par Kulvik, Martti;Färkkilä, Markus;Kallio, Merja;Vähätalo, Jyrki;Buchar, Evzen;Järviluoma, Eija;Rasilainen, Merja;Jääskeläinen, Juha;Křiž, Otomar;Laakso, Juha 
;Ruokonen, Inkeri
Référence European journal of pharmaceutical sciences, 18, 2, page (155-163)
Publication Publié, 2003-02
;Ruokonen, InkeriRéférence European journal of pharmaceutical sciences, 18, 2, page (155-163)
Publication Publié, 2003-02
Article révisé par les pairs
| Résumé : | Boron neutron capture therapy (BNCT) is an experimental therapeutic modality combining a boron pharmaceutical with neutron irradiation. 4-Dihydroxyborylphenylalanine (L-BPA) synthesised via the asymmetric pathway by Malan and Morin [Synlett. 167-168 (1996)] was developed to be the boron containing pharmaceutical in the first series of Finnish BNCT clinical trials. The final product was >98.5% chemically pure L-BPA with L-phenylalanine and L-tyrosine as the residual impurities. The solubility of L-BPA was enhanced by complex formation with fructose (BPA-F). The pH and osmolarity of the BPA-F preparation is in the physiological range. Careful attention was given to the pharmaceutical quality of the BPA-F preparations. Prior to starting clinical trials the acute toxicity of L-BPA was studied in male albino Sprague-Dawley rats. In accordance with earlier studies no adverse effects were observed. After completion of the development work L-BPA solution was administered to brain tumour patients in conjunction with clinical studies for development and testing of BPA-based BNCT. No clinically significant adverse events attributable to the L-BPA i.v. infusions were observed. We conclude that our synthesis development, complementary preclinical and clinical observations justify the safe use of L-BPA up to clinical phase III studies with L-BPA produced by the asymmetric pathway, originally presented by Malan and Morin in 1996. © 2002 Elsevier Science B.V. All rights reserved. |
