The effect of the secondary structure on dissociation of peptide radical cations: fragmentation of angiotensin III and its analogues

Fragmentation of protonated RVYIHPF and RVYIHPF-OMe and the corresponding radical cations was studied using time- and collision energy-resolved surface-induced dissociation (SID) in a Fourier transform ion cyclotron resonance mass spectrometer (FT-ICR MS) specially equipped to perform SID experiments. Peptide radical cations were produced by gas-phase fragmentation of Co (III)(salen)-peptide complexes. Both the energetics and the mechanisms of dissociation of even-electron and odd-electron angiotensin III ions are quite different. Protonated molecules are much more stable toward fragmentation than the corresponding radical cations. RRKM modeling of the experimental data suggests that this stability is largely attributed to differences in threshold energies for dissociation, while activation entropies are very similar. Detailed analysis of the experimental data obtained for radical cations demonstrated the presence of two distinct structures separated by a high free-energy barrier. The two families of structures were ascribed to the canonical and zwitterionic forms of the radical cations produced in our experiments.     

Formation of cationic peptide radicals by gas-phase redox reactions with trivalent chromium, manganese, iron, and cobalt complexes

The collision-induced dissociation (CID) of a series of gas-phase complexes [M(III)(salen)(P)](+) [where M = Cr, Mn, Fe, and Co; P = hexapeptides YGGFLR, WGGFLR, and GGGFLR; and salen = N,N'-ethylenebis(salicylideneaminato)] has been examined with respect to the ability of the complexes to form the corresponding cationic peptide radical ions, P(+)(*), by homolytic cleavage of the metal peptide bond. This is the first example of the use of gas-phase ternary metal peptide complexes to produce the corresponding cationic peptide radical for a metal other than copper(II). The fragmentation reactions competing with radical formation are highly dependent on the metal ion used. In addition, examination of modified complexes in which the periphery of the salen was substituted allowed evaluation of electronic effects on the CID process, presumably without significant change in the geometry surrounding the metal. This substitution demonstrates that the ligand can be used to tune the dissociation chemistry to favor radical formation and suppress unwanted further fragmentation of the peptide radical that is typically observed immediately following its dissociation from the complex.     

Formation of Anionic Peptide Radicals In Vacuo

In this paper, we demonstrate for the first time the formation of radical anionic peptides [M - 2H]*- through a one-electron transfer mechanism upon low-energy collision-induced dissociation (CID) of gas-phase singly charged [Mn(III)(salen)(M - 2H)]*- complex ions [where salen is N,N'-ethylenebis(salicylideneiminato) and M is an angiotensin III derivative]. The types of fragment ions formed from [M - 2H]*- share some similarities with those from the cationic radical peptides M*+ and [M + H]*2+, but differ significantly from those of the corresponding deprotonated peptides [M - H]-. Fragmentation of [M - 2H]*- radical anionic angiotensin III derivatives leads preferentially to product ions of side-chain cleavage of amino acid residues, z-type and minor x-type fragment ions, most of which are types rarely observed in low-energy CID spectra of deprotonated analogs. The degree of competitive dissociation of the complexes is highly dependent on the nature of the substituted salen derivatives. The yields of anionic peptide radicals were enhanced to the greatest extent when electron withdrawing groups were positioned at the 5 and 5' positions, but the effect was rather modest when such groups resided at the 3 and 3' positions. Substituting a cyclohexyl unit of a salen with phenyl or naphthyl moieties at the 8 and 8' positions also facilitated electron-transfer pathways.     

Energetics and dynamics of peptide fragmentation from multiple-collision activation and surface-induced dissociation studies

This account summarizes the energetics and dynamics of peptide fragmentation obtained using a new approach recently developed in our laboratory. The approach involves RRKM modeling of time- and energy- resolved tandem mass spectrometry (MS/MS) data obtained using collisional activation. We demonstrate that surface-induced dissociation (SID) on a long time-scale of Fourier transform ion cyclotron resonance mass spectrometry (FT-ICR MS) is perfectly suited for studying the energetics and dynamics of peptide fragmentation. The advantages provided by SID include very fast ion activation, which eliminates possible discrimination against higher-energy dissociation pathways, and efficient "amplification" of small changes in dissociation parameters. We present a summary of results obtained for small alanine-containing peptides as well as larger peptides including angiotensin analogs and a series of peptides containing the LDIFSDF motif.     

