Studies on the photophysical characteristics of poly(carboxylic acid)s bound protoporphyrin IX and metal complexes of protoporphyrin IX

The copolymers of methacrylic acid with protoporphyrin IX (PPIX) and the metal complexes, zinc protoporphyrin IX and magnesium protoporphyrin IX were synthesised and characterised. Corresponding acrylic acid copolymers were also synthesised. The steady state absorption and fluorescence spectral properties of the macromolecular bound fluorophores PPIX, Zn-PPIX and Mg-PPIX were investigated. Poly(methacrylic acid) bound protoporphyrin IX, zinc protoporphyrin IX and magnesium protoporphyrin IX show an increase in the fluorescence intensity and lifetime with increase in the pH in the range 2-8 with a marked transition around pH 6.0-7.0. The fluorophore concentration in the dilute solution of the copolymers is micromolar and the fluorophore to the carboxylic acid monomer ratios in the copolymer is around 10⁻³. The molecular weight of the copolymers is 100 ± 10 kD. The fluorescence decay curves of all the fluorophore bound polymers follow biexponential decay fit independent of pH. Poly(MAA-co-PPIX) and poly(MAA-co-MgPPIX) undergo well marked pH induced structural transitions in the pH range of 6.0-7.0 whereas poly(MAA-co-ZnPPIX) undergoes pH induced structural transitions in the pH range of 4.0. In the case of polyacrylic acid copolymers the changes observed in the steady state and time resolved fluorescence studies are less marked. The distinct hydrophobic and hydrophilic environments experienced by the fluorophore bound to PMMA are attributed to the dynamics of the macromolecules in dilute aqueous solutions manifested by the α-methyl group present in the copolymer. The studies carried out using the fluorophores in the time windows from 2 ns to 12 ns indicate evolving trends in the dynamic coiling and reverse coiling of poly methacrylic acid chain.     

Preparation and photochemistry of macromolecular bound ruthenium(II) complexes in aqueous solutions

Ruthenium(II) polypyridyl complexes with macromolecular ligands poly(methylolacrylamide-co-vinylpyridine) and poly (acrylamide-co-vinylpyridine) have been synthesized. The macromolecular ruthenium (II) complexes which are soluble in water have been characterized and their absorption and emission properties have been studied in aqueous solution. Photolysis of the complex in aqueous solution leads to photoaquation reactions with release of coordinated pyridines of the polymer. In the case of monomeric complex, cis-[Ru(bpy)₂(py)₂]Cl₂, photolysis in water in presence of Cl^? ions produces only the substitution of the pyridine by water whereas in the polymeric complexes, [Ru(bpy)₂(MAAM-co-VP)₂]Cl₂ photolysis in the presence of chloride produces [Ru(bpy)₂(MAAM-co-VP)Cl]Cl and [Ru(bpy)₂(AM-co-VP)Cl]Cl, respectively. Quantum yields for the photosubstitution reactions have been determined and mechanistic details are outlined.     

First observation in the gas phase of the ultrafast electronic relaxation pathways of the S(2) states of heme and hemin

The time evolution of electronically excited heme (iron II protoporphyrin IX, [Fe(II) PP]) and its associated salt hemin (iron III protoporphyrin IX chloride, [Fe(III) PP-Cl]), has been investigated for the first time in the gas phase by femtosecond pump-probe spectroscopy. The porphyrins were excited at 400 nm in the S(2) state (Soret band) and their relaxation dynamics was probed by multiphoton ionization at 800 nm. This time evolution was compared with that of the excited state of zinc protoporphyrin IX [Zn PP] whose S(2) excited state likely decays to the long lived S(1) state through a conical intersection, in less than 100 fs. Instead, for [Fe(II) PP] and [Fe(III) PP-Cl], the key relaxation step from S(2) is interpreted as an ultrafast charge transfer from the porphyrin excited orbital π* to a vacant d orbital on the iron atom (ligand to metal charge transfer, LMCT). This intermediate LMCT state then relaxes to the ground state within 250 fs. Through this work a new, serendipitous, preparation step was found for Fe(II) porphyrins, in the gas phase.     

Novel interactions between different molecules bound to the same macromolecular chain

The complex of thionine and ruthenium(II) bipyridyl complex has been attached as pendants to poly(methylolacrylamide-co-vinylpyridine). Interaction between the two dyes, mediated by the macromolecular chain, has been observed.     

