Alkaline and enzymatic degradation of L‐lactide copolymers. II. Crystallized films of poly(L‐lactide‐co‐D‐lactide) and poly(L‐lactide) with similar crystallinities

Films of poly(L ‐lactide‐co‐D ‐lactide) [P(LLA‐DLA); 95/5] and poly(L ‐lactide) [i.e., poly(L ‐lactide acid) (PLLA)] were prepared by crystallization from the melt, and a comparative study of the crystallization effects on the alkaline and proteinase K catalyzed hydrolysis of the films was carried out. The hydrolyzed films were investigated with gravimetry, differential scanning calorimetry, polarimetry, and gel permeation chromatography, and the results were compared with those reported for amorphous‐made specimens. The alkaline hydrolyzability of the P(LLA‐DLA) (95/5) and PLLA films was determined solely by the initial crystallinity (X_c) and was not affected by the content of the incorporated D ‐lactide (DLA) unit in the polymer chain; this was in marked contrast to the fact that the enzymatic hydrolyzability depended on not only the initial X_c value but also the DLA unit content. The alkaline hydrolysis rate of the P(LLA‐DLA) (95/5) and PLLA films and the enzymatic hydrolysis rate (R_EH) of the P(LLA‐DLA) (95/5) films decreased linearly as the initial X_c value increased. This meant that the hydrolyzability of the restricted amorphous regions was very similar to that of the free amorphous regions. In contrast, R_EH of the PLLA films decreased nonlinearly with the initial X_c value, and this nonlinear dependence was caused by the fact that in the PLLA films the restricted amorphous regions were much more hydrolysis‐resistant than the free amorphous regions. © 2005 Wiley Periodicals, Inc. J Polym Sci Part B: Polym Phys 43: 1064‐1075, 2005     

Synthesis of star‐shaped poly(D,L‐lactic acid‐alt‐glycolic acid)‐b‐poly(L‐lactic acid) with the poly(D,L‐lactic acid‐alt‐glycolic acid) macroinitiator and stannous octoate catalyst

Two types of three‐arm and four‐arm, star‐shaped poly(D,L ‐lactic acid‐alt‐glycolic acid)‐b‐poly(L ‐lactic acid) (D,L ‐PLGA50‐b‐PLLA) were successfully synthesized via the sequential ring‐opening polymerization of D,L ‐3‐methylglycolide (MG) and L ‐lactide (L ‐LA) with a multifunctional initiator, such as trimethylolpropane and pentaerythritol, and stannous octoate (SnOct₂) as a catalyst. Star‐shaped, hydroxy‐terminated poly(D,L ‐lactic acid‐alt‐glycolic acid) (D,L ‐PLGA50) obtained from the polymerization of MG was used as a macroinitiator to initiate the block polymerization of L ‐LA with the SnOct₂ catalyst in bulk at 130 °C. For the polymerization of L ‐LA with the three‐arm, star‐shaped D,L ‐PLGA50 macroinitiator (number‐average molecular weight = 6800) and the SnOct₂ catalyst, the molecular weight of the resulting D,L ‐PLGA50‐b‐PLLA polymer linearly increased from 12,600 to 27,400 with the increasing molar ratio (1:1 to 3:1) of L ‐LA to MG, and the molecular weight distribution was rather narrow (weight‐average molecular weight/number‐average molecular weight = 1.09–1.15). The ¹H NMR spectrum of the D,L ‐PLGA50‐b‐PLLA block copolymer showed that the molecular weight and unit composition of the block copolymer were controlled by the molar ratio of L ‐LA to the macroinitiator. The ¹³C NMR spectrum of the block copolymer clearly showed its diblock structures, that is, D,L ‐PLGA50 as the first block and poly(L ‐lactic acid) as the second block. © 2001 John Wiley & Sons, Inc. J Polym Sci Part A: Polym Chem 40: 409–415, 2002     

Synthesis and ring‐opening (co)polymerization of L‐lysine N‐carboxyanhydrides containing labile side‐chain protective groups