Effect of the basic residue on the energetics, dynamics, and mechanisms of gas-phase fragmentation of protonated peptides

The effect of the basic residue on the energetics, dynamics, and mechanisms of backbone fragmentation of protonated peptides was investigated. Time-resolved and collision energy-resolved surface-induced dissociation (SID) of singly protonated peptides with the N-terminal arginine residue and their analogues, in which arginine is replaced with less basic lysine and histidine residues, was examined using a specially configured Fourier transform ion cyclotron resonance mass spectrometer (FTICR-MS). SID experiments demonstrated different kinetics of formation of several primary product ions of peptides with and without arginine residue. The energetics and dynamics of these pathways were determined from Rice-Ramsperger-Kassel-Marcus (RRKM) modeling of the experimental data. Comparison between the kinetics and energetics of fragmentation of arginine-containing peptides and the corresponding methyl ester derivatives provides important information on the effect of dissociation pathways involving salt bridge (SB) intermediates on the observed fragmentation behavior. Because pathways involving SB intermediates are characterized by low threshold energies, they efficiently compete with classical oxazolone and imine/enol pathways of arginine-containing peptides on a long time scale of the FTICR instrument. In contrast, fragmentation of histidine- and lysine-containing peptides is largely determined by canonical pathways. Because SB pathways are characterized by negative activation entropies, fragmentation of arginine-containing peptides is kinetically hindered and observed at higher collision energies as compared to their lysine- and histidine-containing analogues.     

Formation of peptide radical ions through dissociative electron transfer in ternary metal-ligand-peptide complexes

The formation and fragmentation of odd-electron ions of peptides and proteins is of interest to applications in biological mass spectrometry. Gas-phase redox chemistry occurring during collision-induced dissociation of ternary metal-ligand-peptide complexes enables the formation of a variety of peptide radicals, including the canonical radical cations, M(+?), radical dications, [M+H](2+?), radical anions, [M-2H](-?) and phosphorylated radical cations. In addition, odd-electron peptide ions with well-defined initial location of the radical site are produced through side-chain losses from the radical ions. Subsequent fragmentation of these species provides information regarding the role of charge and location of the radical site on the competition between radical-induced and proton-driven fragmentation of odd-electron peptide ions. This account summarizes current understanding of the factors that control the efficiency of the intramolecular electron transfer (ET) in ternary metal-ligand-peptide complexes resulting in formation of odd-electron peptide ions. Specifically, we discuss the effect of the metal center, the ligand and the peptide structure on the competition between the ET, proton transfer (PT) and loss of neutral peptide and neutral peptide fragments from the complex. Fundamental studies of the structures, stabilities and the energetics and dynamics of fragmentation of these complexes are also important for detailed molecular-level understanding of photosynthesis and respiration in biological systems.     

Synthesis, structure, and magnetic properties of three 1D chain complexes based on high-spin metal-cyanide clusters: [Mn(III)6M(III)] (M = Cr, Fe, Co)

On the basis of high-spin metal-cyanide clusters of Mn(III)(6)M(III) (M = Cr, Fe, Co), three one-dimensional (1D) chain complexes, [Mn(salen)](6)[Cr(CN)(6)](2)·6CH(3)OH·H(2)O (1), [Mn(5-CH(3))salen)](6)[Fe(CN)(6)](2)·2CH(3)CN·10H(2)O (2), and [Mn(5-CH(3))salen)](6)[Co(CN)(6)](2)·2CH(3)CN·10H(2)O (3) [salen = N,N'-ethylenebis(salicylideneiminato) dianion], have been synthesized and characterized structurally as well as magnetically. Complexes 2 and 3 are isomorphic but slightly different from complex 1. All three complexes contain a 1D chain structure which is comprised of alternating high-spin metal-cyanide clusters of [Mn(6)M](3+) and a bridging group [M(CN)(6)](3-) in the trans mode. Furthermore, the three complexes all exhibit extended 3D supramolecular networks originating from short intermolecular contacts. Magnetic investigation indicates that the coupling mechanisms are intrachain antiferromagnetic interactions for 1 and ferromagnetic interactions for 2, respectively. Complex 3 is a magnetic dilute system due to the diamagnetic nature of Co(III). Further magnetic investigations show that complexes 1 and 2 are dominated by the 3D antiferromagnetic ordering with T(N) = 7.2 K for 1 and 9.5 K for 2. It is worth noting that the weak frequency-dependent phenomenon of AC susceptibilities was observed in the low-temperature region in both 1 and 2, suggesting the presence of slow magnetic relaxations.     