Studies on interpolymer self-organisation behaviour of protoporphyrin IX bound poly(carboxylic acid)s with complimentary polymers by means of fluorescence techniques

Covalently bound protoporphyrin IX was used as a fluorophore to investigate the interpolymer complex formation between the poly(carboxylic acid)s, PMAA/PAA and poly(N-vinyl pyrrolidone), PVP, poly(ethylene oxide), PEO or poly(ethylene glycol), PEG. Absorption and emission spectral properties of protoporphyrin IX bound to PAA, PMAA and PVP have been studied. Protoporphyrin IX in poly(MAA-co-PPIX) was found to be present in the dimer or higher aggregated form at low pH due to the environmental restriction imposed by the polymer whereas in the case of poly(AA-co-PPIX) and poly(VP-co-PPIX), PPIX exists in monomeric form. The fluorescence intensity and lifetime of PPIX bound to poly(carboxylic acid)s increase on complexation through hydrogen bonding with PVP, PEO and PEG due to the displacement of water molecules in the vicinity of the PPIX. Poly(MAA-co-PPIX) shows longer fluorescence lifetime due to the more compact interpolymer complexation as compared to poly(AA-co-PPIX) due to the enhanced hydrophobicity of PMAA. Poly(VP-co-PPIX) shows a decrease in the fluorescence lifetime on complexation with PMAA or PAA due to the hydrophilic and microgel like environment of the fluorophore bound to PVP. The contrasting behaviour of the same polymer adduct with respect to the site of the fluorophore is interpreted to be due to the solvent structure which determines the environment of the fluorophore.     

Self-assembly of highly ordered Peptide amphiphile metalloporphyrin arrays

Long fibers assembled from peptide amphiphiles capable of binding the metalloporphyrin zinc protoporphyrin IX ((PPIX)Zn) have been synthesized. Rational peptide design was employed to generate a peptide, c16-AHL(3)K(3)-CO(2)H, capable of forming a β-sheet structure that propagates into larger fibrous structures. A porphyrin-binding site, a single histidine, was engineered into the peptide sequence in order to bind (PPIX)Zn to provide photophysical functionality. The resulting system indicates control from the molecular level to the macromolecular level with a high order of porphyrin organization. UV/visible and circular dichroism spectroscopies were employed to detail molecular organization, whereas electron microscopy and atomic force microscopy aided in macromolecular characterization. Preliminary picosecond transient absorption data are also reported. Reduced hemin, (PPIX)Fe(II), was also employed to highlight the material's versatility and tunability.     

Grafting of light‐activated antimicrobial materials to nylon films

Protoporphyrin IX and zinc protoporphyrin IX were grafted to the surface of nylon‐6,6 films via an ethylene diamine bridge and a poly(acrylic acid) (PAA) scaffold. X‐ray photoelectron spectroscopy showed that approximately 57% of the nylon surface was covered by PAA and approximately 6% of the carboxylic acid groups in PAA were grafted to the ethylene diamine derivative of protoporphyrin IX or its zinc salt. © 2002 Wiley Periodicals, Inc. J Polym Sci Part A: Polym Chem 41: 41–47, 2003     

A Review of: “Pharmaceutical Applications of Membrane Sensors by Vasile V. Cosofret and Richard P. Buck CRC Press,Inc., Boca Raton,Florida, U.S.A. 1992, x+431pp. US$95.00/Outside US$114.00, ISBN:0-8493-4406-9”

ABSTRACT

The analytical performance of two modified electrodes (a tyrosinase biosensor and a glassy carbon electrode (GCE) covered with poly[Ni-(protoporphyrin IX)dimethyl ester]) in comparison with the bare electrode has been evaluated in a flow injection system using standard solutions of oleuropein and olive oil samples. The tyrosinase biosensor appeared to be an appropriate device for the selective determination of phenols, moreover it can be easily incorporated in an on-line system. This method was used to evaluate the stability of the samples.     

