水对二氧化碳插入TpRu(PPh3)(CH3CN)H生成甲酸根配合物的影响

分别研究了在干燥THF及H2O/THF条件下CO2与TpRu(PPh3)(CH3CN)H(Tp=Hydrotris(pyrazolyl)borate)的反应, 发现水对CO2插入TpRu(PPh3)(CH3CN)H的反应具有显著促进作用. 原位高压NMR研究显示, 在水存在下, CO2插入Ru-H键形成水合甲酸根配合物TpRu(PPh3)(CH3CN)(η1-OCHO)H2O, 其中甲酸根配体与溶剂中水分子形成分子间氢键. B3LYP水平的理论计算表明, CO2插入TpRu(PPh3)(CH3CN)H 中Ru-H键的能垒由于水的存在而显著降低; 在过渡态, CO2分子中碳原子的亲电性由于其氧原子与水分子形成氢键而得到增强. TpRu(PPh3)(CH3CN)(η1-OCHO)*H2O很快转化为另一甲酸根配合物TpRu(PPh3)(H2O)(η1-OCHO), 并与之达成平衡. 后者由于甲酸根配体与水分子配体间形成分子内氢键而稳定.     

单氢钌配合物催化氢化苯乙烯的位阻效应

研究了溶剂分别为 THF, H2O/THF, CH3CN/THF以及ROH/THF (R＝Me, Et, iso-Pr, tert-Bu)条件下TpRuH(PPh3)- (CH3CN) [Tp＝hydrotris(pyrazolyl)borate]催化氢化苯乙烯生成乙基苯的反应, 发现向干燥THF体系中添加微量 H2O, CH3CN或ROH对催化反应都具有显著的促进作用. 催化机理研究表明, 小分子添加物首先取代TpRuH(PPh3)(CH3CN)中的PPh3配体形成中间体TpRuH(CH3CN)L (L＝H2O, CH3CN或ROH), 降低空间位阻, CH3CN配体随后被苯乙烯取代生成中间体 TpRuH(H2C＝CHPh)L; η2-苯乙烯插入Ru—H键后形成的Ru-烷基中间物与H2反应生成η2-H2配合物 TpRu(CH2CH2Ph)(H2)L或TpRu[CH(CH3)Ph](H2)L, 进而发生σ-复分解反应生成乙基苯完成催化循环.     

钌配合物催化氢化CO2生成甲酸反应中的醇促进效应

在水合钌配合物[TpRu(PPh₃)₂(H₂O)]BF₄ [Tp＝hydrotris(pyrazolyl) borate]催化氢化二氧化碳生成甲酸的反应中观察到醇对反应的促进作用. 利用原位高压核磁共振跟踪催化反应过程的结果表明, 在甲醇溶液中, [TpRu(PPh₃)₂(H₂O)]BF₄在三乙胺和H₂作用下转化为TpRu(PPh₃)₂H. 二氧化碳插入Ru—H生成甲酸根配合物TpRu(PPh₃)₂(η¹-OCHO)•HOCH₃, 其中的甲酸根配体与醇分子间形成分子间氢键. 该甲酸根配合物随即转化为另一个甲酸根配合物TpRu(PPh₃)(CH₃OH)(η¹-OCHO)并与之达成平衡, 后者由于存在分子内氢键而稳定. 考虑到这两个甲酸根配合物在催化反应中的稳定性, 它们应该不在主要的催化循环内. 提出了配合物[TpRu(PPh₃)₂(H₂O)]BF₄在几种醇溶液中催化氢化二氧化碳生成甲酸的催化循环机理, 催化循环的关键中间体可能是TpRu(PPh₃)(ROH)H. 该中间体能同时转移负氢及醇配体中的氢质子到接近的二氧化碳分子上生成甲酸, 并吸收H₂生成过渡态TpRu(PPh₃)(OR)(H₂). 该过渡态经过σ-复分解反应重新生成TpRu(PPh₃)(ROH)H完成催化循环.     