This contribution describes the synthesis and ring‐opening (co)polymerization of several L ‐lysine N‐carboxyanhydrides (NCAs) that contain labile protective groups at the ?‐NH₂ position. Four of the following L ‐lysine NCAs were investigated: N^?‐trifluoroacetyl‐L ‐lysine N‐carboxyanhydride, N^?‐(tert‐butoxycarbonyl)‐L ‐lysine N‐carboxyanhydride, N^?‐(9‐fluorenylmethoxycarbonyl)‐L ‐lysine N‐carboxyanhydride, and N^?‐(6‐nitroveratryloxycarbonyl)‐L ‐lysine N‐carboxyanhydride. In contrast to the harsh conditions that are required for acidolysis of benzyl carbamate moieties, which are usually used to protect the ?‐NH₂ position of L ‐lysine during NCA polymerization, the protective groups of the L ‐lysine NCAs presented here can be removed under mildly acidic or basic conditions or by photolysis. As a consequence, these monomers may allow access to novel peptide hybrid materials that cannot be prepared from ?‐benzyloxycarbonyl‐L ‐lysine N‐carboxyanhydride (Z‐Lys NCA) because of side reactions that accompany the removal of the Z groups. By copolymerization of these L ‐lysine NCAs with labile protective groups, either with each other or with γ‐benzyl‐L ‐glutamate N‐carboxyanhydride or Z‐Lys NCA, orthogonally side‐chain‐protected copolypeptides with number‐average degrees of polymerization ≤20 were obtained. Such copolypeptides, which contain different side‐chain protective groups that can be removed independently, are interesting for the synthesis of complex polypeptide architectures or can be used as scaffolds for the preparation of synthetic antigens or protein mimetics. © 2003 Wiley Periodicals, Inc. J Polym Sci Part A: Polym Chem 41: 1167–1187, 2003     

Synthesis and characterization of macroinitiator‐amino terminated PEG and poly(γ‐benzyl‐L‐glutamate)‐PEO‐poly(γ‐benzyl‐L‐glutamate) triblock copolymer

Macroinitiator‐amino terminated poly(ethylene glycol) (PEG) (NH₂‐PEO‐NH₂) was prepared by converting both terminal hydroxyl groups of PEG to more reactive primary amino groups. The synthetic route involved reactions of chloridize, phthalimide and finally hydrazinolysis. Furthermore, poly(γ‐benzyl‐L ‐glutamate)‐poly(ethylene oxide)‐poly(γ‐benzyl‐L ‐glutamate) (PBLG‐PEO‐PBLG) triblock copolymer was synthesized by polymerization of γ‐benzyl‐L ‐glutamate N‐carboxyanhydride (Bz‐L‐GluNCA) using NH₂‐PEO‐NH₂ as macroinitiator. The resultant NH₂‐PEO‐NH₂ and triblock copolymer were characterized by FT‐IR, ¹H‐NMR and gel permeation chromatography (GPC) techniques. The results demonstrated that the degree of amination of the NH₂‐PEO‐NH₂ could be up to 1.95. The molecular weight of the PBLG‐PEO‐PBLG triblock copolymer could be adjusted easily by controlling the molar ratio of Bz‐L ‐Glu NCA to the macroinitiator NH₂‐PEO‐NH₂. Copyright © 2004 John Wiley & Sons, Ltd.     

Stereoselective Synthesis of D‐ and L‐Carbocyclic Nucleosides by Enzymatically Catalyzed Kinetic Resolution

