Trabectedin is a new marine-derived compound that binds the DNA minor groove and interacts with proteins of the DNA repair machinery. Phase I trials have established the standard regimen as 1500 μg/m2 24-hour continuous infusion repeated every 3 weeks. Several phase II trials have shown response in 5%–10% of unselected patients with soft tissue sarcoma failing prior chemotherapy and disease stabilisation in 30%–40%. Furthermore, prolonged disease control has been described in 15%–20% of patients. Toxicities are mainly haematological and hepatic with grade 3–4 neutropenia and thrombocytopenia observed in approximately 50% and 20% of patients respectively, and grade 3–4 elevation of liver enzymes observed in 35%–50% of patients treated with trabectedin. Current research focuses on the identification of predictive factors for patients with soft tissue sarcoma treated with trabectedin

Blay, Jean-Yves

Cassier, Philippe A

Dufresne, Armelle

Fayette, Jérôme

Therapeutics and Clinical Risk Management

English

PubMed

Philippe A Cassier1, Armelle Dufresne1, Jean-Yves Blay1,2,3, J&amp;eacute;r&amp;ocirc;me Fayette2,31Unit&amp;eacute; de Jour d&amp;rsquo;Oncologie M&amp;eacute;dicale Multidisciplinaire, H&amp;ocirc;pital Edouard Herriot, Lyon, France; 2D&amp;eacute;partement d&amp;rsquo;Oncologie M&amp;eacute;dicale, Centre L&amp;eacute;on B&amp;eacute;rard, Lyon, France; 3Unit&amp;eacute; INSERM 590, Equipe Cytokine et Cancer, Centre L&amp;eacute;on B&amp;eacute;rard, Lyon, FranceAbstract: Trabectedin is a new marine-derived compound that binds the DNA minor groove and interacts with proteins of the DNA repair machinery. Phase I trials have established the standard regimen as 1500 &amp;micro;g/m&amp;sup2; 24-hour continuous infusion repeated every 3 weeks. Several phase II trials have shown response in 5%&amp;ndash;10% of unselected patients with soft tissue sarcoma failing prior chemotherapy and disease stabilisation in 30%&amp;ndash;40%. Furthermore, prolonged disease control has been described in 15%&amp;ndash;20% of patients. Toxicities are mainly haematological and hepatic with grade 3&amp;ndash;4 neutropenia and thrombocytopenia observed in approximately 50% and 20% of patients respectively, and grade 3&amp;ndash;4 elevation of liver enzymes observed in 35%&amp;ndash;50% of patients treated with trabectedin. Current research focuses on the identification of predictive factors for patients with soft tissue sarcoma treated with trabectedin.Keywords: chemotherapy, sarcoma, drug development, DNA repai

Philippe A Cassier

Armelle Dufresne

Jean-Yves Blay

J&amp

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Trabectedin and its potential in the treatment of soft tissue sarcoma

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