CT-2103 (XYOTAX(TM), Cell Therapeutics, Inc.) is a conjugate of paclitaxel to a polyglutamate polymer. its macromolecular nature exploits enhanced permeability and retention in tumour tissues. This compound is stable and inactive in aqueous solution and undergoes predominantly intracellular metabolism at the site where active paclitaxel is released. Because it does not require a Cremophor(R) EL vehicle, it can be administered by short infusion into peripheral veins. In preclinical models, compared with the same dose of unconjugated paclitaxel in Cremophor EL-ethanol, CT-2103 yields greater than or equal to12-fold increase in area under the curve in both plasma and tumour tissue. This alteration in drug pharmacokinetics and biodistribution is attributable to the ability of macromolecules to concentrate in areas of vascular leakiness, such as tumour tissue. CT-2103 is taken up by both tumour cells and normal phagocytic cells and is transported to lysosomes, where it is released by specific proteases through enzymatic action. In syngeneic and xenogeneic tumour models, at the maximally tolerated dose, CT-2103 appears to be more active than the standard doses of paclitaxel. it has also demonstrated activity in paclitaxel-resistant tumour models. Its potential enhancement of efficacy and decrease in drug-related toxicities make this agent an attractive option for therapeutic investigation. In Phase I trials it has been relatively well-tolerated, with acceptable toxicity at doses less than or equal to 225 mg/m(2) every 3 weeks. In combination with carboplatin the maximum tolerated dose is 235 mg/m(2) and the recommended Phase II dose 210 mg/m(2). Activity has been demonstrated in both non-small cell lung carcinoma (NSCLC) and in ovarian cancer, Phase III studies are currently testing this agent versus standard paclitaxel as maintenance therapy for first-line treatment-naive ovarian cancer. In addition, CT-2103 at a dose of 210 mg/m(2) (performance status [PS] 0 - 1) or 175 mg/m(2) (PS 2) is being compared with docetaxel (75 mg/m(2)) for the second-line treatment of NSCLC. In front-line PS 2 NSCLC patients, this agent in combination with carboplatin is undergoing comparison with paclitaxel/carboplatin; in a separate effort, single agent CT-2103 is being compared with either gemcitabine or vinorelbine. These studies will determine whether the preclinical and early clinical promise of this agent can be realised in the clinical treatment of solid tumours.
机构:
Kings Coll London, Guys Canc Ctr, Sch Canc & Pharmaceut Sci, CAR Mech Grp, London SE1 9RT, England
Eastbourne Hosp, Dept Immunol, Kings Dr, Eastbourne BN21 2UD, England
Guys Hosp, Leucid Bio Ltd, Great Maze Pond, London SE1 9RT, EnglandKings Coll London, Guys Canc Ctr, Sch Canc & Pharmaceut Sci, CAR Mech Grp, London SE1 9RT, England
Maher, John
Davies, David M.
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Guys Hosp, Leucid Bio Ltd, Great Maze Pond, London SE1 9RT, EnglandKings Coll London, Guys Canc Ctr, Sch Canc & Pharmaceut Sci, CAR Mech Grp, London SE1 9RT, England
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Livestock Farming and Bioresource Technology, Tamil NaduLivestock Farming and Bioresource Technology, Tamil Nadu
Iyer M.
Venugopal A.
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Human Molecular Cytogenetics and Stem Cell Laboratory, Department of Human Genetics and Molecular Biology, Bharathiar University, Coimbatore, 641 046, Tamil NaduLivestock Farming and Bioresource Technology, Tamil Nadu
Venugopal A.
Chandrasekhar M.
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Human Molecular Cytogenetics and Stem Cell Laboratory, Department of Human Genetics and Molecular Biology, Bharathiar University, Coimbatore, 641 046, Tamil NaduLivestock Farming and Bioresource Technology, Tamil Nadu
Chandrasekhar M.
Suriyanarayanan A.
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Human Molecular Cytogenetics and Stem Cell Laboratory, Department of Human Genetics and Molecular Biology, Bharathiar University, Coimbatore, 641 046, Tamil NaduLivestock Farming and Bioresource Technology, Tamil Nadu
Suriyanarayanan A.
Balasubramani K.
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Human Molecular Cytogenetics and Stem Cell Laboratory, Department of Human Genetics and Molecular Biology, Bharathiar University, Coimbatore, 641 046, Tamil NaduLivestock Farming and Bioresource Technology, Tamil Nadu
Balasubramani K.
Sinthai Ilangovan A.
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Human Molecular Cytogenetics and Stem Cell Laboratory, Department of Human Genetics and Molecular Biology, Bharathiar University, Coimbatore, 641 046, Tamil NaduLivestock Farming and Bioresource Technology, Tamil Nadu
Sinthai Ilangovan A.
Kamalakannan S.
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Centre for Medical Entomology & Vector Management, National Centre for Disease Control (NCDC), Ministry of Health and Family Welfare, New Delhi, New DelhiLivestock Farming and Bioresource Technology, Tamil Nadu
Kamalakannan S.
Gunaseelan R.
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Bharathiar School of Management and Entrepreneur Development (BSMED), Bharathiar University, Coimbatore, 641 046, Tamil NaduLivestock Farming and Bioresource Technology, Tamil Nadu
Gunaseelan R.
Ayyadurai N.
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Biochemistry & Biotechnology, CSIR-Central Leather Research Institute, Chennai, 600 020, Tamil NaduLivestock Farming and Bioresource Technology, Tamil Nadu
Ayyadurai N.
Valsala Gopalakrishnan A.
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Department of Biomedical Sciences, School of Biosciences and Technology, Vellore Institute of Technology, Vellore, 632 014, Tamil NaduLivestock Farming and Bioresource Technology, Tamil Nadu
Valsala Gopalakrishnan A.
Rachaiah Balraj L.
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A Level, Delhi Public School, IGCSE, North, BangaloreLivestock Farming and Bioresource Technology, Tamil Nadu
Rachaiah Balraj L.
Aghil I.
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Human Molecular Cytogenetics and Stem Cell Laboratory, Department of Human Genetics and Molecular Biology, Bharathiar University, Coimbatore, 641 046, Tamil NaduLivestock Farming and Bioresource Technology, Tamil Nadu
Aghil I.
Palanisamy S.
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Department of Mechanical Engineering, Dr.N.G.P. Institute of Technology, Coimbatore, 641048, TamilnaduLivestock Farming and Bioresource Technology, Tamil Nadu
Palanisamy S.
Vellingiri B.
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Human Molecular Cytogenetics and Stem Cell Laboratory, Department of Human Genetics and Molecular Biology, Bharathiar University, Coimbatore, 641 046, Tamil NaduLivestock Farming and Bioresource Technology, Tamil Nadu