“Squalenoylcurcumin” Nanoassemblies as Water‐Dispersible Drug Candidates with Antileishmanial Activity

Curcumin, a natural polyphenolic compound, showed antiparasitic potential, including trypanocidal and leishmanicidal activity, in several in vitro and in vivo models. The molecule is well tolerated in humans. However, it is insoluble in water and displays poor oral bioavailability as a result of low absorption. New derivatives of curcumin were prepared by esterification of one or two of its phenolic groups with 1,1′,2‐tris‐norsqualenic acid. These “squalenoylcurcumins” were formulated as water‐dispersible nanoassemblies of homogeneous size, and they proved to be stable. Squalenoylcurcumins were inactive against Trypanosoma brucei brucei trypomastigotes, even as nanoassemblies, in contrast with curcumin. However, against Leishmania donovani promastigotes, the activities of the squalenoylcurcumins and their nanoassemblies were enhanced relative to that of curcumin. In L. donovani axenic and intramacrophagic amastigotes, they showed activity in the range of miltefosine, with good selectivity indexes. In regard to their dispersibility in water and to the safety of curcumin, these nanoassemblies are promising candidates for preclinical study toward the treatment of visceral leishmaniasis.     

Simple “On‐Demand” Production of Bioactive Natural Products

Exchange of the native promoter to the arabinose‐inducible promoter P_BAD was established in entomopathogenic bacteria to silence and/or activate gene clusters involved in natural product biosynthesis. This allowed the “on‐demand” production of GameXPeptides, xenoamicins, and the blue pigment indigoidine. The gene clusters for the novel “mevalagmapeptides” and the highly toxic xenorhabdins were identified by this approach.     

Evaluation of the Calmodulin‐SOX9 Interaction by “Magnetic Fishing” Coupled to Mass Spectrometry

Disruption of calmodulin (CaM)‐based protein interactions has been touted as a potential means for modulating several disease pathways. Among these is SOX9, which is a DNA binding protein that is involved in chrondrocyte differentiation and regulation of the hormones that control sexual development. In this work, we employed a “magnetic fishing”/mass spectrometry assay in conjunction with intrinsic fluorescence to examine the interaction of CaM with the CaM‐binding domain of SOX9 (SOX‐CAL), and to assess the modulation of this interaction by known anti‐CaM compounds. Our data show that there is a high affinity interaction between CaM and SOX‐CAL (27±9 nM ), and that SOX‐CAL bound to the same location as the well‐known CaM antagonist melittin; unexpectedly, we also found that addition of CaM‐binding small molecules initially produced increased SOX‐CAL binding, indicative of binding to both the well‐known high‐affinity CaM binding site and a second, lower‐affinity binding site.     

O6‐Alkylguanine‐DNA Alkyltransferase‐Mediated Repair of O4‐Alkylated 2′‐Deoxyuridines

O⁶‐Alkylguanine‐DNA alkyltransferases (AGTs) are responsible for the removal of O⁶‐alkyl 2′‐deoxyguanosine (dG) and O⁴‐alkyl thymidine (dT) adducts from the genome. Unlike the E. coli OGT (O⁶‐alkylguanine‐DNA‐alkyltransferase) protein, which can repair a range of O⁴‐alkyl dT lesions, human AGT (hAGT) only removes methyl groups poorly. To uncover the influence of the C5 methyl group of dT on AGT repair, oligonucleotides containing O⁴‐alkyl 2′‐deoxyuridines (dU) were prepared. The ability of E. coli AGTs (Ada‐C and OGT), human AGT, and an OGT/hAGT chimera to remove O⁴‐methyl and larger adducts (4‐hydroxybutyl and 7‐hydroxyheptyl) from dU were examined and compared to those relating to the corresponding dT species. The absence of the C5 methyl group resulted in an increase in repair observed for the O⁴‐methyl adducts by hAGT and the chimera. The chimera was proficient at repairing larger adducts at the O⁴ atom of dU. There was no observed correlation between the binding affinities of the AGT homologues to adduct‐containing oligonucleotides and the amounts of repair measured.     

Salt‐Controlled Selectivity in “on Water” and “in Water” Passerini‐Type Multicomponent Reactions

We have demonstrated that simple sodium salts can completely reverse the product ratios of the Passerini reaction in aqueous media. Furthermore, the use of the “salting‐in” salt and a small excess of the nucleophile gives significantly higher yields than the use of the saturated solution of the nucleophile alone.     

The Lab Oddity Prevails: Discovery of Pan‐CDK Inhibitor (R)‐S‐Cyclopropyl‐S‐(4‐{[4‐{[(1R,2R)‐2‐hydroxy‐1‐methylpropyl]oxy}‐5‐(trifluoromethyl)pyrimidin‐2‐yl]amino}phenyl)sulfoximide (BAY 1000394) for the Treatment of Cancer

Lead optimization of a high‐throughput screening hit led to the rapid identification of aminopyrimidine ZK 304709, a multitargeted CDK and VEGF‐R inhibitor that displayed a promising preclinical profile. Nevertheless, ZK 304709 failed in phase I studies due to dose‐limited absorption and high inter‐patient variability, which was attributed to limited aqueous solubility and off‐target activity against carbonic anhydrases. Further lead optimization efforts to address the off‐target activity profile finally resulted in the introduction of a sulfoximine group, which is still a rather unusual approach in medicinal chemistry. However, the sulfoximine series of compounds quickly revealed very interesting properties, culminating in the identification of the nanomolar pan‐CDK inhibitor BAY 1000394, which is currently being investigated in phase I clinical trials.     