An efficient synthesis of (S)‐ or (R)‐3‐(benzyloxy‐methyl)‐cyclopent‐3‐enol was developed by appling an enzyme‐catalyzed kinetic‐resolution approach. This procedure allowed the syntheses of the enantiomeric building blocks (S)‐ and (R)‐cyclopentenol with high optical purity (>98 % ee). In contrast to previous approaches, the key advantage of this procedure is that the resolution is done on the level of enantiomers that only contain one stereogenic center. Owing to this feature, it was possible to chemically convert the enantiomers into each other. By using this route, the starting materials for the syntheses of carbocyclic D ‐ and L ‐nucleoside analogues were readily accessible. 3′,4′‐Unsaturated D ‐ or L ‐carbocyclic nucleosides were obtained from the condensation of various nucleobases with (S)‐ or (R)‐cyclopentenol. Functionalization of the double bond in 3′‐deoxy‐3′,4′‐didehydro‐carba‐D ‐thymidine led to a variety of new nucleoside analogues. By using the cycloSal approach, their corresponding phosphorylated metabolites were readily accessable. Moreover, a new synthetic route to carbocyclic 2′‐deoxy‐nucleosides was developed, thereby leading to D ‐ and L ‐carba‐dT. D ‐Carba‐dT was tested for antiviral activity against multidrug‐resistance HIV‐1 strain E2‐2 and compared to the known antiviral agent d4T, as well as L ‐carba‐dT. Whilst L ‐carba‐dT was found to be inactive, its D ‐analogue showed remarkably high activity against the resistant virus and significantly better than that of d4T. However, against the wild‐type virus strain NL4/3, d4T was found to be more‐active than D ‐carba‐dT.     

Two modes of asymmetric polymerization of phenylacetylenes having an L‐amino alcohol residue and two hydroxy groups

Four novel chiral phenylacetylenes having an L ‐amino alcohol residue and two hydroxymethyl groups were synthesized and polymerized by an achiral catalyst ((nbd)Rh⁺[η⁶‐(C₆H₅)B^?(C₆H₅)₃]) or a chiral catalytic system ([Rh(nbd)Cl]₂/(S)‐ or (R)‐phenylethylamine ((S)‐ or (R)‐PEA)). The two resulting polymers having an L ‐valinol or L ‐phenylalaninol residue showed Cotton effects at wavelengths around 430 nm. This observation indicated that they had an excess of one‐handed helical backbones. Positive and negative Cotton effects were observed only for the polymers having an L ‐valinol residue produced by using (R)‐ and (S)‐PEA as a cocatalyst, respectively, although the monomer had the same chirality. Even when the achiral catalyst was used, the two resulting polymers having an L ‐valinol or L ‐phenylalaninol residue showed Cotton effects despite the long distance between the chiral groups and the main chain. We have found the first example of a new type of chiral monomer, that is, a chiral phenylacetylene monomer having an L ‐amino alcohol residue and two hydroxy groups that was suitable for both modes of asymmetric polymerization, that is, the helix‐sense‐selective polymerization ( HSSP ) with the chiral catalytic system and the asymmetric‐induced polymerization ( AIP ) with the achiral catalyst. The other two monomers having L ‐alaninol and L ‐tyrosinol were found to be unsuitable to neither HSSP nor AIP because of their polymers' low solubility. © 2012 Wiley Periodicals, Inc. J Polym Sci Part A: Polym Chem, 2012     

Controllable ring‐opening copolymerization of L‐lactide and (3S)‐benzyloxymethyl‐(6S)‐methyl‐morpholine‐2,5‐dione initiated by a biogenic compound creatinine acetate

Ring‐opening copolymerization (ROCP) of L ‐lactide (L ‐LA) and (3S)‐benzyloxymethyl‐(6S)‐methyl‐morpholine‐2,5‐dione [(3S, 6S)‐BMMD] initiated by creatinine acetate, a biogenic organic compound, was performed in the bulk at 130 °C. The copolymerization was well controlled as evidenced by that both the measured values of number‐average molecular weight (M_n,NMR(OH) and M_n,NMR(COOH)) and serine molar fraction (F_Bz.ser) of synthesized copolymers were close to the corresponding theoretical values; and that the higher isotacticity of synthesized copolymers (85–86%) and lower racemization degree of the ROCP. After removing O‐benzyls of the copolymers with Et₃SiH/Et₃N/CH₂Cl₂ under catalysis of PdCl₂, functional biodegradable copolymers of L ‐lactic acid (L ‐Lac) and L ‐Ser with designed molar fraction of serine (F_ser 1.35%, 3.57%, 5.41%), narrow molecular weight distribution (polydispersity index 1.10–1.36), and improved hydrophilicity (θ_stat 82.3–89.6°) were finally obtained. © 2012 Wiley Periodicals, Inc. J Polym Sci Part A: Polym Chem, 2012     

Efficient Synthesis of 1,2,3,4,6‐Penta‐O‐acetyl‐L‐idopyranose

An efficient synthesis of 1,2,3,4,6‐penta‐O‐acetyl‐L ‐idopyranose 2 from 3,5‐O‐benzylidene‐1,2‐O‐isopropylidene‐α‐D ‐glucofuranose in five steps in 45% overall yield via hydroboration of enol ether, hydrolysis of L ‐idofuranosyl sugar and acetolysis of 1,6‐anhydro‐β‐L ‐idopyranose as key steps is described here.     

