High-Affinity Small Molecule−Phospholipid Complex Formation: Binding of Siramesine to Phosphatidic Acid
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- 作者:Mikko J. Parry ; Juha-Matti I. Alakoskela ; Himanshu Khandelia ; Subramanian Arun Kumar ; Marja Jä ; ä ; ttelä ; Ajay K. Mahalka ; Paavo K. J. Kinnunen
- 刊名:Journal of the American Chemical Society
- 出版年:2008
- 出版时间:October 1, 2008
- 年:2008
- 卷:130
- 期:39
- 页码:12953-12960
- 全文大小:261K
- 年卷期:v.130,no.39(October 1, 2008)
- ISSN:1520-5126
文摘
Siramesine (SRM) is a σ−2 receptor agonist which has been recently shown to inhibit growth of cancer cells. Fluorescence spectroscopy experiments revealed two distinct binding sites for this drug in phospholipid membranes. More specifically, acidic phospholipids retain siramesine on the bilayer surface due to a high-affinity interaction, reaching saturation at an apparent 1:1 drug−acidic phospholipid stoichiometry, where after the drug penetrates into the hydrocarbon core of the membrane. This behavior was confirmed using Langmuir films. Of the anionic phospholipids, the highest affinity, comparable to the affinities for the binding of small molecule ligands to proteins, was measured for phosphatidic acid (PA, mole fraction of XPA = 0.2 in phosphatidylcholine vesicles), yielding a molecular partition coefficient of 240 ± 80 × 106. An MD simulation on the siramesine:PA interaction was in agreement with the above data. Taking into account the key role of PA as a signaling molecule promoting cell growth our results suggest a new paradigm for the development of anticancer drugs, viz. design of small molecules specifically scavenging phospholipids involved in the signaling cascades controlling cell behavior.