烃基取代茚基钌羰基化合物的合成及晶体结构(英文)

配体C9H7R(R=CH2CH2CH3(1),CH(CH3)2(2),C5H9(3),CH2C6H5(4),CH2CH=CH2(5))分别与Ru3(CO)12在二甲苯或庚烷中加热回流,得到了6个双核配合物[(η5-C9H6R)Ru(CO)(μ-CO)]2(R=CH2CH2CH3(6),CH(CH3)2(7),C5H9(8),CH2C6H5(9),CH2CH=CH2(10))和[(η5-C9H6)(H3CH2C)CHCH(CH2CH3)(η5-C9H6)][Ru(CO)(μ-CO)]2(11)。通过元素分析、红外光谱、核磁共振氢谱对配合物的结构进行了表征,并用X-射线单晶衍射法测定了配合物6,9,10和11的结构。     

新型含2,5-二-（3,5-二甲基吡唑-4-巯基）-1,3,4-噻二唑-M(M=Co2+,Cd2+,Mn2+)配合物的合成、晶体结构及其抑菌活性研究

将配体L[2,5-二-(3,5-二甲基吡唑-4-巯基)-1,3,4-噻二唑]与Co(NO3)2 6H2O,Cd(NO3)2 4H2O和MnCl2 4H2O进行配位反应,得到三个配合物[Co(L)2(H2O)4](NO3)2 4(CH3CH2OH)(1),[Cd(L)2(H2O)4](NO3)2 4(CH3CH2OH)(2),[Mn(L)2(Cl)2(CH3OH)2]2(CH3OH)(3),并用元素分析,FT-IR和X射线单晶衍射进行了表征.分析结果表明,配体L呈"U"形,配合物1～3呈"S"形.配合物中Co(II),Cd(II),Mn(II)的配位环境均为扭曲八面体,每个金属离子同时和两个配体进行配位.配体和配合物体外抑菌活性研究结果表明,配体及其配合物都有一定的抑菌活性.     

Cu(Ⅰ)与乙酰乙酸乙酯、氰基乙酸乙酯、丙二腈及中性膦配合物的电化学合成

用牺牲金属阳极的电化学方法在非水溶剂中合成了一价铜配合物 Cu( ) [CH( CN) 2 ]( PPh3) 2 ,Cu( )( Me COCHCO2 Et) ( PPh3) 2 及 Cu( ) ( CNCHCO2 Et) ( PPh3) 3· Me CN,对配合物进行了元素分析 ,IR,1 H NMR和 1 3C NMR测试及表征 ,并讨论了反应机理。     

不饱和取代水杨醛亚胺镍的合成及其对乙烯聚合的催化性能

 合成了烯丙基对甲基水杨醛亚胺和环戊烯基对甲基水杨醛亚胺配体,并与trans-［NiCl(Ph)(PPh3)2］反应合成了配合物［O-(3-allyl)(5-CH3)C6H2-o-C(H)∶N-2,6-C6H3(i-Pr)2］Ni(PPh3)(Ph)和［O-(3-cyclopentenyl)(5-CH3)C6H2-o-C(H)∶N-2,6-C6H3(i-Pr)2］Ni(PPh3)(Ph),以MS,1H NMR和元素分析对配体及配合物进行了表征. 在Ni(COD)2(COD环辛二烯)助催化下成功地催化乙烯聚合,在808 kPa的压力下,前者配合物的最高活性可达265 kg/(mol·h),聚乙烯的粘均分子量在(0.95～3.85)×104间; 后者配合物的最高活性可达434 kg/(mol·h),聚乙烯的粘均分子量在(0.87～5.81)×104间. 添加THF,CH3COOEt和EtOEt对催化聚合性能无显著影响,添加甲基丙烯酸甲醇则不仅不发生共聚,相反严重降低了催化活性.     

基于两个取代四甲基环戊二烯基配体的金属羰基化合物的合成及晶体结构(英文)

配体[C5Me4HR][R=4-Br Ph(1),(Me C5H3N)CH2(2)]分别与Mo(CO)6,Ru3(CO)12和Fe(CO)5在二甲苯中加热回流,得到了6个双核配合物trans-[η5-C5Me4R]2Mo2(CO)6(3,4),trans-[(η5-C5Me4R)Ru(CO)(μ-CO)]2(5,6)和trans-[η5-(C5Me4R)Fe(CO)(μ-CO)]2(7,8)。通过元素分析、红外光谱、核磁共振氢谱对配合物的结构进行了表征,并用X-射线单晶衍射法测定了配合物3,5,6和8的结构。     