Interrogation of “surface,” “skin,” and “core” orientation in thermotropic liquid‐crystalline copolyester moldings by near‐edge X‐ray absorption fine structure and wide‐angle X‐ray scattering

Injection molding thermotropic liquid‐crystalline polymers (TLCPs) usually results in the fabrication of molded articles that possess complex states of orientation that vary greatly as a function of thickness. “Skin‐core” morphologies are often observed in TLCP moldings. Given that both “core” and “skin” orientation states may often differ both in magnitude and direction, deconvolution of these complex orientation states requires a method to separately characterize molecular orientation in the surface region. A combination of two‐dimensional wide‐angle X‐ray scattering (WAXS) in transmission and near‐edge X‐ray absorption fine structure (NEXAFS) spectroscopy is used to probe the molecular orientation in injection molded plaques fabricated from a 4,4′‐dihydroxy‐α‐methylstilbene (DHαMS)‐based thermotropic liquid crystalline copolyester. Partial electron yield (PEY) mode NEXAFS is a noninvasive ex situ characterization tool with exquisite surface sensitivity that samples to a depth of 2 nm. The effects of plaque geometry and injection molding processing conditions on surface orientation in the regions on‐ and off‐ axis to the centerline of injection molded plaques are presented and discussed. Quantitative comparisons are made between orientation parameters obtained by NEXAFS and those from 2D WAXS in transmission, which are dominated by the microstructure in the skin and core regions. Some qualitative comparisons are also made with 2D WAXS results from the literature. © 2007 Wiley Periodicals, Inc. J Appl Polym Sci 2007     

Synthesis of NR‐g‐PMMA by “grafting from” method using ATRP process

Grafting poly(methyl methacrylate) or PMMA from natural rubber (NR) using ATRP process, NR has to be transformed into bromoalkyl‐functionalized NR (NRBr) acting as ATRP macroinitiator. The NRBr was prepared by two‐step chemical modification i.e., epoxidation and epoxide ring opening reaction using a nucleophile containing bromine atom such as 2‐bromopropionic acid ( A1 ) and 2‐bromo‐2‐methylpropionic acid ( A2 ). The fixation of A1 and A2 on 4‐methyl‐4‐octene, a model representing one repeat unit of NR, modified by epoxidation was prior studied and it was found that the resulting addition products from A2 using as ATRP initiator for MMA gave a better control of M _n,exp and low PDI of PMMA than that from A1 . Then, the NR was transformed into ATRP rubber macroinitiator via epoxidation, followed by epoxide ring addition with only A2 . ¹H NMR was employed to determine the amount of A2 addition units on NR, which is considered to be the same amount of grafting sites for ATRP of MMA. The grafting of PMMA was then successfully carried out from the NR backbone by ATRP process. The PMMA grafts of the NR‐g‐PMMA were indeed linked to the NR backbone via ester linkage of the A2 unit. The PMMA grafts could be cleaved from the NR backbone by acid hydrolysis, while PMMA grafting by other conventional radical reaction could not be done. Then, the average MW of PMMA grafts after separation using acetone extraction was evaluated. © 2011 Wiley Periodicals, Inc. J Appl Polym Sci, 2011     

Theory of “Cohesive” vs “Adhesive” Separation in an Adhering System

It is shown that there is limited validitity to the doctrine that true interfacial separation, in an adhering system, is highly improbable. An analysis employing the Griffith-Irwin crack theory yields these results: The important parameters are, difference in elastic moduli, ΔE; differences in g, the energy dissipation per unit crack extension; thickness, Δ₁ or δ₂, of the region where dissipation occurs; and the presence or absence of strong interfacial bonds. If the forces across the interface are appreciably weaker than the cohesive forces in either phase, there is a strong minimum in g at the interface. For flaws of equal size, an interfacial flaw will be the site of initiation of failure. If strong interfacial bonds are present, then if Δg and ΔE have the same sign, failure is most probable, deep within one phase. If Δg and ΔE have opposite signs, failure may be initiated, and may propagate, at a distance δ from the interface, in the phase with lower g. This may be mistaken for weak-boundary layer failure.     

A Fluorescent “Allosteric Scorpionand” Complex Visualizes a Biological Recognition Event

We describe a new class of fluorescent reporter and its employment to visualize the biotin/avidin binding interaction. Derivatives of the azamacrocycle cyclam that contain a pendant naphthalimide dye are inherently fluorescent when zinc(II) is coordinated. Introducing a second pendant group—biotin—affords an unsymmetrical bis‐triazole‐scorpionand ligand that interacts specifically with avidin. This ligand has been assembled by using a one‐pot “double‐click” strategy and complexed with copper(II) and zinc(II). The zinc(II) complex is fluorescent, and its fluorescence output changes in the presence of avidin. Upon avidin binding, the fluorescence output is diminished by interaction with the protein, at [complex]/[avidin] ratios of up to 4:1. The observed change might arise from a specific quenching effect in the biotin binding pocket or from a binding‐induced change in the coordination geometry of the complex.     

Let's call it “color‐gamut rendering”

The term “color gamut” historically has been associated with color output such as optimal color stimuli and additive and subtractive imaging systems. Recently, this term has been used with input devices such as scanners and digital cameras. It is proposed that the term “color‐gamut rendering” should be used instead of input devices. This clarifies the distinction between input (analysis) and output (synthesis) color systems in terms of the effect of an input system on defining the colorimetric properties of an output system. © 2007 Wiley Periodicals, Inc. Col Res Appl, 32, 334–335, 2007