Syntheses and reactions of porphyrin and metalloporphyrin polymers

Various porphyrin functions such as protoporphyrin IX and chlorin a as well as metalloporphyrin functions such as Mg(II)– and Cu(II)–chlorophyllin a and Fe(III)– and Co(II)–protoporphyrin IX were incorporated into vinyl polymers by preparation and polymerization of their p-vinylbenzyl esters. The porphyrin function was also incorporated by reaction of poly-p-chloromethylstyrene with porphyrins or metalloporphyrins or by the reaction of p-aminostyrene polymers with chlorophyll b through Schiff-base formation. Mg(II)–porphyrin polymers were found to be remarkably effective as catalysts in photoredox systems; porphyrin polymers without central metal atoms were also effective to a lesser extent.     

Liver-targeting macromolecular MRI contrast agents

Macromolecular ligands with liver-targeting group (pyridoxamine, PM) PHEA-DTPA-PM and PAEA-DTPA-PM were prepared by the incorporation of different amount of diethylenetria-minepentaacetic acid monopyridoxamine group (DTPA-PM) into poly-cc, p-[N-(2-hydroxyethyl)-L-aspartamide] (PHEA) and poly-α, β-[N-(2-aminoethyl)-L-aspartamide] (PAEA). The macromolecular ligands thus obtained were further complexed with gadolinium chloride to give macromolecular MRI contrast agents with different Gd(Ⅲ) contents. These macromolecular ligands and their gadolinium complexes were characterized by 1H NMR, 1R, UV and elementary analysis. Relaxivity studies showed that these polyaspartamide gadolinium complexes possess higher relaxation effectiveness than that of the clinically used Gd-DTPA. Magnetic resonance imaging of the liver in rats and experimental data of biodistribution in mice indicate that these macromolecular MRI contrast agents containing pyridoxamine exhibit liver-targeting property.     

Polypyridine block as molecular antenna in photoluminescence of macromolecular systems

Unique effects of π-conjugated polypyridine (PPy) blocks on fluorescence from the following macromolecular systems have been examined: (A) poly(2,2′-bipyridine-5,5′-diyl) (PBpy)-Ru(bpy)₂, (b) block-type copolymer of pyridine and selenophene, and (c) a system containing poly(6-hexylpyridine-2,5-diyl) (6HexPy) and poly(2-methylanthraquinone-1,4-diyl) (P2MeAQ). The PPy blocks in the systems serve as good molecular antennas and transfer the photoactivated energy to other molecular parts of the systems connected to the PPy blocks, thus causing emission of light from the other molecular parts.     

Functional and site-specific macromolecular micelles as high potential drug carriers

Since several years, macromolecular micelles based on amphiphilic block copolymers have attracted much interest as drug carriers. These micelles show a long term blood circulation time resulting from their small diameter and the steric repulsion created by the poly(ethylene oxide) chains which constitute micelle corona, as well as from their high thermodynamic stability. Besides this long term blood circulation time generating a passive targeting, an active targeting, chemical or physical affinity targeting, might allow the preparation of more efficient drug carriers. In order to obtain such double targeting properties, we have prepared two kinds of macromolecular micelles. The first one is based on amphiphilic poly(ethylene oxide)/poly(β-benzyl -aspartate) ---PEO/PBLA--- block copolymers having hydroxy groups at the free end of PEO chains. As a result of their structure, such micelles have hydroxy groups on their outer-shell which can be further modified in order to introduce a targeting moiety (sugar, etc.). The characteristics (diameter, critical micellar concentration (cmc), drug loading capacity) have been determined. Moreover, doxorubicin loaded -hydroxy PEO/PBLA micelles have been shown to be slightly more cytotoxic than the corresponding -methoxy PEO/PBLA micelles. The second type of micelles is based on thermosensitive amphiphilic poly(N-isopropyl acrylamide)/polystyrene ---PIPAAm/PSt--- block copolymers. Such micelles have a small diameter and a low cmc in addition to thermosensitivity properties which are similar to those of PIPAAm.     

Spin trapping reactions with nitric oxides. V. Reactions with unsaturated macromolecular chains - a new spin labeling method

Formation of macromolecular nitroxides (i.e., spin labeled polymer chains) has been detected by Electron Spin Resonance spectroscopy in the reaction of nitric oxide gas with several unsaturated polymers/synthetic polyisoprene, polybutadiene , poly(isoprene-co-isobutylene), poly(butadiene-co-styrene)/dissolved in aromatic hydrocarbons. Spectroscopic evidences of gel formation, precipitation, and of solvent effect have been given.     

