Thamyongkit Patchanita, Bhise Anil D, Taniguchi Masahiko, Lindsey Jonathan S
Department of Chemistry, North Carolina State University, Raleigh, NC 27695-8204, USA.
J Org Chem. 2006 Feb 3;71(3):903-10. doi: 10.1021/jo051806q.
The synthesis of porphyrin precursors requires the successive introduction of substituents at the pyrrole alpha- and alpha'-positions (2- and 5-, respectively). An alpha-pyrrole substituent that serves as a temporary masking agent and is not deactivating would greatly facilitate such syntheses, particularly for beta-(3,4)-unsubstituted pyrroles, but has heretofore not been available. A series of alpha-RS groups (R = Me, Et, n-decyl, Ph) have been investigated in this regard, including the determination of the kinetics of substitution at the pyrrolic 3-, 4-, and 5-positions and the application to dipyrromethane formation. The RS group was readily introduced into the pyrrole alpha-position by the reaction of 2-thiocyanatopyrrole (prepared from pyrrole, ammonium thiocyanate, and iodine) and the corresponding Grignard reagent RMgBr. Each 2-alkylthio group activated the pyrrole ring toward deuteration at the 3- or 5- (vs 4-) position. The dipyrromethane synthesis was carried out using a 2:1 ratio of 2-(RS)pyrrole/benzaldehyde with a catalytic amount of InCl3 at room temperature in the absence of any solvent. The alpha-RS group was removed by hydrodesulfurization using Raney nickel or nickel complexes. This stoichiometric synthesis using the alpha-RS-protected pyrrole is in contrast to the traditional synthesis that employs an aldehyde and 25-100 mol equiv of pyrrole. Six meso-substituted dipyrromethanes were prepared by the reaction of 2-(n-decylthio)pyrrole/aldehyde/InCl3 (2.2:1:0.2 ratio) followed by hydrodesulfurization. Other reactions of the 1,9-bis(RS)dipyrromethane include oxidation to give (i) the 1,9-bis(RS)dipyrrin or (ii) the 1,9-bis(RSO2)dipyrromethane, which underwent subsequent complexation with dibutyltin dichloride. In summary, under mild reaction conditions, the 2-alkylthio group is readily introduced to the pyrrole nucleus, directs electrophilic substitution to the 5-position, and is readily removed as required for elaboration of porphyrinic precursors.
卟啉前体的合成需要在吡咯的α-位和α'-位(分别为2-位和5-位)依次引入取代基。一种作为临时掩蔽剂且不会使反应失活的α-吡咯取代基将极大地促进此类合成,特别是对于β-(3,4)-未取代的吡咯,但迄今为止尚未有可用的此类取代基。在这方面已经研究了一系列α-RS基团(R = 甲基、乙基、正癸基、苯基),包括测定在吡咯的3-位、4-位和5-位的取代动力学以及在二吡咯甲烷形成中的应用。通过2-硫氰基吡咯(由吡咯、硫氰酸铵和碘制备)与相应的格氏试剂RMgBr反应,RS基团很容易引入到吡咯的α-位。每个2-烷硫基使吡咯环在3-位或5-位(相对于4-位)对氘化更具活性。二吡咯甲烷的合成是在室温下,在没有任何溶剂的情况下,使用2-(RS)吡咯/苯甲醛2:1的比例以及催化量的三氯化铟进行的。α-RS基团通过使用阮内镍或镍配合物进行加氢脱硫而被除去。这种使用α-RS保护的吡咯的化学计量合成与采用醛和25 - 100摩尔当量吡咯的传统合成形成对比。通过2-(正癸硫基)吡咯/醛/三氯化铟(2.2:1:0.2的比例)反应然后加氢脱硫制备了六种中位取代的二吡咯甲烷。1,9-双(RS)二吡咯甲烷的其他反应包括氧化生成(i)1,9-双(RS)二吡咯或(ii)1,9-双(RSO₂)二吡咯甲烷,后者随后与二丁基二氯化锡络合。总之,在温和的反应条件下,2-烷硫基很容易引入到吡咯核中,将亲电取代导向5-位,并且根据卟啉前体的制备需要很容易被除去。