Synthesis of Glycaro‐1,5‐lactams and Tetrahydrotetrazolopyridine‐5‐carboxylates: Inhibitors of β‐D‐Glucuronidase and α‐L‐Iduronidase

The known glucaro‐1,5‐lactam 8 , its diastereoisomers 9 – 11 , and the tetrahydrotetrazolopyridine‐5‐carboxylates 12 – 14 were synthesised as potential inhibitors of β‐D ‐glucuronidases and α‐L ‐iduronidases. The known 2,3‐di‐O‐benzyl‐4,6‐O‐benzylidene‐D ‐galactose ( 16 ) was transformed into the D ‐galactaro‐ and L ‐altraro‐1,5‐lactams 9 and 11 via the galactono‐1,5‐lactam 21 in twelve steps and in an overall yield of 13 and 2%, respectively. A divergent strategy, starting from the known tartaric anhydride 41 , led to the D ‐glucaro‐1,5‐lactam 8 , D ‐galactaro‐1,5‐lactam 9 , L ‐idaro‐1,5‐lactam 10 , and L ‐altraro‐1,5‐lactam 11 in ten steps and in an overall yield of 4–20%. The anhydride 41 was transformed into the L ‐threuronate 46 . Olefination of 46 to the (E)‐ or (Z)‐alkene 47 or 48 followed by reagent‐ or substrate‐controlled dihydroxylation, lactonisation, azidation, reduction, and deprotection led to the lactams 8 – 11 . The tetrazoles 12 – 14 were prepared in an overall yield of 61–81% from the lactams 54, 28 , and 67 , respectively, by treatment with Tf₂O and NaN₃, followed by saponification, esterification, and hydrogenolysis. The lactams 8 – 11 and 40 and the tetrazoles 12 – 14 are medium‐to‐strong inhibitors of β‐D ‐glucuronidase from bovine liver. Only the L ‐ido‐configured lactam 10 (K_i = 94 μM ) and the tetrazole 14 (K_i = 1.3 mM ) inhibit human α‐L ‐iduronidase.     

Synthesis of Poly(L‐lactide) with One Terminal D‐Glucose Residue and Wettability of Its Film Surface

To develop the new‐type poly(L ‐lactide)‐based biomedical material having a wettable surface, the synthesis of poly(L ‐lactide) with one terminal D ‐glucose residue was investigated. After the hydroxyl group at 1‐C of α‐tetrabenzyl glucose, α‐Glc(Bzl)₄, was converted to the corresponding potassium alkoxide by using potassium tert‐butoxide, L ‐lactide (L ‐LA) was polymerized in the presence of α‐Glc(Bzl)₄‐OK as an initiator in tetrahydrofuran at room temperature to prepare α‐Glc(Bzl)₄‐polyLA. Subsequently, the removal of O‐protecting benzyl groups in the terminal α‐Glc(Bzl)₄ residue was carried out by hydrogenolysis with Pd/C to obtain the objective D ‐glucose‐end‐capped polyLA, α‐Glc‐polyLA. The wettability of surface of the α‐Glc‐polyLA material is discussed using the difference of the dynamic contact angle between a α‐Glc‐polyLA/homopolyLA blend film and a film of the polyLA homopolymer.     

