Photochemical reactions of substituted cyclopropenium salts.

Photochemical reactions of triphenylcyclopropenium tetrakis(pentafluorophenyl)gallate (TPCPGa) and diphenyl-(2-methoxy-1-naphthyl)-cyclopropenium tetrakis(pentafluorophenyl)gallate (DPMNCPGa) (Chart 1) have been investigated in acetonitrile. Traces of water were required for the photochemical reactions to proceed. The disappearance of both TPCPGa and DPMNCPGa obeys zero-order kinetics with rate constants (k) having a linear dependence on the concentration of water. Electron-transfer from water to the cyclopropenium cation is proposed as the primary process in the formation of the cyclopropenyl radical. The latter dimerizes leading to the photoproducts.

Photoreaction of platinum(II) beta-diketonate complexes with olefins.

Pt(hfac)(2) [hfac = 1,1,1,5,5,5-hexafluoro-2,4-pentanedionato] reacts with ethylene when irradiated at 350 nm to yield a single photoproduct which we have isolated for the first time. X-ray diffraction reveals this to be Pt(hfac)(2)(eta(2)-C(2)H(4)), a five coordinated complex, with two bidentate hfac ligands remaining intact. When Pt(hfac)(2) and ethylene were irradiated at 300 nm, a second product that could not be isolated was detected by (1)H NMR and (19)F NMR. Pt(hfac)(2)(eta(2)-C(2)H(4)) was also shown not to be stable at shorter wavelengths. The corresponding photoproducts of Pt(hfac)(2) with propene and of Pt(tfac)(2) [tfac = 1,1,1-trifluoro-2,4-pentanedionato] with ethylene were detected by (1)H NMR spectroscopy.

Photochemistry and photophysics of triarylmethane dye leuconitriles.

The photochemical reactions of crystal violet leuconitrile (CVCN) were investigated by the means of product analysis and trapping experiments, laser flash and steady-state photolysis, and steady-state fluorescence. The influence of oxygen on the reaction was examined in detail. The photochemistry of malachite green leuconitrile (MGCN), basic fuchsin leuconitrile (BFCN), and crystal violet leucomethyl (CVMe) and leucobenzyl (CVBn), as well as triphenylacetonitrile, was studied. The results suggest ionization occurs from S1, while the di-pi-methane reaction is the photochemical route from T1.

Characterization of iodonium salts differing in the anion.

The properties and reactivity of a series of iodonium salts with different anions were compared. The nucleophilicity of the anions in such compounds can be characterized by their melting points and NMR spectra. When using Quinaldine Red as indicator and CH3CN as solvent, the acid release rate of the iodonium salts correlated very well with their polymerization results in acid-sensitive epoxides.

Ion-induced manipulation of photochemical pathways in crown ether compounds based on fluorinated oligophenylenevinylenes: the border between ultrafast photoswitches and photoproduced nanomaterials.

The photochemical and photophysical properties of the crown ethers trans,trans-1,4-bis[2-(3',4'-benzo 15-crown 5)ethenyl]-2,3,5,6-tetrafluorobenzene (1) and trans,trans-1,4-bis[2-(3',4'-benzo 18-crown 6) ethenyl]-2,3,5,6-tetrafluorobenzene (2) were investigated in the absence and presence of groups I and II metal ions. The photophysical methods used include steady state flurescence, uv spectroscopy, and ultrafast transient absorption spectroscopy. Both compounds showed solvatochromic behavior, due to intramolecular charge transfer state formation, and efficient fluorescence in polar solvents. Photophysical behavior was dependent on the metal ion. The addition of metal ions that completely fit into the crown ether cavity resulted in significant blue shifts in the fluorescence emission spectra (chemosensing properties). Partially fitting ions changed the fluorescence spectra slightly. Transient absorption measurements revealed fast and slow decay components with time constants of 10-20 and 500-600 ps for all fitting ions, respectively. The latter is assigned to a trans-cis photoisomerization process, which decreased in efficiency in the presence of partially fitting ions, i.e., increasing ion size. Steady state irradiation showed clear evidence of a change in the absorption spectra. Trans-cis photoisomerization and [2 + 2] photocycloaddition were found to compete with fluorescence. The ions Li+, Na+, and Ca2+, which fit into the cavity, direct the photoisomerization. Larger ions (K+, Rb+, Sr2+ and Ba2+) that partially fit the cavity cause photocycloaddition. Quantum yields of the photoreaction are between 0.1 and 0.3. Analysis of the photo-product obtained for the 1-Sr2+ system revealed a compound with a molecular weight of nanosize dimension, which was equivalent to seven mass units of 1. The higher molecular weight product was formed due to alternately stacked supramolecular assemblies.

