The mass spectra of 1,6-dibromo-1,6-dideoxyhexitols

Aspects of the biological transport of cytostatically active 1,6-dibronio-l,6-dideoxydulcitol ( D B D ) were studied using "Br-labelled material on dogs and Yoshida tuniorbearing rats. Thirty-five per cent of the DBD dose was excreted in the urine within 12 hours. Besides unchanged DBD, metabolites

## Abstract Under electron impact, 6‐thiotheophyllines eliminate various fragments from the pyrimidine moiety. In a retro Diels‐Alder reaction, they lose the fragment XCNCH~3~ from positions 1 and 2 of the pyrimidine ring. In 6‐sulfinyltheophyllines, the sulfinyl group is the main target for frag

Fragmentation pathways of the title compounds under electron impact were compared to those of their (1aryl)substituted analogs reported earlier. The main fragmentation route of the M Á ions is the sulphamide N-S bond cleavage leading to [M À ArSO 2 ] ions. No loss of the alkyl substituents from the

Fragmentation pathways of the title compounds were studied using accurate mass measurements and collision-induced dissociation spectra. Substituents in the ortho position of the aryl group at the pyrimidine ring were found to play a special role in the electron impact (EI) induced fragmentation of t