Synthesis and characterization of MH···HOR dihydrogen bonded ruthenium and osmium complexes(η~5-C_5H_4CH_2OH)MH(PPh_3)_2(M = Ru,Os)

Treatment of RuCl2(PPh3)3 with 6-dimethylaminopentafulvene in THF in the presence of water produced(η5-C5H4CHO) RuCl(PPh3)2, which was reduced by NaBH4 to give the Ru–H···HO dihydrogen bonded complex(η5-C5H4CH2OH) RuH(PPh3)2. The dihydrogen bonded complex(η5-C5H4CH2OH)RuH(PPh3)2 could also be synthesized by the reduction of complex(η5-C5H4CHO)RuH(PPh3)2, which was obtained by the reaction of RuHCl(PPh3)3 with 6-dimethylaminopentafulvene in the presence of water. The analogous dihydrogen bonded osmium complex(η5-C5H4CH2OH)OsH(PPh3)2 was similarly prepared. Single crystal structures and DFT calculations support the presence of intra-molecular H···H interaction, with separations of around 1.9 to 2.0 .     

含氮原子桥联吡咯基稀土金属双核配合物的合成及催化ε-己内酯的开环聚合反应

RE(CH2SiMe3)3(THF)2和1.5 equiv.(C4H3NHCH2)2NCH3(1)反应合成得到含氮原子桥联吡咯基稀土金属双核配合物[η1∶η1∶η1-(C4H3NCH2)2NCH3]RE{μ-η5∶η5∶η1-(C4H3NCH2)2NCH3}RE[η1∶η1∶η1-(C4H3NCH2)2NCH3](THF)[RE=Y(2),Er(3),Yb(4)],所得配合物经过核磁共振、红外和元素分析表征,配合物2和4经单晶X-Ray进一步确认结构.同时研究了稀土配合物作为单一组分催化剂催化ε-内酯的开环聚合反应.     

单氢钌配合物与水和2,2,2-三氟乙醇的作用机理

利用原位¹H和³¹P NMR对单氢钌配合物TpRu(PPh₃)(CH₃CN)H [Tp＝hydrotris(pyrazolyl)borate]与H₂O和酸性HOCH₂CF₃的反应进行了研究, 结果显示相应的反应产物分别是TpRu(PPh₃)(CH₃CN)(OH) 和TpRu(PPh₃)(CH₃CN)(OCH₂CF₃). 观察到反应过程中Ru-H…HOH和Ru-H…HOCH₂CF₃分子间的氢键作用. 提出了生成TpRu(PPh₃)(CH₃CN)(OH)和TpRu(PPh₃)(CH₃CN)(OCH₂CF₃)的不同作用机理. 在水存在下, TpRu(PPh₃)(CH₃CN)H 与H₂O反应, 经过中间体TpRu(PPh₃)(H₂O)H和TpRu(PPh₃)(OH)(η²-H₂)生成产物TpRu(PPh₃)(CH₃CN)(OH). 而TpRu(PPh₃)(CH₃CN)H与酸性HOCH₂CF₃反应时, 单氢配体被质子化形成中间体[TpRu(PPh₃)(CH₃CN)- (η²-H₂)](OCH₂CF₃), 进而转变成产物TpRu(PPh₃)(CH₃CN)(OCH₂CF₃). TpRu(PPh₃)(CH₃CN)(OCH₂CF₃)与H₂作用, 经中间体TpRu(PPh₃)(HOCH₂CF₃)H生成TpRu(PPh₃)(η²-H₂)H.     

New iridacyclohexadienes and iridabenzenes by [2+2+1] cyclotrimerization of alkynes and facile interconversion between iridacyclohexadienes and iridabenzenes

