TY - JOUR
T1 - Structure-activity relationship study of 16a-thiocamptothecins
T2 - An integrated in vitro and in silico approach
AU - Samorì, Cristian
AU - Beretta, Giovanni L.
AU - Varchi, Greta
AU - Guerrini, Andrea
AU - di Micco, Simone
AU - Basili, Serena
AU - Bifulco, Giuseppe
AU - Riccio, Raffaele
AU - Moro, Stefano
AU - Bombardelli, Ezio
AU - Zunino, Franco
AU - Fontana, Gabriele
PY - 2010/12/3
Y1 - 2010/12/3
N2 - The instability of the hydroxylactone E ring represents a critical drawback of camptothecins, because the lactone ring is recognized to be essential for stabilization of topoisomerase I-mediated DNA cleavage. In an attempt to investigate the effect of the thiopyridone pharmacophofore on the molecular and pharmacological features of the drug, we prepared a series of novel 16 a-thiocamptothecin analogues. Due to the sulfur atom, a destabilization of the hydrogen bond between the hydroxy group in position 17 of the opened E ring and the carbonyl of the pyridone moiety is predicted, thus shifting the equilibrium toward the closed lactone form and increasing the lipophilic properties of the compounds. This feature was associated with superior antiproliferative potency, with reduced interaction with the human serum albumin and with substantial increase of the persistence of the topoisomerase I-DNA cleavable complex. These effects were prominent for thio-SN38, the most active compound of the series. The favorable interactions at the molecular and cellular level of the reported thiocamptothecins confer promising features, and these compounds warrant preclinical development.
AB - The instability of the hydroxylactone E ring represents a critical drawback of camptothecins, because the lactone ring is recognized to be essential for stabilization of topoisomerase I-mediated DNA cleavage. In an attempt to investigate the effect of the thiopyridone pharmacophofore on the molecular and pharmacological features of the drug, we prepared a series of novel 16 a-thiocamptothecin analogues. Due to the sulfur atom, a destabilization of the hydrogen bond between the hydroxy group in position 17 of the opened E ring and the carbonyl of the pyridone moiety is predicted, thus shifting the equilibrium toward the closed lactone form and increasing the lipophilic properties of the compounds. This feature was associated with superior antiproliferative potency, with reduced interaction with the human serum albumin and with substantial increase of the persistence of the topoisomerase I-DNA cleavable complex. These effects were prominent for thio-SN38, the most active compound of the series. The favorable interactions at the molecular and cellular level of the reported thiocamptothecins confer promising features, and these compounds warrant preclinical development.
KW - Antitumor agents
KW - Camptothecins
KW - Cancer
KW - Structure-activity relationships
KW - Topoisomerase I
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U2 - 10.1002/cmdc.201000369
DO - 10.1002/cmdc.201000369
M3 - Article
C2 - 21069656
AN - SCOPUS:78651508219
SN - 1860-7179
VL - 5
SP - 2006
EP - 2015
JO - ChemMedChem
JF - ChemMedChem
IS - 12
ER -