At a
median follow up of 15 months, 41 (61%) patients were men and 26 (39%) were
women, with a median age of 50, and a median KPS of 87. Glioblastoma multiforme
was the most common histological type in 34 (51%) patients, followed by astrocytoma
in 26 (39%) and oligodendroglioma in 7 (10%). 28 (42%) patients underwent total
resection, 31 (46%) partial resection, and 8 (12%) biopsy only. Concurrent
Temozolamide (TMZ) was administered to 76% of patients. All patients completed
treatment, 78% without breaks, and 22% with 1-3 breaks. The most common acute
adverse events were: G1 headache (27%), alopecia (14%), G1 fatigue (11%), and
G1 epidermitis (11%). The most commonly registered chronic adverse events were:
cognitive deficit (23%), partial seizures (23%), and vision change (15%). Acute
toxicity was higher in the 20 fractions scheme (50%), while chronic toxicity
was higher in the 10 fractions scheme (56%). Overall survival (OS) was of 94%,
90%, 75%, and 53% at 3, 6, 12, and 24 months respectively. 36 (54%) patients
were still alive at last follow up. Progression free survival (PFS) was of 92%, 77%, 54%, and 44% at 3, 6, 12, and 24
months, respectively, reaching median PFS at 15 months. Treatment volumen
<290 cc and total or partial resection showed better OS and PFS; Concurrent
TMZ showed better OS; however, in univariate and multivariate analysis, none
proved to be a survival predictive factor. At univariate analysis, age > 50 (p=0.009) and KPS <90 previous to HFRT (p=0.019), and KPS <90 at the end of HFRT (p=0.004), were associated with worse OS. While
in multivariate analysis only age >50 (RR
2.71 p=0.030) and KPS <90 at the
end of HFRT (RR 6.08 p=0.001], proved to be worse OS predictive factors.