Hydrogencyanamide-bridged one-dimensional polymers built on Mn(III)-Schiff base fragments: synthesis, structure, and magnetism

The ability of NCNH(-) to construct transition metal coordination polymers and to transmit magnetic coupling was investigated. By introduction of various tetradentate Schiff base ligands (L) and different solvents (S), nine NCNH(-)-bridged manganese(III) coordination complexes were obtained. Their structures can be divided into three types: I) NCNH-bridged chains built on mononuclear [Mn(III)(L)] units, [Mn(III)(L)(mu(1,3)-NCNH)](n) (L=5-Brsalen (1), 5-Clsalen (2)); II) NCNH-bridged chains built on dinuclear [Mn(III) (2)(L)(2)] units, complexes 3-8, [Mn(III) (2)(L)(2)(mu(1,3)-NCNH)]ClO(4)S (L=salen, 5-Fsalen, 5-Clsalen, 5-OCH(3)salen; S=CH(3)OH or C(2)H(5)OH); III) NCNH-bridged Mn(III) dimers linked by hydrogen bonds into a 1D polymer, {[Mn(III)(3-OCH(3)salen)(H(2)O)](2)(mu(1,3)-NCNH)}ClO(4) x 0.5 H(2)O (9, salen=N,N'-bis(salicylidene)-1,2-diaminoethane). In these complexes, the N[triple chemical bond]C--NH(-) resonance structure dominates the bonding mode of the NCNH(-) ligand adopting the mu(1,3)-bridging mode. Magnetic characterization shows that the asymmetric NCNH(-) bridge transmits antiferromagnetic interaction between Mn(III) ions and often favors the weak ferromagnetism caused by spin canting in these one-dimensional chains. However, these complexes exhibit different magnetic behaviors at low temperatures.     

Metal-mediated formation of gas-phase amino acid radical cations

The results from an investigation of the collision-induced dissociation (CID) of the ternary complexes [Cu(II)(terpy)(AA)](2+) are presented (terpy = 2,2':6',2' '-terpyridine; AA = one of the twenty common amino acids). These complexes show a rich gas-phase chemistry, which depends on the identity of the amino acid. For the histidine-, lysine- and tryptophan-containing complexes, oxidative dissociation of the amino acid is observed, yielding the amino acid radical cation. The results of further mass selection and CID of these amino acid radical cations are presented. The CID of the series [Fe(III)(salen)(AA)](+) (where salen = N,N'-ethylenebis(salicylideneaminato)) is also examined. These complexes undergo loss of the neutral amino acid in all cases, although the radical cation of arginine is also produced and its subsequent fragmentation examined. B3-LYP/6-31G(d) computations were carried out to test aspects of the proposed fragmentation mechanism of the histidine and arginine radical cations.     

Synthesis, structure, magnetic properties and DFT calculations of two hydroxo-bridged complexes based on Mn(III)(Schiff-Bases)

Two hydroxo-bridged complexes, {[Mn(III)(3-CH(3)O)salen](2)[Cr(III)(salen)(OH)(2)]}ClO(4)·6H(2)O (1) and {[Mn(III)(5-CH(3))salen](2)(OH)}ClO(4)·3H(2)O (2) [salen = N,N'-ethylenebis(salicylideneiminato) dianion], have been synthesized by the hydrolysis of the corresponding Mn(III)(Schiff-Bases) derivatives and [Cr(salen)(H(2)O)(2)]Cl precursors. X-Ray structure characterization reveals the discrete linear arched trinuclear structure of 1 and the 1D chain arrangement of 2. Magnetic experimental data and density functional theory (DFT) calculations both indicate the dominant antiferromagnetic interaction mediated by the hydroxo-bridges in both 1 and 2. Frequency-dependent AC susceptibilities reveal slow relaxation of 1 in low temperature. It is worth noting that the structure and magnetic properties of 1 is comparable to a reported cyano-bridged SMM, K[(5-Brsalen)(2)(H(2)O)(2)Mn(2)Cr(CN)(6)]·2H(2)O.     