Iridabenzenes [Ir[=CHCH=CHCH=C(CH2R)](CH3CN)2(PPh3)2]2+ (R=Ph 4 a, R=p-C6H4CH3 4 b) are obtained from the reactions of H+ with iridacyclohexadienes [Ir[-CH=CHCH=CHC(=CH-p-C6H4R')](CO)(PPh3)2]+ (R'=H 3 a, R'=CH3 3 b), which are prepared from [2+2+1] cyclotrimerization of alkynes in the reactions of [Ir(CH3CN)(CO)(PPh3)2]+ with HC[triple chemical bond]CH and HC[triple chemical bond]CR. Iridabenzenes 4 react with CO and CH3CN in the presence of NEt3 to give iridacyclohexadienes [Ir[-CH=CHCH=CHC(=CHR)](CO)2(PPh3)2]+ (6) and [Ir[-CH=CHCH=CHC(=CHR)](CH3CN)2(PPh3)2]+ (7), respectively. Iridacyclohexadienes 6 and 7 also convert to iridabenzenes 4 by the reactions with H+ in the presence of CH3CN. Alkynyl iridacyclohexadienes [Ir[-CH=CHCH=CHC(=CH-p-C6H4R')](-C[triple chemical bond]CH)(PPh3)2] (8) undergo a cleavage of C[triple chemical bond]C bond by H+/H2O to produce [Ir[-CH=CHCH=CHC(=CH-p-C6H4R')](-CH3)(CO)(PPh3)2] (10) via facile inter-conversion between iridacyclohexadienes and iridabenzenes.     

Octahedral Ru(II) amido complexes TpRu(L)(L')(NHR) (Tp = hydridotris(pyrazolyl)borate; L = L' = P(OMe)3 or PMe3 or L = CO and L' = PPh3; R = H,Ph, or tBu): synthesis,characterization, and reactions with weakly acidic C-H bonds

The octahedral Ru(II) amine complexes [TpRu(L)(L')(NH(2)R)][OTf] (L = L' = PMe(3), P(OMe)(3) or L = CO and L' = PPh(3); R = H or (t)Bu) have been synthesized and characterized. Deprotonation of the amine complexes [TpRu(L)(L')(NH(3))][OTf] or [TpRu(PMe(3))(2)(NH(2)(t)Bu)][OTf] yields the Ru(II) amido complexes TpRu(L)(L')(NH(2)) and TpRu(PMe(3))(2)(NH(t)Bu). Reactions of the parent amido complexes or TpRu(PMe(3))(2)(NH(t)Bu) with phenylacetylene at room temperature result in immediate deprotonation to form ruthenium-amine/phenylacetylide ion pairs, and heating a benzene solution of the [TpRu(PMe(3))(2)(NH(2)(t)Bu)][PhC(2)] ion pair results in the formation of the Ru(II) phenylacetylide complex TpRu(PMe(3))(2)(C[triple bond]CPh) in >90% yield. The observation that [TpRu(PMe(3))(2)(NH(2)(t)Bu)][PhC(2)] converts to the Ru(II) acetylide with good yield while heating the ion pairs [TpRu(L)(L')(NH(3))][PhC(2)] yields multiple products is attributed to reluctant dissociation of ammonia compared with the (t)butylamine ligand (i.e., different rates for acetylide/amine exchange). These results are consistent with ligand exchange reactions of Ru(II) amine complexes [TpRu(PMe(3))(2)(NH(2)R)][OTf] (R = H or (t)Bu) with acetonitrile. The previously reported phenyl amido complexes TpRuL(2)(NHPh) [L = PMe(3) or P(OMe)(3)] react with 10 equiv of phenylacetylene at elevated temperature to produce Ru(II) acetylide complexes TpRuL(2)(C[triple bond]CPh) in quantitative yields. Kinetic studies indicate that the reaction of TpRu(PMe(3))(2)(NHPh) with phenylacetylene occurs via a pathway that involves TpRu(PMe(3))(2)(OTf) or [TpRu(PMe(3))(2)(NH(2)Ph)][OTf] as catalyst. Reactions of 1,4-cyclohexadiene with the Ru(II) amido complexes TpRu(L)(L')(NH(2)) (L = L' = PMe(3) or L = CO and L' = PPh(3)) or TpRu(PMe(3))(2)(NH(t)Bu) at elevated temperatures result in the formation of benzene and Ru hydride complexes. TpRu(PMe(3))(2)(H), [Tp(PMe(3))(2)Ru[double bond]C[double bond]C(H)Ph][OTf], [Tp(PMe(3))(2)Ru=C(CH(2)Ph)[N(H)Ph]][OTf], and [TpRu(PMe(3))(3)][OTf] have been independently prepared and characterized. Results from solid-state X-ray diffraction studies of the complexes [TpRu(CO)(PPh(3))(NH(3))][OTf], [TpRu(PMe(3))(2)(NH(3))][OTf], and TpRu(CO)(PPh(3))(C[triple bond]CPh) are reported.     

