Preparation of Neutral trans - cis [Ru(O2CR)2P2(NN)], Cationic [Ru(O2CR)P2(NN)](O2CR) and Pincer [Ru(O2CR)(CNN)P2] (P = PPh3, P2 = diphosphine) Carboxylate Complexes and their Application in the Catalytic Carbonyl Compounds Reduction

Salvatore Baldino; Steven Giboulot; Denise Lovison; Hans Günter Nedden; Alexander Pöthig; Antonio Zanotti-Gerosa; Daniele Zuccaccia; Maurizio Ballico; Walter Baratta

doi:10.1021/acs.organomet.1c00059

Preparation of Neutral trans - cis [Ru(O₂CR)₂P₂(NN)], Cationic [Ru(O₂CR)P₂(NN)](O₂CR) and Pincer [Ru(O₂CR)(CNN)P₂] (P = PPh₃, P₂ = diphosphine) Carboxylate Complexes and their Application in the Catalytic Carbonyl Compounds Reduction

Organometallics. 2021 Apr 26;40(8):1086-1103. doi: 10.1021/acs.organomet.1c00059. Epub 2021 Apr 14.

Authors

Affiliations

¹ Dipartimento DI4A, Università di Udine, Via del Cotonificio 108, I-33100 Udine, Italy.
² Dipartimento di Chimica, Università di Torino, Via Pietro Giuria, 7, I-10125 Torino, Italy.
³ Johnson Matthey, 28 Cambridge Science Park, Milton Road, Cambridge CB4 0FP, United Kingdom.
⁴ Department of Chemistry & Catalysis Research Center, TUM, Lichtenbergstraße 4, 85747 Garching b. München, Germany.

Abstract

The diacetate complexes trans-[Ru(κ¹-OAc)₂(PPh₃)₂(NN)] (NN = ethylenediamine (en) (1), 2-(aminomethyl)pyridine (ampy) (2), 2-(aminomethyl)pyrimidine (ampyrim) (3)) have been isolated in 76-88% yield by reaction of [Ru(κ²-OAc)₂(PPh₃)₂] with the corresponding nitrogen ligands. The ampy-type derivatives 2 and 3 undergo isomerization to the thermodynamically most stable cationic complexes [Ru(κ¹-OAc)(PPh₃)₂(NN)]OAc (2a and 3a) and cis-[Ru(κ¹-OAc)₂(PPh₃)₂(NN)] (2b and 3b) in methanol at RT. The trans-[Ru(κ¹-OAc)₂(P₂)₂] (P₂ = dppm (4), dppe (5)) compounds have been synthesized from [Ru(κ²-OAc)₂(PPh₃)₂] by reaction with the suitable diphosphine in toluene at 95 °C. The complex cis-[Ru(κ¹-OAc)₂(dppm)(ampy)](6) has been obtained from [Ru(κ²-OAc)₂(PPh₃)₂] and dppm in toluene at reflux and reaction with ampy. The derivatives trans-[Ru(κ¹-OAc)₂P₂(NN)] (7-16; NN = en, ampy, ampyrim, 8-aminoquinoline; P₂ = dppp, dppb, dppf, (R)-BINAP) can be easily synthesized from [Ru(κ²-OAc)₂(PPh₃)₂] with a diphosphine and treatment with the NN ligands at RT. Alternatively these compounds have been prepared from trans-[Ru(OAc)₂(PPh₃)₂(NN)] by reaction with the diphosphine in MEK at 50 °C. The use of (R)-BINAP affords trans-[Ru(κ¹-OAc)₂((R)-BINAP)(NN)] (NN = ampy (11), ampyrim (15)) isolated as single stereoisomers. Treatment of the ampy-type complexes 8-15 with methanol at RT leads to isomerization to the cationic derivatives [Ru(κ²-OAc)P₂(NN)]OAc (8a-15a; NN = ampy, ampyrim; P₂ = dppp, dppb, dppf, (R)-BINAP). Similarly to 2, the dipivalate trans-[Ru(κ¹-OPiv)₂(PPh₃)₂(ampy)] (18) is prepared from [Ru(κ²-OPiv)₂(PPh₃)₂] (17) and ampy in CHCl₃. The pincer acetate [Ru(κ¹-OAc)(CNN^OMe)(PPh₃)₂] (19) has been synthesized from [Ru(κ²-OAc)₂(PPh₃)₂] and HCNN^OMe ligand in 2-propanol with NEt₃ at reflux. In addition, the dppb pincer complexes [Ru(κ¹-OAc)(CNN)(dppb)] (CNN = AMTP (20), AMBQ^Ph (21)) have been obtained from [Ru(κ²-OAc)₂(PPh₃)₂], dppb, and HAMTP or HAMBQ^Ph with NEt₃, respectively. The acetate NN and pincer complexes are active in transfer hydrogenation with 2-propanol and hydrogenation with H₂ of carbonyl compounds at S/C values of up to 10000 and with TOF values of up to 160000 h^-1.