Energetics and dynamics of the fragmentation reactions of protonated peptides containing methionine sulfoxide or aspartic acid via energy- and time-resolved surface induced dissociation

The surface-induced dissociation (SID) of six model peptides containing either methionine sulfoxide or aspartic acid (GAILM(O)GAILR, GAILM(O)GAILK, GAILM(O)GAILA, GAILDGAILR, GAILDGAILK, and GAILDGAILA) have been studied using a specially configured Fourier transform ion-cyclotron resonance mass spectrometer (FT-ICR MS). In particular, we have investigated the energetics and dynamics associated with (i) preferential cleavage of the methionine sulfoxide side chain via the loss of CH3SOH (64 Da), and (ii) preferential cleavage of the amide bond C-terminal to aspartic acid. The role of proton mobility in these selective bond cleavage reactions was examined by changing the C-terminal residue of the peptide from arginine (nonmobile proton conditions) to lysine (partially mobile proton conditions) to alanine (mobile proton conditions). Time- and energy-resolved fragmentation efficiency curves (TFECs) reveal that selective cleavages due to the methionine sulfoxide and aspartic acid residues are characterized by slow fragmentation kinetics. RRKM modeling of the experimental data suggests that the slow kinetics is associated with large negative entropy effects and these may be due to the presence of rearrangements prior to fragmentation. It was found that the Arrhenius pre-exponential factor (A) for peptide fragmentations occurring via selective bond cleavages are 1-2 orders of magnitude lower than nonselective peptide fragmentation reactions, while the dissociation threshold (E0) is relatively invariant. This means that selective bond cleavage is kinetically disfavored compared to nonselective amide bond cleavage. It was also found that the energetics and dynamics for the preferential loss of CH3SOH from peptide ions containing methionine sulfoxide are very similar to selective C-terminal amide bond cleavage at the aspartic acid residue. These results suggest that while preferential cleavage can compete with amide bond cleavage energetically, dynamically, these processes are much slower compared to amide bond cleavage, explaining why these selective bond cleavages are not observed if fragmentation is performed under mobile proton conditions. This study further affirms that fragmentation of peptide ions in the gas phase are predominantly governed by entropic effects.     

Cyano-bridged Mn(III)3M(III) (M(III) = Fe, Cr) complexes: synthesis, structure, and magnetic properties

Two cyano-bridged tetranuclear complexes composed of Mn(III) salen (salen = N,N'-ethylene bis(salicylideneiminate)) and hexacyanometalate(III) (M = Fe, Cr) in a stoichiometry of 3:1 have been selectively synthesized using {NH2(n-C12H25)2}3[M(III)(CN)6] (M(III) = Fe, Cr) starting materials: [{Mn(salen)(EtOH)}3{M(CN)6}] (M = Fe, 1; Cr, 2). Compounds 1 and 2 are isostructural with a T-shaped structure, in which [M(CN)6]3- assumes a meridional-tridentate building block to bind three [Mn(salen)(EtOH)]+ units. The strong frequency dependence and observation of hysteresis on the field dependence of the magnetization indicate that 1 is a single-molecule magnet.     

Atom transfer as a preparative tool in coordination chemistry. Synthesis and characterization of Cr(V) nitrido complexes of bidentate ligands

The transfer of a terminal nitrido ligand from Mn(V)(N)(salen) to Cr(III) complexes is explored as a new preparative route to Cr(V) nitrido complexes. Reaction of Mn(V)(N)(salen) with labile CrCl(3)(THF)(3) in acetonitrile solution precipitates [Mn(Cl)(salen)].(CH(3)CN) and yields a solution containing a mixture of Cr(V) nitrido species with only labile auxiliary ligands. From this solution Cr(V) nitrido complexes with bidentate monoanionic ligands can be obtained in high yields. Five coordinate complexes of 8-hydroxoquinolinate (quin), 1,3-diphenylpropane-1,3-dionate (dbm), and pyrrolidinedithiocarbamate (pyr-dtc) have been structurally characterized: Cr(N)(quin)(2) (1) crystallizes as compact orange prisms in the triclinic space group P with cell parameters a = 7.2450(6) A, b = 8.1710(4) A, c = 13.1610(12) A, alpha = 80.519(6) degrees, beta = 75.721(7) degrees, gamma = 75.131(5) degrees, V = 725.47(10) A(3), Z = 2. Cr(N)(dbm)(2) (2) crystallizes as green rhombs in the orthorhombic space group Pbca with cell parameters a = 14.6940(6) A, b = 16.4570(18) A, c = 19.890(3) A, V = 4809.8(8) A(3), Z = 8. Cr(N)(pyr-dtc)(2) (3) crystallizes as orange prisms in the monoclinic space group P21/c with cell parameters a = 14.8592(14) A, b = 8.5575(5) A, c = 11.8267(12) A, beta = 106.528(7) degrees, V = 1441.7(2) A(3), Z = 4. Complexes 2 and 3 represent new coordination environments for first row transition metal nitrido complexes. The d-orbital energy splitting in these systems with relatively weak equatorial donors differs significantly from the pattern in vanadyl and the previously known first row transition metal nitrido complexes. The d(x)2(-)(y)2 orbital in 2 and 3 is lower in energy and well resolved from the M-N pi orbitals [d(zx),d(yz)].     

