Practical way for the synthesis of 3,3′-bis-substituted benzo[d][1,2]oxaphosphole 2-oxides by phosphonylation of in situ generated o-quinone methides

Phosphonylation of the pretreated 2-(hydroxymethyl)phenol derivatives with acetic anhydride using trialkylphosphites as the nucleophilic reagents was reported, providing a practical way to the synthesis of novel highly steric 3,3′-bis-substituted benzo[d][1,2]oxaphosphole 2-oxides.     

A facile and effective synthesis of lamivudine 5′-diphosphate

We report on the first solution synthesis of lamivudine 5′-diphosphate in both high yield and purity. Efficient synthesis of lamivudine 5′-monophosphate was obtained through lamivudine H-phosphonate oxidation by (−)-(8,8-dichlorocamphorylsulfonyl)oxaziridine.Diphosphorylation was performed by nucleophilic substitution of the phosphorimidazolate derivative of lamivudine. HPLC coupled with UV or MS detection was found to be an invaluable tool for the follow-up of phosphorylation reactions.     

Solid‐Phase Synthesis of the Aged‐Nonapeptide‐Nerve‐Agent Adduct of Butyrylcholinesterase as Reference Materials for Analytical Verification

Two pathways were developed and investigated for the synthesis of the ‘aged’‐nonapeptide nerve‐agent bioadduct of human butyrylcholinesterase (BuChE). Considering the fast ageing of nerve‐agent adducts of BuChE in patients and biomedical samples this target molecule is of paramount relevance for quantitative analysis with respect to the Chemical Weapons Convention. Two approaches using a precursor bearing a hydroxyl on its phosphonyl moiety and a benzyl protected precursor were considered. Several impurities were identified and circumvented during the optimization of the peptide synthesis step. The ‘aged’‐nonapeptide adduct was successfully synthesized by solid‐phase‐peptide‐synthesis (SPPS ).     

Aryl-2,3-oxaphosphabicyclo[2.2.2]octene derivatives—the precursors of oxoarylphosphine oxides (aryl metaphosphonates)

The Baeyer-Villiger oxidation of 7-phosphanorbornene 7-oxides with sterically demanding substituents on the phosphorus atom (4a-d) by m-chloroperbenzoic acid afforded the title products (5a-d) as a mixture of two regioisomers (A and B). Isomer A, the result of thermodynamic control, was stable, while isomer B, the product of kinetic control, underwent decomposition and/or epoxidation. Single crystal X-ray analysis of P-(2,4,6-triisopropylphenyl) oxaphosphabicyclooctene (5Ac) was not only useful in the evaluation of its structure, but, for the first time in the literature, a low-coordinated arylmetaphosphonate (15c) formed by fragmentation on X-ray irradiation could also be detected. The precursors (5Aa-c) were utilized in the thermoinduced and UV light-mediated fragmentation-related phosphorylations of alcohols. Beside the well-known elimination-addition mechanism via the metaphosphonate intermediate (15), a novel addition-elimination route involving a species with a pentavalent pentacoordinated phosphorus atom (16) was also substantiated.     

脂肪酰胺水解酶催化三联体膦酰化失活的机理：一个模型体系的理论研究

甲基花生四烯基氟代膦酸酯(MAFP)是脂肪酰胺水解酶(FAAH)的一个抑制剂. FAAH的丝氨酸241(Ser241)-丝氨酸217(Ser217)-赖氨酸142(Lys142)催化三联体被MAFP膦酰化后将导致FAAH失活. 本文采用B3LYP/6-311G(d,p)和MP2/6-311G(d,p)方法及一个简化的计算模型体系对这个膦酰化抑制反应进行理论研究. 考虑了两种反应途径. Path A涉及FAAH的催化三联体的所有残基, 是一个分步的加成-消除过程, 形成两性离子的三角双锥中间体, 其中第一步反应是决速步骤. 在这个反应途径中, Ser217和Lys142对亲核试剂Ser241起到碱催化活化的作用, 而Ser217充作Lys142和Ser241之间的桥梁. 此外, 溶剂中的一个水分子作为Lys142和MAFP间的“氢桥”具有关键的作用, 通过给出和接收质子促进了长距离的质子转移. Path B是催化三联体中的残基Lys142被突变为丙氨酸以后的膦酰化反应, 也是一个分步过程. 水的本体溶剂效应通过极化连续介质模型(PCM)估算. 计算结果显示膦酰化反应的Path A是优势途径, 在水溶液中其决速步骤的活化能垒为64.9 kJ·mol-1. FAAH催化三联体中残基Lys142的变异会降低膦酰化反应的速率, 这与实验结果相一致.     

σ-P Ligands: convenient syntheses of N-methyl-1,3-benzazaphospholes

A convenient three-step route to 1,5-dimethyl-1,3-benzazaphosphole via Cu- or Pd-catalyzed phosphonylation of 2-iodo-4-methylaniline, reduction to 2-phosphino-4-methylaniline, and disproportionative cyclization with excess formaldehyde is reported. N-Methylbenzazaphospholes can be functionalized in the 2-position via α-CH-lithiation with tBuLi and are π-acidic σ²P-ligands.     

Synthesis of 2-phosphonylated imidazo[1,2-a]pyridines under catalyst-free conditions

A series of novel 2-phosphonylated imidazo[1,2-a]pyridines was accessed from CN coupling of chloroethynylphosphonates and commercially available N-unsubstituted 2-aminopyridines. The product yield depends on the nature and position of the substituent in the pyridine ring.     

One-pot synthesis of phosphorodiamidothioates using N-heterocyclic phosphine (NHP)-thiourea

N-heterocyclic phosphine (NHP)-thiourea-promoted thiophosphation of thiols has been developed for the synthesis of phosphorodiamidothioates under additive-, metal-free reaction conditions. This reaction takes place at room temperature and exhibits good functional group tolerance. The key to success is that the thiourea group can serve as an excellent leaving group, which is tethered with NHP moiety.     

New benzotriazole-based reagents for the phosphonylation of various N-, O-, and S-nucleophiles

Benzotriazole surrogates showing higher stabilities than the corresponding chlorophosphates, allow phosphonylation of a variety of N-, O-, and S-nucleophiles in good yields.