Site-directing an intense multipoint covalent attachment (MCA) of mutants of the Geobacillus thermocatenulatus lipase 2 (BTL2): Genetic and chemical amination plus immobilization on a tailor-made support

Immobilized enzymes are preferred over their soluble counterparts due to their robustness in harsh industrial processes; the most stable enzyme derivatives are often produced through multipoint covalent attachment (MCA). However, most enzymes are unable to establish optimal MCA to electrophile-type supports given the heterogeneous distribution and/or low content of primary amino groups on their surfaces; this restricts both the diversity of areas prone to react and the number of attachments to the support. To overcome this we propose combining site-directed immobilization and protein engineering to increase the number of bonds between a specific enzyme surface and a tailor-made support. We applied this novel strategy to engineered mutants of the lipase 2 from Geobacillus thermocatenulatus with one Cys exposed residue, that after genetic amination and/or chemical amination, were immobilized on glyoxyl-disulfide support using a site-directed MCA protocol. Two highly stabilized derivatives of chemically aminated lipase variants, in which site-directed MCA implied the surrounding surface of residues Cys344 or Cys40, were produced: the first one was 2.4-fold more productive than the reference derivative (648 g of hydrolyzed ester); the second derivative was 40% more selective (EPA/DHA molar ratio) and as active (1 μmol g catalyst⁻¹ min⁻¹) as the reference in the production of PUFAs.     

Synthetic α-(aminomethyl)-γ-butyrolactones and their anti-pancreatic cancer activities

Aminated α-methylene-γ-butyrolactones, which are readily synthesized with facile control of the diastereoisomerism, provide an economical and commercially-viable alternative to the use of aminated natural products. These aminoloactones, which exhibit excellent activity against three pancreatic cancer cell lines when measured at 10 μM—Panc-1, MIA PaCa-2, and BxPC-3—and are comparable to or better than parthenolide and dimethylaminoparthenolide (DMAPT, LC-1). It has also been shown that there is an effect on the biological activity depending on the identity of the amine.     

Reservoir catalysis: Rationalization of anomalous reaction orders in Pd-catalyzed amination of aryl halides

Reversible partitioning of a portion of the catalyst away from the active cycle provides a mechanistic rationalization of the anomalous reaction orders observed in the presence of additives. The concept of stable reservoir species leads to a practical protocol for maintaining a robust catalyst system that may be particularly useful for development of reactions under harsh conditions likely to lead to catalyst deactivation and incomplete turnover. Probing Pd-catalyzed amination reactions in the presence of competitive binding events reveals the key role that reservoir species connected reversibly to the catalytic cycle can play.     

One-step synthesis of N-protected glycosylamines from sugar hemiacetals

Protected pentofuranose, hexofuranose and hexopyranose hemiacetals were found to react efficiently with amines carrying a deactivating group (alkoxycarbonyl, tosyl or phosphoryl group) in the presence of a Lewis acid to give the corresponding, stable glycosylamines. Such glycosylamine derivatives are useful substrates for further elaboration into nitrogen-containing natural products and carbohydrate mimetics.     

Lanthanide iodides as promoters of acetonitrile amination. Molecular structure of MeC(NH)NHPr, MeC(NH)NHBu and {Dy[MeC(NH)NEt2]6}I3

Amination of acetonitrile by the amines MeNH₂, PrⁿNH₂, PrⁱNH₂, Bu^tNH₂, and Et₂NH is efficiently promoted by the lanthanide iodides LnI₂ (Ln = Nd, Dy, Tm), LnI₃ (Ln = Pr, Nd, Dy) and LnI₃(THF)₃ (Ln = Pr, Nd, Dy). The formed mono- and N,N′-disubstituted amidines MeC(NH)NHR (R = Prⁱ, Bu^t), MeC(NH)NEt₂, MeC(NR)NHR (R = Me, Prⁿ) were isolated mainly as the complexes with starting iodide of general composition LnI₂(amidine)_x (1) or LnI₃(amidine)_x (2) (x = 3-8). In the products 1, which evidently are the mixtures of LnI²⁺, and LnI₃ derivatives, the metal exists in trivalent state but one of the ligands actually is amidinate anion. A part of the generated amidines remains in the reaction solutions in free form. Heating of the 1 and 2 in vacuum at 150-200 °C affords corresponding amidine and the complexes with reduced amount of the amidine ligands LnI₂(amidine)_y (3) or LnI₃(amidine)_y (4) (y = 2-3). The products 3 and 4 displayed the same catalytic activity in the acetonitrile-amine cross-coupling as the initial iodides. SmI₂ and especially YbI₂ revealed lower activity. The structure of isopropylacetamidine (5), tert-butylacetamidine (6) and {Dy[MeC(NH)NEt₂]₆}I₃(MeCN) (7) were determined by X-ray diffraction analysis.     