Coordination Studies of Iron(II) Protoporphyrin IX and Iron(II) Hematoporphyrin IX with 4,4′-Dipyridyl and other Nitrogenous Bases

Abstract

The results of spectral studies of iron(II) protopor-phyrin IX and iron(II) hematoporphyrin IX with several substituted pyridines are reported. The existence in solution of an iron(II) porphyrin complex coordinated to a water molecule and to a substituted pyridine was shown by isolation of the complex from solution. The complex isolated was dimeric inono-4,4′-dipyridyl diaquo iron(II) hematoporphyrin. Addition of ethanol to the aqueous solvent inhibits coordination of iron(II) porphyrins with substituted pyridines. The protoporphyrin ring enhances coordination relative to the hematoporphyrin ring.     

Targeting of sebocytes by aminolevulinic acid-dependent photosensitization

Photodynamic therapy using 5-aminolevulinic acid-induced protoporphyrin IX has been developed as a very useful therapeutic modality. Recently, several authors have reported on the efficacy of this procedure for acne. This approach is based on the fact that 5-aminolevulinic acid-induced protoporphyrin IX has strong selectivity for sebaceous glands. We used the immortalized human sebaceous gland cell line SZ95 to investigate cellular mechanisms of photodynamic therapy using 5-aminolevulinic acid-induced protoporphyrin IX. Quantification of induced protoporphyrin IX production showed dependence on the applied 5-aminolevulinic acid dose. When SZ95 sebocytes were differentiated by arachidonic acid treatment, there was no difference between them and the control cells with respect to both the amount of 5-aminolevulinic acid-induced protoporphyrin IX and the phototoxic effects. We altered protoporphyrin IX formation rates by growing cells scattered as single cells in the culture dishes. Single cells produced significantly lower protoporphyrin IX levels than those grown with intercellular contacts. Intracellular localization of protoporphyrin IX was imaged using confocal laser scanning microscopy. The differentiation-specific lipid droplets were virtually excluded from protoporphyrin IX fluorescence. In addition to weak mitochondrial and strong membrane fluorescence, distinctive spots with strong fluorescence were observed. These did not colocalize with fluorescent probes for mitochondria, lysosomes or the Golgi apparati.     

New π‐stacked benzofulvene polymer showing thermoreversible polymerization: Studies in macromolecular and aggregate structures and polymerization mechanism

The macromolecular and aggregate structures of poly[ethyl 1‐methylene‐3‐(4‐methylphenyl)‐1H‐indene‐2‐carboxylate] (poly‐ BF1 ; a new polymer based on a functionalized benzofulvene moiety showing interesting properties, i.e., thermoreversible polymerization/depolymerization behavior, high solubility in the most common organic solvents, and susceptibility to molecular manipulation) have been investigated with NMR spectroscopy, absorption and emission spectrophotometry, and transmission electron microscopy (TEM). Moreover, the polymerization mechanism has been studied to obtain further information on the polymer structure. The collected evidence is consistent in indicating for poly‐ BF1 a vinyl (1,2) polymer structure stabilized by means of aromatic stacking interactions. Furthermore, TEM studies performed on metal replicas have shown that the polymer is liable to give nanostructured aggregates. © 2005 Wiley Periodicals, Inc. J Polym Sci Part A: Polym Chem 43: 3289–3304, 2005     

Synthesis and characterization of a novel macromolecular surface modifier for polyethylene

A new macromolecular surface modifier, a copolymer of lauryl methacrylate (LMA) and poly(ethylene glycol) methyl methacrylate (PEGMA), was synthesized through free radical polymerization. The copolymer was characterized by nuclear magnetic resonance spectrum (1H-NMR) and thermogravimetric analysis (TGA). The copolymer was used to blend with polyethylene. The binary blends have been characterized by attenuated total reflection/Fourier transform infrared (ATR-FTIR), contact-angle measurements (CDA) and scanning electron microscopy (SEM). The results indicated that poly(ethylene glycol) methyl methacrylate-co-lauryl methacrylate (PEGMA-co-LMA) could diffuse preferably onto the surface of the polyethylene (PE) film, and thus can be used as an efficient surface modifier for PE.     

