2009
DOI: 10.1007/s00726-009-0429-2
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Metabolism of N-alkylated spermine analogues by polyamine and spermine oxidases

Abstract: SUMMARYN-alkylated polyamine analogues have potential as anticancer and antiparasitic drugs. However, their metabolism in the host has remained incompletely defined thus potentially limiting their utility. Here, we have studied the degradation of three different spermine analogues N, N′-bis-(3-ethylaminopropyl)butane-1,4-diamine (DESPM), N-(3-benzyl-aminopropyl)-N'-(3-ethylaminopropyl)butane-1,4-diamine (BnEtSPM) and N,N′-bis-(3-benzylaminopropyl)butane-1,4-diamine (DBSPM) and related mono-alkylated derivative… Show more

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Cited by 19 publications
(16 citation statements)
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References 47 publications
(88 reference statements)
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“…This is consistent with previous observations reported in the literature. 3,11,18) Based on these results, N The rate of spermidine production rapidly decreased with time, indicating that the enzyme became progressively more inactivated. The apparent molar proportions of spermidine to APAO were approximately 60 and 80 for N 1 -and N 8 -butadienyl Spd, respectively, which were calculated by extrapolating to the point of complete inactivation.…”
Section: Synthesis Of Nmentioning
confidence: 83%
“…This is consistent with previous observations reported in the literature. 3,11,18) Based on these results, N The rate of spermidine production rapidly decreased with time, indicating that the enzyme became progressively more inactivated. The apparent molar proportions of spermidine to APAO were approximately 60 and 80 for N 1 -and N 8 -butadienyl Spd, respectively, which were calculated by extrapolating to the point of complete inactivation.…”
Section: Synthesis Of Nmentioning
confidence: 83%
“…They may act by directly inducing SMO, which is highly responsive to many analogs, and thus reduce spermine and increase ROS (48, 60, 229), by metabolism generating toxic metabolites via SMO or the SSAT/APAO pathways (60, 237) or by additional mechanisms such as blocking binding of polyamines to key sites for normal effects on growth, interfering with polyamine-mediated cell signaling (238) or by acting on the cytoskeleton (230). It should also be noted that the potential of polyamine analogs for therapeutic use is not limited to cancer therapy.…”
Section: Polyamine Analogs and Derivatives As Research Tools And mentioning
confidence: 99%
“…More importantly, the stereospecificity of APAO is changed by supplementing either benzaldehyde (R-activating) or pyridoxal (S-activating) with racemic 1methylspermidine as a substrate [12]. Furthermore, we have characterized earlier the preferred catabolic pathways of symmetrically substituted Spm analogues DESpm and N 1 ,N 12 -dibenzylspermine (DBSpm, N,N'-bis-(3-benzyl-aminopropyl)butane-1,4-diamine) (Figure 1), and unsymmetrically substituted N 1 -benzyl-N 12 -ethylspermine (BnEtSpm, N-(3-benzyl-aminopropyl)-N'-(3-ethylaminopropyl)butane-1,4-diamine) by APAO and SMOX [14]. As protium-deuterium exchange could be used to redirect oxidative metabolism mediated via hydrogen abstraction [1], we synthesized a set of selectively deuterated polyamine analogues ( Figure 1) for a proof-of-concept study to alter the catabolic pathways of synthesized analogues and to study the impact of targeted deuteration on the analogues' biological efficacy.…”
Section: Introductionmentioning
confidence: 99%