Regioselective nucleophilic addition of triphenylphosphine to the nitrosylruthenium alkynyl complexes having a hydrotris(pyrazol-1-yl)borate: formation of phosphonio-alkenyl, alkynyl, and allenyl species

A nitrosylruthenium alkynyl complex of TpRuCl(C[triple bond]CPh)(NO)(1a) was reacted with PPh3 in the presence of HBF4.Et2O at room temperature to give a beta-phosphonio-alkenyl complex (E)-[TpRuCl{CH=C(PPh3)Ph}(NO)]BF4(2.BF4). On the other hand, for gamma-hydroxyalkynyl complexes TpRuCl{C[triple bond]CC(R)2OH}(NO)(R = Me (1b), Ph (1c), H (1d)), similar treatments with PPh3 were found to give gamma-phosphonio-alkynyl [TpRuCl{C[triple bond]CC(Me)2PPh3}(NO)]BF4(3.BF4),alpha-phosphonio-allenyl [TpRuCl{C(PPh3)=C=CPh2}(NO)]BF4(4.BF4), and a novel product of gamma-hydroxy-beta-phosphonio-alkenyl (E)-[TpRuCl{CH=C(PPh3)CH2OH}(NO)]BF4(5.BF4), respectively. Dominant factors for the selectivity in affording 3-5 were associated with the steric congestion and electronic properties at the gamma-carbons, along with those around the metal fragment. From the bis(alkynyl) complex TpRu(C[triple bond]CPh)2(NO)6, a bis(beta-phosphonio-alkenyl)(E,E)-[TpRu{CH=C(PPh3)Ph}2(NO)](BF4)2{7.(BF4)2} was produced at room temperature. However, similar reactions at 0 degrees C gave an alkynyl beta-phosphonio-alkenyl complex (E)-[TpRu(C[triple bondCPh){CH=C(PPh3)Ph}(NO)]BF4(8.BF4) as a sole product, of which additional hydration in the presence of HBF4.Et2O afforded a [small beta]-phosphonio-alkenyl ketonyl (E)-[TpRu{CH2C(O)Ph}{CH=C(PPh3)Ph}(NO)]BF(.9BF4). Five complexes, 2-5 and 7 were crystallographically characterized.     

Dihydrogen-bond-promoted catalysis: catalytic hydration of nitriles with the indenylruthenium hydride complex (eta(5)-C(9)H(7))Ru(dppm)H (dppm = bis(diphenylphosphino)methane)

The indenylruthenium hydride complex (eta(5)-C(9)H(7))Ru(dppm)H was found to be active in catalyzing the hydration of nitriles to amides. The chloro analogue (eta(5)-C(9)H(7))Ru(dppm)Cl was, however, found to be inactive. Density functional theory calculations at the B3LYP level provide explanations for the effectiveness of the hydride complex and the ineffectiveness of the chloro complex in the catalysis. It is learned that the presence of a Ru-H.H-OH dihydrogen-bonding interaction in the transition state lowers the reaction barrier in the case of (eta(5)-C(9)H(7))Ru(dppm)H, but in the chloro system, the corresponding transition state does not contain this type of interaction and the reaction barrier is much higher. A similar dihydrogen-bond-promoting effect is believed to be responsible for the catalytic activity of the hydrotris(pyrazolyl)borato (Tp) ruthenium complex TpRu(PPh(3))(CH(3)CN)H in CH(3)CN hydration. The chloro analogue TpRu(PPh(3))(CH(3)CN)Cl shows no catalytic activity.     

Formation and coordination modes of the C4E4 moiety (E = COOMe) bound to two palladium(II) moieties