Heterospirocyclic N‐(2H‐Azirin‐3‐yl)‐L‐prolinates: New Dipeptide Synthons

The synthesis of methyl N‐(1‐aza‐6‐oxaspiro[2.5]oct‐1‐en‐2‐yl)‐L ‐prolinate ( 1e ) has been performed by consecutive treatment of methyl N‐[(tetrahydro‐2H‐pyran‐4‐yl)thiocarbonyl]‐L ‐prolinate ( 5 ) with COCl₂, 1,4‐diazabicyclo[2.2.2]octane (DABCO), and NaN₃ (Scheme 1). As the first example of a novel class of dipeptide synthons, 1e has been shown to undergo the expected reactions with carboxylic acids and thioacids (Scheme 2). The successful preparation of the nonapeptide 16 , which is an analogue of the C‐terminal nonapeptide of the antibiotic Trichovirin I 1B, proved that 1e can be used in peptide synthesis as a dipeptide building block (Scheme 3). The structure of 7 has been established by X‐ray crystal‐structure analysis (Figs. 1 and 2).     

Controlled surface‐initiated ring‐opening polymerization of L‐lactide from risedronate‐anchored hydroxyapatite nanocrystals: Novel synthesis of biodegradable hydroxyapatite/poly(L‐lactide) nanocomposites

Risedronate‐anchored hydroxyapatite (HA‐RIS) nanocrystals were prepared with 4.1 wt % RIS and used for controlled surface‐initiated ring‐opening polymerization (ROP) of L ‐lactide (L ‐LA). The strong adsorption of RIS to HA surface not only led to enhanced dispersion of HA nanocrystals in water as well as in organic solvents but also provided alkanol groups as active initiating species for ROP of L ‐LA. HA‐RIS was characterized by thermogravimetric analysis, dynamic light scattering, ¹H NMR, Fourier transform infrared spectrometer, and X‐ray diffraction. The graft polymerization of L ‐LA onto HA‐RIS took place smoothly in the presence of stannous octoate in toluene at 120 °C, resulting in HA/poly(L ‐LA) nanocomposites with high yields of 85–90% and high poly(L ‐LA) contents of up to 97.5 wt %. Notably, differential scanning calorimetry measurements revealed that the poly(L ‐LA) in HA/poly(L ‐LA) nanocomposites exhibited considerably higher melting temperatures (T_m = 173.3?178.1 °C) and higher degrees of crystallinity (X_c = 41.0?43.1%) as compared to poly(L ‐LA) homopolymer (T_m = 168.5 °C, X_c =25.7%). In addition, our initial results showed that these HA/poly(L ‐LA) nanocomposites could readily be electrospun into porous matrices. This study presented a novel and controlled synthetic strategy to HA/RIS/poly(L ‐LA) nanocomposites that are promising for orthopedic applications as well as for bone tissue engineering. © 2011 Wiley Periodicals, Inc. J Polym Sci Part A: Polym Chem, 2011     

Synthesis and asymmetric polymerization of (S)‐N‐maleoyl‐L‐leucine propargyl ester

A kind of N‐substituted maleimide (RMI), chiral (S)‐N‐maleoyl‐L ‐leucine propargyl ester ((S)‐PLMI) with a specific rotation of [α]₄₃₅ = ?27.5° was successfully synthesized from maleic anhydride, L ‐leucine, and propargyl alcohol. (S)‐PLMI was polymerized by three polymerization methods to obtain the corresponding optically active polymers. Asymmetric anionic, radical, and transition‐metal‐catalyzed polymerizations were carried out using organometal/chiral ligands, 2,2′‐azobisisobutyronitrile (AIBN) and (bicyclo [2,2,1]hepta‐2,5‐diene) chloro rhodium (I) dimer ([Rh(nbd) Cl]₂), respectively. Poly((S)‐PLMI) obtained by [Rh(nbd)Cl]₂ in DMF showed the highest specific rotation of ?280.6°. Chiroptical properties and structures of the polymers obtained were investigated by GPC, CD, IR, and NMR measurements. Two types of poly((S)‐PLMI)‐bonded‐silica gels as the chiral stationary phase (CSP) were prepared for high‐performance liquid chromatography (HPLC). Their optical resolution abilities were also elucidated. © 2007 Wiley Periodicals, Inc. J Polym Sci Part A: Polym Chem 45: 3722–3738, 2007     