Effects of transition metal ion identity and π-cation interactions in metal-bis(peptide) complexes containing phenylalanine

Electrospray ionization-tandem mass spectrometry was used to study the effects of the metal ion identity and π-cation interactions on the dissociation pathways of metal-bis(peptide) complexes, where the metal is either Mn(2+), Co(2+), Ni(2+), Cu(2+), or Zn(2+); and the peptide is either FGGF, GGGG, GF, or GG, where G is glycine and F is phenylalanine. The [(FGGF)(FGGF-H) + M(2+)](+) and [(GGGG)(GGGG-H) + M(2+)](+) complexes dissociated by losing one FGGF or GGGG, respectively. Relative binding affinities were measured using the crossover points, where the parent and product ions were equal in ion abundance and a normalized-collision energy scale. The results indicate the relative binding affinities for FGGF and GGGG follow the same order with respect to the transition metal ion identity: Cu(2+) < Ni(2+) < Mn(2+) ≈ Zn(2+) < Co(2+), and the π-cation interactions in the FGGF complex have a measureable stabilizing effect. In contrast, the main fragmentation channels of [(GF)(GF-H) + M(2+)]+ and [(GG)(GG-H) + M(2+)](+) are loss of CO(2) and 2CO(2) with the [(GF)(GF-H) + M(2+)](+) complex also exhibiting cinnamic acid ,GF, residual glycine, cinnamate and styrene loss.     

Chiral salen ligands designed to form polymetallic complexes

Chiral salen ligands capable of forming polymetallic complexes have been designed. The ligands possess substituents in the 4,4′-positions, but have no substituent in the 3,3′-positions to allow a second metal ion access to the salen oxygen atoms. Ligands in which a polyether chain links the 4,4′-positions were prepared and complexed to copper. In addition, acyclic ligands with potential metal coordinating substituents in the 4,4′-positions were prepared and complexed to copper and cobalt. The crystal structure of one of the cobalt complexes shows it to be a trimetallic complex in which a Co(II)(OAc)₂ group coordinates to the salen oxygen atoms of two Co(III)(salen)(OAc) units. In contrast, the crystal structure of a Co(salen) complex with tert-butyl groups attached to the 3,3′-positions is found to be mononuclear. All of the complexes were tested as asymmetric phase transfer catalysts for the asymmetric alkylation of an alanine methyl ester, forming (R)-α-methyl phenylalanine methyl ester with up to 85% ee.     

Gold Ion–Angiotensin Peptide Interaction by Mass Spectrometry

Stimulated by the interest in developing gold compounds for treating cancer, gold ion–angiotensin peptide interactions are investigated by mass spectrometry. Under the experimental conditions used, the majority of gold ion–angiotensin peptide complexes contain gold in the oxidation states I and III. Both ESI-MS and MALDI-TOF MS detect singly/multiply charged ions for mononuclear/multinuclear gold-attached peptides, which are represented as [peptide + a Au(I) + b Au(III) + (e - a -3b) H]^e+, where a,b ≥ 0 and e is charge. ESI-MS data shows singly/multiply charged ions of Au(I)-peptide and Au(III)-peptide complexes. This study reveals that MALDI-TOF MS mainly detects singly charged Au(I)-peptide complexes, presumably due to the ionization process. The electrons in the MALDI plume seem to efficiently reduce Au(III) to Au(I). MALDI also tends to enhance the higher polymeric forms of gold-peptide complexes regardless of the laser power used. Collision-induced dissociation experiments of the mononuclear and dinuclear gold-attached peptide ions for angiotensin peptides show that the gold ion (a soft acid) binding sites are in the vicinity of Cys (a soft ligand), His (a major anchor of peptide for metal ion chelation), and the basic residue Arg. Data also suggests that the abundance of gold-attached peptides increases with higher gold concentration until saturation, after which an increase in gold ion concentration leads to the aggregation and/or precipitation of gold-bound peptides.     

