prior to docetaxel. R
esults: Twenty patients were entered onto the study, with 2 considered
inevaluable for response. Sixty cycles of therapy were administered,
with only 2 cycles delivered at a dose of 55 mg/m2 or less. No objecti
ve responses were seen; 1 patient demonstrated a mixed response. Neutr
openia was significant, with 42/60 cycles developing grade 3/4 granulo
cytopenia. Fifty-five percent of patients demonstrated hypersensitivit
y reactions despite the premedication regimen employed, higher than th
at of the phase I studies which established the dose and schedule used
in this trial. Conclusions: 1) Docetaxel is an ineffective agent in a
dvanced renal carcinoma. 2) The high rate of hypersensitivity reaction
s suggests the need for more intensive premedication and/or slower inf
usion times at this dose level.