Graft copolymerization of anhydro sugar derivatives from macromolecular halides

Cationic graft copolymerizations of bicyclic acetals, 1,6-anhydro-2,3,4-tri-O-benzyl-β-D -glucopyranose (LGTBE) and 1,6-anhydro-2,3,4-tri-O-methyl-β-D -glucopyranose (LGTME), were investigated with macromolecular carbenium ions formed from polymers that contain reactive halogens. Macromolecular complex catalysts formed from chlorosulfonated polyethylene or poly(isoprene-co-chloromethylstyrene) by the action of phosphorus pentafluoride yielded graft copolymers with low proportions (0.6–16%) of poly(LGTBE) or poly(LGTBE-co-epichlorohydrin) branchings. It was found that macromolecular complex catalysts formed from poly(styrene-co-fluoromethylstyrene) or poly(methyl methacrylate-co-fluoromethylstyrene) by the action of boron trifluoride etherate give graft copolymers with high proportions (up to 80%) of poly(LGTBE) or poly(LGTME) branchings. In addition, the model reactions for the graft copolymerization of LGTBE were examined with organic halide-PF₅, organic halide-AgPF₆, and organic fluoride-BF₃·OEt₂ catalytic systems, of which the last two indicate that the polymerization is effected by a carbenium ion mechanism.     

Synthesis of protoheme IX derivatives with a covalently linked proximal base and their human serum albumin hybrids as artificial hemoprotein

The simple one-pot reaction of protoporphyrin IX and omega-(N-imidazolyl)alkylamine or O-methyl-L-histidyl-glycine with benzotriazol-1-yl-oxytris(dimethylamino)phosphonium hexafluorophosphate at room temperature produced a series of protoporphyrin IX species with a covalently linked proximal base at the propionate side-chain. The central iron was inserted by the general FeCl2 method, converting the free-base porphyrins to the corresponding protoheme IX derivatives. Mesoporphyrin IX and diacetyldeuteroporphyrin IX analogues were also prepared by the same procedure. The Fe(II) complexes formed dioxygen (O2) adducts in dimethylformamide at 25 degrees C. Some of them were incorporated into the hydrophobic domain of recombinant human serum albumin (rHSA), providing albumin-heme hybrids (rHSA-heme), which can bind and release O2 in aqueous media (pH 7.3, 25 degrees C). The oxidation process of converting the dioxygenated heme in rHSA to the inactive Fe(III) state obeyed first-order kinetics, indicating that the mu-oxo dimer formation was prevented by the immobilization of heme in the albumin scaffold. The rHSA-heme, in which the histidylglycil tail coordinates to the Fe(II) center, showed the most stable O2 adduct complexes.     

EFFECTS OF N-PHENYLIMIDE S-23142 AND N-METHYL MESOPORPHYRIN IX ON THE SYNTHESIS OF THE PHYTOCHROME CHROMOPHORE IN PEA EMBRYONIC AXES

Abstract Treatment of imbibed embryonic axes taken from seeds of Pisum sativum with N-phenylimide S-23142, a herbicide that has been suggested to inhibit protoporphyrin synthesis, or with N -methyl mesoporphyrin IX, an inhibitor of the iron chelatase for heme, resulted in a significant decrease in the amount of spectrophotometrically detectable phytochromc in the axes in both cases. However, the amount of immunochemically detectable phytochrome was not affected by either treatment. If S-23142 inhibits the synthesis of protoporphyrin IX in pea, it appears that the conversion of protoporphyrinogen IX to protoporphyrin IX is involved in the biosynthesis of the phytochrome chromophore. The conversion of protoporphyrin IX to heme (Fe-protoporpbyrin) also appears to be a step in the biosynthesis of the chromophore, since N -methyl mesoporphyrin IX prevented the synthesis of spectrophotometrically detectable phytochrome but did not affect the magnesium chelatase activity required for the synthesis of chlorophyll in pea embryonic axes. The results suggest that protoporphyrinogen IX, protoporphyrin IX and heme are intermediates in the biogenesis of the phytochromc chromophore. The pathway to phytochromobilin might become fixed after protoporphyrin IX, being directed toward the Fe branch for heme rather than to the Mg branch for chlorophyll.