Aminocyclopentitol Inhibitors of α‐L‐Fucosidases

Aminocyclopentitol analogs of α‐L ‐fucose were synthesized stereoselectively from D ‐ribose. Alkyl substituents were attached at the NH₂ group to mimic the glycosidic leaving group. The resulting (alkylamino)cyclopentitols inhibited α‐L ‐fucosidases selectively with inhibition constants in the range of K_i=10⁻⁷ M . Comparisons with stereoisomers and acyclic analogs showed that this inhibition only occurs with N‐alkyl substitution and proper configuration at the cyclopentane, as expected for transition‐state‐analog‐type inhibition. These observations were supported by molecular‐modeling comparisons between inhibitor and transition state.     

Synthesis and Base Pairing Properties of 1′,5′‐Anhydro‐L‐Hexitol Nucleic Acids (L‐HNA)

Oligonucleotides composed of 1′,5′‐anhydro‐arabino‐hexitol nucleosides belonging to the L series (L ‐HNA) were prepared and preliminarily studied as a novel potential base‐pairing system. Synthesis of enantiopure L ‐hexitol nucleotide monomers equipped with a 2′‐(N⁶‐benzoyladenin‐9‐yl) or a 2′‐(thymin‐1‐yl) moiety was carried out by a de novo approach based on a domino reaction as key step. The L oligonucleotide analogues were evaluated in duplex formation with natural complements as well as with unnatural sugar‐modified oligonucleotides. In many cases stable homo‐ and heterochiral associations were found. Besides T_m measurements, detection of heterochiral complexes was unambiguously confirmed by LC‐MS studies. Interestingly, circular dichroism measurements of the most stable duplexes suggested that L ‐HNA form left‐handed helices with both D and L oligonucleotides.     

Pseudopoly(amino acid)s: Copolymerization of trans‐4‐hydroxy‐L‐proline and α‐hydroxy acids

A series of novel copolymers of trans‐4‐hydroxy‐L ‐proline (Hpr) and α‐ hydroxy acids [D,L ‐mandelic acid (DLMA) and D,L ‐lactic acid (DLLA)] were synthesized via direct melt copolymerization with stannous octoate as a catalyst. These new copolymers had pendant amine functional groups along the polymer backbone chain. The optimal reaction conditions for the synthesis of the copolymers were obtained with 4 wt % stannous octoate at 140 °C under vacuum for 16 h. The synthesized copolymers were characterized by IR spectrophotometry, proton nuclear magnetic resonance, differential scanning calorimetry, and Ubbelohde viscometry. The effects of the kinds of comonomers and the comonomer molar ratio on the polycondensation and glass‐transition temperature (T_g) were investigated. The T_g's of the copolymers shifted to lower temperatures with an increasing comonomer molar ratio. As expected, the T_g's of the N‐Z‐Hpr/DLMA copolymers were higher than the N‐Z‐Hpr/DLLA copolymers, the pendant groups on the monomers (N‐Z‐Hpr) became larger and more flexible, and the T_g's of the resulting polymers declined. © 2001 John Wiley & Sons, Inc. J Polym Sci A: Polym Chem 39: 724–731, 2001     

A New Route for Preparation of 5‐Deoxy‐5‐(hydroxyphosphinyl)‐ D‐mannopyranose and ‐L‐gulopyranose Derivatives

Starting from methyl 2,3‐O‐isopropylidene‐α‐D ‐mannofuranoside ( 5 ), methyl 6‐O‐benzyl‐2,3‐O‐isopropylidene‐α‐D ‐lyxo‐hexofuranosid‐5‐ulose ( 12 ) was prepared in three steps. The addition reaction of dimethyl phosphonate to 12 , followed by deoxygenation of 5‐OH group, provided the 5‐deoxy‐5‐dimethoxyphosphinyl‐α‐D ‐mannofuranoside derivative 15a and the β‐L ‐gulofuranoside isomer 15b . Reduction of 15a and 15b with sodium dihydrobis(2‐methoxyethoxy)aluminate, followed by the action of HCl and then H₂O₂, afforded the D ‐mannopyranose ( 17 ) and L ‐gulopyranose analog 21 , each having a phosphinyl group in the hemiacetal ring. These were converted to the corresponding 1,2,3,4,6‐penta‐O‐acetyl‐5‐methoxyphosphinyl derivatives 19 and 23 , respectively, structures and conformations (⁴C₁ or ¹C₄, resp.) of which were established by ¹H‐NMR spectroscopy.     

