Electrospray ion trap mass spectrometry of eight aminoglycoside antibiotics.

Mao-jin ZHOU; Da-fang ZHONG; Yu-ming SUN; Chang-xiao LIU

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Electrospray ion trap mass spectrometry of eight aminoglycoside antibiotics.

Author: Mao-jin ZHOU ¹ ; Da-fang ZHONG ; Yu-ming SUN ; Chang-xiao LIU
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1. Laboratory of Drug Metabolism and Pharmacokinetics, Shenyang Pharmaceutical University, Shenyang 110016, China.
Publication Type:Journal Article
MeSH: Aminoglycosides; analysis; chemistry; Gentamicins; analysis; chemistry; Molecular Structure; Spectrometry, Mass, Electrospray Ionization; methods; Tobramycin; analysis; chemistry
From: Acta Pharmaceutica Sinica 2004;39(10):826-830
CountryChina
Language:Chinese
Abstract:
AIMTo study the dissociation pathways of aminoglycoside antibiotics.
METHODSIn positive mode, eight aminoglycoside antibiotics were elucidated by use of electrospray ion trap mass spectrometry in the multi-stage MS full scan mode.
RESULTSIt was demonstrated that the eight aminoglycoside antibiotics gave abundant product ions at m/z 322 (gentamicin, micronomicin and sisomicin), m/z 350 (etimicin, netilmicin and vetilmicin) and m/z 324 (kanamycin and tobramycin) by loss of the C-ring (amino-alpha-D-glucopyranose) in MS2 full scan mode. In MS3 full scan mode, the prominent fragmentation ions at m/z 163 as well as m/z 191 were formed from the fragmentation ions at m/z 322, m/z 350 and m/z 324 by loss of the A-ring (amino-alpha-D-glucopyranose), separately, while the characteristic fragmentation ions at m/z 160 as well as m/z 162 were formed from m/z 322, m/z 350 and m/z 324 by loss of the B-ring (2-deoxy-D-streptamine), separately.
CONCLUSIONThe structural information was obtained via collision-activated dissociation and these characteristics are applicable to the structural elucidation and quantitative analysis of aminoglycoside compounds.