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5 research outputs found

Concurrent administration of Docetaxel and Stealth® liposomal doxorubicin with radiotherapy in non-small cell lung cancer : excellent tolerance using subcutaneous amifostine for cytoprotection

Author: A Eisbruch
A Kotsakis
AF Walf
B Jeremic
B Reckzeh
C Hennequin
C Schaake-Koning
D Antonadou
F Yuan
G Kyrgias
G Retalis
G V Koukourakis
JA Bonner
K Furuse
K Kayser
K Romanidis
K Tamura
KJ Harrington
KJ Harrington
KJ Harrington
KJ Harrington
L Milas
L Trodella
M Froudarakis
M I Koukourakis
M Koukourakis
M Koukourakis
M Koukourakis
MI Koukourakis
MI Koukourakis
MI Koukourakis
MI Koukourakis
MI Koukourakis
MI Koukourakis
MI Saunders
MV Graham
N Bahlitzanakis
P Marino
PJ Shaw
R Komaki
S Haldar
S Stewart
Publication venue: Nature Publishing Group
Publication date
Field of study

The substantial augmentation of the radiation sequelae during chemo–radiotherapy with novel drugs masks the real potential of such regimens. In this study we examined whether subcutaneous administration of amifostine can reduce the toxicity of a highly aggressive chemo–radiotherapy scheme with Stealth® liposomal doxorubicin (Caelyx®) and Docetaxel (Taxotere®) in non-small cell lung cancer. Twenty-five patients with stage IIIb non-small cell lung cancer were recruited in a phase I/II dose escalation trial. The starting dose of Taxotere® was 20 mg m−2 week and of Caelyx® was 15 mg m−2 every two weeks, during conventionally fractionated radiotherapy (total dose of 64 Gy). The dose of Taxotere®/Caelyx® was, thereafter, increased to 20/25 (five patients) and 30/25 mg m−2 (15 patients). Amifostine 500 mg was given subcutaneously before each radiotherapy fraction, while an i.v. amifostine dose of 1000 mg preceded the infusion of docetaxel. The ‘in-field’ radiation toxicity was low. Grade 3 esophagitis occurred in 9 out of 25 (36%) patients. Apart from a marked reduction of the lymphocyte counts, the regimen was deprived from any haematological toxicity higher than grade 1. No other systemic toxicity was noted. The CR and CR/PR rates in 15 patients treated at the highest dose level was 40% (6 out of 15) and 87% (13 out of 15) respectively. It is concluded that the subcutaneous administration of amifostine during high dose Taxotere®/Caelyx® chemo–radiotherapy is a simple and effective way to render this aggressive regimen perfectly well tolerated, by reducing the systemic and the ‘in-field’ toxicity to the levels expected from simple conventional radiotherapy. The impressive tolerance and the high CR rate obtained encourages the conduct of a relevant randomized trial to assess an eventual survival benefit in patients with non-small cell lung cancer

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PubMed Central

Phase I/II dose escalation study of docetaxel and carboplatin combination supported with amifostine and GM-CSF in patients with incomplete response following docetaxel chemo-radiotherapy: additional chemotherapy enhances regression of residual cancer

Author: A Giatromanolaki
AF Wahl
C Hennequin
CP Belani
DC Betticher
DH Johnson
DJ Glover
DV Skarlos
F Geuritte Voegelein
G Retalis
H Choy
J Brugarolas
JE Mollman
JH Yan
JST Sham
LC Pronk
M Froudarakis
M Graff de
M I Koukourakis
M Koukourakis
MA Bookman
MA Bookman
MI Koukourakis
MI Koukourakis
MJ Bent van den
MJ McKeage
MJ Millward
ML Patchen
MV Blagosklonny
N Bahlitzanakis
P Francis
P Fumoleau
PA Bunn
PH Hilkens
PZ New
RE Langley
RG Hoop van der
RL Capizzi
S Haldar
S Kalokyris
SW Low
T Giannakakis
TC Shea
TH Wang
V Georgoulias
WF Morgan
World Health Organisation
Publication venue: 'Springer Science and Business Media LLC'
Publication date
Field of study

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