Synergistic activity of benzoyl peroxide and erythromycin.

BACKGROUND: Benzoyl peroxide (BP) is the most widely used topical agent for acne since its introduction in the 1960s. Concomitant topical treatment of BP and erythromycin is stated to be superior to BP alone. However, no synergistic activity has been found with this combination. Instead, such combination therapies are hypothesized to gain their efficacy by the coupled action of two effective treatments. The antibiotic kills all susceptible bacteria and the BP eliminates the resistant strains. OBJECTIVE: The purpose was to compare radical production by BP alone and with various antibiotics to determine whether certain antibiotics increase radical formation by BP, as the antibacterial activity of BP may correlate with the amount of radicals it forms. METHODS: Polymerization of tetraethylene glycol dimethacrylate was used as a test of BP radical activity. RESULTS: The results suggest that radical activity increases upon addition of certain antibiotics, such as erythromycin, to a solution of BP. CONCLUSION: Radical activity of BP in tetraethylene glycol dimethacrylate is increased when tested in consort with several antibiotics, such as the macrolides. We propose that the tertiary amines contained on certain antibiotics are responsible for catalysis of BP radical formation. If increased radical formation correlates with enhanced biological effect, then these data reveal the possibility of a biological synergism in mixtures of BP and antibiotics. An understanding of the mechanism of catalysis of BP radical formation by antibiotics may lead to the discovery of improved treatments for acne.

Pharmacological studies of arrhythmias induced by rose bengal photoactivation.

Singlet oxygen and superoxide production by rose bengal photoactivation leads to rapid electrophysiological changes and arrhythmias. To investigate which intermediate is causative and to probe possible mechanisms, hearts (n = at least 6/group) were perfused aerobically for 10 min without rose bengal followed by 5 min with rose bengal before illumination for 20 min. In controls, all or most hearts exhibited ventricular premature beats, ventricular tachycardia, and complete atrioventricular block. Most antioxidants tested had no protective effect; histidine, however, significantly delayed the onset of electrocardiographic (ECG) changes. In further studies, two antiarrhythmic agents (quinidine and verapamil) had no little protective effect, whereas R56865 significantly delayed the onset of ECG changes and reduced the incidence of arrhythmias. However, spectrophotometric and laser pulse radiolysis studies showed that this apparent protective effect might have resulted from an interaction between R56865 and the rose bengal molecule, leading to a reduction in singlet oxygen production. In conclusion, the electrophysiological changes induced by rose bengal photoactivation are likely to be due to singlet oxygen; antiarrhythmic drugs appear to be unable to protect against the injury unless there is some interaction with the photoactivation process.

Readily available fluorescein isothiocyanate-conjugated antibodies can be easily converted into targeted phototoxic agents for antibacterial, antiviral, and anticancer therapy.

Fluorescein-labeled antibodies have little, if any, photodynamic effect because energy acquired by light absorption is rapidly dissipated in fluorescence. However, they can be easily and efficiently converted to selective photodynamic sensitizers by iodination under mild conditions. We have outlined general experimental procedures that can be used to turn a fluorescein-labeled anti-Escherichia coli antibody into a photodynamic sensitizer that selectively kills E. coli while sparing closely related Salmonella typhimurium. These results demonstrate that iodination did not destroy the specificity or activity of the antibody. This technique should be applicable to the large number of fluoresceinated antibodies that are commercially available. Thus, this strategy provides a simple way to rapidly prepare a large number of targeted phototoxic agents that can be used for the selective destruction with light of nearly any type of tissue or organism.