Syntheses, crystal structures, and magnetic characterization of five new dimeric manganese(III) tetradentate Schiff base complexes exhibiting single-molecule-magnet behavior

Tetradentate Schiff base ligands H2L (H2saltmen, H2salen, H2-5-Brsalen, and H2-3,5-Brsalen), derived from the condensation of the corresponding salicylaldehyde or its derivatives with 1,1,2,2-tetramethylethyldiamine or 1, 2-diaminoethane, reacted with Mn(III) acetate or perchlorate salts and sodium azide or sodium cyanate to produce five Mn(III) dimer complexes, [Mn(saltmen)(O2CCH3)]2.2CH3CO2H (1), [Mn(saltmen)(N3)]2 (2), [Mn(salen)(NCO)]2 (3), [Mn(3,5-Brsalen)(3,5-Brsalicylaldehyde)]2 (4), and [Mn(5-Brsalen)(CH3OH)]2(ClO4)2 (5). These new complexes have been characterized by IR, elemental analyses, crystal structural analyses, and magnetic studies. Within these Mn(III) dimeric complexes, two Mn(III) ions are connected by phenolate oxygen atoms with acetate, azide, cyanate, a 3,5-Brsalicyladehyde anion, and a neutral methanol molecule as the axial ligands for complexes 1-5, respectively. Complexes 1-4 exhibit intradimer ferromagnetic exchange and display frequency dependence of ac magnetic susceptibility, possibly showing single-molecule-magnet (SMM) behavior. In contrast, complex 5 shows an intradimer antiferromagnetic coupling probably originating from the relatively shorter Mn-O distance, compared to those of complexes 1-4.     

Probing the reactivity of oxomanganese-salen complexes: an electrospray tandem mass spectrometric study of highly reactive intermediates

Electrospray ionization in combination with tandem mass spectrometric techniques has been employed to study the formation of oxomanganese-salen complexes upon oxidation of [Mn(III)(salen)]+ cations as well as the properties and reactions of the oxidized species in the gas phase. Two species could be characterized as the principal oxidation products: the oxomanganese(v) complex, [Mn=O(salen)]+, which is the actual oxygen-transfer agent in epoxidation reactions, and the dinuclear, mu-oxo bridged [L(salen)Mn-O-Mn(salen)L]2+ with two terminal ligands L; the latter acts as a reservoir species. The effects of various substituents in the 5- and 5'-positions, respectively, of the salen ligand on the reactivity of the epoxidation catalyst were determined quantitatively from CID (collision-induced dissociation) experiments and B3LYP density functional calculations. Accordingly, the effect of axial donor ligands on the reactivity of the epoxidation catalyst was studied. Electron-withdrawing substitutents on the salen ligand and additional axial ligands decrease the stability and thus enhance the reactivity of the Mn=O moiety, while electron-donating salen substituents have a strong stabilizing effect.     

Fragmentation of <Emphasis Type="Italic">α</Emphasis>-radical cations of arginine-containing peptides

Fragmentation pathways of peptide radical cations, M^+·, with well-defined initial location of the radical site were explored using collision-induced dissociation (CID) experiments. Peptide radical cations were produced by gas-phase fragmentation of Co^III(salen)-peptide complexes [salen=N,N′-ethylenebis (salicylideneiminato)]. Subsequent hydrogen abstraction from the β-carbon of the side-chain followed by C_α-C_β bond cleavage results in the loss of a neutral side chain and formation of an α-radical cation with the radical site localized on the α-carbon of the backbone. Similar CID spectra dominated by radical-driven dissociation products were obtained for a number of arginine-containing α-radicals, suggesting that for these systems radical migration precedes fragmentation. In contrast, proton-driven fragmentation dominates CID spectra of α-radicals produced via the loss of the arginine side chain. Radical-driven fragmentation of large M^+· peptide radical cations is dominated by side-chain losses, formation of even-electron a-ions and odd-electron x-ions resulting from C_α-C bond cleavages, formation of odd-electron z-ions, and loss of the N-terminal residue. In contrast, charge-driven fragmentation produces even-electron y-ions and odd-electron b-ions.     

Thermal intramolecular electron transfer reactions of [N,N′-ethylene-bis(salicylideneaminato)](2,4-pentanedionato)cobalt(III) complexes in the solid state

The title complexes with the formula Co(salen)L where L is a series of 2,4-pentanedionates underwent thermally induced one-electron transfer reactions from L to Co(III). The reaction left behind a stoichiometric amount of the crystalline Co^II(salen) complex which took up oxygen in a molar ratio of Co:O₂ = 2:1. The kinetic analyses showed that the electron transfer reaction rate was apparently dominated by activation entropy rather than by activation enthalpy.