RESUMO
A mononuclear manganese(iii)-peroxo complex [MnIII(N3Py2)(O2)]+ (1a) bearing a non-heme N,N'-dimethyl-N-(2-(methyl(pyridin-2-ylmethyl)amino)ethyl)-N'-(pyridin-2-ylmethyl)ethane-1,2-diamine (N3Py2) ligand was synthesized by the reaction of [Mn(N3Py2)(H2O)](ClO4)2 (1) with hydrogen peroxide and triethylamine in CH3CN at 25 °C. The reactivity of 1a in aldehyde deformylation using 2-phenyl propionaldehyde (2-PPA) was studied and the reaction kinetics was monitored by UV-visible spectroscopy. A kinetic isotope effect (KIE) = 1.7 was obtained in the reaction of 1a with 2-PPA and α-[D1]-PPA, suggesting nucleophilic character of 1a. The activation parameters ΔH and ΔS were determined using the Eyring plot while Ea was obtained from the Arrhenius equation by performing the reaction between 288 and 303 K. Hammett constants (σp) of para-substituted benzaldehydes p-X-Ph-CHO (X = Cl, F, H, and Me) were linear with a slope (ρ) = 3.0. Computational study suggested that the side-on structure of 1a is more favored over the end-on structure and facilitates the reactivity of 1a.
RESUMO
Femtosecond time-resolved fluorescence and transient absorption studies are reported for three newly synthesized covalently linked N,N-bis(4'-tert-butylbiphenyl-4-yl)aniline (BBA) and pyrrolidinofullerenes (C60)-based donor-π conjugated bridge-acceptor dyads (D-B-A) as functions of the bridge length (7.1, 9.5 and 11.2 Å for Dyad-1, Dyad-2 and Dyad-3), dielectric constants of the medium and pump wavelengths. In polar solvent, ultrafast fluorescence quenching (kEET ≥ 2 × 1012 s-1) of the BBA moiety upon excitation of the BBA moiety (320 nm) is observed in the dyads and is assigned to a mechanism involving electron exchange energy transfer (EET) from 1BBA* to C60 followed by electron transfer from BBA to 1C60*. Cohesive rise and decay dynamics of conjugated BBAË+-C60Ë- anion pairs confirm the involvement of a distance independent adiabatic charge-separation (CS) process (kCS ≥ 2.2 × 1011 s-1) with near unity quantum efficiency (φCS ≥ 99.7%) and a distance-dependent non-adiabatic charge-recombination (CR) process [kCR â¼ (1010-108) s-1]. In contrast, excitation of the C60 moiety (λex = 430 to 700 nm) illustrates photoinduced electron transfer from BBA to 1C60*, involving non-adiabatic (diabatic) and distance-dependent CS (kCS in the range of 0.59-1.78 × 1011 s-1) with 98.86-99.6% (Dyad-3-Dyad-1) quantum efficiency and a CR process with kCR values [kCR â¼ (1010-108) s-1] up to three orders greater than kCS of the respective dyads. Both the processes, CS and CR, upon C60 excitation and the CR process upon BBA excitation show distance dependent rate constants with exponential factor ß ≤ 0.5 Å-1, and electron transfer is concluded to occur through a covalently linked conjugated π bridge. Global and target analysis of fsTA data reveal the occurrence of two closely lying CS states, thermally hot (CShot) and thermally relaxed (CSeq) states, and two CR processes with two orders of different rate constants. Careful analysis of the kinetic and thermodynamic data allowed us to estimate the total reorganization energy and electronic coupling matrix (V), which decrease exponentially with distance. These novel features of the distance independent adiabatic CS process and the distance-dependent diabatic CR process upon donor excitation are due to extending the π-conjugation between BBA and C60. The demonstrated results may provide a benchmark in the design of light-harvesting molecular devices where ultrafast CS processes and long-lived CS states are essential requirements.
RESUMO
Targeted molecular imaging to detect changes in the structural and functional organization of tissues, at the molecular level, is a promising approach for effective and early diagnosis of diseases. Quantitative and qualitative changes in type I collagen, which is a major component in the extra cellular matrix (ECM) of skin and other vital organs like lung, liver, heart and kidneys, are often associated with the pathophysiology of these organs. We have synthesized a fluorescent probe that comprises collagelin, a specific collagen binding peptide, coupled to fluorescent porphyrin that can effectively detect abnormal deposition of collagen in live tissues by emitting fluorescence in the near infra red (NIR) region. In this report we have presented the methodology for coupling of 5-(4-carboxy phenyl)-10, 15, 20-triphenyl porphyrin (C-TPP) to the N-terminal of collagelin or to another mutant peptide (used as a control). We have evaluated the efficacy of these fluorescent peptides to detect collagen deposition in live normal and abnormal tissues. Our results strongly suggest that porphyrin-tagged collagelin can be used as an effective probe for the non invasive in vivo detection of tissue fibrosis, especially in the liver.