Total Synthesis of Aculeatins A and B from L‐Malic Acid

An efficient total synthesis of the cytotoxic spiroketal natural products aculeatin A and B is described. The synthesis of the 1,3,5‐triol moiety with appropriate configuration was accomplished from the commercially available L ‐malic acid. The key steps in this synthesis are the Barbier allylation, LiAlH₄/LiI‐mediated syn‐stereoselective 1,3‐asymmetric reduction, and phenyliodine bis(trifluoroacetate) (=[bis(trifluoroacetoxy)iodo]benzene; PIFA) mediated oxidative spirocyclization.     

Electrochemical Determination of L‐Lactate Using Phenylboronic Acid Monolayer‐Modified Electrodes

The surface of a gold (Au) disk electrode was modified with a self‐assembled monomolecular layer of dithiobis(4‐butylamino‐m‐phenylboronic acid) (DTBA‐PBA) to prepare L ‐lactate‐sensitive electrodes. The DTBA‐PBA‐modified electrodes exhibited an attenuated cyclic voltammogram (CV) for the Fe(CN)₆^3? ion in the presence of L ‐lactate, as a result of the formation of phenylboronate ester of L ‐lactate accompanied with the addition of OH^? ion to the boron atom. In other words, the negatively charged DTBA‐PBA monolayer blocked the electrode surface from the access of the Fe(CN)₆^3?/4? ions. Thus, the DTBA‐PBA monolayer‐modified Au electrode can be used for determining L ‐lactate on the basis of the change in redox current of Fe(CN)₆^3?/4? ions. The calibration graph useful for determining 1–30 mM L ‐lactate was obtained.     

15N Chemically Induced Dynamic Nuclear Polarization (15N‐CIDNP) Investigations of the Peroxynitrite Decay and Nitration of N‐Acetyl‐L‐tyrosine

During the decay of (¹⁵N)peroxynitrite (O?¹⁵NOO ^? ) in the presence of N‐acetyl‐L ‐tyrosine (Tyrac) in neutral solution and at 268 K, the ¹⁵N‐NMR signals of ¹⁵NO and ¹⁵NO show emission (E) and enhanced absorption (A) as it has already been observed by Butler and co‐workers in the presence of L ‐tyrosine (Tyr). The effects are built up in radical pairs [CO , ¹⁵NO ]^S formed by O? O bond scission of the (¹⁵N)peroxynitrite? CO₂ adduct (O?¹⁵NO? OCO ). In the absence of Tyrac and Tyr, the peroxynitrite decay rate is enhanced, and ¹⁵N‐CIDNP does not occur. This is explained by a chain reaction during the peroxynitrite decay involving N₂O₃ and radicals NO ^. and NO . The interpretation is supported by ¹⁵N‐CIDNP observed with (¹⁵N)peroxynitrite generated in situ during reaction of H₂O₂ with N‐acetyl‐N‐(¹⁵N)nitroso‐dl ‐tryptophan ((¹⁵N)NANT) at 298 K and pH 7.5. In the presence of Na¹⁵NO₂ at pH 7.5 and in acidic solution, ¹⁵N‐CIDNP appears in the nitration products of Tyrac, 1‐(¹⁵N)nitro‐N‐acetyl‐L ‐tyrosine (1‐¹⁵NO₂‐Tyrac) and 3‐(¹⁵N)nitro‐N‐acetyl‐L ‐tyrosine (3‐¹⁵NO₂‐Tyrac). The effects are built up in radical pairs [Tyrac ^. , ¹⁵NO ]^F formed by encounters of independently generated radicals Tyrac ^. and ¹⁵NO . Quantitative ¹⁵N‐CIDNP studies show that nitrogen dioxide dependent reactions are the main if not the only pathways for yielding both nitrate and nitrated products.