Partition of rose bengal anion from aqueous medium into a lipophilic environment in the cell envelope of Salmonella typhimurium: implications for cell-type targeting in photodynamic therapy.

Photodynamic therapy employs photosensitizers for the selective destruction of tumor tissue while sparing the surrounding healthy tissue. Photosensitization may also be applied to the selective eradication of microorganisms. Photosensitized inactivation requires that the sensitizer bind to the target and therefore the factors that determine photosensitizer binding are critical to photosensitization selectivity. This paper reports the determination of some features of the binding site of the potent photosensitizer, Rose Bengal, in Salmonella bacteria and describes some of the factors that affect this binding. The shift in the wavelength of maximum fluorescence and experiments with the fluorescence quencher TNBS indicate that Rose Bengal is located in a non-aqueous compartment such as the outer membrane. The dye does not seem to significantly accumulate inside the cell, but rather to accumulate in the outer membrane. Time-dependent changes in sensitizer localization in two strains of Salmonella typhimurium that differ in cell wall formation, LT-2 and TA1975, correspond to their differences in susceptibility to photosensitized killing. Therefore these results provide clues to the factors that determine photosensitization selectivity. Understanding this phenomenon is essential for the efficient design of selective photosensitizers and for optimizing antitumor and antiviral photodynamic therapy.

Vasopressin: a model for the study of effects of additives on the oral and rectal administration of peptide drugs.

We previously observed, using a relatively primitive assay, that small oral doses (on the order of 1 microgram = 1 nmol = 1000 pmol per rat) of vasopressin can produce antidiuresis in hydrated rats, and that the oral activity was enhanced by simultaneous administration of an inhibitor of intestinal proteolysis. A more sensitive semi-automated computer-linked apparatus was used to conveniently and quickly compare the antidiuretic activities of the two natural and one synthetic vasopressin peptides by several routes of administration. (The approximate dose in pmol that resulted in a 50% decrease in urine flow is indicated in square brackets.) Intravenous lysine vasopressin was used as the benchmark dose [5]. Arginine and lysine vasopressin [3500], and the synthetic analogue, 1-deamino-8-D-arginine vasopressin (DDAVP) [20], were active by oral administration. The oral activities of arginine and lysine vasopressin were always enhanced by the simultaneous administration of aprotinin [1000], a natural inhibitor of trypsin; the effect of aprotinin on the oral activity of DDAVP was inconsistent. The vasopressins were more active when administered by the rectum: arginine vasopressin [20] and DDAVP [10]. The rectal activities of the peptides were increased by the absorption adjuvant, 5-methoxysalicylate (arginine vasopressin [10]; DDAVP [0.5]). The vasopressin peptides were also delivered by mouth in an impermeable coating of an azoaromatic cross-linked polymer, which is degraded by bacteria in the colon, to release the peptides in the upper colon for absorption (lysine vasopressin [525]).(ABSTRACT TRUNCATED AT 250 WORDS)

A new approach to the oral administration of insulin and other peptide drugs.

The oral administration of peptide drugs is well known to be precluded by their digestion in the stomach and small intestine. As a new approach to oral delivery, peptide drugs were coated with polymers cross-linked with azoaromatic groups to form an impervious film to protect orally administered drugs from digestion in the stomach and small intestine. When the azopolymer-coated drug reached the large intestine, the indigenous microflora reduced the azo bonds, broke the cross-links, and degraded the polymer film, thereby releasing the drug into the lumen of the colon for local action or for absorption. The ability of the azopolymer coating to protect and deliver orally administered peptide drugs was demonstrated in rats with the peptide hormones vasopressin and insulin.

Photophysical properties of rose bengal and its derivatives (XII).

We describe herein a series of new derivatives of tetrachloro tetraiodo (rose bengal) and report their emission and absorption characteristics. Photochemists and photobiologists may find several of these derivatives useful as alternative sources of singlet oxygen.