Synthesis of a [3H]-labelled derivative of the microtubular poison taxol

## Abstract 7‐Trietylsilylbaccatin III (11) was coupled with cis‐1‐benzoyl‐3‐triethylsiloxy‐4‐(3′‐bromophenyl)azetidin‐2‐one. Hydrolysis of the silyl groups gave 3″‐bromotaxol which was reduced with tritium gas to give[3″‐^3^H]taxol with specific activity of 19.3 Ci mmol. Reduction of 7‐triethylsil

The s y n t h e s i s o f a new a c e t y l e n i c a n a l o g u e o f t h e C-t e r m i n a l hep t ap ep t i de segment o f c h o l e c y s t o k i n i n ( C C K ) i n which t h e Met28 and Met31 r e s i d u e s a r e r e p l a c e d by two a c e t y l e n i c p r e c u r s o r s o f n o r l e u

The 4gnth-i~ o{ e n d a p d d e a t e (RK 4211 La- beUed w i t h t/tltiwn at ih p o L i n e iuhg u d ~a i b e d . ih, M e f f ' -~~o x p u c c m m u + l wten o t a N-cwtboxyaLh# & m i n e d d v a t i v e IUM aeac-Led w i t h L-[4,5-H J p o 4 i n e and M e urude neac- .tion mixtcute fneaked w i t h d

[3H]Tetrodotoxin [( 3H]TTX) and a [3H]ethylenediamine derivative of TTX are the most widely used ligands for the study of the Na channel. The former ligand presents a low specific radioactivity (1 Ci/mmol) while the latter is highly labeled (30 Ci/mmol). However, its two-step synthesis, i.e., mild o