高等植物中的谷氨酸脱氢酶及其生理作用

谷氨酸脱氢酶普遍存在于植物体内,它虽然不是植物吸收利用氮的主要成员,但在植物氮代谢中起着重要作用,高等植物的谷氨酶主要存在于线粒体中,以烟酰胺腺嘌呤二核苷酸（NADH）为辅酶,该酶分子量为255－258kD,由六个亚基组成,亚基包括α和β两种类型,存在七种同工酶形式,它在植物的衰老过程及逆境如高温和水份胁迫等状况下行使其铵同化功能,但在黑暗或碳胁迫条件下又能氧化脱铵从而为三羧酸循环提供骨架。     

Stereoselective entry into the d-GalNAc series starting from the d-Gal one: a new access to N-acetyl-d-galactosamine and derivatives thereof

A new stereoselective preparation of N-aceyl-d-galactosamine (1b) starting from the known p-methoxyphenyl 3,4-O-isopropylidene-6-O-(1-methoxy-1-methylethyl)-β-d-galactopyranoside (10) is described using a simple strategy based on (a) epimerization at C-2 of 10 via oxidation-reduction to give the talo derivative 11, (b) amination with configurational inversion at C-2 of 11 via a S_N2-type reaction on its 2-imidazylate, (c) anomeric deprotection of the p-methoxyphenyl β-d-galactosamine glycoside 14, (d) complete deprotection. Applying the same protocol to 2,3:5,6:3′,4′-tri-O-isopropylidene-6′-O-(1-methoxy-1-methylethyl)-lactose dimethyl acetal (4), directly obtained through acetonation of lactose, the disaccharide β-d-GalNAcp-(1→4)-d-Glcp (1a) was obtained with complete stereoselectivity in good (40%) overall yield from lactose.     

Synthesis of (2R,5S)-dihydroxymethyl-(3R,4R)-dihydroxypyrrolidine (DGDP) via stereoselective amination using chlorosulfonyl isocyanate

A stereoselective approach for synthesizing (2R,5S)-dihydroxymethyl-(3R,4R)-dihydroxypyrrolidine 1 (2,5-dideoxy-2,5-imino-d-glucitol, DGDP) was achieved using a seven-step approach starting from 2,3,4,6-tetra-O-benzyl-d-mannose (7). Key steps for the preparation of the title compound 1 involved the regioselective and diastereoselective amination of the cinnamyl anti-1,2-polybenzyl ethers 5 and 6 using chlorosulfonyl isocyanate (CSI) and ring cyclization to form the pyrrolidine ring. The reaction between anti-1,2-polybenzyl ether 5 and CSI in toluene at 0 degrees C afforded the corresponding anti-1,2-amino alcohol 4 as a major product with a diastereoselectivity of 16:1 in 76% yield. The mechanism underlying these reactions may be explained by the neighboring-group effect leading to the retention of stereochemistry.     

Improving biocatalytic microenvironment with biocompatible ε-poly-l-lysine for one step gluconic acid production in low pH enzymatic systems

Surface amine modification could not only improve the microenvironment near the active sites of enzyme, but also enhance the multi-point chemical crosslinking between the enzyme and carrier. The linear structured polymer of ε-poly-l-lysine (EPL) is an ideal donor of amino with much more exposed on the surface for enzyme attachment. Analysis of the result of dynamic light scattering (DLS) and circular dichroism (CD) demonstrated the favorable electrostatic interactions and negligible impact on the conformation of enzymes, Glucose Oxidase and Catalase (GOx&CAT). Titration and dissociation curve together with Zeta-potential characterization revealed that enzymes (EPL@GOx&CAT) under the protection of EPL had more stable structure and better activity and stability in acidic reaction environment. Meanwhile, the activity recovery of immobilized EPL@GOx&CAT increased to 1.56 times higher than that of GOx&CAT, and the acid resistance was improved by 1.44 times with the optimum pH shifting to acidic by 0.50 unit. The substrate affinity was raised with the decrease of K_m from 5.98 to 4.35 mg mL⁻¹. Thus, the gluconic acid production in low pH system could be increased by pH-engineering of the enzyme microenvironment via conjugation with positively charged polyelectrolyte.