The transmetallation of the palladacyclopentadiene complex Pd{C(COOMe)C(COOMe)C(COOMe)C(COOMe)}(bipy) with the dicationic Pd(II) complex [Pd(bipy)(CH(3)CN)(2)][BF(4)](2) afforded a terminally σ-palladated diene complex [Pd(2){μ-η(1):η(1)-C(COOMe)C(COOMe)C(COOMe)C(COOMe)}(bipy)(2)(CH(3)CN)(2)][BF(4)](2). It was revealed by X-ray crystallographic analysis that replacement of the acetonitrile ligands in a terminally σ-palladated diene complex with PPh(3) ligands resulted in the conformation change of the σ-palladated diene moiety from skewed s-cis to planar s-trans. Treatment of a bis-triphenylphosphine dipalladium complex [Pd(2)(PPh(3))(2)(CH(3)CN)(4)][PF(6)](2) with dimethoxyacetylene dicarboxylate (DMAD) (1 equiv.) in acetonitrile resulted in the insertion of DMAD to the Pd-Pd bond to afford [Pd(2){μ-η(1):η(1)-C(COOMe)C(COOMe)}(PPh(3))(2)(CH(3)CN)(4)][PF(6)](2). Addition of the second DMAD gave the ylide-type complex [Pd(2){μ-η(2):η(3)-C(COOMe)C(COOMe)C(COOMe)C(COOMe)(PPh(3))}(PPh(3))(2)(CH(3)CN)(3)][PF(6)](2) of which the structure was determined by X-ray crystallographic analysis.     

Platinum(II)-mediated coupling reactions of acetonitrile with the exocyclic nitrogen of 9-methyladenine and 1-methylcytosine. Synthesis, NMR characterization, and X-ray structures of new azametallacycle complexes

The hydroxo complex cis-[L2Pt(mu-OH)]2(NO3)2, (L = PMePh2, 1a), in CH3CN solution, deprotonates the NH2 group of 9-methyladenine (9-MeAd) to give the cyclic trinuclear species cis-[L2Pt[9-MeAd(-H)]]3(NO3)3, (L = PMePh2, 2a), in which the nucleobase binds the metal centers through the N(1), N(6) atoms. In solution at room temperature, 2a slowly reacts with the solvent to form quantitatively the mononuclear azametallacycle cis-[L2PtNH=C(Me)[9-MeAd(-2H)]]NO3 (L = PMePh2, 3a), containing as anionic ligand the deprotonated form of molecule N-(9-methyl-1,9-dihydro-purin-6-ylidene)-acetamidine. In the same experimental conditions, the hydroxo complex with PPh3 (1b) forms immediately the insertion product 3b. Single-crystal X-ray analyses of 3a and 3b show the coordination of the platinum cation at the N(1) site of the purine moiety and to the N atom of the inserted acetonitrile, whereas the exocyclic amino nitrogen binds the carbon atom of the same CN group. The resulting six-membered ring is slightly distorted from planarity, with carbon-nitrogen bond distances for the inserted nitrile typical of a double bond [C(3)-N(2) = 1.292(7) Angstroms in 3a and 1.279(11) Angstroms in 3b], while the remaining CN bonds of the metallocycle are in the range of 1.335(8)-1.397(10) Angstroms. A detailed multinuclear 1H, 31P, 13C, and 15N NMR study shows that the nitrogen atom of the inserted acetonitrile molecule binds a proton suggesting for 3a,b an imino structure in solution. In DMSO and chlorinated solvents, 3a slowly releases the nitrile reforming the trinuclear species 2a, whereas 3b forms the mononuclear derivative cis-[L2Pt[9-MeAd(-H)]]NO3 (L = PPh3, 4b), in which the adeninate ion chelates the metal center through the N(6) and N(7) atoms. Complex 4b is quantitatively obtained when 1b reacts with 9-MeAd in DMSO and can be easily isolated if the reaction is carried out in CH(2)Cl(2). In CH(3)CN solution, at room temperature, 4b slowly converts into 3b indicating that the insertion of acetonitrile is a reversible process. A similar metal-mediated coupling reaction occurs when 1a,b react with 1-methylcytosine (1-MeCy) in CH(3)CN. The resulting complexes, cis-[L(2)PtNH=C(Me)[1-MeCy(-2H)]]NO3, (L = PMePh2, 5a and PPh3, 5b), contain the deprotonated form of the ligand N-(1-methyl-2-oxo-2,3-dihydro-1H-pyrimidin-4-ylidene)-acetamidine. The X-ray analysis of 5a shows the coordination of the metal at the N(3) site of the pyrimidine cycle and to the nitrogen atom of the acetonitrile, with features of the six-membered metallocycle only slightly different from those found in 3a and 3b. In CD3CN/CH3(13)CN solution complexes 5a,b undergo exchange of the inserted nitrile, while in DMSO or chlorinated solvents they irreversibly release CH3CN to form species not yet fully characterized. No insertion of CH3CN occurs when the hydroxo complexes are stabilized by PMe3 and PMe2Ph.